1 of 998 DOCUMENTS
US Fed News
January 25, 2012 Wednesday 2:06 PM EST
GRANT WILL FUND STUDY OF COGNITION AND SCHIZOPHRENIA
LENGTH: 927 words
SACRAMENTO, Calif., Jan. 25 -- The University of California issued the following
press release:
Michael Minzenberg, a UC Davis psychiatry researcher, has been awarded a
prestigious three-year, $200,000 seed grant from the Dana Foundation to study
the brains of patients being treated for schizophrenia to determine how
additional treatment to improve cognition interacts with antipsychotic
medication.
"Cognition is very important in schizophrenia because it is a strong predictor
of outcome. It determines whether a person can be a contributing member of a
community, stay out of the hospital and live independently," said Minzenberg,
associate professor in the Department of Psychiatry and Behavioral Sciences and
a faculty member of the UC Davis Imaging Research Center.
Schizophrenia is a chronic mental disorder characterized by decline in thought
processes and loss of emotional responsiveness. It affects 3.2 million
Americans, the majority of whom are not receiving treatment. It can lead to
auditory hallucinations, paranoia and delusions.
Despite the importance of cognition in the rehabilitation of those with
schizophrenia, there are no U.S. Food and Drug Administration (FDA)-approved
drugs for the improvement of cognition in this patient population.
"Dr. Minzenberg is at the forefront of trying to develop therapies for impaired
cognition in schizophrenia, using powerful new non-invasive brain imaging to
measure the effects of drugs and other treatments on functional networks in the
brain," said Cameron Carter, director of the Center for Neuroscience and the
Imaging Research Center at UC Davis.
"His work is suggesting that some of the other medications that patients are
taking may interfere with the procognitive effects of some of the newer more
promising therapies. If this proves to be true then it will be important to
'fine tune' patients' medications to optimize cognitive outcomes in people with
schizophrenia and other brain disorders."
Modafinil is a drug approved by the FDA for the treatment of narcolepsy. It is
also known by the brand name Provigil. Narcolepsy is a chronic neurological
disease characterized by sudden urges to sleep, episodes of loss of voluntary
muscle tone, vivid dreams while falling asleep or upon awakening, and brief
episodes of total paralysis while waking up from sleep. Both genetic and
environmental factors appear to contribute to narcolepsy. Although no cure
exists, medications can often help restore a patient's quality of life.
Like other stimulants, Modafinil's side effects are relatively mild. It is used
off-label to combat the effects of sedatives. Currently, it is not prescribed on
a long-term basis to schizophrenia patients.
However, Minzenberg and his colleagues conducted a small, unpublished pilot
study that showed Modafinil can improve cognition in patients being treated for
schizophrenia.
"What we understand about how Modafinil works in the brain leads us to believe
that it might be good for improving cognition deficits of our patients,"
Minzenberg said.
Because the cause of schizophrenia is unknown, treatment focuses on eliminating
symptoms. Antipsychotic drugs are effective at reducing its most serious
symptoms: delusions and hallucinations. Any treatment to improve cognition
cannot interact with these drugs in a negative way.
"The use of antipsychotic medications is the standard of care in patients with
schizophrenia. So, before we can move forward with a large clinical trial
involving Modafinil's impact on cognition, we need to know how it interacts with
these drugs."
Cognition refers to a range of high-level brain functions, including the
abilities to learn, remember information, organize, plan, problem-solve and
understand and use language. It is thought to be controlled by an area of the
brain called the locus coeruleus, which controls the body's physiological
responses to stress and panic, commonly referred to as the "fight or flight"
response.
"This area of the brain also serves to coordinate activity in the entire brain
as it performs almost any type of task or behavior," Minzenberg said.
Minzenberg and his colleagues will conduct the study at the UC Davis Early
Diagnosis and Preventive Treatment of Psychosis (EDAPT) Clinic. Researchers will
enroll 60 patients newly diagnosed with schizophrenia. These patients will have
a specialized brain scan performed, called functional magnetic resonance imaging
or fMRI, and will be randomly assigned to an FDA-approved treatment for
schizophrenia.
After eight weeks of treatment, another fMRI scan will be conducted. The
patients, who also will have been assigned to either a control or study group,
will undergo a third scan while performing a cognitive task.
Functional magnetic resonance imaging allows researchers to see changes in blood
flow related to neural activity. Minzenberg and his colleagues will examine
whether patients being treated with Modafinil perform better or worse, as
measured by the changes in activity in locus coeruleus, depending on which
antipsychotic medication they receive.
"We are hoping to find evidence that using Modafinil we can improve brain
function in stable schizophrenia patients," Minzenberg said.
The New York-based Dana Foundation is a private philanthropic organization that
supports clinical research in neuroscience and neuroimmunology and their
interrelationship in human health and disease. For further information, visit
www.dana.org. For any query with respect to this article or any other content
requirement, please contact Editor at htsyndication@hindustantimes.com
LOAD-DATE: January 26, 2012
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2012 HT Media Ltd.
All Rights Reserved
2 of 998 DOCUMENTS
CNS Drug News
November 29, 2011
Modiodal approved for additional indication in Japan
SECTION: NEWS
LENGTH: 154 words
Alfresa Pharma (Alfresa Holdings) has received approval in Japan of a partial
change in the indications of Modiodal (modafinil) Tablets 100mg, a sleep
disorder treatment that has been jointly developed in the country with
Mitsubishi Tanabe Pharma.
Since March 2007, Modiodal has been jointly marketed by the companies as a
treatment for excessive daytime sleepiness associated with narcolepsy. The new
indication, approved for the first time in Japan, is "excessive diurnal
sleepiness accompanied with obstructive sleep apnoea syndrome under treatment
for airway obstruction by continuous positive airway pressure therapy and the
like".
Modafinil is a wakefulness-enhancing agent to which Alfresa acquired the right
to develop, manufacture and market in Japan from Cephalon in June 1998. The drug
is currently approved in more than 30 countries, and in seven, including the US,
it is marketed with approval for the new indication.
LOAD-DATE: November 29, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: CNS Drug News
Copyright 2011 Espicom Business Intelligence
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3 of 998 DOCUMENTS
CNS Drug News
November 29, 2011
Modiodal approved for additional indication in Japan
SECTION: NEWS
LENGTH: 154 words
Alfresa Pharma (Alfresa Holdings) has received approval in Japan of a partial
change in the indications of Modiodal (modafinil) Tablets 100mg, a sleep
disorder treatment that has been jointly developed in the country with
Mitsubishi Tanabe Pharma.
Since March 2007, Modiodal has been jointly marketed by the companies as a
treatment for excessive daytime sleepiness associated with narcolepsy. The new
indication, approved for the first time in Japan, is "excessive diurnal
sleepiness accompanied with obstructive sleep apnoea syndrome under treatment
for airway obstruction by continuous positive airway pressure therapy and the
like".
Modafinil is a wakefulness-enhancing agent to which Alfresa acquired the right
to develop, manufacture and market in Japan from Cephalon in June 1998. The drug
is currently approved in more than 30 countries, and in seven, including the US,
it is marketed with approval for the new indication.
LOAD-DATE: January 6, 2012
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: CNS Drug News
Copyright 2011 Espicom Business Intelligence
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The Pharmaceutical Journal
November 29, 2011 Tuesday
Modafinil indication and dosage error in BNF 62
LENGTH: 80 words
HIGHLIGHT: An error is included under the indications and dosage information for
modafinil that are printed in the British National Formulary 62...
An error is included under the indications and dosage information for modafinil
that are printed in the British National Formulary 62 (section 4.4, pp250-251).
Modafinil is listed as indicated for the treatment of daytime sleepiness
associated with narcolepsy, obstructive sleep apnoea syndrome and chronic shift
work sleep disorder. The entry should list daytime sleepiness associated with
narcolepsy only.
Corrected indication and dosage information is available on the BNF website.
LOAD-DATE: November 29, 2011 Tuesday
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Journal
Copyright 2011 PJ Online
All Rights Reserved
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IPR
November 25, 2011 Friday 3:11 PM EST
India Tender Notice: South Central Railway Seeks "Modafinil 100 Mg Tablets"
LENGTH: 87 words
DATELINE: SECUNDERABAD, Andhra Pradesh
SECUNDERABAD, Andhra Pradesh, Dec. 5 -- South Central Railway has a requirement
for "Modafinil 100 Mg Tablets."
Tender Bidding Type: Domestic Competitive Bidding
According to the description: "Tenders are invited for Supply of Modafinil 100
Mg Tab - 7500 Nos"
The tender ref. no. is L-883/2011-2012.
Project Location: India
The expression of interest should be received by Dec. 5 till 1:00 p.m. For any
query with respect to this article or any other content requirement, please
contact Editor at htsyndication@hindustantimes.com
LOAD-DATE: November 25, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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All Rights Reserved
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Targeted News Service
November 7, 2011 Monday 10:51 PM EST
Teva Pharmaceutical Industries Assigned Patent
BYLINE: Targeted News Service
LENGTH: 238 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Nov. 7 -- Teva Pharmaceutical Industries, Petah Tiqva, Israel,
has been assigned a patent (8,048,222) developed by Arina Ceausu, Rishon Lezion,
Israel, Anita Lieberman, Ramat Aviv, Israel, and Judith Aronhime, Rechovot,
Israel, for a highly pure modafinil.
The abstract of the patent published by the U.S. Patent and Trademark Office
states: "The present invention provides an improved process for preparing
modafinil, whereby it may be isolated in high purity by a single
crystallization. The process produces modafinil free of sulphone products of
over-oxidation and other byproducts. The invention further provides new
crystalline Forms II-VI of modafinil and processes for preparing them. Each of
the new forms is differentiated by a unique powder X-ray diffraction pattern.
The invention further provides pharmaceutical compositions containing novel
modafinil Forms II-IV and VI."
The patent application was filed on Sept. 23, 2004 (10/947,228). The full-text
of the patent can be found at
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO2&Sect2=HITOFF&p=1&u=%2Fnetah
tml%2FPTO%2Fsearch-bool.html&r=1&f=G&l=50&co1=AND&d=PTXT&s1=8,048,222&OS=8,048,2
22&RS=8,048,222
Written by Satyaban Rath; edited by Hemanta Panigrahi.
For more information about Targeted News Service federal patent awards please
contact: Myron Struck, Editor, Direct: 703/866-4708, Cell: 703/304-1897,
Myron@targetednews.com
SR1107HP1107-666772
LOAD-DATE: November 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Targeted News Service LLC
All Rights Reserved
7 of 998 DOCUMENTS
Health Daily Digest
November 4, 2011 Friday
Modafinil may not affect Operating Skills of Weary Surgeons
LENGTH: 164 words
DATELINE: U.S.
U.S., Nov. 4 -- Weary surgeons may benefit with the intake of sleep-fighting
medication modafinil by having an enhanced brain power but it may not bring any
changes in their operating skills, according to a new study.
The research was carried out on 39 young surgeons. They were made to be awake
throughout the night. As many as 50 percent of doctors were given a modafinil
pill and the remaining were provided with a dummy pill. The doctors went through
some psychological tests and did a virtual surgery on a simulator as early as 6
a.m in the morning.
It was observed that having a sleep-fighting medication modafinil improved the
brain power of weary surgeons but it was of no use as far as enhancing their
operating skills in a simulator is concerned.
Written by Manishika Miglani Published by HT Syndication with permission from
Health Daily Digest. For any query with respect to this article or any other
content requirement, please contact Editor at htsyndication@hindustantimes.com
LOAD-DATE: November 15, 2011
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PUBLICATION-TYPE: Newspaper
Copyright 2011 HT Media Ltd.
All Rights Reserved
8 of 998 DOCUMENTS
Indian Patents News
October 22, 2011 Saturday 6:30 AM EST
Cephalon Inc Receives Patent for a Pharmaceutical Composition
LENGTH: 262 words
New Delhi, Oct. 22 -- Cephalon Inc received patent for a pharmaceutical
composition on April 11, 2008. The patent number issued by the Indian Patent
Office is 218719.
Cephalon Inc had filed patent application number IN/PCT/2002/128/KOL for a
pharmaceutical composition on Jan. 25, 2002. The inventors of the patent are
Miller Matthew S and Scammell Thomas E.
The International classification number is A61K31/165.
The PCT International application number of the patent is PCT/US00/22338 and the
application was filed on Aug. 16, 2000.
According to the Controller General of Patents, Designs & Trade Marks, "
Modafinil is effective in improving symptoms of attention deficit hyperactivity
disorder and symptoms of multiple sclerosis fatigue. The administration of
modafinil is also shown to activate the tuberomamillary neurons of the posterior
hypothalamus, and thus exhibits activity in an area of the brain associated with
normal wakefulness functions. A method of identifying a compound that
selectively modulates activity of the tuberomamillary nucleus of the posterior
hypothalamus is also disclosed."
About the Company
Cephalon, Inc. (NASDAQ: CEPH) is a U.S. biopharmaceutical company co-founded in
1987 by Dr. Frank Baldino, Jr., a pharmacologist and former scientist with the
DuPont Company, who served as the company's chairman and chief executive officer
until his death in December 2010.[2] The company's name comes from the adjective
"cephalic" meaning "related to the head or brain," and it was established
primarily to pursue treatments for neurodegenerative diseases.
LOAD-DATE: October 22, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
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9 of 998 DOCUMENTS
World Generic Market
October 21, 2011
Teva completes Cephalon acquisition
SECTION: NEWS
LENGTH: 967 words
Teva Pharmaceutical Industries announced on 14th October 2011 that it had
completed its acquisition of Cephalon. The firm had initially announced it had
acquired all of Cephalon's outstanding shares for US $81.50 per share in cash in
May 2011; the deal amounted to a total enterprise value of some US $6.8 billion.
With the acquisition of Cephalon now completed, Teva commented that the combined
company would have a significant presence in over 60 countries and generated
around US $20 billion in revenues on a pro-forma basis for the year ended June
2011.
The completion of the deal came after two hurdles were cleared. On 7th October
2011, Teva reported that the US Federal Trade Commission had accepted a proposed
consent order in connection with the transaction and granted early termination
of the Hart-Scott-Rodino waiting period. The FTC had complained that the
acquisition as originally proposed would have violated US antitrust law by
reducing competition in three markets: transmucosal fentanyl citrate lozenges
used to treat cancer pain; extended-release cyclobenzaprine hydrochloride used
as a muscle relaxant; and modafinil tablets used to improve wakefulness.
The FTC commented that transmucosal fentanyl citrate lozenges are versions of a
cancer pain drug developed by Cephalon and marketed under the brand name Actiq.
Three generic versions of the drug, manufactured and marketed by Teva, Cephalon
/ Watson Pharmaceuticals and Covidien, currently exist in the US. Teva's
acquisition of Cephalon would have reduced this to two, and would have given
Teva a more than 80% share of the sales of generic Actiq. Extended-release
cyclobenzaprine hydrochloride is the generic form of Amrix. The FTC noted that
Cephalon had acquired the rights to the branded version, which was approved by
the FDA in 2007. Currently, no generic versions of the drug are marketed in the
US, but the FTC argued that Teva and Cephalon were two of only a limited number
of suppliers that could enter the market quickly with a generic version. As a
result, combining the two firms would reduce competition in the future.
Modafinil tablets are generic versions of the brand drug Provigil, marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. The FTC noted again that no companies currently market a generic
version of the product, which had sales worth US $1 billion in 2010. Teva,
Ranbaxy Pharmaceuticals, Mylan Pharmaceutical and Barr Laboratories (another
Teva company) have all taken steps to enter the market, and are all eligible to
seek the 180-days marketing exclusivity allowed under the Hatch-Waxman Act for
being the first to file an ANDA. However, the FTC noted that each company had
also signed an agreement with Cephalon to refrain from marketing a generic
version until April 2012. The FTC contended that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day period.
In order to replace the competition potentially lost through the acquisition,
the FTC proposed a settlement order which would require Teva to sell all of its
rights and assets related to generic Actiq or transmucosal fentanyl citrate
lozenges, Actiq or generic extended-release cyclobenzaprine hydrochloride
capsules, to Par Pharmaceutical Companies. With regard to modafinil, the FTC's
proposed order required Teva to enter into a supply agreement to provide Par
with generic modafinil tablets in the US for one year. This would allow Par to
compete with a generic modafinil product during the 180-day exclusivity period.
In addition, Par may extend the agreement for another year.
Across the Atlantic
The second hurdle to the transaction had been in Europe. In April 2011, before
Teva had announced its acquisition agreement, the European Commission reported
that it had opened a formal antitrust investigation regarding an agreement
between Teva and Cephalon that was unconnected with the acquisition. The EC had
reported that in December 2005, the two firms had settled patent infringement
disputes in the US and UK concerning modafinil, with Teva undertaking as part of
the agreement not to sell its generic version in the European Economic Area
markets before October 2012. The EC was investigating whether this agreement
may have had the object or effect of hindering generic competition for the drug
in the EEA.
On 14th October 2011, the EC formally announced that it had cleared the proposed
acquisition of Cephalon under the EU Merger Regulation. However, the decision
was conditional upon the divestment of Cephalon's generic version of its
Provigil product. The Commission commented that it had examined the effects of
the proposed transaction on the market for modafinil drugs, having had concerns
that the acquisition, as originally proposed, would have significantly reduced
generic competition. The Commission determined that the divestment of
Cephalon's generic pipeline modafinil product, as was offered by the company,
would allow a competitor to emerge and compete effectively with the Teva /
Cephalon combined company. The investigation did not reveal any other
significant modification to the competitive situation and dynamics of other
relevant markets, as a number of significant and credible competitors would
continue to exercise a competitive constraint on the merged entity.
Consequently, the Commission was happy with the modified transaction proposal.
Teva noted that it was required to divest Cephalon's marketing authorisation of
generic modafinil in France and grant to the purchaser of the marketing
authorisation certain additional rights with respect to the entire EEA,
including a covenant not to sue effective as of October 2012.
LOAD-DATE: October 21, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: World Generic Markets
Copyright 2011 Espicom Business Intelligence
All Rights Reserved
10 of 998 DOCUMENTS
World Generic Market
October 21, 2011
Teva completes Cephalon acquisition
SECTION: NEWS
LENGTH: 967 words
Teva Pharmaceutical Industries announced on 14th October 2011 that it had
completed its acquisition of Cephalon. The firm had initially announced it had
acquired all of Cephalon's outstanding shares for US $81.50 per share in cash in
May 2011; the deal amounted to a total enterprise value of some US $6.8 billion.
With the acquisition of Cephalon now completed, Teva commented that the combined
company would have a significant presence in over 60 countries and generated
around US $20 billion in revenues on a pro-forma basis for the year ended June
2011.
The completion of the deal came after two hurdles were cleared. On 7th October
2011, Teva reported that the US Federal Trade Commission had accepted a proposed
consent order in connection with the transaction and granted early termination
of the Hart-Scott-Rodino waiting period. The FTC had complained that the
acquisition as originally proposed would have violated US antitrust law by
reducing competition in three markets: transmucosal fentanyl citrate lozenges
used to treat cancer pain; extended-release cyclobenzaprine hydrochloride used
as a muscle relaxant; and modafinil tablets used to improve wakefulness.
The FTC commented that transmucosal fentanyl citrate lozenges are versions of a
cancer pain drug developed by Cephalon and marketed under the brand name Actiq.
Three generic versions of the drug, manufactured and marketed by Teva, Cephalon
/ Watson Pharmaceuticals and Covidien, currently exist in the US. Teva's
acquisition of Cephalon would have reduced this to two, and would have given
Teva a more than 80% share of the sales of generic Actiq. Extended-release
cyclobenzaprine hydrochloride is the generic form of Amrix. The FTC noted that
Cephalon had acquired the rights to the branded version, which was approved by
the FDA in 2007. Currently, no generic versions of the drug are marketed in the
US, but the FTC argued that Teva and Cephalon were two of only a limited number
of suppliers that could enter the market quickly with a generic version. As a
result, combining the two firms would reduce competition in the future.
Modafinil tablets are generic versions of the brand drug Provigil, marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. The FTC noted again that no companies currently market a generic
version of the product, which had sales worth US $1 billion in 2010. Teva,
Ranbaxy Pharmaceuticals, Mylan Pharmaceutical and Barr Laboratories (another
Teva company) have all taken steps to enter the market, and are all eligible to
seek the 180-days marketing exclusivity allowed under the Hatch-Waxman Act for
being the first to file an ANDA. However, the FTC noted that each company had
also signed an agreement with Cephalon to refrain from marketing a generic
version until April 2012. The FTC contended that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day period.
In order to replace the competition potentially lost through the acquisition,
the FTC proposed a settlement order which would require Teva to sell all of its
rights and assets related to generic Actiq or transmucosal fentanyl citrate
lozenges, Actiq or generic extended-release cyclobenzaprine hydrochloride
capsules, to Par Pharmaceutical Companies. With regard to modafinil, the FTC's
proposed order required Teva to enter into a supply agreement to provide Par
with generic modafinil tablets in the US for one year. This would allow Par to
compete with a generic modafinil product during the 180-day exclusivity period.
In addition, Par may extend the agreement for another year.
Across the Atlantic
The second hurdle to the transaction had been in Europe. In April 2011, before
Teva had announced its acquisition agreement, the European Commission reported
that it had opened a formal antitrust investigation regarding an agreement
between Teva and Cephalon that was unconnected with the acquisition. The EC had
reported that in December 2005, the two firms had settled patent infringement
disputes in the US and UK concerning modafinil, with Teva undertaking as part of
the agreement not to sell its generic version in the European Economic Area
markets before October 2012. The EC was investigating whether this agreement
may have had the object or effect of hindering generic competition for the drug
in the EEA.
On 14th October 2011, the EC formally announced that it had cleared the proposed
acquisition of Cephalon under the EU Merger Regulation. However, the decision
was conditional upon the divestment of Cephalon's generic version of its
Provigil product. The Commission commented that it had examined the effects of
the proposed transaction on the market for modafinil drugs, having had concerns
that the acquisition, as originally proposed, would have significantly reduced
generic competition. The Commission determined that the divestment of
Cephalon's generic pipeline modafinil product, as was offered by the company,
would allow a competitor to emerge and compete effectively with the Teva /
Cephalon combined company. The investigation did not reveal any other
significant modification to the competitive situation and dynamics of other
relevant markets, as a number of significant and credible competitors would
continue to exercise a competitive constraint on the merged entity.
Consequently, the Commission was happy with the modified transaction proposal.
Teva noted that it was required to divest Cephalon's marketing authorisation of
generic modafinil in France and grant to the purchaser of the marketing
authorisation certain additional rights with respect to the entire EEA,
including a covenant not to sue effective as of October 2012.
LOAD-DATE: January 6, 2012
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: World Generic Markets
Copyright 2011 Espicom Business Intelligence
All Rights Reserved
11 of 998 DOCUMENTS
Global Insight
October 19, 2011
Teva Sells Three Generic Products Rights to Par Pharma
BYLINE: Georgette Calnan
SECTION: In Brief
LENGTH: 242 words
US firm Par Pharmaceutical yesterday (18 October) announced the ownership of the
rights to three products from Teva (Israel) as a result of the terms attached by
the US Federal Trade Commission (FTC) to the latter's acquisition of Cephalon
(US). Under the terms of the agreement, Par will now own the Abbreviated New
Drug Applications (ANDAs) of the generic versions of Actiq (fentanyl citrate
lozenges), Amriz (cyclobenzaprine extended-release--ER--capsules), as well as
the US rights to market the generic version of Provigil (modafinil). According
to Par's press release, citing IMS data, Actiq, Provigil and Amrix achieved
annual sales in the US of USD173 million, USD1.1 billion and USD125 million
respectively. Par will begin immediate shipment of all strengths of fentanyl
citrate lozenges which were previously available from Teva. Cyclobenzaprine ER
capsules and modafinil tablets are not yet available.
Significance:The deal was part of the US Federal Trade Commission (FTC)'s
conditional nod of Teva's acquisition of Cephalon. The sale of the ANDAs allowed
Teva to complete its acquisition of Cephalon by its targeted deadline of 14
October. Par's acquisition of the three products preserves competition in all
relevant markets. This will boost the US firm's generic drug portfolio which in
turn could result in increased revenues. The acquisition of Amrix and Provigil
ANDAs will allow Par to enter the generic market for both products next year.
LOAD-DATE: October 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2011 World Markets Research Limited
All Rights Reserved
12 of 998 DOCUMENTS
India Investment News
October 18, 2011 Tuesday 6:30 AM EST
Par Pharmaceutical Acquires Three Generic Products from Teva Pharmaceuticals
LENGTH: 173 words
New Delhi, Oct. 18 -- Par Pharmaceutical Companies Inc. issued the following
news release:
Par Pharmaceutical Companies, Inc. (NYSE: PRX) announced today that it acquired
rights to three products from Teva Pharmaceuticals in connection with Teva's
acquisition of Cephalon. Under terms of the agreement, Par will own the ANDAs of
fentanyl citrate lozenges, a generic version of Actiq, and cyclobenzaprine ER
capsules, the generic version of Amrix, as well as the U.S. rights to market
modafinil tablets, the generic version of Provigil.
According to IMS Health data, annual sales in the U.S. for Actiq and the
equivalent generic products are $173 million. Annual sales in the U.S. for
Provigil and Amrix are approximately $1.1 billion and $125 million,
respectively.
Par is currently shipping to the trade all strengths of fentanyl citrate
lozenges that were previously available from Teva. Cyclobenzaprine ER capsules
and modafinil tablets were not previously marketed by Teva and are not yet
available.
Source: Par Pharmaceutical Companies Inc.
LOAD-DATE: January 3, 2012
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
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All Rights Reserved
13 of 998 DOCUMENTS
Key Pharma News
October 18, 2011 Tuesday
Par acquires three generic products from Teva
SECTION: NEWS
LENGTH: 177 words
Par Pharmaceutical Companies has acquired rights to three products from Teva
Pharmaceutical Industries in connection with the latter's acquisition of
Cephalon.
Under terms of the agreement, Par will own the ANDAs for fentanyl citrate
lozenges, a generic version of Actiq, which is indicated for the management of
breakthrough cancer pain in patients aged >=16 years with malignancies who are
already receiving and tolerant to around-the-clock opioid therapy for their
underlying persistent cancer pain, and cyclobenzaprine extended-release (ER)
capsules, a generic version of Amrix, indicated as an adjunct to rest and
physical therapy for the relief of muscle spasm associated with acute, painful
musculoskeletal conditions, as well as the US rights to market modafinil
tablets, a generic version of Provigil, a wakefulness-promoting agent.
Par is currently shipping all strengths of fentanyl citrate lozenges that were
previously available from Teva. Cyclobenzaprine ER capsules and modafinil
tablets were not previously marketed by Teva, and are not yet available.
LOAD-DATE: October 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: Pharma Company Insight
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14 of 998 DOCUMENTS
Key Pharma News
October 18, 2011 Tuesday
Par acquires three generic products from Teva
SECTION: NEWS
LENGTH: 177 words
Par Pharmaceutical Companies has acquired rights to three products from Teva
Pharmaceutical Industries in connection with the latter's acquisition of
Cephalon.
Under terms of the agreement, Par will own the ANDAs for fentanyl citrate
lozenges, a generic version of Actiq, which is indicated for the management of
breakthrough cancer pain in patients aged >=16 years with malignancies who are
already receiving and tolerant to around-the-clock opioid therapy for their
underlying persistent cancer pain, and cyclobenzaprine extended-release (ER)
capsules, a generic version of Amrix, indicated as an adjunct to rest and
physical therapy for the relief of muscle spasm associated with acute, painful
musculoskeletal conditions, as well as the US rights to market modafinil
tablets, a generic version of Provigil, a wakefulness-promoting agent.
Par is currently shipping all strengths of fentanyl citrate lozenges that were
previously available from Teva. Cyclobenzaprine ER capsules and modafinil
tablets were not previously marketed by Teva, and are not yet available.
LOAD-DATE: January 6, 2012
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: Pharma Company Insight
Copyright 2011 Espicom Business Intelligence
All Rights Reserved
15 of 998 DOCUMENTS
PR Newswire
October 18, 2011 Tuesday 9:00 AM EST
Par Pharmaceutical Acquires Three Generic Products From Teva Pharmaceuticals;
Par Begins Shipping Fentanyl Citrate Lozenges to the Trade Immediately
LENGTH: 453 words
DATELINE: WOODCLIFF LAKE, N.J., Oct. 18, 2011
Par Pharmaceutical Companies, Inc. (NYSE: PRX) announced today that it acquired
rights to three products from Teva Pharmaceuticals in connection with Teva's
acquisition of Cephalon. Under terms of the agreement, Par will own the ANDAs of
fentanyl citrate lozenges, a generic version of Actiq®, and cyclobenzaprine ER
capsules, the generic version of Amrix®, as well as the U.S. rights to market
modafinil tablets, the generic version of Provigil®.
According to IMS Health data, annual sales in the U.S. for Actiq® and the
equivalent generic products are $173 million. Annual sales in the U.S. for
Provigil® and Amrix® are approximately $1.1 billion and $125 million,
respectively.
Par is currently shipping to the trade all strengths of fentanyl citrate
lozenges that were previously available from Teva. Cyclobenzaprine ER capsules
and modafinil tablets were not previously marketed by Teva and are not yet
available.
About Par Pharmaceutical Companies, Inc.
Par Pharmaceutical Companies, Inc. is a US-based specialty pharmaceutical
company. Through its wholly-owned subsidiary's two operating divisions, Par
Pharmaceutical and Strativa Pharmaceuticals, it develops, manufactures and
markets high barrier-to-entry generic drugs and niche, innovative proprietary
pharmaceuticals. For press release and other company information, visit
www.parpharm.com.
Safe Harbor Statement
Certain statements in this news release constitute "forward-looking statements"
within the meaning of the Private Securities Litigation Reform Act of 1995. To
the extent any statements made in this news release contain information that is
not historical, these statements are essentially forward-looking and, as such,
are subject to known and unknown risks, uncertainties and contingencies, many of
which are beyond the control of the Company, which could cause actual results
and outcomes to differ materially from those expressed herein. Risk factors that
might affect such forward-looking statements include those set forth in Item 1A
of the Company's most recent Annual Report on Form 10-K, in other of the
Company's filings with the SEC from time to time, including Quarterly Reports on
Form 10-Q and Current Reports on Form 8-K, and on general industry and economic
conditions. Any forward-looking statements included in this news release are
made as of the date hereof only, based on information available to the Company
as of the date hereof, and, subject to any applicable law to the contrary, the
Company assumes no obligation to update any forward-looking statements.
SOURCE Par Pharmaceutical Companies, Inc.
CONTACT:Allison Wey, Vice President, Investor Relations and Corporate Affairs,
Par Pharmaceutical Companies, Inc., +1-201-802-4000
URL: http://www.prnewswire.com
LOAD-DATE: October 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 PR Newswire Association LLC
All Rights Reserved
16 of 998 DOCUMENTS
Europolitics (daily in English)
October 17, 2011 Monday
MERGERS : ISRAEL'S TEVA CLEARED TO BUY CEPHALON, SUBJECT TO CONDITIONS
BYLINE: Sophie Mosca
SECTION: No. 4286
LENGTH: 246 words
The world's number one generic pharmaceutical company, Teva, obtained the
European Commission's green light, on 13 October, to buy its American
competitor, Cephalon, which is primarily an originator company. The EU executive
nevertheless makes the EUR4.5 billion merger contingent on Cephalon's sale of
its generic version of Provigil, a medicine used to treat excessive daytime
sleepiness.
The Commission determined that the two groups have a similar generic drug based
on the same active ingredient as Provigil, namely modafinil, and that
competition on the generic drug markets where modafinil is sold could be
hampered.
The commitment on the "divestment of Cephalon's generic pipeline modafinil
product, as offered by the company, will allow a competitor to emerge and
compete effectively with the merged entity," explains the EU executive. The
investigation did not reveal any other significant modifications to the
competitive situation and dynamics of other relevant markets, as a number of
credible and significant competitors will continue to exercise a competitive
constraint on the merged entity. The Commission concluded that the proposed
transaction, as modified by the commitment, would not significantly impede
effective competition in the European Economic Area.
The US trade regulator, the Federal Trade Commission, made the merger
conditional on Teva's divestment of its Provigil generic, its Actiq generic used
to treat cancer and Amrix, a muscle relaxant.
LOAD-DATE: October 14, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: EURE
Copyright 2011 Europolitique
All Rights Reserved
17 of 998 DOCUMENTS
The Sunday Times (London)
October 16, 2011 Sunday
Edition 1;
National Edition
Doctors given drug perform better surgery;
Tests of the brain-stimulant modafinil on exhausted surgeons produced remarkable
results, says Jonathan Leake
BYLINE: Jonathan Leake
SECTION: NEWS; Pg. 15
LENGTH: 673 words
IS your doctor on drugs? If not, perhaps they should be. A new study suggests
that surgeons given "smart drugs" perform better, safer operations.
Researchers gave sleepdeprived surgeons a brain stimulant called modafinil,
known to boost memory and brain power, and then tested how good they were at
thinking clearly, solving problems and carrying out simulated operations.
The results were so convincing that scientists believe the medical profession
could even be weaned off its current drug of choice: caffeine.
The study, led by Lord Darzi, professor of surgery at Imperial College London
and a junior health minister in the previous Labour government, suggests that
doctors whose brains have been sharpened by the drug will perform better under
pressure.
What is more, he says, their extra brain power means they would think faster and
react more decisively if something went wrong.
"We found that when surgeons had taken modafinil they saw sharp improvements in
their ability to solve problems and think flexibly. In fact, their performance
was very good," said Barbara Sahakian, professor of psychiatry at Cambridge
University.
The sight of bleary-eyed doctors scrubbing up for surgery after sleepless nights
in hospital has caused widespread concern over the risk to patients. But the
usual remedy of strong coffee, taken orally in large quantities, can cause hand
tremors, the last thing a surgeon needs during a tricky procedure.
Sahakian suggests that modafinil could be a superior substitute for caffeine.
Sahakian and Charlotte Housden, her research colleague, worked with Darzi and
his surgical team in conducting the tests.
Housden said: "Sleep deprivation is like being legally drunk - it causes
problems with learning, memory and increased impulsiveness. This is particularly
important for people with critical jobs like surgeons, pilots and drivers.
"Imaging studies show that the pre-frontal cortex, which is where you do your
thinking, undergoes changes in people who lack sleep."
In the study, Housden and her colleagues tested 39 tired doctors who had worked
all day and then stayed up all night. They were divided into two groups: one was
given 200mg of modafinil while the other took a placebo.
Then, from 6am to 8am, the doctors were subjected to a battery of tests to
measure their cognitive skills, including carrying out virtual operations using
a surgical training system.
Compared with those who received modafinil, the doctors given a placebo achieved
much lower scores on memory tasks, were more impatient, less able to solve
problems and to think flexibly.
Housden said: "Doctors who are deprived of sleep lose their ability to solve
problems and think flexibly. It means that if they encounter a surgical problem
they will find it harder to solve.
"However, when they took modafinil they regained their ability to solve problems
and think flexibly."
Modafinil is currently available only on prescription but it has been approved
in America for shift workers suffering from sleeping problems while at work. It
is, however, widely available from online pharmacies for about 50p a tablet. One
key concern is that modafinil has not been subjected to long-term safety tests.
Sahakian suggests, however, that, subject to safety approval, modafinil could
even be offered over the counter.
In other jobs, the use of modafinil has already become widespread - if hidden.
The military in Britain and America use the drug to keep soldiers and pilots
awake on long missions and in recent years it has become popular with students
and, increasingly, with business executives and other groups.
Darzi says in his paper, published in the Annals of Surgery: "The continuing
discourse over work hours, service provisions, graduate education, fatigue and
patient safety strongly suggests that novel solutions might ultimately be
required."
If modafinil can make even the most exhausted of doctors bright-eyed and
cheerful, then that is a problem solved.
Of course, they could just cut the working hours instead.
Additional reporting: Jan Piotrowski
LOAD-DATE: October 16, 2011
LANGUAGE: ENGLISH
GRAPHIC: Smart drugs might have benefited the medics in Carry on Doctor
ALLSTAR
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: STS
Copyright 2011 Times Newspapers Limited
All Rights Reserved
18 of 998 DOCUMENTS
Tendersinfo News
October 15, 2011 Saturday 6:30 AM EST
BELGIUM : Mergers: Commission approves the acquisition of Cephalon by Teva,
subject to conditions
LENGTH: 338 words
The European Commission has cleared under the EU Merger Regulation the proposed
acquisition of US-based pharmaceutical company Cephalon by the generic
pharmaceutical company Teva of Israel. The decision is conditional upon the
divestment of Cephalon's generic version of its "Provigil" drug. Provigil is
indicated for the treatment of excessive daytime sleepiness associated with
narcolepsy. Teva has also developed a generic version of the drug. In light of
the commitments, the Commission concluded that the transaction does not raise
competition concerns.
The Commission examined the effects of the proposed transaction on the market
for drugs based on Modafinil, the main active pharmaceutical ingredient of
Provigil and the generic version developed by Teva as well as the one Cephalon
has in the pipeline. The Commission was concerned that the proposed transaction,
as initially notified, would have significantly reduced generic competition in
the markets where Modafinil is sold.
The Commission's investigation showed that the divestment of Cephalon's generic
pipeline Modafinil product, as offered by the company, will allow a competitor
to emerge and compete effectively with the merged entity.
The investigation did not reveal any other significant modification to the
competitive situation and dynamics of other relevant markets, as a number of
credible and significant competitors will d continue to exercise a competitive
constraint on the merged entity.
The Commission therefore concluded that the proposed transaction, as modified by
the commitment, would not significantly impede effective competition in the
European Economic Area (EEA)1 or a substantial part of it.
Teva is the world s largest generic pharmaceutical company. Cephalon is a
primarily originator company, but also supplies generic pharmaceuticals in the
EEA.
The transaction was notified to the Commission on 25 August 2011.
LOAD-DATE: October 15, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2011 Tendersinfo News, distributed by Contify.com
All Rights Reserved
19 of 998 DOCUMENTS
Globes (Tel Aviv, Israel)
Distributed by McClatchy-Tribune Business News
October 14, 2011 Friday
Teva receives European approval for Cephalon acquisition
BYLINE: Guy Katsovitch, Globes, Tel Aviv, Israel
SECTION: BUSINESS AND FINANCIAL NEWS
LENGTH: 272 words
Oct. 14--Teva Pharmaceutical Industries Ltd. (Nasdaq: TEVA; TASE: TEVA) and
Cephalon Inc. (Nasdaq: CEPH ) announced today that they received approval from
the European Commission to proceed with Teva's $7 billion acquisition of
innovative drugs company Cephalon.
A condition of the approval is that Teva must divest Cephalon's marketing
authorization of generic modafinil in France and grant to the purchaser of this
marketing authorization certain additional rights with respect to the entire
European Economic Area, including a covenant not to sue effective as of October
2012.
Teva received approval for the US authorities for the merger at the beginning of
the week. Under that approval, Teva is required to divest two ANDAs for fentanyl
citrate lozenges, a generic version of Actiq, and cyclobenzaprine ER capsules,
the generic version of Amrix. Teva will also grant non-exclusive U.S. rights to
an undisclosed company to market modafinil tablets, the generic version of
Provigil, which had annual brand sales in the US of approximately $1.1 billion.
With the European Commission approval, the parties have now obtained all
regulatory approvals required to close the transaction and, accordingly, have
scheduled a closing date of October 14, 2011.
Teva projects that the deal will be accretive on a non-GAAP basis as soon as it
is completed, and on a GAAP basis within four quarters. Teva also expects
synergies of $500 million in the third year after completion.
___ (c)2011 the Globes (Tel Aviv, Israel) Visit the Globes (Tel Aviv, Israel) at
www.globes.co.il/serveen/globes/nodeview.asp?fid=942 Distributed by MCT
Information Services
LOAD-DATE: October 15, 2011
LANGUAGE: ENGLISH
ACC-NO:
20111014-TL-Teva-receives-European-approval-for-Cephalon-acquisition-1014-201110
14
PUBLICATION-TYPE: Newspaper
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Copyright 2011 Globes (Tel Aviv, Israel)
20 of 998 DOCUMENTS
States News Service
October 14, 2011 Friday
MERGERS: COMMISSION APPROVES THE ACQUISITION OF CEPHALON BY TEVA, SUBJECT TO
CONDITIONS
BYLINE: States News Service
LENGTH: 459 words
DATELINE: BRUSSELS
The following information was released by the European Union:
The European Commission has cleared under the EU Merger Regulation the proposed
acquisition of US-based pharmaceutical company Cephalon by the generic
pharmaceutical company Teva of Israel. The decision is conditional upon the
divestment of Cephalon's generic version of its "Provigil" drug. Provigil is
indicated for the treatment of excessive daytime sleepiness associated with
narcolepsy. Teva has also developed a generic version of the drug. In light of
the commitments, the Commission concluded that the transaction does not raise
competition concerns.
The Commission examined the effects of the proposed transaction on the market
for drugs based on Modafinil, the main active pharmaceutical ingredient of
Provigil and the generic version developed by Teva as well as the one Cephalon
has in the pipeline. The Commission was concerned that the proposed transaction,
as initially notified, would have significantly reduced generic competition in
the markets where Modafinil is sold.
The Commission's investigation showed that the divestment of Cephalon's generic
pipeline Modafinil product, as offered by the company, will allow a competitor
to emerge and compete effectively with the merged entity.
The investigation did not reveal any other significant modification to the
competitive situation and dynamics of other relevant markets, as a number of
credible and significant competitors will d continue to exercise a competitive
constraint on the merged entity.
The Commission therefore concluded that the proposed transaction, as modified by
the commitment, would not significantly impede effective competition in the
European Economic Area (EEA)1 or a substantial part of it.
Teva is the world's largest generic pharmaceutical company. Cephalon is a
primarily originator company, but also supplies generic pharmaceuticals in the
EEA.
The transaction was notified to the Commission on 25 August 2011.
Merger control rules and procedures
The Commission, in 1989, was given the power to assess mergers and acquisitions
involving companies with a turnover above certain thresholds (see Article 1 of
the Merger Regulation). Its duty is to prevent concentrations that would
significantly impede effective competition in the EEA or any substantial part of
it.
The vast majority of mergers do not pose competition problems and are cleared
after a routine review. From the moment a transaction is notified, the
Commission generally has a total of 25 working days to decide whether to grant
approval (Phase I) or to start an in-depth investigation (Phase II).
A non-confidential version of today's decision will be available at:
http://ec.europa.eu/competition/elojade/isef/case_details.cfm?proc_code=2_M_6258
LOAD-DATE: October 14, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 States News Service
21 of 998 DOCUMENTS
States News Service
October 14, 2011 Friday
PRELIMINARY STUDY EXAMINES EFFECTS OF 'COGNITIVE ENHANCEMENT' DRUG ON
SLEEP-DEPRIVED DOCTORS
BYLINE: States News Service
LENGTH: 919 words
DATELINE: LONDON
The following information was released by Imperial College London:
Researchers have carried out a preliminary study looking at the effects of the
'cognitive enhancement' drug modafinil on the performance of doctors who had
been deprived of sleep for one night.
Modafinil, discovered in the 1970s, is currently prescribed in the UK for the
treatment of sleepiness associated with narcolepsy, sleep apnoea, and shift work
sleep disorder, a condition that affects people who frequently have to work at
night.
In the new study of 39 people, published today in the Annals of Surgery by
researchers from Imperial College London and the University of Cambridge,
modafinil improved performance in a series of mental tasks when compared with
placebo, but had no effect on the performance of a surgical motor skills task.
The doctors did not interact with any patients during the exercise.
See also:
Annals of Surgery
Imperial College London is not responsible for the content of external internet
sites
Department of Surgery and Cancer
Faculty of Medicine
Long periods without sleep are known to increase doctors' risk of making poor
judgements and committing medical errors. The study was designed as a
preliminary investigation into whether certain drugs might be effective at
reversing some of the effects of fatigue.
Colin Sugden, Clinical Lecturer in Surgery, Department of Surgery and Cancer at
Imperial College London, who led the study, said: "This study set out to explore
whether modafinil, a wakefulness-promoting drug, might help doctors to perform
more effectively under conditions of fatigue when their performance might
otherwise be compromised."
In this randomised double-blind trial, 20 healthy male doctors took modafinil
and 19 took a placebo after one night of sleep deprivation. All were asked to
complete both a series of tasks that are commonly used in psychology research
and a virtual reality surgical motor skills task.
In the psychological tasks, the group that had taken modafinil performed better
in tests of working memory and planning, were less impulsive decision-makers,
and were more responsive to changing demands during a task. However, there was
no significant difference between the two groups on the surgical motor skills
task.
Mr Sugden said: "Participants in the modafinil group were less impulsive,
displayed greater flexibility and solved working memory and planning problems
more efficiently than those in the placebo group. However, no benefit was seen
in the performance of a basic motor skills task. This was a small, short-term
study so we have to be very cautious about how the results are interpreted. Most
importantly, it is not clear how performance on tests of mental function relate
to how someone performs as a doctor."
The researchers stress that these results remain to be confirmed with a larger
sample size and ideally in a longer term study.
The research explored the effects of one dose of modafinil over a short term and
it was not designed to investigate the effects of repeated use, either on a
person's physical and mental health or on their performance.
Mr Sugden said: "Larger studies looking at the performance effects and safety of
longer term use of the drug would need to be performed before we could draw
conclusions about whether or not sleep-deprived doctors might benefit from
taking it. There are also many challenging ethical considerations which will
need to be thought through very carefully.
"We should continue to do everything we can to ensure that doctors aren't in a
situation where fatigue might impact upon their performance. We don't suggest
that anyone should take modafinil to combat sleep deprivation, unless it has
been prescribed by a doctor.
The study was funded by Imperial College London.
-ENDS-
For further information please contact:
Simon Levey
Research Media Officer
Imperial College London
e-mail: s.levey@imperial.ac.uk
Telephone: +44 (0)207 594 6702 or ext. 46702
Out of hours duty Press Officer: +44 (0)7803 886 248
Notes to editors:
1. Journal reference: C. Sugden et al. Effect of pharmacological enhancement on
the cognitive and clinical psychomotor performance of sleep deprived doctors.
Annals of Surgery, 2011 DOI: 10.1097/SLA.0b013e3182306c99
2. About Imperial College London
Consistently rated amongst the world's best universities, Imperial College
London is a science-based institution with a reputation for excellence in
teaching and research that attracts 14,000 students and 6,000 staff of the
highest international quality. Innovative research at the College explores the
interface between science, medicine, engineering and business, delivering
practical solutions that improve quality of life and the environment -
underpinned by a dynamic enterprise culture.
Since its foundation in 1907, Imperial's contributions to society have included
the discovery of penicillin, the development of holography and the foundations
of fibre optics. This commitment to the application of research for the benefit
of all continues today, with current focuses including interdisciplinary
collaborations to improve global health, tackle climate change, develop
sustainable sources of energy and address security challenges.
In 2007, Imperial College London and Imperial College Healthcare NHS Trust
formed the UK's first Academic Health Science Centre. This unique partnership
aims to improve the quality of life of patients and populations by taking new
discoveries and translating them into new therapies as quickly as possible.
Website: www.imperial.ac.uk
LOAD-DATE: October 14, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 States News Service
22 of 998 DOCUMENTS
Globes [online] - Israel's Business Arena
October 13, 2011 Thursday
Teva receives European approval for Cephalon acquisition;
The deal will be closed Friday.
BYLINE: Guy Katsovitch
LENGTH: 267 words
Teva Pharmaceutical Industries Ltd. (Nasdaq: TEVA; TASE: TEVA) and Cephalon Inc.
(Nasdaq: CEPH ) announced today that they received approval from the European
Commission to proceed with Teva's $7 billion acquisition of innovative drugs
company Cephalon.
A condition of the approval is that Teva must divest Cephalon's marketing
authorization of generic modafinil in France and grant to the purchaser of this
marketing authorization certain additional rights with respect to the entire
European Economic Area, including a covenant not to sue effective as of October
2012.
Teva received approval for the US authorities for the merger at the beginning of
the week. Under that approval, Teva is required to divest two ANDAs for fentanyl
citrate lozenges, a generic version of Actiq, and cyclobenzaprine ER capsules,
the generic version of Amrix. Teva will also grant non-exclusive U.S. rights to
an undisclosed company to market modafinil tablets, the generic version of
Provigil, which had annual brand sales in the US of approximately $1.1 billion.
With the European Commission approval, the parties have now obtained all
regulatory approvals required to close the transaction and, accordingly, have
scheduled a closing date of October 14, 2011.
Teva projects that the deal will be accretive on a non-GAAP basis as soon as it
is completed, and on a GAAP basis within four quarters. Teva also expects
synergies of $500 million in the third year after completion.
Published by Globes [online], Israel business news - www.globes-online.com - on
October 13, 2011
© Copyright of Globes Publisher Itonut (1983) Ltd. 2011
LOAD-DATE: October 14, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2011 Globes Publisher Itonut (1983) Ltd.
All Rights Reserved
23 of 998 DOCUMENTS
Globes [online] - Israel's Business Arena
October 13, 2011 Thursday
Teva receives European approval for Cephalon acquisition;
The deal will be closed Friday.
BYLINE: Guy Katsovitch
LENGTH: 267 words
Teva Pharmaceutical Industries Ltd. (Nasdaq: TEVA; TASE: TEVA) and Cephalon Inc.
(Nasdaq: CEPH ) announced today that they received approval from the European
Commission to proceed with Teva's $7 billion acquisition of innovative drugs
company Cephalon.
A condition of the approval is that Teva must divest Cephalon's marketing
authorization of generic modafinil in France and grant to the purchaser of this
marketing authorization certain additional rights with respect to the entire
European Economic Area, including a covenant not to sue effective as of October
2012.
Teva received approval for the US authorities for the merger at the beginning of
the week. Under that approval, Teva is required to divest two ANDAs for fentanyl
citrate lozenges, a generic version of Actiq, and cyclobenzaprine ER capsules,
the generic version of Amrix. Teva will also grant non-exclusive U.S. rights to
an undisclosed company to market modafinil tablets, the generic version of
Provigil, which had annual brand sales in the US of approximately $1.1 billion.
With the European Commission approval, the parties have now obtained all
regulatory approvals required to close the transaction and, accordingly, have
scheduled a closing date of October 14, 2011.
Teva projects that the deal will be accretive on a non-GAAP basis as soon as it
is completed, and on a GAAP basis within four quarters. Teva also expects
synergies of $500 million in the third year after completion.
Published by Globes [online], Israel business news - www.globes-online.com - on
October 13, 2011
© Copyright of Globes Publisher Itonut (1983) Ltd. 2011
LOAD-DATE: October 14, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2011 Globes Publisher Itonut (1983) Ltd.
All Rights Reserved
24 of 998 DOCUMENTS
Federal Trade Commission Documents and Publications
October 7, 2011
FTC Requires Sale of Generic Cancer Pain Drug and Muscle Relaxant as Conditions
of Teva's $6.8 Billion Acquisition of Cephalon
SECTION: OFFICE OF PUBLIC AFFAIRS
LENGTH: 1052 words
For Release: 10/07/2011
FTC Requires Sale of Generic Cancer Pain Drug and Muscle Relaxant as Conditions
of Teva's $6.8 Billion Acquisition of Cephalon
Par Pharmaceuticals Will Acquire Drug Assets, Enter Agreement To Make Generic
Provigil
To protect competition in the market for prescription drugs, the Federal Trade
Commission will require Teva Pharmaceutical Industries Ltd. to sell the rights
and assets related to a generic cancer pain drug and a generic muscle relaxant,
as a condition of its proposed $6.8 billion acquisition of rival drug firm
Cephalon, Inc. In addition, the proposed settlement requires Teva to enter into
a supply agreement that will allow a competing firm to sell a generic version of
Cephalon's wakefulness drug Provigil in 2012.
"This settlement preserves competitive markets for current generic drugs, which
are key to holding down the cost of health care for consumers. It also ensures
there will be competition among generic drugs introduced in the future," said
Richard Feinstein, Director of the FTC's Bureau of Competition.
According to the FTC's complaint
(http://www.ftc.gov/os/caselist/1110166/111007tevacephaloncmpt.pdf), the
acquisition as originally proposed would violate U.S. antitrust law by reducing
competition in three markets: transmucosal fentanyl citrate lozenges used to
treat cancer pain; extended release cyclobenzaprine hydrochloride used as a
muscle relaxant; and modafinil tablets used to improve wakefulness. The markets
for each of these drugs is described below.
Transmucosal fentanyl citrate lozenges are versions of the cancer pain drug
developed by Cephalon and marketed under the brand name Actiq. Three generic
versions of the drug, manufactured and marketed by Teva, Cephalon/Watson
Pharmaceuticals, and Covidien, currently exist in the United States; this number
would be reduced to two after Teva's acquisition of Cephalon. As originally
proposed, the deal would have given Teva more than an 80 percent share of the
sales of the generic Actiq product.
Extended release cyclobenzaprine hydrochloride is an extended release version of
the muscle relaxant Flexeril. Cephalon acquired the rights to the branded
version of the drug, called Amrix, which was approved by the FDA in 2007. While
no companies currently make or market a generic version of Amrix, Teva and
Cephalon are two of only a limited number of suppliers that may be able to enter
the market quickly with a generic product. Combining the two companies would
result in less competition in the future.
Modafinil tablets are versions of the brand name drug Provigil marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. No companies currently market a generic version of Provigil,
which had sales of $1 billion in 2010. Teva, Ranbaxy Pharmaceuticals, Inc.,
Mylan Pharmaceutical Inc., and Barr Laboratories, Inc. - which Teva now owns -
all have taken steps toward entering the market, and all are eligible to seek a
180-day marketing exclusivity provided under federal law. However, each company
also has signed an agreement with Cephalon to refrain from marketing generic
Provigil until April 2012. The FTC contends that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day exclusivity period.
In each of the three markets, Teva's acquisition of Cephalon would harm
consumers by significantly reducing competition, leading to higher prices, the
FTC contends. The proposed settlement order is designed to replace the
competition lost through Teva's acquisition of Cephalon. First, it requires Teva
to sell all of its rights and assets related to generic Actiq or transmucosal
fentanyl citrate lozenges, and Actiq or generic extended release cyclobenzaprine
hydrochloride capsules, to Par Pharmaceuticals, Inc., a generic drug
manufacturer based in New Jersey. This divestiture must be completed within 10
days of the acquisition.
Next, to remedy the consolidation of marketers of modafinil drugs during the
180-day exclusivity period, the proposed order requires Teva to enter into a
supply agreement to provide Par with generic modafinil tablets in the United
States for one year. This will allow Par to compete with a generic modafinil
product during the 180-day exclusivity period. In addition, Par may extend the
modafinil supply agreement for another year.
The Commission vote approving the complaint and proposed consent order was 4-0.
The order will be published in the Federal Register shortly and will be subject
to public comment for 30 days, until November 7, 2011, after which the
Commission will decide whether to make it final. Comments can be submitted
electronically here
(https://ftcpublic.commentworks.com/ftc/tevacephalonconsent).
NOTE: The Commission issues a complaint when it has "reason to believe" that the
law has been or is being violated, and it appears to the Commission that a
proceeding is in the public interest. The issuance of a complaint is not a
finding or ruling that the respondent has violated the law. A consent order is
for settlement purposes only and does not constitute an admission of a law
violation. When the Commission issues a consent order on a final basis, it
carries the force of law with respect to future actions. Each violation of such
an order may result in a civil penalty of up to $16,000.
The FTC's Bureau of Competition works with the Bureau of Economics to
investigate alleged anticompetitive business practices and, when appropriate,
recommends that the Commission take law enforcement action. To inform the Bureau
about particular business practices, call 202-326-3300, send an e-mail to
antitrust@ftc.gov, or write to the Office of Policy and Coordination, Bureau of
Competition, Federal Trade Commission, 601 New Jersey Ave., Room 7117,
Washington, DC 20580. To learn more about the Bureau of Competition, read
Competition Counts (http://www.ftc.gov/competitioncounts). Like the FTC on
Facebook (http://www.ftc.gov/leaving/facebook/index.shtml) and follow us on
Twitter (http://www.ftc.gov/leaving/twitter/index.shtm).
MEDIA CONTACT:
Mitchell J. Katz,
Office of Public Affairs
202-326-2161
STAFF CONTACT:
Kari Wallace,
Bureau of Competition
202-326-3085
(FTC File No. 111-0166)
(Teva-Cephalon.final)
LOAD-DATE: October 7, 2011
LANGUAGE: ENGLISH
JOURNAL-CODE: FTDA
Copyright 2011 Federal Information and News Dispatch, Inc.
25 of 998 DOCUMENTS
States News Service
October 7, 2011 Friday
FTC REQUIRES SALE OF GENERIC CANCER PAIN DRUG AND MUSCLE RELAXANT AS CONDITIONS
OF TEVA'S $6.8 BILLION ACQUISITION OF CEPHALON PAR PHARMACEUTICALS WILL ACQUIRE
DRUG ASSETS, ENTER AGREEMENT TO MAKE GENERIC PROVIGIL
BYLINE: States News Service
LENGTH: 970 words
DATELINE: WASHINGTON
The following information was released by the Federal Trade Commission:
To protect competition in the market for prescription drugs, the Federal Trade
Commission will require Teva Pharmaceutical Industries Ltd. to sell the rights
and assets related to a generic cancer pain drug and a generic muscle relaxant,
as a condition of its proposed $6.8 billion acquisition of rival drug firm
Cephalon, Inc. In addition, the proposed settlement requires Teva to enter into
a supply agreement that will allow a competing firm to sell a generic version of
Cephalons wakefulness drug Provigil in 2012.
This settlement preserves competitive markets for current generic drugs, which
are key to holding down the cost of health care for consumers. It also ensures
there will be competition among generic drugs introduced in the future, said
Richard Feinstein, Director of the FTCs Bureau of Competition.
According to the FTCs complaint, the acquisition as originally proposed would
violate U.S. antitrust law by reducing competition in three markets:
transmucosal fentanyl citrate lozenges used to treat cancer pain; extended
release cyclobenzaprine hydrochloride used as a muscle relaxant; and modafinil
tablets used to improve wakefulness. The markets for each of these drugs is
described below.
Transmucosal fentanyl citrate lozenges are versions of the cancer pain drug
developed by Cephalon and marketed under the brand name Actiq. Three generic
versions of the drug, manufactured and marketed by Teva, Cephalon/Watson
Pharmaceuticals, and Covidien, currently exist in the United States; this number
would be reduced to two after Tevas acquisition of Cephalon. As originally
proposed, the deal would have given Teva more than an 80 percent share of the
sales of the generic Actiq product.
Extended release cyclobenzaprine hydrochloride is an extended release version of
the muscle relaxant Flexeril. Cephalon acquired the rights to the branded
version of the drug, called Amrix, which was approved by the FDA in 2007. While
no companies currently make or market a generic version of Amrix, Teva and
Cephalon are two of only a limited number of suppliers that may be able to enter
the market quickly with a generic product. Combining the two companies would
result in less competition in the future.
Modafinil tablets are versions of the brand name drug Provigil marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. No companies currently market a generic version of Provigil,
which had sales of $1 billion in 2010. Teva, Ranbaxy Pharmaceuticals, Inc.,
Mylan Pharmaceutical Inc., and Barr Laboratories, Inc. which Teva now owns all
have taken steps toward entering the market, and all are eligible to seek a
180-day marketing exclusivity provided under federal law. However, each company
also has signed an agreement with Cephalon to refrain from marketing generic
Provigil until April 2012. The FTC contends that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day exclusivity period.
In each of the three markets, Tevas acquisition of Cephalon would harm consumers
by significantly reducing competition, leading to higher prices, the FTC
contends. The proposed settlement order is designed to replace the competition
lost through Tevas acquisition of Cephalon. First, it requires Teva to sell all
of its rights and assets related to generic Actiq or transmucosal fentanyl
citrate lozenges, and Actiq or generic extended release cyclobenzaprine
hydrochloride capsules, to Par Pharmaceuticals, Inc., a generic drug
manufacturer based in New Jersey. This divestiture must be completed within 10
days of the acquisition.
Next, to remedy the consolidation of marketers of modafinil drugs during the
180-day exclusivity period, the proposed order requires Teva to enter into a
supply agreement to provide Par with generic modafinil tablets in the United
States for one year. This will allow Par to compete with a generic modafinil
product during the 180-day exclusivity period. In addition, Par may extend the
modafinil supply agreement for another year.
The Commission vote approving the complaint and proposed consent order was 4-0.
The order will be published in the Federal Register shortly and will be subject
to public comment for 30 days, until November 7, 2011, after which the
Commission will decide whether to make it final. Comments can be submitted
electronically here.
NOTE: The Commission issues a complaint when it has reason to believe that the
law has been or is being violated, and it appears to the Commission that a
proceeding is in the public interest. The issuance of a complaint is not a
finding or ruling that the respondent has violated the law. A consent order is
for settlement purposes only and does not constitute an admission of a law
violation. When the Commission issues a consent order on a final basis, it
carries the force of law with respect to future actions. Each violation of such
an order may result in a civil penalty of up to $16,000.
The FTCs Bureau of Competition works with the Bureau of Economics to investigate
alleged anticompetitive business practices and, when appropriate, recommends
that the Commission take law enforcement action. To inform the Bureau about
particular business practices, call 202-326-3300, send an e-mail to
antitrust@ftc.gov, or write to the Office of Policy and Coordination, Bureau of
Competition, Federal Trade Commission, 601 New Jersey Ave., Room 7117,
Washington, DC 20580. To learn more about the Bureau of Competition, read
Competition Counts. Like the FTC on Facebook and follow us on Twitter.
MEDIA CONTACT:
Mitchell J. Katz,
Office of Public Affairs
202-326-2161
STAFF CONTACT:
Kari Wallace,
Bureau of Competition
202-326-3085
LOAD-DATE: October 8, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 States News Service
26 of 998 DOCUMENTS
Targeted News Service
October 7, 2011 Friday 2:16 AM EST
FTC Requires Sale of Generic Cancer Pain Drug and Muscle Relaxant as Conditions
of Teva's $6.8 Billion Acquisition of Cephalon
BYLINE: Targeted News Service
LENGTH: 968 words
DATELINE: WASHINGTON
The Federal Trade Commission issued the following news release:
To protect competition in the market for prescription drugs, the Federal Trade
Commission will require Teva Pharmaceutical Industries Ltd. to sell the rights
and assets related to a generic cancer pain drug and a generic muscle relaxant,
as a condition of its proposed $6.8 billion acquisition of rival drug firm
Cephalon, Inc. In addition, the proposed settlement requires Teva to enter into
a supply agreement that will allow a competing firm to sell a generic version of
Cephalon's wakefulness drug Provigil in 2012.
"This settlement preserves competitive markets for current generic drugs, which
are key to holding down the cost of health care for consumers. It also ensures
there will be competition among generic drugs introduced in the future," said
Richard Feinstein, Director of the FTC's Bureau of Competition.
According to the FTC's complaint, the acquisition as originally proposed would
violate U.S. antitrust law by reducing competition in three markets:
transmucosal fentanyl citrate lozenges used to treat cancer pain; extended
release cyclobenzaprine hydrochloride used as a muscle relaxant; and modafinil
tablets used to improve wakefulness. The markets for each of these drugs is
described below.
Transmucosal fentanyl citrate lozenges are versions of the cancer pain drug
developed by Cephalon and marketed under the brand name Actiq. Three generic
versions of the drug, manufactured and marketed by Teva, Cephalon/Watson
Pharmaceuticals, and Covidien, currently exist in the United States; this number
would be reduced to two after Teva's acquisition of Cephalon. As originally
proposed, the deal would have given Teva more than an 80 percent share of the
sales of the generic Actiq product.
Extended release cyclobenzaprine hydrochloride is an extended release version of
the muscle relaxant Flexeril. Cephalon acquired the rights to the branded
version of the drug, called Amrix, which was approved by the FDA in 2007. While
no companies currently make or market a generic version of Amrix, Teva and
Cephalon are two of only a limited number of suppliers that may be able to enter
the market quickly with a generic product. Combining the two companies would
result in less competition in the future.
Modafinil tablets are versions of the brand name drug Provigil marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. No companies currently market a generic version of Provigil,
which had sales of $1 billion in 2010. Teva, Ranbaxy Pharmaceuticals, Inc.,
Mylan Pharmaceutical Inc., and Barr Laboratories, Inc. - which Teva now owns -
all have taken steps toward entering the market, and all are eligible to seek a
180-day marketing exclusivity provided under federal law. However, each company
also has signed an agreement with Cephalon to refrain from marketing generic
Provigil until April 2012. The FTC contends that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day exclusivity period.
In each of the three markets, Teva's acquisition of Cephalon would harm
consumers by significantly reducing competition, leading to higher prices, the
FTC contends. The proposed settlement order is designed to replace the
competition lost through Teva's acquisition of Cephalon. First, it requires Teva
to sell all of its rights and assets related to generic Actiq or transmucosal
fentanyl citrate lozenges, and Actiq or generic extended release cyclobenzaprine
hydrochloride capsules, to Par Pharmaceuticals, Inc., a generic drug
manufacturer based in New Jersey. This divestiture must be completed within 10
days of the acquisition.
Next, to remedy the consolidation of marketers of modafinil drugs during the
180-day exclusivity period, the proposed order requires Teva to enter into a
supply agreement to provide Par with generic modafinil tablets in the United
States for one year. This will allow Par to compete with a generic modafinil
product during the 180-day exclusivity period. In addition, Par may extend the
modafinil supply agreement for another year.
The Commission vote approving the complaint and proposed consent order was 4-0.
The order will be published in the Federal Register shortly and will be subject
to public comment for 30 days, until November 7, 2011, after which the
Commission will decide whether to make it final. Comments can be submitted
electronically here.
NOTE: The Commission issues a complaint when it has "reason to believe" that the
law has been or is being violated, and it appears to the Commission that a
proceeding is in the public interest. The issuance of a complaint is not a
finding or ruling that the respondent has violated the law. A consent order is
for settlement purposes only and does not constitute an admission of a law
violation. When the Commission issues a consent order on a final basis, it
carries the force of law with respect to future actions. Each violation of such
an order may result in a civil penalty of up to $16,000.
The FTC's Bureau of Competition works with the Bureau of Economics to
investigate alleged anticompetitive business practices and, when appropriate,
recommends that the Commission take law enforcement action. To inform the Bureau
about particular business practices, call 202-326-3300, send an e-mail to
antitrust@ftc.gov, or write to the Office of Policy and Coordination, Bureau of
Competition, Federal Trade Commission, 601 New Jersey Ave., Room 7117,
Washington, DC 20580. To learn more about the Bureau of Competition, read
Competition Counts. Like the FTC on Facebook and follow us on Twitter.
Contact: Mitchell J. Katz, 202/326-2161
Copyright Targeted News Services
TNS MT93 111008-3622578 61MarlizTagarum
LOAD-DATE: October 8, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Targeted News Service LLC
All Rights Reserved
27 of 998 DOCUMENTS
US Fed News
October 7, 2011 Friday 2:07 PM EST
FTC REQUIRES SALE OF GENERIC CANCER PAIN DRUG AND MUSCLE RELAXANT AS CONDITIONS
OF TEVA'S $6.8B ACQUISITION OF CEPHALON
LENGTH: 788 words
WASHINGTON, Oct. 7 -- The Federal Trade Commission issued the following press
release:
To protect competition in the market for prescription drugs, the Federal Trade
Commission will require Teva Pharmaceutical Industries Ltd. to sell the rights
and assets related to a generic cancer pain drug and a generic muscle relaxant,
as a condition of its proposed $6.8 billion acquisition of rival drug firm
Cephalon, Inc. In addition, the proposed settlement requires Teva to enter into
a supply agreement that will allow a competing firm to sell a generic version of
Cephalon's wakefulness drug Provigil in 2012.
"This settlement preserves competitive markets for current generic drugs, which
are key to holding down the cost of health care for consumers. It also ensures
there will be competition among generic drugs introduced in the future," said
Richard Feinstein, Director of the FTC's Bureau of Competition.
According to the FTC's complaint, the acquisition as originally proposed would
violate U.S. antitrust law by reducing competition in three markets:
transmucosal fentanyl citrate lozenges used to treat cancer pain; extended
release cyclobenzaprine hydrochloride used as a muscle relaxant; and modafinil
tablets used to improve wakefulness. The markets for each of these drugs is
described below.
Transmucosal fentanyl citrate lozenges are versions of the cancer pain drug
developed by Cephalon and marketed under the brand name Actiq. Three generic
versions of the drug, manufactured and marketed by Teva, Cephalon/Watson
Pharmaceuticals, and Covidien, currently exist in the United States; this number
would be reduced to two after Teva's acquisition of Cephalon. As originally
proposed, the deal would have given Teva more than an 80 percent share of the
sales of the generic Actiq product.
Extended release cyclobenzaprine hydrochloride is an extended release version of
the muscle relaxant Flexeril. Cephalon acquired the rights to the branded
version of the drug, called Amrix, which was approved by the FDA in 2007. While
no companies currently make or market a generic version of Amrix, Teva and
Cephalon are two of only a limited number of suppliers that may be able to enter
the market quickly with a generic product. Combining the two companies would
result in less competition in the future.
Modafinil tablets are versions of the brand name drug Provigil marketed by
Cephalon and used to treat excessive sleepiness caused by narcolepsy or shift
work disorder. No companies currently market a generic version of Provigil,
which had sales of $1 billion in 2010. Teva, Ranbaxy Pharmaceuticals, Inc.,
Mylan Pharmaceutical Inc., and Barr Laboratories, Inc. - which Teva now owns -
all have taken steps toward entering the market, and all are eligible to seek a
180-day marketing exclusivity provided under federal law. However, each company
also has signed an agreement with Cephalon to refrain from marketing generic
Provigil until April 2012. The FTC contends that without the proposed
settlement, Teva and Cephalon would have been two of only a limited number of
suppliers of generic Provigil during the 180-day exclusivity period.
In each of the three markets, Teva's acquisition of Cephalon would harm
consumers by significantly reducing competition, leading to higher prices, the
FTC contends. The proposed settlement order is designed to replace the
competition lost through Teva's acquisition of Cephalon. First, it requires Teva
to sell all of its rights and assets related to generic Actiq or transmucosal
fentanyl citrate lozenges, and Actiq or generic extended release cyclobenzaprine
hydrochloride capsules, to Par Pharmaceuticals, Inc., a generic drug
manufacturer based in New Jersey. This divestiture must be completed within 10
days of the acquisition.
Next, to remedy the consolidation of marketers of modafinil drugs during the
180-day exclusivity period, the proposed order requires Teva to enter into a
supply agreement to provide Par with generic modafinil tablets in the United
States for one year. This will allow Par to compete with a generic modafinil
product during the 180-day exclusivity period. In addition, Par may extend the
modafinil supply agreement for another year.
The Commission vote approving the complaint and proposed consent order was 4-0.
The order will be published in the Federal Register shortly and will be subject
to public comment for 30 days, until November 7, 2011, after which the
Commission will decide whether to make it final. Comments can be submitted
electronically here
(https://ftcpublic.commentworks.com/ftc/tevacephalonconsent). For any query with
respect to this article or any other content requirement, please contact Editor
at htsyndication@hindustantimes.com
LOAD-DATE: October 10, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 HT Media Ltd.
All Rights Reserved
28 of 998 DOCUMENTS
Indian Patents News
September 13, 2011 Tuesday 6:30 AM EST
Cephalon Inc Receives Patent for Novel Pharmaceutical Formulations of Modafinil
LENGTH: 262 words
New Delhi, Sept. 13 -- Cephalon Inc received patent for novel pharmaceutical
formulations of modafinil on Dec. 14, 2007. The patent number issued by the
Indian Patent Office is 212727.
Cephalon Inc had filed patent application number 633/KOLNP/2005 for novel
pharmaceutical formulations of modafinil on April 13, 2005. The inventors of the
patent are Vincent Corvari, George Grandolfi and Alpa Parikh.
The International classification number is A61K7/28.
The PCT International application number of the patent is PCT/US03/028528 and
the application was filed on Sept. 11, 2003.
According to the Controller General of Patents, Designs & Trade Marks, "A
composition comprising modafinil, wherein modafinil comprises about 90% by
weight of the composition; a lactose monohydrate which comprises about 3-10% of
the composition by weight; a cross-linked sodium carboxymethyl cellulose, which
comprises about 2-5% of the composition by weight; a polyvinyl pyrrolidone,
which comprises about 2-5% of the composition by weight; and magnesium stearate,
which comprises about 0.2-2.0% of the composition by weight."
About the Company
Cephalon, Inc. (NASDAQ: CEPH) is a U.S. biopharmaceutical company co-founded in
1987 by Dr. Frank Baldino, Jr., a pharmacologist and former scientist with the
DuPont Company, who served as the company's chairman and chief executive officer
until his death in December 2010. The company's name comes from the adjective
"cephalic" meaning "related to the head or brain," and it was established
primarily to pursue treatments for neurodegenerative diseases.
LOAD-DATE: September 13, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
29 of 998 DOCUMENTS
Indian Patents News
August 18, 2011 Thursday 6:30 AM EST
Cephalon Inc Files Patent Application for Modafinil Pharmaceutical Compositions
LENGTH: 275 words
New Delhi, Aug. 18 -- USA based Cephalon Inc filed patent application for
modafinil pharmaceutical compositions. The inventors are Heacock Craig, Parikh
Alpa and Patel Piyush R.
Cephalon Inc filed the patent application on Feb. 11, 2005. The patent
application number is 00172/KOLNP/2005 A. The international classification
number is A61K31/165.
According to the Controller General of Patents, Designs & Trade Marks,
"Pharmaceutical compositions comprising modafinil in the form of particles of
defined size. The particle size of modafinil can have a significant effect on
the potency and safety profile of the drug."
About the Company
Cephalon, Inc. (Public, NASDAQ:CEPH) is an international biopharmaceutical
company engaged in the discovery, development and commercialization of products
in four core therapeutic areas: central nervous system (CNS), pain, oncology and
inflammatory disease. In addition to conducting an active research and
development program, it markets seven products in the United States and numerous
products in various countries throughout Europe and the world. Its principal
product are its wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and
NUVIGIL (armodafinil) Tablets [C-IV], which comprised 51% of its total
consolidated net sales during the year ended December 31, 2009. During 2009,
Cephalon, Inc. acquired an exclusive, worldwide license to the ImmuPharma
investigational compound, LUPUZOR, which is in Phase IIb development for the
treatment of systemic lupus erythematosus. In August 2009, Cephalon, Inc.
acquired Arana Therapeutics Limited. In April 2010, the Company acquired Mepha,
a pharmaceutical company.
LOAD-DATE: August 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
30 of 998 DOCUMENTS
Indian Patents News
August 18, 2011 Thursday 6:30 AM EST
Alembic Limited Files Patent Application for Process for the Preparation of
2-[(diphenylmethyl) Thio] Acetamide
LENGTH: 342 words
New Delhi, Aug. 18 -- India based Alembic Limited filed patent application for
process for the preparation of 2-[(diphenylmethyl) thio] acetamide. The
inventors are Bhatt Surendra B, Patel Jiten R, Panchasara Dinesh, Shah Hetal R,
Deo Keshav and Kansal Vinod Kumar.
Alembic Limited filed the patent application on Jan. 31, 2003. The patent
application number is 130/MUM/2003. The international classification numbers are
A61K31/165, C07C317/44 and C07C323/29.
According to the Controller General of Patents, Designs & Trade Marks, "Process
for the preparation of 2-[(diphenylmethyl) thioacetamide, an intermediate for
the preparation of Modafinil which is a CNS stimulant and used for the treatment
of narcolepsia. The process comprises reacting 2-[dipenylmethyl) thio] acetic
acid with alcohols, in presence of catalytic amount of inorganic acid or organic
acid at reflux temperature of alcohol to obtain corresponding ester which is
reacted with ammonia to give 2- [(diphenylmethyl)thio]acetamide. If desired 2-
[(diphenylmethyl) thioacetamide thus produced is reacted with hydrogen peroxide
to produce Modafinil."
About the Company
Alembic Limited (Public, BOM:506235) is engaged in manufacturing synthetic
active pharmaceutical ingredients (APIs), consisting of independent
manufacturing blocks for Macrolides, non-steroidal anti-inflammatory drugs
(NSAIDs) and other drugs. The Company's veterinary products include
antibiotics/anti-microbials injectables/orals, speciality injectables,
endectocides, boli, feed supplements and poultry. The Company's therapeutic
category includes anti-infectives, caphalosporins, anti-protozoal, musculo
skeletal, erectile dtsfunction, anti-parkinsons, anti-depressants,
anti-epileptics, CNS stimulant, anti anziety and cardiovascular. Its basket of
formulation products contain 150 products in several forms belonging to diverse
therapeutic segments, including anti-infective, cough and cold products to
cardiovascular and oral anti-diabetics. The wholly owned subsidiary of the
Company is Alembic Global Holding SA.
LOAD-DATE: August 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
31 of 998 DOCUMENTS
Targeted News Service
August 6, 2011 Saturday 3:52 AM EST
SRI International, HealthPartners Research Foundation Assigned Patent
BYLINE: Targeted News Service
LENGTH: 267 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Aug. 6 -- SRI International, Menlo Park, Calif., and
HealthPartners Research Foundation, Minneapolis, have been assigned a patent
(7,989,502) developed by five co-inventors for an "intranasal delivery of
modafinil." The co-inventors are Mary Ann Katherine Greco, San Francisco,
William Howard Frey II, White Bear Lake, Minn., Jacqueline DeRose, Santa Clara,
Calif., Rachel Beth Matthews, Dayton, Minn., and Leah Ranae Bresin Hanson,
Vadnais Heights, Minn.
The abstract of the patent published by the U.S. Patent and Trademark Office
states: "Modafinil is selectively delivered to the brain, minimizing delivery to
the blood, of a person in need thereof by administering to the person a
therapeutically-effective dosage of modafinil, wherein the dosage is less than 1
mg, formulated in a lipid microemulsion (LME) and selectively delivered to the
upper third of the nasal cavity. The method may be implemented with an
intranasal pharmaceutical delivery device loaded with a modafinil composition
and adapted to deliver the dosage to the upper third of the nasal cavity."
The patent application was filed on Feb. 6, 2009 (12/367,496). The full-text of
the patent can be found at
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,989,502.PN.&OS=PN/7,989,502&RS=
PN/7,989,502
Written by Shabnam Sheikh; edited by Jaya Anand.
For more information about Targeted News Service federal patent awards please
contact: Myron Struck, Editor, Direct: 703/866-4708, Cell: 703/304-1897,
Myron@targetednews.com
SH0806JA0806-604728
LOAD-DATE: September 22, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Targeted News Service LLC
All Rights Reserved
32 of 998 DOCUMENTS
Indian Patents News
July 31, 2011 Sunday 6:30 AM EST
Alembic Limited Files Patent Application for Process for the Preparation of
Modafinil of Formula II
LENGTH: 314 words
New Delhi, July 31 -- India based Alembic Limited filed patent application for
process for the preparation of Modafinil of formula II. The inventors are Bhatt
Surendra B, Patel Jiten R, Panchasara Dinesh, Shah Hetal R, Deo Keshav and
Kansal Vinod Kumar.
Alembic Limited filed the patent application on Dec. 21, 2004. The patent
application number is 1387/MUM/2004 A. The international classification number
is A61K31/400.
According to the Controller General of Patents, Designs & Trade Marks, "Process
for the preparation of Modafinil which is a CNS stimulant and used for the
treatment of narcolepsia. The process comprises reacting
2-[(diphenylmethyl)thio]acetic acid with alcohols, in presence of catalytic
amount of inorganic acid or organic acid at reflux temperature of alcohol to
obtain corresponding ester which is reacted with ammonia to give
2-[(diphenylmethyl)thio]acetamide, which is reacted with hydrogen peroxide to
produce Modafinil."
About the Company
Alembic Limited (Public, BOM:506235) is engaged in manufacturing synthetic
active pharmaceutical ingredients (APIs), consisting of independent
manufacturing blocks for Macrolides, non-steroidal anti-inflammatory drugs
(NSAIDs) and other drugs. The Company's veterinary products include
antibiotics/anti-microbials injectables/orals, speciality injectables,
endectocides, boli, feed supplements and poultry. The Company's therapeutic
category includes anti-infectives, caphalosporins, anti-protozoal, musculo
skeletal, erectile dtsfunction, anti-parkinsons, anti-depressants,
anti-epileptics, CNS stimulant, anti anziety and cardiovascular. Its basket of
formulation products contain 150 products in several forms belonging to diverse
therapeutic segments, including anti-infective, cough and cold products to
cardiovascular and oral anti-diabetics. The wholly owned subsidiary of the
Company is Alembic Global Holding SA.
LOAD-DATE: July 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
33 of 998 DOCUMENTS
Spicy IP
July 30, 2011 Saturday 9:00 PM EST
Does size matter: the case of an anti-narcoleptic drug, modafinil?
BYLINE: Rajiv Kr. Choudhry
LENGTH: 1245 words
Long post follows: About a month ago, the UK Chancery division patents courts
(England and Wales) rendered an opinion
(http://www.bailii.org/ew/cases/EWHC/Patents/2011/1591.html) (Justice Floyd)
regarding claim construction in defining size of particles of an
anti-narcoleptic drug, modafinil, in pharmaceutical compositions. The patent
court construed patent claims to determine whether there is an infringement, if
any.
Facts: The dispute involves three patents related to the drug modafinil, used
to treat sleep disorders such as narcolepsy. Orchid Europe is the manufacturer
of generic modafinil and Mylan intended to manufacture the drug in UK.
Cephalon is the proprietor, an exclusive licensee in the UK and a sub-licensee
of the patents involved (European Patents
(https://data.epo.org/publication-server/?lg=en) (UK) Numbers 0 731 698 ("698"),
0 966 962 ("962") and 1 088 549 ("549")). These patents contain a very similar
disclosure with differentiated claims, and they all claim a priority date of 6th
October 1994. Mylan denied infringement and challenged the validity of all three
Cephalon patents on the grounds of lack of inventive step and insufficiency.
Background: Modafinil, the active substance, was discovered and developed by a
French company, Lafon. Cephalon licensed modafinil in the USA in 1994 and
conducted further tests on it to bring it to the market as an agent to treat
sleep disorders. In the course of the tests in the US, modafinil caused more
side effects than in Europe in corresponding trials involving equivalent doses.
The cause was traced to smaller particle size of the input active pharmaceutical
ingredient ("API") of the lots used in the US trials. In the first human trials
performed on non-commercial samples of modafinil ("early lots"), the median
particle size diameter was between 80 and 150 m. The studies in US involved
"late lots", revealed unanticipated side effects at doses of 800 mg per day.
These late lots employed a particle size of 30 to 50 m. This led the patentee to
conclude that the late lots could be more readily absorbed than the early lots,
and therefore leading to an increased plasma concentration (increased
bioavailability) of modafinil. Claims: Each patent claimed different
formulations of modafinil, with different particle sizes. The relevant
portions of the first independent claims of each patent are reproduced below.
'698 patent '962 patent '549 patent
....comprising .... .... ... wherein at least about
modafinil particles, wherein comprising 95% of the cumulative total of
at least about 95% of the modafinil said modafinil particles in
cumulative total of particles said composition have a
modafinil particles in said having a diameter of less than about 200
composition have a diameter median m and wherein the median
of less than about 200 particle size particle size is about 10 to 60
micrometers (m). of about 2 to m.
about 60 m...
Issue: "Whether the claims were referring to the particle size within the
composition (Cephalon's contention) or whether they were referring to the
particle size in the active ingredient used to make the composition (Mylan's
contention)." Additionally, during the tabletting process, the size of the
particles in the final finished tablet differed from that in the API from which
the tablets are made. Therefore, the sizes of the particles in the API did not
correspond to the size of the particles in the finished tablets, and vice versa.
Claim construction and analysis: In the claim construction, both sides pointed
to claim language that supported their particular construction. For example,
Cephalon pointed to the '698 patent, which claimed 'compositions comprising'
modafinil particles and hence referring to the size of the particles in the
final tablets. Mylan pointed to the claims in the '962 patent for use of '
modafinil particles ...at least about 95% of the cumulative total of said
particles have a diameter of less than about 200 micrometers for the manufacture
of a pharmaceutical composition " and hence points to the particle size in the
input API, as it is used in the manufacturing process.Several industry practices
were listed to aid in the interpretation of claims, one of which was, "[A]
general practice in the pharmaceutical industry was not to measure particle size
in a solid formulation, but to make measurements on the input API." Conclusion:
Based on the common knowledge, the Judge concluded that the patentee must have
meant particle size to be measured on the bulk API. "Particle size is never
measured in the dosage form, and the skilled person would not know how to do
so." Although it routine industry practice to measure the particle size of API,
the particle size in finished tablets could not have been measured at the
priority date of the patents (1994). Additionally, particle size of the API has
a direct correlation with bioavailability in the final tablet. Therefore
contentions of Mylan were accepted. Infringement: Both parties agreed that
if Mylan's construction of the claims was the correct one, there was no
infringement. Obviousness: Mylan contended that the patents were invalid in
view of prior publications, 'Drugs of the future, and Nguyen, a PCT application
applied for by Lafon. On the basis of 'common general knowledge' and the
knowledge of the relationship between lower particle size and improved plasma
concentration or bioavailability, it was held that it would be routine to
investigate the particle size to improve the bioavailability of a compound, with
the expectation that this investigation would be fruitful. Hence Cephalon
patents were obvious in view of the first publication. As regards the Nguyen
publication, no dosage for modafinil specified but it did provide a formulation
with a particle size of 2-5 m. J. Floyd rejected the contention that it would
require significant experimentation/investment to the results of Nguyen to reach
an appropriate dosage for modafinil. "The skilled person is entitled to
implement a disclosure in a technically obvious way, even if doing so might not
appear commercially attractive. Had I not come to the conclusions I had already
reached in relation to obviousness, I would have required the claims to be
limited so as to avoid the attack."Significance to Indian scenario:Shamnad, in a
previous post
(http://spicyipindia.blogspot.com/2007/09/section-3d-and-efficacy-more-cases_09.
html), referred to a need for having broad guidelines for defining 'efficacy.'
In that post, the question was whether increased bioavailability would
constitute as a significant enhancement in efficacy. If this case was decided
under the Indian law, increased bioavailability and (therefore efficacy) would
have been the argument to counter a 3(d) opposition and it would have overcome
the challenge. This case therefore highlights when the patent office should
undertake the 3(d) analysis: Only when the basic issues (inventive and
non-obvious) should the Controller decide the issue of patentability under
section 3(d). This case also highlights whether it makes sense to equate
bioavailability to efficacy. The exclusionary test
(http://spicyipindia.blogspot.com/2010/08/exclusionary-definition-for-term.html)
may perhaps make more sense in such a scenario for formulation applications like
the one described here.
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Indian Patents News
July 19, 2011 Tuesday 6:30 AM EST
Cephalon Inc Files Patent Application for Pharmaceutical Formulations of
Modafinil
LENGTH: 286 words
New Delhi, July 19 -- USA based Cephalon Inc filed patent application for
pharmaceutical formulations of modafinil. The inventors are Craig Heacock, Alpa
Parikh and Piyush Patel.
Cephalon Inc filed the patent application on April 13, 2005. The patent
application number is 00632/KOLNP/2005 A. The international classification
numbers are A61K 31/165 and A61P 25/00.
According to the Controller General of Patents, Designs & Trade Marks,
"Compositions of modafinil and methods of treating neurologically related
conditions with the administration of modafinil. Also compositions that include
modafinil and one or more excipients such as diluents, disintegrants, binders
and lubricants."
About the Company
Cephalon, Inc. (Public, NASDAQ:CEPH) is an international biopharmaceutical
company engaged in the discovery, development and commercialization of products
in four core therapeutic areas: central nervous system (CNS), pain, oncology and
inflammatory disease. In addition to conducting an active research and
development program, it markets seven products in the United States and numerous
products in various countries throughout Europe and the world. Its principal
product are its wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and
NUVIGIL (armodafinil) Tablets [C-IV], which comprised 51% of its total
consolidated net sales during the year ended December 31, 2009. During 2009,
Cephalon, Inc. acquired an exclusive, worldwide license to the ImmuPharma
investigational compound, LUPUZOR, which is in Phase IIb development for the
treatment of systemic lupus erythematosus. In August 2009, Cephalon, Inc.
acquired Arana Therapeutics Limited. In April 2010, the Company acquired Mepha,
a pharmaceutical company.
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Washington Drug Letter
July 11, 2011 Monday
Barr Must Produce Settlement Docs in Provigil Pay-for-Delay Case
SECTION: Vol. 43 No. 27
LENGTH: 153 words
A federal court is ordering Teva subsidiary Barr Pharmaceuticals to disclose a
number of previously withheld documents in a long-running Provigil antitrust
case.
The 18 documents "relate to the settlement between Barr and Provigil maker
Cephalon and how, financially, the settlement terms would affect Chemagis,"
Barr's active pharmaceutical ingredient supplier and partner in developing
generic Provigil (modafinil). Barr must produce the documents by July 12,
according to the Tuesday filing in the U.S. District court for the Eastern
District of Pennsylvania.
The case, King Drug Company of Florence, Inc. et al. v. Cephalon, Inc. et al.,
concerns settlements made between Cephalon and several generic-drug makers to
delay generic versions of sleepiness drug Provigil (modafinil). The suit was
initially filed in 2006.
Teva did not return a request for comment by press time. -- Kevin O'Rourke
Release date: July 11, 2011
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Drug Industry Daily
July 7, 2011 Thursday
Court Orders Barr to Produce Settlement Documents in Provigil Pay-for-Delay Case
SECTION: Vol. 10 No. 132
LENGTH: 391 words
A federal court is ordering Teva subsidiary Barr Pharmaceuticals to disclose a
number of previously withheld documents in a long-running Provigil antitrust
case.
The 18 documents "relate to the settlement between Barr and Cephalon and how,
financially, the settlement terms would affect Chemagis," Barr's active
pharmaceutical ingredient supplier and partner in developing generic Provigil (
modafinil). Barr must produce the documents by July 12.
The case, King Drug Company of Florence, Inc. et al. v. Cephalon, Inc. et al.,
concerns settlements made between Cephalon and several generic-drug makers to
delay generic versions of Cephalon's sleepiness drug Provigil (modafinil). The
suit was initially filed in 2006.
A collection of distributors and pharmacies, including CVS, allege the
settlements "constitute an unlawful restraint of trade" and have sued Cephalon,
Barr and three other generic companies for antitrust violations, according to
Tuesday's filing in the U.S. District court for the Eastern District of
Pennsylvania.
The plaintiffs are seeking access to communications between Barr and Chemagis
between December 2005 and January 2006 -- prior to Barr's February 2006
agreement with Cephalon regarding generic Provigil.
The plaintiffs also argued that Barr waived attorney-client privilege on other
communications from the settlement with Cephalon, and must allow discovery of
the documents, but presiding judge Mitchell Goldberg denied that motion.
Since the case began, Teva has acquired a number of the companies involved,
including Barr. In a twist that shocked many analysts, Teva outbid Valeant in
May to buy Cephalon for $6.8 billion (DID, May 3).
The Provigil agreement has been the subject of government scrutiny for several
years. In 2006, the FTC asked Cephalon for information about settlements it made
with generic companies (DID, March 17, 2006). The European Commission also
recently announced that it had launched an investigation into the agreement
between Cephalon and Teva to delay generic Provigil (DID, May 2).
An FTC report released in May found deals struck between brand and generic
pharmaceutical companies are on the rise, despite efforts to restrict agreements
that delay market entry of cheaper drugs (DID, May 5).
Teva did not return a request for comment by press time. -- Kevin O'Rourke
Release date: July 7, 2011
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Indian Patents News
July 1, 2011 Friday 6:30 AM EST
Cephalon Inc. Files Patent Application for Novel Pharmaceutical Formulations of
Modafinil
LENGTH: 282 words
New Delhi, July 1 -- USA based Cephalon Inc. filed patent application for novel
pharmaceutical formulations of modafinil. The inventors are Corvari Vincent,
Grandolfi George and Parikh Alpa.
Cephalon Inc. filed the patent application on Dec. 12, 2003. The patent
application number is 01616/KOLNP/2003 A. The international classification
numbers are A61K31/165, 9/20 and 9/16.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention is related to compositions of modafinil, including
compositions of modafinil and one or more diluents, disintegrants, binders and
lubricants, and the processes for the preparation thereof."
About the Company
Cephalon, Inc. (Public, NASDAQ:CEPH) is an international biopharmaceutical
company engaged in the discovery, development and commercialization of products
in four core therapeutic areas: central nervous system (CNS), pain, oncology and
inflammatory disease. In addition to conducting an active research and
development program, it markets seven products in the United States and numerous
products in various countries throughout Europe and the world. Its principal
product are its wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and
NUVIGIL (armodafinil) Tablets [C-IV], which comprised 51% of its total
consolidated net sales during the year ended December 31, 2009. During 2009,
Cephalon, Inc. acquired an exclusive, worldwide license to the ImmuPharma
investigational compound, LUPUZOR, which is in Phase IIb development for the
treatment of systemic lupus erythematosus. In August 2009, Cephalon, Inc.
acquired Arana Therapeutics Limited. In April 2010, the Company acquired Mepha,
a pharmaceutical company.
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Indian Patents News
June 30, 2011 Thursday 6:30 AM EST
Cephalon Inc Files Patent Application for Novel Pharmaceutical Formulations of
Modafinil
LENGTH: 283 words
New Delhi, June 30 -- USA based Cephalon Inc filed patent application for novel
pharmaceutical formulations of modafinil. The inventors are Vincent Corvari,
George Grandolfi and Alpa Parikh.
Cephalon Inc filed the patent application on April 13, 2005. The patent
application number is 00633/KOLNP/2005A. The international classification
numbers are A61K 31/165
9/16,9/20 and 9/48.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention is related to compositions of modafinil, including
compositions of modafinil and one or more diluents, disintegrants, binders and
lubricants, and the processes for their preparation thereof."
About the Company
Cephalon, Inc. (Public, NASDAQ:CEPH) is an international biopharmaceutical
company engaged in the discovery, development and commercialization of products
in four core therapeutic areas: central nervous system (CNS), pain, oncology and
inflammatory disease. In addition to conducting an active research and
development program, it markets seven products in the United States and numerous
products in various countries throughout Europe and the world. Its principal
product are its wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and
NUVIGIL (armodafinil) Tablets [C-IV], which comprised 51% of its total
consolidated net sales during the year ended December 31, 2009. During 2009,
Cephalon, Inc. acquired an exclusive, worldwide license to the ImmuPharma
investigational compound, LUPUZOR, which is in Phase IIb development for the
treatment of systemic lupus erythematosus. In August 2009, Cephalon, Inc.
acquired Arana Therapeutics Limited. In April 2010, the Company acquired Mepha,
a pharmaceutical company.
LOAD-DATE: June 30, 2011
LANGUAGE: ENGLISH
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39 of 998 DOCUMENTS
The Irish Times
May 17, 2011 Tuesday
Student abuse of wakefulness drug leads to restrictions
BYLINE: DR MUIRIS HOUSTON
SECTION: HEALTH; Health News; Pg. 2
LENGTH: 417 words
DOCTORS HAVE been warned to severely restrict their use of a wakefulness
promoting drug with a history of abuse by students seeking to boost exam
performance because of new concerns about its safety.
In its latest Drug Safety newsletter, the Irish Medicines Board has advised
prescribers that the drug Modafinil must no longer be used to treat excessive
sleepiness associated with sleep apnoea (a condition where breathing stops
during sleep), chronic shift work sleep disorder and other causes of
hypersomnia.
Modafinil, which is marketed under the trade name Provigil, may now only be
prescribed for adults with excessive drowsiness due to narcolepsy.
Although never sanctioned by global drugs regulators for short-term use by
students preparing for exams or facing imminent project deadlines, there is some
evidence that Modafinil has been used in this way.
A 2009 survey of Cambridge University students found 10 per cent of students had
said they used performance-enhancing drugs to help them study.
In the US, it has been reported that up to 25 per cent of students at some US
universities have been purchasing drugs such as Ritalin and Provigil in an
effort to boost memory and concentration.
A recent systematic review by German doctors found Modafinil improved attention
for well-rested individuals, while maintaining wakefulness, memory and executive
functions to a significantly higher degree in sleep-deprived individuals than
did a placebo (dummy pill).
However, repeated doses of Modafinil appeared to induce overconfidence in a
person s own cognitive performance and the drug lost its potency as sleep
deprivation increased.
But the European Medicines Agency has carried out a safety review of the
wakefulness drug and concluded that the risk-benefit balance was positive only
for patients with the sleep disorder narcolepsy.
It has also expressly forbidden the use of Modafinil in people up to the age of
18 and in patients with uncontrolled high blood pressure.
It wants doctors to carry out an electrocardiogram of the heart before starting
the drug and it wants those prescribed Modafinil to have their blood pressure
and heart rate monitored regularly.
The IMB advises that the drug must be used with caution in patients with a
history of psychosis, depression or mania.
It also wants doctors to review the treatment of patients taking Modafinil at
their next routine appointment.
Modafinil should be withdrawn in patients who experience skin reactions or
psychiatric symptoms, the regulator says.
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The Irish Times
May 17, 2011 Tuesday
Waking up to the use and abuse of 'study drugs' in Irish colleges
BYLINE: LOUISE HOLDEN
SECTION: HEALTH; Your Health; Pg. 5
LENGTH: 833 words
Will Irish students follow their US counterparts by using neuro-enhancing drugs
in the run-up to exams?
STUDY DRUGS are an established feature of American campus life and there is
increasing evidence to suggest that pressured employees are using
neuro-enhancing drugs to improve performance in the workplace.
These drugs, which are prescribed to treat disorders such as ADHD and
narcolepsy, have also been found to increase concentration and energy for
specific tasks.
American children who grew up on drug treatments for disorders such as ADHD are
finding that when they reach third level, and beyond, their prescribed bottle of
Ritalin or Adderall is a prized commodity.
These drugs, as well as the narcolepsy treatment Modafinil, are now widely used
off-label in the US, especially by students hoping to boost their study
performance and employees seeking a competitive edge.
All through college I took Ritalin in the weeks coming up to my exams. I would
take a pill, stay up for 14 hours studying, then take another and sit the exam.
Then I d sleep. It was common practice on campus, a recent graduate of the
University of Mississippi told The Irish Times. This graduate would buy from
other students who got prescribed Ritalin to treat symptoms of ADHD and sold
them on for about $5 a pill.
Is there any evidence that these drugs are being used in Irish universities or
workplaces?
Dr Ciara Kelly, a GP in Co Wicklow, believes that while there is likely to be
some abuse of neuro-enhancing drugs in Ireland, it is on a very small scale. She
cautions against patients experimenting with these drugs.
In some users, Ritalin has been linked with anxiety, raised blood pressure and
palpitations. There are probably users who boost their concentration and energy
levels without any negative side effects, but for other users the effect could
be disastrous, she says.
Modafinil (often sold under the name Provigil) is another prescription drug that
has found favour among students looking for an academic edge.
Usually prescribed for people suffering from sleep apnoea or narcolepsy, the
drug is reported to help the user stay awake, and on task, for long periods an
obvious attraction for a hassled student counting down to exams.
The perception among some students is that these drugs are harmless, but this
week the Irish Medicines Board has issued a warning to GPs to severely restrict
the prescription of Modafinil/Provigil to adult sufferers of narcolepsy. The IMB
has warned that doctors should not prescribe the drug for excessive sleepiness,
due to concerns about its safety.
Both Modafinil and Ritalin/Adderall have been linked to increased blood
pressure. Doctors have this week been warned to carry out electrocardiograms on
patients prior to prescribing Modafinil.
Another cause of concern is the potential interaction between these drugs and
prescribed medications in users. Any substance that interferes with the binding
of other drugs to proteins in the blood could make prescribed drugs, such as the
contraceptive pill, less effective, says Orla Hardiman, consultant neurologist
at the Beaumont Hospital in Dublin.
However, she says that she has not come across incidents of off-label Ritalin or
Modafinil use in Ireland.
These drugs can cause seizures in students prone to epilepsy. If they were in
wide use here, I would expect to be treating seizures as result. I am not.
Dr Hardiman is not concerned about the issue in Ireland for the moment because,
she says, these drugs are not widely available here. These are controlled
substances and they are not easy to get, she says.
However, given the routine use of these drugs in the US, and growing concerns
about their impact in the UK, do we need to be watchful here?
Gary Redmond of the Union of Students in Ireland does not believe there is
widespread use of study drugs in Ireland, and has come across only a small
number of incidents here.
However, he is concerned about the level of stress that students are under, now
that the jobs market is so small. He worries that the new economic reality might
feed an appetite for drugs that are perceived to enhance academic performance.
A couple of years ago final year students already had jobs lined up before
graduating, says Redmond. Now they know they will be competing for a small
pool of jobs, and with many planning to emigrate, they will be competing with
the top students from international universities.
Students are under unprecedented pressure to get top grades.
Gary believes the best way to protect students against the creep of
drug-enhanced study is to reform assessment practices at both second and third
level.
Final terminal exams that account for a large proportion of the overall grade
are too stressful for students. This is an even bigger problem at Leaving Cert
level, where students are also at risk from these types of drugs. We need to
take a step back and look at new ways of assessing students that would make the
abuse of study drugs less attractive.
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Drug Industry Daily
May 2, 2011 Monday
EC Launches Pay-For-Delay Investigation into Cephalon, Teva Over Provigil
SECTION: Vol. 10 No. 86
LENGTH: 243 words
The European Commission (EC) has launched an informal investigation into a
potential pay-for-delay agreement between Cephalon and Teva Pharmaceutical
regarding the narcolepsy treatment Provigil.
The EC's ex officio investigation will examine a December 2005 patent dispute
settlement and additional side deals between the companies to see if it hindered
the entry of generic Provigil (modafinil) in Europe, which would breach an EU
regulation on restrictive business practices.
Under the settlement, Teva agreed to not sell generic modafinil before October
2012.
There has been no finding that Cephalon's actions were improper and the EC is
simply investigating, Natalie de Vane, a Cephalon spokeswoman, told DID.
Cephalon is also under investigation from the FTC for an alleged pay-for-delay
deal with Watson over Provigil (DID, Jan. 25).
But Cephalon views the settlement with Teva and its conduct as entirely proper
and intends to fully cooperate with the EC, de Vane said.
She also pointed out the EC is examining the impact of patent settlements on
competition.
The EC has requested copies of patent-settlement agreements from some
pharmaceutical companies to ensure generic medicines are not delayed from the
market (DID, Jan. 18).
The EC has become more forceful with pharmaceutical companies, such as raiding
them for pay-for-delay agreement information, instead of requesting copies of
such documents (DID, Dec. 6, 2010). -- Molly Cohen
Release date: May 2, 2011
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Europolitics (daily in English)
May 2, 2011 Monday
ANTI-TRUST POLICY : EU LAUNCHES PROBE INTO MODAFINIL DEAL
BYLINE: Eric van Puyvelde
SECTION: No. 4192
LENGTH: 289 words
An agreement between the American pharmaceutical company Cephalon and Teva, an
Israeli manufacturer of generic medicines, could prevent the arrival of the
generic product Modafinil on the European Economic Area (EEA) market. On April
28, the European Commission opened an inquiry into this agreement, based on EU
rules relating to restrictive commercial practises (Article 101). Modafinil is a
medication used in the treatment of sleep problems.
In December 2005, Cephalon and Teva resolved litigation relating to patents in
the United Kingdom and the United States concerning Modafinil (commercial brand
name Provigil®) via a friendly agreement, which saw Teva agreeing not to sell
its product Modafinil on the EEA market before October 2012. A series of
accessory agreements was included in the friendly accord, which is also the
subject of a litigation procedure by the United States' anti-trust authority,
the FTC, for abuse of a leading position on the market.
In the last few years, the European Commission has been leading a drive against
pharmaceutical laboratories suspected of impeding the arrival on the EU market
of generic and less expensive versions of their star' medicines. In 2008 and
2009, the Commission carried out a huge inquiry into the sector, which resulted
in the launch of legal proceedings against several companies: in July 2009,
against the French company Servier, and a series of manufacturers of generic
medicines, including Teva, suspected of working together to delay the
commercialisation of certain generic medicines, and in January 2010 against the
Danish group Lundbeck. In December 2010, the Commission carried out further
inquiries into the sector, notably into the British company AstraZeneca.
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PharmaGossip
April 29, 2011 Friday 11:05 AM EST
Antitrust: Commission opens investigation against pharmaceutical companies
Cephalon and Teva
BYLINE: insider
LENGTH: 744 words
Apr. 29, 2011 (PharmaGossip delivered by Newstex) --
IP/11/511
Brussels, 28 April 2011
Antitrust: Commission opens investigation against pharmaceutical companies
Cephalon and Teva
The European Commission has opened a formal antitrust investigation to assess
whether an agreement between US-based pharmaceutical company Cephalon and
Israel-based generic drugs firm Teva may have had the object or effect of
hindering the entry of generic Modafinil in the European Economic Area.
Modafinil is a medicine used for the treatment of certain types of sleeping
disorders. The opening of proceedings does not mean that the Commission has
conclusive proof of an infringement, only that it will investigate the case as a
matter of priority.
The Commission has started an ex officio investigation to assess an agreement
between Cephalon, Inc. (NASDAQ:CEPH) and Teva Pharmaceutical Industries Ltd.
(NASDAQ:TEVA) that may have the object or effect of hindering the entry of
generic Modafinil products in the markets of the European Economic Area. In
particular it is assessed whether the agreement is in breach of the EU Treaty's
rules on restrictive business practices (Article 101).
In December 2005 Cephalon and Teva settled patent infringement disputes in the
United Kingdom and the United States concerning Modafinil (brand name
Provigil®). As part of the settlement agreement Teva undertook not to sell its
generic Modafinil products in the EEA markets before October 2012. A series of
side deals were included into the settlement agreement, which is also subject to
antitrust litigation in the United States initiated by the US antitrust
authority FTC.
The opening of proceedings does not mean that the Commission has a definitive
finding of an infringement, but indicates that it will investigate the case as a
matter of priority.
There is no legal deadline to complete inquiries into anticompetitive conduct.
Their duration depends on a number of factors, including the complexity of each
case, the extent to which the undertakings concerned co-operate with the
Commission and the exercise of the rights of defence.
Background to antitrust investigations
Article 101 of the Treaty on the Functioning of the EU prohibits agreements and
concerted practices which may affect trade and prevent or restrict competition.
The implementation of this provision is defined in the Antitrust Regulation
(Council Regulation No 1/2003) which can be applied by the Commission and by the
national competition authorities of EU Member States.
Article 11(6) of the Antitrust Regulation provides that the initiation of
proceedings by the Commission relieves the competition authorities of the Member
States of their competence to also apply Articles 101 and 102 (ban on abuse of a
dominant market position) to the practices concerned. Article 16(1) provides
that national courts must avoid giving decisions which would conflict with a
decision contemplated by the Commission in proceedings that it has initiated.
The Commission has informed the parties and the competition authorities of the
Member States, that it has opened proceedings in this case.
Background on investigation of the pharma sector
In 2008 and 2009 the Commission carried out a broad inquiry of the
pharmaceutical sector. Among others, the inquiry pointed to significant risks
for European consumers stemming from certain types of patent settlements between
originator and generic companies aimed at delaying the arrival into the market
of cheaper generic medicines (sometimes also referred to as "pay-for-delay"
settlements). The Commission regularly monitors potentially problematic patent
settlements. The second such monitoring exercise was launched in January and the
results are expected before the summer break (see IP/10/887 and IP/11/40).
The Commission has a number of ongoing individual investigations into suspected
anti-competitive practice. In July 2010, the Commission took warmth from the
confirmation, by the General Court, of the Commission's decision in the
AstraZeneca case, which was its first abuse decision in the pharmaceutical
sector. The company had misused the regulatory framework to prevent or, in the
very least, delay the market entry of competing generic products, something that
has now clearly been ruled as illegal. AstraZeneca (NYSE:AZN) has appealed the
decision of the General Court.
via europa.eu
Posted via email from Jack's posterous
Newstex ID: PHAG-0001-103327812
LOAD-DATE: April 29, 2011
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not necessarily
the views of Newstex or its re-distributors. Posts from such authors are
provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs on Demand® are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs on Demand® is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs on Demand® shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs on Demand®. Reader's comments reflect their
individual opinion and their publication within Blogs on Demand® shall not infer
or connote an endorsement by Newstex or its re-distributors of such reader's
comments or views. Newstex and its re-distributors expressly reserve the right
to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2011 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2011 PharmaGossip
44 of 998 DOCUMENTS
Agence France Presse -- English
April 28, 2011 Thursday 3:38 PM GMT
EU opens anti-trust probe into stay-awake drug deal
LENGTH: 346 words
DATELINE: BRUSSELS, April 28 2011
European antitrust authorities announced Thursday the opening of a formal
antitrust probe into US drugs company Cephalon and Israel-based generic drugs
firm Teva over stay-awake drug Modafinil.
The controversial anti-tiredness drug, marketed under the brand-name Provigil,
can keep people awake for days and is normally used to treat the rare sleeping
disorder narcolepsy. But it became popular among night-workers such as truckers
and was even tested in its early days for military use.
The probe concerns a deal struck between the two that "may have had the object
or effect of hindering the entry of generic Modafinil" into the European
Economic Area.
The European Commission "has started an ex officio investigation to assess an
agreement between Cephalon, Inc. and Teva Pharmaceutical Industries Ltd.," a
statement said.
A probe does not indicate "a definitive finding of an infringement," it
stressed, but means it will be investigated as "a matter of priority," although
there is no set deadline for an outcome.
The case arises from a December 2005 deal to settle patent infringement disputes
in Britain and the United States, which saw Teva undertake not to sell its
generic Modafinil products in the European single market before October 2012.
Side deals are also under investigation by US antitrust authorities.
The EU has been probing the sector repeatedly since a report showed that the
number of new drugs reaching the market annually had dropped by over a third
since 2000 and that people were being deprived of innovative, affordable and
safe medicine.
Generic drugs are far cheaper -- the report said they cost on average 40 percent
less two years after they enter the market -- and save patients and insurance
firms money without compromising on effectiveness.
Among initial tactics often used to hold up generic entry, drug developers were
found to file multiple patent applications for the same medicine, leaving little
scope for generics to be developed.
In the worst example uncovered, 1,300 separate filings were made for a single
medicine across the 27-nation EU.
LOAD-DATE: April 29, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Agence France Presse
All Rights Reserved
45 of 998 DOCUMENTS
Kuwait News Agency (KUNA)
April 28, 2011 Thursday
EU probes US, Israeli firms for preventing entry of cheap generic drugs to
LENGTH: 212 words
The European Commission opened Thursday a
formal investigation to assess whether an agreement between US-based
pharmaceutical company Cephalon and Israel-based generic drugs firm Teva may
have had the object or effect of hindering the entry of generic Modafinil in
the European market.
Modafinil is a medicine used for the treatment of certain types of sleeping
disorders.
In particular the probe will assess whether the agreement is in breach of
the EU competition rules, said the EU's executive body in a statement.
In December 2005, Cephalon and Teva settled patent infringement disputes in
the United Kingdom and the United States concerning Modafinil (brand name
Provigil).
As part of the settlement agreement Teva undertook not to sell its generic
Modafinil products in the European markets before October 2012.
EU rules prohibit agreements and practices which may affect trade and
prevent or restrict competition.
In 2008 and 2009, the European Commission carried out a broad inquiry of
the pharmaceutical sector. Among others, the inquiry pointed to significant
risks for European consumers stemming from certain types of patent settlements
between originator and generic companies aimed at delaying the arrival into
the market of cheaper generic medicines.
LOAD-DATE: May 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
JOURNAL-CODE: 365
Copyright 2011 KUNA.
All Rights Reserved
Syndigate.info, Al Bawaba.com
46 of 998 DOCUMENTS
M2 PressWIRE
April 28, 2011 Thursday
Antitrust: Commission opens investigation against pharmaceutical companies
Cephalon and Teva
LENGTH: 696 words
April 28, 2011
Brussels --The European Commission has opened a formal antitrust investigation
to assess whether an agreement between US-based pharmaceutical company Cephalon
and Israel-based generic drugs firm Teva may have had the object or effect of
hindering the entry of generic Modafinil in the European Economic Area.
Modafinil is a medicine used for the treatment of certain types of sleeping
disorders. The opening of proceedings does not mean that the Commission has
conclusive proof of an infringement, only that it will investigate the case as a
matter of priority.
The Commission has started an ex officio investigation to assess an agreement
between Cephalon, Inc. and Teva Pharmaceutical Industries Ltd. that may have the
object or effect of hindering the entry of generic Modafinil products in the
markets of the European Economic Area. In particular it is assessed whether the
agreement is in breach of the EU Treaty's rules on restrictive business
practices (Article 101).
In December 2005 Cephalon and Teva settled patent infringement disputes in the
United Kingdom and the United States concerning Modafinil (brand name
Provigil®). As part of the settlement agreement Teva undertook not to sell its
generic Modafinil products in the EEA markets before October 2012. A series of
side deals were included into the settlement agreement, which is also subject to
antitrust litigation in the United States initiated by the US antitrust
authority FTC.
The opening of proceedings does not mean that the Commission has a definitive
finding of an infringement, but indicates that it will investigate the case as a
matter of priority.
There is no legal deadline to complete inquiries into anticompetitive conduct.
Their duration depends on a number of factors, including the complexity of each
case, the extent to which the undertakings concerned co-operate with the
Commission and the exercise of the rights of defence.
Background to antitrust investigations
Article 101 of the Treaty on the Functioning of the EU prohibits agreements and
concerted practices which may affect trade and prevent or restrict competition.
The implementation of this provision is defined in the Antitrust Regulation
(Council Regulation No 1/2003) which can be applied by the Commission and by the
national competition authorities of EU Member States.
Article 11(6) of the Antitrust Regulation provides that the initiation of
proceedings by the Commission relieves the competition authorities of the Member
States of their competence to also apply Articles 101 and 102 (ban on abuse of a
dominant market position) to the practices concerned. Article 16(1) provides
that national courts must avoid giving decisions which would conflict with a
decision contemplated by the Commission in proceedings that it has initiated.
The Commission has informed the parties and the competition authorities of the
Member States, that it has opened proceedings in this case.
Background on investigation of the pharma sector
In 2008 and 2009 the Commission carried out a broad inquiry of the
pharmaceutical sector. Among others, the inquiry pointed to significant risks
for European consumers stemming from certain types of patent settlements between
originator and generic companies aimed at delaying the arrival into the market
of cheaper generic medicines (sometimes also referred to as "pay-for-delay"
settlements). The Commission regularly monitors potentially problematic patent
settlements. The second such monitoring exercise was launched in January and the
results are expected before the summer break (see IP/10/887 and IP/11/40).
The Commission has a number of ongoing individual investigations into suspected
anti-competitive practice. In July 2010, the Commission took warmth from the
confirmation, by the General Court, of the Commission's decision in the
AstraZeneca case, which was its first abuse decision in the pharmaceutical
sector. The company had misused the regulatory framework to prevent or, in the
very least, delay the market entry of competing generic products, something that
has now clearly been ruled as illegal. AstraZeneca has appealed the decision of
the General Court.
LOAD-DATE: April 28, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
JOURNAL-CODE: M2PW
Copyright 2011 Normans Media Limited
All Rights Reserved
47 of 998 DOCUMENTS
States News Service
April 28, 2011 Thursday
ANTITRUST: COMMISSION OPENS INVESTIGATION AGAINST PHARMACEUTICAL COMPANIES
CEPHALON AND TEVA
BYLINE: States News Service
LENGTH: 699 words
DATELINE: BRUSSELS
The following information was released by the European Union:
The European Commission has opened a formal antitrust investigation to assess
whether an agreement between US-based pharmaceutical company Cephalon and
Israel-based generic drugs firm Teva may have had the object or effect of
hindering the entry of generic Modafinil in the European Economic Area.
Modafinil is a medicine used for the treatment of certain types of sleeping
disorders. The opening of proceedings does not mean that the Commission has
conclusive proof of an infringement, only that it will investigate the case as a
matter of priority.
The Commission has started an ex officio investigation to assess an agreement
between Cephalon, Inc. and Teva Pharmaceutical Industries Ltd. that may have the
object or effect of hindering the entry of generic Modafinil products in the
markets of the European Economic Area. In particular it is assessed whether the
agreement is in breach of the EU Treaty's rules on restrictive business
practices (Article 101).
In December 2005 Cephalon and Teva settled patent infringement disputes in the
United Kingdom and the United States concerning Modafinil (brand name Provigil).
As part of the settlement agreement Teva undertook not to sell its generic
Modafinil products in the EEA markets before October 2012. A series of side
deals were included into the settlement agreement, which is also subject to
antitrust litigation in the United States initiated by the US antitrust
authority FTC.
The opening of proceedings does not mean that the Commission has a definitive
finding of an infringement, but indicates that it will investigate the case as a
matter of priority.
There is no legal deadline to complete inquiries into anticompetitive conduct.
Their duration depends on a number of factors, including the complexity of each
case, the extent to which the undertakings concerned co-operate with the
Commission and the exercise of the rights of defence.
Background to antitrust investigations
Article 101 of the Treaty on the Functioning of the EU prohibits agreements and
concerted practices which may affect trade and prevent or restrict competition.
The implementation of this provision is defined in the Antitrust Regulation
(Council Regulation No 1/2003) which can be applied by the Commission and by the
national competition authorities of EU Member States.
Article 11(6) of the Antitrust Regulation provides that the initiation of
proceedings by the Commission relieves the competition authorities of the Member
States of their competence to also apply Articles 101 and 102 (ban on abuse of a
dominant market position) to the practices concerned. Article 16(1) provides
that national courts must avoid giving decisions which would conflict with a
decision contemplated by the Commission in proceedings that it has initiated.
The Commission has informed the parties and the competition authorities of the
Member States, that it has opened proceedings in this case.
Background on investigation of the pharma sector
In 2008 and 2009 the Commission carried out a broad inquiry of the
pharmaceutical sector. Among others, the inquiry pointed to significant risks
for European consumers stemming from certain types of patent settlements between
originator and generic companies aimed at delaying the arrival into the market
of cheaper generic medicines (sometimes also referred to as "pay-for-delay"
settlements). The Commission regularly monitors potentially problematic patent
settlements. The second such monitoring exercise was launched in January and the
results are expected before the summer break (see IP/10/887 and IP/11/40).
The Commission has a number of ongoing individual investigations into suspected
anti-competitive practice. In July 2010, the Commission took warmth from the
confirmation, by the General Court, of the Commission's decision in the
AstraZeneca case, which was its first abuse decision in the pharmaceutical
sector. The company had misused the regulatory framework to prevent or, in the
very least, delay the market entry of competing generic products, something that
has now clearly been ruled as illegal. AstraZeneca has appealed the decision of
the General Court.
LOAD-DATE: April 28, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 States News Service
48 of 998 DOCUMENTS
Xinhua General News Service
April 28, 2011 Thursday 4:27 PM EST
EU launches antitrust probe into Cephalon, Teva
SECTION: WORLD NEWS; Political
LENGTH: 162 words
DATELINE: BRUSSELS April 28
The European Union (EU) antitrust regulator said on Thursday it had launched a
probe into pharmaceutical companies Cephalon and Teva for possible collusion
to keep a generic drug out of the EU market.
The U.S.-based Cephalon and Israel-based Teva, the two leading generic drugs
makers in the world, in December 2005 settled patent infringement disputes in
Britain and the United States concerning Modafinil, a sleep-disorder drug with
brand name Provigil.
As part of the settlement agreement Teva undertook not to sell its generic
Modafinil products in European markets before October 2012.
The investigation is to assess whether the agreement "may have had the object
or effect of hindering the entry of generic Modafinil," the European Commission
said.
The commission said the opening of proceedings does not mean that it has a
definitive finding of an infringement, but indicates that it will investigate
the case as a matter of priority.
LOAD-DATE: April 29, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Xinhua News Agency
49 of 998 DOCUMENTS
Xinhua General News Service
April 28, 2011 Thursday 1:20 AM EST
EU launches antitrust probe into Cephalon, Teva
SECTION: WORLD NEWS; Political
LENGTH: 162 words
DATELINE: BRUSSELS April 28
The European Union (EU) antitrust regulator said on Thursday it had launched a
probe into pharmaceutical companies Cephalon and Teva for possible collusion
to keep a generic drug out of the EU market.
The U.S.-based Cephalon and Israel-based Teva, the two leading generic drugs
makers in the world, in December 2005 settled patent infringement disputes in
Britain and the United States concerning Modafinil, a sleep-disorder drug with
brand name Provigil.
As part of the settlement agreement Teva undertook not to sell its generic
Modafinil products in European markets before October 2012.
The investigation is to assess whether the agreement "may have had the object
or effect of hindering the entry of generic Modafinil," the European Commission
said.
The commission said the opening of proceedings does not mean that it has a
definitive finding of an infringement, but indicates that it will investigate
the case as a matter of priority.
LOAD-DATE: April 30, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Xinhua News Agency
50 of 998 DOCUMENTS
The Pharmaceutical Journal
February 23, 2011 Wednesday
Modafinil's indications restricted
LENGTH: 256 words
Modafinil (Provigil) has had its licensed indications restricted and can now
only be used to treat excessive sleepiness in adult patients with narcolepsy.
The drug is no longer licensed for treatment of excessive sleepiness associated
with obstructive sleep apnoea/hypopnoea syndrome and moderate to severe chronic
shift work sleep disorder.
The move follows an assessment by the European Medicines Agency's Committee for
Medicinal Products for Human Use (CHMP), which has concluded that the
benefit/risk profile for modafinil is no longer favourable for these conditions.
Cephalon (UK) Ltd, the company that markets Provigil, has written to healthcare
professionals in the UK advising them of the change.
In its letter the company explains that safety concerns, including psychiatric
and serious skin reactions and the potential for cardiovascular adverse effects
are now considered to outweigh the limited benefits of modafinil in obstructive
sleep apnoea and chronic shift work sleep disorder.
As well as restricting modafinil's indications, the CHMP has concluded that it
should not be used by children, pregnant or lactating women or by patients with
uncontrolled hypertension or cardiac arrhythmias. It also recommends that the
starting daily dose is 200mg and that the drug is used with caution in patients
with a history of psychosis, depression or mania, or substance abuse.
Cephalon says there is no need for patients to stop treatment immediately but
that they should have their treatment reviewed at their next routine
appointment.
LOAD-DATE: February 23, 2011 Wednesday
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Journal
Copyright 2011 PJ Online
All Rights Reserved
51 of 998 DOCUMENTS
The Associated Press
February 18, 2011 Friday 01:58 PM GMT
Turkish team to sue lab for Taurasi doping report
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 462 words
DATELINE: ANKARA, Turkey
Diana Taurasi's Turkish club demanded an apology Friday and the resignation of
the directors of the doping lab that issued an apparent "false positive" report
on the American basketball player.
Fenerbahce also said it would take legal action.
Sekip Mosturoglu, a member of Fenerbahce's executive board, accused the
Ankara-based lab of "inadequacies" and said its report declaring Taurasi's "A"
and "B" samples positive for the banned stimulant modafinil had sullied both the
reputation of both the WNBA star and Fenerbahce.
"This is the greatest scandal in world sports," Mosturoglu said. "They cannot
get away with simple apologies."
Fenerbahce terminated Taurasi's contract after she tested positive following a
Nov. 13 league game. The Turkish Basketball Federation subsequently suspended
her from play but lifted the suspension Wednesday.
Mosturoglu said Taurasi's absence had put Fenerbahce's chances to win the
Euroleague at "risk."
He also faulted some Turkish Basketball Federation officials for refusing to
allow Taurasi's "B" sample to be tested at another lab and demanded their
resignations, too.
"Our club will take every kind of legal action to the compensation of our
losses," Mosturoglu said.
Taurasi insisted all along that she never used performance-enhancing drugs. The
28-year-old American will be able to compete at the 2012 Olympics now that she
has been cleared of the doping charges.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Mosturoglu said Fenerbahce would work hard to convince Taurasi and teammate
Penny Taylor to return. Taylor left Fenerbahce in a show of solidarity with
Taurasi.
But Taurasi, who plans to return to the WNBA when the season begins in June,
told The Associated Press on Wednesday that her return to the Turkish league was
"pretty unlikely."
Nevertheless, thousands of Turkish fans urged the star to come back, posting
messages on the specially-created comebackdiana.com website.
The World Anti-Doping Agency, which can suspend or revoke the accreditation for
doping labs, said it has asked the lab to explain why it declared Taurasi
positive for modafinil. WADA, which has 35 accredited labs worldwide, previously
suspended the Ankara facility for three months in 2009 for failing to meet
international standards.
Mosturoglu said the lab had accepted its mistake only after an international
drug-testing expert looking into the Taurasi case pointed out the lab's error.
The federation this week also lifted the provisional suspension for American
player Monique Coker, who plays for Ceyhan Belediyesi and had tested positive
for modafinil in tests carried out at the same lab.
Associated Press Writer Selcan Hacaoglu contributed to this report.
LOAD-DATE: February 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
52 of 998 DOCUMENTS
Associated Press Worldstream
February 18, 2011 Friday 1:51 PM GMT
Fenerbahce to sue lab for Taurasi doping report
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 469 words
DATELINE: ANKARA Turkey
Diana Taurasi's Turkish club demanded an apology Friday and the resignation of
the directors of the local doping lab that issued an apparent "false positive"
report on the American basketball player.
Fenerbahce also said it would take legal action against those responsible.
Sekip Mosturoglu, a member of Fenerbahce's executive board, accused the
Ankara-based lab of "inadequacies" and said its report declaring Taurasi's "A"
and "B" samples positive for the banned stimulant modafinil had sullied both the
reputation of both the WNBA star and Fenerbahce.
"This is the greatest scandal in world sports," Mosturoglu said. "They cannot
get away with simple apologies."
Fenerbahce terminated Taurasi's contract after she tested positive following a
Nov. 13 league game. The Turkish Basketball Federation subsequently suspended
her from play but lifted the suspension Wednesday.
Mosturoglu said Taurasi's absence had put Fenerbahce's chances to win the
Euroleague at "risk."
He also faulted some Turkish Basketball Federation officials for refusing to
allow Taurasi's "B" sample to be tested at another lab and demanded their
resignations, too.
"Our club will take every kind of legal action to the compensation of our
losses," Mosturoglu said.
Taurasi insisted all along that she never used performance-enhancing drugs. The
28-year-old American will be able to compete at the 2012 Olympics now that she
has been cleared of the doping charges.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Mosturoglu said Fenerbahce would work hard to convince Taurasi and teammate
Penny Taylor to return. Taylor left Fenerbahce in a show of solidarity with
Taurasi.
But Taurasi, who plans to return to the WNBA when the season begins in June,
told The Associated Press on Wednesday that her return to the Turkish league was
"pretty unlikely."
Nevertheless, thousands of Turkish fans urged the star to come back, posting
messages on the specially-created comebackdiana.com website.
The World Anti-Doping Agency, which can suspend or revoke the accreditation for
doping labs, said it has asked the Ankara lab to explain why it declared Taurasi
positive for modafinil. WADA, which has 35 accredited labs worldwide, previously
suspended the Ankara facility for three months in 2009 for failing to meet
international standards.
Mosturoglu said the lab had accepted its mistake only after an international
drug-testing expert looking into the Taurasi case pointed out the lab's error.
The federation this week also lifted the provisional suspension for American
player Monique Coker, who plays for Ceyhan Belediyesi and had tested positive
for modafinil in tests carried out at the same lab.
Associated Press writer Selcan Hacaoglu contributed to this report.
LOAD-DATE: February 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
53 of 998 DOCUMENTS
Associated Press Online
February 18, 2011 Friday 1:58 PM GMT
Turkish team to sue lab for Taurasi doping report
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 462 words
DATELINE: ANKARA Turkey
Diana Taurasi's Turkish club demanded an apology Friday and the resignation of
the directors of the doping lab that issued an apparent "false positive" report
on the American basketball player.
Fenerbahce also said it would take legal action.
Sekip Mosturoglu, a member of Fenerbahce's executive board, accused the
Ankara-based lab of "inadequacies" and said its report declaring Taurasi's "A"
and "B" samples positive for the banned stimulant modafinil had sullied both the
reputation of both the WNBA star and Fenerbahce.
"This is the greatest scandal in world sports," Mosturoglu said. "They cannot
get away with simple apologies."
Fenerbahce terminated Taurasi's contract after she tested positive following a
Nov. 13 league game. The Turkish Basketball Federation subsequently suspended
her from play but lifted the suspension Wednesday.
Mosturoglu said Taurasi's absence had put Fenerbahce's chances to win the
Euroleague at "risk."
He also faulted some Turkish Basketball Federation officials for refusing to
allow Taurasi's "B" sample to be tested at another lab and demanded their
resignations, too.
"Our club will take every kind of legal action to the compensation of our
losses," Mosturoglu said.
Taurasi insisted all along that she never used performance-enhancing drugs. The
28-year-old American will be able to compete at the 2012 Olympics now that she
has been cleared of the doping charges.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Mosturoglu said Fenerbahce would work hard to convince Taurasi and teammate
Penny Taylor to return. Taylor left Fenerbahce in a show of solidarity with
Taurasi.
But Taurasi, who plans to return to the WNBA when the season begins in June,
told The Associated Press on Wednesday that her return to the Turkish league was
"pretty unlikely."
Nevertheless, thousands of Turkish fans urged the star to come back, posting
messages on the specially-created comebackdiana.com website.
The World Anti-Doping Agency, which can suspend or revoke the accreditation for
doping labs, said it has asked the lab to explain why it declared Taurasi
positive for modafinil. WADA, which has 35 accredited labs worldwide, previously
suspended the Ankara facility for three months in 2009 for failing to meet
international standards.
Mosturoglu said the lab had accepted its mistake only after an international
drug-testing expert looking into the Taurasi case pointed out the lab's error.
The federation this week also lifted the provisional suspension for American
player Monique Coker, who plays for Ceyhan Belediyesi and had tested positive
for modafinil in tests carried out at the same lab.
Associated Press Writer Selcan Hacaoglu contributed to this report.
LOAD-DATE: February 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
54 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 18, 2011 Friday 1:58 PM GMT
Turkish team to sue lab for Taurasi doping report
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 462 words
DATELINE: ANKARA Turkey
Diana Taurasi's Turkish club demanded an apology Friday and the resignation of
the directors of the doping lab that issued an apparent "false positive" report
on the American basketball player.
Fenerbahce also said it would take legal action.
Sekip Mosturoglu, a member of Fenerbahce's executive board, accused the
Ankara-based lab of "inadequacies" and said its report declaring Taurasi's "A"
and "B" samples positive for the banned stimulant modafinil had sullied both the
reputation of both the WNBA star and Fenerbahce.
"This is the greatest scandal in world sports," Mosturoglu said. "They cannot
get away with simple apologies."
Fenerbahce terminated Taurasi's contract after she tested positive following a
Nov. 13 league game. The Turkish Basketball Federation subsequently suspended
her from play but lifted the suspension Wednesday.
Mosturoglu said Taurasi's absence had put Fenerbahce's chances to win the
Euroleague at "risk."
He also faulted some Turkish Basketball Federation officials for refusing to
allow Taurasi's "B" sample to be tested at another lab and demanded their
resignations, too.
"Our club will take every kind of legal action to the compensation of our
losses," Mosturoglu said.
Taurasi insisted all along that she never used performance-enhancing drugs. The
28-year-old American will be able to compete at the 2012 Olympics now that she
has been cleared of the doping charges.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Mosturoglu said Fenerbahce would work hard to convince Taurasi and teammate
Penny Taylor to return. Taylor left Fenerbahce in a show of solidarity with
Taurasi.
But Taurasi, who plans to return to the WNBA when the season begins in June,
told The Associated Press on Wednesday that her return to the Turkish league was
"pretty unlikely."
Nevertheless, thousands of Turkish fans urged the star to come back, posting
messages on the specially-created comebackdiana.com website.
The World Anti-Doping Agency, which can suspend or revoke the accreditation for
doping labs, said it has asked the lab to explain why it declared Taurasi
positive for modafinil. WADA, which has 35 accredited labs worldwide, previously
suspended the Ankara facility for three months in 2009 for failing to meet
international standards.
Mosturoglu said the lab had accepted its mistake only after an international
drug-testing expert looking into the Taurasi case pointed out the lab's error.
The federation this week also lifted the provisional suspension for American
player Monique Coker, who plays for Ceyhan Belediyesi and had tested positive
for modafinil in tests carried out at the same lab.
Associated Press Writer Selcan Hacaoglu contributed to this report.
LOAD-DATE: February 19, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
55 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 18, 2011 Friday 1:58 PM GMT
LENGTH: 507 words
BC-BKL--Doping-Taurasi, 1st Ld-Writethru,0657
Turkish team to sue lab for Taurasi doping report
2030
Eds: Updates with details; adds byline.
AP Photo NY150, NY161
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By SUZAN FRASER
Associated Press
ANKARA, Turkey (AP) Diana Taurasi's Turkish club demanded an apology Friday and
the resignation of the directors of the doping lab that issued an apparent
"false positive" report on the American basketball player.
Fenerbahce also said it would take legal action.
Sekip Mosturoglu, a member of Fenerbahce's executive board, accused the
Ankara-based lab of "inadequacies" and said its report declaring Taurasi's "A"
and "B" samples positive for the banned stimulant modafinil had sullied both the
reputation of both the WNBA star and Fenerbahce.
"This is the greatest scandal in world sports," Mosturoglu said. "They cannot
get away with simple apologies."
Fenerbahce terminated Taurasi's contract after she tested positive following a
Nov. 13 league game. The Turkish Basketball Federation subsequently suspended
her from play but lifted the suspension Wednesday.
Mosturoglu said Taurasi's absence had put Fenerbahce's chances to win the
Euroleague at "risk."
He also faulted some Turkish Basketball Federation officials for refusing to
allow Taurasi's "B" sample to be tested at another lab and demanded their
resignations, too.
"Our club will take every kind of legal action to the compensation of our
losses," Mosturoglu said.
Taurasi insisted all along that she never used performance-enhancing drugs. The
28-year-old American will be able to compete at the 2012 Olympics now that she
has been cleared of the doping charges.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Mosturoglu said Fenerbahce would work hard to convince Taurasi and teammate
Penny Taylor to return. Taylor left Fenerbahce in a show of solidarity with
Taurasi.
But Taurasi, who plans to return to the WNBA when the season begins in June,
told The Associated Press on Wednesday that her return to the Turkish league was
"pretty unlikely."
Nevertheless, thousands of Turkish fans urged the star to come back, posting
messages on the specially-created comebackdiana.com website.
The World Anti-Doping Agency, which can suspend or revoke the accreditation for
doping labs, said it has asked the lab to explain why it declared Taurasi
positive for modafinil. WADA, which has 35 accredited labs worldwide, previously
suspended the Ankara facility for three months in 2009 for failing to meet
international standards.
Mosturoglu said the lab had accepted its mistake only after an international
drug-testing expert looking into the Taurasi case pointed out the lab's error.
The federation this week also lifted the provisional suspension for American
player Monique Coker, who plays for Ceyhan Belediyesi and had tested positive
for modafinil in tests carried out at the same lab.
Associated Press Writer Selcan Hacaoglu contributed to this report.
LOAD-DATE: February 19, 2011
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PUBLICATION-TYPE: Newswire
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The Associated Press
February 17, 2011 Thursday 05:48 PM GMT
WADA could suspend Turkish lab in Taurasi case
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: SPORTS NEWS
LENGTH: 732 words
DATELINE: LONDON
The World Anti-Doping Agency could suspend the Turkish drug-testing laboratory
that reported an apparent "false positive" for American basketball star Diana
Taurasi.
WADA director general David Howman told The Associated Press on Thursday the
agency has asked the Ankara lab to explain why it declared Taurasi's samples
positive for the banned stimulant modafinil, a decision which led to her
contract being terminated by her Turkish club.
"We are still awaiting all the information from the laboratory," Howman said.
"It appears that it was a false positive. In any of those cases we need to
review all the data to determine whether any steps need to be taken, including
any steps against the laboratory."
WADA can suspend and revoke the accreditation of doping labs. WADA, which has 35
accredited labs worldwide, previously suspended the Ankara center for three
months in 2009 for failing to meet international standards.
"Anything which goes wrong has to be a worry," Howman said. "That's why we have
to investigate it pretty thoroughly. The reputation of the athlete who's been
aggrieved is pretty important, too, and that has to be acknowledged."
The Turkish lab reported that Taurasi's "A" and "B" samples both tested positive
for modafinil following a Turkish league game on Nov. 13. Her club, Fenerbahce,
terminated her contract last month and she was suspended by the Turkish
Basketball Federation.
The federation lifted the suspension Wednesday, saying the lab retracted its
positive finding after it "evaluated" Taurasi's statements in her defense.
The federation also lifted the provisional suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in tests carried out by the same lab.
False positives are rare in international drug testing.
"We have more of an issue with false negatives," Howman said.
The WADA-accredited lab in Malaysia was suspended for false positives last year.
The lab is appealing the decision to the Court of Arbitration for Sport.
"There is a process that has to be followed, including the gathering of all the
data," Howman said in a telephone interview from Montreal. "If it's sufficiently
bad, then the lab should go to a disciplinary panel and have a hearing. They've
got a right to put every excuse and reasoning before the panel."
Taurasi insisted all along that she never used performance-enhancing drugs.
"It's really good that the facts came out and the truth came out," Taurasi told
the AP on Wednesday. "Life can throw you curveballs at any given time. I can be
mad and angry, but I will move forward."
The 28-year-old Taurasi intends to return to the WNBA when the season begins in
June. The Mercury guard has led the U.S. league in scoring the last four
seasons. She is also now eligible to compete for the U.S. at the 2012 London
Olympics.
The Turkish Doping Control Center at the Hacettepe University declined to
comment on the case Thursday. But the HaberTurk newspaper quoted Ugur Erdener,
dean of the university, as admitting the lab made a mistake.
"There are two evaluations to analyze the test results and the average of them
is taken. The (lab) officials' evaluation was based on one data. However, the
average should have been taken as the base," Erdener was quoted as saying.
Fenerbahce President Aziz Yildirim met Turkey's Prime Minister Recep Tayyip
Erdogan to discuss the case Thursday. No statement was made after the meeting
but Ali Koc, a club official, denied reports that Fenerbahce asked authorities
to shut down the doping lab.
Turgay Demirel, president of the Turkish Basketball Federation, said two soccer
players were also cleared of doping after the lab retracted its reports about
them.
"It is very sad for our country that an institution accredited to WADA committed
such a huge mistake," he said. "Both Turkey, Turkish sports and Turkish
basketball could pay a fairly high price for this. Sportsmen and federations or
clubs in their countries and even us could file compensation suits against this
institution."
Demirel said about 3,500 doping tests have been carried out annually in Turkey,
with most analyzed by the Ankara lab.
"From now on, I don't think the certificate of Hacettepe University can remain
valid," Demirel said. "But we will have to use centers in Lisbon, Cologne or
maybe Athens."
Associated Press writer Selcan Hacaoglu in Ankara contributed to this report.
LOAD-DATE: February 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
57 of 998 DOCUMENTS
The Houston Chronicle
February 17, 2011 Thursday
3 STAR EDITION
Taurasi cleared of doping charge WNBA star will be eligible for 2012 Games
BYLINE: CHRONICLE NEWS SERVICES
SECTION: SPORTS; Pg. 2
LENGTH: 330 words
Diana Taurasi was always confident she would be cleared of doping allegations.
It finally happened on Wednesday.
Taurasi had her provisional suspension lifted by the Turkish Basketball
Federation, which said the lab that returned a positive test retracted its
report after it "evaluated" Taurasi's statements in her defense. The federation
did not say whether the lab made a mistake.
"I got the news this morning at 5 a.m. and was in shock," Taurasi told the
Associated Press by phone from her Phoenix home. "It was kind of like the first
time when I heard the test result had come back positive. It's really good that
the facts came out and the truth came out."
Taurasi had insisted that she never used performance-enhancing drugs, even
though she had her contract terminated by Turkish club Fenerbahce last month.
The lab that tested her sample said the results came back positive for the
stimulant modafinil.
"Life can throw you curveballs at any given time," said Taurasi, who will also
be able to compete in the 2012 Olympics. "I can be mad and angry, but I will
move forward ."
With the lifting of the suspension, Taurasi is free to continue playing in the
Turkish basketball league, although she doesn't plan on going back there.
"That's pretty unlikely," the 28-year-old WNBA star said. "I'm here in Phoenix
working out and am more focused on getting myself in the best shape of my life
and going from there."
She intends to return to the WNBA when the season begins in June. The Mercury
guard has led the league in scoring the last four seasons and signed a multiyear
extension last August.
Fenerbahce had terminated Taurasi's contract after the lab within Hacettepe
University confirmed that her "A" and "B" samples tested positive for modafinil
following a Turkish league game Nov. 13. Taurasi had been suspended by
Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
GRAPHIC: ROSS D. FRANKLIN: AP REVERSAL: After months of uncertainty, Diana
Taurasi received good news from the Turkish Basketball Federation.
PUBLICATION-TYPE: Newspaper
Copyright 2011 The Houston Chronicle Publishing Company
All Rights Reserved
58 of 998 DOCUMENTS
Associated Press Worldstream
February 17, 2011 Thursday 5:25 PM GMT
WADA could suspend Turkish lab in Taurasi case
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: SPORTS NEWS
LENGTH: 733 words
DATELINE: LONDON
The World Anti-Doping Agency could suspend the Turkish drug-testing laboratory
that reported an apparent "false positive" for American basketball star Diana
Taurasi.
WADA director general David Howman told The Associated Press on Thursday the
agency has asked the Ankara lab to explain why it declared Taurasi's samples
positive for the banned stimulant modafinil, a decision which led to her
contract being terminated by her Turkish club.
"We are still awaiting all the information from the laboratory," Howman said.
"It appears that it was a false positive. In any of those cases we need to
review all the data to determine whether any steps need to be taken, including
any steps against the laboratory."
WADA can suspend and revoke the accreditation of doping labs. WADA, which has 35
accredited labs worldwide, previously suspended the Ankara center for three
months in 2009 for failing to meet international standards.
"Anything which goes wrong has to be a worry," Howman said. "That's why we have
to investigate it pretty thoroughly. The reputation of the athlete who's been
aggrieved is pretty important, too, and that has to be acknowledged."
The Turkish lab reported that Taurasi's "A" and "B" samples both tested positive
for modafinil following a Turkish league game on Nov. 13. Her club, Fenerbahce,
terminated her contract last month and she was suspended by the Turkish
Basketball Federation.
The federation lifted the suspension Wednesday, saying the lab retracted its
positive finding after it "evaluated" Taurasi's statements in her defense.
The federation also lifted the provisional suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in tests carried out by the same lab.
False positives are rare in international drug testing.
"We have more of an issue with false negatives," Howman said.
The WADA-accredited lab in Malaysia was suspended for false positives last year.
The lab is appealing the decision to the Court of Arbitration for Sport.
"There is a process that has to be followed, including the gathering of all the
data," Howman said in a telephone interview from Montreal. "If it's sufficiently
bad, then the lab should go to a disciplinary panel and have a hearing. They've
got a right to put every excuse and reasoning before the panel."
Taurasi insisted all along that she never used performance-enhancing drugs.
"It's really good that the facts came out and the truth came out," Taurasi told
the AP on Wednesday. "Life can throw you curveballs at any given time. I can be
made and angry, but I will move forward."
The 28-year-old Taurasi intends to return to the WNBA when the season begins in
June. The Mercury guard has led the U.S. league in scoring the last four
seasons. She is also now eligible to compete for the U.S. at the 2012 London
Olympics.
The Turkish Doping Control Center at the Hacettepe University declined to
comment on the case Thursday. But the HaberTurk newspaper quoted Ugur Erdener,
dean of the university, as admitting the lab made a mistake.
"There are two evaluations to analyze the test results and the average of them
is taken. The (lab) officials' evaluation was based on one data. However, the
average should have been taken as the base," Erdener was quoted as saying.
Fenerbahce President Aziz Yildirim met Turkey's Prime Minister Recep Tayyip
Erdogan to discuss the case Thursday. No statement was made after the meeting
but Ali Koc, a club official, denied reports that Fenerbahce asked authorities
to shut down the doping lab.
Turgay Demirel, president of the Turkish Basketball Federation, said two
football players were also cleared of doping after the lab retracted its reports
about them.
"It is very sad for our country that an institution accredited to WADA committed
such a huge mistake," he said. "Both Turkey, Turkish sports and Turkish
basketball could pay a fairly high price for this. Sportsmen and federations or
clubs in their countries and even us could file compensation suits against this
institution."
Demirel said about 3,500 doping tests have been carried out annually in Turkey,
with most analyzed by the Ankara lab.
"From now on, I don't think the certificate of Hacettepe University can remain
valid," Demirel said. "But we will have to use centers in Lisbon, Cologne or
maybe Athens."
Associated Press writer Selcan Hacaoglu in Ankara contributed to this report.
LOAD-DATE: February 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
59 of 998 DOCUMENTS
Associated Press Online
February 17, 2011 Thursday 5:48 PM GMT
WADA could suspend Turkish lab in Taurasi case
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: SPORTS NEWS
LENGTH: 732 words
DATELINE: LONDON
The World Anti-Doping Agency could suspend the Turkish drug-testing laboratory
that reported an apparent "false positive" for American basketball star Diana
Taurasi.
WADA director general David Howman told The Associated Press on Thursday the
agency has asked the Ankara lab to explain why it declared Taurasi's samples
positive for the banned stimulant modafinil, a decision which led to her
contract being terminated by her Turkish club.
"We are still awaiting all the information from the laboratory," Howman said.
"It appears that it was a false positive. In any of those cases we need to
review all the data to determine whether any steps need to be taken, including
any steps against the laboratory."
WADA can suspend and revoke the accreditation of doping labs. WADA, which has 35
accredited labs worldwide, previously suspended the Ankara center for three
months in 2009 for failing to meet international standards.
"Anything which goes wrong has to be a worry," Howman said. "That's why we have
to investigate it pretty thoroughly. The reputation of the athlete who's been
aggrieved is pretty important, too, and that has to be acknowledged."
The Turkish lab reported that Taurasi's "A" and "B" samples both tested positive
for modafinil following a Turkish league game on Nov. 13. Her club, Fenerbahce,
terminated her contract last month and she was suspended by the Turkish
Basketball Federation.
The federation lifted the suspension Wednesday, saying the lab retracted its
positive finding after it "evaluated" Taurasi's statements in her defense.
The federation also lifted the provisional suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in tests carried out by the same lab.
False positives are rare in international drug testing.
"We have more of an issue with false negatives," Howman said.
The WADA-accredited lab in Malaysia was suspended for false positives last year.
The lab is appealing the decision to the Court of Arbitration for Sport.
"There is a process that has to be followed, including the gathering of all the
data," Howman said in a telephone interview from Montreal. "If it's sufficiently
bad, then the lab should go to a disciplinary panel and have a hearing. They've
got a right to put every excuse and reasoning before the panel."
Taurasi insisted all along that she never used performance-enhancing drugs.
"It's really good that the facts came out and the truth came out," Taurasi told
the AP on Wednesday. "Life can throw you curveballs at any given time. I can be
mad and angry, but I will move forward."
The 28-year-old Taurasi intends to return to the WNBA when the season begins in
June. The Mercury guard has led the U.S. league in scoring the last four
seasons. She is also now eligible to compete for the U.S. at the 2012 London
Olympics.
The Turkish Doping Control Center at the Hacettepe University declined to
comment on the case Thursday. But the HaberTurk newspaper quoted Ugur Erdener,
dean of the university, as admitting the lab made a mistake.
"There are two evaluations to analyze the test results and the average of them
is taken. The (lab) officials' evaluation was based on one data. However, the
average should have been taken as the base," Erdener was quoted as saying.
Fenerbahce President Aziz Yildirim met Turkey's Prime Minister Recep Tayyip
Erdogan to discuss the case Thursday. No statement was made after the meeting
but Ali Koc, a club official, denied reports that Fenerbahce asked authorities
to shut down the doping lab.
Turgay Demirel, president of the Turkish Basketball Federation, said two soccer
players were also cleared of doping after the lab retracted its reports about
them.
"It is very sad for our country that an institution accredited to WADA committed
such a huge mistake," he said. "Both Turkey, Turkish sports and Turkish
basketball could pay a fairly high price for this. Sportsmen and federations or
clubs in their countries and even us could file compensation suits against this
institution."
Demirel said about 3,500 doping tests have been carried out annually in Turkey,
with most analyzed by the Ankara lab.
"From now on, I don't think the certificate of Hacettepe University can remain
valid," Demirel said. "But we will have to use centers in Lisbon, Cologne or
maybe Athens."
Associated Press writer Selcan Hacaoglu in Ankara contributed to this report.
LOAD-DATE: February 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
60 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 17, 2011 Thursday 5:48 PM GMT
WADA could suspend Turkish lab in Taurasi case
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: SPORTS NEWS
LENGTH: 732 words
DATELINE: LONDON
The World Anti-Doping Agency could suspend the Turkish drug-testing laboratory
that reported an apparent "false positive" for American basketball star Diana
Taurasi.
WADA director general David Howman told The Associated Press on Thursday the
agency has asked the Ankara lab to explain why it declared Taurasi's samples
positive for the banned stimulant modafinil, a decision which led to her
contract being terminated by her Turkish club.
"We are still awaiting all the information from the laboratory," Howman said.
"It appears that it was a false positive. In any of those cases we need to
review all the data to determine whether any steps need to be taken, including
any steps against the laboratory."
WADA can suspend and revoke the accreditation of doping labs. WADA, which has 35
accredited labs worldwide, previously suspended the Ankara center for three
months in 2009 for failing to meet international standards.
"Anything which goes wrong has to be a worry," Howman said. "That's why we have
to investigate it pretty thoroughly. The reputation of the athlete who's been
aggrieved is pretty important, too, and that has to be acknowledged."
The Turkish lab reported that Taurasi's "A" and "B" samples both tested positive
for modafinil following a Turkish league game on Nov. 13. Her club, Fenerbahce,
terminated her contract last month and she was suspended by the Turkish
Basketball Federation.
The federation lifted the suspension Wednesday, saying the lab retracted its
positive finding after it "evaluated" Taurasi's statements in her defense.
The federation also lifted the provisional suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in tests carried out by the same lab.
False positives are rare in international drug testing.
"We have more of an issue with false negatives," Howman said.
The WADA-accredited lab in Malaysia was suspended for false positives last year.
The lab is appealing the decision to the Court of Arbitration for Sport.
"There is a process that has to be followed, including the gathering of all the
data," Howman said in a telephone interview from Montreal. "If it's sufficiently
bad, then the lab should go to a disciplinary panel and have a hearing. They've
got a right to put every excuse and reasoning before the panel."
Taurasi insisted all along that she never used performance-enhancing drugs.
"It's really good that the facts came out and the truth came out," Taurasi told
the AP on Wednesday. "Life can throw you curveballs at any given time. I can be
mad and angry, but I will move forward."
The 28-year-old Taurasi intends to return to the WNBA when the season begins in
June. The Mercury guard has led the U.S. league in scoring the last four
seasons. She is also now eligible to compete for the U.S. at the 2012 London
Olympics.
The Turkish Doping Control Center at the Hacettepe University declined to
comment on the case Thursday. But the HaberTurk newspaper quoted Ugur Erdener,
dean of the university, as admitting the lab made a mistake.
"There are two evaluations to analyze the test results and the average of them
is taken. The (lab) officials' evaluation was based on one data. However, the
average should have been taken as the base," Erdener was quoted as saying.
Fenerbahce President Aziz Yildirim met Turkey's Prime Minister Recep Tayyip
Erdogan to discuss the case Thursday. No statement was made after the meeting
but Ali Koc, a club official, denied reports that Fenerbahce asked authorities
to shut down the doping lab.
Turgay Demirel, president of the Turkish Basketball Federation, said two soccer
players were also cleared of doping after the lab retracted its reports about
them.
"It is very sad for our country that an institution accredited to WADA committed
such a huge mistake," he said. "Both Turkey, Turkish sports and Turkish
basketball could pay a fairly high price for this. Sportsmen and federations or
clubs in their countries and even us could file compensation suits against this
institution."
Demirel said about 3,500 doping tests have been carried out annually in Turkey,
with most analyzed by the Ankara lab.
"From now on, I don't think the certificate of Hacettepe University can remain
valid," Demirel said. "But we will have to use centers in Lisbon, Cologne or
maybe Athens."
Associated Press writer Selcan Hacaoglu in Ankara contributed to this report.
LOAD-DATE: February 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
61 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 17, 2011 Thursday 5:48 PM GMT
LENGTH: 775 words
BC-BKL--WADA-Doping-Taurasi, 1st Ld-Writethru,0936
WADA could suspend Turkish lab in Taurasi case
2030
Eds: Updates with detail, quotes.
AP Photo NY161, NY150
sptd/rrosenblatt elfd/lon/clehourites fasst4922 fasst4921
By STEPHEN WILSON
AP Sports Writer
LONDON (AP) The World Anti-Doping Agency could suspend the Turkish drug-testing
laboratory that reported an apparent "false positive" for American basketball
star Diana Taurasi.
WADA director general David Howman told The Associated Press on Thursday the
agency has asked the Ankara lab to explain why it declared Taurasi's samples
positive for the banned stimulant modafinil, a decision which led to her
contract being terminated by her Turkish club.
"We are still awaiting all the information from the laboratory," Howman said.
"It appears that it was a false positive. In any of those cases we need to
review all the data to determine whether any steps need to be taken, including
any steps against the laboratory."
WADA can suspend and revoke the accreditation of doping labs. WADA, which has 35
accredited labs worldwide, previously suspended the Ankara center for three
months in 2009 for failing to meet international standards.
"Anything which goes wrong has to be a worry," Howman said. "That's why we have
to investigate it pretty thoroughly. The reputation of the athlete who's been
aggrieved is pretty important, too, and that has to be acknowledged."
The Turkish lab reported that Taurasi's "A" and "B" samples both tested positive
for modafinil following a Turkish league game on Nov. 13. Her club, Fenerbahce,
terminated her contract last month and she was suspended by the Turkish
Basketball Federation.
The federation lifted the suspension Wednesday, saying the lab retracted its
positive finding after it "evaluated" Taurasi's statements in her defense.
The federation also lifted the provisional suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in tests carried out by the same lab.
False positives are rare in international drug testing.
"We have more of an issue with false negatives," Howman said.
The WADA-accredited lab in Malaysia was suspended for false positives last year.
The lab is appealing the decision to the Court of Arbitration for Sport.
"There is a process that has to be followed, including the gathering of all the
data," Howman said in a telephone interview from Montreal. "If it's sufficiently
bad, then the lab should go to a disciplinary panel and have a hearing. They've
got a right to put every excuse and reasoning before the panel."
Taurasi insisted all along that she never used performance-enhancing drugs.
"It's really good that the facts came out and the truth came out," Taurasi told
the AP on Wednesday. "Life can throw you curveballs at any given time. I can be
mad and angry, but I will move forward."
The 28-year-old Taurasi intends to return to the WNBA when the season begins in
June. The Mercury guard has led the U.S. league in scoring the last four
seasons. She is also now eligible to compete for the U.S. at the 2012 London
Olympics.
The Turkish Doping Control Center at the Hacettepe University declined to
comment on the case Thursday. But the HaberTurk newspaper quoted Ugur Erdener,
dean of the university, as admitting the lab made a mistake.
"There are two evaluations to analyze the test results and the average of them
is taken. The (lab) officials' evaluation was based on one data. However, the
average should have been taken as the base," Erdener was quoted as saying.
Fenerbahce President Aziz Yildirim met Turkey's Prime Minister Recep Tayyip
Erdogan to discuss the case Thursday. No statement was made after the meeting
but Ali Koc, a club official, denied reports that Fenerbahce asked authorities
to shut down the doping lab.
Turgay Demirel, president of the Turkish Basketball Federation, said two soccer
players were also cleared of doping after the lab retracted its reports about
them.
"It is very sad for our country that an institution accredited to WADA committed
such a huge mistake," he said. "Both Turkey, Turkish sports and Turkish
basketball could pay a fairly high price for this. Sportsmen and federations or
clubs in their countries and even us could file compensation suits against this
institution."
Demirel said about 3,500 doping tests have been carried out annually in Turkey,
with most analyzed by the Ankara lab.
"From now on, I don't think the certificate of Hacettepe University can remain
valid," Demirel said. "But we will have to use centers in Lisbon, Cologne or
maybe Athens."
Associated Press writer Selcan Hacaoglu in Ankara contributed to this report.
LOAD-DATE: February 18, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
62 of 998 DOCUMENTS
The Associated Press
February 16, 2011 Wednesday 08:56 PM GMT
Taurasi cleared of doping charges
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 702 words
Diana Taurasi was always confident she would be cleared of doping allegations.
It finally happened on Wednesday.
Taurasi had her provisional suspension lifted by the Turkish Basketball
Federation, which said the lab that returned a positive test retracted its
report after it "evaluated" Taurasi's statements in her defense. The federation
did not say whether the lab made a mistake.
"I got the news this morning at 5 a.m. and was in shock," Taurasi told The
Associated Press by phone from her Phoenix home. "It was kind of like the first
time when I heard the test result had come back positive. It's really good that
the facts came out and the truth came out."
Taurasi had insisted that she never used performance-enhancing drugs, even
though she had her contract terminated by Turkish club Fenerbahce last month.
The lab that tested her sample had said the results came back positive for the
stimulant modafinil.
"Life can throw you curveballs at any given time," said Taurasi, who will also
be able to compete in the 2012 Olympics. "I can be mad and angry, but I will
move forward. Not everyone has the same financial resources I did. Hopefully
this will let people know every process has holes and to wait for the facts to
come out before making decisions."
With the lifting of the suspension, Taurasi is also free to continue playing in
the Turkish basketball league, although she doesn't plan on going back there
anytime soon.
"That's pretty unlikely," the 28-year-old WNBA star said. "I'm here in Phoenix
working out and am more focused on getting myself in the best shape of my life
and going from there."
She intends to return to the WNBA when the season begins in June. The Mercury
guard has led the league in scoring the last four seasons and signed a multiyear
extension last August.
The last two months haven't been easy for the former UConn star. Yet she kept
her faith that she would be cleared.
"I tried to handle it as best as possible," Taurasi said. "There might have been
times in my own private moments when I was angry or questioned why me, but I am
glad the truth came out. It's scary that our careers can be taken away from us."
Taurasi was the first prominent WNBA player to test positive for a banned
substance. Had she not been cleared, Taurasi could have missed the London Games,
because the International Olympic Committee bars any athlete given a doping
penalty of six months or more from competing.
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her "A" and "B" samples tested positive for
modafinil following a Turkish league game Nov. 13. Taurasi had been suspended by
Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
"It's always great when the right result happens," Taurasi's lawyer Howard
Jacobs said. "When it happens reasonably quickly it's even better."
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
"I was thrilled to read today's report that the precautionary ban on Diana had
been lifted by the Turkish Federation," UConn and U.S. basketball coach Geno
Auriemma said in a statement.
"Throughout this entire ordeal, Dee maintained her innocence and for her to be
exonerated makes me incredibly happy for her," Auriemma said. "I hope she can
put this behind her and focus all her efforts on continuing to be the best
player in the world."
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championship this past
October.
"We're delighted that Diana has been cleared and can now put this behind her and
continue her remarkable basketball career," USA Basketball executive director
Jim Tooley said in a statement. "She has been an exemplary member of numerous
USA Basketball teams since 2000, and we look forward to her continued
involvement with USA Basketball."
Associated Press writers Selcan Hacaoglu and Suzan Fraser in Ankara contributed
to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
63 of 998 DOCUMENTS
Associated Press Worldstream
February 16, 2011 Wednesday 1:55 PM GMT
Turkey lifts provisional doping ban on Taurasi
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 463 words
DATELINE: ANKARA Turkey
Turkey's basketball federation lifted American star Diana Taurasi's provisional
doping suspension Wednesday after a lab retracted its finding that she tested
positive.
The Turkish Basketball Federation said the lab retracted its report after it
"evaluated" Taurasi's statements in her defense. The federation did not say
outright if the lab had made a mistake.
The federation said Taurasi was free to continue playing in the Turkish
basketball league, a decision which is also likely to revive her chances of
playing for the United States at the 2012 London Olympics.
"The federation has decided to lift the precautionary ban imposed on player
Diana Lorena Taurasi to prevent the club and the player from being aggrieved
further," the Turkish body said in a statement.
Taurasi, who has insisted that she never used performance-enhancing drugs, had
her contract terminated by Turkish club Fenerbahce last month after the lab said
she tested positive for modafinil in December. It was not clear if Taurasi would
return to Turkey.
Taurasi said in an interview with The Associated Press last month that "there's
no way I've ever taken anything. ... Only thing that I'm guilty of is taking too
many jump shots."
Taurasi intends to return to the WNBA when the season begins in June. The
Phoenix guard has led the U.S. league in scoring the last four seasons and
signed a multiyear extension last August.
Fenerbahce President Aziz Yildirim said Wednesday he was furious that Taurasi
had been banned even though she was apparently innocent.
"Our player was right. We will pursue this. We have documents," the club's
website quoted Yildirim as saying. "This is a disgrace ... it probably cost us
the European Championship."
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her both "A" and "B" samples tested positive
for the banned stimulant modafinil following a Turkish league game on Nov. 13.
Taurasi had been suspended by Fenerbahce ever since.
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Wednesday's decision is expected to clear the way for Taurasi to play in the
Olympics. The International Olympic Committee bars any athlete given a doping
penalty of six months or more from competing in the next games.
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championships.
Associated Press Writer Suzan Fraser contributed to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
64 of 998 DOCUMENTS
Associated Press Online
February 16, 2011 Wednesday 4:48 PM GMT
Turkey lifts provisional doping ban on Taurasi
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 543 words
DATELINE: ANKARA Turkey
Turkey's basketball federation lifted American star Diana Taurasi's provisional
doping suspension Wednesday after a lab retracted its finding that she tested
positive for a performance-enhancing substance.
The Turkish Basketball Federation said the lab retracted its report after it
"evaluated" Taurasi's statements in her defense. The federation did not say
whether the lab made a mistake.
Taurasi not only is free to continue playing in the Turkish basketball league,
she also is cleared to participate for the United States at the 2012 London
Olympics.
"The Federation has decided to lift the precautionary ban imposed on player
Diana Lorena Taurasi to prevent the club and the player from being aggrieved
further," the Turkish body said in a statement Wednesday.
Taurasi, who has insisted that she never used performance-enhancing drugs, had
her contract terminated by Turkish club Fenerbahce last month after the lab said
she tested positive for modafinil in December. It was not clear whether Taurasi
would return to Turkey.
Taurasi said in an interview with The Associated Press last month that "there's
no way I've ever taken anything. ... Only thing that I'm guilty of is taking too
many jump shots."
Taurasi intends to return to the WNBA when the season begins in June. The
Phoenix guard has led the league in scoring the last four seasons and signed a
multiyear extension last August.
Fenerbahce President Aziz Yildirim said Wednesday he was furious that Taurasi
had been banned even though she was apparently innocent.
"Our player was right. We will pursue this. We have documents," Yildirim said on
the club's website. "This is a disgrace. ... It probably cost us the European
Championship."
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her "A" and "B" samples tested positive for
the stimulant modafinil following a Turkish league game Nov. 13. Taurasi had
been suspended by Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
The decision Wednesday is expected to clear the way for Taurasi to play in the
Olympics. The International Olympic Committee bars any athlete who receives a
doping penalty of six months or more from competing in the next games.
"I was thrilled to read today's report that the precautionary ban on Diana had
been lifted by the Turkish Federation," UConn and U.S. basketball coach Geno
Auriemma said in a statement.
"Throughout this entire ordeal, Dee maintained her innocence and for her to be
exonerated makes me incredibly happy for her," Auriemma said. "I hope she can
put this behind her and focus all her efforts on continuing to be the best
player in the world."
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championships.
Associated Press Writer Suzan Fraser in Ankara and AP Basketball Writer Doug
Feinberg in New York contributed to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
65 of 998 DOCUMENTS
Associated Press Online
February 16, 2011 Wednesday 8:57 PM GMT
Taurasi cleared of doping charges
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 702 words
Diana Taurasi was always confident she would be cleared of doping allegations.
It finally happened on Wednesday.
Taurasi had her provisional suspension lifted by the Turkish Basketball
Federation, which said the lab that returned a positive test retracted its
report after it "evaluated" Taurasi's statements in her defense. The federation
did not say whether the lab made a mistake.
"I got the news this morning at 5 a.m. and was in shock," Taurasi told The
Associated Press by phone from her Phoenix home. "It was kind of like the first
time when I heard the test result had come back positive. It's really good that
the facts came out and the truth came out."
Taurasi had insisted that she never used performance-enhancing drugs, even
though she had her contract terminated by Turkish club Fenerbahce last month.
The lab that tested her sample had said the results came back positive for the
stimulant modafinil.
"Life can throw you curveballs at any given time," said Taurasi, who will also
be able to compete in the 2012 Olympics. "I can be mad and angry, but I will
move forward. Not everyone has the same financial resources I did. Hopefully
this will let people know every process has holes and to wait for the facts to
come out before making decisions."
With the lifting of the suspension, Taurasi is also free to continue playing in
the Turkish basketball league, although she doesn't plan on going back there
anytime soon.
"That's pretty unlikely," the 28-year-old WNBA star said. "I'm here in Phoenix
working out and am more focused on getting myself in the best shape of my life
and going from there."
She intends to return to the WNBA when the season begins in June. The Mercury
guard has led the league in scoring the last four seasons and signed a multiyear
extension last August.
The last two months haven't been easy for the former UConn star. Yet she kept
her faith that she would be cleared.
"I tried to handle it as best as possible," Taurasi said. "There might have been
times in my own private moments when I was angry or questioned why me, but I am
glad the truth came out. It's scary that our careers can be taken away from us."
Taurasi was the first prominent WNBA player to test positive for a banned
substance. Had she not been cleared, Taurasi could have missed the London Games,
because the International Olympic Committee bars any athlete given a doping
penalty of six months or more from competing.
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her "A" and "B" samples tested positive for
modafinil following a Turkish league game Nov. 13. Taurasi had been suspended by
Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
"It's always great when the right result happens," Taurasi's lawyer Howard
Jacobs said. "When it happens reasonably quickly it's even better."
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
"I was thrilled to read today's report that the precautionary ban on Diana had
been lifted by the Turkish Federation," UConn and U.S. basketball coach Geno
Auriemma said in a statement.
"Throughout this entire ordeal, Dee maintained her innocence and for her to be
exonerated makes me incredibly happy for her," Auriemma said. "I hope she can
put this behind her and focus all her efforts on continuing to be the best
player in the world."
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championship this past
October.
"We're delighted that Diana has been cleared and can now put this behind her and
continue her remarkable basketball career," USA Basketball executive director
Jim Tooley said in a statement. "She has been an exemplary member of numerous
USA Basketball teams since 2000, and we look forward to her continued
involvement with USA Basketball."
Associated Press writers Selcan Hacaoglu and Suzan Fraser in Ankara contributed
to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
66 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 16, 2011 Wednesday 5:09 PM GMT
Turkey lifts provisional doping ban on Taurasi
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 550 words
DATELINE: ANKARA Turkey
Turkey's basketball federation lifted American star Diana Taurasi's provisional
doping suspension Wednesday after a lab retracted its finding that she tested
positive for a performance-enhancing substance.
The Turkish Basketball Federation said the lab retracted its report after it
"evaluated" Taurasi's statements in her defense. The federation did not say
whether the lab made a mistake.
Taurasi not only is free to continue playing in the Turkish basketball league,
she also is cleared to participate for the United States at the 2012 London
Olympics.
"The Federation has decided to lift the precautionary ban imposed on player
Diana Lorena Taurasi to prevent the club and the player from being aggrieved
further," the Turkish body said in a statement Wednesday.
The former Connecticut women's basketball star, who has insisted that she never
used performance-enhancing drugs, had her contract terminated by Turkish club
Fenerbahce last month after the lab said she tested positive for modafinil in
December. It was not clear whether Taurasi would return to Turkey.
Taurasi said in an interview with The Associated Press last month that "there's
no way I've ever taken anything. ... Only thing that I'm guilty of is taking too
many jump shots."
Taurasi intends to return to the WNBA when the season begins in June. The
Phoenix guard has led the league in scoring the last four seasons and signed a
multiyear extension last August.
Fenerbahce President Aziz Yildirim said Wednesday he was furious that Taurasi
had been banned even though she was apparently innocent.
"Our player was right. We will pursue this. We have documents," Yildirim said on
the club's website. "This is a disgrace. ... It probably cost us the European
Championship."
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her "A" and "B" samples tested positive for
the stimulant modafinil following a Turkish league game Nov. 13. Taurasi had
been suspended by Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
The decision Wednesday is expected to clear the way for Taurasi to play in the
Olympics. The International Olympic Committee bars any athlete who receives a
doping penalty of six months or more from competing in the next games.
"I was thrilled to read today's report that the precautionary ban on Diana had
been lifted by the Turkish Federation," UConn and U.S. basketball coach Geno
Auriemma said in a statement.
"Throughout this entire ordeal, Dee maintained her innocence and for her to be
exonerated makes me incredibly happy for her," Auriemma said. "I hope she can
put this behind her and focus all her efforts on continuing to be the best
player in the world."
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championships.
Associated Press Writer Suzan Fraser in Ankara and AP Basketball Writer Doug
Feinberg in New York contributed to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
67 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 16, 2011 Wednesday 5:09 PM GMT
LENGTH: 595 words
BC-BKL--Doping-Taurasi, 3rd Ld-Writethru,0548
Turkey lifts provisional doping ban on Taurasi
Eds: Adds comment from Geno Auriemma.
usae/swingfield sptd/dskretta elfd/lon/srwilson elfd/lon/clehourites fasst4922
fasst4921
By SELCAN HACAOGLU
Associated Press
ANKARA, Turkey (AP) Turkey's basketball federation lifted American star Diana
Taurasi's provisional doping suspension Wednesday after a lab retracted its
finding that she tested positive for a performance-enhancing substance.
The Turkish Basketball Federation said the lab retracted its report after it
"evaluated" Taurasi's statements in her defense. The federation did not say
whether the lab made a mistake.
Taurasi not only is free to continue playing in the Turkish basketball league,
she also is cleared to participate for the United States at the 2012 London
Olympics.
"The Federation has decided to lift the precautionary ban imposed on player
Diana Lorena Taurasi to prevent the club and the player from being aggrieved
further," the Turkish body said in a statement Wednesday.
The former Connecticut women's basketball star, who has insisted that she never
used performance-enhancing drugs, had her contract terminated by Turkish club
Fenerbahce last month after the lab said she tested positive for modafinil in
December. It was not clear whether Taurasi would return to Turkey.
Taurasi said in an interview with The Associated Press last month that "there's
no way I've ever taken anything. ... Only thing that I'm guilty of is taking too
many jump shots."
Taurasi intends to return to the WNBA when the season begins in June. The
Phoenix guard has led the league in scoring the last four seasons and signed a
multiyear extension last August.
Fenerbahce President Aziz Yildirim said Wednesday he was furious that Taurasi
had been banned even though she was apparently innocent.
"Our player was right. We will pursue this. We have documents," Yildirim said on
the club's website. "This is a disgrace. ... It probably cost us the European
Championship."
Fenerbahce had terminated Taurasi's contract after the Ankara-based lab within
Hacettepe University confirmed that her "A" and "B" samples tested positive for
the stimulant modafinil following a Turkish league game Nov. 13. Taurasi had
been suspended by Fenerbahce ever since.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
The federation also lifted the provisional doping suspension for American player
Monique Coker, who plays for Ceyhan Belediyesi and had tested positive for
modafinil in doping tests carried out by the same lab.
The decision Wednesday is expected to clear the way for Taurasi to play in the
Olympics. The International Olympic Committee bars any athlete who receives a
doping penalty of six months or more from competing in the next games.
"I was thrilled to read today's report that the precautionary ban on Diana had
been lifted by the Turkish Federation," UConn and U.S. basketball coach Geno
Auriemma said in a statement.
"Throughout this entire ordeal, Dee maintained her innocence and for her to be
exonerated makes me incredibly happy for her," Auriemma said. "I hope she can
put this behind her and focus all her efforts on continuing to be the best
player in the world."
Taurasi helped the Americans win gold medals at the past two Olympics and was
the leading scorer when the U.S. won the women's world championships.
Associated Press Writer Suzan Fraser in Ankara and AP Basketball Writer Doug
Feinberg in New York contributed to this report.
LOAD-DATE: February 17, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
68 of 998 DOCUMENTS
Cancer Drug News
February 10, 2011
Lundbeck granted commercial rights to Cephalon products in Canada and/or Latin
America
SECTION: NEWS
LENGTH: 447 words
Lundbeck has been granted commercial rights to several Cephalon products in
Canada and Latin America. As part of the agreement, Lundbeck will register and
commercialise several key products that are currently available in the US and/or
Europe on behalf of Cephalon. Key products in the agreement include Fentora
(fentanyl buccal tablet) [C-II], Provigil (modafinil), Treanda (bendamustine),
Trisenox (arsenic trioxide) injection, Myocet (liposomal doxorubicin) and
Nuvigil (armodafinil).
According to Lundbeck, the Cephalon brands will significantly strengthen its
position in these markets while leveraging on existing sales and marketing
capabilities, adding significant sales in Canada and Latin America from 2012.
The Cephalon products for improving wakefulness, Provigil and Nuvigil, as well
as the pain product, Fentora, are considered to have a strong fit to Lundbeck's
already strong central nervous system franchise. Lundbeck is currently
successfully promoting modafinil in Mexico. Nuvigil is expected to be approved
in Canada and Latin America in the 2012-2014 time period, and Lundbeck expects
to promote these products with the existing sales and marketing organisation.
Also included in the deal is the Cephalon oncology product, Treanda, which is to
be commercialised by Lundbeck in Canada. The new oncology franchise in Canada
will be complemented by Trisenox and the pain product, Fentora. Treanda has
proven clinical activity in the treatment of haematological malignancies,
including those refractory to conventional anticancer agents. Treanda is
expected to be filed during 2011 in Canada, and Lundbeck will establish a
dedicated oncology sales organisation in Latin America and Canada in order to
achieve the full potential of the oncology portfolio.
The financial terms were not disclosed, but Lundbeck is to pay double-digit
royalties on sales, which will be the main overall revenue stream for Cephalon
from these products in these territories.
Product Indication Territory
Provigil, Improve wakefulness in adults who Canada (Nuvigil only)
Nuvigil experience excessive sleepiness and Latin America
due to treated obstructive sleep
apnoea, shift work disorder, or
narcolepsy
Treanda Treatment of indolent B-cell Canada
non-Hodgkin's lymphoma and chronic
lymphocytic leukaemia
Fentora Compound for breakthrough pain in Canada and Latin America
opioid-tolerant patients with
cancer
Trisenox Cytotoxin for acute promyelocytic Canada
leukaemia
Myocet1 Cytotoxin for metastatic breast Latin America
cancer
1Myocet will be included in the agreement at a later stage.
Cephalon holds exclusive rights to market and develop Treanda, which is licensed
from Astellas Deutschland (Astellas Pharma
LOAD-DATE: February 10, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: Cancer Drug News
Copyright 2011 Espicom Business Intelligence
All Rights Reserved
69 of 998 DOCUMENTS
Drug Delivery Insight
February 9, 2011
Lundbeck expands commercial opportunities in Canada/Latin America with help from
Cephalon
SECTION: NEWS
LENGTH: 404 words
Lundbeck has been granted commercial rights to a number of Cephalon products in
Canada and Latin America. As part of the agreement, Lundbeck will register and
commercialise several key products that are currently available in the US and/or
Europe, on behalf of Cephalon. Key products in the agreement include Fentora
(fentanyl buccal tablet) [C-II], Provigil (modafinil tablet), Treanda
(bendamustine hydrochloride injection), Trisenox (arsenic trioxide injection),
Myocet (liposomal- doxorubicin) and Nuvigil (armodafinil tablet).
The Cephalon products for improving wakefulness, Provigil and Nuvigil, as well
as the pain product, Fentora, have a strong fit to Lundbeck's CNS franchise and
will contribute to the continued growth in both Canada and Latin America.
Lundbeck is currently successfully promoting modafinil in Mexico. Provigil and
Nuvigil address a market with a substantial under-diagnosed and under-treated
patient group. Nuvigil is expected to be approved in Canada and Latin America in
the 2012 to 2014 time period. In 2009, Cephalon realised revenue of US $73
million in the US on Nuvigil and in the first nine months of 2010, revenues were
US $127 million. Lundbeck expects to promote these products with the existing
sales and marketing organisation.
Also included in the deal is the leading Cephalon oncology product Treanda,
which is to be commercialised by Lundbeck in Canada. Treanda will add
significantly to revenue and earnings in Lundbeck's Canadian business. The new
oncology franchise in Canada will be complemented by Trisenox and Fentora.
Treanda has proven clinical activity in the treatment of haematological
malignancies, including those refractory to conventional anti-cancer agents. In
2008, the American Society of Clinical Oncology recognised Treanda as one of the
major advances in cancer treatment. In 2009, Cephalon realised total revenue of
US $222 million on the product and in the first nine months of 2010, revenue
reached US $285 million in the US. Treanda is expected to be filed during 2011
in Canada and Lundbeck will establish a dedicated oncology sales organisation in
Latin America and Canada in order to achieve the full potential of the oncology
portfolio.
The financial terms of the agreement have not been disclosed, but Lundbeck is to
pay double-digit royalties on sales which will be the main overall revenue
stream for Cephalon from these products in these territories.
LOAD-DATE: February 9, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: Drug Delivery Insight
Copyright 2011 Espicom Business Intelligence
All Rights Reserved
70 of 998 DOCUMENTS
US Fed News
February 9, 2011 Wednesday 10:00 AM EST
US Patent Issued to NeuroHealing Pharmaceuticals on Feb. 8 for "Modafinil-Based
Treatment for Premature Ejaculation" (Massachusetts Inventor)
LENGTH: 142 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., Feb. 9 -- United States Patent no. 7,884,135, issued on Feb. 8,
was assigned to NeuroHealing Pharmaceuticals Inc. (Newton, Mass.).
"Modafinil-Based Treatment for Premature Ejaculation" was invented by Daniel E.
Katzman (Newton, Mass.).
According to the abstract released by the U.S. Patent & Trademark Office:
"Methods and compositions comprising modafinil are described for treating
premature ejaculation in a male individual."
The patent was filed on Aug. 13, 2007, under Application No. 12/310,175.
For further information please visit:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO2&Sect2=HITOFF&p=1&u=%2Fnetah
tml%2FPTO%2Fsearch-bool.html&r=1&f=G&l=50&co1=AND&d=PTXT&s1=7884135&OS=7884135&R
S=7884135
For any query with respect to this article or any other content requirement,
please contact Editor at htsyndication@hindustantimes.com
LOAD-DATE: February 11, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 HT Media Ltd.
All Rights Reserved
71 of 998 DOCUMENTS
Global Insight
February 8, 2011
Lundbeck Obtains Commercial Rights to Several Cephalon Products in Canada, Latin
America
BYLINE: Anne-Charlotte Honore
SECTION: In Brief
LENGTH: 324 words
Danish firm Lundbeck has been granted commercial rights to several Cephalon
products in Canada and/or Latin America. Under the terms of agreement, Lundbeck
will register and commercialise Provigil (modafinil) and Nuvigil (armodafinil)
in Canada (Nuvigil only) and Latin America; Treanda (bendamustine HCI) in
Canada; Fentora (fentanyl buccal tablet) in Canada and Latin America; Trisenox
(arsenic trioxide) in Canada and at a later stage Myocet (liposomal doxorubicin)
in Latin America. Lundbeck will pay double-digit royalties on sales to Cephalon.
Financial terms were not disclosed.
Significance:All products in-licensed from Cephalon are already approved in the
United States, meaning that the clinical and regulatory risk is minimal for
Lundbeck which takes here the opportunity to expand its presence in Latin
America and Canada while strengthening its CNS and oncology franchises.
Cephalon's drugs Treanda (bendamustine HCI), Provigil (modafinil) and Nuvigil
(armodafinil) are expected to boost Lundbeck's sales performance in Canada and
Latin America from 2012 onwards. Nuvigil is expected to be approved in the
period 2012-14 in Canada and Latin America while Treanda is set to be filed
during 2011 in Canada. Lundbeck said it will set a "dedicated oncology sales
organisation in Latin America and Canada in order to achieve the full potential
of the oncology portfolio". Its new oncology franchise in Canada will be
composed of Treanda (bendamustine HCI) for the treatment of indolent B-cell
non-Hodgkin's lymphoma (NHL) and chronic lymphocytic leukaemia (CLL), Fentora
(fentanyl buccal tablet) for breakthrough pain in opioid-tolerant patients with
cancer and of Trisenox (arsenic trioxide) for acute promyelocytic leukaemia
(APL). Fentora (fentanyl buccal tablet) will be the only oncology-related
Cephalon product commercialised by Lundbeck in Latin America until Myocet
(liposomal doxorubicin) is included in the deal at a later stage.
LOAD-DATE: April 30, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2011 World Markets Research Limited
All Rights Reserved
72 of 998 DOCUMENTS
Cynic Central
February 5, 2011 Saturday 10:09 PM EST
Losers and plastic dolls, women's basketball remains boring and Serbia gets in
on a Week O' Riots
BYLINE: andy
LENGTH: 2072 words
Feb. 5, 2011 (Cynic Central delivered by Newstex) --
- If I actually cared about womens basketball (or anyone else did), then this
would be a fascinating story. One of the most accomplished players in the
history of a sport embroiled in a scandal over whether or not she used
performance-enhancing drugs, with the added intrigue of an international
component to the saga.
But alas, it is womens basketball and so Diana Taurasi testing positive in
Turkey for the banned stimulant Modafinil and subsequently passing a polygraph
test last month in which she insisted she never took the drug isnt a big deal.
Taurasi used the polygraph results as part of a written defense that Taurasi
sent to the Turkish Basketball Federation last week in which she seeks dismissal
of the case against her. The test was conducted by former Chicago police officer
John Fritz, who said he asked Taurasi two "relevant" questions Jan. 18: Did you
at any time take the drug Modafinil or any similar generic brand name drug? And
did you lie to club management when you denied ever using the drug Modafinil or
any similar generic brand name drug? Fritz's report states that her score showed
"that Subject was truthful when she answered 'no' to the above relevant
questions." So whats at stake here? For the average sports fan, nothing. That
average sports fan doesnt pay attention to the WNBA, so he or she surely pays
even less attention to international womens hoops. For Taurasi, there is much
more to lose. She was fired by her Turkish club, Fenerbahce, in December and
faces a ban of up to two years that endangers her chance to play for the United
States at the 2012 London Olympics. Also, if she is ultimately found guilty and
officially suspended, Taurasi would also be subject to a World Anti-Doping
Agency (WADA) rule that would erase any time she served if she went to play for
the WNBA. The rule is intended to prevent banned athletes from merely going to
play in leagues not regulated by WADA to sidestep a ban. Taurasi's Los Angeles
defense attorney, Howard Jacobs, is arguing for dismissal of her case and has
criticized several irregularities in the way her case was handled by Turkish
authorities. Chief among those criticisms is the handling of her urine samples
prior to testing, including a seven-day period, he says, during which there was
no documentation indicating where they were kept during transportation from
Istanbul to Ankara. That could be a problem because WADA maintains specific
criteria for identifying Modafinil in labs and Jacobs insists Taurasi's results
fell outside the agency's allowable margin of error. Questioning this particular
lab in Ankara is a wise move because the lab had its drug-testing credentials
suspended by WADA for three months in 2009 due to problems with its methods. As
for Modafinil, it is a stimulant prescribed to treat narcolepsy patients who
suffer (OOTC:WLVTQ) from excessive sleepiness and need help staying up - the
very sort of thing that would help anyone trying to watch womens professional
basketball. The next step in the process for Taurasi is to wait for the Turkish
Basketball Federation to rule. After that, the first appeal would be to the
Turkish Sports and Youth Arbitration Association, and if necessary, the
international Court for Arbitration in Sport, which is the Supreme Court for
doping cases. The legal battle could take a few months, but odds are it won't be
any more boring than your typical WNBA game.........
- Attention, Massachusetts residents: Rep. Cleon Turner or a member of his staff
will soon be coming to your driveway or parking lot to clean the snow and ice
off your car before you get out on the road......wait, you mean thats not going
to happen? Then Turners idea for a law that would fine drivers for not cleaning
winter debris off their car before pulling onto the road is just asinine. Sure,
having snow and chunks of ice come flying off the car in front of you can be
tough, but a little bit of safe driving on your part can alleviate much of the
danger. The incident that took place Friday morning on I-93 in Andover, when ice
flew off of a tractor trailer in front of a Honda Civic and landed so hard that
it cracked the windshield is scary, to be certain, but the driver of that car
was unharmed and the incident was nothing more than a blip on the radar. Its
certainly no reason to overreact, but overreact someone must in every situation
and in this case, its Rep. Cleon Turner. oeIm more concerned about having
legislation there or a statute there eventually that will give police the tools
they need to stop a vehicle and say, [#x2dc]Look. You need to clean the snow off
your vehicle because its dangerous, said Rep. Turner. Great, an alarmist
lawmaker looking to make a name for himself. And by making a name for himself, I
mean this kook wants to fine people $500 for not brushing the snow and ice off
their ride. Left unsaid is exactly what the standard will be. After all, if you
brush off 95 percent of the snow on the roof of your SUV but miss one chunk that
flies off and a cop sees it, then what? Or how about someone elses debris flies
off their car, lands on your roof and then flies off your roof, but the cop only
sees it come from your vehicle? Its a ginormous can of worms youre opening here,
Rep. Cleon Turner, quite a can of worms..........
- My bad In writing about Fridays riots in Sri Lanka, I made it seem like they
were the capper on a week of uprisings stretching from north Africa to the
Middle East to Asia, but that was a mistake. To imply that would be to overlook
the great riot effort turned in by tens of thousands of Serbian opposition
supporters who have rallied against their government, calling for early
elections and economic reforms. This group of outraged Serbs was led in their
uprising by the Serbian Progressive Party. SPP leader Tomislav Nikolic addressed
the crowd in front of the parliament building in the capital, Belgrade. While
the gathering may not have produced the sort of furor and awe-inspiring violence
that the clashes in Egypt have produced this week, the numbers were impressive.
Serbian police estimate at least 55,000 people gathered for the rally, but
objective observers put the number closer to 70,000. In his remarks, Nikolic did
a solid job of inflaming the crowd by calling for higher wages and an end to
government corruption. Claiming that the other side is corrupt and dishonest is
always a solid play and so is referencing the recent protests in Tunisia and
Egypt and saying that governments around the world are learning they need to
listen to the people. Even if your situation has nothing to do with theirs and
nothing in common with what they are going through, try to tie it to a higher
cause. I like it.....check that, I love it. Even though parliamentary elections
are scheduled for 2012 in Serbia, the opposition wants them held sooner. Much
like President Hosni Mubarak is dragging his feet and trying to prolong his
reign of terror in Egypt by promising not to seek re-election but refusing to
resign early, the current regime in Serbia seems content to take the same course
even as rising prices, unemployment and poverty have led to discontent with the
pro-European Union government. Unfortunately, protests have remained mostly
peaceful thus far and only a handful of dissidents have been arrested. The time
has come to change that if those demanding change actually want to see it
happen............
- How do you know your life is waaaaaay out of control? When youre texting
multiple porn stars from rehab to inform them that your partying days are
finished, thats when. Im looking right at you, Charlie Sheen (not that I needed
to specify) because youre the one breaking out the BlackBerry from Promises or
whatever rehab facility youve checked in to this time and firing off texts to
Bambi, Ginger, Destiny and the girls to let them know that no longer will you be
renting $1,000-a-night hotel room with hot tubs and balconies and using those
rooms to have massive porn-star-and-coke orgies until you pass out and are
rushed to the hospital. On some level, I suppose you could give the "Two and a
Half Men" star credit for attempting to get clean and return to the show by the
end of February, but thats the sort of vow were heard from Sheen before and it
always ends the same way - with him face down in a pile of the Bolivian marching
powder, surrounded by women who take some on film from strangers for money. But
hey, maybe this is that moment of clarity for Sheen, the one where everything
comes into focus. Lets check out his texts to his porn star pals: "Please lose
the number, we are closed ... please drive through ... thank you," he wrote to
one. "Right now we are on lockdown," he texted another. Hang on.....right now?
So youre on lockdown for the time being, but maybe not for long? And no, I dont
care that sheen urged these women not to contact him when his treatment ends.
There are too many porn stars out there and too much Colombian nose candy to be
snorted for Sheen to stay down for too long. Yes, an alleged 36-hour cocaine and
drinking bender with several porn actresses led to his hospitalization Jan. 28,
but coke addicts are not renowned for their commitment to anything but blow and
a relapse would surprise no one. On account of not wanting to see anyone snort
themselves into an early grave, I hope Im wrong, but I doubt it............
- One of my biggest pet peeves in life: people who pretend that a) dogs are
human members of their family or b) anyone who acts as if fictional characters
are real. This story involves the latter half of that beef and it centers on
Mattel, the world's largest toy company, which has launched a digital marketing
campaign in hopes of reuniting none other than Barbie and Ken. If you remember,
Mattel oebroke up the two plastic dolls on Valentine's Day in 2004. Since then,
they have led separate, but successful lives. However, Mattel has pretended that
Ken is something other than an overpriced piece of plastic crap made by
sweatshop workers in Indonesia and had him revamping his mind, body and soul to
win Barbie back since 2006. That quest has now kicked into high gear, as Ken
hopes to win back his plastic woman in time for Valentine's Day, with a little
help from the social networking universe. Thats right, Mattel is asking
Facebook, Twitter, Foursquare and YouTube losers who have far, far too much time
on their hands and have wasted a sufficient amount of time on Facebook oeYes/No
quizzes and oeLike my status and Ill post on your wall ploys to vote on whether
Barbie should "take Ken back" or not. From those platforms, losers are directed
to barbieandken.com, where users can vote and check out a Love-O-Meter, gauging
voters' feelings on the topic. The campaign marks Ken's 50th anniversary and
comes just in time for the release of a new "Sweet Talking Ken" doll that Mattel
describes as "the ultimate boyfriend for every occasion," because he "says
whatever you want him to say!" Oh Mattel, how I love your feeble attempts and
relationship humor. The extent of the online world Mattel has crafted for Ken is
truly disturbing. On Facebook, Twitter and Foursquare, fans can follow Ken's
adventures to win back the love of his plastic, inanimate life, follow along
with tweets promoting his romantic efforts and even get involved in a text
campaign, where users can text THUMBS UP or THUMBS DOWN to 51684 to vote on
whether the two dolls should get together again. According to the tiny plastic
dolls Twitter page, Ken is also busy following his favorite sports team, the
Lakers, and reading Men's Health and Esquire. Hes oevisited the Metropolitan
Museum of Art in an attempt to infuse culture into his fake life. Sadly, there
are kooks out there who are actually interacting with Ken as if they would a
real person. Oh, and Ken is an Apple fan, using a MacBook Prop and enjoying his
Internet time by browsing on Google (NASDAQ:GOOG) Chrome. Mattel has really
embarrassed itself on this whole project, going back to last year's Fashion's
Night Out event in New York City where it staged a "Catch Me If You Ken"
promotion. Perhaps the most absurd part of the show has been Ken appearing on
Canadian entertainment show ETalk and buying a spot in Us Weekly to confess his
love. Now please excuse me while I go find something to vomit into............
Newstex ID: CYNC-0001-100440633
LOAD-DATE: February 6, 2011
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not necessarily
the views of Newstex or its re-distributors. Posts from such authors are
provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs on Demand® are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs on Demand® is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs on Demand® shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs on Demand®. Reader's comments reflect their
individual opinion and their publication within Blogs on Demand® shall not infer
or connote an endorsement by Newstex or its re-distributors of such reader's
comments or views. Newstex and its re-distributors expressly reserve the right
to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2011 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2011 Cynic Central
73 of 998 DOCUMENTS
Star-News (Wilmington, NC)
February 1, 2011 Tuesday
1ST Edition
SECTION: Pg. 2C
LENGTH: 430 words
Taurasi denies taking modafinil
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told the Associated Press by
telephone Sunday night from her parents' home in Chino, Calif.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
said she intends to return to the WNBA when the season begins in June.
Tennis rankings truly global
LONDON | For the first time, the top 10 players in the women's tennis rankings
represent 10 different countries.
Eleven different nations are represented among the top 11 spots and 30 different
countries among the top 60 in Monday's rankings.
"Having 10 different players represent the top 10 rankings shows how truly
global tennis has become," WTA Chair and CEO Stacey Allaster said.
Denmark's Caroline Wozniacki remained No. 1, followed by Australian Open
champion Kim Clijsters of Belgium, Russia's Vera Zvonareva, Italy's Francesca
Schiavone and Australia's Sam Stosur.
The next five: Venus Williams of the United States, China's Li Na, Jelena
Jankovic of Serbia, Victoria Azarenka of Belarus and Poland's Agnieszka
Radwanska. Israel's Shahar Peer moved to a career high of No. 11.
King's son: Mets' talk premature
NEW YORK | Martin Luther King Jr.'s oldest son says any discussion of his
potential interest in becoming a minority owner of the New York Mets is
premature.
Martin Luther King III said he was contacted Saturday by television executive
Larry Meli, who is interested in putting together a group that would include
former Mets first baseman Ed Kranepool and Donn Clendenon Jr., whose father was
MVP of the Mets' 1969 World Series victory.
King said he encouraged Meli because it would increase diversity. But King also
said he was not actively putting together a group.
in other baseball news | Pitcher R.A. Dickey has agreed to a $7.8 million,
two-year contract with the New York Mets and outfielder Angel Pagan has agreed
to a $3.5 million, one-year deal. Dickey, a 36-year-old knuckleballer who
revived his career last season, gets a $1 million signing bonus. ...
Right-hander Edinson Volquez and the Cincinnati Reds have agreed to a one-year
contract worth $1,625,000. The deal, which avoided salary arbitration, includes
$50,000 in performance bonuses: $25,000 each for 24 and 28 starts.
- From wire service reports
LOAD-DATE: February 4, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2011 Star-News, Inc.
All Rights Reserved
74 of 998 DOCUMENTS
The Associated Press
January 31, 2011 Monday 04:00 AM GMT
AP Interview: Taurasi denies taking modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 777 words
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told The Associated Press by
telephone Sunday night from her parents' home in Chino, Calif.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
75 of 998 DOCUMENTS
The Associated Press
January 31, 2011 Monday 06:52 PM GMT
AP Interview: Taurasi denies taking stimulant
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 892 words
Diana Taurasi insists she did nothing wrong.
The former Connecticut women's basketball star says she hadn't even heard of the
banned stimulant modafinil until she found out she had tested positive for it.
And no matter what those results showed, Taurasi is adamant that she never used
performance-enhancing drugs.
"I've never needed anything to help me. Only thing that I'm guilty of is taking
too many jump shots," she told The Associated Press by telephone Sunday night
from her parents' home in Chino, Calif.
In her first interview since testing positive in December for modafinil, Taurasi
and her lawyer blamed the Turkish lab where the sample was analyzed.
"There's no way I've ever taken anything," she said.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward.
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce this month
after both her A and B samples tested positive. The Turkish federation still
hasn't announced a punishment the organization was awaiting a response from
Taurasi. Her lawyer, Howard Jacobs, said it was delivered Monday. Despite
reports of Taurasi's positive test surfacing last month, Jacobs only received
the official report from the federation on Wednesday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
WADA spokesman Catherine Coley wrote in an e-mail to the AP that the
organization won't comment until the case is resolved "in order to protect the
integrity of the proceedings."
For Taurasi's part, her lawyers noted she passed a polygraph test and that the
Turkish lab was suspended by WADA for three months in 2009. The player's legal
team also contends that the lab has failed to properly identify modafinil and
that there are questions about the chain of custody for Taurasi's test.
After Taurasi tested positive, two of her teammates in Turkey refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first time Taurasi has run into trouble during her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it might be tough to get rid of the stigma that she's
doping even if she's vindicated.
"I trust that the truth will come out," she said. "At the end of the day you can
try and convince the whole world, but if you know it's true and you've never
taken performance-enhancing drugs, that's what you have to live by."
LOAD-DATE: February 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
76 of 998 DOCUMENTS
The Bismarck Tribune
January 31, 2011 Monday
SECTION: SPORTS
LENGTH: 764 words
Taurasi denies taking modafinil
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she said Sunday.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi intends to return to the WNBA when the season begins in June. The
Phoenix guard has led the league in scoring the last four seasons and signed a
multiyear extension with the Mercury.
The 28-year-old also plans to play for the U.S. team and Geno Auriemma in the
2012 Olympics.
She's already helped the Americans win the last two gold medals. Taurasi has
talked to Auriemma, who coached her in college, at length since she tested
positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment - the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2011 The Bismarck Tribune, a division of Lee Enterprises
All Rights Reserved
77 of 998 DOCUMENTS
Jezebel
January 31, 2011 Monday 2:21 PM EST
Could Diana Taurasi Be Exonerated For Doping? [Sports]
LENGTH: 515 words
Jan. 31, 2011 (Gawker Media delivered by Newstex) --
Basketball star Diana Taurasi tested positive for a banned drug, and her shot at
the 2012 Olympics could be in jeopardy. But she swears she didn't take anything
" we asked an expert if she could be telling the truth.
The former UConn star dropped from her Turkish team earlier this month when a
second sample of her urine tested positive for the banned stimulant modafinil.
The Turkish league hasn't formally suspended her, but if they do, she could be
barred from competing in the 2012 Olympics " any suspension of six months or
longer would make her ineligible. Yesterday, she told the AP she hadn't taken
the drug: "I've never needed anything to help me. Only thing that I'm guilty of
is taking too many jump shots." And her lawyer Howard Jacobs is projecting
confidence, saying, "This will be resolved well in advance of 2012." So could
Taurasi really be innocent?
Daniel M. Rosen, author of Dope: A History of Performance Enhancement in Sports
from the Nineteenth Century to Today told me Taurasi could be telling the truth.
He explains,
Lab testing is a curious thing. One of the things we need to know about it is
that no test is perfect. Just because the A and the B samples actually give the
same result doesn't necessarily mean that the result is correct. There are these
funny things called false positives. [...] The fact that the lab got the same
result both times only means that the test was consistent, but the way the
anti-doping system works is that there's really no taking into account the idea
of false positives, [...] so if the lab says you're positive, you're basically
screwed.
And even if modafinil did show up in Taurasi's bloodstream, she might not have
intentionally put it there. Rosen gave me numerous examples of athletes who
tested positive for banned substances after accidentally consuming them in
supplements, over-the-counter medications, and even contaminated meat. If
Taurasi can show that she inadvertently ingested the modafinil, she might be
able to get a reduced punishment. Her best shot at full exoneration, though, is
to show sloppy handling of her sample or some "break in the chain of custody"
that might have led to contamination. Jacobs notes that the lab in question has
been suspended in the past by the World Anti-Doping Agency " Rosen says such
suspensions can occur for a variety of reasons, including simply not performing
enough tests, but questions about the lab's bona fides could help Taurasi's
defense.
When it comes to an Olympic bid, though, time is not on her side. Says Rosen,
"some of these appeals take forever, and it all depends on how fast the various
arbitration panels move, and how fast the arbitrators come up with their
decisions." Even if Taurasi's appeal makes it all the way to the highest
authority, Court of Arbitration for Sport, their decision could take six months.
So despite Jacobs's optimism, Rosen says, "I'm afraid that she's probably not
going to be able to compete."
AP Interview: Taurasi Denies Taking Stimulant [AP]
Newstex ID: GAWK-0016-100296348
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not necessarily
the views of Newstex or its re-distributors. Posts from such authors are
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such blog content. All content on Blogs on Demand® shall be construed as
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PUBLICATION-TYPE: Web Blog
Copyright 2011 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2011 Jezebel
78 of 998 DOCUMENTS
Associated Press Worldstream
January 31, 2011 Monday 4:02 AM GMT
AP Interview: Taurasi denies taking modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 773 words
Women's basketball star Diana Taurasi is adamant: No matter what the test
results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told The Associated Press by
telephone Sunday from her parents' home in California.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
79 of 998 DOCUMENTS
Associated Press Online
January 31, 2011 Monday 6:53 PM GMT
AP Interview: Taurasi denies taking stimulant
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 892 words
Diana Taurasi insists she did nothing wrong.
The former Connecticut women's basketball star says she hadn't even heard of the
banned stimulant modafinil until she found out she had tested positive for it.
And no matter what those results showed, Taurasi is adamant that she never used
performance-enhancing drugs.
"I've never needed anything to help me. Only thing that I'm guilty of is taking
too many jump shots," she told The Associated Press by telephone Sunday night
from her parents' home in Chino, Calif.
In her first interview since testing positive in December for modafinil, Taurasi
and her lawyer blamed the Turkish lab where the sample was analyzed.
"There's no way I've ever taken anything," she said.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward.
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce this month
after both her A and B samples tested positive. The Turkish federation still
hasn't announced a punishment the organization was awaiting a response from
Taurasi. Her lawyer, Howard Jacobs, said it was delivered Monday. Despite
reports of Taurasi's positive test surfacing last month, Jacobs only received
the official report from the federation on Wednesday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
WADA spokesman Catherine Coley wrote in an e-mail to the AP that the
organization won't comment until the case is resolved "in order to protect the
integrity of the proceedings."
For Taurasi's part, her lawyers noted she passed a polygraph test and that the
Turkish lab was suspended by WADA for three months in 2009. The player's legal
team also contends that the lab has failed to properly identify modafinil and
that there are questions about the chain of custody for Taurasi's test.
After Taurasi tested positive, two of her teammates in Turkey refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first time Taurasi has run into trouble during her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it might be tough to get rid of the stigma that she's
doping even if she's vindicated.
"I trust that the truth will come out," she said. "At the end of the day you can
try and convince the whole world, but if you know it's true and you've never
taken performance-enhancing drugs, that's what you have to live by."
LOAD-DATE: February 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
80 of 998 DOCUMENTS
Associated Press Online
January 31, 2011 Monday 9:20 AM GMT
AP Interview: Taurasi denies taking modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 777 words
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told The Associated Press by
telephone Sunday night from her parents' home in Chino, Calif.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: February 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
81 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 31, 2011 Monday 4:00 AM GMT
AP Interview: Taurasi denies taking modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 777 words
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told The Associated Press by
telephone Sunday night from her parents' home in Chino, Calif.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
82 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 31, 2011 Monday 4:00 AM GMT
LENGTH: 810 words
BC-BKL--Taurasi Speaks, 1st Ld-Writethru,0958
AP Interview: Taurasi denies taking modafinil
2030
Eds: Updates with details, quotes.
AP Photo NY157
sptd/rrusso fasst4921
By DOUG FEINBERG
AP Basketball Writer
Former UConn women's basketball star Diana Taurasi is adamant: No matter what
the test results showed, she never used performance-enhancing drugs.
"There's no way I've ever taken anything," she told The Associated Press by
telephone Sunday night from her parents' home in Chino, Calif.
In her first interview since testing positive in December for the stimulant
modafinil, Taurasi and her lawyer blamed the Turkish lab where the sample was
analyzed.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward."
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce earlier this
month after both her and A and B samples tested positive. The Turkish federation
still hasn't announced a punishment the organization was awaiting a response
from Taurasi, and her lawyer, Howard Jacobs, said it would be delivered by
Monday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
Efforts to reach WADA officials by telephone for comment were not immediately
successful.
After Taurasi's positive test, two of her Turkish teammates refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said. "I've never needing anything to help me. Only thing that I'm guilty of is
taking too many jump shots.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first trouble Taurasi has run into trouble in her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it may be tough to get rid of the stigma that she's doping
even if she's vindicated.
"I trust that the truth will come out. At the end of the day you can try and
convince the whole world but if you know it's true and you've never taken
performance-enhancing drugs that's what you have to live by."
LOAD-DATE: January 31, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
83 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 31, 2011 Monday 6:53 PM GMT
AP Interview: Taurasi denies taking stimulant
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 892 words
Diana Taurasi insists she did nothing wrong.
The former Connecticut women's basketball star says she hadn't even heard of the
banned stimulant modafinil until she found out she had tested positive for it.
And no matter what those results showed, Taurasi is adamant that she never used
performance-enhancing drugs.
"I've never needed anything to help me. Only thing that I'm guilty of is taking
too many jump shots," she told The Associated Press by telephone Sunday night
from her parents' home in Chino, Calif.
In her first interview since testing positive in December for modafinil, Taurasi
and her lawyer blamed the Turkish lab where the sample was analyzed.
"There's no way I've ever taken anything," she said.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward.
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce this month
after both her A and B samples tested positive. The Turkish federation still
hasn't announced a punishment the organization was awaiting a response from
Taurasi. Her lawyer, Howard Jacobs, said it was delivered Monday. Despite
reports of Taurasi's positive test surfacing last month, Jacobs only received
the official report from the federation on Wednesday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
WADA spokesman Catherine Coley wrote in an e-mail to the AP that the
organization won't comment until the case is resolved "in order to protect the
integrity of the proceedings."
For Taurasi's part, her lawyers noted she passed a polygraph test and that the
Turkish lab was suspended by WADA for three months in 2009. The player's legal
team also contends that the lab has failed to properly identify modafinil and
that there are questions about the chain of custody for Taurasi's test.
After Taurasi tested positive, two of her teammates in Turkey refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first time Taurasi has run into trouble during her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it might be tough to get rid of the stigma that she's
doping even if she's vindicated.
"I trust that the truth will come out," she said. "At the end of the day you can
try and convince the whole world, but if you know it's true and you've never
taken performance-enhancing drugs, that's what you have to live by."
LOAD-DATE: February 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
84 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 31, 2011 Monday 6:53 PM GMT
LENGTH: 935 words
BC-BKL--Taurasi Speaks, 1st Ld-Writethru,1172
AP Interview: Taurasi denies taking stimulant
2030
Eds: Updates with WADA comment and details of Taurasi's defense.
AP Photo NY157
sptd/jaffleck sptd/mfitzpatrick sptd/rrusso fasst4921
By DOUG FEINBERG
AP Basketball Writer
Diana Taurasi insists she did nothing wrong.
The former Connecticut women's basketball star says she hadn't even heard of the
banned stimulant modafinil until she found out she had tested positive for it.
And no matter what those results showed, Taurasi is adamant that she never used
performance-enhancing drugs.
"I've never needed anything to help me. Only thing that I'm guilty of is taking
too many jump shots," she told The Associated Press by telephone Sunday night
from her parents' home in Chino, Calif.
In her first interview since testing positive in December for modafinil, Taurasi
and her lawyer blamed the Turkish lab where the sample was analyzed.
"There's no way I've ever taken anything," she said.
Taurasi is regarded by many as one of the best women's players in the world. She
was the first prominent WNBA player to test positive for a banned substance.
Taurasi said she intends to return to the WNBA when the season begins in June.
The Phoenix guard has led the league in scoring the last four seasons and signed
a multiyear extension with the Mercury last August.
The 28-year-old also plans to play for the U.S. team and coach Geno Auriemma in
the 2012 Olympics. She's already helped the Americans win the last two gold
medals. Taurasi has talked to Auriemma, who coached her in college, at length
since she tested positive. He said he'll stand by her.
"My goal has been to play basketball," she said. "Things have come up in my
life, but that's life for you. ... This one was an unexpected one. I've been
doing the right thing for my career. I'll take this and move forward.
"I went from being really angry to wondering, 'Why me?' I won't let it bring me
down," she said.
Taurasi's contract was terminated by the Turkish club Fenerbahce this month
after both her A and B samples tested positive. The Turkish federation still
hasn't announced a punishment the organization was awaiting a response from
Taurasi. Her lawyer, Howard Jacobs, said it was delivered Monday. Despite
reports of Taurasi's positive test surfacing last month, Jacobs only received
the official report from the federation on Wednesday.
Taurasi faces a ban of up to two years and said she will appeal any suspension.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"This will be resolved well in advance of 2012," Jacobs said. "My understanding
is that we have the right of appeal to the sport of arbitration body in Turkey.
That could take a couple of months. All the appeals should be done by the end of
this year."
Taurasi said she was at her home in Turkey, on her couch, when the Fenerbahce
general manager handed her the paper stating that she had tested positive for
modafinil.
Taurasi said the news shocked her.
"I had never heard of it and couldn't pronounce it," she said. "I had to Google
it to find out the side effects. I never have come in contact with it."
The drug has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances. Modafinil is used to counter excessive sleepiness due to
narcolepsy, shift-work sleep disorder or sleep apnea, according to drug
manufacturers.
Jacobs said he's handled about 75 athlete drug cases, including those of Floyd
Landis and Marion Jones. He's questioning the lab's handling of Taurasi's sample
and pointed out that it had been suspended by WADA.
WADA spokesman Catherine Coley wrote in an e-mail to the AP that the
organization won't comment until the case is resolved "in order to protect the
integrity of the proceedings."
For Taurasi's part, her lawyers noted she passed a polygraph test and that the
Turkish lab was suspended by WADA for three months in 2009. The player's legal
team also contends that the lab has failed to properly identify modafinil and
that there are questions about the chain of custody for Taurasi's test.
After Taurasi tested positive, two of her teammates in Turkey refused to have
their samples examined by that same lab.
"I have the most respect for the testing process. When it's not done the right
way, when protocol isn't followed, I do have some problems with it," Taurasi
said.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
This isn't the first time Taurasi has run into trouble during her career. She
served one day in jail and was suspended by the Mercury for two games in 2009
after pleading guilty to a DUI charge.
"The DUI was a mistake I made and I owned up to and I did my time," she said.
"That really did help me in the long run growing up as a person. This is
different, waking up one morning and having something pinned on you that you had
no clue about. It's been a difficult month coming to terms with everything. I
know I've never taken it."
Taurasi, who said she's been tested at least three times a year since joining
the WNBA, knows that it might be tough to get rid of the stigma that she's
doping even if she's vindicated.
"I trust that the truth will come out," she said. "At the end of the day you can
try and convince the whole world, but if you know it's true and you've never
taken performance-enhancing drugs, that's what you have to live by."
LOAD-DATE: February 1, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
85 of 998 DOCUMENTS
Indian Patents News
January 25, 2011 Tuesday 6:30 AM EST
Cephalon Inc. Files Patent Application for Methods for the Separation of
Modafinil
LENGTH: 258 words
New Delhi, Jan. 25 -- USA based Cephalon Inc. filed patent application for
methods for the separation of modafinil. The inventors are Wilhelm Hauck, Oliver
Ludemann-Hombourger, Yvan Ruland, Nelson Landmesser and John Mallamo.
Cephalon Inc. filed the patent application on Feb. 7, 2007. The patent
application number is 465/KOLNP/2007 A. The international classification numbers
are C07B57/00 and C07C317/24.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention is directed to a process for the isolation of the enantiomeric
forms of modafinil with high enantiomeric purity and high overall yields by
means of a continuous chromatographic process."
Cephalon, Inc. is an international biopharmaceutical company engaged in the
discovery, development and commercialization of products in four core
therapeutic areas: central nervous system (CNS), pain, oncology and inflammatory
disease. In addition to conducting an active research and development program,
it markets seven products in the United States and numerous products in various
countries throughout Europe and the world. Its principal product are its
wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and NUVIGIL
(armodafinil) Tablets [C-IV], which comprised 51% of its total consolidated net
sales during the year ended December 31, 2009. During 2009, Cephalon, Inc.
acquired an exclusive, worldwide license to the ImmuPharma investigational
compound, LUPUZOR, which is in Phase IIb development for the treatment of
systemic lupus erythematosus.
LOAD-DATE: January 25, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
86 of 998 DOCUMENTS
Chicago Daily Herald
January 8, 2011 Saturday
L2 Edition
Taurasi's breach damages WNBA
SECTION: SPORTS; Pg. 2
LENGTH: 587 words
What a dope Diana Taurasi appears to be.
On Thursday, Taurasi, arguably the best female basketball player in the world,
had her contract with the Turkish team she plays for during the WNBA's
off-season voided. For doping.
She has reportedly denied the charges in conversations with her former college
coach, Geno Auriemma of Connecticut. It will be interesting to see what her next
move is.
For now, this certainly is a surreal development, to say the least.
In the world of professional sports, women's basketball is the closest thing to
squeaky clean.
For more than a decade, the WNBA has being trying to emulate its professional
sports brethren by developing a quality and high-level sports entertainment
option.
Just without the drugs.
It's no secret that just about every men's professional sports league has had
bouts with drug problems over the course of their histories. From Major League
Baseball to the NFL to the NBA, we've seen athletes ruin their careers with
steroids, hard-core street drugs and even the misuse of prescription
medications.
Fifteen years into its existence, the WNBA hasn't really had to face those
demons.
"I'd say that only 2 to 5 percent of the players in the WNBA even risk violating
the substance policy," said Chicago Sky strength and conditioning coach Ann
Crosby. "When I say that, people are always like, 'Really?' But it's true. The
WNBA really doesn't have the problems that a lot of sports leagues have with
drugs."
Yes, but when it rains on the WNBA, it apparently pours.
This isn't a benchwarmer in trouble. This is the face of the league.
Not good news for the WNBA.
Taurasi, who has been an A-list superstar ever since she was drafted by the
Phoenix Mercury in 2004, has tested positive for the banned stimulant modafinil.
On Thursday, her second sample, or "B" sample, confirmed what her original
sample read in November. Taurasi's team in Turkey made its decision to terminate
her contract after the "B" sample also came back positive.
Modafinil is used to counter excessive sleepiness due to narcolepsy, sleep apnea
and other sleep disorders.
It is on the World Anti-Doping Agency's list and is the substance that got
American sprinter Kelli White into trouble in 2004. She won gold medals in the
100 and 200 meters at the 2003 World Championships. But those results were
stricken from the records in the wake of news that White tested positive for
modafinil as well as the steroid THG.
White received a two-year ban from competition.
Taurasi also faces tough repercussions. She could be banned for up to two years
from the Turkish league. And that would comprise her standing with the U.S.
women's national basketball team for the 2012 Olympics in London.
Already a two-time gold medalist, Taurasi would not be allowed to participate in
any Olympic event if she is saddled with a ban of two years or more by any other
athletic agency.
On top of all that, Taurasi would likely be faced with a punishment from the
WNBA for the 2011 season.
"She could be hit with a triple whammy, and that's such a bummer for the league
because she is such a draw. People come out to see her play," said Crosby, who
confirmed that the Sky has never had a substance violation in its six years of
existence.
Crosby helps to ensure every Sky player is in compliance.
"I'm not sure how the WNBA will deal with it, but I would think she would get
some kind of suspension, whether it be for two or three games or more," Crosby
said. "Things like this are really dealt with on a case-by-case basis."
pbabcock@dailyherald.com
LOAD-DATE: January 10, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2011 Paddock Publications, Inc.
87 of 998 DOCUMENTS
The New York Times
January 7, 2011 Friday
Late Edition - Final
Taurasi's Deal Terminated As Test Confirms Violation
BYLINE: By JERE LONGMAN
SECTION: Section B; Column 0; Sports Desk; Pg. 11
LENGTH: 373 words
Diana Taurasi's Olympic and professional basketball career grew more uncertain
Thursday when the Turkish basketball federation said it had confirmed her doping
violation and that her club team in Istanbul had terminated her contract.
Taurasi, 28, considered by many the world's top women's basketball player, had
been suspended from her Istanbul team since the ''A'' sample of a two-part
urinalysis tested positive last month for the banned stimulant modafinil.
The ''B'' sample also tested positive, the Turkish basketball federation said
Thursday on its Web site. The federation also posted a notice saying that
Taurasi's team, Fenerbahce, had dropped her.
No sanctions were announced, but Taurasi now faces a suspension from
international competition of up to two years, according to the rules of the
World Anti-Doping Agency. Through her lawyer, she has denied knowingly taking
any prohibited substances.
A suspension longer than six months would leave Taurasi ineligible to compete
for the United States at the 2012 London Games, according to a rule implemented
by the International Olympic Committee. Any proposed suspension by the Turkish
federation was not likely to be for less than six months, said Taurasi's lawyer,
Howard L. Jacobs. She could appeal any suspension. Jacobs said he could not take
his next step until he received official notification of a doping violation.
''At some point, they're going to have to tell me and provide me with lab
documents,'' Jacobs said. ''So far that has not happened.''
Earlier this week, Geno Auriemma, who coached Taurasi at Connecticut and will be
the 2012 United States Olympic coach, said that Taurasi told him she never took
modafinil, an alertness drug designed to treat sleep disorders. Taurasi plays
for the Phoenix Mercury of the W.N.B.A. during the summer and for Fenerbahce
during the league's off-season. It remained unclear whether Taurasi's W.N.B.A.
eligibility would be affected.
The Turkish lab that performed Taurasi's urinalysis has previously been
suspended for a brief period by WADA, Jacobs noted. Two of Taurasi's teammates
at Fenerbahce recently agreed to provide urine samples only if they would be
tested in Germany.
''The whole thing is unbelievably stressful,'' Jacobs said.
URL: http://www.nytimes.com
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: Diana Taurasi, playing in a W.N.B.A. playoff game for the
Phoenix Mercury in 2010, tested positive for the stimulant modafinil.
(PHOTOGRAPH BY ERIC GAY/ASSOCIATED PRESS)
PUBLICATION-TYPE: Newspaper
Copyright 2011 The New York Times Company
88 of 998 DOCUMENTS
The Associated Press
January 6, 2011 Thursday 04:21 PM GMT
Taurasi has Turkish contract voided for doping
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 447 words
DATELINE: ANKARA, Turkey
American basketball star Diana Taurasi had her contract terminated by Turkish
club Fenerbahce on Thursday after her "B" sample tested positive for doping.
The Istanbul-based club made its decision after the Turkish Basketball
Federation announced the results of the doping test on its website. Taurasi
faces a ban of up to two years, putting in jeopardy her chances of playing for
the United States at the 2012 London Olympics.
The federation has not announced a decision on Taurasi's punishment.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil following a Turkish league game on Nov. 13. Taurasi had been suspended
by Fenerbahce ever since.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games. Taurasi helped the
Americans win gold medals at the past two Olympics and was the leading scorer
when the U.S. won the women's world championships.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
On Tuesday, Geno Auriemma, the United States coach for the 2012 Olympics, said
the former University of Connecticut star told him that she did not take
modafinil. He also said he didn't know if Taurasi had any problems with
sleeplessness.
One of the most decorated women's players in history, Taurasi led the WNBA in
scoring for a league-record fourth straight year, averaging 22.6 points last
season. The five-time All-Star and two-time WNBA champion signed a multiyear
contract extension with Phoenix in August.
The Mercury have not commented publicly on the doping case.
Taurasi is one of many American stars who play overseas in the winter because
salaries are significantly higher than in the WNBA. She played in Russia for
four years for Spartak before joining the Turkish league this season.
Taurasi was leading the league in scoring with 24.6 points per game.
Two of Taurasi's teammates at Fenerbahce have resisted doping tests in Turkey
because they do not trust the lab that tests the samples. Australian player
Penny Taylor and Czech teammate Hana Horakova provided samples only after the
Turkish federation agreed to send them to Germany for testing at a lab in
Cologne.
The two players were tested after Fenerbahce's Turkish league game on Sunday.
Modafinil has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
89 of 998 DOCUMENTS
Indian Patents News
January 6, 2011 Thursday 6:30 AM EST
Organisation De Synthese Mondiale Orsymonde Files Patent Application for
Modafinil Synthesis Process
LENGTH: 140 words
New Delhi, Jan. 6 -- France based Organisation De Synthese Mondiale Orsymonde
filed patent application for modafinil synthesis process. The inventor is Rose
Sebastien.
Organisation De Synthese Mondiale Orsymonde filed the patent application on Nov.
16, 2006. The patent application number is 3018/CHENP/2005 A. The international
classification number is C07C 315/00.
According to the Controller General of Patents, Designs & Trade Marks, "The
invention relates to a process for preparing modafinil having a defined
granulometry which comprises the steps of: a) preparing a solution of DMSAM ; b)
contacting the solution obtained with NH3 at a predetermined temperature and a
predetermined stirring; and c) isolating the modafinil formed, wherein said
temperature and said stirring are predetermined in order to obtain said defined
granulometry."
LOAD-DATE: January 6, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
90 of 998 DOCUMENTS
Associated Press Worldstream
January 6, 2011 Thursday 4:03 PM GMT
Taurasi's 'B' sample positive for banned stimulant
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 435 words
DATELINE: ANKARA Turkey
American basketball star Diana Taurasi's "B" sample tested positive for doping,
a result which threatens her chances of playing for the United States at the
2012 London Olympics.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil following a Turkish league game on Nov. 13. The Fenerbahce player, who
faces a two-year doping ban, had her contract with the club terminated Thursday
following the announcement of the positive result on the website of the Turkish
Basketball Federation.
The federation, however, has yet to make a decision on Tauarsi's punishment.
If Taurasi is suspended for more than six months it would put her 2012 Olympic
status in jeopardy. She helped the team win gold medals at the past two Olympics
and was the leading scorer at the women's world championships, which the
Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
On Tuesday, Geno Auriemma, the United States coach for the 2012 Olympics, said
the former University of Connecticut star told him that she did not take
modafinil. He also said he didn't know if Taurasi had any problems with
sleeplessness.
Taurasi led the WNBA in scoring for a league-record fourth straight year,
averaging 22.6 points. The five-time All-Star and two-time WNBA champion signed
a multiyear contract extension with Phoenix in August.
Taurasi is one of many American stars who play overseas in the winter because
salaries are significantly higher than in the WNBA. She played in Russia for
four years for Spartak before joining the Turkish league this season. Taurasi
was leading the league in scoring with 24.6 points per game.
Two of Taurasi's teammates at Fenerbahce have resisted doping tests in Turkey
because they do not trust the lab that tested her samples. Australian player
Penny Taylor and Czech teammate Hana Horakova provided samples only after the
Turkish federation agreed to send them to Germany for testing at a lab in
Cologne.
The two players were tested after Fenerbahce's Turkish league game against
Besiktas on Sunday.
Modafinil has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
91 of 998 DOCUMENTS
Associated Press Online
January 6, 2011 Thursday 3:45 PM GMT
Taurasi's 'B' sample positive for banned stimulant
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 440 words
DATELINE: ANKARA Turkey
Diana Taurasi's "B" sample tested positive for doping, putting in jeopardy her
chances of playing for the United States at the 2012 London Olympics.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil following a Turkish league game on Nov. 13. The Fenerbahce player, who
has been provisionally suspended by the team, could now be banned for two years.
The Turkish Basketball Federation, which announced the positive "B" sample
result Thursday on its website, said there was no immediate decision on
Tauarsi's punishment. Fenerbahce said the club would make a final decision on
her case at a later date.
If Taurasi is suspended for more than six months it could keep her from playing
in the 2012 Olympics. She helped the team win gold medals at the past two
Olympics and was the leading scorer at the women's world championships, which
the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
On Tuesday, Geno Auriemma, the U.S. coach for the 2012 Olympics, said the former
University of Connecticut star told him that she did not take modafinil. He also
said he didn't know if Taurasi had any problems with sleeplessness.
Taurasi led the WNBA in scoring for a league-record fourth straight year,
averaging 22.6 points last season. The five-time All-Star and two-time WNBA
champion signed a multiyear contract extension with Phoenix in August.
Taurasi is one of many American stars who play overseas in the winter because
salaries are significantly higher than in the WNBA. She played in Russia for
four years for Spartak before joining the Turkish league this season. Taurasi
was leading the league in scoring with 24.6 points per game.
Two of Taurasi's teammates at Fenerbahce have resisted doping tests in Turkey
because they do not trust the lab that tested her samples. Australian player
Penny Taylor and Czech teammate Hana Horakova provided samples only after the
Turkish federation agreed to send them to Germany for testing at a lab in
Cologne.
The two players were tested after Fenerbahce's Turkish league game on Sunday.
Modafinil has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both of her medals were stripped after she tested positive for the
stimulant.
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
92 of 998 DOCUMENTS
Associated Press Online
January 6, 2011 Thursday 3:59 PM GMT
Taurasi has Turkish contract voided for doping
BYLINE: By SELCAN HACAOGLU, Associated Press
SECTION: SPORTS NEWS
LENGTH: 583 words
DATELINE: ANKARA Turkey
American basketball star Diana Taurasi has had her contract terminated by
Turkish club Fenerbahce after her "B" sample tested positive for doping.
The Istanbul club says the decision was made Thursday following the results
announcement by the Turkish Basketball Federation. Taurasi faces a ban of up to
two years, putting in jeopardy her chances of playing for the United States at
the 2012 London Olympics.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil following a Turkish league game on Nov. 13. Taurasi had been suspended
by Fenerbahce ever since.
The Turkish federation, which announced the positive "B" sample result on its
website, says there has been no immediate decision on Taurasi's punishment.
THIS IS A BREAKING NEWS UPDATE. Check back soon for further information. AP's
earlier story is below.
ANKARA, Turkey (AP) Diana Taurasi's "B" sample tested positive for doping,
putting in jeopardy her chances of playing for the United States at the 2012
London Olympics.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil following a Turkish league game on Nov. 13. The Fenerbahce player, who
has been provisionally suspended by the team, could now be banned for two years.
The Turkish Basketball Federation, which announced the positive "B" sample
result Thursday on its website, said there was no immediate decision on
Tauarsi's punishment. Fenerbahce said the club would make a final decision on
her case at a later date.
If Taurasi is suspended for more than six months it could keep her from playing
in the 2012 Olympics. She helped the team win gold medals at the past two
Olympics and was the leading scorer at the women's world championships, which
the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
On Tuesday, Geno Auriemma, the U.S. coach for the 2012 Olympics, said the former
University of Connecticut star told him that she did not take modafinil. He also
said he didn't know if Taurasi had any problems with sleeplessness.
Taurasi led the WNBA in scoring for a league-record fourth straight year,
averaging 22.6 points last season. The five-time All-Star and two-time WNBA
champion signed a multiyear contract extension with Phoenix in August.
Taurasi is one of many American stars who play overseas in the winter because
salaries are significantly higher than in the WNBA. She played in Russia for
four years for Spartak before joining the Turkish league this season. Taurasi
was leading the league in scoring with 24.6 points per game.
Two of Taurasi's teammates at Fenerbahce have resisted doping tests in Turkey
because they do not trust the lab that tested her samples. Australian player
Penny Taylor and Czech teammate Hana Horakova provided samples only after the
Turkish federation agreed to send them to Germany for testing at a lab in
Cologne.
The two players were tested after Fenerbahce's Turkish league game on Sunday.
Modafinil has been involved in several major doping cases, including that of
American sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both of her medals were stripped after she tested positive for the
stimulant.
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
93 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 6, 2011 Thursday 3:07 PM GMT
Taurasi's 'B' sample positive for banned stimulant
SECTION: SPORTS NEWS
LENGTH: 136 words
DATELINE: ANKARA Turkey
The Turkish Basketball Federation says American star Diana Taurasi's "B" sample
tested positive for doping.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil, following a Turkish league game on Nov. 13. The Fenerbahce player,
who has been provisionally suspended by the team, could be banned for two years.
If Taurasi is suspended for more than six months it would put her 2012 Olympics
status with the U.S. national basketball team in jeopardy.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Taurasi led the WNBA in scoring for a league-record fourth straight year this
past season, averaging 22.6 points. The five-time All-Star signed a multiyear
contract extension with Phoenix in August.
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LANGUAGE: ENGLISH
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The Associated Press State & Local Wire
January 6, 2011 Thursday 3:07 PM GMT
LENGTH: 167 words
BC-BKL--Doping-Taurasi,0289
Taurasi's 'B' sample positive for banned stimulant
2030
Eds: APNewsNow.
AP Photo TXEG107
sptd/dskretta elfd/lon/clehourites fasst4922 fasst4921
ANKARA, Turkey (AP) The Turkish Basketball Federation says American star Diana
Taurasi's "B" sample tested positive for doping.
Taurasi's "A" sample tested positive last month for the banned stimulant
modafinil, following a Turkish league game on Nov. 13. The Fenerbahce player,
who has been provisionally suspended by the team, could be banned for two years.
If Taurasi is suspended for more than six months it would put her 2012 Olympics
status with the U.S. national basketball team in jeopardy.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
Taurasi led the WNBA in scoring for a league-record fourth straight year this
past season, averaging 22.6 points. The five-time All-Star signed a multiyear
contract extension with Phoenix in August.
LOAD-DATE: January 7, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
95 of 998 DOCUMENTS
Indian Patents News
January 5, 2011 Wednesday 6:30 AM EST
Mallinckrodt Inc. Files Patent Application for Improved Process for Preparing
Benzhydrylthioacetamide
LENGTH: 252 words
New Delhi, Jan. 5 -- USA based Mallinckrodt Inc. filed patent application for
improved process for preparing benzhydrylthioacetamide. The inventor is Liang
Sidney.
Mallinckrodt Inc. filed the patent application on April 21, 2006. The patent
application number is 1383/CHENP/2006 A. The international classification number
is C07C317/44.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention is directed to an improved process for preparing modafinil
wherein benzhydrylthioacetate is prepared in high yield and purity by the
reaction of a haloacetate with the reaction product of thiourea and benzhydrol.
The reaction employing the haloacetate is conducted in a solvent comprising an
organic solvent such as methanol having dissolved therein an organic base or an
inorganic basic salt such as sodium bicarbonate. The resulting
benzhydrylthioacetate can be amidated and then oxidized to provide the
pharmaceutical grade modafinil in high yield and purity."
Mallinckrodt, Inc. designs, manufactures, and distributes respiratory care,
imaging products, and prescription pharmaceuticals. It offers contrast media and
delivery systems, radiopharmaceuticals, and urology imaging systems for the
diagnosis and treatment of diseases in various imaging procedures. The company
also provides peptide products, including amino acid derivatives and resins, as
well as solid liquid phase peptides, and hybrid fragment synthesis; and active
pharmaceutical ingredients and specialty generics.
LOAD-DATE: January 5, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Indian Patents News, distributed by Contify.com
All Rights Reserved
96 of 998 DOCUMENTS
Associated Press Worldstream
January 3, 2011 Monday 6:16 PM GMT
Report: Diana Taurasi's B sample also positive
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 494 words
DATELINE: ANKARA Turkey
Diana Taurasi's backup doping sample also came back positive for a banned
substance and the American basketball star faces a possible two-year ban,
Turkish news reports said Monday.
The Turkish basketball federation did not immediately confirm the reports by the
Dogan News agency and private NTV news channel, and neither news outlet cited a
source for their reports. An official at Taurasi's Turkish club, Fenerbahce,
also would not confirm the report and said the team had not yet been notified of
the result.
WNBA standout and former University of Connecticut star Taurasi tested positive
for the stimulant modafinil while playing in Turkey's professional women's
league. She was tested following a league game on Nov. 13 and the positive
result was confirmed last month.
Taurasi had been provisionally suspended by Fenerbahce pending the result of her
"B" sample test, which was analyzed at the doping lab at Hacettepe University in
Ankara.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to drug manufacturers.
The stimulant has been involved in several major doping cases, including that of
U.S. sprinter Kelli White, and is on the World Anti-Doping Agency's list of
banned substances.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
If the positive "B" sample finding is confirmed by Turkey's basketball
federation, it could lead to a ban of up to two years for Taurasi. It could also
put Taurasi's 2012 Olympics standing with the U.S. national basketball team in
jeopardy. She has helped the team win gold medals at the past two Olympics and
was the leading scorer at the women's world championships, which the Americans
won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
Meanwhile, two of Taurasi's teammates at Fenerbahce resisted doping tests in
Turkey because they do not trust the lab that tested her samples, Turkey's
Haberturk newspaper said.
Australian forward Penny Taylor and Hana Horakova of the Czech Republic provided
samples only after the Turkish federation agreed to send them to Germany for
testing at a lab in Cologne.
The two players were tested after Fenerbahce's Turkish league game against
Besiktas late Sunday. A Fenerbahce official confirmed the report.
Taurasi led the WNBA in scoring for a league-record fourth straight year,
averaging 22.6 points per game. The five-time All-Star and two-time WNBA
champion signed a multiyear contract extension with the Phoenix Mercury in
August.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. Taurasi was leading the league in scoring this
season with 24.6 points a game.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries.
LOAD-DATE: January 4, 2011
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2011 Associated Press
All Rights Reserved
97 of 998 DOCUMENTS
Indian Patents News
December 28, 2010 Tuesday 6:30 AM EST
Cephalon Inc Files Patent Application for Modafinil Compositions
LENGTH: 199 words
New Delhi, Dec. 28 -- USA based Cephalon Inc filed patent application for
modafinil compositions. The inventors are Magali Bourghol Hickey, Matthew
Peterson, Orn Almarsson and Mark Oliveria.
Cephalon Inc filed the patent application on Feb. 20, 2006. The patent
application number is 00371/KOLNP/2006 A. The international classification
number is A61K.
According to the Controller General of Patents, Designs & Trade Marks,
"Co-crystals and solvates of racemic, enantiomerically pure and enantiomerically
mixed modafinil are formed and several important physical properties are
modulated. The solubility, dissolution, bioavailability, dose response, and
stability of modafinil can be modulated to improve efficacy in pharmaceutical
compositions."
Cephalon, Inc. (NASDAQ: CEPH) is a U.S. biopharmaceutical company co-founded in
1987 by Dr. Frank Baldino, Jr., a pharmacologist and former scientist with the
DuPont Company, who served as the company's chairman and chief executive officer
until his death in December 2010. The company's name comes from the adjective
"cephalic" meaning "related to the head or brain," and it was established
primarily to pursue treatments for neurodegenerative diseases.
LOAD-DATE: December 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
98 of 998 DOCUMENTS
Indian Patents News
December 27, 2010 Monday 6:30 AM EST
Cephalon Inc Files Patent Application for Modafinil Compositions
LENGTH: 283 words
New Delhi, Dec. 27 -- UAE based Cephalon Inc filed patent application for
modafinil compositions. The inventors are Magali Bourghol Hickey, Matthew
Peterson, Orn Almarssonh and Mark Oliveira.
Cephalon Inc filed the patent application on Sept. 4, 2006. The patent
application number is 2534/KOLNP/2006 A. The international classification number
is C07C 317/10.
According to the Controller General of Patents, Designs & Trade Marks,
"Polymorphs and solvates of racemic, enantiomerieally pure, and enantiomeriealiy
mixed modafinil and formed and discussed, In addition, said forms are described
as useful for the treatment of many conditions including, but not limited to,
narcolepsy."
Cephalon, Inc. (Public, NASDAQ:CEPH) is an international biopharmaceutical
company engaged in the discovery, development and commercialization of products
in four core therapeutic areas: central nervous system (CNS), pain, oncology and
inflammatory disease. In addition to conducting an active research and
development program, it markets seven products in the United States and numerous
products in various countries throughout Europe and the world. Its principal
product are its wakefulness products, PROVIGIL (modafinil) Tablets [C-IV] and
NUVIGIL (armodafinil) Tablets [C-IV], which comprised 51% of its total
consolidated net sales during the year ended December 31, 2009. During 2009,
Cephalon, Inc. acquired an exclusive, worldwide license to the ImmuPharma
investigational compound, LUPUZOR, which is in Phase IIb development for the
treatment of systemic lupus erythematosus. In August 2009, Cephalon, Inc.
acquired Arana Therapeutics Limited. In April 2010, the Company acquired Mepha,
a pharmaceutical company.
LOAD-DATE: December 27, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
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PR Newswire
December 27, 2010 Monday 8:30 AM EST
Cephalon Receives Complete Response Letter for NUVIGIL for the Treatment of
Excessive Sleepiness Associated With Jet Lag Disorder
LENGTH: 822 words
DATELINE: FRAZER, Pa., Dec. 27, 2010
FRAZER, Pa., Dec. 27, 2010 /PRNewswire/ -- Cephalon, Inc. (Nasdaq: CEPH) today
announced that the company received a second Complete Response Letter from the
U.S. Food and Drug Administration (FDA) for the supplemental new drug
application (sNDA) for NUVIGIL(R) (armodafinil) Tablets [C-IV] for the treatment
of patients with excessive sleepiness associated with jet lag disorder resulting
from eastbound travel. In its letter to the company, the FDA reiterated its
previously stated concerns regarding the NUVIGIL sNDA.
"Cephalon believes we met the agreed upon safety and efficacy endpoints in the
NUVIGIL sNDA clinical study conducted under a Special Protocol Assessment.
However, following several conversations with the agency, and given this second
complete response letter, the company believes that further communications with
the FDA will not result in an approval of this application," said Dr. Lesley
Russell, Chief Medical Officer at Cephalon. "As a result, the company is no
longer pursuing this indication."
About NUVIGIL
NUVIGIL is indicated to improve wakefulness in patients with excessive
sleepiness associated with treated obstructive sleep apnea (OSA), shift work
disorder (SWD), or narcolepsy. In patients with OSA, NUVIGIL is used along with
airway treatments for this condition. The NUVIGIL (armodafinil) label includes a
bolded warning for serious or life-threatening rash, including Stevens-Johnson
Syndrome, requiring hospitalization and discontinuation of treatment, that has
been reported in adults in association with the use of modafinil and armodafinil
and in children in association with the use of modafinil, a racemic mixture of S
and R modafinil (the latter is armodafinil, the active ingredient in NUVIGIL).
NUVIGIL is not approved for use in pediatric patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) in labeled indications were headache, nausea, dizziness, and insomnia.
Full prescribing information for NUVIGIL is available at www.nuvigil.com.
About Cephalon, Inc.
Cephalon is a global biopharmaceutical company dedicated to discovering,
developing and bringing to market medications to improve the quality of life of
individuals around the world. Since its inception in 1987, Cephalon has brought
first-in-class and best-in-class medicines to patients in several therapeutic
areas. Cephalon has the distinction of being one of the world's fastest-growing
biopharmaceutical companies, now among the Fortune 1000 and a member of the S&P
500 Index, employing approximately 4,000 people worldwide. The company sells
numerous branded and generic products around the world. In total, Cephalon sells
more than 150 products in nearly 100 countries. More information on Cephalon and
its products is available at www.cephalon.com.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide the Cephalon current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results; prospects for regulatory approval; manufacturing development
and capabilities; market prospects for its products; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
Contacts:
Media:
Candace Steele Flippin
610-727-6231 (office)
csteele@cephalon.com
Investor Relations:
Chip Merritt
610-738-6376 (office)
cmerritt@cephalon.com
Joseph Marczely
610-883-5894 (office)
jmarczely@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media: Candace Steele Flippin, +1-610-727-6231 (office),
csteele@cephalon.com, or Investor Relations: Chip Merritt, +1-610-738-6376
(office), cmerritt@cephalon.com, or Joseph Marczely, +1-610-883-5894 (office),
jmarczely@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: December 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 PR Newswire Association LLC
All Rights Reserved
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The Sunday Times (Australia)
December 26, 2010 Sunday
6 - Early Edition
SHORTPASSES
SECTION: Pg. 105
LENGTH: 397 words
Murphy, Kelly back
V8 SUPERCARS: Holden legend Greg Murphy's career is set to continue with former
teammate Rick Kelly throwing the Kiwi icon a V8 lifeline. The former Bathurst
winner is set to sign with Kelly Brothers Racing in a move that evokes memories
of the famous K-Mart racing team. Murphy and Kelly won back-to-back Bathurst
titles together in 2003-04. The duo will return to the golden days next year,
with the talented veteran joining his former partner in a Pepsi-backed car.
Maradona: I'm clean
SOCCER: Diego Maradona says he is taking the president of the Argentine Football
Association to court, accusing Julio Grondona of spreading false information
about his problems with drugs and alcohol. Maradona says he has not had drugs or
alcohol for six years. Grondona implied in a television interview this week that
Maradona was using again. ``There are reasons for what happens (with Maradona)
and everybody knows them,'' Grondona said.
Taurasi drug shock
BASKETBALL: American star Diana Taurasi tested positive for Modafinil while
playing in a professional women's league in Turkey, the country's federation
said. Neither her lawyer nor her team, Fenerbahce, would confirm Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of US sprinter Kelli White. Modafinil is used to counter
excessive sleepiness due to narcolepsy or sleep apnea.
Smith all-a-Twitter
CRICKET: South African captain Graeme Smith appealed for help on Twitter after
discovering his much-loved Test cap had been stolen ahead of the Second Test
against India. Smith said his green Proteas cap, which he was given for his
first Test in 2002, had gone missing while travelling from Cape Town to Durban
for the match beginning today. ``Realise this is a long shot, but had my test
cap that I've used since my 1st test for proteas stolen on travel up to durbs,''
Smith tweeted.
Leonardo's big leap
SOCCER: Leonardo has crossed the great San Siro divide, with the former AC Milan
coach being named as the successor to Rafael Benitez as boss of Inter Milan. The
appointment makes him the first person to have coached both Milan giants. Long
on personality, short on managerial experience, Leonardo Nascimento de Araujo
was appointed AC Milan manager in May 2009, succeeding Chelsea-bound Carlo
Ancelotti when still lacking the required managerial badges.
LOAD-DATE: December 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: SDT
Copyright 2010 Nationwide News Pty Limited
All Rights Reserved
101 of 998 DOCUMENTS
Buffalo News (New York)
December 25, 2010 Saturday
FINAL EDITION
Around & About / News and notes
SECTION: SPORTS; Pg. C3
LENGTH: 535 words
Heat, Lakers ready to play
Kobe Bryant and Lakers coach Phil Jackson haven't really checked out the Miami
Heat much this season. They've caught late-night highlights and maybe logged a
few minutes with a game from the opposite coast, but not a whole lot more.
It's finally time for the two-time champions to get an up-close look at their
most intriguing challengers.
When LeBron James, Chris Bosh and -- maybe -- Dwyane Wade take on the Lakers in
the NBA's Christmas showcase today (5 p.m., Chs. 7, 11), most players in both
uniforms hesitate to pile any extra significance onto a television-manufactured
event. Most minimize every aspect of it, saying it's no more than a holiday
amusement for fans seeking a break from present-opening and eggnog-drinking.
"I don't think it's a measuring stick for us," James said. "It's just another
game."
Yet competitiveness usually trumps Christmas for elite NBA players. Just ask
Bryant -- or don't, since he tellingly hasn't spoken to the media since getting
ejected from the Lakers' last game.
"The personalities that are going to be matching up in this game, I don't know
if it can get any bigger," said Derek Fisher, the Lakers point guard.
The contest is one of five on the NBA schedule for today; all will be televised.
-----
Taurasi fails test
Diana Taurasi is facing one of the most difficult challenges to her stellar
basketball career.
The WNBA standout and former UConn star tested positive for a mild stimulant
while playing in a pro league in Turkey, her lawyer told The Associated Press on
Thursday night.
Howard Jacobs said Taurasi's "A" sample came back positive from a lab in Turkey
last week. He said the substance "was not a steroid or recreational drug," and
that Taurasi has asked that her "B" sample be tested.
The Turkish basketball federation said Friday that the substance in Taurasi's
positive test was modafinil. Modafinil is used to counter excessive sleepiness
due to narcolepsy, shift work sleep disorder or sleep apnea, according to the
website for prescription drug Provigil, which contains the substance.
Neither Jacobs nor Taurasi's team, Fenerbahce, would confirm it was modafinil,
which has been involved in several major doping cases.
-----
Fay will step down
David Fay is retiring from the U.S. Golf Association, his two decades as
executive director marked by a steady push for golf's return to the Olympics and
for the U.S. Open to be held on golf courses that anyone could play at a
reasonable price.
Fay's announcement Friday was somewhat of a surprise, although he turned 60 two
months ago and said it was an important milestone for cancer survivors. He
joined the USGA in 1978 and became its sixth executive director in 1989, serving
under 12 presidents.
Mike Butz, the deputy executive director since 1995, will take over Jan. 1 until
a national search to find Fay's replacement.
"Things are in good order," Fay said in a statement. "Our senior staff leaders,
each of whom I have put into place, are highly talented and motivated. And
looking ahead, there are a number of multiyear projects on the drawing board ...
which makes this, for me, a good time to move on. Leave on a high note, as
Seinfeld would say."
From News and wire service reports.
LOAD-DATE: December 27, 2010
LANGUAGE: ENGLISH
DOCUMENT-TYPE: Briefs
PUBLICATION-TYPE: Newspaper
Copyright 2010 The Buffalo News
All Rights Reserved
102 of 998 DOCUMENTS
The Houston Chronicle
December 25, 2010 Saturday
3 STAR EDITION
Taurasi's woes compound Positive test could jeopardize Olympic status
BYLINE: CHRONICLE NEWS SERVICES
SECTION: SPORTS; Pg. 2
LENGTH: 436 words
NEW YORK - WNBA standout and former Con- necticut star Diana Taurasi tested
positive for modafinil while playing in a professional women's league in Turkey,
the country's basketball federation said Friday.
Neither her lawyer nor Fenerbahce, her team, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Howard Jacobs, Taurasi's lawyer,
told the Associated Press. "We'll revisit it after the 'B' sample returns. They
shouldn't be speaking about it at all."
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi, 28, has been provisionally suspended pending the testing of her "B"
sample, early next month.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy.
She has helped the team win gold medals at the past two Olympics and was the
leading scorer at the women's world championships, which the Americans won in
early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next Games.
She has missed three games with Fenerbahce. The team's website said she and
another player were asked to submit to a test Nov. 13, after the game against
Istanbul.
It said they were selected as a result of a draw. The other player tested
negative.
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national titles as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
LOAD-DATE: December 27, 2010
LANGUAGE: ENGLISH
GRAPHIC: TAURASI
PUBLICATION-TYPE: Newspaper
Copyright 2010 The Houston Chronicle Publishing Company
All Rights Reserved
103 of 998 DOCUMENTS
Lewiston Morning Tribune (Idaho)
December 25, 2010 Saturday
Officials say substance in Taurasi case is modafinil :Turkish officials claim
U.S. star tested positive for stimulant typically used to treat sleep disorders
BYLINE: DOUG FEINBERG
LENGTH: 735 words
NEW YORK - WNBA standout and former UConn star Diana Taurasi tested positive for
modafinil while playing in a professional women's league in Turkey, the
country's basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
---
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
GRAPHIC: No Caption: Diana Taurasi drives on Laura Summerton during an
exhibition game this year between the U.S. and Australia.
PUBLICATION-TYPE: Newspaper
Copyright 2010 Tribune Publishing Co.
All Rights Reserved
104 of 998 DOCUMENTS
Monterey County Herald (California)
December 25, 2010 Saturday
Taurasi tests positive for stimulant in Turkey
BYLINE: The Monterey County Herald
SECTION: SPORTS
LENGTH: 736 words
NEW YORK (AP) WNBA standout and former UConn star Diana Taurasi tested
positive for modafinil while playing in a professional women's league in Turkey,
the country's basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
GRAPHIC:
PUBLICATION-TYPE: Newspaper
Copyright 2010 The Monterey County Herald
All Rights Reserved
105 of 998 DOCUMENTS
The New York Times
December 25, 2010 Saturday
Late Edition - Final
Positive Test Could Mean Olympic Ban For Taurasi
BYLINE: By JERE LONGMAN
SECTION: Section B; Column 0; Sports Desk; Pg. 7
LENGTH: 958 words
The Turkish basketball federation said Friday that the star player Diana Taurasi
had tested positive for a stimulant that was identified as modafinil, a drug
that enhances wakefulness and vigilance and is designed to treat narcolepsy,
sleep apnea and sleep disorders related to shift work. Modafinil is also used
off-label to combat jet lag and attention deficit disorder and recreationally to
enhance alertness. The stimulant does not cause the anxiety and jitteriness
associated with amphetamines.
Athletes who use modafinil as a banned performance-enhancing substance, however,
face suspension from competition for up to two years, according to the rules of
the World Anti-Doping Agency. That could keep Taurasi from playing in the 2012
Olympics.
Taurasi's case could still be declared a false positive and dismissed. But even
if it were determined that Taurasi had taken the stimulant inadvertently, and a
two-year ban were reduced, she could still face the loss of her Olympic
eligibility.
The International Olympic Committee instituted a controversial rule in 2008 that
prohibits athletes from competing in the next Winter or Summer Games if they
have served a doping suspension of six months or longer.
Taurasi has been provisionally suspended by her Turkish club team, Fenerbahce of
Istanbul, until the drug testing is completed, Howard L. Jacobs, Taurasi's
California-based lawyer, said Friday. So far, she has missed two or three games,
Jacobs said. Her doping case was first reported by The Associated Press.
''She doesn't believe that she's ever taken anything that's banned; the most
logical explanation at this point is that the test is simply wrong,'' Jacobs
said in a telephone interview.
Taurasi, 28, a six-foot guard and forward, starred at the University of
Connecticut and has won two league titles with the Phoenix Mercury of the
W.N.B.A. She was named the league's most valuable player in 2009 and has led the
league in scoring four times. She and Australia's Lauren Jackson are regarded by
many as the two best women's players in the world.
Taurasi played on the United States teams that won gold at the 2004 and 2008
Olympics, and in October, she helped lead the Americans to a gold medal at the
world championships. She is considered vital to the Americans' chances of
winning another gold at the 2012 London Olympics, where the favored Americans
will be coached by Geno Auriemma, Taurasi's college coach.
The news about Taurasi emerged only days after UConn set the major-college
basketball record with its 89th consecutive victory. And although her doping
case is unresolved, it was the second recent public embarrassment for Taurasi,
who spent a day in jail in 2009 and was briefly suspended by the Mercury after
pleading guilty to a charge of driving under the influence.
A routine drug test was administered to Taurasi after a Fenerbahce game in early
November, Jacobs said. Each urine sample is divided into two parts, an A sample
and B sample. The A sample has tested positive, but the B sample has yet to be
tested, Jacobs said.
If an athlete's B sample comes back negative, the A sample is considered to have
been a false positive, and the case is dismissed.
Jacobs said that he hoped the B sample would be tested ''as soon as possible,''
perhaps the first week in January, but that the holidays ''were complicating
things.''
Taurasi was upset that news about her test leaked before the testing was
completed, Jacobs said. And because the entire case would be thrown out with a
negative B sample, he said it was premature to talk about any possible sanctions
like Olympic ineligibility.
''That's jumping three or four steps down the road,'' Jacobs said. ''Right now,
we're focusing on getting the B sample tested. If it's negative, all this goes
away.''
If the B sample does test positive, Jacobs will probably argue that Taurasi took
the stimulant without her knowledge, perhaps in a mislabeled product like a
supplement.
''When you're in a foreign country where you don't speak the language, it opens
up possibilities,'' Jacobs said.
It is unclear what sanctions would be applied by the Turkish basketball
federation if the B sample returned positive, Jacobs said. Under the rules of
the World Anti-Doping Agency, modafinil belongs to a class of drugs that calls
for a two-year suspension from competition. It is also uncertain how Taurasi's
W.N.B.A. eligibility would be affected.
There are relatively few cases of known use of modafinil by athletes, especially
not in association with other substances. Perhaps the most notorious case
involved the American sprinter Kelli White, who tested positive for the
stimulant while winning the 100 and 200 meters at the 2003 world track and field
championships in Paris.
White was later stripped of her medals upon admitting that modafinil was used
with a cocktail of other prohibited substances as part of the Bay Area
Laboratory Co-operative scandal. Other sports stars like Barry Bonds and Marion
Jones were eventually linked to Balco.
Dr. Gary Wadler of New York, chairman of the antidoping agency's prohibited list
committee, said the illicit use by athletes of modafinil to gain an edge was
''another example of the advances of modern medicine being bastardized for
non-legitimate purposes.''
''It has stimulant effects akin to amphetamines,'' Wadler said.
If Taurasi's B sample does test positive, and any suspension is reduced to six
months to two years, her Olympic eligibility could still remain unsettled until
shortly before the London Olympics. As of now, the International Olympic
Committee does not permit a waiver request until an athlete is named to the
team, Jacobs said.
''Somebody before London is going to challenge that rule,'' Jacobs said. ''It's
a virtual certainty.''
URL: http://www.nytimes.com
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: The former UConn star Diana Taurasi, right, helped lead the
United States to a gold medal at the world championships in October. (PHOTOGRAPH
BY JAROSLAV OZANA/CTK, VIA ASSOCIATED PRESS)
PUBLICATION-TYPE: Newspaper
Copyright 2010 The New York Times Company
106 of 998 DOCUMENTS
St. Louis Post-Dispatch (Missouri)
December 25, 2010 Saturday
THIRD EDITION
Sports Digest
SECTION: SPORTS; Pg. B2
LENGTH: 510 words
DATELINE: 0
Taurasi's Olympic status in limbo after drug test
Basketball player Diana Taurasi's positive test for a banned stimulant while
playing professionally in Turkey could threaten her eligibility to play for the
United States in the 2012 London Olympics. The Turkish basketball federation
said Friday that she tested positive for a stimulant that was identified as
modafinil, a drug that enhances wakefulness and vigilance and is designed to
treat narcolepsy, sleep apnea and sleep disorders related to shift work. It also
is used off-label to combat jet lag and attention deficit disorder, and it is
used recreationally to enhance alertness.
Athletes who use modafinil as a banned performance-enhancing substance, however,
face suspension from competition for up to 2 years, according to the rules of
the World Anti-Doping Agency. Taurasi's case still could be declared a false
positive and dismissed. But even if it were determined that Taurasi took the
stimulant inadvertently, and a 2-year ban was reduced, she still could face the
loss of Olympic eligibility. She has been provisionally suspended by her Turkish
club team, Fenerbahce of Istanbul, until the drug-testing procedure is
completed.
"She doesn't believe that she's ever taken anything that's banned; the most
logical explanation at this point is that the test is simply wrong," said Howard
L. Jacobs, Taurasi's lawyer.
Taurasi, 28, a 6-foot guard, starred at the University of Connecticut and has
won 2 WNBA titles while with Phoenix. She was named the WNBA's most valuable
player in 2009 and has led the league in scoring 4 times. Taurasi played on the
U.S. teams that won gold at the 2004 and 2008 Olympics. (New York Times)
Fay to leave USGA - David Fay, 60, has decided to retire from the U.S. Golf
Association after 21 years as the executive director, leaving a legacy that
includes his successful push to stage the U.S. Open on public golf courses. Mike
Butz, the deputy executive director, will replace Fay on an interim basis. Fay
was behind bringing the U.S. Open to Bethpage Black in New York in 2002. It was
such a big success that it returned in 2009, along with going to another public
course at Torrey Pines in 2008. In coming years the U.S. Open will go to
Chambers Bay outside Seattle and Erin Hills in Wisconsin, also public courses.
(AP)
Elsewhere - Diego Maradona says he is taking the president of Argentina's soccer
federation to court, accusing Julio Grondona of spreading false information
about his problems with drugs and alcohol. Maradona said he has not had drugs or
alcohol for 6 years. Grondona implied in a TV interview this week that Maradona
was using again. Maradona has been involved in a spat with Grondona since July,
when Maradona's contract as national coach was not renewed. ... Former Clemson
baseball coach Bill Wilhelm, who led the Tigers to more than 1,100 wins and 6
College World Series berths, died in Columbia, S.C., at age 81. A cause of death
was not given. He coached the Tigers from 1958-1993 and never had a losing year.
He had a record of 1,161-536-10. (AP)
LOAD-DATE: December 27, 2010
LANGUAGE: ENGLISH
DOCUMENT-TYPE: BRIEF
PUBLICATION-TYPE: Newspaper
Copyright 2010 St. Louis Post-Dispatch, Inc.
All Rights Reserved
107 of 998 DOCUMENTS
Tulsa World (Oklahoma)
December 25, 2010 Saturday
Final Edition
Sports FYI
BYLINE: Staff and Wire Reports
SECTION: Sports; Pg. B2
LENGTH: 477 words
Basketball Taurasi tests positive for modafinil: WNBA standout and former UConn
star Diana Taurasi tested positive for modafinil while playing in a professional
women's league in Turkey, the country's basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant. Modafinil is used to counter excessive sleepiness
due to narcolepsy, shift-work sleep disorder or sleep apnea, according to the
website for the prescription drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency. "We're not going to confirm what the drug is,"
Taurasi's lawyer, Howard Jacobs said. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all." The team's website said:
"(Taurasi) is extremely disturbed that her right to confidentiality has been
breached and doping claims have been made even before the results of her test
are out." If the "B' sample comes back positive, it could put her 2012 Olympics
status in jeopardy. Players suspended for fighting in stands: The two
Mississippi State players caught on camera fighting in the stands of the Diamond
Head Classic have been suspended indefinitely and sent home from Hawaii. Renardo
Sidney and Elgin Bailey, who are roommates, were involved in a fistfight after
the Bulldogs' game Thursday night. The altercation lasted for several minutes
before being broken up by teammates and coaches. MSU athletic director Scott
Stricklin sent out a tweet on Friday saying "The actions that took place in
Hawaii were embarrassing to all of us who love Mississippi State. This behavior
will not be tolerated." Coach Rick Stansbury expressed his disappointment in a
press release: "In my 13 years as a head coach, we've never had anything like
this happen before," he said. It's the latest in a string of issues for Sidney.
The NCAA ruled last March he had to repay $11,800 in improper benefits and sit
out the remainder of the 2010 season and nine more games this season. Baseball
Padres sign Hawpe: The San Diego Padres have agreed to terms of a one-year
contract with Brad Hawpe to play first base, two people with knowledge said on
Friday. Hawpe will replace three-time All-Star Adrian Gonzalez, who was traded
to the Boston Red Sox earlier this month. Hawpe has mostly been an outfielder in
seven big league seasons, with a handful of starts at first base. He was
released by Colorado in August and signed by Tampa Bay.
LOAD-DATE: December 26, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2010 The Tulsa World
108 of 998 DOCUMENTS
The Washington Post
December 25, 2010 Saturday
Suburban Edition
Taurasi tested positive for modafinil
SECTION: SPORTS; Pg. D02
LENGTH: 757 words
WNBA standout and former Connecticut star Diana Taurasi tested positive for
modafinil while playing in a professional women's league in Turkey, the
country's basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the Web site for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "the urine sample taken from Diana Taurasi as a
part of the regular process, after a game between Istanbul University and
Fenerbahce . . . tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's attorney, Howard
Jacobs, told the Associated Press. "We'll revisit it after the 'B' sample
returns. They shouldn't be speaking about it at all."
Right-handed pitcher Ricky Nolasco has signed a three-year, $26.5 million
contract with the Florida Marlins. Nolasco is expected to earn $6 million in
2011, $9 million in 2012 and $11.5 in 2013.
He made $3.8 million last season, when he went 14-9 with a 4.51 ERA. The
28-year-old missed the final month after undergoing arthroscopic right knee
surgery. . . .
The San Diego Padres have agreed to terms of a one-year contract with Brad Hawpe
to play first base, two people with knowledge of the deal told the Associated
Press. They spoke on condition of anonymity because the deal is pending Hawpe
passing a physical exam. Hawpe will replace three-time all-star Adrian Gonzalez,
who was traded to the Boston Red Sox earlier this month. . . .
The Pittsburgh Pirates claimed minor league left-hander Aaron Thompson off
waivers and designated left-hander Wil Ledezma for assignment. Thompson was left
unprotected by the Washington Nationals, who acquired him from Florida for first
baseman Nick Johnson in 2009. Thompson, who made 26 starts at Class AA
Harrisburg last season, was a first-round pick in 2005.
Buffalo Sabres leading scorer Derek Roy will miss the rest of the season after
tearing his left quadriceps tendon. General Manager Darcy Regier announced the
center is expected to miss between four to six months, and will have surgery to
repair the injury in the next couple of days.
Roy was hurt Thursday in the first period of a 4-3 loss to Florida when he was
driven into the boards by Dmitry Kulikov. . . .
David Fay is retiring from the U.S. Golf Association, his two decades as
executive director marked by a steady push for golf's return to the Olympics and
for the U.S. Open to be held on golf courses that anyone could play.
Fay's announcement was somewhat of a surprise, although he turned 60 two months
ago and said it was an important milestone for cancer survivors. He joined the
USGA in 1978 and became its sixth executive director in 1989.
Mike Butz, the deputy executive director since 1995, will take over Jan. 1 until
a national search to find Fay's replacement. . . .
The two Mississippi State players caught on camera fighting in the stands of the
Diamond Head Classic in Honolulu have been suspended indefinitely and sent home
from Hawaii.
Renardo Sidney and Elgin Bailey, who are roommates, were involved in a fistfight
after the Bulldogs' game Thursday night. The altercation lasted for several
minutes before being broken up by teammates and coaches.
"I'm very sorry for this incident," Sidney said in a statement released by the
university. "I had no intention of this ever happening. I apologize for
embarrassing my family, all the Mississippi State fans, my teammates and
coaches. I will learn from this and move on."
MSU Athletic Director Scott Stricklin sent out a tweet, saying "The actions that
took place in Hawaii were embarrassing to all of us who love Mississippi State.
This behavior will not be tolerated."
In a release from the university, Coach Rick Stansbury expressed his
disappointment.
"In my 13 years as a head coach, we've never had anything like this happen
before," he said. "I am very disappointed in the actions of Elgin Bailey and
Renardo Sidney and in no way does it reflect the overall picture of our program.
It is not how we want our men's basketball team to be viewed nationally."
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
DISTRIBUTION: Every Zone
PUBLICATION-TYPE: Newspaper
Copyright 2010 The Washington Post
All Rights Reserved
109 of 998 DOCUMENTS
The Associated Press
December 24, 2010 Friday 10:18 PM GMT
Federation: Taurasi tests positive for modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 733 words
DATELINE: NEW YORK
WNBA standout and former UConn star Diana Taurasi tested positive for modafinil
while playing in a professional women's league in Turkey, the country's
basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
110 of 998 DOCUMENTS
Breaking News from globeandmail.com
December 24, 2010 Friday 2:37 PM GMT
WNBA's Taurasi tests positive for banned substance;
Women s league All-Star fails drug test while playing in Turkish pro league
BYLINE: DOUG FEINBERG New York AP
SECTION: GLOBESPORTS
LENGTH: 736 words
ABSTRACT
Women s league All-Star fails drug test while playing in Turkish pro league
FULL TEXT
Diana Taurasi is facing one of the most difficult challenges to her stellar
basketball career.
The WNBA standout and former UConn star tested positive for a mild stimulant
while playing in a pro league in Turkey, her lawyer told The Associated Press on
Thursday night.
Howard Jacobs said Taurasi's "A" sample came back positive from a lab in Turkey
last week. He said the substance "was not a steroid or recreational drug," and
that Taurasi has asked that her "B" sample be tested.
The Turkish basketball federation said Friday that the substance in Taurasi's
positive test was modafinil. Modafinil is used to counter excessive sleepiness
due to narcolepsy, shift work sleep disorder or sleep apnea, according to the
website for prescription drug Provigil, which contains the substance.
Neither Jacobs nor Taurasi's team, Fenerbahce, would confirm it was modafinil,
which has been involved in several major doping cases, including that of U.S.
sprinter Kelli White.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Taurasi has been provisionally suspended pending the testing of her "B" sample
in the first week of January. She has already missed three games with
Fenerbahce.
In a statement posted on its website, the team said Taurasi was upset that the
doping claims broke before the testing process was finalized.
"She is extremely disturbed that her right to confidentially has been breached
and doping claims have been made even before the results of her test are out,"
the team said.
Taurasi's positive test came to light two days after the top-ranked Huskies won
their 89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
"We're taking it one step at a time," Jacobs said. "I'd rather not say what it
is at this stage, they've only tested the 'A' sample. Somehow it leaked over in
Turkey. We're waiting for the 'B' sample to be tested. We've had some difficulty
with getting a date so far, mostly because of the holidays. We're hoping to get
it as soon as we can."
UConn coach Geno Auriemma could not be reached for comment by telephone.
"While she is fully cooperating with authorities, there are serious doubts about
the accuracy of the test results," Jacobs said in a statement to the AP. "We are
confident that Diana will be fully vindicated once all the evidence is reviewed.
She regrets that someone has violated the confidentiality rules of this process,
and will make no further statement at this time."
WNBA spokesman Ron Howard said the league had no comment.
"In the 10 years of competition at the collegiate, professional and Olympic
level," said Jacobs. "Diana Taurasi has never taken, been suspected of using, or
tested positive for any performance enhancing substance."
Jacobs said he didn't know what the length of the suspension would be, nor was
he familiar with the details of the Turkish league's anti-doping code. He also
said it was too early to know how this might affect Taurasi's eligibility for
the London 2012 Olympics. The International Olympic Committee bars any athlete
given a doping penalty of six months or more from competing in the next games.
Taurasi, who has won two Olympic gold medals, helped guide the U.S. national
team to the world championship in early October. She led the WNBA in scoring for
a league-record fourth straight year, averaging 22.6 points per game. The
five-time All-Star and two-time WNBA champion signed a multiyear contract
extension with the Phoenix Mercury in August.
Reached at the Miami Heat-Phoenix Suns game, Rick Weltz, president of the Suns
and Mercury, said the team had no comment.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 24, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2010 The Globe and Mail, a division of CTVglobemedia Publishing Inc.
All Rights Reserved
111 of 998 DOCUMENTS
St. Paul Pioneer Press (Minnesota)
December 24, 2010 Friday
Quick Hits / Taurasi may face Olympic ban
BYLINE: From news services
SECTION: SPORTS
LENGTH: 510 words
Diana Taurasi's positive test for a banned stimulant while playing
professionally in Turkey could threaten her eligibility to play for the United
States in the 2012 London Olympics.
The Turkish basketball federation said Friday that Taurasi had tested positive
for a stimulant identified as modafinil, a drug designed to treat narcolepsy,
sleep apnea and sleep.
It also is used off-label to combat jet lag and to enhance alertness.
Athletes who use modafinil as a banned performance-enhancing substance face
suspension from competition for up to two years, according to World Anti-Doping
Agency rules.
Even if it were determined that Taurasi took the stimulant inadvertently, and a
two-year ban were reduced, she still could face the loss of Olympic
eligibility.Colleges / NCAA weighs tougher penalties
The NCAA has been busy this year investigating schools from Auburn to Georgia to
North Carolina while trying to crack down on problems tied to sports agents.
Most of the investigations are open cases with unknown consequences for the
schools.
But recommendations made by an NCAA panel two years ago for stricter punishments
for schools tabbed as serious rules violators remain under consideration and
could mark the first substantive revision to the NCAA's penalty system since
1985.
"It's definitely not a dead issue," NCAA spokeswoman Stacey Osburn said.
The panel's report is confidential. But interviews with the group's former
chairman and others knowledgeable about its contents indicate the
recommendations include:
· A requirement that all schools found guilty of major violations lose
scholarships. Current NCAA rules list that sanction as a "presumptive"
penalty.
· TV bans, a penalty not applied to Division I violators since 1996.
· Clarified penalties for repeat offenders. The "death penalty" -- a
program-crippling blow that keeps a team off the field while banning
recruiting and scholarship awards -- has been on the books for 25
years but applied only once, to Southern Methodist for a pay-for-play
football scandal in 1987.
Repeat violators are defined as schools that run afoul of the NCAA more than
once every five years. Miscellaneous / Marlins' Nolasco signs 3-year deal
Right-handed pitcher Ricky Nolasco has signed a three-year, $26.5 million
contract with the Florida Marlins.
Nolasco, 28, made $3.8 million last season, when he went 14-9 with a 4.51
earned-run average.
· The San Diego Padres agreed to terms of a one-year contract with Brad
Hawpe to play first base, two people with knowledge of the deal told
the Associated Press.
Hawpe will replace three-time all-star Adrian Gonzalez, who was traded to the
Boston Red Sox this month.
· Former Clemson baseball coach Bill Wilhelm, who led the Tigers to more
than 1,100 wins and six College World Series appearances, died in a
Clemson, S.C., hospital. He was 81.
· David Fay, 60, is retiring from the U.S. Golf Association, his two
decades as executive director marked by a steady push for golf's
return to the Olympics and for the U.S. Open to be held on golf
courses that anyone could play at a reasonable price.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
GRAPHIC:
PUBLICATION-TYPE: Newspaper
Copyright 2010 St. Paul Pioneer Press
All Rights Reserved
112 of 998 DOCUMENTS
Associated Press Worldstream
December 24, 2010 Friday 2:31 PM GMT
Federation: Taurasi tested positive for modafinil
BYLINE: By SUZAN FRASER, Associated Press
SECTION: SPORTS NEWS
LENGTH: 608 words
DATELINE: ANKARA Turkey
Basketball great Diana Taurasi tested positive for the stimulant modafinil and
was provisionally suspended pending the result of her "B" sample test in
January, Turkey's basketball federation and team officials said Friday.
Taurasi was tested last month, following a Turkish league game between her team
Fenerbahce and Istanbul University. A lab in the capital Ankara detected the
stimulant in her "A" sample, the federation said in a statement.
"A final decision (on her situation) will be taken as soon as the process
leading to the opening of the 'B' sample is complete," the federation said.
Taurasi's lawyer, Howard Jacobs, told The Associated Press Thursday that the
player, who has so far missed three games with Fenerbahce, has stayed away from
performance enhancing substances throughout her 10 years of competition at
college, professional and Olympic level.
"Diana Taurasi has never taken, been suspected of using, or tested positive for
any performance enhancing substance," he said.
Fenerbahce said in a statement posted on its website that Taurasi was upset that
the doping claims broke before the testing process was finalized.
Taurasi and teammate Anna Vajda were routinely tested following the Nov. 13
league game, the club said. Vajda tested negative for any banned substances, it
said.
Taurasi requested the "B" sample test, with the result to be disclosed on Jan. 2
or Jan. 4 in the presence of lawyers, Fenerbahce said.
"She is extremely disturbed that her right to confidentially has been breached
and doping claims have been made even before the results of her test are out,"
Fenerbahce said.
Neither Jacobs nor Fenerbahce confirmed that Taurasi tested positive for
modafinil, a banned stimulant involved in several major doping cases, including
that of Kelli White.
White won the 100 and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for modafinil.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift work
sleep disorder or sleep apnea, according to the website for prescription drug
Provigil, which contains the substance.
Jacobs told the AP in a statement that while the player was fully cooperating
with authorities, "there are serious doubts about the accuracy of the test
results."
"We are confident that Diana will be fully vindicated once all the evidence is
reviewed."
Jacobs said it was too early to tell how this might affect Taurasi's eligibility
for the 2012 Olympics in London. The International Olympic Committee bars any
athlete given a doping penalty of six months or more from competing in the
subsequent games.
Taurasi helped lead the University of Connecticut to three straight national
championships as well as 70 consecutive victories from 2001-03. She was the AP
Player of the Year in 2003.
Taurasi, who has won two Olympic gold medals, helped guide the U.S. national
team to the world championship in early October. She led the WNBA in scoring for
a league-record four straight years, averaging 22.6 points per game. The
five-time All-Star and two-time WNBA champion signed a multiyear contract
extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a drunk-driving charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi leads the league in scoring with 24.6 points a game.
AP Basketball Writer Doug Feinberg in New York and Erol Israfil in Istanbul
contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
113 of 998 DOCUMENTS
Associated Press Worldstream
December 24, 2010 Friday 10:07 PM GMT
Federation: Taurasi tests positive for modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 728 words
DATELINE: NEW YORK
Basketball great Diana Taurasi tested positive for modafinil while playing in a
professional women's league in Turkey, the country's federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
114 of 998 DOCUMENTS
Associated Press Online
December 24, 2010 Friday 6:24 PM GMT
WNBA's Taurasi tests positive for banned substance
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 721 words
DATELINE: NEW YORK
Diana Taurasi is facing one of the most difficult challenges to her stellar
basketball career.
The WNBA standout and former UConn star tested positive for a mild stimulant
while playing in a pro league in Turkey, her lawyer told The Associated Press on
Thursday night.
Howard Jacobs said Taurasi's "A" sample came back positive from a lab in Turkey
last week. He said the substance "was not a steroid or recreational drug," and
that Taurasi has asked that her "B" sample be tested.
The Turkish basketball federation said Friday that the substance in Taurasi's
positive test was modafinil. Modafinil is used to counter excessive sleepiness
due to narcolepsy, shift work sleep disorder or sleep apnea, according to the
website for prescription drug Provigil, which contains the substance.
Neither Jacobs nor Taurasi's team, Fenerbahce, would confirm it was modafinil,
which has been involved in several major doping cases, including that of U.S.
sprinter Kelli White.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Taurasi has been provisionally suspended pending the testing of her "B" sample
in the first week of January. She has already missed three games with
Fenerbahce.
In a statement posted on its website, the team said Taurasi was upset that the
doping claims broke before the testing process was finalized.
"She is extremely disturbed that her right to confidentially has been breached
and doping claims have been made even before the results of her test are out,"
the team said.
Taurasi's positive test came to light two days after the top-ranked Huskies won
their 89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
"We're taking it one step at a time," Jacobs said. "I'd rather not say what it
is at this stage, they've only tested the 'A' sample. Somehow it leaked over in
Turkey. We're waiting for the 'B' sample to be tested. We've had some difficulty
with getting a date so far, mostly because of the holidays. We're hoping to get
it as soon as we can."
UConn coach Geno Auriemma could not be reached for comment by telephone.
"While she is fully cooperating with authorities, there are serious doubts about
the accuracy of the test results," Jacobs said in a statement to the AP. "We are
confident that Diana will be fully vindicated once all the evidence is reviewed.
She regrets that someone has violated the confidentiality rules of this process,
and will make no further statement at this time."
WNBA spokesman Ron Howard said the league had no comment.
"In the 10 years of competition at the collegiate, professional and Olympic
level," said Jacobs. "Diana Taurasi has never taken, been suspected of using, or
tested positive for any performance enhancing substance."
Jacobs said he didn't know what the length of the suspension would be, nor was
he familiar with the details of the Turkish league's anti-doping code. He also
said it was too early to know how this might affect Taurasi's eligibility for
the London 2012 Olympics. The International Olympic Committee bars any athlete
given a doping penalty of six months or more from competing in the next games.
Taurasi, who has won two Olympic gold medals, helped guide the U.S. national
team to the world championship in early October. She led the WNBA in scoring for
a league-record fourth straight year, averaging 22.6 points per game. The
five-time All-Star and two-time WNBA champion signed a multiyear contract
extension with the Phoenix Mercury in August.
Reached at the Miami Heat-Phoenix Suns game, Rick Weltz, president of the Suns
and Mercury, said the team had no comment.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
115 of 998 DOCUMENTS
Associated Press Online
December 24, 2010 Friday 10:18 PM GMT
Federation: Taurasi tests positive for modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: SPORTS NEWS
LENGTH: 740 words
DATELINE: NEW YORK
WNBA standout and former UConn star Diana Taurasi tested positive for modafinil
while playing in a professional women's league in Turkey, the country's
basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
(This version CORRECTS to "confidentiality")
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
116 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 24, 2010 Friday 6:24 PM GMT
WNBA's Taurasi tests positive for banned substance
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: STATE AND REGIONAL
LENGTH: 721 words
DATELINE: NEW YORK
Diana Taurasi is facing one of the most difficult challenges to her stellar
basketball career.
The WNBA standout and former UConn star tested positive for a mild stimulant
while playing in a pro league in Turkey, her lawyer told The Associated Press on
Thursday night.
Howard Jacobs said Taurasi's "A" sample came back positive from a lab in Turkey
last week. He said the substance "was not a steroid or recreational drug," and
that Taurasi has asked that her "B" sample be tested.
The Turkish basketball federation said Friday that the substance in Taurasi's
positive test was modafinil. Modafinil is used to counter excessive sleepiness
due to narcolepsy, shift work sleep disorder or sleep apnea, according to the
website for prescription drug Provigil, which contains the substance.
Neither Jacobs nor Taurasi's team, Fenerbahce, would confirm it was modafinil,
which has been involved in several major doping cases, including that of U.S.
sprinter Kelli White.
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Taurasi has been provisionally suspended pending the testing of her "B" sample
in the first week of January. She has already missed three games with
Fenerbahce.
In a statement posted on its website, the team said Taurasi was upset that the
doping claims broke before the testing process was finalized.
"She is extremely disturbed that her right to confidentially has been breached
and doping claims have been made even before the results of her test are out,"
the team said.
Taurasi's positive test came to light two days after the top-ranked Huskies won
their 89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
"We're taking it one step at a time," Jacobs said. "I'd rather not say what it
is at this stage, they've only tested the 'A' sample. Somehow it leaked over in
Turkey. We're waiting for the 'B' sample to be tested. We've had some difficulty
with getting a date so far, mostly because of the holidays. We're hoping to get
it as soon as we can."
UConn coach Geno Auriemma could not be reached for comment by telephone.
"While she is fully cooperating with authorities, there are serious doubts about
the accuracy of the test results," Jacobs said in a statement to the AP. "We are
confident that Diana will be fully vindicated once all the evidence is reviewed.
She regrets that someone has violated the confidentiality rules of this process,
and will make no further statement at this time."
WNBA spokesman Ron Howard said the league had no comment.
"In the 10 years of competition at the collegiate, professional and Olympic
level," said Jacobs. "Diana Taurasi has never taken, been suspected of using, or
tested positive for any performance enhancing substance."
Jacobs said he didn't know what the length of the suspension would be, nor was
he familiar with the details of the Turkish league's anti-doping code. He also
said it was too early to know how this might affect Taurasi's eligibility for
the London 2012 Olympics. The International Olympic Committee bars any athlete
given a doping penalty of six months or more from competing in the next games.
Taurasi, who has won two Olympic gold medals, helped guide the U.S. national
team to the world championship in early October. She led the WNBA in scoring for
a league-record fourth straight year, averaging 22.6 points per game. The
five-time All-Star and two-time WNBA champion signed a multiyear contract
extension with the Phoenix Mercury in August.
Reached at the Miami Heat-Phoenix Suns game, Rick Weltz, president of the Suns
and Mercury, said the team had no comment.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
117 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 24, 2010 Friday 10:18 PM GMT
LENGTH: 791 words
BC-BKL--Taurasi-Banned Substance, 7th Ld-Writethru,0982
Federation: Taurasi tests positive for modafinil
2030
Eds: Corrects to "confidentiality.". This story is part of AP's general news and
sports services.
AP Photo NY164, NY163, NY133
sptd/rrosenblatt sptd/sbuttar sptd/hrumberg sptd/jkosik fasst4921
By DOUG FEINBERG
AP Basketball Writer
NEW YORK (AP) WNBA standout and former UConn star Diana Taurasi tested positive
for modafinil while playing in a professional women's league in Turkey, the
country's basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
118 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 24, 2010 Friday 10:18 PM GMT
Federation: Taurasi tests positive for modafinil
BYLINE: By DOUG FEINBERG, AP Basketball Writer
SECTION: STATE AND REGIONAL
LENGTH: 733 words
DATELINE: NEW YORK
WNBA standout and former UConn star Diana Taurasi tested positive for modafinil
while playing in a professional women's league in Turkey, the country's
basketball federation said Friday.
Neither her lawyer nor her team, Fenerbahce, would confirm that Taurasi tested
positive for the stimulant, which has been involved in several major doping
cases, including that of U.S. sprinter Kelli White.
Modafinil is used to counter excessive sleepiness due to narcolepsy, shift-work
sleep disorder or sleep apnea, according to the website for the prescription
drug Provigil, which contains the substance.
The Turkish Basketball Federation statement cited a report from the lab at
Hacettepe University and said: "... the urine sample taken from Diana Taurasi as
a part of the regular process, after a game between Istanbul University and
Fenerbahce ... tested positive for modafinil, one of the illegal substances on
WADA's banned stimulants list, according to preliminary test results." WADA is
the World Anti-Doping Agency.
"We're not going to confirm what the drug is," Taurasi's lawyer, Howard Jacobs,
told The Associated Press Friday. "We'll revisit it after the "B" sample
returns. They shouldn't be speaking about it at all."
White won the 100- and 200-meter races at the 2003 world championships in Paris,
but both her medals were stripped after she tested positive for the stimulant.
Jacobs said Taurasi's "A" sample came back positive last week and that the
substance "was not a steroid or recreational drug."
Taurasi has been provisionally suspended pending the testing of her "B" sample,
sometime early next month. She has already missed three games with Fenerbahce.
The team's website said she and another player were asked to submit to a test on
Nov. 13, following the game against Istanbul. It said they were selected as a
result of a draw. The other player tested negative.
Fenerbahce said Taurasi was upset that the doping claims broke before the
testing process was finalized.
"She is extremely disturbed that her right to confidentiality has been breached
and doping claims have been made even before the results of her test are out,"
the team's website said.
If the "B' sample comes back positive, it could put her 2012 Olympics status
with the U.S. national basketball team in jeopardy. She has helped the team win
gold medals at the past two Olympics and was the leading scorer at the women's
world championships, which the Americans won in early October.
The International Olympic Committee bars any athlete given a doping penalty of
six months or more from competing in the next games.
"At this point we're aware of the situation and we're monitoring things and
letting the process take its course," USA Basketball spokesman Craig Miller
said. "Until that happens we can't comment."
Taurasi's test came to light two days after the top-ranked Huskies won their
89th straight game, surpassing the UCLA men's winning streak from 1971-74.
Taurasi helped lead UConn to three straight national championships as well as 70
consecutive victories from 2001-03. She was the AP Player of the Year in 2003.
UConn's Geno Auriemma, who coached Taurasi and will lead the 2012 Olympic team,
couldn't be reached for comment by telephone Friday.
At the WNBA All-Star game last summer, Taurasi said the grind of playing
basketball continuously for seven straight years was beginning to wear on her.
At the time, she indicated fatigue could eventually force her to skip either the
WNBA or European seasons.
Taurasi is one of many WNBA stars who play overseas in the winter because of
higher salaries. The best players can make up to 10 times their WNBA salaries,
which top out at about $100,000.
She led the WNBA in scoring for a league-record fourth straight year, averaging
22.6 points per game. The five-time All-Star and two-time WNBA champion signed a
multiyear contract extension with the Phoenix Mercury in August.
Taurasi served one day in jail and was suspended by the team for two games in
2009 after pleading guilty to a DUI charge.
She played in Russia for four years for powerhouse Spartak before joining the
Turkish League this season. That league also features WNBA stars Sylvia Fowles,
Penny Taylor and Seimone Augustus.
Taurasi is leading the league in scoring this season with 24.6 points a game.
Associated Press Writers Suzan Fraser in Ankara, Turkey, and Erol Israfil in
Istanbul contributed to the report.
LOAD-DATE: December 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Associated Press
All Rights Reserved
119 of 998 DOCUMENTS
Canadian Medical Association. Journal
December 14, 2010
Uplifting tales of life in the emergency department
BYLINE: Deady, Brian
SECTION: Pg. E870 Vol. 182 No. 18 ISSN: 0820-3946; CODEN: CMAJAX
LENGTH: 688 words
Books Uplifting tales of life in the emergency department The Night Shift: Real
Life in the Heart of the E.R. Dr. Brian Goldman HarperCollins Publishers Ltd.,
2010.
Brian Goldman is one of those rare individuals who simultaneously pursues two
careers. He has toiled for more than 20 years as an emergency physician at Mount
Sinai Hospital in Toronto, Ontario while working as a medical journalist for the
CBC, currently as host of CBC radio's White Coat, Black Art. Without claiming
the same far-reaching influence of American media darlings, Oprah's Dr. Oz or
CNN's Dr. Sanjay Gupta, he is as close as we get in this country to a medical
celebrity.
Goldman trades on his media personality with a book of his experiences in the
emergency department and I am happy to report that it's a satisfying read. The
storyline proceeds as if over one night shift, but the author concedes in the
introduction that the book is a composite of his most interesting cases over the
many years of his career. In addition to being a medical memoir, it's also a
compilation of other physician's stories.
The Night Shift rolls out along a timeline that begins at 9:15 pm one Friday
evening as Goldman sets off to work. He arrives for a 10 pm start and is
immediately thrust into the action. Cases are then laid out in chronological
order, each one allowing the writer to riff onto other anecdotes. Along the way,
the author weighs in on the many topics fundamental to emergency physicians
including interactions with patients, police, consultants, residents and nurses,
medical error and the schadenfreude that we sometimes feel (but shouldn't) when
talking about a colleague's diagnostic blunder.
Trauma care is central to the idea of what makes emergency medicine absorbing -
at least in the public's mind - and Mount Sinai is not a trauma hospital, but
this obstacle is neatly hurdled when our doctor-journalist draws on his radio
interviews to bring the stories of other Canadian emergency physicians to the
page. Reading like a who's who of Canadian emergency medicine, their narratives
add considerable storytelling muscle to the book's physique. I was particularly
struck by former Vancouver General emergency specialist, Bruce Campana, who is
quoted throughout the volume. He should consider writing his own book.
The pace is fast and the writing is engaging, but make no mistake, this is a
book written for the nonmedical public. To that end, while the reader in me
enjoyed the tour, my inner physician was sometimes nonplussed with the clinical
explanations. For example, in describing the writhing discomfort of a
30-year-old woman, we learn that "It (the patient's abdomen) was rigid, which
now suggested peritonitis, an inflammation of the membrane that lines part of
the abdominal cavity, often caused by infection and treatable with antibiotics."
While the patient, it quickly becomes apparent, is not suffering from this
condition, the statement as presented is incomplete. Although I doubt it would
detract from the flow of the paragraph for most readers, surely this gross
simplification is likely to induce metaphorical scalpscratching among MDs.
Goldman himself comes across as earnest, dedicated and diagnostically astute.
And while he didn't have to do so, he bravely discusses his own perceived
weaknesses as an emergency physician, medical miscalculations, sleep disorder
and use of a prescription drug modafinil to stay alert during night shifts.
Goldman admits to disliking criticism but these tablets serve as an example of
the occasionally weak editing of the text. For example, at 9:15 pm on the way to
his shift, "I popped a couple of modafinil pills." At 2:44 am, "I took a
modafinil and headed to my next patient." At 5:18 am, "I resisted the urge to
pop another modafinil. ... I do worry that one day I'll need three pills, then
four, then five." Dear Brian, either that day has arrived or your editor needs a
little pharmacologic assistance in the awake and alert department.
But these comments seem like mere grousing. I finished the book surprisingly
uplifted and proud to be part of the club which Goldman so ably describes.
LOAD-DATE: December 20, 2010
LANGUAGE: ENGLISH
ACC-NO: 2216346761
GRAPHIC: Photographs
DOCUMENT-TYPE: Book Review-Favorable
PUBLICATION-TYPE: Other (Periodical)
JOURNAL-CODE: CMAJ
Copyright 2010 Micromedia Limited
All Rights Reserved
Canadian Business and Current Affairs
Copyright 2010 Canadian Medical Association
120 of 998 DOCUMENTS
Indian Patents News
December 14, 2010 Tuesday 6:30 AM EST
Teva Pharmaceutical Industries Ltd Files Patent Application for Crystalline and
Pure Modafinil and Process of Preparing the Same
LENGTH: 348 words
New Delhi, Dec. 14 -- Israel based Teva Pharmaceutical Industries Ltd filed
patent application for crystalline and pure modafinil and process of preparing
the same. The Inventors are Claude Singer, Neomi Gershon, Arina Ceausu, Anita
Lieberman and Judith Aronhime.
Teva Pharmaceutical Industries Ltd filed the patent application Oct. 26, 2006.
The patent application number is 1259/MUMNP/2006 A. The International
classification numbers are A61K31/165, C07C315/02 and C07C315/06.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention provides an improved process for preparing modafinil, whereby
it may be isolated in high purity by a single crystallization. The process
produces modafinil free of sulphone products of over-oxidation and other
byproducts. The invention further provides new crystalline Forms II-VI of
modafinil and processes for preparing them. Each of the new forms is
differentiated by a unique powder X-ray diffraction pattern. The invention
further provides pharmaceutical compositions containing novel modafinil Forms
II-IV and VI."
Teva Pharmaceutical Industries Limited (Teva) (Public, NASDAQ:TEVA) is a global
pharmaceutical company that develops, produces and markets generic drugs
covering all treatment categories. The Company has a pharmaceutical business,
whose principal products are Copaxone for multiple sclerosis and Azilect for
Parkinson's disease, respiratory products and women's health products. Teva's
active pharmaceutical ingredient (API) business provides vertical integration to
Teva's own pharmaceutical production. The Company's global operations are
conducted in North America, Europe, Latin America, Asia and Israel. Teva has
operations in more than 60 countries, including 38 finished dosage
pharmaceutical manufacturing sites in 17 countries, 15 generic research and
development (R&D) centers operating mostly within certain manufacturing sites
and 21 API manufacturing sites around the world. On January 29, 2009, the
Company sold its Israeli animal health product line to Phibro Animal Health
Corporation.
LOAD-DATE: December 14, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
121 of 998 DOCUMENTS
The Times (London)
December 7, 2010 Tuesday
Edition 1;
National Edition
Pop go the pep pills;
Jaded students, housewives, even doctors, have turned to smart drugs. Dr
Margaret McCartney asks whether it is such a wise move
BYLINE: Margaret McCartney
SECTION: T2;FEATURES; Pg. 9
LENGTH: 1004 words
It's the middle of the night and I'm e-mailing my anesthesiologist friend in the
US. "I'm tired," I moan, although with the time-difference it is already evening
for him. He, however, is organised and bright of eye.
"You need modafinil," he replies, his e-mail pert and swift. "Seriously, it's
the best thing."
As a Scottish GP with too much to do, I harbour a suspicion of most drugs,
prescribed or not. But as I cast my eyes around the room, piled with washing and
ironing, and contemplate the week's taxi service requirements for my children, I
realise that he is merely telling me what I'd rather not know: that lots of
people, from students to housewives, have turned to "smart drugs".
In 2000, it became apparent that the American Armed Forces were using such
drugs, including Dexedrine and Restoril, to "prevent fatigue and maintain
combat-ready performance" in pilots, according to a report.
Only a few months ago, the British Medical Journal ran an editorial,
"Pharmacological enhancement of performance in doctors", in which the authors,
who were doctors and scientists, stated that the use of caffeine, Viagra,
antidepressants and multivitamins was common and acceptable. Although the issues
relating to the use of such medication might be complex, they wrote,
"performance-enhancing drugs may have benefits for healthy, non-fatigued
individuals".
They concluded that "early indications are that members of society are more
likely to agree with cognitive enhancement [of doctors] if motivations for using
them are seen to be unselfish".
But what's the reality behind the alluring prospect of better fighter pilots and
more effective surgeons? Do "smart drugs" have the potential to make us smarter
or do the side-effects do more harm than good? Amphetamines What are they: This
group of drugs includes Dexedrine and treatments prescribed for attention
deficit hyperactivity disorder (ADHD).
Amphetamines are Class B drugs, also known as speed, which have long been
favoured by clubbers keen to dance the night away. The drugs have been used in
diet pills, for their effect on increasing metabolism, and are still sold
illegally for this purpose. Useful for a boost? Even in cases of ADHD, they
should be used only after other psychological and behavioural measures have been
tried, according to NICE, the health service's treatment watchdog.
Studies that suggest that there are benefits from taking amphetamines have
involved only small numbers of patients - the studies that the BMJ report
referred to involved 70 men and no women, and focused on lab tests, rather than
real-life tasks.
What are the side-effects: Addiction, cardiac problems, overdose, jitteriness
and paranoia. There is a lack of research into the effects of amphetamines on
routine tasks, including driving.
Modafinil What is it: This drug, marketed as Provigil, can be prescribed to deal
with "daytime sleepiness" caused by shift working or for narcolepsy (a condition
where the person falls asleep without warning). However it is available on the
internet, allowing buyers to use it for tiredness unrelated to shift work.
Useful for a boost? A study published in the New England Journal of Medicine in
2005 compared 209 people with "shift-work disorder" who were given either
modafinil or a placebo. Those taking modafinil reported less sleepiness during
their night shift, but the real revelation was the proportion of people who
reported an accident or a near accident on their commute home to bed.
In the placebo group, it was 58 per cent and in the modafinil group, a third. So
although fewer people in the group taking the drug were at risk of an accident,
the proportion was still worryingly high.
Another study claiming that emergency doctors worked smarter with modafinil was
widely publicised, even though it had only 25 participants and the results were
measured with paper-based tests rather than real-life outcomes.
Modafinil was put on the list of banned drugs for athletes in 2004. What are the
side-effects? Anxiety, high blood pressure, agitation and decreased libido as
well as mania and suicidal thoughts. As many studies have been short, the
longer-term effects, good or bad, aren't known. Some studies using MRI scans
have suggested that the drug affects not just cognitive circuits but emotional
ones. Is this a good thing? No one knows.
Donepezil What is it: Known as Aricept, the drug for treating dementia, studies
have recently suggested that it improves learning in people without dementia
better than a placebo. It is not, at present, licensed for use to treat anything
other than Alzheimer's. Useful for a boost? The study had just 12 people in it
and has to be regarded as very preliminary. Other studies - notably from the US
- have examined the use of Aricept in older adults and haven't found medium or
longer-term boosts to learning or memory. Internet chatrooms are full of
students who swear by it but, on the evidence at present, they'd be better off
swotting instead.
What are the side-effects? Heart irregularities but, in people who are
prescribed it, it's usually tolerated.
Pro-plus What is it: This is the older version of the modern smart pill, known
to students everywhere. The makers say it "gives you a fast-acting caffeine
boost that relieves fatigue and tiredness and helps you feel more awake". Two
tablets contain 100mg of caffeine: in Starbucks, a small (short) coffee contains
160mg caffeine, with the biggest containing 400mg. Useful for a boost? Caffeine
raises the heart rate and blood pressure, waking up tired minds. It's a quick
fix that rapidly wears off so the dose has to be topped up. A Cochrane review -
which examines all the evidence available - found some evidence that caffeine
improved performance and memory in shift workers.
What are the side-effects? Caffeine is legal, easy to obtain and delicious to
drink. But we all know that getting to sleep after too much is difficult, and,
of course, if sleep is what you really need, caffeine might end up being your
enemy rather than your friend.
LOAD-DATE: December 7, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: TIM
Copyright 2010 Times Newspapers Limited
All Rights Reserved
122 of 998 DOCUMENTS
Indian Patents News
November 19, 2010 Friday 6:30 AM EST
Universitatsklinikum Freiburg Files Patent Application for the Gene PRV-1 and
its Use
LENGTH: 249 words
New Delhi, Nov. 19 -- Germany based Universitatsklinikum Freiburg filed patent
application for the gene PRV-1 and its use. The inventor is Heike Pahl.
Universitatsklinikum Freiburg filed the patent application on March 27, 2002.
The patent application number is IN/PCT/2002/00335/DEL A. The international
classification number is A61K31/16.
According to the Controller General of Patents, Designs & Trade Marks, "This
invention relates to new uses of Modafinil and its D/L enantiomers, particularly
the new uses in the pharmaceutical preparation field. This invention provides
new uses of Modafinil and its D/L enantiomers in preparing the medicine for
increasing and enhancing the quantity and quality of normal spermatozoa in male
mammals, the medicine for enhancing the pregnant capacity in female mammals, the
medicine for treating infertility, subfertility and sex dysfunction in male and
female mammals, and the medicine for enhancing the sexual function in mammals."
The University Medical Center Freiburg (Universitatsklinikum Freiburg) in
Freiburg, Germany is the teaching hospital and part of the medical research unit
of the University of Freiburg and home to its Faculty of Medicine. The medical
center is one of the largest and most reputable in Europe, due to its extensive
clinical capabilities and advances in research. Medical services at the
University of Freiburg date back to the university's founding in 1457, as the
Faculty of Medicine was one of the four founding faculties.
LOAD-DATE: November 19, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
123 of 998 DOCUMENTS
CNS Drug News
October 25, 2010
FDA approves REMS for Nuvigil and Provigil
SECTION: NEWS
LENGTH: 252 words
On 21st October, Risk Evaluation and Mitigation Strategies (REMS) for Cephalon's
medications, Nuvigil (armodafinil) Tablets [C-IV] and Provigil (modafinil)
Tablets [C-IV], were approved by the FDA.
Nuvigil, the longer-lasting isomer of modafinil, is indicated to improve
wakefulness in patients with excessive sleepiness associated with treated
obstructive sleep apnoea (OSA), shift work disorder (SWD) or narcolepsy.
Meanwhile, Provigil is indicated to improve wakefulness in patients with
excessive sleepiness associated with treated OSA, shift work sleep disorder,
also known as SWD, and narcolepsy.
Both the Nuvigil and Provigil REMS consist of a medication guide to inform
patients about the potential risks associated with the use of these medications,
a communication plan and a timetable for submission of assessments of the REMS.
The communication plan includes a "Dear Healthcare Professional" letter, a
prescriber brochure, a pharmacist action letter and a dedicated REMS internet
site.
The goal of each REMS is to inform healthcare providers, patients and caregivers
about the risks associated with these medications, including serious skin rash
and hypersensitivity reactions. The current product labelling for both
medications contains a bolded warning that includes these risks. Neither
medication is approved for use in the paediatric population for any indication.
In accordance with the approved REMS, the company is currently updating Nuvigil
and Provigil labelling to include the medication guide.
LOAD-DATE: October 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: CNS Drug News
Copyright 2010 Espicom Business Intelligence
All Rights Reserved
124 of 998 DOCUMENTS
PR Newswire
October 22, 2010 Friday 4:38 PM EST
Cephalon Announces FDA Approval of Risk Evaluation and Mitigation Strategies for
NUVIGIL and PROVIGIL;
REMS Addresses Potential Risks Currently Included In Labeling
LENGTH: 1087 words
DATELINE: FRAZER, Pa., Oct. 22
FRAZER, Pa., Oct. 22 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced that Risk Evaluation and Mitigation Strategies (REMS) for its
medications NUVIGIL® (armodafinil) Tablets [C-IV] and PROVIGIL® (modafinil)
Tablets [C-IV] have been approved by the U.S. Food and Drug Administration
(FDA). Both the NUVIGIL and PROVIGIL REMS consist of a Medication Guide to
inform patients about the potential risks associated with the use of these
medications, a communication plan and a timetable for submission of assessments
of the REMS. The communication plan includes a Dear Healthcare Professional
Letter, a Prescriber Brochure, a Pharmacist Action Letter and a dedicated REMS
Internet Site. The introduction of the NUVIGIL and PROVIGIL REMS programs is
consistent with the company's commitment to safe and appropriate use of its
medications.
The goal of each REMS is to inform healthcare providers, patients and caregivers
about the risks associated with these medications, including serious skin rash
and hypersensitivity reactions. The current product labeling for both
medications contains a bolded warning that includes these risks. Neither
medication is approved for use in the pediatric population for any indication.
In accordance with the approved REMS, the company is currently updating NUVIGIL
and PROVIGIL labeling to include the Medication Guide.
The NUVIGIL and PROVIGIL Medication Guides will be available on each product
website, www.nuvigil.com and www.provigil.com, and will be dispensed with every
prescription. Information on both products is also available by calling
1-800-896-5855. More information on Cephalon and its products is available at
www.cephalon.com.
About NUVIGIL
NUVIGIL is indicated to improve wakefulness in patients with excessive
sleepiness associated with treated obstructive sleep apnea (OSA), shift work
disorder (SWD), or narcolepsy. In patients with OSA, NUVIGIL is used along with
other medical treatments for this condition. The NUVIGIL (armodafinil) label
includes a bolded warning for serious or life-threatening rash, including
Stevens-Johnson Syndrome, requiring hospitalization and discontinuation of
treatment, that has been reported in adults in association with the use of
modafinil and armodafinil and in children in association with the use of
modafinil, a racemic mixture of S and R modafinil (the latter is armodafinil,
the active ingredient in NUVIGIL). NUVIGIL is not approved for use in pediatric
patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness, and insomnia. Full prescribing
information for NUVIGIL is available at www.nuvigil.com.
About PROVIGIL
PROVIGIL is indicated to improve wakefulness in patients with excessive
sleepiness associated with treated obstructive sleep apnea (OSA), shift work
sleep disorder, also known as shift work disorder (SWD), and narcolepsy. In
patients with OSA, PROVIGIL is used along with other medical treatments for this
condition. The PROVIGIL label includes a bolded warning for serious or
life-threatening rash, including Stevens-Johnson Syndrome, requiring
hospitalization and discontinuation of treatment, that has been reported in
adults and children taking modafinil. PROVIGIL is not approved for use in
pediatric patients for any indication.
The most common adverse events in controlled clinical trials (greater than five
percent) were headache, nausea, nervousness, rhinitis, diarrhea, back pain,
anxiety, insomnia, dizziness and dyspepsia. Full prescribing information for
PROVIGIL is available at www.provigil.com.
About Cephalon, Inc.
Cephalon is a global biopharmaceutical company dedicated to discovering,
developing and bringing to market medications to improve the quality of life of
individuals around the world. Since its inception in 1987, Cephalon has brought
first-in-class and best-in-class medicines to patients in several therapeutic
areas. Cephalon has the distinction of being one of the world's fastest-growing
biopharmaceutical companies, now among the Fortune 1000 and a member of the S&P
500 Index, employing approximately 4,000 people worldwide. The company sells
numerous branded and generic products around the world. In total, Cephalon sells
more than 150 products in nearly 100 countries. More information on Cephalon and
its products is available at www.cephalon.com.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide the Cephalon current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results; prospects for regulatory approval; manufacturing development
and capabilities; market prospects for its products; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
Contacts:
Media:
Candace Steele Flippin
610-727-6231 (office)
csteele@cephalon.com
Investor Relations:
Chip Merritt
610-738-6376 (office)
cmerritt@cephalon.com
Joseph Marczely
610-883-5894 (office)
jmarczely@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:CONTACT: Media: Candace Steele Flippin, +1-610-727-6231,
csteele@cephalon.com, or Investor Relations: Chip Merritt, +1-610-738-6376,
cmerritt@cephalon.com, or Joseph Marczely, +1-610-883-5894,
jmarczely@cephalon.com, all of Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: October 23, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 PR Newswire Association LLC
All Rights Reserved
125 of 998 DOCUMENTS
Indian Patents News
October 15, 2010 Friday 6:30 AM EST
Wockhardt Ltd Files Patent Application for Bilayer Tablet Composition of
Modafinil
LENGTH: 284 words
New Delhi, Oct. 15 -- India based Wockhardt Ltd filed patent application for
bilayer tablet composition of modafinil. The inventors are Jain Nitin Anand
Kumar, Murali Narayanan and Jain Girish Kumar.
Wockhardt Ltd filed the patent application on April 27, 2007. The patent
application number is 811/MUM/2007 A. The International classification number is
A61K9/20.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention provides a bilayer tablet comprising modafinil or
pharmaceutical^ acceptable salts thereof wherein the tablet comprises micronized
and unmicronized modafinil particles. Modafinil is a wakefulness-promoting agent
indicated to improve wakefulness in patients with excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome, and shift
work sleep disorder. It has molecular weight of 273.36. The chemical name of
modafinil is (2-[(diphenylmethyl) sulfinyl] acetamide. Its empirical formula is
C15H15NO2S."
Wockhardt Limited (WL) (Public, BOM:532300) is an India-based an integrated
pharmaceutical, biotechnology and healthcare company. The Company is a
subsidiary of Khorakwala Holdings and Investments Private Limited. The Company's
cardiology division covers lifestyle diseases, which include diabetes and
nephrology, supported by biotechnology products, such as Wosulin, Glaritus and
Wepox. As of March 31, 2010, the Company had seven hospitals with 800 inpatient
beds. The Company's subsidiaries includes Wockhardt Biopharm Limited, Vinton
Healthcare Limited, Wockhardt Infrastructure Development Limited, Wockhardt UK
Holdings Limited, CP Pharmaceuticals Limited, Wallis Group Limited and The
Wallis Laboratory Limited.
LOAD-DATE: October 15, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
126 of 998 DOCUMENTS
Indian Patents News
October 15, 2010 Friday 6:30 AM EST
Wockhardt Ltd Files Patent Application for Pharmaceutical Composition of
Modafinil or Salts Thereof
LENGTH: 241 words
New Delhi, Oct. 15 -- India based Wockhardt Ltd filed patent application for
pharmaceutical composition of modafinil or salts thereof. The inventors are Huda
Inderjeetsingh, Murali Narayanan and Jain Girish Kumar.
Wockhardt Ltd filed the patent application on April 27, 2007. The patent
application number is 810/MUM/2007 A. The International classification number is
A61K9/16.
According to the Controller General of Patents, Designs & Trade Marks, "The
present invention provides a pharmaceutical composition of modafinil or
pharmaceutical^ acceptable salts thereof comprising mixture of micronized and
unmicronized modafinil particles, sodium starch glycolate in admixture with one
or more pharmaceutically acceptable excipients."
Wockhardt Limited (WL) (Public, BOM:532300) is an India-based an integrated
pharmaceutical, biotechnology and healthcare company. The Company is a
subsidiary of Khorakwala Holdings and Investments Private Limited. The Company's
cardiology division covers lifestyle diseases, which include diabetes and
nephrology, supported by biotechnology products, such as Wosulin, Glaritus and
Wepox. As of March 31, 2010, the Company had seven hospitals with 800 inpatient
beds. The Company's subsidiaries includes Wockhardt Biopharm Limited, Vinton
Healthcare Limited, Wockhardt Infrastructure Development Limited, Wockhardt UK
Holdings Limited, CP Pharmaceuticals Limited, Wallis Group Limited and The
Wallis Laboratory Limited.
LOAD-DATE: October 15, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
127 of 998 DOCUMENTS
Mondaq
September 22, 2010 Wednesday 12:00 AM EST
"Grave Consequences" Defence may be Asserted Against a Generic in a Section 8
Action Under The PM(NOC) Regulations
BYLINE: Mr Intellectual Property Group
LENGTH: 869 words
Sep. 22, 2010 (Mondaq delivered by Newstex) --
Apotex Inc. v. Shire Canada Inc., 2010 FC 828
In an action brought by Apotex Inc. (Apotex) to recover damages under section 8
of the Patented Medicines (Notice of Compliance) Regulations
(SOR/93-133)(Regulations) in respect of the medicine modafinil, Shire Canada
Inc. (Shire) brought this motion for leave to amend its statement of defence,
alleging two new defences. Apotex opposed Shire's motion, arguing that the
proposed amendments did not disclose a reasonable defence and ought not to be
permitted. The prothonotary struck out the first proposed amendment, finding
that a defence based on the outcome of a separate infringement action to which
Shire was not a party would be speculative and hypothetical, but permitted the
second proposed amendment which alleged a "grave consequences" defence.
Background
Apotex filed an abbreviated new drug submission (ANDS), seeking a notice of
compliance (NOC) that would allow it to market its generic Apo-modafinil
tablets, by comparing its tablets to Shire's modafinil product. Shire had listed
Canadian patent no. 2,201,967 (the '967 patent) on the patent register in
respect of its modafinil tablets. On March 16, 2006, Apotex served a notice of
allegation (NOA) on Shire, alleging that the claims of its '967 patent were
invalid, void and of no effect. In response, Shire commenced an application for
an order prohibiting the issuance of a NOC to Apotex. This application was
dismissed two years later, on April 25, 2008. Apotex obtained a NOC shortly
after the judgment was released and now seeks damages under section 8 of the
Regulations for the delay in issuance of the NOC resulting from Shire's
unsuccessful application for a prohibition order.
Defence based on a separate action by Cephalon Inc. (NASDAQ:CEPH)
For its first proposed new defence, Shire proposed to rely on the outcome of a
separate infringement action against Apotex commenced by the owner of the '967
patent, Cephalon Inc. (Cephalon). Shire argued that, should the '967 patent be
found to be valid and infringed in that other action, Apotex should not be
entitled to recover any damages in the present proceeding based on the loss of
infringing sales.
The prothonotary struck this proposed defence, finding that the outcome of the
Cephalon action was an uncertain future event which was not susceptible of being
determined or even influenced in the context of the present action. This was the
essence of a speculative and hypothetical pleading that ought to be struck.
Moreover, these issues could not be determined unless and until the proceedings
by Cephalon in the other court file were resolved. This would unreasonably
delay, embarrass and prejudice the trial of the present action by Apotex againt
Shire.
Defence based on the "Grave Consequences" Doctrine
For its second proposed new defence, Shire sought to rely on the existence of
Canadian patent no. 2,165,824 (the '824 patent), a second patent listed on the
patent register against Shire's modafinil tablets. In particular, in a NOA
served on Shire by Apotex, dated August 30, 2005, Apotex alleged that it would
not infringe the '824 patent on the basis of its draft product monograph and
gave an undertaking that it would not make, use or sell its tablets for the
patented use of treatment of sleep apnea or ventilation problems of central
origin. However, according to Shire, Apotex's product monograph does include the
patented indication, and Apotex has sold its modafinil tablets for such use in
breach of its undertaking. Shire therefore seeks to allege that Apotex breached
this undertaking, giving rise to the possible finding of "grave consequences",
alluded to by the Federal Court of Appeal, in the form of a denial of any remedy
for delayed entry into the market pursuant to section 8 of the Regulations.
Apotex argued that subsection 8(5) of the Regulations, which requires the court
to take into account "all matters that it considers relevant to the assessment
of the amount, including any conduct [of the parties] which contributed to delay
the disposition of the application", should be interpreted as any valid defence
arising exclusively in the context of the very prohibition proceeding that was
dismissed or discontinued.
The prothonotary, however, found that Apotex's argument raised a difficult
question that should not be determined on a motion to strike. It was reasonably
arguable that the Court could conclude that Apotex's breach of an undertaking,
if established, could affect the assessment of damages. Apotex therefore did not
meet the very heavy onus of showing that this proposed defence was plainly and
obviously devoid of any merit and stood no chance of success whatsoever.
The content of this article is intended to provide a general guide to the
subject matter. Specialist advice should be sought about your specific
circumstances.
Mr Intellectual Property Group Stikeman Elliott LLP Suite 5300 Commerce Court
West 199 Bay Street Toronto M5L 1B9 CANADA Tel: 4168695500 Fax: 4169470866
E-mail: info@stikeman.com URL: www.stikeman.com
Click Here for related articles(c) Mondaq Ltd, 2010 - Tel. +44 (0)20 8544 8300 -
Newstex ID: MNDQ-5508-48970758
LOAD-DATE: September 22, 2010
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not necessarily
the views of Newstex or its re-distributors. Posts from such authors are
provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs on Demand® are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs on Demand® is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs on Demand® shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs on Demand®. Reader's comments reflect their
individual opinion and their publication within Blogs on Demand® shall not infer
or connote an endorsement by Newstex or its re-distributors of such reader's
comments or views. Newstex and its re-distributors expressly reserve the right
to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2010 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2010 Mondaq
128 of 998 DOCUMENTS
Mondaq Business Briefing
September 22, 2010
Canada: "Grave Consequences" Defence may be Asserted Against a Generic in a
Section 8 Action Under The PM(NOC) Regulations
BYLINE: Intellectual Property Group
LENGTH: 839 words
Apotex Inc. v. Shire Canada Inc., 2010 FC 828
In an action brought by Apotex Inc. (Apotex) to recover damages under section 8
of the Patented Medicines (Notice of Compliance) Regulations (SOR/93-133)
(Regulations) in respect of the medicine modafinil, Shire Canada Inc. (Shire)
brought this motion for leave to amend its statement of defence, alleging two
new defences. Apotex opposed Shire's motion, arguing that the proposed
amendments did not disclose a reasonable defence and ought not to be permitted.
The prothonotary struck out the first proposed amendment, finding that a defence
based on the outcome of a separate infringement action to which Shire was not a
party would be speculative and hypothetical, but permitted the second proposed
amendment which alleged a "grave consequences" defence.
Background
Apotex filed an abbreviated new drug submission (ANDS), seeking a notice of
compliance (NOC) that would allow it to market its generic Apo-modafinil
tablets, by comparing its tablets to Shire's modafinil product. Shire had listed
Canadian patent no. 2,201,967 (the '967 patent) on the patent register in
respect of its modafinil tablets. On March 16, 2006, Apotex served a notice of
allegation (NOA) on Shire, alleging that the claims of its '967 patent were
invalid, void and of no effect. In response, Shire commenced an application for
an order prohibiting the issuance of a NOC to Apotex. This application was
dismissed two years later, on April 25, 2008. Apotex obtained a NOC shortly
after the judgment was released and now seeks damages under section 8 of the
Regulations for the delay in issuance of the NOC resulting from Shire's
unsuccessful application for a prohibition order.
Defence based on a separate action by Cephalon Inc.
For its first proposed new defence, Shire proposed to rely on the outcome of a
separate infringement action against Apotex commenced by the owner of the '967
patent, Cephalon Inc. (Cephalon). Shire argued that, should the '967 patent be
found to be valid and infringed in that other action, Apotex should not be
entitled to recover any damages in the present proceeding based on the loss of
infringing sales.
The prothonotary struck this proposed defence, finding that the outcome of the
Cephalon action was an uncertain future event which was not susceptible of being
determined or even influenced in the context of the present action. This was the
essence of a speculative and hypothetical pleading that ought to be struck.
Moreover, these issues could not be determined unless and until the proceedings
by Cephalon in the other court file were resolved. This would unreasonably
delay, embarrass and prejudice the trial of the present action by Apotex againt
Shire.
Defence based on the "Grave Consequences" Doctrine
For its second proposed new defence, Shire sought to rely on the existence of
Canadian patent no. 2,165,824 (the '824 patent), a second patent listed on the
patent register against Shire's modafinil tablets. In particular, in a NOA
served on Shire by Apotex, dated August 30, 2005, Apotex alleged that it would
not infringe the '824 patent on the basis of its draft product monograph and
gave an undertaking that it would not make, use or sell its tablets for the
patented use of treatment of sleep apnea or ventilation problems of central
origin. However, according to Shire, Apotex's product monograph does include the
patented indication, and Apotex has sold its modafinil tablets for such use in
breach of its undertaking. Shire therefore seeks to allege that Apotex breached
this undertaking, giving rise to the possible finding of "grave consequences",
alluded to by the Federal Court of Appeal, in the form of a denial of any remedy
for delayed entry into the market pursuant to section 8 of the Regulations.
Apotex argued that subsection 8(5) of the Regulations, which requires the court
to take into account "all matters that it considers relevant to the assessment
of the amount, including any conduct [of the parties] which contributed to delay
the disposition of the application", should be interpreted as any valid defence
arising exclusively in the context of the very prohibition proceeding that was
dismissed or discontinued.
The prothonotary, however, found that Apotex's argument raised a difficult
question that should not be determined on a motion to strike. It was reasonably
arguable that the Court could conclude that Apotex's breach of an undertaking,
if established, could affect the assessment of damages. Apotex therefore did not
meet the very heavy onus of showing that this proposed defence was plainly and
obviously devoid of any merit and stood no chance of success whatsoever.
The content of this article is intended to provide a general guide to the
subject matter. Specialist advice should be sought about your specific
circumstances.
Mr Intellectual Property Group
Stikeman Elliott LLP
Suite 5300
Commerce Court West
199 Bay Street
Toronto
M5L 1B9
CANADA
Tel: 4168695500
Fax: 4169470866
E-mail: info@stikeman.com
URL: www.stikeman.com
LOAD-DATE: October 4, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Mondaq Ltd.
All Rights Reserved
129 of 998 DOCUMENTS
Reuters Health Medical News
September 15, 2010 Wednesday 9:00 PM EST
Armodafinil does not improve cognitive deficits in schizophrenia
SECTION: DRUG & DEVICE DEVELOPMENT
LENGTH: 408 words
DATELINE: NEW YORK
Adjunctive armodafinil, the longer-lasting isomer of modafinil, doesn't improve
cognitive deficits in patients with schizophrenia, researchers report in an
August 24th online paper in the Journal of Clinical Psychiatry.
Dr. John M. Kane, of The Zucker Hillside Hospital in Glen Oaks, New York, and
colleagues randomized 60 patients (mean age 43 years) with stable schizophrenia
to adjunctive treatment with once-daily placebo or armodafinil 50, 100, or 200
mg.
Fifteen patients were assigned to each group; 49 (82%) completed the 4-week
study. Changes in cognitive deficits from baseline to the final visit were
similar following armodafinil or placebo, as measured by the Measurement and
Treatment Research to Improve Cognition in Schizophrenia (MATRICS) composite
score. Mean changes ranged from 1.9 with 50 mg to 2.9 with 200 mg; scores in the
placebo group fell in the middle.
In two previous trials, modafinil-treated patients didn't differ from
placebo-treated patients in the Scale for the Assessment of Negative Symptoms
(SANS) scores. Similarly, in the current study, there were no clinically
meaningful reductions in the SANS total score.
Armodafinil was generally well tolerated. The most common adverse events were
diarrhea and headache. Treatment did not cause psychosis to worsen.
Patients who received armodafinil 200 mg did have greater improvement in the
Positive and Negative Syndrome Scale for Schizophrenia (PANSS) than those who
received placebo, but the results were not statistically significant.
The mechanism of action of armodafinil is not known. "A weak DAT (dopamine
transporter) inhibitor such as armodafinil, which may preferentially influence
the dopaminergic activity in the prefrontal cortex but not in the limbic system,
could, hypothetically, reduce negative symptoms without worsening positive
symptoms--the effect suggested in this study," Dr. Kane and colleagues write.
They also say that "treating negative symptoms of schizophrenia is important
because these symptoms are debilitating for patients and because antipsychotic
therapies are often not adequate to treat them."
Their conclusion is that more study is needed to determine the potential
efficacy of modafinil on negative symptoms.
The study was sponsored by Cephalon, the manufacturer of armodafinil, which
either employs or has financial relationships with all the paper's seven
authors.
SOURCE: http://link.reuters.com/fek83p
SOURCE: J Clin Psychiatry 2010.
LOAD-DATE: September 16, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Reuters Health
All Rights Reserved
130 of 998 DOCUMENTS
Generic Line
August 4, 2010 Wednesday
FTC Denies Improper Behavior in Watson Pay-for-Delay Case
SECTION: Vol. 27 No. 15
LENGTH: 575 words
The FTC says it did not engage in improper behavior as part of its pay-for-delay
investigation into Watson Pharmaceuticals and has reaffirmed its request to
subpoena CEO Paul Bisaro to see if the company brokered an illicit deal to keep
Provigil generics off the market.
The commission also rebuts an accusation from Bisaro that it attempted to broker
a deal between Watson and Apotex to produce a generic version of Provigil (
modafinil), according to a detailed FTC filing to the U.S. District Court for
the District of Columbia.
The FTC is still waiting for Bisaro to explain whether a 2006 agreement Watson
entered into with Cephalon, Provigil's manufacturer, included a stipulation that
Watson delay launching generic modafinil in exchange for payments, it says.
The commission was required to answer questions from Bisaro's lawyers as part of
an order issued last month by Judge Alan Kay (Generic Line, July 21).
"This Court finds that the facts before it present a strong possibility that the
FTC did share confidential information with Watson's competitor, that it did
attempt to broker a deal between Apotex and Watson that would require Watson to
relinquish any statutory 'first filer' rights it had acquired, and that it did
initiate this investigation to pressure Watson to relinquish these rights and to
harass it when it refused," Kay wrote.
During conversations with Watson counsel Steven Sunshine in March 2009, Markus
Meier, assistant director in the FTC's Bureau of Competition, brought up an idea
"through a series of hypothetical questions" that would involve Watson
licensing, relinquishing or sharing its 180-day marketing exclusivity, the
commission says. Sunshine then authorized Meier to contact Apotex regarding a
possible deal between the two companies, the FTC adds.
After informing Apotex of Watson's interests, the FTC says it didn't play any
role in further discussions between the companies, nor did it divulge
proprietary information as claimed by Bisaro.
But Kay sided with Watson, saying that the commission pressured the company to
enter into the deal.
"The facts before us suggest that the FTC sought to place Watson between a rock
and a hard place, where the only way Watson could clear its name and escape
further FTC scrutiny was to give in to the pressure the FTC was placing on
Watson to enter into the business deal with Apotex," Kay said.
Heightened Suspicions
The FTC's suspicions into Watson's actions were heightened in January 2009 when
it learned that on the same day a second patent related to Provigil was listed
in the FDA's Orange Book, Watson filed an ANDA challenging it. That would give
Watson "first-filer" status.
"FTC staff sought to understand practically how a generic company would be aware
of a later-issued patent so that it would be in the position to file an ANDA
amendment on precisely the same day that the brand company listed such later
issued patent with the FDA," the commission says in its filing.
"Put simply, FTC staff was trying to assess whether a generic company was likely
to have such information independently or whether such information was likely
available to the generic only as a result of collusion with the brand company to
create an additional barrier to impede potential generic entry," it continues.
Watson told Generic Line it would not respond to the FTC's filing in keeping
with its policy of not commenting on ongoing litigation. -- Jonathan Block
Release date: Aug. 4, 2010
LOAD-DATE: August 6, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
131 of 998 DOCUMENTS
Washington Drug Letter
August 2, 2010 Monday
FTC: Nothing Improper Done in Investigation of Watson
SECTION: Vol. 42 No. 30
LENGTH: 306 words
The FTC says it did not engage in improper behavior as part of its pay-for-delay
investigation into Watson Pharmaceuticals and has reaffirmed its request to
subpoena CEO Paul Bisaro to see if the company brokered an illicit deal to keep
Provigil generics off the market.
The commission also rebuts an accusation from Bisaro that it attempted to broker
a deal between Watson and Apotex to produce a generic version of Provigil (
modafinil), according to a detailed FTC filing to the U.S. District Court for
the District of Columbia.
The FTC is still waiting for Bisaro to explain whether a 2006 agreement Watson
entered into with Cephalon, Provigil's manufacturer, included a stipulation that
Watson delay launching generic modafinil in exchange for payments, it says.
The commission was required to answer questions from Bisaro's lawyers as part of
an order issued earlier this month by Judge Alan Kay (WDL, July 19).
The FTC's suspicions into Watson's actions were heightened in January 2009 when
it learned that on the same day a second patent related to Provigil was listed
in the FDA's Orange Book, Watson filed an ANDA challenging it. That would give
Watson "first-filer" status.
"FTC staff sought to understand practically how a generic company would be aware
of a later-issued patent so that it would be in the position to file an ANDA
amendment on precisely the same day that the brand company listed such later
issued patent with the FDA," the commission says in its filing.
"Put simply, FTC staff was trying to assess whether a generic company was likely
to have such information independently or whether such information was likely
available to the generic only as a result of collusion with the brand company to
create an additional barrier to impede potential generic entry," it continues.
-- Jonathan Block
Release date: Aug. 2, 2010
LOAD-DATE: August 2, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
132 of 998 DOCUMENTS
Global Insight
July 29, 2010
EMA Recommends Limiting Use of Modafinil to Narcolepsy Treatment
BYLINE: Brendan Melck
SECTION: In Brief
LENGTH: 228 words
The Committee for Medicinal Products for Human Use (CHMP) of the European
Medicines Agency (EMA) has concluded a safety review of drugs including the
active pharmaceutical ingredient modafinil, concluding with the recommendation
that drugs including this API should only be used to treat narcolepsy. The drug
should no longer be used in the treatment of idiopathic hypersomnia, shift-work
sleep disorder, or excessive sleepiness associated with obstructive sleep
apnoea, the committee concluded. The safety review was initiated due to concerns
relating to potential skin and subcutaneous tissue reactions and psychiatric
disorders resulting from the use of modafinil. The CHMP decided that only in the
case of narcolepsy did modafinil's benefits outweigh its risks, and so all other
indications should be removed from its marketing authorisation. Its
recommendations have now been passed to the European Commission for final
approval.
Significance:The decision of the CHMP (assuming the Commission gives it binding
approval) will certainly have some effect on producers of drugs containing
modafinil, such as the drug's developer Cephalon (U.S.), with its Provigil
product, Mitsubishi Tanabe of Japan, with its Modiodal, and generics producers.
Such producers can expect to suffer some consequences in reduced revenues from
these products if the recommendation is approved.
LOAD-DATE: July 29, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2010 World Markets Research Limited
All Rights Reserved
133 of 998 DOCUMENTS
Drug Industry Daily
July 26, 2010 Monday
FTC Denies Improper Behavior in Watson Pay-for-Delay Investigation
SECTION: Vol. 9 No. 143
LENGTH: 468 words
The FTC says it did not engage in improper behavior as part of its pay-for-delay
investigation into Watson Pharmaceuticals and has reaffirmed its request to
subpoena CEO Paul Bisaro to see if the company brokered an illicit deal to keep
Provigil generics off the market.
The commission also rebutted an accusation from Bisaro that it attempted to
broker a deal between Watson and Apotex to produce a generic version of Provigil
(modafinil), according to a detailed filing to the U.S. District Court for the
District of Columbia on Thursday.
The FTC says it is still waiting for the executive to explain whether a 2006
agreement Watson entered into with Cephalon, Provigil's manufacturer, included a
stipulation that Watson delay launching generic modafinil in exchange for
payments.
The commission was required to answer questions from Bisaro's lawyers as part of
an order given earlier this month by Judge Alan Kay (DID, July 15).
According to the FTC, during conversations with Watson counsel Steven Sunshine
in March 2009, Markus Meier, assistant director in the agency's Bureau of
Competition, brought up an idea "through a series of hypothetical questions"
that would involve Watson licensing, relinquishing or sharing its 180-day
marketing exclusivity. The commission says Sunshine then authorized Meier to
contact Apotex regarding a possible deal between Apotex and Watson.
The FTC further states that after informing Apotex of Watson's interests, it
didn't play any role in further discussions between the two companies, nor did
it ever divulge proprietary information as claimed by Bisaro.
The FTC's suspicions into Watson were heightened in January 2009, after finding
out that on the same day a second patent related to Provigil was listed in the
FDA's Orange Book, Watson filed an ANDA challenging it. That would give Watson
"first-filer" status.
"FTC staff sought to understand practically how a generic company would be aware
of a later-issued patent so that it would be in the position to file an ANDA
amendment on precisely the same day that the brand company listed such later
issued patent with the FDA," according to the commission's filing.
"Put simply, FTC staff was trying to assess whether a generic company was likely
to have such information independently or whether such information was likely
available to the generic only as a result of collusion with the brand company to
create an additional barrier to impede potential generic entry."
Watson told DID it would not respond to the FTC's filing, as it has a policy of
not commenting on ongoing litigation.
Congress is attempting to scuttle pay-for-delay deals in the future. A provision
in the supplemental war appropriations bill, currently before the Senate, would
ban the practice (DID, July 6). -- Jonathan Block
Release date: July 26, 2010
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Global Insight
July 26, 2010
New Zealand's Pharmac Seeks Feedback on Modavigil Application
BYLINE: Aparna Krishnan
SECTION: In Brief
LENGTH: 202 words
New Zealand's drug reimbursement agency, Pharmac, has proposed funding CSL
Biotherapies' Modavigil (modafinil) under the restricted Special Authority
criteria. The drug is intended for patients with narcolepsy, but the agency has
sought to restrict its use to patients with narcolepsy who cannot tolerate
methylphenidate or dexamphetamine or in whom both methylphenidate and
dexamphetamine are contraindicated. Pharmac has sought feedback on the proposal
in view of the proposed drug funding from 1 October 2010.
Significance:If approved, modafinil 100-mg tablets would be listed in Section B
of the Pharmaceutical Schedule at a price and subsidy of NZ$72.50 (US$52.8) per
pack of 30 tablets. The scope of overall reimbursement revenues from the drug is
expected to be affected due to the restrictions. It is significant to note that
the Pharmacology and Therapeutics Advisory Committee reviewed CSL's application
for modafinil in February 2007 and recommended restricted listing use to
patients with diagnosed excessive daytime sleepiness associated with narcolepsy
and who cannot tolerate methylphenidate and dexamphetamine or in whom
methylphenidate and dexamphetamine were contraindicated, with a low priority.
LOAD-DATE: July 27, 2010
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The Pharmaceutical Journal
July 26, 2010
Modafinil use should be restricted to narcolepsy, says European Medicines Agency
LENGTH: 246 words
Modafinil should be used for the treatment of narcolepsy only, the European
Medicines Agency has advised.
Currently, modafinil is licensed for the treatment of daytime sleepiness
associated with narcolepsy, obstructive sleep apnoea syndrome and chronic shift
work.
However, a review by the agency's Committee for Medicinal Products for Human Use
concluded that the benefits of modafinil only outweigh the risks when used for
the treatment of narcolepsy - and that all other indications should be withdrawn
from the medicine's marketing authorisation.
The review was initiated because of safety concerns about psychiatric disorders
and serious skin and subcutaneous tissue reactions associated with modafinil.
The CHMP found the risk of developing skin and hypersensitivity reactions to be
higher in children than in adults and also recommend that modafinil should not
be prescribed for people under 18 years of age.
The CHMP also identified a number of cardiovascular risks associated with the
drug and advised that it should be contraindicated in patients with uncontrolled
moderate-to-severe hypertension and in patients with cardiac arrhythmias.
The CHMP's recommendations have been forwarded to the European Commission for
the adoption of a binding decision valid throughout the EU. The decision-making
phase usually takes two to three months and the European Commission follows the
CHMP's scientific opinion in almost all cases, a spokeswoman for the EMA told PJ
Online.
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PUBLICATION-TYPE: Journal
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CNS Drug News
July 23, 2010
EMA recommends restricting use of modafinil
SECTION: NEWS
LENGTH: 361 words
The European Medicines Agency (EMA) has recommended restricting the use of
modafinil-containing medicines. The medicine should only be used to treat
sleepiness associated with narcolepsy. Doctors and patients should no longer use
the medicine for the treatment of idiopathic hypersomnia, excessive sleepiness
associated with obstructive sleep apnoea and chronic shift work sleep disorder.
Modafinil is a wakefulness-promoting agent, currently licensed in 21 countries
in Europe. It is available as Modasomil, Modiodal, Provigil and Vigil (from
Cephalon), and as generic medicines. The review by the Agency's CHMP was
initiated because of a number of safety concerns, relating to psychiatric
disorders, skin and subcutaneous tissue reactions, as well as significant
off-label use and potential for abuse.
On the basis of the available data, the Committee concluded that the benefits of
these medicines only outweighed their risks in the therapeutic indication of
narcolepsy. For all other indications, the Committee found that the risk for
development of skin or hypersensitivity reactions and neuropsychiatric disorders
outweighed the evidence for clinically-important efficacy. Therefore, the
Committee concluded that all other indications should be withdrawn from the
marketing authorisations of these medicines.
The risk of development of serious skin and hypersensitivity adverse reactions
appears to be higher in children than in adults. The Committee concluded that
the product information should carry a recommendation saying that modafinil
should not be prescribed to children. The CHMP also identified particular
cardiovascular risks with modafinil and recommended that the use of the medicine
be contraindicated in patients with uncontrolled moderate-to-severe hypertension
and in patients with cardiac arrhythmias.
There are some reports that modafinil is being used recreationally for
"performance enhancement". However, the data seen by the Committee did not allow
it to make firm recommendations regarding this risk. The CHMP has requested that
the marketing authorisation holders continue to provide further information to
monitor the potential for abuse.
LOAD-DATE: July 23, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: CNS Drug News
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137 of 998 DOCUMENTS
Elsevier Global Medical News
July 22, 2010 Thursday 08:06 PM GMT
EMA Announces Review Findings, Decisions on Modafinil, Rotarix, and More
BYLINE: By Jennie Smith, Elsevier Global Medical News
LENGTH: 774 words
A number of drugs ranging from treat sleep apnea medications to vaccines have
been under review by the European Medicines Agency, and these review findings,
as well as other decisions made by the agency were announced July 22.
In a written statement, the agency reported that it would restrict the
prescribing of medicines containing modafinil to people with narcolepsy only -
preferably laboratory-confirmed narcolepsy - and requested that manufacturers
change their product labeling accordingly.
Concluding a 3-year review of the medications, the EMA cited concerns about
abuse of the wakefulness-promoting drug, along with reports of psychiatric
reactions including psychosis, adverse cardiovascular reactions, and serious
allergic skin reactions, in its decision.
The drug should no longer be used to treat obstructive sleep apnea, shift-work
sleep disorder, or idiopathic hypersomnia, the agency said, all indications for
which it is licensed in the European Union. The new, restricted indication must
be approved by the European Commission before it becomes binding.
According to the EMA's new prescribing information, modafinil should be used
"only in patients who have had a complete evaluation of their excessive
sleepiness, and in whom a diagnosis of narcolepsy has been made in accordance
with ICSD [International Classification of Sleep Disorders] diagnostic criteria.
Such an evaluation usually consists, in addition to the patient's history, of
sleep measurements testing in a laboratory setting."
The agency said it also was asking manufacturers to collect data on why
modafinil was being prescribed off label and investigating reports of its abuse
among university students.
Also on July 22, the EMA said it had concluded a review of topical medicines
containing the nonsteroidal anti-inflammatory drug ketoprofen. The drug has been
licensed since 1978 in all European countries but the Netherlands, but recently
has been plagued by reports of increased skin photosensitivity, photoallergy
even in dim light, and cosensitization with octocrylene, a chemical used in
sunscreens.
In December 2009, France suspended the marketing authorization of medicines
containing ketoprofen and asked the EMA to consider a similar ban in the EU.
Though the EMA did not follow suit, concluding that the risk of reaction was
very low, it did advise that topical ketoprofen be used only when prescribed and
that manufacturers strengthen product warnings on sun exposure and octocrylene.
These recommendations, too, await European Commission approval before they are
binding.
The EMA found that the porcine circovirus type 1 (PCV1) particles present in the
Rotarix vaccine posed no health risk to the public. Rotarix is an oral vaccine
used in infants, particularly in developing countries, to protect against
gastroenteritis-causing rotavirus infections. The agency began its review of the
vaccine after the surprise discovery of PCV1 in batches of the vaccine in March
(J. Virol. 2010;84:6033-40).
Data from tests carried out by the manufacturer, GlaxoSmithKline, "showed that
the vaccine contained only very small amounts of live PCV1. The viral particles
may have always been present in the vaccine, and have been found in the raw
material used to make the vaccine. Their presence was detected only now because
of the emergence of new technology," the agency said. Nonetheless, the EMA
noted, the manufacturer has since pledged to eliminate PCV1 from future batches
of vaccine.
Earlier in the month, July 9, the EMA announced that it was reviewing medicines
containing rosiglitazone, a second-line diabetes treatment used alone (Avandia)
or in combination with metformin (Avandamet) or glimepiride (Avaglim). Since
rosiglitazone's initial EU marketing authorization 10 years ago,
rosiglitazone-containing regimens been associated with increased cardiovascular
risks that product information and warnings have been altered to reflect.
The EMA said on July 22 that it was continuing to evaluate newly published
findings on rosiglitazone and cardiovascular events, including myocardial
infarction, heart failure, and stroke (JAMA 2010;304 [doi:10.1001/jama.2010.920]
and Arch. Intern Med. 2010;170 [doi:10.1001/archinternmed.2010.207]).
The rosiglitazone review, the EMA said, would not be finished until September
2010. Until then, it cautioned clinicians to adhere closely to existing warnings
and not prescribe rosiglitazone for patients with current or previous heart
failure, acute coronary syndrome, ischemic heart disease, or peripheral arterial
disease. Rosiglitazone and insulin can be used together only in exceptional
cases and under close supervision.
LOAD-DATE: July 22, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: NewsWire
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138 of 998 DOCUMENTS
Generic Line
July 21, 2010 Wednesday
Judge Orders FTC to Answer for Tactics in Provigil Case
SECTION: Vol. 27 No. 14
LENGTH: 506 words
A federal judge has ordered the FTC to answer questions about allegations it
released proprietary information as it tried to thwart a reverse-payment
settlement between Watson Pharmaceuticals and Cephalon over Cephalon's drug
Provigil.
Judge Alan Kay of the U.S. District Court of the District of Columbia this month
issued an order instructing the FTC to answer questions posed in a motion by
Watson CEO Paul Bisaro, who claims the commission shared proprietary company
information with Apotex.
The FTC challenged Watson's licensing agreement -- a "pay-for-delay" deal -- for
the excessive sleepiness drug Provigil (modafinil) and tried to broker an
agreement between Watson and Apotex instead, hoping the result would be cheaper
modafinil generics.
"This Court finds that the facts before it present a strong possibility that the
FTC did share confidential information with Watson's competitor, that it did
attempt to broker a deal between Apotex and Watson that would require Watson to
relinquish any statutory 'first filer' rights it had acquired, and that it did
initiate this investigation to pressure Watson to relinquish these rights and to
harass it when it refused," Kay wrote.
Bisaro has claimed that the FTC's efforts to subpoena him as part of a
pay-for-delay investigation was tantamount to harassment, prompting his lawyers
to file a request that the commission answer questions related to its alleged
information sharing (Generic Line, June 9).
The FTC must provide the court, by July 23, descriptions of communications it
had with the FDA and third parties regarding potential marketing exclusivity for
generic modafinil and whether any confidential information was disclosed.
'Rock and a Hard Place'
"The facts before us suggest that the FTC sought to place Watson between a rock
and a hard place, where the only way Watson could clear its name and escape
further FTC scrutiny was to give in to the pressure the FTC was placing on
Watson to enter into the business deal with Apotex," Kay added.
Glenn Lammi, an attorney with the Washington Legal Foundation, told Generic Line
Kay's ruling was "extraordinary, considering how infrequently judges allow
discoveries in these cases."
Kay, however, rejected a request from Bisaro's lawyers to depose Markus Meier,
assistant director of the FTC's Bureau of Competition Health Care Division. Last
month, two senators pressed FTC Chairman Jon Leibowitz on the agency's alleged
action in the Watson matter, with Leibowitz claiming Meier did not breach the
company's confidentiality (Generic Line, June 23).
FTC Bureau of Competition Director Richard Feinstein disagreed with Kay's
ruling, adding the agency has done nothing improper.
The FTC "is simply trying to complete a law enforcement investigation into
whether there is an agreement to keep generic drugs off the market and out of
the hands of consumers," Feinstein said. "We are disappointed that our
investigation has been sidetracked by the unfounded implications of opposing
counsel." -- Jonathan Block
Release date: July 21, 2010
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Global Insight
July 21, 2010
U.S. Court Reprimands FTC over Provigil Decision
BYLINE: Aparna Krishnan
SECTION: In Brief
LENGTH: 265 words
The U.S. Federal Trade Commission (FTC) has been reprimanded by a U.S. court,
which indicated a "strong possibility" of engaging improperly in litigation
relating to the sleep drug Provigil (modafinil). According to a written order by
the judge at the U.S. District Court for the District of Columbia, the improper
conduct refers to the FTC's sharing of confidential information about Provigil
marketer, Watson Pharma, with its competitor, the generics firm Apotex (Canada),
in an attempt to broker a deal between the two. The judge noted, "the FTC sought
to place Watson between a rock and a hard place, where the only way Watson could
clear its name and escape further FTC scrutiny was to give in to the pressure
the FTC was placing on Watson to enter into the business deal with Apotex". The
full order can be accessedhere. However, in an email statement to Reuters, the
FTC Competition Bureau Director, Richard Feinstein, has strongly denied
wrongdoing.
Significance:The public reproach of the FTC's actions reflects on the federal
agency's attempts to intervene in such generic drug deals. The FTC has been a
strong and vocal advocator of prohibiting the "pay-for-delay" generic deals and
has suggested that such agreements between innovators and generic drug makers
keep lower cost generic drugs off the market. On the Provigil case, Watson
Pharma entered into an agreement with Cephalon (U.S.) along with other generic
drug makers to sell modafinil. The innovator, Cephalon, recently lost its bid to
dismiss the pay-for-delay lawsuit in Pennsylvania (seeUnited States: 31 March
2010:).
LOAD-DATE: July 21, 2010
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140 of 998 DOCUMENTS
Washington Drug Letter
July 19, 2010 Monday
Judge Orders FTC to Answer Watson CEO's Allegations
SECTION: Vol. 42 No. 28
LENGTH: 496 words
A federal judge has ordered the FTC to answer questions about allegations it
released proprietary information as it tried to thwart a reverse-payment
settlement between Watson Pharmaceuticals and Cephalon over Cephalon's drug
Provigil.
Judge Alan Kay of the U.S. District Court of the District of Columbia Tuesday
issued an order instructing the FTC to answer questions posed in a motion by
Watson CEO Paul Bisaro, who claims the commission shared proprietary company
information with Apotex. The FTC challenged Watson's licensing agreement -- a
"pay-for-delay" deal -- for the excessive sleepiness drug Provigil (modafinil)
and tried to broker an agreement between Watson and Apotex instead, hoping the
result would be cheaper modafinil generics.
"This Court finds that the facts before it present a strong possibility that the
FTC did share confidential information with Watson's competitor, that it did
attempt to broker a deal between Apotex and Watson that would require Watson to
relinquish any statutory 'first filer' rights it had acquired, and that it did
initiate this investigation to pressure Watson to relinquish these rights and to
harass it when it refused," Kay wrote.
Bisaro has claimed the FTC's efforts to subpoena him as part of a pay-for-delay
investigation was tantamount to harassment, prompting his lawyers to file a
request that the commission answer questions related to its alleged information
sharing (WDL, June 7).
The FTC must provide the court, by July 23, descriptions of communications it
had with the FDA and third parties regarding potential marketing exclusivity for
generic modafinil and whether any confidential information was disclosed.
"The facts before us suggest that the FTC sought to place Watson between a rock
and a hard place, where the only way Watson could clear its name and escape
further FTC scrutiny was to give in to the pressure the FTC was placing on
Watson to enter into the business deal with Apotex," Kay added.
Glenn Lammi, an attorney with the Washington Legal Foundation, told WDL Kay's
ruling was "extraordinary, considering how infrequently judges allow discoveries
in these cases."
Kay, however, rejected a request from Bisaro's lawyers to depose Markus Meier,
assistant director of the FTC's Bureau of Competition Health Care Division. Last
month, two senators pressed FTC Chairman Jon Leibowitz on the agency's alleged
action in the Watson matter, with Leibowitz claiming Meier did not breach the
company's confidentiality (WDL, June 14).
FTC Bureau of Competition Director Richard Feinstein disagreed with Kay's
ruling, adding the agency has done nothing improper.
The FTC "is simply trying to complete a law enforcement investigation into
whether there is an agreement to keep generic drugs off the market and out of
the hands of consumers," Feinstein said. "We are disappointed that our
investigation has been sidetracked by the unfounded implications of opposing
counsel." -- Jonathan Block
Release date: July 19, 2010
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LANGUAGE: ENGLISH
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Drug Industry Daily
July 15, 2010 Thursday
Judge Orders FTC to Answer Watson CEO's Allegations
SECTION: Vol. 9 No. 136
LENGTH: 497 words
A federal judge has ordered the FTC to answer questions about allegations it
released proprietary information as it tried to thwart a reverse-payment
settlement between Watson Pharmaceuticals and Cephalon over Cephalon's drug
Provigil.
Judge Alan Kay of the U.S. District Court of the District of Columbia Tuesday
issued an order instructing the FTC to answer questions posed in a motion by
Watson CEO Paul Bisaro, who claims the commission shared proprietary company
information with Apotex. The FTC challenged Watson's licensing agreement -- a
"pay-for-delay" deal -- for the excessive sleepiness drug Provigil (modafinil)
and tried to broker an agreement between Watson and Apotex instead, hoping the
result would be cheaper modafinil generics.
"This Court finds that the facts before it present a strong possibility that the
FTC did share confidential information with Watson's competitor, that it did
attempt to broker a deal between Apotex and Watson that would require Watson to
relinquish any statutory 'first filer' rights it had acquired, and that it did
initiate this investigation to pressure Watson to relinquish these rights and to
harass it when it refused," Kay wrote.
Bisaro has claimed that the FTC's efforts to subpoena him as part of a
pay-for-delay investigation was tantamount to harassment, prompting his lawyers
to file a request that the commission answer questions related to its alleged
information sharing (DID, June 1).
The FTC must provide the court, by July 23, descriptions of communications it
had with the FDA and third parties regarding potential marketing exclusivity for
generic modafinil and whether any confidential information was disclosed.
"The facts before us suggest that the FTC sought to place Watson between a rock
and a hard place, where the only way Watson could clear its name and escape
further FTC scrutiny was to give in to the pressure the FTC was placing on
Watson to enter into the business deal with Apotex," Kay added.
Glenn Lammi, an attorney with the Washington Legal Foundation, told DID Kay's
ruling was "extraordinary, considering how infrequently judges allow discoveries
in these cases."
Kay, however, rejected a request from Bisaro's lawyers to depose Markus Meier,
assistant director of the FTC's Bureau of Competition Health Care Division. Last
month, two senators pressed FTC Chairman Jon Leibowitz on the agency's alleged
action in the Watson matter, with Leibowitz claiming Meier did not breach the
company's confidentiality (DID, June 11).
FTC Bureau of Competition Director Richard Feinstein disagreed with Kay's
ruling, adding the agency has done nothing improper.
The FTC "is simply trying to complete a law enforcement investigation into
whether there is an agreement to keep generic drugs off the market and out of
the hands of consumers," Feinstein said. "We are disappointed that our
investigation has been sidetracked by the unfounded implications of opposing
counsel." -- Jonathan Block
Release date: July 15, 2010
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LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
142 of 998 DOCUMENTS
Indian Patents News
July 12, 2010 Monday 6:30 AM EST
French Inventors Develop 'Combination of Modafinil and an Antagonist or Inverse
Agonist of the H3 Receptor'
LENGTH: 107 words
New Delhi, July 12 -- Schwartz Jean-Charles and Lecomte Jeanne-Marie of
Bioprojet, Paris, France have developed 'combination of modafinil and an
antagonist or inverse agonist of the H3 receptor'.Bioprojet filed the patent
application on Feb. 18, 2009. The patent application number is 380/MUMNP/2009
A.According to the Controller General of Patents, Designs & Trade Marks, "The
invention relates to the combination of modafinil and at least one antagonist or
inverse agonist of the histamine H3 receptor, which is particularly useful for
the treatment of narcolepsy-cataplexy and more generally for sleeping, vigilance
or attention disorders."
LOAD-DATE: July 12, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
143 of 998 DOCUMENTS
The Express
July 7, 2010 Wednesday
Edition 1;
National Edition
'Smart drugs' help students pass exams
BYLINE: Sarah OGrady
SECTION: NEWS; Pg. 7
LENGTH: 246 words
MORE students than ever are using "smart drugs" to boost their exam performance,
senior drug advisers warn.
A growing number of undergraduates - and their professors - are buying
prescription drugs such as Modafinil and Ritalin over the internet from
suppliers as far away as India.
Barbara Sahakian, professor of clinical neuropsychology at the University of
Cambridge, said: "I've seen students tear open the envelope from Mumbai in
excitement.
"But when you are accessing drugs over the internet it's completely
unsupervised.
"You might be on other drugs or have some preexisting condition that means you
shouldn't be taking it."
Studies show Modafinil increases motivation and ability to concentrate, but it
can be dangerous for people with high blood pressure. Side effects of Ritalin
can include mood swings, increased heart rate, dizziness and insomnia.
Prof Sahakian was asked to research the problem by the Advisory Council for the
Misuse of Drugs. She has called for a Government policy review on smart drugs.
A recent survey of 1,000 Cambridge undergraduates showed that one in 10 had used
cognitive-enhancing drugs - also known as "professor's little helpers".
Another third said they would use them if they had access to them. One in five
academics also admitted taking the drugs.
But fears are growing that students who order the drugs online could be exposing
themselves to health risks or buying counterfeit drugs.
They can also get hooked and can't wean themselves off them.
LOAD-DATE: July 7, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: DXP
Copyright 2010 Express Newspapers
All Rights Reserved
144 of 998 DOCUMENTS
Indian Patents News
June 24, 2010 Thursday 6:30 AM EST
Irish Inventors Develop Nanoparticulate Formulations of Modafinil
LENGTH: 173 words
New Delhi, June 24 -- Jenkins Scott, Liversidge Gary and Manser David of Elan
Corporation, PLC, Dublin, Ireland have developed nanoparticulate formulations of
modafinil.Elan Corporation, PLC filed the patent application on Jan. 16, 2009.
The patent application number is 210/KOLNP/2009 A.According to the Controller
General of Patents, Designs & Trade Marks, "The present invention is directed to
compositions comprising a nanoparticulate modafinil compositions, or a salt(s),
or an enantiomer(s), or a prodrug(s), or a polymorph(s) or derivative thereof,
having improved bioavailability. The nanoparticulate modafinil composition
formulation particles of the composition have an effective average particle size
of less than about 2000 nm and are useful in the treatment of dyssomnias,
including but not limited to, narcolepsy, chronic fatigue, eating disorders,
compulsive behaviors, ADIID, addictions, substance abuse, sleepiness, nervous
system diseases, conditions, syndromes, and symptoms and related diseases,
conditions, and symptoms."
LOAD-DATE: June 24, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
145 of 998 DOCUMENTS
Generic Line
June 9, 2010 Wednesday
Watson CEO Alleges FTC Harassment in Provigil Pay-for-Delay Case
SECTION: Vol. 27 No. 12
LENGTH: 339 words
Watson Pharmaceuticals CEO Paul Bisaro is accusing the FTC of harassment in its
effort to get him to testify in an ongoing case regarding a pay-for-delay
settlement with Cephalon.
"The FTC's pursuit of the subpoena demonstrates that its conduct is nothing
short of harassment," Bisaro's lawyers claim in a document submitted recently to
the U.S. District Court for the District of Columbia. Enforcing the subpoena
would be tantamount to abuse of the court's process, they add.
The FTC challenged Watson's licensing agreement for Cephalon's excessive
sleepiness drug Provigil (modafinil) and tried to broker an agreement between
Watson and Apotex instead, hoping to provide cheaper modafinil generics,
according to court documents.
Cephalon reached the settlement with Watson in 2006, allowing Watson partner
Carlsbad Technology to manufacture the modafinil generic prior to patent expiry.
Four other generic-drug makers also made deals with Cephalon on Provigil
generics (Generic Line, May 12).
The deals have been the subject of several lawsuits against the companies
involved, the latest of which came May 27 when the supermarket and pharmacy
chain Giant Eagle challenged the settlements in a suit filed in the U.S.
District Court for the Northern District of Ohio. Cephalon's settlements with
the various generic makers delay competition and amount to an effort to
monopolize the market for Provigil, the suit says.
In his action, Bisaro claims he should not be subpoenaed in Federal Trade
Commission v. Paul M. Bisaro since he was not employed by Watson when the
agreement with Cephalon was signed.
The FTC is pursuing the subpoena either to pressure Watson into reaching an
agreement with Apotex or to retaliate against the company, Bisaro's lawyers say.
They also accuse the FTC of sharing with Apotex some of Watson's privileged
information, submitted to the FDA, as evidenced by an internal email Apotex
forwarded to Watson.
The FTC has said ending pay-for-delay settlements is a top priority. -- Jonathan
Block
Release date: June 9, 2010
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LANGUAGE: ENGLISH
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All Rights Reserved
146 of 998 DOCUMENTS
Washington Drug Letter
June 7, 2010 Monday
Watson CEO Claims FTC Subpoena Is Harassment or Retaliation
SECTION: Vol. 42 No. 23
LENGTH: 341 words
Watson Pharmaceuticals CEO Paul Bisaro is accusing the FTC of harassment in its
effort to get him to testify in an ongoing case regarding a pay-for-delay
settlement with Cephalon.
"The FTC's pursuit of the subpoena demonstrates that its conduct is nothing
short of harassment," Bisaro's lawyers claim in a document submitted recently to
the U.S. District Court for the District of Columbia. Enforcing the subpoena
would be tantamount to abuse of the court's process, they add.
The FTC challenged Watson's licensing agreement for Cephalon's excessive
sleepiness drug Provigil (modafinil) and tried to broker an agreement between
Watson and Apotex instead, hoping to provide cheaper modafinil generics,
according to court documents.
Cephalon reached the settlement with Watson in 2006, allowing Watson partner
Carlsbad Technology to manufacture the modafinil generic prior to patent expiry.
Four other generic-drug makers also made deals with Cephalon on Provigil
generics (WDL, May 3).
Settlements Challenged
The deals have been the subject of several lawsuits against the companies
involved, the latest of which came May 27 when the supermarket and pharmacy
chain Giant Eagle challenged the settlements in a suit filed in the U.S.
District Court for the Northern District of Ohio. Cephalon's settlements with
the various generic makers delay competition and amount to an effort to
monopolize the market for Provigil, the suit says.
In his action, Bisaro claims he should not be subpoenaed in Federal Trade
Commission v. Paul M. Bisaro since he was not employed by Watson when the
agreement with Cephalon was signed.
The FTC is pursuing the subpoena either to pressure Watson into reaching an
agreement with Apotex or to retaliate against the company, Bisaro's lawyers say.
They also accuse the FTC of sharing some of Watson's privileged information,
submitted to the FDA, with Apotex, as evidenced by an internal email Apotex
forwarded to Watson.
The FTC has said ending pay-for-delay settlements is a top priority. -- Jonathan
Block
Release date: June 7, 2010
LOAD-DATE: June 7, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
147 of 998 DOCUMENTS
PR Newswire
June 2, 2010 Wednesday 4:30 PM EST
Cephalon Provides Clinical Update on Phase II Study of NUVIGIL as an Adjunctive
Therapy in Adults with Schizophrenia
LENGTH: 947 words
DATELINE: FRAZER, Pa., June 2
FRAZER, Pa., June 2 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced that the primary endpoint was not met in a Phase II clinical
trial that examined NUVIGIL® (armodafinil) Tablets [C-IV] as an adjunctive
therapy for the treatment of the negative symptoms of schizophrenia, which
include problems with motivation and emotional withdrawal. The analysis of the
data showed that treatment with armodafinil did not lessen the severity of the
negative symptoms of schizophrenia compared to placebo in the 24-week study. As
a result of the outcome of this trial, Cephalon has decided not to move forward
with this clinical program.
The trial was designed to evaluate whether armodafinil treatment (150, 200, or
250 mg/day) was more effective than placebo treatment as an adjunctive therapy
to antipsychotic medication in alleviating the negative symptoms of
schizophrenia, as assessed by the primary outcome measure of the Positive and
Negative Syndrome Scale. Although an interim analysis showed a trend towards a
positive dose dependent treatment effect, it was not statistically significant
and not maintained in the final analysis of all patients. Armodafinil was
generally well tolerated in the study and the side effects were consistent with
the known safety profile. Results of this study will be presented at a future
medical meeting.
"While we are disappointed that the results of this study did not demonstrate a
benefit for this patient population, Cephalon remains committed to the NUVIGIL
clinical development plan," said Dr. Lesley Russell, Chief Medical Officer at
Cephalon. "We are continuing our discussions with the agency on our application
for excessive sleepiness associated with jet lag disorder and Phase III trials
are on track evaluating armodafinil in bipolar depression and excessive
sleepiness resulting from traumatic brain injury."
About NUVIGIL
NUVIGIL is the longer-lasting isomer of modafinil. It is indicated to improve
wakefulness in patients with excessive sleepiness associated with treated
obstructive sleep apnea (OSA), shift work disorder (SWD), or narcolepsy. NUVIGIL
is not approved as a treatment for jet lag disorder, bipolar depression,
traumatic brain injury, or their associated symptoms. The NUVIGIL (armodafinil)
label includes a bolded warning for serious or life-threatening rash, including
Stevens-Johnson Syndrome, that has been reported in adults in association with
the use of armodafinil and in adults and children in association with the use of
modafinil, a racemic mixture of S and R modafinil (the latter is armodafinil,
the active ingredient in NUVIGIL). NUVIGIL is not approved for use in pediatric
patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness, and insomnia. Full prescribing
information for NUVIGIL is available at http://www.nuvigil.com/.
About Cephalon, Inc.
Cephalon is a global biopharmaceutical company dedicated to discovering,
developing and bringing to market medications to improve the quality of life of
individuals around the world. Since its inception in 1987, Cephalon has brought
first-in-class and best-in-class medicines to patients in several therapeutic
areas. Cephalon has the distinction of being one of the world's fastest-growing
biopharmaceutical companies, now among the Fortune 1000 and a member of the S&P
500 Index, employing approximately 4,000 people worldwide. The company sells
numerous branded and generic products around the world. In total, Cephalon sells
more than 150 products in nearly 100 countries. More information on Cephalon and
its products is available at http://www.cephalon.com/.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results; prospects for regulatory approval; manufacturing development
and capabilities; market prospects for its products; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
Contacts:
Media: Investor Relations:
Candace Steele Flippin Chip Merritt
610-727-6231 (office) 610-738-6376 (office)
csteele@cephalon.com cmerritt@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media: Candace Steele Flippin, +1-610-727-6231 (office),
csteele@cephalon.com, Investor Relations: Chip Merritt, +1-610-738-6376
(office), cmerritt@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: June 3, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 PR Newswire Association LLC
All Rights Reserved
148 of 998 DOCUMENTS
Drug Industry Daily
June 1, 2010 Tuesday
Watson CEO Accuses FTC of Harassment in Pay-for-Delay Case
SECTION: Vol. 9 No. 105
LENGTH: 337 words
Watson Pharmaceuticals CEO Paul Bisaro is accusing the FTC of harassment in its
effort to get him to testify in an ongoing case regarding a pay-for-delay
settlement with Cephalon.
"The FTC's pursuit of the subpoena demonstrates that its conduct is nothing
short of harassment," Bisaro's lawyers claim in a document submitted recently to
the U.S. District Court for the District of Columbia. Enforcing the subpoena
would be tantamount to abuse of the court's process, they add.
The FTC challenged Watson's licensing agreement for Cephalon's excessive
sleepiness drug Provigil (modafinil) and tried to broker an agreement between
Watson and Apotex instead, hoping to provide cheaper modafinil generics,
according to court documents.
Cephalon reached the settlement with Watson in 2006, allowing Watson partner
Carlsbad Technology to manufacture the modafinil generic prior to patent expiry.
Four other generic-drug makers also made deals with Cephalon on Provigil
generics (DID, April 27).
The deals have been the subject of several lawsuits against the companies
involved, the latest of which came Thursday when the supermarket and pharmacy
chain Giant Eagle challenged the settlements in a suit filed in the U.S.
District Court for the Northern District of Ohio. Cephalon's settlements with
the various generic makers delay competition and amount to an effort to
monopolize the market for Provigil, the suit says.
In his action, Bisaro claims he should not be subpoenaed in Federal Trade
Commission v. Paul M. Bisaro since he was not employed by Watson when the
agreement with Cephalon was signed.
The FTC is pursuing the subpoena either to pressure Watson into reaching an
agreement with Apotex or to retaliate against the company, Bisaro's lawyers say.
They also accuse the FTC of sharing some of Watson's privileged information,
submitted to the FDA, with Apotex, citing an internal email Apotex forwarded to
Watson.
The FTC has said ending pay-for-delay settlements is a top priority. -- Jonathan
Block
Release date: June 1, 2010
LOAD-DATE: June 1, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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All Rights Reserved
149 of 998 DOCUMENTS
Fleet Owner
June 1, 2010
Help in a pill or a cup
SECTION: Pg. 35
LENGTH: 498 words
Songwriters may love to romanticize outlaw truckers who take amphetamines to
keep driving for days, but the reality is drivers (who are routinely tested for
illegal drug use) favor the same stimulant everyone else uses in our Starbucks
culture - caffeine.
When it comes to staying alert behind the driver's wheel, "caffeine is a very
useful tool," according to Todd Dawson of Circadian. "It does what it's supposed
to - it boosts reaction times, but it's overused in our society. Taken in high
amounts, caffeine can not only create health problems, but you build up a
tolerance."
Instead of drinking coffee throughout the day, perhaps consuming as much as
eight cups, truck drivers should drink a cup or two at the start of their
workday and then another one or two cups only when they begin to feel drowsy
later in the day. "The [caffeine] benefit is much higher when it's used
carefully," Dawson says.
Gerald Krueger, who is putting together a report on stimulants, hypnotics and
nutritional supplements for the Transportation Research Board, agrees that
caffeine used properly is a practical tool to help retain alertness. What
concerns him are the "energy boost" products and other supplements marketed at
truckstops. While caffeine is often a major component in these products,
"there's not been much good, solid medical research published to be able to
assess whether they're good or bad," says Krueger.
Prescription stimulant drugs have much stronger effects than caffeine, but most
of the well-known ones such as amphetamines have serious side effects.
However, lately there's been a good deal of attention focused on a new stimulant
compound known as Modafinil, which is available in the U.S. as the prescription
drug Provigil. Krueger says that while Modafinil does boost alertness much like
caffeine, an attractive feature is that "while under the influence of Modafinil,
one can apparently still decide to go to sleep, for example, something no other
stimulant would permit you to do."
Krueger also said that the U.S. military administers prescription stimulants,
including Modafinil, in some very select operational circumstances, but only
after evaluating how individuals perform when taking the drugs in controlled
settings and then monitoring them closely if they do take them in the field.
"Currently, there doesn't seem to be any practical application in trucking for
stimulants other than using caffeine because there's no way to control their use
with a large population like truck drivers," says Krueger. "But we shouldn't
hide our head in the sand. We should be doing good quality medical research on
these compounds to see if there are practical applications for newer compounds
as they are developed."
For now, though, Krueger believes the best solution for drivers is "the natural
way." Combining proper sleep habits with an understanding of circadian rhythms,
"they can use the strengths of knowing more about their own body's physiology to
help manage fatigue," he says.
LOAD-DATE: June 10, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
Copyright 2010 Penton Business Media, Inc.
All Rights Reserved
150 of 998 DOCUMENTS
Indian Patents News
May 31, 2010 Monday 6:30 AM EST
American Inventors Develop Pharmaceutical Formulations of Modafinil
LENGTH: 136 words
New Delhi, May 31 -- Craig Heacock, Alpa Parikh and Piyush Patel of Cephalon,
Inc, West Chester, USA have developed pharmaceutical formulations of modafinil
.Cephalon, Inc filed the patent application on Aug. 10, 2007. The patent
application number is 2937/KOLNP/2007 A.According to the Controller General of
Patents, Designs & Trade Marks, "Use of a composition consisting essentially of
about 250 to about 450 mg of solid modafinil and one or more diluents, each
independently chosen from a starch, a lactose monohydrate or a microcrystalline
cellulose; one or more disintegrates, each independently chosen from a pre
gelatinized starch or a cross-linked sodium carboxymethly cellulose; a binder;
and a lubricant for preparation of a medicament for treating attention deficit
hyperactivity disorder in a human subject."
LOAD-DATE: June 21, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
151 of 998 DOCUMENTS
Prospect
May 27, 2010
Going mental
BYLINE: Barbara J Sahakian and Ahmed D Mohamed
LENGTH: 748 words
Who could object to drugs that help people affected by mental disorders such as
schizophrenia? Such treatments, known as pharmacological cognitive enhancers
(PCEs) can improve memory, attention and motivation. Methylphenidate (Ritalin),
for example, helps children with attention deficit hyperactivity disorder (ADHD)
focus better in school, often making an important difference to their lives.
Modafinil (Provigil) helps people stay awake and is licensed for the treatment
of narcolepsy, a condition that causes sufferers to fall asleep involuntarily.
So far, so good. But the past few years have seen an unprecedented rise in the
use of PCEs by healthy people. For many students, the temptation to pop a few
pills to aid concentration-especially at exam time-is hard to resist. Most of
them see it as harmless and ethically acceptable. Others see it as cheating and,
as yet, few universities have formal policies on the issue.
According to a 2004 report in the Journal of the American Medical Association,
around 90 per cent of modafinil is used by healthy, non-sleep-deprived
individuals. In March 2009, an informal survey of 1,000 students by the
Cambridge University student newspaper Varsity showed that one in ten were
taking prescription drugs for cognitive enhancement. The year before, Nature
conducted a poll of 1,400 scientists from 60 different countries. One in five
respondents used drugs for cognitive enhancement, of which 62 per cent reported
taking methylphenidate and 44 per cent modafinil, mainly to improve
concentration. Fifteen per cent said they took beta-blockers for anxiety, when
such drugs are normally prescribed to reduce blood pressure or irregular heart
rhythms.
One American professor said he obtained his drugs through his primary care
doctor by claiming to have jet lag, while one British professor got his through
the internet to "enhance productivity" and "for important intellectual
challenges." More worrying, a 2009 survey by the US National Institute on Drug
Abuse (Nida) found that 1.8 per cent of 13 to 14 year olds, 3.6 per cent of 15
to 16 year olds and 2.1 per cent of 17 to 18 year olds abused methylphenidate.
The widespread use of cognition- enhancing drugs is perhaps not surprising given
that the Academy of Medical Sciences's 2008 report on brain science, addiction
and drugs suggested that a 10 per cent improvement in memory score could lead to
a higher A-level grade or degree classification. Small improvements in
intellectual performance can lead to significant improvements in outcomes.
But what are the advantages and disadvantages of healthy people using PCEs? On
the plus side, since PCEs may help those with low cognitive performance, it
might be possible to mitigate the effects of poverty on the brain through their
use. This could have positive effects on society and the economy as a whole: it
has been estimated that a 3 per cent population-wide increase in IQ could reduce
poverty rates by up to 25 per cent and increase GDP by up to 1.5 per cent.
Of course, even healthy adults who normally function well do not necessarily do
their best all the time, because of sleep deprivation, jet lag or other
stressors. And PCEs might also enable us to perform better in pleasurable and
competitive situations. For instance, Anjan Chatterjee, a neurologist at the
University of Pennsylvania, reported that musicians often use beta-blockers to
dampen physical tremors, improving their performance. Psychostimulants have also
been used to boost soldiers in combat, shift workers and pilots.
But not enough is known about the long-term side effects of PCEs, especially in
the developing brain. A 2009 report by Nida found that modafinil stimulated
areas in the brain known to trigger drug seeking behaviour and addiction.
We must also consider why these drugs are being used. Is the pressure to do well
in exams, clinch a business deal, or keep up with our "24/7 society" pushing
people to use them, instead of traditional means of boosting cognition, such as
exercise?
Clearly, neuroscientists need to work together with social scientists,
philosophers, ethicists, policymakers and other experts to establish clear, safe
and ethical rules for PCE use in healthy people. This is the only way that the
major advances now being made in brain science can be put to maximum benefit-and
minimal harm.
Barbara J Sahakian is a professor of clinical neuropsychology at Cambridge
University. Ahmed D Mohamed is a PhD student at Clare Hall, Cambridge
?
LOAD-DATE: May 21, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
Copyright 2010 Prospect Magazine
All Rights Reserved
152 of 998 DOCUMENTS
Generic Line
May 12, 2010 Wednesday
FTC Labels Pay-for-Delay Fight an Agency Top Priority in 2010
SECTION: Vol. 27 No. 10
LENGTH: 502 words
The FTC is making its fight against pay-for-delay settlements between brand- and
generic-drug makers a top priority this year.
The patent settlements, in which brand companies reward generic-drug makers to
delay the introduction of less expensive versions of their medicines, keep
generic drugs off the market for an average of 17 months longer than agreements
without payments and will cost consumers and taxpayers $35 billion over the next
10 years, the commission says in its annual report.
The FTC also is pursuing actions against drugmakers in federal court cases. In
one case, the agency lodged a complaint against Cephalon in 2008, alleging the
drugmaker paid four companies to refrain from selling generic versions of its
sleep drug Provigil (modafinil) until 2012 (Generic Line, Feb. 20, 2008).
The company entered into seemingly separate transactions worth a total of more
than $200 million, the FTC said in 2008 (Generic Line, May 28, 2008). For
example, Teva Pharmaceuticals agreed not to launch generic Provigil until April
2012 in exchange for a license agreement relating to its modafinil patents and
patent applications worth up to $125 million in Provigil royalties. Cephalon
also agreed to buy modafinil active pharmaceutical ingredient from Teva at
prices higher than what it had been paying, the commission alleged at the time.
The case is still pending in the U.S. District Court for the Eastern District of
Pennsylvania, the FTC says.
In a separate case, the commission obtained $2.1 million from Bristol-Myers
Squibb (BMS) for failing to inform the FTC of agreements reached with Canadian
drugmaker Apotex regarding potential generic competition for blockbuster drug
Plavix, according to the report. The commission charged that, as part of a
patent settlement with Apotex, BMS promised it would not compete with Apotex
during the first 180 days that Apotex marketed its generic version of the drug.
The FTC suffered a defeat, however, in a case in which it claimed reverse
payment, or pay-for-delay, settlements Solvay Pharmaceuticals made with Watson
Pharmaceuticals, Par Pharmaceutical and Paddock Laboratories for the marketing
of generic AndroGel (testosterone) violated federal antitrust laws.
The U.S. District Court for the Northern District of Georgia dismissed the case
in February, saying patent litigation is too complex and the results too
uncertain to assert such a claim (Generic Line, March 3).
The agency also had hoped that a ban on the agreements would be included in
healthcare overhaul legislation signed into law earlier this year, but the
provision was not included in the final bill. Sen. Herb Kohl (D-Wis.) has
indicated he will fight for his pay-for-delay bill, Preserve Access to
Affordable Generics Act, S. 369, to be considered as an individual piece of
legislation by the full Senate or piggyback on another bill (Generic Line, March
31).
The FTC annual report is available at
www.ftc.gov/os/2010/04/2010ChairmansReport_screen.pdf. -- David Belian
Release date: May 12, 2010
LOAD-DATE: May 12, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
153 of 998 DOCUMENTS
Penton Insight
May 11, 2010
Helping drivers stay alert
BYLINE: By Jim Mele, editor-in-chief
LENGTH: 561 words
When it comes to staying alert behind the driver's wheel,"caffeine is a very
useful tool," according to ToddDawson, vp of the fatigue management company
Circadian. "It does what it'ssupposed to - it boosts reaction times, but
it'soverused in our society. Taken in high amounts, caffeine can notonly create
health problems, but you build up atolerance."
The stimulant effect of the caffeine in two cups of coffee lastsfive to seven
hours, he said. Instead of drinking coffee throughoutthe day, perhaps consuming
as much as eight cups, truck driversshould drink a cup or two at the start of
their work day and thenanother one or two cups only when they begin to feel
drowsy laterin the day.
"The benefit [from caffeine] is much higher whenit's used carefully," Dawson
said
Gerald Krueger, a well-known researcher who is currentlyputting together a
report on stimulants, hypnotics and nutritionalsupplements for the
Transportation Research Board, agrees thatcaffeine used properly is a practical
tool to help truck driversretain alertness during those naturally occurring
times when aperson becomes drowsy.
What concerns him are the "energy boost" productsand other nutritional
supplements commonly marketed to drivers attruckstops. While caffeine is often
a major component inthese products, "there's not been much good solidmedical
research published to be able to assess whetherthey're good or bad, or whether
they produce interactionswith other substances like allergy medicines,"
Kruegersaid.
Prescription stimulant drugs have much stronger effects thancaffeine, but most
of the well-known ones such as amphetamines haveserious side effects that after
long-term use might includeinsomnia and addiction. However lately there's been
agood deal of attention focused on a new stimulant compound known asmodafinil
which is available in the U.S. as the prescription drugProVigil. Krueger said
that while modafinil does boostalertness much like caffeine, an attractive
feature is that"while under the influence of modafinil, one can apparentlystill
decide to go to sleep, to take a nap for example, somethingno other stimulant
would permit you to do."
Krueger also said that the U.S. military administersprescription stimulants,
including modafinil, in some very selectoperational circumstances, but only
after evaluating howindividuals perform when taking the drugs in controlled
settingsand then monitoring them closely if they do take them in thefield.
"Currently there doesn't seem to be any practicalapplication in trucking for
stimulants other than using caffeinebecause there's no way to control their use
with alarge population like truck drivers," said Krueger.
"But we shouldn't hide our head in the sand,"said Krueger. "We should be doing
good quality medicalresearch on these compounds to see if there are
practicalapplications for some newer compounds as they aredeveloped." For
example, he pointed out that the U.S.military explored and now safely issues
caffeinated chewing gum totired troops, and this would seem to be an appropriate
applicationfor commercial drivers as well.
For now, though, Krueger believes the best solution for driversis "the natural
way." Combining proper sleep habitswith an understanding for their circadian
rhythms, "they canuse the strengths of knowing more about their own
body'sphysiology to help manage fatigue," Krueger noted.
LOAD-DATE: May 12, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2010 Penton Business Media, Inc.
All Rights Reserved
154 of 998 DOCUMENTS
Washington Drug Letter
May 3, 2010 Monday
FTC Fight Against Pay-for-Delay Becomes a Top Priority in 2010
SECTION: Vol. 42 No. 18
LENGTH: 496 words
The FTC is making its fight against pay-for-delay settlements between brand- and
generic-drug makers a top priority this year.
The patent settlements, in which brand companies reward generic-drug makers to
delay the introduction of less expensive versions of their medicines, keep
generic drugs off the market for an average of 17 months longer than agreements
without payments and will cost consumers and taxpayers $35 billion over the next
10 years, the commission says in its annual report.
The FTC also is pursuing actions against drugmakers in federal court cases. In
one case, the agency lodged a complaint against Cephalon in 2008, alleging the
drugmaker paid four companies to refrain from selling generic versions of its
sleep drug Provigil (modafinil) until 2012 (WDL, Feb. 18, 2008).
The company entered into seemingly separate transactions worth a total of more
than $200 million, the FTC said in 2008 (WDL, May 26, 2008). For example, Teva
Pharmaceuticals agreed not to launch generic Provigil until April 2012 in
exchange for a license agreement relating to its modafinil patents and patent
applications worth up to $125 million in Provigil royalties. Cephalon also
agreed to buy modafinil active pharmaceutical ingredient from Teva at prices
higher than what it had been paying, the commission alleged at the time.
The case is still pending in the U.S. District Court for the Eastern District of
Pennsylvania, the FTC says.
In a separate case, the commission obtained $2.1 million from Bristol-Myers
Squibb (BMS) for failing to inform the FTC of agreements reached with Canadian
drugmaker Apotex regarding potential generic competition for blockbuster drug
Plavix, according to the report. The commission charged that, as part of a
patent settlement with Apotex, BMS promised it would not compete with Apotex
during the first 180 days that Apotex marketed its generic version of the drug.
The FTC suffered a defeat, however, in a case in which it claimed reverse
payment, or pay-for-delay, settlements Solvay Pharmaceuticals made with Watson
Pharmaceuticals, Par Pharmaceutical and Paddock Laboratories for the marketing
of generic AndroGel (testosterone) violated federal antitrust laws.
The U.S. District Court for the Northern District of Georgia dismissed the case
in February, saying patent litigation is too complex and the results too
uncertain to assert such a claim (WDL, March 1).
The agency also had hoped that a ban on the agreements would be included in
healthcare overhaul legislation signed into law earlier this year, but the
provision was not included in the final bill. Sen. Herb Kohl (D-Wis.) has
indicated he will fight for his pay-for-delay bill, Preserve Access to
Affordable Generics Act, S. 369, to be considered as an individual piece of
legislation by the full Senate or piggyback on another bill (WDL, March 22).
The FTC annual report is available at
www.ftc.gov/os/2010/04/2010ChairmansReport_screen.pdf. -- David Belian
Release date: May 3, 2010
LOAD-DATE: May 3, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
155 of 998 DOCUMENTS
Drug Industry Daily
April 27, 2010 Tuesday
FTC: Ending Pay-for-Delay Settlements is Top Priority
SECTION: Vol. 9 No. 81
LENGTH: 503 words
The FTC is making its fight against pay-for-delay settlements between brand- and
generic-drug makers a top priority this year.
The patent settlements, in which brand companies reward generic-drug makers to
delay the introduction of less expensive versions of their medicines, keep
generic drugs off the market for an average of 17 months longer than agreements
without payments and will cost consumers and taxpayers $35 billion over the next
10 years, the commission says in its annual report.
The FTC also is pursuing actions against drugmakers in federal court cases. In
one case, the agency lodged a complaint against Cephalon in 2008, alleging the
drugmaker paid four companies to refrain from selling generic versions of its
sleep drug Provigil (modafinil) until 2012 (DID, Feb. 15, 2008).
The company entered into seemingly separate transactions worth a total of more
than $200 million, the FTC said in 2008 (DID, May 23, 2008). For example, Teva
Pharmaceuticals agreed not to launch generic Provigil until April 2012 in
exchange for a license agreement relating to its modafinil patents and patent
applications worth up to $125 million in Provigil royalties. Cephalon also
agreed to buy modafinil active pharmaceutical ingredient from Teva at prices
higher than what it had been paying, the commission alleged at the time.
The case is still pending in the U.S. District Court for the Eastern District of
Pennsylvania, the FTC says.
In a separate case, the commission obtained $2.1 million from Bristol-Myers
Squibb (BMS) for failing to inform the FTC of agreements reached with Canadian
drugmaker Apotex regarding potential generic competition for blockbuster drug
Plavix, the commission says in the report. The commission charged that, as part
of a patent settlement with Apotex, BMS promised that it would not compete with
Apotex during the first 180 days that Apotex marketed its generic version of the
drug.
The agency suffered a defeat, however, in a case in which it claimed reverse
payment, or pay-for-delay, settlements Solvay Pharmaceuticals made with Watson
Pharmaceuticals, Par Pharmaceutical and Paddock Laboratories for the marketing
of generic AndroGel (testosterone) violated federal antitrust laws.
The U.S. District Court for the Northern District of Georgia dismissed the case
in February, saying patent litigation is too complex and the results too
uncertain to assert such a claim (DID, Feb. 25).
The agency had also hoped that a ban on the agreements would be included in
healthcare overhaul legislation signed into law earlier this year, but the
provision failed to be included in the final bill. Sen. Herb Kohl (D-Wis.),
however, has indicated that he will fight for his pay-for-delay bill Preserve
Access to Affordable Generics Act, S. 369, to be considered as an individual
piece of legislation by the full Senate or piggyback on another bill (DID, March
23).
The FTC annual report can be found at
www.ftc.gov/os/2010/04/2010ChairmansReport_screen.pdf. -- David Belian
Release date: April 27, 2010
LOAD-DATE: April 27, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2010 Washington Business Information, Inc.
All Rights Reserved
156 of 998 DOCUMENTS
The Guardian (London) - Final Edition
April 6, 2010 Tuesday
Education: Smart work: Students are increasingly taking neuroenhancing drugs to
fight fatigue and help them concentrate. But how safe are they - and is it
cheating?
BYLINE: Catherine Nixey
SECTION: GUARDIAN EDUCATION PAGES; Pg. 1
LENGTH: 1362 words
It is an all too common story: a diligent student works hard and finally
achieves a coveted place at Cambridge University. Once there, the pressure
becomes too great and they turn to drugs. These days, however, the old narrative
has changed. Instead of the spliffs that apparently so delighted generations of
our politicians, the latest fad is for educational, not recreational, drugs.
"It was the summer term of my second year," explains Raj Perera, in his final
year of a natural sciences degree at Cambridge University. "I'm an international
student, which means my parents are paying £20,000 for every year I am here.
That sort of money puts a huge pressure on you. But last summer, I had two weeks
to go before my exams, and I had done pretty much no revision. It was a
make-or-break moment. So I bought modafinil."
Modafinil is one of the new neuroenhancing "smart drugs" now being taken by
growing numbers of students. It was originally developed for the treatment of
narcolepsy, but is now used by students to combat fatigue. Another popular
choice is Ritalin, originally designed as a treatment for attention deficit
hyperactivity disorder (ADHD). Both increase levels of dopamine levels in the
brain - and the alertness and wakefulness of those taking them.
So popular have these drugs become that last month Barbara Sahakian, professor
of clinical neuropsychology at Cambridge University's psychiatry department,
warned that their use has "enormous implications" and that universities must act
on them - even mentioning dope testing as one possibility. But this is not
happening. "What universities are doing about (them) is nothing," she says.
Last year, Sahakian was co-opted on to a committee, set up by the Medical
Advisory Council on the Misuse of Drugs, to look at the use of cognitive
enhancing drugs by healthy people. One American study, cited in the journal
Nature, estimated that up to 25% of students at some campuses had taken
neuroenhancing drugs in the past year.
Many hear of these drugs through friends, others independently. "I read an
article in the student press on them," says Lawrence Price, a third-year arts
student at Sheffield Hallam University. "It was criticising them, but I thought
they sounded great." Perera, similarly, found out about smart drugs through the
media. "I read an article in Nature on them," he says. "They seemed a pretty
good idea."
Students believe the drugs enable them to do more work. "I take them when I need
to get through lectures and I have a terrible hangover," says Price.
At the other extreme, Lucy Makepeace, a postgraduate student at Cambridge, uses
them less from a lack of diligence than an excess of it. Extremely hard working,
she takes modafinil once or twice a week. "With study, work and sport I have a
very full timetable," she says. "I want to do everything, but I don't want to do
any of it at a mediocre level. Taking modafinil helps me to do it all."
Perera similarly turned to modafinil from time pressures - which were, in his
case, extreme. "Due to difficulty getting my visa last year, I couldn't return
at the start of the summer term," he says. "When I eventually got my visa, I
arrived back with just a fortnight before my exams, and no revision behind me."
All the students are clear on the drug's effects. "Modafinil increases my
enthusiasm for studying," says Perera. "It makes me feel that lazing around is
the last thing I want to do." Price agrees: "Modafinil gives me the motivation I
would otherwise lack." Makepeace, who clearly doesn't lack motivation, instead
takes modafinil to stay alert. "Once I've taken a pill I can stay up all night
without stopping. It just works so well," she says. "I need it."
The way the students obtain the drugs varies. Some get them from friends, but
many purchase them from online chemists. "I just Googled them," says Perera.
"The cost, including shipping, came to about £2 each." "I bought them from an
online pharmacy," says Price. "You just sign a disclaimer saying you won't sue
them for selling you prescription drugs without a prescription, then they send
you them."
Unknown quantity
Such a convenient process might please the consumer, but it is not one that
impresses Sahakian. "When you get a drug off the internet, you don't know what
it is, or whether you have some pre-existing condition that means you shouldn't
be taking it," she says. "If you get a drug from your GP, they would check
that."
Even if the drugs are what they purport to be, they are not risk-free. Such
smart drugs have only been developed relatively recently, and, says Sahakian
(who has herself researched the effects of modafinil on healthy volunteers), it
is therefore too early to feel confident that they are safe. "It's a real worry
that students are taking these drugs, as we just don't know whether they are
safe in the long term. They're so new. How could we know?"
In addition to concerns about the drugs' physical effects, there are also moral
issues. "Do we want to solve all our problems in this way?" Sahakian asks.
"There are other ways of coping - like exercise, or sleep." Such methods would
not only be physiologically better, but also psychologically. "It's nice to feel
that what you have achieved is your achievement. Take a pill and you might not
feel that," she says.
For some, chemically enhanced achievement is reprehensible. "Students who are
not taking them, feel (to do so) is cheating," says Sahakian. "They feel that
(taking these) could just make the difference between a 2.1 and a first. At that
point, students who don't want to take them start to feel coerced into doing so
because everyone else is." But the accusation of bending the rules is denied
unanimously. "I'm not cheating," says Makepeace. "Taking a pill is no different
to having a cup of coffee. It's just more effective." Perera agrees: "I don't
think this is cheating. I read a nice analogy, which said that people with a bad
memory are no different to people who have bad eyesight. You let people with bad
eyesight have glasses; why not let people with a bad memory have these pills?"
At present, the actual status of such drug-taking remains undefined by
universities, something that Sahakian hopes they will soon address.
"Universities need to think about whether they want their students to be on
drugs or not when they come into their exams. There needs to be some debate
within the universities. Do we care about this? Is this cheating? Is it the way
we want our society to be going?"
Professor John Rallison, pro vice-chancellor for education at Cambridge
University, said the university "does not approve of any non-medicinal
drug-taking", and welfare officers at the university's union said that they were
concerned about such usage.
The view is echoed by Universities UK, the body representing the heads of
British universities, which says it has "grave concerns about students taking
drugs not prescribed to them", because it "poses health risks to those
students". Instead, it advises pressurised students to seek help from university
counselling services or the GP.
A spokesman for Sheffield Hallam University said: "We are not aware of any
student taking this drug and if any students do have difficulties with their
studies we encourage them to make use of our support services."
Given the habits of academics themselves, the topic is a sensitive one:
according to a recent survey by Nature, whose readership tends to be academics
and researchers, one in five respondents said that they had used smart drugs.
Something of which Sahakian herself has personal experience. "I was at a
conference in America recently," she says. "I'd just flown in that day from the
UK. I saw I was timetabled to give a lecture that afternoon. I wanted to do a
good job of it, but I was just feeling so jetlagged. I mentioned to a colleague
how I felt and he immediately said to me, 'Oh, do you want to take some of my
modafinil?'"
She didn't, for the record, accept.
All student names have been changed
Captions:
Modafinil is one of the new 'smart drugs' being used by students to help them
keep going Photograph: Will Boase
Staying alert is one reason students give for taking modafinil Alamy
LOAD-DATE: April 6, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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All Rights Reserved
157 of 998 DOCUMENTS
Indian Patents News
April 2, 2010 Friday 6:30 AM EST
American Inventors Develop Processes for the Preparation of Modafinil and
Analogs Thereof
LENGTH: 118 words
New Delhi, April 2 -- Liang Sidney, Duchek John R and Schaffer Carl J of
Mallinckrodt Inc, St. Louis, USA have developed processes for the preparation of
modafinil and analogs thereof.Mallinckrodt Inc filed the patent application on
June 9, 2008. The patent application number is 2877/CHENP/2008 A.According to
the Controller General of Patents, Designs & Trade Marks, "The present invention
generally relates to an improved process for preparing modafinil and analogs
thereof. The process minimizes impurities and improves the overall yield by
oxidizing a modafinil intermediate compound in a reaction mixture including an
alcohol and an organic acid at a ratio of from about 1:1 to about 80:1 (by
volume)."
LOAD-DATE: May 4, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Indian Patents News, distributed by Contify.com
All Rights Reserved
158 of 998 DOCUMENTS
PR Newswire
March 29, 2010 Monday 4:47 PM EST
Cephalon Receives Complete Response Letter for NUVIGIL for the Treatment of
Excessive Sleepiness Associated with Jet Lag Disorder
LENGTH: 1058 words
DATELINE: FRAZER, Pa., March 29
FRAZER, Pa., March 29 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced the company has received a Complete Response letter from the
U.S. Food and Drug Administration (FDA) for its supplemental new drug
application for NUVIGIL® (armodafinil) Tablets [C-IV] in the treatment of
patients with excessive sleepiness associated with jet lag disorder resulting
from eastbound travel.
As the first company to study a treatment option to improve wakefulness
associated with jet lag disorder, Cephalon worked closely with the FDA to design
a special protocol assessment (SPA) that would evaluate the experience of a
typical eastbound airline traveler. Clinical efficacy was evaluated using two
primary endpoints: an objective assessment -- the Multiple Sleep Latency Test
(MSLT), and a subjective assessment -- the Patient Global Impression of Severity
(PGI-S). Patients taking NUVIGIL (150 mg/day) showed a statistically significant
improvement over placebo as measured by the MSLT [p<0.0001] and the PGI-S
[p=0.044]. The most common adverse events associated with NUVIGIL treatment
(five percent or greater) were headache, nausea, insomnia, diarrhea and
palpitations. There were no reports of serious rash observed in the trial
participants, and no new safety signals were observed in the clinical trial.
"Although we reached statistical significance on both primary endpoints, the
Complete Response letter raised questions regarding the robustness of the PGI-S
data," said Dr. Lesley Russell, Cephalon's Chief Medical Officer. "We have
already reviewed this issue with the FDA and will be scheduling a meeting with
the Agency in the near future to discuss it further."
About NUVIGIL
NUVIGIL, the longer-lasting isomer of modafinil, was launched in the United
States in June 2009. It is indicated to improve wakefulness in patients with
excessive sleepiness associated with treated obstructive sleep apnea (OSA),
shift work disorder (SWD), or narcolepsy. NUVIGIL is not approved as a treatment
for jet lag disorder or its associated symptoms. The NUVIGIL (armodafinil) label
includes a bolded warning for serious or life-threatening rash, including
Stevens-Johnson Syndrome, that has been reported in adults in association with
the use of armodafinil and in adults and children in association with the use of
modafinil, a racemic mixture of S and R modafinil (the latter is armodafinil,
the active ingredient in NUVIGIL). NUVIGIL is not approved for use in pediatric
patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness, and insomnia. Full prescribing
information for NUVIGIL is available at www.NUVIGIL.com.
About Cephalon, Inc.
Cephalon is an international biopharmaceutical company dedicated to discovering,
developing and bringing to market medications for difficult to treat and rare
conditions. Since its inception in 1987, Cephalon has brought first-in-class and
best-in-class medicines to patients around the world in several therapeutic
areas. Cephalon has the distinction of being one of the world's fastest-growing
biopharmaceutical companies, now among the Fortune 1000 and a member of the S&P
500 Index, employing approximately 3,000 people worldwide.
Cephalon has a growing presence in Europe, the Middle East and Africa. The
Cephalon European headquarters and pre-clinical development center are located
in Maisons-Alfort, France, just outside of Paris. Key business units are located
in England, Ireland, France, Germany, Italy, Spain, the Netherlands for the
Benelux countries, and Poland for Eastern and Central European countries.
The company's proprietary products in the United States include: NUVIGIL,
TREANDA® (bendamustine hydrochloride) for Injection, AMRIX® (cyclobenzaprine
hydrochloride extended-release capsules), FENTORA® (fentanyl buccal tablet)
[C-II], PROVIGIL® (modafinil) Tablets [C-IV], TRISENOX® (arsenic trioxide)
injection, GABITRIL® (tiagabine hydrochloride), and ACTIQ® (oral transmucosal
fentanyl citrate) [C-II]. The company also markets numerous products
internationally. Full prescribing information on its U.S. products is available
at http://www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, clinical development of NUVIGIL, prospects for and frequency
of filing new indications for NUVIGIL, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
Contacts:
Media: Investor Relations:
Candace Steele Flippin Chip Merritt
610-727-6231 (office) 610-738-6376 (office)
csteele@cephalon.com cmerritt@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media: Candace Steele Flippin, +1-610-727-6231 (office),
csteele@cephalon.com; Investor Relations: Chip Merritt, +1-610-738-6376
(office), cmerritt@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: March 30, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 PR Newswire Association LLC
All Rights Reserved
159 of 998 DOCUMENTS
Agence France Presse -- English
March 19, 2010 Friday 9:11 PM GMT
Cycling: US rider Clinger banned for two years
LENGTH: 218 words
DATELINE: colorado springs, Colorado, March 19 2010
David Clinger, runner-up in last year's US national road race championships, has
been slapped with a two-year ban after testing positive for
performance-enhancing drugs.
The 32-year-old American tested positive for synthetic testosterone and
modafinil in July at the 2009 national championships in Bend, Oregon, the US
Anti-Doping Agency announced on Friday.
"Synthetic testosterone is prohibited as an anabolic agent and modafinil is
prohibited as a stimulant on the World Anti-Doping Agency Prohibited List,"
USADA said in a news release.
This is the latest setback for Clinger, who is a former US Postal teammate of
Lance Armstrong and Floyd Landis.
He has been in and out of drug rehab facilities. He is also known for an unusual
New Zealand Maori-inspired tattoo which covers his entire face like a mask.
USADA said the suspension is retroactive to the date Clinger was first notified
of the ban by US officials meaning he will be eligible to compete again in 19
months. His has also been stripped of his race results.
Clinger told the discipline panel that he was taking the drugs on the advice of
his personal doctor in Utah and that he declared the use of testosterone on the
forms that accompanied his test sample.
The disciplinary panel rejected USADA's request for a longer suspension than two
years.
gph/dj10
LOAD-DATE: March 20, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Agence France Presse
All Rights Reserved
160 of 998 DOCUMENTS
Xinhua General News Service
March 19, 2010 Friday 9:10 PM EST
U.S. rider Clinger banned for two years
SECTION: WORLD NEWS; Sports
LENGTH: 179 words
DATELINE: WASHINGTON March 19
David Clinger, runner-up in last year's U.S. national road race championships,
has been banned for two years after testing positive for performance-enhancing
drugs.
The 32-year-old American tested positive for synthetic testosterone and
modafinil in July at the 2009 national championships in Bend, Oregon, the US
Anti-Doping Agency announced on Friday.
"Synthetic testosterone is prohibited as an anabolic agent and modafinil is
prohibited as a stimulant on the World Anti-Doping Agency Prohibited List,"
USADA said in a news release.
USADA said the suspension is retroactive to the date Clinger was first notified
of the ban by U.S. officials meaning he will be eligible to compete again in 19
months. He has also been stripped of his race results.
Clinger told the discipline panel that he was taking the drugs on the advice of
his personal doctor in Utah and that he declared the use of testosterone on the
forms that accompanied his test sample.
The disciplinary panel rejected USADA's request for a longer suspension than
two years.
LOAD-DATE: March 20, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Xinhua News Agency
161 of 998 DOCUMENTS
Xinhua General News Service
March 19, 2010 Friday 1:18 AM EST
U.S. rider Clinger banned for two years
SECTION: WORLD NEWS; Sports
LENGTH: 179 words
DATELINE: WASHINGTON March 19
David Clinger, runner-up in last year's U.S. national road race championships,
has been banned for two years after testing positive for performance-enhancing
drugs.
The 32-year-old American tested positive for synthetic testosterone and
modafinil in July at the 2009 national championships in Bend, Oregon, the US
Anti-Doping Agency announced on Friday.
"Synthetic testosterone is prohibited as an anabolic agent and modafinil is
prohibited as a stimulant on the World Anti-Doping Agency Prohibited List,"
USADA said in a news release.
USADA said the suspension is retroactive to the date Clinger was first notified
of the ban by U.S. officials meaning he will be eligible to compete again in 19
months. He has also been stripped of his race results.
Clinger told the discipline panel that he was taking the drugs on the advice of
his personal doctor in Utah and that he declared the use of testosterone on the
forms that accompanied his test sample.
The disciplinary panel rejected USADA's request for a longer suspension than
two years.
LOAD-DATE: March 21, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Xinhua News Agency
162 of 998 DOCUMENTS
Business Day (South Africa)
March 17, 2010
Health News Edition
NEUROLOGY. Perpetual motion for the brain
BYLINE: Graeme Addison
SECTION: HEALTH
LENGTH: 1209 words
NEUROLOGY
Perpetual motion for the brain
It may be time to sound a 'subculture alert' that there are people out there who
think we should never sleep, but use our lives more productively by remaining
awake and ever active. Are they right? investigates
ADRUG called modafinil can keep you awake for many days and nights without
apparently serious side effects. Considering that we humans spend up to a third
of our lives sleeping, it seems only rational - the next step in our evolution -
that we should attempt to extend our waking hours and get more done.
There are those who believe that we need to sleep less, or not sleep at all. The
usual suspects dosing themselves on stimulants such as caffeine and amphetamines
include students cramming for exams, executives preparing for that big
presentation, emergency workers at disaster scenes, and soldiers in battle.
They - and others such as journalists on perpetual deadlines - are prime
candidates for modafinil.
The drug is a unique wake-promoting stimulant of the central nervous system,
approved in the US in 1998 and in SA in 2004 as a treatment for narcolepsy (the
tendency to fall asleep).
It was discovered in the 1970s by Prof Micheal Jouvet, experimenting with
antidepressants at the French firm Lafon. Students of Jouvet who tried the pill
showed an "amazing" improvement in their work.
It was speculated at the time that it could keep an army on its feet and
fighting for three days and nights with no major negative side effects.
Modafinil is one of only two drugs in a unique class called eugeroics, which
literally means good arousal, and is a sold on prescription as Provigil,
Modiodal and Alertec.
Some users have been known to stay awake for up to four days and nights,
recovering with only a normal eight-hour bout of sleep. In clinical trials the
most commonly observed side effects in more than 5% of patients are headache,
upper respiratory tract infection, nausea, nervousness, anxiety and insomnia.
According to the Biogenesis Laboratories, which sells a variety of
life-extension, anti-ageing, anti-depressant and cognitive enhancement drugs
over the internet in SA, modafinil increases alertness and concentration,
reducing the desire to nap, and yet at the same time displays no addictive or
"coming-down" side-effects. It keeps you steadily awake for up to eight hours
after swallowing a 100mg tablet.
One participant in the online global Drugs Forum reported: "Small euphoria -
seems to build when longer in the experience - getting the whole time absorbed
into things, which have to be done (almost neurotic behaviour). Sleeplessness.
More energy. Impulsive behavior."
For that user modafinil lived up to its reputation as a mood-brightening psycho
stimulant.
The big question is where such stimulation may be taking us. Modafinil is
probably not the last "go-pill" that will emerge from modern pharmacology. There
is a real prospect of keeping people awake indefinitely. As with research into
anti-ageing - promising death's end - the end of sleep would fundamentally
change the nature of our species.
What would we do with ourselves? For some, this lidless future - making us like
snakes with ever-open eyes - is too horrible to contemplate. It would
reconstruct our lives around activities lasting all day and night, pausing for
rest and recovery only to think (consciously) about the next thing to do.
The Swiss psychiatrist Calr Jung would turn in his grave, although he did say
"that consciousness acts upon our nightly life just as much as the unconscious
overshadows our daily life".
Perhaps we could learn more about ourselves by simply staying awake.
The fact is that medical science has struggled to explain why we need sleep
anyway.
According to the journal Science, the function of sleep is one of the 100 or so
greatest unsolved mysteries in science. Theories range from brain "maintenance"
- including memory consolidation and pruning - to reversing damage from
oxidative stress suffered while awake.
Dr Jerome Siegel, a University of California, Los Angeles, professor of
psychiatry and director of the university's Centre for Sleep Research at the
Semel Institute for Neuroscience and Human Behaviour, has studied sleep in a
broad range of animals from the platypus to the walrus.
In the online journal Nature Reviews Neuroscience last year, he concluded that
sleep's primary function is to increase the efficiency of animals and minimise
risk.
We stay alert and active when we need to and relax our guard when there is less
danger or less call for action.
"We see sleep as lying on a continuum that ranges from these dormant states like
torpor and hibernation, on to periods of continuous activity without any sleep,
such as during migration, where birds can fly for days on end without stopping,"
said Siegel.
Airmen, unfortunately, cannot fly for days for days on end. This problem has
mightily exercised military researchers.
But hopes that modafinil would be the solution have been dashed by a number of
studies of its effectiveness. Harvard law student Douglas Kim pulled the
findings together in a 2007 paper on "vigilance" as a military priority.
"In certain studies, modafinil's efficacy as compared to caffeine and
amphetamines were of questionable conclusion," he wrote.
"Researchers also noticed modafinil produced unexpected side-effects including
an increase in core temperature, an inability to discern when the drug has begun
to perform, and an additional 'over-confidence' effect in self-reported
questionnaires - all side-effects that are of real concern when superimposed on
sustained military operations."
If you ask busy people whether they would like to stay awake for long periods,
you get some intriguing responses, as I did to my question on Facebook.
"I would never give up sleeping, I need it too much," said one South African
business executive now working in the US. He might well have quoted Shakespeare,
whose nervously overwrought Macbeth feared that he was cursed to sleep no more.
"You've got to love the ICU in hospital," wrote another, "it's the only place
you actually get intensive nursing care but absolutely NO sleep."
And a sportsman friend wrote: "Thankful for sleep... Best time of our lives
sometimes."
As to getting more done by not sleeping, a rather despairing note sounded in
this response: "As an insomniac, I question that assumption."
Efficiency and productivity may not be enhanced simply by staying awake, because
the body and mind need to regenerate through sleep.
Jung believed that in sleep our dreams reconnect us with the collective
unconscious of our species, the myths and archetypes that underlie our wakeful
reality and shape our lives.
If so, we cannot do without it, and any attempt to drug ourselves into a state
of perpetual sleeplessness will smash our psyche to pieces.
To be cursed with sleep, or with sleeplessness: which is it to be? Birds know
the answer, we don't - though perhaps only for now.
The fact is that medical science has struggled to explain why we need sleep
anyway
AIMING EVER HIGHER: Night time is no time to nod off, say those who believe we
should be spending more hours awake. Less time sleeping means more opportunity
to make optimum use of our time and remain productive, they say. Picture:
iSTOCKPHOTO
LOAD-DATE: March 18, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2010 BDFM Publishers PTY Ltd.
All Rights Reserved
163 of 998 DOCUMENTS
Business Day (South Africa)
March 17, 2010
Health News Edition
NEUROLOGY. Perpetual motion for the brain
BYLINE: Graeme Addison
SECTION: HEALTH
LENGTH: 1209 words
NEUROLOGY
Perpetual motion for the brain
It may be time to sound a 'subculture alert' that there are people out there who
think we should never sleep, but use our lives more productively by remaining
awake and ever active. Are they right? investigates
ADRUG called modafinil can keep you awake for many days and nights without
apparently serious side effects. Considering that we humans spend up to a third
of our lives sleeping, it seems only rational - the next step in our evolution -
that we should attempt to extend our waking hours and get more done.
There are those who believe that we need to sleep less, or not sleep at all. The
usual suspects dosing themselves on stimulants such as caffeine and amphetamines
include students cramming for exams, executives preparing for that big
presentation, emergency workers at disaster scenes, and soldiers in battle.
They - and others such as journalists on perpetual deadlines - are prime
candidates for modafinil.
The drug is a unique wake-promoting stimulant of the central nervous system,
approved in the US in 1998 and in SA in 2004 as a treatment for narcolepsy (the
tendency to fall asleep).
It was discovered in the 1970s by Prof Micheal Jouvet, experimenting with
antidepressants at the French firm Lafon. Students of Jouvet who tried the pill
showed an "amazing" improvement in their work.
It was speculated at the time that it could keep an army on its feet and
fighting for three days and nights with no major negative side effects.
Modafinil is one of only two drugs in a unique class called eugeroics, which
literally means good arousal, and is a sold on prescription as Provigil,
Modiodal and Alertec.
Some users have been known to stay awake for up to four days and nights,
recovering with only a normal eight-hour bout of sleep. In clinical trials the
most commonly observed side effects in more than 5% of patients are headache,
upper respiratory tract infection, nausea, nervousness, anxiety and insomnia.
According to the Biogenesis Laboratories, which sells a variety of
life-extension, anti-ageing, anti-depressant and cognitive enhancement drugs
over the internet in SA, modafinil increases alertness and concentration,
reducing the desire to nap, and yet at the same time displays no addictive or
"coming-down" side-effects. It keeps you steadily awake for up to eight hours
after swallowing a 100mg tablet.
One participant in the online global Drugs Forum reported: "Small euphoria -
seems to build when longer in the experience - getting the whole time absorbed
into things, which have to be done (almost neurotic behaviour). Sleeplessness.
More energy. Impulsive behavior."
For that user modafinil lived up to its reputation as a mood-brightening psycho
stimulant.
The big question is where such stimulation may be taking us. Modafinil is
probably not the last "go-pill" that will emerge from modern pharmacology. There
is a real prospect of keeping people awake indefinitely. As with research into
anti-ageing - promising death's end - the end of sleep would fundamentally
change the nature of our species.
What would we do with ourselves? For some, this lidless future - making us like
snakes with ever-open eyes - is too horrible to contemplate. It would
reconstruct our lives around activities lasting all day and night, pausing for
rest and recovery only to think (consciously) about the next thing to do.
The Swiss psychiatrist Calr Jung would turn in his grave, although he did say
"that consciousness acts upon our nightly life just as much as the unconscious
overshadows our daily life".
Perhaps we could learn more about ourselves by simply staying awake.
The fact is that medical science has struggled to explain why we need sleep
anyway.
According to the journal Science, the function of sleep is one of the 100 or so
greatest unsolved mysteries in science. Theories range from brain "maintenance"
- including memory consolidation and pruning - to reversing damage from
oxidative stress suffered while awake.
Dr Jerome Siegel, a University of California, Los Angeles, professor of
psychiatry and director of the university's Centre for Sleep Research at the
Semel Institute for Neuroscience and Human Behaviour, has studied sleep in a
broad range of animals from the platypus to the walrus.
In the online journal Nature Reviews Neuroscience last year, he concluded that
sleep's primary function is to increase the efficiency of animals and minimise
risk.
We stay alert and active when we need to and relax our guard when there is less
danger or less call for action.
"We see sleep as lying on a continuum that ranges from these dormant states like
torpor and hibernation, on to periods of continuous activity without any sleep,
such as during migration, where birds can fly for days on end without stopping,"
said Siegel.
Airmen, unfortunately, cannot fly for days for days on end. This problem has
mightily exercised military researchers.
But hopes that modafinil would be the solution have been dashed by a number of
studies of its effectiveness. Harvard law student Douglas Kim pulled the
findings together in a 2007 paper on "vigilance" as a military priority.
"In certain studies, modafinil's efficacy as compared to caffeine and
amphetamines were of questionable conclusion," he wrote.
"Researchers also noticed modafinil produced unexpected side-effects including
an increase in core temperature, an inability to discern when the drug has begun
to perform, and an additional 'over-confidence' effect in self-reported
questionnaires - all side-effects that are of real concern when superimposed on
sustained military operations."
If you ask busy people whether they would like to stay awake for long periods,
you get some intriguing responses, as I did to my question on Facebook.
"I would never give up sleeping, I need it too much," said one South African
business executive now working in the US. He might well have quoted Shakespeare,
whose nervously overwrought Macbeth feared that he was cursed to sleep no more.
"You've got to love the ICU in hospital," wrote another, "it's the only place
you actually get intensive nursing care but absolutely NO sleep."
And a sportsman friend wrote: "Thankful for sleep... Best time of our lives
sometimes."
As to getting more done by not sleeping, a rather despairing note sounded in
this response: "As an insomniac, I question that assumption."
Efficiency and productivity may not be enhanced simply by staying awake, because
the body and mind need to regenerate through sleep.
Jung believed that in sleep our dreams reconnect us with the collective
unconscious of our species, the myths and archetypes that underlie our wakeful
reality and shape our lives.
If so, we cannot do without it, and any attempt to drug ourselves into a state
of perpetual sleeplessness will smash our psyche to pieces.
To be cursed with sleep, or with sleeplessness: which is it to be? Birds know
the answer, we don't - though perhaps only for now.
The fact is that medical science has struggled to explain why we need sleep
anyway
AIMING EVER HIGHER: Night time is no time to nod off, say those who believe we
should be spending more hours awake. Less time sleeping means more opportunity
to make optimum use of our time and remain productive, they say. Picture:
iSTOCKPHOTO
LOAD-DATE: March 19, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2010 BDFM Publishers PTY Ltd.
All Rights Reserved
164 of 998 DOCUMENTS
Business Day (South Africa)
March 17, 2010
Health News Edition
NEUROLOGY. Perpetual motion for the brain
BYLINE: Graeme Addison
SECTION: HEALTH
LENGTH: 1209 words
NEUROLOGY
Perpetual motion for the brain
It may be time to sound a 'subculture alert' that there are people out there who
think we should never sleep, but use our lives more productively by remaining
awake and ever active. Are they right? investigates
ADRUG called modafinil can keep you awake for many days and nights without
apparently serious side effects. Considering that we humans spend up to a third
of our lives sleeping, it seems only rational - the next step in our evolution -
that we should attempt to extend our waking hours and get more done.
There are those who believe that we need to sleep less, or not sleep at all. The
usual suspects dosing themselves on stimulants such as caffeine and amphetamines
include students cramming for exams, executives preparing for that big
presentation, emergency workers at disaster scenes, and soldiers in battle.
They - and others such as journalists on perpetual deadlines - are prime
candidates for modafinil.
The drug is a unique wake-promoting stimulant of the central nervous system,
approved in the US in 1998 and in SA in 2004 as a treatment for narcolepsy (the
tendency to fall asleep).
It was discovered in the 1970s by Prof Micheal Jouvet, experimenting with
antidepressants at the French firm Lafon. Students of Jouvet who tried the pill
showed an "amazing" improvement in their work.
It was speculated at the time that it could keep an army on its feet and
fighting for three days and nights with no major negative side effects.
Modafinil is one of only two drugs in a unique class called eugeroics, which
literally means good arousal, and is a sold on prescription as Provigil,
Modiodal and Alertec.
Some users have been known to stay awake for up to four days and nights,
recovering with only a normal eight-hour bout of sleep. In clinical trials the
most commonly observed side effects in more than 5% of patients are headache,
upper respiratory tract infection, nausea, nervousness, anxiety and insomnia.
According to the Biogenesis Laboratories, which sells a variety of
life-extension, anti-ageing, anti-depressant and cognitive enhancement drugs
over the internet in SA, modafinil increases alertness and concentration,
reducing the desire to nap, and yet at the same time displays no addictive or
"coming-down" side-effects. It keeps you steadily awake for up to eight hours
after swallowing a 100mg tablet.
One participant in the online global Drugs Forum reported: "Small euphoria -
seems to build when longer in the experience - getting the whole time absorbed
into things, which have to be done (almost neurotic behaviour). Sleeplessness.
More energy. Impulsive behavior."
For that user modafinil lived up to its reputation as a mood-brightening psycho
stimulant.
The big question is where such stimulation may be taking us. Modafinil is
probably not the last "go-pill" that will emerge from modern pharmacology. There
is a real prospect of keeping people awake indefinitely. As with research into
anti-ageing - promising death's end - the end of sleep would fundamentally
change the nature of our species.
What would we do with ourselves? For some, this lidless future - making us like
snakes with ever-open eyes - is too horrible to contemplate. It would
reconstruct our lives around activities lasting all day and night, pausing for
rest and recovery only to think (consciously) about the next thing to do.
The Swiss psychiatrist Calr Jung would turn in his grave, although he did say
"that consciousness acts upon our nightly life just as much as the unconscious
overshadows our daily life".
Perhaps we could learn more about ourselves by simply staying awake.
The fact is that medical science has struggled to explain why we need sleep
anyway.
According to the journal Science, the function of sleep is one of the 100 or so
greatest unsolved mysteries in science. Theories range from brain "maintenance"
- including memory consolidation and pruning - to reversing damage from
oxidative stress suffered while awake.
Dr Jerome Siegel, a University of California, Los Angeles, professor of
psychiatry and director of the university's Centre for Sleep Research at the
Semel Institute for Neuroscience and Human Behaviour, has studied sleep in a
broad range of animals from the platypus to the walrus.
In the online journal Nature Reviews Neuroscience last year, he concluded that
sleep's primary function is to increase the efficiency of animals and minimise
risk.
We stay alert and active when we need to and relax our guard when there is less
danger or less call for action.
"We see sleep as lying on a continuum that ranges from these dormant states like
torpor and hibernation, on to periods of continuous activity without any sleep,
such as during migration, where birds can fly for days on end without stopping,"
said Siegel.
Airmen, unfortunately, cannot fly for days for days on end. This problem has
mightily exercised military researchers.
But hopes that modafinil would be the solution have been dashed by a number of
studies of its effectiveness. Harvard law student Douglas Kim pulled the
findings together in a 2007 paper on "vigilance" as a military priority.
"In certain studies, modafinil's efficacy as compared to caffeine and
amphetamines were of questionable conclusion," he wrote.
"Researchers also noticed modafinil produced unexpected side-effects including
an increase in core temperature, an inability to discern when the drug has begun
to perform, and an additional 'over-confidence' effect in self-reported
questionnaires - all side-effects that are of real concern when superimposed on
sustained military operations."
If you ask busy people whether they would like to stay awake for long periods,
you get some intriguing responses, as I did to my question on Facebook.
"I would never give up sleeping, I need it too much," said one South African
business executive now working in the US. He might well have quoted Shakespeare,
whose nervously overwrought Macbeth feared that he was cursed to sleep no more.
"You've got to love the ICU in hospital," wrote another, "it's the only place
you actually get intensive nursing care but absolutely NO sleep."
And a sportsman friend wrote: "Thankful for sleep... Best time of our lives
sometimes."
As to getting more done by not sleeping, a rather despairing note sounded in
this response: "As an insomniac, I question that assumption."
Efficiency and productivity may not be enhanced simply by staying awake, because
the body and mind need to regenerate through sleep.
Jung believed that in sleep our dreams reconnect us with the collective
unconscious of our species, the myths and archetypes that underlie our wakeful
reality and shape our lives.
If so, we cannot do without it, and any attempt to drug ourselves into a state
of perpetual sleeplessness will smash our psyche to pieces.
To be cursed with sleep, or with sleeplessness: which is it to be? Birds know
the answer, we don't - though perhaps only for now.
The fact is that medical science has struggled to explain why we need sleep
anyway
AIMING EVER HIGHER: Night time is no time to nod off, say those who believe we
should be spending more hours awake. Less time sleeping means more opportunity
to make optimum use of our time and remain productive, they say. Picture:
iSTOCKPHOTO
LOAD-DATE: March 20, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2010 BDFM Publishers PTY Ltd.
All Rights Reserved
165 of 998 DOCUMENTS
Reuters Health Medical News
March 15, 2010 Monday 9:00 PM EST
Guideline urges treatment for nonmotor symptoms of Parkinson's disease
SECTION: CLINICAL
LENGTH: 579 words
DATELINE: NEW YORK
A new practice parameter from the American Academy of Neurology calls for
doctors to identify and treat nonmotor symptoms in patients with Parkinson's
disease (PD).
Nonmotor symptoms - autonomic dysfunction, sleep disorders, psychological and
cognitive problems, and sensory abnormalities - are major, often unrecognized
causes of morbidity in PD. In 2006 and 2008, the Academy issued guidelines
pertaining to cognitive and mood dysfunction in PD as well as treatment of
sialorrhea with botulinum toxin.
To evaluate treatment options for other nonmotor PD symptoms, Dr. Theresa A.
Zesiewicz from the University of South Florida in Tampa and associates searched
MEDLINE, EMBASE, and the Science Citation Index and identified 46 controlled
trials published between 1966 and 2008.
Most trials supporting specific treatments provided only level C evidence, the
researchers report in the March 16th issue of Neurology. The only recommendation
backed by level B evidence was the use of levodopa/carbidopa (Atamet, Sinemet)
to treat periodic limb movements of sleep.
One trial evaluated the efficacy of sildenafil (Viagra) in 12 patients with
erectile dysfunction. Sildenafil was more effective than placebo at enabling
men to achieve and maintain an erection, with minimal changes in blood pressure.
The authors advise a complete medical evaluation to rule out other treatable
causes of erectile dysfunction.
For excessive daytime sleepiness, modafinil (Provigil) might be useful. However,
modafinil might improve patients' perception of wakefulness without improving
objective measures of sleepiness, creating a potential safety hazard if patients
engage in activities such as driving.
Methylphenidate (Ritalin) might help patients with fatigue, but the authors warn
of the potential for abuse. They note that PD patients "have a risk for dopamine
dysregulation syndrome and impulse control disorders that share many clinical
and functional imaging features with addiction."
Isosmotic macrogol (polyethylene glycol or Miralax) possibly improved
constipation in one study. Increased water and dietary fiber intake have also
been helpful.
However, for many conditions considered - orthostatic hypotension, urinary
incontinence, insomnia, rapid eye movement sleep behavior disorder, and anxiety
-- the authors found insufficient evidence to support or refute treatments.
Dr. Zesiewicz and associates advise physicians to diagnose nonmotor symptoms in
PD using tools such as the NMS Quest study questionnaire and the updated version
of the Unified Parkinson's Disease Rating Scale.
Concluding, the investigators write, "There are few dedicated controlled trials
of drugs to treat nonmotor symptoms in PD. Such trials are urgently required."
However, co-author Dr. William J. Weiner commented in an interview with Reuters
Health, "The truth is that when we do these very formal surveys of the
literature looking for evidence in a rigorous manner, it's quite common that we
can't find much evidence." That doesn't mean that many of the measures that
physicians commonly use to treat nonmotor PD symptoms aren't helpful, he added.
Dr. Weiner, from the University of Maryland Medical Center, Baltimore,
continued, "It's also helpful for patients to know that they don't have another
disease (when they develop these symptoms), so they don't have to see a
cardiologist or a GI specialist or a urologist; that in fact it's part of what
is going on with them."
SOURCE: Neurology 2010;74:924-931.
LOAD-DATE: March 16, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Reuters Health
All Rights Reserved
166 of 998 DOCUMENTS
DAILY MAIL (London)
March 9, 2010 Tuesday
TEENAGERS ARE NOW BUYING ILLEGAL 'SMART DRUGS' ONLINE TO BOOST EXAM PERFORMANCE.
BUT AS THIS SPECIAL REPORT SHOWS,THE EFFECT ON THEIR HEALTH CAN BE CATASTROPHIC
BYLINE: BY STEVE BOGGAN AND TIM STEWART
LENGTH: 1799 words
JOSH has an exam and, like most of the other boys at his prestigious public
school, he's keen to put his best foot forward. He's eaten breakfast and dressed
smartly, but before he sets off for class, he reaches for a white pill and pops
it into his mouth.
He bought 30 of the tablets online for £40 from the U.S., but for all Josh knows
they might well have been knocked up in an illegal backstreet 'pharmacy' in
India. Still, the drug modafinil -- usually used to treat sleeping disorders --
has worked before for him and if it works again he is sure to get top marks.
Welcome to the world of 'smart drugs', otherwise known as cognitive enhancement
pharmaceuticals. This is a world where pupils as young as 15 self-medicate,
participate in illegal online drug trafficking and swap notes on the best pill
cocktails for good grades.
Concern over smart drugs has been growing for some time among academics,
politicians and pharmacologists, but it has been brought into sharp focus with
the announcement that the former health minister, Lord Darzi of Denham, is
heading a study at Imperial College, London, into their effects.
This might seem odd because most of these drugs have been around for decades for
the treatment of conditions such as Attention Deficit Hyperactivity Disorder
(ADHD) and narcolepsy, and have been found to be safe.
But no one has monitored their chaotic use in healthy young people taking
inappropriate doses to boost their intellectual prowess.
And some experts believe this kind of use in brains that are still developing
could cause addiction and permanent damage.
Josh is an intelligent, articulate 17-year-old, so you wonder why he needs extra
help to feel smart. He has been taking modafinil (sold as the prescription-only
drugs Provigil, Alertec, Modavigil and Modalert) since he was 16, but has
friends who began using smart pharmaceuticals at 15. He lives in London and his
parents are lawyers.
'I read about modafinil in a newspaper and then researched it on the internet
and spoke to some of my friends about it,' he says.
'It appealed to me as an inexpensive method for highly concentrated revision,
for which I would otherwise depend on coffee, tea or Red Bull. Modafinil gives
you heightened alertness, stamina and productivity. I find it helpful for focus
and memory.
'I find I can memorise a graph after drawing it once instead of several times. I
would say it makes me 40 to 50 per cent more productive in a day, but it does
not make me any cleverer.
'While revising for my last set of exams, I was taking 100mg of modafinil a day
for six or seven days a week for three weeks.
'Around half-term, I stepped it up to 150mg to 200mg a day and in the last two
or three weeks up to the exams I took 200mg to 300mg a day and worked 18-hour
days.
'I find you can get by on four to six hours of
sleep for up to three weeks and then, at the end, the body needs to rest and
catch up. I take a whole day off and sleep for 24 hours.
'Taking it is no different from having other stimulants such as coffee, ProPlus
caffeine tablets or Red Bull. It is no different from taking painkillers for a
headache.
'I use it specifically for exams and will carry on at university. I would
recommend it to anyone who is informed about it and knows what they are doing.
'I haven't told my parents about using modafinil. They wouldn't know what it is
and they wouldn't approve of me using it.'
Josh's use of modafinil is not unusual. A quick scan of student web forums
uncovers a world where drug advice is swapped.
The benefits of Ritalin and Adderall, which are meant to be used to treat ADHD,
are compared with Provigil, Modalert and a group of drugs called ampakines --
prescription pharmaceuticals that are showing promise in the treatment of
Alzheimer's and Parkinson's.
The problem in telling students not to take them is that tests have shown these
drugs can help with focus, memory, concentration and alertness by interacting in
different ways with neurotransmitters -- chemical messengers -- in the brain.
the ADHD treatments contain amphetamines, which can result in addiction, and
there are suspicions that sleep disorder treatments such as modafinil could be
addictive.
Barbara Sahakian, Professor of Clinical Neuropsychology at Cambridge University,
says scientists understand how drugs such as Ritalin work by stimulating levels
of the neurotransmitters dopamine and noradrenaline in the brain.
These affect mood, cognition and memory. 'However, there is an optimal dose for
ideal performance,' she says.
'Levels beyond that could cause problems with addiction. With modafinil, no one
really knows how exactly the drug acts in the brain to boost cognition.'
Evidence is emerging, however, that modafinil -- long thought not to be
addictive -- also affects the levels of dopamine. This is significant because
dopamine production can lead to addictive behaviour.
Sometimes referred to as the 'reward' drug, dopamine is released during
experiences such as the enjoyment of sex, food and drugs. We are programmed to
repeat rewarding experiences, a cycle that can result in addiction.
A study published in the Journal of the American Medical Association last year
looked at ten healthy men taking modafinil and found it did increase levels of
dopamine. The research was conducted by the National Institute on Drug Abuse
(Nida) in the U.S.
'[Modafinil] has the signature that it could potentially be addictive,' says
Nida's director Dr Nora Volkow.
'Studies have shown consistently that all of the drugs of abuse . . . have a
common effect of increasing dopamine in the nucleus accumbens [area of the
brain].
'That is believed to be crucial for their reinforcing effect and ultimately
their underlying potential for producing addiction.'
The jury is still out on whether modafinil is addictive. Scientists regard tests
on just ten people as being far from definitive.
Sahakian has called on the Government to hold a public debate on the use of
smart drugs.
On the one hand, she feels they could be of real benefit to society if proven to
be safe.
On the other, she wonders whether in some dystopian future people will be
pressured into taking them to work longer and harder.
Already, there is evidence that students feel pressured into taking smart drugs
to compete with highachieving classmates who are using them. And some pushy
parents appear to be condoning their use.
One third-year student studying computer science at London Metropolitan
University told us that taking modafinil is a 'lifesaver' in helping him to
complete assignments.
'I am aware of school children who have taken modafinil. They were aged between
16 and 18,' he says.
'Their father [a computer programmer], my friend, used to take it occasionally.
The parents had extremely high expectations for their children and they were
taking exams.
'My friend's daughter was advised to take modafinil by her classmates.
Unfortunately, this was a terrible decision.
'She was taken to hospital after five days of sleep deprivation. She had high
blood pressure, was anxious and experienced some kind of hallucinations and
psychosis.
'She was taking extremely high doses of modafinil. I was told she had felt some
kind of euphoria and kept taking more and more. It is proof that modafinil can
be addictive for some people.'
If Nida in the U.S. is correct and all these drugs affect dopamine levels in
some way, then concern is likely to focus on students self-medicating
inappropriate dosages and using them over a long time.
Dr Daniel Amen, a psychiatrist and Fellow of the American Psychiatric
Association, says that while treating young ADHD patients with carefully
controlled doses of Ritalin can improve their lives immeasurably, unmonitored
doses taken by healthy youngsters could be damaging.
'A therapeutic dose arrived at by careful monitoring by a physician might be
anywhere from 5mg to 60mg a day,' he says.
'We know that can enhance brain function in many people by stimulating levels of
dopamine.
'But where you have some of these students taking concentrations of 100mg to
500mg, that could cause some problems.
'The extra dopamine produced constricts blood flow to the brain and, over the
long term, that could cause permanent damage.
'The adolescent brain, especially the pre-frontal cortex -- the most thoughtful
part of the brain -- is developing rapidly. Anything that disrupts or interferes
with this process can cause lasting problems.'
There is debate on student forums over whether using smart drugs amounts to
cheating.
Some say it does, while others argue that those who want to ban them should be
prepared to give up commonplace stimulants, such as caffeine and nicotine. Even
academics are divided.
Dr Anders Sandberg, a philosophy lecturer specialising in bioethics at Oxford
University, tried modafinil as part of his research three years ago and now uses
it openly.
In common with students who take it, Dr Sandberg is on the legal side of an
illegal transaction. Under the 1963 Medicines Act, it is an offence to supply a
drug without a prescription, but not to buy one.
'When I take it, it is like having a little electric motor in the back of my
head running through lists of things I need to do,' he says. 'Then, instead of
putting them off until tomorrow, I go ahead and do them.
'I use the drugs only occasionally if I have a paper to write or need to fly
long distances to attend a conference or deliver a speech. I find that instead
of having jet-lag, I can focus on the job at hand.'
But isn't that sending the wrong message to students?
'This is something I have spent a lot of time considering, but in general I
believe people should have control over their own bodies,' he says. 'That right
is important, but you need to use it appropriately and that's why youngsters
shouldn't take responsibility for managing drugs, alcohol or enhancers.
'These drugs are like stepladders. If you need them to attain something that
would otherwise be out of your reach, then use them. But if you can reach those
heights anyway, then you're just being lazy.'
However, health professionals take a dim view of anyone misusing drugs.
'Anyone taking prescription drugs without a prescription obtained through a
consultation with a health professional is making a big mistake,' says Neal
Patel, a pharmacist and spokesman for the Royal Pharmaceutical Society.
'It's dangerous to experiment with medicines and the sideeffects of cognitive
enhancement drugs are significant -- they can cause abdominal pain, nausea,
heart problems and changes in blood pressure.
'These side- effects are dose dependent -- the more you take, the greater your
risk of being affected and seriously harmed.'
Professor Sahakian and Dr Amen say there are other, less risky yet proven
remedies for improving brain function: sleep, exercise and a healthy diet.
Apparently, they work.
LOAD-DATE: March 9, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Papers
Copyright 2010 Associated Newspapers Ltd.
All Rights Reserved
167 of 998 DOCUMENTS
Irish Independent
March 6, 2010 Saturday
They call it the professional's pill
SECTION: FEATURES
LENGTH: 1264 words
Why more middle-class people are taking a drug they believe will make them
smarter
Sandra is an air steward. She pops a tab every time she crosses the Atlantic to
make sure she's perky on landing. Gerry uses them during exams to give his
concentration a boost. Simon, a junior doctor, takes one during the night shift
to keep sleep at bay and his brain sharp.
You won't find their pill of choice on the shelves of your local head shop but
there's growing evidence that high-flying professionals and stressed-out
students are relying on brain-boosting drugs to quicken their thinking and keep
them awake.
This week in Britain, scientists urged the government to bring the closet
phenomenon of so-called smart drugs into the open, claiming their use is
spreading across all sectors of society from surgeons to soldiers.
Researchers from Cambridge University warned that the drugs, which were designed
to help people with neurological disorders like attention-deficit hyperactivity
disorder, Alzheimer's and brain injury, are now being used for reasons far
beyond their original purpose by uptight executives, multi-tasking mothers and
exhausted shift-workers who need a chemical pick-me-up.
No self-respecting GP would prescribe these powerful brain-changing drugs to a
patient suffering from poor concentration or tiredness, so users are turning to
the internet, where a multitude of websites offer them for sale.
In Ireland, customs officers are at the coalface of this new craze, with
increasing quantities of cognitive-enhancement drugs such as Modafinil and
Ritalin being shipped into the country illegally every year.
In 2008, 1,250 tablets of Modafinil, a sleep inhibitor, were seized at ports and
airports, rising to 1,920 last year.
In the first two months of this year, 170 tablets were found. Seizures of
Ritalin, dubbed 'kiddie cocaine' in the US where it is doled outlike candy to
school-going children, have been lower but significant all the same with more
than 612 units found since 2007.
Here, Modafinil is sold under the trade name Provigil. In November, its
manufacturers Cephalon were granted permission by the Irish Medicines Board to
market the drug for the treatment of excessive daytime sleepiness associated
with sleep apnoea.
Taoiseach Brian Cowen is among those who suffer from this condition, which
periodically causes breathing to stop during sleep.
Originally developed in France, Modafinil, which is also licensed to treat
narcolepsy -- a disorder marked by sudden uncontrollable attacks of daytime
sleep -- is the first of a new generation of wake-promoting drugs which targets
the sleep/wake centres in the brain. It works by activating sleep-suppressing
neurons fooling the mind into believing it is time to be alert.
This pharmaceutical prototype has the power to keep a person awake and focussed
for up to 90 hours running, without the jitteriness or poor concentration that
other stimulants like amphetamines or caffeine are known to produce.
Proponents say it works without causing a crash after its effects have worn off
and does not create any sense of euphoria in the brain thereby limiting its
potential for abuse.
The use of Modafinil within the American military is well-documented where it
has been approved for use on air force missions, allowing troops to stay awake
for days at a time and complete operations as quickly as possible.
In Britain, the drug was approved for use in 2002, and since then has surged in
popularity. The number of prescriptions for stimulants like it has nearly
doubled in recent years, rising from 458,000 in 2004 to 751,000 in 2008. A
Nature magazine poll of 1,400 respondents, mostly scientists and academics,
suggested that one in five had used 'smart drugs'.
Fears that stay-awake pills are increasingly being used as 'lifestyle drugs' are
strengthening, especially since their long-term effects on the brain are still
unknown.
Some neuroscientists also worry that drugs like this will turn humans into
mechanistic beings who pop a pill when they need a brain boost rather than
opting for a brisk walk or a good night's sleep.
Pharmaceutical advances like this could make cosmetic neurology as popular as
beauty enhancements, they claim. And there are ethical concerns about the unfair
advantage such drugs give to users over their peers in academic settings. In the
US, surveys show that an estimated 16-20pc of US college students take smart
drugs to help their memory and keep them alert. The drugs may especially help in
subjects like mathematics and science by aiding students to complete puzzles and
remember long chains of digits.
Last week, one of Britain's leading psychologists called for an official
university-wide strategy to tackle student misuse of prescription drugs like
Modafinil.
Barbara Sahakian, professor of clinical neuropsychology at Cambridge University,
whose work is at the forefront of research into cognitive enhancement drugs, has
even raised the prospect of dope testing of exam students as a possible
safeguard against their use.
"This is something that universities really have to discuss," she says.
"It has enormous implications. The coercion aspect is a strong one. Some
students say they feel it is cheating and it puts pressure on them to feel they
have to use drugs when they don't really want to.
"You have to consider there are things that could be beneficial about such drugs
because we have an ageing population: people will have to work for longer and
their pensions may not be performing.
"The big question is, are we all going to be taking drugs in the next 10 years
and boosting our brain power in this way? And if we are, will we use them to
have a shorter working week, so we can go home, spend more time with our
families and have a good work/life balance? Or will we go headlong into a 24/7
society were we work all the time because we can work all the time'"
Improving brain power and its ability to stay awake is certainly where drug
companies think the future lies as the market for treatments for neurological
and psychiatric illnesses continues to outstrip that for painkillers and
cardiovascular drugs in the western world.
Dozens of neuro-enhancing drugs are currently in the research pipeline and their
use in the coming years is expected to soar.
Advocates argue that smart drugs will remove disparities in society and give
those who are mentally challenged a better chance of self-improvement and
success.
They also claim it is better for high-risk professionals like surgeons and
pilots to take a medically-controlled tablet rather than dosing themselves up on
caffeine and ending up with a shaky hand and a twitchy disposition But for those
dealing with the downside of chemical consumption, the advent of smart drugs is
a worrying prospect.
"As with any stimulant that alters the central nervous system, you have to stop
and think of the long-term consequences of using these drugs," says Dr Fiona
Weldon, clinical director of the Rutland Centre, Dublin's leading addiction
therapy centre.
"We are unsure about the extent to which these drugs are being used in Ireland
but it would be naive to think it isn't happening and it is something we should
be very worried about," she says.
"I've seen students become reliant on the likes of Ritalin. They claim it makes
them work better but before you know it there is a dependency.
"There is such a tendency now to seek out a quick chemical fix as the solution
to our stresses but if you over-stimulate the brain in a false way, the system
will eventually crash and the side effects are incredible."
LOAD-DATE: March 6, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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All Rights Reserved
168 of 998 DOCUMENTS
The Times (London)
February 27, 2010 Saturday
Edition 1;
National Edition
Get smart drugs out of the closet, scientists urge
BYLINE: Lucy Bannerman
SECTION: NEWS; Pg. 28,29
LENGTH: 574 words
Scientists have urged the Government to bring the "closet phenomenon" of
so-called smart drugs out into the open, suggesting that regulated use of the
stimulants could help groups such as surgeons, soldiers, and jurors to maximise
their benefit to society.
The calls coincide with a new study, headed by the former health minister and
surgeon Lord Darzi of Denham, that will monitor the effects of "cognitive
enhancement drugs" on the memory, concentration and decisionmaking skills of
healthy adults.
There is little data on the long-term safety of the performance-enhancing
effects of Ritalin and Modafinil, which are available only on prescription for
those diagnosed with conditions such as attention deficit hyperactivity disorder
(ADHD) or narcolepsy. Anecdotal evidence suggests, however, that the pills'
illicit promise of increased brain power and long bouts of uninterrupted
concentration is attracting numbers of healthy high-fliers. Professor Barbara
Sahakian, a neuroscientist from the University of Cambridge, is working with
Lord Darzi's team at Imperial College London.
Making the drugs available over the counter would be one way of prompting the
clinical trials, which she believes are needed to explore just how far they can
improve the human mind.
Until then, Professor Sahakian warns that ambitious executives, multitasking
mothers and students under pressure will continue to take risks with drugs
procured over the internet, or other people's prescriptions, while the rest of
society risks losing out. "This is a closet phenomenon," she told The Times. "We
know that people are doing these drugs anyway but we don't know about their
long-term safety. The Government has a responsibility to think about what they
should do about that. Maybe they should be letting pharmaceutical companies
brand these medications via a safe route. Wouldn't that be better?" Government
health statistics for England show that the number of prescriptions for
stimulants such as Ritalin and Modafinil has nearly doubled in recent years -
rising from 458,000 in 2004 to 751,000 in 2008.
"I'm rather careful about my brain," said Dr Anders Sandberg, 37, as one might
well expect from a philosophy lecturer who specialises in bioethics at the
University of Oxford.
He first took Modafinil three years ago, after consulting a pharmacologist
friend, and procuring about thirty 50mg doses from a website. He now takes it on
average once a month - "not chronically, but only on days when I decide, 'OK, I
need to get something done'." Days when he has conferences, seminars, papers to
write.
He also wants to remove the stigma attached to those who seek artificial
improvement for their attention span.
"When the cellphone first arrived, we weren't sure when to use it. But we learnt
to invent rules, so that it's generally not OK to use them in restaurants but
it's OK walking outside. We need to achieve the same with enhancement drugs. We
need the right culture surrounding it. And the only way we can do that is by
being honest about its consumption, and face up to the fact it is going on."
A spokeswoman for the Department of Health said a report had been commissioned
in 2008 investigating the issue of cognitive-enhancing drugs. She said: "We
strongly urge anyone thinking about taking a prescriptiononly medicine, not
intended for their personal use, to consult their GP first."
Online Health news, features and expert advice timesonline.co.
uk/health
LOAD-DATE: February 27, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: TIM
Copyright 2010 Times Newspapers Limited
All Rights Reserved
169 of 998 DOCUMENTS
The Times (London)
February 27, 2010 Saturday
Edition 1;
Ireland
Get smart drugs out of the closet, scientists urge
BYLINE: Lucy Bannerman
SECTION: NEWS; Pg. 36,37
LENGTH: 574 words
Scientists have urged the Government to bring the "closet phenomenon" of
so-called smart drugs out into the open, suggesting that regulated use of the
stimulants could help groups such as surgeons, soldiers, and jurors to maximise
their benefit to society.
The calls coincide with a new study, headed by the former health minister and
surgeon Lord Darzi of Denham, that will monitor the effects of "cognitive
enhancement drugs" on the memory, concentration and decisionmaking skills of
healthy adults.
There is little data on the long-term safety of the performance-enhancing
effects of Ritalin and Modafinil, which are available only on prescription for
those diagnosed with conditions such as attention deficit hyperactivity disorder
(ADHD) or narcolepsy. Anecdotal evidence suggests, however, that the pills'
illicit promise of increased brain power and long bouts of uninterrupted
concentration is attracting numbers of healthy high-fliers. Professor Barbara
Sahakian, a neuroscientist from the University of Cambridge, is working with
Lord Darzi's team at Imperial College London.
Making the drugs available over the counter would be one way of prompting the
clinical trials, which she believes are needed to explore just how far they can
improve the human mind.
Until then, Professor Sahakian warns that ambitious executives, multitasking
mothers and students under pressure will continue to take risks with drugs
procured over the internet, or other people's prescriptions, while the rest of
society risks losing out. "This is a closet phenomenon," she told The Times. "We
know that people are doing these drugs anyway but we don't know about their
long-term safety. The Government has a responsibility to think about what they
should do about that. Maybe they should be letting pharmaceutical companies
brand these medications via a safe route. Wouldn't that be better?" Government
health statistics for England show that the number of prescriptions for
stimulants such as Ritalin and Modafinil has nearly doubled in recent years -
rising from 458,000 in 2004 to 751,000 in 2008.
"I'm rather careful about my brain," said Dr Anders Sandberg, 37, as one might
well expect from a philosophy lecturer who specialises in bioethics at the
University of Oxford.
He first took Modafinil three years ago, after consulting a pharmacologist
friend, and procuring about thirty 50mg doses from a website. He now takes it on
average once a month - "not chronically, but only on days when I decide, 'OK, I
need to get something done'." Days when he has conferences, seminars, papers to
write.
He also wants to remove the stigma attached to those who seek artificial
improvement for their attention span.
"When the cellphone first arrived, we weren't sure when to use it. But we learnt
to invent rules, so that it's generally not OK to use them in restaurants but
it's OK walking outside. We need to achieve the same with enhancement drugs. We
need the right culture surrounding it. And the only way we can do that is by
being honest about its consumption, and face up to the fact it is going on."
A spokeswoman for the Department of Health said a report had been commissioned
in 2008 investigating the issue of cognitive-enhancing drugs. She said: "We
strongly urge anyone thinking about taking a prescriptiononly medicine, not
intended for their personal use, to consult their GP first."
Online Health news, features and expert advice timesonline.co.
uk/health
LOAD-DATE: February 27, 2010
LANGUAGE: ENGLISH
GRAPHIC: The Times writer David Aaronovich said that the Ritalin-type tablets he
took brought unexpected benefits
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: TIM
Copyright 2010 Times Newspapers Limited
All Rights Reserved
170 of 998 DOCUMENTS
Herald Sun (Australia)
February 26, 2010 Friday
1 - FIRST Edition
Dangerous increase in prescription drug abuse `Smart pills' alarm
BYLINE: Felicity Williams social trends reporter
SECTION: NEWS; Pg. 29
LENGTH: 476 words
OVERWORKED Melbourne professionals and students are popping speed-like drugs in
growing numbers to help them get through the day.
The number of prescriptions for modafinil, a treatment for sleep disorders also
known to improve alertness and concentration, has almost doubled in Victoria in
the past three years.
Prescription drug abusers are also engaging in the dangerous practice of using
modafinil -- sold here as Modavigil -- without a doctor's authority by buying it
on the black market.
The Herald Sun can reveal that Melbourne professionals and students have openly
discussed the effects, dosage, price and their experiences obtaining the drug
without a prescription in an online drugs forum with a Russian domain name.
A computer programmer in the discussion thread described the effect of modafinil
as ``like amphetamine''.
``Modafinil seems to make me feel sharper . . . I don't know how else to
describe it,'' he wrote. ``I usually take it when I feel I should be getting
something done.''
Another user admitted he and his colleagues took the drugs before night meetings
when he was selling commercial real estate.
A student described it as ``the best study aid ever'' despite side-effects such
as ``nasty headaches'' and ``feeling scattered''.
According to the Pharmaceutical Benefits Scheme website, Victorian pharmacies
dispensed 723 items of modafinil last year, up from 370 in 2007.
It is also easy to obtain modafinil and other ``smart pills'' such as Ritalin,
for hyperactivity, and donepezil, for dementia, without a prescription at online
pharmacies.
The Herald Sun arranged for the purchase and shipment to Australia of one packet
of modafinil tablets but withdrew when the website requested credit card
details.
Australian Medical Association vice-president Dr Steve Hambleton said illicit
use of prescription drugs as smart pills was a major concern.
``There are a range of side-effects, particularly when people aren't taking
regular amounts,'' he said.
Tweet with Felicity Williams about the latest trends twitter.com/flickwilliams
MODAFINIL (Modavigil)
Treats sleep disorders such as narcolepsy
Used by prescription drug abusers to promote wakefulness
Side-effects include dependency, rashes, mania, delusions, hallucinations,
suicidal thoughts, high blood pressure, birth defects
DONEPEZIL (Aricept)
Treats Alzheimer's disease
Used by prescription drug abusers to boost mental performance
Side-effects include abnormally slow heart rate, fainting, diarrhoea, nausea,
vomiting, headaches, insomnia
May increase risk of stomach ulcers, seizures, asthma
RITALIN
Treats attention deficit hyperactivity disorder
Used by prescription drug abusers to enhance concentration
Side-effects include dependency, psychotic episodes, severe depression, suicidal
thoughts, high blood pressure
Linked to sudden death in children, teenagers and adults with serious heart
problems
LOAD-DATE: February 25, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: DHS
Copyright 2010 Nationwide News Pty Limited
All Rights Reserved
171 of 998 DOCUMENTS
Guardian Unlimited
February 23, 2010 Tuesday
A Pandora's box full of smart drugs
BYLINE: Ann Robinsonguardian.co.uk
LENGTH: 737 words
ABSTRACT
Ann Robinson: We should think very carefully before we start routinely taking
drugs such as Modafinil to boost cognitive function
FULL TEXT
Here's a thoroughly modern ethical dilemma to chew over. You go for a job
interview but are pipped to the post by another person who seems wholly
underwhelming and is less well qualified. The feedback is that she came across
as more zappy and focused. Over coffee, she shares that she's popped a tab of
before the interview. How does that make you feel?
Or here's another one. Senior members of the academic department that you work
in share their tip for being able to fly over to the US and deliver a lecture
the same day while looking fresh and sounding perky. They regularly take the
drug to counter jet lag and enhance their cognitive function. You're not keen,
but as a junior member of the team, you want to perform as well as possible. So
do you try to get your GP to prescribe some or, like most of your workmates, buy
some on line?
These challenges aren't theoretical but real. Cognitive-enhancing drugs, also
known as "smart" drugs are already being used to help people with Alzheimer's
disease, schizophrenia, attention deficit hyperactivity disorder (ADHD) and
brain injury. But is there burgeoning use among university students and others
wishing to boost their brain power? It is this that's posing the ethical
dilemmas.
, professor of clinical neuropsychology at Cambridge University, described how
the smart drugs fit in to our quest to keep our minds functioning longer and
better in our ageing population, in a , organised by Prospect magazine.
The three drugs in common use are (Ritalin), (Provigil) and (Strattera). All
boost neurotransmitter chemicals (noradrenaline, acetylcholine, dopamine) at the
junction between nerves to improve transmission or electrical activity.
Even modest improvements in cognitive function can make a big difference to
people's lives. It can make the difference between someone with schizophrenia
being able to live independently or not. Or a kid with ADHD being able to stop
his impulsive behaviour and stay out of trouble at school. And there are huge
financial implications in being able to reduce the cost of long-term care for
people with Alzheimer's if a drug can slow their cognitive decline by even 1%.
Professor Sahakian said that the smart drugs are just one approach to boosting
cognitive function. Exercise (three brisk walks a week will do, she said) and
learning new things throughout life are most important. And connecting with
others, giving of yourself and maintaining your curiosity about life are the
other cornerstones of mental wellbeing.
She warns against the potential dangers of people under 20, whose brains are
still developing, taking smart drugs like Ritalin unless they have a condition
such as ADHD. But an estimated 16-20% of US college students take smart drugs
and there is reason to believe its spreading to the UK.
The field of is developing to look at challenges posed by advances in the
neurosciences. Some arguments for smart drugs include removing disparity in
society and boosting performance. In a lengthy operation, it is best to have one
surgeon do the whole job and a tab of Modafinil may be better than caffeine
which, in high doses, can cause tremor.
The US army is interested in smart drugs to allow troops to complete military
operations as quickly as possible. But the potential harms include the fact that
we don't know about long-term effects, especially in developing brains. People
may feel coerced into taking them. There's a potential for abuse and you may get
unwanted effects like persistent memories. Is it cheating to take the drugs?
Will it turn us into mechanistic beings who don't feel we've earned the right to
feel proud of our achievements? Will working hard and being motivated become
antiquated concepts? Will we become a homogenous society and will we lose
creativity?
The last concern is practical. There is no licence for prescribing smart drugs
unless you have a specified condition. No self-respecting GP is likely to
prescribe it. And buying drugs online is fraught with dangers. You have to check
you have no contraindications, that it won't interact with any other medication
and that what you get in the post is what it says on the box.
LOAD-DATE: February 23, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2010 Guardian Unlimited
All Rights Reserved
172 of 998 DOCUMENTS
Reuters Health Medical News
January 28, 2010 Thursday 9:00 PM EST
Stimulants better than nonstimulants for adult ADHD: meta-analysis
SECTION: CLINICAL
LENGTH: 588 words
DATELINE: NEW YORK
Stimulant medications show greater efficacy than nonstimulants for treating
attention-deficit/hyperactivity disorder (ADHD) in adults, according to a new
meta-analysis.
Study authors Dr. Stephen V. Faraone and Dr. Stephen J. Glatt note that
stimulants have been the mainstay of ADHD pharmacotherapy for decades. Several
nonstimulant medications have also been shown effective - tricyclic
antidepressants, bupropion, modafinil, monoamine oxidase inhibitors, guanfacine,
atomoxetine, and clonidine.
However, it's been difficult to compare different drugs or drug classes due to
the lack of head-to-head trials.
Drs. Faraone and Glatt, both from SUNY Upstate Medical University in Syracuse,
New York, searched the medical literature for double-blind, placebo-controlled
studies of ADHD in adults published after 1979, in which subjects were followed
for at least 2 weeks. They identified 18 articles that involved more than 2000
subjects and evaluated 13 drugs.
In their report, which appeared online December 29 in the Journal of Clinical
Psychiatry, effect size is expressed as the standardized mean difference, in
which a 1-point difference is equivalent to 1 standard deviation on the outcome
measure.
Five trials studied 4 long-acting stimulants (mixed amphetamine salts extended
release, osmotic-release oral system methylphenidate, dexmethylphenidate
extended release, and lisdexamfetamine dimesylate) in 637 participants. The
mean effect size was 0.73.
The 3 short-acting stimulants evaluated in 7 trials (n = 459) were mixed
amphetamine salts, dextroamphetamine, and methylphenidate. The effect size was
0.96.
Nine trials with 968 subjects examined the efficacy of 6 nonstimulants
(atomoxetine, bupropion SR, modafinil, bupropion XL, paroxetine, and an
investigational drug ABT-418). The mean effect size was 0.39.
There was significant heterogeneity among effect sizes, and evidence of
publication bias, only in the trials of short-acting stimulants. Correction for
publication bias revealed an effect size of 0.86, which did not differ
significantly from that of long-acting stimulants.
There was also no significant difference between methylphenidate- and
amphetamine-based medications.
On the other hand, the effect sizes for nonstimulant medications were
significantly less than those for long-acting stimulants. After correcting for
differences in study design, nonstimulants did not differ from short-acting
stimulants.
Dr. Faraone and Dr. Glatt note that the effect sizes are robust and similar to
those reported for medication treatment studies of children with ADHD. Only one
medication, paroxetine, was worse than placebo.
Numbers needed to treat (NNT) ranged from 2 to 3 for long-acting stimulants,
from 2 to 4 for short-acting stimulants, and from 2 to 5 for nonstimulants.
Among nonstimulants, only modafinil had a NNT of less than 3.
The authors point out that the response rates are less than those reported in
the literature, because the latter are not placebo adjusted.
"The NNT results...suggest that most patients will need more than 1 drug trial
to achieve a positive outcome that cannot be attributed to a placebo effect."
Still, in the absence of head-to-head trials, the researchers urge caution in
comparing effects of different medications across studies.
The study was funded by a grant from Shire US, whose products include
lisdexamfetamine dimesylate (Vyvanse), methylphenidate transdermal (Daytrana),
methylphenidate hydrochloride (Equasym), and guanfacine (Intuniv).
SOURCE: J Clin Psychiatry 2009.
LOAD-DATE: January 29, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2010 Reuters Health
All Rights Reserved
173 of 998 DOCUMENTS
US Fed News
January 20, 2010 Wednesday 10:37 AM EST
Patent No. 7,649,020 Issued on Jan. 19, Assigned to Cephalon France for
Modafinil Polymorphic Forms (French Inventors)
LENGTH: 187 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., Jan. 21 -- Armand Frydman of Verrieres-le-Buisson, France,
Veronique Broquaire of Noisy-le-Grand, France, Laurent Courvoisier of
Laigneville, France, Franck Mallet of Blangy sur Bresle, France, Gerard Coquerel
of Boos, France, and Michel Broquaire of Le Perreux, France, have developed
modafinil polymorphic forms. The inventors were issued U.S. Patent No. 7,649,020
on Jan. 19. The patent has been assigned to Cephalon France, Maisons-Alfort,
France. According to the abstract released by the U.S. Patent & Trademark
Office: "Polymorphic forms of modafinil racemate, methods of preparation
thereof, pharmaceutical compositions and methods of therapeutic treatment
involving modafinil polymorphic forms." The original application was filed on
Dec. 14, 2007. For further information please visit:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO2&Sect2=HITOFF&p=1&u=%2Fnetah
tml%2FPTO%2Fsearch-bool.html&r=1&f=G&l=50&co1=AND&d=PTXT&s1=7649020&OS=7649020&R
S=7649020 For more information about US Fed News contract awards please contact:
Sarabjit Jagirdar, US Fed News, Email:- htsyndication@hindustantimes.com
LOAD-DATE: January 21, 2010
LANGUAGE: ENGLISH
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174 of 998 DOCUMENTS
Reuters Health Medical News
January 19, 2010 Tuesday 9:00 PM EST
No improvements in schizophrenia symptoms seen with modafinil
SECTION: CLINICAL
LENGTH: 410 words
DATELINE: NEW YORK
The "wakefulness promoting" agent modafinil does not appear to help
schizophrenic patients who don't respond well to clozapine, researchers report
in the December issue of the Journal of Clinical Psychiatry.
Clozapine "mostly treats positive symptoms," the researchers explain, "with
meager efficacy at best" for negative symptoms or cognitive deficits.
Furthermore, "clozapine-induced sedation can worsen cognition and impair social
and occupational functioning," lead investigator Dr. Oliver Freudenreich of
Harvard Medical School, Boston, and colleagues point out.
Modafinil, which is sold in the US as Provigil, is approved to treat narcolepsy
and shift work sleep disorder. Three previous controlled trials that assessed
the safety and efficacy of modafinil add-on therapy in schizophrenia had
inconsistent results, according to Dr. Freudenreich and his associates.
In a double-blind, placebo-controlled, flexible-dose pilot trial in 35 patients,
the researchers evaluated the safety, tolerability, and effect of modafinil on
negative symptoms, cognition, and wakefulness/fatigue.
All subjects were outpatients with stable schizophrenia, and all were taking
clozapine. For the 8-week study, they were randomized to receive up to 300
mg/day of modafinil (n=19) in addition to clozapine, or placebo (n=16).
The patients were an average of 45.2 years old and their mean duration of
illness was 19.5 years. Adherence was over 75% for most subjects. At the end
of treatment, the average dose of modafinil was 250 mg/d.
"Modafinil was well-tolerated, with no clear tolerability problem in this small
sample," the researchers note. "We did not detect worsening of psychosis, one
of the safety concerns that has been raised with modafinil."
But, they add, there was no reduction in cognitive deficits, negative symptoms
or wakefulness and fatigue with modafinil compared with placebo.
"Our power to detect differences between modafinil and placebo was limited by
sample size," the authors said, adding that larger trials might show a benefit
with modafinil.
They also caution that physicians who prescribe this agent on a case-by-case
off-label basis should keep in mind that rare instances of psychosis, rashes,
and Stevens-Johnson syndrome have been reported with modafinil use.
The pilot trial was sponsored by Cephalon Inc, the manufacturer of modafinil.
Two of the authors receive grant and research support from Cephalon.
SOURCE: J Clin Psychiatry 2009;70:1674-1680.
LOAD-DATE: January 20, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
175 of 998 DOCUMENTS
PR Newswire
December 21, 2009 Monday 4:30 PM EST
Cephalon Provides Update on Regulatory Review of NUVIGIL for the Treatment of
Excessive Sleepiness Associated with Jet Lag Disorder;
Company Expects FDA Decision by End of First Quarter 2010
LENGTH: 1014 words
DATELINE: FRAZER, Pa., Dec. 21
FRAZER, Pa., Dec. 21 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced that the U.S. Food and Drug Administration (FDA) has extended
the action date to March 29, 2010, for its review of the supplemental New Drug
Application (sNDA) for NUVIGIL® (armodafinil) Tablets [C-IV]. The sNDA is for
the indication of improved wakefulness in patients with excessive sleepiness
associated with jet lag disorder due to eastbound travel.
"We will continue to work closely with the FDA to assist them in completing
their review of our application in a timely manner and do not anticipate any
further delays beyond the March 29, 2010, action date," said Dr. Lesley Russell,
Chief Medical Officer at Cephalon. "We remain excited about this opportunity as
there are no medications approved by the FDA to treat excessive sleepiness
associated with eastbound jet lag disorder."
This sNDA for NUVIGIL was filed with the FDA on June 29, 2009, and given the
action date of December 29, 2009, under the Prescription Drug User Fee Act
(PDUFA). The company submitted additional information within 90 days of the
assigned action date. Subsequently, the FDA informed the company that the agency
required more time for a full review of the submission and, therefore, would
extend the action date by three months.
About NUVIGIL
NUVIGIL, the longer-lasting isomer of modafinil, was launched in the United
States in June 2009. It is indicated to improve wakefulness in patients with
excessive sleepiness associated with treated obstructive sleep apnea (OSA),
shift work disorder (SWD), or narcolepsy. NUVIGIL is not approved as a treatment
for jet lag disorder or its associated symptoms. The NUVIGIL label includes a
bolded warning for serious or life-threatening rash, including Stevens-Johnson
Syndrome, that has been reported in adults and children taking modafinil, a
racemic mixture of S- and R-modafinil (the latter is armodafinil, the active
ingredient in NUVIGIL). NUVIGIL is not approved for use in pediatric patients
for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness, and insomnia. Full prescribing
information for NUVIGIL is available at www.NUVIGIL.com.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and commercialization of many unique
products in four core therapeutic areas: central nervous system, inflammatory
diseases, pain and oncology. A member of the Fortune 1000 and the S&P 500 Index,
Cephalon currently employs approximately 3,000 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, Pennsylvania,
and offices, laboratories or manufacturing facilities in West Chester,
Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis, Minnesota.
Cephalon has a growing presence in Europe, the Middle East and Africa. The
Cephalon European headquarters and pre-clinical development center are located
in Maisons-Alfort, France, just outside of Paris. Key business units are located
in England, Ireland, France, Germany, Italy, Spain, the Netherlands for the
Benelux countries, and Poland for Eastern and Central European countries.
Cephalon Europe markets more than 30 products in four areas: central nervous
system, pain, primary care and oncology.
The company's proprietary products in the United States include: NUVIGIL,
TREANDA® (bendamustine hydrochloride) for Injection, AMRIX® (cyclobenzaprine
hydrochloride extended-release capsules), FENTORA® (fentanyl buccal tablet)
[C-II], TRISENOX® (arsenic trioxide) injection, GABITRIL® (tiagabine
hydrochloride), PROVIGIL® (modafinil) Tablets [C-IV] and ACTIQ® (oral
transmucosal fentanyl citrate) [C-II]. The company also markets numerous
products internationally. Full prescribing information on its U.S. products is
available at http://www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, clinical development of NUVIGIL, prospects for and frequency
of filing new indications for NUVIGIL, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
Contacts:
Media: Investor Relations:
Candace Steele Flippin Chip Merritt
610-727-6231 (office) 610-738-6376 (office)
csteele@cephalon.com cmerritt@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media, Candace Steele Flippin, +1-610-727-6231, csteele@cephalon.com, or
Investor Relations, Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com, both
of Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: December 22, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 PR Newswire Association LLC
All Rights Reserved
176 of 998 DOCUMENTS
The Age (Melbourne, Australia)
October 2, 2009 Friday
First Edition
Call for testing on 'smart drugs'
BYLINE: JULIA MEDEW HEALTH REPORTER
SECTION: NEWS; Pg. 7
LENGTH: 466 words
INCREASING use of "smart drugs" among students aiming to improve their memory
and cognitive function could prompt authorities to start drug-testing students
before exams, an Australian researcher says.
Vince Cakic, a researcher from the University of Sydney's school of psychology,
said students were increasingly using psychostimulants â[#x20ac]" drugs usually
prescribed for neuropsychiatric disorders and sleep disorders â[#x20ac]" to
enhance their academic performance.
He said drugs such as selegiline, usually prescribed for Parkinson's disease,
were touted as a motivation enhancer, while others, such as modafinil and
piracetam, were known for keeping people alert and improving their memory
respectively.
Collectively, the drugs are known as "nootropics" or "smart drugs", he said,
because of the Greek words noo (mind) and troppo (to turn or change).
Although research recently published in the US suggested modafinil was
addictive, Mr Cakic said it was particularly popular among students because it
kept them awake and alert without making them hyperactive.
"I would say a lot of students are using that now," he said. "Memory enhancers
like piracetam are also very popular."
Mr Cakic said the drugs were easily purchased over the internet through online
pharmacies in South-East Asia, Mexico and India, but he said amphetamines such
as Dexedrine were harder to buy because they were controlled substances.
In an article published in the Journal of Medical Ethics today, Mr Cakic said
although some of the drugs had well-known side effects, including addictive
qualities and the potential to aggravate mental illness, it was unclear how
dangerous most of them were for healthy people long term.
"It remains to be seen whether nootropics represent a pharmacological 'free
lunch' or if the enhancement of some cognitive functions can only be realised at
the expense of others," he wrote.
Mr Cakic said increasing use among students could prompt people to treat them
like performance-enhancing drugs in professional sport. If it was perceived they
offered students an unfair advantage, drug tests could follow.
Australian Drug Foundation chief executive John Rogerson said anecdotal reports
suggested young people were talking more about these drugs, but he said there
was no indication it was a big problem in Australia.
"We haven't got evidence of this, but there's no doubt that kids are taking
stimulants like Ritalin to get a short-term advantage," he said.
"We would encourage young people to stay away from it."
SO-CALLED SMART DRUGS
METHYLPHENIDATE (Ritalin, Concerta)
MODAFINIL (Provigil, Modavigil)
AMPAKINES
PIRACETAM (Nootropil, Avigilen)
ERGOLOID (Hydergine, Cicanol)
BETA-BLOCKERS (Propranolol)
NOTE: THE AGE DOES NOT CONDONE THE USE OF ANY OF THESE DRUGS WITHOUT A
PRESCRIPTION AND APPROPRIATE MEDICAL ADVICE.
LOAD-DATE: October 1, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 The Age Company Limited
All Rights Reserved
177 of 998 DOCUMENTS
The Age (Melbourne, Australia)
October 2, 2009 Friday
Second Edition
'Smart' students could sit drug tests
BYLINE: JULIA MEDEW, HEALTH REPORTER
SECTION: NEWS; Pg. 3
LENGTH: 454 words
INCREASING use of "smart drugs" among students aiming to improve their memory
and cognitive function could prompt authorities to drug-test students before
exams, an Australian researcher says.
Vince Cakic, a researcher from the University of Sydney's school of psychology,
said students were increasingly using psychostimulants â[#x20ac]" drugs usually
prescribed for neuropsychiatric disorders and sleep disorders â[#x20ac]" to
enhance their academic performance.
He said drugs such as selegiline, usually prescribed for Parkinson's disease,
were touted as a motivation enhancer, while others, such as modafinil and
piracetam, were known for keeping people alert and improving their memory
respectively.
Collectively, the drugs are known as "nootropics" or "smart drugs".
Although research recently published in the US suggested modafinil was
addictive, Mr Cakic said it was particularly popular among students because it
kept them awake and alert without making them hyperactive.
"I would say that a lot of students are using that now," he said. "Memory
enhancers like piracetam are also very popular."
Mr Cakic said the drugs were easily purchased over the internet through online
pharmacies in South-East Asia, Mexico and India, but he said amphetamines such
as Dexedrine were harder to buy because they were controlled substances.
In an article published in the Journal of Medical Ethics today, Mr Cakic said
although some of the drugs had well-known side effects, including addictive
qualities and the potential to aggravate mental illness, it was unclear how
dangerous most of them were for healthy people long term.
"It remains to be seen whether nootropics represent a pharmacological 'free
lunch' or if the enhancement of some cognitive functions can only be realised at
the expense of others," he wrote.
Mr Cakic said increasing use among students could prompt people to view this
issue in the same light as performance-enhancing drugs in professional sport. If
it was perceived that drugs offered students an unfair advantage and were
dangerous, drug tests could follow.
Australian Drug Foundation chief executive John Rogerson said anecdotal reports
suggested young people were talking more about these drugs, but he said there
was no indication it was a big problem in Australia.
"There's no doubt that kids are taking stimulants like Ritalin to get a
short-term advantage," he said.
"Some of this stuff is being bought off the internet, which is very risky," he
said.
SO-CALLED SMART DRUGS
*METHYLPHENIDATE
(Ritalin, Concerta)
*MODAFINIL (Provigil, Modavigil)
*AMPAKINES
*PIRACETAM (Nootropil, Avigilen)
*ERGOLOID (Hydergine, Cicanol)
*BETA-BLOCKERS (Propranolol)
NOTE: THE AGE DOES NOT CONDONE THE USE OF
ANY OF THESE DRUGS WITHOUT A PRESCRIPTION
LOAD-DATE: October 2, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 The Age Company Limited
All Rights Reserved
178 of 998 DOCUMENTS
MX Brisbane (Queensland, Australia)
October 2, 2009 Friday
1 - BRIS Edition
Sample exams - Call for urine tests to tackle `smart drug'
BYLINE: Alex Dickinson
SECTION: MX; Pg. 1
LENGTH: 308 words
University students using ``smart drugs'' to get an edge in class could soon
face sports-style urine tests before exams.
Research from the University of Sydney has warned that students are increasingly
using ``performance enhancing'' psychostimulants usually prescribed for
Alzheimer's, Parkinson's or sleep disorders, to enhance their academic
performance.
Among those being taken are the ADD drug Ritalin, Aricept used to treat dementia
and the ``wide-awake'' drug Modafinil.
The drugs are being easily purchased over the internet through pharmacies in
South-East Asia, Mexico and India.
Researcher Vince Cakic, whose findings have been published in the Journal of
Medical Ethics, said purchasing ``smartness in a bottle'' is likely to have
broad appeal to students seeking to gain an advantage in an increasingly
competitive world.
He said the drugs are near-impossible to monitor, but a sports-style urine tests
would detect them.
``One conjures to mind the scenario of students taken to one side, cup in hand,
and asked to provide a urine sample to test officials,'' Cakic said.
He said that Modafinil was very popular among students in the US because it kept
them awake without making them hyperactive.
``So far, these drugs offer only a modest perk in performance, but more powerful
versions are in the pharmaceutical pipeline and may well have a potent allure,''
Cakic said.
But the proposal to set up urine tests before exams has angered student groups.
General secretary of the Queensland University of Technology Student Guild, Kat
Henderson, said urine tests on students was ``ridiculous''.
``There's nowhere in the world that a guild would allow the university to start
drug-testing students,'' Henderson said.
``I've never heard of using drugs for concentration as being a big problem. To
test students would be infringing on their basic rights.''
LOAD-DATE: October 2, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: MXB
Copyright 2009 Nationwide News Pty Limited
All Rights Reserved
179 of 998 DOCUMENTS
PR Newswire
September 24, 2009 Thursday 8:30 AM EST
Cephalon Announces that FDA Grants Priority Review of its Supplemental New Drug
Application for NUVIGIL as a Treatment for Excessive Sleepiness Associated with
Jet Lag Disorder
LENGTH: 957 words
DATELINE: FRAZER, Pa., Sept. 24
FRAZER, Pa., Sept. 24 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced the U.S. Food and Drug Administration (FDA) has granted a
priority review for its supplemental New Drug Application (sNDA) for NUVIGIL(R)
(armodafinil) Tablets [C-IV], which was filed in June of this year. The FDA
decision on approval of NUVIGIL as a treatment for improving wakefulness in
patients with excessive sleepiness associated with jet lag disorder due to
eastbound travel is expected by December 29, 2009. There currently is no
FDA-approved treatment for jet lag disorder.
The NUVIGIL sNDA is based on data from a Phase III pivotal study that evaluated
the efficacy and safety of NUVIGIL (50 or 150 mg/day) in 427 healthy adults over
three days during travel from the United States to Europe. These data were
presented earlier this year at the SLEEP 2009 23rd Annual Meeting of the
Associated Professional Sleep Societies.
About NUVIGIL
NUVIGIL, the longer-lasting isomer of modafinil, was launched in the United
States in June 2009 and is indicated to improve wakefulness in patients with
excessive sleepiness associated with treated obstructive sleep apnea, shift work
sleep disorder, also known as shift work disorder (SWD), and narcolepsy. NUVIGIL
is not approved as a treatment for jet lag disorder or its associated symptoms.
The NUVIGIL label includes a bolded warning for serious or life-threatening
rash, including Stevens-Johnson syndrome, that has been reported in adults and
children taking modafinil, a racemic mixture of S and R modafinil (the latter is
armodafinil, the active ingredient in NUVIGIL). NUVIGIL is not approved for use
in pediatric patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness and insomnia. Full prescribing
information for NUVIGIL is available at www.NUVIGIL.com.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and commercialization of many unique
products in four core therapeutic areas: central nervous system, inflammatory
diseases, pain and oncology. A member of the Fortune 1000 and the S&P 500 Index,
Cephalon currently employs approximately 3,000 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, Pennsylvania,
and offices, laboratories or manufacturing facilities in West Chester,
Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis, Minnesota.
Cephalon has a growing presence in Europe, the Middle East and Africa. The
Cephalon European headquarters and pre-clinical development center are located
in Maisons-Alfort, France, just outside of Paris. Key business units are located
in England, Ireland, France, Germany, Italy, Spain, the Netherlands for the
Benelux countries, and Poland for Eastern and Central European countries.
Cephalon Europe markets more than 30 products in four areas: central nervous
system, pain, primary care and oncology.
The company's proprietary products in the United States include: NUVIGIL,
TREANDA(R) (bendamustine hydrochloride) for Injection, AMRIX(R) (cyclobenzaprine
hydrochloride extended-release capsules), FENTORA(R) (fentanyl buccal tablet)
[C-II], TRISENOX(R) (arsenic trioxide) injection, GABITRIL(R) (tiagabine
hydrochloride), PROVIGIL(R) (modafinil) Tablets [C-IV], and ACTIQ(R) (oral
transmucosal fentanyl citrate) (C-II). The company also markets numerous
products internationally. Full prescribing information on its U.S. products is
available at www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, clinical development of NUVIGIL, timing of FDA decisions,
prospects for regulatory approval, manufacturing development and capabilities,
market prospects for its products, sales and earnings guidance, and other
statements regarding matters that are not historical facts. You may identify
some of these forward-looking statements by the use of words in the statements
such as "anticipate," "estimate," "expect," "project," "intend," "plan,"
"believe" or other words and terms of similar meaning. Cephalon's performance
and financial results could differ materially from those reflected in these
forward-looking statements due to general financial, economic, regulatory and
political conditions affecting the biotechnology and pharmaceutical industries
as well as more specific risks and uncertainties facing Cephalon such as those
set forth in its reports on Form 8-K, 10-Q and 10-K filed with the U.S.
Securities and Exchange Commission. Given these risks and uncertainties, any or
all of these forward-looking statements may prove to be incorrect. Therefore,
you should not rely on any such factors or forward-looking statements.
Furthermore, Cephalon does not intend to update publicly any forward-looking
statement, except as required by law. The Private Securities Litigation Reform
Act of 1995 permits this discussion.
Contacts:
Media
Sheryl Williams
610-738-6493
swilliam@cephalon.com
Investor Relations
Chip Merritt
(610) 738-6376
cmerritt@cephalon.com
Web Site:
www.cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media, Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com, or
Investor Relations, Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com, both
of Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: September 25, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
180 of 998 DOCUMENTS
Independent Extra
September 22, 2009 Tuesday
First Edition
The brain buzz you may live to regret;
So-called 'smart drugs' have been seized upon by undergraduates as a means to
stay alert and improve mental performance. But the long-term effects remain
unknown. Rob Sharp investigates - and gets students' verdicts on the effects
BYLINE: Rob Sharp
SECTION: INDEPENDENT LIFE; Pg. 10
LENGTH: 1501 words
Two mates in their mid-to-late 20s are joking around. One of them pulls a silver
blister pack from his pocket. It contains a rare drug, two pills of which he
pops from the shiny wrapper that he holds in his hand. He gives one pill to his
pal. They stand still for a moment, consider what they are about to do, before
placing the capsules into their mouths and washing them down with a swig of
water. They complete the move with a couple of mock-grimaces.
The drug in question is Modafinil, a form of prescription medication normally
used to treat narcolepsy, but which is increasingly being abused by students
across the US and UK for its stimulating properties: in small doses it can
improve your memory, increase your focus and prevent you from falling asleep
(proving especially handy in the run-up to exams). It is one of a group of
cognitive enhancers or "smart pills" that also includes Ritalin and Adderall,
both used to treat ADHD (attention-deficit/hyperactivity disorder), that have
similar properties.
A study by Cincinnati Children's Hospital published in the British Medical
Journal last month indicated that use of these latter two drugs in the US has
increased by 75 per cent between 1998 and 2005. What's more, a 2005 survey of
more than 10,000 US university students found that 4 to 7 per cent of them had
tried ADHD drugs at least once to pull pre-exam all-nighters. At some
institutions, more than one in four students said they'd sampled the pills. The
subject is relatively unstudied in the UK but the trend is the subject of a
forthcoming documentary, Wasted Britain, set to air on Current TV on 28
September.
"The problem is you don't know what you're getting," says Barbara Sahakian,
professor of clinical neuropsychology at Cambridge University's psychiatry
department. "We don't know about the effects of long-term use of drugs like
Modafinil. We should wait for the studies to show the effect of it on healthy
human beings. There are pressures on people but these quick fixes are not the
way forward; education and exercise are both good ways of enhancing cognition,
too."
Perhaps what is so worrying about the Current TV programme is the means by which
its participants, Steve Middleditch and Christian Boyd, first got hold of
Modafinil. "When the producers first told me to buy it I had never heard of it,"
says Middleditch. "So I began doing some research on the internet. I discovered
that with a few clicks I could get hold of it by filling in a phoney
prescription online. I said I had jet lag." A week later a pack of 30 pills
arrived, postmarked Mumbai.
To conduct his experiment, Steve woke up one day at 3am to make himself
fatigued, and took the pills at midday the following day. He describes the
experience of taking the drug as odd, to say the least. "It's difficult to
explain," he continues. "You get this massive buzz; it's a bit like drinking
five cups of coffee in one go. You get a definite buzz off it. It affects areas
of the brain rather than the heart. My hands were moving a bit. I definitely got
the jitters. It's the sort of thing that not only keeps you awake, it keeps you
blathering on. I certainly felt more focused. It was definitely stronger than I
thought it would be."
The effects of the drug are well-proven. In 2003, Cambridge University
researchers found a single dose helped male university students perform in
mental planning tests, accurately complete puzzles and remember long chains of
digits; it has also been tested by the US and British forces to allow soldiers
to complete all-night operations. Scientists believe Modafinil can give its user
48 hours of continuous wakefulness (though there are some side effects:
headaches are the most common, though there are plenty of others). The most
remarkable thing, however, is that its users don't have to pay back sleep "debt"
- a standard eight hours is enough to compensate for no sleep on the previous
night: could this mean a future of 22-hour days? Our bosses may hope so.
"I would take Modafinil again because for me the problem is concentration and
focus," says Boyd. "It allowed me to get down to what I wanted to do; I never
felt like being distracted, so it was great." Philip Harvey, a professor at
Emory University in Atlanta, says his work has been helped by Modafinil, which
he takes to combat jet lag. Unlike in the UK, American doctors can prescribe the
drug to night-shift workers as well as to narcoleptics. "I often fly to Europe
to give talks," he says. "I used to travel the day before to give myself time to
recover, but with Modafinil I can now give a talk the same day I arrive and feel
like I've had a normal night's sleep."
Modafinil is not a golden drug, though. Its other side-effects may include
insomnia, agitation, anxiety, agitation, and heart problems. And then there are
the ethics of taking something that might give you an unfair advantage over your
peers. "It's all in your personal preference," concludes Middleditch. "But I
don't think it is a good thing. I can see why some people might take them. We've
all had a deadline and been knackered and that pill will help you reach that
deadline. In some scenarios where people need it I can also agree with it - some
troops in combat might use it, or a paramedic might need it to stay focused.
Perhaps there's some warrant in that. But personally it's not something I would
take again, but that's just my feeling because it doesn't feel right. You become
this person that you are kind of not. It's a strange feeling - the day after you
still have this strange sensation in your head."
Ritalin and Adderall, which are defined by their active ingredients of mixed
amphetamine salts and methylphenidate, as well as increasing concentration (in
the right doses) can also be taken for the buzz they create. They are often used
in combination with other drugs such as alcohol, or cocaine. Research conducted
by Harry Sumnall, a psychopharmacologist at the Centre for Public Health at
Liverpool's John Moores University, claims that research he has conducted in
Merseyside shows that children with prescriptions for ADHD treatments were
routinely selling their drugs; in some cases, so were their parents. "At least
in the US they're looking out for the problem and routinely including Ritalin
misuse in high school drugs surveys, for example," he says. "We might have to do
the same here." These drugs are also less effective than Modafinil at enhancing
performance.
"The biggest issue with these drugs, certainly with the likes of Adderall, is
that it is very difficult to know how much to take; very quickly they can go
from enhancing your performance to making you of no use whatsoever," says John
Marsden, a reader in addiction psychology at the Institute of Psychiatry.
"Though the principal issue is that if people were using these drugs it might
set in train a process where people were using them more and more and become
addicted to them."
'Wasted Britain' is aired on Current TV (Sky channel 183/Virgin channel 155) on
Monday 28 September
Cognitive enhancers
Is it smart to take them?
Modafinil
Modafinil often comes in the form of the branded Provigil and is a
memory-enhancing and mood-brightening stimulant, which enhances wakefulness. It
stimulates activity within the brain and spinal cord (central nervous system).
It is used to treat narcolepsy and sleep apnoea. It was rejected in 2006 by the
Food and Drug Administration in America for prescribing to children with ADHD,
but it is prescribed in the UK. Some of the side effects include unstable moods,
blurred vision and difficulty sleeping. Ritalin - Tablets of Ritalin, one of the
most widely known drug used to treat ADHD in children, contain the active
ingredient methylphenidate hydrochloride. This is a stimulant and it is also
possible to buy methylphenidate tablets on their own in an unbranded form. As
well as calming hyperactive kids, it is used illegally by students to boost
concentration and effectiveness at exams. The drug is still illegal without
prescription in the UK, and is lawfully rated as class B in this instance.
Concerta
This is another branded version of methylphenidate hydrochloride, which has very
similar effects as Ritalin. It is one of the newer brands on the market used to
treat children with ADHD. The side effects seem less pronounced in children than
Ritalin but there are still many, such as abdominal pain, nervousness and
hostility. It is used less than Ritalin by students but for the same effects.
Adderall
Contains both amphetamines and dextro-amphetamines (amphetamine salts) and is
widely prescribed as a drug to treat ADHD. It has four component salts which are
claimed to metabolise at different rates. Manufacturers suggest that this makes
the effects smoother. It is also used to treat narcolepsy and sometimes severe
depression. The patient or drug user experiences more intense and sustained
periods of concentration. It can cause psychotic episodes in those with a
history of psychosis, though this is rare.
LOAD-DATE: September 21, 2009
LANGUAGE: ENGLISH
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JOURNAL-CODE: IE
Copyright 2009 Independent Print Ltd
All Rights Reserved
181 of 998 DOCUMENTS
US Fed News
August 21, 2009 Friday 1:04 PM EST
Patent No. 7,576,133 Issued on Aug. 18 for Modafinil Nasal Administration
(Illinois Inventors)
LENGTH: 116 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., Aug. 21 -- Carl Henry Lawyer, Matthew Carl Lawyer and Edward
Zadok Lawyer, all from Springfield, Ill., have developed a composition for nasal
administration of modafinil. The inventors were issued U.S. Patent No. 7,576,133
on Aug. 18.
According to the abstract released by the U.S. Patent & Trademark Office:
"Systemic delivery of Modafinil to the nasal mucous membrane elicits rapid
systemic therapeutic response with reduced side effects compared to current
methods of administration."
The original application was filed on March 7, 2003. For more information about
US Fed News contract awards please contact: Sarabjit Jagirdar, US Fed News,
Email:- htsyndication@hindustantimes.com
LOAD-DATE: September 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
182 of 998 DOCUMENTS
Clinical Advisor
August 12, 2009
Agent battles excessive sleepiness
SECTION: NEWS; Drug Updates from MPR
LENGTH: 619 words
HIGHLIGHT: Nuvigil promotes wakefulness in patients with various sleep disorders
Product: Nuvigil
Company: Cephalon
Pharmacologic class: Wakefulness promoter
Active ingredient: Armodafinil 50 mg, 150 mg, 250 mg; tabs.
Indication: To improve wakefulness in patients with excessive sleepiness
associated with obstructive sleep apnea/hypopnea syndrome (OSAHS), narcolepsy,
and shift-work sleep disorder (SWSD). Adjunct to standard treatment for
underlying airway obstruction in OSAHS.
Pharmacology: Armodafinil is the R-enantiomer of modafinil (Provigil). Of the
two enantiomers that comprise modafinil, the R-form is longer lasting. Both of
these drugs have wakefulness- promoting effects similar to those of
sympathomimetics such as amphetamines and methylphenidate.
Clinical trials: Two 12-week studies were conducted to establish the safety and
efficacy of armodafinil in OSAHS. In the first study, patients were given either
armodafinil 150 mg or 250 mg/day, or placebo. The second trial compared the
effects of armodafinil 150 mg/day and placebo. Both studies indicated that
patients given armodafinil showed improvements in their ability to remain awake
and in their overall clinical condition.
The results of a 12-week study indicated that armodafinil was effective in
improving wakefulness in patients with excessive sleepiness associated with
narcolepsy. Patients treated with armodafinil 150 mg or 250 mg/day showed a
significantly enhanced ability to remain awake, and more of the patients given
armodafinil had an improved overall clinical condition than those given placebo.
A 12-week trial was conducted to establish the efficacy of armodafinil in
patients with chronic SWSD. Patients were randomized to receive either
armodafinil 150 mg/day or placebo. Those given the study drug showed a
significant prolongation in the time to sleep onset, as measured by a sleep
latency test conducted during a simulated night shift at the final visit,
compared with those given placebo. Also, more patients treated with armodafinil
experienced an improvement in overall clinical condition, compared with patients
given the placebo.
Adults: > 17 years: OSAHS, narcolepsy: 150 mg or 250 mg once daily in the am.
SWSD: 150 mg one hour before starting shift. Severe hepatic impairment: reduce
dose.
Children: <17 years: not recommended.
Precautions: Discontinue if rash appears (unless clearly not drug-related), or
if angioedema, anaphylaxis, or multi- organ hypersensitivity reaction occurs.
OSAHS: treat underlying obstruction; maintain continuous positive airway
pressure use if indicated. History of left ventricle hypertrophy or mitral valve
prolapse syndrome (e.g., ischemic ECG changes, chest pain, arrhythmias
associated with central nervous system [CNS] stimulants): not recommended.
Recent MI. Unstable angina. Monitor BP. Psychosis. Depression. Mania. Severe
hepatic or renal impairment. Re- evaluate periodically. Elderly (may need to
reduce dose). Labor and delivery. Pregnancy (Cat. C). Nursing mothers.
Interactions: May antagonize hormonal contraceptives; use alternative or
additional contraception during and for one month after. Avoid alcohol. Caution
with monoamine oxidase inhibitors. Armodafinil levels may be decreased by CYP3A4
inducers (e.g., carbamazepine, phenobarbital, rifampin) and increased by CYP3A4
inhibitors (e.g., ketoconazole, erythromycin). May reduce levels of drugs
metabolized by CYP3A4 (e.g., cyclosporine). May increase levels of drugs
metabolized by CYP2C9 (e.g., warfarin) or CYP2C19 (e.g., phenytoin, diazepam,
propranolol).
Adverse reactions: Headache, insomnia, other CNS effects, GI upset; rash (may be
serious, e.g., Stevens-Johnson, toxic epidermal necrolysis).
How supplied: Tabs-60
For more information, call 800.896.5855 or visit www.Nuvigil.com.
LOAD-DATE: November 3, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
JOURNAL-CODE: 6
Copyright 2009 Haymarket Media.
All Rights Reserved
183 of 998 DOCUMENTS
US Fed News
August 3, 2009 Monday 11:07 AM EST
Patent No.7,566,805 Issued on July 28, Assigned to Cephalon for Modafinil
Compositions (Massachusetts Inventors)
LENGTH: 156 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., Aug. 3 -- Magali Bourghol Hickey of Medford, Mass., Matthew
Peterson of Hopkinton, Mass., Orn Almarsson of Shrewsbury, Mass., and Mark
Oliveira of Framingham, Mass., have developed a modafinil compositions. The
inventors were issued U.S. Patent No. 7,566,805 on July 28.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
According to the abstract released by the U.S. Patent & Trademark Office:
"Co-crystals and solvates of racemic, enantiomerically pure, and
enantiomerically mixed modafinil are formed and several important physical
properties are modulated. The solubility, dissolution, bioavailability, dose
response, and stability of modafinil can be modulated to improve efficacy in
pharmaceutical compositions."
The original application was filed on Sept. 4, 2004.For more information about
US Fed News contract awards please contact: Sarabjit Jagirdar, US Fed News,
Email:- htsyndication@hindustantimes.com
LOAD-DATE: August 3, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 HT Media Ltd.
All Rights Reserved
184 of 998 DOCUMENTS
Pediatric News
August 2009
Editorial Data Needed on Cognition-Enhancing Drugs
BYLINE: Richard N. Rosenthal, M.D.
SECTION: Pg. 14 Vol. 43 No. 8 ISSN: 0031-398X
LENGTH: 853 words
DR. ROSENTHAL is chairman of psychiatry at St. Luke's-Roosevelt Hospital
Center and professor of clinical psychiatry at Columbia University, both in New
York, and a past president of the American Academy of Addiction Psychiatry. Dr.
Rosenthal disclosed that he receives research grants from Titan Pharmaceuticals
Inc. and Forest Research Institute. To respond to this editorial, e-mail Dr.
Rosenthal at pdnews@elsevier.com
If we had drugs that would make people smarter, wouldn't that benefit
society? And would using drugs in this way be a bad thing?
The reality is: We do have such drugs. And, more and more, we are hearing
accounts of normal people taking agents to enhance their mental acuity and
alertness at work and in school.
The journal Nature did a survey last year that looked at 1,400 of its
scientist readers from 60 countries (Nature 2008;456:702-5). The survey found
that 20% of them had used cognitive enhancement in the form of modafinil or
methylphenidate or had used beta-blockers to calm them and help them focus when
they had to give presentations. Interestingly, 80% of them were in favor of
being able to obtain the drugs at their own discretion, as opposed to having to
go to a doctor or visit the Internet to get a prescription.
Cognition-enhancing drugs give a competitive edge, and in our society the
pressure to succeed is huge. Strikingly, one-third of those responding to the
Nature survey said they would feel obligated to give cognition-enhancing drugs
to their children if the other children in school were taking them.
Some of us may think that the use of such performance-enhancing drugs in
"normal" people is wrong. Others see the practice as cheating. The use of a pill
to make us smarter somehow goes against the Judeo-Christian ethic, which tells
us there is no gain without pain-that gain without pain weakens our character.
But does it automatically follow that taking a drug solely to satisfy a person's
desires is objectionable?
The notion of improving performance using psychopharmacology is not a new
one. Examples include the use of alcohol, caffeine, and herbs, as well as
pharmaceutical agents.
In a study of commercial pilots, those who took 5 mg/day of the
cholinesterase inhibitor donezepil (Aricept) for 1 month did better in flight
simulation tests did than their counterparts who took placebo, especially in
emergency situations. Think about that. If you are a passenger, wouldn't you
rather have your pilot on donezepil?
Many people use caffeine for its stimulant properties. Caffeine improves
concentration and increases the capacity for information processing in the
brain. Glucose priming also enhances learning and memory, so coffee with sugar
is a powerful combination. Is a sweet espresso an unfair advantage at work? If
it reduces accidents in an industrial setting, why wouldn't you want people to
consume caffeine?
Methylphenidate (Ritalin) improves concentration, working memory, and
attention in people with attention-deficit/hyperactivity disorder. In healthy
adults, it improves executive functioning. It's well known on college campuses
for use as a study aid, but college students may ignore traditional dosing and
snort it at high doses before taking exams or writing papers.
Modafinil (Provigil), approved for narcolepsy and shift-work sleep disorders,
reduces attention deficits attributable to sleep deprivation. In normal adults,
it significantly improves fatigue levels, motivation, vigilance, performance on
digital pattern recognition, memory, and reaction time. Reportedly, modafinil is
the entrepreneur's drug of choice in Silicon Valley.
There's a lot of nonmedical use of modafinil out there, and this begs the
question about people using it this way-not just people, but also our
colleagues.
The pharmaceutical industry is working to develop a drug aimed at inhibiting
memory formation to prevent posttraumatic stress disorder after a traumatic
event. This is primary prevention, and it is a good idea.
But what about using such a drug simply to prevent an unpleasant memory? Is
that okay? How should use of cognition-enhancing drugs be regulated in healthy
people? Should their use always be monitored by health care professionals?
These people are not patients; they are healthy members of society. Their
rationale for using medication is for self-enhancement, not therapy. But many of
these medications are supposed to be available only by prescription.
We need to do scientific work in this area. There may be evils associated
with such use, such as increased social inequity. But there may also be real
benefits to our society. I fear that if we do not attempt to answer some of
these questions and create some guidelines, the government will do so. And when
the government does it, the outcome often falls short.
Whatever our views on the matter, society is moving this way. The train has
left the station, and there appears to be no conductor on board. Do we want to
get on and steer, or do we want to stand by and let someone else deal with this
increasingly important issue?
LOAD-DATE: August 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: PDNEWS
Copyright 2009 Elsevier Inc., International Medical News Group
All Rights Reserved
185 of 998 DOCUMENTS
Irish Independent
July 7, 2009 Tuesday
A stimulating debate
SECTION: FEATURES
LENGTH: 214 words
Ritalin
A stimulant drug introduced in 1956 for the treatment of Attention Deficit
Hyperactivity Disorder (ADHD) in children, it has become increasingly widely
used, especially in the US. Recent reports have emerged of it being abused by
students seeking aids to help them through their exams.
Amphetamines
The stimulant was first synthesised more than a century ago and has been used
and abused to boost energy, increase wakefulness and prolong endurance.
Its users have been as diverse as long distance lorry drivers wanting to ward
off drowsiness and women trying to lose weight.
Today it is prescribed for ADHD and narcolepsy, and has been investigated for
its role in helping stroke victims re-learn motor skills.
Donepezil
Scientists in aviation medicine and in the military have been examining
medicines which might increase alertness and concentration to minimise risk of
pilot error and maximise endurance. Donepezil, used to treat dementia, has been
shown to boost the performance of pilots on flight simulators.
Modafinil
Modafinil, a drug used to treat the sleep disorder narcolepsy, has also been
tested on pilots and other members of the armed forces.
Tests on helicopter pilots flying on simulators who had been deprived of sleep
showed the drug boosted performance.
LOAD-DATE: July 7, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 Independent News and Media Ltd.
All Rights Reserved
186 of 998 DOCUMENTS
US Fed News
July 6, 2009 Monday 1:14 PM EST
Patent No. 7,553,646 Issued on June 30, Assigned to University of Iowa Research
Foundation for Synthesis Methods (Iowa Inventors)
LENGTH: 186 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., July 6 -- Horacio F. Olivo and Antonio Victor Osorio-Lozada,
both of Iowa City, Iowa, have developed synthesis methods. The inventors were
issued U.S. Patent No. 7,553,646 on June 30.
The patent has been assigned to University of Iowa Research Foundation, Iowa
City. According to the abstract released by the U.S. Patent & Trademark Office:
"The present invention provides novel methods for the synthesis of racemic and
enantiomers of modafinil via microbial oxidation-amidation transformation. The
methods include the successive oxidation-amidation of benzhydrylsulfanyl
carboxylic acid to produce racemic and enantiomers of modafinil using at least
one microorganism of yeast, bacteria, or fungus. Also disclosed are
pharmaceutical compositions of racemic and enantiomers of modafinil along with
their use in the treatment of diseases, including attention deficit
hyperactivity disorder and drug addiction." The original application was filed
on July 27, 2006.For more information about US Fed News contract awards please
contact: Sarabjit Jagirdar, US Fed News, Email:-
htsyndication@hindustantimes.com
LOAD-DATE: July 6, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 HT Media Ltd.
All Rights Reserved
187 of 998 DOCUMENTS
PR Newswire
June 30, 2009 Tuesday 8:00 AM GMT
Cephalon Submits NUVIGIL Supplemental New Drug Application for the Treatment of
Excessive Sleepiness Associated with Jet Lag Disorder
LENGTH: 1189 words
DATELINE: FRAZER, Pa., June 30
FRAZER, Pa., June 30 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq: CEPH)
today announced that it has submitted a supplemental New Drug Application (sNDA)
to the U.S. Food and Drug Administration (FDA) requesting approval of NUVIGIL(R)
(armodafinil) Tablets [C-IV] for the indication of improved wakefulness in
patients with excessive sleepiness associated with jet lag disorder resulting
from eastbound travel. Jet lag disorder is an acute condition that occurs when a
person's internal body clock becomes disrupted as a result of rapid travel
across several time zones. Based on U.S. Bureau of Labor Statistics findings, an
estimated 70 million American travelers experience jet lag annually. Currently,
there are no FDA-approved medications to improve wakefulness in travelers who
experience the excessive sleepiness commonly associated with long flights.
"This supplemental New Drug Application for a new use of NUVIGIL is another
important milestone for Cephalon. We hope that this will be the first of many
new indications for NUVIGIL over the next five years," said Dr. Lesley Russell,
Chief Medical Officer and Executive Vice President at Cephalon.
The NUVIGIL sNDA for the treatment of excessive sleepiness associated with jet
lag disorder is based on data from a Phase 3 study, recently presented at the
SLEEP 2009 23rd Annual Meeting of the Associated Professional Sleep Societies in
Seattle, Washington. The data from this novel placebo-controlled pivotal study,
which involved overseas air travel, included an evaluation of the efficacy and
safety of NUVIGIL (50 or 150 mg/day) in 427 healthy men and women who all had
experienced jet lag symptoms at least once during the previous five years.
Clinical efficacy was evaluated using two primary endpoints: an objective
assessment -- the Multiple Sleep Latency Test (MSLT), and a subjective
assessment -- the Patient Global Impression of Severity (PGI-S). Patients taking
NUVIGIL (150 mg/day) showed a statistically significant improvement over placebo
as measured by the MSLT [p<0.0001] and the PGI-S [p<0.05]. The most common
adverse events associated with NUVIGIL treatment (five percent or greater) were
headache, nausea, diarrhea, and palpitations.
About NUVIGIL
NUVIGIL, the longer-lasting form of modafinil, was launched in the United States
in June 2009 and is indicated to improve wakefulness in patients with excessive
sleepiness associated with treated obstructive sleep apnea (OSA), shift work
sleep disorder, also known as shift work disorder (SWD), and narcolepsy. NUVIGIL
is not currently indicated for the treatment of jet lag disorder or its
associated symptoms. The NUVIGIL label includes a bolded warning for serious or
life-threatening rash, including Stevens-Johnson Syndrome, that has been
reported in adults and children taking modafinil, a racemic mixture of S- and R-
modafinil (the latter is armodafinil, the active ingredient in NUVIGIL). NUVIGIL
is not approved for use in pediatric patients for any indication.
The most common adverse events in controlled clinical trials (five percent or
greater) were headache, nausea, dizziness, and insomnia. Full prescribing
information for NUVIGIL is available at www.NUVIGIL.com.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and commercialization of many unique
products in four core therapeutic areas: central nervous system, inflammatory
diseases, pain and oncology. A member of the Fortune 1000 and the S&P 500 Index,
Cephalon currently employs approximately 3,000 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, Pennsylvania,
and offices, laboratories or manufacturing facilities in West Chester,
Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis, Minnesota.
Cephalon has a growing presence in Europe, the Middle East and Africa. The
Cephalon European headquarters and pre-clinical development center are located
in Maisons-Alfort, France, just outside of Paris. Key affiliates are located in
England, Ireland, France, Germany, Italy, Spain, the Netherlands for the Benelux
countries, and Poland for Eastern and Central European countries. Cephalon
Europe markets more than 30 products in four areas: central nervous system,
pain, primary care and oncology.
The company's proprietary products in the United States include: NUVIGIL,
TREANDA(R) (bendamustine hydrochloride) for Injection, AMRIX(R) (cyclobenzaprine
hydrochloride extended-release capsules), FENTORA(R) (fentanyl buccal tablet)
[C-II], TRISENOX(R) (arsenic trioxide) injection, GABITRIL(R) (tiagabine
hydrochloride), PROVIGIL(R) (modafinil) Tablets [C-IV], and ACTIQ(R) (oral
transmucosal fentanyl citrate) [C-II]. The company also markets numerous
products internationally. Full prescribing information on its U.S. products is
available at http://www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, clinical development of NUVIGIL, prospects for and frequency
of filing new indications for NUVIGIL, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
Contacts:
Media: Investor Relations:
Candace Steele Chip Merritt
610-727-6231 (office) 610-738-6376 (office)
csteele@cephalon.com cmerritt@cephalon.com
SOURCE Cephalon, Inc.
CONTACT:Media, Candace Steele, +1-610-727-6231 (office), csteele@cephalon.com,
or Investor Relations, Chip Merritt, +1-610-738-6376 (office),
cmerritt@cephalon.com, both of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: July 1, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 PR Newswire Association LLC
All Rights Reserved
188 of 998 DOCUMENTS
US Fed News
June 5, 2009 Friday 4:26 PM EST
Patent No. 7,541,493 Issued on June 2, Assigned to Cephalon France for Modafinil
Preparation Process (French Inventor)
LENGTH: 162 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., June 5 -- Sebastien Rose, Arsy, France, has developed a process
for preparing modafinil with a defined granulometry. The inventor was issued
U.S. Patent No. 7,541,493 on June 2.
The patent has been assigned to Cephalon France, Maisons Alfort, France.
According to the abstract released by the U.S. Patent & Trademark Office: "The
invention relates to a process for preparing modafinil having a defined
granulometry which comprises the steps of: a) preparing a solution of methyl
diphenylmethylsulphinyl-acetate; b) contacting the solution obtained with NH3 at
a predetermined temperature and a predetermined stirring; and c) isolating the
modafinil formed, wherein said temperature and said stirring are predetermined
in order to obtain said defined granulometry." The original application was
filed on May 5, 2004.For more information about US Fed News contract awards
please contact: Sarabjit Jagirdar, US Fed News, Email:-
htsyndication@hindustantimes.com
LOAD-DATE: June 5, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 HT Media Ltd.
All Rights Reserved
189 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
June 3, 2009
Nuvigil available in US for treatment of excessive sleepiness
LENGTH: 449 words
Cephalon's Nuvigil (armodafinil) Tablets [C-IV], a longer-lasting formulation of
modafinil, is now available in the US. It is indicated to improve wakefulness
throughout the day for patients who struggle with excessive sleepiness
associated with treated obstructive sleep apnoea, shift work sleep disorder and
narcolepsy. Cephalon has finalised the commercialisation plans for the product
and any patient with a Nuvigil prescription should now be able to obtain the
medication from their pharmacy or have it filled within 24 hours.
As part of the launch of Nuvigil, the company is introducing several new
programmes designed to expand access for both patients and healthcare providers.
To assist insured patients with co-pay costs for the drug, Cephalon will offer
the Nuvigil Prescription Savings Program. Through this programme, eligible
patients will receive a co-pay savings at the pharmacy to reduce their
out-of-pocket costs to fill the prescription. Further, to help patients and
healthcare providers navigate the authorisation and reimbursement process,
Cephalon established the Nuvigil Reimbursement Hotline. The company is also
working with managed care organisations in order to provide greater patient
access for Nuvigil through health plans nationwide. In addition, this year
Cephalon created the CephalonCares Foundation to provide free medication to
eligible patients. Cephalon is also exploring the potential for Nuvigil to treat
the symptoms associated with an array of medical disorders. The company recently
announced results from a Phase III trial of the drug as a treatment for patients
with excessive sleepiness associated with jet lag disorder. Those data are
expected to be submitted as part of an sNDA later this year. In addition, the
company has an extensive clinical development programme in place to further
study the efficacy and safety of Nuvigil in bipolar depression, the negative
symptoms of schizophrenia, cancer treatment-related fatigue and excessive
sleepiness associated with traumatic brain injury. Nuvigil is indicated to
improve wakefulness in patients with excessive sleepiness associated with
treated obstructive sleep apnoea, shift work sleep disorder and narcolepsy. The
Nuvigil label includes a bolded warning for serious or life-threatening rash,
including Stevens-Johnson syndrome, that has been reported in adults and
children taking modafinil, a racaemic mixture of S and R modafinil (the latter
is armodafinil, the active ingredient in Nuvigil). Nuvigil is not approved for
use in paediatric patients for any indication. The most common adverse events in
controlled clinical trials (>5 per cent) were headache, nausea, dizziness and
insomnia.
LOAD-DATE: June 3, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 ESPICOM Business Intelligence Ltd.
All Rights Reserved
190 of 998 DOCUMENTS
CNS Drug News
June 3, 2009
Nuvigil available in US for treatment of excessive sleepiness
SECTION: NEWS
LENGTH: 448 words
Cephalon's Nuvigil (armodafinil) Tablets [C-IV], a longer-lasting formulation of
modafinil, is now available in the US. It is indicated to improve wakefulness
throughout the day for patients who struggle with excessive sleepiness
associated with treated obstructive sleep apnoea, shift work sleep disorder and
narcolepsy. Cephalon has finalised the commercialisation plans for the product
and any patient with a Nuvigil prescription should now be able to obtain the
medication from their pharmacy or have it filled within 24 hours.
As part of the launch of Nuvigil, the company is introducing several new
programmes designed to expand access for both patients and healthcare providers.
To assist insured patients with co-pay costs for the drug, Cephalon will offer
the Nuvigil Prescription Savings Program. Through this programme, eligible
patients will receive a co-pay savings at the pharmacy to reduce their
out-of-pocket costs to fill the prescription. Further, to help patients and
healthcare providers navigate the authorisation and reimbursement process,
Cephalon established the Nuvigil Reimbursement Hotline. The company is also
working with managed care organisations in order to provide greater patient
access for Nuvigil through health plans nationwide. In addition, this year
Cephalon created the CephalonCares Foundation to provide free medication to
eligible patients.
Cephalon is also exploring the potential for Nuvigil to treat the symptoms
associated with an array of medical disorders. The company recently announced
results from a Phase III trial of the drug as a treatment for patients with
excessive sleepiness associated with jet lag disorder. Those data are expected
to be submitted as part of an sNDA later this year. In addition, the company has
an extensive clinical development programme in place to further study the
efficacy and safety of Nuvigil in bipolar depression, the negative symptoms of
schizophrenia, cancer treatment-related fatigue and excessive sleepiness
associated with traumatic brain injury.
Nuvigil is indicated to improve wakefulness in patients with excessive
sleepiness associated with treated obstructive sleep apnoea, shift work sleep
disorder and narcolepsy. The Nuvigil label includes a bolded warning for serious
or life-threatening rash, including Stevens-Johnson syndrome, that has been
reported in adults and children taking modafinil, a racaemic mixture of S and R
modafinil (the latter is armodafinil, the active ingredient in Nuvigil). Nuvigil
is not approved for use in paediatric patients for any indication. The most
common adverse events in controlled clinical trials (>5 per cent) were headache,
nausea, dizziness and insomnia.
LOAD-DATE: December 29, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
JOURNAL-CODE: CNS Drug News
Copyright 2009 Espicom Business Intelligence
All Rights Reserved
191 of 998 DOCUMENTS
Internal Medicine News
June 1, 2009
Editorial Data Needed on Cognitive-Enhancing Drugs
BYLINE: Richard N. Rosenthal, M.D.
SECTION: Pg. 9 Vol. 42 No. 11 ISSN: 1097-8690
LENGTH: 918 words
DR. ROSENTHAL is chairman of psychiatry at St. Luke's-Roosevelt Hospital
Center, professor of clinical psychiatry at Columbia University, both in New
York, and a past president of the American Academy of Addiction Psychiatry. Dr.
Rosenthal disclosed that he receives research grants from Titan Pharmaceuticals
Inc. and Forest Research Institute.
If we had drugs that would make people smarter, wouldn't that benefit
society? And would using drugs in this way be a bad thing?
The reality is: We do have such drugs. And, more and more, we are hearing
accounts of normal people taking agents to enhance their mental acuity and
alertness at work and in school.
The journal Nature did a survey last year that looked at 1,400 of its
scientist readers from 60 countries (Nature 2008;456:702-5). The survey found
that 20% of them had used cognitive enhancement in the form of modafinil or
methylphenidate or had used beta-blockers to calm them and help them focus when
they had to give presentations. Interestingly, 80% of them were in favor of
being able to obtain the drugs at their own discretion, as opposed to having to
go to a doctor or through the Internet for a prescription.
Cognitive-enhancing drugs give a competitive edge, and in our society the
pressure to succeed is huge. Strikingly, one-third of those responding to the
Nature survey said they would feel obligated to give cognition-enhancing drugs
to their children if the other children in school were taking them.
Some of us may think that the use of such performance-enhancing drugs in
"normal" people is wrong. Others see the practice as cheating. The use of a pill
to make us smarter somehow goes against the Judeo-Christian ethic, which tells
us there is no gain without pain-that gain without pain weakens our character.
But does it automatically follow that taking a drug solely to satisfy a person's
desires is objectionable?
The notion of improving performance using psychopharmacology is not a new
one. The use of alcohol, caffeine, and herbs, as well as pharmaceutical agents,
are examples.
Another is the use of Viagra for erectile dysfunction. Is erectile
dysfunction part of the normal male aging process? Is a lower free testosterone
level because of decreased sex hormone-binding globulin in aging men pathologic?
If erectile dysfunction is tied to normal aging, is it "cheating" to take
Viagra? One purpose of medicine is to improve quality of life in addition to
alleviating suffering. So, if we have the ability to enhance cognition, should
we do it?
In a study of commercial pilots, those who took 5 mg per day of the
cholinesterase inhibitor donezepil (Aricept) for 1 month did better in flight
simulation tests did than their counterparts who took placebo, especially in
emergency situations. Think about that. If you are a passenger, wouldn't you
rather have your pilot on donezepil?
Many people use caffeine for its stimulant properties. Caffeine improves
concentration and increases capacity for information processing in the brain.
Glucose priming also enhances learning and memory, so coffee with sugar is a
powerful combination. Is a sweet espresso an unfair advantage at work? If it
reduces accidents in an industrial setting, why wouldn't you want people to
consume caffeine?
Methylphenidate (Ritalin) improves concentration, working memory, and
attention in people with attention-deficit/hyperactivity disorder. In healthy
adults, it improves executive functioning. It's well known on college campuses
for use as a study aid, but college students may ignore traditional dosing and
snort it at high doses before taking exams or writing papers.
Modafinil (Provigil), approved for narcolepsy and shift-work sleep disorders,
reduces attention deficits attributable to sleep deprivation. In normal adults,
it significantly improves fatigue levels, motivation, vigilance, performance on
digital pattern recognition, memory, and reaction time. Reportedly, modafinil is
the entrepreneur's drug of choice in Silicon Valley. There's a lot of nonmedical
use of modafinil out there, and this begs the question about people using it
this way. Not just people, but also our colleagues.
The pharmaceutical industry is working to develop a drug aimed at inhibiting
memory formation to prevent posttraumatic stress disorder after a traumatic
event. This is primary prevention, and it is a good idea. But what about using
such a drug simply to prevent an unpleasant memory? Is that okay?
How should use of cognitive-enhancing drugs be regulated in healthy people?
Should their use always be monitored by health care professionals? These people
are not patients; they are healthy members of society. Their rationale for using
medication is for self-enhancement, not therapy. But many of these medications
are supposed to be available only by prescription.
We need to do scientific work in this area. There may be evils associated
with such use, such as increased social inequity. But there may also be real
benefits to our society.
I fear that if we do not attempt to answer some of these questions and create
some guidelines, the government will do so. And when the government does it, the
outcome often falls short.
Whatever our views on the matter, society is moving this way. The train has
left the station, and there appears to be no conductor on board. Do we want to
get on and steer, or do we want to stand by and let someone else deal with this
increasingly important issue?
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2009 Elsevier Inc., International Medical News Group
All Rights Reserved
192 of 998 DOCUMENTS
US Fed News
May 12, 2009 Tuesday 11:39 AM EST
Patent No. 7,528,172 Issued on May 5, Assigned to Cooper Health System for
Improving Recovery Method (Pennsylvania Inventors)
LENGTH: 145 words
DATELINE: ALEXANDRIA, Va.
ALEXANDRIA, Va., May 12 -- Ghassem E. Larijani of Villanova, Pa., and Michael E.
Goldberg of Philadelphia, have developed a method for improving recovery after
general anesthesia. The inventors were issued U.S. Patent No. 7,528,172 on May
5.
The patent has been assigned to Cooper Health System Inc., Camden, N.J.
According to the abstract released by the U.S. Patent & Trademark Office:
"Compositions and methods for improving recovery following general anesthesia
are provided. The composition comprises an effective dose of modafinil.
Modafinil has been shown to reduce the symptoms associated with post-operative
general anesthesia, improving the recovery form anesthesia." The original
application was filed on Oct. 2, 2003.For more information about US Fed News
contract awards please contact: Sarabjit Jagirdar, US Fed News, Email:-
htsyndication@hindustantimes.com
LOAD-DATE: May 12, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 HT Media Ltd.
All Rights Reserved
193 of 998 DOCUMENTS
The Sunday Times (London)
May 3, 2009
Edition 1
Essay-enhancing drugs;
More and more students are taking 'smart pills' to help boost their results in
exams - but are they safe, asks Tariq Tahir
BYLINE: Tariq Tahir
SECTION: NEWS REVIEW;FEATURES; Pg. 9
LENGTH: 1004 words
Gemma is a recent Oxford University graduate. As a student of experimental
psychology, she wrote three essays a week, in addition to spending 40 hours in
lectures and labs. At night she worked for the student newspaper.
In her final year things began to pile up but the 22-year-old was reluctant to
drop any of her activities. She started taking Modafinil to make possible a life
that was fast becoming impossible.
Modafinil is a stimulant most commonly prescribed as a prescription drug to
treat sleeping disorders, particularly narcolepsy.
But increasingly this drug, and two other stimulants, Ritalin and Adderall, are
being bought illegally over the internet by high-achieving, overstretched
students in British universities to sharpen their focus, concentration and
memory.
Like many other high-flyers who use so-called "study" or "smart" drugs, Gemma
felt a desire to be on top of her game all the time. Modafinil helped her to
stay awake long enough to complete her assignments.
"I had a few American friends who regularly used Ritalin and sang its praises
but I was suspicious of it," she says. "But my friend bought some Modafinil
online, said it was fantastic and could keep you awake for ever so I bought some
from him.
"Taking Modafinil meant that I could just keep working. It didn't make me any
more gifted but it meant that my day lasted anything up to 36 hours." The other
popular stimulants, Ritalin and Adderall, are legally prescribed for children
who have been given a diagnosis of attention-deficit hyperactivity disorder
(ADHD). But since it has been demonstrated in scientific trials that these drugs
can boost cognitive performance, their unofficial use has rocketed.
Yet, even as students pop the pills and brag about their advantages in chat
rooms, some experts are asking how much damage they are doing to their bodies.
Others are speculating that, if the risks are found to be slight, the use of
such drugs could become the norm for the brightest, most competitive young
people in our society.
Like many users Gemma soon discovered the downsides. She describes feeling
shaky, although "this might just have been me not going to sleep. I didn't feel
tired and I didn't feel hungry. It stopped my body clock. I lost all track of
time and whether I was meant to be eating or not. I would have long bursts of
concentration".
More worryingly, she also experienced bouts of obsession. "One night I made 10
Facebook photo albums for no good reason other than the fact that I was set on
doing it," she says.
Tackling the problem is difficult. Figures that reveal who is taking what are
not readily available. Last year the scientific journal Nature published the
results of an online survey of 1,400 adults. It showed that 20% of readers had
taken "smart drugs", but no definitive figures exist on the extent of their use
in British universities.
Research at the University of Michigan in the United States reveals that 8% of
American undergraduates have used such drugs at one time or another to improve
alertness. Other studies suggest the figure could be as high as one in six.
Emmanuel Akpan-Inwang, a student union welfare officer at the London School of
Economics, says that as students approach their exams at the end of the year
many are experimenting with "anything that will enhance their performance.
"Adderall is the most popular drug at the moment," he reveals.
Such people include Claire, a 22-yearold final-year Cambridge University
philosophy student. She opted to try Adderall, a drug that is composed of mixed
amphetamine salts, in the run-up to her second-year exams last year. She had no
difficulty getting hold of it.
"I was sitting around in our college rooms with friends and someone mentioned
that the engineering students had this drug that they used to help them study,"
she says. "A friend who was in the year above had a lot of it, which he had
bought on the internet, and so he gave me some." She took a capsule the next day
before going to the library and was delighted to sail through a highly
productive session of study. "I really found my concentration levels went up,"
she says. "I thought, oh wow, I've been sitting in the library for five hours
and haven't been distracted by people walking around like I usually am.
It was very helpful." With her finals coming up in a few weeks, she is planning
to use Adderall again to keep her concentration at peak levels. Nor are the
prices prohibitive: Ritalin costs £290 for 150 10mg pills, Adderall £230 for 120
30mg capsules and Modafinil £75 for 100 200mg doses.
Information on the risks of such drugs is highly anecdotal. Users report side
effects such as headaches and depression, but no definitive research has been
done on the long-term effects of their use on healthy people. This in itself is
worrying many, including Barbara Sahakian, professor of neuropsychology at
Cambridge University. Sahakian first became interested in the drugs when,
arriving jet lagged at a conference in the United States, she was offered
Modafinil. After speaking to her colleagues she discovered the extent to which
it, and other similar drugs, were in circulation, both among her academic peers
and their students.
In a paper entitled Professor's Little Helper, she spelt out her concerns. "The
trouble is that people in the UK are getting these drugs off the internet," she
says.
"That's worrying, because you are not really sure what you are getting. And even
if the drug is pure, you may have another medical condition that means you
shouldn't take it. A person having a bad reaction to one of these drugs is, I
think, a horrible accident waiting to happen." For other academics, such as John
Harris, professor of bioethics at Manchester University, it is only a matter of
time before smart pills are available, without prescription, on the high street.
"If these drugs are shown to be safe, I can see a time when bright, competitive
people will be able to access them as easily as you can get the morning-after
pill now," he says.
Some names have been changed
LOAD-DATE: May 4, 2009
LANGUAGE: ENGLISH
GRAPHIC: Students take the drugs to avoid feeling drowsy
TETRA IMAGES
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: STS
Copyright 2009 Times Newspapers Limited
All Rights Reserved
194 of 998 DOCUMENTS
The Sunday Times (London)
May 3, 2009
Edition 1
Drugs to write essays by;
More and more students are taking 'smart pills' to help boost their results in
exams - but are they safe, asks Tariq Tahir
BYLINE: Tariq Tahir
SECTION: ECOSSE;FEATURES; Pg. 12
LENGTH: 963 words
Gemma is a recent Oxford University graduate. As a student of experimental
psychology, she wrote three essays a week, in addition to spending 40 hours in
lectures and labs. At night she worked for the student newspaper. In her final
year, things began to pile up, but the 22-year-old was reluctant to drop any of
her activities. She started taking Modafinil to make possible a life that was
fast becoming impossible.
Modafinil is a stimulant most commonly prescribed to treat sleeping disorders.
But increasingly this drug, and two other stimulants, Ritalin and Adderall, are
being bought illegally over the internet by highachieving, overstretched
students in British and American universities to sharpen their focus,
concentration and memory.
Like many other high-flyers who use study drugs, Gemma felt a desire to be on
top of her game all the time. For her, Modafinil helped her stay awake long
enough to complete her assignments.
"I had a few American friends who regularly used Ritalin and sang its praises
but I was suspicious of it," she reveals. "But my friend bought some Modafinil
online, said it was fantastic and could keep you awake forever so I bought some
from him.
"Taking Modafinil meant that I could just keep working. It didn't make me any
more gifted but it meant that my working day lasted anything up to 36 hours."
The other popular stimulants, Ritalin and Adderall, are legally prescribed for
children who have been given a diagnosis of attention-deficit hyperactivity
disorder (ADHD). But since it has been demonstrated in scientific trials that
these "study" or "smart" drugs, as they have now become known, can boost
cognitive performance, their unofficial use for non-medical purposes has
rocketed.
So as students pop the pills, and brag about their advantages in chat rooms,
some experts are asking how much damage they are doing to their bodies. Others
are speculating that, if the risks are found to be slight, the use of such drugs
could become the norm for the brightest, most competitive young people in our
society.
Like many users, Gemma soon discovered the downsides. She describes feeling
shaky, although "this might just have been me not going to sleep. I just didn't
feel tired and I didn't feel hungry. It stopped my body clock. I lost all track
of time and whether I was meant to be eating or not. I would have long bursts of
concentration." More worryingly, she also experienced bouts of obsession. "One
night I made 10 Facebook photo albums for no good reason other than the fact
that I was set on doing it," she says.
Tackling the problem is, however, difficult.
Figures that reveal who is taking what are not readily available. Last year the
scientific journal Nature published the results of an online survey of 1,400
adults that revealed that 20% of readers had taken smart drugs to sharpen their
concentration or memory, but no definitive figures exist on the extent of smart
drug use in British universities. Research at the University of Michigan reveals
that 8% of American undergraduates have used such drugs at one time or another
to improve alertness. Other studies suggest the figure could be as high as one
in six..
Emmanuel Akpan-Inwang, a student union welfare officer at the London School of
Economics, is only too aware of the level of use as students approach their
exams at the end of the year. "Adderall is the most popular one at the moment,"
he reveals.
"Most people will do anything they can to enhance their performance during the
exam period." People such as Claire, a 22-year-old final-year Cambridge
University philosophy student. She opted to experiment with Adderall, a drug
that is composed of mixed amphetamine salts, in the run-up to her second-year
exams last year. She had no difficulty getting hold of it.
"I was sitting around in our college rooms with friends, talking about our
exams, and someone mentioned that the engineering students had this drug that
they used to help them study," she says.
"A friend who was in the year above had a lot of it, which he had bought on the
internet, and so he gave me some." She took some the next day before going to
the library and was delighted to sail through a highly productive session of
study. With her finals coming up in a few weeks, she's planning to use it again
to keep her concentration at peak levels.
Information on the risks of such drugs is equally anecdotal. Users report side
effects such as headaches and depression, but no definitive research has been
done on the long-term effects of their use on healthy people.
This in itself is worrying many, such as Barbara Sahakian, professor of
neuropsychology at Cambridge University. She first became interested in the
drugs when, arriving jet lagged at a conference in America, she was offered
Modafinil. After speaking to her colleagues she discovered the extent to which
Modafinil, and other similar drugs, were in circulation among her academic
colleagues and their students.
In a paper entitled Professor's Little Helper, she spelt out her concerns. "The
trouble is that people in the UK are getting these drugs off the internet," she
says.
"That's worrying, because you are not really sure what you are getting. And even
if the drug is pure, you may have another medical condition that means you
shouldn't take it. A person having a bad reaction to one of these drugs is, I
think, a horrible accident waiting to happen." For other academics, however,
such as John Harris, professor of bioethics at Manchester University, it is only
a matter of time before smart pills are available on the high street. "If these
drugs are shown to be safe, I can see a time when bright, competitive people
will be able to access them as easily as you can get the morning-after pill
now," he says.
Some names have been changed
LOAD-DATE: May 4, 2009
LANGUAGE: ENGLISH
GRAPHIC: Students take the drugs to avoid feeling drowsy
TETRA IMAGES
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: STS
Copyright 2009 Times Newspapers Limited
All Rights Reserved
195 of 998 DOCUMENTS
Clinical Psychiatry News
May 2009
Modafinil's Mechanism of Action Raises Abuse Risk
BYLINE: Mary Ann Moon
SECTION: Pg. 18 Vol. 37 No. 5 ISSN: 0270-6644
LENGTH: 213 words
The wake-promoting drug modafinil raises dopamine levels in the brain, data
from a pilot study of 10 men show.
Until now, modafinil's mechanism of action has been uncertain, and it was
thought to involve several other central nervous system substances but not
dopamine. That hypothesis must now be reconsidered, said Dr. Nora D. Volkow of
the National Institute on Drug Abuse, Bethesda, Md., and her associates.
More important, the drug's effect on dopamine means that it has a heightened
potential for abuse. Given its growing popularity for a variety of uses,
clinicians and patients alike must be made aware of the increased risk of
addiction, the investigators noted.
The study subjects, who were aged 23-46 years, were given the 200-mg dose
that is recommended to treat narcolepsy as well as the 400-mg dose that is
thought to be beneficial for attention-deficit/hyperactivity disorder, at
different times. They then underwent positron-emission tomography with different
radiotracers to measure the effects on extracellular dopamine and dopamine
transporters in the brain (JAMA 2009;301:1148-54).
Modafinil was found to increase dopamine in the brain by blocking dopamine
transporters, Dr. Volkow and her colleagues said
The investigators had no conflicts.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2009 Elsevier Inc., International Medical News Group
All Rights Reserved
196 of 998 DOCUMENTS
Clinical Oncology Alert
May 1, 2009
Pharmacology Watch
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
Pharmacology Watch
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
197 of 998 DOCUMENTS
Critical Care Alert
May 1, 2009
Pharmacology Watch: FDA Warning: Pharmaceuticals in "Natural" Products
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Pharmacology Watch
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
198 of 998 DOCUMENTS
Emergency Medicine Reports
May 1, 2009
Modafinil's abuse potential
LENGTH: 213 words
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
199 of 998 DOCUMENTS
Infectious Disease Alert
May 1, 2009
Pharmacology Watch: FDA Warning: Pharmaceuticals in "Natural" Products
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
Pharmacology Watch
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
200 of 998 DOCUMENTS
Neurology Alert
May 1, 2009
Pharmacology Watch
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
Pharmacology Watch
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
201 of 998 DOCUMENTS
OB/GYN Clinical Alert
May 1, 2009
Pharmacology Watch: FDA Warning: Pharmaceuticals in
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
Pharmacology Watch
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
202 of 998 DOCUMENTS
Primary Care Reports
May 1, 2009
Pharmacology Watch
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Pharmacology Watch
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
203 of 998 DOCUMENTS
Travel Medicine Advisor
May 1, 2009
Pharmacology Watch: FDA Warning: Pharmaceuticals in "Natural" Products
LENGTH: 1371 words
FDA Warning: Pharmaceuticals in "Natural" Products
In this issue: Aspirin dose and cardioprotection; uncovering modafinil's abuse
potential; proton-pump inhibitors and clopidogrel; FDA actions.
Finding pharmaceuticals in natural products
Some natural products are not so "natural" after all. The FDA has warned
consumers for several months that a number of weight-loss products contain
undeclared pharmaceutical ingredients. The newest products to join the list are
Herbal Xenicol which contains cetilistat (a drug similar to orlistat that is not
approved in this country), as well as Slimbionic and Xsvelten, both of which
contain sibutramine (the prescription medication also known as Meridia®). The
FDA's list of over-the-counter weight-loss agents that contain undeclared active
pharmaceutical ingredients now includes 72 products. Some of the other
undeclared pharmaceutical ingredients found in these products include
fenproporex (an amphetamine derivative no longer available in this country),
fluoxetine (Prozac®, an SSRI), furosemide (Lasix®, a loop diuretic), and even
phenytoin (Dilantin®, an antiseizure medication). The FDA is seeking recalls on
many of these products; however, some are available only on-line and previous
recall efforts have proved inadequate.
Pharmacology Watch
In a related story, the FDA has announced a voluntary recall of Zencore Plus,
the heavily marketed product for "natural male enhancement," which has been
found to contain benzamidenafil, a new PDE5 inhibitor not yet available in this
country. Benzamidenafil is similar in action to sildenafil (Viagra®) and
tadalafil (Cialis®). PDE5 inhibitors are noted to have a drug interaction with
nitrates, leading to potential life-threatening risk of sudden and profound drop
in blood pressure. Zencore Plus is distributed by Hi-Tech Pharmaceuticals in
Norcross, GA, and is widely sold in health food stores, by mail order, and by
Internet sales.
Aspirin dose and cardioprotection
What is the best dose of aspirin for patients taking dual therapy with
clopidogrel to prevent cardiovascular events? Investigators looked at 15,595
patients with cardiovascular disease or multiple risk factors in an
observational analysis from a double-blind, placebo-controlled randomized trial.
Patients were randomized to doses of aspirin less than 100 mg (75 mg or 81 mg),
100 mg, or greater than 100 mg (150 mg or 162 mg) with or without clopidogrel.
The primary efficacy outcome was the composite of myocardial infarction, stroke,
or cardiovascular death and the primary safety endpoint was severe
life-threatening bleeding. In patients given aspirin alone, the hazard ratio for
the efficacy and safety endpoints were the same regardless of aspirin dose. In
patients given aspirin with clopidogrel, there was a statistically
nonsignificant associated reduction in efficacy with aspirin doses over 100 mg,
and a significantly higher increase in harm (hazard ratio, 1.30 with clopidogrel
plus aspirin greater than 100 mg). The authors conclude that daily doses of
aspirin greater than 100 mg were not associated with benefit and may be
associated with harm in patients also taking clopidogrel. Therefore, daily doses
of aspirin 75-81 mg optimize efficacy and safety in patients requiring long-term
aspirin therapy, especially in patients receiving dual antiplatelet therapy (Ann
Intern Med 2009;150:379-386). This is especially important given the recent U.S.
Preventive Services Task Force recommendation that encourages men ages 45-79
years to take aspirin preventively when the potential benefit of a reduction of
myocardial infarction outweighs the potential harm of an increase in
gastrointestinal hemorrhage. Women ages 55-79 years are also encouraged to use
aspirin when the potential benefit of a reduction in ischemic stroke outweighs
the potential harm of increased gastrointestinal hemorrhage (Ann Intern Med
2009;150:396-404).
PPIs and clopidogrel
Increasing evidence suggests that proton pump inhibitors (PPIs) may attenuate
the effect of clopidogrel on platelet aggregation. PPIs are often used
prophylactically in patients with acute coronary syndrome (ACS), as patients on
clopidogrel and aspirin may be at higher risk for GI bleeding. A new study from
VA researchers was set up to determine if there are clinical implications from
the interaction between PPIs and clopidogrel.
In a retrospective cohort study of 8205 patients with ACS taking clopidogrel,
63.9% were also prescribed a PPI at discharge, during follow-up, or both. Death
or rehospitalization for ACS occurred in 20.8% of patients taking clopidogrel
without a PPI and 29.8% patients taking clopidogrel with a PPI. Use of
clopidogrel plus a PPI was associated with an increased risk of death or
rehospitalization for ACS compared with use of clopidogrel without a PPI
(adjusted odds ratio, 1.25; 95% confidence interval, 1.11-1.41). Patients taking
a combination of the two drugs were at higher risk for hospitalizations for ACS
and revascularization procedures, but not for all-cause mortality. Patients
taking a PPI without clopidogrel were not at higher risk for rehospitalization.
The authors conclude that concomitant use of clopidogrel and a PPI after
hospital discharge for ACS is associated with an increase risk of adverse
outcomes, suggesting that PPIs may attenuate the benefits of clopidogrel, and
that PPIs should only be used with clopidogrel if there is a clear indication,
and not for routine prophylaxis (JAMA 2009;301:937-944).
Modafinil's abuse potential
Modafinil (Provigil®) is a wake-promoting medication used to treat narcolepsy
and other sleep disorders. Recently, the drug has be used off-label to enhance
cognition in psychiatric patients and even in healthy patients seeking a memory
boost. Modafinil has been touted as having a low abuse potential; however, a new
study questions that assumption. Most stimulant medications, such as
methylphenidate and amphetamine, increase brain dopamine levels. Modafinil was
thought to exert its effect in the brain on pathways other than dopamine, but
now there is evidence that dopamine is involved. Researchers from the National
Institute on Drug Abuse looked at 10 healthy male volunteers to measure the
effects of modafinil at therapeutic dosing of 200 mg and 400 mg given orally.
PET scans were used to measure the effect of modafinil on extracellular dopamine
and dopamine transporters. Modafinil increased extracellular dopamine and showed
evidence of occupancy of dopamine transporters, effects similar to drugs with
the potential for abuse. The authors conclude that, considering the increasing
use of modafinil, there needs to be heightened awareness for potential abuse of
and dependence on modafinil in vulnerable populations (JAMA 2009;301:1148-1154).
FDA Actions
The FDA is requiring the manufacturers of metoclopramide (Reglan®) include a
boxed warning on their labeling regarding the risk of long-term or high-dose use
and tardive dyskinesia. Manufacturers will also be required to implement a risk
evaluation and medication strategy (REMS) to ensure patients are provided with a
medication guide that discusses the risk. Metoclopramide is approved for the
treatment of gastric motility problems associated with GERD, diabetic
gastroparesis, and nausea and vomiting.
A new proton pump inhibitor has been approved by the FDA, bringing the number of
PPIs on the market to six. Dexlansoprazole is the purified active isomer of
lansoprazole (Pepcid®). The drug has a delayed-release formulation designed to
provide two separate releases of the medication. It is approved for the
treatment of GERD and erosive esophagitis. Takeda Pharmaceuticals will market
dexlansoprazole as Kapidex[TM].
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5468. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2009 AHC Media LLC
All Rights Reserved
204 of 998 DOCUMENTS
Pharmacy News (Australia)
April 1, 2009
Sleep disorder drug open to abuse
BYLINE: Mark Gertskis
SECTION:
LENGTH: 336 words
A DRUG used to treat sleeping disorders and boost cognitive functions has the
potential to be abused as an addictive stimulant.
A new study in the Journal of the American Medical Association (JAMA) has
revealed that modafinil, marketed as Modavigil in Australia, has the potential
to be addictive due to its effect on levels of the dopamine hormone.
"Modafinil blocked dopamine transporters and increased dopamine in the human
brain (including the nucleus accumbens)," the study's authors wrote.
"Because drugs that increase dopamine in the nucleus accumbens have the
potential for abuse, and considering the increasing use of modafinil, these
results highlight the need for heightened awareness for potential abuse of and
dependence on modafinil in vulnerable populations."
Modafinil is designed to improve daytime wakefulness in people suffering from
narcolepsy, sleep apnoea and shift work sleep disorder.
The study's authors noted that it is also being increasingly used as a cognitive
enhancer for conditions such as attention deficit hyperactivity disorder.
"Although initially launched as distinct from stimulants that increase
extracellular dopamine by targeting dopamine transporters, recent preclinical
studies suggest otherwise," the authors wrote.
Modafinil consumer medicine information states, however, that the drug differs
from other stimulants because it does not "overstimulate or produce a 'high'
feeling".
The drug's US manufacturer, Cephalon, said JAMA's findings were consistent with
what was already known about modafinil, marketed as Provigil in the US.
"We believe that there is a low relative potential for abuse with modafinil," a
Cephalon statement said.
"It has some potential for abuse and dependence.
"It is important to note that the product label for Provigil advises physicians
to follow patients closely, especially those with a history of drug and/or
stimulant (e.g. methylphenidate, amphetamine or cocaine) abuse and to observe
patients for signs of misuse or abuse or drug-seeking behavior."
LOAD-DATE: June 24, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
JOURNAL-CODE: PN
Copyright 2009 Reed Business Information Ltd.
All Rights Reserved
205 of 998 DOCUMENTS
M2 PressWIRE
March 30, 2009 Monday
visiongain: Visiongain is proud to announce the release of the brand new report
"Sleep Disorders: Market Analysis 2008-2018"
LENGTH: 1035 words
the release of the brand new report "Sleep Disorders: Market Analysis
2008-2018"
More than 80 sleep disorders have been identified. They affect over 200
million people worldwide. The report focuses on the market for
following sleep disorders:
* Insomnia
* Restless legs syndrome (RLS)
* Narcolepsy and
* Obstructive Sleep Apnoea / Hypopnea Syndrome (OSAHS)
The market penetration for insomnia drugs has not reached saturation
point. Opportunities remain. But with the introduction of several new
products the market is set to see changes, but expansion. This
expansion is based on increased general awareness physicians better
comprehension of the significance of this disease and the positive role
that a sleep medication prescription plays.
At present time there are several prescription sleeping medications
available to treat insomnia. The market-focus has been driven by the
production of sleep medications with less side-effects and danger of
overdose. Prescription benzodiazepines and newer non-benzodiazepine
hypnotics developed in the 1990s, such as Imovane, Ambien and Sonata
will continue to be the most prescribed. Benzodiazepines are widely
used to treat an underlying neurological disorder which is often the
underlying cause of insomnia, e.g. anxiety and depression.
Visiongain predicts that market share by volume for insomnia in the US
will change significantly from 2008 to 2018. Ambien IR lost its patent
protection in April 2007, which opened to generic competition for
Zolpidem. Ambien will remain the market leader for the short term, but
what will over take it? A generic version of Ambien is expected to
achieve strong market share by volume as there is a great demand for
zolpidem tartrate for insomnia.
The market share for insomnia treatment will gradually rise after 2012,
which will be due to:
* Market expansion of existing expensive medications into Europe and
Japan in particular
* Market penetration of new medications currently in pipeline.
Other drugs dealt with in this report include:
* Modafinil (Provigil) is the first in a new class of wake-promoting
drugs and is currently approved in more than 20 countries for the
treatment of excessive daytime sleepiness associated with narcolepsy.
* Provigil is quickly replacing Ritalin, and other CNS stimulants, as
the medication of choice for treating daytime sleepiness in narcolepsy.
The FDA granted modafinil (Provigil) orphan drug status in 1993.
* Modafinil was initially launched in the US in 1999 for the treatment
of narcolepsy. In 2004, modafinil became FDA-approved prescription
medicine for the treatment of excessive sleepiness associated with
Obstructive Sleep Apnoea/Hypopnea Syndrome (OSAHS) and Shift Workers
Sleep Disorder (SWSD).
* Requip (ropinirole) became the first and only FDA-approved drug
treatment for moderate to severe primary Restless Legs Syndrome (RLS)
in 2005.
Key findings that will broaden the scope of the sleep disorders market:
* Over the next decade, the development and improvement of sleep
disorders therapies will primarily depend on the success of burgeoning
technology and innovative approaches.
* It is possible to purchase prescription medications online without
producing a prescription. Purchase of online sleep medications has
increased and will continue to evolve over the next years.
* The impact of DTC advertising has created an improved awareness of
available insomnia treatment.
* This is likely to increase as DTC advertising continues to prosper
and the culture becomes more accepting towards insomnia treatment.
Visiongain expects the market for sleep disorders to increase, driven
by a growing awareness of sleep disorders and by campaigns to promote
sleep medications, both by DTC advertising and consumer education. The
relaxation of DTC marketing restrictions in the 1990s in the US set the
stage for a flow for both branded and unbranded advertising and
promotional programmes. Those regulations are prompting more
responsible DTC advertising on the industry's part.
* The FDA has requested that all manufacturers of sedative-hypnotic
drug products, a class of drugs used to induce and/or maintain sleep,
strengthen their product labelling to include stronger warnings
concerning potential risks.
* The Committee for Medicinal Products in Human Use (CHMP) of the
European Medicines Agency (EMEA) approved Neurim's Circadin a
prolonged-release melatonin as monotherapy for the short-term treatment
of primary insomnia characterised by poor quality of sleep in patients
aged 55 or over. Neurim is actively seeking strategic alliances for the
major European markets.
What questions does the report answer?
* Which current or future therapies will drive the sleep disorders
market from 2008 to 2018?
* The key companies involved in the market and their analysis?
* What is the patient identification rate for each of the therapeutic
areas?
* What is the present state of the disease awareness?
* What R&D opportunities exist for 'new comers'?
Why should you buy this report?
* This report focuses on the marketed medications and the pipeline
development for sleep disorders from 2008 to 2018. It also discusses
the strength and weakness of products, along with the opportunities and
threats facing the market.
* The report describes world market situation for sleep disorders,
namely insomnia, narcolepsy, RLS and OSAHS, with forecasts made for all
key products. It also describes the insomnia market situation in the
seven major world markets for sleep medications: the US, Japan, France,
Germany, Italy, Spain and the UK, with forecasts for key products.
* The report provides transcripts of visiongain's interviews with
experts in the field of sleep disorders, which reviews the future
direction of the sleep disorders treatment market.
Visiongain ltd.
Report.aspx?rid=274 Or http://www.visiongain.com
CONTACT: Suvitha Damodaran, Visiongain ltd
e-mail: suvitha.damodaran@visiongainglobal.com
e-mail: info@visiongainglobal.com
Tel: +44 (0)20 7549 9946
Tel: +44 (0)20 7336 6100
Fax: +44 (0) 20 7549 9930
WWW: http://www.visiongain.com
((M2 Communications Ltd disclaims all liability for information
provided within
Further information on
http://www.presswire.net on the world wide web. Inquiries to
info@m2.com)).
LOAD-DATE: April 4, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
JOURNAL-CODE: M2P
Copyright 2009 M2 PressWIRE
All Rights Reserved
206 of 998 DOCUMENTS
Flesh and Stone
March 24, 2009 Tuesday 12:52 PM EST
Neuro Scans
LENGTH: 958 words
Mar. 24, 2009 (Flesh and Stone delivered by Newstex) --
Stem cell ban lifted but researchers must remain vigilant to protect scientific
integrity
Earlier this month, President Obama through executive order lifted the ban on
federal funding for embryonic stem cell research.
The ban put in place by President Bush in 2001 limited research funding to
approximately two dozen existing embryonic stem cells lines. The ban was viewed
as politically motivated by many researchers and the public which overwhelmingly
favored increased research that might lead to cures for diabetes, Alzheimers,
Parkinsons, spinal cord injuries, and other neurological disorders. Some
researchers insist America has lost almost a decade of research time that could
have resulted in medical advancements. A possible silver lining to the ban is
that many researchers developed new partnerships with colleagues in foreign
institutions in order to continue their research.
With the lifting of the ban, hundreds of lines developed since 2001 will be
eligible for federal funding. Obama science advisor Harold Varmus, president of
Memorial Sloan-Kettering Cancer Center in New York and former head of the
National Institutes of Health, recently co-authored an editorial in Science on
Obama's stem cell research and scientific integrity policies (registration
required). In the editorial Varmus encourages scientists to stay involved in
policy discussions because preserving scientific integrity in a highly
politicized environment will require vigilance.
When lifting the ban, Obama also pledged through a memorandum to appoint only
credentialed experts to federal positions that involve evaluating scientific
information.
Wakefulness drug modafinil may be addictive
Modafinil (Provigil), approved by the FDA for the treatment of narcolepsy, has
also come into wider use as a cognitive performance enhancer as it was generally
believed to be a safer alternative to amphetamines. A recent study by NIH and
collaborating institutions published in JAMA, however, found that the drug
blocked dopamine transporters and increased dopamine in the brain. These changes
in the brains pleasure center could lead to dependence and abuse, say
researchers.
Using positron emission tomography (PET), researchers measured the effects of
200 mg and 400 mg, common therapeutic dosages given in pill form, on
extracellular dopamine and on dopamine transporters in 10 healthy male brains.
The study is preliminary, given such a small sample, but the findings warrant
further study, especially since modafinil has been approved for use by the U.S.
military beginning in 2003.
Approved initially for certain Air Force personnel, returning Army and National
Guard soldiers have said the drug is readily available to those in combat
situations, and clinicians have concerns that returning soldiers may have
developed a dependency on the drug. The drug is also increasing in popularity
among college students and others who say the drug improves performance,
enhances mood and allows better concentration.
Citation:
JAMA. 2009;301(11):1148-1154.
Closer to a consensus on when brain death occurs?
The medical community, particularly neurologists, have been grappling with the
definition of brain death and striving to reach a consensus on when brain death
occurs for decades. JAMA first published a landmark article that quantitatively
defined the clinical and laboratory criteria used to measure the presence of
brain death in 1968. But different protocols at different institutions left
openings for disagreements and legal entanglements.
The work took on new urgency in 2005 when the Terry Schiavo case became a
national political wedge issue. Not limited to medical experts and ethicists,
the case galvanized religious activists, conservative politicians, and
celebrities who grandstanded before an eager media.
Adding to the high drama, President Bush made a midnight flight from his ranch
in Crawford, Texas, to Washington, DC, to sign a law passed by an emotionally
charged Congress that forced doctors to re-insert the feeding tube that had kept
Schiavo alive in a vegetative state for 15 years. After all Congressional and
legal maneuvers were exhausted, Florida judge George Greer ruled that Schiavo
could be removed from life support as her legal guardian had requested for seven
years. Schiavo died from dehydration on March 30, 2005.
After intense study, an ad hoc committee of experts from Harvard Medical School
has just issued a new definition on when brain death occurs: Consciousness,
Coma, and Brain Death"2009, A Definition of Irreversible Coma: Report of the Ad
Hoc Committee of the Harvard Medical School to Examine the Definition of Brain
Death. Will it be the final word?
Left: CAT scan of normal brain. Right: Terri Schiavo's 2002 CAT scan provided by
Ronald E. Cranford, MD, then assistant chief of neurology at the Hennepin County
Medical Center, Minneapolis. (The image is fair use, since the doctor released
his image to the public.)
Wrapping it up with a bow tie workshop
The American Academy of Neurology, known for hosting an intense dawn to dusk
(and beyond) annual meeting, is gearing up for its 61st in Seattle, April 25-May
2.
While the conference attendees work hard, they also know how to have competitive
fun at the wildly popular NeuroBowl quiz show and Neuro Idol talent show. The
organization does, on occasion, poke a little fun at itself.
This year the AAN is hosting a oebow-tying booth at the meeting in honor of the
bowtie which, along with pale blue blazers, is ubiquitous among neurologists.
Ill be attending the meeting and filing stories for some free lance clients and
doing some news blogging from the meeting here on Flesh & Stone.
Newstex ID: FLST-0001-33400535
LOAD-DATE: March 24, 2009
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not necessarily
the views of Newstex or its re-distributors. Posts from such authors are
provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs on Demand® are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs on Demand® is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs on Demand® shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs on Demand®. Reader's comments reflect their
individual opinion and their publication within Blogs on Demand® shall not infer
or connote an endorsement by Newstex or its re-distributors of such reader's
comments or views. Newstex and its re-distributors expressly reserve the right
to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2009 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2009 Flesh and Stone
207 of 998 DOCUMENTS
The Times & Transcript (New Brunswick)
March 23, 2009 Monday
'Smart drug' may be addictive; Study suggests Provigil may be habit- forming
SECTION: LIFE; Pg. D2
LENGTH: 339 words
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure centre, very much like potentially habit-
forming classic stimulants. Modafinil, the drug's generic name, is sometimes
used as an illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side-effects."
The study, appearing in the Journal of the American Medical Association, may
bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and it sales topped $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an air force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
LOAD-DATE: March 23, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 CanWest Interactive, a division of CanWest MediaWorks
Publications Inc.
All Rights Reserved
208 of 998 DOCUMENTS
The Philadelphia Inquirer
March 18, 2009 Wednesday
CITY-D Edition
Study says Provigil may be addictive;
It affected the brain just as other addictive drugs did, the research found.
BYLINE: By Miriam Hill; Inquirer Staff Writer
SECTION: BUSINESS; P-com Biz; Pg. C01
LENGTH: 619 words
Smart drugs may not be so smart after all.
A new federal government study steps up concerns that Cephalon Inc.'s
top-selling drug, Provigil, is addictive.
The research arrives amid reports that college students and some professionals
increasingly pop Provigil, Adderal and Ritalin to improve focus and stay awake.
Many people now call these pills "brain boosters" or "smart drugs."
The findings, published yesterday in the Journal of the American Medical
Association, found that taking Provigil caused changes in the pleasure centers
of the brains of 10 men.
The changes resembled those caused by other addictive drugs, such as
amphetamines, said Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist.
Cephalon is based in Frazer.
A recent article in the journal Nature said people without medical problems
should be able to use these drugs to work harder and longer.
"The Nature article was cavalier, equating it to dangers of drinking coffee, and
that was incorrect," she said. "The implication that these drugs are safe, I
think, is very misleading."
Provigil is approved to treat excessive drowsiness associated with narcolepsy,
obstructive sleep apnea, and shift-work sleep disorder.
University of Pennsylvania brain scientist Martha Farah co-authored the Nature
paper. Yesterday, she told the Associated Press that the new study "goes to show
that we need a little caution and a little humility when we're messing around
with our brain chemistry."
She added that "even now, after all the years that [Provigil] has been on the
market, we are still learning things about it that are relevant to its safety."
The Provigil label has included information about the risk of abuse and
addiction since the U.S. Food and Drug Administration approved the drug in 1998,
Cephalon's chief scientific officer Jeffry Vaught said. He said the company
agreed with Volkow that doctors should not prescribe Provigil to healthy people.
Provigil's U.S. sales totaled $943 million last year, according to data provider
IMS Health. Analysts have estimated that 80 percent of Provigil prescriptions
are for "off-label" treatment of sleepiness and fatigue from illnesses such as
depression, Parkinson's disease and multiple sclerosis.
The company is developing a longer-acting version of the drug, called Nuvigil.
Yesterday, Cephalon shares jumped 9.3 percent, to close at $69.06 each, after
the company reported that Nuvigil met key study goals in a Phase II clinical
trial involving adults with bipolar disorder.
Volkow and her group studied 10 men 23 to 46 years old. They received either a
dummy pill or modafinil - the generic name for Provigil. PET scans showed higher
levels of dopamine among those who took modafinil.
Modafinil also increased dopamine in the nucleus accumbens, a part of the brain
believed to be involved with addiction.
Volkow said her research was the first evidence that Provigil affects dopamine
transporters in human brains. Although the study was small, Volkow said the
clear correlation between Provigil and dopamine levels in the scans was good
evidence.
Earlier research had showed the same results in mice and monkeys.
In a September agreement with the Philadelphia office of the U.S. Attorney,
Cephalon said it would pay $425 million to settle criminal and civil charges
that it illegally marketed three of its drugs, including Provigil, for so-called
off-label uses.
Doctors can prescribe a drug for any use, but drug companies can market them
only for uses approved by the U.S. Food and Drug Administration. Marketing them
for other purposes is known as "off-label."
Contact staff writer Miriam Hill at 215-854-5520 or hillmb@phillynews.com.
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 Philadelphia Newspapers, LLC
All Rights Reserved
209 of 998 DOCUMENTS
Reuters Health Medical News
March 18, 2009 Wednesday 9:00 PM EST
Modafinil has addictive potential in vulnerable populations
SECTION: CLINICAL
LENGTH: 273 words
DATELINE: NEW YORK
Modafinil, a wake-promoting drug initially used to treat narcolepsy, increases
extracellular dopamine -- an effect that increases the drug's potential for
abuse -- results of a pilot study indicate.
"The growing use of modafinil in clinical medicine and as a cognitive enhancing
agent and the uncertainties surrounding the mechanisms underlying its
pharmacological effects highlight the need to better understand its mechanisms
of action," the research team explains in the Journal of the American Medical
Association for March 18.
Led by Dr. Nora D. Volkow at the National Institute on Drug Abuse in Bethesda,
Maryland, the investigators measured the effects of modafinil in 10 healthy men.
Positron emission tomography was used to compare the effects of modafinil
(therapeutic doses of 200 mg or 400 mg) versus placebo on extracellular dopamine
and on dopamine transporters.
Results showed that modafinil produces elevations in brain dopamine through
blockade of dopamine transporters similar in magnitude to those produced by
methylphenidate, which is used to treat attention deficit/hyperactivity
disorder.
"The dopamine-enhancing effects of modafinil in the nucleus accumbens may help
explain reports of its abuse, since this pharmacological effect is considered
crucial for drug reinforcement," Dr. Volkow and colleagues write.
Despite the fact that "modafinil is much less potent as a reinforcer than
stimulant drugs, and reports of modafinil abuse are rare and much less frequent
than those for stimulant drugs," the team warns that "risk for addiction in
vulnerable persons merits heightened awareness."
SOURCE: JAMA 2009;301:1148-1154.
LOAD-DATE: March 19, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Reuters Health
All Rights Reserved
210 of 998 DOCUMENTS
St. Louis Post-Dispatch (Missouri)
March 18, 2009 Wednesday
THIRD EDITION
MEDICAL DIGEST
BYLINE: FROM NEWS SERVICES
SECTION: NEWS; Pg. A2
LENGTH: 372 words
DATELINE: 0
Study questions safety of Modafinil
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in today's Journal of the American Medical Association, may
bust the myth that the drug is safe for healthy people, experts said.
'Observation stay' being questioned
Hospitals are using a little-known category of medical care called the
"observation stay" more than ever, and patients are reporting that they weren't
aware that many standard hospital services are not covered by insurance when a
patient is admitted on this basis.
Paula Biever filed a complaint with Medicare and the Minnesota attorney
general's office when her father, 79, was billed $17,820 over an observation
stay.
Experts say hospitals are turning to "observation stays" when they believe a
patient is too sick to go home but not sick enough to meet guidelines for
admittance. Medicare officials said observation care is supposed to be for a
day, but that longer stays are happening. Medicare is looking into it.
Briefly
- Obesity problems: Being obese can take years off your life and in some cases
may be as dangerous as smoking, according to a study being published today in
the medical journal Lancet that was paid for by Britain's Medical Research
Council, the British Heart Foundation, Cancer Research UK and others.
- Brain waves: Brain waves generated when trying to hear were sharply reduced in
people with schizophrenia, suggesting a connection, according to a study by
researchers at Harvard-affiliated McLean Hospital published in the Schizophrenia
Bulletin.
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
NOTES: medical Digest
DOCUMENT-TYPE: BRIEF
PUBLICATION-TYPE: Newspaper
Copyright 2009 St. Louis Post-Dispatch, Inc.
All Rights Reserved
211 of 998 DOCUMENTS
USA TODAY
March 18, 2009 Wednesday
FINAL EDITION
A warning on off-label use of sleep-disorder drug;
Modafinil meant for snoozing, not for 'smarts'
BYLINE: Rita Rubin
SECTION: LIFE; Pg. 6D
LENGTH: 454 words
A drug approved to help people with sleep disorders stay awake during the day is
also being used off-label by healthy people who think it helps them perform
better on the job or at school. But new research into how the medication affects
the brain suggests the risk of abuse or addiction, while low, might be greater
than previously thought.
The conventional wisdom has been that modafinil is different from other
stimulant drugs, such as amphetamines or methylphenidate -- marketed as Ritalin
for attention deficit hyperactivity disorder -- in that it doesn't increase
dopamine in the brain, researchers write in the Journal of the American Medical
Association.
Dopamine is a neurotransmitter that carries messages from nerve cell to nerve
cell or other tissues. Drugs that increase dopamine have the potential for
abuse.
Modafinil, marketed as Provigil, has been available in the USA since 1999. Like
benzodiazipines such as Valium, it is a Schedule IV controlled substance, with
relatively low abuse potential.
In the new study, scientists used positron emission tomography, or PET, to scan
the brains of 10 healthy men given 200 milligrams of modafinil, the recommended
daily dose for treating sleep disorders, or 400 milligrams.
Both doses raise dopamine levels as much as methylphenidate does, but not as
much as amphetamines do.
Lead author Nora Volkow, director of the National Institute on Drug Abuse, says
she hopes the pilot study will lead to more research.
Volkow says no one knows how many people are using modafinil off-label as a
"cognitive enhancer" to improve their thinking ability and work for hours on
end.
"It's not like anyone has done a proper survey to actually document that,"
Volkow says.
The potential for abuse isn't the only reason healthy people shouldn't take
modafinil or other "smart drugs," she says. They can have serious effects, such
as brief psychotic episodes, she says, and there's little evidence they improve
cognition.
Jeffry Vaught, chief scientific officer for the medication's maker, Cephalon,
calls modafinil "a very serious medication for serious medical disease. This is
for pathological sleep disruption, not for people who've stayed awake for 24
hours." Animal studies have long suggested that modafinil raises dopamine in
humans' brains, Vaught says, but "to date, we've just not seen any signals that
there's a problem" with abuse or addiction.
Although Volkow says no cases of modafinil addiction have been reported in the
scientific literature, psychiatrist Stefan Kruszewski of Harrisburg, Pa., says
he is treating his third case.
"I had two doctors back-to-back who were addicted to modafinil, so I became
alarmed," Kruszewski says. Both of them also were alcoholics, he says.
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, B/W, National Institute on Drug Abuse
PUBLICATION-TYPE: NEWSPAPER
Copyright 2009 Gannett Company, Inc.
All Rights Reserved
212 of 998 DOCUMENTS
Associated Press Online
March 18, 2009 Wednesday 12:05 AM GMT
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: DOMESTIC NEWS
LENGTH: 577 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests. Scans of 10
healthy men showed that the prescription drug Provigil caused changes in the
brain's pleasure center, very much like potentially habit-forming classic
stimulants. Modafinil, the drug's generic name, is sometimes used as an illegal
study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and its sales approached $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
(This version CORRECTS that Provigil's sales "approached" $1 billion.))
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
213 of 998 DOCUMENTS
The Associated Press State & Local Wire
March 18, 2009 Wednesday 7:28 AM GMT
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: STATE AND REGIONAL
LENGTH: 565 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and its sales approached $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
LOAD-DATE: March 19, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
214 of 998 DOCUMENTS
Associated Press Financial Wire
March 17, 2009 Tuesday 8:08 PM GMT
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: BUSINESS NEWS
LENGTH: 565 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and its sales approached $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
215 of 998 DOCUMENTS
The Associated Press
March 17, 2009 Tuesday
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: BUSINESS NEWS
LENGTH: 565 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and its sales approached $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
216 of 998 DOCUMENTS
Elsevier Global Medical News
March 17, 2009 Tuesday 05:25 PM GMT
Modafinil Boosts Brain Dopamine, Raising Addiction Risk
BYLINE: By Mary Ann Moon, Elsevier Global Medical News
LENGTH: 378 words
The wake-promoting drug modafinil, often used off-label to boost cognitive
performance in attention-deficit/hyperactivity disorder and even in healthy
individuals, was found to raise dopamine levels in the brain, according to a
report in the March 18 issue of JAMA.
Until now, modafinil's mechanism of action has been uncertain, and it was
thought to involve several other central nervous system substances but not
dopamine. That hypothesis must now be reconsidered, said Dr. Nora D. Volkow of
the National Institute on Drug Abuse, Bethesda, Md., and her associates.
More important, the drug's effect on dopamine means that it has a heightened
potential for abuse. Given its growing popularity for a variety of uses,
clinicians and patients alike must be made aware of the increased risk of
addiction, the investigators noted.
They assessed modafinil's effects on the brain in a pilot study of 10 healthy
men aged 23-46 years.
The study subjects were given the 200-mg dose that is recommended to treat
narcolepsy as well as the 400-mg dose that is thought to be beneficial for
attention-deficit/hyperactivity disorder, at different times. They then
underwent positron emission tomography with different radiotracers to measure
the effects on extracellular dopamine and dopamine transporters in the brain.
Modafinil was found to increase dopamine in the brain by blocking dopamine
transporters. The elevations in dopamine were comparable with those produced by
therapeutic doses of methylphenidate, Dr. Volkow and her colleagues said (JAMA
2009;301:1148-54).
Modafinil was developed as a drug that "could have a nondopaminergic target for
its wake-promoting effects." However, these findings, together with preclinical
study results, document that modafinil has clear dopamine-enhancing effects,
they added.
Modafinil appears to be "much less potent as a reinforcer" than stimulant drugs
are, making its abuse less common. "Nevertheless, considering the broadening use
of modafinil and the results in this study showing that it increases dopamine in
the nucleus accumbens at therapeutic doses, its potential for abuse should not
be disregarded," the investigators noted.
Dr. Volkow and her associates had no financial disclosures to make in relation
to the study.
Nora D. Volkow
LOAD-DATE: June 10, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: NewsWire
Copyright 2009 Elsevier Inc., International Medical News Group
All Rights Reserved
217 of 998 DOCUMENTS
States News Service
March 17, 2009 Tuesday
NARCOLEPSY DRUG BEING USED TO IMPROVE COGNITIVE PERFORMANCE AFFECTS BRAIN
DOPAMINE ACTIVITY
BYLINE: States News Service
LENGTH: 642 words
DATELINE: CHICAGO
The following information was released by Brookhaven National Laboratory:
Preliminary research in healthy men suggests that the narcolepsy drug modafinil,
increasingly being used to enhance cognitive abilities, affects the activity of
dopamine in the brain in a way that may create the potential for abuse and
dependence, according to a study in the March 18 issue of JAMA.
Brookhaven senior chemist Joanna Fowler: "Like cocaine and methylphenidate,
Modafinil blocks dopamine transporters thereby increasing dopamine levels in the
brain. This study raises awareness about Modafinil's potential for abuse and
addiction in vulnerable populations and signals the need to monitor its use."
Modafinil, a wake-promoting drug used in the treatment of sleep disorders, may
enhance cognition and is used off-label for the treatment of cognitive
dysfunction in some psychiatric disorders (i.e., schizophrenia,
attention-deficit/hyperactivity disorder [ADHD]). The Physicians' Desk Reference
cautions that it can produce psychoactive and euphoric effects typical of
central nervous system stimulant drugs, and there is debate surrounding its
potential for abuse, according to background information in the article. The
mechanisms of action of modafinil are not well understood but are believed to
differ from those of stimulant medications (such as methylphenidate and
amphetamine), which increase dopamine (a neurotransmitter in the brain essential
for the normal functioning of the central nervous system) in the brain by
targeting the dopamine transporters, a mechanism that underlies the abuse
potential of these drugs. However, there is growing evidence that dopamine may
also play a role in the mode of action of modafinil.
Nora D. Volkow, M.D., of the National Institute on Alcohol Abuse and Alcoholism,
Bethesda, Md., and colleagues at Brookhaven National Laboratory conducted a
study to test whether modafinil, at therapeutic doses, would elevate
extracellular (located or occurring outside of cells) dopamine in the brain by
blocking the dopamine transporter. The study included 10 healthy men, between
the ages of 23-46 years, who received either placebo or modafinil: 200 mg, the
dose recommended for narcolepsy; or 400 mg, a dose shown to be beneficial for
the treatment of ADHD. The effects of modafinil on extracellular dopamine and on
dopamine transporters were measured by positron emission tomography (a
radiographic technique used to examine biochemical activity in tissue).
The researchers found: In this pilot study, modafinil acutely increased dopamine
levels and blocked dopamine transporters in the human brain. Because drugs that
increase dopamine have the potential for abuse, and considering the increasing
use of modafinil for multiple purposes, these results suggest that risk for
addiction in vulnerable persons merits heightened awareness.
PET images of the brain show that subjects given modafinil had lower levels of
the radiotracer [11C]raclopride bound to dopamine receptors than subjects given
a placebo. Red represents the highest amount of binding. This signal indicates
higher levels of dopamine release in the modafinil subjects. (Dopamine competes
with the radiotracer so higher levels of dopamine "push" the tracers out.)
Modafinil also increased dopamine in the nucleus accumbens, a brain region
critical for the rewarding effects of drugs of abuse.
Modafinil was developed with an expectation that a medication could have a
non-dopaminergic target for its wake-promoting effects. However, the current
findings in humans, along with preclinical studies, documenting the
indispensable role of dopamine in the wake-promoting effects of modafinil,
support modafinil's dopamine-enhancing effects as a mechanism for its
therapeutic actions.
(JAMA. 2009;301[11]:1148-1154. Available pre-embargo to the media at
http://www.jamamedia.org)
LOAD-DATE: April 29, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 States News Service
218 of 998 DOCUMENTS
Associated Press Worldstream
March 17, 2009 Tuesday 8:16 PM GMT
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: DOMESTIC NEWS
LENGTH: 566 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pennsylvania, and it sales approached $1 billion last year. The company is
developing a spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
219 of 998 DOCUMENTS
The Associated Press State & Local Wire
March 17, 2009 Tuesday 8:26 PM GMT
Study: 'Smart drug' Provigil may be habit-forming
BYLINE: By CARLA K. JOHNSON, AP Medical Writer
SECTION: STATE AND REGIONAL
LENGTH: 565 words
DATELINE: CHICAGO
A so-called "smart drug" popular with young people may carry more of an
addiction risk than thought, a small government study suggests.
Scans of 10 healthy men showed that the prescription drug Provigil caused
changes in the brain's pleasure center, very much like potentially habit-forming
classic stimulants. Modafinil, the drug's generic name, is sometimes used as an
illegal study aid by college students.
"It would be wonderful if one could take a drug and be smarter, faster or have
more energy," said Dr. Nora Volkow, director of the National Institute on Drug
Abuse, who led the study with a Brookhaven National Laboratory scientist. "But
that is like fairy tales. We currently have nothing that has those benefits
without side effects."
The study, appearing in Wednesday's Journal of the American Medical Association,
may bust the myth that the drug is safe for healthy people, experts said.
Provigil is approved to treat excessive daytime sleepiness caused by narcolepsy.
On the market since 1999, it's the flagship product of Cephalon Inc. of Frazer,
Pa., and its sales approached $1 billion last year. The company is developing a
spin-off called Nuvigil.
Modafinil's reputation as a brain enhancer stems from an Air Force study that
found it improved the performance of sleep-deprived fighter pilots. College
students buy and sell it illegally, as they do Ritalin and Adderall, to stay
alert while studying.
Several scientists recently wrote in the journal Nature that healthy people
should have the right to boost their brains with pills like Provigil. One author
of that commentary, brain scientist Martha Farah of the University of
Pennsylvania, said the new study "goes to show that we need a little caution and
a little humility when we're messing around with our brain chemistry."
"But even now, after all the years that it has been on the market, we are still
learning things about it that are relevant to its safety," Farah said.
The men in the study were 23 to 46 years old. They received either a dummy pill
or modafinil. Effects were measured by PET scans, which showed that the drug
increased dopamine, the brain's "feel-good" neurotransmitters.
Modafinil once was thought to be safer than conventional stimulants because it
was believed that it did not engage the brain's dopamine system, which is linked
with addiction. Studies in mice and monkeys suggested otherwise.
The new study is the first human evidence that a typical dose of modafinil
affects dopamine in the brain as much as a dose of Ritalin, a controlled
substance with clear potential for dependence.
Volkow said modafinil acts slowly when swallowed and is difficult to inject,
making it less likely to be abused. Its high price, about $10 per pill compared
to Ritalin at $2 per pill, also makes it less attractive to people seeking a
high. That may change when generics become available in 2012, Volkow said.
Jeffry Vaught, chief science officer for Cephalon, said the company has seen no
evidence the drug is highly abused.
"If abuse is a problem with modafinil, it's minimal at best," Vaught said.
"We're not seeing it used at rave scenes."
Prescribing information for the drug warns of severe rashes and other side
effects such as headache, nausea and anxiety. Cephalon doesn't support the
drug's use as a cognitive enhancer.
"There's no substitute for sleep," Vaught said.
On the Net:
JAMA: http://jama.ama-assn.org
LOAD-DATE: March 18, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2009 Associated Press
All Rights Reserved
220 of 998 DOCUMENTS
Business Wire
February 10, 2009 Tuesday 2:40 PM GMT
Research and Markets: Narcolepsy - Entry-Point to a Lucrative Fatigue-Associated
Market - Provigil (Modafinil), Expected To Launch In 2012
LENGTH: 484 words
DATELINE: DUBLIN, Ireland
Research and Markets(
http://www.researchandmarkets.com/research/30c8d6/stakeholder_opinio ) has
announced the addition of the " Stakeholder Opinions: Narcolepsy - Entry-point
to a Lucrative Fatigue-Associated Market " report to their offering.
Introduction
Narcolepsy is a chronic sleep disorder, which affects fewer than 500,000
sufferers across the seven major markets (7MM). The narcolepsy market value has
grown considerably since 2004 to reach $230m in 2007 driven largely by the
significant penetration of Provigil (modafinil; Cephalon) and Xyrem (sodium
oxybate; Jazz Pharma) and the associated increase in the awareness of the
disorder.
Scope
· Patient potential including disease definition, etiology, prevalence,
diagnosis, and treatment guideline review.
· Review of the key unmet needs in the treatment of narcolepsy as
identified by key opinion leaders interviewed for the report.
· Analysis of narcolepsy market IMS sales data from 2004 to 2007 for
major marketed narcolepsy drugs: Provigil and Xyrem.
· Pipeline analysis with detailed profile for Nuvigil (armodafinil,
Cephalon) and the theory behind potential label expansions beyond
narcolepsy.
Highlights
Although generic versions of Cephalons market leading treatment, Provigil (
modafinil), are expected to launch in 2012, Cephalon is expected to retain a
significant position in the narcolepsy market by switching patients over from
Provigil to its follow-up product, Nuvigil (armodafinil).
Despite Xyrems (sodium oxybate) proven efficacy and its broader narcolepsy
coverage than Provigil, Xyrems sales continue to be limited because of its black
box warning, restricted distribution and comparatively high price.
Targeting narcolepsy as a primary indication and then expanding Provigils label
coverage to other sleep disorders has proven commercially successful for
Cephalon. Datamonitor believes companies could take this strategy a step further
by using narcolepsy as an entry point to access the broader fatigue- or
sleepiness-associated market.
Reasons to Purchase
· Quantify the narcolepsy market value in the US, 5EU and Japan and
identify the drivers and resistors in this market.
· Understand key opinion leader (KOL) views on topical issues in the
current and future treatment of narcolepsy and associated disorders.
· Appreciate the potential of off-label prescribing and indication
expansions for treatments possessing narcolepsy as the primary
indication.
Key Topics Covered:
· CHAPTER 1 EXECUTIVE SUMMARY
· CHAPTER 2 MARKET DEFINITION AND OVERVIEW
· CHAPTER 3 DISEASE OVERVIEW
· CHAPTER 4 UNMET NEEDS
· CHAPTER 5 BRAND DYNAMICS
· CHAPTER 6 PIPELINE ANALYSIS
· BIBLIOGRAPHY
· APPENDIX
· List of Tables
· List of Figures
For more information visit
http://www.researchandmarkets.com/research/30c8d6/stakeholder_opinio .
Source: Datamonitor
CONTACT: Research and Markets
Laura Wood
Senior Manager
press@researchandmarkets.com
Fax from USA: 646-607-1907
Fax from rest of the world: +353-1-481-1716
URL: http://www.businesswire.com
LOAD-DATE: February 11, 2009
LANGUAGE: ENGLISH
DISTRIBUTION: Business Editors
PUBLICATION-TYPE: Newswire
Copyright 2009 Business Wire, Inc.
221 of 998 DOCUMENTS
M2 PressWIRE
February 10, 2009 Tuesday
Research and Markets: Narcolepsy - Entry-Point to a Lucrative Fatigue-Associated
Market - Provigil (Modafinil), Expected To Launch In 2012
LENGTH: 540 words
Entry-Point to a Lucrative Fatigue-Associated Market - Provigil
(Modafinil), Expected To Launch In 2012
Dublin - Research and
Markets(http://www.researchandmarkets.com/research/f49f45/stakeholder_op
inio) has announced the addition of the "Stakeholder Opinions:
Narcolepsy - Entry-point to a Lucrative Fatigue-Associated Market"
report to their offering.
Introduction
Narcolepsy is a chronic sleep disorder, which affects fewer than
500,000 sufferers across the seven major markets (7MM). The narcolepsy
market value has grown considerably since 2004 to reach $ 230m in 2007
driven largely by the significant penetration of Provigil (modafinil;
Cephalon) and Xyrem (sodium oxybate; Jazz Pharma) and the associated
increase in the awareness of the disorder.
Scope
- Patient Patient potential including disease definition, etiology,
prevalence, diagnosis, and treatment guideline review.
- Review of the key unmet needs in the treatment of narcolepsy as
identified by key opinion leaders interviewed for the report.
- Analysis of narcolepsy market IMS sales data from 2004 to 2007 for
major marketed narcolepsy drugs: Provigil and Xyrem.
- Pipeline analysis with detailed profile for Nuvigil (armodafinil,
Cephalon) and the theory behind potential label expansions beyond
narcolepsy.
Highlights
Although generic versions of Cephalons market leading treatment,
Provigil (modafinil), are expected to launch in 2012, Cephalon is
expected to retain a significant position in the narcolepsy market by
switching patients over from Provigil to its follow-up product, Nuvigil
(armodafinil).
Despite Xyrems (sodium oxybate) proven efficacy and its broader
narcolepsy coverage than Provigil, Xyrems sales continue to be limited
because of its black box warning, restricted distribution and
comparatively high price.
Targeting narcolepsy as a primary indication and then expanding
Provigils label coverage to other sleep disorders has proven
commercially successful for Cephalon. Datamonitor believes companies
could take this strategy a step further by using narcolepsy as an entry
point to access the broader fatigue- or sleepiness-associated market.
Reasons to Purchase
- Quantify the narcolepsy market value in the US, 5EU and Japan and
identify the drivers and resistors in this market.
- Understand key opinion leader (KOL) views on topical issues in the
current and future treatment of narcolepsy and associated disorders.
- Appreciate the potential of off-label prescribing and indication
expansions for treatments possessing narcolepsy as the primary
indication.
Key Topics Covered:
- CHAPTER 1 EXECUTIVE SUMMARY
- CHAPTER 2 MARKET DEFINITION AND OVERVIEW
- CHAPTER 3 DISEASE OVERVIEW
- CHAPTER 4 UNMET NEEDS
- CHAPTER 5 BRAND DYNAMICS
- CHAPTER 6 PIPELINE ANALYSIS
- BIBLIOGRAPHY
- APPENDIX
- List of Tables
- List of Figures
For more information visit
http://www.researchandmarkets.com/research/f49f45/stakeholder_opinio
Source: Datamonitor
CONTACT: Laura Wood, Senior Manager, Research and Markets
Fax: +1 646 607 1907 (US)
Fax: +353 1 481 1716 (Rest of World)
e-mail: press@researchandmarkets.com
((M2 Communications Ltd disclaims all liability for information
provided within
Further information on
http://www.presswire.net on the world wide web. Inquiries to
info@m2.com)).
LOAD-DATE: February 12, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
JOURNAL-CODE: M2P
Copyright 2009 M2 PressWIRE
All Rights Reserved
222 of 998 DOCUMENTS
Guardian Unlimited
January 13, 2009
The not-so-clever pills
LENGTH: 494 words
HIGHLIGHT: Robert Fox: Cognitive-enhancement pills are nothing new - and neither
is their power to disappoint us
The generalised use of Modafinil, the "clever pill" advocated in Nature magazine
last month and by its online editor Adam Rutherford on this website, may not be
quite so clever as it appears.
In the Nature article, Professor Henry Greely marshals a distinguished panel of
experts and co-writers to argue that cognitive-enhancement drugs are so
generally used by students in the US, occasionally illegally, that it is time to
put them on a sensible footing. If need be, the authors suggest, there should be
licensing or regulation.
The article claims that some 7% of all US college students now use Ritalin, a
drug prescribed for attention-deficiency hyperactivity disorder (ADHD), to help
them concentrate and stay alert while studying for exams. Another favourite is
the pharmaceutical psychostimulant sold under the commercial name of Adderall,
also prescribed for ADHD cases. It is suggested that on some campuses up to 25%
of all students are using one of these two stimulants.
Greely and Rutherford argue that a wider use of Modafinil, commonly sold as
Provigil for narcolepsy and similar cases, can only be beneficial to
concentration, learning and study. There seem to be few side-effects, if any,
and such use should be for self-improvement and the better education of humanity
in general. After all, he rightly suggests, humanity has always tried to master
and adapt nature for its own benefit.
Greely, the Director of Stanford Law School's Center for Law and Biosciences,
suggests that dishing out cognitive-enhancing drugs to students isn't
necessarily tipping the level playing field of competition in the same way as
giving performance-enhancing drugs to athletes. After all, he suggests,
differences in schooling and previous learning experience, also make for
inequality between examinees. Fair enough, but from a little research I'm not
entirely convinced about the invidious comparison with performance-enhancers,
for different reasons.
Of course, we have been through the arguments about the liberal and libertarian
approaches to recreational and mind-expanding drugs since the priestesses got
stoned at the shrine of Apollo at Delphi and da Quincy and Coleridge got high on
opium. In our own day we have a cult of psychotropic drugs. Aldous Huxley
cautiously suggested that mescaline might open the doors of perception to
greater spiritual awareness and unity with creation - and gave the name to Jim
Morrison's visionaries The Doors. Hunter S Thompson took on a load of pills to
fuel his quest for the American dream in Fear and Loathing in Las Vegas.
All of them thought the drugs made them better and powerful performers and
thinkers. Coleridge was doing fine as he sketched his path through Xanadu, Alph
the sacred river and the sunless sea, until the man from Porlock broke in on the
spell. The muse fled and Kubla Khan remains a fragmented, broken spell.
The problem is that the man from Porlock is always lurking in the corner to be a
spoil-sport.
LOAD-DATE: January 13, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2009 Guardian Unlimited (© Guardian Newspapers Limited)
All rights reserved
223 of 998 DOCUMENTS
Daily Mail (London)
January 6, 2009 Tuesday
1ST Edition
CAN A PILL MAKE YOU BRAINIER?;
Students and the military are using drugs to boost their brainpower. But do they
work -- and are they safe? This intrepid writer decided to find out
BYLINE: ANGUS WATSON
SECTION: Pg. 45
LENGTH: 1423 words
A PILL that makes you more intelligent, boosts your memory, improves your
concentration and reduces tiredness? It sounds like the stuff of science
fiction. In fact, it is already available, and academics in America and Britain
have apparently been taking it for years.
Last week, John Harris, a professor of bioethics at the University of
Manchester, said students should be allowed to take 'smart' drugs (or 'Viagra
for the brain', as they've been dubbed) to boost their academic performance.
He claimed a sizeable body of evidence showed that pills such as Ritalin, which
is prescribed for ADHD (Attention- Deficit/Hyperactivity Disorder), Adderall,
another ADHD drug, and Modafinil significantly improved concentration and should
be available without prescription.
Modafinil -- better known as Provigil -- is the pill the academics have been
taking.
Officially, it's used to treat conditions that cause daytime sleepiness, such as
narcolepsy. But off-prescription, it's being used, not only by academics and
students, but reportedly by the U.S. and UK military, to improve mental energy.
There are no figures on the numbers of people using Modafinil as an
off-prescription stimulant (it can be obtained through the internet). However,
according to my sources, and judging by the large chunk of the internet devoted
to the subject, the use -- or abuse -- of Modafinil is widespread.
'Plenty of people use Modafinil,' agrees Barbara Sahakian, professor of Clinical
Neuropsychology at the University of Cambridge. 'I know an Oxford University
professor who takes it fortnightly for one day of really hard work and a
colleague at Cambridge who takes it at parties, while another takes it for
jet-lag.'
Nobody is certain how Modafinil works, according to Sahakian. It does seem
clear, however, that it specifically tackles drowsiness without affecting other
parts of the brain. This sets it apart from other stimulants such as
amphetamines, which make you less tired, but can also compel you to talk too
much.
Working at home as a freelance writer, I'm OK in the mornings, but my afternoon
work ethic would shame a siesta-loving Spaniard.
A pill to increase my post-lunch productivity would be marvellous. I decided to
see for myself if Modafinil worked.
THE fact that it definitely does something to one's brain, but nobody's quite
sure what, was a niggling worry. It didn't help when I talked to Baroness Susan
Greenfield, the neuroscientist, about my plans to take it.
'You're taking a risk,' she said firmly. 'Our brains are hugely delicate and
responsive to drugs. If you take too much vitamin C, it's excreted in your
urine. That's not the case with brain-altering drugs.
Any influence -- especially the direct chemical manipulation that you're
suggesting -- could have a long-term, negative effect on brain cells. You're
risking your life.'
So trying Modafinil might damage my brain for ever. And there were other
potential, and more immediate side-effects. I read of a vast range of possible
nasties, including headaches, nausea, nervousness, diarrhoea, back pain, reduced
appetite and abnormal ejaculation.
It was all pretty frightening. But a reckless part of me wondered if it was all
worthwhile if the pills did make me branier.
First there was the problem of getting prescription-only drugs without being
ill. I asked a doctor friend if she'd write me a prescription.
She said I was an idiot.
So I ordered them online, but they never came. Finally, I tried a randomly
picked doctor. Fortunately, his standards weren't as high as my friend's, and he
gave me a prescription for a £5 'admin fee'.
The guilt of using an ill-gained prescription wore off when the chemist charged
me £75 for 30 100mg tablets. He explained, that's how much privately-prescribed
drugs cost.
The label gave no dosage advice, but the internet suggested 200mg daily. I'd
told the doctor this was my plan, and he agreed that it seemed reasonable. I
decided to start with a 100mg pill at 9am.
Given all those potential sideeffects I reasoned it would be best to be wary.
I popped the pill and began a big writing project I'd been putting off.
An hour later I wasn't dead -- I was perfectly happy, although I had no appetite
for breakfast. Perhaps I was working harder -- it was difficult to tell since I
usually work well in the morning. By 10am, I was still alive and sane, and,
apart from my lack of appetite, all seemed normal.
So I took a second 100mg pill. Half an hour later I was lightheaded and
euphoric. I began singing along to the radio and my computer keyboard felt oddly
fizzy, as if I had pins and needles in my fingertips. At 10am, alone in my flat,
it felt like I'd downed four glasses of champagne.
Modafinil was meant to improve my work ethic and focus, but there was no way I
could concentrate. My mind was rushing, so much so that I got a little scared. I
worried that I might have a heart attack, or perhaps my head might explode.
So I went for a walk by the Thames. I've always found that watching ducks can
allay pretty much any affliction, and this was no exception. I calmed down, came
home, forced myself to eat and felt better. My mind was still on overdrive but
it was my most productive working afternoon -- ever.
That evening, I had dinner with a friend. I was conscious of being chatty, but
also witty and incisive.
Before we parted, I told her about the Modafinil trial. 'You were a little more
obnoxious than usual,' she commented.
Back home, I found myself standing in the bathroom doing a sudoku puzzle at
1.30am, and didn't get to sleep until 2am. Next morning I took 200mg in one go.
Soon I felt a bit sick, muddle-headed, panicky and sweaty. But I calmed down,
and did a good morning's work.
A night later, I met my new girlfriend's friends for the first time in a trendy
restaurant. I was extremely talkative as I knocked back gallons of wine, and
became astonishingly extrovert, dancing with people and coercing a group of
reluctant revellers to sing Under Pressure by Queen. I remember nothing of the
taxi ride home.
The next morning, I had a horrendous hangover but was cheered by reports from my
girlfriend, who said her friends thought I was the life and soul of the party.
Was that a euphemism for loudmouth buffoon, I asked? 'No, really, you were fun',
she insisted.
I recovered by Sunday and, settling into the Modafinil, my work took off. Panic
disappeared, I felt absolutely fine. Concentration and output sky-rocketed and I
felt fantastic. In fact, during my two weeks of Modafinil-enhanced life I did
tons of good work, gained two new regular slots in newspapers, lost 4lb in
weight and cleared an Augean stable of admin.
But I'm not sure Modafinil really increases your memory or makes you more
intelligent. It makes you think you're more intelligent. I took part in a pub
quiz -- we won -- but despite, rather than because of me. I was convinced I was
right every time, but was consistently wrong.
WHAT'S the driest place in the world? 'Atacama Desert!' I cried, full of
confidence.
'Isn't it Antarctica?', asked someone. 'No, no, Atacama,' I insisted
patronisingly. Of course, the answer was Antarctica.
And then there are those lingering health doubts. It's said that Turkish leader
Kemal Ataturk only functioned after he overcame his crushing shyness with vast
quantities of the spirit of Raki.
And he defeated every major European power and founded modern Turkey. So it
worked for him. But he did die of cirrhosis at the age of 58.
Another danger comes with buying the Modafinil online. As with all illegally
supplied drugs, you have no control over what you're getting.
You could be sold something useless or, worse, dangerous.
And then there's that fundamental question: is false brain enhancement morally
acceptable? And if it is, could it also ever be made safe? Neuroscientist
Greenfield thinks not. 'Drugs will always have sideeffects.
If you want to improve your output, you should look at your lifestyle and goals.
Not take drugs.' Professor Sahakian treads a middle ground. 'There are better
ways to enhance ourselves, such as education and exercise. If there are clean
drugs that could make work easier and improve our lives, that would be great,
but we'd have to be careful not to push ourselves to unpleasant limits.'
Cephalon, who manufacture Provigil, said it only supported approved uses for the
drug. It is 'naturally opposed to all forms of purchases which are not under the
control of physicians such as online sales,' their spokesman added.
So -- expensive, 'illegal' and a potential health risk. Think I'll stick to
early nights instead..
LOAD-DATE: January 6, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Papers
Copyright 2009 Associated Newspapers Ltd.
All Rights Reserved
224 of 998 DOCUMENTS
The International Herald Tribune
November 3, 2008 Monday
Narcoleptic allowed to race again;
Cycling
BYLINE: Samuel Abt - The New York Times Media Group
SECTION: SPORT; Pg. 20
LENGTH: 609 words
Rise and shine, up and at 'em: After four years of legal and medical battles,
Franck Bouyer can return to work.
''I can dream again,'' he said with no hint of irony. Bouyer's problem has been
that of course he can dream - anywhere, at any time - since he is a victim of
narcolepsy, or sleeping sickness.
The genetic disease, which is marked by unpredictable episodes of sleep during
normal waking hours and disturbed sleep at night, afflicts about one in 200,000
people. Except for Bouyer, none of them is a professional bicycle racer.
That job is impossible for a narcoleptic without medical treatment since Bouyer
works amid a pack of other men on bicycles. Let the sandman call and Bouyer
swerve, the result can be a mass crash.
Although that has not happened yet, he has been known to fall asleep during a
training ride and wake up sprawled in the courtyard of a farm. Once or twice,
feeling himself nodding off, he has had to pull to the side of the road during a
race.
''With medicine, no problem,'' he said in a telephone interview this week from
his home in western France. ''Without medicine, lots of problems.''
But the medicine that is commonly used to treat narcolepsy is modafinil, which
is on the list of drugs prohibited by the International Cycling Union because
they enhance performance.
So Bouyer has been caught between two arguments: For safety's sake, doctors for
the French Cycling Federation refused to issue him a license unless he was using
modafinil, but the highest governors of the sport refused to let him race if he
did use the drug.
Back and forth the legal battle went, with the International Cycling Union
barring Bouyer, the World Anti-Doping Agency first ruling against him and then
for him and the Court of Arbitration for Sport turning down his appeal.
''It went on so long,'' he said this week. ''So much time, so much money. It
killed my career.''
Now 34 years old, Bouyer has long been a solid midlevel rider. Since he turned
professional in 1995 and joined the first of six French teams, he has finished,
albeit far back, five Tours de France.
He has had his share of victories, though. In 2001, he won the Tour of the
Limousin and in 2002, the Tour of the Vendée, both French races. His best year
was 2004, when he won Paris-Camembert and a stage in the Circuit of the Sarthe.
That was also the year, however, that he learned he had narcolepsy.
Since then, he has raced only briefly late in 2005 and early in 2006 while the
legal battles were in abeyance.
His breakthrough occurred early this year when a doctor prescribed another
medicine, Xyrem, to treat his disease. It worked as well as modafinil and was
not on the list of prohibited drugs, according to the International Cycling
Union when Bouyer phoned its doctors.
''So that was that,'' he said. ''I applied for my racing license in July and got
it. Since August, I've been training constantly.''
Why did nobody prescribe the legal drug years ago? Good question, said Bouyer,
unable to answer it.
He will join his Bouygues Télécom teammates this week at a training camp and
will be a paid rider for the first time in two years.
''It's really strange,'' Bouyer said, ''I thought it was all over and now I'll
be back. Such a long wait.''
He has no great hopes for immediate success, not after years away from the
sport.
''Lance Armstrong might be able to do that,'' he said, ''but I don't have his
motor. I hope to be riding at a correct level, mostly for the pleasure of it
all. Yes, for the satisfaction of competing again.''
As for the races he will enter next year, it's too early to decide, but he will
give it a lot of thought, he said. In other words, he'll sleep on it.
LOAD-DATE: November 3, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2008 International Herald Tribune
All Rights Reserved
225 of 998 DOCUMENTS
The Times (South Africa)
October 20, 2008 Monday
Stay wired awake
BYLINE: Caspar Greeff
SECTION: LIFESTYLE & LEISURE; Pg. 20
LENGTH: 422 words
POKER is not yet an Olympic sport, which means that players are not monitored by
the World Anti-Doping Agency, nor are they subject to the rules of the World
Anti-Doping Code.
This is a pity because I am sure that two of the more senior members of our
Thursday night poker school (both of them are 87- years- old) are on
performance-enhancing drugs. How else do they win all my money week after week?
One poker player who openly admits his use of stimulants is former computer
programmer Paul "Dot Com" Phillips, who has career winnings of more than
$2.3-million.
Phillips told Slate magazine: "I've long been an enthusiastic believer in better
living through chemistry. That's why, when I was diagnosed with
attention-deficit hyperactive disorder two years ago, I didn't hesitate to fill
a prescription for Adderall. A few months later, I won almost $500000 in a World
Poker Tour event, then another $1.1-million in another WPT event soon after."
"With Adderall in my system, I am like an information sponge, able to process
data from several players at once while considering my next action. It improved
my patience.
"This year, I have a new chemical weapon: Modafinil. It stimulates wakefulness
and enhances focus but without the side effects of an amphetamine - for me,
reduced appetite and insomnia. With Modafinil, I feel well-rested even on
limited sleep. Through judicious use of both I can operate at my full potential
for days on end."
Modafinil, also called Provigil, is a nootropic or cognitive enhancer used in
the treatment of narcolepsy, shift work sleep disorder and obstructive sleep
apnea. It is also described as a "memory-improving and mood-brightening
psychostimulant".
The US military has given Modafinil to its air force pilots in the Gulf War and
Iraq, and the French government admits that the Foreign Legion has used it
during " covert operations".
Modafinil expert Trevor Robbins, professor of cognitive neuroscience at
Cambridge University, says: "It works like a mental manager. It's great on tasks
requiring reflection and planning, plus it inhibits impulsiveness - and blurting
out the wrong thing."
What are the side effects?
The website provigil.com warns: "If you experience chest pain, depression,
anxiety, hallucinations, psychosis, mania, thoughts of suicide, aggression, or
other mental problems, stop taking Provigil [Modafinil] and call your doctor or
get emergency treatment."
Funny, I get all those symptoms every time I lose money at poker, and that's
without any performance-enhancing stimulant.
LOAD-DATE: June 2, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: The Times
Copyright 2008 AVUSA Media LTD
All Rights Reserved
226 of 998 DOCUMENTS
US Fed News
September 19, 2008 Friday 6:05 AM EST
French Inventors Develop Therapeutic Treatment Method
BYLINE: US Fed News
LENGTH: 192 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Sept. 19 -- Veronique Broquaire of Noisy-le-Grand, France,
Ludovic Broquaire of Frejus, France, Laurent Courvoisier of Laigneville, France,
Gerard Coquerel of Boos, France, Franck Mallet of Blangy sur Bresle, France, and
Michel Broquaire of Le Perreux, France, have developed a therapeutic treatment
system.
According to the abstract released by the U.S. Patent & Trademark Office: "
Modafinil polymorphic forms of modafinil racemate, methods of preparation
thereof, pharmaceutical compositions and methods of therapeutic treatment
involving modafinil polymorphic forms."
The inventors were issued U.S. Patent No. on July 29.
The patent has been assigned to Cephalon France, Maisons Alfort, France.
The original application was filed on Oct. 12, 2005, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,405,323.PN.&OS=PN/7,405,323&RS=
PN/7,405,323.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
LOAD-DATE: September 19, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 HT Media Ltd.
All Rights Reserved
227 of 998 DOCUMENTS
US Fed News
September 19, 2008 Friday 6:05 AM EST
French Inventors Develop Therapeutic Treatment Method
BYLINE: US Fed News
LENGTH: 193 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Sept. 19 -- Veronique Broquaire of Noisy-le-Grand, France,
Ludovic Broquaire of Frejus, France, Laurent Courvoisier of Laigneville, France,
Gerard Coquerel of Boos, France, Franck Mallet of Blangy sur Bresle, France, and
Michel Broquaire of Le Perreux, France, have developed a therapeutic treatment
system.
According to the abstract released by the U.S. Patent & Trademark Office: "
Modafinil polymorphic forms of modafinil racemate, methods of preparation
thereof, pharmaceutical compositions and methods of therapeutic treatment
involving modafinil polymorphic forms."
The inventors were issued U.S. Patent No. 7,405,323 on July 29.
The patent has been assigned to Cephalon France, Maisons Alfort, France.
The original application was filed on Oct. 12, 2005, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,405,323.PN.&OS=PN/7,405,323&RS=
PN/7,405,323.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
LOAD-DATE: September 19, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 HT Media Ltd.
All Rights Reserved
228 of 998 DOCUMENTS
Daily Mail (London)
August 19, 2008 Tuesday
1ST Edition
Fears for 'smart pill' generation
BYLINE: Sarah Harris
SECTION: Pg. 60
LENGTH: 761 words
THE A-level and GCSE exam season is over for another year. Pupils -- and parents
-- will be relieved that the stress, last-minute cramming and hard work is
behind them.
Last week saw record A-level results.
The pattern is expected to be repeated this Thursday when hundreds of thousands
of GCSE pupils discover how well they did.
But experts are questioning how far pupils and their families are prepared to go
to get the best results.
Rising numbers of stressed students are feared to be popping so-called 'smart
pills' to boost their exam performance.
They are taking drugs used to treat hyperactive children and people with sleep
problems to improve their brain power, despite being healthy.
Doctors have warned that parents may be tempted to condone or even encourage
this risky practice to give their youngsters a competitive edge.
The British Medical Association claims that despite a lack of information about
the possible long-term side-effects, 'there is already evidence of demand' for
these cognitive enhancers in the UK.
The problem is thought to be spreading due to the growth of online pharmacies
selling Ritalin and Modafinil -- the most popular cognitive enhancers -- from
60p per pill without prescription.
Experts believe parents are also duping doctors into giving them Ritalin for
their children on prescription when there is no medical justification for using
the drug.
The number of prescriptions given to pupils for behaviour-altering drugs such as
Ritalin and Modafinil has risen tenfold in the past decade, from around 48,000
in 1996-7 to more than 450,000 last year.
Ritalin is used to calm and focus children with attention deficit hyperactivity
disorder (ADHD). It increases alertness and improves concentration and memory.
Modafinil is sold to treat narcolepsy (characterised by sudden attacks of
sleepiness), but it can also stave off tiredness in those without a diagnosed
sleep disorder.
The BMA has warned that - cognitive enhancers are already being used
'surreptitiously' by students in the States as study aids. In a recent report,
it says: 'Modern-day UK society is highly competitive.
Children are judged from a young age on the basis of success in examinations,
competition for university places, for openings in prestigious and highly paid
professions, and pressure to succeed in one's chosen pursuits.
' In such an environment, it is perhaps not surprising that anything that gives
an individual a competitive edge over his or her peers is seen as beneficial.'
AND THE BMA says there is a 'strong advantage' for parents in trying to ensure
their child, rather than somebody else's, gains an in-demand university place.
'So, those who could afford the interventions for their children would have a
competitive advantage,' the report says.
'The result may well be pressure on parents to choose cognitive enhancers, and
those who abstain risk holding their children back.'
It asks 'whether we want to live in a society in which the use of cognitive
enhancements are routine'.
The use of brain-boosting drugs is rife among students in the U.S. Research by
the National Institute on Drug Abuse found 2.5 per cent of eighth graders (13-
to 14-year-olds) and 5.1per cent of 12th graders (17- to 18-year-olds) took
'smart pills' either for the 'rush' or as a study aid.
Other studies show that on some U.S. campuses, 16 per cent of students are
taking the drugs.
Experts say that a similar problem is 'almost certainly happening here' among
the student population.
Barbara Sahakian, a professor of clinical neuropsychology at Cambridge
University and author of studies into cognitive enhancers, says that
prescriptions of Ritalin are increasing in the UK.
She explains: 'When doctors see children, it's only for a short period of time.
They're taking information provided by the parent about how they behave at
school and home.
It's self-reporting and it is open to abuse.
For those children with ADHD it is a very effective form of treatment, but it
shouldn't be used for all children.'
Paul Cooper, professor of education at Leicester University, says teachers have
told him that parents are buying Ritalin for their children off the internet.
This is a 'dangerous risk' as they do not know if the drug is genuine or has
been adulterated. They may also administer the wrong dose or mix it with other
medicines.
'I think it's likely that parents are using Ritalin to try to improve their
children's performance,' he says.
'If you think about the pressures that students and their parents are under --
short of outright cheating, I think they will go to extreme lengths.'
LOAD-DATE: August 26, 2008
LANGUAGE: ENGLISH
GRAPHIC: Under pressure: The use of brain-boosting drugs is on the increase
PUBLICATION-TYPE: Papers
Copyright 2008 Associated Newspapers Ltd.
All Rights Reserved
229 of 998 DOCUMENTS
Clinical Psychiatry News
August 2008
Modafinil Reduces Severe Cancer Fatigue
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 52 Vol. 36 No. 8 ISSN: 0270-6644
LENGTH: 362 words
CHICAGO - The wakefulness-promoting drug modafinil reduced self-reported
severe fatigue, according to a study of more than 600 cancer patients undergoing
chemotherapy that was presented at the annual meeting of the American Society of
Clinical Oncology.
Gary R. Morrow, Ph.D., of the University of Rochester (N.Y.) and his
colleagues randomized 631 patients undergoing four cycles of chemotherapy to
receive either 200 mg modafinil (Provigil) daily or placebo.
Among those with severe fatigue at baseline, patients on modafinil had
significantly greater reductions in fatigue, compared with those on placebo.
Participants were asked to rate their level of fatigue at baseline (during
the second cycle of chemotherapy) and during the final cycle. They rated fatigue
on a 10-point scale: mild (1-4), moderate (5-6), and severe (7-10).
A total of 67 patients reported mild fatigue at baseline; 106 and 458
reported moderate and severe fatigue, respectively..
Among patients with mild and moderate fatigue, modafinil also reduced
fatigue, compared with placebo, but the differences were not significant. This
was not surprising, Dr. Morrow said during a press briefing. "With side effects,
quite often the potency of the effect is somewhat dependent on where you began,"
he said.
Modafinil-a nonamphetamine stimulant-is currently indicated for the treatment
of excessive sleepiness resulting from obstructive sleep apnea, shift-work sleep
disorder, and narcolepsy. Last year, researchers also at the University of
Rochester reported success with modafinil in treating "chemo brain," a reduction
in cognitive function that has been associated with chemotherapy.
There may be some overlap between chemo brain and fatigue, Dr. Morrow said in
an interview. Problems with executive function are commonly described in chemo
brain. Cancer-related fatigue appears to particularly affect tasks associated
with executive function. Cancer patients complain of not being able to "get
around" to doing things they know they should do.
Cephalon Inc. provided modafinil and placebo for the trial. Dr. Morrow
reported that he has no relevant financial relationships.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
230 of 998 DOCUMENTS
Internal Medicine News
August 1, 2008
Modafinil Helps Reduce Severe Cancer-Related Fatigue
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 33 Vol. 41 No. 15 ISSN: 1097-8690
LENGTH: 361 words
CHICAGO - The wakefulness-promoting drug modafinil (Provigil) reduced
self-reported severe fatigue, according to a study of more than 600 cancer
patients undergoing chemotherapy that was presented at the annual meeting of the
American Society of Clinical Oncology.
Gary R. Morrow, Ph.D., of the University of Rochester (N.Y.) and his
colleagues randomized 631 patients undergoing four cycles of chemotherapy to
receive either 200 mg modafinil daily or placebo. Among those with severe
fatigue at baseline, patients on modafinil had significantly greater reductions
in fatigue, compared with those on placebo.
The participants were asked to rate their level of fatigue at baseline
(during the second cycle of chemotherapy) and during the final cycle. They rated
fatigue on a 10-point scale: mild (1-4), moderate (5-6), and severe (7-10). A
total of 67 patients reported mild fatigue at baseline; 106 and 458 reported
moderate and severe fatigue, respectively.
Among patients with mild and moderate fatigue, modafinil also reduced
fatigue, compared with placebo, but the differences were not significant. This
was not surprising, Dr. Morrow said during a press briefing. "With side effects,
quite often the potency of the effect is somewhat dependent on where you began,"
he said.
Modafinil-a nonamphetamine stimulant-is currently indicated for the treatment
of excessive sleepiness resulting from obstructive sleep apnea, shift-work sleep
disorder, and narcolepsy. Last year, researchers also at the University of
Rochester reported success with modafinil in treating "chemo brain," a reduction
in cognitive function that has been associated with chemotherapy.
There may be some overlap between chemo brain and fatigue, Dr. Morrow said in
an interview. Problems with executive function are commonly described in chemo
brain. Cancer-related fatigue appears to particularly affect tasks associated
with executive function. Cancer patients complain of not being able to "get
around" to doing things they know they should do.
Cephalon Inc. provided modafinil and placebo for the trial. Dr. Morrow
reported that he has no relevant financial relationships.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
231 of 998 DOCUMENTS
The Sunday Times (London)
July 20, 2008
There's a buzz about Modafinil
BYLINE: Fleur Britten
SECTION: FEATURES; Style; Pg.36
LENGTH: 1335 words
There's a buzz about Modafinil, the 'smart' drug that is meant to make you
sharper, brighter and more energised, but the idea of popping a pill to boost
your brain - without any nasty side effects - is a little hard to swallow. Fleur
Britten plays guinea pig
Is your memory so perforated that you fear early-onset Alzheimer's? Your
attention so centrifugal that you've self-diagnosed attention deficit
hyperactivity disorder (ADHD)? Perhaps you don't have time to sleep, or maybe
you would just like to function as a super-you. The sci-fi solution we have all
been waiting for is already here, and it's circulating in student unions and
school. These days, the kids are all on "smart drugs".
A group of pharmaceuticals designed for sufferers of narcolepsy, Alzheimer's and
ADHD, smart drugs are increasingly being used "off label" (unsupervised, as a
lifestyle choice) by healthy people, who procure them from online pharmacies,
friendly physicians and illicit prescription sales. "This stuff is being passed
around all the time," says one male A-level student with something of a
smart-drug habit - "this stuff" largely being Ritalin, usually prescribed for
children with ADHD, and Modafinil, which is used to treat narcolepsy. Students
are rejoicing and cramming for exams with smart-drug- fuelled all-nighters. One
told me that he buys his from a mate who sells on his larger-than-necessary
prescription; another offered to put me in touch with her "very kind doctor".
The government, meanwhile, is sweating. It recently commissioned a report on
brain science that concluded more work is needed. What students and the
government both know is that in Ritalin improves attention, memory and cognitive
flexibility in healthy subjects; Modafinil improves attention, memory, planning
and decision- making and leaves you in a state of wakefulness without the wired
bit, liability of addiction or "obvious toxic effects". So what's not to like?
Imbued with visions of a new, improved me, I visit that conveniently unregulated
online pharmacy. Ritalin costs £ 58 for 10 pills; Modafinil, £ 10 for 10. No
questions asked, no electrocardiograph tests required. I plump for cheapo
Modafinil. My sister, a doctor, phones with a warning: "I've been discussing
your drugs trial with a colleague, and we don't think it's safe to experiment
with your brain like this." I fall silent as she explains there are scant
statistics on Modafinil's long-term effects, even fewer on the effects on
healthy subjects. Plus, as with all neurological drugs, there can be atypical
side effects. And a new report claims three in five medicines bought online are
fake, some dangerously so.
A dodgy package arrives in the post. Wrapped in low-grade manila, wonkily
stamped "Mumbai - India", is a loose strip of 10 x 200mg legit-looking Modafinil
pills (the website was recommended by a genuine American pharmacy that refused
to ship to the UK). There are no instructions, no warnings of harmful
contraindications, only this: "Dosage: as directed by the neurologist/
psychiatrist/specialist." I turn to my old friend the internet to check the dose
(one or two pills) and side effects (insomnia, decreased appetite, anxiety,
headache and rapid heartbeat). Some, of course, may see these cons as pros.
First thing the next morning, down it goes, and I await the "eureka!" moment.
It never comes, but an hour later, I feel undoubtedly alert. Actually, I feel
pretty normal (no cleverer, no less hungry), if a little edgy. A persistent, dry
headache develops, like I have drunk one too many coffees (after all, caffeine
and Modafinil both stimulate the central nervous system), but where my attention
usually drifts, today it can't. Streams of consciousness babble endlessly; I
feel spirited and industrious. The steady energy endures with no 4pm fogs, and I
fantasise about Thatcher-style productivity. Perhaps this is the key to the
mythological 25-hour day?
There are stories of off-label users finally conquering their intellectual
Everests (lifelong battles with War and Peace); the American poker player Paul
Phillips claimed that when he was prescribed Modafinil, it helped him win more
than £ 1.7m. One A-level student told me: "On Ritalin and Modafinil, no matter
what you're doing, you're interested. I studied politics, which usually I
couldn't give a toss about. Four hours in, you have the choice to work or not,
and you prefer to work. I screwed around all year and then worked really hard
for my exams - on drugs. Some say it's cheating, but it's not like in sport,
where you can be banned for taking steroids."
According to the Department of Health, buying these drugs from illegal
organisations is not against the law, as they are legal.
It is time to find out what is going on in my head, so I call the Modafinil
expert, Trevor Robbins, professor of cognitive neuroscience at Cambridge
University and one of the academics behind the government's recent brain science
report. He is unambiguously excited. "It works like a mental manager, optimising
the performance of several different faculties," he says. "It's great on tasks
requiring reflection and planning, plus it inhibits impulsiveness - and blurting
out the wrong thing."
Does he see it as cheating? "Coffee is a cognition enhancer," he argues. "People
don't think of them as the same, but they're both chemicals. It's like taking a
vitamin pill." Except that Modafinil is much more sophisticated and active. But
where was super-me?
"Modafinil operates on an inverted U-shaped curve," Robbins says. "If you're
already functioning at the top of it, you can only go down." Depressing. He adds
that some may not be genetically optimal for enhancement. Has Robbins tried
Modafinil? "Never.
I perform optimally already."
Disturbingly, nobody knows exactly how Modafinil works, although it's generally
considered safe (provided, of course, you're not taking the fakes). Made by
Cephalon, it's been licensed for narcolepsy (as Provigil) for 10 years in the
UK. In America, where the licensing regulations are more lenient, plenty of
academics have it on repeat prescription. Cephalon refuses to answer my
questions about off-label use, saying it has no direct involvement with tests on
healthy volunteers, nor any plans for over-the-counter sales.
It was after dark that Modafinil's potential for 48-hour wakefulness appeared -
annoyingly. (I was only after the "smart" bit.) Wide-eyed at 2am, I reached for
a sleeping pill. And another. Predisposed to poor sleep, I ended up taking three
times the normal dose, yet getting barely two hours' kip.
Many claim to sleep fine and that there is no sleep debt after all-nighters,
provided you get eight hours' kip the following night. I'm not convinced. The
next day, I'm still alert, but I need an extra jolt of caffeine. By 6pm, I'm
broken. I see that upper- downer cycle winking at me: Exhausted? Take this
little pill. Can't sleep? Try this.
And I did, a few days later, this time on a hangover. With the stuffing already
knocked out of me, I wondered whether Modafinil could be the ultimate hangover
cure. But no - I had the same sleep issues (none, all night) and a whole new
hangover to deal with. The day after, I felt heavy, woolly and strung out, with
a stubborn, brittle headache - not dissimilar to the aftermath of a drugs
bender. Unsurprisingly.
According to the US military, sequential dosing has diminishing returns:
Modafinil can work for 48 hours, but then people need sleep. After all, people
eventually die from sleep deprivation. As far as I can work out, it doesn't do
to mess with your circadian cycle: power pills are no substitute for real sleep.
But in these time-obsessed days, off-label use is predicted to rise, and more
cognition-enhancing drugs are in development. I haven't touched my stash since,
but if I were a truckie or on the eve of exams, I could be tempted. But you
would be foolish to treat smart drugs like the new coffee. 1
FOTOFIT
LOAD-DATE: July 25, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: sb
Copyright 2008 Times Newspapers Limited
All Rights Reserved
232 of 998 DOCUMENTS
Pallimed
July 2, 2008 Wednesday 2:03 PM EST
2008 ASCO: methadone, genetics, modafinil
BYLINE: Drew Rosielle MD
LENGTH: 289 words
Jul. 2, 2008 (Pallimed delivered by Newstex) -- The 2008 American Society of
Clinical Oncology meeting was last month. Every year the palliative care,
supportive care, and end-of-life care abstracts are worth browsing (abstracts
here).I wanted to particularly point out 3:First is a case series about one
center's experience with initiating and rotating to methadone in outpatients.
Very little has been published about rotating to methadone in the outpatient
setting despite it being a relatively common practice (that's my sense at least)
- most of the publications about methadone rotations have been in inpatients.
The data presented here suggest it's safe (no one falling over dead from
torsades) and has salutary effects on pain.Second is one looking at genetic
polymorphisms (of cytokine genes) and their associations with pain and opioid
dose (certain polymorphisms in this lung cancer population were associated both
with pain and opioid dose). I'm probably prematurely excited about the growing
trickle of research (in actual real live humans in pain) into the genetic basis
of the variable response to opioids, but there you go.Third, outcome data from a
randomized, placebo controlled trial of modafinil for cancer-related fatigue was
presented.
Patients were all initiating chemotherapy, and those who reported severe fatigue
(but not mild or moderate) seemed to benefit from modafinil over placebo. The
magnitude of the benefit, while statistically significant, is unclear from the
abstract. I've used modafinil occasionally, with (of course) mixed results;
these are the first placebo controlled data I've seen on it in our population.
I'm curious as to readers' experience with it. Newstex ID: PALL-0001-26407116
LOAD-DATE: July 3, 2008
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs on Demand®") are solely the author's and not
necessarily the views of Newstex or its re-distributors. Posts from such authors
are provided "AS IS", with no warranties, and confer no rights. The material and
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and should not, in any respect, be relied on as professional advice. No content
on such Blogs on Demand® is "read and approved" before it is posted.
Accordingly, neither Newstex nor its re-distributors make any claims, promises
or guarantees about the accuracy, completeness, or adequacy of the information
contained therein or linked to from such blogs, nor take responsibility for any
aspect of such blog content. All content on Blogs on Demand® shall be
construed as author-based content and commentary. Accordingly, no warranties or
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or anything else offered on such Blogs on Demand®. Reader's comments reflect
their individual opinion and their publication within Blogs on Demand® shall
not infer or connote an endorsement by Newstex or its re-distributors of such
reader's comments or views. Newstex and its re-distributors expressly reserve
the right to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2008 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2008 Pallimed
233 of 998 DOCUMENTS
Family Practice News
July 1, 2008
Modafinil Reduces Severe Cancer-Related Fatigue
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 45 Vol. 38 No. 13 ISSN: 0300-7073
LENGTH: 307 words
CHICAGO - The wakefulness-promoting drug modafinil (Provigil) reduced
self-reported severe fatigue, according to a study presented at the annual
meeting of the American Society of Clinical Oncology.
Gary R. Morrow, Ph.D., of the University of Rochester (N.Y.) and his
colleagues randomized 631 patients undergoing four cycles of chemotherapy to
receive either 200 mg modafinil daily or placebo. Among those with severe
fatigue at baseline, patients on modafinil had significantly greater reductions
in fatigue, compared with those on placebo.
The subjects were asked to rate their level of fatigue at baseline (during
the second cycle of chemotherapy) and during the final cycle. They rated fatigue
on a 10-point scale: mild (1-4), moderate (5-6), and severe (7-10). A total of
67 patients reported mild fatigue at baseline; 106 and 458 reported moderate and
severe fatigue, respectively.
In patients with mild and moderate fatigue, modafinil also reduced fatigue,
compared with placebo, but the differences were not significant.
Modafinil, a nonamphetamine stimulant, is indicated for the treatment of
excessive sleepiness resulting from obstructive sleep apnea, shift-work, and
narcolepsy. Last year, researchers also at the University of Rochester reported
success with modafinil in treating "chemo brain," a reduction in cognitive
function associated with chemotherapy.
There may be some overlap between chemo brain and fatigue. Problems with
executive function are commonly described in chemo brain. Cancer-related fatigue
appears to particularly affect tasks associated with executive function. Cancer
patients often complain of not being able to do things they know they should do,
Dr. Morrow said.
Cephalon Inc. provided modafinil and placebo for the trial. Dr. Morrow said
he has no relevant financial relationships.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
234 of 998 DOCUMENTS
Ob/Gyn. News
June 15, 2008
Modafinil May Cut Fatigue In Patients During Chemo
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 14 Vol. 43 No. 12 ISSN: 0029-7437
LENGTH: 361 words
CHICAGO - The wakefulness-promoting drug modafinil (Provigil) reduced
self-reported severe fatigue, according to a study of more than 600 cancer
patients undergoing chemotherapy that was presented at the annual meeting of the
American Society of Clinical Oncology.
Gary R. Morrow, Ph.D., of the University of Rochester (N.Y.) and his
colleagues randomized 631 patients undergoing four cycles of chemotherapy to
receive either 200 mg modafinil daily or placebo. Among those with severe
fatigue at baseline, patients on modafinil had significantly greater reductions
in fatigue, compared with those on placebo.
Participants were asked to rate their level of fatigue at baseline (during
the second cycle of chemotherapy) and during the final cycle. They rated fatigue
on a 10-point scale: mild (1-4), moderate (5-6), and severe (7-10). A total of
67 patients reported mild fatigue at baseline; 106 and 458 reported moderate and
severe fatigue, respectively.
Among patients with mild and moderate fatigue, modafinil also reduced
fatigue, compared with placebo, but the differences were not significant. This
was not surprising, Dr. Morrow said during a press briefing. "With side effects,
quite often the potency of the effect is somewhat dependent on where you began,"
he said.
Modafinil-a nonamphetamine stimulant-is currently indicated for the treatment
of excessive sleepiness resulting from obstructive sleep apnea, shift-work sleep
disorder, and narcolepsy.
Last year, researchers also at the University of Rochester reported success
with modafinil in treating "chemo brain," a reduction in cognitive function that
has been associated with chemotherapy.
There may be some overlap between chemo brain and fatigue, Dr. Morrow said in
an interview. Problems with executive function are commonly described in chemo
brain. Cancer-related fatigue appears to particularly affect tasks associated
with executive function. Cancer patients complain of not being able to "get
around" to doing things they know they should do.
Cephalon Inc. provided modafinil and placebo for the trial. Dr. Morrow
reported that he has no relevant financial relationships.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: OBNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
235 of 998 DOCUMENTS
The Age (Melbourne, Australia)
June 6, 2008 Friday
First Edition
'Smart drugs' need smarter risk-handling;
'What if you could go into Starbucks and ask for your latte with a shot of
(smart drug) modafinil?'
BYLINE: Nick Miller, Health Editor
SECTION: NEWS; Pg. 3
LENGTH: 844 words
"SMART drugs" could be the fluoride of the new millennium, says a visiting
expert.
But they could also be a social scourge as we dope ourselves and our children to
work harder and longer, warned Cambridge University professor Barbara Sahakian,
who is visiting Melbourne for the 2008 Alfred Deakin Lectures.
Academics, students and high-octane executives are already seeking a new
generation of pills that improve cognition, planning skills and memory, with
minimal side effects. "This could be the way of the future," Professor Sahakian
said. "What if you could go into Starbucks and ask for your latte with a shot of
(smart drug) modafinil?"
Other experts have even suggested cognitive enhancers be put in the water
alongside fluoride, she said.
Developed to treat disorders such as narcolepsy or Alzheimer's, some new drugs
were found to improve cognition in normal, healthy people. Those in the know are
buying drugs such as modafinil through under-regulated internet pharmacies, or
friendly doctors who bend strict prescription rules.
They are handed around at conferences and swapped before exams. A recent Nature
magazine survey found one-fifth of its readers had used smart drugs to boost
their concentration or memory.
"We're not always working at our best - young mothers with babies, people
travelling all the time," Professor Sahakian said. "I went to a meeting in
Florida and I said to a colleague 'I'm suffering from jetlag', and he said to me
'would you like some of my modafinil?' A lot of my colleagues (are) using it."
Newer smart drugs are proving safer than predecessors such as Ritalin.
"New drugs such as modafinil have a much lower side effects profile and don't
seem to have a substance abuse potential. It really is something a healthy human
might be tempted to try."
But that temptation can lead to danger. Many people are sourcing smart drugs
from internet pharmacies, unsure what they are getting and without advice about
their effect on existing conditions and medication. "I'm keen to have some kind
of governmental regulatory approach, so people are getting safe and effective
cognitive drugs," Professor Sahakian said.
Beyond medical safety, society might be hurt by smart drugs. "What if some
people can afford cognitive-enhancing drugs, but other people can't?" she said.
"What happens to the work-life balance . . . are we going to improve that using
these drugs, to get a good day's work and come home early? Or are we just going
to work more?"
Professor Sahakian also worries that the focus on "quick fix" pills ignores the
cognitive benefits of exercise and education. On the other hand, these drugs
could keep an ageing population mentally active.
There are at least 40 new cognitive drugs in development, such as "ampakines"
that seem to boost memory. Modafinil is available on Australia's Pharmaceutical
Benefits Scheme when prescribed for severe sleep disorders. The makers warn it
has been associated with severe rashes in children. There may also be unknown
side effects.
"We don't know about the long-term effects (of modafinil) in the developing
brain," Professor Sahakian said. If smart drugs became popular parents would
feel pressure to give them to children, especially if schoolmates used them.
Drug educator Paul Dillon said in the past 12 to 18 months he had noticed a
sharp increase in interest from high school students in drugs that could help
them study.
"I have had quite a substantial number of questions from year 11s and 12s asking
about Ritalin and its effects," he said.
"They say 'a friend is using it to study'. Ritalin has always been used in
non-medical ways, to get a 'buzz', but this is something new. You have to ask
why - is it because of greater pressure to achieve?"
There was a risk, especially with young people, if they didn't get the desired
effect from one pill they would take 10 the next time, he said.
Professor Sahakian delivers tonight's Deakin lecture: www.deakinlectures.net
SMART DRUGS
METHYLPHENIDATE
(Drug names Ritalin, Concerta)
A stimulant commonly used to treat attention deficit disorders and chronic
fatigue.
Healthy users believe it helps them focus on tasks and stay awake.
MODAFINIL
(Drug names Provigil, Modavigil)
Another stimulant with less severe side-effects than Ritalin. Prescribed to
treat severe sleep problems.
Some studies suggest it improves short-term memory, concentration and pattern
recognition.
AMPAKINES
Still experimental, drugs such as CX717 are believed to affect the
neurotransmitter glutamate, possibly improving cognitive function and memory.
PIRACETAM
(Drug names Nootropil, Avigilen)
Normally used to treat alcoholism, dementia or stroke.
May improve memory and learning in healthy people.
ERGOLOID
(Drug names Hydergine, Cicanol)
An anti-dementia treatment believed to promote alertness, memory and cognitive
abilities.
BETA-BLOCKERS
(Propranolol, for example)
An old treatment for high blood pressure, sometimes used to prevent anxiety in
public speakers and musicians.
NOTE: The Age does not condone the use of any of these drugs without a
prescription and appropriate medical advice.
LOAD-DATE: June 5, 2008
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: Cambridge University Professor Barbara Sahakian, who says
emerging "smart" drugs could be the new fluoride or a scourge if misused.
PICTURE: JASON SOUTH
PUBLICATION-TYPE: Newspaper
Copyright 2008 The Age Company Limited
All Rights Reserved
236 of 998 DOCUMENTS
The Age (Melbourne, Australia)
June 6, 2008 Friday
Second Edition
'Smart drugs' need smarter risk-handling;
'What if you could go into Starbucks and ask for your latte with a shot of
(smart drug) modafinil?'
BYLINE: Nick Miller, Health Editor
SECTION: NEWS; Pg. 3
LENGTH: 839 words
"SMART drugs" could be the fluoride of the new millennium, says a visiting
expert.
But they could also be a social scourge as we dope ourselves and our children to
work harder and longer, warned Cambridge University professor Barbara Sahakian,
who is visiting Melbourne for the 2008 Alfred Deakin Lectures.
Academics, students and high-octane executives are already seeking a new
generation of pills that improve cognition, planning skills and memory, with
minimal side effects. "This could be the way of the future," Professor Sahakian
said. "What if you could go into Starbucks and ask for your latte with a shot of
(smart drug) modafinil?"
Other experts have even suggested cognitive enhancers be put in the water
alongside fluoride, she said.
Developed to treat disorders such as narcolepsy or Alzheimer's, some new drugs
were found to improve cognition in healthy people. Those in the know are buying
drugs such as modafinil through under-regulated internet pharmacies, or friendly
doctors who bend strict prescription rules.
They are handed around at conferences and swapped before exams. A recent Nature
magazine survey found one-fifth of its readers had used smart drugs to boost
their concentration or memory.
"We're not always working at our best - young mothers with babies, people
travelling all the time," Professor Sahakian said. "I went to a meeting in
Florida and I said to a colleague 'I'm suffering from jetlag', and he said to me
'would you like some of my modafinil?' A lot of my colleagues (are) using it."
Newer smart drugs are proving safer than predecessors such as Ritalin.
"New drugs such as modafinil have a much lower side effects profile and don't
seem to have a substance abuse potential. It really is something a healthy human
might be tempted to try."
But that temptation can lead to danger. Many people are sourcing smart drugs
from internet pharmacies, unsure what they are getting and without advice about
their effect on existing conditions and medication. "I'm keen to have some kind
of governmental regulatory approach, so people are getting safe and effective
cognitive drugs," Professor Sahakian said.
Beyond medical safety, society might be hurt by smart drugs. "What if some
people can afford cognitive-enhancing drugs, but other people can't?" she said.
"What happens to the work-life balance . . . are we going to improve that using
these drugs, to get a good day's work and come home early? Or are we just going
to work more?"
Professor Sahakian also worries that the focus on "quick fix" pills ignores the
cognitive benefits of exercise and education. On the other hand, these drugs
could keep an ageing population mentally active.
There are at least 40 new cognitive drugs in development, such as "ampakines"
that seem to boost memory. Modafinil is available on Australia's Pharmaceutical
Benefits Scheme when prescribed for severe sleep disorders. The makers warn it
has been associated with severe rashes in children. There may also be unknown
side effects.
"We don't know about the long-term effects (of modafinil) in the developing
brain," Professor Sahakian said. If smart drugs became popular parents would
feel pressure to give them to children, especially if schoolmates used them.
Drug educator Paul Dillon said in the past 12 to 18 months he had noticed a
sharp increase in interest from high school students in drugs that could help
them study.
"I have had quite a substantial number of questions from year 11s and 12s asking
about Ritalin and its effects," he said.
"They say 'a friend is using it to study'. Ritalin has always been used in
non-medical ways, to get a 'buzz', but this is something new. You have to ask
why - is it because of greater pressure to achieve?"
There was a risk, especially with young people, if they didn't get the desired
effect from one pill they would take 10 the next time, he said.
Professor Sahakian delivers tonight's Deakin lecture: www.deakinlectures.net
SMART DRUGS
METHYLPHENIDATE
(Drug names Ritalin, Concerta)
A stimulant commonly used to treat attention deficit disorders and chronic
fatigue.
Healthy users believe it helps them focus on tasks and stay awake.
MODAFINIL
(Drug names Provigil, Modavigil)
Another stimulant with less severe side-effects than Ritalin. Prescribed to
treat severe sleep problems.
Some studies suggest it improves short-term memory, concentration and pattern
recognition.
AMPAKINES
Still experimental, drugs such as CX717 are believed to affect the
neurotransmitter glutamate, possibly improving cognitive function and memory.
PIRACETAM
(Drug names Nootropil, Avigilen)
Normally used to treat alcoholism, dementia or stroke.
May improve memory and learning in healthy people.
ERGOLOID
(Drug names Hydergine, Cicanol)
An anti-dementia treatment believed to promote alertness, memory and cognitive
abilities.
BETA-BLOCKERS
(Propranolol, for example)
An old treatment for high blood pressure, sometimes used to prevent anxiety in
public speakers and musicians.
NOTE: These drugs should not be used without a prescription and appropriate
medical advice.
LOAD-DATE: June 5, 2008
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: Cambridge University Professor Barbara Sahakian, who says
emerging "smart" drugs could be the new fluoride or a scourge if misused.
PICTURE: JASON SOUTH
PUBLICATION-TYPE: Newspaper
Copyright 2008 The Age Company Limited
All Rights Reserved
237 of 998 DOCUMENTS
Clinical Psychiatry News
June 2008
APA Meeting News Modafinil May Keep Weight Gain From Olanzapine to Minimum
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 20 Vol. 36 No. 6 ISSN: 0270-6644
LENGTH: 435 words
WASHINGTON - The wakefulness drug modafinil appears to reduce weight gain
associated with the use of the atypical antipsychotic olanzapine, based on a
study of healthy subjects presented at the annual meeting of the American
Psychiatric Association.
Participants concurrently on olanzapine (Zyprexa) and modafinil (Provigil)
gained roughly half the weight of those on olanzapine and placebo, reported
James Roerig, Pharm.D., of the University of North Dakota, Grand Forks. Dr.
Roerig reported that this study was supported through an investigator-initiated
trial grant from Eli Lilly & Co., maker of olanzapine.
The etiology behind atypical antipsychotic-associated weight gain is unclear.
Olanzapine is known to block the histamine H1 receptor. A significant increase
in AMP-activated protein kinase (AMPK) has been associated with the antagonism
of H1 receptors by olanzapine. AMPK is associated with the control of appetite
and mediation of the effects of leptin and insulin. Modafinil is approved for
the treatment of excessive sleepiness associated with narcolepsy, obstructive
sleep apnea/hypopnea syndrome, and shift work sleep disorder. The mechanism of
action for modafinil is unclear, but research suggests that it acts on receptors
that in turn act on histamine receptors.
For this study, the researchers recruited 50 healthy control volunteers. At
baseline, their weight was recorded and they underwent a feeding laboratory
assessment. All participants were titrated up to 10 mg/day olanzapine over 5
days. They were also randomized to receive placebo or modafinil, titrated to 200
mg/day over 5 days.
Because of adverse events, 10 patients dropped out-which left 20 patients in
each study arm. At the end of 3 weeks, the participants were weighed and
underwent another feeding laboratory assessment.
During the feeding laboratory assessment, participants were given a 550-kcal
breakfast and a 600-kcal lunch. For dinner, they were given a choice of
unlimited amounts of three food items; they were told to eat until they were not
hungry. During the dinner session, patients were assessed for energy intake,
sleepiness, hunger/satiety, and adverse events.
The placebo group showed a significantly greater increase in body mass index
than did the modafinil group, Dr. Roerig said. This difference was significant
at week 1 and until the end of the trial. Likewise, the placebo group gained
more weight (2.67 kg on average) than the modafinil group (1.33 kg on average).
This difference was significant at weeks 1 and 2 but only approached
significance at week 3.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
238 of 998 DOCUMENTS
Clinical Neurology News
June 2008
Modafinil Reduced Severe Fatigue in Cancer Patients
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 11 Vol. 4 No. 6 ISSN: 1553-3212
LENGTH: 381 words
CHICAGO - The wakefulness-promoting drug modafinil (marketed as Provigil)
reduced self-reported severe fatigue, according to a recent study of more than
600 cancer patients who were undergoing chemotherapy.
Gary R. Morrow, Ph.D., of the University of Rochester (N.Y.) and his
colleagues randomized 631 patients undergoing four cycles of chemotherapy to
receive either 200 mg modafinil daily or placebo. Among those with severe
fatigue at baseline, patients on modafinil had significantly greater reductions
in fatigue, compared with those on placebo.
Dr. Morrow presented his study's findings at the annual meeting of the
American Society of Clinical Oncology.
Study participants were asked to rate their level of fatigue at baseline
(during the second cycle of chemotherapy) and during the final cycle.
They rated fatigue on a 10-point scale: mild (1-4), moderate (5-6), and
severe (7-10).
A total of 67 patients reported mild fatigue at baseline; 106 and 458
reported moderate and severe fatigue, respectively.
Among patients with mild and moderate fatigue, modafinil also reduced
fatigue, compared with placebo, but the differences were not significant.
This was not surprising, Dr. Morrow commented during a press briefing.
"With side effects, quite often the potency of the effect is somewhat
dependent on where you began," he said.
Modafinil-a nonamphetamine stimulant-is currently indicated for the treatment
of excessive sleepiness resulting from obstructive sleep apnea, shift-work sleep
disorder, and narcolepsy. Last year, researchers also at the University of
Rochester reported success with modafinil in treating "chemobrain," a reduction
in cognitive function that has been associated with chemotherapy.
There may be some overlap between chemobrain and fatigue, Dr. Morrow said in
an interview. Problems with executive function are commonly described in
chemobrain.
Cancer-related fatigue appears to particularly affect tasks associated with
executive function.
Cancer patients complain of not being able to "get around" to doing things
they know they should do.
The pharmaceutical company Cephalon Inc. provided modafinil and placebo for
the trial.
Dr. Morrow reported that he has no relevant financial relationships to
disclose.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CNNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
239 of 998 DOCUMENTS
The Sunday Times (London)
May 25, 2008
Dopers in the dock
BYLINE: David Walsh, Chief Sports Writer
SECTION: SPORT; Sport; Pg.21
LENGTH: 1148 words
The trial of coach Trevor Graham is revealing just how widespread drugs in
athletics were
How did Michael Johnson feel as he read reports of Antonio Pettigrew's testimony
in a San Francisco courtroom last week? Pettigrew was a witness in the case
against athletics coach Trevor Graham, who is accused of lying to federal
investigators. During his testimony, Pettigrew explained he had been put in
touch with a drug supplier, Angel "Memo" Heredia, by Graham and that he
continued receiving banned substances from Heredia until 2001.
Johnson would have paid attention to Pettigrew's evidence because not only were
they rivals on the track, they raced together on US relay teams. Regarded as the
greatest of all 400m runners, Johnson's final race was the 4x400m relay in
Sydney on September 30, 2000, where he anchored the US team to a clear victory.
Pettigrew ran the second leg in that final and played his part in Johnson
receiving the baton with an insurmountable lead.
By his own admission, Pettigrew was doping at the time. One wonders if Johnson
now feels that the last medal is tainted and unworthy of a place among his
collection of 19 championship golds. The other two members of that 400m relay
team in Sydney were the twins, Calvin and Alvin Harrison, who were given doping
bans in 2004 for offences committed after the 2000 Olympics. Calvin tested
positive for modafinil, a stimulant once used by athletes connected to the Balco
laboratory run by Victor Conte, while Alvin was shown to have used EPO, the
steroid tetrahydro-gestrinone (THG), testosterone, human growth hormone, insulin
and modafinil. Alvin was given a four-year ban and became the first male athlete
to be sanctioned without having failed a drug test.
Johnson will know how this story is likely to unfold. Jim Scherr, chief
executive of the United States Olympic Committee, weighed up Pettigrew's
evidence. "If an athlete who ran in the finals knowingly and purposefully
engaged in cheating, the medals won by the entire team are tarnished and, in our
view, should be returned."
There is a precedent for this sorry episode. At the same 2000 Olympics in
Sydney, the women's 4x400m relay was won by a US team containing Marion Jones,
who has since admitted she doped before the Games. Last month the International
Olympic Committee (IOC) stripped that US team of its medals. They must now do
the same with the US men's team and declare second-placed Nigeria as the gold
medallists.
Johnson never tested positive for doping, nor has he been implicated in any
doping controversy, and since his retirement in 2000 he has been consistently
critical of those who use drugs. What does he now think about the gold he won in
that Sydney relay? At least one of his teammates was cheating at the time and
given how well the Harrisons were running in Sydney, he may wonder if they
started down the doping road before the 2000 Olympics. The bottom line is clear:
that 4x400m gold medal is tarnished and worthless. The only good that can come
from this is that by returning it, Johnson can say he wants nothing to do with
any award or victory achieved with the help of drugs. It would be nice, too, if
the 400m world record-holder returned that medal voluntarily, before the IOC
order him to.
Of course, the International Association of Athletics Federations (IAAF) and the
IOC dislike talk of medals being returned and history being rewritten because
there is no end to the problem. If all doping-affected results were re-evaluated
and the cheats removed, there would be no time to organise the Games. When the
IOC decided to strip the US women of their medals in the 4x100m and 4x400m
relays (Jones was also in the 4x100m relay team) from the Sydney Olympics, they
took a decision that involved more than 30 athletes in a process that would see
some lose their medals, others change the colour of theirs and still others
receive medals more than seven years after they had missed out.
Three months before the start of the Beijing Olympics, the Graham trial is the
last thing sports officials wanted. The Balco investigation is continuing to do
significant damage to sport's battered image. It is not just athletics that has
suffered in the fallout to the Balco investigation but also baseball and
American football.
Such was the cynicism that underpinned Conte's operation and the sheer scale of
his doping programme that the investigation was always going to have serious
consequences, but the situation has been exacerbated by athletes and their
coaches believing they could tell the same lies to federal investigators that
for years they have been telling to the public. That is why Jones ended up in
prison, why the US cyclist Tammy Thomas awaits sentencing after her perjury
conviction, why Graham is facing perjury charges.
Graham's case is typical. He has been one of America's most successful track
coaches and when it was discovered he was the person who tipped off US anti
doping authorities about Conte's operation in San Francisco, he was praised for
what seemed a strong anti-doping statement. But during the course of the Balco
investigation, federal agents received information that suggested Graham was
helping his athletes to dope.
They interviewed him and agreed to his request for immunity from prosecution
provided he was truthful. According to his testimony, Graham was never involved
in doping. After speaking with other witnesses, in particular the Mexican-born
steroid dealer Heredia, the investigators concluded that Graham had lied and
charged him with perjury. For the first four days of last week, a jury in San
Francisco heard the case against Graham and it was substantial. He had told the
government investigators he had never met Heredia and had not spoken to him on
the phone since 1997. A photograph showed Heredia and Graham together in
Heredia's apartment in 1996, and phone records indicated Graham had spoken more
than 100 times to the supplier since 1997.
If the prosecution's case against Graham rested solely on Heredia's evidence, it
would be difficult to prove because Heredia supplied drugs to many athletes and
was not truthful in his initial interview with federal officers. The case
against Graham, however, rests as much on the testimony of his former athletes.
Pettigrew testified that Graham suggested he should consider using EPO and human
growth hormone and that he would introduce him to a supplier Heredia), while
Jerome Young, also a member of America's tarnished 4x400m team at the 2000
Olympics, told the court Graham introduced him to EPO. Dennis Mitchell, who won
4x100m gold for America at the 1992 Olympics, testified that Graham injected him
with human growth hormone and Duane Ross, a retired American hurdler, said he
fell out with Graham because he refused to use performance-enhancing drugs.
The case resumes on Tuesday.
LOAD-DATE: May 26, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: st
Copyright 2008 Times Newspapers Limited
All Rights Reserved
240 of 998 DOCUMENTS
Canadian Corporate Newswire
May 12, 2008 Monday 11:13 PM EST
Get a Deep Insight into the Sleep Disorders Market Analysis 2008-2018
LENGTH: 2262 words
LONDON, UNITED KINGDOM--(Marketwire - May 12, 2008) - Reportlinker.com
announces that a new market research report related to the Pharmaceutical
industry industry is available in its catalogue.
Sleep Disorders Market Analysis 2008-2018
http://www.reportlinker.com/p089492/Sleep-Disorders-Market-Analysis-2008-201
8.html
More than 80 sleep disorders have been identified. They affect over 200 million
people worldwide. The report focuses on the market for following sleep
disorders:
- Insomnia
- Restless legs syndrome (RLS)
- Narcolepsy and
- Obstructive Sleep Apnoea / Hypopnea Syndrome (OSAHS)
The market penetration for insomnia drugs has not reached saturation point.
Opportunities remain. But with the introduction of several new products the
market is set to see changes, but expansion. This expansion is based on
increased general awareness physicians better comprehension of the significance
of this disease and the positive role that a sleep medication prescription
plays.
At present time there are several prescription sleeping medications available
to treat insomnia. The market-focus has been driven by the production of sleep
medications with less side-effects and danger of overdose. Prescription
benzodiazepines and newer non-benzodiazepine hypnotics developed in the 1990s,
such as Imovane, Ambien and Sonata will continue to be the most prescribed.
Benzodiazepines are widely used to treat an underlying neurological disorder
which is often the underlying cause of insomnia, e.g. anxiety and depression.
Visiongain predicts that market share by volume for insomnia in the US will
change significantly from 2008 to 2018. Ambien IR lost its patent protection in
April 2007, which opened to generic competition for Zolpidem. Ambien will
remain the market leader for the short term, but what will over take it? A
generic version of Ambien is expected to achieve strong market share by volume
as there is a great demand for zolpidem tartrate for insomnia.
The market share for insomnia treatment will gradually rise after 2012, which
will be due to:
- Market expansion of existing expensive medications into Europe and Japan in
particular
- Market penetration of new medications currently in pipeline.
Other drugs dealt with in this report include:
- Modafinil (Provigil) is the first in a new class of wake-promoting drugs and
is currently approved in more than 20 countries for the treatment of excessive
daytime sleepiness associated with narcolepsy. Provigil is quickly replacing
Ritalin, and other CNS stimulants, as the medication of choice for treating
daytime sleepiness in narcolepsy. The FDA granted modafinil (Provigil) orphan
drug status in 1993. Modafinil was initially launched in the US in 1999 for the
treatment of narcolepsy. In 2004, modafinil became FDA-approved prescription
medicine for the treatment of excessive sleepiness associated with Obstructive
Sleep Apnoea/Hypopnea Syndrome (OSAHS) and Shift Workers Sleep Disorder (SWSD).
- Requip (ropinirole) became the first and only FDA-approved drug treatment for
moderate to severe primary Restless Legs Syndrome (RLS) in 2005.
Key findings that will broaden the scope of the sleep disorders market:
- Over the next decade, the development and improvement of sleep disorders
therapies will primarily depend on the success of burgeoning technology and
innovative approaches.
- It is possible to purchase prescription medications online without producing
a prescription. Purchase of online sleep medications has increased and will
continue to evolve over the next years.
- The impact of DTC advertising has created an improved awareness of available
insomnia treatment. This is likely to increase as DTC advertising continues to
prosper and the culture becomes more accepting towards insomnia treatment.
Visiongain expects the market for sleep disorders to increase, driven by a
growing awareness of sleep disorders and by campaigns to promote sleep
medications, both by DTC advertising and consumer education. The relaxation of
DTC marketing restrictions in the 1990s in the US set the stage for a flow for
both branded and unbranded advertising and promotional programmes. Those
regulations are prompting more responsible DTC advertising on the industry's
part.
- The FDA has requested that all manufacturers of sedative-hypnotic drug
products, a class of drugs used to induce and/or maintain sleep, strengthen
their product labelling to include stronger warnings concerning potential
risks.
- The Committee for Medicinal Products in Human Use (CHMP) of the European
Medicines Agency (EMEA) approved Neurim's Circadin a prolonged-release
melatonin as monotherapy for the short-term treatment of primary insomnia
characterised by poor quality of sleep in patients aged 55 or over. Neurim is
actively seeking strategic alliances for the major European markets.
What questions does the report answer?
- Which current or future therapies will drive the sleep disorders market from
2008 to 2018?
- The key companies involved in the market and their analysis?
- What is the patient identification rate for each of the therapeutic areas?
- What is the present state of the disease awareness?
- What R&D opportunities exist for 'new comers'?
Why should you buy this report?
- This report focuses on the marketed medications and the pipeline development
for sleep disorders from 2008 to 2018. It also discusses the strength and
weakness of products, along with the opportunities and threats facing the
market.
- The report describes world market situation for sleep disorders, namely
insomnia, narcolepsy, RLS and OSAHS, with forecasts made for all key products.
It also describes the insomnia market situation in the seven major world
markets for sleep medications: the US, Japan, France, Germany, Italy, Spain and
the UK, with forecasts for key products.
- The report provides transcripts of visiongain's interviews with experts in
the field of sleep disorders, which reviews the future direction of the sleep
disorders treatment market.
Unique benefits to you when you order this report
- You can access your report whichever country you are in without using
harddrive space
- Primary research throughout. You will not find this information anywhere else
- Full searchable report when you buy the company or corporate editions
- Copies can be printed off for offline reading
- Packed with charts, analysis, figures, graphs and table
Please Note: Reports are sold based on the user licenses indicated. The
Publisher delivers the report in Flash format via the publisher website,
allowing viewing and printing capabilities only. Within one to two business
days after placing the order, the Publisher will email the client with
information on accessing their purchase. Prior to initiating fulfillment of an
order, the client will be required to sign a document detailing the purchase
terms for a publication from this publisher.
1 Executive Summary: Pharmaceutical Treatment of Sleep Disorders 2008-2018
1.1 Current Prospects of Sleep Disorders Market
1.1.1 Market Growth Estimate
1.1.2 Generic Pharmaceutical Market
1.1.3 Market Expansion
1.1.4 Market Demand for Short Elimination Half-Life
1.1.5 Medications Targeting M1 and M2 Receptors
1.1.6 Medications Targeting 5HT2A Receptor Receptors
1.1.7 Product Line Extension Activities
1.1.8 Effect of Direct-To-Consumer Advertising (DTCA)
1.1.9 Safety Measures for Online Consumers
1.2 Aim, Scope, and Format Of This Report
2 Introduction to Sleep Disorders and their Pharmaceutical Treatment
2.1 Introduction to Sleep Disorders
2.2 Overview of Chapter
2.3 Introduction to Insomnia
2.4 Discovery of Barbiturates
2.5 Market Entry for Non-Barbiturates
2.6 Arrival of Benzodiazepines
2.7 Non-benzodiazepines the Revolutionary Compound
2.7.1 Prescription Medicines and OTCs
2.8 Pharmacodynamics of Hypnotics
2.9 Introducing New Scope for Insomnia
2.10 Many Forms of Sleep Disturbances
2.10.1 Sleep Deprivation
2.11 Shift Workers Sleep Disorder (SWSD)
2.11.1 Melatonin
2.11.2 Valerian
2.12 Treatment for insomnia in Depression
2.13 Restless Legs Syndrome
2.13.1 Off-label Prescription for Restless Legs Syndrome
2.14 Other Medical Conditions
2.15 Narcolepsy
2.15.1 Xyrem for Cataplexy
2.15.2 Orphan Disease Status
2.15.3 Other Medications for Cataplexy
2.16 Obstructive Sleep Apnea / Hypopnea Syndrome (OSAHS)
2.17 Insomnia - A Common Disease
2.18 Patient Identification Rate
3 Analysis of Current Market for Insomnia
3.1 Market Share for World Insomnia Market
3.2 Market Dominance Continues for Ambien
3.3 Lunesta as Ambien's Contender
3.4 Sonata Continues to Form Niche Market
3.5 Imovane / Amoban Go Down in Insomnia Market
3.6 Benzodiazepines Survived as Low Priced Sleep Aid
3.6.1 Lendormin (brotizolam)
3.6.2 Halcion (triazolam)
3.6.3 Noctamid (Lormetazepam)
3.6.4 Doral (quazepam)
3.6.5 Dalmane (flurazepam)
3.6.6 Rohypnol (flunitrazepam)
3.6.7 Restoril (temazepam)
3.6.8 Eurodin or ProSom (estazolam)
3.6.9 Rhythmy (rilmazafone)
3.6.10 Rhythmy (rilmazafone)
3.6.10 Valium (diazepam)
3.7 Rozerem Market Up-and-Coming
4 Insomnia Market Analysis by World Regions
4.1 US has the Highest Market Share for Insomnia Treatments
4.2 Europe as a Significant Market for Insomnia Treatments
4.3 The Japanese Market for Insomnia is Expanding
5 Market Developments for Narcolepsy, Shift Work Sleep Disorder, and
Restless Legs Syndrome
5.1 Provigil Wins Label Extension
5.2 Adrafinil is a Isomer of Provigil
5.3 Ritalin/ Ritalin SR
5.4 Concerta is an Extension Version of Ritalin
5.5 Adderall as Stimulant
5.6 Xyrem for Cataplexy and Excessive Daytime Sleepiness
5.7 Recent FDA Activities for Restless Legs Syndrome
6 Products in Development for Sleep Disorders
6.1 FDA Approves Generic Ambien
6.2 Circadin a Prolonged-Release Melatonin
6.3 GHB analogue Generally Regarded as Safe
6.4 Clinical Trial Product List for Insomnia
6.5 Indiplon for Insomnia in Pre-Registration Stage
6.6 Caraco's Prospect in Narcolepsy Market
6.7 Lundbeck Faces Setback in Insomnia Market
6.8 Phase III Trial Begins on Posidorm for Insomnia
6.9 Hope for Physiological Sleep with Almorexant
6.10 5HT2A Antagonist for Insomnia
6.11 Agonist at the Serotonin 5-HT1A Receptor
6.12 VEC-162 Future Contender for Rozerem
6.13 Zolpidem as Oral Spray
6.14 Cephalon Adds Nuvigil Alongside Provigil
6.15 Dopamine Patch for RLS
6.16 Transported Prodrug of Gabapentin
7 Recommendations for Ideal Pharmaceutical Treatment for Sleep Disorders
7.1 Firsthand Interview for Expert Opinion 1
7.1.1 Prospect for Sleep Disorders Market
7.1.2 Prospect for Generic Market
7.1.3 Product Line Extension
7.1.4 Prospect for Niche Market
7.1.5 Future of Benzodiazepines Market
7.1.6 Future of Controlled Drug Market
7.1.7 Effect of Direct-to-Consumer Market
7.1.8 Future of Non-Hypnotics Medications
7.1.9 Future Medications for Sleep Apnoea
7.1.10 Prospect for Hypnotics as OTCs
7.1.12 Unmet Needs for Sleep Disorders Market
7.2 Firsthand Interview for Expert Opinion 2
7.2.1 Drug Therapies for the Future
7.2.2 Technological Advance in Sleep Disorders Treatment
7.2.3 New Effective Sleep Medications
7.2.4 Future of Sleep Disorders Market in the Developed Nations
7.2.5 Unmet Needs for Sleep Disorders Treatment
7.2.6 Favourable Medication for the Coming Decade
7.2.7 Side-Effect Profile for Future Drug Development
7.2.8 Sleep Disorders Market in Developing Nations
8 Market Force and Limitation of Sleep Disorders Market
8.1 Table for SWOT Analysis of Sleep Disorders Market
8.2 Market Analysis of Products Unapproved for Sleep Disorders by
Regulatory Bodies and Niche Market
8.2.1 Unapproved Insomnia Medications: Benadryl,
Unisom, Tylenol PM, Nytol
8.2.3 Purchase of Prescription Medications Online
8.3 Drug Safety Issues and Side-Effects of Drugs
8.3.1 Hypnotics are not Without Side-Effects
8.3.2 Labelling to include Potential Risks
8.3.3 Rohypnol and Xyrem have Potential for Abuse
8.4.4 Consumer Led Campaign
8.4 Unmet needs of Pharmaceutical Treatment for Sleep Disorders
8.5 Non-product Related Drivers and Restraints
8.5.1 National Policies Recommendations
8.5.2 National Policies Advising Prescription of Particular Drugs
8.5.3 Agreed Guidelines
8.5.4 Market Status Quo
8.6 Success of Direct-to-Consumer Advertising
9 Conclusions
9.1 Insomnia Market Will Show High Growth
9.2 Other Sleep Disorders of Interest
9.3 Life-Cycle Management
9.4 New Markets
More Details
Organisations mentioned in the report
Abbott
Actelion
Alliance
American Insomnia Association
Andx
Apotex
Arena
Astellas
Avant
Aventis
Bayer
Boehringer Ingelheim
Caraco
Carlsbad
Cephalon
Dr. Reddy's
Elan
Eli Lilly
Drug Enforcement Administration (DEA)
European Patent Office
FDA
Genpharm
GlaxoSmithKline
Hoffman-Roche
Hypnion
Ipsen
Johnson & Johnson
King
Lek
Lundbeck
Mallinckrodt
Merck
Mutual
MHRA
Mylan
National Sleep Foundation
NCSDR
Neurim
Neurocrine
Neurogen
NHLBI
NICE
NIH
NovaDel
Novartis
Orphan
Pfizer
Pharmaceutical Researchers and Manufacturers of America (PhRMA)
Questcor
Ranbaxy
Roche
Rhone-Poulenc Rorer
Roxane
Royal Pharmaceutical Society of Great Britain (RPSGB)
Sanofi-Aventis
Schering-Plough
Sepracor
Shionogi
Shire
Skye
Synthon
Takeda
Teva
Tikvah
UCB
Valeant
Vanda
Watson
Wyeth
XenoPort
To order this report:
Sleep Disorders Market Analysis 2008-2018
http://www.reportlinker.com/p089492/Sleep-Disorders-Market-Analysis-2008-201
8.html
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FOR FURTHER INFORMATION PLEASE CONTACT:
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(718) 887-3024
Email: nbo@reportlinker.com
Healthcare - Healthcare, Medical and Healthcare - Surgery and Treatments
LOAD-DATE: May 12, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 PIMS Canada, Inc., doing business as CCNMatthews
All Rights Reserved
241 of 998 DOCUMENTS
Market Wire
May 12, 2008 Monday 8:12 PM GMT
Get a Deep Insight into the Sleep Disorders Market Analysis 2008-2018
LENGTH: 2222 words
DATELINE: LONDON, UNITED KINGDOM; May 12, 2008
Reportlinker.com announces that a new market research report related to the
Pharmaceutical industry industry is available in its catalogue.
Sleep Disorders Market Analysis 2008-2018
http://www.reportlinker.com/p089492/Sleep-Disorders-Market-Analysis-2008-2018.ht
ml
More than 80 sleep disorders have been identified. They affect over 200 million
people worldwide. The report focuses on the market for following sleep
disorders:
- Insomnia
- Restless legs syndrome (RLS)
- Narcolepsy and
- Obstructive Sleep Apnoea / Hypopnea Syndrome (OSAHS)
The market penetration for insomnia drugs has not reached saturation point.
Opportunities remain. But with the introduction of several new products the
market is set to see changes, but expansion. This expansion is based on
increased general awareness physicians better comprehension of the significance
of this disease and the positive role that a sleep medication prescription
plays.
At present time there are several prescription sleeping medications available to
treat insomnia. The market-focus has been driven by the production of sleep
medications with less side-effects and danger of overdose. Prescription
benzodiazepines and newer non-benzodiazepine hypnotics developed in the 1990s,
such as Imovane, Ambien and Sonata will continue to be the most prescribed.
Benzodiazepines are widely used to treat an underlying neurological disorder
which is often the underlying cause of insomnia, e.g. anxiety and depression.
Visiongain predicts that market share by volume for insomnia in the US will
change significantly from 2008 to 2018. Ambien IR lost its patent protection in
April 2007, which opened to generic competition for Zolpidem. Ambien will remain
the market leader for the short term, but what will over take it? A generic
version of Ambien is expected to achieve strong market share by volume as there
is a great demand for zolpidem tartrate for insomnia.
The market share for insomnia treatment will gradually rise after 2012, which
will be due to:
- Market expansion of existing expensive medications into Europe and Japan in
particular
- Market penetration of new medications currently in pipeline.
Other drugs dealt with in this report include:
- Modafinil (Provigil) is the first in a new class of wake-promoting drugs and
is currently approved in more than 20 countries for the treatment of excessive
daytime sleepiness associated with narcolepsy. Provigil is quickly replacing
Ritalin, and other CNS stimulants, as the medication of choice for treating
daytime sleepiness in narcolepsy. The FDA granted modafinil (Provigil) orphan
drug status in 1993. Modafinil was initially launched in the US in 1999 for the
treatment of narcolepsy. In 2004, modafinil became FDA-approved prescription
medicine for the treatment of excessive sleepiness associated with Obstructive
Sleep Apnoea/Hypopnea Syndrome (OSAHS) and Shift Workers Sleep Disorder (SWSD).
- Requip (ropinirole) became the first and only FDA-approved drug treatment for
moderate to severe primary Restless Legs Syndrome (RLS) in 2005.
Key findings that will broaden the scope of the sleep disorders market:
- Over the next decade, the development and improvement of sleep disorders
therapies will primarily depend on the success of burgeoning technology and
innovative approaches.
- It is possible to purchase prescription medications online without producing a
prescription. Purchase of online sleep medications has increased and will
continue to evolve over the next years.
- The impact of DTC advertising has created an improved awareness of available
insomnia treatment. This is likely to increase as DTC advertising continues to
prosper and the culture becomes more accepting towards insomnia treatment.
Visiongain expects the market for sleep disorders to increase, driven by a
growing awareness of sleep disorders and by campaigns to promote sleep
medications, both by DTC advertising and consumer education. The relaxation of
DTC marketing restrictions in the 1990s in the US set the stage for a flow for
both branded and unbranded advertising and promotional programmes. Those
regulations are prompting more responsible DTC advertising on the industry's
part.
- The FDA has requested that all manufacturers of sedative-hypnotic drug
products, a class of drugs used to induce and/or maintain sleep, strengthen
their product labelling to include stronger warnings concerning potential risks.
- The Committee for Medicinal Products in Human Use (CHMP) of the European
Medicines Agency (EMEA) approved Neurim's Circadin a prolonged-release melatonin
as monotherapy for the short-term treatment of primary insomnia characterised by
poor quality of sleep in patients aged 55 or over. Neurim is actively seeking
strategic alliances for the major European markets.
What questions does the report answer?
- Which current or future therapies will drive the sleep disorders market from
2008 to 2018?
- The key companies involved in the market and their analysis?
- What is the patient identification rate for each of the therapeutic areas?
- What is the present state of the disease awareness?
- What R&D opportunities exist for 'new comers'?
Why should you buy this report?
- This report focuses on the marketed medications and the pipeline development
for sleep disorders from 2008 to 2018. It also discusses the strength and
weakness of products, along with the opportunities and threats facing the
market.
- The report describes world market situation for sleep disorders, namely
insomnia, narcolepsy, RLS and OSAHS, with forecasts made for all key products.
It also describes the insomnia market situation in the seven major world markets
for sleep medications: the US, Japan, France, Germany, Italy, Spain and the UK,
with forecasts for key products.
- The report provides transcripts of visiongain's interviews with experts in the
field of sleep disorders, which reviews the future direction of the sleep
disorders treatment market.
Unique benefits to you when you order this report
- You can access your report whichever country you are in without using
harddrive space
- Primary research throughout. You will not find this information anywhere else
- Full searchable report when you buy the company or corporate editions
- Copies can be printed off for offline reading
- Packed with charts, analysis, figures, graphs and table
Please Note: Reports are sold based on the user licenses indicated. The
Publisher delivers the report in Flash format via the publisher website,
allowing viewing and printing capabilities only. Within one to two business days
after placing the order, the Publisher will email the client with information on
accessing their purchase. Prior to initiating fulfillment of an order, the
client will be required to sign a document detailing the purchase terms for a
publication from this publisher.
1 Executive Summary: Pharmaceutical Treatment of Sleep Disorders 2008-2018
1.1 Current Prospects of Sleep Disorders Market
1.1.1 Market Growth Estimate
1.1.2 Generic Pharmaceutical Market
1.1.3 Market Expansion
1.1.4 Market Demand for Short Elimination Half-Life
1.1.5 Medications Targeting M1 and M2 Receptors
1.1.6 Medications Targeting 5HT2A Receptor Receptors
1.1.7 Product Line Extension Activities
1.1.8 Effect of Direct-To-Consumer Advertising (DTCA)
1.1.9 Safety Measures for Online Consumers
1.2 Aim, Scope, and Format Of This Report
2 Introduction to Sleep Disorders and their Pharmaceutical Treatment
2.1 Introduction to Sleep Disorders
2.2 Overview of Chapter
2.3 Introduction to Insomnia
2.4 Discovery of Barbiturates
2.5 Market Entry for Non-Barbiturates
2.6 Arrival of Benzodiazepines
2.7 Non-benzodiazepines the Revolutionary Compound
2.7.1 Prescription Medicines and OTCs
2.8 Pharmacodynamics of Hypnotics
2.9 Introducing New Scope for Insomnia
2.10 Many Forms of Sleep Disturbances
2.10.1 Sleep Deprivation
2.11 Shift Workers Sleep Disorder (SWSD)
2.11.1 Melatonin
2.11.2 Valerian
2.12 Treatment for insomnia in Depression
2.13 Restless Legs Syndrome
2.13.1 Off-label Prescription for Restless Legs Syndrome
2.14 Other Medical Conditions
2.15 Narcolepsy
2.15.1 Xyrem for Cataplexy
2.15.2 Orphan Disease Status
2.15.3 Other Medications for Cataplexy
2.16 Obstructive Sleep Apnea / Hypopnea Syndrome (OSAHS)
2.17 Insomnia - A Common Disease
2.18 Patient Identification Rate
3 Analysis of Current Market for Insomnia
3.1 Market Share for World Insomnia Market
3.2 Market Dominance Continues for Ambien
3.3 Lunesta as Ambien's Contender
3.4 Sonata Continues to Form Niche Market
3.5 Imovane / Amoban Go Down in Insomnia Market
3.6 Benzodiazepines Survived as Low Priced Sleep Aid
3.6.1 Lendormin (brotizolam)
3.6.2 Halcion (triazolam)
3.6.3 Noctamid (Lormetazepam)
3.6.4 Doral (quazepam)
3.6.5 Dalmane (flurazepam)
3.6.6 Rohypnol (flunitrazepam)
3.6.7 Restoril (temazepam)
3.6.8 Eurodin or ProSom (estazolam)
3.6.9 Rhythmy (rilmazafone)
3.6.10 Rhythmy (rilmazafone)
3.6.10 Valium (diazepam)
3.7 Rozerem Market Up-and-Coming
4 Insomnia Market Analysis by World Regions
4.1 US has the Highest Market Share for Insomnia Treatments
4.2 Europe as a Significant Market for Insomnia Treatments
4.3 The Japanese Market for Insomnia is Expanding
5 Market Developments for Narcolepsy, Shift Work Sleep Disorder, and
Restless Legs Syndrome
5.1 Provigil Wins Label Extension
5.2 Adrafinil is a Isomer of Provigil
5.3 Ritalin/ Ritalin SR
5.4 Concerta is an Extension Version of Ritalin
5.5 Adderall as Stimulant
5.6 Xyrem for Cataplexy and Excessive Daytime Sleepiness
5.7 Recent FDA Activities for Restless Legs Syndrome
6 Products in Development for Sleep Disorders
6.1 FDA Approves Generic Ambien6.2 Circadin a Prolonged-Release Melatonin
6.3 GHB analogue Generally Regarded as Safe
6.4 Clinical Trial Product List for Insomnia
6.5 Indiplon for Insomnia in Pre-Registration Stage
6.6 Caraco's Prospect in Narcolepsy Market
6.7 Lundbeck Faces Setback in Insomnia Market
6.8 Phase III Trial Begins on Posidorm for Insomnia
6.9 Hope for Physiological Sleep with Almorexant
6.10 5HT2A Antagonist for Insomnia
6.11 Agonist at the Serotonin 5-HT1A Receptor
6.12 VEC-162 Future Contender for Rozerem
6.13 Zolpidem as Oral Spray
6.14 Cephalon Adds Nuvigil Alongside Provigil
6.15 Dopamine Patch for RLS
6.16 Transported Prodrug of Gabapentin
7 Recommendations for Ideal Pharmaceutical Treatment for Sleep Disorders
7.1 Firsthand Interview for Expert Opinion 1
7.1.1 Prospect for Sleep Disorders Market
7.1.2 Prospect for Generic Market
7.1.3 Product Line Extension
7.1.4 Prospect for Niche Market
7.1.5 Future of Benzodiazepines Market
7.1.6 Future of Controlled Drug Market
7.1.7 Effect of Direct-to-Consumer Market
7.1.8 Future of Non-Hypnotics Medications
7.1.9 Future Medications for Sleep Apnoea
7.1.10 Prospect for Hypnotics as OTCs
7.1.12 Unmet Needs for Sleep Disorders Market
7.2 Firsthand Interview for Expert Opinion 2
7.2.1 Drug Therapies for the Future
7.2.2 Technological Advance in Sleep Disorders Treatment
7.2.3 New Effective Sleep Medications
7.2.4 Future of Sleep Disorders Market in the Developed Nations
7.2.5 Unmet Needs for Sleep Disorders Treatment
7.2.6 Favourable Medication for the Coming Decade
7.2.7 Side-Effect Profile for Future Drug Development
7.2.8 Sleep Disorders Market in Developing Nations
8 Market Force and Limitation of Sleep Disorders Market
8.1 Table for SWOT Analysis of Sleep Disorders Market
8.2 Market Analysis of Products Unapproved for Sleep Disorders by
Regulatory Bodies and Niche Market
8.2.1 Unapproved Insomnia Medications: Benadryl,
Unisom, Tylenol PM, Nytol
8.2.3 Purchase of Prescription Medications Online
8.3 Drug Safety Issues and Side-Effects of Drugs
8.3.1 Hypnotics are not Without Side-Effects
8.3.2 Labelling to include Potential Risks
8.3.3 Rohypnol and Xyrem have Potential for Abuse
8.4.4 Consumer Led Campaign
8.4 Unmet needs of Pharmaceutical Treatment for Sleep Disorders
8.5 Non-product Related Drivers and Restraints
8.5.1 National Policies Recommendations
8.5.2 National Policies Advising Prescription of Particular Drugs
8.5.3 Agreed Guidelines
8.5.4 Market Status Quo
8.6 Success of Direct-to-Consumer Advertising
9 Conclusions
9.1 Insomnia Market Will Show High Growth
9.2 Other Sleep Disorders of Interest
9.3 Life-Cycle Management
9.4 New Markets
More Details
Organisations mentioned in the report
Abbott
Actelion
Alliance
American Insomnia Association
Andx
Apotex
Arena
Astellas
Avant
Aventis
Bayer
Boehringer Ingelheim
Caraco
Carlsbad
Cephalon
Dr. Reddy's
Elan
Eli Lilly
Drug Enforcement Administration (DEA)
European Patent Office
FDA
Genpharm
GlaxoSmithKline
Hoffman-Roche
Hypnion
Ipsen
Johnson & Johnson
King
Lek
Lundbeck
Mallinckrodt
Merck
Mutual
MHRA
Mylan
National Sleep Foundation
NCSDR
Neurim
Neurocrine
Neurogen
NHLBI
NICE
NIH
NovaDel
Novartis
Orphan
Pfizer
Pharmaceutical Researchers and Manufacturers of America (PhRMA)
Questcor
Ranbaxy
Roche
Rhone-Poulenc Rorer
Roxane
Royal Pharmaceutical Society of Great Britain (RPSGB)
Sanofi-Aventis
Schering-Plough
Sepracor
Shionogi
Shire
Skye
Synthon
Takeda
Teva
Tikvah
UCB
Valeant
Vanda
Watson
Wyeth
XenoPort
To order this report:
Sleep Disorders Market Analysis 2008-2018
http://www.reportlinker.com/p089492/Sleep-Disorders-Market-Analysis-2008-2018.ht
ml
More market research reports here!
Contacts:
Reportlinker.com
Nicolas
(718) 887-3024
Email: nbo@reportlinker.com
SOURCE: Reportlinker.com
LOAD-DATE: May 13, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 Market Wire, Incorporated
All Rights Reserved
242 of 998 DOCUMENTS
The Evening Standard (London)
May 6, 2008 Tuesday
Can a pill boost your brain?;
They call it Viagra for the mind. Modafinil is a drug designed for narcoleptics
that's now being abused by students to improve their memories - and their IQs.
This is what happened when our writer took it for a fortnight ...
BYLINE: JOHANN HARI
SECTION: A; Pg. 22
LENGTH: 1572 words
SOME time in March, in the drizzle, I realised my brain was burned out. Like a
rusty engine, I could hear it chug-chug and splutter but it would never quite
run at top speed. I had just come back from a month-long worktrip to Bangladesh,
and I had an Everest of work in front of me. It was all fascinating and urgent
but I was plodding though it at half my normal speed. I needed to be performing
at my best; instead, I was at my worst. I stared at the London rain and slogged
on.
That's when I stumbled across a small story in an American scientific magazine.
It said there was a spiky debate across America's universities about the
increasing use by students of a drug called modafinil. It was, they said, Viagra
for the brain. Originally designed for narcoleptics in the Seventies, clinical
trials had uncovered something odd: if you give it to non-narcoleptics, they
just become smarter. Their memory and concentration improve, as does their IQ.
It's not an amphetamine or a stimulant, the article explained. It doesn't make
you high, or wired. It seems to work by restricting the parts of your brain that
make you sluggish or sleepy. No significant negative effects have been
discovered.
Now students are using it in the run-up to exams as a "smart drug" a steroid for
the mind.
It sounded perfect. A few clicks online and I found I could order it from a
foreign pharmacy, for just £30 for a month's supply.
I called a friend who is a GP; she'd heard of people using the drug, and went
away and looked up the details. "I think it's a stupid thing to do because you
shouldn't ever take drugs you don't need," she said when she called back. "Do I
think it'll seriously harm you? No, I don't. But you'd be much better off taking
a long holiday than narcolepsy pills." Then she warned me: "There is one known
side-effect." Oh damn, I thought.
A downside. "It often causes people to lose weight." Are you mad? You become
cleverer and thinner? I whipped out my Visa card immediately.
A week later, the little white pills arrived in the post. I sat down and took
one 200mg tablet with a glass of water. It didn't seem odd: for years, I took an
antidepressant. Then I pottered about the flat for an hour before sitting down
on the settee. I picked up a book about quantum physics and super-string theory
I had been meaning to read for ages, for a column I was thinking of writing.
Five hours later, I realised I had hit the last page. I looked up. It was
getting dark. I was hungry. I hadn't noticed anything, except the words I was
reading, and they came in cool, clear passages; I didn't stop or stumble once.
PERPLEXED, I got up, made a sandwich and was overcome with the urge to write an
article that had been kicking around my subconscious for months. It rushed out
of me in a few hours, and was better than usual. My mood wasn't any different; I
wasn't high.
My heart wasn't beating any faster. I was just able to glide into a state of
deep, cool, effortless concentration. It was as if I had opened a window in my
brain and all the stuffy air had seeped out, to be replaced by a calm breeze.
Once that article was finished, I wanted to do more. I wrote another piece, all
of it springing out of my mind effortlessly.
Then I went to dinner with friends. At the end, my mate Jess turned to me and
said, "You seem very thoughtful tonight." That night, I couldn't sleep. I wasn't
restless but I kept thinking very clearly, and I wanted to write it all down. I
remembered there's a long history of people in high-pressure jobs using
stimulants when their brains lost their sponginess: Anthony Eden was taking
Benzedrine all through the Suez Crisis, and Jean-Paul Sartre wrote several of
his novels while pumped on mescaline.
Admittedly, these precedents aren't encouraging: Eden had a breakdown, and
Sartre's brain was so cooked that for the rest of his life, he had the recurring
fear he was being followed by a giant lobster. Am I making a stupid mistake? The
next morning I woke up and felt immediately alert. Normally it takes a coffee
and an hour to kick-start my brain; today I'm ready to go from the second I
rise. And so it continues like this, for five days: I inhale books and exhale
articles effortlessly. My friends all say I seem more contemplative, less rushed
which is odd, because I'm doing more than normal. I keep waiting for an
exhausted crash, and it doesn't seem to come.
When the American journalist David Plotz took modafinil, he said it should be
given a slogan. Just as Valium was marketed as "the housewife's little helper",
he said this should be sold as "the boss's little helper". It makes you work
better and harder than before.
It's hard to explain modafinil's effects beyond that. Normally, one day out of
seven I have a day when I'm working at my best I've slept really well, and
everything comes easily and fast.
modafinil makes every day into that kind of day. It's as if I have been upgraded
to a new operating system: Johann 3.0. On discussion boards, I talk to American
student doctors taking the drug, who say they feel the same way. "I keep
thinking where's the catch?" one says. It turns out it is being given to US
soldiers, too.
It was then that I noticed I wasn't very hungry. I am normally porcine; my ex
once seriously considered having a trough made for me. But on modafinil, I was
filled up by a bowl of soup and a piece of bread. I would feel stuffed halfway
through my normal meals. A friend howled: "Who are you, and what have you done
with the real Johann?" Is all this just the placebo effect: I expect it to do
this to me, so it does? Perhaps.
But in the clinical trials, it worked much better than the placebo. But then I
began to worry again. We don't know the long-term effects of this drug. What if
it causes your brain to deplete its resources and wear out? My wonderful
grandmother has dementia, her life and personality dissolving in lost memories;
no short-term concentration is worth that. A friend says to me, "Why do you
always feel like you're not good enough, and you need some kind of chemical
enhancement?" It makes me wonder. So after five days on, I decided to take three
days off, to see what would happen.
It was easy. I sagged back to my former somewhat-depleted state, as though the
modafinil had never happened. I worked in my usual stop-start bursts. I ate my
usual portions-and-a-half. I stared sadly at the pack of pills, and every time I
hit a mental stumbling block, I had to discipline myself not to crack out a
modafinil.
As soon as my three days were up and I started again, my brain revved back into
super-speed and my stomach began to shrivel. But this time I began to worry
about the ethics of it all. If this drug had been available during my A-levels
or finals, I would have been the first to guzzle it down. But isn't that
cheating? What's the difference between modafinil for students and steroids for
athletes? And if this drug becomes as popular as, say, antidepressants or
Ritalin, won't there be a social pressure for workers to take it, and for
parents to drug away their child's disobedience? Professor Anjan Chatterjee
says: "This age of cosmetic neurology is coming, and we need to know it's
coming." The use of modafinil and its progeny will be mainstream and mainlined
in just a few years, he argues, and this made me feel excited and anxious.
As the end of my final five days approached, I had to decide what to do. Do I
order another pack? Do I think all my thoughts at a faster pace from here on in
with the power of modafinil? I finally concluded that taking narcolepsy drugs
when you don't have narcolepsy is just stupid. Our lack of knowledge about what
it does to your brain was, in the end, a dealbreaker for me. So I have made a
pact with myself.
I am keeping a pack for the days when I am really knackered and have to work
fast and fluently but I won't take more than two or three a month.
As I put the tablets aside, I look out over my flat. My desk is piled high with
the vast quantities of work I have pumped out. My cupboards are full of uneaten
food. The whole place is freakishly clean. Ah, modafinil, you are a gorgeous
temptress. With a sad sigh, I close the bathroom cabinet and stumble back to my
slow, patchy life, with my slow, patchy brain.
¡ Johann Hari writes for The Independent..
A DOCTOR'S WARNING
"MODAFINIL (trade name Provigil) is a brain stimulant drug and the accepted
first-line treatment for narcolepsy, a rare condition where the chemical
'switch' that turns sleep on and off is not working properly. Narcoleptics fall
asleep in the daytime but also wake frequently at night.
"No one knows precisely how modafinil works, not even the company (Cephalon)
that developed it. It probably keeps people awake by acting on deep-seated parts
of the brain.
"Side-effects from modafinil are few although there have been some reports of
liver dysfunction. But buying prescription drugs over the internet with no
medical control is fraught with hazards. Cognitive ability may be impaired and
an untoward event could occur. A case is bound to pop up sooner or later when
something awful happens because of someone staying awake too long using
stimulants.
" Restricted sleep is part of the 24/7 society and there is lots of research
beginning to look at the effects on the immune system. But for now the message
is 'you mess with these drugs at your peril'."
Dr Peter Venn, director of sleep studies at Queen Victoria Hospital, West
Sussex..
LOAD-DATE: May 6, 2008
LANGUAGE: ENGLISH
GRAPHIC: Cleverer by half: with Progivil, Hari could read fast and absorb ideas
effortlessly
PUBLICATION-TYPE: Newspaper
Copyright 2008 Associated Newspapers Ltd.
All Rights Reserved
243 of 998 DOCUMENTS
The Pharmaceutical Journal
May 2, 2008
Caution in use alert / SPC changes / Prescription products
BYLINE: Old_manager
LENGTH: 622 words
HIGHLIGHT: Prescription Products Meningitec Meningitec
(meningococcal serogroup C oligosaccharide conjugate vaccine [adsorbed];
Wyeth) is now available in prefilled syringes. The 10 x 0.5ml vials are
no longer available. Childhood immunisation programme supplies are
available from Movianto UK on 0870 871 1891.
Prescription Products
Meningitec
Meningitec (meningococcal serogroup C oligosaccharide conjugate vaccine
[adsorbed]; Wyeth) is now available in prefilled syringes. The 10 x 0.5ml
vials are no longer available. Childhood immunisation programme supplies
are available from Movianto UK on 0870 871 1891.
Net price: 10 x 0.5ml prefilled syringe, £75
Legal category: POM
Pentasa
Pentasa 2g sachets (mesalazine prolonged release granules) are now available
from Ferring Pharmaceuticals.
Net price: 60 x 2g sachets, £72.05
Legal category: POM
SPC changes
Accessing SPCs
The summaries of product characteristics and patient information
leaflets for medicines licensed in the UK are available online
Corticosteroids
The summaries of product characteristics for Medrone (methylprednisolone;
Pharmacia) tablets, Solu-Medrone (methylprednisolone sodium succinate;
Pharmacia) injections and Solu-Cortef (hydrocortisone sodium succinate;
Pharmacia) injection have been updated to include a warning about potential
psychiatric side effects occurring with systemic steroids.
Hepsera
In lamivudine-resistant patients, Hepsera (adefovir dipivoxil; Gilead)
should be used in combination with lamivudine, not as monotherapy, to
reduce the risk of resistance, the summary of product characteristics for
Hepsera now states.
It adds: "In order to reduce the risk of resistance in patients
receiving adefovir dipivoxil monotherapy, a modification of treatment
should be considered if serum HBV DNA remains above 1,000 copies/ml at or
beyond one year of treatment."
The SPC also warns that resistance to Hepsera can result in viral
load rebound, which could result in exacerbation of hepatitis B and,
if hepatic function is reduced, lead to liver decompensation and
mortality.
Virological response should be monitored closely and if viral rebound
occurs resistance testing should be performed.
Renal failure, Fanconi syndrome, hypophosphatemia, proximal
renal tubulopathy and associated myopathy and osteomalacia have
been added to the list of undesirable effects (frequency not known)
from post-marketing surveillance.
Provigil
Serious rash requiring admission to hospital and discontinuation of treatment
has been reported with the use of Provigil (modafinil; Cephalon), occurring
one to five weeks after treatment initiation, the summary of product
characteristics for Provigil now states.
Isolated cases of serious rash have been reported after prolonged
treatment (eg, three months), the SPC adds. It also says that
patients with major anxiety should only receive treatment with Provigil
in a specialist unit.
Psychiatric adverse experiences, including suicidal ideation, have
been reported in patients treated with modafinil. In such
circumstances, modafinil should be discontinued and not restarted.
Caution should be exercised in administering modafinil to patients
with a history of psychosis, depression or mania, the SPC says.
Sandimmun
Patients on Sandimmun (ciclosporin; Novartis) concentrate for infusion
should be warned to avoid excess ultraviolet light exposure in view of
the potential risk of skin malignancy, the product's summary of product
characteristics now says.
The SPC also now states that renal function should be monitored with
particular care in elderly patients and that caution should be
exercised when co-administering lercanidipine with ciclosporin.
LOAD-DATE: November 10, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Journal
Copyright 2008 PJ Online
All Rights Reserved
244 of 998 DOCUMENTS
Clinical Psychiatry News
May 2008
Options Expanding For Bipolar Disorder
BYLINE: Bruce Jancin, Denver Bureau
SECTION: Pg. 10 Vol. 36 No. 5 ISSN: 0270-6644
LENGTH: 775 words
VIENNA - A growing list of innovative therapies with novel mechanisms of
action in bipolar disorder is available for tough-to-treat cases, Dr. Benedikt
L. Amann said at the annual congress of the European College of
Neuropsychopharmacology.
All of these candidates have demonstrated promise in open-label or small,
controlled, proof-of-concept studies, but they all clearly require larger
confirmatory trials. In the interim, psychiatrists are likely to find some of
these agents beneficial for off-label use in the many patients with bipolar
disorder who respond inadequately to current guideline-directed treatments, said
Dr. Amann of the University of Barcelona.
Although he discussed promising new therapies for mania, he gave greater
emphasis to progress in the treatment of bipolar depressive episodes because the
need is more pressing.
"We do very well with our manic patients on a symptomatic level, but we still
do very badly with depressive patients," he observed.
Options for Bipolar Depression
The wakefulness drug modafinil (Provigil) improved symptoms of bipolar
depression in a recent randomized, placebo-controlled, 85-patient, multicenter
study.
All enrollees were inadequately responsive to a mood stabilizer. By week 2,
the modafinil-treated group, on a mean dosage of 177 mg/day, showed
significantly greater improvement than did controls on the clinician-rated
Inventory of Depressive Symptomatology. The remission rate at the end of the
6-week trial was 39% in the modafinil group, compared with 18% with placebo.
There was no difference between the two groups in treatment-emergent mania or
hypomania (Am. J. Psychiatry 2007;164:1242-9).
In Dr. Amann's 2-year, open-label study of 30 patients with refractory severe
bipolar depression, the nutritional supplement chromium was associated with a
mean 40% decrease in Montgomery-Åsberg Depression Rating Scale (MADRS) scores
(J. Clin. Psychopharmacol. 2007;27:104-6). Like the modafinil trial, the
chromium study was funded by the Stanley Medical Research Institute.
In the first double-blind, placebo-controlled trial conducted of a potential
treatment for acute bipolar II depression, pramipexole (Mirapex) showed
significant benefit, with 60% of patients treated to a target dosage of 1-3
mg/day demonstrating a greater than 50% reduction in MADRS scores after 6 weeks,
compared with 9% of those on placebo. One patient on pramipexole and two on
placebo developed hypomanic symptoms (Biol. Psychiatry 2004;56:54-60).
Pramipexole, a neurotrophic dopamine agonist with selectivity for the D2
receptor subfamily, is approved by the Food and Drug Administration for the
treatment of Parkinson's disease. Results of the 21-patient bipolar depression
study, led by investigators at the National Institute of Mental Health,
implicate the dopaminergic system in the pathophysiology of bipolar depression.
Novel Mania Treatments
What do lithium and valproate share besides an antimanic effect? The two
structurally dissimilar agents inhibit protein kinase C, an enzyme which
regulates pre- and postsynaptic neurotransmission. So does tamoxifen, the
estrogen receptor modifier used by huge numbers of women for primary or
secondary prevention of breast cancer. Indeed, tamoxifen is also the only
selective protein kinase C inhibitor that crosses the blood-brain barrier.
That insight prompted NIMH investigators to conduct a double-blind,
placebo-controlled, 3-week pilot study in 16 bipolar patients with acute mania
or a mixed state. The response rates, as assessed by the Young Mania Rating
Scale, were 63% with tamoxifen at 20-140 mg/day and 13% for placebo (Bipolar
Disord. 2007;9:561-70).
"Protein kinase C will probably become an important enzyme in the future in
bipolar disorder," Dr. Amann predicted. "Its activation impairs cognition. ...
And inhibitors of protein kinase C in the limbic system appear to be relevant to
the treatment of mania."
The atypical antipsychotic zotepine, which is marketed in Europe and
elsewhere but not in the United States, showed a rapid therapeutic effect in Dr.
Amann's open-label pilot study of 12 patients with severe acute mania. Two
patients dropped out after 2 days, but 9 of the remaining 10 were classified as
responders, with 5 patients experiencing at least a 50% reduction in the Young
Mania Rating Scale score within 4 days (Bipolar Disord. 2005;7:471-6).
With regard to mood stabilizers, he asserted that, despite intensive studies
of anticonvulsants and atypical antipsychotics in the last decade, nothing has
been shown to be more effective than lithium.
"The real mood stabilizer is waiting to be found," he observed.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
245 of 998 DOCUMENTS
Family Practice News
May 1, 2008
Modafinil Improves ADHD Symptoms in Different Subtypes
BYLINE: Heidi Splete, Senior Writer
SECTION: Pg. 29 Vol. 38 No. 9 ISSN: 0300-7073
LENGTH: 568 words
Modafinil significantly improved symptoms in children with inattentive and
combined subtypes of attention-deficit/hyperactivity disorder, based on data
from 638 children aged 6-17 years.
Pooled results from one 7-week study and two 9-week studies showed that
modafinil was well tolerated and improved attention-deficit hyperactivity
disorder (ADHD) symptoms both at home and in school. The studies were funded by
Cephalon Inc., which markets modafinil as Provigil in the United States.
Dr. Joseph Biederman of Massachusetts General Hospital, Boston, and Dr.
Steven R. Pliszka of the University of Texas Health Science Center, San Antonio,
reviewed the pooled data to analyze the effectiveness of modafinil on three ADHD
subtypes: inattentive, combined, and hyperactive impulsive (J. Pediatr.
2008;152:394-9). Few studies have examined the effectiveness of drug treatments
for ADHD by subtype.
In the 7-week study, children were randomized to receive 340 mg or 425 mg of
modafinil or a placebo daily. In the 9-week studies, children were randomized to
receive a flexible dose from 170 mg to 425 mg or a placebo daily. A total of 423
children received modafinil and 215 received a placebo.
The researchers used the ADHD-RS-IV School Version, which includes teacher
and investigator ratings to assess symptoms.
Children in the inattentive and combined subgroups who received modafinil
showed significant improvements in the ADHD-RS-IV School Version total scores,
compared with placebo patients. Children in the hyperactive-impulsive subgroup
who received modafinil showed a greater improvement in total scores
(demonstrated by lower numbers) than placebo patients, but this difference was
not statistically significant.
The average score for modafinil patients across all subgroups was 57 at the
study's end versus 73 for placebo patients. Results were similar for scores on
the ADHD-RS-IV Home Version, which were detailed in a separate analysis.
Forty-eight percent of the inattentive subgroup who received modafinil versus
15% of those who were given a placebo received "much improved" or "very much
improved" ratings from investigators. Similarly, 44% of the combined subgroup
who received modafinil versus 18% of those who received placebo were rated "much
improved" or "very much improved" by the investigators.
Children in the inattentive and combined subtype groups who received
modafinil showed significant improvements in subscale scores for cognitive
problems/inattention, hyperactivity, and the ADHD index, compared with placebo
patients.
The combined subtype of ADHD is the most commonly diagnosed and is most often
associated with psychiatric comorbidity and other behavioral, social, and
academic problems, the researchers noted. A total of 65% of the children met
criteria for the combined ADHD subtype, and this group had the largest
percentage (18%) of children who were ranked "severely ill" or "extremely ill"
at baseline.
Dr. Biederman receives research support from multiple drug companies,
including this study's sponsor, Cephalon (for whom he also serves as a speaker
and a member of the advisory board). He also serves as a speaker and advisory
board member for many other pharmaceutical companies.
Dr. Pliszka receives research support from Cephalon and Eli Lilly & Co., and
serves on speakers bureaus sponsored by Shire Pharmaceuticals and McNeil.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2008 Elsevier Inc., International Medical News Group
All Rights Reserved
246 of 998 DOCUMENTS
US Fed News
April 14, 2008 Monday 2:41 AM EST
Missouri Inventor Develops Benzhydrylthioacetamide Preparation Process
BYLINE: US Fed News
LENGTH: 234 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., April 14 -- Sidney Liang of Olivette, Mo., has developed a
benzhydrylthioacetamide preparation process.
According to the U.S. Patent & Trademark Office: "The present invention is
directed to an improved process for preparing modafinil wherein
benzhydrylthioacetate is prepared in high yield and purity by the reaction of a
haloacetate with the reaction product of thiourea and benzhydrol."
An abstract of the invention, released by the Patent Office, said: "The reaction
employing the haloacetate is conducted in a solvent comprising an organic
solvent such as methanol having dissolved therein an organic base or an
inorganic basic salt such as sodium bicarbonate. The resulting
benzhydrylthioacetate can be amidated and then oxidized to provide the
pharmaceutical grade modafinil in high yield and purity."
The inventor was issued U.S. Patent No. 7,345,188 on March 18.
The patent has been assigned to Mallinckrodt Inc., Hazelwood, Mo.
The original application was filed on Oct. 22, 2004, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,345,188.PN.&OS=PN/7,345,188&RS=
PN/7,345,188.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
LOAD-DATE: April 14, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 HT Media Ltd.
All Rights Reserved
247 of 998 DOCUMENTS
Irish Independent
April 9, 2008 Wednesday
Just like Viagra for your brain...
SECTION: FEATURES
LENGTH: 987 words
Professionals use them for jet lag, students to pass exams, soldiers to stay
alert. Brain-enhancing drugs are the latest fix -- and they're legal. By Simon
Usborne
Do you face a mid-afternoon lull that even a double espresso cannot break? Is
jetlag the bane of your life, or does that pile of revision seem insurmountable?
Or perhaps you're just fed up yawning your way out of the pub at 9.30pm.
Whether modern life leaves you struggling to keep up or just totally exhausted,
the answer could be as simple as popping a pill.
Using drugs to improve performance in sport is nothing new -- expect doping to
be a hot topic at this summer's Beijing Olympics -- but what about pills that do
nothing to enhance biceps, glutes or abs, and instead target the body's most
powerful 'muscle' -- the brain?
The idea that pills could boost memory or allow weary workers to put in 24-hour
shifts evokes the dystopia of Aldous Huxley's 1932 science-fiction novel Brave
New World, in which humanity depends on a government-prescribed "happy" drug
called Soma.
Some scientists are warning that a generation of artificially enhanced thinkers
could soon become science-fact, as an increasing number of people, from
stockbrokers and soldiers to students and shelf-stackers, look for something
moreeffective than caffeine to boost performance.
The medicines they use are called cognitive- or brain-enhancing drugs. But you
won't find a dedicated shelf in your local pharmacy. Instead, healthy people are
popping prescription pills designed to treat conditions such as attention
deficit hyperactivitydisorder (ADHD), narcolepsy or even Alzheimer's.
The drugs of choice are Ritalin and Modafinil. Prescribed to ADHD sufferers to
help calm them down, Ritalin, dubbed 'kiddie coke' by some, can boost
concentration and alertness in healthy people. Modafinil, meanwhile, is designed
to combat narcolepsy, but it can also stave off tiredness in those without a
diagnosed sleep disorder.
A 2005 survey of more than 10,000 US university students found that 4pc-7pc of
them had tried ADHD drugs at least once to pull pre-exam all-nighters. At some
institutions, more than one in four students said they'd sampled the pills.
Anecdotal evidence suggests as many as three in four classical musicians in the
US take beta blockers such as Inderal, which block adrenaline receptors in the
brain, helping to control conditions such as high blood pressureor stage fright
in jitterymusicians.
Philip Harvey, a professor at Emory University in Atlanta, says his work has
been transformed by Modafinil, which he takes to combat jet lag.
Unlike here, American doctors can prescribe the drug to night-shift workers as
well as to narcoleptics.
"I often fly to Europe to give talks," Harvey says. "I used to travel the day
before to give myself time to recover, but with Modafinil I can now give a talk
the same day I arrive and feel like I've had a normal night's sleep."
Harvey says he has no urge to take the drug more frequently, but many do. And
it's easy to understand why.
In 2003, scientists at Cambridge University found a single dose of Modafinil
helped healthy male university students perform better at mental planning tests,
complete puzzles more accurately and remember longer chains of digits.
The drug has also been tested by British and American armed forces, where it has
been shown to help soldiers stay alert during night-time operations. Scientists
say that the drug allows 48 hours of continuous wakefulness with few side
effects, mild headaches being the most common.
Perhaps the most remarkable thing about Modafinil is that users don't have to
pay back sleep 'debt' -- a standard eight hours is apparently enough to make up
for no sleep the night before. Such impressive results have led some scientists
to predict a world with little or no need for sleep, where drugs will allow us
to put in 22-hour days. Little wonder, then, that the drugs companies are
reportedly racing to develop the world's first marketed brain-enhancing drugs.
If, or when, they do, they could make the launch of the impotence drug Viagra
look like a damp squib.
"It could change society as we know it," says Barbara Sahakian, a psychiatrist
at Cambridge University, who has studied cognitive-enhancing drugs. "The drive
for the self-enhancement of brain power is likely to be as strong, if not
stronger, as in the realms of enhancement of beauty or sexual function."
But that is not necessarily a good thing, Sahakian warns. "One concern I have is
the lack of regulation when people buy these drugs on the internet, where they
can't be absolutely certain what they are getting, or whether they should be
taking them. More seriously, we have to ask how this might affect society. We
control drug-use in sport, so will we do the same for students who take drugs
before exams, forexample?
"And if some students or workers take them, will theothers feel pressure to do
the same to keep up?
"We also have to ask what this says about us -- why is it that we are always
looking for the quickest way around the problem? And why do we so often look to
the answer in drugs rather than trying psychological therapies -- or just making
more time to sleep?"
Whether or not these questions can be answered, brain enhancers look set to
challenge caffeine as the pick-me-up of choice in the world's offices,
classrooms and war zones. Last year Foresight, a British government think-tank,
said drugs such as Modafinil could be "as common as coffee" within a decade or
two.
That will delight hard-working professionals such as Philip Harvey, who want to
improve their work-life balance.But Barbara Sahakian's parting words are
cautionary: "One person might say cognitive enhancing drugs are good because
they allow us to get home early because we finish our work sooner, but others
worry that we are working towards a 24-hours-a-day society pushed to the limits
of human endurance."
LOAD-DATE: April 9, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2008 Independent News and Media Ltd.
All Rights Reserved
248 of 998 DOCUMENTS
Reuters Health Medical News
April 9, 2008 Wednesday 9:00 PM EST
Use of cognition-enhancing drugs common among academics
SECTION: HUMAN INTEREST
LENGTH: 503 words
DATELINE: NEW YORK
An informal survey of individuals who read the journal Nature reveals that
roughly one in five use prescription agents to improve their focus,
concentration, or memory.
As reported in the April 10th issue of the journal, 1400 people from 60
countries responded to the online survey. The subjects were asked specifically
about the use of three drugs: 1.) methylphenidate (Ritalin), which is used to
treat ADHD, but is considered on college campuses as a "study aid"; 2.)
modafinil (Provigil), which is prescribed for sleep disorders, but is used
off-label to fight general fatigue or jet lag; 3.) beta blockers,
anti-arrhythmic agents that are also known for their anti-anxiety effect.
Brendan Maher, a feature and commentary editor with Nature, analyzed the results
and found that among those "who choose to use," methylphenidate was the most
popular agent: 62% of users reported taking it. Modafinil was taken by 44% of
users and beta blockers by 15%. Thus, many of the subjects were using more than
one agent.
When asked about use of other agents, many of the subjects reported taking
Adderall, an amphetamine similar to methylphenidate. Other drugs used included
centrophenoxine, piractem, Dexedrine, and alternative medicines, including
ginkgo and omega-3 fatty acids.
Use of cognition-enhancing drugs did not vary by age group, the report
indicates. Maher said this may be surprising to some people since prior
research has suggested increased usage in 18- to 25-years-olds.
Improving concentration was the main reason cited for using these drugs with
enhancing focus on a specific task being a close second.
Usage patterns were evenly split between daily, weekly, monthly, or no more than
once a year. Unpleasant side effects, including headache and jitteriness, among
others, were reported by roughly half of users. The emergence of side effects
did not correlate with decreased frequency of use, however.
Four-fifths of respondents believed that healthy adults should be permitted to
take cognition-enhancing agents if they want to and 69% said they would risk
mild adverse effects to take the drugs themselves. Eighty-six percent of
respondents said that children under 16 years should be restricted from using
these drugs, yet one-third of respondents said they would feel pressured to give
their child these agents if other children were taking them.
In a related commentary, Dr. Barbara Sahakian and Dr. Sharon Morein-Zamir, UK
researchers whose 2007 study of cognition-enhancing drug use prompted the
current survey, caution that "although the appeal of pharmaceutical cognitive
enhancers...is understandable, potential users, both healthy and diseased, must
consider the pros and cons of their choices."
Drs. Sahakian and Morein-Zamir, neuroscientists with the University of
Cambridge, add that "scientists, doctors, and policy-makers should provide easy
access to information about the advantages and dangers of using
cognitive-enhancing drugs and set out clear guidelines for their future use."
LOAD-DATE: April 10, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2008 Reuters Health
All Rights Reserved
249 of 998 DOCUMENTS
Independent Extra
April 8, 2008 Tuesday
First Edition
Like Viagra for your brain;
Professionals use them for jet lag, students to pass exams, soldiers to stay
alert. Brain-enhancing drugs are the latest fix - and they're legal. By Simon
Usborne
BYLINE: Simon Usborne
SECTION: EXTRA; Pg. 12
LENGTH: 1014 words
Do you face a mid-afternoon lull that even a double espresso cannot break? Is
jet lag the bane of your life, or does that pile of revision seem
insurmountable? Or perhaps you're just fed up yawning your way out of the pub at
9.30pm. Whether modern life leaves you struggling to keep up or just totally
exhausted, the answer could be as simple as popping a pill.
Using drugs to improve performance in sport is nothing new - expect doping to be
a hot topic at this summer's Beijing Olympics - but what about pills that do
nothing to enhance biceps, glutes, or abs, and instead target the body's most
powerful "muscle" - the brain?
The idea that pills could boost memory or allow weary workers to put in 24-hour
shifts evokes the dystopia of Aldous Huxley's 1932 science-fiction novel Brave
New World, in which humanity depends on a government-prescribed "happy" drug
called Soma.
Some scientists are warning that a generation of artificially enhanced thinkers
could soon become science-fact, as an increasing number of people, from
stockbrokers and soldiers to students and shelf-stackers, look for something
more effective than caffeine to boost performance.
The medicines they use are called cognitive- or brain-enhancing drugs. But you
won't find a dedicated shelf in your local chemist's. Instead, healthy people
are popping prescription pills designed to treat conditions such as attention
deficit hyperactivity disorder (ADHD), narcolepsy or even Alzheimer's.
The drugs of choice are Ritalin and Modafinil. Prescribed to ADHD sufferers to
help calm them down, Ritalin, dubbed "kiddie coke" by some, can boost
concentration and alertness in healthy people. Modafinil, meanwhile, is designed
to combat narcolepsy, but it can also stave off tiredness in those without a
diagnosed sleep disorder.
The British Medical Association believes this kind of drug abuse is growing
rapidly, as healthy pill-poppers dupe doctors into writing prescriptions, or buy
medicines from unlicensed online pharmacies, usually based abroad.
The true scale of the problem in the UK is unknown but studies in America
suggest brain-boosting drug use is rife. A 2005 survey of more than 10,000 US
university students found that 4-7 per cent of them had tried ADHD drugs at
least once to pull pre-exam all-nighters. At some institutions, more than one in
four students said they'd sampled the pills.
Anecdotal evidence suggests as many as three in four classical musicians in the
US take beta blockers such as Inderal, which block adrenalin receptors in the
brain, helping to control conditions such as high blood pressure, or stage
fright in jittery musicians.
Philip Harvey, a professor at Emory University in Atlanta, says his work has
been transformed by Modafinil, which he takes to combat jet lag. Unlike in the
UK, American doctors can prescribe the drug to night-shift workers as well as to
narcoleptics. "I often fly to Europe to give talks," Harvey says. "I used to
travel the day before to give myself time to recover, but with Modafinil I can
now give a talk the same day I arrive and feel like I've had a normal night's
sleep."
Harvey says he has no urge to take the drug more frequently, but many do. And
it's not difficult to understand why. In 2003, scientists at Cambridge
University found a single dose of Modafinil helped healthy male university
students perform better at mental planning tests, complete puzzles more
accurately and remember longer chains of digits.
The drug has also been tested by British and American armed forces, where it has
been shown to help soldiers stay alert during night-time operations. Scientists
say that the drug allows 48 hours of continuous wakefulness with few side
effects, mild headaches being the most common.
Perhaps the most remarkable thing about Modafinil is that users don't have to
pay back sleep "debt"; a standard eight hours is apparently enough to make up
for no sleep the night before. Such impressive results have led some scientists
to predict a world with little or no need for sleep, where drugs will allow us
to put in 22-hour days. Little wonder, then, that the drugs companies are
reportedly racing to develop the world's first marketed brain- enhancing drugs.
If, or when, they do, they could make the launch of the impotence drug Viagra
look like a damp squib.
"It could change society as we know it," says Barbara Sahakian, a psychiatrist
at Cambridge University, who has studied cognitive-enhancing drugs. "The drive
for the self-enhancement of brain power is likely to be as strong if not
stronger as in the realms of enhancement of beauty or sexual function."
But that is not necessarily a good thing, Sahakian warns. "One concern I have is
the lack of regulation when people buy these drugs on the internet, where they
can't be absolutely certain what they are getting, or whether they should be
taking them. More seriously, we have to ask how this might affect society. We
control drug use in sport, so will we do the same for students who take drugs
before exams, for example? And if some students or workers take them, will the
others feel pressure to do the same to keep up?
"We also have to ask what this says about us - why is it that we are always
looking for the quickest way around the problem? And why do we so often look to
the answer in drugs rather than trying psychological therapies - or just making
more time to sleep?"
Whether or not these questions can be answered, brain enhancers look set to
challenge caffeine as the pick-me-up of choice in the world's offices,
classrooms and war zones. Last year, Foresight, a Government think tank, said
drugs such as Modafinil could be "as common as coffee" within a decade or two.
That will delight hard-working professionals like Philip Harvey, who want to
improve their work-life balance. But Barbara Sahakian's parting words are
cautionary: "One person might say cognitive enhancing drugs are good because
they allow us to get home early because we finish our work sooner, but others
worry that we are working towards a 24-hours-a-day society pushed to the limits
of human endurance."
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Drug Formulary Review
April 1, 2008
Drug Criteria & Outcomes: An Awakening to Narcolepsy
LENGTH: 871 words
Drug Criteria & Outcomes
An Awakening to Narcolepsy
By Lori Lawson, PharmD Candidate, Harrison School of Pharmacy, Auburn University
Narcolepsy is a chronic neurological disorder, mistakenly thought to occur only
rarely. However, approximately 5% of patients seen at the American Academy of
Sleep Medicine in the United States have this disease and it is estimated that
as many as one in 2,000 Americans have narcolepsy.1,2
Narcolepsy is characterized by uncontrollable sleepiness and intermittent
manifestations of REM sleep at periods when a person should normally be awake.
Most patients also experience cataplexy, which is partial or generalized loss of
skeletal muscle tone and power in response to emotion, especially amusement,
anger, and elation. Other common symptoms include: sleep paralysis, hypnagogic
hallucinations (vivid, dream-like experiences at the start of sleep), disturbed
nocturnal sleep, and automatic behavior.3
This disease has many clinical facets. Sleep attacks can occur at any time and
can be very disabling. Patients may involuntarily fall asleep while driving,
eating, working, or talking. Hence, this is a dangerous disease that could lead
to accidents and loss of employment.
Researchers have identified a potential biochemical basis of narcolepsy. In
humans, hypocretin, a neurotransmitter, is reduced or undetectable in many but
not all patients with narcolepsy associated with cataplexy. Research data on
hypocretin continue to be accumulate and in the future hypocretin therapy may be
an option.
Treatment options
Treatment can make a significant difference in these patients' lives. The
excessive daytime sleepiness is most commonly treated with stimulants. In 1999,
the FDA approved modafinil (Provigil®), a novel stimulant with an unclear
mechanism of action that may increase hypocretin activity. Apart from modafinil,
all stimulants are centrally acting sympathomimetic agents that increase the
release of monoamines in the synaptic cleft and block their reuptake.4 Modafinil
is now considered first-line treatment for narcolepsy.2 Modafinil is not a
psychostimulant and it does not cause psychomotor agitation, disruption of
night-time sleep, inappropriate mood shifts, or the potential for addiction. In
June 2007, the FDA approved the active isomer of modafinil, armodafinil (Nuvigil
®), also indicated for narcolepsy. Armodafinil has very similar
pharmacokinetics, dosing, and adverse effects as compared to modafinil, and at
this time, armodafinil appears to have no clinical advantages over modafinil.5,6
Other stimulants used to treat excessive daytime sleepiness include amphetamine,
methamphetamine, dextroamphetmaine, and methylphenidate.1 These drugs can cause
insomnia, hypertension, palpitations, and irritability. However, many patients
tolerate these drugs without significant side effects. Tolerance to these
medications may also occur, necessitating an increase in dose to achieve the
same control of symptoms.2
The goal of stimulant therapy is to treat to near normal alertness with minimal
adverse effects. Dosages should be started out low and increased as needed and
as tolerated. Many physicians are weary of increasing the dose for fear of
inducing tolerance or dependence. While tolerance does occur in some patients,
abuse is rare in patients who do not have a history.4
Selegiline, a monoamine oxidase inhibitor, is an effective treatment for all
narcoleptic symptoms. However, experience with the high doses needed for
narcolepsy is limited and diet-induced hypertension is a danger at effective
doses.1
Unfortunately, stimulants do not treat cataplexy effectively. Common drug
therapies include tricyclic antidepressants such as protriptyline, imipramine,
and clomipramine, and selective serotonin reuptake inhibitors such as fluoxetine
and paroxetine. Sodium oxybate or gammahydroxybutyrate (GHB) was granted FDA
approval in 2002 for the treatment of cataplexy and daytime sleepiness in
patients with narcolepsy. It is an old sedative drug with considerable abuse
potential, and is available only from one national specialty pharmacy on a
named-patient basis. Sodium oxybate is a neurotransmitter found in the brain,
and research demonstrates that nightly administration of sodium oxybate helps
produce sleep patterns more closely resembling normal sleep patterns.2
Nonpharmacological therapies include maintaining regular sleep and wake times,
avoiding shift work, and working in a stimulating environment. It is often said
that naps throughout the day are helpful, but objective data are contradictory.1
References
· Littner M, Johnson S, McCall V, et al. Practice parameters for the
treatment of narcolepsy: An update for 2000. Sleep 2001;24:451-466.
· Feldman N. Narcolepsy. South Med J 2003;96:277-282.
· Zeman A, Britton T, Douglas N, et al. Narcolepsy and excessive daytime
sleepiness. BMJ 2004;329:724-728.
· Krahn L, Black J, Silber H. Narcolepsy: New understanding of
irresistible sleep. Mayo Clin Proc 2001;76:185-194.
· Lexi-Drugs. Hudson, OH: Lexi-Comp, Inc.; 2007.
· Harsh J, Hyaduk R, Wesnes K, et al. The efficacy and safety of
armodafinil as treatment for adults with excessive sleepiness
associated with narcolepsy. Curr Med Res Opin 2006;22:761-774.
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io9
March 25, 2008 Tuesday 5:28 PM EST
Provigil is the Cocaine of the Twenty-First Century [Pharmaceuticals]
LENGTH: 367 words
Mar. 25, 2008 (io9 delivered by Newstex) --
Provigil (AKA modafinil) has been called a wonder drug: it can keep you awake
and alert for hours without side-effects, and it's even recommended as "the
professor's little helper" by neuroscience researchers writing in the
prestigious journal Nature. Provigil, approved by the US food and drug
administration for the treatment of narcolepsy, is often prescribed "off label"
for ailments like severe jet lag, ADHD, and even problems with sleep cycles. But
this drug, which is supposed to be a non-addictive stimulant because it doesn't
get you high, turns out to be potentially as euphoria-inducing and addictive as
cocaine.
In March 2006, researcher Stefan Kruszewski wrote in The American Journal of
Psychiatry: Modanifil is reinforcing, as evidenced by its self-administration in
monkeys previously trained to self-administer cocaine. And back in 2002, an
article published in Behavioral Pharmacology states: Modafinil and cocaine
dose-dependently increased heart rate and blood pressure. The results of the
present study suggest that modafinil has minimal abuse potential, but should be
viewed cautiously because of the relatively small sample size. Future studies
should further characterize the abuse potential of modafinil using other
behavioral arrangements, such as drug discrimination or drug
self-administration. A full characterization of the abuse potential of modafinil
will become important as the use of this drug increases. Other reports suggest
that Provigil isn't addictive at all, and would in fact work well as a cure for
methamphetamine addiction. Here's a snippet from a 2006 article from Current
Psychiatry Reports: In early trials, several candidate medications--bupropion,
modafinil, and, to a lesser extent, baclofen--have shown promise in treating
aspects of methamphetamine dependence, including aiding memory function
necessary to more effectively participate in and benefit from behavioral
therapies. With more and more people getting prescriptions for Provigil, and the
drug fast catching up with Viagra for most spammy ads online, shouldn't someone
be investigating just how addictive it is?
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LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs via Newstex") are solely the author's and not
necessarily the views of Newstex or its re-distributors. Posts from such authors
are provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs via Newstex are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs via Newstex is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs via Newstex shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs via Newstex. Reader's comments reflect their
individual opinion and their publication within Blogs via Newstex shall not
infer or connote an endorsement by Newstex or its re-distributors of such
reader's comments or views. Newstex and its re-distributors expressly reserve
the right to delete posts and comments at its and their sole discretion.
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252 of 998 DOCUMENTS
World Generic Markets
Pharmaceuticals
February 22, 2008
FTC files complaint against Cephalon charging unlawful blockage of generic
modafinil
LENGTH: 327 words
The FTC has filed a complaint against Cephalon in the US District Court for the
District of Columbia, alleging that the company has undertaken a course of
anticompetitive conduct to prevent competition against its proprietary drug,
Provigil (modafinil), thus denying patients access to generic equivalents. The
complaint challenges the validity of certain agreements entered into by the
company in late 2005 and early 2006 to settle modafinil patent infringement
litigation; it seeks to permanently enjoin the company from maintaining or
enforcing these agreements. According to the complaint, Cephalon entered into
agreements with four generic drug manufacturers that each planned to sell a
generic version of Provigil: Teva Pharmaceutical Industries, Ranbaxy
Laboratories, Mylan Pharmaceuticals and Barr Laboratories.
These companies had challenged the only remaining patent covering modafinil,
which related to the size of particles used in the product. The complaint
charges that Cephalon was able to induce each of the generic companies to
abandon its patent challenge and agree to refrain from selling a generic version
of the drug until 2012, by agreeing to pay the companies a total amount in
excess of $200US million. The FTC is seeking a permanent injunction against
Cephalon that would allow generic modafinil entry before 2012. Furthermore, it
is seeking a final court judgement against the company, declaring that its
course of conduct, including its agreements, violates Section 5(a) of the FTC
Act and barring Cephalon from engaging in similar or related conduct in the
future. In response, Cephalon has stated that it stands by the strength and
validity of its modafinil patents and the legal basis for the settlements; the
company clarified that it is prepared to vigorously defend itself in this
matter. Modafinil is approved to treat excessive sleepiness in patients with
sleep apnoea, narcolepsy and shift-work sleep disorder. 13th February 2008
LOAD-DATE: February 22, 2008
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The Sun (England)
February 21, 2008 Thursday
Would you trust a pill to make you smart?
BYLINE: Pat Hagan
SECTION: SUN HEALTH
LENGTH: 1121 words
DRUGS WITH DESIGNS ON YOUR MIND
FORGET morning caffeine boosts. In future, we could all be popping
brain-boosting "smart" pills to give us the edge in school and at work.
In fact, thousands of people are already using powerful prescription medicines
to sharpen their minds.
But experts are warning too little is known about the long-term effects of the
new generation of smart pills.
Oxford University students swotting through the night for exams confess to
downing Ritalin, the drug used to treat hyperactivity in kids. They say it
boosts concentration and attention span.
Some education experts say they know parents who buy the drug on the internet
and feed it to their kids to try to beef up exam results.
Meanwhile, pilots, soldiers and shift workers are turning to a pill called
modafinil (Provigil) to stay awake. The drug was originally developed to treat
narcolepsy, a condition where people suddenly fall asleep dozens of times a day.
Tests show that, as well as keeping the brain awake for up to 40 hours at a
time, it can actually BOOST short-term memory and the ability to plan properly.
Battle
Even jet-lagged scientists attending conferences are reported to use the drug to
pep up their presentations.
Psychiatrist Professor Philip Harvey takes modafinil to ward off jet lag. He
says: "It makes me feel alert, like I had more sleep."
The medic, from Emory University in Atlanta, Georgia, claims the drug doesn't
create a high like other stimulants but does focus the mind.
The Ministry of Defence is said to have given it to soldiers exhausted by
battle. Other drugs that perk up brain cells include amphetamines and ampakines,
a new class of medicines that bolster memory.
However, thousands of users are thought to be buying them on the internet
without getting clearance from their GPs.
The British Medical Association believes a growing number of healthy people are
using brain-boosting drugs that should only be taken on prescription, buying
stimulants like Ritalin for as little as 67p a pill.
Apart from potential long-term side-effects, this raises the risk of dangerous
interactions with other medicines.
A report last year by Government think-tank Foresight said brain boosters like
modafinil could be "as common as coffee" within 20 years. The Government has
asked the Academy of Medical Sciences to investigate the use of so-called
"intelligence drugs".
Professor Barbara Sahakian, from Cambridge University, says if studies prove
drugs like modafinil are safe, adults could one day buy them over the counter to
help them cope with long hours. That would be safer than buying them from
unknown suppliers on the internet.
Party
She says: "I know scientists who buy modafinil on the internet and take it a few
hours before a presentation. But some then start to use it when they are busy.
One even took it to stay up late for a party. It may be that one day you could
go into Boots and buy these pills.
"As we get more effective drugs, people will definitely want to use them. But it
may be that you have to be over 16 to get them because we have to be careful
about the long-term effects on the developing brain."
In the US, research at the University of Michigan shows just over eight per cent
of undergraduates have used prescription stimulants. And the National Institute
On Drug Abuse found one in twenty 17 and 18-year olds had used amphetamines.
But how exactly do "smart pills" increase brain power and what are the risks in
taking them?
Sun Health investigates, and looks at other mind-boosting solutions.
HOW TO BOOST YOUR BRAIN
SMART DRUGS
Amphetamines: Used for: Little medical use these days, apart from Dexedrine, a
drug given to help people with narcolepsy.
Affect on brain: Stimulates the brain through increased heart rate, promoting
alertness.
An estimated 72million amphetamine tablets were issued to British Forces during
the Second World War.
Side-effects: Long-term use can lead to delusions, panic attacks and paranoia.
Ritalin: Used for: Hyper- activity in children.
Affect on brain: Increases activity of chemicals in parts of the brain that
control attention and behaviour.
Studies also show just one pill boosts mental performance in healthy, young male
students.
Side-effects: Although generally safe, some people can suffer severe liver
problems.
Cost: About 67p a pill on the internet.
Modafinil: Used for: Narcolepsy, the sudden onset of sleep.
Affect on brain: Keeps the brain awake for up to 40 hours at a time with high
levels of concentration.
Side-effects: Very few but can cause dizziness and blurred vision.
Cost: About £ 1.43 per pill on the internet.
Ampakines: Used for: Experimental drugs that could treat Alzheimer's and jet
lag.
Affect on brain: They boost the activity of glutamate, a chemical that helps the
brain store and retrieve memories.
Even a small dose can protect the brain against sleep loss.
Side-effects: Not yet known
Cost: Not yet available.
NATURAL BRAIN BOOSTERS
Smart pills may be one way to give your brain cells a lift. But there are other
reliable methods that don't rely on a chemical cocktail found in a pill.
Fish oils: Oils rich in Omega-3 are thought to aid learning and concentration by
keeping nerve connections in the brain healthy. A major trial involving 1,000
young offenders is about to launch in the UK to see if fish oil capsules and
other supplements will improve behaviour by bolstering brain activity.
Caffeine: Strong coffee and caffeine-rich drinks like Red Bull can give the
brain a short-term boost.
Israeli scientists found caffeine makes existing brain cells swell and new ones
grow.
It may also protect the female brain against dementia.
French researchers found that women over 65 who drank more than three coffees a
day suffered less memory loss.
Vitamins: Certain vitamins may be crucial in keeping the brain healthy.
Scientists at Johns Hopkins University in the US found taking vitamins C and E
together seemed to have the most powerful effect, protecting brain cells against
damage by highly destructive molecules called free radicals.
Folic acid: A daily dose of folic acid boosts the ageing brain, according to a
study last year in The Lancet.
Men and women aged 50 to 70 who took daily supplements had similar mental
abilities to people five years younger.
COMPUTER GAMES
Kids who play on computer games before lessons do better in exams.
Scottish pupils as young as nine who spent 20 minutes each day on the Nintendo
Dr Kawashima Brain Training games made dramatic improvements in maths tests.
EXERCISE
Children who exercise regularly get better exam results.
Exeter University researchers found that 79 per cent of 11-year-olds with better
than average English results exercised at least three times a week.
Among below average pupils, only 38 per cent exercised.
LOAD-DATE: February 21, 2008
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PUBLICATION-TYPE: Newspaper
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Generic Line
February 20, 2008 Wednesday
FTC Accuses Cephalon of Buying Off Generic Competition
SECTION: Vol. 25 No. 4
LENGTH: 1225 words
Cephalon's "anticompetitive conduct" aimed at protecting sales of its
top-selling product, which involved paying four firms to refrain from selling
generic Provigil until 2012, extended the company's monopoly on the drug beyond
the scope of its patent protection and cost patients and payers millions of
dollars a year, the FTC alleged in a complaint against the company.
But the FTC hasn't filed suit against any of the generic companies involved in
the agreements -- Teva Pharmaceuticals, Ranbaxy Pharmaceuticals, Mylan and Barr
Laboratories -- because the allegations focus more on the monopolistic actions
of Cephalon, rather than the nature of the deals, an FTC staffer told Generic
Line.
However, FTC Commissioner Jon Leibowitz issued a statement dissenting in part
with the 5-0 vote approving the Feb. 13 complaint, saying he would have
initiated action against the generic firms as well unless they chose to
relinquish their 180-day exclusivity on generic Provigil (modafinil), allowing
other companies to receive final approval and launch before 2012.
Provigil, originally approved in 1998, is indicated for improving wakefulness in
adults who experience excessive sleepiness due to obstructive sleep apnea, shift
work sleep disorder or narcolepsy. The drug is unique among wakefulness
treatments and is considered the gold standard for treating excessive
sleepiness, according to the FTC's complaint, filed in the U.S. District Court
for the District of Columbia. Cephalon's recent earnings announcement showed
that Provigil had U.S. sales of more than $800 million in 2007.
Because Cephalon's compound patent for modafinil expired in 2001, Provigil is
only protected by the '516 formulation patent relating to particle size that
generic companies could easily design around, the FTC said.
In 2002, Teva, Ranbaxy, Mylan and Barr simultaneously submitted abbreviated new
drug applications (ANDAs) for generic Provigil with Paragraph IV certifications
that the '516 patent was invalid or that their products would not infringe on
the patent, which expires in 2015.
As first filers, the four companies would share 180-day exclusivity for generic
Provigil, and under the Hatch-Waxman Act, the FDA would not be able to approve
any other generic versions of the drug until the exclusivity ended.
Cephalon filed separate patent infringement suits against the generic drugmakers
in 2003, triggering a 30-month stay of approval of the ANDAs. The FTC said in
its complaint that Cephalon would likely not have prevailed in litigation
against all four companies. However, before the litigation could conclude,
Cephalon set about settling with each of the defendants.
Cephalon agreed to allow the generic companies to launch their products in April
2012, but the company "had to provide other inducements to the first filers to
secure their agreement to refrain from competing," the FTC wrote.
The company achieved this by entering into seemingly separate transactions with
the generic firms worth more than $200 million total, the agency said. For
example, Teva agreed not to launch generic Provigil until April 2012 in exchange
for a license agreement relating to Teva's modafinil patents and patent
applications worth up to $125 million in Provigil royalties. Cephalon also
agreed to buy modafinil active pharmaceutical ingredient from Teva at prices
higher than what it was already paying.
The FTC alleged that Cephalon did not need the license or supply agreement
because it was already successfully making and selling Provigil. Cephalon
executed similar deals with the other generic firms.
Cephalon said in a statement that the settlement agreements sought to allow
generic Provigil entry three years prior to the expiration of the drug's patent
protection, but the FTC argued that some or all of the first filers would have
launched their generics in 2006 at the end of the 30-month stay or upon a
favorable ruling.
The agency noted that many parties had expected to see generic Provigil entry in
2006, and Cephalon even made plans to launch an authorized generic and introduce
its successor product, Nuvigil (armodafinil).
Therefore, the FTC concluded that Cephalon harmed consumers, "abused" the
Hatch-Waxman Act and violated the FTC Act. Not only did the agreements eliminate
potential competition from the four generic firms involved, they prevented any
other generic drugmakers from obtaining approval for and launching generic
Provigil.
"Cephalon prevented competition to Provigil by agreeing to share its future
monopoly profits with generic drugmakers poised to enter the market, in exchange
for delayed generic entry," FTC Bureau of Competition Director Jeffrey Schmidt
said in a statement. "Such conduct is at the core of what the antitrust laws
proscribe."
The FTC asked the court to issue a permanent injunction preventing Cephalon from
enforcing the settlement agreements or from entering into similar deals in the
future. Cephalon said it is "prepared to vigorously defend itself in this matter
and expects to prevail."
In his statement, Leibowitz said the lawsuit would probably go on for years, and
he recommended that Congress act on legislation -- the Preserve Access to
Affordable Generics Act, S. 316 and H.R. 1432 -- that would ban settlements
involving payments in exchange for delayed generic entry.
"Morever, as it is drafting much-needed legislation to create a pathway for
generic biologics, Congress should try to ensure that it does not create a
loophole that lets pharmaceutical companies conspire to exploit consumers
through yet a new avenue of pay-for-delay deals," he wrote. "Sadly,
pay-for-delay settlements, if not stopped, will continue to grow exponentially
-- costing consumers and the federal government (which pays more than 30 percent
of prescription drug costs) literally billions of dollars in excess charges."
GPhA does not support the Preserve Access to Affordable Generics Act, and last
year after the House Energy and Commerce Committee held a hearing on H.R. 1432,
the group asked Congress to continue to allow patent settlement agreements to be
reviewed by the FTC on a case-by-case basis. "Limiting a generic company's
ability to settle patent disputes would lead to fewer patent challenges and, in
the end, delay market entry with a substantial loss in savings for consumers,"
the group said.
Call to Give Up Exclusivity
Leibowitz suggested in his statement that Congress ask Teva, Mylan, Ranbaxy and
Barr whether they are willing to waive their 180-day exclusivity periods, which
he argued have "very little financial value to them when the benefits of waivers
to American consumers seem so substantial." He noted that if the companies wait
four more years to launch generic Provigil, they will be competing with the
drug's successor product, Nuvigil, and even more generics.
"So why would a generic company refuse to relinquish its exclusivity when that
exclusivity arguable has little value to the generic but creates near iron-clad
protection of Cephalon's Provigil monopoly?" he wrote. "Here, the
non-relinquishing generics appear to be sending a clear signal to PhRMA
companies: You can do business with us in the future; we will protect your
monopolies."
Teva, Mylan and Ranbaxy said they had no comment on the suit. Barr could not be
reached for comment by press time. -- Breda Lund
Release date: Feb. 20, 2008
LOAD-DATE: February 20, 2008
LANGUAGE: ENGLISH
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FDAnews Drug Daily Bulletin
February 18, 2008 Monday
FTC Accuses Cephalon of Buying Off Generic Competition
SECTION: Vol. 5 No. 33
LENGTH: 285 words
Cephalon's "anticompetitive conduct" to protect its top-selling product, which
involved paying four firms to refrain from selling generic versions of Provigil
until 2012, extended the company's monopoly on the drug beyond the scope of its
patent protection and cost patients and payers millions of dollars a year, the
FTC alleges in a complaint against the company.
Provigil (modafinil), originally approved in 1998, is indicated for improving
wakefulness in adults who experience excessive sleepiness due to obstructive
sleep apnea, shift work sleep disorder or narcolepsy.
Because Cephalon's compound patent for modafinil expired in 2001, Provigil is
only protected by the '516 formulation patent relating to particle size that
generic companies could easily design around, the FTC says.
Teva Pharmaceuticals, Ranbaxy Pharmaceuticals, Mylan and Barr Laboratories
simultaneously submitted abbreviated new drug applications (ANDAs) for generic
Provigil in 2002 with Paragraph IV certifications that the '516 patent was
invalid or that their products would not infringe on the patent, which expires
in 2015.
Cephalon filed separate patent infringement suits against the generic drugmakers
in 2003, triggering a 30-month stay of approval of the ANDAs. The FTC says in
its complaint that Cephalon would not have prevailed in litigation against all
four companies. However, before the litigation could conclude, Cephalon set
about settling with each of the defendants.
Cephalon agreed to allow the generic companies to launch their products in April
2012, but the company "had to provide other inducements to the first filers to
secure their agreement to refrain from competing," the FTC writes.
Release date: Feb. 18, 2008
LOAD-DATE: February 15, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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256 of 998 DOCUMENTS
Washington Drug Letter
February 18, 2008 Monday
FTC Accuses Cephalon of Buying Off Generic Competition
SECTION: Vol. 40 No. 7
LENGTH: 914 words
Cephalon's "anticompetitive conduct" to protect its top-selling product, which
involved paying four firms to refrain from selling generic versions of Provigil
until 2012, extended the company's monopoly on the drug beyond the scope of its
patent protection and cost patients and payers millions of dollars a year, the
FTC alleges in a complaint against the company.
Provigil (modafinil), originally approved in 1998, is indicated for improving
wakefulness in adults who experience excessive sleepiness due to obstructive
sleep apnea, shift work sleep disorder or narcolepsy. The drug is unique among
wakefulness treatments and is considered the gold standard for treating
excessive sleepiness, according to the FTC's Feb. 13 complaint, filed in the
U.S. District Court for the District of Columbia. Cephalon's recent earnings
announcement showed that Provigil had U.S. sales of more than $800 million in
2007.
Because Cephalon's compound patent for modafinil expired in 2001, Provigil is
only protected by the '516 formulation patent relating to particle size that
generic companies could easily design around, the FTC says.
In fact, in 2002 Teva Pharmaceuticals, Ranbaxy Pharmaceuticals, Mylan and Barr
Laboratories simultaneously submitted abbreviated new drug applications (ANDAs)
for generic Provigil with Paragraph IV certifications that the '516 patent was
invalid or that their products would not infringe on the patent, which expires
in 2015. As first filers, the four companies would have shared 180-day
exclusivity for generic Provigil, and under Hatch-Waxman, the FDA would not have
been able to approve any other generic versions of the drug until the
exclusivity expired.
Cephalon filed separate patent infringement suits against the generic drugmakers
in 2003, triggering a 30-month stay of approval of the ANDAs. The FTC says in
its complaint that Cephalon would not have prevailed in litigation against all
four companies. However, before the litigation could conclude, Cephalon set
about settling with each of the defendants.
Cephalon agreed to allow the generic companies to launch their products in April
2012, but the company "had to provide other inducements to the first filers to
secure their agreement to refrain from competing," the FTC writes.
Deals Delaying Generic Entry
The company achieved this by entering into seemingly separate transactions with
the generic firms worth more than $200 million total, the agency says. For
example, Teva agreed not to launch generic Provigil until April 2012 in exchange
for a license agreement relating to Teva's modafinil patents and patent
applications worth up to $125 million in Provigil royalties. Cephalon also
agreed to buy modafinil active pharmaceutical ingredient from Teva at prices
higher than what it was already paying.
The FTC alleges that Cephalon did not need the license or supply agreement
because it was already successfully making and selling Provigil. Cephalon
executed similar deals with the other generic firms. Cephalon says in a
statement that the settlement agreements seek to allow generic Provigil entry
three years prior to the expiration of the drug's patent protection, but the FTC
argues that some or all of the first filers would have launched their generics
in June 2006 at the end of the 30-month stay or upon a favorable ruling.
The agency notes that many parties had expected to see generic Provigil entry in
2006, and Cephalon had made plans to launch an authorized generic and introduce
its successor product, Nuvigil (armodafinil). Therefore, the FTC concludes that
Cephalon harmed consumers, "abused" the Hatch-Waxman Act and violated the FTC
Act. Not only did the agreements eliminate potential competition from the four
generic firms involved, they prevented any other generic drugmakers from
obtaining approval for and launching generic Provigil.
"Cephalon prevented competition to Provigil by agreeing to share its future
monopoly profits with generic drugmakers poised to enter the market, in exchange
for delayed generic entry," FTC Bureau of Competition Director Jeffrey Schmidt
says in a statement. "Such conduct is at the core of what the antitrust laws
proscribe."
The FTC asks the court to issue a permanent injunction preventing Cephalon from
enforcing the settlement agreements or from executing similar deals in the
future. Cephalon says it is "prepared to vigorously defend itself in this matter
and expects to prevail."
While the FTC vote approving the complaint was 5-0, Commissioner Jon Leibowitz
issued a statement dissenting in part. He says he would have named the generic
companies as defendants in the case unless they chose to relinquish their
180-day exclusivity, allowing other companies that have received tentative
approval for their generic Provigil ANDAs to receive final approval and launch.
He recommends that Congress act on legislation -- the Preserve Access to
Affordable Generics Act, S. 316 and H.R. 1432 -- that would ban settlements
involving payments in exchange for delayed generic entry. He also suggests that
Congress "consider asking these [generic companies] whether they are willing to
waive [180-day exclusivity] that arguably has very little financial value to
them when the benefits of waivers to American consumers seem so substantial --
and if not, why not."
Teva said it had no comment on the status of its agreement with Cephalon.
Ranbaxy, Mylan and Barr could not be reached for comment by press time. -- Breda
Lund
Release date: Feb. 18, 2008
LOAD-DATE: February 15, 2008
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All Rights Reserved
257 of 998 DOCUMENTS
Drug Industry Daily
February 15, 2008 Friday
FTC Accuses Cephalon of Buying Off Generic Competition
SECTION: Vol. 7 No. 32
LENGTH: 918 words
Cephalon's "anticompetitive conduct" to protect its top-selling product, which
involved paying four firms to refrain from selling generic versions of Provigil
until 2012, extended the company's monopoly on the drug beyond the scope of its
patent protection and cost patients and payers millions of dollars a year, the
FTC alleges in a complaint against the company.
Provigil (modafinil), originally approved in 1998, is indicated for improving
wakefulness in adults who experience excessive sleepiness due to obstructive
sleep apnea, shift work sleep disorder or narcolepsy. The drug is unique among
wakefulness treatments and is considered the gold standard for treating
excessive sleepiness, according to the FTC's Feb. 13 complaint, filed in the
U.S. District Court for the District of Columbia. Cephalon's recent earnings
announcement showed that Provigil had U.S. sales of more than $800 million in
2007.
Because Cephalon's compound patent for modafinil expired in 2001, Provigil is
only protected by the '516 formulation patent relating to particle size that
generic companies could easily design around, the FTC said.
In fact, in 2002 Teva Pharmaceuticals, Ranbaxy Pharmaceuticals, Mylan and Barr
Laboratories simultaneously submitted abbreviated new drug applications (ANDAs)
for generic Provigil with Paragraph IV certifications that the '516 patent was
invalid or that their products would not infringe on the patent, which expires
in 2015.
As first filers, the four companies would have shared 180-day exclusivity for
generic Provigil, and under Hatch-Waxman, the FDA would not have been able to
approve any other generic versions of the drug until the exclusivity expired.
Cephalon filed separate patent infringement suits against the generic drugmakers
in 2003, triggering a 30-month stay of approval of the ANDAs. The FTC said in
its complaint that Cephalon would not have prevailed in litigation against all
four companies. However, before the litigation could conclude, Cephalon set
about settling with each of the defendants.
Cephalon agreed to allow the generic companies to launch their products in April
2012, but the company "had to provide other inducements to the first filers to
secure their agreement to refrain from competing," the FTC wrote.
Deals Delaying Generic Entry
The company achieved this by entering into seemingly separate transactions with
the generic firms worth more than $200 million total, the agency said. For
example, Teva agreed not to launch generic Provigil until April 2012 in exchange
for a license agreement relating to Teva's modafinil patents and patent
applications worth up to $125 million in Provigil royalties. Cephalon also
agreed to buy modafinil active pharmaceutical ingredient from Teva at prices
higher than what it was already paying.
The FTC alleged that Cephalon did not need the license or supply agreement
because it was already successfully making and selling Provigil. Cephalon
executed similar deals with the other generic firms.
Cephalon said in a statement that the settlement agreements seek to allow
generic Provigil entry three years prior to the expiration of the drug's patent
protection, but the FTC argued that some or all of the first filers would have
launched their generics in June 2006 at the end of the 30-month stay or upon a
favorable ruling.
The agency noted that many parties had expected to see generic Provigil entry in
2006, and Cephalon had made plans to launch an authorized generic and introduce
its successor product, Nuvigil (armodafinil).
Therefore, the FTC concluded that Cephalon harmed consumers, "abused" the
Hatch-Waxman Act and violated the FTC Act. Not only did the agreements eliminate
potential competition from the four generic firms involved, they prevented any
other generic drugmakers from obtaining approval for and launching generic
Provigil.
"Cephalon prevented competition to Provigil by agreeing to share its future
monopoly profits with generic drugmakers poised to enter the market, in exchange
for delayed generic entry," FTC Bureau of Competition Director Jeffrey Schmidt
said in a statement. "Such conduct is at the core of what the antitrust laws
proscribe."
The FTC asked the court to issue a permanent injunction preventing Cephalon from
enforcing the settlement agreements or from executing similar deals in the
future. Cephalon said it is "prepared to vigorously defend itself in this matter
and expects to prevail."
Generics Off the Hook
While the FTC vote approving the complaint was 5-0, Commissioner Jon Leibowitz
issued a statement dissenting in part. He said he would have named the generic
companies as defendants in the case unless they chose to relinquish their
180-day exclusivity, allowing other companies that have received tentative
approval for their generic Provigil ANDAs to receive final approval and launch.
He recommended that Congress act on legislation -- the Preserve Access to
Affordable Generics Act, S. 316 and H.R. 1432 -- that would ban settlements
involving payments in exchange for delayed generic entry. He also suggested that
Congress "consider asking these [generic companies] whether they are willing to
waive [180-day exclusivity] that arguably has very little financial value to
them when the benefits of waivers to American consumers seem so substantial --
and if not, why not."
Teva said it had no comment on the status of its agreement with Cephalon.
Ranbaxy, Mylan and Barr could not be reached for comment by press time. -- Breda
Lund
Release date: Feb. 15, 2008
LOAD-DATE: February 14, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2008 Washington Business Information, Inc.
All Rights Reserved
258 of 998 DOCUMENTS
Daily Mail (London)
February 12, 2008 Tuesday
ADHD drug can tackle tinnitus;
GOOD HEALTH
SECTION: 1ST; Pg. 48
LENGTH: 123 words
A DRUG used to treat hyperactivity and sleep disorders is being prescribed to
people with tinnitus.
Patients with the condition are being given a two-week course of daily modafinil
as part of a clinical trial at Arkansas University, in the U.S.
Researchers believe that brain activity associated with tinnitus buzzing,
whistling, ringing or hissing in the ear can be reduced by the therapy. It may
also help with associated insomnia and depression.
Modafinil is already being used to treat narcolepsy, an extreme form of daytime
sleepiness, and attention deficit hyperactive disorder.
How it works on tinnitus is not yet clear, but in narcolepsy it changes the
amounts of chemicals in the area of the brain that controls sleep and
wakefulness..
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PUBLICATION-TYPE: Papers
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259 of 998 DOCUMENTS
Clinical Psychiatry News
February 2008
Modafinil Helps Some Cocaine Dependence
BYLINE: Bruce Jancin, Denver Bureau
SECTION: Pgs. 40-41 Vol. 36 No. 2 ISSN: 0270-6644
LENGTH: 595 words
VIENNA - Modafinil has now been found to be effective for the treatment of
cocaine dependence in two randomized clinical trials, Frank J. Vocci, Ph.D.,
reported at the annual congress of the European College of
Neuropsychopharmacology.
The caveat is that modafinil (Provigil) does not appear to work in
individuals who are both cocaine and alcohol dependent, which is a common
situation among cocaine users, said Dr. Vocci, director of the division of
pharmacotherapies and medical consequences of drug abuse at the National
Institute of Mental Health, Bethesda, Md.
Modafinil is approved by the Food and Drug Administration to promote
wakefulness in adults who have excessive daytime sleepiness that is associated
with sleep apnea/hypopnea syndrome, narcolepsy, or shift work sleep disorder.
The drug has several effects making it of interest as a potential treatment
for cocaine dependence, including increases in brain glutamate and gamma amino
butyric acid (GABA).
In laboratory studies, modafinil produced clinical effects opposite to those
seen in cocaine withdrawal, reduced cocaine self-administration, diminished
cocaine-induced euphoria, attenuated the cardiovascular effects of large doses
of cocaine, and showed no untoward effects in combination with the drug of
abuse. However, "we still don't have any idea how it's working [as a treatment
for cocaine dependence] in terms of mechanisms," Dr. Vocci said.
The first clinical trial to demonstrate efficacy was an 8-week, randomized
double-blind study involving 62 treatment-seeking cocaine-dependent patients at
the University of Pennsylvania. Participants received a single daily morning
dose of 400 mg of modafinil or placebo plus twice-weekly manual-guided
cognitive-behavioral therapy (CBT).
The primary outcome-the mean proportion of clean urine samples during the 8
weeks-was 42% in the modafinil group and 24% with placebo. Moreover, 33% of the
patients in the modafinil arm achieved 3 consecutive weeks of clean urine
samples at some point during the study period, compared with 13% of the
controls.
There were, however, no significant differences between the two study groups
in any secondary outcome measures, including craving scores and patient-reported
cocaine use (Neuropsychopharmacology 2005;30:205-11).
In a recently completed, not yet published phase II multicenter double-blind
trial, 210 cocaine-dependent patients were randomized to receive modafinil at
200 mg or 400 mg once daily or placebo for 12 weeks. All subjects received
manualized CBT once a week. A total of 122 participants completed the study.
The primary outcome measure was the maximum number of consecutive days
without cocaine use as determined by urine testing and patient self-report.
The mean maximum was 8.8 days with placebo, 12.6 days with 200 mg/day of
modafinil, and 12 days with modafinil at 400 mg daily.
That is a less robust treatment effect than had been seen in the earlier
single-center trial. But patients with comorbid alcohol dependence were excluded
from that earlier trial while roughly 40% in the larger trial were both cocaine
and alcohol dependent.
Upon closer analysis of the multicenter trial data, researchers found a
statistically significant benefit for modafinil in reducing cocaine use that was
confined to the non-alcohol-dependent subgroup, Dr. Vocci said.
Both trials were funded by the National Institute on Drug Abuse.
Despite several decades of research, there remains no approved
pharmacotherapy for cocaine dependence.
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The Chronicle of Higher Education
January 11, 2008 Friday
Mind-Boosting Drugs in the Faculty Lounge Create Controversy
BYLINE: RICHARD MONASTERSKY
SECTION: THE FACULTY; Pg. 14 Vol. 54 No. 18
LENGTH: 884 words
While caffeine reigns as the supreme drug of the professoriate, some university
faculty members have started popping "smart" pills to enhance their mental
energy and ability to work long hours, according to two University of Cambridge
scientists.
In a commentary published in the journal Nature last month, Barbara Sahakian and
Sharon Morein-Zamir revealed the results of their informal survey of a handful
of colleagues who study drugs that help people perform better mentally.
Ms. Morein-Zamir said they asked "fewer than 10" colleagues who have done
research on cognitive-enhancing drugs, such as Provigil, which is approved in
the United States to treat narcolepsy and other severe sleep disorders. "We know
that some people, academics -- they could be philosophers or ethicists or people
who do neuroscience -- they chose to take some of these drugs," said Ms.
Morein-Zamir.
But brain boosting raises hackles in some parts of academe. "It smells to me a
lot like taking steroids for physical prowess," said Barbara Prudhomme White, an
associate professor of occupational therapy at the University of New Hampshire,
who has studied the abuse of Ritalin by college students. After recent
revelations about the use of performance-enhancing drugs in professional
baseball, she sees parallels between athletes and assistant professors. "You're
expected to publish and teach, and the stakes are high. So young professors have
to work their tails off to get that golden nugget of tenure."
The poll was not meant to be a comprehensive study, said Ms. Morein-Zamir, a
research associate at Cambridge. Rather, the essay, "Professor's Little Helper,"
was intended to provoke a public discussion of whether society in general, and
universities in particular, should regulate the use of available compounds and
medications that might be developed in the future. "If a drug helps you be more
alert but also make better decisions, how does society feel about that?" she
asked.
The colleagues they contacted had not used stimulants such as Ritalin or
Adderall but had used Provigil, known generically as modafinil. Although it is
approved only to treat sleep-related disorders, there have been hints that
modafinil can also improve cognitive performance.
In 2003, Ms. Sahakian and colleagues reported that normal subjects performed
better on certain types of cognitive tests and felt more alert after taking
modafinil, compared with people who had taken a placebo. Soldiers in Iraq,
according to reports, have also used the drug.
The Thinking Man's Drug
When the Cambridge researchers asked their colleagues why they used modafinil,
the answers included "to stay awake, to stay focused, to be on the ball, for
sustained hard thinking, to stay focused for extended amounts of time," said Ms.
Morein-Zamir. One academic in the United States obtained the drug from a
primary-care doctor and uses it to combat jet lag. A British researcher, who got
modafinil via an Internet site, said he used it fortnightly to enhance
productivity and for important intellectual challenges.
Although the drug is not approved to treat jet lag, many doctors are apparently
willing to prescribe it for that purpose. "I would say it's fairly common, by
which I mean that I know several people who use it occasionally for purposes of
counteracting jet lag," said Martha J. Farah, a professor of psychology at the
University of Pennsylvania. She notes that she has used it herself on two
overseas trips. "Many academics do take it for that purpose, often after getting
a prescription from their physician."
Neuroscientists may be the early adopters in academe because they know more
about the drug. And some go beyond using it for jet lag. After Ms. Farah gave a
talk on cognitive-enhancing drugs, a graduate student approached her to say that
he takes modafinil at the end of each week to finish all his work. The drug
enables him to work all night.
Ms. Farah said that she was tempted to use the drug regularly, but that she
decided against it. "This is a little too good to be true," she said. "I think
as society becomes more experienced with these medications, we'll have a better
sense of what are their hidden downsides." For example, she notes, cheating the
body of sleep suppresses the immune system and impairs brain function. "There's
no reason to believe that modafinil is protecting you from these really bad
effects."
In fact, although cognitive-enhancing drugs have been on the market for decades,
it sometimes takes that long for side effects to become apparent. A major study
published in August showed that children with ADHD who had taken stimulants grew
less than children with ADHD who did not take the drugs.
Modafinil is widely regarded as having fewer side effects than stimulants like
Ritalin, but the Food and Drug Administration warned doctors in October about
some rare but potentially life-threatening conditions associated with the drug:
skin rashes, hypersensitivity that can damage organs, and adverse psychiatric
reactions.
Even with such warnings, the allure of chemicals that confer an advantage may be
hard to resist for academics, given the pressures they face. If there were a
cognitive-enhancing drug that did not have side effects, said Ms. Prudhomme
White, "would I be tempted? Damn right I would. Who wouldn't be?"
LOAD-DATE: January 8, 2008
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The Herald (Glasgow)
January 3, 2008 Thursday
Final Edition
Brain-boosting drugs could soon become the smart choice;
SCIENCE NOTEBOOK
BYLINE: James Morgan
SECTION: FEATURES; Pg. 17
LENGTH: 874 words
DURING a quiet moment in the pub over Christmas, a friend of mine leaned over
and whispered in my ear. "Do you know where I can get my hands on some smart
pills?"
Like me, the friend . . . who works for an engineering firm . . . had heard the
rumours about modafinil, one of a powerful new breed of brainboosting drugs that
enhance concentration, memory and mental aptitude. Medicines which were designed
to treat brain injury, dementia and ADHD are now becoming popular pick-me ups.
Businessmen take them to beat jet lag, academics pop them to sharpen their minds
and shift workers take them to stay alert.
Online you can find web chat rooms full of glowing testimonies from users, but
as the popularity of smart pills spirals, experts are warning that, with no real
knowledge of long-term health risks, users are making themselves guinea pigs. In
a recent commentary in the journal Nature, Professor Barbara Sahakian and Dr
Sharon Morein-Zamir called for a national debate on "cognitive enhancers" and
their potential impact on society. Are smart pills "unfair", they ask, and
should we do anything to regulate them?
To address their questions, we should begin by looking at currently available
cognitive enhancers. Perhaps the nearest thing we have to the ideal "smart pill"
is modafinil, a drug designed to treat narcolepsy, which is reportedly being
used by businessmen and others to overcome tiredness.
"We know that a number of our scientific colleagues in the US and the UK already
use modafinil to counteract the effects of jetlag, to enhance productivity or
mental energy, or to deal with demanding and important intellectual challenges"
says Sahakian.
Recent paparazzi shots revealed a packet of a brand of modafinil . . . Provigil
. . . in Britney Spears's handbag.
Although there are side effects . . . headaches and nausea . . . they appear to
be mild. One survey found that as many as 10% of students at American
universities are using Ritalin and Adderall . . . ADHD drugs . . . to improve
their performance.
Ritalin helps hyperactive children to focus on one thing at a time, but when
used in otherwise healthy adults it makes them feel more alert and full of
energy . . . unsurprising when you find out that the active ingredient is
amphetamine. However, its side effects include sleeplessness, loss of appetite
and in rare cases, hallucinations.
Other so-called smart pills include Aricept (donepezil), an Alzheimer's drug,
which studies found could improve the memory of fighter pilots learning new
moves on a flight simulator. Finally and potentially the most powerful of all
are ampakines, a new untested class of drug designed to boost memory and improve
alertness, without giving users the dreaded caffeine shakes.
Does that sound tempting?
Most of us can imagine a situation at work where we would benefit from a little
cognitive enhancement. And is that really such a crime?
"People have all sorts of natural advantages . . . some are cleverer, stronger
or more beautiful than others, " says Michael Gazzaniga, president of the
Cognitive Neuroscience Institute in America. "If we can boost our abilities to
make up for the ones Mother Nature didn't give us, what is wrong with that?"
After all, as the Nature authors point out: "Most readers would not consider
that having a double shot of espresso or a soft drink containing caffeine would
confer an unfair advantage at work. [So] does it matter if it is delivered as a
pill or a drink?"
Indeed, they argue that there are situations in which the use of drugs to
improve concentration or planning "may be tolerated, if not encouraged", such as
by "airtraffic controllers, surgeons and nurses who work long shifts,
airport-security screeners, or by soldiers in active combat".
However, they are quick to point out the f lipside. "Universities may have to
decide whether to ban drug use altogether, or to tolerate it in some situations
. . . whether to enable all-night study sessions or to boost alertness during
lectures, " they say.
Their biggest concern is for children. The long-term effects of many cognitive
enhancers on the developing brains is still unknown.
So what form should any regulation take? Should they only be available on
prescription?
"We believe it would be difficult to stop the spread in use of cognitive
enhancers given a global market in pharmaceuticals with increasingly easy online
access. They call on scientists, doctors and policymakers to "provide easy
access to information about the advantages and dangers of using
cognitive-enhancing drugs and set out clear guidelines for their future use."
A softer approach is possible, they say, because at present, cognitive enhancers
are "relatively safe" and yield "only moderate effects". But, with increasingly
sophisticated and even genetically-tailored treatments, truly smart drugs with
dangerous large effects on cognition will become feasible.
"Fears have been raised of an overworked 24/7 society pushed to the limits of
human endurance, or of direct and indirect coercion into taking such drugs, "
they say.
"If other colleagues at work, or children at your child's school, are taking
cognitive-enhancing drugs, will you feel pressure to take them yourself?"
For many, this is no longer a theoretical question.
LOAD-DATE: January 8, 2008
LANGUAGE: ENGLISH
GRAPHIC: CLEVER THINKING: Use of mind enhancing drugs is on the rise.
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Clinical Psychiatry News
January 2008
News From The FDA Revised Modafinil Label Cites Psychiatric Risks
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 3 Vol. 36 No. 1 ISSN: 0270-6644
LENGTH: 660 words
Warnings about serious rashes-including Stevens-Johnson syndrome and
hypersensitivity reactions-as well as psychiatric symptoms have been added to
the label of modafinil, according to a MedWatch notice issued by the Food and
Drug Administration.
Modafinil, described as a "wakefulness-promoting agent," is marketed as
Provigil by Cephalon Inc., and was first approved as a treatment for narcolepsy
in 1998. It is approved for improving wakefulness in adults with excessive
sleepiness associated with narcolepsy, obstructive sleep apnea/hypopnea
syndrome, and shift-work sleep disorder. It is not approved for any pediatric
indications, the advisory emphasizes, although some reports have been in
children.
The MedWatch notice and a "Dear Healthcare Professional" letter issued by
Cephalon late last year, describe worldwide postmarketing reports of
life-threatening rash, including toxic epidermal necrolysis (TEN), and drug rash
with eosinophilia and systemic symptoms (DRESS) in adults and children. There
have also been postmarketing reports of angioedema and multiorgan
hypersensitivity reactions.
The reporting rate-which is considered an underestimate, because
postmarketing reports of adverse events tend to be underreported-of TEN and
Stevens-Johnson syndrome (SJS) associated with modafinil use is higher than the
background incidence rate, according to the letter. The background in the
general population is estimated at 1-2 million cases per million person-years.
The potential for benign rashes-which have been associated with modafinil
use-to develop into serious rashes cannot be reliably predicted, so "modafinil
should ordinarily be discontinued at the first sign of rash, unless the rash is
clearly not drug-related," the letter says. However, stopping treatment "may not
prevent a rash from becoming life-threatening or permanently disabling or
disfiguring."
Because of postmarketing reports of angioedema, the letter says that patients
should be advised to stop treatment and "immediately report to their physician
any signs of symptoms suggesting angioedema or anaphylaxis," which includes
swelling of the face, eyes, lips, tongue, or larynx; difficult breathing or
swallowing; and hoarseness. There have also been postmarketing reports of
multiorgan hypersensitivity reactions, including at least one fatal case, which
have occurred "in close temporal association to the initiation of modafinil."
Modafinil should be discontinued if such a rash is suspected.
The letter also recommends that discontinuation of the drug should be
considered in patients who develop psychiatric symptoms during treatment,
because mania, anxiety, hallucinations, and suicidal ideation are among the
psychiatric adverse reactions reported in people treated with modafinil. In
addition, "caution should be exercised" when the drug is prescribed to patients
with a history of psychosis, depression, or mania.
Cephalon had pursued approval of modafinil as a treatment for
attention-deficit/hyperactivity disorder in children and adolescents, but in
March 2006, the FDA's Psychopharmacologic Drugs Advisory Panel agreed that the
drug was not safe for treating children and adolescents, largely because of
concerns about its potential to cause SJS in this population. Last summer,
Cephalon announced that it had received a "non-approvable" letter from the FDA
for this indication and had stopped developing the drug.
The "Dear Healthcare Professional" letter says that in studies, the incidence
of rash resulting in discontinuation of the drug in pediatric patients (younger
than age 17 years) was 0.8% (13 of 1,585); these cases included one case of
possible SJS and one case of what appeared to be a multiorgan hypersensitivity
reaction.
Adverse reactions should be reported to the FDA's MedWatch program at
800-332-1088 or www.fda.gov/medwatch. For more information, visit
www.fda.gov/medwatch/safety/2007/safety07.htm#Provigil.
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The Herald (Glasgow)
January 1, 2008 Tuesday
Final Edition
Brain-boosting drugs could soon become the smart choice;
SCIENCE NOTEBOOK
BYLINE: James Morgan
SECTION: FEATURES; Pg. 17
LENGTH: 874 words
DURING a quiet moment in the pub over Christmas, a friend of mine leaned over
and whispered in my ear. "Do you know where I can get my hands on some smart
pills?"
Like me, the friend . . . who works for an engineering firm . . . had heard the
rumours about modafinil, one of a powerful new breed of brainboosting drugs that
enhance concentration, memory and mental aptitude. Medicines which were designed
to treat brain injury, dementia and ADHD are now becoming popular pick-me ups.
Businessmen take them to beat jet lag, academics pop them to sharpen their minds
and shift workers take them to stay alert.
Online you can find web chat rooms full of glowing testimonies from users, but
as the popularity of smart pills spirals, experts are warning that, with no real
knowledge of long-term health risks, users are making themselves guinea pigs. In
a recent commentary in the journal Nature, Professor Barbara Sahakian and Dr
Sharon Morein-Zamir called for a national debate on "cognitive enhancers" and
their potential impact on society. Are smart pills "unfair", they ask, and
should we do anything to regulate them?
To address their questions, we should begin by looking at currently available
cognitive enhancers. Perhaps the nearest thing we have to the ideal "smart pill"
is modafinil, a drug designed to treat narcolepsy, which is reportedly being
used by businessmen and others to overcome tiredness.
"We know that a number of our scientific colleagues in the US and the UK already
use modafinil to counteract the effects of jetlag, to enhance productivity or
mental energy, or to deal with demanding and important intellectual challenges"
says Sahakian.
Recent paparazzi shots revealed a packet of a brand of modafinil . . . Provigil
. . . in Britney Spears's handbag.
Although there are side effects . . . headaches and nausea . . . they appear to
be mild. One survey found that as many as 10% of students at American
universities are using Ritalin and Adderall . . . ADHD drugs . . . to improve
their performance.
Ritalin helps hyperactive children to focus on one thing at a time, but when
used in otherwise healthy adults it makes them feel more alert and full of
energy . . . unsurprising when you find out that the active ingredient is
amphetamine. However, its side effects include sleeplessness, loss of appetite
and in rare cases, hallucinations.
Other so-called smart pills include Aricept (donepezil), an Alzheimer's drug,
which studies found could improve the memory of fighter pilots learning new
moves on a flight simulator. Finally and potentially the most powerful of all
are ampakines, a new untested class of drug designed to boost memory and improve
alertness, without giving users the dreaded caffeine shakes.
Does that sound tempting?
Most of us can imagine a situation at work where we would benefit from a little
cognitive enhancement. And is that really such a crime?
"People have all sorts of natural advantages . . . some are cleverer, stronger
or more beautiful than others, " says Michael Gazzaniga, president of the
Cognitive Neuroscience Institute in America. "If we can boost our abilities to
make up for the ones Mother Nature didn't give us, what is wrong with that?"
After all, as the Nature authors point out: "Most readers would not consider
that having a double shot of espresso or a soft drink containing caffeine would
confer an unfair advantage at work. [So] does it matter if it is delivered as a
pill or a drink?"
Indeed, they argue that there are situations in which the use of drugs to
improve concentration or planning "may be tolerated, if not encouraged", such as
by "airtraffic controllers, surgeons and nurses who work long shifts,
airport-security screeners, or by soldiers in active combat".
However, they are quick to point out the f lipside. "Universities may have to
decide whether to ban drug use altogether, or to tolerate it in some situations
. . . whether to enable all-night study sessions or to boost alertness during
lectures, " they say.
Their biggest concern is for children. The long-term effects of many cognitive
enhancers on the developing brains is still unknown.
So what form should any regulation take? Should they only be available on
prescription?
"We believe it would be difficult to stop the spread in use of cognitive
enhancers given a global market in pharmaceuticals with increasingly easy online
access. They call on scientists, doctors and policymakers to "provide easy
access to information about the advantages and dangers of using
cognitive-enhancing drugs and set out clear guidelines for their future use."
A softer approach is possible, they say, because at present, cognitive enhancers
are "relatively safe" and yield "only moderate effects". But, with increasingly
sophisticated and even genetically-tailored treatments, truly smart drugs with
dangerous large effects on cognition will become feasible.
"Fears have been raised of an overworked 24/7 society pushed to the limits of
human endurance, or of direct and indirect coercion into taking such drugs, "
they say.
"If other colleagues at work, or children at your child's school, are taking
cognitive-enhancing drugs, will you feel pressure to take them yourself?"
For many, this is no longer a theoretical question.
LOAD-DATE: January 4, 2008
LANGUAGE: ENGLISH
GRAPHIC: CLEVER THINKING: Use of mind enhancing drugs is on the rise.
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: GH
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Internal Medicine News
January 1, 2008
Postmarket Reports Spur New Modafinil Warnings
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 24 Vol. 41 No. 1 ISSN: 1097-8690
LENGTH: 628 words
Warnings about serious rashes-including Stevens-Johnson syndrome and
hypersensitivity reactions-as well as psychiatric symptoms have been added to
the label of modafinil, according to a MedWatch notice issued by the Food and
Drug Administration.
Modafinil, described as a "wakefulness-promoting agent," is marketed as
Provigil by Cephalon Inc., and is approved for improving wakefulness in adults
with excessive sleepiness associated with narcolepsy, obstructive sleep
apnea/hypopnea syndrome, and shift-work sleep disorder. It is not approved for
any pediatric indications, the advisory emphasizes, although some reports have
been in children.
The MedWatch notice and a "Dear Healthcare Professional" letter issued by
Cephalon describe worldwide postmarketing reports of life-threatening rash,
including toxic epidermal necrolysis (TEN), and drug rash with eosinophilia and
systemic symptoms in adults and children. There have also been reports of
angioedema and multiorgan hypersensitivity reactions.
The reporting rate-which is considered an underestimate, because
postmarketing reports of adverse events tend to be underreported-of TEN and
Stevens-Johnson syndrome (SJS) associated with modafinil use is higher than the
background incidence rate, according to the letter. The background in the
general population is estimated at 1-2 million cases per million person-years.
The potential for benign rashes-which have been associated with modafinil
use-to develop into serious rashes cannot be reliably predicted, so "modafinil
should ordinarily be discontinued at the first sign of rash, unless the rash is
clearly not drug-related," the letter says. However, stopping treatment "may not
prevent a rash from becoming life-threatening or permanently disabling or
disfiguring."
Because of postmarketing reports of angioedema, the letter says that patients
should be advised to stop treatment and "immediately report to their physician
any signs of symptoms suggesting angioedema or anaphylaxis," which includes
swelling of the face, eyes, lips, tongue, or larynx; difficulty breathing or
swallowing; and hoarseness. There have also been postmarketing reports of
multiorgan hypersensitivity reactions, including at least one fatal case, which
have occurred "in close temporal association to the initiation of modafinil."
The letter also recommends that discontinuation of the drug should be
considered in patients who develop psychiatric symptoms during treatment,
because mania, anxiety, hallucinations, and suicidal ideation are among the
psychiatric adverse reactions reported in people treated with modafinil. In
addition, "caution should be exercised" when the drug is prescribed to patients
with as history of psychosis, depression, or mania.
Cephalon had pursued approval of modafinil as a treatment for ADHD in
children and adolescents, but in March 2006, the FDA's Psychopharmacologic Drugs
Advisory Panel agreed that the drug was not safe for treating children and
adolescents, largely because of concerns about its potential to cause SJS in
this population. Last summer, Cephalon announced that it had received a
"non-approvable" letter from the FDA for this indication and had stopped
developing the drug.
The "Dear Healthcare Professional" letter states that in studies, the
incidence of rash resulting in discontinuation of the drug in pediatric patients
(younger than age 17 years) was 0.8% (13 of 1,585); these cases included one
case of possible SJS and one case of what appeared to be a multiorgan
hypersensitivity reaction.
Adverse reactions should be reported to the FDA's MedWatch program at
800-332-1088 or www.fda.gov/medwatch. More information is available at
www.fda.gov/medwatch/safety/2007/safety07.htm#Provigil.
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The Times (London)
December 22, 2007, Saturday
Can new pills boost brains?
BYLINE: Mark henderson
SECTION: FEATURES; Body & Soul; Pg. 4
LENGTH: 653 words
Ritalin is well known as a treatment for attention deficit hyperactivity
disorder, and modafinil is widely prescribed for narcolepsy. These drugs,
however, also have a more controversial application. They are the first wave of
"cognitive enhancers", which can not only treat brain conditions but improve
healthy people's mental capabilities as well.
Modafinil, for example, can improve alertness, accuracy and short-term memory.
It is reportedly used by the US military to assist concentration, and it is
widely used in academia. Barbara Sahakian and Sharon Morein-Zamir, of the
University of Cambridge, write in this week's Nature that colleagues use it
freely to counter jet lag or to enhance productivity. There is also anecdotal
evidence that modafinil and Ritalin are popular with students, replacing coffee
and ProPlus pills as essay-crisis aids.
The idea of cognitive enhancement makes people uneasy. Some critics liken it to
the use of drugs in sport and consider it a form of academic cheating. Most of
these drugs are fairly new and there's only limited evidence that long-term use
is safe.
Another common objection is that "brain doping" amounts to buying intelligence,
and could widen the gap between haves and have-nots. The better off already have
academic advantages, and the benefits of cognitive enhancement could be limited
to those who can afford them. The left-leaning think-tank Demos has suggested
that universities back a ban with testing, to secure equal-opportunity brain
chemistry.
Neither argument, however, is entirely convincing. Chemical stimulation has long
been a part of higher education: the difference between modafinil and espresso
is one of degree. The doping analogy falls down because the drugs lack the known
serious side-effects of steroids: Ritalin, for example, has been taken safely by
millions of children.
Cognitive enhancers also improve concentration and alertness only for a
transient period: they do not influence underlying ability or diligence. A poor
student will be no cleverer on Ritalin, just better equipped to pull an
all-nighter. He'll not suddenly understand concepts he'd failed to grasp before.
Intellect and hard work will still be rewarded.
As for cost, while it is permitted for a child's parents to spend £ 20,000 a
year on private school fees, it's hard to object to pills that cost no more than
a Starbucks latte.
There is some merit in the view that individual liberty trumps concern, and that
adults should be allowed to decide for themselves what to put into their bodies.
It is also unlikely that prohibition would work. Cognitive enhancers are now
available very cheaply online and it would take international legislation to
control supply.
A British Medical Association report last month found that increasing use was
"imminent and inevitable", and a government report has predicted they will
become "as common as coffee".
Experience with drugs such as cannabis and Ecstasy has shown that bans do not
necessarily affect demand. Cognitive enhancers seem to have greater benefits and
fewer risks, and some people are going to want them.
Sahakian and Morein-Zamir, indeed, argue that a ban could be counterproductive
as well as pointless. One of the biggest dangers of these drugs is interactions
with other medications, and they make a sound case that it would be better for
GPs to supervise access than to leave the market to the internet. That way,
people will at least be reliably informed about safety evidence before they take
a decision.
It is welcome that society is starting to consider this issue. The debate,
though, should start from the premise that cognitive enhancers are already with
us and here to stay. Even if attempting to hold them back would be desirable,
which is far from clear, it would probably be futile. It will be far more
fruitful to think about how best to manage their implications.
Mark Henderson is Science Editor of The Times
LOAD-DATE: December 22, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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Hindustan Times
December 2, 2007 Sunday 11:36 AM EST
Drugs for sleep disorder also helps ice addicts
BYLINE: Report from Asian News International brought to you by HT Syndication.
LENGTH: 377 words
DATELINE: Sydney
Sydney, Dec. 2 -- A research has revealed that the medication used for the
treatment of sleep disorders could help ice addicts cut their drug use to half.
The study, led by James Shearer from the National Drug and Alcohol Research
Centre at the University of NSW, followed 80 heavy users of crystal
methamphetamine over 10 weeks and found a daily dose of modafinil, marketed as
Modavigil in Australia, significantly reduced their cravings for ice, saving
each user about 500 dollars a month.
Modafinil prevents nerve cells from re-absorbing dopamine once they release it
into the brain but does not cause the dramatic highs and lows associated with
most stimulants. It is not water-soluble and is destroyed at high temperatures
so cannot be injected or smoked, reducing the chances of it being abused, and is
not addictive.
James said the users, who all either injected or smoked ice at least 20 days a
month and spent about 100 dollars a day on the drug, were given one tablet of
modafinil a day or a placebo.
About 12 weeks after the trial, those who had been given modafinil were using
ice about eight days in every 28, compared to the placebo group who were using
an average of 13.5 days.
After 22 weeks, those on modafinil were using 11 days a month, and the placebo
group 16 days.
"Six months after the trial, we still have better outcomes," the Sydney Morning
Herald quoted Shearer, as saying.
He added: "It is the first medication to show a demonstrable positive effect in
heavy methamphetamine users and represents a major medical breakthrough in
Australia.
"Modafinil doesn't give them that euphoric feeling, but it does give them a bit
of get up and go."
He said that like methadone, it would not be used as a maintenance drug, but
could be given to people in conjunction with extensive counselling and support.
The use of crystal methamphetamine has decreased in recent months for the first
time in a decade, which experts have attributed to the drug's negative effects.
Ice use has been associated with a steady rise in psychosis cases and deaths in
recent years.
The study's findings were presented at the World Psychiatric Association
Congress in Melbourne.
Published by HT Syndication with permission from Asian News International.
LOAD-DATE: December 2, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
267 of 998 DOCUMENTS
ABC Premium News (Australia)
December 1, 2007 Saturday 1:44 PM AEST
Sleep medicine 'can help ice addicts quit'
BYLINE: Michael Turtle
LENGTH: 444 words
Australian researchers say they have discovered a way to rehabilitate people
addicted to the drug 'ice'.
In what they call a world first, researchers from the National Drug and Alcohol
Research Centre say they have discovered that Modafinil, a medication currently
used to treat sleep disorders, can help ice addicts quit.
The discovery of Modafinil's potential for fighting ice addiction comes after
much media attention on what some experts say is an ice epidemic.
The latest national figures show that as many as 70,000 people use ice -
otherwise known as crystal methamphetamine hydrochloride.
Researcher James Shearer explains how ice affects the brain.
"What ice, or crystal, does is it actually hooks into your reward system in the
brain, and the reward system is designed so that you can recognise positive
stimuli, remember them, act on them," he said.
"But by overdoing it, by chronic use, you end up with a depletion of these
neurotransmitters."
He says Modafinil is normally used to treat sleeping problems like narcolepsy or
shift work sleep disorder, and acts on the same parts of the brain as ice does.
"Modafinil actually works in those parts of the brain to kind of restore areas
of those neurotransmitters," he said.
"So that's what we think kind of reinforces the addiction in people, because
they've got this neurotransmitter imbalance, as soon as they stop using ice, or
crystal, they go into withdrawal.
"So what we're hoping, by using Modafinil, is that they will be able to resist
those kind of relapse situations."
What this means is that Modafinil does not necessarily stop someone wanting to
use ice, but will help people who want to stop using it.
"As with all dependence - whether it's tobacco, alcohol, anything - you do need
the person themselves to be quite committed to making changes, because otherwise
these drugs don't work at all," he said.
"So it's really a supportive drug for someone who's making an effort to quit."
Mr Shearer says the finding is ground-breaking.
"This drug has been tested in the [United] States with cocaine, with very good
results," he said.
"What we've found in this study is we've exactly replicated those results from
the US, because cocaine, methamphetamine, they're all stimulants and they
actually do work in the same way in the brain."
"So we're all very excited and, frankly, relieved that we've actually found a
drug which helps."
The researchers now plan to do a larger study to confirm their results.
If Modafinil begins to be used in the general community, it could be prescribed
by doctors, rather than drug clinics. That's because, unlike something like
methadone, it would not be classed as a drug of addiction.
LOAD-DATE: December 1, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
268 of 998 DOCUMENTS
ABC Transcripts (Australia)
December 1, 2007 Saturday 8:15 AM AEST
SHOW: AM 8:15 AM AEST ABC
Sleep disorder medication may rehabilitate 'ice' addicts
REPORTERS: Michael Turtle
LENGTH: 490 words
ELIZABETH JACKSON: Australian researchers say they've discovered a way to
rehabilitate addicts of the drug 'ice'.
In what they call a world-first, the scientists say they've discovered a
medication, which already exists and is used to treat sleep disorders, can help
addicts quit.
Michael Turtle reports.
MICHAEL TURTLE: There's been much said in the media in the last year or so about
the increase in the use of crystal methamphetamine, or ice.
The latest figures show there could up to 70,000 users in Australia, and some
experts even say that the nation is in the grip of 'an ice epidemic'.
But now researchers from the National Drug and Alcohol Research Centre believe
they've found a medication that will help in battling the scourge.
The drug is called Modafinil and is normally used to treat sleeping problems
like narcolepsy or shift work sleep disorder.
Researcher James Shearer explains how it works:
JAMES SHEARER: What ice, or crystal, does is it actually hooks into your reward
system in the brain, and the reward system is designed so that you can recognise
positive stimuli, remember them, act on them. But by overdoing it, by chronic
use, you end up with a depletion of these neurotransmitters.
So this drug, Modafinil, actually works in those parts of the brain to kind of
restore areas of those neurotransmitters.
So that's what we think kind of reinforces the addiction in people, because
they've got this neurotransmitter imbalance, as soon as they stop using ice, or
crystal, they go into withdrawal. So what we're hoping, by using Modafinil, is
that they will be able to resist those kind of relapse situations.
MICHAEL TURTLE: So it doesn't necessarily stop someone wanting to use ice, but
for people who want to stop using it, it will help them.
JAMES SHEARER: Absolutely. Absolutely. As with all dependence, whether it's
tobacco, alcohol, anything, you do need the person themselves to be quite
committed to making changes, because otherwise these drugs don't work at all.
So it's really a supportive drug for someone who's making an effort to quit.
MICHAEL TURTLE: And is this quite ground-breaking? Have we seen this kind of
treatment for ice before?
JAMES SHEARER: Ah, this is ground-breaking in terms of ice. This drug has been
tested in the States with cocaine, with very good results.
What we've found in this study is we've exactly replicated those results from
the US, because cocaine, methamphetamine, they're all stimulants and they
actually do work in the same way in the brain.
So we're all very excited and, frankly, relieved that we've actually found a
drug which helps.
MICHAEL TURTLE: The researchers now plan to do a larger study to confirm their
results, and if Modafinil started to be used in the general community, it could
be prescribed by doctors, rather than drug clinics. That's because, unlike
something like methadone, it wouldn't be classed as a drug of addiction.
ELIZABETH JACKSON: Michael Turtle reporting.
LOAD-DATE: December 1, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Transcript
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All Rights Reserved
269 of 998 DOCUMENTS
Geelong Advertiser (Australia)
December 1, 2007 Saturday
Drug helps addicts break the ice habit
SECTION: NEWS; Pg. 40
LENGTH: 200 words
A DRUG that keeps narcoleptics awake and another that controls hyperactive kids
have been found to help Australian ice addicts kick their dangerous habit.
Fresh findings from two Australian drug trials have delivered new hope that
much-needed medications to treat crystal methamphetamine addiction are on the
horizon.
One world-first study by Sydney researchers found that the drug modafinil, used
to treat excessive sleepiness and fatigue, could help quash cravings in the
heaviest ice users.
Another medication, dexamphetamine, used widely to treat ADHD, was found by
Adelaide scientists to help wean users off the stimulant.
There is no treatment available for the 73,000 Australians addicted to
methamphetamines, renowned for causing extreme violence and psychosis.
The Sydney-based National Drug and Alcohol Research Centre presented the
findings from its modafinil study at the World Psychiatry Association conference
in Melbourne, with researchers labelling the effects ''dramatic''.
More than 80 users took either modafinil or a dummy medication daily for 10
weeks. Those who received modafinil cut their methamphetamine use by more than
half, significantly better than those who received the placebo.
LOAD-DATE: December 3, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: GAT
Copyright 2007 Nationwide News Pty Limited
All Rights Reserved
270 of 998 DOCUMENTS
Skin & Allergy News
December 2007
Modafinil: Rash Warning Is Issued by FDA, Manufacturer
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 8 Vol. 38 No. 12 ISSN: 0037-6337
LENGTH: 604 words
Warnings about serious rashes-including Stevens-Johnson syndrome and
hypersensitivity reactions-as well as psychiatric symptoms have been added to
the label of modafinil, according to a MedWatch notice issued by the Food and
Drug Administration.
Modafinil, described as a "wakefulness-promoting agent," is marketed as
Provigil by Cephalon Inc., and was first approved as a treatment for narcolepsy
in 1998.
It is approved for improving wakefulness in adults with excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome, and
shift-work sleep disorder. It is not approved for any pediatric indications, the
advisory emphasizes, although some reports have been in children.
The MedWatch notice and a "Dear Healthcare Professional" letter issued by
Cephalon describe worldwide postmarketing reports of life-threatening rash,
including toxic epidermal necrolysis (TEN), and drug rash with eosinophilia and
systemic symptoms (DRESS) in adults and children.
There have also been postmarketing reports of angioedema and multiorgan
hypersensitivity reactions.
The reporting rate of TEN and Stevens-Johnson syndrome (SJS) associated with
modafinil use is higher than the background incidence rate, according to the
letter.
The background in the general population is estimated at 1-2 million cases
per million person-years.
The potential for benign rashes-which have been associated with modafinil
use-to develop into serious rashes cannot be reliably predicted, so "modafinil
should ordinarily be discontinued at the first sign of rash, unless the rash is
clearly not drug-related," the letter says.
However, stopping treatment "may not prevent a rash from becoming
life-threatening or permanently disabling or disfiguring."
Because of postmarketing reports of angioedema, the letter says that patients
should be advised to stop treatment and "immediately report to their physician
any signs of symptoms suggesting angioedema or anaphylaxis," which includes
swelling of the face, eyes, lips, tongue, or larynx; difficult breathing or
swallowing; and hoarseness. There have also been postmarketing reports of
multiorgan hypersensitivity reactions, including at least one fatal case, which
have occurred "in close temporal association to the initiation of modafinil."
Modafinil should be discontinued if such a rash is suspected.
The letter also recommends that discontinuation of the drug should be
considered in patients who develop psychiatric symptoms during treatment,
because mania, anxiety, hallucinations, and suicidal ideation are among the
psychiatric adverse reactions reported in people treated with modafinil. In
addition, "caution should be exercised" when the drug is prescribed to patients
with a history of psychosis, depression, or mania.
Cephalon had pursued approval of modafinil as a treatment for
attention-deficit/hyperactivity disorder in children and adolescents, but in
March 2006, the FDA's Psychopharmacologic Drugs Advisory Panel agreed that the
drug was not safe for treating children and adolescents, largely because of
concerns about its potential to cause SJS in this population. Last summer,
Cephalon announced that it had received a "non-approvable" letter from the FDA
for this indication and had stopped developing the drug.
The "Dear Healthcare Professional" letter says that in studies, the incidence
of rash resulting in discontinuation of the drug in pediatric patients (younger
than age 17 years) was 0.8% (13 of 1,585).
More information is available at
http://www.fda.gov/medwatch/safety/2007/safety07.htm#Provigil.
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Sydney Morning Herald (Australia)
December 1, 2007 Saturday
First Edition
Sleep drug can halve ice addicts' cravings;
STUDY
BYLINE: Kate Benson Medical Reporter
SECTION: NEWS AND FEATURES; Pg. 12
LENGTH: 345 words
A MEDICATION used to treat sleep disorders has helped ice addicts cut their drug
use in half, researchers say.
The Sydney study followed 80 heavy users of crystal methamphetamine over 10
weeks and found a daily dose of modafinil, marketed as Modavigil in Australia,
significantly reduced their cravings for ice, saving each user about $500 a
month.
Modafinil prevents nerve cells from re-absorbing dopamine once they release it
into the brain but does not cause the dramatic highs and lows associated with
most stimulants. It is not water-soluble and is destroyed at high temperatures
so cannot be injected or smoked, reducing the chances of it being abused, and is
not addictive.
The study's author, James Shearer from the National Drug and Alcohol Research
Centre at the University of NSW, said the users, who all either injected or
smoked ice at least 20 days a month and spent about $100 a day on the drug, were
given one tablet of modafinil a day or a placebo.
About 12 weeks after the trial, those who had been given modafinil were using
ice about eight days in every 28, compared to the placebo group who were using
an average of 13.5 days.
At 22 weeks, those on modafinil were using 11 days a month, and the placebo
group 16 days.
"Six months after the trial, we still have better outcomes," Mr Shearer said.
"It is the first medication to show a demonstrable positive effect in heavy
methamphetamine users and represents a major medical breakthrough in Australia.
"Modafinil doesn't give them that euphoric feeling, but it does give them a bit
of get up and go."
It would not be used as a maintenance drug, like methadone, but could be given
to people in conjunction with extensive counselling and support, he said.
The use of crystal methamphetamine has dropped in recent months for the first
time in a decade, which experts have attributed to the drug's negative effects.
Ice use has been associated with a steady rise in psychosis cases and deaths in
recent years.
The study's findings were presented yesterday at the World Psychiatric
Association Congress in Melbourne.
LOAD-DATE: November 30, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 John Fairfax Publications Pty Ltd
All Rights Reserved
272 of 998 DOCUMENTS
Weekend Australian
December 1, 2007 Saturday
All-round Country Edition
Drug 'aids addicts to quit ice'
BYLINE: Adam Cresswell, Health editor
SECTION: LOCAL; Pg. 3
LENGTH: 343 words
USERS of methamphetamine could get a new treatment to help them quit the drug
after a world-first Australian study showed a medicine already on the shelves
helped addicts cut their use by more than 50 per cent.
The drug modafinil, used to treat sleep disorders, has been shown to help treat
cocaine addiction in the US. Now a federally funded Australian trial has shown
it could be a new treatment for methamphetamine addiction, by helping users
overcome their craving.
Experts welcomed the findings, saying doctors had few options to help people
hooked on methamphetamine, also known as ice.
Researchers from the National Drug and Alcohol Research Centre recruited 80
methamphetamine users trying to stop their habit and divided them into two
groups. All participants had used methamphetamine on an average of 20 days in
the previous 28 days.
One group received a daily dose of modafinil, while the other received a dummy
pill. For the duration of the 10-week trial, neither patients nor treating
doctors knew which patients were receiving the real pills.
Those receiving modafinil cut their use of methamphetamine from the average of
20 days at the start of the trial to eight days. Those in the placebo group only
cut their usage to an average of 14 days in the previous 28.
No serious side-effects were reported.
Researcher James Shearer, a PhD student at the centre, presented the results
yesterday at the World Psychiatric Association congress in Melbourne.
Mr Shearer said the drug was best thought of as similar to the anti-smoking drug
Zyban, which helps to kill the cravings and withdrawal symptoms while a smoker
is trying to quit.
It was believed to work by boosting the activity of the frontal cortex, which
helps users overcome the poor impulse control seen in ice addicts.
''You still need commitment to change a lot of things -- where you live, who you
hang around with -- and it's only a short-term thing,'' Mr Shearer said. ''What
we now need is national trials to conclude that the drug does work and should be
on the Pharmaceutical Benefits Scheme.''
LOAD-DATE: November 30, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: AUS
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273 of 998 DOCUMENTS
Weekend Australian
December 1, 2007 Saturday
All-round First Edition
Sleep drug 'helps addicts to give up ice'
BYLINE: Adam Cresswell
SECTION: LOCAL; Pg. 11
LENGTH: 251 words
USERS of methamphetamine could get a new treatment to help them quit the drug
after a world-first Australian study showed a medicine already on the shelves
helped addicts cut their use by more than 50 per cent.
The drug modafinil, used to treat sleep disorders, has been shown to help treat
cocaine addiction in the US. Now a federally funded Australian trial has shown
it could be a new treatment for methamphetamine addiction, by helping users
overcome their craving.
Experts welcomed the findings, saying doctors had few options to help people
hooked on methamphetamine, also known as ice. Researchers from the National Drug
and Alcohol Research Centre recruited 80 ice users trying to stop their habit
and divided them into two groups. All participants had used the drug on an
average of 20 days in the previous 28 days.
One group received a daily dose of modafinil, while the other received a dummy
pill. During the 10-week trial, neither patients nor doctors knew which patients
were receiving the real pills.
Those receiving modafinil cut their use of ice from the average of 20 days at
the start of the trial to eight days. Those in the placebo group only cut their
usage to an average of 14 days in the previous 28.
No serious side effects were reported.
Presenting the results at the World Psychiatric Association congress in
Melbourne yesterday, researcher James Shearer, a PhD student at the centre, said
the drug was like the anti-smoking drug Zyban, which helps kill cravings and
withdrawal symptoms.
LOAD-DATE: December 1, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: AUS
Copyright 2007 Nationwide News Pty Limited
All Rights Reserved
274 of 998 DOCUMENTS
AAP Newsfeed
November 30, 2007 Friday 12:22 PM AEST
Fed: Sleepiness drug helps ice addicts break their habit: study
BYLINE: Tamara McLean, Medical Writer
SECTION: DOMESTIC NEWS
LENGTH: 478 words
DATELINE: MELBOURNE Nov 30
A drug that keeps narcoleptics awake and another that controls hyperactive
kids have been found to help Australian ice addicts kick their dangerous habit,
studies show.
Fresh findings from two Australian drug trials have delivered new hope that
much-needed medications to treat crystal methamphetamine addiction are on the
horizon.
One world-first study by Sydney researchers found that the drug modafinil,
used to treat excessive sleepiness and fatigue, could help quash cravings in
the heaviest ice users.
Another medication, dexamphetamine, used widely to treat ADHD in Australian
children, was found by Adelaide scientists to help wean users off the
stimulant.
Currently, there is no medical treatment available for the 73,000
Australians addicted to methamphetamines, renowned for causing extreme violence
and psychosis. Treating physicians have been calling out for medications to
relieve the addiction.
The Sydney-based National Drug and Alcohol Research Centre (NDARC) presented
the latest findings from its modafinil study at the World Psychiatry
Association (WPA) conference in Melbourne, with researchers labelling the
effects "dramatic".
More than 80 dependent methamphetamine users took either modafinil or a
dummy medication daily for 10 weeks. Those who received modafinil cut their
methamphetamine use by more than half, significantly better than those who
received the placebo.
"It has a brilliant effect on a third, a slight effect on another third and
no effect at all on the last group," said researcher James Shearer, a PhD
student at NDARC.
"That's very significant, given we've never seen results like this with
ice."
The drug also appeared to be non-addictive and safe, with no serious side
effects.
It works by restoring the levels of neurotransmitters or chemicals in the
brain that may be depleted after heavy or long-term methamphetamine use, Mr
Shearer said.
Users withdrawing from ice can take modafinil instead, giving them a
non-amphetamine coffee-like high that still allows them to concentrate.
"Just getting up in the morning and trying to to do any of the normal things
in life without ice was near impossible for these people, but the modafinil is
really helping them," Mr Shearer said.
The team is currently seeking a larger clinic trial to verify their
findings.
Preliminary results from the dexamphetamine trial were also reported to the
congress today, with researcher Professor Jason White from the University of
Adelaide saying they looked promising.
Dexamphetamine, which works as a methadone-like drug substitute, led to a
decrease in methamphetamine use among 87 per cent of the addicts who took it.
This compared to 70 per cent of those on a placebo.
However, the studies were not definitive, and drug approval processes could
mean the treatment would not be available for several years.
LOAD-DATE: November 30, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 Australian Associated Press Pty. Ltd.
275 of 998 DOCUMENTS
Mental Health Update
November 27, 2007 Tuesday 5:51 AM EST
Modafinil for schizophrenia
BYLINE: John Gale
LENGTH: 234 words
Nov. 27, 2007 (Mental Health Update delivered by Newstex) -- Schizophrenia is
considered the most important cause of chronic psychiatric disability. In recent
years the cognitive and motivational impairment seen in schizophrenia have been
determined to be one of the main causes of the profound and persistent
disability typically produced by the disorder. Although the psychotic symptoms
of schizophrenia may improve following treatment a range of cognitive deficits
will often persist and the disability resulting from them has recently been
considered to have a greater impact on long-term functioning than delusions and
hallucinations. Recently a drug called modafinil has emerged as a possible drug
to improve cognition in schizophrenia. It was initially prescribed to reduce the
fatigue and sedation induced by antipsychotic medication but a review of studies
into the drug shows that it may lead to better executive functioning and
attention performance in patients with schizophrenia. The drugs effectiveness is
affected by the patients' current levels of cognitive functioning, genetic
make-up and the other drugs that they are taking at the time allowing for future
treatment to be targeted at those most likely to
Morein-Zamir, Sharon, Turner, Danielle C. and Sahakian, Barbara J. - A review of
the effects of modafinil on cognition in schizophrenia Schizophrenia Bulletin
November 2007, 33(6),
LOAD-DATE: November 27, 2007
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs via Newstex") are solely the author's and not
necessarily the views of Newstex or its re-distributors. Posts from such authors
are provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs via Newstex are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs via Newstex is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs via Newstex shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs via Newstex. Reader's comments reflect their
individual opinion and their publication within Blogs via Newstex shall not
infer or connote an endorsement by Newstex or its re-distributors of such
reader's comments or views. Newstex and its re-distributors expressly reserve
the right to delete posts and comments at its and their sole discretion.
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Newstex Web Blogs
Copyright 2007 Mental Health Update
276 of 998 DOCUMENTS
Targeted News Service
November 22, 2007 Thursday 2:03 PM EST
U.S. Patents Awarded to Inventors in Delaware (Nov. 22)
BYLINE: Targeted News service Targeted News Service
LENGTH: 207 words
DATELINE: Alexandria, VA.
ALEXANDRIA, Va., Nov. 22 -- The following federal patents were awarded to
inventors in Delaware.
***
Indiana, Ohio, Delaware Inventors Develop Modafinil Pharmaceutical Formulation
ALEXANDRIA, Va., Nov. 22 -- Vincent Corvari of Carmel, Ind., George Grandolfi of
Millford, Ohio, and Alpa Parikh of Hockessin, Del., have developed
pharmaceutical formulations of modafinil.
According to the U.S. Patent & Trademark Office: "The present invention is
related to compositions of modafinil, including compositions of modafinil and
one or more diluents, disintegrants, binders and lubricants, and the processes
for their preparation thereof."
The inventors were issued U.S. Patent No. 7,297,346 on Nov. 20.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on May 23, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,346.PN.&OS=PN/7,297,346&RS=
PN/7,297,346.
For more information about Targeted News Service's products, including its
federal contract report, please contact: Myron Struck, Myron@targetednews.com,
Editor, Targeted News Service LLC, Springfield, Va. (Managing Edi
-537400
LOAD-DATE: November 22, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 Targeted News Service LLC.
All Rights Reserved
277 of 998 DOCUMENTS
Targeted News Service
November 22, 2007 Thursday 2:03 PM EST
U.S. Patents Awarded to Inventors in Indiana (Nov. 22)
BYLINE: Targeted News service Targeted News Service
LENGTH: 486 words
DATELINE: Alexandria, VA.
ALEXANDRIA, Va., Nov. 22 -- The following federal patents were awarded to
inventors in Indiana.
***
New York, Minnesota, Indiana, Iowa Inventor Develops Protein Material Treatment
Method
ALEXANDRIA, Va., Nov. 22 -- Tim Emerson of Churchville, N.Y., Christopher S.
Penet of Henrietta, N.Y., Mary R. Higgins of Fridley, Minn., Madhu Kakade of
Roseville, Minn., Jane Kitchar of Elkhart, Ind., and Bill L. Miller of Fort
Dodge, Iowa, have developed a method of reducing the antigenicity of vegetable
proteins.
According to the U.S. Patent & Trademark Office, the invention relates to a
"method of treating a proteinaceous material having a first concentration of
beta-conglycinin, the method including combining the proteinaceous material with
an enzyme to form a reaction mixture, the reaction mixture initially having a
potential of Hydrogen (pH) of at least about 7.0 standard pH units, allowing the
enzyme to hydrolyze beta-conglycinin present in the reaction mixture to form a
proteinaceous intermediate, and inactivating the enzyme present in the reaction
mixture after a reaction period to form a proteinaceous product, the
proteinaceous product having a second concentration of beta-conglycinin, the
second concentration of beta-conglycinin being at least 99 percent less than the
first concentration of beta-conglycinin."
The inventors were issued U.S. Patent No. 7,297,354 on Nov. 20.
The patent has been assigned to Land O'Lakes Inc., Arden Hills, Minn.,
and Genencor International Inc., Palo Alto, Calif.
The original application was filed on April 26, 2001, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,354.PN.&OS=PN/7,297,354&RS=
PN/7,297,354.
***
Indiana, Ohio, Delaware Inventors Develop Modafinil Pharmaceutical Formulation
ALEXANDRIA, Va., Nov. 22 -- Vincent Corvari of Carmel, Ind., George Grandolfi of
Millford, Ohio, and Alpa Parikh of Hockessin, Del., have developed
pharmaceutical formulations of modafinil.
According to the U.S. Patent & Trademark Office: "The present invention is
related to compositions of modafinil, including compositions of modafinil and
one or more diluents, disintegrants, binders and lubricants, and the processes
for their preparation thereof."
The inventors were issued U.S. Patent No. 7,297,346 on Nov. 20.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on May 23, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,346.PN.&OS=PN/7,297,346&RS=
PN/7,297,346.
For more information about Targeted News Service's products, including its
federal contract report, please contact: Myron Struck, Myron@targetednews.com,
Editor, Targeted News Service LLC, Springfield, Va. (Managing Edi
-537407
LOAD-DATE: November 22, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 Targeted News Service LLC.
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278 of 998 DOCUMENTS
Targeted News Service
November 22, 2007 Thursday 2:03 PM EST
U.S. Patents Awarded to Inventors in Ohio (Nov. 22)
BYLINE: Targeted News service Targeted News Service
LENGTH: 1102 words
DATELINE: Alexandria, VA.
ALEXANDRIA, Va., Nov. 22 -- The following federal patents were awarded to
inventors in Ohio.
***
Ohio Inventor Develops Barrier Operator Controller
ALEXANDRIA, Va., Nov. 22 -- Michael T. McMahon of Salem, Ohio, has developed a
barrier operator controller.
According to the U.S. Patent & Trademark Office: "A control unit for a moveable
barrier, such as a garage door, includes a microcontroller connected to a motor
speed detector, motor current sensor or a sensor for determining forces exerted
on or by the barrier. A user interface includes user actuatable switches for
setting a first maximum force value to be exerted on or by the barrier when
moving in one direction and the microcontroller automatically sets the value of
a second maximum force to be exerted on or by the barrier when moving in the
opposite direction."
An abstract of the invention, released by the Patent Office, said: "The second
force value may be based on the force value set by the user or the second force
value may be a preset value. Both force limits may be automatically set as a
function of a maximum force exerted on said barrier during movement thereof,
during a force learning operation."
The inventor was issued U.S. Patent No. 7,298,107 on Nov. 20.
The patent has been assigned to Overhead Door Corp., Lewisville, Texas.
The original application was filed on Feb. 16, 2006, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,298,107.PN.&OS=PN/7,298,107&RS=
PN/7,298,107.
***
Michigan, California, Florida, Ohio Inventors Develop Model Toy Train Motor
Arrangement
ALEXANDRIA, Va., Nov. 22 -- Gary L. Moreau of Rochester, Mich., Martin Pierson
of Howell, Mich., Neil P. Young of Redwood City, Calif., Robert Grubba of Ormond
Beach, Fla., and Dennis J. Denen of Westerville, Ohio, have developed a model
toy train motor arrangement.
According to the U.S. Patent & Trademark Office: "A control and motor
arrangement in accordance with the present invention includes a motor configured
to generate a locomotive force for propelling the model train. The control and
motor arragement further includes a command control interface configured to
receive commands from a command control unit wherein the commands correspond to
a desired speed. The control and motor arrangement still further includes a
plurality of detectors configured to detect speed information of the motor, and
a process control arrangement configured to receive the speed information from
the sensors."
An abstract of the invention, released by the Patent Office, said: "The process
control arrangement is further configured and arranged to generate a plurality
of motor control signals based on the speed information for controlling the
speed of said motor. The control and motor arrangement yet still further
includes a motor control arrangement configured to cause power to be applied to
the motor at different times in response to the motor control signals."
The inventors were issued U.S. Patent No. 7,298,103 on Nov. 20.
The patent has been assigned to Lionel LLC, Chesterfield, Mich.
The original application was filed on May 8, 2006, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,298,103.PN.&OS=PN/7,298,103&RS=
PN/7,298,103.
***
Ohio Inventors Develop Dehydrated Starch Ingredients Making Process
ALEXANDRIA, Va., Nov. 22 -- David Cammiade Gruber and Paul Seiden, both of
Cincinnati, Peter Yau Tak Lin of Liberty, Ohio, and Maria Dolores Martinez-Serna
Villagran of Mason, Ohio, have developed dehydrated starch ingredients making
emulsifier system.
According to the U.S. Patent & Trademark Office: "Described is an improved
emulsifier system suitable for use in making dehydrated starch ingredients. Also
disclosed are a process for making the dehydrated ingredients using the improved
emulsifier systems, doughs made using the dehydrated ingredients and the process
for making those doughs, and food products containing the dehydrated
ingredients."
The inventors were issued U.S. Patent No. 7,297,358 on Nov. 20.
The patent has been assigned to The Procter & Gamble Co., Cincinnati.
The original application was filed on July 29, 2004, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,358.PN.&OS=PN/7,297,358&RS=
PN/7,297,358.
***
Indiana, Ohio, Delaware Inventors Develop Modafinil Pharmaceutical Formulation
ALEXANDRIA, Va., Nov. 22 -- Vincent Corvari of Carmel, Ind., George Grandolfi of
Millford, Ohio, and Alpa Parikh of Hockessin, Del., have developed
pharmaceutical formulations of modafinil.
According to the U.S. Patent & Trademark Office: "The present invention is
related to compositions of modafinil, including compositions of modafinil and
one or more diluents, disintegrants, binders and lubricants, and the processes
for their preparation thereof."
The inventors were issued U.S. Patent No. 7,297,346 on Nov. 20.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on May 23, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,346.PN.&OS=PN/7,297,346&RS=
PN/7,297,346.
***
Ohio Inventors Develop Boron Nitride Production Process
ALEXANDRIA, Va., Nov. 22 -- Laurence Maniccia of Lyndhurst, Ohio, and Donald
William Pultz Jr., of Parma, Ohio, have developed a hexagonal boron nitride
compound production process.
According to the U.S. Patent & Trademark Office, the invention relates to a
"process for producing boron nitride using a boron containing ore as a starting
material, by reacting naturally occurring ulexite with ammonia at high
temperature, for a boron nitride with high impurity and at a high yield."
The inventors were issued U.S. Patent No. 7,297,317 on Nov. 20.
The patent has been assigned to Momentive Performance Materials Inc., Wilton,
Conn.
The original application was filed on Nov. 3, 2005, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,317.PN.&OS=PN/7,297,317&RS=
PN/7,297,317.
For more information about Targeted News Service's products, including its
federal contract report, please contact: Myron Struck, Myron@targetednews.com,
Editor, Targeted News Service LLC, Springfield, Va. (Managing Edi
-537423
LOAD-DATE: November 22, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 Targeted News Service LLC.
All Rights Reserved
279 of 998 DOCUMENTS
US Fed News
November 22, 2007 Thursday 12:47 AM EST
Indiana, Ohio, Delaware Inventors Develop Modafinil Pharmaceutical Formulation
BYLINE: US Fed News
LENGTH: 170 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Nov. 22 -- Vincent Corvari of Carmel, Ind., George Grandolfi of
Millford, Ohio, and Alpa Parikh of Hockessin, Del., have developed
pharmaceutical formulations of modafinil.
According to the U.S. Patent & Trademark Office: "The present invention is
related to compositions of modafinil, including compositions of modafinil and
one or more diluents, disintegrants, binders and lubricants, and the processes
for their preparation thereof."
The inventors were issued U.S. Patent No. 7,297,346 on Nov. 20.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on May 23, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,297,346.PN.&OS=PN/7,297,346&RS=
PN/7,297,346.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
LOAD-DATE: November 22, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
280 of 998 DOCUMENTS
The Guardian (London) - Final Edition
November 8, 2007 Thursday
G2: Ways to make you think better: Students and exhausted workers have been
abusing stimulants for decades. But these days, if you're keen to feel sharper,
and work for longer, the drugs available are more effective than they once were
- and less likely to make you feel awful afterwards. No wonder then that the
abuse of pills such as Ritalin and modafinil is becoming a major problem.
Katharine Hibbert reports on the rise of cognitive-enhancing drugs - and
doctors' fears over their long-term safety
BYLINE: Katharine Hibbert
SECTION: GUARDIAN FEATURES PAGES; Pg. 7
LENGTH: 2095 words
Mark is a good student. Intelligent and diligent, he won a place to read modern
languages at one of Britain's top 10 universities. But in the run-up to his
finals this summer, with a towering pile of revision still to go, the
23-year-old decided he wasn't going to be good enough. So he went on the
internet, found an online pharmacy based in Turkey, and bought a pack of
modafinil. It's a prescription drug given to narcoleptics, but it has also been
shown to boost alertness and mental agility in healthy users. After a week of
taking a tablet a day, sleeping only four hours a night, then, thanks to the
drug, waking up refreshed, Mark took his exams. He got a first. Would he have
done so well without pharmaceutical help? "Unlikely," he says.
Mark is not the only one. The British Medical Association believes that a
growing number of healthy people in this country are illicitly using
brain-boosting drugs that should really only be taken on prescription. More
specifically, they're taking modafinil and Ritalin, a drug licensed for use in
those suffering from attention deficit hyperactivity disorder (ADHD). Some
people may find a way to obtain the drugs from a doctor, but if not, they are
available from websites based abroad. The going rate for a dose is around £3.
Although the scale of the problem is as yet undefined in this country, there is
evidence that self-dosing with brain-boosting drugs is already rife in the
United States. There's thought to be a particular problem among students (some
of whom have nicknamed Ritalin "Vitamin R"): in a survey of 1,025 students at a
north-eastern US university, published in the Journal of American College Health
last year, one in six of those who responded admitted taking prescription drugs
illicitly, mainly to improve concentration and alertness. But even beyond the
world of student panic, abuse of Ritalin (also known as "kiddie coke") is
widespread. Meanwhile many millions of people who have problems with tiredness -
truckers, for example, and night workers - are using modafinil. It's even been
found in the systems of top American athletes during dope testing.
The BMA is so concerned about the use of such drugs on this side of the Atlantic
that its medical ethics committee is today publishing a discussion paper on the
ethics of cognitive-enhancement. The paper predicts that increasing use of
Ritalin and modafinil in Britain is "both imminent and inevitable". One of the
experts who pro duced the report, Barbara Sahakian, professor of neuropsychology
at Cambridge University, knows at first-hand how widely used the drugs already
are. "I have been offered modafinil on several occasions when I've been at
conferences, without asking for it," she says.
"My fellow academics have taken it to counteract jetlag and tiredness, and I've
been offered it when I've complained about my own jet lag, or having been
allocated a slot to talk late in the day. I haven't taken it - I work in the lab
where we have many of these substances, so it would be unethical for me to be
taking things off the shelves. But the use of these drugs is clearly quite
widespread within the profession."
Such anecdotal evidence isn't hard to uncover; these are the sort of drugs that
students talk about nowadays. Anna, 24, now a junior doctor, says that her use
of prescription drugs to boost her ability to work was unexceptional while she
was studying medicine at a Scottish university. "We'd have these revision
parties. It was usually about three of us, we'd get wired on Ritalin, and I'd do
my anatomy revision, another would work on her economics coursework, and the
other would do a history of art essay. We'd sit there working like mad, really
racing through it, totally focused, turning out good quality work for hours and
hours.
"I ended up taking Ritalin in every exam during the first semester at medical
school - I was just so snowed under that I couldn't cope with the work
otherwise, and I was positive I was going to fail. I remember in the exam that I
was pulling in knowledge from when I was at school. It all seemed to come into
my head much better than it would normally - it might just have been
psychosomatic, but it felt like it helped. And I passed every exam."
Dosing up on stimulants to improve focus and ward off tiredness is nothing new.
Caffeine, amphetamines and other, harder drugs have long been used by people
seeking ways to make their brains work better, for longer. The difference with
modern drugs such as Ritalin - which is actually an amphetamine, but far more
subtle than old-fashioned "speed" - is that they have been developed to minimise
both unpleasant side-effects and the risk of addiction.
Ritalin, the trade name in the UK for the drug methylphenidate, was invented in
1954 and first prescribed to ADHD sufferers in the 1960s, but its use rocketed
during the 90s. In the US, doctors write 3m prescriptions for the drug every
month; here doctors average more than 30,000 a month. Although Ritalin is
medically a stimulant, it calms those who suffer from ADHD, making them more
able to concentrate on the task in hand, and has similar effects on healthy
users (although it can also cause insomnia, headaches and heart palpitations.)
The fact that it's currently so widely prescribed to even very young children
makes many adults think that it must be perfectly safe to take.
Modafinil, meanwhile, has been prescribed in the UK since 1997, and has similar
effects, but it also works to stave off tiredness without the slight euphoric
high and cardiovascular effects brought on by Ritalin, which can be dangerous
for those with weak hearts. Neither drug is considered addictive at the doses
normally prescribed - although it is possible to develop a psychological
dependence.
Sahakian and a team of researchers at Cambridge tested modafinil on healthy male
undergraduates in 2003. Those who took a single 200mg dose were found to use
information more efficiently within two hours of taking it. They were better at
mental planning tests, completed puzzles more accurately, could remember longer
strings of digits and recognise pictures more quickly. Long-term memory was not
enhanced, but the increased ability to concentrate for longer periods of time
would, the researchers say, allow them to learn more. Modafinil has also been
tested by both the British and American armed forces, and could one day offer a
substitute for the caffeine and amphetamine "go pills" the US army and air force
have long relied on for night-time operations.
But the new BMA paper emphasises that the long-term side-effects of using such
drugs are unknown: they may turn out to be harmful. Such risks may be worthwhile
for those suffering from the conditions the drugs were created to treat, but
perhaps not for a healthy user. The report highlights speculation among
academics that there could be particular dangers for children and younger people
who take the drugs while their brains are developing, and that people who use
cognitive-enhancing pharmaceuticals in their youth may become more susceptible
to premature cognitive decline as they age. "We simply do not know what the
long-term effect of the use of such drugs in healthy populations will be," the
report concludes. Whether or not the drugs should be so widely prescribed,
especially to primary school children, is a matter of some controversy. But it
seems clear that healthy young adults are taking a gamble when they dabble with
them.
This may not be enough to put everyone off. Modafinil's apparent harmlessness
persuaded John, who is studying for a neuroscience PhD in London, to try it.
"When I was thinking about taking modafinil, I read the scientific studies," the
29-year-old says. "I've never even taken cannabis, let alone any harder drugs,
but I thought modafinil might benefit me. Sometimes I find it hard to
concentrate, some days I'm just tired out and I need to work. A friend who's a
doctor wrote me a prescription - he uses it occasionally himself. I've also
bought it off the internet. For me, it's something to have in the medicine
cupboard in case you're totally exhausted and just need to get through the day.
I only use it maybe once or twice a month - it's just a nice backup. It doesn't
feel like much, it just stops you from feeling sleepy, takes away that
mid-afternoon drop-off . You certainly wouldn't take it for enjoyment, for its
own sake. I don't notice any side-effects - sometimes my mouth goes a bit dry,
but that's all."
The idea of competing with pharmaceutically enhanced peers at work or university
will strike many as deeply unfair. "It may not be a fair thing that I took
modafinil," Mark says, "but so many students have Ritalin and other drugs, some
who have been prescribed it for more or less spurious reasons, or others who can
just get hold of it one way or another. Loads of students I knew were using it
to stay up and write essays. And at that particular time, this particular drug
seemed quite helpful to me, so I didn't feel too bad about taking it."
And the playing field isn't exactly level anyway, since many students will be
legitimately prescribed drugs by doctors even if their peers might not consider
them ill. "Prescribing Ritalin for ADHD brings a grey area," Sahakian says.
"It's a spectrum disorder, and while at one end it can be deeply debilitating,
many people are diagnosed for much more minor symptoms. Studies in America have
shown a huge variation in diagnosis rates - in some areas up to one in five
children have it prescribed to them. The line between enhancement and treatment
is a subjective decision, and if students have found someone who will prescribe
where other doctors might not, then they are already going into exams on drugs,
where other students, with similar symptoms, are not. The pressure to compete is
already boosting prescribed use of these drugs - we hear about parents putting
pressure on doctors to prescribe Ritalin because they think that everyone else's
children are taking it.
"And maybe people who have the money will be able to afford cognitive-enhancing
drugs that aren't prescribed - so people who are already limited in finances and
background will be even more disadvantaged. But then that's already the case, as
they can afford better education, better food, more extra-curricular lessons."
Trevor Robbins, professor of neuroscience at Cambridge University, who has
carried out extensive research on drugs for cognitive enhancement and on drug
abuse, is surprisingly sanguine about the use of these drugs by healthy adults.
"We already enhance our performance in all sorts of ways," he says. "Some of us
wear contact lenses, some of us drink coffee. Some may be horrified that normal
people would take drugs to improve their performance, but if you called it a
food or a drink, they wouldn't bat an eyelid - people take fish oil because it
may make their brains work better, but drugs have a stigma to them.
"I don't really see any argument against self-improvement in itself, except in a
competitive situation - in exams, for example. Then it's analogous with doping
in competitive sport. But what can you do? Even if you do drug tests in the exam
hall, people might have used modafinil to improve their learning on a course in
November, for instance, then taken the exam in July. How are you going to test
it by then?"
Both Robbins and Sahakian believe that the use of the drugs is set to grow, no
matter what regulation is put in place. The BMA report concurs, acknowledging
that even if the drugs were banned in Britain, it would take international laws
to prevent them from being sold over the internet. And right now there are more
mind-sharpening medicines in development, and those who want to enhance their
mental performance may soon be able to choose, legally or illegally, from a
wider range of drugs, each operating on different parts of the brain. The
Alzheimer's drug Donepezil, for example, has been shown to delay loss of mental
ability in patients, and improve memory in those without dementia. Early
clinical trials, meanwhile, suggest that a new and so far unlicensed class of
drugs, ampakines, may enhance learning capacity and memory in healthy users, as
well as increasing attention span and alertness.
Drugs may not negate the need for talent, creativity and self-discipline in
achieving success. But even if the ethics and the uncertainties about long-term
risks are hard to swallow, more and more people may soon find themselves tempted
by the chance to be sharper, smarter and more alert if it's on offer in tablet
form.
LOAD-DATE: November 8, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 Guardian Newspapers Limited
All Rights Reserved
281 of 998 DOCUMENTS
Clinical Neurology News
November 2007
SJS, Rash Warnings Added to Modafinil Label
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 4 Vol. 3 No. 11 ISSN: 1553-3212
LENGTH: 652 words
Adverse reactions should be reported to the FDA's MedWatch program at
800-332-1088 or www.fda.gov/medwatch. More information is available at
www.fda.gov/medwatch/safety/2007/safety07.htm#Provigil.
Warnings about Stevens-Johnson syndrome, hypersensitivity reactions, and
psychiatric symptoms have been added to the label of modafinil, according to a
MedWatch notice issued by the Food and Drug Administration on Oct. 24.
Modafinil, a "wakefulness-promoting agent," is marketed as Provigil by
Cephalon Inc., and was first approved as a treatment for narcolepsy in 1998. It
is approved for improving wakefulness in adults with excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome, and
shift-work sleep disorder. It is not approved for any pediatric indications,
though some reports have been in children.
The MedWatch notice and a "Dear Healthcare Professional" letter issued by
Cephalon describe worldwide postmarketing reports of life-threatening rash,
including toxic epidermal necrolysis (TEN), and drug rash with eosinophilia and
systemic symptoms (DRESS) in adults and children. There have also been
postmarketing reports of angioedema and multiorgan hypersensitivity reactions.
The reporting rate-considered an underestimate, because postmarketing reports
of adverse events tend to be underreported-of TEN and Stevens-Johnson syndrome
(SJS) associated with modafinil is higher than the background incidence rate,
according to the letter. The background in the general population is estimated
at 1-2 million cases per million person-years.
The potential for benign rashes-which have been associated with modafinil
use-to develop into serious rashes cannot be reliably predicted, so "modafinil
should ordinarily be discontinued at the first sign of rash, unless the rash is
clearly not drug-related," the letter says. However, stopping treatment "may not
prevent a rash from becoming life-threatening or permanently disabling or
disfiguring."
Because of postmarketing reports of angioedema, the letter says that patients
should be advised to stop treatment and "immediately report to their physician
any signs of symptoms suggesting angioedema or anaphylaxis," which includes
swelling of the face, eyes, lips, tongue, or larynx; difficult breathing or
swallowing; and hoarseness. There have also been postmarketing reports of
multiorgan hypersensitivity reactions, including at least one fatal case, which
have occurred "in close temporal association to the initiation of modafinil."
Modafinil should be discontinued if such a rash is suspected.
The letter also recommends that discontinuation of the drug should be
considered in patients who develop psychiatric symptoms during treatment,
because mania, anxiety, hallucinations, and suicidal ideation are among the
psychiatric adverse reactions reported in people treated with modafinil. In
addition, "caution should be exercised" when the drug is prescribed to patients
with as history of psychosis, depression, or mania.
Cephalon had pursued approval of modafinil as a treatment for
attention-deficit/hyperactivity disorder in children and adolescents, but in
March 2006, the FDA's Psychopharmacologic Drugs Advisory Panel agreed that the
drug was not safe for treating children and adolescents, largely because of
concerns about its potential to cause SJS in this population. Last summer,
Cephalon announced that it had received a "non-approvable" letter from the FDA
for this indication and had stopped developing the drug.
The "Dear Healthcare Professional" letter says in studies, the incidence of
rash resulting in discontinuation of the drug in pediatric patients (younger
than 17 years) was 0.8% (13 of 1,585); these included one case of possible SJS
and one case of a possible multiorgan hypersensitivity reaction. There were no
such cases among 380 pediatric patients on placebo.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CNNEWS
Copyright 2007 Elsevier Inc., International Medical News Group
All Rights Reserved
282 of 998 DOCUMENTS
The International Herald Tribune
October 18, 2007 Thursday
Rider nears victory in bid to stay awake;
CYCLING
BYLINE: Samuel Abt - The New York Times Media Group
SECTION: SPORT; Pg. 19
LENGTH: 602 words
DATELINE: PARIS
Franck Bouyer sounds raring to go, up and at 'em, as bright-eyed and
bushy-tailed as a fellow with sleeping sickness can be.
After three years of legal struggle to regain his place as a bicycle racer,
Bouyer says the happy ending is finally in sight. He has succeeded, he feels, in
sending the overlords of the sport a wake-up call.
''Yes,'' he said in a phone interview from his home near Cholet in western
France, ''things are looking good. I'm trying not to get too excited about my
chances since I've had so many setbacks before, but this time it really looks
good.
''This time, if all goes well, they'll have to do the right thing by me.''
Unless, that is, somebody is asleep at the switch. Often, that has been Bouyer.
The 33-year-old Frenchman has narcolepsy, a disorder marked by recurring and
unpredictable episodes of sleep during normal waking hours and disturbed sleep
at night. He was diagnosed with the genetic disease, which is believed to
afflict one person in 200,000, late in 2003 and since then his life has been, as
he says without irony, a nightmare.
It's not just that he tosses and turns while trying to grab some shut-eye. When
the sun is up, he sometimes dozes off on training rides and finds himself
suddenly on the ground.
''One time, I found myself in the courtyard of a farm, woken up by a barking dog
without knowing how I got there,'' he has said. This has not happened in a race,
where the result could be a mass crash.
Bouyer can master his disorder by taking a drug called modafinil. But, in
addition to keeping him awake and alert, modafinil is classified by the
International Cycling Union, which governs the sport, as an illegal
performance-enhancing drug.
The World Anti-Doping Agency disagrees in Bouyer's case and ruled in 2005 that
he could take the drug while competing. That decision, a reversal of the
agency's ruling the same year, followed one of many lawsuits.
For a brief period late in 2005 and early last year, Bouyer returned to racing
for the Bouygues T[#x17d]l[#x17d]com team from France.
Then the cycling union appealed the World Anti-Doping Agency's decision to the
Court of Arbitration for Sport, and Bouyer lost.
''I have a sickness, you know,'' Bouyer explained last year. ''I'm not trying to
cheat, I'm trying to compete.''
This year, he turned to a French court to obtain what is called a Therapeutic
Use Exemption for modafinil. Last month, the court upheld him.
''Finally somebody agrees with me and considers me ill,'' he told the sports
newspaper L'[#x192]quipe. On the phone last week, he elaborated: ''The case goes
now to a doctor named by the court. He's an expert. If he says I have a right to
use modafinil, I should be racing next year.
''I'm so hopeful that I've already resumed training. Whew, it's hard. Such a
long time since I've been in a race or even training. There wasn't much point in
training while I was going from one courtroom to another.
''Now I think all this may finally be over. Time to start getting my legs
ready.''
The Bouygues team, which has supported him throughout the legal process, has
said that it will welcome him back. Although Bouyer has never been a star, he
has won such races as Paris-Camembert, the Tour of the Vend[#x17d]e and the Tour
of the Limousin since he turned professional in 1994.
''I understand that I don't have too many years left as a racer,'' he said.
''But that's how I'd like to finish my career, as a racer, not a spectator.
''Once again, I'm waiting for a ruling. So many doctors, so many courts.
''This time, maybe somebody will say, 'He's sick. He needs his medicine. There's
nothing wrong with that. Sick people have rights too.' ''
LOAD-DATE: October 31, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 International Herald Tribune
All Rights Reserved
283 of 998 DOCUMENTS
Pharma Company Insight
Pharmaceuticals
September 21, 2007
Cephalon completes Provigil label updates
LENGTH: 177 words
Cephalon has finalised and shared with healthcare professionals revisions to the
label for Provigil ( modafinil ) Tablets [C-IV], its wake-promoting agent. As
announced by the company in both March and June, these changes were necessary to
make the Provigil label consistent with the Nuvigil ( armodafinil ) Tablets
[C-IV] label that was approved and made available by the FDA in June. Nuvigil is
the single isomer formulation of modafinil, the active ingredient contained in
Provigil. Provigil and Nuvigil are indicated to improve wakefulness in adults
with excessive sleepiness associated with obstructive sleep apnoea/hypopnoea
syndrome (OSAHS), shift work sleep disorder and narcolepsy. In OSAHS, Provigil
and Nuvigil are indicated as adjuncts to standard treatments for the underlying
obstruction. Cephalon's ongoing development programme is evaluating the use of
Nuvigil as a treatment for serious psychiatric and neurological medical
conditions. Currently, the company plans a commercial launch of the product once
additional clinical data have been amassed.
LOAD-DATE: September 21, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2007 ESPICOM Business Intelligence Ltd.
All Rights Reserved
284 of 998 DOCUMENTS
Daily International Pharma Alert
September 18, 2007 Tuesday
Cephalon Completes Provigil Label Updates
SECTION: Vol. 4 No. 183
LENGTH: 114 words
Cephalon has finalized revisions to the label for Provigil tablets, its product
to improve wakefulness in adults with obstructive sleep apnea/hypopnea syndrome,
shift work sleep disorder and narcolepsy.
Cephalon said these changes were necessary to make the Provigil (modafinil)
label consistent with the Nuvigil (armodafinil) label approved by the FDA in
June. Nuvigil is the single isomer formulation of modafinil.
Cephalon's ongoing development program is evaluating Nuvigil as a treatment for
serious psychiatric and neurological medical conditions. The company said it
plans a commercial launch of Nuvigil once additional clinical data has been
amassed.
Release date: Sept. 18, 2007
LOAD-DATE: September 19, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2007 Washington Business Information, Inc.
All Rights Reserved
285 of 998 DOCUMENTS
Reuters Health Medical News
August 23, 2007 Thursday 9:00 PM EST
Modafinil seen beneficial in bipolar disorder
SECTION: DRUG & DEVICE DEVELOPMENT
LENGTH: 497 words
DATELINE: NEW YORK
Modafinil improves depressive symptoms in patients with bipolar disorder that
responds inadequately to a mood stabilizer, according to a report in the August
issue of the American Journal of Psychiatry.
Modafinil is currently approved in the U.S. for improving wakefulness in
patients with excessive sleepiness associated with narcolepsy, obstructive sleep
apnea or hypopnea syndrome, and shift-work sleep disorder, the authors explain,
but it may also be effective for attention deficit hyperactivity disorder
(ADHD), cocaine dependence, and unipolar depression.
Dr. Mark A. Frye from the Mayo Clinic, Rochester, Minnesota and associates
investigated the efficacy and safety of adjunctive modafinil versus placebo for
6 weeks in the treatment of 85 patients with bipolar depression. They had had
an inadequate response on a mood stabilizer with or without concomitant
antidepressant therapy
The endpoint scores on the Inventory of Depressive Symptoms (IDS), four-item
fatigue-and-energy subset of the IDS, and Clinical Global Impression-Bipolar
Disorder depression severity item were significantly improved in the modafinil
group compared with the placebo group, the investigators found.
Concomitant antidepressant therapy did not contribute to the difference between
groups in these scores, the report indicates.
Significantly more patients in the modafinil group (43.9%) than in the placebo
group (22.7%) achieved at least a 50% improvement in their IDS score, and
similar differential response rates were seen for the other two measures.
These improvements were evident at every visit from week 2 through week 6,
except for week 3, the investigators say.
"Although an antidepressant effect was observed for modafinil," the researchers
note, "no reduction in sleepiness, as measured by the Epworth Sleepiness Scale,
or in fatigue, as measured by the Fatigue Severity Scale, was observed."
There were no differences between the groups in treatment-emergent hypomania or
mania or in hospitalizations for mania.
"Our results in this 6-week trial suggest that adjunctive modafinil at doses of
100-200 mg a day may improve symptoms of bipolar depression without mood
destabilization," the authors conclude. "It will be important in our 4-month
open-trial continuation phase of this study to assess ongoing antidepressant
response and stability."
"It is biologically plausible that modafinil might be useful in some cases of
bipolar depression, and the present results in 85 patients support this
possibility," writes Dr. R. H. Belmaker from Ben-Gurion University of the Negev,
Beer-Sheba, Israel in a related editorial.
"We should avoid assuming that a statistical benefit of one treatment for
bipolar depression as a diagnostic entity is relevant for every patient with
this heterogeneous condition," cautions Dr. Belmaker. "The patients in the
present study were all taking mood stabilizers. Starting a mood stabilizer would
be the first choice for any patient not being so treated."
LOAD-DATE: March 4, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 Reuters Health
All Rights Reserved
286 of 998 DOCUMENTS
Straight From the Doc
August 8, 2007 Wednesday 12:30 AM EST
Wake-up Pill Modafinil May Help Bipolar Disorder Patients
LENGTH: 220 words
Aug. 8, 2007 (Straight From the Doc delivered by Newstex) -- Modafinil is a drug
approved by the US FDA for the treatment of patients suffering from excessive
sleepiness associated with narcolepsy, obstructive sleep apnea and shift work
sleep
>
Now, this "wake-up pill" has been found to control the depressive symptoms
associated with bipolar disorder - a condition characterized by an alternating
pattern of emotional highs (mania) and lows (depression),which (according to the
National Institute of Mental Health) is suffered by some 5.7 million adults in
the United
>
Appearing in the August 2007 issue of the American Journal of Psychiatry,
according to the study's author, Mark Frye, M.D., director of the Mayo Clinic
Mood Disorders Clinic and Research
>
At least 44 percent of the participants in the study reported improved symptoms,
a noteworthy improvement for a disorder in which new treatments are
>
There are very few treatments for the depressive phase of bipolar disorder and
as a result there is an urgent need to evaluate potential
>
Mood stabilizers in general are better at treating mania than depression, but
the depressive phase of the illness is far more common. We really need continued
research in this
>
Modafinil is manufactured by Cephalon Inc. and is sold under the brand name
Provigil.>
>
Mayo Clinic>
LOAD-DATE: August 8, 2007
LANGUAGE: ENGLISH
NOTES: The views expressed on blogs distributed by Newstex and its
re-distributors ("Blogs via Newstex") are solely the author's and not
necessarily the views of Newstex or its re-distributors. Posts from such authors
are provided "AS IS", with no warranties, and confer no rights. The material and
information provided in Blogs via Newstex are for general information only and
should not, in any respect, be relied on as professional advice. No content on
such Blogs via Newstex is "read and approved" before it is posted. Accordingly,
neither Newstex nor its re-distributors make any claims, promises or guarantees
about the accuracy, completeness, or adequacy of the information contained
therein or linked to from such blogs, nor take responsibility for any aspect of
such blog content. All content on Blogs via Newstex shall be construed as
author-based content and commentary. Accordingly, no warranties or other
guarantees will be offered as to the quality of the opinions, commentary or
anything else offered on such Blogs via Newstex. Reader's comments reflect their
individual opinion and their publication within Blogs via Newstex shall not
infer or connote an endorsement by Newstex or its re-distributors of such
reader's comments or views. Newstex and its re-distributors expressly reserve
the right to delete posts and comments at its and their sole discretion.
PUBLICATION-TYPE: Web Blog
Copyright 2007 Newstex LLC
All Rights Reserved
Newstex Web Blogs
Copyright 2007 Straight From the Doc
287 of 998 DOCUMENTS
Food and Drug Adminstration Documents and Publications
August 7, 2007
Summaries of Medical and Clinical Pharmacology Reviews of Pediatric Studies;
Availability
SECTION: FOOD AND DRUG ADMINISTRATION - REGULATORY DOCUMENTS
LENGTH: 581 words
SUMMARY: The Food and Drug Administration (FDA) is announcing the availability
of summaries of medical and clinical pharmacology reviews of pediatric studies
submitted in supplements for ACTIQ (fentanyl), ALDARA (imiquimod), AMBIEN
(zolpidem), COREG (carvedilol), PROVIGIL (modafinil), and ZYPREXA (olanzapine).
These summaries are being made available consistent with the Best
Pharmaceuticals for Children Act (the BPCA). For all pediatric supplements
submitted under the BPCA, the BPCA requires FDA to make available to the public
a summary of the medical and clinical pharmacology reviews of the pediatric
studies conducted for the supplement.
ADDRESSES: Submit written requests for single copies of the summaries to the
Division of Drug Information (HFD-240), Center for Drug Evaluation and Research,
Food and Drug Administration, 5600 Fishers Lane, Rockville, MD 20857. Please
specify by product name which summary or summaries you are requesting. Send one
self-addressed adhesive label to assist that office in processing your requests.
See the SUPPLEMENTARY INFORMATION section for electronic access to the
summaries.
FOR FURTHER INFORMATION CONTACT: Grace Carmouze, Center for Drug Evaluation and
Research, Food and Drug Administration, 10903 New Hampshire Ave., Bldg. 22, Rm.
6460, Silver Spring, MD 20993-0002, 301-796-0700, e-mail:
grace.carmouze@fda.hhs.gov
SUPPLEMENTARY INFORMATION: FDA is announcing the availability of summaries of
medical and clinical pharmacology reviews of pediatric studies conducted for
ACTIQ (fentanyl), ALDARA (imiquimod), AMBIEN (zolpidem), COREG (carvedilol),
PROVIGIL (modafinil), and ZYPREXA (olanzapine). The summaries are being made
available consistent with section 9 of the BPCA (Public Law 107-109). Enacted on
January 4, 2002, the BPCA reauthorizes, with certain important changes, the
pediatric exclusivity program described in section 505A of the Federal Food,
Drug, and Cosmetic Act (the act) (21 U.S.C. 355a). Section 505A of the act
permits certain applications to obtain 6 months of marketing exclusivity if, in
accordance with the requirements of the statute, the sponsor submits requested
information relating to the use of the drug in the pediatric population.
One of the provisions the BPCA added to the pediatric exclusivity program
pertains to the dissemination of pediatric information. Specifically, for all
pediatric supplements submitted under the BPCA, the BPCA requires FDA to make
available to the public a summary of the medical and clinical pharmacology
reviews of pediatric studies conducted for the supplement (21 U.S.C.
355a(m)(1)). The summaries are to be made available not later than 180 days
after the report on the pediatric study is submitted to FDA (21 U.S.C.
355a(m)(1)). Consistent with this provision of the BPCA, FDA has posted on the
Internet at http://www.fda.gov/cder/pediatric/index.htm summaries of medical and
clinical pharmacology reviews of pediatric studies submitted in supplements for
ACTIQ (fentanyl), ALDARA (imiquimod), AMBIEN (zolpidem), COREG (carvedilol),
PROVIGIL (modafinil), and ZYPREXA (olanzapine). Copies are also available by
mail (see ADDRESSES).
II. Electronic Access
Persons with access to the Internet may obtain the document at
http://www.fda.gov/cder/pediatric/index.htm.
Dated: July 30, 2007.
Randall W. Lutter,
Deputy Commissioner for Policy.
[FR Doc. E7-15234 Filed 8-6-07; 8:45 am]
BILLING CODE 4160-01-S
Notice.
Citation: "72 FR 44161"
Federal Register Page Number: "44161"
"Notices"
LOAD-DATE: August 7, 2007
LANGUAGE: ENGLISH
Copyright 2007 Federal Information and News Dispatch, Inc.
288 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
August 3, 2007
Modafinil shows potential for BPD
LENGTH: 247 words
A preliminary study of 85 patients with bipolar disorder (BPD) has indicated
that modafinil , a drug used to treat patients with sleep disorders, might also
control the depressive symptoms associated with BPD. Modafinil is approved by
the FDA to treat patients who suffer from excessive sleepiness associated with
narcolepsy, obstructive sleep apnoea and shift work sleep disorder, and is
marketed as Provigil by Cephalon . During the depressive phase of BPD, the
symptoms include excessive sleepiness and fatigue, therefore researchers
wondered if modafinil could address these symptoms in patients with this
disorder.
Half of the patients in the randomised, double-blind, placebo-controlled study,
which was conducted at five sites and published in the August issue of the
American Journal of Psychiatry (2007;164:1242-1249), were given modafinil
100-200mg/day, while the other half were given placebo over a six-week period.
While the trial was small, 44 per cent of those receiving modafinil reported
feeling better, while 39 per cent said their symptoms were in remission after
six weeks. This compares to 23 and 18 per cent, respectively, in the control
group. Modafinil was not associated with any greater risk of the manic and
depressive mood swings associated with BPD. How exactly modafinil works to
promote wakefulness or improve mood in BPD is not completely understood. Indeed,
it appears to have an entirely different mechanism of action compared to other
psychostimulants.
LOAD-DATE: August 3, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2007 ESPICOM Business Intelligence Ltd.
All Rights Reserved
289 of 998 DOCUMENTS
M2 EquityBites
July 23, 2007
Caraco Pharmaceutical Laboratories Ltd receives tentative FDA approval for
Generic Provigil
LENGTH: 150 words
M2 EQUITYBITES-23 July 2007-Caraco Pharmaceutical Laboratories Ltd receives
tentative FDA approval for Generic Provigil ©2007 M2 COMMUNICATIONS LTD
http://www.m2.com
Caraco Pharmaceutical Laboratories Ltd (Amex: CPD), which develops,
manufactures, markets and distributes generic and private-label pharmaceuticals,
reported on 20 July that the company has received tentative approval for its
Abbreviated New Drug Application (ANDA) for Modafinil Tablets (modafinil), 100mg
and 200mg from the US Food and Drug Administration (FDA).
Modafinil is indicated to improve wakefulness in patients with excessive
sleepiness associated with narcolepsy. The new product is the bioequivalent to
Provigil, a registered trademark of Cephalon Inc.
Provigil tablets had US sales of approximately USD753m for the 12-month period
ended 31 March 2007, according to IMS Data.
(Comments on this story may be sent to admin@m2.com)
LOAD-DATE: July 23, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 M2 Communications Ltd
All rights reserved
290 of 998 DOCUMENTS
Knobias.com
This content is provided to LexisNexis by Comtex News Network, Inc.
July 20, 2007 Friday 2:37 PM EST
CPD: FDA Grants Tentative Approval for Generic Provigil(R)
LENGTH: 373 words
DATELINE: Ridgeland, MS
By Fain Hughes, fhughes@knobias.com
Caraco Pharmaceutical Laboratories, Ltd. (CPD) announced that the FDA has
granted tentative approval for the Company's Abbreviated New Drug Application
(ANDA) for Modafinil Tablets (modafinil), 100mg and 200mg.
Modafinil is indicated to improve wakefulness in patients with excessive
sleepiness associated with narcolepsy. This new product is the bioequivalent to
Provigil(R), a registered trademark of Cephalon, Inc. (CEPH). Provigil(R)
tablets had U.S. sales of approximately $753 million for the 12-month period
ended March 31, 2007, according to IMS Data.
KNOBIAS DISCLAIMER: All statements made in this article were made by the Company
and do not in any way reflect the opinions of Knobias. Knobias is not a
registered broker-dealer, nor investment advisor, and does not endorse or
recommend any securities mentioned. This story is provided for informational
purposes only and is not intended for trading purposes. Knobias shall not be
liable for any actions taken in reliance of any information provided herein.
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without prior written consent of Knobias.com, LLC.
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As of Monday, 07-16-2007 23:59, the latest Comtex SmarTrend® Alert, an automated
pattern recognition system, indicated a DOWNTREND on 05-19-2006 for CPD @
$11.48. For more information on SmarTrend, contact your market data provider or
go to www.mysmartrend.com SmarTrend is a registered trademark of Comtex News
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reserved.
LOAD-DATE: July 21, 2007
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This content is provided to LexisNexis by Comtex News Network, Inc.
July 20, 2007 Friday 2:35 PM EST
CPD, CEPH: Hot Stocks
LENGTH: 166 words
14:34 EDT Caraco Pharm-CPD announces tenative approval for generic Provigil -
Caraco announced that the FDA has granted tentative approval for the company's
Abbreviated New Drug Application (ANDA) for Modafinil Tablets, 100mg and 200mg.
Modafinil is indicated to improve wakefulness in patients with excessive
sleepiness associated with narcolepsy. This new product is the bioequivalent to
Provigil, a registered trademark of Cephalon (CEPH).
As of Monday, 07-16-2007 23:59, the latest Comtex SmarTrend® Alert, an automated
pattern recognition system, indicated an UPTREND on 07-12-2007 for CEPH @
$82.86. As of Monday, 07-16-2007 23:59, the latest Comtex SmarTrend Alert, an
automated pattern recognition system, indicated a DOWNTREND on 05-19-2006 for
CPD @ $11.48. For more information on SmarTrend, contact your market data
provider or go to www.mysmartrend.com SmarTrend is a registered trademark of
Comtex News Network, Inc. Copyright © 2004-2007 Comtex News Network, Inc. All
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UPI
July 20, 2007 Friday 4:04 PM EST
Caraco close to OK on generic Provigil
LENGTH: 144 words
DATELINE: DETROIT, July 20
Caraco Pharmaceutical Laboratories said Friday it has been granted tentative
U.S. approval to market a generic version of Cephalon's Provigil.
The company said the Food and Drug Administration has granted tentative approval
to its modafinil tablets in 100-mg and 200-mg strengths, indicated to improve
wakefulness in patients with excessive sleepiness associated with narcolepsy.
Caraco said Provigil tablets had U.S. sales of roughly $753 million for the
12-month period ending March 31, based on IMS data.
"We are extremely pleased to receive this tentative approval," said Daniel
Movens, Caraco's CEO. "Modafinil was filed with a paragraph IV certification
that we do not infringe and or that the Cephalon patent is invalid. We were not
sued by Cephalon. We looked forward to marketing this product subsequent to the
expiration of the patent and exclusivity period."
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US Fed News
July 18, 2007 Wednesday 7:15 AM EST
Missouri Inventors Develop Benzhydrylthioacetamide Preparation Process
BYLINE: US Fed News
LENGTH: 234 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., July 18 -- Sidney Liang of Olivette, Mo., has developed a
process for preparing benzhydrylthioacetamide.
According to the U.S. Patent & Trademark Office: "The reaction employing the
haloacetamide is conducted in a solvent comprising water and an organic solvent
such as dimethylformamide having dissolved therein a basic salt such as
potassium carbonate. The resulting benzhydrylthioacetamide can be oxidized to
provide the pharmaceutical modafinil."
An abstract of the invention, released by the Patent Office, said: "The reaction
employing the haloacetamide is conducted in a solvent comprising water and an
organic solvent such as dimethylformamide having dissolved therein a basic salt
such as potassium carbonate. The resulting benzhydrylthioacetamide can be
oxidized to provide the pharmaceutical modafinil."
The inventor was issued U.S. Patent No. 7,244,865 on July 17.
The patent has been assigned to Mallinckrodt Inc, Hazelwood, Mo.
The original application was filed on Feb. 23, 2004, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,244,865.PN.&OS=PN/7,244,865&RS=
PN/7,244,865.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
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The Sunday Times (London)
July 15, 2007
Tired professors take 'smart' pills to perk up lectures
BYLINE: Will Iredale
SECTION: HOME NEWS; News; Pg. 7
LENGTH: 456 words
UNIVERSITY academics are using a "smart" prescription drug that enhances memory
and boosts concentration to give them the edge over their rivals when giving
presentations.
Studies into the effects of Modafinil, an American drug, have shown it can
improve mental ability without the side effects of stimulants such as
amphetamines or caffeine.
Modafinil was created to help sufferers from sleep disorders. It is also stocked
by the American army for use by exhausted soldiers.
Those academics who use the drug often do so because they fly round the world
giving lectures. They take Modafinil to perk themselves up after long flights so
that they can make their presentations despite jetlag.
Philip Harvey, professor of psychiatry and behavioural sciences at Emory
University school of medicine in Atlanta, said he had recently taken a Modafinil
tablet before flying to Britain to give a presentation the afternoon he landed.
"Ratings I have received for those presentations when I have used Modafinil have
been the same as at other times (when not jetlagged)," said Harvey. "It makes
you seem less tired and helps you perform the same as usual under less than
optimal conditions."
Barbara Sahakian, professor of neuropsychology at Cambridge University, who has
researched Modafinil, said academics she knew had started using the drug after
hearing about it through their work.
"I flew over to a conference in Florida and one of my colleagues offered me some
Modafinil. I found at least four colleagues took it and that was without me even
asking them. One was at Oxford, two were from The Hague and one was in
Washington," said Sahakian.
Researchers at Cambridge University who examined the effects of Modafinil found
that it dramatically improved memory function in healthy people who were not
sleep deprived.
Danielle Turner, from the department of psychiatry at Cambridge, tested 60
healthy young males on their ability to use touch-sensitive computer screens
after they had received either a placebo or a Modafinil tablet.
She found the volunteers given Modafinil performed significantly better and
showed less impulsive responding and an increased tendency to reflect on the
tasks they were given.
Modafinil can be bought over the internet or as a prescription drug in Britain
to treat sleep disorders such as narcolepsy. Although it can have mild side
effects, such as headaches, it is not addictive.
In April Foresight, a government think tank, said "cognitive enhancers" such as
Modafinil could be "as common as coffee" within a couple of decades to help a
person think faster and sleep more efficiently.
The Department of Health has asked The Academy of Medical Sciences to assess the
impact of such substances and a report is due in November.
LOAD-DATE: July 15, 2007
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Ob/Gyn. News
July 1, 2007
Modafinil May Help Patients With Chemo Brain
BYLINE: Kerri Wachter, Senior Writer
SECTION: Pg. 4 Vol. 42 No. 13 ISSN: 0029-7437
LENGTH: 649 words
CHICAGO - The narcolepsy drug modafinil (Provigil) appears to improve
attention and memory in breast cancer patients with chemo brain, a reduction in
cognitive function that has been associated with chemotherapy, according to data
presented at the annual meeting of the American Society of Clinical Oncology.
In a secondary analysis, Sadhna Kohli, Ph.D., of the University of Rochester
(N.Y.), and her colleagues assessed the effect of modafinil on memory and
attention in 68 women with breast cancer who had completed chemotherapy. The
study's primary end point was fatigue. The researchers hypothesized that
improvements in fatigue would be associated with improvements in cognition as
well. "Our results are the first to suggest that modafinil should be further
investigated as a new therapy for treating cognitive dysfunction after breast
cancer therapy," said Dr. Kohli.
Persistent cognitive impairment is a recognized side effect of chemotherapy
for cancer. The condition is often referred to as "chemo brain" or "chemo fog."
Dr. Kohli previously reported that 82% of cancer patients who underwent
chemotherapy experienced problems with memory and concentration.
The study began with 82 women who had scores of at least two on question No.
3 of the Brief Inventory of Fatigue (0-10 rating of worst fatigue in the past 24
hours) and had been off chemotherapy for an average of 22 months. They received
200 mg modafinil once daily for 4 weeks in the open-label portion of the trial.
A total of 76 women completed this portion of the trial. Following the
open-label phase, 68 women were randomized to receive either 200 mg modafinil or
placebo daily.
Tests of memory and attention, selected from the Cognitive Drug Research
computerized cognitive assessment, were performed at baseline and after
completing the open-label and randomized phases. The validity, test-retest
reliability, and sensitivity of this assessment tool had been demonstrated in
several populations, including those with normal aging, depression, and
drug-induced cognitive changes.
In particular, the researchers looked at five memory/attention components:
quality of episodic memory, speed of memory, continuity of attention, quality of
working memory, and power of attention.
There was a statistically significant improvement in the quality of episodic
memory (immediate word recall, word recognition accuracy, and picture
recognition accuracy) and speed of memory (two memory tasks and two recognition
tasks) from baseline to week 4 (the open-label phase).
At 4-8 weeks (the randomized phase), patients on modafinil had a larger
improvement in speed of picture recognition (a subsummary measure of memory
speed) than those on placebo. Likewise, patients on modafinil had a greater
improvement in immediate word recall (a subsummary measure of quality of
episodic memory).
Although there was no statistically significant difference in the improvement
of continuity of attention between baseline and week 4 (when all women were on
modafinil), women who continued on the drug did show a statistically significant
improvement at week 8, compared with week 4. "Taking modafinil for a longer
period does improve attention skills," said Dr. Kohli. In addition to being
faster, patients were also more accurate at retrieving information from memory.
Improvement in the quality of episodic memory indicates that patients on
modafinil were better able to store, retain, and retrieve both verbal and
pictorial information.
Modafinil is a central nervous system stimulant that is indicated to improve
wakefulness in patients with excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome, and shift-work sleep disorder. The
drug has been shown to reduce fatigue and improve declining mental performance
in military personnel performing continuous cognitive work.
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JOURNAL-CODE: OBNEWS
Copyright 2007 Elsevier Inc., International Medical News Group
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296 of 998 DOCUMENTS
The Daily Telegraph (LONDON)
June 23, 2007 Saturday
Students using prescription drug to boost performance in exams
BYLINE: Laura Clout
SECTION: NEWS; Pg. 10
LENGTH: 420 words
STUDENTS are using a controversial prescription drug that can keep them awake
for days and boost their short-term memory to improve their exam performance,
experts claimed last night.
Modafinil pills, known on the drugs scene as "zombies'', are among a new breed
of cognitive enhancers, or "smart drugs''.
Widely used in America and easily available on the internet, they appear to be
satisfying a growing demand for chemical mental enhancement among students when
revising for important exams.
It was reported this year that students at Oxford University were rejecting the
traditional choices, caffeine and ginseng, in favour of the anti-hyperactivity
drug Ritalin.
Drug trials suggest that Modafinil leads to an increase in energy and alertness,
boosts short-term memory and enables users to go for long periods without sleep.
Its makers say there are no side-effects, but experts are worried about the
potential for the drug to be abused.
In the United States, where Modafinil is used by students, clubbers and office
workers, there is anecdotal evidence that high doses of the drug cause anxiety
and headaches.
Paul Cooper, the director of education at Leicester University, has called for a
debate on whether such drugs, which are banned for athletes, should be permitted
for students in exams.
He said last night: "Should we regard these drugs as a pharmaceutical version of
the pocket calculator - something that students now rely on in exams as a matter
of course? This is a debate that needs to happen.''
Barbara Sahakian, professor of clinical neuropsychology at Cambridge University,
agreed that a debate was needed about how smart drugs should be treated given
their benefits.
She said: "We've done studies on Modafinil. It's very effective and it doesn't
have the same side-effects as Ritalin. I've been at meetings where I've been
offered Modafinil by colleagues, to combat jet lag.
"This is one of the first drugs where it doesn't seem to have abuse potential.
It seems to be a good enhancing agent with minimal side-effects.''
But she added: "The question is, what do we do? Should we treat it like
coffee?''
If the answer is yes, the next question facing universities may be whether they
should encourage students to take drugs. Foresight, the Government think-tank,
has said such drugs could be "as common as coffee'' within a couple of decades.
Such is the concern that the Department of Health has asked the Academy of
Medical Sciences to assess their potential impact in a report due to be
published in November.
LOAD-DATE: June 23, 2007
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The Times (London)
June 23, 2007, Saturday
Cheating students turn to 'smart drug' for edge in exams
BYLINE: Alexandra Frean Patrick Foster
SECTION: HOME NEWS; Pg. 16
LENGTH: 546 words
Students say they are turning to a powerful prescription drug that is stocked by
the Army to keep combat troops alert.
Modafinil, used to treat sleep disorders such as narcolepsy, appears to be
overtaking the anti-hyperactivity medicine Ritalin as the "smart drug" of choice
on university campuses.
Drug trials suggest that modafinil, which can be bought on the internet, is
highly effective at enhancing short-term memory and enabling users to stay up
for extended periods.
But experts say overuse can produce adverse side-effects. Some are also
beginning to question why a performance-enhancing drug that is banned for
athletes in the Olympics should be allowed for students in exams.
Paul Cooper, director of education at Leicester University, said that, although
universities had been aware for some time that students were using drugs such as
Ritalin and modafinil to get them through their exams, there had been no proper
consideration of whether this constituted cheating.
"As a society we need to ask whether we are happy about people who have no
impairments using these drugs to enhance their exam performance -we don't allow
it in sport, so why at university? Should we regard these drugs as a
pharmaceutical version of the pocket calculator -something that students now
rely on in exams as a matter of course? This is a debate that needs to happen."
Barbara Sahakian, Professor of Clinical Neuropsychology at Cambridge University,
agreed that it was difficult to know where to draw the line. "We've done studies
on modafinil. It's very effective and it doesn't have the same side-effects as
Ritalin. I've been at meetings where I've been offered modafinil by colleagues
to combat jet lag," she said.
"This is one of the first drugs where it doesn't seem to have abuse potential.
It seems to be a good enhancing agent with minimal side-effects. The question is
what do we do? Should we treat it like coffee?"
If the answer is yes, the next question facing universities may be this: should
students be encouraged to take such drugs?
Students have used drugs to boost their study performance in the past. Caffeine
and ginseng are traditional favourites. But recently the use of more powerful,
restricted drugs, particularly Ritalin, has spread from campuses in the US.
At present the debate within British universities remains focused on the health
risks faced by students taking prescription drugs. But students appear not to
share these concerns. An undergraduate at Oxford told The Times that he was
selling modafinil tablets to other students. "I bought the tablets on a Canadian
website but they were produced in India," he said. "I paid less than £ 1 per
tablet and sold them on for £ 8 to £ 12 a hit. I made over £ 3,000 in less than
two months. It got even more popular as finals approached." He said that he
would get up at 5am, take a tablet and then go back to sleep for an hour.
"I'd get up and feel completely refreshed, and I could work all the way through
until going to bed at 1am the next morning."
A spokesman for Oxford University said that any student aware of drug dealing
should report it to the police. Veronica King, head of welfare at the National
Union of Students, said that such dealing may be a sign of the increasing
pressures placed on today's students.
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The Times (London)
June 23, 2007, Saturday
It might be useful for judges and soldiers -but there are drawbacks
BYLINE: Dr Thomas Stuttaford
SECTION: HOME NEWS; Pg. 16
LENGTH: 521 words
Modafinil first came to the public notice when it was suggested that this was
the ideal pill to ensure that judges stayed awake in the court room and that it
might have the additional advantage that it might make their already-keen brains
even sharper.
Reports about the clinical use of modafinil first appeared in the journal
Neurology in 1997; the following year an even larger study was published in the
Annals of Neurology about an American trial of the drug. Following these initial
research papers there has been a host of other papers describing its use in
different neurological conditions. It is now the drug of choice in treating
narcolepsy, which can cause an overwhelming need to go to sleep, often at
inconvenient moments. Modafinil is also prescribed to counteract the tiredness
associated with shift working, and in those who suffer from sleepiness or lack
of energy as the result of obstructive sleep apnoea (loud snoring and restless
sleep).
The Army, which during the Second World War used amphetamines to keep soldiers
awake, is said to have stocks of modafinil as it is safer than amphetamines and
is not thought to be addictive. However, psychological dependence can develop
and it has many potential side-effects. It should not be taken by those who have
cardiovascular problems, liver or kidney disease.
Within the past two or three years it has been tried as a drug that might
sharpen up the intellects of people who have suffered strokes, and in general it
does seem to have the ability to improve short-term memory.
As with any useful drug there is the possibility of abuse and misuse. Some
students take modafinil so they can work all hours of the day and night. They
don't realise that the brain, like any other organ, needs periods of rest in
between activity if it is to give its best performance.
If someone continuously takes a stimulant day after day to cut down on sleep,
they are likely to become sleep deprived. They will then become tense, edgy,
irritable, aggressive and even confused and paranoid. Not the ideal mindset to
have before sitting an exam.
There is a well-known danger that athletics contests can degenerate into a
competition between pharmacologists rather than sportsmen.
It would be even more socially destructive if the difference between a first and
a second at a university was determined by the skill of the student doctors' and
their understanding of pharmacology rather than the inherent ability of the
student.
The drugs
Modafinil
Licensed in 1997, it is used to treat narcolepsy and other sleep disorders.
Helps users to stay awake when needed but still sleep at night. Is not a cure
but reduces sleepiness Sold under the name Provigil; modafinil is the active
ingredient Less likely than Ritalin to cause jitteriness; side-effects can
include headaches
Ritalin
Licensed in 1997, it is used for attention-deficit hyperactivity disorder.
Children with ADHD tend to be restless and find it difficult to concentrate Its
active ingredient is methylphenidate hydrochloride Side-effects can include
headaches, loss of appetite and jitteriness Sources: Cephalon/provigil.com;
Novartis
LOAD-DATE: June 23, 2007
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299 of 998 DOCUMENTS
PR Newswire US
June 18, 2007 Monday 10:55 AM GMT
Cephalon Receives FDA Approval of NUVIGIL(TM) for the Treatment of Excessive
Sleepiness Associated with Three Disorders
LENGTH: 1082 words
DATELINE: FRAZER, Pa. June 18
FRAZER, Pa., June 18 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
today announced that it has received approval from the U.S. Food and Drug
Administration to market NUVIGIL(TM) (armodafinil) Tablets [C- IV], a
non-amphetamine wake-promoting agent for the treatment of excessive sleepiness
associated with obstructive sleep apnea/hypopnea syndrome (OSAHS), narcolepsy,
and shift work sleep disorder (SWSD). In OSAHS, NUVIGIL is indicated as an
adjunct to standard treatment(s) for the underlying obstruction. NUVIGIL is the
single-isomer formulation of modafinil, the active pharmaceutical ingredient
contained in PROVIGIL(R) (modafinil) Tablets [C-IV], which was approved by FDA
in 1998 to improve wakefulness.
"FDA approval of NUVIGIL is a major accomplishment and the result of
collaborative efforts with the scientific and regulatory communities," said Dr.
Lesley Russell, Executive Vice President, Worldwide Medical and Regulatory
Operations. "We are excited about the future of NUVIGIL and we have initiated
additional clinical work to explore its potential in a wide range of medical
disorders."
Cephalon's clinical program will evaluate the use of NUVIGIL as a treatment for
serious medical conditions such as bipolar depression, cognition associated with
schizophrenia, excessive sleepiness in medical conditions such as Parkinson's
disease, and fatigue in patients who are being treated for cancer. The company
currently plans a commercial launch of NUVIGIL once additional clinical data has
been amassed.
"The approval of NUVIGIL allows us to preserve our current leadership position
in the area of wakefulness," said Frank Baldino, Jr., Ph.D., Chairman and CEO,
Cephalon. "More importantly, we now have a longer-term opportunity to further
characterize the utility of this compound beyond wakefulness." NUVIGIL is
protected by a U.S. patent expiring in 2023.
The agency has approved final labeling for NUVIGIL, including a bolded warning,
which is consistent with the draft labeling received by the company in March
2007. Full prescribing information will be available on the FDA website or on
the company's website at:
http://www.cephalon.com/newsroom/assets/Nuvigil_Prescribing_Information.pdf . As
expected, the agency also has indicated that it will request similar language in
the label for PROVIGIL.
About NUVIGIL
The active pharmaceutical ingredient in NUVIGIL, armodafinil, is the
longer-lived r-enantiomer of modafinil, the active ingredient in PROVIGIL. The
approval of NUVIGIL is based on positive results of four double-blind,
randomized, placebo-controlled studies in patients with excessive sleepiness
associated with either narcolepsy, SWSD or OSAHS. In these studies, NUVIGIL was
generally well tolerated. The most common side effects were mild to moderate in
intensity and included nausea, headaches, dizziness, diarrhea, decreased
appetite and upset stomach.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon has delivered a seven-year compound annual growth rate
(CAGR) greater than 75% and 2006 revenue of $1.760 billion. A member of the
Fortune 1000, Cephalon currently employs approximately 3,000 people in the
United States and Europe. U.S. sites include the company's headquarters in
Frazer, Pennsylvania, and offices, laboratories or manufacturing facilities in
West Chester, Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis,
Minnesota. Cephalon's European headquarters are located in Maisons-Alfort,
France.
The company's proprietary products in the United States include: PROVIGIL,
FENTORA(R) (fentanyl buccal tablet) [C-II], TRISENOX(R) (arsenic trioxide)
injection, VIVITROL(R) (naltrexone for extended-release injectable suspension),
GABITRIL(R) (tiagabine hydrochloride), and ACTIQ(R) (oral transmucosal fentanyl
citrate) [C-II]. The Company also markets numerous products internationally.
Full prescribing information on its U.S. products is available at
http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products, including any
additional clinical programs with respect to NUVIGIL; interpretation of clinical
results, particularly with respect to the NUVIGIL clinical trials; manufacturing
development and capabilities; market prospects for its products, including the
timing of the commercial launch of NUVIGIL, the clinical utility of NUVIGIL and
the longer-term opportunities with NUVIGIL beyond its current indication; sales
and earnings guidance; and other statements regarding matters that are not
historical facts, including the protection afforded by any patents covering
NUVIGIL. You may identify some of these forward-looking statements by the use of
words in the statements such as "anticipate," "estimate," "expect," "project,"
"intend," "plan," "believe" or other words and terms of similar meaning.
Cephalon's performance and financial results could differ materially from those
reflected in these forward-looking statements due to general financial,
economic, regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Jenifer Antonacci, +1-610-738-6674,
jantonacci@cephalon.com , or Investors: Robert (Chip) Merritt, +1-610-738-6376,
cmerritt@cephalon.com , both of Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: June 19, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 PR Newswire Association LLC.
All Rights Reserved.
300 of 998 DOCUMENTS
US Fed News
June 12, 2007 Tuesday 4:42 AM EST
Indiana, Ohio, Delaware Inventors Develop Modafinil Pharmaceutical Formulations
BYLINE: US Fed News
LENGTH: 157 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., June 12 -- Vincent Corvari of Carmel, Ind., George Grandolfi of
Milford, Ohio, and Alpa Parikh of Hockessin, Del., have developed compositions
of modafinil, including compositions of modafinil and one or more diluents,
disintegrants, binders and lubricants, and the processes for their preparation
thereof, the U.S. Patent & Trademark Office announced.
The inventors were issued U.S. Patent No. 7,229,644 on June 12.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on Sept. 13, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,229,644.PN.&OS=PN/7,229,644&RS=
PN/7,229,644.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com
LOAD-DATE: June 12, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
301 of 998 DOCUMENTS
CTV Television, Inc.
June 3, 2007 Sunday
SHOW: CTV NEWS 23:00:00 ET
Latest cancer research and treatments
ANCHORS: SANDIE RINALDO
LENGTH: 396 words
SANDIE RINALDO: Some of the world's leading cancer experts are in Chicago this
weekend to discuss the latest research and treatments, and today they're talking
about a little pill that's showing big promise. It's used to stimulate brain
activity in people with neurological disorders, but researchers found it's also
very effective in easing some of the debilitating side-effects of chemotherapy.
CTV's Denelle Balfour has the details.
DENELLE BALFOUR (Reporter): Diagnosed with breast cancer six years ago, Brenda
Oathout faced her disease with courage and resolve to survive. But it was the
side-effects of the treatment that nearly destroyed her will to go on.
BRENDA OATHOUT (Cancer Survivor): It was hard for me to be a mother and a wife
and to take care of my home.
BALFOUR: She suffered from chemo brain or chemo fog, a long misunderstood and
untreated side-effect of chemotherapy in some patients.
OATHOUT: You forget phone numbers. You forget how to get to places. It's just,
you draw a blank. You just simply draw a blank. It's scary.
BALFOUR: Now there could be help in a drug described by some as a genius pill
because it's often sought out by sleep deprived students and athletes. It's
called Modafinil, most often used to treat narcolepsy.
SADHNA KOHLI (University of Rochester Medical Centre): And what we found was
that Modafinil did improve fatigue and memory and did improve memory and
attention skills.
BALFOUR: In a first of its kind study, New York researchers, funded by the drug
maker, tested the effects of Modafinil on 68 women being treated for breast
cancer. Oathout was one of them.
OATHOUT: It was instantaneous. The very first thing I noticed was the fatigue
was gone, and then I noticed the struggle wasn't there.
BALFOUR: All of the women took Modafinil for the first four weeks of the trial.
For the next month, half of the women were given a placebo, but only the women
who continued to take Modafinil reported less fatigue and better concentration.
DR. BARBARA COLLINS (Ottawa Hospital): What this study is I think doing is
giving some hope that perhaps there is a treatment for this, and also validation
I think of patients' complaints.
BALFOUR: It's hoped this study will lead to an approach in the medical community
that is not only focused on beating the cancer, but also improving quality of
life during treatment. Denelle Balfour, CTV News, Toronto.
LOAD-DATE: June 4, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Transcript
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All Rights Reserved
302 of 998 DOCUMENTS
Internal Medicine News
May 15, 2007
FDA Cites Provigil Maker for Unapproved 'Fatigue' Promotion
BYLINE: Elizabeth Mechcatie
SECTION: Pg. 6 Vol. 40 No. 10 ISSN: 1097-8690
LENGTH: 269 words
The Food and Drug Administration has sent a warning letter to the
manufacturer of modafinil about promoting the drug for treating fatigue
associated with some neurologic and psychiatric disorders for which the drug is
not approved.
Promoting a drug for an indication that is not approved by the FDA is a
violation of the Federal Food, Drug, and Cosmetic Act.
Modafinil, marketed as Provigil by Cephalon, is approved for improving
wakefulness in people with excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSAHS), and shift-work sleep
disorder. It is also approved for people with OSAHS as an adjunct to standard
treatment for the underlying obstruction.
But a warning letter sent by the FDA to Cephalon said that as part of a
presentation made on behalf of the company at a meeting of the Maryland
Department of Health and Hygiene's Pharmacy and Therapeutics Committee in August
2006, a handout was provided on the use of modafinil in the medical and
psychiatric population.
The handout was "false and misleading," because it "states or suggests that
Provigil is safe and effective in the treatment of various disorders associated
with fatigue, sleepiness, or inattentiveness, when in fact, Provigil is not
indicated for fatigue at all and is indicated only for specific groups of
patients with excessive sleepiness," according to the FDA letter.
A spokesperson for Cephalon said that the company takes its regulatory
responsibility seriously and has "worked diligently to develop procedures and
policies to ensure that our products are lawfully promoted."
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
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303 of 998 DOCUMENTS
The Times (London)
May 14, 2007, Monday
Smart drugs for straight As
BYLINE: Peta Bee
SECTION: FEATURES; Times2; Pg. 8
LENGTH: 1820 words
Boosting your brain power by taking a pill could become a reality in the next
few years - but such drugs raise serious ethical and medical issues. PETA BEE
investigates It is probably fair to say that Bjorn Stenger was not at the back
of the queue when brains were being handed out. In fact, many might think there
was little room for improvement, given that he had graduated with a PhD in
engineering from Cambridge University. Within an hour of taking a drug called
Modafinil, though, Stenger appeared to become cleverer.
Taking part in a study at the university, Stenger, 33, took the drug, commonly
used to treat sleep disorders such as narcolepsy, and then performed some
computerised tests. Results showed improvements in his short-term memory,
attention span and reaction time. "I definitely felt a change," he says. "It was
a bit like the feeling you get after drinking strong coffee. I was somewhat more
alert, but not as jittery as after I have drunk coffee. I became very focused on
those tests."
Caffeine, guarana and other stimulants have long been used to ward off tiredness
or give an instant lift when needed. But their boost to the brain, by firing the
entire nervous system, is short-lived. Modafinil, though, is one of a new breed
of "smart" drugs that offer targeted, more powerful mental sharpening.
They are already widely used in America -studies have indicated that the black
market for such drugs is rife, particularly among university students -and there
are indications that the demand for chemical mental enhancement is about to take
off in the UK. Modafinil is easily purchased on the internet -I bought a packet
of the green tablets for £ 64. Such is the concern that the Government has
commissioned research to review the safety of brain-boosting pills. A report by
the Academy of Medical Sciences (AMS), commissioned by the Department of Health,
is due to be published and presented to the Government by November.
Dr Danielle Turner, a researcher in the department of experimental psychology at
Cambridge University who is working on the AMS review, says there is growing
evidence that certain drugs do help the brain work better. "So far, we do not
know enough about the full range of drugs that can affect thinking, but in the
case of Modafinil the side-effects appear to be benign," Turner says. "It seems
to improve short-term memory, the ability to plan and process information, and
helps a person to be less impulsive and more reflective about their
decision-making, which lends itself to greater accuracy."
In a 2003 study with Barbara Sahakian, a professor of clinical neuropsychology
at Cambridge, Turner found that healthy, male Cambridge students such as Stenger
who took a standard 200mg dose of Modafinil were found to use information more
effectively and efficiently. When confronted with conflicting stimuli, the
people who had taken Modafinil moved from one task to the next more smoothly and
adjusted swiftly without getting stressed or anxious. Sahakian suggested that
Modafinil "may be the first real smart drug" and that "a lot of people will
probably take it. I suspect they do already."
Last year it was revealed that Modafinil has been tested by British Armed Forces
and was reportedly stockpiled by the Ministry of Defence before the Iraq War,
although it was never given to combat personnel. But Modafinil does not stand
alone in its ability to sharpen the mind. A drug prescribed for Alzheimer's
disease -donepezil -has been shown to delay loss of mental ability in patients
and, more recently, to boost performance in tests of cognitive skill. In one
trial, published in the journal Neurology, pilots who took donepezil for a month
performed better in flight simulator tests than pilots who had taken a placebo.
Another drug, propanolol, seems to erase the negative emotions associated with
bad memories so that people who have taken it reel off disturbing stories as if
they were reading a food label.
Ritalin, best known as a treatment for attention-deficit hyperactivity disorder,
improves concentration and the ability to plan, perhaps appealing to adults who
want an edge in mental multitasking. Studies have also shown that the drug
boosts spatial working memory and the ability to remember graphs and diagrams,
and anecdotal evidence suggests that it improves concentration levels. A study
of 2,200 American students published in the journal Pharmacotherapy in 2004
found that 66 of them admitted using Ritalin as a study aid in the previous 12
months.
Chat rooms on US-based websites such as the Student Doctor Network frequently
discuss the purported merits of taking Ritalin and other drugs to boost mental
output in preparation for exams. Research at the University of Michigan shows
that 8 per cent of undergraduates report having illegally used prescription
drugs most commonly to improve alertness and attention.
In many cases, scientists have stumbled across cognition-enhancing effects of
drugs while researching their applications for serious neurological conditions.
Stroke patients who took small doses of amphetamines an hour before therapy were
found to perform better in simple motor skills (the tying of shoelaces and using
cutlery, for example) and scientists confirmed that the drugs seem to promote
"neuroplasticity" or the strengthening of brain connections. That led some,
including Dr Anjan Chatterjee, a neurologist at the University of Pennsylvania,
to question whether amphetamines might help healthy adults to learn skills more
easily.
Other potential smart drugs, each operating on different parts of the brain, are
in development (see box) and, provided they pass safety and effectiveness tests,
are likely to become available in the next few years. One is a new class of
drugs called ampakines that have already proved to be effective memory-boosters
in early trials.
In marketing terms, the potential for such drugs has never been greater. By
2012, about 41 per cent of the UK population (23.8 million people) will be over
50, an age at which memory and mental acuity demonstrate a significant decline.
For the baby boomer generation, the anxiety of watching their parents slip into
dementia means that the prospect of delaying their own mental decline is likely
to become as enticing as the possibility of preserving a youthful appearance.
Like Botox (originally developed for eye muscle problems), each of the drugs
identified as having cognition-boosting effects also has genuine medical
applications. Yet, potentially, they could follow the same marketing pattern as
the drug that has become better known as a wrinkle eraser.
Dr Chatterjee goes so far as to suggest that the trend for what he terms
"cosmetic neurology" will one day mean not only sharpening intelligence but
enhancement of other dictates of the brain -attention span, memory and reflexes.
Writing in the journal Neurology three years ago, he said the day when healthy
individuals pop a pill before an exam or a golf lesson "is coming, and we need
to know it's coming".
It presents an overwhelming ethical dilemma, he wrote, namely that "if the
purpose of medicine is to improve the quality of life of individuals who happen
to be sick, then should medical knowledge also be used to enhance the life
quality of those who happen to be healthy?" That is, should drugs with known
cognitive benefits be restricted for use only by those with illnesses such as
Alzheimer's.
The emergence of brain-boosting drugs raises serious ethical questions. Drugs
such as Modafinil can cost as much as £ 4 a dose on the black market: will the
rich simply get smarter and the poor be destined never to catch up? In an
interview with the Los Angeles Times, Professor James McGaugh, a neurobiology
professor at the University of California, suggested that it is inevitable that
pushy parents will one day give mind-enhancing pills to their children.
"If there is a drug that is safe and effective and not too expensive for
enhancing memory in normal adults, why not normal children?" he proposed. "After
all, they're going to school and what's more important than the education of the
young? And what would be more important than giving them a little chemical
edge?" But will those who don't take them at work or school be at a
disadvantage, and will the taking of drugs to boost performance become, in
essence, a form of cheating and be deemed as unethical as doping in sport?
There are concerns, too, about the long-term effects of healthy people using
such drugs. All drugs have side-effects, says Turner. In cases where people
require them for medical reasons, they are often prepared to overlook those side
effects if the medication improves their condition. But, she says, "it would be
devastating to learn that a dazzling youth of successful cognitive enhancement
meant a middle-age of premature memory loss and cognitive decline".
Perhaps most worrying is the way that these drugs might change who we are. To be
human is to be in possession of a personality with a unique blend of traits;
some scientists argue that changing one mental function might have an effect on
others.
To tinker with the mind, then, might result in better memory, focus and
attention in particular tests, but limit ability to shift attention and
interpret anything new or different. In short, cognitive enhancers might enable
us to know everything, but to lose our sense of individuality and opinion and to
understand nothing.
BRAIN-BOOSTERS: WHAT'S ON THE HORIZON?
Ampakines: research has indicated that this group of memory-modulating drugs,
developed for the treatment of Alzheimer's disease, has cognitive enhancing
effects.
Donepezil: a cholinesterase inhibitor developed for the treatment of dementia
that has also been shown to boost the brain function of healthy people. It
increases the concentration of a neurotransmitter called acetylcholine, boosting
the power of certain electrical transmissions between brain cells.
Modafinil: developed to treat the sleeping disorder narcolepsy, it has been
shown in clinical trials to boost the cognitive performance of healthy young
people and of helicopter pilots deprived of sleep.
Ritalin: a stimulant with a medical use as a treatment for attention deficit
hyperactivity disorder (ADHD) in children. It's easily obtained on the internet
or black market (it is dubbed "vitamin R") and studies reveal widespread use
among American students looking to improve concentration and alertness.
Propranolol: a beta-blocker shown in tests to neutralise emotionally-distressing
memories. A study in the journal Biological Psychiatry showed that patients in
A&E departments who were given the drug had a lower incidence of post-traumatic
stress symptoms.
Mem compounds: three separate compounds are under development by the US company
Memory Pharmaceuticals Corporation as possible treatments for Alzheimer's
disease.
Animal studies suggest that they can help to restore memory.
LOAD-DATE: May 14, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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304 of 998 DOCUMENTS
Clinical Psychiatry News
May 2007
Provigil Maker Cited After Promotion Of Unapproved 'Fatigue' Indication
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 3 Vol. 35 No. 5 ISSN: 0270-6644
LENGTH: 354 words
The Food and Drug Administration has sent a warning letter to the
manufacturer of modafinil about promoting the drug for the treatment of fatigue
associated with some neurologic and psychiatric disorders for which it is not
approved.
Promoting a drug for an indication not approved by the FDA is a violation of
the Federal Food, Drug and Cosmetic Act.
Modafinil, marketed as Provigil by Cephalon, is approved for improving
wakefulness in people with excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSAHS), and shift work sleep disorder
(SWSD). It is also approved for people with OSAHS as an adjunct to standard
treatment for the underlying obstruction.
But a warning letter sent by the FDA to Cephalon, dated Feb. 27, said that as
part of a presentation made on behalf of the company at a meeting of the
Maryland Department of Health and Hygiene's Pharmacy and Therapeutics Committee
in August 2006, a handout was provided on the use of modafinil in the medical
and psychiatric population. The handout was "false and misleading," because it
"states or suggests that Provigil is safe and effective in the treatment of
various disorders associated with fatigue, sleepiness, or inattentiveness, when
in fact, Provigil is not indicated for fatigue at all and is indicated only for
specific groups of patients with excessive sleepiness," according to the FDA
letter.
The promotional piece included the statement that modafinil "has utility" in
treating the following neurologic and psychiatric disorders associated with
fatigue, sleeplessness or inattentiveness: multiple sclerosis-related fatigue;
Parkinson's disease-related fatigue; chronic fatigue syndrome, fibromyalgia and
chronic pain conditions; attention-deficit disorder; and depression.
As requested by the FDA, Cephalon submitted a response to the letter by March
12, according to a company spokesperson, who said that the company takes its
regulatory responsibility seriously and that the company has "worked diligently
to develop procedures and policies to ensure that our products are lawfully
promoted."
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2007 Elsevier Inc., International Medical News Group
All Rights Reserved
305 of 998 DOCUMENTS
Clinical Neurology News
May 2007
News From The FDA Provigil Maker Cited for False 'Fatigue' Promotion
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 8 Vol. 3 No. 5 ISSN: 1553-3212
LENGTH: 337 words
The Food and Drug Administration has sent a warning letter to the
manufacturer of modafinil about promoting the drug for the treatment of fatigue
associated with some neurologic and psychiatric disorders for which the drug is
not approved.
Modafinil, marketed as Provigil by Cephalon, is approved for improving
wakefulness in people with excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSAHS), and shift work sleep disorder
(SWSD). It is also approved for people with OSAHS as an adjunct to standard
treatment for the underlying obstruction.
But a warning letter sent by the FDA to Cephalon, dated Feb. 27, said that as
part of a presentation made on behalf of the company at a meeting of the
Maryland Department of Health and Hygiene's Pharmacy and Therapeutics Committee
in August 2006, a handout was provided on the use of modafinil in the medical
and psychiatric population.
The handout was "false and misleading," because it "states or suggests that
Provigil is safe and effective in the treatment of various disorders associated
with fatigue, sleepiness, or inattentiveness, when in fact, Provigil is not
indicated for fatigue at all and is indicated only for specific groups of
patients with excessive sleepiness," according to the letter.
The promotional piece included the statement that modafinil "has utility" in
treating the following neurologic and psychiatric disorders associated with
fatigue, sleeplessness or inattentiveness: multiple sclerosis-related fatigue;
Parkinson's disease-related fatigue; chronic fatigue syndrome, fibromyalgia and
chronic pain conditions; attention deficit disorder; and depression.
As requested by the Food and Drug Administration, Cephalon submitted a
response to the letter, according to a company spokesperson, who said that the
company takes its regulatory responsibility seriously and that the company has
"worked diligently to develop procedures and policies to ensure that our
products are lawfully promoted."
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CNNEWS
Copyright 2007 Elsevier Inc., International Medical News Group
All Rights Reserved
306 of 998 DOCUMENTS
Hindustan Times
April 29, 2007 Sunday 12:19 PM EST
Jury is out on wakefulness drug
BYLINE: Hindustan Times
LENGTH: 354 words
DATELINE: NEW DELHI, India
NEW DELHI, India, April 29 -- MEDICAL EXPERTS are saying highly stressed
individuals in India - call center workers, corporate honchos and even students
- have lately been using Modalert or Modafinil to cut down on sleeping time and
enhancing alertness.
Before you think it is yet another high inducing 'upper' like Amphetamine or
Speed, here is what the drug actually is. Last week, Britain's Department of
Health asked the Academy of Medical Sciences to assess Modafinil as a
cognition-enhancing drug.
In India, the medicine has been around for three years. It is given to
narcoleptics, people with a neurological disorder marked by uncontrollable
attacks of daytime sleep. A prescription drug, Modalert is manufactured by Sun
Pharma and sold at Rs 60 for a strip of 10. Psychiatrist Dr Samir Parikh says,
"we do not know the long term effects" of the "relatively new drug".
"I have to work for long hours. I heard about Modalert from a friend and tried
it. I was awake for 26 hours at a stretch, " says 29-year-old web designer,
Raman Shah, who works in a publishing outsourcing firm. Dr Rajesh Sagar,
associate professor, psychiatry, AIIMS, says he frequently gets patients who
demand the drug. "We turn them away, as this drug may have serious side effects
in the long run." He also says Modalert is often used by medical students at
AIIMS for extended study sessions.
"Recently, a patient wanted me to prescribe Modalert: he claimed he had to work
long hours, he wanted to cut down on his sleep, yet stay alert," says Dr Anoop
Misra, Head of the Diabetics and Metabolism, Fortis Hospital. While doctors in
India are suspicious about the trend, the Department of Clinical Neurosciences
in Cambridge University has examined the effects of Modafinil on healthy
volunteers, and the results have been "dramatic".
"With Modafinil they [the volunteers] seemed to think a bit longer and they were
more accurate," Dr Danielle Turner, who headed the study, told the BBC.
So, will Modalert be the new wonder drug? Don't try it out till the debate is
settled.
The Hindustan Times is provided through HT Syndication, New Delhi.
LOAD-DATE: April 30, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
307 of 998 DOCUMENTS
Hindustan Times
April 28, 2007 Saturday 12:28 PM EST
Disaster pill for staying awake
BYLINE: Hindustan Times
LENGTH: 353 words
DATELINE: NEW DELHI, India
NEW DELHI, India, April 28 -- MODAFINIL, A medicine prescribed for a rare sleep
disorder, is being lapped up by students, call centre workers, corporate honchos
- in fact, anyone leading a high stress 24/7 lifestyle - to help them stay
alert, and not feel sleepy for as long as 36 hours. The medicine has been around
in India for a little over three years and is normally given to people who
suffer from narcolepsy, a neurological disorder marked by uncontrollable attacks
of daytime sleep. In India, Modalert is manufactured by Sun Pharma and is sold
for Rs 60 for a strip of 10.
Last month, a white-collar corporate worker approached Dr Anoop Misra, head of
the diabetics and metabolism, Fortis Hospital, requesting him for a prescription
for Modalert. "He claimed he had to work long hours, he wanted to cut down on
his sleep, yet stay alert", says Dr Misra. "Narcolepsy is a rare disease and one
must understand Modafinil is a not a replacement for sleep."
Dr Rajesh Sagar, associate professor, psychiatry, AIIMS, says that he regularly
gets patients who demand the drug. "We turn away these people, as this drug may
have serious side effects in the long run. It is not meant for healthy
individuals". "We issue regular warnings to students about the harm of sleep
deprivation", he says. "I have to work for long hours. I heard about Modalert
from a friend and tried it. I was awake for 26 hours at a stretch", says
29-year-old web designer, Raman Shah (name changed).
One reason for the rampant abuse of the drug are conflicting research findings.
While clinical practitioners warn about the harmful effects of Modafilin,
researchers are exploring its positive effects on human cognition. Last week,
the BBC reported that researchers at the Department of Clinical Neurosciences in
Cambridge University had examined the effects of Modafinil on healthy
volunteers. The results were dramatic. "With Modafinil they [the volunteers]
seemed to think a bit longer and they were more accurate," said Dr Danielle
Turner, who headed the study, to the BBC.
The Hindustan Times is provided through HT Syndication, New Delhi.
LOAD-DATE: April 29, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
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Hindustan Times
April 28, 2007 Saturday 12:08 PM EST
Jury is out on wakefulness drug
BYLINE: Hindustan Times
LENGTH: 354 words
DATELINE: NEW DELHI, India
NEW DELHI, India, April 28 -- MEDICAL EXPERTS are saying highly stressed
individuals in India - call center workers, corporate honchos and even students
- have lately been using Modalert or Modafinil to cut down on sleeping time and
enhancing alertness. Before you think it is yet another high inducing 'upper'
like Amphetamine or Speed, here is what the drug actually is. Last week,
Britain's Department of Health asked the Academy of Medical Sciences to assess
Modafinil as a cognition-enhancing drug.
In India, the medicine has been around for three years. It is given to
narcoleptics, people with a neurological disorder marked by uncontrollable
attacks of daytime sleep. A prescription drug, Modalert is manufactured by Sun
Pharma and sold at Rs 60 for a strip of 10. Psychiatrist Dr Samir Parikh says,
"we do not know the long term effects" of the "relatively new drug".
"I have to work for long hours. I heard about Modalert from a friend and tried
it. I was awake for 26 hours at a stretch, " says 29-year-old web designer,
Raman Shah, who works in a publishing outsourcing firm. Dr Rajesh Sagar,
associate professor, psychiatry, AIIMS, says he frequently gets patients who
demand the drug. "We turn them away, as this drug may have serious side effects
in the long run." He also says Modalert is often used by medical students at
AIIMS for extended study sessions.
"Recently, a patient wanted me to prescribe Modalert: he claimed he had to work
long hours, he wanted to cut down on his sleep, yet stay alert," says Dr Anoop
Misra, Head of the Diabetics and Metabolism, Fortis Hospital. While doctors in
India are suspicious about the trend, the Department of Clinical Neurosciences
in Cambridge University has examined the effects of Modafinil on healthy
volunteers, and the results have been "dramatic".
"With Modafinil they [the volunteers] seemed to think a bit longer and they were
more accurate," Dr Danielle Turner, who headed the study, told the BBC.
So, will Modalert be the new wonder drug? Don't try it out till the debate is
settled.
The Hindustan Times is provided through HT Syndication, New Delhi.
LOAD-DATE: April 29, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
309 of 998 DOCUMENTS
Sydney Morning Herald (Australia)
April 28, 2007 Saturday
First Edition
Perchance to dream;
The office
BYLINE: Lissa Christopher
SECTION: MY CAREER; Pg. 2
LENGTH: 550 words
Drugs to keep you awake would be a nightmare, writes Lissa Christopher.
Last night I was awake for hours worrying about Allan Moss, the managing
director of Macquarie Bank. I couldn't remember if his salary package last year
was $20 million or $21 million. Either way, I thought, as the clock showed
3:07am in sickening green, why is he still working at all? Surely any balanced
person who earned that much money in one year would work for precisely one year
and then quit to do a whole lot of shopping and lying around looking smug.
Are you all right, Allan? Why do you stay? And could you spare us $50 until
payday?
By 4am I had moved on to fretting about Richard Fairbank from Capital One
Financial, who is the highest paid chief executive in the United States. In
2005, he earned US$249.42 million ($299 million), according to Forbes magazine.
And, like Moss, he's still working. (He also calls himself Rich rather than
Richard, which does strange things to my gag reflex.)
If I earned that kind of money, there's no way I'd still be working. Frankly,
I'd consider hiring someone to blink for me. Yet Fairbank has been head of COF
for 11 years and on he plugs. It's another one of life's little mysteries.
Thanks to all that stewing over executive salaries in the hour of the wolf, I
now have a sleep debt that would rival your average Sydney mortgage. I have
heard, however, that sleepiness - indeed, sleep itself - may soon be a thing of
the past.
A "wakefulness promoting agent" called Modafinil has been available on
prescription in the UK for some time. It's meant for people with sleep-inducing
conditions, such as narcolepsy. It's not a nasty amphetamine and it improves
cognitive performance as well as reducing the need for sleep. It has scientists
excited.
New Scientist says everyone may soon be able to take Modafinil-like medications
which could alleviate the need for sleep altogether. And I can just imagine what
Australian Workplace Agreements will look like when that happens.
I don't want to give up sleep. I'm really good at it. And dreaming gives me an
exciting second life. I have been chased by a herd of marauding 10-litre buckets
and had a fight with a tiny orange witch who wanted to hurt me with anchovies.
And, just like you, I've had a few Kamasutra-esqe encounters with work
colleagues with whom, when I'm awake, I can hardly bear to share an office
complex.
Anyway, apparently some perfectly healthy innovative types have bought Modafinil
illegally via the internet and are using it to give them the edge at work, says
London's Daily Telegraph. The British health department has commissioned a
report into what might happen if everyone starts doing the same thing.
"In a world that is increasingly non-stop and competitive," the report says,
"the use of such substances may move from the fringe to the norm, with cognition
enhancers used as coffee is today."
The ethics of using cognitive enhancers in the workplace and elsewhere, it says,
will take years to resolve.
In the meantime, office workers could come to resemble elite athletes in one of
those sports where everyone takes performance-enhancing drugs but no one admits
it. To apply for a job, you will need to send in your resume and a urine sample.
No one will sleep. The orange witch and her anchovies will be lonely.
LOAD-DATE: July 17, 2007
LANGUAGE: ENGLISH
GRAPHIC: CARTOON: By aweldon
PUBLICATION-TYPE: Newspaper
Copyright 2007 John Fairfax Publications Pty Ltd
All Rights Reserved
310 of 998 DOCUMENTS
The Associated Press
April 25, 2007 Wednesday 5:59 PM GMT
License of doctor in BALCO steroids scandal suspended
SECTION: SPORTS NEWS
LENGTH: 234 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
has been suspended from practicing medicine after investigators found he
prescribed a stimulant to a sprinter without examining her.
Dr. Brian Halevie-Goldman, a psychiatrist who was medical director for the Bay
Area Laboratory Co-Operative that provided steroids to top athletes, was
suspended for 90 days by the state medical board.
Halevie-Goldman also was placed on five years' probation and ordered to undergo
a psychiatric evaluation for allegedly providing the drug modafinil to the
athlete at the request of BALCO founder Victor Conte, who served four months in
federal prison for dealing steroids.
Goldman told the board Conte provided him with false information about the
sprinter's medical condition in order to obtain drugs for her. The doctor had no
immediate comment when contacted Wednesday by The Associated Press.
The medical board's accusation said the athlete, identified only as K.W., tested
positive for modafinil at an international track meet in August 2003 and
accepted a two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
LOAD-DATE: April 26, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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THE SAN FRANCISCO CHRONICLE (California)
April 25, 2007 Wednesday
FINAL Edition
THE BALCO CASE;
Doctor who provided stimulant is suspended;
State Medical Board calls sprinter's case 'gross negligence'
BYLINE: Lance Williams, Mark Fainaru-Wada, Chronicle Staff Writers
SECTION: BAY AREA; Pg. B3
LENGTH: 708 words
The former medical director of BALCO, the Burlingame laboratory at the center of
the sports steroids scandal, has been suspended from practicing medicine for 90
days because he provided prescription stimulants to a champion sprinter without
ever examining her.
The state Medical Board also put Dr. Brian Halevie-Goldman on five years'
probation, ordered him to undergo a psychiatric evaluation and imposed other
restrictions on his medical practice, saying he was guilty of "gross negligence"
for misconduct in a high-profile sports doping case in 2003.
In its decision, the board said Goldman had provided the powerful stimulant
modafinil for the sprinter it identified only by the initials KW simply because
he was asked to do so by BALCO founder Victor Conte, who later pleaded guilty to
providing banned drugs to elite athletes.
When KW failed a doping test after a track meet, Goldman faked a medical history
and diagnosis in an effort to help her avoid punishment for using banned drugs
before the race, the board said.
Though the Medical Board withheld identification of the sprinter, the case
involves elite sprinter Kelli White of Union City, a BALCO client who tested
positive for modafinil after winning two gold medals at the World Championships
in Paris in 2003.
White later confessed to using banned drugs and was suspended from competition
for two years. Saying she wanted to help clean up sports, White has testified at
several athletes' disciplinary hearings conducted by the U.S. Anti-Doping
Agency.
Documents show Goldman told the Medical Board he had been "set up" by Conte,
complaining that the BALCO founder had provided him with false information about
the sprinter's medical condition in order to obtain drugs for her. Goldman
didn't respond to a phone message Tuesday.
Goldman is a psychiatrist who has worked at Fairfield's Amen Clinic. In 1984, he
began moonlighting as medical director at Conte's Bay Area Laboratory
Co-Operative in Burlingame. At some point Goldman stopped working there, but
BALCO continued to list him on state documents as the lab's medical director,
and he and Conte stayed in touch.
In January 2003, according to the Medical Board, Conte asked Goldman to give him
modafinil for White and, without ever talking with White, Goldman gave Conte
samples of modafinil for her. At the time, Conte was providing the banned
stimulant to several sprinters to help them run faster, according to court
records.
In August 2003, White won both the 100- and 200-meter races at the Paris world
championships. Two days later, authorities announced that she had tested
positive for modafinil.
With Goldman's help, White tried to fight the charges. Goldman wrote a letter
falsely claiming that White had a family history of narcolepsy and that he had
given her the drug to treat the ailment, the Medical Board said. Goldman also
wrote a letter to the International Association of Athletics Federations arguing
that modafinil could not enhance athletic performance. Goldman was paid $5,000
for the letters, the Medical Board said.
White later acknowledged that she had never suffered from narcolepsy, saying
Goldman's diagnosis was part of a false alibi concocted by Conte.
White said Conte and her coach, Remi Korchemny, had provided her many other
banned drugs, including the undetectable steroid known as "the clear."
Conte served four months in federal prison on his guilty plea in the BALCO
steroids conspiracy case. Korchemny, who also pleaded guilty to steroid dealing,
was put on probation.
When Goldman was interviewed by the Medical Board, he acknowledged that he had
first examined White on Oct. 1, 2003, weeks after she was suspended for using
modafinil. At first, Goldman told investigators that he had consulted with White
by phone before providing her with the drug, but he later admitted that he
couldn't remember talking to her, the Medical Board said.
In its April 16 decision, the board said Goldman "needs to gain insight into
what caused him to participate in such unethical and dishonest conduct." In
addition to the psychiatric examination, the board ordered him to take a course
in medical ethics. Goldman also must hire a physician to monitor his medical
practice and make regular reports to the medical board.
LOAD-DATE: April 25, 2007
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Associated Press Worldstream
April 25, 2007 Wednesday 6:17 PM GMT
License of doctor in BALCO steroids scandal suspended
SECTION: SPORTS NEWS
LENGTH: 234 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
has been suspended from practicing medicine after investigators found he
prescribed a stimulant to a sprinter without examining her.
Dr. Brian Halevie-Goldman, a psychiatrist who was medical director for the Bay
Area Laboratory Co-Operative that provided steroids to top athletes, was
suspended for 90 days by the state medical board.
Halevie-Goldman also was placed on five years' probation and ordered to undergo
a psychiatric evaluation for allegedly providing the drug modafinil to the
athlete at the request of BALCO founder Victor Conte, who served four months in
federal prison for dealing steroids.
Goldman told the board Conte provided him with false information about the
sprinter's medical condition in order to obtain drugs for her. The doctor had no
immediate comment when contacted Wednesday by The Associated Press.
The medical board's accusation said the athlete, identified only as K.W., tested
positive for modafinil at an international track meet in August 2003 and
accepted a two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
LOAD-DATE: April 26, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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The Associated Press State & Local Wire
April 25, 2007 Wednesday 5:59 PM GMT
License of doctor in BALCO steroids scandal suspended
SECTION: SPORTS NEWS
LENGTH: 234 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
has been suspended from practicing medicine after investigators found he
prescribed a stimulant to a sprinter without examining her.
Dr. Brian Halevie-Goldman, a psychiatrist who was medical director for the Bay
Area Laboratory Co-Operative that provided steroids to top athletes, was
suspended for 90 days by the state medical board.
Halevie-Goldman also was placed on five years' probation and ordered to undergo
a psychiatric evaluation for allegedly providing the drug modafinil to the
athlete at the request of BALCO founder Victor Conte, who served four months in
federal prison for dealing steroids.
Goldman told the board Conte provided him with false information about the
sprinter's medical condition in order to obtain drugs for her. The doctor had no
immediate comment when contacted Wednesday by The Associated Press.
The medical board's accusation said the athlete, identified only as K.W., tested
positive for modafinil at an international track meet in August 2003 and
accepted a two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
LOAD-DATE: April 26, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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Daily Mail (London)
April 18, 2007 Wednesday
Fears over drugs that can boost your brain
BYLINE: JENNY HOPE
SECTION: ED 1ST; Pg. 17
LENGTH: 674 words
NEW drugs that can boost brainpower could be given to children by pushy parents,
it was claimed yesterday.
There are also fears that high- flying professionals might take the 'cognition
enhancers' to gain a competitive edge at work.
The warnings came as Government backed researchers examine the potential of the
drugs which previous research has shown to improve memory, concentration and
learning ability.
Critics say users can put themselves at risk of sleep deprivation and suffer
damage to their brain and central nervous systems.
In the U.S., cognition drugs are taken by people such as long-distance truckers,
students and taxi drivers because it 'turns off' the need to sleep while
allowing them to remain mentally alert for days.
One of the drugs modafinil is licensed in the UK only to treat narcolepsy, a
rare condition in which sufferers fall asleep without warning.
It emerged last year that the UK military has tested modafinil and reportedly
stockpiled thousands of pills ahead of the Iraq war. It has, however, never been
given to combat troops.
The drug has been banned by the International Olympic Committee, along with
another stimulant, ephedrine, which has also been tested by the Ministry of
Defence.
Sales have risen by 39 per cent since modafinil was launched in 2004. The
Academy of Medical Sciences is heading an independent official review of all
medical substances that come under the banner of cognition enhancers.
Professor John Bell, the academy's president, said: 'Our knowledge of how the
brain works, how genes influence its behaviour and how it is influenced by
chemicals, is developing at such a pace that we could be nearing a new era of
drug use where we have medicines that can enhance our performance as well as
improve our health.' But reaction from public workshops held by the academy
across the country brought forth fears that students and workers might misuse
the drugs.
One respondent wondered whether she would be putting her children at a
disadvantage if she did not give them access to such drugs.
Another expressed concern that workers would have to take the drugs to keep up
with colleagues.
The review, commissioned by the Department of Health, follows research carried
out by the Government's Foresight programme on brain science, addiction and
drugs.
It looked at the potential development of cognitive enhancers over the next 20
years and concluded they could become as 'common as coffee'.
Professor Leslie Iversen, a member of the review team, told a London seminar it
was vital to gauge public reaction.
He said: 'We need to know the answer to the question Should cognition enhancers
become available?
'We need evidence-based clarification of the effects of illegal and legal drugs
and we can't exclude legal drugs from causing harm.' Research carried out at
Cambridge University in 2002 found that healthy volunteers taking modafinil
scored higher on computer games designed to test their mental functions than
those given a placebo.
Amphetamine-style drugs have been used in the past in an attempt to improve some
aspects of performance when subjects are tired.
But they can cause impairments in other functions and may be addictive.
The review team will send a report to the Government in November.
j.hope@dailymail.co.uk
WIDESPREAD sale of ' cognition enhancers' could change the face of work and
study, according to experts.
For decades caffeine and vitamins have been the mainstays of students needing to
stave off sleep to improve their performance in revision and exams.
But the next generation of drugs could herald an era of 'mental cosmetics' that
promises to enhance the brain power of millions. Prescription drugs used for
Alzheimer's and sleep disorders have been tested on healthy volunteers with
startling results.
They were able to memorise more words than normal, concentrate better and work
tirelessly for longer.
But the potential abuse of these products has raised ethical and health
concerns.
Should children face dope tests before taking exams and should the sale of the
drugs be restricted?
LOAD-DATE: April 18, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Papers
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ABC Transcripts (Australia)
April 17, 2007 Tuesday 12:54 PM AEST
SHOW: The World Today 12:54 PM AEST ABC
Smart drugs under examination
REPORTERS: Rafael Epstein
LENGTH: 480 words
EMMA ALBERICI: They're calling it the thinking person's Viagra; a group of drugs
that some scientists say could make you smarter.
The British government is assessing the impact of these substances, as Europe
Correspondent, Rafael Epstein reports.
RAFAEL EPSTEIN: Britain's Department of Health has asked the Academy of Medical
Sciences here to have a look at the so-called "cognition enhancing" drugs, some
of which are already available in the US and Australia.
Modafinil was created to help people who can't stop themselves falling asleep.
It's now used by many to work and play longer and harder with less sleep.
At Cambridge University Dr Danielle Turner gave the drug to 60 volunteers.
DANIELLE TURNER: After one day, about two hours after they had the dose, they
were better at remembering strings of numbers, they were better at planning,
they were less impulsive, they were better at inhibiting impulsive actions that
they were making.
They remembered longer strings of numbers, their short term memory was improved,
and that might help you if you were for example a receptionist or something,
where somebody tells you, you know, this is my phone number, can you actually
write, down the phone number without...
RAFAEL EPSTEIN: And say your boss gives you four things, four tasks very
quickly, perhaps you could remember that better?
DANIELLE TURNER: Yes, exactly.
RAFAEL EPSTEIN: The idea of looking for what other people might call lifestyle
drugs, do you have any of those concerns about looking at these sorts of
effects.
DANIELLE TURNER: There are so many different viewpoints. Do you think it's a
good idea that we enhance ourselves and should we make it compulsory for
everyone to take whatever they've got, in the same way that people need to take
vaccinations or have to learn to read, so could cognitive enhancers go that way?
Or do we want to ban them which is what the sporting world has done, so the
sporting world has banned modafinil, that in fact... I've just applied for
funding to look at comparing modafinil and caffeine, because in some ways, I
don't think modafinil is a wonder drug, it doesn't make you Einstein or
anything, it just improves your performance a little bit.
RAFAEL EPSTEIN: Are you saying that you just think it's like a lot of good
coffee or is it something more than that?
DANIELLE TURNER: Well, that's what we don't know and, you know, is it just
because it's a pharmaceutical drug that they're concerned about it. We don't
know yet what the long term effects are, we don't really have a good idea of
what happens if you take it every day for several years.
RAFAEL EPSTEIN: Drugs like this work by boosting the activity of glutamate, a
key neurotransmitter that makes it easier to learn and encode memory. The drugs
could change the rules about what it takes to create a memory, and how strong
those memories can be.
EMMA ALBERICI: Rafael Epstein.
LOAD-DATE: April 17, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Transcript
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BioWorld Insight
April 9, 2007
Cephalon Opinion Spectrum Wide After Latest On Nuvigil
LENGTH: 1177 words
West Coast Editor
The FDA's blessing of Cephalon Inc.'s sleepiness drug Nuvigil came right on
time, but brought a demand for boldface label warnings about skin rash - and
didn't do much to soothe investors chafing over a government investigation of
the firm's marketing practices.
A single-isomer formulation of modafinil, Nuvigil improves wakefulness in
particularly groggy narcoleptics, as well as those with shift-work sleep
disorder and obstructive sleep apnea/hypopnea syndrome. The FDA got Cephalon'
new drug application for Nuvigil in March 2005, and sent back the first
approvable letter a year ago.
In the latest letter, the agency does not ask for new trials, but wants a
standard safety update on Nuvigil from research conducted since June, and wants
to see the introductory promotional materials. Earlier this year, Cephalon got a
warning letter from the FDA about efforts to push Provigil (modafinil), the
company's approved narcolepsy drug. Regulators said the one-shot marketing
message created new intended uses and did not provided information about risks.
Another shadow on Nuvigil is the history of Sparlon, a different formulation of
modafinil intended for attention-deficit/hyperactivity disorder, declared not
approvable by the FDA and dropped by Cephalon last summer. Sparlon was
associated with a single suspected case of a rare but serious skin rash called
Stevens-Johnson syndrome, and the FDA's Psychopharmacologic Drugs Advisory
Committee had voted unanimously that the drug is effective for its intended use
but also recommended that the company put together more safety data in children
and adolescents.
Some speculated that Sparlon, yet another potential ADHD drug, might have been
turned down partly because the agency was fed up with the proliferation of
therapies for the condition and the high rate of prescriptions written by
doctors. Still, the rash possibility was enough to make the FDA insist that
Cephalon smack the label warning not only on Nuvigil, but add it to the Provigil
label as well.
Most suspicion of regulatory disfavor for ADHD drugs was dispelled by later FDA
actions, such as the approval in February of Vyvanse from Shire plc and New
River Pharmaceuticals Inc., who planned to push to switch prescribers from
Adderall XR, Shire's ADHD capsule. Shire is buying New River for $2.6 billion in
cash.
Separately for Cephalon, there's the probe demanded by Rep. Henry Waxman
(D-Calif.), chairman of the House Committee on Oversight and Government Reform
(a panel that keeps tabs on pharmaceutical marketing practices) into the way
Cephalon markets the narcotics Actiq and Fentora, which are approved for cancer
breakthrough pain and often prescribed off label.
Another for Cephalon involves competitors with generic versions of Provigil. The
firm's deals with generic drug makers caused Apotex Corp. to file a lawsuit
against Cephalon last June, alleging that the settlements - which keep cheaper
versions of Provigil off the market until 2012 - create a monopoly, in a
situation that also drew the interest of the Federal Trade Commission. In the
legal action, Apotex named Cephalon and the licensees involved: Barr
Laboratories Inc., Mylan Laboratories Inc., Teva Pharmaceutical Industries Ltd.,
and Ranbaxy Laboratories Ltd. Cephalon's plan is to shift Provigil patients to
Nuvigil in 2009, ahead of the launch of the generics.
Russell McAllister, analyst with Merriman Curhan Ford & Co., put the matter
plainly in a research report: "Although full approval of Nuvigil would moderate
Provigil risk exposure, we continue to see two distinct sources of risk for
Cephalon - aggressive marketing and related off-label usage of both
Actiq/Fentora and Provigil/Nuvigil," and Cephalon's settlements with the generic
filers. McAllister maintained his "sell" rating on Cephalon shares this month.
At the other end of the spectrum, though, analysts at Robert W. Baird & Co.
stayed with an "outperform" rating and predicted approval of Nuvigil in late
June, only three months later than previously expected. Analyst David Windley
with Jefferies & Co. upgraded the stock from "hold" to "buy," and hiked his
price target to $88 from $69.
Analysts at UBS, who had initiated coverage of Cephalon in late March with a
"buy" rating (target price: $85), reiterated their opinion after the Nuvigil
news. JMP Securities held to their "strong buy," with a target price of $80.
Banc of America Securities, later in the week, started coverage of Cephalon with
a "neutral" opinion and $75 price target.
Megan Murphy at Lazard Capital Markets deemed the stock worth holding. The
situation could worsen if the boldface warning finds its way onto Nuvigil's
promotional materials as well as the label, but if it were limited to the label,
"we wouldn't expect anyone to know about it other than the FDA and Wall Street,"
Murphy wrote in a research report.
Clinical proof that Nuvigil boasts broader utility than Provigil would provide
"higher confidence that this franchise can continue to grow and expand after
eight years rather than merely be sustained," Murphy wrote, and another question
is whether Nuvigil can hold ground against the generic Provigil, "be it two
years after Nuvigil launches or perhaps much earlier."
She pointed to Nuvigil study data offered at a scientific meeting in 2006 that
showed the secondary endpoints of attention and speed of memory were not better
than placebo, and quality of episodic memory was met in the 150 mg study but not
in the larger 150 mg and 250 mg study.
"They haven't expanded the [Provigil] label, and separate from that is whether
the sales force expansion has played out in the scrip growth," Murphy told
BioWorld Financial Watch. Cephalon added 500 reps to the sales force last June
and, three months ago, another 250, but the prescriptions have not jumped
appreciably, and growth is settling into the 10 percent to 12 percent range.
The question becomes whether Provigil users can be converted to Nuvigil - and,
ultimately, how much the sleep franchise can grow, especially with the advent of
Provigil generics, which might well reach the market sooner than 2012, Murphy
believes.
She compared Cephalon's Provigil to the likes of Endo Pharmaceuticals Inc.'s
Lidoderm, a 5 percent lidocaine topical patch for the treatment of post-herpetic
neuralgia. Endo investors are nervous about a Lidoderm generic threat, and the
stock is trading lower even before one has been disclosed - even though Endo has
a more robust pipeline than Cephalon.
She also pointed to Forest Laboratories Inc., whose blockbuster antidepressant
Lexopro (escitalopram oxalate) also faces trouble similar to Cephalon's, albeit
not until around the time Cephalon expects Provigil's competition to arrive, if
the settlements hold. Last summer, a court determined that Forest's patent
covering escitalopram is valid and enforceable and is infringed by a proposed
generic IVAX Pharmaceuticals Inc. and Teva Pharmaceuticals Industries Ltd. The
judge found in favor of Forest and partner H. Lundbeck A/S.
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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Global Insight
April 4, 2007
FDA Issues Second Approvable Letter for Cephalon's Nuvigil
BYLINE: Milena Izmirlieva
SECTION: In Brief
LENGTH: 320 words
U.S. drug-maker Cephalon announced it has received a second approvable letter
from the FDA for its investigational drug Nuvigil (armodafinil) Tablets [C-IV]
for the treatment of excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSAHS) and shift work sleep disorder
(SWSD). The company is not required to conduct additional clinical trials but
will have to provide a standard safety update on trials conducted since its last
update submission in June 2006. In addition, Cephalon will have to supply the
FDA with its launch promotional materials for the drug. Nuvigil is a
single-isomer formulation of modafinil; the active ingredient contained in
Cephalon's drug Provigil, which is marketed for the same indications.
Significance: The issuing of a second approvable letter is actually good news
for Cephalon. It puts an end to the period of uncertainty following the FDA's
first approvable letter, particularly with respect to the labelling of the drug.
Nuvigil will carry a bolded warning section detailing the risk of a skin rash
and hypersensitivity in patients taking modafinil and amodafinil reactions seen
with the drug's predecessor Provigil but the language of the warning is expected
to be rather mild. There is now finally a timeline for the approval of Nuvigil:
Cephalon will file its response to the FDA within 30 days and FDA approval is
expected within 60 days thereafter. The Nuvigil approval delay could have been a
problem for Cephalon if Provigil had lost its patent protection in the meantime,
but the threat of this was effectively postponed (see United States: 12 December
2005: ). Upon its launch, Nuvigil will cannibalise sales of Cephalon's own
Provigil, but this is a risk well worth taking considering that the successful
launch of Nuvigil will ensure that Cephalon retains exclusive access to part of
the modafinil market until 2023 via the successor drug.
LOAD-DATE: April 4, 2007
LANGUAGE: ENGLISH
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Pharma Marketletter
April 3, 2007 Tuesday
Cephalon's Nuvigil gets tentative OK from FDA
LENGTH: 245 words
US drugmaker Cephalon has received an approvable letter, together with draft
labeling from the Food and Drug Administration for its New Drug Application for
Nuvigil (armodafinil) tablets for the treatment of excessive sleepiness
associated with narcolepsy, obstructive sleep apnea (OSAHS) and shift-work sleep
disorder (SWSD).
The draft labeling includes a proposed bolded warning section that characterizes
the potential occurrence of skin rash and hypersensitivity in patients taking
modafinil and armodafinil and Cephalon's first-generation wakefulness drug
Provigil (modafinil).
Among other things, the agency has requested that the company provides a
standard safety update from clinical trials conducted since the last update in
June 2006, and introductory promotional materials to be used for the product.
The company's response will be submitted within 30 days and will be considered a
Class I response; the agency is expected to complete its review within 60 days
thereafter and has not requested any additional studies prior to final approval
of Nuvigil.
Nuvigil is a single-isomer formulation of modafinil, the active pharmaceutical
ingredient contained in Provigil which is FDA-approved for the treatment of
excessive sleepiness associated with narcolepsy, OSAHS and SWSD. The Nuvigil NDA
is based on positive results of four double-blind, randomized,
placebo-controlled studies in patients with excessive sleepiness associated with
any of the three indications.
LOAD-DATE: April 3, 2007
LANGUAGE: ENGLISH
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CNS Drug News
Pharmaceuticals
April 2, 2007
Cephalon provides update on Nuvigil NDA
LENGTH: 371 words
Cephalon has received an approvable letter, together with draft labelling, from
the FDA for its NDA for Nuvigil ( armodafinil ) Tablets [C-IV], for the
treatment of excessive sleepiness associated with narcolepsy, obstructive sleep
apnoea/hypopnoea syndrome (OSAHS) and shift work sleep disorder (SWSD). The
draft labelling includes a proposed bolded warning section that characterises
the potential occurrence of skin rash and hypersensitivity in patients taking
modafinil and armodafinil. As expected, the Agency also indicated that it will
request similar language in the label for Provigil ( modafinil ) Tablets [C-IV].
Among other things, the Agency requested that Cephalon provide a standard safety
update from clinical trials conducted since the last update in June 2006, and
introductory promotional materials to be used for the product. The company's
response will be submitted within 30 days and considered a Class I response; the
FDA, which has not requested any additional studies prior to final approval of
Nuvigil, is expected to complete its review within 60 days thereafter.
Editor's note: Nuvigil is a single-isomer formulation of modafinil, the active
pharmaceutical ingredient contained in Provigil, which is FDA-approved for the
treatment of excessive sleepiness associated with narcolepsy, OSAHS and SWSD.
The Nuvigil NDA is based on positive results of four double-blind, randomised,
placebo-controlled studies in patients with excessive sleepiness associated with
either narcolepsy, SWSD or OSAHS. In these studies, the product was generally
well tolerated, with the most common side effects being mild-to-moderate in
intensity and including nausea, headaches, dizziness, diarrhoea, decreased
appetite and upset stomach. The company submitted its NDA for Nuvigil, which is
protected by a US patent expiring in 2023 that claims the Form 1 polymorph of
armodafinil, to the FDA in March 2005 and received an initial approvable letter
in April 2006. Furthermore, Cephalon also plans to conduct clinical trials
evaluating the use of Nuvigil as a treatment for bipolar depression, cognition
associated with schizophrenia, and excessive sleepiness and fatigue in
conditions such as Parkinson's disease and cancer.
LOAD-DATE: April 2, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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Clinical Psychiatry News
April 2007
Try Inhibiting Serotonin to Return Executive Functioning
BYLINE: Damian Mcnamara, Miami Bureau
SECTION: Pg. 34 Vol. 35 No. 4 ISSN: 0270-6644
LENGTH: 686 words
ORLANDO - Alterations in brain circuitry and chemistry mediated through the
dorsolateral prefrontal cortex can cause executive dysfunction in multiple
disorders, according to a presentation at a psychopharmacology congress
sponsored by the Neuroscience Education Institute.
"Executive dysfunction is there. It hits you in the face if you are dealing
with schizophrenia," said Dr. Thomas L. Schwartz. "But in depression you may
have to look for it. I was always looking for that in the background-insomnia,
fatigue, and executive dysfunction-the key residual symptoms of depression
treatment."
Decreased metabolism in the dorsal and medial prefrontal cortex and the
anterior cingulate are neurobiologic factors that might contribute to executive
dysfunction in depression, Dr. Schwartz said. A decrease in N-acetyl aspartate,
a marker or neuronal function, also may play a role. "It's another way to look
at the brain, and in depressed folks you can show the brain is not doing what it
is supposed to," said Dr. Schwartz, director of the depression and anxiety
disorders research program at the State University of New York, Syracuse.
Executive dysfunction is associated with noradrenergic, dopaminergic, and
histaminergic projections to the dorsolateral prefrontal cortex. One tactic to
get more norepinephrine to flow in that circuitry is to manipulate the serotonin
levels, Dr. Schwartz said.
"Too much serotonin can be a bad thing in the frontal lobes. If you inhibit
the inhibitor you can get more norepinephrine up there and help return executive
functioning," he added.
Pharmacologic agents that might increase norepinephrine, dopamine, and/or
histamine and help improve executive function include drugs such as bupropion,
atomoxetine (Straterra), and modafinil (Provigil), and drug classes such as
stimulants and atypical antipsychotics, Dr. Schwartz said.
"Use of atomoxetine for executive dysfunction in depression makes biological
sense and circuitry sense," he said. "But there are no controlled studies [of
atomoxetine] in executive dysfunction in depression."
Executive dysfunction also is associated with sleep disorders. "Your brain
wants you to have a homeostatic amount of sleep. If you get sleep deprived, no
matter what the cause, you function poorly and make errors in omission and
commission," Dr. Schwartz said. Again, "there is poor metabolism in the
prefrontal cortex."
Addition of a sleep aid can have positive effects on next-day functioning.
Stimulants, modafinil, or armodafinil can improve attention and concentration
during the day, Dr. Schwartz said. "If you can keep people more awake during the
day, and they avoid napping, they may not need a sleeping pill at night."
Insomnia is comorbid with depression in around 85% of people (J. Clin.
Psychiatry 2004;65:27-32). "That is a lot of people," Dr. Schwartz said. Some
antidepressant medications can have a direct effect on sleep, he added. For
example, bupropion increases REM sleep and sleep latency, but reduces sleep
continuity. Trazodone decreases REM sleep time and may cause daytime sedation.
In contrast, nefazodone increases REM sleep time and is associated with minimal
daytime sedation.
Sleep aids are a treatment option. Examples include zolpidem (Ambien),
eszopiclone (Lunesta), and zaleplon (Sonata). "I don't think one is better than
the other, so choose based on half-life," Dr. Schwartz suggested. Sonata has the
shorter half life; Ambien is in the middle; Lunesta has the longest. "Which one
can you take at 3 a.m, if you need to work at 9 in the morning? Sonata."
Modafinil is another pharmacologic option in patients with executive
dysfunction and other adverse effects of impaired sleep. "This will not save
every one of your patients but you can try it," Dr. Schwartz said. "It's the
only product that raises histamine that I know of, and histamine going up to the
cortex is good for executive function."
Dr. Schwartz said, "Modafinil is a funny drug-doses above 300 mg backfire in
certain populations. Lower doses may be better for treatment of executive
dysfunction."
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2007 Elsevier Inc., International Medical News Group
All Rights Reserved
321 of 998 DOCUMENTS
PR Newswire US
March 30, 2007 Friday 8:51 PM GMT
Cephalon Provides Update Related to NUVIGIL(TM) New Drug Application
LENGTH: 1090 words
DATELINE: FRAZER, Pa. March 30
FRAZER, Pa., March 30 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
today announced that it has received an approvable letter, together with draft
labeling, from the U.S. Food and Drug Administration (FDA) for its new drug
application (NDA) for NUVIGIL(TM) (armodafinil) Tablets [C-IV] for the treatment
of excessive sleepiness associated with narcolepsy, obstructive sleep
apnea/hypopnea syndrome (OSAHS) and shift work sleep disorder (SWSD).
The draft labeling includes a proposed bolded warning section that characterizes
the potential occurrence of skin rash and hypersensitivity in patients taking
modafinil and armodafinil. As expected, the agency also has indicated that it
will request similar language in the label for PROVIGIL(R) (modafinil) Tablets
[C-IV]. The proposed labeling is subject to final approval by the FDA.
"We have worked diligently with the FDA over the past six months on this issue,
and they have now informed us that their review is complete. We are very pleased
that the proposed warning language appropriately describes the product's safety
profile," said Dr. Lesley Russell, Executive Vice President, Worldwide Medical
and Regulatory Operations.
Among other things, the agency has requested that the company provide a standard
safety update from clinical trials conducted since the last update in June 2006,
and introductory promotional materials to be used for the product. The company's
response will be submitted within 30 days and will be considered a Class I
response; the agency is expected to complete its review within 60 days
thereafter. The agency has not requested any additional studies prior to final
approval of NUVIGIL.
"While we fully appreciate that this regulatory review has been difficult and
lengthy for stockholders and others interested in the outcome, we are convinced
that in this unusual situation where multiple products may be affected, the
final result will prove to be worth the investment of time and effort," said
Frank Baldino Jr., Ph.D., Chairman and CEO of Cephalon.
About NUVIGIL
NUVIGIL is a single-isomer formulation of modafinil, the active pharmaceutical
ingredient contained in PROVIGIL which is FDA-approved for the treatment of
excessive sleepiness associated with narcolepsy, OSAHS and SWSD. The NUVIGIL NDA
is based on positive results of four double-blind, randomized,
placebo-controlled studies in patients with excessive sleepiness associated with
either narcolepsy, SWSD or OSAHS. In these studies, NUVIGIL was generally well
tolerated. The most common side effects were mild to moderate in intensity and
included nausea, headaches, dizziness, diarrhea, decreased appetite and upset
stomach.
The company submitted its NDA for NUVIGIL to FDA in March 2005 and received an
initial approvable letter in April 2006.
Cephalon also plans to conduct clinical trials evaluating the use of NUVIGIL as
a treatment for serious medical conditions such as bipolar depression, cognition
associated with schizophrenia, and excessive sleepiness and fatigue in
conditions such as Parkinson's disease and cancer.
NUVIGIL is protected by a U.S. patent expiring in 2023 that claims the Form 1
polymorph of armodafinil.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. Cephalon's U.S. headquarters are located in Frazer,
Pennsylvania, with offices, laboratories and manufacturing facilities in West
Chester, Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis,
Minnesota. Cephalon's European headquarters are located in Maisons-Alfort,
France.
The company currently markets six proprietary products in the United States:
PROVIGIL, FENTORA(R) (fentanyl buccal tablet) [C-II], ACTIQ(R) (oral
transmucosal fentanyl citrate) [C-II], GABITRIL(R) (tiagabine hydrochloride),
TRISENOX(R) (arsenic trioxide) injection, and VIVITROL(R) (naltrexone for
extended-release injectable suspension). Full prescribing information on its
U.S. products is available at http://www.cephalon.com/ or by calling
1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products, including future
clinical development plans for NUVIGIL; interpretation of clinical results,
particularly with respect to the NUVIGIL Phase 3 trials; prospects for
regulatory approval of NUVIGIL, including the likelihood of receiving final
approval from FDA and the characterization of serious skin rash, among other
things, in the final approved labeling for NUVIGIL; manufacturing development
and capabilities; market prospects for its products; sales and earnings
guidance; and other statements regarding matters that are not historical facts.
You may identify some of these forward-looking statements by the use of words in
the statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Jenifer Antonacci, +1-610-738-6674,
jantonac@cephalon.com ; Investors: Robert (Chip) Merritt, +1-610-738-6376,
cmerritt@cephalon.com , both of Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: March 31, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 PR Newswire Association LLC.
All Rights Reserved.
322 of 998 DOCUMENTS
US Fed News
March 12, 2007 Monday 2:44 AM EST
Indian Inventors Develop 2-[(Diphenylmethyl) Thio] Acetamide Preparation Process
BYLINE: US Fed News
LENGTH: 261 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., March 12 -- Surendra B. Bhatt, Jiten R. Patel, Dinesh
Panchasara, Hetal R. Shah, Keshav Deo and Vinod Kumar Kansal, all from Vadodara,
India, have developed a process for the preparation of 2-[(diphenylmethyl) thio]
acetamide.
According to the U.S. Patent & Trademark Office, the invention relates to a
"process for the preparation of 2-[(diphenylmethyl)thioacetamide, an
intermediate for the preparation of Modafinil which is a central nervous system
stimulant and used for the treatment of narcolepsia."
An abstract of the invention, released by the Patent Office, said: "The process
comprises reacting 2-[(diphenylmethyl)thio]acetic acid with alcohols, in
presence of catalytic amount of inorganic acid or organic acid at reflux
temperature of alcohol to obtain corresponding ester which is reacted with
ammonia to give 2-[(diphenylmethyl)thio]acetamide. If desired
2-[(diphenylmethyl)thioacetamide thus produced is reacted with hydrogen peroxide
to produce Modafinil."
The inventors were issued U.S. Patent No. 7,186,860 on March 6.
The patent has been assigned to Alembic Ltd., Gujarat, India.
The original application was filed on Jan. 30, 2004, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,186,860.PN.&OS=PN/7,186,860&RS=
PN/7,186,860.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com.
LOAD-DATE: March 13, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
323 of 998 DOCUMENTS
Australian Doctor
March 9, 2007
BYLINE: By Gabrielle Babbington
LENGTH: 257 words
PATIENTS with wet age-related macular degeneration are closer to having
affordable sight-saving treatment.
At their latest meeting, the Australian Drug Evaluation Committee approved
ranibizumab (Lucentis) intravitreal injection for registration.
A spokeswoman for the drug's manufacturer Novartis said the decision paved the
way for pursuing PBS listing of the drug.
Ranibizumab had been shown to improve sight in patients with wet age-related
macular degeneration - the leading cause of blindness in the elderly, she said.
The move to increase access to the drug would not necessarily increase its
availability because there were already 85 authorised prescribers registered
with the Therapeutic Goods Administration, which probably included all of
Australia's retinal specialists and a few ophthalmologists, she said.
The current supply arrangement still stood, whereby Novartis provided the drug
on physician request at an initial patient cost of $6000 for three treatments
and gratis thereafter, she said.
ADEC has also extended the indications for the wakefulness-promoting drug
modafinil (Modavigil).
The tablets were approved for patients with obstructive sleep apnoea who have
persisting excessive sleepiness, despite interventions such as lifestyle
measures and continuous positive airway pressure (CPAP).
Modafinil was also approved to treat moderate-to-severe chronic shiftwork sleep
disorder.
Associate Professor Ron Grunstein, head of the sleep research group at the
Woolcock Institute in Sydney, said Modafinil was not a substitute for sleep.
LOAD-DATE: March 8, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
JOURNAL-CODE: AD
Copyright 2007 Reed Business Information Ltd.
All Rights Reserved
324 of 998 DOCUMENTS
University Wire
March 8, 2007 Thursday
U. Kentucky study follows up on drug to aid smoking withdrawal
BYLINE: By Erica Mitchell, Kentucky Kernel; SOURCE: U. Kentucky
LENGTH: 471 words
DATELINE: LEXINGTON, Ky.
Galen Winthrow has a love-hate relationship with smoking.
"Smoking is a harsh mistress," said the philosophy and political science
sophomore. "One second she is the cure-all drug but when she leaves your system,
the anxiety, the stress, the shakes start."
Winthrow would like to quit but more factors than nicotine play a role.
"I'd love to quit, but withdrawal can be excruciating," Winthrow said. "If you
have papers, tests, a job or anything else you need to do, it can drive you
insane."
But a new pill may help ease the side effects of giving up cigarettes.
UK is looking for participants for a follow-up study on modafinil, a drug that
may help alleviate nicotine cravings, concentration problems, hunger and weight
gain -- all symptoms that make giving up nicotine difficult for smokers, said
Dr. Catherine Martin.
Martin, the principle investigator in the study being conducted by the
Psychiatry Research Center, said the drug was originally used to treat excessive
sleepiness associated with narcolepsy, obstructive sleep apnea-hypopnea syndrome
and shift work sleep disorder.
"Modafinil is a promising medication for helping with addiction," Martin said.
"It may help with nicotine withdrawal symptoms and it may help with some
predisposing symptoms that contribute to people starting and continuing to
smoke."
Participants in the trial will be randomly assigned to receive either modafinil
or a placebo. Investigators will monitor participants for changes in behavior
for 13 days out of a 20-week period.
The study is a double-blind placebo controlled trial, where neither the
participants nor the investigators know who receives the actual drug, which is
designed to reduce bias and self-deception.
The Department of Psychiatry has already tested modafinil on smokers in two
human laboratory studies. Afterward, researchers concluded that modafinil and
nicotine are safe to use together. The studies also showed smokers had decreased
cravings, hunger and improved concentration on days when they took modafinil,
Martin said.
The new study is a larger clinical follow up to the previous one.
Smoking increases the risk of lung cancer, heart disease and chronic obstructive
pulmonary disease (emphysema) among other things. About 28.7 percent of adults
in Kentucky smoke and more than 8,000 people in Kentucky die of tobacco-related
illnesses each year, according to the Kentucky Cabinet for Health and Family
Services.
But the health benefits of quitting don't make it any easier for many.
"Stopping smoking is one of the most difficult challenges smokers face," Martin
said. "We think modafinil may help smokers stop smoking."
Daily smokers between the ages of 18 and 45, in good health and interested in
participating in the study can call (859) 257-9341 or (859) 230-3220 for more
information.
(C) 2007 Kentucky Kernel via U-WIRE
LOAD-DATE: March 8, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 Kentucky Kernel via U-Wire
325 of 998 DOCUMENTS
University Wire
March 7, 2007 Wednesday
U. Kentucky study follows up on drug to aid smoking withdrawal
BYLINE: By Erica Mitchell, Kentucky Kernel; SOURCE: U. Kentucky
LENGTH: 450 words
DATELINE: LEXINGTON, Ky.
Galen Winthrow has a love-hate relationship with smoking.
"Smoking is a harsh mistress," said the philosophy and political science
sophomore at the University of Kentucky. "One second she is the cure-all drug,
but when she leaves your system, the anxiety, the stress, the shakes start."
Winthrow would like to quit, but more factors than nicotine play a role.
"I'd love to quit, but withdrawal can be excruciating," Winthrow said. "If you
have papers, tests, a job or anything else you need to do, it can drive you
insane."
But a new pill may help ease the side effects of giving up cigarettes.
The University is looking for participants for a follow-up study on modafinil, a
drug that may help alleviate nicotine cravings, concentration problems, hunger
and weight gain -- all symptoms that make giving up nicotine difficult for
smokers, said Dr. Catherine Martin.
Martin, the principle investigator in the study being conducted by the
Psychiatry Research Center, said the drug was originally used to treat excessive
sleepiness associated with narcolepsy, obstructive sleep apnea-hypopnea syndrome
and shift work sleep disorder.
"Modafinil is a promising medication for helping with addiction," Martin said.
"It may help with nicotine withdrawal symptoms and it may help with some
predisposing symptoms that contribute to people starting and continuing to
smoke."
Participants in the trial will be randomly assigned to receive either modafinil
or a placebo. Investigators will monitor participants for changes in behavior
for 13 days out of a 20-week period.
The study is a double-blind placebo controlled trial, where neither the
participants nor the investigators know who receives the actual drug, which is
designed to reduce bias and self-deception.
The Department of Psychiatry has already tested modafinil on smokers in two
human laboratory studies. Afterward, researchers concluded that modafinil and
nicotine are safe to use together. The studies also showed smokers had decreased
cravings, hunger and improved concentration on days when they took modafinil,
Martin said.
The new study is a larger clinical follow up to the previous one.
Smoking increases the risk of lung cancer, heart disease and chronic obstructive
pulmonary disease (emphysema) among other things. About 28.7 percent of adults
in Kentucky smoke and more than 8,000 people in Kentucky die of tobacco related
illnesses each year, according to the Kentucky Cabinet for Health and Family
Services.
But the health benefits of quitting don't make it any easier for many.
"Stopping smoking is one of the most difficult challenges smokers face," Martin
said. "We think modafinil may help smokers stop smoking."
(C) 2007 Kentucky Kernel via U-WIRE
LOAD-DATE: March 7, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 Kentucky Kernel via U-Wire
326 of 998 DOCUMENTS
Charleston Gazette (West Virginia)
March 4, 2007, Sunday
Competitor paid off Mylan, suit alleges
BYLINE: Paul J. Nyden
SECTION: NEWS; Pg. P1B
LENGTH: 1014 words
pjnyden@wvgazette.com
A lawsuit charges that Mylan Laboratories Inc. was one of four generic-drug
companies paid off by a brand-name drug company to delay marketing cheaper
versions of a sleep-disorder pill.
The Prescription Action Litigation Project, a consumer coalition, filed the suit
against Cephalon Inc., maker of Provigil, which treats sleep disorders.
The suit, filed in federal court in October, alleges Frazier, Pa.-based Cephalon
paid $136 million to Mylan and three other generic pharmaceutical companies so
they would hold off on marketing generic Provigil until 2011 or 2012.
Generic drugs, the suit states, typically cost 30 percent less than brand drugs
with a single generic competitor. Generic drugs cost between 50 percent and 80
percent less when there are multiple generic competitors on the market.
Mylan is based in Canonsburg, Pa., and was founded in White Sulphur Springs. Its
biggest production facility is in Morgantown.
The three other generic companies accused in the suit are: Barr Laboratories of
Pomona, N.Y.; Ranbaxy Laboratories, based in New Dehli, India, with offices in
Princeton, N.J.; and Teva Pharmaceutical Industries, based in Petach Tikva,
Israel, with offices in North Wales, Pa.
Cephalon and those four companies are all defendants in the lawsuit. The
plaintiffs include: Vista Healthplan Inc., a Florida health-benefits provider;
the Pennsylvania Turnpike Commission, which pays medical benefits for more than
2,000 employees; and the Pennsylvania Employees Benefit Trust Fund, which
provides health coverage to more than 270,000 beneficiaries.
The U.S. Food and Drug Administration originally approved Provigil in December
1998, giving Cephalon exclusive marketing rights for five years.
Then, in December 2002, a year before those marketing rights expired, each of
the four generic drug makers filed applications with the FDA to market modafinil
, the generic name of Provigil.
Modafinil counters narcolepsy, a rare sleep disorder making it difficult for
people to get up in the morning and stay awake during the day. Provigil is also
prescribed to treat fatigue, depression, sleepiness and attention-deficit
disorders.
The lawsuit focuses on "Cephalon's illegal conduct" that allegedly increased the
costs for modafinil by discouraging competitors from "marketing generic versions
of Provigil."
Provigil sales increased from $417 million in 2004 to $588 million in 2005,
according to a related lawsuit by Apotex Inc., a drug manufacturer based in
Weston, Ontario.
Prices for prescription drugs have recently been rising at rates between 14
percent and 18 percent a year, the lawsuit states.
The pharmaceutical industry, the lawsuit adds, "is one of the most profitable
industries in the United States. The U.S. market accounts for more than 40
percent of the world's prescription pharmaceutical revenues."
Both suits are pending in the U.S. District Court for the Eastern District of
Pennsylvania in Philadelphia.
The Prescription Action Litigation Project, based in Boston, is a coalition of
more than 125 organizations in 36 states and Washington, D.C., including
consumer, senior, health care, labor and women's health groups. The West
Virginia Citizen Action Group is a member.
The suit is one of 26 class actions Prescription Action has filed seeking to
lower prices of pharmaceutical drugs. Settlements in four suits have allowed
consumers to collect money they were overcharged.
Telephone calls to Mylan's offices on Thursday and Friday were not returned.
The lawsuit alleges the goal of "Cephalon's scheme was to prevent, delay and/or
minimize the success of the entry of generic modafinil competitors which would
have sold ... at prices significantly below [Cephalon's] prices for Provigil."
Alex Sugerman-Brozan, Prescription Action's director, said the lawsuit's
allegations are "very timely" because of new federal legislation.
Last week, the Senate Judiciary Committee unanimously approved a bill called the
Preserve Access to Affordable Generics Act, sending it to the full Senate for
its consideration.
The bill's supporters include: Sens. Herb Kohl and Russ Feingold, both D-Wis.;
Charles Grassley, R-Iowa; Patrick Leahy, D-Vermont; Ted Kennedy, D-Mass.; and
Charles Schumer, D-N.Y.
"That bill would ban lawsuit settlement agreements that keep generics from being
available to people," Sugerman-Brozan said during a telephone interview from his
offices in Boston on Friday.
"Pharmaceutical companies usually have 10 or 12 years without any competition
for a new drug. But other drug companies can challenge the uniqueness of a
patent and say they should be able to market a generic alternative.
"The original manufacturer can then sue [generic drug companies] for patent
infringement. Typically, the brand-name company then gets a 30-month extension
of its patent. For a blockbuster drug that earns billions of dollars, that is a
lot of extra sales.
"So brand-name companies are often willing to settle lawsuits with generic
companies by paying them. 'We will give you millions if you delay the entry of
your drug into the marketplace.'"
Sugerman-Brozan said the practice of paying competitors to delay selling
generics, under "reverse payment settlements," is becoming more common.
"When companies conspire to keep drugs away from citizens who need them to
maintain their health, they should be called on the carpet," said Gary Zuckett,
director of the West Virginia Citizen Action Group. "There is supposed to be a
free market. If drug companies conspire to keep prices artificially high, that
is unfair to the individual consumer."
Such action affects West Virginia in that it pays for prescription drugs for
Public Employee Insurance Agency beneficiaries and for Medicare and Medicaid
patients, Zuckett said. "This hurts everybody. ... Drug prices should not be
fixed behind closed doors."
Sugerman-Brozan said: "Pharmaceutical companies make products vital to people's
health and well-being. Their products can be lifesaving. They should not put
medications beyond people's reach."
To contact staff writer Paul J. Nyden, use e-mail or call 348-5164.
LOAD-DATE: March 5, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2007 Charleston Newspapers
327 of 998 DOCUMENTS
US States News
February 28, 2007 Wednesday 5:59 AM EST
STUDY TO FURTHER INVESTIGATE MODAFINIL AS SMOKING CESSATION AID
BYLINE: US States News
LENGTH: 213 words
DATELINE: LEXINGTON, Ky.
The University of Kentucky issued the following news release:
Most cigarette smokers trying to quit often fail because of nicotine cravings,
increased appetite and weight gain, and problems with inattention. Researchers
at the University of Kentucky have studied the difficulties associated with
trying to quit smoking. In a laboratory setting, smokers underwent multiple
measures of performance on tasks and feelings after not smoking for 24 hours.
All smokers received modafinil and a placebo on different laboratory days.
Researchers discovered that smokers had decreased cravings, hunger, and improved
attention span on days when they took modafinil as compared to laboratory days
when they received only a placebo. Because increases in cigarette cravings and
hunger and the associated weight gain are major factors in smokers relapsing,
this study suggests that modafinil may help smokers quit. A new study at the
University of Kentucky will further investigate modafinil as a smoking cessation
aid. If you are a daily smoker between the ages of 18 and 45, in generally good
health, and would like to stop smoking, you might qualify to be part of this
research study. For more information, please call (859) 257-9341 or (859)
230-3220.
Contact: Melanie Jackson, 859/323-6363.
LOAD-DATE: June 11, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2007 HT Media Ltd.
All Rights Reserved
328 of 998 DOCUMENTS
The Sunday Times (London)
December 17, 2006
MoD tests drugs for 'supertroops'
BYLINE: Jonathan Leake
SECTION: HOME NEWS; News; Pg. 7
LENGTH: 338 words
THE Ministry of Defence has been testing controversial drugs aimed at making
military personnel stronger, faster-thinking and quicker at recovering from
fatigue, writes Jonathan Leake.
The drugs -some banned from Olympic sports -range from modafinil, which raises
the IQ, to creatine, used by bodybuilders.
Defence scientists have also been experimenting with prescription sedatives like
temazepam and diazepam, aimed at helping soldiers get vital sleep between bouts
of combat. And they have looked at pemoline, a drug designed to help children
concentrate.
Details of the experiments emerged after a researcher from Qinetiq, one of the
contractors doing the testing, was asked to give evidence to MPs. "There is a
lot of research funded by the MoD into substances like modafinil, ephedrine,
those types of things," Anna Casey told a select committee investigating drug
misuse in sport. "It does not mean such substances are being used
(operationally) but it does mean they are keeping an open mind."
The research is linked to a £ 20m MoD programme to find novel ways to improve
the performance of soldiers.
Besides Qinetiq, the money is being given to six universities -Nottingham,
Loughborough, Birmingham, Cardiff, Glasgow and Cranfield School of Management -
and a dozen firms that specialise in boosting human performance.
This weekend the MoD released a list of the substances it has been researching,
including dichloroacetate and ubiquinone, thought to reduce fatigue and aid
recovery, and ephedrine, a stimulant.
A US military study has shown combat stress can hit soldiers' performance. After
a week of combat exercises they performed worse than if they were drunk or
sedated.
But there are risks. The practice of offering US aircrew amphetamines was
criticised after two F-16 pilots bombed a Canadian unit in Afghanistan in 2002,
killing four soldiers.
Colonel Bob Stewart, who served in Bosnia in the early 1990s, said such drugs
could assist troops. "When you have to stay awake for a long time they could be
a great help."
LOAD-DATE: December 17, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 Times Newspapers Limited
All Rights Reserved
329 of 998 DOCUMENTS
University Wire
December 14, 2006 Thursday
Modafinil may be as bad as amphetamine relatives
BYLINE: By Ben Dedman, The Guilfordian; SOURCE: Guilford College
SECTION: COLUMN
LENGTH: 723 words
DATELINE: GREENSBORO, N.C.
According to a 2005 survey published by America's Office of National Drug
Control Policy, 13.8 percent of Americans older than 12, or 33.7 million people,
had tried cocaine at some point in their life.
Of these, 8.8% of college students have tried it in their lives and 5.7% have
tried it in the last year.
However, as pressure levels rise with the upcoming exam week, cocaine is
certainly not the most prominent, or even the most dangerous drug in student
circles. Many students are ready to "taste the rainbow" in an attempt to stay
awake and alert, eating a kaleidoscope of yellow, blue, white, and yellow pills
as if they were Skittles.
Amphetamines, including Ritalin, Adderall, Conserta, and Focalin, are much
easier for most college students to find than cocaine, and the negative stigmas
attached to cocaine often don't carry over. This creates an increased likelihood
to abuse the pills, leading to harmful side effects and addiction. But, with the
increased availability of a relatively new "superdrug," amphetamines may not be
the biggest danger.
Modafinil, also known as Provigil, was released by the drug company Cephalon in
1998 to treat narcolepsy, a sleep disorder, and was re-released as generics by
competing companies earlier this year, making it cheaper and perhaps even more
accessible.
Though it is not an amphetamine, Modafinil has many similar effects. A single
dose can sustain wakefulness and alertness for up to forty-eight hours and,
unlike amphetamines, when you finally go to sleep you can become fully rested in
only six hours, not the eight usually required to catch up. And, perhaps most
appealing to college students, if taken just before bed, eight hours of restful
sleep can be crammed into half the time.
Modafinil is supposedly non-addictive and, according to the National Institute
on Drug Abuse, it can even help to kick a cocaine addiction. According to the
study, "More than twice as many Modafinil patients as placebo patients (33
percent compared with 13 percent) were able to attain abstinence [from cocaine]
for 3 weeks or more."
Militaries, including those in France, the United Kingdom, and the United States
have researched the drug, perhaps looking to replace amphetamines they have used
in the past. According to one study of helicopter pilots, three doses, 600 mg
total, might be able keep pilots alert over a span of 88 hours with only eight
hours of sleep.
In the past, the U.S. military has used amphetamines to keep pilots alert on
long missions. According to ABC news, on April 17, 2002 American pilots
complaining of fatigue before a mission were advised to take amphetamines before
a mission in Afghanistan. During the mission, the American pilots bombed
Canadian infantry participating in a live-fire training exercise, killing four
Canadian soldiers and wounding eight.
Modafinil could potentially offer a way to stop many of the negative effects of
amphetamines, while substantially increasing the benefits. But, the pill should
still not be taken lightly because and if even more stigmas are removed from
Modafinil the results could be disastrous.
According to an estimate in Adrugrecall.com, at least 40 million Americans have
been prescribed amphetamines since 1996. Modafinil is less likely to be
prescribed, making it less accessible to students either legally or illegally,
but as is the case with most drugs, if there is a will to find it then there is
a way.
Amphetamines are more popular than candy to college students - even health food
fanatics won't even think before knocking a couple back. And now, with the
stigma of addiction and the juiced-up buzz gone, Modafinil has the potential to
become even more popular. Maybe, instead of drowning your drowsiness with pills,
you should reconsider those classic remedies, caffeine and a Snickers bar, as
safer remedies on those long nights of studying.
David Poltz, writing for Slate.com, experimented with Modafinil to help him
crunch for a deadline. Writing about his first day on the drug, Poltz said,
"Today I am my own Superman, dosed on 100 milligrams of Modafinil." Though he
loved the drug's short term effects, an unexpected addiction kicks in and he
later says, "I end my experiment after two days. I am acting like a lunatic."
That's just what we all need - even more lunatics at Guilford.
(C) 2006 The Guilfordian via U-WIRE
LOAD-DATE: December 14, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 The Guilfordian via U-Wire
330 of 998 DOCUMENTS
FDAnews Drug Pipeline Alert
December 11, 2006 Monday
CEPHALON WORKING WITH FDA TO FINALIZE NUVIGIL LABELING
SECTION: Vol. 3 No. 492
LENGTH: 191 words
Cephalon has provided an update on the status of its new drug application (NDA)
for Nuvigil (armodafinil). The company announced that the FDA said it is
continuing to evaluate the single case of serious rash reported in a clinical
study of Sparlon (modafinil). The agency has requested additional information to
help place this isolated case in the context of the safety profile of modafinil.
The FDA has not requested any additional information related to Nuvigil and is
working with the company to finalize the product's label.
Nuvigil is a single-isomer formulation of modafinil. The Nuvigil NDA is based on
positive results of four double-blind, randomized, placebo-controlled studies in
patients with excessive sleepiness. In these studies, Nuvigil was generally
well-tolerated.
In May the company announced that it had received an approvable letter from the
FDA for the NDA requesting approval of Nuvigil for the treatment of excessive
sleepiness associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome
and shift work sleep disorder. FDA approval of Nuvigil is contingent upon
finalizing the product label.
Release date: Dec. 11, 2006
LOAD-DATE: December 8, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 Washington Business Information, Inc.
All Rights Reserved
331 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
December 8, 2006
Cephalon provides update on final Nuvigil labelling
LENGTH: 338 words
The Division of Neurology Products of the FDA has informed Cephalon that it is
continuing to evaluate the single case of serious rash reported in a clinical
study of Sparlon ( modafinil ) Tablets [C-IV]. The Division has requested
additional information to help place this isolated case in the context of the
safety profile for modafinil, but has not requested any additional information
related to Nuvigil (armodafinil) Tablets, and is working with the company to
finalise the product's label. Cephalon has held discussions with the FDA
concerning this case. The company is in the process of collecting the requested
information and expects to make the submission to the Agency within the next few
weeks.
However, the submission may be considered a major amendment and result in an
extension of the 31st December PDUFA date. In May, Cephalon reported that it had
received an approvable letter from the FDA for the NDA requesting approval of
Nuvigil for the treatment of excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSA/HS) and shift work sleep disorder
(SWSD). FDA approval of Nuvigil is contingent upon finalising the product label.
Nuvigil is a single-isomer formulation of modafinil, the active pharmaceutical
ingredient contained in Provigil . It is protected by a composition of matter
patent that will expire on 18th December 2023 and covers a novel polymorphic
form of armodafinil. The Nuvigil NDA is based on positive results of four
double-blind, randomised, placebo-controlled studies in patients with excessive
sleepiness associated with either narcolepsy, SWSD or OSA/HS. In these studies,
Nuvigil was generally well tolerated, with a safety profile consistent with that
observed in studies of Provigil. The most common adverse effects observed
included headache, nausea, dizziness, insomnia and anxiety. In 2007, the company
expects to initiate new clinical programmes with Nuvigil in fatigue and
cognition, with the longer-term objective of expanding the product's label.
LOAD-DATE: December 8, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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332 of 998 DOCUMENTS
Global Insight
December 8, 2006
Cephalon Says that FDA Decision on Approving Nuvigil May Be Delayed
BYLINE: Dr Jonathan Goodall
SECTION: In Brief
LENGTH: 354 words
The U.S. FDA has requested additional information on Sparlon (modafinil), as
part of its ongoing assessment of Cephalon s experimental attention deficit
disorder drug, the company announced yesterday. This is to help the agency place
a single case of serious rash observed in the clinical programme for this drug
in the context of the safety profile of the modafinil molecule, the company
explained. The FDA has not requested any additional information on the marketing
application for Nuvigil (armodafinil), which is Cephalon s follow-up to its
flagship narcolepsy treatment Provigil. However, the company acknowledged that
because the active ingredient in Nuvigil is closely related to modafinil, the
submission of this additional material may be considered a major amendment to
Nuvigil's application. As a result, the company warned that this request may
delay the FDA's action on Nuvigil beyond its current 31 December PDUFA date (see
United States: 10 August 2006: ).
Significance: In May, Cephalon received an FDA approvable letter regarding its
new drug application (NDA) for Nuvigil as a treatment of excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome and shift
work sleep disorder. Final approval for the drug is contingent on the company
finalising the product labelling. With respect to this, Cephalon officials
remain upbeat about the potential delay that the additional information request
may impose on Nuvigil's approval. Robert Grupp, a spokesperson for Cephalon,
told Bloomberg that the company was "delighted that the agency is taking time to
ask about that single case", adding that it would allow safety information to be
reflected in the label. In part, this relaxed approach may be down to the
company's confidence that, at the lower doses used in Nuvigil compared to
Sparlon, modafinil and its related molecules have a proven safety track record.
The company s confidence might also come from the fact that the risk that
generic competition poses to Nuvigil's predecessor, Provigil, has considerably
eased over the last year (see United States: 12 December 2005:).
LOAD-DATE: December 8, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2006 World Markets Research Limited
All Rights Reserved
333 of 998 DOCUMENTS
M2 Presswire
December 7, 2006
WorldTradeStocks.com: Cephalon Says FDA Continues To Evaluate Rash Case Of
Sparlon Study; Nuvigil Pending For Label Finalization [NASDAQ:CEPH]
LENGTH: 1013 words
M2 PRESSWIRE-DECEMBER 7, 2006-WorldTradeStocks.com: Cephalon Says FDA Continues
To Evaluate Rash Case Of Sparlon Study; Nuvigil Pending For Label Finalization
[NASDAQ:CEPH] ©1994-2006 M2 COMMUNICATIONS LTD
NEW YORK, WORLDTRADESTOCKS.COM -On Thursday, Cephalon, Inc. (NASDAQ:CEPH), a
pharmaceutical company, revealed that the Division of Neurology Products of the
U.S. Food and Drug Administration continues to evaluate a case of serious rash
reported in a Sparlon - modafinil tablets clinical study. The FDA had also asked
for additional information on Sparlon relative to its safety profile established
over a period of time.
The Frazer, Pennsylvania based company said the U.S. Food and Drug
Administration is working with the company to finalize the label for Nuvigil -
armodafinil. Nuvigil is indicated in the treatment of excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome and shift
work sleep disorder. Cephalon said the FDA's approvable letter relating to
Nuvigil is contingent upon finalizing the product label. The company clarified
the 2007 sales and earnings guidance announced earlier would remain in effect,
notwithstanding any delay in the PDUFA date that may result from this
submission. The company expects to initiate in 2007 new clinical programs with
Nuvigil related to fatigue and cognition, with the longer-term objective of
expanding Nuvigil's label. [NASDAQ:CEPH]
Dr. Lesley Russell, Executive Vice President, Worldwide Medical and Regulatory
Operations, Cephalon, said, "We are pleased that the agency continues to work
with us and outside experts in trying to better understand this case in the
context of modafinil's generally benign side effect profile. Although this
submission may be considered a major amendment and result in an extension of the
December 31, 2006 PDUFA date, we see this as an important opportunity to ensure
that the final label for NUVIGIL reflects the actual medical condition of this
child."
Cephalon said it was in the process of accumulating information on Sparlon as
requested by the FDA and was likely to make forward the same within the next few
weeks.
About Cephalon, Inc
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. U.S. sites include the company's headquarters in Frazer, Pa.,
and offices, laboratories or manufacturing facilities in West Chester, Pa., Salt
Lake City, and suburban Minneapolis. Cephalon's European headquarters are
located in Maisons-Alfort, France.
The company currently markets six proprietary products in the United States:
PROVIGIL(R) (modafinil) Tablets [C-IV], FENTORA(TM) (fentanyl buccal tablet)
[C-II], ACTIQ(R) (oral transmucosal fentanyl citrate) [C-II], GABITRIL(R)
(tiagabine hydrochloride), TRISENOX(R) (arsenic trioxide) injection, and
VIVITROL(R) (naltrexone for extended-release injectable suspension). Full
prescribing information on its U.S. products is available at
http://www.cephalon.com or by calling 1-800-896-5855.
About WorldTradestocks.com
WorldTradestocks.com an infomation research company , provides stock market
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investing
This release contains "forward-looking statements" within the meaning of Section
27A of the Securities Act of 1933, as amended, and Section 21E the Securities
Exchange Act of 1934, as amended and such forward-looking statements are made
pursuant to the safe harbor provisions of the Private Securities Litigation
Reform Act of 1995. "Forward-looking statements" describe future expectations,
plans, results, or strategies and are generally preceded by words such as "may",
"future", "plan" or "planned", "will" or "should", "expected," "anticipates",
"draft", "eventually" or "projected". You are cautioned that such statements are
subject to a multitude of risks and uncertainties that could cause future
circumstances, events, or results to differ materially from those projected in
the forward-looking statements, including the risks that actual results may
differ materially from those projected in the forward-looking statements as a
result of various factors, and other risks identified in a companies' annual
report on Form 10-K or 10-KSB and other filings made by such company with the
Securities and Exchange Commission.
CONTACT: J Rubiano, Infomation Specialist e-mail: info@worldtradestocks.com
(M2 Communications Ltd disclaims all liability for information provided within
M2 PressWIRE. Data supplied by named party/parties. Further information on M2
PressWIRE can be obtained at http://www.presswire.net on the world wide web.
Inquiries to info@m2.com).
LOAD-DATE: December 7, 2006
LANGUAGE: ENGLISH
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334 of 998 DOCUMENTS
Pharma Marketletter
December 7, 2006 Thursday
Cephalon updates on final Nuvigil labeling
LENGTH: 229 words
Cephalon says that the Division of Neurology Products of the US Food and Drug
Administration has informed the company that it is continuing to evaluate the
single case of serious rash reported in a child taking part in a Sparlon (
modafinil) tablets [C-IV] clinical study.
The Division has requested additional information to help place this isolated
case in the context of the safety profile for modafinil that has been
established over more than a decade of commercial use. It has not requested any
additional information related to Nuvigil (armodafinil) tablets and is working
with the company to finalize the product's label.
Lesley Russell, Cephalon's executive vice president, worldwide medical and
regulatory operations, said: "although this submission may be considered a major
amendment and result in an extension of the December 31, 2006, PDUFA
[Prescription Drug User Fee Act] date, we see this as an important opportunity
to ensure that the final label for Nuvigil reflects the actual medical condition
of this child."
On May 1, the company said it had received an approvable letter from the FDA for
the New Drug Application requesting approval of Nuvigil for the treatment of
excessive sleepiness associated with narcolepsy, obstructive sleep
apnea/hypopnea syndrome and shift work sleep disorder. FDA approval of the drug
is contingent on finalizing the product label.
LOAD-DATE: December 7, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 Marketletter Publications Ltd.
All Rights Reserved
335 of 998 DOCUMENTS
PR Newswire US
December 7, 2006 Thursday 1:00 PM GMT
Cephalon Provides Update Related to Final NUVIGIL(TM) Labeling
LENGTH: 1060 words
DATELINE: FRAZER, Pa. Dec. 7
FRAZER, Pa., Dec. 7 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that the Division of Neurology Products of the U.S. Food and
Drug Administration (FDA) has informed the company that it is continuing to
evaluate the single case of serious rash reported in a SPARLON(TM) (modafinil)
Tablets [C-IV] clinical study. The division has requested additional
information to help place this isolated case in the context of the safety
profile for modafinil that has been established over more than a decade of
commercial use. The division has not requested any additional information
related to NUVIGIL (armodafinil) Tablets and is working with the company to
finalize the product's label.
"We are pleased that the agency continues to work with us and outside experts in
trying to better understand this case in the context of modafinil's generally
benign side effect profile," said Dr. Lesley Russell, Executive Vice President,
Worldwide Medical and Regulatory Operations. "Although this submission may be
considered a major amendment and result in an extension of the December 31, 2006
PDUFA date, we see this as an important opportunity to ensure that the final
label for NUVIGIL reflects the actual medical condition of this child."
As the company disclosed in its November 2, 2006 earnings conference call, it
has had discussions with the FDA concerning this case. The company is in the
process of collecting the requested information and expects to make the
submission to the FDA within the next few weeks. On May 1, 2006, the company
announced that it had received an approvable letter from the FDA for the NDA
requesting approval of NUVIGIL for the treatment of excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome (OSA/HS)
and shift work sleep disorder (SWSD). FDA approval of NUVIGIL is contingent
upon finalizing the product label.
The company's previously issued 2007 sales and earnings guidance will remain in
effect, notwithstanding any delay in the PDUFA date that may result from this
submission. As previously disclosed, the company expects to initiate in 2007
new clinical programs with NUVIGIL in fatigue and cognition, with the
longer-term objective of expanding NUVIGIL's label.
About NUVIGIL
NUVIGIL is a single-isomer formulation of modafinil, the active pharmaceutical
ingredient contained in PROVIGIL. The NUVIGIL NDA is based on positive results
of four double-blind, randomized, placebo-controlled studies in patients with
excessive sleepiness associated with either narcolepsy, SWSD or OSA/HS. In
these studies, NUVIGIL was generally well tolerated, with a safety profile
consistent with that observed in studies of PROVIGIL. The most common adverse
effects observed included headache, nausea, dizziness, insomnia and anxiety.
NUVIGIL is protected by a composition of matter patent that will expire on
December 18, 2023 and covers a novel polymorphic form of armodafinil, the active
pharmaceutical ingredient in NUVIGIL.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. U.S. sites include the company's headquarters in Frazer,
Pa., and offices, laboratories or manufacturing facilities in West Chester, Pa.,
Salt Lake City, and suburban Minneapolis. Cephalon's European headquarters are
located in Maisons-Alfort, France.
The company currently markets six proprietary products in the United States:
PROVIGIL(R) (modafinil) Tablets [C-IV], FENTORA(TM) (fentanyl buccal tablet)
[C-II], ACTIQ(R) (oral transmucosal fentanyl citrate) [C-II], GABITRIL(R)
(tiagabine hydrochloride), TRISENOX(R) (arsenic trioxide) injection, and
VIVITROL(R) (naltrexone for extended-release injectable suspension). Full
prescribing information on its U.S. products is available at
http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results; prospects for regulatory approval, including the timing of the
submission of additional data to FDA, the possibility of a delay in the NUVIGIL
PDUFA action date and the likelihood that the final label for NUVIGIL reflects
the actual medical condition of the single case of serious rash seen in the
SPARLON clinical trials; manufacturing development and capabilities; market
prospects for its products; sales and earnings guidance; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
CONTACT: Media: Robert W. Grupp, +1-610-738-6402, rgrupp@cephalon.com ,
or Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com ,
both of Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: December 8, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
336 of 998 DOCUMENTS
Reuters Health Medical News
November 16, 2006 Thursday 9:00 PM EST
Modafinil counteracts adverse effects of sleep deprivation
SECTION: CLINICAL
LENGTH: 296 words
DATELINE: NEW YORK (Reuters Health) The non
amphetamine, wake-promoting drug, modafinil counters the adverse effects of
sleep deprivation on working memory, researchers report in the November 1st
issue of Sleep.
In a randomized, double-blind study, Dr. Robert Joseph Thomas, of Beth Israel
Deaconess Medical Center, Boston, and Dr. Kenneth K. Kwong of Massachusetts
General Hospital, Charlestown examined the effect of modafinil on working memory
and brain activation in the executive network following overnight sleep
deprivation.
Functional magnetic resonance imaging was used to assess the functional
neurobiology of executive function in eight sleep-deprived medication-free men
(ages 21 to 35 years) treated with 200 mg of modafinil or placebo. They
underwent a verbal working-memory task with 3 levels of difficulty.
Subjects in the sleep-deprived condition, had approximately 28 hours of
continuous wakefulness, and in the rested condition, had 8 hours of scheduled
sleep opportunity. The team assessed brain activation patterns and regional
signal intensity based on the blood-oxygen level-dependent signal.
Modafinil effectively countered the ill effects of sleep deprivation on working
memory, but only when the task difficulty was moderate, according to the
researchers.
"Effects when sleep deprived are clearly task load dependent," Dr. Thomas said
in an interview with Reuters Health. "When the task is easy, it offers no
benefit." However, "the moderate levels of task difficulty, typical of what we
face in real-life conditions, seem best enhanced neurobiologically."
The most obvious use of the agent, he continued, would be in "those on extended
duty hours due to unexpected circumstances." Moreover, he concluded that the
results "support military use, where sleep deprivation is rampant in combat."
LOAD-DATE: March 4, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Reuters Health
All Rights Reserved
337 of 998 DOCUMENTS
US Fed News
November 9, 2006 Thursday 3:51 AM EST
French Inventors Develop Crystalline Forms Production Method
BYLINE: US Fed News
LENGTH: 221 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Nov. 9 -- Olivier Neckebrock of Ponteau Combault, France, and
Pierre Leproust of Creteil, France, have developed a method for the production
of crystalline forms and crystalline forms of optical enantiomers of modafinil.
According to the U.S. Patent & Trademark Office: "The invention relates to a
process for the preparation of crystalline forms of the optical enantiomers of
modafinil, comprising stages comprising: dissolving one of the optical
enantiomers of modafinil in a solvent other than ethanol, crystallising the
modafinil enantiomer, recovering the crystalline form of the modafinil
enantiomer so obtained. The invention also relates to a process for the
preparation of the optical enantiomers of modafinil."
The inventors were issued U.S. Patent No. 7,132,570 on Nov. 7.
The patent has been assigned to Cephalon France, Maisons-Alfort Cedex, France.
The original application was filed on Dec. 18, 2003, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,132,570.PN.&OS=PN/7,132,570&RS=
PN/7,132,570.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com.
LOAD-DATE: November 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 HT Media Ltd.
All Rights Reserved
338 of 998 DOCUMENTS
Hindustan Times
November 2, 2006 Thursday 2:02 PM EST
Exercise is still the best fatigue buster
BYLINE: Report from the Asian News International brought to you by the Hindustan
Times
LENGTH: 301 words
DATELINE: Washington
Washington, Nov 2 -- The time has come to flush all those energy drinks down the
loo, for a new study by researchers at the University of Georgia has found that
nothing is as effective as boosting energy levels, and reducing fatigue, as
regular exercise.
As a part of the study, professor Patrick O'Connor, co-director of the UGA
exercise psychology laboratory, kinesiology professor Rod Dishman and lead
author Tim Puetz analyzed 70 randomized, controlled trials that enrolled a total
of 6,807 subjects.
The researchers quantified the magnitude of the effect of exercise and found
that it was stronger than the treatment of fatigued people with drugs such as
the narcolepsy drug modafinil.
They found that exercise increased energy and reduced fatigue by 0.37 standard
deviations when compared to control groups, whereas participants in a previous
study taking modafinil had an improvement of 0.23 standard deviations.
"A lot of times when people are fatigued the last thing they want to do is
exercise. But if you're physically inactive and fatigued, being just a bit more
active will help," said O'Connor.
Tim Puetz added that though energy drinks were becoming increasingly popular
among people, the study showed that the best way to up energy levels and beat
fatigue was to exercise.
"We live in a society where people are always looking for the next sports drink,
energy bar or cup of coffee that will give them the extra edge to get through
the day. But it may be that lacing up your tennis shoes and getting out and
doing some physical activity every morning can provide that spark of energy that
people are looking for," Puetz said.
The study is published in the November issue of the journal Psychological
Bulletin.
Published by HT Media Ltd. with permission from Asian News International.
LOAD-DATE: November 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 HT Media Ltd.
All Rights Reserved
339 of 998 DOCUMENTS
The Toronto Star
October 29, 2006 Sunday
ON THE ALERTEyes wide open
BYLINE: Andrew Chung, Toronto Star
SECTION: NEWS; Pg. A11
LENGTH: 858 words
"Could I have a non-fat cappuccino with modafinil to go?"
It's quite possible that a few years from now, that will be the wake-up mantra
for millions of people around the world. Modafinil, distributed in Canada as
Alertec, is a chemical first made in France in the 1970s for treating
narcolepsy. But in the past few years, it has been used more and more to combat
daytime sleepiness among shift workers. Doctors say it is safe, and that it can
"turn off" the urge to sleep.
"Maybe there will be a soft drink with Alertec in it," says Dr. James
MacFarlane, director of the sleep laboratory at Toronto's Hospital for Sick
Children. "It may be just that safe."
Our stimulant of choice right now, of course, is caffeine, which is safe if
taken in moderate amounts. But it can raise blood pressure and induce the
jitters.
Modafinil, meanwhile, is attracting more and more attention in various quarters.
In some large U.S. cities, it's giving a boost to the party circuit. And the
British, U.S. and French militaries have been testing it for use as a drug safer
than amphetamines to keep infantries alert.
The surging interest in modafinil is part of the growing focus on sleep and
wakefulness in medical and pharmaceutical circles as we strive to further
manipulate our circadian rhythms. It's just one of a flurry of drugs in
production or development that are heralding a brave new world where we will
finally be able to take complete control of sleep and wakefulness."I think
people want their personal biology to be more like a square wave these days,"
says MacFarlane.
But it's not a future MacFarlane sees positively. "If you try to make it that
way, you eventually pay the price."
On modafinil, one of a growing class of so-called "wakefulness promoters,"
people could theoretically stay awake for days. And while it is considered to be
very very safe and effective, MacFarlane cautions: "You're not reducing the need
for sleep, you're just improving performance during 'wake.' So, basically,
you're taking a stimulant, you're taking cocaine, even though it's not cocaine.
It does not in any way reduce your sleep requirement."
Using these drugs as lifestyle aids is a symptom of our increasingly fast-paced
and overworked society. North America's growing numbers of shift workers, for
example, often have trouble adjusting their sleep patterns, so they reach for
chemical solutions.
In the absence of a medical or psychiatric illness, their sleep/wake problems
arise from their jobs, leaving physicians loath to prescribe drugs like
modafinil. At the same time, though, many doctors understand the need."At first
I thought it's not such a good idea," says sleep expert and neurologist Dr.
Brian Murray at the Sunnybrook Health Sciences Centre. "But on the other hand
it's probably better than crashing your car. So that's why I think maybe we, or
I, need to have a more open mind to this."
Other such substances currently under study include modafinil's chemical cousin
armodafinil, as well as a group of drugs called ampakines, which boost
glutamate, the brain's excitatory neurotransmitter.
Sleep aids have also vastly improved from the highly addictive barbituates of
the 1950s, and the benzodiazepines that started coming on strong in the '70s.
Though many new medications still target the brain's GABA system, part of the
circuitry that puts people to sleep - and come with hangover effects - the
newest drugs mimic the effect of melatonin, a naturally occurring hormone that's
present in the blood at night and promotes sleep. (Though many of the newest
drugs - such as the popular Ambien and Lunestra - are available in the U.S., few
have made their way to Canada.)
Canada's military is currently studying melatonin, available in health food
stores, and photo therapy to figure out the best combination, and when to give
it, to reduce jet lag and shift-work problems in soldiers sent out to
battlefield or on warships, often in far-off places like Afghanistan. Any
serious military these days is 24/7.
"They have equipment for owning the night, and to exploit that capability they
have to be vigilant around the clock," says Michel Paul, defence scientist at
the Defence Research and Development Canada facility in Toronto.
The Canadian military currently gives no special wakefulness agents to
personnel, other than coffee. Paul stresses if the military expresses a desire
for drugs to maintain alertness, modafinil, and not amphetamines, would be the
route to take.
Other research underway includes drugs to increase the amount of time a person
spends in the most restorative phase of sleep, called slow wave. In the future,
people might be able to get a better-quality sleep in less time.
Will sleep ever become obsolete? That seems to be the goal of some research. But
few think it will ever happen. Murray points out the positive effects sleep has
on the immune system. "It's doubtful modafinil would cover up those effects. So
there's no replacement at this point for natural sleep."
Amid a tide of new chemical helpers, doctors today still recommend one
particular remedy for restoring the body and staying awake the next day: eight
hours of sleep.
LOAD-DATE: October 30, 2006
LANGUAGE: ENGLISH
GRAPHIC: Sleep research has led to a host of new drugs, including such
"wakefulness promoters" as Alertec.
DOCUMENT-TYPE: COLUMN
PUBLICATION-TYPE: NEWSPAPER
Copyright 2006 Toronto Star Newspapers, Ltd.
340 of 998 DOCUMENTS
The Sun Herald (Sydney, Australia)
October 15, 2006 Sunday
First Edition
'Ice' drug trial bid to help users kick habit
BYLINE: LOUISE HALL HEALTH REPORTER
SECTION: NEWS; Pg. 35
LENGTH: 317 words
ADDICTS of the dangerous party drug "ice" are taking part in a world-first trial
in Sydney that could help users kick their destructive habit.
Researchers are testing whether a drug normally used to treat the excessive
sleep disorder narcolepsy can wean addicts off the illegal methamphetamine
described as a "scourge on Australian society".
The National Drug and Alcohol Research Centre (NDARC) is conducting a clinical
trial of Modafinil, a non-habit forming stimulant medication. Forty users are
taking part in the 10-week trial.
Unlike heroin, there is no easily available drug to get addicts off "meth" or
deal with the violent and psychotic tendencies it induces.
Ice, the crystalline form of methamphetamine, is a powerfully addictive
synthetic drug that works by quickly boosting levels of dopamine, the brain
chemical responsible for movement, emotion, motivation and feelings of pleasure.
But long-term abuse can impede the body's ability to produce dopamine and cause
paranoic and violent rages, as well as depression and sleeplessness.
There has been a rapid rise in methamphetamine use in recent years. NDARC
figures suggest there are about 37,000 regular amphetamine users in NSW aged
between 15 and 49 and 28,000 are dependant on the drug.
Ice has been recognised by the Federal Government as the "nation's worst drug
problem".
Parliamentary secretary for health Christopher Pyne, who is responsible for drug
policy, told a newspaper last week that ice was causing more community problems
than heroin.
"Ice is a scourge on Australian society," he said.
Modafinil (marketed as Modavigil in Australia) has shown great promise in
treating cocaine users in US trials.
It reduces cravings and restores proper dopamine function.
James Shearer, from NDARC, said this was one of the first trials to extend
modafinil to methamphetamine users.
The NRARC wants 50 more recruits. Call James Shearer on 0414 385 149.
LOAD-DATE: June 20, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 John Fairfax Publications Pty Ltd
All Rights Reserved
341 of 998 DOCUMENTS
MediaNet Press Release Wire
October 4, 2006 Wednesday 7:07 AM AEST
Media Release 4 October 2006
LENGTH: 322 words
Treatment trials for amphetamine dependence
Mental health problems, dependence, polydrug use and unsafe sex and injecting
practices are all associated with amphetamine use. While there are a number of
medications available to treat problems such as anxiety or depression, there
are no specific pharmacotherapies to optimally treat amphetamine withdrawal and
relapse.
Turning Point Alcohol and Drug Centre is working to improve the health and
well-being of people with amphetamine dependence by examining withdrawal and
treatment options. A clinical trial of modafinil with a small group of
amphetamine users is currently being facilitated by Turning Point and Western
Hospital. Modafinil, a "wakefulness drug" possesses some stimulant properties
without euphoric effects and has shown preliminary potential for treating
cocaine dependence.
Professor Ernest Drucker, a US-based leading authority on drug addiction,
AIDS and human rights, has been invited by Turning Point to provide insight on
amphetamines and other stimulants.
"There is cause for optimism about the use of substitution stimulant drugs to
treat amphetamine dependency," says Dr Drucker. "Over twenty published reports
going back to the 1980s show that orally administered drugs with longer-term
effects such as modafinil have considerable promise."
Dr Drucker will speak on the subject of "Responding to the global epidemic of
amphetamines" at Turning Point's annual oration later today. The Honourable
Daniel Andrews, Parliamentary Secretary for Health will also launch the
2005-2006 Turning Point Annual Report.
The oration is being held on Wednesday 4th October at 5.30pm in The Age
Theatre, Lower Ground Level, Melbourne Museum, Carlton Gardens, Carlton.
For more information, please contact:
Professor Ernest Drucker
M: 0427 597 612
Professor Nick Crofts
T: 8413 8400
M: 0417 363 449
SOURCE: Turning Point Alcohol and Drug Centre
LOAD-DATE: October 4, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Australian Associated Press Pty. Ltd.
342 of 998 DOCUMENTS
Pharmacy News (Australia)
September 14, 2006
LENGTH: 293 words
ADHD drug snag
It had been touted as a safer alternative to the amphetamine-like stimulants
prescribed to millions of hyperactive children and young adults. Now concerns
about a potentially fatal side effect have crushed plans to market modafinil as
a treatment for attention deficit hyperactivity disorder (ADHD).
Modafinil, which boosts wakefulness and focus, is approved for adults with
excessive sleepiness. A proposal to market it for treating ADHD hit a snag in
March when one of 933 children taking part in a clinical trial developed a
life-threatening skin condition. The manufacturer, Cephalon, tried to convince
the US Food and Drug Administration that the child's rash was not a reaction to
the drug. But it has now abandoned its ADHD plans after the FDA refused to
approve modafinil without further extensive safety studies.
Pill pushing
Fancy a free trial of an impotence drug? How about a free course of sleeping
pills? USconsumer groups are worried about the way pharmaceutical companies give
away coupons offering discounts on their prescription drugs or free trials.
"The incentive for you to buy it is irrelevant to whether that's the best
medication for you or not," said Susan Sherry, of the health pressure group
Community Catalyst, which has joined 22 other groups calling on the FDA to ban
the practice.
The companies have responded that coupons help to lower health care costs and
increase access. "We believe this programme benefits patients," said a
spokeswoman for Sanofi-Aventis, which offers a free seven-day trial of its
insomnia pill Ambien. Patients still need to get a prescription from their
doctor. "We're taking a look to see if FDA action is needed,' said an agency
spokeswoman.
Stories are from the 19 August issue of New Scientist.
LOAD-DATE: September 11, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
JOURNAL-CODE: PN
Copyright 2006 Reed Business Information Ltd.
All Rights Reserved
343 of 998 DOCUMENTS
The Associated Press
September 8, 2006 Friday 9:29 PM GMT
Doctor in BALCO steroids scandal could lose license
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: DOMESTIC NEWS
LENGTH: 288 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
could lose his license for allegedly prescribing a stimulant to a track and
field athlete without examining her.
The state medical board is seeking to revoke or suspend the license of
psychiatrist Brian Halevie-Goldman, who was medical director for the Bay Area
Laboratory Co-Operative that provided steroids to top athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the athlete at the request of BALCO founder Victor Conte, who
served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy. The medical board's accusation, filed in May, said K.W. tested positive
for modafinil at an international track meet in August 2003 and accepted a
two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
Modafinil is used to treat narcolepsy, a sleep disorder.
The medical board has scheduled a hearing on the allegations Nov. 13, said
spokeswoman Candis Cohen.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
344 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 8, 2006 Friday 9:29 PM GMT
Doctor in BALCO steroids scandal could lose license
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: SPORTS NEWS
LENGTH: 288 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
could lose his license for allegedly prescribing a stimulant to a track and
field athlete without examining her.
The state medical board is seeking to revoke or suspend the license of
psychiatrist Brian Halevie-Goldman, who was medical director for the Bay Area
Laboratory Co-Operative that provided steroids to top athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the athlete at the request of BALCO founder Victor Conte, who
served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy. The medical board's accusation, filed in May, said K.W. tested positive
for modafinil at an international track meet in August 2003 and accepted a
two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
Modafinil is used to treat narcolepsy, a sleep disorder.
The medical board has scheduled a hearing on the allegations Nov. 13, said
spokeswoman Candis Cohen.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
345 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 8, 2006 Friday 8:47 PM GMT
Doctor in BALCO steroids scandal could lose license
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: STATE AND REGIONAL
LENGTH: 529 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic at the center of a massive
sports-doping scandal could lose his license for allegedly prescribing a
stimulant to a track-and-field athlete without examining her.
The state medical board is seeking to revoke or suspend the medical license of
Fairfield psychiatrist Dr. Brian Halevie-Goldman, who was medical director for
the Bay Area Laboratory Co-operative that peddled steroids to top athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the unnamed athlete at the request of BALCO founder Victor Conte,
who served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy.
The report indicates the initials could be those of elite sprinter Kelli White,
a BALCO client who tested positive for modafinil after winning gold medals in
the 100- and 200-meter races at the World Championships in Paris in August 2003.
White was stripped of her gold medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board's accusation, filed in May, said K.W. tested positive for
modafinil at an international track meet in August 2003 and accepted a two-year
suspension for admitting to its use in 2004.
White provided information to the U.S. Anti-Doping Agency on Conte and her
former coach Remi Korchemny.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
In June 2003, the charts indicate Halevie-Goldman gave K.W. prescriptions for
the painkiller Motrin, the sedative Ambien and two medications to treat a rash,
though he had never seen or examined her, the medical board said.
After K.W. tested positive for modafinil in August 2003, Halevie-Goldman sent a
letter to her agents saying he had dispensed modafinil samples to treat her
narcolepsy, though he had never met her as a patient, according to the board's
accusation.
Halevie-Goldman's records show he examined K.W. in October 2003, after she
tested positive for the stimulant, the medical board said. He later wrote a memo
blaming Conte, the athlete and her mother for deceiving him about K.W.'s
condition.
The medical board has scheduled a hearing on the allegations Nov. 13, said
spokeswoman Candis Cohen.
BALCO peddled performance-enhancing drugs designed to avoid detection by the
USADA and professional sporting leagues, including Major League Baseball and the
National Football League.
The names of several prominent athletes have surfaced in the federal probe,
including other track stars and baseball players, such as Giants slugger Barry
Bonds.
The BALCO probe brought guilty pleas in U.S. District Court from Conte, Bonds'
trainer Greg Anderson, BALCO vice president James Valente, Korchemny and Patrick
Arnold, the chemist who designed a previously undetectable steroid.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
346 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 8, 2006 Friday 8:46 PM GMT
Doctor in BALCO steroids scandal could lose license
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: SPORTS NEWS
LENGTH: 529 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic at the center of a massive
sports-doping scandal could lose his license for allegedly prescribing a
stimulant to a track-and-field athlete without examining her.
The state medical board is seeking to revoke or suspend the medical license of
Fairfield psychiatrist Dr. Brian Halevie-Goldman, who was medical director for
the Bay Area Laboratory Co-operative that peddled steroids to top athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the unnamed athlete at the request of BALCO founder Victor Conte,
who served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy.
The report indicates the initials could be those of elite sprinter Kelli White,
a BALCO client who tested positive for modafinil after winning gold medals in
the 100- and 200-meter races at the World Championships in Paris in August 2003.
White was stripped of her gold medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board's accusation, filed in May, said K.W. tested positive for
modafinil at an international track meet in August 2003 and accepted a two-year
suspension for admitting to its use in 2004.
White provided information to the U.S. Anti-Doping Agency on Conte and her
former coach Remi Korchemny.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
In June 2003, the charts indicate Halevie-Goldman gave K.W. prescriptions for
the painkiller Motrin, the sedative Ambien and two medications to treat a rash,
though he had never seen or examined her, the medical board said.
After K.W. tested positive for modafinil in August 2003, Halevie-Goldman sent a
letter to her agents saying he had dispensed modafinil samples to treat her
narcolepsy, though he had never met her as a patient, according to the board's
accusation.
Halevie-Goldman's records show he examined K.W. in October 2003, after she
tested positive for the stimulant, the medical board said. He later wrote a memo
blaming Conte, the athlete and her mother for deceiving him about K.W.'s
condition.
The medical board has scheduled a hearing on the allegations Nov. 13, said
spokeswoman Candis Cohen.
BALCO peddled performance-enhancing drugs designed to avoid detection by the
USADA and professional sporting leagues, including Major League Baseball and the
National Football League.
The names of several prominent athletes have surfaced in the federal probe,
including other track stars and baseball players, such as Giants slugger Barry
Bonds.
The BALCO probe brought guilty pleas in U.S. District Court from Conte, Bonds'
trainer Greg Anderson, BALCO vice president James Valente, Korchemny and Patrick
Arnold, the chemist who designed a previously undetectable steroid.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
347 of 998 DOCUMENTS
THE SAN FRANCISCO CHRONICLE (California)
September 8, 2006 Friday
FINAL Edition
THE BALCO CASE;
Doctor who gave sprinter stimulant may lose license
BYLINE: Lance Williams, Mark Fainaru-Wada, Chronicle Staff Writers
SECTION: BAY AREA; Pg. B2
LENGTH: 831 words
The former medical director at BALCO, the laboratory implicated in an
international sports-doping scandal, has been accused of gross negligence for
allegedly giving the prescription stimulant modafinil to a champion sprinter
without ever examining her.
In a pending accusation, the state Medical Board said it was seeking to revoke
or suspend the medical license of Dr. Brian Halevie-Goldman for allegedly
providing the drug to the athlete simply because he was asked to do so by BALCO
founder and confessed steroid dealer Victor Conte.
When the athlete tested positive for the stimulant at a track meet, Goldman
concocted a medical history and diagnosis in an effort to excuse the doping
offense, the Medical Board charged.
Goldman blamed Conte for deceiving him about the athlete's medical condition,
according to the Medical Board. The doctor did not respond to telephone messages
and a letter faxed to his office requesting comment.
The Medical Board identified the athlete by the initials KW. But the allegations
in the filing obviously refer to elite sprinter Kelli White, a BALCO client who
tested positive for modafinil after winning gold medals in the 100- and
200-meter races at the World Championships in Paris in 2003.
White, of Union City, later admitted using several banned drugs and was
suspended from competition for two years. Saying she wanted to help clean up
sports, she gave interviews about her drug use and testified at disciplinary
hearings conducted by the U.S. Anti-Doping Agency.
Goldman is a psychiatrist who has worked at Fairfield's Amen Clinic and at
Diablo Behavioral Healthcare Center in Danville. In 1984, he began moonlighting
as medical director at Conte's Bay Area Laboratory Co-Operative in Burlingame.
At some point Goldman stopped working there, but BALCO continued to list him on
state documents as the lab's medical director, and he and Conte stayed in touch.
In January 2003, according to the Medical Board, Conte contacted Goldman,
seeking modafinil for White. According to the Medical Board, Conte told Goldman
that White was suffering from fatigue and sleeplessness. Goldman recommended
evaluating her for the sleep disorder narcolepsy. But instead of examining
White, Goldman gave Conte samples of modafinil, an anti-narcolepsy drug. At the
time, Conte was providing the banned stimulant to several sprinters to help them
run faster, according to court records.
In June 2003, even though Goldman still hadn't examined White, the Medical Board
said he began prescribing other drugs for her: two medicines to treat a skin
rash; the painkiller Motrin; and the sedative Ambien.
In August 2003, White became the first American woman ever to win both the 100-
and 200-meter races at the World Championships. Two days later, authorities
announced she had tested positive for modafinil.
At first, with Goldman's help, White fought the charges. Goldman gave White a
letter falsely claiming that she had a family history of narcolepsy and that he
had provided her with the drug to treat the ailment, the Medical Board said.
Goldman also wrote a letter to the International Association of Athletics
Federations arguing that modafinil could not enhance athletic performance.
Goldman was paid $5,000 for the letters, the Medical Board said.
In a 2004 interview with The Chronicle and other newspapers, White acknowledged
she had never suffered from narcolepsy, saying Goldman's diagnosis was part of a
false story devised by Conte to excuse her use of drugs.
White said Conte and her coach, Remi Korchemny, also had provided her many other
banned drugs, including the undetectable steroid known as "the clear."
Conte served four months in federal prison on his guilty plea in the BALCO
steroids conspiracy case. Korchemny, who also pleaded guilty to steroid dealing,
was put on probation.
When Goldman was interviewed by the Medical Board, he admitted he had only
examined White once -- on Oct. 1, 2003, weeks after she was suspended for using
modafinil. At first, Goldman told investigators that he had consulted with White
by phone before providing her with the drug, but he later admitted he couldn't
remember talking to her, the Medical Board said.
Federal authorities investigating BALCO were told of another instance where
Goldman allegedly prescribed a drug for an athlete at Conte's request.
Former world champion sprinter Tim Montgomery told authorities that in 2001 he
got the women's fertility drug Clomid via a phony prescription written by
Goldman, The Chronicle has reported. Montgomery said Conte advised him to use
Clomid, which is sometimes used to mask steroids in drug tests. Montgomery said
Conte called Goldman, who by his account wrote a prescription for Montgomery
using a false name so it would not be traceable. Goldman disputed Montgomery's
allegations, telling The Chronicle in 2004, "Everything is a lie."
The Medical Board's accusation was filed against Goldman in May, said board
spokeswoman Candis Cohen. A hearing has been set for Nov. 13.
LOAD-DATE: September 8, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 San Francisco Chronicle
All Rights Reserved
348 of 998 DOCUMENTS
Associated Press Worldstream
September 8, 2006 Friday 9:56 PM GMT
Doctor in BALCO steroids scandal could lose license
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: SPORTS NEWS
LENGTH: 293 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a U.S. sports doping
scandal could lose his license for allegedly prescribing a stimulant to a track
and field athlete without examining her.
The California state medical board is seeking to revoke or suspend the license
of psychiatrist Brian Halevie-Goldman, who was medical director for the Bay Area
Laboratory Co-Operative that provided steroids to top American athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the athlete at the request of BALCO founder Victor Conte, who
served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls on Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy. The medical board's accusation, filed in May, said K.W. tested positive
for modafinil at an international track meet in August 2003 and accepted a
two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
Modafinil is used to treat narcolepsy, a sleep disorder.
The medical board has scheduled a hearing on the allegations on Nov. 13, said
spokeswoman Candis Cohen.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
349 of 998 DOCUMENTS
Associated Press Online
September 8, 2006 Friday 9:35 PM GMT
Doc in Steroids Scandal May Lose License
BYLINE: By MARCUS WOHLSEN, Associated Press Writer
SECTION: SPORTS NEWS
LENGTH: 288 words
DATELINE: SAN FRANCISCO
The former medical director of the clinic involved in a sports doping scandal
could lose his license for allegedly prescribing a stimulant to a track and
field athlete without examining her.
The state medical board is seeking to revoke or suspend the license of
psychiatrist Brian Halevie-Goldman, who was medical director for the Bay Area
Laboratory Co-Operative that provided steroids to top athletes.
Halevie-Goldman was accused of gross negligence for allegedly providing the drug
modafinil to the athlete at the request of BALCO founder Victor Conte, who
served four months in federal prison for dealing steroids.
The doctor, who now specializes in childhood autism at two San Francisco Bay
area clinics, did not immediately return calls Friday seeking comment.
The athlete in the case was identified by her initials, K.W., to protect her
privacy. The medical board's accusation, filed in May, said K.W. tested positive
for modafinil at an international track meet in August 2003 and accepted a
two-year suspension for admitting to its use in 2004.
Kelli White, a BALCO client who tested positive for modafinil after winning gold
medals in the 100- and 200-meter races at the world championships in Paris in
August 2003, was stripped of those medals and suspended for two years after
admitting in 2004 to using the banned stimulant.
The medical board said investigators examined medical charts kept by
Halevie-Goldman that showed he diagnosed K.W. with narcolepsy in January 2003
without examining her, basing his analysis solely on a description of symptoms
provided by Conte.
Modafinil is used to treat narcolepsy, a sleep disorder.
The medical board has scheduled a hearing on the allegations Nov. 13, said
spokeswoman Candis Cohen.
LOAD-DATE: September 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
350 of 998 DOCUMENTS
Clinical Psychiatry News
September 2006
FDA Cites Stevens-Johnson in Modafinil's ADHD Rejection
BYLINE: Elizabeth Mechcatie
SECTION: Pg. 7 Vol. 34 No. 9 ISSN: 0270-6644
LENGTH: 390 words
Modafinil, first approved for narcolepsy almost a decade ago, will not be
among the Food and Drug Administration-approved options for treating
attention-deficit hyperactivity disorder in children and adolescents.
In response to the FDA's decision not to approve the drug for this
indication, the manufacturer, Cephalon Inc., has announced that it will stop
development of the drug for this indication.
The company said in early August that the FDA had issued a nonapprovable
letter for the drug for treating children and adolescents with ADHD. Had it been
approved for this use, Cephalon would have marketed it under the trade name
Sparlon.
The FDA does not typically comment on nonapprovable decisions.
Modafinil, described as a "wakefulness-promoting agent" in its label, was
approved in 1998 for improving wakefulness in narcolepsy, and in 2004 to improve
wakefulness in patients with excessive sleepiness associated with obstructive
sleep apnea/hypopnea syndrome and shift work sleep disorder.
At a meeting in March, convened by the FDA to review the safety of modafinil
for the ADHD indication, the FDA's Psychopharmacologic Drugs Advisory Panel
noted in a 12 to 1 vote that modafinil was not safe for treating children and
adolescents. The panel agreed the drug was effective but was mainly concerned
about its potential to cause Stevens-Johnson syndrome (SJS) in this population.
In a group of 933 children and adolescents treated with modafinil in trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or were suggestive of EM or SJS, according to an
FDA reviewer at the meeting.
One case was considered most likely to be SJS, for a risk of about 1 in
1,000. Although there were no reports of SJS among 36,000 children prescribed
the drug off-label between 2002 and 2005, there was concern that some cases
could occur with wider use of the drug, and the panel recommended that the
company conduct a 3,000 patient study to further clarify the risk.
In the Cephalon release, Chairman and Chief Executive Officer Frank Baldino
Jr., Ph.D., said the company was "surprised that the agency disagreed with the
opinions of our experts, which were based on photographic and other evidence
concerning a single suspected case of Stevens Johnson syndrome."
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Pediatric News
September 2006
Modafinil to Treat ADHD Is Rejected by the FDA
BYLINE: Elizabeth Mechcatie, Senior Writer
SECTION: Pg. 11 Vol. 40 No. 9 ISSN: 0031-398X
LENGTH: 387 words
Modafinil, first approved for narcolepsy almost a decade ago, will not be
among the Food and Drug Administration-approved options for treating
attention-deficit hyperactivity disorder in children and adolescents.
In response to the FDA's decision not to approve the drug for this
indication, the manufacturer, Cephalon Inc., has announced that it will stop
development of the drug for this indication.
On August 9, the company announced that the FDA had issued a nonapprovable
letter for the drug for treating children and adolescents with ADHD. If it had
been approved for this use, Cephalon would have marketed it under the trade name
Sparlon.
The FDA does not typically comment on nonapprovable decisions.
Modafinil, described as a "wakefulness-promoting agent" in its label, was
approved in 1998 for improving wakefulness in narcolepsy, and in 2004 to improve
wakefulness in patients with excessive sleepiness associated with obstructive
sleep apnea/hypopnea syndrome and shift work sleep disorder.
At a meeting in March, convened by the FDA to review the safety of modafinil
for the ADHD indication, the FDA's Psychopharmacologic Drugs Advisory Panel
noted in a 12 to 1 vote that modafinil was not safe for treating children and
adolescents. The panel agreed the drug was effective but was mainly concerned
about its poential to cause Stevens-Johnson syndrome (SJS) in this population.
In a group of 933 children and adolescents treated with modafinil in trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or were suggestive of EM or SJS, according to an
FDA reviewer at the meeting. One case was considered most likely to be SJS, for
a risk of about 1 in 1,000. Although there were no reports of SJS among 36,000
children prescribed the drug off-label between 2002 and 2005, there was concern
that some cases could occur with wider use of the drug, and the panel
recommended that the company conduct a 3,000-patient study to further clarify
the risk.
In the Cephalon release, chairman and CEO Frank Baldino Jr., Ph.D., said the
company was "surprised that the agency disagreed with the opinions of our
experts, which were based on photographic and other evidence concerning a single
suspected case of Stevens Johnson syndrome."
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WALL STREET JOURNAL ABSTRACTS
August 31, 2006 Thursday
BARR PHARMACEUTICALS INC
SECTION: Section D; Column 3; Pg. 7
LENGTH: 43 words
Barr Pharmaceuticals Inc says the FTC has asked it to submit information
regarding a settlement agreement for the sleep-disorder drug Modafinil; the FTC
is investigating whether Barr and others violated federal trade laws by
restricting the sale of Modafinil (S)
LOAD-DATE: September 1, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Abstract
JOURNAL-CODE: WSJ
Copyright 2006 The New York Times Company
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Information Bank Abstracts
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New Scientist
August 19, 2006
ADHD drug snag
BYLINE: Staff
SECTION: NEWS; Upfront; Pg. 7
LENGTH: 187 words
IT HAD been touted as a safer alternative to the amphetamine-like stimulants
prescribed to millions of hyperactive children and young adults. Now concerns
about a potentially fatal side effect have crushed plans to market modafinil as
a treatment for attention deficit hyperactivity disorder (ADHD).
Modafinil, which boosts wakefulness and focus, is approved for adults with
excessive sleepiness. A proposal to market it for treating ADHD hit a snag in
March when one of 933 children taking part in a clinical trial developed a
life-threatening skin condition (New Scientist , 1 April, p 8).
Manufacturer Cephalon of Frazer, Pennsylvania, tried to convince the Food and
Drug Administration that the child's rash was not a reaction to the drug. It has
now abandoned its ADHD plans after the FDA refused to approve modafinil without
further extensive safety studies.
"It's really unfortunate," says James Swanson, a psychologist at the University
of California, Irvine, who was involved in Cephalon's ADHD trials. He still
believes modafinil is safer than other stimulants, which may cause
hallucinations in a minority of children.
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PUBLICATION-TYPE: Magazine
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Pharma Marketletter
August 17, 2006 Thursday
Stock Commentary - New York - week to Aug 14, 2006
LENGTH: 377 words
NEW YORK: equities finished the reporting period to August 14 in negative
territory, with the Dow Jones falling 1.1%, in a week that was impacted by
escalating oil prices on the back of alleged terrorist activities in the UK.
Drug and biotechnology stocks were also mostly weaker, with 15 of those tracked
rising, 26 falling.
Better-than-expected second-quarter adjusted earnings helped Watson move up a
little more than 11% during the reported week, with generics accounting for over
80% of the revenue (see page 6). Though the generic industry is showing some
weak fundamentals generally, David Maris of Banc of America feels Watson shares
still could see a nice rise. He has set a $26 target for the stock, and puts the
same figure on Andrx (down 0.6%), which said its merger with Watson is still
progressing on target, with antitrust concerns being addressed. But Andrx'
earnings figures were not as positive, with it pointing to fees to try to clear
up some issues with the Food and Drug Administration. Concerns are mounting for
Cephalon, whose stock fell 16.3%. The news that it would give up development of
Sparlon (modafinil) for attention-deficit hyperactivity disorder (see page 20)
led several brokers to downgrade the shares to sell, and some investors sold off
the stock. The safety issues for Sparlon raised worries about Provigil (
modafinil) and Nuvigil (r-modafinil). S & P's Equity Research Services
downgraded Cephalon to hold from buy, on concerns over Nuvigil and Jefferies &
Co, with a hold rating, said it would reserve $8.6 million as of June 30 for
unused Sparlon inventory. Optimists now feel that the firm can concentrate on
marketing Nuvigil, leveraging its existing sales force and its doctor contacts
to switch patients to the newer product before modafinil comes off patent in
2011. A 12.3% drop in ImClone signaled investor unhappiness with the company's
decision to stay independent (see page 2). While the firm pointed to strong
sales of Erbitux (cetuximab), the cancer drug could soon face competition from
an Amgen product. Investor Carl Icahn, the firm's largest shareholder aside from
Bristol-Myers Squibb, has not yet decided whether to join ImClone's board, and
investors are not convinced he could solve the company's problems.
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Datamonitor CommentWire
August 11, 2006
Cephalon: Sparlon rejection could prove a blessing in disguise;
Cephalon has received non-approvable letter from the FDA regarding the use of
Sparlon in ADHD.
LENGTH: 287 words
HIGHLIGHT: Cephalon has received a non-approvable letter from the FDA for its
application to market Sparlon (modafinil) for the treatment of ADHD in children
and adolescents. Although the rejection is a blow for Cephalon, the company is
now free to concentrate its marketing efforts on modafinil's follow-up drug
Nuvigil in sleep disorders, which
Modafinil is currently marketed under the name Provigil for the treatment of
narcolepsy and idiopathic hypersomnia, and generated sales of $513 million in
2005. The attempt to expand the drug's indication into ADHD was part of
Cephalon's strategy to minimize the effect of generic competition to modafinil
on revenues.
The FDA's rejection of Sparlon is due to concerns regarding the possible
induction of Stevens-Johnson syndrome, a hypersensitivity complex affecting the
skin and mucous membranes.
While Cephalon expressed its disappointment at the FDA ruling in a statement,
the regulator's decision should not come as a surprise to either Cephalon's
management or the investment community as an FDA scientific advisory panel voted
not to recommend approval of the drug in March. Perhaps tellingly, in light of
this recommendation, the company reduced its 2006 sales guidance by $100 million
to between $1.45 billion and $1.50 billion.
Although the non-approvable letter is a clearly a blow to Cephalon, this sales
guidance suggests that Cephalon may have actually overestimated the earnings
potential for Sparlon. In May 2005, Datamonitor estimated that, if approved,
Sparlon would generate annual sales revenue of $3 million in 2006, reaching $100
million in 2008 and peaking at between $210 million and $230 million between
2010 and 2015.
The regulatory setback could also act as a blessing in disguise for Cephalon, as
the company can now focus its efforts on its modafinil follow-on drug, Nuvigil
(r-modafinil). Cephalon should be able to leverage the experience of its
existing sales force and relationships with sleep specialists to ensure a smooth
switch to the new product before modafinil comes off patent in 2011.
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Pharma Marketletter
August 11, 2006 Friday
FDA rejects Cephalon's Sparlon for ADHD
LENGTH: 242 words
US drugmaker Cephalon has received a letter from the Food and Drug
Administration rejecting its supplemental New Drug Application Sparlon (
modafinil) tablets, a prop rietary dosage form for this drug for the treatment
of atten tion- deficit/hyperactivity disorder in children and adolesc ents. In
light of the FDA's "not approvable" letter, the firm says it will not develop
Sparlon further. On the day of the news, August 10, the firm's share price fell
11% to $28.86.
Frank Baldino, the company's chief executive, noted his surprise that the agency
had disagreed with the opinions of Cepha lon's experts, which were based on
photographic and other evidence concerning a single suspected case of Stevens
Johnson syndrome, but he stressed that the decision has no impact on the
company's previously-iss ued sales and earnings guidance or on its expectations
for strong earnings in 2007.
Late last year, the company received an approvable letter from the FDA to market
the agent, which is a proprietary dosage form of modafinil, the active
ingredient of the narcolepsy drug Provigilne, requesting additional information,
but Cephalon still hoped to launch the drug early this year (Marketletter
October 31, 2005).
The company has decided to fully reserve the $8.6 million of net Sparlon
inventory on its balance sheet but stressed that its previously-reported
adjusted income per common share for the three and six months ended June 30,
2006, remains unchanged.
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Global Insight
August 10, 2006
FDA Rejects Cephalon's Hyperactivity Drug Sparlon
BYLINE: Dr Jonathan Goodall
LENGTH: 874 words
U.S. drug-maker Cephalon has received a not approvable letter from the U.S. FDA
for its supplemental new drug application (sNDA) for Sparlon (modafinil); an
experimental drug for the treatment of attention-deficit/hyperactivity disorder
(ADHD) in children.
Global Insight Perspective
Significance
U.S.-based drug-maker Cephalon has received
a not approvable letter from the U.S.
regulatory authority, regarding its sNDA for
experimental ADHD treatment Sparlon.
Implications
This is a major setback for the company,
since Sparlon was expected to prove an
important franchise extension for its
flagship product Provigil, which is close to
facing generic challenges.
Outlook
Another major concern for Cephalon and its
investors is that this decision could affect
approval for the follow-on to Provigil;
Nuvigil. However, observers generally feel
that any potential link between Nuvigil and
the severe skin rash Stevens-Johnson Syndrome
(SJS) can be managed through more stringent
labelling of Nuvigil.
The central nervous system (CNS) research specialist Cephalon confirmed
yesterday that it had received a letter from the U.S. FDA stating that its sNDA
for Sparlon (modafinil) is not approvable. As a result, Cephalon announced that
it will not pursue further development of the drug, which is a proprietary
higher-dosage form of its flagship narcolepsy drug, Provigil (modafinil).
This decision was not entirely unexpected. Sparlon received the thumbs-down from
the agency s paediatric advisory panel on 23 March, over concerns that the sNDA
submission did not contain sufficient information about whether the drug could
cause the severe and potentially fatal skin rash, Stevens-Johnson Syndrome
(SJS). The panel s decision caused the FDA to issue an approvable letter for the
drug back in April of this year.
A theoretical risk linking modafinil to SJS was discovered during post-marketing
surveillance for Provigil. Although the rate of SJS occurrence was about the
same as that which would be observed in the general population, the FDA s panel
decided that, without further data, the risk of approving Sparlon was
unacceptable. Reuters reports that as recently as last month, Cephalon s
management appeared optimistic about Sparlon s chances of gaining approval, on
the basis of new safety data that it provided to the agency. However, it appears
that the FDA remained unconvinced about the safety of the drug. In a press
release, Cephalon s Chairman and Chief Executive Officer, Frank Baldino, stated
that Cephalon is extremely disappointed and surprised that the FDA disagreed
with the opinion of its] experts, which was based on photographic and other
evidence concerning a single suspected case of Stevens Johnson Syndrome .
Outlook and Implications
The decision to reject Sparlon deals a significant blow to Cephalon, which has
now lost what was once thought by many to be an extremely promising product
candidate. Many observers thought the approval of Sparlon would be fairly
straightforward, due to it sharing the same active pharmaceutical ingredient as
Provigil. Cephalon s flagship drug has gained widespread market acceptance in
the treatment of excessive daytime sleepiness, and generated US$177.0 million in
sales in the second quarter of 2006.
Sparlon was considered an important line franchise extension for Provigil. It
had been widely anticipated to gain market share in the ADHD treatment market,
on account of the fact that it was not considered a stimulant (although its
exact action mechanism was not well characterised). However, Cephalon s
inability to demonstrate to the FDA s satisfaction that Sparlon was not
associated with SJS seems to have caused its demise. This is despite the company
s announcement in April that it had submitted additional information to the FDA,
which it believed indicated that the skin rash observed in clinical trials was
not SJS.
As the FDA s decision was expected, Cephalon has already factored in the loss of
Sparlon into its full-year financial projections. According to Cephalon, this
decision will not impact previously-issued sales and earnings guidance, nor its
expectations of strong earnings in 2007. Nevertheless, this rejection of Sparlon
does pose a certain risk to Cephalon s optimistic future forecasts.
Specifically, there is concern that this rejection may influence the FDA s
decision over Cephalon s follow-up to Provigil, Nuvigil (armodafinil), which is
currently under review by the agency. Nuvigil is a single isomer formulation of
modafinil, designed to improve wakefulness in patients suffering from excessive
sleepiness associated with narcolepsy, shift-work sleep disorder and obstructive
sleep apnea/hypopnea syndrome. However, many observers believe that that Sparlon
s rejection will not unduly affect the approval of Nuvigil, even if it is
believed there is a theoretical link between modafinil and SJS. They note that
if similar concerns persist with Nuvigil, they will probably be addressed
through more stringent labelling of the product.
Related Articles
United States: 14 July 2006:
United States: 25 April 2006:
United States: 24 March 2006:
United States: 2 February 2006:
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The Philadelphia Inquirer
August 10, 2006 Thursday
Cephalon shares plunge on discontinuation of Sparlon
BYLINE: Linda Loyd, INQUIRER STAFF WRITER
LENGTH: 211 words
Shares of Cephalon Inc. plunged today after the company said it was abandoning
development of Sparlon, a treatment for attention deficit hyperactivity
disorder, because the Food and Drug Administration rejected the drug.
Shares of the Frazer company were down 13.2 percent, or $8.45, to $55.50 in
late-morning trading on the Nasdaq.
Cephalon announced late Wednesday after the stock markets closed that it
received a "non-approvable" letter from the FDA for Sparlon to treat ADHD in
children.
The company said it would not pursue further development of the drug, adding
that regulators were particularly concerned that the drug had triggered a
suspected case of Stevens-Johnson syndrome, a potentially fatal skin rash.
Sparlon contains the same main ingredient, modafinil, that is in Cephalon's
biggest-selling drug, Provigil, for sleep disorders. Cephalon said that its
discontinuation of Sparlon would have no impact on previously issued financial
guidance for 2007.
Cephalon is developing another formulation of modafinil in a new drug, called
Nuvigil. The FDA's rejection of Sparlon could cast doubt on the future of
Nuvigil, which may have to carry additional warning labels, some analysts said.
Contact staff writer Linda Loyd at 215-854-2831 or lloyd@phillynews.com.
LOAD-DATE: August 10, 2006
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August 10, 2006 Thursday 7:15 AM Eastern Time
CEPH: Hot Stocks
LENGTH: 164 words
19:45 EDT Cephalon-CEPH says FDA says Sparlon is not approvable, will not pursue
development - CEPH announced Wednesday day that it has received a letter from
the U.S. Food and Drug Administrationstating that the company's supplemental new
drug application (sNDA) for SPARLON (modafinil) Tablets [C-IV], a proprietary
dosage form of modafinil for the treatment of attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, is not approvable. In consideration
of the FDA's decision, the company has determined that it will not pursue
further development of Sparlon.
As of Sunday, 08-06-2006 23:59, the latest Comtex SmarTrend(SM) Alert, an
automated pattern recognition system, indicated an UPTREND on 06-30-2006 for
CEPH @ $59.83. For more information on Comtex SmarTrend® Alert, contact your
market data provider or go to CSTADirect.com SmarTrend is a registered trademark
of Comtex News Network, Inc. Copyright © 2004-2006 Comtex News Network, Inc. All
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US Fed News
August 10, 2006 Thursday 12:03 AM EST
Pennsylvania, Massachusetts Inventors Develop Modafinil
BYLINE: US Fed News
LENGTH: 202 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Aug. 10 -- Matthew S. Miller of Newtown, Pa., and Thomas E.
Scammell of Wellesley, Ma., have developed compositions including modafinil for
treatment of attention deficit hyperactivity disorder and multiple sclerosis
fatigue.
According to the U.S. Patent & Trademark Office: "Modafinil is effective in
improving symptoms of attention deficit hyperactivity disorder and symptoms of
multiple sclerosis fatigue. The administration of modafinil is also shown to
activate the tuberomamillary neurons of the posterior hypothalamus, and thus
exhibits activity in an area of the brain associated with normal wakefulness
functions."
The inventors were issued U.S. Patent No. 7,087,647 on Aug. 8.
The patent has been assigned to Cephalon Inc., Frazer, Pa.
The original application was filed on Oct. 30, 2002, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO1&Sect2=HITOFF&d=PALL&p=1&u=%
2Fnetahtml%2FPTO%2Fsrchnum.htm&r=1&f=G&l=50&s1=7,087,647.PN.&OS=PN/7,087,647&RS=
PN/7,087,647.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com.
LOAD-DATE: August 15, 2006
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PR Newswire US
August 9, 2006 Wednesday 9:01 PM GMT
Cephalon Receives Non-Approvable Letter on SPARLON(TM);
Company Will Not Pursue Further Development of the Product
LENGTH: 873 words
DATELINE: FRAZER, Pa. Aug. 9
FRAZER, Pa., Aug. 9 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that it has received a letter from the U.S. Food and Drug
Administration (FDA) stating that the company's supplemental new drug
application (sNDA) for SPARLON(TM) (modafinil) Tablets [C-IV], a proprietary
dosage form of modafinil for the treatment of attention- deficit/hyperactivity
disorder (ADHD) in children and adolescents, is not approvable. In consideration
of the FDA's decision, the company has determined that it will not pursue
further development of SPARLON.
"Obviously, we are extremely disappointed and surprised that the agency
disagreed with the opinions of our experts, which were based on photographic and
other evidence concerning a single suspected case of Stevens Johnson syndrome,"
said Frank Baldino, Jr., Ph.D., Chairman and CEO.
This decision by the FDA has no impact on the company's previously issued sales
and earnings guidance or on its expectations for strong earnings in 2007.
Second Quarter 2006 Financial Results
The company's August 3, 2006 press release announcing its unaudited financial
results for the three- and six-month periods ended June 30, 2006 did not reflect
the impact of FDA's decision today on the SPARLON sNDA. The company has now
determined to fully reserve the $8.6 million of net SPARLON inventory on its
balance sheet as of June 30, 2006. The Company's previously reported adjusted
income per common share for the three and six months ended June 30, 2006 does
not change.
The company expects to file its Form 10-Q for the quarterly period ended June
30, 2006 no later than August 14, 2006, which will reflect the impact of this
event on the financial statements and related disclosures.
Conference Call Scheduled
Cephalon's management will discuss SPARLON in a conference call with investors
beginning at 5:30 p.m. EDT today, Wednesday, August 9, 2006. To participate in
the conference call, dial +1-888-856-9426 and refer to conference code 4413648.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. U.S. sites include the company's headquarters in Frazer,
Pennsylvania, and offices, laboratories or manufacturing facilities in West
Chester, Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis,
Minnesota. Cephalon's European headquarters are located in Maisons-Alfort,
France.
The company currently markets five proprietary products in the United States:
PROVIGIL(R) (modafinil) Tablets [C-IV], GABITRIL(R) (tiagabine hydrochloride),
ACTIQ(R) (oral transmucosal fentanyl citrate) [C-II], TRISENOX(R) (arsenic
trioxide) injection, VIVITROL(TM) (naltrexone for extended-release injectable
suspension) and numerous products internationally. Full prescribing information
on its U.S. products is available at http://www.cephalon.com/ or by calling
1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
guidance, including the impact of the FDA's action on the SPARLON sNDA on sales
and earnings guidance for 2006 and the outlook for strong earnings growth in
2007; and other statements regarding matters that are not historical facts. You
may identify some of these forward-looking statements by the use of words in the
statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: media, Robert Grupp, +1-610-738-6402, or rgrupp@cephalon.com ,
or investors, Robert (Chip) Merritt, +1-610-738-6376, or
cmerritt@cephalon.com , both of Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
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August 9, 2006 Wednesday 7:45 PM Eastern Time
CEPH: Hot Stocks
LENGTH: 165 words
19:45 EDT Cephalon-CEPH says FDA says Sparlon is not approvable, will not pursue
development - CEPH announced Wednesday day that it has received a letter from
the U.S. Food and Drug Administrationstating that the company's supplemental new
drug application (sNDA) for SPARLON (modafinil) Tablets [C-IV], a proprietary
dosage form of modafinil for the treatment of attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, is not approvable. In consideration
of the FDA's decision, the company has determined that it will not pursue
further development of Sparlon.
As of Saturday, 08-05-2006 23:59, the latest Comtex SmarTrend(SM) Alert, an
automated pattern recognition system, indicated an UPTREND on 06-30-2006 for
CEPH @ $59.83. For more information on Comtex SmarTrend® Alert, contact your
market data provider or go to CSTADirect.com SmarTrend is a registered trademark
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Theflyonthewall.com
This content is provided to LexisNexis by Comtex News Network, Inc.
August 9, 2006 Wednesday 7:45 PM Eastern Time
CEPH: Hot Stocks
LENGTH: 165 words
19:45 EDT Cephalon-CEPH says FDA says Sparlon is not approvable, will not pursue
development - CEPH announced Wednesday day that it has received a letter from
the U.S. Food and Drug Administrationstating that the company's supplemental new
drug application (sNDA) for SPARLON (modafinil) Tablets [C-IV], a proprietary
dosage form of modafinil for the treatment of attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, is not approvable. In consideration
of the FDA's decision, the company has determined that it will not pursue
further development of Sparlon.
As of Saturday, 08-05-2006 23:59, the latest Comtex SmarTrend(SM) Alert, an
automated pattern recognition system, indicated an UPTREND on 06-30-2006 for
CEPH @ $59.83. For more information on Comtex SmarTrend® Alert, contact your
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Clinical Neurology News
July 2006
Sleep Medication Improves Cognition, Mood in Brain Tumor Patients
BYLINE: Fran Lowry, Orlando Bureau
SECTION: Pg. 6 Vol. 2 No. 7 ISSN: 1553-3212
LENGTH: 417 words
ATLANTA - Modafinil, a medication commonly used to treat sleep disorders,
improves cognitive function, fatigue, and depression in adult brain tumor
patients, according to results of a pilot study presented at the American
Society of Clinical Oncology.
"Patients with brain cancer develop neurobehavioral dysfunction and fatigue
that seriously compromise their quality of life. Modafinil has been used to
treat the fatigue associated with multiple sclerosis, Parkinson's disease,
stroke, and HIV infection, and we decided to see if it would be of help in this
medically fragile patient population," said Thomas A. Kaleita, Ph.D., of the
department of psychiatry at the University of California, Los Angeles.
In comparison with baseline measures, self-reported test scores in cognitive
abilities, mood, and fatigue improved by an average of 21%, 35%, and 47%,
respectively, after 8 weeks of modafinil therapy. All improvements were
statistically significant, with P values less than .0001, Dr. Kaleita reported.
The study included 30 patients aged 21-65 years old with primary malignant
and nonmalignant tumors. Eighteen patients had high-grade gliomas, 10 had
low-grade gliomas, 1 had meningioma, and 1 had CNS lymphoma. All patients were
treated with neurosurgical resection and radiotherapy, and some patients also
received chemotherapy.
After treatment patients were randomized, in a double-blind fashion, to 200
mg or 400 mg of modafinil per day for 3 weeks. After a 1-week washout period,
the study was extended for an 8-week open-label phase, in which patients were
given modafinil at what was deemed to be their optimal dose, which ranged from
50 mg to 600 mg per day, Dr. Kaleita explained.
There was a lack of response in three patients, which Dr. Kaleita attributed
to the size of the tumor or psychological factors. The drug was "generally well
tolerated," he added; no serious adverse events were reported.
The most common side effects were headache in 42% of patients (which was "not
surprising in this patient population," Dr. Kaleita noted), insomnia, dizziness,
and nausea. These generally resolved after the dose of modafinil was adjusted.
"We find these preliminary results from this small study very encouraging,
because they show that it is possible to improve the quality of life in people
with brain cancer. Our next step is to determine long-term outcomes and verify
that modafinil does not create a tolerance or loses its efficacy over time,"
said Dr. Kaleita.
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The Leader-Post (Regina, Saskatchewan)
June 29, 2006 Thursday
Final Edition
Scientists working on sleep/wake equation
BYLINE: Ed Willett, Special to The Leader-Post
SECTION: ARTS & LIFE; Science; Pg. A6
LENGTH: 686 words
Do you have trouble falling asleep?
Do you have trouble waking up?
By one estimate, 75 per cent of adults have some kind of sleep problem every
week, so it's not surprising some people use artificial means to both get to
sleep and to wake up. According to a 1998 study from the Henry Ford Health
Sciences Research Institute in Detroit, 13 per cent of adult Americans had used
alcohol to get to sleep in the previous year, and 18 per cent had used sleeping
pills.
On the flip side, plenty of people try to keep themselves awake after a
sleepless night by the use of stimulants such as caffeine or nicotine. Sometimes
they're the same people, trapped in a "stimulant-sedative loop."
It would be wonderful if we could do away with pharmaceutical sleep aids or
stimulants altogether--but that seems unlikely. Instead, as a recent article in
New Scientist magazine makes clear, scientists are working hard to come up with
less damaging and more effective wake-you-up and put-you-to-sleep pills.
Most sleeping pills currently on the market work (as does alcohol) by making
neurons in the brain more sensitive to a neurotransmitter called GABA, what New
Scientist called "the brain's all-purpose dimmer switch."
However, the resulting sleep is short on the most restful "slow-wave" stage of
sleep. A new drug called gaboxadol, on the other hand, which could be on the
market next year, is a "slow-wave sleep promoter." There's at least one other in
the works. The hope is these drugs can make a relatively short period of sleep
more restful by filling it up with slow-wave sleep: they're power-nap pills, as
it were.
There are several other new approaches in the works for sleeping pills. One from
Japan called Rozerem, which appeared last year, mimics the effect of the hormone
melatonin, which promotes sleep.
Meanwhile, on the more stimulating side of the sleep/wake equation, there's even
more action, not least because the military has a strong interest in keeping
personnel awake and alert.
One stimulant that's been on the market for about seven years now is modafinil.
It's marketed for the treatment of sleep disorders such as narcolepsy, but it
has also become popular as a "lifestyle" drug because it can keep you awake
without apparent side effects. (It's called a "eugeroic," which means "good
arousal" in Greek.)
Modafinil's effects are so subtle most people aren't even aware of them -- they
just don't think about being tired. People taking it for medical reasons just
take enough to get through the day. The U.S. military has experimented with
sequential doses, and found it works for about 48 hours. After that, sleep is
required -- but rather than needing 16 hours of sleep after staying awake for
48, modafinil users catch up just fine with about eight.
Another drug in development, currently called CX717, successfully kept 11 rhesus
monkeys at Wake Forest University in Winstom-Salem, North Carolina, awake for 36
hours -- after which they actually performed better on short-term memory and
general alertness test than undrugged monkeys did after normal sleep! A test on
humans showed that the drug could reverse the cognitive decline that you'd
normally expect after 24 hours of sleep deprivation.
CX717 is an ampakine, a type of drug that increases brain activity by enhancing
the action of glutamate, the brain's main excitatory neurotransmitter.
Within a decade or two, we may be able to structure our sleep/wake cycle to suit
our lifestyles: staying awake when we need to, sleeping when it suits us. We
might be able to, say, stay awake for 22 hours and get all the rest we need in
just two.
There may be long-term effects to messing with the natural sleep-cycle, even
with these new, safer drugs, that we don't know about yet.
But in a world where people are already buying modafinil from online pharmacies
just so they can party longer on weekends, it seems inevitable that the age-old
cycle of 16 hours awake, eight hours asleep is about to become a dusty old
relic, stored permanently beneath the bed of history.
- Willett is a Regina freelance writer. E-mail comments or questions to
edward@edwardwillett.com.
LOAD-DATE: June 29, 2006
LANGUAGE: ENGLISH
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Inc.
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366 of 998 DOCUMENTS
Cancer Drug News
Pharmaceuticals
June 15, 2006
Modasomil improves neurobehavioural dysfunction and fatigue in adult patients
with brain tumours
LENGTH: 403 words
According to data presented at the 42nd Annual Meeting of the American Society
for Clinical Oncology (ASCO), held from 2nd to 6th June in Atlanta, GA, a
University of California , Los Angeles, study has found that Cephalon 's drug,
Modasomil ( modafinil ), which is generally used to treat sleep disorders, can
enhance the quality of life in patients with brain cancer by improving cognitive
functions, mood and fatigue levels, with a low incidence of negative side
effects. The 30 patients in the study had a variety of brain tumour types, and
most were categorised as having severe attention, memory and fatigue problems.
All of the patients had received some combination of neurosurgery, radiation
therapy and chemotherapy treatments, and several were receiving chemotherapy
whilst participating in the study.
The first part of the study was double-blind and patients were randomised
between two different dosage levels of the drug for three weeks. After a
one-week period in which patients did not receive the drug at all, there was an
eight-week open-label phase in which all patients received modafinil at what was
determined to be each patients optimal dose, which varied between 50 and
600mg/day. Patients were evaluated at specified times with various measures,
including standardised tests of concentration and attention, fatigue
self-ratings and a structured interview. In addition, patients received
comprehensive neurological examinations at specified times as well as brain
MRIs, which were performed before, during and after completion of this
therapeutic trial. Comparing patient scores before they started taking modafinil
to their scores after they had been on it for two to three months, the majority
of subjects exhibited clinically meaningful improvements in all areas. Test
scores in cognitive abilities improved by an average of 21 per cent, mood
improved by 35 per cent and fatigue improved by 47 per cent. The site of the
tumour or psychological factors were believed to be responsible for a lack of
response to the drug in three patients. Modafinil was generally well tolerated
and there were no serious adverse events. The most common side effects were
headache (42 per cent), insomnia (26 per cent), dizziness (23 per cent) and
nausea (13 per cent). These side effects were considered mild-to-moderate in
severity and typically resolved after adjustments in dose and scheduling of
medication.
LOAD-DATE: June 15, 2006
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Jiji Press Ticker Service
June 13, 2006 Tuesday 6:32 PM JST
Takeda to Sell Cephalon's Wake-Promoting Agent in U.S.
LENGTH: 183 words
DATELINE: Osaka, June 13
Japan's Takeda Pharmaceutical Co. said Tuesday that Takeda Pharmaceutical North
America Inc., a U.S. unit, and U.S. drug maker Cephalon Inc. will jointly
promote Cephalon's Provigil, a wake-promoting agent, in the United States.
In July, 500 Takeda sales representatives will begin promoting Provigil, or
modafinil, to primary care physicians and other appropriate health care
professionals in the United States.
The copromotion agreement will run for three years with an annual option to
renew.
Cephalon, based in Frazer, Pennsylvania, will pay the Takeda unit based in
Lincolnshire, Illinois, a royalty based on certain sales criteria for the
product.
Modafinil is the first and only medication in a new class of wake-promoting
agents believed to work selectively through the brain's sleep/wake centers to
activate the cortex of the brain, Cephalon said.
The medication has been approved in more than 20 countries and is available
under several brand names including Provigil.
In 2004, the U.S. Food and Drug Administration approved Provigil for improving
wakefulness in patients with excessive sleepiness.
LOAD-DATE: June 13, 2006
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UPI
June 7, 2006 Wednesday 4:16 PM EST
Analysis: Sleep drug has brain-tumor use
BYLINE: ED SUSMAN
LENGTH: 611 words
DATELINE: ATLANTA, June 7
A drug often prescribed to help people overcome drowsiness caused by shift work
or other conditions appears to improve depression, fatigue and difficulty in
maintaining attention to the activities of daily living that often accompanies
people battling brain cancer.
While most cancers that arise in the brain are incurable and are difficult to
treat, recent advances with precise surgery, new drugs and devices that actually
can be placed in the brain to combat the disease have lengthened survival
considerably for people with these diseases.
At this week's American Society of Clinical Oncology meeting, researchers
described how they markedly improved quality of life of patients by
administering modafinil -- sold as Cephalon's Provigil -- a drug primarily used
to treat patients with narcolepsy -- a condition in which people suddenly fall
asleep at inappropriate times, and the lethargy that accompanies people who work
odd hours.
"We were able to see clinically meaningful outcomes in this trial," said Thomas
Kaleita, assistant professor of psychiatry at the University of California, Los
Angeles. In his trial of 30 individuals -- 19 men and 11 women -- statistically
significant improvement was seen in tests of mental acuity, in measurements of
depression and in tests of fatigue.
"The improvements that were seen in this trial were huge," said Jeff Sloan, a
researcher in oncology at the Mayo Clinic Comprehensive Cancer Center in
Rochester, Minn.
Sloan, who commented on the study at the ASCO meeting, said that the effect of
the treatments were likely to make meaningful differences in the lives of the
patients. The study was among hundreds presented to the 25,000 health care
professionals attending the sessions in Atlanta.
"This is very encouraging study," Suzan Streichenwein, a psychiatrist based in
West Palm Beach, Fla., told United Press International. "Oncologists are
concerned about quantity of life but equally important is the quality of life."
She said that often, these patients are so sluggish due to their medications and
disease, they can barely move around.
In the study, Kaleita administered several psychological tests to the patients.
The patients took between 50 milligrams of modafinil and 600 mg a day. He said
he saw across-the-board improvement. Cognitive abilities increased 21 percent,
mood improved by 35 percent, fatigue improved by 47 percent and depression
improved 43 percent.
All the changes from the start of the trial through 12 weeks of the study proved
to be highly statistically significant.
For example, in one test of fatigue levels, patients were asked to measure their
fatigue on a 0 to 10 scale with 10 representing extreme fatigue. They averaged a
score of "4" -- or moderate fatigue -- when they began the test. After 10 weeks
of modafinil, their average fatigue scores dropped by 3 points, indicating a 75
decline in fatigue, and after 12 weeks, there was an 83 percent decline in
scores.
Sloan said those fatigue scores really represent more than a doubling in how
well a patient feels, recognizing that this improvement occurred even while the
patient was struggling with brain cancer.
"The improvements with this drug are important," said Streichenwein, but she
cautioned that some dosages of modafinil used in the study are above that
normally prescribed for depression, and added that the drug is expensive.
Sloan said the studies show there is a complex, complicated system involved in
brain cancer and that fatigue plays a major role in a patient's well being.
"This study shows there is hope for people with brain cancer, and that there are
interventions that can improve quality of life," Kaleita said.
LOAD-DATE: June 8, 2006
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The Herald (Glasgow)
June 6, 2006
I WISH ... You make a wish. We find the people who could make it happen;
THIS WEEK: I wish I could live without sleep
BYLINE: James Morgan
SECTION: TUESDAY; Pg. 11
LENGTH: 290 words
Sleeping is a pleasure. I want more not less.
That's only because you're tired. What if you could party all night and wake up
the next morning feeling alert and refreshed? A new drug being developed will
make two hours' sleep feel like a full night's rest. After a late night in the
office, or on the town, you pop the pill before bedtime and wake up two hours
later feeling fully recovered.
Two hours? Come on, Even Margaret Thatcher needed four.
Wake up. There are already thousands of high-fliers in the US who use a new
stimulant - modafinil - to get by on four hours a night. Modafinil users report
up to 48 hours of continuous wakefulness without any ill effects, and,
afterwards, only need eight hours to sleep the tiredness off. Officially
prescribed only for "medical" sleepiness, it is fast becoming a lifestyle drug.
Sales reached GBP330m in 2005. Now its creators, Cephalon, are working on a
successor, armodafinil, which would halve that to just two hours a night. Both
drugs are known as "eugeroics", meaning "good arousal" in Greek. Basically, they
block the actions of the neurotransmitters dopamine and noradrenaline.
Isn't it dangerous to disobey our body's natural circadian rhythms?
Many of us already do, by relying on generic stimulants such as caffeine and
sleeping pills. So why not, say some sleep experts, develop more precise drugs?
There are no side effects yet reported for modafinil, and the race is on to
develop even more powerful sleep-control drugs. The US military is funding
development of another stimulant, CX717, which could keep soldiers awake for 72
hours. Then there's gaboxadol, a pill that delivers the ultimate power nap by
stimulating deep, healing "long-wave" sleep over shallow short-wave slumber.
LOAD-DATE: June 6, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: NEWSPAPER
JOURNAL-CODE: GHERLD
Copyright 2006 Newsquest Media Group
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370 of 998 DOCUMENTS
The Sunday Times (London)
June 4, 2006
No 10 scientist urges brain pills for all
BYLINE: David Cracknell and Steven Swinford
SECTION: HOME NEWS; News; Pg. 3
LENGTH: 578 words
SMART drugs to make people think faster, improve their memory and reduce
tiredness will be commonplace within 20 years, according to the government's
chief scientific adviser.
Sir David King told ministers at a presentation in Downing Street that a new
generation of "recreational psychoactive substances" could be given to healthy
people to enhance their lives.
He said that brain enhancing chemicals could also "revolutionise" treatment for
mental disorders and create new treatments to fight drug addiction.
King's report adds to calls from scientists for the removal of restrictions on
"cognitive enhancers" which have been dubbed "cosmetic neurology" or "nip and
tuck" for the mind.
It also cements King's reputation as an increasingly influential figure in the
government -a civil servant who is unafraid to speak his mind on topics ranging
from climate change to drought and drugs.
Ritalin and Modafinil, the first generation of mind enhancing drugs, were
originally intended to treat disorders but have since been adopted by people
from across the social spectrum because of their ability to enhance performance.
Ritalin was originally intended as a treatment for children and adults with
hyperactivity problems, but has since been adopted by students to help them to
concentrate. A study in America last year revealed that 20% of healthy American
college students use Ritalin before exams.
Modafinil is generally prescribed for the treatment of narcolepsy, a condition
which causes people suddenly to fall asleep. It is now becoming popular for its
ability to help people to think clearly and make decisions when tired.
Scientists are keen to see restrictions removed on more drugs to make them
available without prescription.
Dr Andrea Malizia, a consultant senior lecturer in the Department of
Psychopharmacology at Bristol University, is calling for Donepezil, an
Alzheimer's treatment, to be more available. Donepezil has a "remarkable impact"
on a wide range of functions, including memory, concentration and the ability to
learn.
"The potential for these drugs is enormous. People already buy vitamins and take
caffeine to improve mental functions but these drugs will offer a whole new
dimension," said Malizia.
"Studies have shown that people who take these drugs are able to memorise more
words than they normally could -and increase their general brainpower.
"We have used them to treat mental disease with great effect, but there is
obviously the market for healthy people to take them just to get smarter."
Other scientists remain concerned about smart drugs. Dr Paul Howard-Jones,
neuroscience and education network co-ordinator at Bristol University, said that
the drugs needed to be carefully regulated.
"The (smart) pills are likely to be available to the general public in a few
years. But we do not know how they will be regulated -it may be that they are
only sold on prescription, or it may be that they are sold on supermarket
shelves like vitamin pills," he said.
"There could be restrictions placed on their sale, but that might mean people
buy them illegally. I would call on people to start discussing their impact
before they start causing tremendous problems in society."
This concern was also raised by King during his cabinet briefing. "Should we
change regulatory structures to enable new procedures in non-medical
psychoactive substances?" he said.
"Are 'cognitive enhancers' a great market for social opportunity or
destabilising and divisive?"
LOAD-DATE: June 4, 2006
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Clinical Psychiatry News
June 2006
Panel Cites Potential for Severe Rash; Stalls Modafinil for Children
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pg. 7 Vol. 34 No. 6 ISSN: 0270-6644
LENGTH: 798 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee said
modafinil is not safe for treating ADHD in children and adolescents by a 12-1
vote, although committee members unanimously agreed the drug was effective for
that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often attributable to
a hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
In a group of 933 children and adolescents exposed to the drug during trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of
1.29%, said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products.
The panel's discussion focused on one case that seemed most likely to be
SJS-indicating a 1 in 1,000 risk. But they weren't certain that was the true
risk.
Dr. Bigby and Dr. Mannheim said more cases could occur once modafinil
(Provigil) is more widely used--even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19, there could be 500-3,250 cases of EM or
SJS, and 25-488 deaths, Dr. Mannheim said.
The dichotomy between postmarketing experience and the trial data prompted
the FDA to seek its advisers' input, said Dr. Robert J. Temple, director of the
FDA's office of medical policy.
The FDA usually follows the advice of its panels.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily.
The primary outcome was the total score on the school ADHD rating scale. In
all three trials, children taking modafinil had a more significant drop in
scores than those taking placebo. The total score for modafinil recipients was
close to the normative score for a 10-year-old male, according to a statement
made by Cephalon.
Panelists did not dispute the drug's efficacy, although many said it would
not be a first-line choice.
Lesley Russell, Cephalon's senior vice president of worldwide clinical
research, said modafinil offers clinicians an alternative, especially when
children don't respond to other marketed drugs.
But Dr. Temple said that even though it's plausible that modafinil might work
in nonresponsive children, the company had not proved that. "The mere fact that
people given a second drug respond after failing to respond to the first tells
you nothing at all."
According to a company statement, modafinil may be less addictive and less
apt to be diverted because it does not offer a "high" to recreational users.
Jeffrey L. Vaught, executive vice president of research and development at
Cephalon, said the drug is not water soluble and is not stable at high heat,
which makes it difficult to crush for injection or smoke. Studies show that
modafinil does not activate reward centers, and that it does not cause release
of dopamine in vitro or in vivo.
The Drug Enforcement Administration has deemed modafinil a schedule IV drug;
other stimulants used to treat ADHD, such as Ritalin, are schedule II.
Despite potential advantages, the panel did not want modafinil to be marketed
for children yet.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
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Hindustan Times
May 30, 2006 Tuesday 11:23 AM EST
Amphetamine salts most effective for treating ADHD
BYLINE: Hindustan Times
LENGTH: 264 words
DATELINE: Washington
Washington, May 30 -- Stimulant medications, such as mixed amphetamine salts
(MAS) and methylphenidates are significantly more effective than nonstimulant
ADHD medications or novel stimulants, such as modafinil, in the treatment of
children with attention-deficit/hyperactivity disorder (ADHD).
This conclusion is based on a meta-analysis of 29 controlled-treatment studies
representing the past 25 years of research involving nearly 4,500 children with
ADHD presented recently at the 2006 American Psychiatric Association meeting in
Toronto, Canada.
Among stimulant medications classes, long-acting mixed amphetamine salts (MAS
XR) and immediate-release mixed amphetamine salts showed a similar level of
efficacy to short- or long-acting methylphenidates. The effectiveness of short-
and long-acting stimulants did not differ from one another.
"The larger effect sizes we calculated for stimulant ADHD medications, compared
to nonstimulants or the novel stimulant modafinil, leads us to conclude that
amphetamine and methylphenidate based stimulant medications are more effective
in treating symptoms of ADHD," said Stephen V. Faraone, Ph.D., lead researcher
and director of child and adolescent psychiatry at SUNY Upstate Medical
University.
The researchers compared study outcomes using effect sizes, a commonly used,
standard statistical measure to determine the magnitude of a particular effect
resulting from an intervention, such as a drug used on a population,
irrespective of the population size.
Published by HT Media Ltd. with permission from Asian News International.
LOAD-DATE: June 1, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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UPI
May 30, 2006 Tuesday 5:36 PM EST
Stimulant drugs most effective for ADHD
LENGTH: 276 words
DATELINE: WASHINGTON, May 30
Stimulants are better than non-stimulants or novel stimulants for children with
attention-deficit/hyperactivity disorder.
That's the finding of a new study recently released at the 2006 meeting of the
American Psychiatric Association in Toronto.
Stephen Faraone and colleagues at SUNY Upstate Medical University conducted a
meta-analysis of 29 double-blind, placebo-controlled studies on the
effectiveness of ADHD medication in children who were treated during the last 25
years. The studies enrolled nearly 4,500 subjects.
The team found that stimulant medications -- such as mixed amphetamine salts and
methylphenidates -- treated the symptoms of ADHD much more effectively than
either non-stimulants or novel stimulants.
Fifteen medications were tested and 17 measures of ADHD symptoms were reviewed,
including hyperactivity, inattentiveness, impulsiveness and oppositional
behavior.
The non-stimulant/novel stimulant drugs involved were atomoxetine, bupropion,
modafinil and desipramine.
The analysis used effect sizes, a standard statistical measure, to determine
each drug's usefulness. Effect sizes are usually categorized as small (0.2),
medium (0.5) and large (0.8).
After adjusting for the influence of individual study designs, the effect size
was calculated based on total ADHD scores.
Long- and short-acting stimulant medications had the largest effect size (0.83
and 0.9, respectively), followed by non-stimulants/modafinil-based stimulants (E
= 0.62).
Statistically significant differences in effect size occurred between
non-stimulants/modafinil-based stimulants and both short-acting stimulants (p =
0.002) and long-acting stimulants (0.004).
LOAD-DATE: May 31, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 U.P.I.
All Rights Reserved
374 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
May 26, 2006
Mixed amphetamine salts may be most effective in treating ADHD in youths
LENGTH: 444 words
Stimulant medications, such as mixed amphetamine salts and methylphenidate s are
significantly more effective than non-stimulant attention deficit hyperactivity
disorder (ADHD) medications or novel stimulants, such as modafinil , in the
treatment of children with the disorder. This conclusion is based on a
meta-analysis that was presented at the Annual Meeting of the American
Psychiatric Association, held from 20th to 25th May, in Toronto, Canada. For the
analysis, Dr Stephen V Faraone, lead researcher and director of child and
adolescent psychiatry at SUNY Upstate Medical University, and his colleagues
used data from 29 treatment studies of 4,465 children with ADHD, with an average
age of ten years, published during or after 1980. Designs for all of the studies
were randomised and double-blind, with placebo controls that lasted for two or
more weeks in populations diagnosed with ADHD, as defined using criteria from
the DSM-IIIR or DSM-IV.
This study was supported by Shire , whose product, Adderall XR (mixed
amphetamine salts), is indicated for the treatment of ADHD. The analysis
included 15 drugs using 17 different outcome measures of ADHD symptoms,
including hyperactive, inattentive, impulsive or oppositional behaviour. The
most commonly-identified treatments included both methylphenidate and
amphetamine compounds. Non-stimulant drugs included in the analysis were Eli
Lilly 's Strattera ( atomoxetine ), bupropion , modafinil and desipramine .
Among stimulant medication classes, long-acting mixed amphetamine salts and
immediate-release mixed amphetamine salts showed a similar level of efficacy to
short- or long-acting methylphenidates. The effectiveness of short- and
long-acting stimulants did not differ from one another. The researchers compared
study outcomes using effect sizes. After adjusting for the influence of
individual study design features, effect size was calculated based on Total ADHD
scores. Long- and short-acting stimulant medications showed the largest effect
size among all medications (E=0.83 and 0.9, respectively), followed by
non-stimulant or modafinil-based stimulants medications (E=0.62). Statistically
significant differences in effect size occurred in comparisons between
non-stimulant/modafinil-based stimulant medications and long-acting (p=0.004),
as well as short-acting, stimulants (p=0.002). According to Faraone, the larger
effect sizes that the researchers calculated for stimulant ADHD medications,
compared to non-stimulants or the novel stimulant, modafinil, leads them to
conclude that amphetamine and methylphenidate-based stimulant medications are
more effective in treating symptoms of ADHD.
LOAD-DATE: May 26, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
375 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
May 26, 2006
Mixed amphetamine salts may be most effective in treating ADHD in youths
LENGTH: 444 words
Stimulant medications, such as mixed amphetamine salts and methylphenidate s are
significantly more effective than non-stimulant attention deficit hyperactivity
disorder (ADHD) medications or novel stimulants, such as modafinil , in the
treatment of children with the disorder. This conclusion is based on a
meta-analysis that was presented at the Annual Meeting of the American
Psychiatric Association, held from 20th to 25th May, in Toronto, Canada. For the
analysis, Dr Stephen V Faraone, lead researcher and director of child and
adolescent psychiatry at SUNY Upstate Medical University, and his colleagues
used data from 29 treatment studies of 4,465 children with ADHD, with an average
age of ten years, published during or after 1980. Designs for all of the studies
were randomised and double-blind, with placebo controls that lasted for two or
more weeks in populations diagnosed with ADHD, as defined using criteria from
the DSM-IIIR or DSM-IV.
This study was supported by Shire , whose product, Adderall XR (mixed
amphetamine salts), is indicated for the treatment of ADHD. The analysis
included 15 drugs using 17 different outcome measures of ADHD symptoms,
including hyperactive, inattentive, impulsive or oppositional behaviour. The
most commonly-identified treatments included both methylphenidate and
amphetamine compounds. Non-stimulant drugs included in the analysis were Eli
Lilly 's Strattera ( atomoxetine ), bupropion , modafinil and desipramine .
Among stimulant medication classes, long-acting mixed amphetamine salts and
immediate-release mixed amphetamine salts showed a similar level of efficacy to
short- or long-acting methylphenidates. The effectiveness of short- and
long-acting stimulants did not differ from one another. The researchers compared
study outcomes using effect sizes. After adjusting for the influence of
individual study design features, effect size was calculated based on Total ADHD
scores. Long- and short-acting stimulant medications showed the largest effect
size among all medications (E=0.83 and 0.9, respectively), followed by
non-stimulant or modafinil-based stimulants medications (E=0.62). Statistically
significant differences in effect size occurred in comparisons between
non-stimulant/modafinil-based stimulant medications and long-acting (p=0.004),
as well as short-acting, stimulants (p=0.002). According to Faraone, the larger
effect sizes that the researchers calculated for stimulant ADHD medications,
compared to non-stimulants or the novel stimulant, modafinil, leads them to
conclude that amphetamine and methylphenidate-based stimulant medications are
more effective in treating symptoms of ADHD.
LOAD-DATE: May 29, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
376 of 998 DOCUMENTS
PR Newswire US
May 24, 2006 Wednesday 4:00 PM GMT
Mixed Amphetamine Salts Most Effective in the Treatment of ADHD in Youths
Reports the SUNY Upstate Medical Center;
Analysis of data from nearly 4,500 children presented at the 2006 American
Psychiatric Association Meeting
LENGTH: 1123 words
DATELINE: TORONTO May 24
TORONTO, May 24 /PRNewswire/ -- Stimulant medications, such as mixed
amphetamine salts (MAS) and methylphenidates are significantly more effective
than nonstimulant ADHD medications or novel stimulants, such as modafinil, in
the treatment of children with attention-deficit/hyperactivity disorder (ADHD).
This conclusion is based on a meta-analysis of 29 controlled-treatment studies
representing the past 25 years of research involving nearly 4,500 children with
ADHD presented today at the 2006 American Psychiatric Association meeting in
Toronto, Canada.
Among stimulant medications classes, long-acting mixed amphetamine salts (MAS
XR) and immediate-release mixed amphetamine salts showed a similar level of
efficacy to short- or long-acting methylphenidates. The effectiveness of short-
and long-acting stimulants did not differ from one another.
"The larger effect sizes we calculated for stimulant ADHD medications, compared
to nonstimulants or the novel stimulant modafinil, leads us to conclude that
amphetamine and methylphenidate based stimulant medications are more effective
in treating symptoms of ADHD," said Stephen V. Faraone, Ph.D., lead researcher
and director of child and adolescent psychiatry at SUNY Upstate Medical
University. "Our results should help physicians who have had to rely on
qualitative comparisons among published trials, along with their own clinical
experience, to draw conclusions about an ADHD medication's relative efficacy
because of largely absent direct head-to-head drug comparisons."
The researchers compared study outcomes using effect sizes, a commonly used,
standard statistical measure to determine the magnitude of a particular effect
resulting from an intervention, such as a drug used on a population,
irrespective of the population size. Effect sizes are generally categorized as
small (0.2), medium (0.5) and large (0.8). Standardized mean averages, or
effect sizes, for dependent measures in each study were computed by taking the
mean of the active drug group minus the mean of the placebo group and dividing
the result by the pooled standard deviation of the groups.
After adjusting for the influence of individual study design features, the
researchers calculated effect size based on Total ADHD scores. Long-acting and
short-acting stimulant medications showed the largest effect size among all
medications (E = 0.83 and E = 0.9 respectively), followed by nonstimulant or
modafinil based stimulants medications (E = 0.62). Statistically significant
differences in effect size occurred in comparisons between nonstimulant/
modafinil based stimulant medications and long-acting (p = 0.004) as well as
short-acting stimulants (p = 0.002).
For the analysis, Faraone and his colleagues used data from 29 double-blind,
placebo-controlled treatment studies of 4,465 children with ADHD, with an
average age 10 years, published during or after 1980. Designs for all of the
studies were randomized, double-blind with placebo controls that lasted for two
or more weeks in populations diagnosed with ADHD as defined using criteria from
the American Psychiatric Association's Diagnostic and Statistical Manual of
Mental Disorders, Revised Third Edition or Fourth Edition (DSM).
The analysis included 15 drugs using 17 different outcome measures of ADHD
symptoms, including hyperactive, inattentive, impulsive or oppositional
behavior. The most commonly identified treatments included both methylphenidate
and amphetamine compounds. Nonstimulant drugs included in the analysis were
atomoxetine, bupropion, modafinil and desipramine.
Shire US Inc. supported the study.
About ADHD
ADHD is a neurological brain disorder that manifests as a persistent pattern of
inattention and/or hyperactivity-impulsivity that is more frequent and severe
than typically observed in individuals at a comparable age and maturity level.
Because everyone shows signs of these behaviors at times, the behaviors must
appear early in life (before age 7 years) and continue for at least six months,
according to the ADHD diagnosis criteria as defined in DSM-IV-TR(R). Up to 65
percent of children with ADHD may still exhibit symptoms into adulthood. In
fact, approximately eight million American adults currently struggle with the
inattention, impulsivity and hyperactivity symptoms of ADHD.
Without an effective treatment program, the symptoms of ADHD may lead to
potentially serious consequences. A survey has shown that when compared to
adults without ADHD symptoms, adults with untreated ADHD were more than twice as
likely to have been arrested, 47 percent more likely to have received more than
one speeding ticket in the last year, twice as likely to have been divorced and
twice as likely to have held six or more jobs in the past decade.
Further, evidence suggests that many adults with untreated ADHD may be at risk
for other problems, including poor performance in the workplace and poor
self-image. Although there is no cure for ADHD, physicians and advocates are
finding ways to help people with the condition learn to adapt to their school,
home, social and work settings. ADHD usually can be successfully managed with
behavioral therapy, structured coping techniques and medication. Psychostimulant
medications are thought to stimulate areas of the brain that control attention,
impulses, and self-regulation of behavior, remain among the most successful
treatments for people with ADHD. Up to 70 percent of children with ADHD respond
positively to psychostimulants. Medication should be considered part of an
overall multi-modal treatment plan for ADHD.
For further information on ADHD please visit http://www.adhdsupport.com/ ,
http://www.chadd.org/ or http://www.nmha.org/ .
About SUNY Upstate Medical University
SUNY Upstate Medical University, located in Syracuse, N.Y., is a comprehensive
academic medical center featuring an aggressive program of biomedical research
with world experts in the areas of ADHD, neural coding, heart arrhythmias,
enzyme structure and function and human retro viruses. In addition to its
research program, the university features the colleges of Graduate Studies,
Health Profession, Medicine and Nursing, and a teaching hospital, University
Hospital that sees more than 130,000 patient visits annually.
Poster # NR 652: Comparing the Efficacy of Medications for ADHD Using
Meta-Analysis. Stephen V. Faraone, Ph.D.
CONTACT: Darryl Geddes of SUNY Upstate Medical Center, +1-315-464-4828;
or Priya Namjoshi, +1-212-601-8337, +1-609-213-8987 on-site, or Marion Glick,
+1-212-601-8273 or on site: +1-917-301-4206, both of Porter Novelli for Shire
Web site: http://www.adhdsupport.com/
http://www.chadd.org/
http://www.nmha.org/
SOURCE SUNY Upstate Medical Center
URL: http://www.prnewswire.com
LOAD-DATE: May 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
377 of 998 DOCUMENTS
The Age (Melbourne, Australia)
May 9, 2006 Tuesday
First Edition
Anti-sleep drug use on the rise;
Fears pill may fuel '24-hour lifestyle'
BYLINE: MELISSA FYFE HEALTH EDITOR
SECTION: NEWS; Pg. 7
LENGTH: 495 words
AUSTRALIAN doctors are increasingly prescribing an anti-sleep pill that has
become a lifestyle drug in Britain and the US.
Modafinil, a stimulant designed to treat sufferers of narcolepsy - the
uncontrolled desire for sleep - has been available in Australia since 2002. But
anecdotal reports suggest doctors are increasingly prescribing it to people who
simply want to stay awake for longer.
In the US, the drug is now prescribed for shift workers.
Figures from Medicare Australia show doctors are writing more prescriptions for
modafinil, also known as Modavigil. There were 289 prescriptions written last
year and 224 in the year to date. No figures are available for earlier years.
The drug's distributor in Australia, CSL Limited, said it had heard occasional
reports of doctors prescribing the drug "off label" (for purposes other than its
intended use).
"We don't want to see a situation where an employer is suggesting people use the
drug so they can spend longer on the job," said spokeswoman Rachel David. "It is
not appropriate in Australia . . . It could easily be used as a drug of
dependence."
She said CSL would monitor sales of the pill to ensure it did not become a
lifestyle drug.
Under Federal Government regulations, only specialist sleep doctors can
prescribe the drug.
The comments come as Monash University prepares to analyse data from a new study
on the effects of modafinil on mood, driving and intellectual performance.
Little is known about the drug - even how it works to promote wakefulness - and
the Monash study hopes to clarify the drug's psychological effects, especially
if it becomes popular, which most observers tip it will.
"If you have a drug that has all the good effects of things such as amphetamines
and coffee, but with not as many side effects, quite a lot of people are going
to want to get a hold of it," said Clint Gurtman, who is conducting the study at
Monash.
"With drug tests now for driving, people will want to steer away from illicit
drugs. Why wouldn't you go out and get a script for this sort of thing?"
The drug, which has been used in France for more than a decade, allows people to
survive on less sleep, but without the agitation or euphoria caused by
amphetamine-based drugs.
However, side effects include headaches and the possibility that it could
trigger a psychotic episode in people with bipolar disorder (manic depression).
The drug peaks after about three hours and is effective for 13 hours.
Mr Gurtman queried whether it was right to introduce a drug to counter fatigue.
"What are the implications if we are going to become a 24-hour society? If we
say people don't need sleep, what are going to be the negative consequences of
that?" he asked.
His supervisor, Associate Professor Jenny Redman, said there was a huge market
in drugs that could promote wakefulness.
Mr Gurtman said groups who could be interested in modafinil included truck and
taxi drivers, doctors, computer programmers, nightclubbers and shift workers.
LOAD-DATE: June 18, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 The Age Company Limited
All Rights Reserved
378 of 998 DOCUMENTS
The Philadelphia Inquirer
May 2, 2006 Tuesday
Business news in brief
SECTION: BRIEFS; Pg. D03
LENGTH: 1271 words
IN THE REGION
Phila. airport near top in passenger-traffic growth
Philadelphia International Airport led North America in 2005 in
passenger-traffic growth, and was outpaced among the world's 30 busiest airports
only by Beijing, a trade group said. A record 31.5 million passengers, 10.5
percent more than in 2004, got on or off flights at Philadelphia, making it the
15th-busiest U.S. airport and the 27th-busiest in the world, according to
statistics released by the Airports Council International - North America.
Beijing's traffic increased 17.5 percent last year compared with 2004, the
council said. Earlier, the airports group said that Philadelphia was the
ninth-busiest airport in the United States and the world last year in takeoffs
and landings, with a record 565,666 aircraft operations.- Tom Belden
Region's unemployment rate fell in March to 4.4%
The unemployment rate in the Philadelphia area fell two-tenths of a percentage
point, to 4.4 percent in March, the Pennsylvania Department of Labor and
Industry said. For the month, the number of unemployed people declined 4,300, to
131,400. Meanwhile, employment rose 10,000 to 2,822,700. In March last year, the
local jobless rate was 4.8 percent. The local area consists of Philadelphia,
Bucks, Delaware, Montgomery and Chester Counties in Pennsylvania; Burlington,
Camden, Gloucester and Salem Counties in New Jersey; New Castle County in
Delaware; and Cecil County in Maryland. In Philadelphia, the March jobless rate
was 6.4 percent, unchanged from February but down from 7.0 percent in March
2005.- Paul Schweizer
Cephalon gets initial OK for drug to treat sleepiness
Cephalon Inc. said U.S. regulators granted conditional approval to the Frazer
company to sell Nuvigil tablets to treat excessive sleepiness caused by certain
sleep disorders. The Food and Drug Administration withheld final approval until
Nuvigil's product label is made final, Cephalon said after the stock markets
closed. Modafinil, the active ingredient in Nuvigil, can cause skin rashes. The
FDA said, in an "approvable" letter for Nuvigil, that until regulators decide
the outcome of another experimental Cephalon drug, Sparlon, which contains
modafinil to treat attention deficit hyperactivity disorder in children, the FDA
will wait to make final Nuvigil's product label. The company's best-selling
sleep-disorder medicine, Provigil, contains modafinil and bears a label warning
of possible serious skin rashes.- Linda Loyd
Verticalnet to appeal Nasdaq's delisting notification
Verticalnet Inc. said it would appeal a delisting notification it received last
week from Nasdaq. The stock exchange told Verticalnet it was subject to
delisting from the Nasdaq Capital Market this Friday because Verticalnet shares
had not maintained the minimum $1 bid price required by Nasdaq rules.
Verticalnet said it expected its appeal to prevent delisting until it received a
hearing from Nasdaq's listing-qualifications panel. Among the proposals listed
in Verticalnet's proxy statement for its May 19 shareholder meeting is a request
to perform a reverse stock split. That would, in effect, raise the company's
share price while reducing the number of outstanding shares. Verticalnet's
shares closed yesterday at 37 cents, down 3 cents.- Akweli Parker
Rohm & Haas looking to make some acquisitions
Rohm & Haas Co. chief executive officer Raj L. Gupta said the company was
looking for acquisitions for the first time in several years. The Philadelphia
specialty-chemicals company could spend $400 million to $500 million a year on
companies that will boost its specialty-chemicals and electronics businesses,
Gupta said.- Bob Fernandez
Teva wins U.S. court ruling on generic Zocor
Teva Pharmaceutical Industries Ltd. said a U.S. court ruled in its favor,
sending the issue of exclusive marketing rights to make a generic form of Zocor,
the blockbuster cholesterol-lowering drug, back to federal regulators to
reconsider. The Food and Drug Administration had rejected a bid by Teva's Ivax
unit and Ranbaxy Laboratories Ltd. to receive a six-month period of marketing
exclusivity to sell Zocor when the drug's main patent expired in June.
Israel-based Teva has its U.S. headquarters in North Wales, Montgomery County. A
six-month period of marketing exclusivity is key to generic companies, which can
charge higher prices before other generic competitors can sell their own generic
versions of a brand-name drug. Merck has an agreement with Dr. Reddy's
Laboratories Ltd. to sell an "authorized" generic version of Zocor when the
Zocor patent expires. Teva's shares closed up $1.61, to $42.11, on the Nasdaq.
Merck shares were down 18 cents at $34.18 on the New York Stock Exchange.- Linda
Loyd
Cardiokine raises $50 million for clinical drug trials
Cardiokine Inc., a Philadelphia specialty-pharmaceutical company, announced it
had raised $50 million in venture financing to begin Phase 3 clinical trials for
its lead drug candidate, Lixivaptan. The financing brings to $87 million the
total amount raised from private-equity investors by Cardiokine, which is
developing treatments for congestive heart failure and has licensed Lixivaptan
from Wyeth. Cardiokine's latest financing was led by Advent Venture Partners and
Fidelity Biosciences, joined by Teachers' Private Capital.- Linda Loyd
Comcast makes deal with IGN Entertainment
Comcast Corp., Philadelphia, said it had signed an agreement with IGN
Entertainment to launch "Game Invasion," a package of high-speed Internet
service and gaming content. Customers who subscribe to Comcast's 8-megabit
Internet service, which costs $52.95 monthly, will get IGN premium gaming
content at no extra cost. IGN premium, whose Internet content includes TeamXbox
and FilePlanet, normally costs $120 yearly. Comcast also said it had completed
the purchase of Susquehanna Communications, the cable-television and
broadband-services division of Susquehanna Pfaltzgraff. Comcast paid about $540
million in cash, or $440 million after taking into account certain tax benefits,
for about 301,000 basic- and digital-cable customers and 86,000
high-speed-Internet customers. Comcast previously owned about 30 percent of
Susquehanna Communications. - Miriam Hill
Business group wins contract to provide training
The MidAtlantic Employers' Association, a membership organization representing
about 700 midsize companies in the area, landed an $80,000 contract to provide
human-resource training and organizational development for the Philadelphia
Workforce Development Corp. The Valley Forge association will develop workbooks
and provide facilitator guides for PWDC's employee-training programs.- Jane M.
Von Bergen
ELSEWHERE
Ford resumes work after fixing transmission problems
Ford Motor Co. resumed production at seven plants yesterday after fixing a
problem it discovered in its engine transmissions, Ford spokeswoman Anne Marie
Gattari said. Ford halted production at the plants late Thursday and continued
the shutdown all day Friday, idling about 15,000 workers.- AP
T-bill rates reach highest levels in more than five years
Interest rates on short-term Treasury bills rose in yesterday's auction to the
highest levels in more than five years. The Treasury Department auctioned $15
billion in three-month bills at a discount rate of 4.685 percent, up from 4.635
percent last week. An additional $14 billion in six-month bills was auctioned at
a discount rate of 4.780 percent, up from 4.735 percent last week. The discount
rates reflect that the bills sell for less than face value. For a $10,000 bill,
the three-month price was $9,881.57 while a six-month bill sold for $9,758.34.-
AP
LOAD-DATE: May 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 Philadelphia Newspapers, LLC
All Rights Reserved
379 of 998 DOCUMENTS
Internal Medicine News
May 1, 2006
Panel: Modafinil Not Safe for ADHD in Teens
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pgs. 36-37 Vol. 39 No. 9 ISSN: 1097-8690
LENGTH: 793 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee
declared that modafinil is not safe for treating ADHD in children and
adolescents by a 12-1 vote, although committee members unanimously agreed the
drug was effective for that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often due to a
hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
Among 933 children and adolescents exposed to the drug during trials, there
were 12 cases that could have been definite erythema multiforme (EM) or SJS,
early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of 1.29%,
said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products.
The panel's discussion focused on one case that seemed most likely to be
SJS-indicating a 1 in 1,000 risk. But they were not certain that was the true
risk.
Dr. Bigby and Dr. Mannheim said that more cases could occur once modafinil
(Provigil) is more widely used-even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off-label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19 (based on other stimulants' sales), there
could be 500-3,250 cases of EM or SJS, and 25-488 deaths, said Dr. Mannheim.
The dichotomy between the postmarketing experience and the trial data
prompted the FDA to seek its advisers' input, said Dr. Robert J. Temple,
director of the FDA's office of medical policy.
The FDA usually follows the advice of its panels.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily. The primary outcome was the total score
on the school ADHD rating scale. In all three trials, children taking modafinil
had a more significant drop in scores than those taking placebo. The total score
for modafinil recipients-just over 20-was close to the normative score for a
10-year-old male, according to a Cephalon statement.
Panelists did not dispute the drug's efficacy, although many said it would
not be a first-line choice.
Lesley Russell, Cephalon's senior vice president of worldwide clinical
research, said modafinil offers clinicians an alternative, especially when
children don't respond to other marketed drugs.
But Dr. Temple said that even though it's plausible that modafinil might work
in nonresponsive children, the company had not proved that.
"The mere fact that people given a second drug respond after failing to
respond to the first tells you nothing at all," he said.
According to a company statement, modafinil may be less addictive and less
apt to be diverted because it does not offer a "high" to recreational users.
Jeffrey L. Vaught, executive vice president of research and development at
Cephalon, said the drug is not water soluble and is not stable at high heat,
which makes it difficult to crush for injection or smoking. Studies have shown
that modafinil does not activate reward centers in the brain, and that it does
not cause release of dopamine in vitro or in vivo.
The Drug Enforcement Administration has deemed modafinil a schedule IV drug;
other stimulants used to treat ADHD, such as Ritalin, are schedule II.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2006 Elsevier Inc., International Medical News Group
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380 of 998 DOCUMENTS
PR Newswire US
May 1, 2006 Monday 8:45 PM GMT
Cephalon Receives Approvable Letter for NUVIGIL(TM) (armodafinil)
LENGTH: 1024 words
DATELINE: FRAZER, Pa. May 1
FRAZER, Pa., May 1 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that it has received an approvable letter from the U.S. Food and
Drug Administration (FDA) for NUVIGIL(TM) (armodafinil) Tablets. The company
submitted a new drug application (NDA) on March 31, 2005, seeking to market
NUVIGIL for the treatment of excessive sleepiness associated with narcolepsy,
obstructive sleep apnea/hypopnea syndrome (OSA/HS) and shift work sleep disorder
(SWSD). FDA approval of NUVIGIL is contingent upon finalizing the product
label.
"We are working closely with the FDA to move this application to an approval and
expand our offering of wake-promotion choices for patients," said Dr. Paul
Blake, Executive Vice President, Worldwide Medical and Regulatory Operations.
"Based on the clinical trials, NUVIGIL demonstrated a long duration of effect
throughout the waking hours and we are excited at the potential to offer broader
options to meet the needs of patients and physicians seeking treatment for
excessive sleepiness."
Armodafinil is a single-isomer formulation of modafinil, the active
pharmaceutical ingredient contained in PROVIGIL(R) (modafinil) Tablets [C-IV].
Cephalon submitted data from four double-blind, randomized, placebo-controlled
studies of NUVIGIL in patients with excessive sleepiness associated with either
narcolepsy, OSA/HS or SWSD to FDA for evaluation as part of the NDA. In these
studies, NUVIGIL was generally well tolerated, with a safety profile consistent
with that observed in studies of PROVIGIL. The most common adverse effects
observed included headache, nausea, dizziness, insomnia and anxiety.
As previously announced, the company submitted additional information to the FDA
related to a possible case of Stevens Johnson Syndrome associated with its
SPARLON(TM) (modafinil) application. In its NUVIGIL approvable letter, the FDA
indicated that the outcome of its review of this new information will be
addressed directly in the label for NUVIGIL.
About Excessive Sleepiness (Hypersomnolence)
Excessive sleepiness, medically known as hypersomnolence, is the primary symptom
-- and often the most debilitating feature -- experienced by the millions of
Americans who suffer from narcolepsy, OSA/HS, and SWSD. Despite this fact, it
is estimated that 50 to 90 percent of the time, health care professionals fail
to recognize that these patients are suffering from excessive sleepiness. The
defining characteristic of excessive sleepiness is a consistent inability to
stay awake and alert enough to safely and successfully accomplish tasks of daily
living. Persons experiencing excessive sleepiness who seek medical attention
typically complain of fatigue, tiredness, lapses of attention, lack of energy,
low motivation, difficulty concentrating, disrupted sleep, snoring or
difficulties at work.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. U.S. sites include the company's headquarters in Frazer,
Pennsylvania, and offices, laboratories or manufacturing facilities in West
Chester, Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis,
Minnesota. Cephalon's European headquarters are located in Maisons-Alfort,
France.
Cephalon currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II], and TRISENOX(R) (arsenic trioxide) injection. In
addition, VIVITROL(TM) (naltrexone for extended-release suspension) was recently
approved in the United States and is expected to be available in June 2006.
Cephalon also markets numerous products internationally. Full prescribing
information for Cephalon products in the United States is available at
http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products, interpretation of
clinical results, including the results of the clinical trials of NUVIGIL;
prospects for regulatory approval, including for final FDA approval of NUVIGIL;
manufacturing development and capabilities; market prospects for its products;
sales and earnings guidance; and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission.
Given these risks and uncertainties, any or all of these forward-looking
statements may prove to be incorrect. Therefore, you should not rely on any such
factors or forward-looking statements. Furthermore, Cephalon does not intend to
update publicly any forward-looking statement, except as required by law. The
Private Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com ,
or Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com ,
both of Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: May 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
381 of 998 DOCUMENTS
PSYCHIATRIC TIMES
May 1, 2006
FDA Committees Examine Concerns About Psychiatric Drugs Used by Children
BYLINE: Stephen Barlas
SECTION: WASHINGTON REPORT; Pg. 25
LENGTH: 1786 words
HIGHLIGHT: Concerns about the appropriate use of psychiatric medications in
children continue to be the subject of discussion by regulatory agencies. In
late 2004, the issues were possible suicidal ideation and suicide attempts as
side effects of selective serotonin reuptake inhibitors (SSRIs) and other
antidepressants. This past February, concerns arose about potential
cardiovascular effects of drugs used to manage attention-deficit/hyperactivity
disorder (ADHD). At the same time, questions remain about the effectiveness of
SSRIs for depression in children.
The FDA's Pediatric Advisory Committee met on March 22, a month after the Drug
Safety and Risk Management Advisory Committee first raised questions about
possible cardiovascular adverse effects caused by stimulants used to treat
children with ADHD. The Drug Safety Committee had voted 8 to 7 in February to
recommend that the FDA require drug companies selling stimulants to put a
black-box warning on the professional labeling, a measure the agency had
required in 2004 for labels of antidepressants.
The Pediatric Committee looked at a report from the FDA staff on adverse event
reports possibly related to 4 drugs, 1 of which was a
dextroamphetamine/amphetamine combination product (Adderall). In continuation of
a previous committee discussion of adverse events for the class of
methylphenidate products used to treat ADHD, the committee discussed
neuropsychiatric adverse events possibly related to other approved ADHD
medications. The committee received an update on efforts to better understand
cardiovascular adverse events possibly related to ADHD medications.
The FDA's Psychopharmacologic Drugs Advisory Committee met the following day to
examine the safety and efficacy of modafinil (Provigil) for ADHD in children.
Cephalon already markets modafinil as a wake-enhancing drug for patients with
sleep problems. The issue of possible cardiovascular effects and psychiatric
adverse events came up during this meeting too. Sheryl Williams, a spokeswoman
for Cephalon, said that modafinil has a different chemical structure from that
of the stimulants targeted by the drug safety committee. "There have never been
any sudden cardiac events associated with our product, even in patients with
obstructive sleep apnea who may have underlying cardiac problems."
Antidepressant effectiveness, treatment duration
Not only is the safety of psychiatric drugs taken by children a growing issue so
is their effectiveness. In a recent article in Biological Psychiatry,
researchers from the psychiatry department at The Johns Hopkins University
Medical School and Daniel Pine, MD, the head of pediatric mood and anxiety
research at the intramural program at the National Institute of Mental Health
(NIMH), discuss clinical trial data for SSRIs tested on children and
adolescents. The article states that there is "reasonably strong evidence for
efficacy of fluoxetine [Prozac]" and that "the efficacy of the remaining SSRIs
is modest at best."
The article's conclusion on fluoxetine is based on 4 clinical trials, including
1 (which showed no benefit) that was tossed out because of the small size of the
sample (40 adolescents). In the other 3 trials, the spread between the positive
effect of fluoxetine and that of a placebo was never more than 26 percentage
points. In 2 cases, the difference was 12 and 14 percentage points. The number
of children in the 3 trials was 96, 219, and 439, and none of the patients
participated for more than 12 weeks.
Three-month or shorter clinical trials with fewer than 500 participants are
typical of the evidence pharmaceutical companies submit to the FDA to prove
efficacy and an acceptable adverse- effects profile for already-approved drugs
and existing chemical entities that are seeking labels for new indications or
new methods of administration. Some drug companies "roll over" some of the
participants in those trials into open label trials, mostly to see how well
patients tolerate the drug over slightly longer periods (but never longer than 1
to 2 years and sometimes as little as 6 months).
In interviews with Psychiatric Times, Pine, whose formal title is chief of
developmental studies, mood and anxiety disorders program, NIMH, and Thomas
Laughren, MD, director, division of psychiatry products at the FDA, stated that
a 30 percentage point spread between drug and placebo was strong evidence of
efficacy. But both expressed some reservations about results from 12-week
clinical trials and emphasized that current efficacy and safety data on SSRIs
leave much to be desired. Pine, for example, noted that SSRI data in children
are much stronger for anxiety than for depression. "That is a point that people
haven't picked up on," he said. When asked why the spreads for SSRI
antidepressants are so narrow, Pine added, "That is the $64,000 question."
Laughren said it is more difficult to conduct reliable clinical trials with
antidepressants. "That is because we don't understand most psychiatric disorders
at a biological level," he explained. "All we have is the phenomenology of the
disease. It is not like some types of heart disease or cancer where you
understand the disease at the pathological level and have a better chance of
distinguishing between different subgroups of patients who might respond
differently to one drug or another."
Laughren compared the shakier SSRI efficacy data with those for ADHD drugs,
which include methylphenidate (Concerta, Ritalin) and amphetamines (Adderall
XR). He said it isn't unusual to see an ADHD drug trial in which 80% of those
taking the active drug improve while only 20% of those taking placebo improve.
"There is fairly robust evidence for this class of drugs," Laughren stated. "You
see a more predictable drug effect and less of a placebo effect."
Nevertheless, Laughren admitted, "There is only a limited amount you can learn
from a short-term clinical trial which lasts only a few weeks. You need
longer-term trials to learn about longer-term risks and also benefits."
In the case of Cephalon's application for an ADHD label for modafinil, the
company did 3 clinical trials, each lasting 9 weeks, in which 400 children aged
9 to 16 years were given progressively titrated doses of modafinil. The drug was
considered effective because the 300 children who were given a placebo showed a
mean 8-point improvement on the ADHD rating scale used in the study, while those
who took modafinil showed a mean improvement of 16 points.
But even for methylphenidate, which has been around since the 1950s, there have
been few clinical studies extending for a year or more and involving large
populations. There have not been enough dose-response tests, much less
brain-imaging testing, which looks at the effect of stimulants or
antidepressants on the brain development of children 10 or 20 years after the
fact.
Gerardo Torres, vice president, Central Nervous System Therapeutic Area at
Shire, maker of Adderall, which has been on the market since 1996, explained,
"We have not systematically looked at [that]. We have postmarketing
surveillance. If we picked up anything, we would begin to address it."
Pine called the lack of brain-imaging testing "a very legitimate question."
Laughren explained that there are impediments in some instances to longer, more
detailed clinical trials with children. For example, a parent of a severely
depressed child might be very hesitant to enroll him or her in a long-term
randomized trial in which there was the possibility the child would be receiving
a placebo. In addition, Laughren pointed out, the FDA has to weigh the benefits
of holding up a new medication-even if efficacy data are unimpressive-against
the costs of depriving those in need of relief from a debilitating condition.
Nonetheless, the FDA has pushed for some additional testing. Last October,
Laughren asked the Psychopharmacologic Drugs Advisory Committee whether the FDA
ought to require relapse prevention trials for antidepressants as a condition of
approval. These trials monitor successfully treated children after
antidepressants are discontinued to see whether the children experience a
relapse; the goal is to determine the optimal period for which a depressed child
should be taking an SSRI, a question that few clinical trials in children have
examined.
"How long do you need to use this drug? That is what we think really needs to be
explored," explained Laughren. "But everybody on the advisory committee said
'no,' it would be too burdensome to companies to require this prior to initial
approval." He added that, for adults at least, companies do usually conduct such
trials within a few years of initial approval of the drug.
While the members of the advisory committee are mostly academics, 8 of the 11
members had relationships with drug companies whose products could have been
affected by decisions the advisory committee made that day. Before the meeting
started, Karen M. Templeton-Somers, PhD, acting executive secretary, read off a
list of those members and their relationships. She noted that the advisory
committee's chairperson, Wayne Goodman, MD, works for 2 employers (the
University of Florida College of Medicine and the McKnight Brain Institute at
the University of Florida) that have 4 separate contracts-2 with firms funded at
less than $100,000 per year and 2 others with separate drug firms funded at
between $100,001 and $300,000 per year.
Goodman pointed out that those relationships pertained to contracts held by
other investigators in his department with a company developing a drug that
would be a competitor to selegiline (Emsam), the first transdermal patch
medication used for treating major depression. The committee voted to recommend
Emsam's approval on the second day of that October meeting, and the FDA approved
the drug on February 28, 2006. Emsam was developed by Somerset Pharmaceuticals,
Inc. In December 2004, Bristol-Myers Squibb and Somerset entered into an
agreement that provides Bristol-Myers Squibb with distribution rights to market
Emsam.
Goodman did not address whether he himself has contracts with companies like
Wyeth, for example, that oppose an FDA requirement on relapse prevention trials
for new psychiatric drugs for children. But he pointed out that he did vote in
favor of a suicidality black-box warning for antidepressants when that issue
came up in the advisory committee in 2004. He noted that this probably didn't
sit all that well with drug companies with whom he may have contracts. "I'm so
clean I am sterile," he said.
Laughren stated that the FDA is still thinking about "how to change things
because of all the controversy," which, he added, has dampened the interest of
industry in studying children." He explained that he knows of 1 situation in
which a company had positive clinical trial results with a drug tested for a
psychiatric condition in children but was unwilling to submit an application for
approval for fear of running into a public buzz saw.
Goodman added, "There is no question we need to do long-term clinical trials
with kids and psychiatric drugs." He said the companies, the FDA, and the NIMH
should pool their money and establish those trials.
http://www.psychiatrictimes.com/
Copyright © 2006 CMP Media LLC. All rights reserved.
LOAD-DATE: June 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
JOURNAL-CODE: PTM
Copyright 2006 CMP Media LLC
All Rights Reserved
382 of 998 DOCUMENTS
Skin & Allergy News
May 2006
FDA Panel: Modafinil Not Safe for ADHD in Children
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pg. 5 Vol. 37 No. 5 ISSN: 0037-6337
LENGTH: 852 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee said
modafinil is not safe for treating ADHD in children and adolescents by a 12-1
vote, although committee members unanimously agreed the drug was effective for
that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often due to a
hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
In a group of 933 children and adolescents exposed to the drug in trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of
1.29%, said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products.
The panel's discussion focused on one case that seemed most likely to be
SJS-indicating a 1 in 1,000 risk. But they weren't certain that was the true
risk.
Dr. Bigby and Dr. Mannheim said more cases could occur once modafinil
(Provigil) is more widely used, even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off-label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19 (based on other stimulants' sales), there
could be 500-3,250 cases of EM or SJS, and 25-488 deaths, said Dr. Mannheim.
The dichotomy between the postmarketing experience and the trial data
prompted the FDA to seek its advisers' input, said Dr. Robert J. Temple,
director of the FDA's office of medical policy.
The FDA usually follows the recommendations of its advisory panels.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily.
The primary outcome was the total score on the school ADHD rating scale. In
all three trials, children taking modafinil had a more significant drop in
scores than those taking placebo. The total score for modafinil recipients-just
over 20-was close to normal for a 10-year-old male, according to a Cephalon
statement.
Panelists did not dispute the drug's efficacy, although many said it would
not be a first-line choice.
Lesley Russell, Cephalon's senior vice president of worldwide clinical
research, said modafinil offers clinicians an alternative, especially when
children don't respond to other marketed drugs.
But Dr. Temple said that even though it's plausible that modafinil might work
in nonresponsive children, the company had not proved that. "The mere fact that
people given a second drug respond after failing to respond to the first tells
you nothing at all."
According to a company statement, modafinil may be less addictive and less
apt to be diverted because it does not offer a "high" to recreational users.
Jeffrey L. Vaught, executive vice president of research and development at
Cephalon, said the drug is not water soluble and is not stable at high heat,
which makes it difficult to crush for injection or smoking. Studies have shown
that modafinil does not activate reward centers in the brain, and that it does
not cause release of dopamine in vitro or in vivo.
Despite potential advantages, the panel did not want modafinil to be marketed
for children yet.
"I think we did err on the side of consumer protection," said Dr. Goodman.
In a statement after the meeting, Dr. Paul Blake, Cephalon's executive vice
president of worldwide medical and regulatory operations, said, "We are
obviously disappointed with the recommendation of the advisory committee. We
will continue our discussions with the FDA to determine the next steps in the
review of this drug application."
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: SANEWS
Copyright 2006 Elsevier Inc., International Medical News Group
All Rights Reserved
383 of 998 DOCUMENTS
St. Petersburg Times (Florida)
April 25, 2006 Tuesday
0 South Pinellas Edition
Narcolepsy pill may blunt cocaine craving
SECTION: NATIONAL; Pg. 6A
LENGTH: 554 words
DATELINE: WASHINGTON
The hottest topic in cocaine addiction is another drug: a medicine already sold
to wake up narcoleptics.
Hundreds of cocaine users are testing whether that legal pill, called modafinil,
could help them kick the addiction, and there's early evidence that it may.
In addition to easing cocaine's notorious cravings, modafinil also might counter
the damage that cocaine wreaks on users' brain circuits - damage that in turn
fuels the cycle of addiction.
That prospect has the National Institutes of Health spending $10.8-million
researching modafinil as a potential cocaine treatment. Results from the first
of three key clinical trials could arrive by year's end.
Scientists are cautious. But for Dr. Nora Volkow, director of the National
Institute on Drug Abuse, the narcolepsy medicine tops the list of potential
therapies. It may help restore proper function of a crucial brain chemical,
dopamine, that addiction hijacks.
And in describing why he's hopeful, one leading researcher recounts the man who
accused his drug dealer of selling bad coke before realizing modafinil had kept
him from getting high - and several other modafinil testers who told of flushing
cocaine down the toilet.
"I've been treating cocaine-addicted patients for something like 25 years, more,
and I've never heard of anybody throwing away cocaine," says Dr. Charles Dackis
of the University of Pennsylvania, who led a pilot study that suggested
modafinil more than doubled addicts' chances of going cocaine-free for at least
three weeks.
That study enrolled just 62 people, but the results were significant enough for
the NIH to fund research enrolling about 650 cocaine users to see if modafinil
really does work.
The main side effect so far: insomnia, not surprising as modafinil is sold today
to help narcolepsy patients fend off that neurologic disease's sudden sleep
attacks.
Close relationships slow
the effects of Alzheimer's
Patients with Alzheimer's disease who have rich social networks lose mental
ability more slowly and function better than those without such networks, a
large study found.
Maintaining close relationships with friends and relatives, being able to call
on others for help and meeting people regularly reduced the impact of
Alzheimer's, the study found. The disease appeared to cause as much damage to
the brains of patients who had many social ties, but it did not have the same
effect on behavior and functioning.
The study suggests that disease processes only partly explain how quickly
patients decline, said David A. Bennett, an Alzheimer's expert at Rush
University Medical Center in Chicago: "Some people can tolerate a lot of
pathology without losing their thinking ability, and others can have only a
little pathology and lose a lot."
The difference apparently lies in people's reserves - their ability to tolerate
stress and damage. "The extent of social networks, or something related to
social networks, provides some type of reserve which reduces the deleterious
effect of Alzheimer's disease pathology on cognitive abilities in old age,"
Bennett and a team of researchers wrote online this month in the journal Lancet
Neurology.
Bennett said that while the study could not say whether seeking out more social
ties could reduce the effects of dementia, "being socially engaged is good for
you for a whole host of reasons."
LOAD-DATE: April 25, 2006
LANGUAGE: ENGLISH
DOCUMENT-TYPE: DIGEST
PUBLICATION-TYPE: Newspaper
Copyright 2006 Times Publishing Company
All Rights Reserved
384 of 998 DOCUMENTS
Wilkes Barre Times Leader (Pennsylvania)
April 25, 2006 Tuesday
In brief
SECTION: A; Pg. 4
LENGTH: 509 words
Iran might exit nuclear treaty Iranian President Mahmoud Ahmadinejad said
Monday he is thinking about withdrawing from the nuclear nonproliferation
treaty if the United Nations atomic agency tries to prevent his country from
enriching uranium. At a rare news conference in Tehran, Ahmadinejad also
predicted the U.N. Security Council will not impose sanctions on Iran, which is
facing a deadline Friday to halt enrichment.
WASHINGTON
Drug might combat cocaine
The hottest topic in cocaine addiction is another drug - a medicine already sold
to wake up narcoleptics.
Hundreds of cocaine users are testing whether that legal pill, called modafinil,
could help them beat the addiction, and there's early evidence it might.
In addition to blunting cocaine's notorious cravings, modafinil also might
counter the damage that cocaine wreaks on users' brain circuits - damage that in
turn fuels the cycle of addiction.
Cocaine is highly addictive: About 16 percent of people who try it become
hooked, often rapidly. In 2003, the latest data, the government estimated that
more than 1.5 million Americans were dependent on or abusing cocaine, and more
reported recently experimenting with it.
KATMANDU, Nepal
Beleaguered king relenting
Nepal's embattled king appeared to defuse weeks of mass protests that have
pushed this Himalayan country near the brink of anarchy, reinstating the lower
house of parliament on Monday as his opponents had demanded.
With few choices left and hoping to avoid a bloody showdown between
demonstrators and his security forces, Gyanendra's announcement cleared the way
for the creation of a new constitution that could leave him largely powerless,
or even eliminate the monarchy.
Gyanendra also expressed his sympathies for the 14 demonstrators killed by his
security forces in nearly three weeks of protests.
Nepal's three largest opposition.
INDIANAPOLIS
Workers face sex charges
Nine former employees of a county juvenile detention center were charged Monday
with using their positions of authority to have sex with teenage girls.
The nine workers were accused of having sex with six girls who were 13 to 15
years old at the time.
Marion County prosecutor Carl Brizzi said one girl was raped by one of the
defendants. The five others agreed to have sex with one or more of the men, but
in Indiana the age of sexual consent is 16.
Brizzi said the defendants sent the victims love letters and even a teddy bear
bearing the words "I love you."
PORTLAND, Maine
Sex offender case widens
A man suspected of killing two people on the state's online sex offender
registry appears to have visited the homes of other sex offenders during a
five-hour gap between the killings, police said Monday.
Detectives have gathered evidence suggesting Stephen Marshall drove to homes
belonging to registered sex offenders on Easter morning, said Detective Brian
Strout, a state police investigator in Bangor.
The information about Marshall's travels was based on global positioning
software contained on his laptop, The Canadian Press reported.
From Times Leader wire services
LOAD-DATE: April 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 Wilkes Barre Times Leader
All Rights Reserved
385 of 998 DOCUMENTS
Associated Press Online
April 25, 2006 Tuesday 12:30 AM GMT
Narcolepsy Drug Eyed for Cocaine Users
BYLINE: By LAURAN NEERGAARD, AP Medical Writer
SECTION: WASHINGTON DATELINE
LENGTH: 824 words
DATELINE: WASHINGTON
The hottest topic in cocaine addiction is another drug a medicine already sold
to wake up narcoleptics.
Hundreds of cocaine users are testing whether that legal pill, called modafinil,
could help them kick the addiction, and there's early evidence that it may.
In addition to blunting cocaine's notorious cravings, modafinil might also
counter the damage that cocaine wreaks on users' brain circuits damage that in
turn fuels the cycle of addiction.
The prospect of that double-whammy has the National Institutes of Health
spending $10.8 million researching modafinil as a potential cocaine treatment.
Results from the first of three key clinical trials could arrive by year's end.
Scientists are cautious: In a hunt spanning two decades, no one has found a
medication to help treat cocaine addiction, and there's no guarantee that
modafinil will pan out.
But for Dr. Nora Volkow, director of NIH's National Institute on Drug Abuse, the
narcolepsy medicine tops the list of promising potential therapies. It may help
restore proper function of a crucial brain chemical, dopamine, that addiction
hijacks.
And in describing why he's hopeful, one leading researcher recounts the man who
accused his drug dealer of selling bad coke before realizing modafinil had kept
him from getting high and several other modafinil testers who told of flushing
cocaine down the toilet.
"I've been treating cocaine-addicted patients for something like 25 years, more,
and I've never heard of anybody throwing away cocaine," says Dr. Charles Dackis
of the University of Pennsylvania, who led a pilot study that suggested
modafinil more than doubled addicts' chances of going cocaine-free for at least
three weeks.
That study enrolled just 62 people, but the results were significant enough for
NIH to fund new research at Pennsylvania, the University of Texas in Houston,
Boston University and other sites enrolling about 650 cocaine users to see if
modafinil really does work.
The main side effect so far: insomnia, not surprising as modafinil is sold today
to help narcolepsy patients fend off that neurologic disease's sudden sleep
attacks.
Addiction specialists gave it a look because even though modafinil isn't a
classic stimulant, it triggered something in the brain to also improve patients'
mood, energy levels and ability to concentrate effects that might counter
cocaine withdrawal. Then came the surprises:
Cocaine intensely stimulates the brain's pleasure centers, producing not just a
"buzz" or a "rush," but outright euphoria. In a small safety study to ensure
that modafinil didn't make cocaine worse, some users found the once-a-day pill
blocked that high. "We didn't expect that at all," Dackis says.
Potentially more important, he says, modafinil seems to increase activity in the
prefrontal cortex, the brain's decision-making command center and the spot that
allows reasoning to override impulse or emotion. Cocaine reduces activity in
that key brain region, making it even harder for would-be quitters to ignore
cravings and resist another hit.
Modafinil also increases the ability to think strategically, a means of weighing
variables and risks to make decisions, says Frank Vocci, NIDA's pharmacotherapy
chief.
"The effects on cognitive processes are very subtle, and very interesting,"
Vocci says and that's the reason that of half a dozen medications being studied
as potential cocaine treatments, the government's biggest emphasis is on
modafinil.
Cocaine is highly addictive: About 16 percent of people who try it become
hooked, often rapidly. In 2003, the latest data, the government estimated that
more than 1.5 million Americans were dependent on or abusing cocaine, and more
reported recently experimenting with it.
Addictions in general rewire the brain, says Volkow, the NIDA director. Drugs
cause a feel-good rush by increasing amounts of the brain chemical dopamine. The
brain reacts by tamping down regular dopamine production, making users feel
lousy between hits and setting up the cycle of addiction.
At the same time, the dopamine surge also creates memory circuits that
eventually establish so-called "cue-induced cravings": If an addict passes the
crack house or sees friends he did drugs with, his brain literally sends a
strong impulse to use again.
"One of the strategies of course, in terms of treatment ... is how can we help
recover the function of the dopamine system, so the person that's addicted can
become sensitive to natural stimuli," Volkow explains.
Modafinil seems to affect chemicals that in turn regulate dopamine production, a
different pathway than cocaine takes in altering normal dopamine, and thus one
that might counter it, adds Dackis.
"You can't assume this is going to work," he cautions. But if it pans out, a
drug that could help cognition instead of just numb cravings would be "a big
benefit in treatment."
EDITOR'S NOTE Lauran Neergaard covers health and medical issues for The
Associated Press in Washington.
LOAD-DATE: April 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
386 of 998 DOCUMENTS
The Associated Press
April 24, 2006 Monday 7:51 PM GMT
HEALTHBEAT: Could narcolepsy wake-up drug fight cocaine addiction?
BYLINE: By LAURAN NEERGAARD, AP Medical Writer
SECTION: WASHINGTON DATELINE
LENGTH: 824 words
DATELINE: WASHINGTON
The hottest topic in cocaine addiction is another drug a medicine already sold
to wake up narcoleptics.
Hundreds of cocaine users are testing whether that legal pill, called modafinil,
could help them kick the addiction, and there's early evidence that it may.
In addition to blunting cocaine's notorious cravings, modafinil might also
counter the damage that cocaine wreaks on users' brain circuits damage that in
turn fuels the cycle of addiction.
The prospect of that double-whammy has the National Institutes of Health
spending $10.8 million researching modafinil as a potential cocaine treatment.
Results from the first of three key clinical trials could arrive by year's end.
Scientists are cautious: In a hunt spanning two decades, no one has found a
medication to help treat cocaine addiction, and there's no guarantee that
modafinil will pan out.
But for Dr. Nora Volkow, director of NIH's National Institute on Drug Abuse, the
narcolepsy medicine tops the list of promising potential therapies. It may help
restore proper function of a crucial brain chemical, dopamine, that addiction
hijacks.
And in describing why he's hopeful, one leading researcher recounts the man who
accused his drug dealer of selling bad coke before realizing modafinil had kept
him from getting high and several other modafinil testers who told of flushing
cocaine down the toilet.
"I've been treating cocaine-addicted patients for something like 25 years, more,
and I've never heard of anybody throwing away cocaine," says Dr. Charles Dackis
of the University of Pennsylvania, who led a pilot study that suggested
modafinil more than doubled addicts' chances of going cocaine-free for at least
three weeks.
That study enrolled just 62 people, but the results were significant enough for
NIH to fund new research at Pennsylvania, the University of Texas in Houston,
Boston University and other sites enrolling about 650 cocaine users to see if
modafinil really does work.
The main side effect so far: insomnia, not surprising as modafinil is sold today
to help narcolepsy patients fend off that neurologic disease's sudden sleep
attacks.
Addiction specialists gave it a look because even though modafinil isn't a
classic stimulant, it triggered something in the brain to also improve patients'
mood, energy levels and ability to concentrate effects that might counter
cocaine withdrawal. Then came the surprises:
Cocaine intensely stimulates the brain's pleasure centers, producing not just a
"buzz" or a "rush," but outright euphoria. In a small safety study to ensure
that modafinil didn't make cocaine worse, some users found the once-a-day pill
blocked that high. "We didn't expect that at all," Dackis says.
Potentially more important, he says, modafinil seems to increase activity in the
prefrontal cortex, the brain's decision-making command center and the spot that
allows reasoning to override impulse or emotion. Cocaine reduces activity in
that key brain region, making it even harder for would-be quitters to ignore
cravings and resist another hit.
Modafinil also increases the ability to think strategically, a means of weighing
variables and risks to make decisions, says Frank Vocci, NIDA's pharmacotherapy
chief.
"The effects on cognitive processes are very subtle, and very interesting,"
Vocci says and that's the reason that of half a dozen medications being studied
as potential cocaine treatments, the government's biggest emphasis is on
modafinil.
Cocaine is highly addictive: About 16 percent of people who try it become
hooked, often rapidly. In 2003, the latest data, the government estimated that
more than 1.5 million Americans were dependent on or abusing cocaine, and more
reported recently experimenting with it.
Addictions in general rewire the brain, says Volkow, the NIDA director. Drugs
cause a feel-good rush by increasing amounts of the brain chemical dopamine. The
brain reacts by tamping down regular dopamine production, making users feel
lousy between hits and setting up the cycle of addiction.
At the same time, the dopamine surge also creates memory circuits that
eventually establish so-called "cue-induced cravings": If an addict passes the
crack house or sees friends he did drugs with, his brain literally sends a
strong impulse to use again.
"One of the strategies of course, in terms of treatment ... is how can we help
recover the function of the dopamine system, so the person that's addicted can
become sensitive to natural stimuli," Volkow explains.
Modafinil seems to affect chemicals that in turn regulate dopamine production, a
different pathway than cocaine takes in altering normal dopamine, and thus one
that might counter it, adds Dackis.
"You can't assume this is going to work," he cautions. But if it pans out, a
drug that could help cognition instead of just numb cravings would be "a big
benefit in treatment."
EDITOR'S NOTE Lauran Neergaard covers health and medical issues for The
Associated Press in Washington.
LOAD-DATE: April 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
387 of 998 DOCUMENTS
Associated Press Worldstream
April 24, 2006 Monday 7:54 PM GMT
Could narcolepsy wake-up drug fight cocaine addiction?
BYLINE: By LAURAN NEERGAARD, AP Medical Writer
SECTION: INTERNATIONAL NEWS
LENGTH: 829 words
DATELINE: WASHINGTON
The hottest topic in cocaine addiction is another drug, a medicine already sold
to wake up narcoleptics.
Hundreds of cocaine users are testing whether that legal pill, called modafinil,
could help them kick the addiction, and there is intriguing early evidence that
it might.
In addition to blunting cocaine's notorious cravings, modafinil might also
counter the damage that cocaine wreaks on users' brain circuits damage that in
turn fuels the cycle of addiction.
The prospect of that double-whammy has the National Institutes of Health
spending $10.8 million (euro8.75 million) researching modafinil as a potential
cocaine treatment. Results from the first of three crucial clinical trials could
arrive by year's end.
Scientists are cautious: In a hunt spanning two decades, no one has found a
medication to help treat cocaine addiction, and there is no guarantee that
modafinil will pan out.
But for Dr. Nora Volkow, director of NIH's National Institute on Drug Abuse, the
narcolepsy medicine tops the list of promising potential therapies. It may help
restore proper function of a crucial brain chemical, dopamine, that addiction
hijacks.
And in describing why he is hopeful, one leading researcher recalls the man who
accused his drug dealer of selling bad coke before realizing that modafinil had
kept him from getting high and several other modafinil testers who told of
flushing cocaine down the toilet.
"I've been treating cocaine-addicted patients for something like 25 years, more,
and I've never heard of anybody throwing away cocaine," says Dr. Charles Dackis
of the University of Pennsylvania, who led a pilot study that suggested
modafinil more than doubled addicts' chances of going cocaine-free for at least
three weeks.
That study enrolled just 62 people, but the results were significant enough for
NIH to pay for new research at Pennsylvania, the University of Texas in Houston,
Boston University and other sites enrolling about 650 cocaine users to see if
modafinil works.
The main side effect so far: insomnia, not surprising as modafinil is sold today
to help narcolepsy patients fend off that neurologic disease's sudden sleep
attacks.
Addiction specialists gave it a look because even though modafinil is not a
classic stimulant, it triggered something in the brain that also improves
patients' moods, energy levels and ability to concentrate. Those effects might
counter cocaine withdrawal. Then came the surprises:
Cocaine intensely stimulates the brain's pleasure centers, producing not just a
"buzz" or a "rush," but outright euphoria. In a small safety study to ensure
that modafinil did not make cocaine worse, some users found the once-a-day pill
blocked that high. "We didn't expect that at all," Dackis says.
Potentially more important, he says, modafinil seems to increase activity in the
prefrontal cortex, the brain's decision-making command center and the spot that
allows reasoning to override impulse or emotion. Cocaine reduces activity in
that key brain region, making it even harder for would-be quitters to ignore
cravings and resist another hit.
Modafinil also increases the ability to think strategically, a means of weighing
variables and risks to make decisions, says Frank Vocci, NIDA's pharmacotherapy
chief.
"The effects on cognitive processes are very subtle, and very interesting,"
Vocci says, and the reason that of a half-dozen medications being studied as
potential cocaine treatments, the government's biggest emphasis is on modafinil.
Cocaine is highly addictive: About 16 percent of people who try it become
hooked, often rapidly. In 2003, the latest data, the government estimated that
more than 1.5 million Americans were dependent on or abusing cocaine, and more
reported recently experimenting with it.
Addictions in general rewire the brain, says Volkow, the NIDA director. Drugs
cause a feel-good rush by increasing amounts of the brain chemical dopamine. The
brain reacts by tamping down regular dopamine production, making users feel
lousy between hits and setting up the cycle of addiction.
At the same time, the dopamine surge also creates memory circuits that
eventually establish so-called "cue-induced cravings": If an addict passes the
crack house or sees friends he did drugs with, his brain literally sends a
strong impulse to use again.
"One of the strategies of course, in terms of treatment ... is how can we help
recover the function of the dopamine system, so the person that's addicted can
become sensitive to natural stimuli," Volkow explains.
Modafinil seems to affect chemicals that in turn regulate dopamine production, a
different pathway than cocaine takes to strike dopamine, and thus one that might
counter it, adds Dackis.
"You can't assume this is going to work," he cautions. But if it pans out, a
drug that could help cognition instead of just numb cravings would "be a big
benefit in treatment."
EDITOR'S NOTE Lauran Neergaard covers health and medical issues for The
Associated Press in Washington.
LOAD-DATE: April 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
388 of 998 DOCUMENTS
Agence France Presse -- English
April 16, 2006 Sunday 9:12 AM GMT
No planned comeback for disgraced sprinter White
LENGTH: 322 words
DATELINE: SAN FRANCISCO, April 16 2006
Disgraced American sprint star Kelli White will not return to competition when
her two-year doping ban expires next month, her attorney confirmed.
White was stripped of her two gold medals from the 2003 world championships and
banned for two years in May 2004 after admitting using banned steroids and
doping methods. Her ban expires on May 17.
"She does not intend to return to competition," attorney Jerrold Colton told The
San Francisco Chronicle.
"At this point it's unlikely. These last two years have been tough on her and
she doesn't want to deal with this anymore."
White's rise was as rapid as her fall.
Although she won a bronze medal in the 200m at the 2001 world championships, it
was not until 2003 that she dominated when, helped by the doping programme of
BALCO founder Victor Conte, she became the first American woman to win both
sprints at the world championships in Paris in personal best times.
Soon after the victories, White tested positive for the drug modafinil, which
she claimed she needed to treat a sleeping disorder.
She later admitted using several banned substances, including the designer
steroid THG, the endurance-boosting drug EPO, a form of testosterone and the
stimulant modafinil.
At the time White insisted she would return to competition but now aged 29 and
recovering from major surgery to her knee cap she has seen the rise of sprint
stars Allyson Felix and Lauryn Williams.
"She feels pretty good but she's not sure if she wants to get out there and test
it," her father Willie White said.
"A lot of people wish things hadn't happened, but they did," he said. "You've
got to move on. Everybody makes decisions. People make choices. You have to live
with them and deal with them."
All of White's competitive results from December 15, 2000 were wiped out as a
result of the ban. She last competed on May 14, 2004 in Doha where she ran the
200m in 23.42, 1.37 seconds slower than her best time.
bur/ea06
LOAD-DATE: April 17, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Agence France Presse
All Rights Reserved
389 of 998 DOCUMENTS
Family Practice News
April 15, 2006
FDA Panel: Modafinil Is Not Safe for Treating ADHD in Teens
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pg. 38 Vol. 36 No. 8 ISSN: 0300-7073
LENGTH: 821 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee said
modafinil is not safe for treating ADHD in children and adolescents by a 12-1
vote, although committee members unanimously agreed the drug was effective for
that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often due to a
hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
Among 933 children and adolescents exposed to the drug during trials, there
were 12 cases that could have been definite erythema multiforme (EM) or SJS,
early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of 1.29%,
said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products.
The panel's discussion focused on one case that seemed most likely to be
SJS-indicating a 1 in 1,000 risk. But they were not certain that was the true
risk.
Dr. Bigby and Dr. Mannheim said more cases could occur once modafinil
(Provigil) is more widely used-even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off-label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19 (based on other stimulants' sales), there
could be 500-3,250 cases of EM or SJS, and 25-488 deaths, said Dr. Mannheim.
The dichotomy between the postmarketing experience and the trial data
prompted the FDA to seek its advisers' input, said Dr. Robert J. Temple,
director of the FDA's office of medical policy.
The FDA usually follows the advice of its panels.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily.
The primary outcome was the total score on the school ADHD rating scale. In
all three trials, children taking modafinil had a more significant drop in
scores than those taking placebo. The total score for modafinil recipients-just
over 20-was close to the normative score for a 10-year-old male, according to a
Cephalon statement.
Panelists did not dispute the drug's efficacy, although many said it would
not be a first-line choice.
Lesley Russell, Cephalon's senior vice president of worldwide clinical
research, said modafinil offers clinicians an alternative, especially when
children don't respond to other marketed drugs.
But Dr. Temple said that even though it's plausible that modafinil might work
in nonresponsive children, the company had not proved that.
"The mere fact that people given a second drug respond after failing to
respond to the first tells you nothing at all," he said.
According to a company statement, modafinil may be less addictive and less
apt to be diverted because it does not offer a "high" to recreational users.
Jeffrey L. Vaught, executive vice president of research and development at
Cephalon, said the drug is not water soluble and is not stable at high heat,
which makes it difficult to crush for injection or smoking. Studies have shown
that modafinil does not activate reward centers in the brain, and that it does
not cause release of dopamine in vitro or in vivo.
The Drug Enforcement Administration has deemed modafinil a schedule IV drug;
other stimulants used to treat ADHD, such as Ritalin, are schedule II.
Despite potential advantages, the panel did not want modafinil to be marketed
for children yet.
"I think we did err on the side of consumer protection," said Dr. Goodman.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2006 Elsevier Inc., International Medical News Group
All Rights Reserved
390 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
April 6, 2006
Alfresa/Tanabe to co-develop modafinil in Japan
LENGTH: 225 words
Alfresa Pharma ( Alfresa Holdings ) and Tanabe have concluded a co-development
agreement regarding the right to co-market modafinil for the treatment of
narcolepsy, as well as to co-develop other new indications for the product in
Japan. Application for manufacturing and marketing approval of modafinil for
narcolepsy has been filed by Alfresa. Modafinil is a wakefulness-enhancing
agent, to which Alfresa acquired the right to develop, manufacture and market in
Japan from Cephalon in June 1998. Products containing modafinil are currently
marketed in over 30 countries in the world as treatment for the excessive
daytime sleepiness associated with narcolepsy. It has also been approved in the
US and certain major European countries as an agent for obstructive sleep apnoea
and excessive sleepiness in shift-work sleep disorder patients. In Japan,
Alfresa has been developing it for the treatment of narcolepsy as an orphan drug
designated by the Ministry of Health, Labour and Welfare and is currently
waiting for early approval. Upon approval, each of the companies will market
modafinil using its own sales channel under the same tradename, Modiodal . The
companies also plan to seek necessary approvals for further indications of
modafinil in Japan, such as obstructive sleep apnoea syndrome and paediatric
attention deficit hyperactivity disorder.
LOAD-DATE: April 7, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
391 of 998 DOCUMENTS
Japan Corporate News Network
April 05, 2006 Wednesday 06:45 PM JST
Alfresa Pharma, Tanabe Seiyaku to Collaborate in Development and Sales of
Narcolepsy Drug Modafinil
BYLINE: jcn
LENGTH: 118 words
DATELINE: Tokyo, Japan
Tokyo, Apr 5, 2006 - (JCN) - Alfresa Pharma, a wholly owned subsidiary of
Alfresa Holdings, has signed an agreement with Tanabe Seiyaku on modafinil, an
agent for treating narcolepsy.
Upon receiving approval, the two companies will co-promote the agent under the
trade name of Modiodal in Japan. Further, they will proceed with research on the
agent with the aim of expanding indications including obstructive sleep apnea
syndrome and pediatric ADHD (attention-deficit hyperactivity disorder).
Modafinil is an arousal-enhancing agent for which Alfresa Pharma has obtained
rights to develop, manufacture and develop in Japan from US company Cephalon.
Currently, the agent is available in over 30 countries worldwide.
LOAD-DATE: April 6, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Japan Corporate News Network
All Rights Reserved
392 of 998 DOCUMENTS
Breaking News from globeandmail.com
April 1, 2006 6:47 PM EST
Sleep no more
BYLINE: Alexandra Gill; From Saturday's Globe and Mail
SECTION: CAT6,B; specialScienceandHealth; Front
LENGTH: 1646 words
HIGHLIGHT: If you're having trouble getting decent shut-eye, why bother?
Pharmacists say they have a remedy
Every morning, I wake up to a pounding wail of thunder, feeling shaken, spent
and thoroughly unsatisfied. Then I roll over, hit the snooze button, and do it
again.
This bleary-eyed ritual, which must be repeated several times to drag my weary
body out of its deprived state of slumber, is the symptom of a widespread
hunger.
"Sleep is the new sex." So says Arthur J. Spielman, a New York psychologist and
co-author of The Insomnia Answer. "People want it, need it and can't get
enough."
This weekend, as we spring forward to daylight time, and lose yet another
precious hour of shut-eye, it's the same old story: We're getting less and less
sleep.
The National Sleep Foundation (NSF) estimates that the average sleep time in the
United States has dropped by more than 20 per cent in the past century. By last
year, 71 per cent of people were getting by with less than the eight hours of
sleep the body needs (up from 63 per cent in 1998). According to the latest
numbers from Statistics Canada, one in seven Canadians -- 3.3 million people --
have trouble going to sleep and staying asleep.
Things are now so bad that the Monday after the annual switch to daylight time
has been declared National Napping Day, and this year the goal is to have us
catch 40 winks while on the job.
"We live in a time famine," says Harvey Moldofsky, director of the Centre for
Sleep and Chronobiology at the University of Toronto. "There isn't enough time
in our waking periods to accomplish all of the expectations industrialized
society requires of us."
The 24/7, BlackBerry-buzzing, on-demand lifestyle is taking its toll. We pummel
ourselves through a vicious cycle, jolting up on caffeine during the day and
knocking ourselves out with hypnotics at night. Last year, 42 million
sleeping-pill prescriptions were filled in the United States, up 60 per cent
since 2000, according to a study by Forbes magazine.
This cranky, edgy, worn-out state of being leaves us vulnerable to anxiety,
depression and weakened immunity. Studies have shown that a lack of sleep
affects memory loss and dexterity and has contributed to rising rates of
obesity. Not surprisingly, it also diminishes our sex drive. In last year's
Sleep in America poll conducted by the NSF, nearly one-quarter of partnered
adults said they have lost interest in sex, or have it less often because they
are just too darn tired.
There has to be a better way. Perhaps there is.
What if you were offered a magic pill that made you feel alert throughout the
entire day, without the jitter, buzz, euphoria, crash, addictive qualities or
potential for paranoid delusion that come with amphetamines and caffeine? Would
you be interested in a pill that lets you bounce back from a late night,
bright-eyed and bushy-tailed, after just four hours of sleep?
Meet modafinil, "the first wave of new lifestyle drugs that promise to do for
sleep what the contraceptive pill did for sex -- unshackle it from nature," New
Scientist magazine trumpets in a recent cover story.
"Modafinil has made it possible to have 48 hours of continuous wakefulness with
few, if any, ill effects," Graham Lawton writes, almost giddily, about the brave
new world of 24-hour living.
"New classes of sleeping pills are on the horizon that promise to deliver sleep
that is deeper and more refreshing than the real thing," he continues. "Further
down the line are even more radical interventions -- wakefulness promoters that
can safely abolish sleep for several days at a stretch, and sleeping pills that
deliver what feels like eight hours of sleep in half the time."
Modafinil, a stimulant trademarked as Provigil in the United States and Alertec
in Canada, was approved by the U.S. Federal Drug Administration in 1998 to treat
narcolepsy, a chronic neurological disorder that causes excessive daytime
sleepiness, loss of voluntary muscle tone, vivid hallucinations and brief
episodes of total paralysis.
The way modafinil works is not clearly understood. It seems to target regions of
the brain believed to regulate normal wakefulness and cognitive functions,
perhaps by slowing the release of GABA (a sleep promoter in the brain) or acting
on the histamine pathways (connected to sleep regulation). And unlike
amphetamines, cocaine and most other pick-me-ups, it doesn't appear to fire up
the neurotransmitters that cause dopamine to flood the brain, which then sets
the heart racing, makes you feel high and causes twitchiness.
"It works," Dr. Moldofsky says. "It's not a panacea, but our studies have shown
that, for narcolepsy, it can be very helpful. It literally can change the lives
of these people overnight."
Although modafinil is still approved only for narcolepsy, there are many who
would like to put it to other uses. The U.S. Defence Department has been testing
it heavily as a replacement for dexedrine, the "go pill" taken by the two U.S.
Air Force bomber pilots who accidentally killed four Canadian soldiers in
Afghanistan.
Last winter, researchers at the University of Pennsylvania published the results
of a small study, which found that modafinil may help recovering cocaine addicts
fight their addiction. Some professional athletes were using it to enhance their
performance, until the International Olympic Committee and World Anti-Doping
Agency listed it as a banned substance in 2004. And increasingly, sleep-deprived
professionals are using it to pursue a more active lifestyle.
In 2002, the FDA issued a warning to Cephalon, the Pennsylvania-based
pharmaceutical company that licensed the drug from France's Laboratoire Lafon
and conducted its clinical trials, about misleading promotional materials that
encouraged off-label use for general sleepiness, lack of energy and fatigue.
As reported by The Washington Post, Americans bought $150-million (U.S.) worth
of modafinil in 2001; three-quarters of the pills were swallowed by people who
didn't have narcolepsy.
Cephalon amended its marketing, but modafinil's underground use shows no sign of
slacking.
"If I take a dose just before I go to bed, I can wake up after four or five
hours and feel refreshed," one user told the New Scientist reporter. "The alarm
goes off and I'm like, 'Let's go!' "
The 31-year-old old software developer from Seattle, who has been popping the
pills for three years and buys them on-line, says the drug doesn't make him any
more alert or less sleepy.
"It's just that thoughts of tiredness don't occur to me. I find I can be very
productive at work. I'm more organized and more motivated. And it means I can go
out partying on a Friday night and still go skiing early on Saturday morning."
Hmm, that sounds awfully seductive. I must try to get some -- after I take a
nap.
"I've never heard of it," says the doctor on duty at my neighbourhood walk-in
clinic.
"They say it's quite safe," I implore, pushing the article into his hands, after
explaining the travails of my restless nights and daytime exhaustion.
Frowning, he skims through the piece, then picks up the hefty 2005 edition of
the Canadian Pharmacists Association's Compendium of Pharmaceuticals and
Specialties, and starts flipping.
"Oh, it's here," he says, mildly surprised. "Can cause headaches, nausea,
dizziness, overconfidence and psychosis. Do you have any problems with your
liver? Well, there are no big red flags."
Psychosis isn't a big red flag?
"Lots of drugs cause psychosis," he says, peering sternly over the book. "Pot
makes some people psychotic, but we seem to think that's okay."
Jonathan Fleming, co-director of the Sleep Disorder Clinic at the University of
British Columbia Hospital, warns that doctors must be cautious in their
dispersal of modafinil.
"The research evidence shows it works, and, as a drug, it's very safe. But the
research protocols were very clear. This is not for people who have been out
until 5 a.m., and have to get work the next day. That's a misuse," he says,
sighing impatiently over the phone.
"Having said that, people misuse medication all the time," he continues. "And we
all self-medicate with coffee or Wake Ups. But if you're using it for sleep
deprivation, at some point, you're going to have to address that sleep debt.
Getting adequate sleep is the appropriate response."
Modafinil, which doesn't prevent you from falling asleep when you want to, cuts
the recovery time of sleep debt in half. You can stay awake for 48 hours and
need only eight hours of sleep, instead of 16, to catch up. But researchers are
doubtful that anyone could take it every day without consequences. Sleep is
necessary for the endocrine system, immune function and hormonal growth.
Yet, there is already a new class of drugs being developed that may, it is
hoped, eliminate sleep debt altogether. A trial compound called CX717, one of
the "ampakine" drugs originally developed to fight Alzheimer's, has shown
remarkable restorative powers. According to New Scientist, the Defence Advanced
Research Projects Agency plans tests this year "that will push volunteers
through four consecutive nights of hard work with only four hours of recovery
sleep in between."
But even if Mother Nature is conquered some day, there are still big societal
questions to contend with. If we can safely skip on sleep, what's to keep us
from working around the clock? Will people who choose to sleep be overlooked for
promotions? Will the super sleep drugs, which are not likely to be covered by
health insurance, cause even greater class divisions?
Back at the clinic, the doctor says he is uncomfortable prescribing modafinil.
"How's your thyroid?" he asks, filling out a laboratory requisition for a
battery of blood tests. Then he hands me several photocopied pages, modafinil's
monograph from the pharmaceutical encyclopedia.
"We'll see how the tests go. And in the meantime I want you to read this. Maybe
it will scare you to sleep."
Alexandra Gill is The Globe and Mail's western arts correspondent, based in
Vancouver.
LOAD-DATE: April 12, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2006 Bell Globemedia Publishing Inc. and its licensors.
All Rights Reserved
393 of 998 DOCUMENTS
Clinical Psychiatry News
April 2006
Treatments for Sleepiness Vary in Cost, Side Effects
BYLINE: Sherry Boschert, San Francisco Bureau
SECTION: Pg. 54 Vol. 34 No. 4 ISSN: 0270-6644
LENGTH: 677 words
SAN DIEGO - All three main treatments for problem sleepiness can perk
patients up, but they differ in cost and side effects, Dr. Milton Erman said at
a psychopharmacology congress sponsored by the Neuroscience Education Institute.
Caffeine is the cheapest, most accessible, and most widely used stimulant.
The two other treatment options are prescription medications, which are more
expensive: modafinil or CNS stimulants (most commonly amphetamines or
methylphenidate).
Caffeine tolerance develops rapidly, however, and there's a moderate risk for
dependence. Stopping a daily caffeine habit too quickly can trigger a "caffeine
headache." Side effects from regular caffeine use include nervousness,
irritability, insomnia, and GI problems, said Dr. Erman of the University of
California, San Diego.
"Many of my insomniac patients tell me proudly that they aren't using
caffeine" to indicate that caffeine can't be blamed for their insomnia, he said.
Ironically, a bit of caffeine in the morning may be just what they need. "The
problem with many of these insomniac patients is that they can't get going, get
functioning in the morning," he said. Limited caffeine use in the morning may
help them function better.
Use of CNS stimulants also leads to tolerance, and there is a high potential
for dependence. Side effects include nervousness, headaches, insomnia, anorexia,
GI problems, and mood changes. General CNS stimulants such as amphetamines have
a high risk of abuse and hyperactivity because of their broad mechanism of
action.
One experimental study of sleep deprivation that compared amphetamines with
modafinil treatment to maintain wakefulness suggested that the two drugs are
equally potent. In real life, however, "I think amphetamines are more potent,"
he said. Patients with narcolepsy who have used amphetamines in the past often
aren't satisfied with the effects of modafinil.
Modafinil works more specifically on wakefulness circuits and has fewer side
effects than other stimulants. Tolerance is not an issue-it maintains most of
its efficacy over time-and use of the drug does not lead to dependence. Side
effects include headache, nausea, dry mouth, insomnia, and hyperactivity.
The risk of headache relates to the dosing of modafinil. In early research on
the drug, headache appeared primarily in patients who titrated up to a dose of
400 mg/day by the third day. In subsequent research that gave patients 7-9 days
to titrate up to 400 mg/day, headache was much less of a problem, Dr. Erman
said.
"Modafinil works quite well, particularly if we're not talking about the most
severely hypersomnolent patients," such as narcoleptics who have become
accustomed to taking stimulants, he said.
Dr. Erman is a speaker and consultant for, and has received research funding
from, the company that makes modafinil, Cephalon Inc. Modafinil is approved to
treat sleepiness from shift work, narcolepsy, and sleep apnea.
The most common cause of problem sleepiness is sleep apnea, which occurs in
perhaps 10% of the population, he said. Restless leg syndrome can interrupt
sleep and lead to daytime sleepiness. Narcolepsy is fairly uncommon. Insomnia
can cause excessive sleepiness, but more often, insomniac patients are
hypervigilant. "If anything, they are more alert" than they want to be, he said.
Secondary causes of sleepiness include chronic pain and any medical condition
that causes pain or discomfort, which may interrupt sleep. Medications used to
alleviate pain also can lead to daytime sleepiness because they affect breathing
during sleep and increase the risk for sleep apnea.
Check to see if patients who complain of sleepiness are taking drugs that
cause sedation or that disrupt sleep, Dr. Erman added, and consider alternative
therapies.
Lifestyle issues, such as graveyard shift work, also contribute to excessive
sleepiness,. The pace of U.S. culture commonly leads to chronic sleep
deprivation that affects daytime function. "As a society, we really haven't
dealt with this," he said.
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The Globe and Mail (Canada)
April 1, 2006 Saturday
HEALTH;
If you're having trouble getting decent shut-eye, why bother? Pharmacists say
they have a drug that can keep you awake for two days without side effects,
ALEXANDRA GILL reports. And on the horizon: pills that could make bedtime
completely a thing of the past
BYLINE: ALEXANDRA GILL
SECTION: FOCUS; Pg. F9
LENGTH: 1654 words
Every morning, I wake up to a pounding wail of thunder, feeling shaken, spent
and thoroughly unsatisfied. Then I roll over, hit the snooze button, and do it
again.
This bleary-eyed ritual, which must be repeated several times to drag my weary
body out of its deprived state of slumber, is the symptom of a widespread
hunger.
"Sleep is the new sex." So says Arthur J. Spielman, a New York psychologist and
co-author of The Insomnia Answer. "People want it, need it and can't get
enough."
This weekend, as we spring forward to daylight time, and lose yet another
precious hour of shut-eye, it's the same old story: We're getting less and less
sleep.
The National Sleep Foundation (NSF) estimates that the average sleep time in the
United States has dropped by more than 20 per cent in the past century. By last
year, 71 per cent of people were getting by with less than the eight hours of
sleep the body needs (up from 63 per cent in 1998). According to the latest
numbers from Statistics Canada, one in seven Canadians - 3.3 million people -
have trouble going to sleep and staying asleep.
Things are now so bad that the Monday after the annual switch to daylight time
has been declared National Napping Day, and this year the goal is to have us
catch 40 winks while on the job.
"We live in a time famine," says Harvey Moldofsky, director of the Centre for
Sleep and Chronobiology at the University of Toronto. "There isn't enough time
in our waking periods to accomplish all of the expectations industrialized
society requires of us."
The 24/7, BlackBerry-buzzing, on-demand lifestyle is taking its toll. We pummel
ourselves through a vicious cycle, jolting up on caffeine during the day and
knocking ourselves out with hypnotics at night. Last year, 42 million
sleeping-pill prescriptions were filled in the United States, up 60 per cent
since 2000, according to a study by Forbes magazine.
This cranky, edgy, worn-out state of being leaves us vulnerable to anxiety,
depression and weakened immunity. Studies have shown that a lack of sleep
affects memory loss and dexterity and has contributed to rising rates of
obesity. Not surprisingly, it also diminishes our sex drive. In last year's
Sleep in America poll conducted by the NSF, nearly one-quarter of partnered
adults said they have lost interest in sex, or have it less often because they
are just too darn tired.
There has to be a better way. Perhaps there is.
What if you were offered a magic pill that made you feel alert throughout the
entire day, without the jitter, buzz, euphoria, crash, addictive qualities or
potential for paranoid delusion that come with amphetamines and caffeine? Would
you be interested in a pill that lets you bounce back from a late night,
bright-eyed and bushy-tailed, after just four hours of sleep?
Meet modafinil, "the first wave of new lifestyle drugs that promise to do for
sleep what the contraceptive pill did for sex - unshackle it from nature," New
Scientist magazine trumpets in a recent cover story.
"Modafinil has made it possible to have 48 hours of continuous wakefulness with
few, if any, ill effects," Graham Lawton writes, almost giddily, about the brave
new world of 24-hour living.
"New classes of sleeping pills are on the horizon that promise to deliver sleep
that is deeper and more refreshing than the real thing," he continues. "Further
down the line are even more radical interventions - wakefulness promoters that
can safely abolish sleep for several days at a stretch, and sleeping pills that
deliver what feels like eight hours of sleep in half the time."
Modafinil, a stimulant trademarked as Provigil in the United States and Alertec
in Canada, was approved by the U.S. Federal Drug Administration in 1998 to treat
narcolepsy, a chronic neurological disorder that causes excessive daytime
sleepiness, loss of voluntary muscle tone, vivid hallucinations and brief
episodes of total paralysis.
The way modafinil works is not clearly understood. It seems to target regions of
the brain believed to regulate normal wakefulness and cognitive functions,
perhaps by slowing the release of GABA (a sleep promoter in the brain) or acting
on the histamine pathways (connected to sleep regulation). And unlike
amphetamines, cocaine and most other pick-me-ups, it doesn't appear to fire up
the neurotransmitters that cause dopamine to flood the brain, which then sets
the heart racing, makes you feel high and causes twitchiness.
"It works," Dr. Moldofsky says. "It's not a panacea, but our studies have shown
that, for narcolepsy, it can be very helpful. It literally can change the lives
of these people overnight."
Although modafinil is still approved only for narcolepsy, there are many who
would like to put it to other uses. The U.S. Defence Department has been testing
it heavily as a replacement for dexedrine, the "go pill" taken by the two U.S.
Air Force bomber pilots who accidentally killed four Canadian soldiers in
Afghanistan.
Last winter, researchers at the University of Pennsylvania published the results
of a small study, which found that modafinil may help recovering cocaine addicts
fight their addiction. Some professional athletes were using it to enhance their
performance, until the International Olympic Committee and World Anti-Doping
Agency listed it as a banned substance in 2004. And increasingly, sleep-deprived
professionals are using it to pursue a more active lifestyle.
In 2002, the FDA issued a warning to Cephalon, the Pennsylvania-based
pharmaceutical company that licensed the drug from France's Laboratoire Lafon
and conducted its clinical trials, about misleading promotional materials that
encouraged off-label use for general sleepiness, lack of energy and fatigue.
As reported by The Washington Post, Americans bought $150-million (U.S.) worth
of modafinil in 2001; three-quarters of the pills were swallowed by people who
didn't have narcolepsy.
Cephalon amended its marketing, but modafinil's underground use shows no sign of
slacking.
"If I take a dose just before I go to bed, I can wake up after four or five
hours and feel refreshed," one user told the New Scientist reporter. "The alarm
goes off and I'm like, 'Let's go!' "
The 31-year-old old software developer from Seattle, who has been popping the
pills for three years and buys them on-line, says the drug doesn't make him any
more alert or less sleepy.
"It's just that thoughts of tiredness don't occur to me. I find I can be very
productive at work. I'm more organized and more motivated. And it means I can go
out partying on a Friday night and still go skiing early on Saturday morning."
Hmm, that sounds awfully seductive. I must try to get some - after I take a nap.
"I've never heard of it," says the doctor on duty at my neighbourhood walk-in
clinic.
"They say it's quite safe," I implore, pushing the article into his hands, after
explaining the travails of my restless nights and daytime exhaustion.
Frowning, he skims through the piece, then picks up the hefty 2005 edition of
the Canadian Pharmacists Association's Compendium of Pharmaceuticals and
Specialties, and starts flipping.
"Oh, it's here," he says, mildly surprised. "Can cause headaches, nausea,
dizziness, overconfidence and psychosis. Do you have any problems with your
liver? Well, there are no big red flags."
Psychosis isn't a big red flag?
"Lots of drugs cause psychosis," he says, peering sternly over the book. "Pot
makes some people psychotic, but we seem to think that's okay."
Jonathan Fleming, co-director of the Sleep Disorder Clinic at the University of
British Columbia Hospital, warns that doctors must be cautious in their
dispersal of modafinil.
"The research evidence shows it works, and, as a drug, it's very safe. But the
research protocols were very clear. This is not for people who have been out
until 5 a.m., and have to get work the next day. That's a misuse," he says,
sighing impatiently over the phone.
"Having said that, people misuse medication all the time," he continues. "And we
all self-medicate with coffee or Wake Ups. But if you're using it for sleep
deprivation, at some point, you're going to have to address that sleep debt.
Getting adequate sleep is the appropriate response."
Modafinil, which doesn't prevent you from falling asleep when you want to, cuts
the recovery time of sleep debt in half. You can stay awake for 48 hours and
need only eight hours of sleep, instead of 16, to catch up. But researchers are
doubtful that anyone could take it every day without consequences. Sleep is
necessary for the endocrine system, immune function and hormonal growth.
Yet, there is already a new class of drugs being developed that may, it is
hoped, eliminate sleep debt altogether. A trial compound called CX717, one of
the "ampakine" drugs originally developed to fight Alzheimer's, has shown
remarkable restorative powers. According to New Scientist, the Defence Advanced
Research Projects Agency plans tests this year "that will push volunteers
through four consecutive nights of hard work with only four hours of recovery
sleep in between."
But even if Mother Nature is conquered some day, there are still big societal
questions to contend with. If we can safely skip on sleep, what's to keep us
from working around the clock? Will people who choose to sleep be overlooked for
promotions? Will the super sleep drugs, which are not likely to be covered by
health insurance, cause even greater class divisions?
Back at the clinic, the doctor says he is uncomfortable prescribing modafinil.
"How's your thyroid?" he asks, filling out a laboratory requisition for a
battery of blood tests. Then he hands me several photocopied pages, modafinil's
monograph from the pharmaceutical encyclopedia.
"We'll see how the tests go. And in the meantime I want you to read this. Maybe
it will scare you to sleep."
Alexandra Gill is The Globe and Mail's western arts correspondent, based in
Vancouver.
LOAD-DATE: September 15, 2006
LANGUAGE: ENGLISH
GRAPHIC: Illustration
PUBLICATION-TYPE: Newspaper
Copyright 2006 The Globe and Mail, a division of CTVglobemedia Publishing Inc.
All Rights Reserved
395 of 998 DOCUMENTS
Pediatric News
April 2006
FDA Panel: Modafinil Not Safe for Children
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pg. 7 Vol. 40 No. 4 ISSN: 0031-398X
LENGTH: 955 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee said
modafinil is not safe for treating ADHD in children and adolescents by a 12-1
vote, although committee members unanimously agreed the drug was effective for
that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often due to a
hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
In a group of 933 children and adolescents exposed to the drug during trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of
1.29%, said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products. The panel's discussion focused on one case that seemed most
likely to be SJS-i.e., a 1-in-1,000 risk. But they weren't certain that was the
true risk.
Dr. Bigby and Dr. Mannheim said more cases could occur once modafinil
(Provigil) is more widely used-even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off-label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19 (based on other stimulants' sales), there
could be 500-3,250 cases of EM or SJS, and 25-488 deaths, said Dr. Mannheim.
The dichotomy between the postmarketing experience and the trial data
prompted the FDA to seek its advisers' input, said Dr. Robert J. Temple,
director of the FDA's office of medical policy. The FDA usually follows its
panels' advice.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
The committee was less concerned about cardiac and psychiatric side effects,
partly because both had a thorough airing at a hearing on ADHD drugs the day
before (see p. 1). There were five psychosis events and six suicidal events in
the modafinil trials, said Dr. Mannheim.
Cephalon proposed to add warnings to modafinil's label on the potential for
psychiatric adverse events. Modafinil's label already warns against use in
patients with hypertrophy or bicuspid aortic valve.
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily.
The primary outcome was the total score on the school ADHD rating scale. In
all three trials, children taking modafinil had a more significant drop in
scores than those taking placebo. The total score for modafinil recipients-just
over 20-was close to the normative score for a 10-year-old male, according to a
Cephalon statement. Panelists did not dispute the drug's efficacy, although many
said it would not be a first-line choice.
Lesley Russell, Cephalon's senior vice president of worldwide clinical
research, said modafinil offers clinicians an alternative, especially when
children don't respond to other marketed drugs.
But Dr. Temple said that even though it's plausible that modafinil might work
in nonresponsive children, the company had not proved that. "The mere fact that
people given a second drug respond after failing to respond to the first tells
you nothing at all."
According to a company statement, modafinil may be less addictive and less
apt to be diverted because it does not offer a "high" to recreational users.
Jeffrey L. Vaught, executive vice president of research and development at
Cephalon, said the drug is not water soluble and is not stable at high heat,
which makes it difficult to crush for injection or smoking.
Studies have shown that modafinil does not activate reward centers in the
brain, and that it does not cause release of dopamine in vitro or in vivo.
The Drug Enforcement Administration has deemed modafinil a schedule IV drug;
other stimulants used to treat ADHD, such as Ritalin, are schedule II.
Despite potential advantages, the panel did not want modafinil to be marketed
for children yet.
"I think we did err on the side of consumer protection," said Dr. Goodman.
In a statement after the meeting, Dr. Paul Blake, Cephalon's executive vice
president of worldwide medical and regulatory operations, said, "We are
obviously disappointed with the recommendation of the advisory committee. We
will continue our discussions with the FDA to determine the next steps in the
review of this drug application."
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396 of 998 DOCUMENTS
Rheumatology News
April 2006
Modafinil Held to Be Unsafe for Treating ADHD in Children
BYLINE: Alicia Ault, Associate Editor, Practice Trends
SECTION: Pg. 42 Vol. 5 No. 4 ISSN: 1541-9800
LENGTH: 584 words
GAITHERSBURG, MD. - A Food and Drug Administration advisory committee said
modafinil is not safe for treating ADHD in children and adolescents by a 12-1
vote, although committee members unanimously agreed the drug was effective for
that indication.
At a meeting of the FDA's Psychopharmacologic Drugs Advisory Committee, the
panel members were mainly concerned about modafinil's potential to cause
Stevens-Johnson syndrome (SJS). The severe rash, which is often due to a
hypersensitivity reaction to a drug, can be fatal in up to 5% of cases,
according to Dr. Michael E. Bigby of the dermatology department at Harvard
Medical School, Boston, and consultant to the panel.
In a group of 933 children and adolescents exposed to the drug during trials,
there were 12 cases that could have been definite erythema multiforme (EM) or
SJS, early prodromal EM or SJS, or suggestive of prodromal EM or SJS-a rate of
1.29%, said Dr. Glenn B. Mannheim, a medical reviewer in the FDA's division of
psychiatry products.
The panel's discussion focused on one case that seemed most likely to be
SJS-indicating a 1 in 1,000 risk. But they weren't certain that was the true
risk. Dr. Bigby and Dr. Mannheim said more cases could occur once modafinil
(Provigil) is more widely used-even though there have been no reports of SJS in
the 36,000 children who were prescribed the drug off-label in 2002-2005.
Given the trial data and the assumption that modafinil could capture 10% of
the market for children under age 19 (based on other stimulants' sales), there
could be 500-3,250 cases of EM or SJS, and 25-488 deaths, said Dr. Mannheim.
The dichotomy between the postmarketing experience and the trial data
prompted the FDA to seek its advisers' input, said Dr. Robert J. Temple,
director of the FDA's office of medical policy.
The FDA usually follows its panels' advice.
The FDA has received six reports of serious skin reactions in adults, said
Dr. Mannheim.
"I'd like to see an opportunity for the company to come back with additional
data. That will give us additional assurance that this case was a fluke," said
panel chair Dr. Wayne K. Goodman, chair of the department of psychiatry at the
University of Florida, Gainesville.
The committee said modafinil's manufacturer, Cephalon Inc., should conduct a
3,000-patient, open-label study to further clarify the risk of SJS.
After the meeting, Dr. Thomas Laughren, director of the FDA's division of
psychiatry products, told reporters that if a case turns up in such a study,
"then they have a problem."
It was not clear why children had higher rates of skin-related adverse events
than adults, but Dr. Mannheim noted that lab tests indicated that they had a
7-16 times higher area under the curve ratio of modafinil sulfone, a metabolite.
The levels could not be explained by higher milligram-per-kilogram dosing, he
said.
In two of the three phase III studies, children were given a flexible dose
with weekly titration (170 mg, 255 mg, 340 mg, or 425 mg). In the third study
they were given a fixed dose, with those under 30 kg receiving 340 mg daily, and
those over 30 kg receiving 425 mg daily.
The primary outcome was the total score on the school ADHD rating scale. In
all three trials, children taking modafinil had a more significant drop in
scores than those taking placebo. The total score for modafinil recipients-just
over 20-was close to the normative score for a 10-year-old male, according to a
Cephalon statement.
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LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: RHNEWS
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397 of 998 DOCUMENTS
Akron Beacon Journal (Ohio)
March 24, 2006 Friday
In the Nation
SECTION: BRIEFS; Pg. 3
LENGTH: 445 words
WASHINGTON
Drug's use opposed
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday. A
Food and Drug Administration advisory committee voted 12-1 against recommending
modafinil as safe for children with ADHD.
China-trade tension
The Bush administration told China on Thursday that it will be looking for
concrete actions to lower trade tensions between the two nations in advance of a
U.S. visit next month by Chinese President Hu Jintao. Commerce Secretary Carlos
Gutierrez, who will hold talks with Chinese officials next week in Beijing, said
his message will be that the administration is looking for China to play a
responsible role in the global-trading community.
Bush signs trade law
President Bush signed a law Thursday that ended Cold War-era trade restrictions
on Ukraine, opening the way for the former Soviet republic to join the World
Trade Organization.
ATLANTA
TB resistance rises
Federal and international health officials said Thursday they are seeing what
appears to be a disturbing increase around the world in tuberculosis infections
resistant to both the first- and second-line antibiotics used against TB. ``It's
basically a death sentence. If people are failing first- and second-line drugs,
and we don't have in the pipeline a new drug for immediate use, that's a
crisis,'' said Dr. Marcos Espinale, executive secretary of the World Health
Organization's Stop TB Partnership.
SELMER, TENN.
Pastor shot dead
A minister was found shot to death in his parsonage, and authorities searched
Thursday for his wife and three young daughters. The family of Matthew Winkler
was found safe later Thursday in southern Alabama. Police said they want to find
out what his wife, Mary, may know about the slaying.
MELBOURNE, FLA.
3 die in plane crash
A small plane crashed into a parking lot about a mile from an airport runway
Thursday, killing all three people aboard, officials said. Witnesses said the
plane's engines appeared to have shut down before the crash. J.D. Byrider
Systems Inc., a used-car finance company based in Carmel, Ind., identified two
of the passengers as James DeVoe, the company's founder, president and CEO, and
Steele Gudal, DeVoe's son-in-law. The company didn't know the pilot's identity.
TOPEKA, KAN.
House overrides veto
The Kansas House on Thursday overrode Gov. Kathleen Sebelius' veto of a
concealed-weapons bill, allowing it to become law this summer. The vote was
91-33, giving supporters seven votes more than the required two-thirds majority.
Compiled from wire reports.
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 Akron Beacon Journal
All Rights Reserved
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The Associated Press State & Local Wire
March 24, 2006 Friday 12:47 AM GMT
Committee says drug needs more study as possible ADHD treatment
BYLINE: By ANDREW BRIDGES, Associated Press Writer
SECTION: BUSINESS NEWS
LENGTH: 361 words
DATELINE: WASHINGTON
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday.
A Food and Drug Administration advisory committee voted 12-1 against
recommending modafinil as safe for children with ADHD. Earlier Thursday, the
psychopharmacologic drugs panel agreed unanimously that the modafinil works in
treating ADHD.
The FDA is not required to follow the recommendations of its advisory committees
but usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine what risk modafinil may pose for Stevens-Johnson Syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to The Merck Manual.
The FDA's drug chief, Dr. Robert Temple, said one out of roughly 900 children
involved in earlier studies of the drug developed the disease.
Temple and Cephalon spokeswoman Jenifer Antonacci said the agency and company
would discuss the committee's recommendation. The Frazer, Pa.-based company does
not see a "clear link" between its drug and the skin disease, Antonacci said.
In December 1998, the FDA originally approved modafinil, under the brand name
Provigil, to treat adults with sleepiness associated with narcolepsy. The
company has proposed calling a higher-dose version of the pill Sparlon when used
to treat ADHD.
Other drugs already approved by the FDA for ADHD include Ritalin, Strattera and
Adderall.
A different advisory committee recommended on Wednesday that the FDA add
warnings to the labels of those and other ADHD drugs on the market alerting
doctors and parents to the possible risk of hallucinations in the more than 3
million children receiving the popular medications.
Narcolepsy is marked by recurring episodes of daytime sleep, lasting from a few
seconds to an hour. The disease can be merely inconvenient to some people, but
disabling and dangerous to others who may fall asleep while driving or operating
machinery.
On the Net:
Food and Drug Administration: http://www.fda.gov
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
399 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
March 24, 2006
FDA Advisory Committee recommends against approval of Sparlon
LENGTH: 211 words
The FDA's Psychopharmacologic Drugs Advisory Committee has voted not to
recommend FDA approval of Sparlon ( modafinil ) Tablets [C-IV], Cephalon 's
investigational medication for the treatment of attention deficit hyperactivity
disorder (ADHD) in children and adolescents. The Committee voted unanimously
that Sparlon is effective for its intended use, but recommended that the company
collect additional data to support the safety of the drug in children and
adolescents with ADHD. Cephalon is to continue its discussions with the FDA, to
determine the next steps in the review of the drug application. The Committee's
recommendation will be considered by the FDA in its review of the sNDA that
Cephalon submitted for Sparlon in December 2004. Cephalon received an approvable
letter from the FDA with respect to Sparlon in October 2005. Sparlon is a new
formulation and proprietary dosage strength of modafinil, the active ingredient
in Provigil Tablets [C-IV], which is approved for the treatment of adults with
excessive sleepiness associated with narcolepsy, obstructive sleep
apnoea/hypopnoea syndrome and shift work sleep disorder. Sparlon is chemically
distinct from currently approved therapies and if approved, would provide a
unique option for ADHD treatment.
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
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All Rights Reserved
400 of 998 DOCUMENTS
FDAnews Drug Daily Bulletin
March 24, 2006 Friday
REVIEWER RECOMMENDS 'NONAPPROVABLE' ACTION FOR PROVIGIL ADHD INDICATION
SECTION: Vol. 2 No. 311
LENGTH: 347 words
An FDA reviewer is urging the agency not to approve Cephalon's bid to market its
narcolepsy drug Provigil as a treatment for attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, arguing the drug presents
unacceptable risks to that patient population.
The agency's Psychopharmacologic Drugs Advisory Committee is scheduled to
convene March 23 to consider Cephalon's supplemental new drug application (sNDA)
for an ADHD indication for Provigil (modafinil). The company submitted its sNDA
in December 2004, and the FDA issued an approvable letter in October 2005. The
agency decided to hold the advisory committee meeting to address reported risks
associated with the drug, including incidents of skin rash and psychiatric
adverse events.
In background documents released recently, one FDA reviewer said clinical
studies show modafinil was "significantly better than placebo in terms of
efficacy" for treating children and adolescents with ADHD.
But another FDA reviewer said the studies identified "worrisome safety signals,"
including Stevens-Johnson Syndrome and other rashes of unclear significance, a
possible Reye's Syndrome case, and various psychiatric disorders such as
suicidality, depression, agitation, psychosis and phobias. Other safety signals
associated with the drug versus placebo included insomnia (27 percent versus 4
percent), anorexia (16 percent versus 3 percent) and headaches (20 percent
versus 13 percent), the reviewer said.
"Despite the demonstration of clinical efficacy, the safety profile demonstrates
increased and -- in this reviewer's opinion -- unacceptable risks to children
and adolescents, resulting in the recommendation that the agency take a
nonapprovable action on this submission," the reviewer said.
The FDA is not required to follow the advice of its advisers, but usually does.
For background materials on the meeting, access
http://www.fda.gov/oc/advisory/accalendar/2006/cder12544d032306.html
(http://www.fda.gov/oc/advisory/accalendar/2006/cder12544d032306.html).
(http://www.fdanews.com/did)
Release date: March 24, 2006
LOAD-DATE: March 23, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 Washington Business Information, Inc.
All Rights Reserved
401 of 998 DOCUMENTS
National Public Radio (NPR)
March 24, 2006 Friday
SHOW: Morning Edition 10:00 AM EST
FDA Committee Rejects ADHD use for Modafinil
ANCHORS: RENEE MONTAGNE
REPORTERS: JON HAMILTON
LENGTH: 659 words
RENEE MONTAGNE, host:
An expert panel has advised the Food and Drug Administration not to approve a
new drug for attention deficit hyperactivity disorder. Panel members say the
drug isn't safe enough to give to millions of children.
NPR's Jon Hamilton reports.
JON HAMILTON reporting:
Modafinil is already approved for people with sleep disorders. It helps them
stay alert. The company that makes Modafinil, Cephalon, was hoping to expand
into the much larger market for ADHD drugs. The advisory panel has dimmed that
hope.
Its recommendation came at the end of an all-day meeting in Gaithersburg,
Maryland. But the tone was set by the day's first speaker. Dr. Glen Manheim(ph),
an FDA scientist, described children who developed severe skin rashes after
taking Modafinil.
Mr. GLEN MANHEIM (scientist for the Food and Drug Administration): One subject
had peeling and blistering over the entire body, with lips and urinary tract
involvement. The drug was stopped, but the rash progressed to involve peeling,
blistering, mucosal involvement, over days.
HAMILTON: Manheim said the drug appeared to have caused an extremely rare skin
problem called Stevens-Johnson syndrome. This was a mild case, but Manheim says
the condition often requires treatment in a hospital burn unit, and some
patients die.
Manheim says there might be big problems if even 10 percent of the 2.5 million
children on ADHD drugs switched to Modafinil.
Mr. MANHEIM: Based on the known mortality associated with (unintelligible) with
Steven-Johnson, we would expect from 25 to over 400 deaths to occur.
HAMILTON: Other FDA officials were less concerned. And Cephalon argued that
millions of people around the world have taken the drug without problems.
It was also unclear just how many children had actually developed severe skin
problems. Dr. Daniel Pine, a panel member from the National Institutes of
Health, asked for help during the discussion.
Dr. DANIEL PINE (Chief, Section on Development and Affective Neuroscience): So
do we have three cases where everybody would agree that these are concerning
dermatologic issues? Do we have one case? Do we have two that are somewhat
concerning, a third that's suggestive? And, you know, can we get some agreement
on that?
HAMILTON: In the end, the panelists could only agree about the one case. And
records showed the boy's skin condition never even kept him home from school.
The panelists also heard an impassioned plea from Dr. Joseph Biederman, a
Harvard Psychiatrist who's done research on Modafinil for Cephalon. Biederman
says ADHD patients need choices beyond the traditional stimulants they're
usually prescribed.
Dr. JOSEPH BIEDERMAN (Professor of Psychiatry, Harvard Medical School): Although
the stimulants are clearly an effective treatment for ADHD, a sizable number, in
the order of 40 percent are non-responsive or not tolerating this treatment,
calling for alternative treatment for this condition.
HAMILTON: Ultimately, the panel took the cautious road. Twelve of thirteen
panelists said the FDA should not approve Modafinil.
Their recommendation came a day after a different FDA committee heard a litany
of concerns about existing drugs for ADHD. These drugs have been linked to heart
problems and suicidal thoughts. The recommendation is a major blow for the drug
company, Cephalon. Gary Nachman is a pharmaceutical analyst for the investment
company, Leerink. He said approval would have meant a lot of money for Cephalon.
Mr. GARY NACHMAN (Director Analyst, Equity Research at Leerink Swann & Company):
I forecast sales of about 120 million this year, growing to a little bit over
400 million in 2010. And, at that point, it would represent about 20 to 25
percent of the company's total sales.
HAMILTON: Nachman said the FDA panel didn't slam the door on Modafinil. Members
suggested that a new study of several thousand children could show whether
severe skin problems are a major issue or just a rare occurrence.
Jon Hamilton, NPR News.
LOAD-DATE: April 17, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Transcript
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All Rights Reserved
402 of 998 DOCUMENTS
The Washington Post
March 24, 2006 Friday
Final Edition
Use of Drug to Treat ADHD in Children Opposed
BYLINE: Associated Press
SECTION: A Section; A11
LENGTH: 227 words
The narcolepsy drug modafinil should not be approved as a treatment for
attention-deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said yesterday.
A Food and Drug Administration advisory committee voted 12 to 1 against
recommending modafinil as safe for children with ADHD. Earlier, the
psychopharmacologic drugs panel unanimously agreed that modafinil works as a
treatment for ADHD.
The FDA is not required to follow the recommendations of its advisory panels but
usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine the risk modafinil may pose for Stevens-Johnson syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to the Merck Manual.
The FDA's drug evaluation chief, Robert J. Temple, said one out of 900 children
involved in earlier studies of the drug developed the disease. He and Cephalon
spokeswoman Jenifer Antonacci said the agency and the company will discuss the
committee's recommendation.
In December 1998, the FDA approved modafinil, under the brand name Provigil, for
treating adults with sleepiness associated with narcolepsy. Other drugs approved
by the FDA for ADHD include Ritalin, Strattera and Adderall.
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 The Washington Post
403 of 998 DOCUMENTS
Xinhua General News Service
March 24, 2006 Friday 1:15 AM EST
FDA panel recommends against treating ADHD with modafinil
SECTION: WORLD NEWS
LENGTH: 149 words
DATELINE: WASHINGTON
A U.S. Food and Drug Administration (FDA) advisory committee on Thursday
recommended against using the narcolepsy drug modafinil to treat attention
deficit hyperactivity disorder (ADHD) in children and teenagers.
The psychopharmacologic drugs panel voted 12-1 against the recommendation.
It concluded that the drug is effective against ADHD, but can't be regarded as
safe for the use by children for the time being, reports reaching here said.
The panel was most concerned about a possible link with skin rashes and
recommended that the drug's manufacturer, Cephalon Inc., conduct a 3,000-patient
trial to measure the risk.
The drug is also found in link with psychiatric effects including mania and
aggression.
Modafinil is being marketed as Provigil for treating sleep disorders. Cephalon
is seeking to sell the drug under the name Sparlon for children with ADHD.
LOAD-DATE: March 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Xinhua News Agency
404 of 998 DOCUMENTS
Associated Press Online
March 24, 2006 Friday 10:10 PM GMT
Panel: Drug Shouldn't Be Used for ADHD Yet
BYLINE: By ANDREW BRIDGES, Associated Press Writer
SECTION: WASHINGTON DATELINE
LENGTH: 361 words
DATELINE: WASHINGTON
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday.
A Food and Drug Administration advisory committee voted 12-1 against
recommending modafinil as safe for children with ADHD. Earlier Thursday, the
psychopharmacologic drugs panel agreed unanimously that the modafinil works in
treating ADHD.
The FDA is not required to follow the recommendations of its advisory committees
but usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine what risk modafinil may pose for Stevens-Johnson Syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to The Merck Manual.
The FDA's drug chief, Dr. Robert Temple, said one out of roughly 900 children
involved in earlier studies of the drug developed the disease.
Temple and Cephalon spokeswoman Jenifer Antonacci said the agency and company
would discuss the committee's recommendation. The Frazer, Pa.-based company does
not see a "clear link" between its drug and the skin disease, Antonacci said.
In December 1998, the FDA originally approved modafinil, under the brand name
Provigil, to treat adults with sleepiness associated with narcolepsy. The
company has proposed calling a higher-dose version of the pill Sparlon when used
to treat ADHD.
Other drugs already approved by the FDA for ADHD include Ritalin, Strattera and
Adderall.
A different advisory committee recommended on Wednesday that the FDA add
warnings to the labels of those and other ADHD drugs on the market alerting
doctors and parents to the possible risk of hallucinations in the more than 3
million children receiving the popular medications.
Narcolepsy is marked by recurring episodes of daytime sleep, lasting from a few
seconds to an hour. The disease can be merely inconvenient to some people, but
disabling and dangerous to others who may fall asleep while driving or operating
machinery.
On the Net:
Food and Drug Administration: http://www.fda.gov
LOAD-DATE: March 25, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
405 of 998 DOCUMENTS
Associated Press Financial Wire
March 23, 2006 Thursday 11:22 PM GMT
Narcolepsy drug needs more study as possible ADHD treatment, federal advisers
say
BYLINE: By ANDREW BRIDGES, Associated Press Writer
SECTION: BUSINESS NEWS
LENGTH: 381 words
DATELINE: WASHINGTON
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday.
A Food and Drug Administration advisory committee voted 12-1 against
recommending modafinil as safe for children with ADHD. Earlier Thursday, the
psychopharmacologic drugs panel agreed unanimously that the modafinil works in
treating ADHD.
The FDA is not required to follow the recommendations of its advisory committees
but usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine what risk modafinil may pose for Stevens-Johnson Syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to The Merck Manual.
The FDA's drug chief, Dr. Robert Temple, said one out of roughly 900 children
involved in earlier studies of the drug developed the disease.
Temple and Cephalon spokeswoman Jenifer Antonacci said the agency and company
would discuss the committee's recommendation. The Frazer, Pa.-based company does
not see a "clear link" between its drug and the skin disease, Antonacci said.
In December 1998, the FDA originally approved modafinil, under the brand name
Provigil, to treat adults with sleepiness associated with narcolepsy. The
company has proposed calling a higher-dose version of the pill Sparlon when used
to treat ADHD.
The ADHD drugs include Ritalin, manufactured by Novartis Pharmaceuticals Corp.
and in generic form by other companies; Adderall, made by Shire Pharmaceuticals
Inc.; and Strattera, produced by Eli Lilly and Co.
A different advisory committee recommended on Wednesday that the FDA add
warnings to the labels of those and other ADHD drugs on the market alerting
doctors and parents to the possible risk of hallucinations in the more than 3
million children receiving the popular medications.
Narcolepsy is marked by recurring episodes of daytime sleep, lasting from a few
seconds to an hour. The disease can be merely inconvenient to some people, but
disabling and dangerous to others who may fall asleep while driving or operating
machinery.
On the Net:
Food and Drug Administration: http://www.fda.gov
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
406 of 998 DOCUMENTS
The Associated Press
March 23, 2006 Thursday 11:22 PM GMT
Narcolepsy drug needs more study as possible ADHD treatment, federal advisers
say
BYLINE: By ANDREW BRIDGES, Associated Press Writer
SECTION: BUSINESS NEWS
LENGTH: 381 words
DATELINE: WASHINGTON
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday.
A Food and Drug Administration advisory committee voted 12-1 against
recommending modafinil as safe for children with ADHD. Earlier Thursday, the
psychopharmacologic drugs panel agreed unanimously that the modafinil works in
treating ADHD.
The FDA is not required to follow the recommendations of its advisory committees
but usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine what risk modafinil may pose for Stevens-Johnson Syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to The Merck Manual.
The FDA's drug chief, Dr. Robert Temple, said one out of roughly 900 children
involved in earlier studies of the drug developed the disease.
Temple and Cephalon spokeswoman Jenifer Antonacci said the agency and company
would discuss the committee's recommendation. The Frazer, Pa.-based company does
not see a "clear link" between its drug and the skin disease, Antonacci said.
In December 1998, the FDA originally approved modafinil, under the brand name
Provigil, to treat adults with sleepiness associated with narcolepsy. The
company has proposed calling a higher-dose version of the pill Sparlon when used
to treat ADHD.
The ADHD drugs include Ritalin, manufactured by Novartis Pharmaceuticals Corp.
and in generic form by other companies; Adderall, made by Shire Pharmaceuticals
Inc.; and Strattera, produced by Eli Lilly and Co.
A different advisory committee recommended on Wednesday that the FDA add
warnings to the labels of those and other ADHD drugs on the market alerting
doctors and parents to the possible risk of hallucinations in the more than 3
million children receiving the popular medications.
Narcolepsy is marked by recurring episodes of daytime sleep, lasting from a few
seconds to an hour. The disease can be merely inconvenient to some people, but
disabling and dangerous to others who may fall asleep while driving or operating
machinery.
On the Net:
Food and Drug Administration: http://www.fda.gov
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Associated Press
All Rights Reserved
407 of 998 DOCUMENTS
Drug Industry Daily
March 23, 2006 Thursday
FDA Reviewer Recommends 'Nonapprovable' Action for Provigil ADHD Indication
SECTION: Vol. 5 No. 58
LENGTH: 661 words
An FDA reviewer is urging the agency not to approve Cephalon's bid to market its
narcolepsy drug Provigil as a treatment for attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, arguing the drug presents
unacceptable risks to that patient population.
The agency's Psychopharmacologic Drugs Advisory Committee is scheduled to
convene March 23 to consider Cephalon's supplemental new drug application (sNDA)
for an ADHD indication for Provigil (modafinil). The company submitted its sNDA
in December 2004, and the FDA issued an approvable letter in October 2005. The
agency decided to hold the advisory committee meeting to address reported risks
associated with the drug, including incidents of skin rash and psychiatric
adverse events.
In background documents released March 22, one FDA reviewer said clinical
studies show modafinil was "significantly better than placebo in terms of
efficacy" for treating children and adolescents with ADHD.
But another FDA reviewer said the studies identified "worrisome safety signals,"
including Stevens-Johnson Syndrome and other rashes of unclear significance, a
possible Reye's Syndrome case, and various psychiatric disorders such as
suicidality, depression, agitation, psychosis and phobias. Other safety signals
associated with the drug versus placebo included insomnia (27 percent versus 4
percent), anorexia (16 percent versus 3 percent) and headaches (20 percent
versus 13 percent), the reviewer said.
"Despite the demonstration of clinical efficacy, the safety profile demonstrates
increased and -- in this reviewer's opinion -- unacceptable risks to children
and adolescents, resulting in the recommendation that the agency take a
nonapprovable action on this submission," the reviewer said.
By contrast, Cephalon said the treatment of modafinil is "generally safe and
well tolerated" in children and adolescents with ADHD. The drug has been tested
in 933 ADHD patients from this population group, the firm said in a document
prepared for the advisory committee meeting.
Studies found a low occurrence of serious adverse events and adverse events
leading to withdrawal, the company noted. The most common adverse events --
insomnia, anorexia and headache -- are common to drugs that affect the central
nervous system, Cephalon said. "These events were usually mild to moderate in
severity and seldom required discontinuation of treatment with the study drug,"
the firm noted.
The firm also reported few adverse events of "special interest" such as skin
rash and psychiatric episodes. There were two cases of children with possible
Stevens-Johnson Syndrome, which is manifested as skin blistering, the firm said.
Neither of those patients was hospitalized. There were a "relatively small
number of psychiatric adverse events" in all modafinil development programs, the
firm said. In addition, the studies found no cardiovascular safety issues.
"Because current medications for ADHD may not be optimal for up to 40 percent of
patients, there is a need for additional safe and effective pharmacologic
treatment options for children and adolescents with ADHD," Cephalon said. The
company is proposing to market the drug under the brand name Sparlon.
FDA advisers will vote on whether modafinil has been shown to be effective and
"acceptably safe" in the treatment of ADHD in this population. Assuming the drug
is to be considered for approval, the agency also will ask the panel's advice on
what kind of risk management plan should be implemented regarding the serious
skin rash signal, how the concern about skin rashes should be addressed in
product labeling, and if there should be a requirement for a postmarketing study
to better understand serious skin rashes.
The FDA is not required to follow the advice of its advisers, but usually does.
For background materials on the meeting, access
http://www.fda.gov/oc/advisory/accalendar/2006/cder12544d032306.html. -- Neal
Learner
Release date: March 23, 2006
LOAD-DATE: March 22, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 Washington Business Information, Inc.
All Rights Reserved
408 of 998 DOCUMENTS
Drug Industry Daily
March 23, 2006 Thursday
Full Issue
SECTION: Vol. 5 No. 58
LENGTH: 3081 words
Vol. 5, No. 58
FDA Reviewer Recommends 'Nonapprovable' Action for Provigil ADHD Indication
An FDA reviewer is urging the agency not to approve Cephalon's bid to market its
narcolepsy drug Provigil as a treatment for attention-deficit/hyperactivity
disorder (ADHD) in children and adolescents, arguing the drug presents
unacceptable risks to that patient population.
The agency's Psychopharmacologic Drugs Advisory Committee is scheduled to
convene March 23 to consider Cephalon's supplemental new drug application (sNDA)
for an ADHD indication for Provigil (modafinil). The company submitted its sNDA
in December 2004, and the FDA issued an approvable letter in October 2005. The
agency decided to hold the advisory committee meeting to address reported risks
associated with the drug, including incidents of skin rash and psychiatric
adverse events.
In background documents released March 22, one FDA reviewer said clinical
studies show modafinil was "significantly better than placebo in terms of
efficacy" for treating children and adolescents with ADHD.
But another FDA reviewer said the studies identified "worrisome safety signals,"
including Stevens-Johnson Syndrome and other rashes of unclear significance, a
possible Reye's Syndrome case, and various psychiatric disorders such as
suicidality, depression, agitation, psychosis and phobias. Other safety signals
associated with the drug versus placebo included insomnia (27 percent versus 4
percent), anorexia (16 percent versus 3 percent) and headaches (20 percent
versus 13 percent), the reviewer said.
"Despite the demonstration of clinical efficacy, the safety profile demonstrates
increased and -- in this reviewer's opinion -- unacceptable risks to children
and adolescents, resulting in the recommendation that the agency take a
nonapprovable action on this submission," the reviewer said.
By contrast, Cephalon said the treatment of modafinil is "generally safe and
well tolerated" in children and adolescents with ADHD. The drug has been tested
in 933 ADHD patients from this population group, the firm said in a document
prepared for the advisory committee meeting.
Studies found a low occurrence of serious adverse events and adverse events
leading to withdrawal, the company noted. The most common adverse events --
insomnia, anorexia and headache -- are common to drugs that affect the central
nervous system, Cephalon said. "These events were usually mild to moderate in
severity and seldom required discontinuation of treatment with the study drug,"
the firm noted.
The firm also reported few adverse events of "special interest" such as skin
rash and psychiatric episodes. There were two cases of children with possible
Stevens-Johnson Syndrome, which is manifested as skin blistering, the firm said.
Neither of those patients was hospitalized. There were a "relatively small
number of psychiatric adverse events" in all modafinil development programs, the
firm said. In addition, the studies found no cardiovascular safety issues.
"Because current medications for ADHD may not be optimal for up to 40 percent of
patients, there is a need for additional safe and effective pharmacologic
treatment options for children and adolescents with ADHD," Cephalon said. The
company is proposing to market the drug under the brand name Sparlon.
FDA advisers will vote on whether modafinil has been shown to be effective and
"acceptably safe" in the treatment of ADHD in this population. Assuming the drug
is to be considered for approval, the agency also will ask the panel's advice on
what kind of risk management plan should be implemented regarding the serious
skin rash signal, how the concern about skin rashes should be addressed in
product labeling, and if there should be a requirement for a postmarketing study
to better understand serious skin rashes.
The FDA is not required to follow the advice of its advisers, but usually does.
For background materials on the meeting, access
http://www.fda.gov/oc/advisory/accalendar/2006/cder12544d032306.html. -- Neal
Learner
FDA Advisory Committee Considers Psychosis Warning for ADHD Drugs
The FDA's Pediatric Advisory Committee discussed the need for new warnings about
the increased risk of psychosis and mania events associated with attention
deficit/hyperactivity disorder (ADHD) drugs at its March 22 meeting, but the
panel had not made any recommendations by DID press time.
FDA drug-safety reviewers earlier had called for new warnings regarding these
conditions (DID, March 16). According to the agency, the predominance of
patients reporting hallucinations involving insects, snakes or worms is striking
and deserves further evaluation. In many patients, the events ceased after they
stopped taking the drug, the FDA reviewers added.
The committee's scheduled recommendation late March 22 follows its
recommendation last month to include a black box warning that highlights
possible links to heart attack and stroke (DID, Feb. 13). Over the past year,
ADHD drugs have been linked to hypertension, chest pain, arrhythmia and
tachycardia, among other conditions.
The ADHD drug market generated more than $3 billion in sales in 2004 and ACHD
drugs are prescribed to 2.5 million children between the ages of 4 and 17.
These drugs also are increasingly prescribed to young adults between the ages of
20 and 44, according to Medco Health Solutions. The number of adults taking
these medicines grew more than 139 percent from 2000 to 2005, outpacing
increases in children 19 years and younger by a margin of 82 percent, Medco
said.
Adult use of these drugs can lead to heart problems, the group added. "The
possible cardiovascular issues associated with ADHD drugs should be weighted
very seriously when prescribing these drugs for adults since they're at a
greater risk of heart disease and stroke than children," said Robert Epstein,
Medco's chief medical officer.
An executive with Eli Lilly, which makes the ADHD drug Strattera (atomoxetine),
could not comment on the financial effect of a potential black box warning for
psychosis. "I don't know the impact, because [Strattera] is still a top seller"
even with existing warnings, Albert Allen, Eli Lilly's medical director, told
DID.
FDA Extends Review Period for Reintroduction of Tysabri
The FDA will extend its review period for the reintroduction of Elan and Biogen
Idec's multiple sclerosis (MS) drug Tysabri by up to 90 days, according to the
companies, which pulled the drug last year following reports that it may be
linked to a rare brain disease.
The agency requires additional time to review the company's information for a
Tysabri (natalizumab) risk management plan, the firms said March 22. Under the
revised timeline, Elan and Biogen anticipate a decision from the FDA by June 28.
The firms withdrew Tysabri in February 2005 following reports that three
patients taking the drug had developed progressive multifocal
leukoencephalopathy (PML), a rare and deadly nerve disease (DID, March 1, 2005,
Page 1).
On March 8, an FDA advisory panel voted unanimously in favor of returning the
product to the market under certain conditions (DID, March 9). The panel
recommended the companies establish a patient registry to monitor side effects.
The advisers also voted 7 to 5 to allow Tysabri on the market as a first-line
treatment. FDA reviewers have suggested various restrictions for Tysabri if it
is reintroduced, including limits on prescribing and dispensing the drug (DID,
Feb. 7).
One pharmaceutical analyst said the FDA may take a more conservative view of the
drug's risks and benefits than the advisory committee. There is a 25 percent
probability the agency will only reapprove Tysabri as a second-line therapy to
treat MS patients who have shown intolerance or failed to respond to other MS
therapies, Merrill Lynch research analyst Erica Whittaker said in a March 22
research note.
Elan's share prices are in line with peak Tysabri sales of over $2 billion,
which means treating over 100,000 patients, Whittaker noted. "We believe this
scenario is only possible if prescribing and distribution restrictions are
lifted following no further cases of PML or other serious infections, which we
think is unlikely," she said.
Merrill Lynch's sales forecast for Tysabri remains about $500 million in 2010,
based on the firm's discussions with multiple clinicians who say they would use
Tysabri on average in less than 10 percent of their patients, Whittaker said. --
Neal Learner
Bristol-Myers, Sanofi-Aventis Settle With Apotex Over Plavix
Bristol-Myers Squibb (BMS) and sanofi-aventis have reached a settlement with
Apotex over the generic firm's patent challenge to the blood thinner Plavix.
But the brand firms also acknowledged there is a "significant risk" the FTC will
not approve the agreement because of antitrust concerns. If the FTC does not
approve the settlement, Apotex will receive an undisclosed payment from the two
companies and litigation will resume, BMS and sanofi-aventis said March 21.
BMS distributes Plavix (clopidogrel bisulfate) in the U.S. for sanofi-aventis.
The drug had sales of $5.9 billion in 2005, according to IMS Health.
A patent trial had been scheduled for June in the U.S. District Court for the
Southern District of New York, BMS and sanofi-aventis said.
Under the agreement, Apotex would be able to launch generic Plavix eight months
before the Plavix patent expires in November 2011, or in May 2012 if Plavix
receives a pediatric extension of the patent. Apotex also could launch its
generic earlier if another generic enters the market before this time. BMS and
sanofi-aventis have proposed a similar settlement with generic firm Dr. Reddy's.
The FDA granted final approval to Apotex' application to market generic Plavix
in January. But analysts have said Apotex would not launch the product until the
U.S. litigation was resolved (DID, Jan. 26). Apotex unsuccessfully challenged
the Plavix patent in a Canadian court in 2005 (DID, March 24, 2005, Page 1).
Meanwhile, Teva Pharmaceutical and Canadian drugmaker Cobalt Pharmaceuticals
have also challenged the Plavix patent. BMS and sanofi-aventis said they will
"communicate with them in due course." -- Dar Haddix
Study Finds Levitra Effective in Men Taking Blood Pressure Drugs
A clinical study has found GlaxoSmithKline (GSK) and Schering-Plough's erectile
dysfunction (ED) drug Levitra is effective in men taking high blood pressure
drugs, the firms announced.
According to data published in the Journal of Sexual Medicine, patients treated
with Levitra (vardenafil HCl), a PDE5 inhibitor, experienced an 83 percent
overall success rate in erectile function while also receiving one or more
antihypertensive drugs, the companies said March 22.
"This study demonstrated that Levitra was well-tolerated when used concomitantly
with antihypertensive medications in patients not previously treated with PDE5
inhibitors," said study author Hermann van Ahlen of the University of Munster in
Germany.
Hypertension is a major risk factor for ED and affects 29.4 million men in the
U.S., according to the firms. Many blood-pressure-lowering drugs may adversely
affect erectile function, the companies added.
The study gave either Levitra or a placebo to 354 men who were taking
hypertension drugs -- not including alpha blockers -- and had experienced ED for
more than 6 months. In the Levitra group, 83 percent of men reported having an
erection compared to 58 percent of men taking the placebo.
NitroMed Executives Quit; Sales of BiDil Lag
Two top executives at NitroMed have resigned amid slow sales of the
heart-failure drug BiDil, the first product indicated specifically for African
Americans.
NitroMed announced the resignations March 21 of CEO Michael Loberg and chief
financial officer (CFO) Lawrence Bloch. The company has appointed Argeris
Karabelas as interim CEO and Kenneth Bate as CFO.
During a conference call March 22, Karabelas said NitroMed's board "felt it was
time for a course correction."
Sales of BiDil (isosorbide dinitrate/hydralazine hydrochloride) have not met
expectations because of problems with insurance reimbursement, sales
productivity and product promotion, executives said during the conference call.
BiDil sales were only $4.5 million in 2005, well below analyst estimates.
The drug was launched last July after a study found that black patients with
heart failure experienced a 43 percent improvement in survival after taking
BiDil, compared to those taking standard heart-failure therapy plus a placebo
(DID, July 17, Page 2).
NitroMed has struggled to get insurance companies to put BiDil on their list of
preferred drugs, because it is composed of two generics already available to
patients.
"There is absolutely no question of the value of BiDil in the treatment of
congestive heart failure in African Americans," Karabelas said. "We need to
forcefully get this point across to managed care and also to be flexible in our
contracts so we can achieve access, which is what we need to drive sales."
Karabelas said the company has appointed a senior manager with "exceptional
leadership" who "has the right ideas for increasing the productivity of the
sales force." The company downsized its sales force in January from 195 to 144
sales representatives, eliminating positions in less productive sales
territories.
Another problem has been getting doctors to switch patients to BiDil if their
condition has already stabilized on their current drug regimen. "What's been
difficult to explain is that patients who are stabilized need the benefit of
this drug," Karabelas said. "Doctors are not comfortable switching a patient's
prescription when they're stable," he noted.
The company's key objectives include exploring copromotion opportunities for
BiDil -- especially in hospital settings where many cardiologists are based --
and improving BiDil's formulary status with managed care companies, Karabelas
said. -- Dar Haddix
PBM Disclosure Proponents Lose State Ballot Initiatives, But Predict Long-Term
Success
A national push to increase the transparency of financial dealings between
drugmakers and pharmaceutical benefit managers (PBMs) in Medicaid negotiations
has suffered numerous setbacks in state legislatures this year, but proponents
argue that upcoming legal battles could turn the tide.
The National Legislative Association of Prescription Drug Prices (NLARX) is
undertaking a multistate effort to pass legislation that would require PBMs to
disclose the prices they pay for different drugs and require any rebates they
receive be sent to the states. NLARX is a nonprofit organization managed by
state legislators working across state lines to make prescription drugs more
affordable and accessible to consumers, with its primary focus on lowering drug
prices.
The organization's effort comes as states face higher costs for their Medicaid
programs, which are growing by 8 to 9 percent per year and accounting for a
bigger chunk of state budgets than education (DID, Jan. 3).
But many such efforts have failed, with defeats this year in Colorado,
Connecticut, New Hampshire, Oklahoma, Virginia and Washington State. What had
seemed like a trend toward greater disclosure in recent years -- with victories
in Maine and Washington, D.C. -- seems to have dried up, according to opponents
such as the Pharmaceutical Care Management Association (PCMA), which represents
the PBM industry. These efforts are failing "literally from coast to coast,"
said Phil Blando, PCMA's spokesman.
Maine's Unfair Prescription Drug Practices Act, enacted in June 2003, requires
PBMs to disclose pricing information negotiated with drugmakers and pass on the
savings to consumers to avoid conflicts of interest.
But PCMA believes recent efforts have been defeated because state legislatures
have realized that greater disclosure would result in higher prices for health
plans, employers and PBMs and actually lead to higher drug costs for consumers.
It is "very clear there is a cost impact," said Blando, noting that the recent
push for disclosure is "failing to gain traction at the state level."
Greater disclosure creates an artificial price floor that drug companies will
not go below, Blando said. Making this information public is "like playing poker
with all your cards up," he added, and tilts "contracts and bargaining in favor
of the drug companies." PCMA will continue lobbying state legislatures to oppose
future disclosure proposals, Blando said.
But proponents argue there are key legal battles that could change the tide
toward greater disclosure. Currently, PBMs are challenging the Maine and
Washington, D.C., plans in court and are using the legal uncertainty this is
causing to undermine efforts in other states, said Sharon Treat, NLARX's
executive director.
"When there's uncertainty, there's a tendency to just vote 'no,'" on
legislation, Treat said. But if NLARX wins in these two cases, the group will
argue that there is no longer the legal uncertainty about disclosure laws, which
should enhance state legislative support for these bills, she said.
The group also disputes PCMA's contention that greater disclosure equals higher
prices. Proposed state legislation contains confidentiality requirements that
prevent negotiating parties from revealing the prices they paid. These bills
include heavy fines for disclosure of this data so that competitors will not
know what the other is paying, and there will therefore be no artificial price
floor, Treat said.
Greater disclosure puts the client -- the states -- "in a better bargaining
position and that's what [PBMs] don't want," Treat said. A track record of price
savings is becoming evident in states that require disclosure, she noted. The
multimillion-dollar settlements PBMs have paid for improper Medicaid
negotiations with states are another sign of the savings that would be reaped if
these dealings were transparent, according to Treat.
Meanwhile, PCMA is appealing to the U.S. Supreme Court a decision by the U.S.
Federal Court of Appeals for the First Circuit last November to uphold the Maine
law. Their petition for review will be submitted by April 10, Blando said. The
group also is waiting for the U.S. District Court for the District of Columbia
to decide whether the Washington, D.C., law represents an illegal taking of PBM
trade secrets and represents improper state regulation of areas -- such as the
Employee Retirement Income Security Act of 1974 -- which are under the purview
of the federal government. -- Stephen Langel
Release date: March 23, 2006
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March 23, 2006 Thursday
FDA ADVISORY COMMITTEE DISCUSSES NEW ADHD DRUG APPLICATION PROVIGIL
SECTION: FDA ADVISORY COMMITTEE MEETING
LENGTH: 53395 words
DATELINE: GAITHERSBURG, MARYLAND
FOOD AND DRUG ADMINISTRATION PSYCHOPHARMACOLOGIC DRUGS ADVISORY COMMITTEE
DISCUSSES NEW ADHD DRUG APPLICATION PROVIGIL
MARCH 23, 2006
SPEAKERS: PSYCHOPHARMACOLOGIC DRUGS ADVISORY COMMITTEE:
WAYNE K. GOODMAN, M.D., CHAIR CICELY REESE, PHARM.D., EXECUTIVE SECRETARY JORGE
ARMENTEROS, M.D. JEAN BRONSTEIN, R.N., M.S. ANDREW C. LEON, M.D. DANIEL S. PINE,
M.D. DELBERT ROBINSON, M.D. PHILIP WANG, M.D., DR.P.H. BARBARA WELLS, PHARM.D.
TEMPORARY VOTING MEMBERS:
MICHAEL BIGBY, M.D. DEBORAH DOKKEN, MPA RICHARD MALONE, M.D. CYNTHIA PFEFFER,
M.D. MARSHA RAPPLEY, M.D.
NON-VOTING MEMBER:
DILIP MEHTA, M.D., PH.D.
FDA PARTICIPANTS:
ROBERT TEMPLE, M.D. THOMAS P. LAUGHREN, M.D. PAUL J. ANDREASON, M.D. GLENN
MANNHEIM, M.D. SPONSOR REPRESENTATIVES:
VICTOR RACZKOWSKI, M.D. JOSEPH BIEDERMAN, M.D. SRDJAN STANKOVIC, M.D. LESLEY
RUSSELL, M.R.C.P.
[*] GOODMAN: We expect a few more people to join us around the table but I want
to make sure that we start on time. Welcome, everyone, to the
Psychopharmacologic Drugs Advisory Committee, or the PDAC.
We have been asked today by the FDA to advise them on a new drug application for
modafinil in the treatment of attention deficit hyperactivity disorder, ADHD.
Most of the questions, as will be articulated by the FDA, concern safety issues.
Yesterday there was a meeting of the Pediatric Advisory Committee which
discussed a range of safety issues concerning medications used in the treatment
of ADHD, the stimulants as well as Strattera, and actually some data emerged on
modafinil as well during those discussions. I was present as an observer during
those meetings. I am glad I was there.
Some of the members of the committee that are here today were also present
yesterday so I think a lot of heavy lifting was done yesterday on some of these
important side effect issues that will help inform us in our deliberations
today.
My remarks are going to be unusually brief, in part because my voice is
strained. My voice has not been cooperating for the last few days. In fact,
sometimes I am not sure it is my voice -- I don't know what kind of symptom that
would mean. But we have a backup plan. Danny Pine, when he comes here, in case
my voice fails, he will become my voice.
I also want to put you on notice that Cicely Reese may deliver at any moment! I
am not kidding! So, we have plans for her transportation and replacement should
that occur. Please bear with us under these circumstances.
Now I would just like to go around the table and ask everyone to introduce
themselves.
Let's start from the FDA end.
LAUGHREN: Tom Laughren, from the Division of Psychiatry Products.
ANDREASON: Paul Andreason, Division of Psychiatry Products.
MANNHEIM: Glenn Mannheim, Division of Psychiatry Products.
BIGBY: I am Michael Bigby, dermatologist from Boston.
RAPPLEY: Marsha Rappley, Developmental Behavior Pediatrics, Michigan State
University.
WANG: Phil Wang, psychiatrist and epidemiologist from Harvard Medical School.
REESE: Cicely Reese, executive secretary.
GOODMAN: Wayne Goodman, chair of this committee as well as chair of the
Department of Psychiatry, University of Florida.
LEON: I am Andrew Leon, professor of biostatistics at Cornell Medical School.
ROBINSON: I am Delbert Robinson. I am a psychiatrist at the Zucker Hillside
Hospital and the Albert Einstein College of Medicine.
PFEFFER: I am Cynthia Pfeffer, child and adolescent psychiatrist at Weill
Medical College of Cornell University.
ARMENTEROS: Jorge Armenteros, child and adolescent psychiatrist in Miami,
Florida.
WELLS: Barbara Wells, I am dean of the School of Pharmacy at the University of
Mississippi.
DOKKEN: I am Deborah Dokken. I am the patient family rep. on the Pediatric
Advisory Committee.
MALONE: I am Richard Malone, a child psychiatrist from Drexel University College
of Medicine.
MEHTA: Dilip Mehta, retired physician from the drug industry. I am the industry
representative on the committee.
GOODMAN: Thank you all very much. I think Daniel Pine will be joining us
shortly. I would now like to turn the microphone over to Cicely Reese to go over
some housekeeping, particularly the conflict of interest statements.
REESE: The following announcement addresses the issue of conflict of interest
and is made part of the record to preclude even the appearance of such at this
meeting.
Based on the submitted agenda and all financial interests reported by the
committee's participants, it has been determined that all interests in firms
regulated by the Center for Drug Evaluation and Research present no potential
for an appearance of a conflict of interest at this meeting with the following
exceptions:
In accordance with 18 USC, Section 208(b)(3), Dr. Wayne Goodman has been granted
a full waiver for his employer's related contract with a competitor, funded
between $100,001 and $300,000 per year. His employer also has related contracts
with another competitor, funded for less than $100,001 per year.
Dr. Andrew Leon has been granted a waiver under 21 USC, 355(n)(4) for his
ownership of stock in a competitor. This stock is valued from $5,001 to $25,000.
A copy of the waiver statements may be obtained by submitting a written request
to the agency's Freedom of Information Office, Room 12A-30 of the Parklawn
Building.
We would also like to note that Dr. Dilip Mehta has been invited to participate
as an industry representative, acting on behalf of regulated industry. Dr.
Mehta's role on this committee is to represent industry interests in general and
not any one particular company. Dr. Mehta is retired from Pfizer.
In the event that the discussions involve any other products or firms not
already on the agenda for which the FDA participant has a financial interest,
the participants are aware of the need to exclude themselves from such
involvement and their exclusion will be noted for the record.
With respect to all other participants, we ask in the interest of fairness that
they address any current or previous financial involvement with any firms whose
products they wish to comment upon.
Thank you.
GOODMAN: Dr. Daniel Pine just joined us so I wonder if you could introduce
yourself.
PINE: Danny Pine, Chief of Developmental Studies, Mood and Anxiety Disorders
Program, National Institute of Mental Health Intramural Research Program and I
am a child and adolescent psychiatrist.
GOODMAN: In a moment I will turn over the floor to Dr. Laughren who will give us
the introductory remarks. I think for all of us who have read through these
briefing materials one of the issues that emerges, that didn't surface during
yesterday's discussions, are questions about dermatological reactions.
I see that we will also have the benefit of an intensive review of those issues
as well to help us in our decision-making today.
So, Tom, would you please come forward?
Thank you.
LAUGHREN: I would like to welcome everyone to today's meeting. Before I
introduce the topics for today's meeting I would like to acknowledge the service
of one of your colleagues on this committee whose term is ending in June, and
that colleague is Wayne Goodman.
This has been a particularly busy time for the committee, as you know, and Wayne
has, of course, been the chair of the committee for much of this time.
Serving on this committee, again as all of you know, is a very demanding and
sometimes stressful task and I hope that you all understand how much we
appreciate the help that you give us. Now, Wayne told me after the September,
2004 meeting on antidepressants and suicidality in pediatric patients that he
didn't have any friends anymore in the academic and clinical community. I just
want to assure him that he always has friends here, at FDA.
(LAUGHTER)
So, thank you, Wayne. This is a small token of our appreciation.
GOODMAN: Thank you very much. I used to have a voice before I started this!
(APPLAUSE)
LAUGHREN: Now, on to the topic for today's meeting, we are going to focus on NDA
20-717, supplement 19. This is for modafinil in the treatment of attention
deficit hyperactivity disorder.
As you know, modafinil is marketed as Provigil to improve wakefulness in adults
with excessive sleepiness associated with narcolepsy, obstructive sleep apnea
syndrome and shift work sleep disorder. It is a Schedule IV drug and the
recommended dose in these disorders in adults is 200 mg.
Now, Cephalon has provided us data in support of a claim for the safety and the
short-term effectiveness of modafinil in the treatment of ADHD at a slightly
higher dose, at a dose of 340 mg per day in children less than 30 kg and 425 mg
per day in children greater than 30 kg.
This supplement was submitted in December of 2004 and, as you know, we issued an
approvable letter in October of last year.
Though we did issue an approvable letter, the letter addressed three concerns
that we wanted to have further addressed. One of those was serious skin rashes;
a second was psychiatric adverse events; and, finally, there were three patients
with transaminase elevations for which we wanted additional data.
The sponsor responded to our approvable letter, in November of last year, and
today you will hear from several FDA staff. You will hear from the primary
reviewer, Glenn Mannheim who, as you know having seen his review, has
recommended against approving this drug based on his concerns about rash and
several other adverse events.
You will also hear from Dr. Paul Andreason who will provide some additional
comments on safety. Our presentations are going to focus entirely on the safety
issues because we agree with the company on efficacy. But you will hear from the
company on efficacy and, as well, you also have our reviews.
In addition, we have obtained advice on the dermatologic problems from our own
internal consultants from Dermatology. You have their reviews, and Dr. Markham
Luke, from the Dermatology Division, is here to address any questions you might
have. In addition, we have Dr. Michael Bigby, who is the chair of the
Dermatology Advisory Committee, who will be making a presentation on serious
drug-related rashes and he will be participating in the discussion as well.
Now, I want to be clear that the Division of Psychiatry Products has not reached
a conclusion yet about this application. We have these concerns and that is
precisely why we are coming to you to ask for your advice.
After you have heard the findings and the arguments we are going to ask you to
vote on two questions. The first question is focusing on efficacy questions,
whether or not you believe that the company has demonstrated that this product
is effective in the treatment of ADHD.
Secondly, we will ask you to vote on the question of whether or not it has been
shown to be acceptably safe in the treatment of this disorder.
In addition, we are going to be asking for your comments on several other issues
related mostly to rash. First of all, if the drug were to be approved for this
indication we would like your advice on a risk management plan. We would like
your advice on labeling, particularly for rash.
Finally, we would like your advice on any postmarketing studies that you think
might be useful to further clarify this problem. I think I will stop there and
Dr. Mannheim will be presenting his findings.
Thank you.
MANNHEIM: As Dr. Laughren explained, I reviewed the initial submission for
modafinil for this indication. I will review with you today the information
specific to safety.
Here is an outline of what I will be covering. I will be reviewing a little bit
of the background and history of modafinil; an overview of the safety database;
common adverse events in Cephalon's clinical trial; other adverse events of
significance; psychiatric adverse events; and, most importantly, rashes and what
I think the potential public health impact may be.
Then I will give you some closing comments, and I will be followed by Dr.
Andreason.
In 1998 modafinil was approved as a wakefulness-promoting agent in adults with
excessive daytime sleepiness associated with narcolepsy. Additional indications
were granted by FDA in 2003 for excessive daytime sleepiness associated with
obstructive sleep apnea/hypopnea syndrome and shift work sleep disorder.
The important thing that I would like you to notice from this slide is the dose.
The recommended dosing was 200 mg once a day which, based on a 65 kg adult,
comes to about 2.67 or 2.7 mg/kg. I want you to remember those numbers since we
will come to it in other slides.
Recommendations were to give modafinil, Provigil, as a single morning dose for
narcolepsy or obstructive sleep apnea or for shift work sleep disorder one hour
prior to the start of the work shift. No additional benefit was shown for doses
more than 200 mg.
The current application is for use of modafinil in children and adolescents with
ADHD.
Two doses have been proposed by Cephalon. For children less than 65 lbs or 30
kg, they would be getting a single daily dose of 340 mg. For children or
adolescents more than 65 lbs or 30 kg, they would be getting a dose of 425 mg a
day.
Now, remember the number 2.6. For the highest dose in children, on a
milligram/kilogram basis, the children would be getting 21 mg/kg or about 8
times higher than the adult dose. For those over 65 lbs or 30 kg the highest
dose would be 5.3 times higher than the adult dose.
Cephalon is recommending that children or adolescents start the drug at initial
doses of 85 mg and slowly titrate up, based on tolerability, by incremental
steps of 85 mg to the targeted dose of 340 mg or 425 mg a day.
This shows the population which was studied in the submission. It was children
and adolescents 6-17 years of age with DSM-IV ADHD who attended a full-time
school. These were moderately to severely ill children. They had minimal
learning difficulties. As it relates to adverse events, children with
psychiatric comorbidities were excluded.
Stimulant non-responders were not allowed in the trial. Those with abnormal
laboratory or medical conditions one month prior to the start of the study were
also excluded.
There are three studies which are called the pivotal studies for this. Study 309
and 311 were 2 9-week, double-blind, flexible dose, weekly titration studies.
Study 310 was a 7-week, double-blind, fixed dose study, followed by a 2-week
randomized withdrawal to modafinil or placebo.
Children less than 65 lbs went on 340 mg a day and those over 65 lbs went on 425
mg a day.
This slide shows the total number of subjects and doses used in the Phase 3
double-blind, placebo-controlled trial. Of note, 420 subjects were treated with
modafinil and 213 subjects were treated with placebo. The important thing to
note here is the numbers 102, 256 or 358.
Children and adolescents only received the proposed labeled efficacious doses.
This slide comes from Cephalon's briefing document which was submitted for your
consideration by Cephalon. It summarizes the pediatric trials. The 420 comes
from the Phase 3 double-blind exposure. The number I want to show here is the
number 933 because this constitutes the core safety database of this
supplemental NDA.
This slide indicates that additional 303 children were exposed to modafinil in
an open-label ongoing Phase 3 trial. About 400 other children for obstructive
sleep apnea and narcolepsy are the legacy studies.
As far as the purposes of this submission, we are only considering the number
933 since we don't have an integrated safety database for the other 689 children
and they were not part of this submission.
It certainly would be reassuring if there were no adverse events in these
subjects but we really don't know at this point.
This slide is a little busy and I apologize for that. It shows exposure to
modafinil and modafinil metabolites and compares it with what one sees in
clinically used doses in adults with those proposed for children.
What I want to bring your attention to is the exposure of the modafinil sulfone
as measured by the total exposure area under the curve. In adults, with an
initial dose of 200 mg, the average area under the curve is 38 or close to 40.
Going to the highest child, receiving 425 mg, the area under the curve of the
sulfone is about 250. This is 6.5 times higher than the exposure seen in adults.
Going to the lowest dose of children receiving 340 mg, the average area under
the curve is around 630. This is 16 times higher than that seen in adults with
clinical dosing. This cannot be explained by differences in dosing on a
milligram/kilogram basis.
These are clinically used doses and with them one sees that the sulfone
metabolite is much higher compared to adults.
Now we are going to look at the adverse event data.
The incidence of common treatment-emergent adverse events in the Phase 3
double-blind, placebo-controlled trial is listed. Of note, insomnia occurred in
27 percent of subjects on modafinil and 4 percent of subjects on placebo.
Anorexia occurred in 16 percent of subjects on modafinil and 3 percent of
subjects on placebo.
Perhaps associated with that, there was weight loss in 4 percent of subjects on
modafinil and 1 percent of subjects on placebo.
Notable psychiatric adverse events include psychosis in 0.5 percent, as listed
here, and suicidal events in 6 subjects, 0.6 percent. The suicidal events
included 5 ideations; 1 attempt. None were completed. Yesterday Dr. Mosholder
reported on a pooled analysis of the ADHD trials and that suicidal behavior was
infrequent among the non-medicated ADHD placebo subjects.
Other clinically significant adverse events which were noted in this trial
consisted of gastric or duodenal ulcers in 2 subjects. One case of note was a
child who was admitted to the hospital with a moderate metabolic acidosis who
had an H. pylori infection.
There were 9 cases of syncope in the total exposure. Of note is a child who,
according to the vignette information, had a 40-minute bradycardia, hypotensive
syncopal episode and one week later an EKG was performed which showed AV
dissociation with adjunctional rhythm. There were 24 children who were quoted as
having asthma.
Of note is a subject in one of the pivotal trials, 310, who, 8 days after being
started on modafinil at a dose of 340 mg collapsed at school during gym, stopped
breathing momentarily and was given an inhaler and began breathing normally.
This was diagnosed as an acute asthma attack and the child was discontinued from
the study on day 9.
There were 3 subjects who had dehydration, and of note is a subject in the
open-label continuation trial who, on day 147 of treatment, was admitted to
hospital with severe dehydration, moderate ketoacidosis and hypoglycemia which
was found secondary to a strep. throat.
Sixteen subjects had laboratory evidence of hepatocellular injury based on
transaminases being greater than 3 times the upper limit of normal. Of note,
there were no cases of jaundice or liver failure, or no significant bilirubin
elevations.
Now I am going to talk to you about the rashes but I am not a dermatologist and
I am relying on FDA's dermatologist, Dr. Porres who did a consult, and someone
from FDA from Dermatology is here to answer some questions.
When you look at all the subjects who were exposed, rashes were present in 5
percent of all subjects compared to 4 percent that you saw in the Phase 3
double-blind, placebo-controlled trial versus 2 percent in placebo.
Only 1 subject dropped out in the double-blind, placebo- controlled Phase 3
trial, which was an 8-week, study, because of a rash.
When you look at all the studies, including the open-label safety study, 101
subjects dropped out because of an adverse event, of which 26 percent were noted
to have a rash in their vignettes although it may not have been coded as a
reason for discontinuation.
In one-half of these subjects, or 13 subjects, the rash was coded as a primary
reason for discontinuation. The rashes varied in spectrum of severity. Eight
with rash also had fever; 2 with rash had elevated liver function tests, one
with a transaminase of 17 times the upper limit of normal.
I am now going to discuss some of the serious skin rashes, primarily the
erythema multiforme, Stevens-Johnson which, from my standing as a pediatric
neurologist are usually hypersensitivity reactions to drugs. There were 2 rashes
which were thought to be erythema multiforme, Stevens-Johnson.
One subject had peeling and blistering over the entire body, with lips and
urinary tract involvement, in study 311. The drug was stopped but the rash
progressed to involve peeling, blistering, mucosal involvement over days.
In another subject in study 207 the drug was stopped but the rash progressed.
The child was hospitalized.
Other rashes of note included a child in study 207 with vesiculobullous cheeks
with severe lip blisters. In study 312 another subject had a rash where there is
no clear description but the rash was obviously severe enough that he was
treated with systemic steroids, prednisone and given Benadryl.
The rash recurred when restarted at 85 mg on day 34. There are two cases of
positive, you know, rechallenge.
Other skin reactions of note -- there were possible allergic events in about 22
of the subjects out of the total exposure of 933 subjects, at 2.4 percent. They
included hives, urticaria; facial edema; pruritus; allergic reactions; red lips;
eczema with increased LFTs.
There were some non-allergic events of alopecia, tongue blotches, Herpes zoster,
plantar warts and ringworm.
Now I would like to give some more details about the index cases here. Case
number one was a young girl with an unremarkable medical history who had
attention deficit disorder. She was started and then titrated over 2 weeks to a
target dose of either 340 mg or 425 mg a day, but it differs in 2 different
vignettes.
Two days later, on day 16, the child developed a fever of almost 102, sore
throat, mild rash which was described as red bumps.
The next day the child was seen in the emergency room. My understanding is they
thought the child had strep. throat and they gave one dose of amoxicillin which
was subsequently stopped. The next day, day 18, the modafinil was stopped. Over
the next 4 days the rash worsened and progressed.
There were multiple pruritic areas over the arms and stomach. On day 22 the rash
progressed to involve the face. On day 23 mucosal involvement was said to be
present in 2 areas. It burned when the child urinated so there was involvement
of the urethra. The child had swollen and crusty lips. At some time later -- the
exact course is uncertain from the vignettes -- there was extensive skin peeling
involving the palms and soles. No new lesions were said to be present by day 30
and the event was said to be resolved.
By day 31 or day 26 -- it differs in 2 vignettes -- the child was given 1 more
dose of modafinil by the mother for unclear reasons and the itching returned.
On day 44 the child was withdrawn from the study and the vignette indicates the
Stevens-Johnson syndrome resolved but the erythema multiforme continued.
This case involves a young child with inattentive deficit disorder who also had
Turner's syndrome and bed-wetting, who was on somatotropin for the Turner
syndrome for 7.5 years prior and desmopressin for the bed-wetting for 4 months
prior.
She was started, titrated on modafinil 200 mg a day for week 1 of the study and
then 100 mg a day for week 2 of the study. By day 4 she developed fever,
abdominal pain and diarrhea. This lasted for 9 days.
By day 14 the child was seen in the emergency room for pruritic urticaria
involving the face and chest. The drug was stopped. The child was treated with
diphenhydramine. The rash worsened by day 15. The child was then hospitalized
with a provisional diagnosis of Stevens-Johnson.
The child was seen by a dermatologist who found no evidence of mucosal
involvement but was diagnosed as a moderate morbilliform rash. The child was
treated with hydroxyzine. This rash resolved in 1 week. This case was accepted
by Cephalon as being compatible with Stevens- Johnson syndrome.
Another subject of note is a young boy who was started on modafinil at 400 mg a
day for 2.5 weeks, and on day 14 developed fever and a moderate rash on the
cheeks. The rash progressed. By day 17 there was severe blistering on the lips.
The rash was described as vesiculobullous.
On day 19 the modafinil was stopped. The time course of everything else was not
specified in the vignette and no more information is available. The child was
treated with cephalexin for the rash and Tylenol with codeine for fever and
pain.
Dr. Porres, of the Division of Dermatology at FDA, reviewed the 21 cases
identified in my initial review and the entire safety database of this
submission. He divided the cases into three categories, definite cases
representing erythema multiforme, Stevens- Johnson.
There are 2 subjects there or 0.2 percent; subjects who had a history consistent
with early prodromal erythema multiforme and Stevens-Johnson, there were 3
subjects, 0.32 percent; and then there were 7 additional subjects who had a
history suggestive of prodromal erythema multiforme, Stevens-Johnson. So, 10
more subjects plus the 2 subjects, or 12 subjects, so this is a total of 1.25
percent of subjects with definite and potential erythema multiforme,
Stevens-Johnson.
When one looks at the postmarketing experience with modafinil, there were 6
reports of serious skin reactions. All occurred in adults 18 and over. There
were 5 biopsy confirmed cases of erythema multiforme, Stevens-Johnson.
Four were hospitalized and 1 died, but this case was really confounded by other
medications and medical conditions. There was 1 dermatitis bullous.
Because of the under-reporting, the true number of cases is probably likely to
be greater. But the take-home message that I would like to say is that this
slide shows that biopsy confirmed Stevens- Johnson syndrome occurred in adults
at lower exposures than those received by children.
Erythema multiforme or Stevens-Johnson syndrome is generally thought to be
hypersensitivity reactions to drugs.
One of the cases which was really interesting involved a child who developed
urticaria, facial edema, fever and a 17-fold elevation in transaminase between
10-14 days after starting the drug. The child had a history of allergy to
sulfamethoxazole trimethoprim.
Sulfamethoxazole is a sulfonamide and is one of the drugs known to cause
Stevens-Johnson. It is structurally similar to modafinil sulfone, which raises
the question of a possible cross-sensitivity to the sulfone metabolite.
What is the potential public health impact of these findings? Two recent
estimates of the background rate for erythema multiforme, Stevens-Johnson was
1-2/million/year.
In this submission there were 2 subjects with erythema multiforme and 10 other
possible cases of a significant rash. The total range of risk is anywhere
between 0.2 percent to 1.3 percent.
A recent CDC study estimated that 2.5 million children, ages 4- 17, were on ADHD
medication. Now, if we assume that only 10 percent of these children will try
modafinil at some point, then we ask the next question, how many cases would
result.
We estimated that there would be a range between 500 and 3,000 cases which will
occur based on the 0.2 percent to the 1.3 percent incidence among the 10 percent
who are switched to modafinil.
Based on the known mortality associated with erythema multiforme,
Stevens-Johnson, we would expect from 15 to over 400 deaths to occur. We
conclude that even though a crude estimate can only be made at this time, a
potential exists for a significant number of cases to occur post-approval since
ADHD is so prevalent.
The question is can one label for this? Can we prevent this? Dr. Le Grenade and
her co-authors at FDA recently published a paper on Stevens-Johnson syndrome and
toxic epidermal necrolysis in association with selective COX-2 inhibitors.
I quote from her and I italicized certain areas: There is no satisfactory method
for determining who is at greatest risk for developing drug-associated
Stevens-Johnson syndrome and toxic epidermal necrolysis and hence of preventing
it, short of avoiding drugs altogether.
There has been a single study suggesting that early withdrawal of the agent at
the first sign of illness may improve the outcome. Although this intuitively
makes sense, this study needs to be replicated.
Even if it is proven correct, its practical application will be limited because
it is very difficult to identify the very earliest lesion in a timely manner
because of the rapidly progressive nature of this illness and the non-specific
features of its prodrome.
In the cases observed with modafinil in this submission in children no deaths
occurred.
The rash progressed after the drug was stopped and the children recovered. It
may not be so next time.
ADHD is a serious condition -- I will give you closing comments -- it is a
serious condition which is usually not considered to be associated with a fatal
outcome. Exposure to a sulfone metabolite is significantly greater, up to 16
times more in children than in adults.
This raises questions about the relevancy of the adult safety experiences to
pediatric use.
The relationship of this metabolite to rash is purely speculative but it has
structural similarities to drugs known to cause erythema multiforme and
Stevens-Johnson syndrome which can be fatal.
The incidence of erythema multiforme, Stevens-Johnson syndrome observed in these
studies is, at a minimum, hundreds of times the background.
The age ranges of the rashes appear skewed towards subjects less than 12 years,
those having a higher sulfone exposure. Doses lower than 340 mg have been shown
to limit efficacy, hence, dose reduction is not a reliable option.
Although some cases with rash got better, there were 2 positive rechallenges and
one case progressed after discontinuing the drug. One subject with rash was
hospitalized but there was disagreement about the diagnosis.
One child with a history of reactions to sulfa drugs developed a
hypersensitivity reaction with transaminase elevation 17 times the upper limit
of normal, with urticaria, fever and facial edema 10 days after starting
modafinil, which raises the hypothesis of cross- sensitivity with sulfa drugs.
Psychosis and suicidality, although not standardly significant, were more
frequent in subjects on modafinil than with placebo. Insomnia was present in 27
percent of subjects on modafinil versus 4 percent in placebo, and anorexia
occurred in 16 percent of subjects on modafinil versus 3 percent on placebo in
the double-blind, Phase 3 trials.
This review was very much a team effort of my many colleagues at FDA, some of
whom I am blessed to call my friends.
Thank you.
GOODMAN: Before you step down, could you review any cardiovascular effects,
effects on heart rate and blood pressure?
MANNHEIM: Dr. Andreason is going to do that.
ANDREASON: Good morning.
My name is Paul Andreason and I am the Acting Deputy Director of the Division of
Psychiatry Products. I would like to talk to you this morning about modafinil in
the treatment of ADHD.
Dr. Mannheim has outlined the concerns that he has about modafinil in the
treatment of ADHD, and I think what we are faced with as we look especially at
the skin rashes is what I like to call incongruity of data. I will get into that
in a little bit.
I would also like to acknowledge the Neurology Products Division where the drug
resides -- it is kind of its home since it was approved there first -- and the
safety team for helping us out with the background rates for Stevens-Johnson and
looking at the adverse event reports through the Adverse Event Reporting System
and their epidemiologic expertise.
Glenn did the primary review on the first submission. June Cai helped out with
the review of the response to the approval letter.
In the Division of Dermatology, I would like to thank Joe Porres and Markham
Luke, who is here with us today -- Markham is here with us today. Joe took
another job and he is not with the Division of Dermatology right now.
Then, in the Division of Drug Risk Evaluation, I would like to thank Andy
Mosholder and Kate Gelperin who, as part of their presentation yesterday, did an
analysis of the psychiatric adverse events that are associated with modafinil
use.
Just as a quick review of how we workup safety problems with drugs or safety
profiles of drugs, I should say, when we look at a drug we look at deaths,
serious adverse events, adverse dropouts, potentially clinically significant
labs, ECG and vital signs and then we develop information on comparative common
and drug-related adverse events, all these things from controlled trials. We
also do special searches, especially in this case with modafinil and many
psychiatric drugs -- well, all psychiatric drugs, for psychiatric adverse
events; in this case, for Stevens-Johnson syndrome and neutropenia because these
were things that kind of popped up; and then the recent interest in blood
pressure, pulse and cardiovascular adverse events.
Then with the response to the approvable letter we get a safety update. In that
safety update we focus on serious adverse events and deaths, if they occur. We
develop our profile of the common and drug- related adverse events from the
controlled trial data, as well as the comparative information on labs, ECGs and
vital signs.
Modafinil is a marketed product and we got some information from Verispan about
the exposure to modafinil at this point. These are numbers not in patient-years
but in unique patients.
At all ages at this point between the years 2002 to 2005 there were 1,087,000,
roughly 1,088,000 exposures in all ages, and for children ages 0-17 there were
roughly 36,000 exposures.
I kind of want you to keep that in mind because this is the first piece of what
I would call inconsistent data about rash. It is almost unheard of to see cases
of Stevens-Johnson syndrome in controlled trial data and here we have at least
nominally 2 cases that have been identified as such.
At that kind of a rate you would expect to see something in the adverse event
reporting data.
Dr. Mannheim said, well, based on these numbers, these would be the projected
number of cases that we would see after marketing. The piece of incongruity here
is that the drug is already marketed. We have 36,000 exposures in the age ranges
that were studied, and in the 0-12 group right around 11,000 and we have no
AERS-reported cases.
Now, one of the cases from the controlled trial data actually is a duplicate
case. It got reported in AERS but there are no spontaneous reported cases. So,
given that kind of projection, I would expect to see some cases reported in AERS
and we haven't seen that yet.
This is, again, a review of patient exposure in the controlled trial database.
In the safety update we did get some information on serious adverse events and
dropouts, as well as deaths, and Stevens- Johnson syndrome would be considered
in that group.
So, as more and more information comes in, you know, that denominator of cases
reported per amount of exposure changes, however, even with 2 cases in 1,600
that would still be a large number.
I think the problem that comes about when we look at Stevens- Johnson -- and we
will hear more from Dr. Bigby in a moment about how that ascertainment is made
-- is that in these two cases one was hospitalized and one was not.
Neither of them were in a burn unit or the ICU and we don't have biopsy
information on those kids.
These are tables that you have already seen. It reviews the numbers of patients
exposed in the three pivotal trials.
Now, this is a table that shows you the common adverse event profile. Our usual
definition of common and drug-related is adverse events that occur at least 5
percent of the time and occur at a rate that is twice placebo. In italics you
will see that anorexia and insomnia meet that criteria.
There are a couple of other adverse events that are close but don't quite make
that cutoff. This is the table actually that is proposed in labeling and is the
usual kind of table that we have in labeling.
Just as a quick overview of the safety results from the controlled trials, there
were no deaths and, of the adverse events of note, there were these 2 cases that
were identified as either Stevens- Johnson or erythema multiforme.
There were no new cases of leukopenia in the AERS system update, and we could
see no real signal for leukopenia in the controlled trial data.
As far as psychiatric events, there were 4 suicide-related adverse events, no
completed suicides. I will talk more about those in a moment. There were none in
the placebo group.
As far as mean blood pressure changes, modafinil actually showed a slight
decrease compared to placebo in mean blood pressure. However, the numbers of
patients that met the outlier criteria of systolic blood pressure of greater
than 130 and an increase in greater than 20 mmHg were 9/420 for modafinil and
1/213.
With pulse there was no difference in the mean value either, and the numbers for
outliers are 6/420 versus 2/213. The 6 versus 2 in those 2 groups is, in my
opinion, not terribly different. There was some weight loss, 0.7 kg weight loss
with modafinil versus 1.0 kg mean weight gain in the placebo group.
So, did that answer your question about blood pressure?
GOODMAN: Yes.
ANDREASON: Great! As far as psychiatric adverse events, this is drawn from one
of Andy Mosholder's slides from yesterday. These were the comparative numbers
with patient-year exposure, and these are real years.
They are not multiplied. So, with 33 patient-years exposure in placebo you have
no cases of mania or psychosis or suicide-related adverse events. But there were
5 cases of aggression, spontaneously reported aggression.
Zero cells are kind of tough to deal with when you are doing statistical
analysis, but oftentimes you can use a Fisher's exact test to get at least some
idea of whether or not something is statistically significant. I will show you
that for the suicide-related adverse events on the next slide.
You will notice that numerically the cases of aggression are slightly less with
modafinil than they are with placebo. As Dr. Mosholder stated yesterday, that
was not a significant difference but it is not, by the same token, greater. In
the open-label data it shows that the rates are lower.
That doesn't necessarily mean -- well, let me put it this way, these are
patients, once they reach open-label, who have tolerated the drug and I think
that probably the best comparison for this is the controlled trial data.
These are the results of the Fisher's exact test for suicide- related adverse
events. You see here that you have the 4 cases in the modafinil and that is
compared to no suicide-related adverse events in the 660 in placebo. So, that
ends up with a 2-tail value of p of 0.31 and 1-tailed p of 0.22.
Just to give you kind of a comparison with, say, Strattera that has received
labeling for suicide-related adverse events, with Strattera there were 6/1357
versus 0/851. Because of the increased sample size, those numbers ended up being
statistically significant. There were 5 cases of ideation and 1 attempt in the
FDA defined cases.
I would like to note that Eli Lilly has slightly different numbers because they
had a slightly different definition of the suicide-related adverse events. They
had 7 versus 1 out of 1357 and 851 respectively. That p value ended up being
0.07.
Traditionally, for safety-related topics we don't necessarily use a p of 0.05
like we do for efficacy. We use a p of 0.1. So, using a cutoff of a p of 0.1,
the 0.7 would still be statistically significant. And, Strattera has a boxed
warning.
Now, with the modafinil there are 4/664 versus 0/308. This is not statistically
significant by Fisher's exact and all were cases of ideation and 3 of the cases
actually resolved without discontinuation of the drug. The sponsor proposes
warning language in labeling as opposed to boxed language.
As far as the cases of severe rash that are identified as Stevens-Johnson
syndrome, we will hear more about that, again, from Dr. Bigby, and Dr. Markham
Luke is here today to talk about the cases individually if people have questions
on those.
The problem that we have with almost any adverse event report ascertainment,
there was no histopathology with either of these cases. With Stevens-Johnson
syndrome admission to burn units and ICUs is common.
One of the kids was hospitalized but not in an ICU or burn unit. The other child
was treated as an outpatient. You have heard about the cases. I can go back to
those if anyone has any questions. Again, there were no children in the
postmarketing Adverse Event Reporting System, other than the one case that is
the duplicate from the controlled trial.
There were 4 adults in the AERS postmarketing database, and it turned out that 3
had confirmatory histopathology and the other one was erythema multiforme
without histopathology.
There were no adults with Stevens-Johnson identified in the adult controlled
trial database.
So, what we are left with from this controlled trial database, along with the
open-label material that goes with it, is 2 serious cases, one admitted to the
hospital, neither to the ICU or burn unit; none in the placebo group; 10
dropouts due to rash versus no dropouts due to rash in the placebo group.
Spontaneous adverse events in the controlled trial, about 4 percent for
modafinil versus 1 percent for rash, for all kinds of rash.
But then, the incongruity here is that there are no other children with either
Stevens-Johnson syndrome in the postmarketing adverse event database with about
36,000 kids exposed.
Again, with that kind of exposure and the projected numbers of cases of SJS,
based on 2/933 or even 2/1,600, one would expect to see more in the Adverse
Event Reporting System.
So, just to compare and contrast labeling with Lamictal that carries a boxed
warning for Stevens-Johnson syndrome, in that boxed warning there are some
fairly hard numbers. For example, they did a prospective registry study and
there was one death due to Stevens- Johnson syndrome with Lamictal out of 1983
patients.
There was also information on rates in adults with different kinds of diagnoses,
for example, 8/1000 in children with Lennox Gasteau and 3/1000 adults. Then in
the bipolar population it was 1.3/1000 adults on adjunctive therapy for bipolar
disorder. So, those are some fairly hard numbers.
On the modafinil side, the sponsor proposes warning language and I have listed
under here the points to compare and contrast with Lamictal. There are no deaths
reported. Actually, on one of the slides that Dr. Mannheim presented, he said
there was one death.
That case was a fellow who came in to the hospital and had a subarachnoid
hemorrhage and was treated with several drugs, one of which was phenytoin, known
to be associated with Stevens-Johnson syndrome.
He developed Stevens-Johnson syndrome as part of the course of his
hospitalization and apparently was treated with modafinil prior to that
hospitalization.
So, I think that case is terribly confounded and I wouldn't count that as drug
related, or I don't think we could count that one as a good drug-related case.
So, based on my exclusion of that case, there would be no deaths so far due to
Stevens-Johnson.
The child cases were not severe enough to require burn unit or ICU. Now, again
back to this, there are at least 2 nominally identified cases out of the 933 in
the submission that were identified but there is no biopsy confirmation.
Back to the other part of the incongruity, there are 36,000 exposures already
with no cases. Then back to the other side, you have 3 confirmed cases of adult
SJS in the postmarketing but that is with 1.5 million.
So, that is getting close to the background.
Depending on how you factor in under-reporting, you know, there could be
association and increased risk for Stevens-Johnson.
So, I guess in the end the question that you need to think about is if there is
an increased risk of Stevens-Johnson syndrome associated with modafinil, what
would be an acceptable risk.
And, if modafinil were considered for approval, what kind of risk management
program would you want to implement, and how should the concern about serious
skin rashes be addressed in product labeling.
Again, you have the examples of labeling and I can go over those a little more
if you would like. And, should there be a requirement for postmarketing studies,
if approved, to better understand the skin rashes?
There was one slide, as a bit of a digression that Dr. Mannheim showed about
liver enzymes, he included GGT in a slide, along with ALT and AST as a
percentage of increased liver enzymes under the heading of hepatocellular
injury.
Usually we look at ALT, AST and bilirubin as signs of hepatocellular injury and
don't necessarily include GGT. Excluding GGT, there were 3/420 cases of
elevation of ALT and AST of greater than 3 times the upper limit of normal, for
a percentage of 0.7.
In placebo there was 1/213, for a percentage of 0.5, and I don't see that as
meaningfully different.
So, that concludes my remarks about modafinil and I would be happy to entertain
any questions.
GOODMAN: Thank you. I understand there is going to be a change of technology
before the next presentation. Is that correct? Yes? So, why don't we start doing
that but I wonder if you can stay for questions that this committee may have.
Let me start that off.
Of the 35,000 or so children who have been exposed to modafinil postmarketing,
how many of them were on the doses that are proposed to be used in ADHD? I would
suppose further that that would be mostly for Mexico where it is already
approved. ANDREASON: I am not sure. By the way, those numbers are for the United
States only.
GOODMAN: So, if they are for the United States only let me go back and rephrase
it.
How many of them would be in the dose range that is proposed for ADHD?
ANDREASON: Yes, we tried to track that down and found that it was impossible to
get that kind of information. I think the only thing you could do would be to
assume that they had received the maximum recommended dose, which was only 200.
GOODMAN: We have one of our committee members that I would like to see introduce
herself, Jean Bronstein.
BRONSTEIN: Good morning. I am Jean Bronstein. I am a nurse and consumer
representative for the committee, and I apologize for being a little late. But I
do have a question.
I am trying to understand some 300 patients, I believe, that have dropped out of
the study, and I am wondering if the rash numbers are also representative of all
patients having dropped out of the study at some point. Is that clear?
ANDREASON: The patients who dropped out due to rash are included in those
numbers, yes.
BRONSTEIN: They are? Thank you.
GOODMAN: Any other questions around the table or are we ready to proceed with
the presentation?
WANG: It is actually a follow-up to Wayne's question. In the negotiations for
these pivotal trials how were the doses chosen? Why was, you know, 300 mg, 400
mg chosen? For the wakefulness indication it is 200 with no additional benefit.
LAUGHREN: Paul, you may be able to say more about this, but my understanding is
that there was a Phase 2 study, a fixed dose study that looked at different
doses, I think running from 100-400, that basically showed effects only at the
higher doses and that was the basis for focusing on the higher doses in the
pivotal trials.
ANDREASON: I am sorry, I thought you were looking at Cephalon when you asked
that question. But, yes, that is correct. Two of the studies were flexible dose
studies in the pivotal trials and one of them was a fixed dose study.
WANG: There is no data in here to suggest something that you have raised, Dr.
Mannheim, that there is no potential benefit to trying lower doses. They don't
look to be, you know, sort of clinically efficacious, which these data don't
suggest.
MANNHEIM: My understanding from the earlier Phase 2 trials was that lower doses
didn't work and they had to get to these doses in order to show efficacy in
ADHD. Cephalon can respond to that.
GOODMAN: Yes, maybe we can hear more about that from the sponsor during their
presentation. We have Dr. Leon and then Dr. Mehta.
LEON: I would like to follow-up on the number of exposed. Is that based strictly
on the 7- or 9-week clinical trials out of which maybe about 40 percent dropped
out? Or, does that include the follow- up as well? Is there slide on person-week
exposure?
ANDREASON: Oh, as far as the number of patients that are exposed for an adequate
amount of time to count, I think what we came up with was as an estimate that
was around 600. Again, if you say 2 cases out of 600, that makes the rate of it
seem even higher. Then, it even makes it seem more implausible that we don't see
anything in postmarketing.
So, I think you are right, if Stevens-Johnson is something that shows up in the
first 2-8 weeks of treatment the numbers in the controlled trials would be right
around 600. The 900 includes patients that dropped out. It includes patients
that were in Phase 2 studies -- excuse me, I take that back.
The 933 includes patients that were in the open-label trials, so patients that
were exposed for much longer.
When we looked at postmarketing data and estimates of exposure we didn't look at
patient-year exposure because we wanted to focus on the fact that
Stevens-Johnson we probably likely to show up in the first 2-8 weeks and if we
looked at patient-year exposure the rate of background would start to drop with
extended exposure if you looked at patient years instead of unique patients.
That is why we chose to look at it that way.
GOODMAN: Dr. Mehta?
MEHTA: Is the dose of the drug relevant to the occurrence of Stevens-Johnson
syndrome? I would have thought that this is a sensitivity reaction so it doesn't
matter what came out of the drug that is used, that is, the dosage is irrelevant
for the occurrence of SJS.
ANDREASON: You will see from the presentation coming up from the company that it
didn't appear that the sulfone metabolite was increased any higher, than in
other patients that didn't have rash, in the 2 patients that were identified as
having rash. The expert is here to talk about that.
BIGBY: Can I just make a quick comment about that?
GOODMAN: Go ahead.
BIGBY: It shouldn't make any difference in terms of the incidence of the rash.
I think you are correct in that regard. The only way that I think it could
affect the disorder is in outcome in terms of at a higher dose it will take a
little bit longer to be cleared from the body so that the prognosis might be
worse if you start with a higher dose because it may take longer to be
eliminated.
GOODMAN: Dr. Malone?
MALONE: I just had a question about dosing. The stimulants are also used for
daytime sleepiness disorders. Is the dose used for ADHD a lot different than the
dose used for daytime sleepiness?
ANDREASON: Yes, it is higher.
Daytime sleepiness and obstructive sleep apnea doses are 200. Right, Glenn?
Then, for ADHD it is 300 and 425.
RAPPLEY: No, I think he is asking about comparing the other stimulants? So, are
the doses for Adderall or Ritalin higher for ADHD than they are...
ANDREASON: I am sorry, I don't have that right at the top of my head.
GOODMAN: Dr. Pfeffer?
PFEFFER: I have a question about the pharmacokinetics of this drug, with the
dose being so much higher in children, especially younger children, how is the
drug metabolized? Also, is there a way of understanding if there are children
who are slower metabolizers of this drug and, therefore, this is higher? Can we
understand that?
Is there a way of understanding also if there are certain children that might be
assessed in terms of the metabolism and understand that relative risk?
ANDREASON: I can't really answer that question. I think we have somebody who can
answer that question. Let me preface it by this though, I don't necessarily
believe that ruling out the sulfone would be necessarily a guarantee of safety.
In my opinion, I think the sulfone may be a bit of a red herring. I think with
Lamictal we have no real idea why SJS occurs and it is much more common in kids
than it is in adults. If they could come up with some kind of marker that would
show what the risk was, that would be wonderful. I don't think in this case the
sulfone reaches that kind of state.
First of all, we have to identify whether or not there is a signal. Then, if one
came to the conclusion that there was a signal, I still don't think that the
sulfone would give us any assurance of safety regardless at this point.
GOODMAN: Dr. Temple and then I want to go to Dr. Bigby's presentation.
TEMPLE: I just wanted to observe that on the dose relatedness matter it is sort
of unusual to have almost an order of magnitude difference between what one
group gets and what the other group gets. So, a lot of our experience with drugs
will be looking at, you know, one- or two-fold differences and things like that.
I am not sure one really could say that a marked difference in blood levels or
exposure might not be related to rate. It could.
ANDREASON: Ron Cavanaugh was the human biopharmacologist on this.
GOODMAN: But then definitely Dr. Bigby.
CAVANAUGH: Thank you. I agree with Dr. Andreason that at this point for the
sulfone we really don't know any relationship for certain. It is purely at this
point a plausible hypothesis.
It is very structurally similar to the one drug which causes the highest
incidence of Stevens-Johnson, blethamide, which is slightly different than many
of the other sulfonamides in that it has a third oxygen in addition to the
nitrogen and the sulfone.
Modafinil also has that third oxygen in the same position. We do not know.
Basically, the only reason we looked at the sulfone was because of the dramatic
higher amounts, as well as when Glenn asked me about the sulfone I immediately
thought Stevens-Johnson and immediately thought sulfonamide. So, at this point
we don't know.
In terms of the kinetics, from what I have seen, the metabolism does not seem to
be particularly well defined. So, I really do not know at this point, you know,
anything in terms of could specific metabolic pathways result in higher sulfone
concentrations in some kids versus others.
The concentrations that I see, and it is very poor, do not lead me to believe
that the sulfone concentrations in these particular children -- and there was
only one child who had any measurement of the sulfone who had any of the
Stevens-Johnson or other severe dermatologic reactions, and that sample was
taken several days after the drug was discontinued.
If I back calculate, it basically seems that for that one child the
concentration was in the approximate range. In terms of dose response, which was
raised, we really have too few numbers here. You are also dealing with, you
know, population numbers and you are dealing with 0.1 percent difference, 0.2
percent differences. There is no way you can be certain.
In terms of a dose related to hapten and degree of what is the likelihood of
Stevens-Johnson or a hypersensitivity of any sort, I am not an immunologist; I
do not know. One of the reasons we focused on AUC is because that gives you an
idea of total exposure.
When someone has already developed hypersensitivity and they have already had a
history with a sulfonamide, they can get Stevens-Johnson with the very first
dose of a drop, and there have been deaths in cases like that.
Really we are more talking about the development of hypersensitivity, and what
you are developing as it being a hapten, my understanding is that it is the
combination of, you know, developing hypersensitivity to the combination of the
drug bound to certain proteins, or other things in the body.
So, with the higher exposure you are going to get more of this binding and,
therefore, more antigenic exposure. The numbers are so small, we don't know.
Also, with longer duration you would expect more stimulation.
I would really refer you to an immunologist. I really don't know, but the whole
issue of dose response and everything else in terms of developing
hypersensitivity, to me, is not clear.
GOODMAN: Thank you. Thank you for being patient, Dr. Bigby. We are running
behind schedule but the way I hope we may be able to make up some time is that I
am going to cut lunch and I don't think we have that many public speakers.
But I am determined to end at least at our scheduled time. During the sponsor
presentations I would ask the committee members to restrict their questions to
ones of clarification.
BIGBY: Good morning.
I am always impressed when I come down to sort of work in FDA committee meetings
about the seriousness of what goes on here, and also the dedication that people
have to trying to make rational decisions, and I hope my comments are helpful in
your deliberations.
What I was going to talk about is serious adverse cutaneous reactions to drugs,
and in order to do so I am going to cover three things. One is how to identify a
drug eruption as a drug eruption and pin it down to a specific drug.
We will look specifically at common eruptions, the serious eruptions, and I will
end by showing you some things that are commonly mistaken for drug eruptions.
This is sort of a gold standard for determining that a rash is due to a drug.
First you have to be sure that the rash you are looking at is a morphology that
can be caused by drugs.
You have to exclude alternative causes. You have to examine the relationship
between the exposure to the development of a rash in terms of the time interval;
note the response to drug withdrawal, i.e., the rash will go away.
For many drugs there is information known about their proclivity to produce
rashes, so what the frequency of rash is for a particular drugs.
Then, in those rare cases where you actually do have a re- exposure, to
determine what happens on re-exposure so you can be positive that it is a drug
rash and looks like an eruption that is a classic eruption for drugs. You have
excluded alternative causes; the interval from exposure to the development of a
rash is correct in terms of what is known about that drug and that eruption.
It goes away. Often I think the mistake people make about the response to
withdrawal is that you expect it to go away very quickly when you withdraw the
drug. For most eruptions that is not the case and the rash will actually take
much, much longer than most people think to go away after you withdraw the drug.
Then, oddly enough, re-exposure doesn't always produce the rash but when it
does, then you can be absolutely sure that you are looking at a definite cause.
Where some of these things are missing, are judged to be probable or unlikely or
not due to the drug at all.
Very quickly, we are going to look at these three common drug eruptions:
exanthem which is the most common, urticaria and fixed- drug eruption. This is a
patient with a widespread exanthematous drug eruption. It usually starts within
the first 3 days after exposure to the drug.
For some drugs like antibiotics and allopurinol that exposure window can be up
to about 2 weeks.
The rash is best described as small, erythematous papules that may coalesce.
These patients have pruritus but they are not generally ill. Mucous membrane
involvement is rare. It is a benign condition in that as the drug is withdrawn
the patient gets better.
They can often later in the course of the disease desquamate but they don't
develop blisters and they don't have epidermal detachment. There is very good
data about this type of reaction. It has been studied in several prospectively
collected data sets.
One was the Boston Collaborative Drug Program. There is data on I think
something like 35,000 exposures over about, you know, a 10- year period,
collected in many hospitals.
You can say with fair certainty that there are certain drugs that have higher
rates than others, and in this list the highest tends to be antibiotics. The
highest rates are for amoxicillin and co- trimoxazole.
It is also helpful to know that there is a large list of drugs that are almost
never associated with reactions. So, if a patient is on multiple drugs, which
they often are, it is useful to refer to this type of list to exclude the ones
that are least likely to be the culprit.
Urticaria you all know how to recognize.
It is areas of swelling. There are usually plaque type lesions, and the key
about urticaria is any individual lesion generally will last for less than 24
hours. Here is one of the perfect examples.
If you identify the cause and you withdraw it patients will often have urticaria
after such an exposure for weeks and even months even though you have identified
the correct drug and withdrawn it.
The list of drugs that cause urticaria is very similar to the ones that produce
exanthem.
Lastly, this is a fixed-drug eruption. A fixed-drug eruption is a really
peculiar thing in that it tends to occur only on certain areas and to recur in
those areas on re-exposure. It is the one instance where people will often be
re-exposed because it is not so clear to the providers that this was, in fact, a
drug eruption.
The other reason that this is quite relevant is that the histopathology of a
fixed-drug eruption is very similar to what you see in erythema multiforme and,
to a lesser degree, in Stevens-Johnson syndrome and toxic epidermal necrolysis.
Again, if you look at the drugs that cause fixed-drug eruptions, there is a lot
of overlap between the drugs that most commonly cause all of these types of
eruptions.
The three serious drug reactions that I want to talk about are the ones that I
think are the most relevant to this question that you are asking today, and that
is toxic epidermal necrolysis, Stevens- Johnson syndrome and the drug
hypersensitivity syndrome.
Of all of the things which I have to say today, this is the slide that I want
you to remember the most. These are two patients that I saw personally. These
are people with toxic epidermal necrolysis. The most obvious and important thing
about these patients is, number one, that they are sick. They often have
multiple mucous membranes involved.
In severe cases not only are the sort of distal mucous membranes involved, but
it can affect the trachea and even the bronchi.
The second most important thing is that they have widespread areas of cutaneous
involvement and, in the case on the right, they often shed full-thickness
necrotic skin over very large areas, and they have basically the equivalent of a
widespread burn.
The summary of toxic epidermal necrolysis in terms of its clinical features is
also a prodrome of fever and malaise. This usually lasts one to two days. The
eruption is predominantly on the face and torso.
The lesions are best described as pruritic plaques. They can have bullae.
Multiple mucosa are commonly involved. Patients with toxic epidermal necrolysis,
however, do not have true target lesions.
Probably by the best definition of toxic epidermal necrolysis, it has to involve
at least 30 percent of the body surface area, and the mortality for such
described toxic epidermal necrolysis is quite high, around 30 percent.
The majority of deaths are due to either infection or problems with respiratory
distress that are either due to pneumonia or to the fact that the airway linings
are involved. As has already been mentioned, it is a relatively rare phenomenon
so that in most population studies the incidence is about one case per million
patient years; 95 percent of the cases clearly have a drug etiology, and there
are certain drugs for which the incidence is much higher.
Based on a case-controlled study that was published in the New England Journal
years ago, this was a study that carefully ascertained cases in France, Germany
and Italy and to drug exposure histories from patients in three age and gender
matched controls, and came up with an estimate of the number of cases per
million exposures that one would see per week.
It was highest for sulfonamides. If you do the arithmetic, this turns out to be
something in the order of 1 case in 200.00 or 250,000 for some of these drugs.
The drugs commonly associated with TEN are listed here. Again, these lists are
very similar to the ones that cause benign eruptions and the same sort of drugs
keep showing up: sulfonamides, hydantoins, some but not all of the nonsteroidals
and allopurinol.
This is a patient with Stevens-Johnson syndrome, Stevens-Johnson syndrome and
toxic epidermal necrolysis are dissimilar disorders in a continuum. The
difference between Stevens-Johnson and TEN is one of degree of epidermal
detachment.
The symptoms are very similar. There is prodrome often of fever and malaise. The
lesions are very similar. In Stevens-Johnson syndrome the area of involvement is
usually defined as being less than 10 percent. It has a much lower mortality.
The other interesting thing is that if you look at the etiology of
Stevens-Johnson syndrome, it can be attributed to drugs in only about 50 percent
of cases. Now, that seems to be in congress with TEN and SJS being part of a
spectrum.
I think the problem is that there is a lot of confusion about mixing up cases of
erythema multiforme, which I think is a quite separable disease, with
Stevens-Johnson syndrome. I think that explains why drug etiology is less
commonly identified. I will have more to say about erythema multiforme at the
very end.
Again, the incidence is about one per million per year, drug induced in about 50
percent.
There is a higher incidence with some drugs and it is that same list of drugs,
you should note.
Now, what I was saying about the relationship between SJS and TEN, TEN is
defined as those cases where the area of involvement is more than 30 percent.
SJS is less than 10 percent.
Then, there are people who are kind of in the middle, between 10- 30 percent,
that are called SJS/TEN overlap. The other thing to note is that erythema
multiforme is not mentioned anywhere on this slide or in my previous comments
because, as I said, I think it is a distinct disorder.
The last serious reaction that I wanted to talk to you about is the
hypersensitivity syndrome.
That is what this slide is an example of. It looks very similar to exanthem
except for two things.
When you have seen a few of these patients it always strikes you that the color
in the hypersensitivity syndrome is a much brighter and darker red and the
amount of confluence of the rash is much higher.
Symptomatically, these people have exanthem. They have fever, lymphadenopathy,
often have hepatitis, some of them have arthritis. This is a disorder that has a
significant mortality.
It is not clear how patients should be treated and, again, the list of drugs
that cause this that are already known and sort of identified as such is very
similar to the list of drugs that cause drug rashes in general.
This is a slide from a paper that was done by Roujeau and Stern, in the New
England Journal, and it is a very busy slide.
The only thing I want you to note is that the fatality rate for the
hypersensitivity syndrome is about 10 percent. For TEN it is about 30 percent.
For Stevens-Johnson syndrome, because of the area of involvement and severity it
is much less; it is lower.
Finally, exposure to rash for TEN and SJS is in the order of weeks, so 1-3 weeks
is noted in the third column in this slide. Skin biopsies are very helpful
because in TEN and SJS they tend to show full-thickness epidermal necrosis,
detachment of the skin at the dermal/epidermal junction, and often there is
very, very little inflammation in the dermis associated with the rash.
Finally, I would like to conclude by showing you examples of things that are
often called drug eruptions but are not, primarily erythema multiforme. Now,
erythema multiforme -- you can't make that diagnosis unless patients have
typical target lesions.
Typical target lesions have three rings, either a dusky or bullous center, an
area of erythema around that and then a surrounding area of edemous skin.
You can often actually have rings beyond that but if you have the three rings it
is I think easily identifiable as erythema multiforme.
In terms of the distribution, another thing that is helpful is that erythema
multiforme predominantly affects the face and the extremities.
The torso is much less commonly and much less extensively involved. The majority
of cases of erythema multiforme are actually associated with infection, herpes
simplex being the most common one and, although it can be caused by drugs, drugs
are a much, much less common etiologic factor for erythema multiforme. The other
thing is that erythema multiforme, by and large, is a benign disorder.
Patients recover and deaths are extremely rare for erythema multiforme. I think
people shouldn't combine erythema multiforme, even erythema multiforme major
with mucosal involvement with Stevens- Johnson because I think they are distinct
entities.
Grover's disease is another one that looks to the world like a drug eruption. It
tends to occur commonly in hospitalized males on their back and, you know, a lot
of the times we get called for drug eruptions and it turns out to be just this
scenario, elderly men with Grover's disease predominantly on their back.
Lastly, extensive cases of pityriasis rosea can be mistaken for drug eruptions.
The key there is that, you know, the history is usually pretty classic. The
distribution is classic as well and if you have the herald patches, as noted in
the right-hand slide, there is not a lot of confusion.
The last two things on this list, the viral exanthem and graft versus host
disease, no one can really distinguish those from drug exanthems or several
other drug eruptions and it is a matter of great difficulty.
That is where I will stop. Thank you.
GOODMAN: Thank you. Questions from the committee?
Dr. Pine?
PINE: I guess I am struggling a little bit, kind of like Dr. Andreason was. On
the one hand, you know, the rashes were very concerning that were described. On
the other hand, there are no cases in the spontaneous reporting.
I was just wondering, given your background as somebody who sees this kind of
thing every day presumably, or frequently, what was your impression when you
reviewed the cases in terms of how convincing they were, number one and, number
two, when you combine that with what you would expect to see how concerned, as a
dermatologist who spends a lot of time thinking about this, were you about the
data that you saw and the cases that you saw?
BIGBY: I think that the 7 year-old child that was described, to me, was a
probable case of SJS that was drug related. After looking at the material, I
think that the drug is going to be, and probably already is, associated with
sort of an excess of cases of SJS/TEN.
PINE: Thanks.
GOODMAN: Dr. Rappley?
RAPPLEY: I looked over 26 cases, I think it was, that had rash and I noted that
many of those cases presented on a continuum that included fever, pharyngitis,
rash, and it went from very mild to very severe. That is something in pediatrics
that we see as a reaction with immunosuppression or reaction that, you know,
reminds of Kawasaki's -- not exactly but it makes me think of that. It reminds
me of drug reactions.
It reminds me of neutropenia. So, my question is do you see that as a continuum,
those symptoms as related?
BIGBY: I am actually not sure I understand your question. I mean, of the
material that I saw, I think that there was one case that probably had SJS. I
think that the other sort of rashes described...
RAPPLEY: So, you don't see that as a continuum?
(UNKNOWN): No...
RAPPLEY: You see Stevens-Johnson as a very discrete...
BIGBY: Yes, right. You know, I think that eruptions are sort of specific things
to dermatologists and these things don't sort of fit together as a gestalt for a
kind of reaction to that drug, no.
RAPPLEY: OK.
GOODMAN: What I would like to do is take an unscheduled quick break, seven
minutes.
Before we do that, just an admonishment, I would like to remind the committee
that, in the spirit of the Federal Advisory Committee Act and Sunshine
Amendment, discussions about today's topic should take place in the forum of
this meeting only and not during lunch breaks or in private sessions.
We ask that the press honor the obligations of the committee as well. If you
will allow the committee members to exit the room first to take their break, we
will reconvene in seven minutes.
Thank you.
(RECESS)
GOODMAN: We are resuming now with a series of presentations from the sponsors.
Please, committee members, restrict any burning questions to those of
clarification. I think that we will go to lunch at 12:30 instead of 12:00, which
means that we save time for more detailed questions of the sponsor after the
public presentations.
Please go ahead.
RACZKOWSKI: Good morning.
Dr. Goodman, members of the advisory committee, Dr. Laughren, FDA
representatives, ladies and gentlemen, today we will be discussing the
application for Sparlon tablets for approval for treatment in pediatric patients
with ADHD.
My name is Victor Raczkowski and I am the vice president for worldwide
regulatory affairs at Cephalon.
Our proposed indication for Sparlon is for the treatment of ADHD in children as
well as adolescent patients. We filed our application in December of 2004 and we
received an approvable letter about 10 months later. We submitted a complete
response then to the agency in November of last year.
Sparlon contains the active ingredient modafinil which is also contained in
Provigil tablets. So, modafinil is not a new chemical entity. Sparlon tablets
have been formulated to facilitate administration to pediatric patients.
That is, on a milligram/kilogram basis of modafinil they are smaller than
Provigil tablets. They come in dosage that ranges in strength from 85-425 mg and
are intended for once daily administration in the morning.
Provigil has been marketed in the United States since 1999 and is currently
marketed in 28 countries worldwide. Provigil is a wakefulness promoting product
and it is approved in the United States in adults with excessive sleepiness
associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome or shift
work sleep disorder.
We have estimated exposure globally through the end of February 2006 as being
approximately 780,000 patient-treatment years, of which 30,000 patient-treatment
years are in pediatric patients. Modafinil is also listed in Schedule IV of the
Controlled Substances Act.
You have been asked to address a number of questions today and the two voting
questions are on the efficacy and safety of Sparlon. We hope to be able to show
you with our data today that not only is Sparlon effective for the treatment of
ADHD, but it has also been shown to be acceptably safe for the treatment of ADHD
in pediatric patients.
We have also been asked to address the dermatological safety of Sparlon tablets.
Just by way of orientation, this slide represents cases of SJS in pediatric
patients in clinical trials as well as in our postmarketing experience.
Other speakers are going to go into this in much more detail. This is just to
orient you that an earlier review by our experts indicted that there was one
case of probable SJS in our clinical trial program out of 1622 patients exposed.
However, that case is of uncertain etiology. In addition, if the committee has
questions or interest in the clinical course of that patient, we do have the
investigator here at the meeting today who can describe the clinical course of
that patient.
In our pediatric postmarketing experience we have seen no pediatric cases of SJS
in over 30,000 pediatric patient-treatment years.
We will have a number of presentations today, beginning with an overview of
attention deficit hyperactivity disorder by Dr. Joseph Biederman. That will be
followed by a review of both the clinical pharmacology and efficacy by Dr.
Lesley Russell.
Dr. Srdjan Stankovic will then provide an overview of the safety and then Dr.
Russell will conclude with an overall benefit-risk assessment.
We have a number of consultant experts in the field with us today representing
various disciplines including psychiatry/ADHD, dermatology, addiction medicine,
cardiology, child development as well as epidemiology.
I would just like to highlight one name since dermatology is a major issue in
today's presentation, we do have an individual, Dr. Neil Shear, with us today
who has published extensively in peer reviewed journals on SJS as well as other
dermatological disorders.
I would also like to note, as you can see on this slide, that we have a number
of investigators with us today.
With that, I would now like to introduce Dr. Joseph Biederman, who is professor
of psychiatry at Harvard Medical School.
Dr. Biederman?
BIEDERMAN: It is a pleasure to be here. I would like to offer you a very brief
overview of ADHD as a very serious illness of genetic etiology affecting the
brain that has a bad prognosis. I strongly believe that without understanding
the assessment of benefit-risk alternative treatment is impossible.
First of all, I think that it is important to note that ADHD is a highly
heterogeneous illness like all psychiatric illnesses. We know that genes are
important, as I am going to show you in moment -- perhaps the most important
risk factor.
We know quite a bit about heterogeneous neuroanatomy and neurochemistry. We know
that CNS insults, if affecting key regions of the brain like the prefrontal
cortex, can produce very similar problems as those produced by genes. Even
environmental factors can be important in ADHD.
We need to consider that environmental factors are not bad mothers or bad
teachers, like frequently thought, but include things like poverty, exposure to
parental psychopathology, et cetera, et cetera, things that in themselves can be
driven by genes. So, heterogeneous illness requires different treatment.
Different patients require different alternative therapeutic options.
Another thing that has been highlighted today but I would like to stress again
is that ADHD is a worldwide condition, not only an American invention. It
affects children in the 5-10 percent range worldwide. Data are coming from Asia
now, from China and Japan and data from South American, Western and Eastern
Europe and, of course, North and South American point to the fact that no matter
what criteria you want to use, it is an extraordinarily common disease.
You have to remember that at least 50 percent -- at least 50 percent of the
children of today are going to be adults tomorrow and we now know that ADHD
affects at least 4 percent or 5 percent of adults in this country, not only that
it affects them but it is very morbid and dysfunctional.
I would like to stress that the yardstick of considering the severity of an
illness just by mortality may not be an adequate yardstick. Many conditions are
devastating to our patients, even though they are not necessarily lethal in the
traditional sense, like malignancies.
This is a condition that profoundly affects the lives of those affected and
everybody around them.
Many of the MRI studies that have been conducted have been small and many of the
children participating in them have been medicated, creating the suspicion that
perhaps what we see in MRI studies may reflect the toxic effects of medications.
Therefore, this study that I briefly want to review for you is extraordinarily
important. This study is large. It was published in a very prestigious medical
journal, JAMA. It was done by colleagues at the National Institute of Mental
Health. The lead author is Dr. Castellanos.
And, 152 children and adolescents of both genders and a similar number of
controls of both genders were assessed longitudinally. The specific objective of
the study was to assess the issue of medication status, whether medication is
important in brain abnormalities.
What this study found is that the brain of children and adolescents with ADHD
was significantly smaller, in the 3 percent range, independently of medication
status. These volumetric abnormalities were persistent over time so this is not
a neurodegenerative disease. It is early disease that persists into adult life.
There were no gender differences and there was some evidence of an association
between severity of ADHD and brain findings. The visual of this study shows the
brains -- these are males up to the age of 20; females out to age 15.
You can see that both genders have significantly smaller brains and the lines
are flat over time.
The conclusion of this study is that either genetic or early environmental
influences on brain development are operant in ADHD. These are fixed,
nonprogressive and unrelated to stimulant treatment.
If you look at key regions of the brain that are involved in attention and
executive function, anyone of us in this room irrespective of having or not
having ADHD, we have this area of the brain -- this is the cingulate gyrus; this
is the dorsal anterior cingulate associated with executive control; dorsolateral
prefrontal cortex associated with selective attention; and the right frontal
lobe associated with alerting.
These are interconnected areas, key regions for cognition and attention. Their
disruption will cause symptoms of ADHD.
This is a recent study that we just submitted for publication from our program
at the Mass. General. This is a three-dimensional reconstruction of the anterior
cingulate. What you see here is a study of adults with ADHD. The anterior
cingulate area is 13 percent smaller in individuals with ADHD compared with
controls.
With imaging studies you can do not only volume, as I just showed you with the
three-dimensional reconstruction so you can measure volume of this region --
this is the cingulate gyrus again -- but you can also measure the thickness of
the cortex, how thick or thin is the cortex in critical brain regions.
So, this is another study that we have done in our program of cortical
thickness. This has not yet been published but I promise you it will be
published. What you see, first of all, in red here is a statistical comparison
between the brains of ADHD individuals compared with controls.
What this depicts, in orange and yellow, is significant differences in cortical
thinness.
These areas are selectively thinner in these regions. So, you don't see thinness
across the entire brain; you see thinness in critical cortical regions involved
with executive control and attention. This is the dorsal anterior cingulate.
This region hovers between the cognitive and emotional division of the anterior
cingulate -- very important issues for clinical understanding of the symptoms of
this condition. This is, of course, the dorsolateral prefrontal cortex that is
clearly involved in cognition and in the symptoms that subserve this illness.
We have also done this analysis. It is very exciting. This is diffusion tensor
imaging that measures white tracts. What you see here is that we are documenting
disruptions in the perigenual area of the anterior cingulate and dorsal anterior
cingulate selectively.
So, this area of the brain that is involved in cognition, executive functions
and regulatory controls is smaller in volume, is thinner in cortical thickness
and has other abnormalities as well.
I am not aware of many other psychiatric illnesses can claim such conversion of
information, focusing on the same brain regions that could certainly account for
the clinical picture.
If you look at functional MRI in the same region, if you look at the coronal
view of the brain, if you put people without ADHD on the scanner you can very
nicely activate anterior cingulate doing a very mild cognitive task.
If you put adults with ADHD, they fail to activate the same region and, instead,
they activate insular so these adults can do the task but they are not using the
part of the brain that is specifically wired to do the task at hand. We have
very exciting new data that you can correct this malfunction with medications.
These findings on neuroimaging are extraordinarily congruent with
conceptualization from neuropsychology. As you know, ADHD is considered a
neuropsychological disease. What is called directed attention, the circuit that
allows people to pay attention to things that they are not interested in is
disrupted.
Inhibitory deficits, the person fails to inhibit when destructions occur; and
executive dysfunction issues of planning and organization, working memory, et
cetera, et cetera are disturbed. These are the regions that are in this part of
the brain where we are documenting abnormalities.
Another circuit that is involved in ADHD is called fascination reward circuit.
People with ADHD have difficulties with delayed gratification; difficulties with
regulating mood.
This kind of hot temper that characterizes people with ADHD and some of the road
rages that lead to accidents, and so on and so forth, may be accounted for by
these neuropsychological deficits.
Another key aspect to document that ADHD is a neurobiological disorder is
genetic research.
ADHD clearly runs in families. There is a 5- to 7-fold increased risk of ADHD in
first-degree relatives of children with ADHD. Of course, that is not evidence
for genetics so we need to have additional information to make a genetic
hypothesis or genetic claim.
Twin studies are very important because twins come from two varieties,
monozygotic and dizygotic twins. For genetic illnesses, you expect that
monozygotic twins will have a higher level of concordance than dizygotic or
fraternal twins.
Twin studies are also very important because they can allow us to compute
coefficients of heritability that I will tell you about in a moment.
Adoption studies are important because with genetic illness you expect to have a
higher rate of the disease in biological rather than adopting relatives.
Finally, molecular genetic studies will look at specific genes that may be
associated with this condition.
Coefficients of heritability are based on twin studies. I would like to point
out to you that there are a lot of twin studies in ADHD.
Coefficients of heritability range from zero/zero percent of the variance
accounted for by genes to 100/100 percent of the variance accounted for by
genes. The congruence of the genetic studies for the coefficient of heritability
in ADHD is remarkable. Even though the studies use different methods, parent
support, teacher support, structured interviews questionnaires, look how
consistent this is. On average, coefficients of heritability are close to 80
percent, in other words, 80 percent of the variance of ADHD can be accounted for
by genes.
For example, height, a very genetic trait, is about 90 percent genetic;
schizophrenia and bipolar illness, very genetic.
Recognized genetic illnesses are equally genetic as ADHD, 80 percent. Panic
disorder and major depression are genetic as well, about 50 percent, 0.5 for
coefficient of variability; other medical conditions like asthma or breast
cancer at 0.3, 0.4 coefficients of heritability. So, we are dealing with a very
genetic brain disorder here.
Specific genes have been associated with ADHD. The first genes that were looked
at in ADHD are genes that are associated with the dopamine system, candidate
genes because the drugs that we usually use to treat this condition are
dopaminergic drugs.
Mutation in a dopamine transporter gene, what is called DAT1 or DAT10; mutation
in the dopamine receptor of D4 and D5 genes -- these are cortically distributed
receptors.
There is also an association between a very rare thyroid disease on chromosome
3. People that have this mutation also have ADHD, but this probably accounts for
very little of ADHD out there.
So, the genes that have bee associated with ADHD in a consistent fashion are the
dopamine transporter genes that bring back dopamine to the presynaptic neuron.
This gene over-expresses the dopamine transporter, make more it active or more
transported, too much dopamine to the presynaptic neuron. Cortically distributed
genes are the D4 and D5. There is also a gene, SNAP25, that is involved in the
presynaptic encapsulation of dopamine.
Well, I see this slide is totally degenerated. I am very sorry. But what I would
like to say is that Dr. Faraone published in Biological Psychiatry a review of a
meta-analysis.
There are certain genes, about seven genes that consistently have been
associated with ADHD, several genes in the serotonergic system, DBH, dopamine
transporter gene and also dopamine receptor DR D4 and DR D5.
These genes have been found in multiple studies in meta-analyses of these
specific genes to be associated with ADHD. You probably have these details in
the handout, as well as the reference for the paper that support these claims.
The treatments that we have available are clearly effective. This study was not
done by industry. It was funded by the NIMH on the multi-modal treatment of
ADHD. This study studied close to 600 children 7-9 years of age in this country,
in 5 sites.
This was a study in which children were randomized to very aggressive medication
management, very aggressive, comprehensive behavioral treatment, a behavioral
treatment that was so comprehensive that you could not possibly improve on it,
and it is so expensive that it is not doable.
But that was the purpose of the study. Children received both medication and
behavioral management and community-based treatment.
What this study found, and I would like to point this out to you, is that these
two arms, the very aggressive medication arm and combination treatment were
superior to just behavioral treatment and community based treatment that
consisted largely of communication too.
This group, here, is a group that received the best treatment that we can offer,
very aggressive pharmacotherapy and very aggressive behavioral treatment.
And, even using the best we can, the response is 60 percent, leaving 40 percent
of our patients inadequately treated with intolerable side effects or with
difficulty tolerating this treatment.
Stimulants are Schedule II drugs. About 40 percent or perhaps more do not
tolerate or to not respond to these treatments.
The side effect profile of sleep, appetite, difficulties with mood and anxiety
can seriously hinder our ability to treat all the patients that otherwise could
benefit, and concerns about growth suppression and tic development continue to
plague stimulant treatment in ADHD, although the data is generally reassuring,
people continue to be concerned about these issues.
ADHD not only affects school and school performance, it is clearly a life
disease.
For example, ADHD has been shown to be associated with a significantly increased
risk for automobile accidents, and automobile accidents, as you know, are the
leading cause of death in our young.
So, patients not only have poor grades in school or may not reach college but
may not reach adult life altogether or may kill somebody in the process of
driving and not paying attention to the road.
So, if you look at the morbidity of ADHD as a serious -- perhaps not a lethal
illness but a very devastating illness to the individual, the family and society
secondary to under-achievement, under- employment, marital difficulties, drugs
and substance abuse, legal difficulties, or morbidity, we are dealing with an
extraordinarily morbid disease that can profoundly affect those afflicted with
this condition.
So, in summary, ADHD is a neurobehavioral disorder with complex etiology. It is
a disorder that affects the brain; has a strong genetic component, as I alluded
to; affects millions of people worldwide, both sexes. It is highly persistent in
the majority of those affected. It has a negative impact on the life of the
individual affected and everybody around.
Although the stimulants are clearly an effective treatment for ADHD, a sizeable
number, in the order of magnitude of 40 percent, are non-responsive or not
tolerating this treatment, calling for alternative treatment for this condition.
Thank you very much for your attention.
The next presentation will be by Dr. Lesley Russell who will be talking about
clinical pharmacology and efficacy.
RUSSELL: Thank you, Dr. Biederman.
Today I would like to briefly overview the clinical pharmacokinetics of
modafinil in children, and then summarize for you the efficacy findings of our
program in ADHD.
Just to begin with, here is an outline of the development program that Cephalon
undertook in children and adolescents with ADHD. The three Phase 3 studies,
studies 309, 310 and 311, formed the basis of the efficacy and safety that will
be discussed today.
In addition, we had two pharmacokinetic studies, studies 113 and study 206, that
outline the pharmacokinetic parameters of modafinil in children. In addition, we
conducted two studies, 207 and 213, to help us define the dose required for the
Phase 3 studies.
All patients in the Phase 3 studies and some from the Phase 2 studies were
allowed to enroll into study 312 which is an ongoing open-label extension
program.
Following submission of the sNDA, we initiated a further study, study 3044, in
which 303 patients were enrolled. This study is still ongoing.
I would now like to briefly summarize the pharmacokinetics of modafinil in
children.
As shown on this slide, the pharmacokinetics and exposure are dose-proportional
over the dose range studied. The absorption is rapid, with a maximum
concentration observed 2-3 hours after administration. When administered with
food, there is an approximate 1 hour delay in the time to Cmax although the
overall absorption is not affected.
The volume of distribution increases in children linearly with their weight. The
metabolism of modafinil is primarily hepatic, with less than 10 percent excreted
unchanged in the urine. There are 2 primary metabolites, modafinil acid and
modafinil sulfone.
As you heard earlier, we did observe higher levels of modafinil sulfone in the
younger children. The elimination of modafinil is time- and age-dependent. We
observe a decrease in clearance over time with steady state being reached by
about week 6 of treatment. There is a gradual decrease in clearance with age,
with a pronounced shift between 9-11 years of age.
So, we see that there is a half-life in the younger children of approximately 7
hours which is compared to a half-life of 15 hours in the adults.
I would now like to outline for you the basis of the dose selection that we used
in the Phase 3 studies. Study 207 was a relatively small, double-blind,
randomized, 4-period crossover study, and this was the first program undertaken
to assess the efficacy of modafinil in the treatment of ADHD.
The results shown for you are the total scores on the ADHD rating scale as
assessed by the parent. With the caveats of this being a small study, you can
see that those patients who received 100 mg barely discriminated from placebo.
A slightly larger treatment effect was seen with the 200 mg dose group and a
larger treatment effect was seen with the 300 mg or 400 mg dose group.
And, I should reiterate here that the 300/400 mg doses were administered based
on weight, with the 300 given to children less than 30 kg and the 400 to those
children weighing at least 30 kg or more.
The next study we undertook was study 213, and this was designed to see the best
way of administering a single dose of 300 mg either as a single dose
administered first thing in the morning, which is depicted in blue, or as a
split dose of 200 mg in the morning and 100 mg at lunch, depicted in orange, 100
mg in the morning and 200 mg at lunch time, depicted in pink and compared to
placebo.
As you can see from the slide, there appeared to be little benefit to splitting
the dose and the largest response we saw was in the 300 mg dose group
administered as a single dose.
As you can see on the right-hand side of the slide, this is for all patients,
but when we looked at it stratified by weight you can see that it is clearly the
younger and lighter children that had the larger response.
So, from this study we concluded that older and heavier children may require a
higher dose. This slide identifies the systemic exposure that we saw following
these dosing regimens.
In the middle, here, are those children weighing less than 30 kg who received
300 mg. Here are those children weighing more than 30 kg who received. You can
see that the systemic exposure associated with the lighter children is clearly
higher than the systemic exposure with the heavier children.
Using these data and the clinical efficacy results from the Phase 2 studies, we
developed a pharmacokinetic/pharmacodynamic model and estimated that the
systemic exposure which would be associated with a consistent pharmacodynamic
effect would be in the order of 150 mcg/hour/ml, and that the doses that would
be required to achieve this exposure at steady state would be 340 mg for those
children weighing less than 30 kg and 425 mg for those children weighing 30 kg
or more.
Following the Phase 3 program which included sampling from population
pharmacokinetics, we went back to test this hypothesis.
As you can see from this slide, we pretty much got it right in that here are the
children weighing less than 30 kg who received 340 mg and here are those heavier
children who received 425 mg, and the systemic exposure in those groups is
pretty similar, around 150 mcg/hour/ml.
As you will see from the next slides, these doses were associated with
substantial efficacy.
Here are the designs of the 3 pivotal studies that were undertaken. All studies
were double-blind, randomized, placebo- controlled and had a 2:1 randomization.
Study 309 and 311 were identical in design. Both were 9 weeks in duration and
employed a flexible dose titration regimen whereby children could be titrated
from a minimum dose of 170 mg to a maximum dose of 425 mg based on perceived
efficacy and their tolerability to treatment. The dosing increments occurred on
a weekly basis at 85 mg.
Study 310 was slightly different. This study had a 7-week efficacy period and a
2-week period that assessed abrupt discontinuation of the drug, the results of
which I will not show you today.
This study was also a fixed dose study and patients were titrated at 85 mg
increments every 2 days to their target dose based on weight, so 340 mg for the
children weighing less than 30 kg and 425 mg for those children weighing 30 kg
or more.
The patients enrolled in the study were very similar. All patients were 6-17
years of age with a diagnosis or ADHD according to the Diagnostic and
Statistical Manual of Mental Disorders.
The children were required to be at least moderately ill on the Clinical Global
Impression of severity and have an ADHD rating scale which was at least 1.5
standard deviations above the norm for age and gender. Patients were required to
be of normal intelligence with no learning disability and attend school full
time.
Patients were excluded from study if they failed to respond to 2 or more
adequate courses of stimulant therapy, although it should be noted that patients
who had failed one stimulant therapy were allowed to be enrolled.
Patients were also excluded if they had psychiatric comorbidities requiring
current pharmacotherapy and were well controlled with their current ADHD therapy
and had no good reason to change treatments.
The efficacy assessments were identical for each of the 3 studies. The primary
outcome measure was the change from baseline in the Total Score ADHD Rating
Scale as assessed by the teacher.
Secondary outcome measures included a change from baseline in the Home ADHD
Rating Scale as assessed by the parents in the evening between 6:00 and 8:00 at
night; the Clinical Global Impression of change as assessed by the treating
physician; the Conners' Parent Rating Scale as assessed by the parent; the test
of Variables of Attention, which is a continuous performance test; the Social
Skill Rating Scale and the Child Health Questionnaire.
As you can see, the average age of patients entering into the program was around
10, with the majority of patients being less than 12 years of age. The majority
were boys and white, and about two- thirds of the patients actually weighed 30
kg or more.
As per inclusion criteria, patients were required to be at least moderately ill
on the Clinical Global Impression of severity and, as you can see from the
slide, about 50 percent of the patients were considered to be moderately ill and
the other 50 percent were considered to be markedly or severely ill.
Around two-thirds of the patients had the combined inattentive and hyperactive
subtype of ADHD. About a third were predominantly inattentive and very few were
purely hyperactive.
The baseline ADHD rating scale at entry was on average 37, which is well above
the norm for a 10-year boy which is roughly 18.
A total of 638 patients were randomized into the study and 630 received
treatment, 420 in the modafinil treatment group and 213 in the placebo treatment
group.
Around two-thirds of the patients completed the double-blind treatment period,
with the reasons for discontinuation outlined here.
As you can see, some of the main reasons for discontinuation were lack of
efficacy with a much higher proportion in the placebo treatment group, and
adverse events with the higher proportion in the modafinil treatment group. The
other reasons are listed for you here.
The following three slides will show the outcomes of the primary efficacy
variables for each individual study. Here are the results for study 309, the
first of the flexible dose studies.
Just to orient you, on the Y axis is the Total ADHD Rating Scale with the lowest
score showing benefit, and across the X axis is the duration of the treatment
period in weeks.
Just as a reminder, the primary outcome variable was the change from baseline to
endpoint using the last observation carried forward analysis. As you can see
from this slide, there was a statistically significant difference in favor of
those patients being treated with modafinil.
More specifically, the treatment effect on the modafinil treatment group was
17.5 points with the treatment effect on the placebo group of 9.7 points for an
effect estimate, which is the difference between the 2 treatment groups using
the Lee squared means of 7.4.
In addition, statistically significant results were seen using the observed
cases analysis.
A similar result was seen in study 311 which is the second flexible dose study.
At endpoint the treatment effect on the modafinil treatment group was 15 points
and a treatment effect on the placebo group was 7.3 points for an effect
estimate of 8. Again, this is statistically significant both at endpoint and
using the observed case analysis.
The last study is study 310 and, again, a very consistent treatment effect was
seen in this study, with a treatment effect of minus 17.2 points on the
modafinil group versus 8.2 points on the placebo treatment group for an effect
estimate of 9.
Outlined for you on this slide is just another way of viewing the data. On the
left-hand side of the screen is the modafinil treatment group at baseline and at
endpoint. On the right-hand screen is the placebo group at baseline and at
endpoint.
This slide illustrates the remarkably consistent effect seen not only in the
modafinil treatment group but in the placebo treatment group.
The red line depicts what would be considered to be a normative value on the
ADHD rating scale for a 10 year-old boy. As you can see, those patients treated
with modafinil are beginning to approach this normative value.
We also assessed the effect of treatment using a responder analysis on the
School ADHD Rating Scale with those patients who had at least a 30 percent
reduction in their scores from baseline to endpoint or a 50 percent reduction
from baseline to endpoint.
As you can see, in all 3 studies a significantly higher proportion of patients
treated with modafinil had either a 30 percent or a 50 percent reduction in
their ADHD symptoms.
This slide shows for you in all 3 studies the home version of the ADHD Rating
Scale. As a reminder, this was assessed by the parents in the early evening.
The results seen here very much mirror the results we saw using the school
version of the ADHD Rating Scale, with significant differences seen both at
endpoint and in the observed case analyses in all 3 studies in favor of the
modafinil treatment group.
Depicted here is the responder analysis on the Clinical Global Impression of
improvement.
Outlined for you are those patients who were either considered to be much or
very much improved by the treating physician. Again, in all 3 studies we see a
very consistent treatment effect, with a significantly higher proportion of
patients considered to be much or very much improved on this scale by the
treating physician. Another commonly used scale for assessing ADHD and their
response to medication is the Conners' Parent Rating Scale. Again, you can see
in each of the 3 studies, using this scale, a very similar effect to the
observation seen using the ADHD rating scale, with improvements on the modafinil
treatment group in cognitive problems and in attention, hyperactivity and their
total ADHD index.
This scale also allows the assessment of treatment on the oppositional behavior.
As you can see, in all 3 studies there appears to be a treatment effect in favor
of modafinil, although this is only statistically significant in study 311.
The one inconsistent effect that we saw was using the Test of Variable
Attention. Outlined for you in this study is the pooled analysis using data from
all 3 studies.
Although you can see that those patients treated with modafinil tend to do
better than those patients treated with placebo, it should be noted that this is
actually a decline in performance rather than an improvement in performance over
time.
Children with ADHD often have poor peer to peer relationships and difficulties
with socialization. We wanted to assess the effects of treatment on these
parameters and we used the Social Skills Rating Scale. Again, this is the data
from all 3 studies pooled. The individual studies did show a consistent
treatment effect.
As you can see, there appears to be an improvement in many of these parameters
when treated with modafinil, including the Social Skills Total Scale.
A similar improvement was seen in other problem behaviors as measured by this
scale. It should be noted that these results were only seen in the children in
grades kindergarten to 6th grade and we observed no major differences between
treatment groups in the older age groups.
Lastly, here are the results of the Child Health Questionnaire, a global sort of
quality of life instrument that assesses many behaviors that can be impaired
with ADHD. Again, this is the pooled analysis of all 3 studies.
As you can see from this slide, there appears to be an improvement in many of
the behavioral aspects seen for those patients treated with modafinil --
including an improvement in the total psychosocial summary. We did not see
significant improvements in the physical functioning domain, although it should
be noted that these values were normal at baseline.
We have undertaken many subgroup analyses, many of which are outlined in your
briefing document. Here I just want to show for you the subgroup analysis for
those patients who were either stimulant naive at study entry, and that was for
about 50 percent of the patients, and those patients who had received a prior
stimulant before enrolling into the study, which was again about 50 percent of
the patients. Here you can see that treatment with modafinil was effective even
in those patients who had had prior stimulant therapy, although it should be
noted that the treatment effect appears to be larger in those who were stimulant
naive.
In conclusion, we saw consistent efficacy results across 3 pivotal studies. The
improvement in ADHD symptoms was seen by the teachers, the parents and the
treating physicians. Improvements were seen at school, at home and across the
day.
As well as improvement in the core ADHD symptoms, we did observe improvement in
other psychosocial domains. Finally, we saw efficacy in stimulant naive patients
and in patients who had had prior stimulant experience.
I would now like to hand over to Dr. Srdjan Stankovic who will outline safety
for you.
STANKOVIC: Thank you. My name is Serge Stankovic and I am with the Cephalon
clinical research group.
My presentation this morning on modafinil safety is organized as follows: I will
review overall modafinil exposure in clinical trials.
Following that, I will review the safety data for the modafinil ADHD program in
children and adolescents, and this will include review of general safety and
events of special interest such as skin reactions and psychiatric events.
In the balance of my presentation I will briefly summarize high level safety
information from our development program in excessive sleepiness in pediatric
patients. Finally, I will review modafinil information coming from our
postmarketing safety surveillance.
Overall, safety data for 933 patients with ADHD were included in the
supplemental NDA, submitted in December of 2004. Of these, in the 3 Phase 3
placebo-controlled trials, 420 patients were treated with modafinil and 213
patients were treated with placebo.
Please note these numbers as I will often refer back to them when I am
presenting data from our controlled trials.
Following the sNDA submission, one additional open-label study in children with
ADHD was initiated.
With that, as of February, 2006, a total number of pediatric ADHD patients
exposed to modafinil was 1236. Additional pediatric exposure comes from our
development program in excessive sleepiness, 270 pediatric patients, and from
pediatric patients exposed to a variety of foreign studies for various
indications, 116 patients.
Finally, just a reminder that 4000 adult patients were exposed to modafinil in
the development program for excessive sleepiness and in other clinical trials.
Looking at patient exposure in the pediatric ADHD program, this slide presents
exposure by modal dose and duration for 933 patients as of February 1, 2006. A
total of 246 patients were treated with modafinil for a minimum of 12 months,
and as many as 164 were on drug for 18 months or longer.
About half of the patients received modafinil at the modal dose of 425 mg a day,
while about one-third at the modal dose of 340 mg a day. The total exposure to
modafinil in the pediatric ADHD program is 575 patient-years.
Next I will discuss adverse events observed in ADHD studies of children and
adolescents. A general overview of adverse events reported in 3 Phase 3
placebo-controlled studies is presented on this table.
While the majority of patients in both groups experienced at least one adverse
event, a higher incidence was observed in the modafinil treatment group.
Relatively few of these events were reported to be severe, were reported to be a
reason for study discontinuation or were reported to be a serious regulatory
definition of that word.
The most commonly observed adverse events in the Phase 3 placebo- controlled
studies were insomnia, headache and anorexia. The COSTART term of anorexia used
here includes both loss of appetite and decreased appetite.
In fact, about 70 percent of patients reporting anorexia experienced decreased
appetite. Insomnia and anorexia were reported at a substantively higher rate in
the modafinil group compared to placebo. Review of these two events indicated
that very few were reported as severe, specifically 9 out of 115 events for
insomnia and 1 event for anorexia.
Likewise, only 5 events in insomnia led to discontinuation, while 2 patients
reporting anorexia discontinued study due to that adverse event. In most
instances, these 2 events first occurred in the initial 2 weeks of treatment and
the median duration reported was about 2 weeks.
Out of 933 patients included in the sNDA, 18 patients experienced at least one
serious adverse event by the time of the 10-month safety update submitted in
November of 2005.
Four of these patients were enrolled in the 3 placebo-controlled Phase 3 studies
and all of them were in the modafinil treatment group.
From the 2 ongoing pediatric studies in ADHD, 3 patients experienced a serious
adverse event during the period up to February, 2006. Discussion of serious skin
adverse events as well as psychiatric events in more detail with be part of the
discussion of special safety.
In the next four slides I will review relevant information related to laboratory
evaluations from the pediatric ADHD studies. Data for selective hematology and
blood chemistry parameters will be reviewed in more detail.
Although included in your background package, data for other laboratory
parameters did not raise questions or concerns and, therefore, will not be
presented here today.
Based on some early observations from the Phase 2 studies, concern was raised
regarding modafinil treatment effects on absolute neutrophil count and white
blood cell count in children.
Our Phase 3 controlled data did not show a meaningful difference in mean change
from baseline or incidence in clinically significant values between modafinil
and placebo.
Furthermore, as presented on this slide, when the lowest on treatment values are
grouped by range there was no meaningful difference between modafinil and
placebo treatment groups.
With respect to serum chemistry, as in adults, we did observe a difference in
mean change from baseline between modafinil and placebo for alkaline phosphatase
and GGT.
In the Phase 3 placebo-controlled studies there were few patients experiencing a
clinically significant change on any of the parameters, with no apparent
imbalance between treatment groups.
On the next slide we will discuss LFT elevations highlighted in the background
document as cases of possible concern.
These cases are included in this table in the column for all modafinil studies.
In the FDA approvable letter it was stated that although controlled trials data
did not reveal a signal for drug-related mean increase in transaminase values or
in drug-related outliers, there were 3 modafinil-treated patients who had
transaminase increases of concern, but insufficient other information to further
assess the significance of these changes. Details related to these 3 patients
are presented on the slide.
In all 3 cases, total bilirubin values both at the time of observation of
abnormal LFT values and throughout the study were normal. In one case laboratory
abnormalities returned to normal while patients continued treatment with
modafinil.
In the second case treatment was continued for an additional 6 months prior to
study discontinuation. At that time, all abnormal LFT values returned to normal
except for a mild elevation in ALT.
In the third patient abnormal values returned to normal after withdrawal of
modafinil. This case will be discussed later in relation to possible
hypersensitivity reactions.
The next segment of the safety presentation is focused on cardiovascular safety.
I will review blood pressure and pulse data, ECG information including QTc
interval and cardiovascular adverse events from the Phase 3 placebo-controlled
trials. It should be noted that the vital signs measurements in ECGs were
recorded in these studies at variable time points during the day and in relation
to the intake of study medication.
With respect to blood pressure, no notable effects in sitting blood pressure
were observed in the Phase 3 controlled studies. Presented on this slide are box
plots for systolic blood pressure on the left side of the screen and diastolic
blood pressure on the right side of the screen in modafinil and placebo
treatment arms respectively.
Changes from baseline for both systolic and diastolic blood pressure were
similar in the 2 treatment groups with respect to both mean values, overall
distribution and extreme outliers.
This graph presents the distribution of observed change from baseline in sitting
pulse for the 2 treatment groups. As presented, we observed similar distribution
between the 2 treatment arms and the occurrence of outliers.
Review of the ECG tracings from the ADHD pediatric studies did not reveal
specific concerns both with respect to morphology or interval measures.
This slide presents an overview of QTc interval data from the 3
placebo-controlled trials expressed as maximum change from baseline or as
maximum duration observed.
The slide presents data for QTc using the Fridericia correction, but the
findings are similar when other corrections are used. Either way, there is no
apparent effect on QTc interval or imbalance between treatment arms.
Finally, when reported adverse events are reviewed, we observe relatively few
cardiovascular events. Only a small fraction of these, 2 patients on modafinil
and 1 on placebo, reported events leading to treatment discontinuation.
In all 3 cases the stated reason for discontinuation was tachycardia. None of
the reported cardiovascular events were reported to be serious.
Important consideration in the safety evaluation of any ADHD compound is
assessment of its effects on growth. In the placebo- controlled Phase 3 studies
modafinil treatment of up to 9 weeks duration led to relative weight loss
compared to weight gain observed in the placebo group.
Similarly, a significantly higher proportion of modafinil-treated patients
experienced clinically significant weight loss, defined as at least 7 percent in
weight reduction. To be precise, 9 percent of modafinil-treated patients versus
1 percent of placebo-treated patients experienced significant weight loss during
the study.
Naturally, we did look at the longer term treatment data related to weight and
growth in general. As you know, for accurate evaluation of growth effect in
children, we need to evaluate them relative to norms. To achieve this, we
expressed changes in weight and height using Z-scores.
Just a quick reminder, Z-score is a statistical measure that quantifies the
distance measured in standard deviations of a patient data point, in this case
individual weight or height, from the population mean, in this case CDC growth
norm for corresponding age and gender.
This graph presents mean weight and height Z-scores over 12 months of treatment
with modafinil. A decline in Z-score is observed initially in the first 3 months
of treatment consistent with the reported weight loss in our short-term trials.
In the following months the line remains horizontal, meaning that the normative
pattern of growth is regained. Using the same presentation, it is apparent that
there was no indication of adverse effects on height over the 12 months of
treatment with modafinil.
In the course of the modafinil ADHD pediatric development cases of serious skin
reactions were reported. Some of these were indicative of a possible
Stevens-Johnson syndrome or hypersensitivity reaction, generally a rare but very
serious complication of treatment. Cephalon shares the important concerns raised
by our colleagues at FDA in regard to these events.
Therefore, I will review skin events in greater detail.
To bring everybody on the same page with respect to cases of interest, I will
start with the list of events, included in the FDA briefing document, in the
second dermatology consult report dated February 27, 2006.
In this report the events were grouped in 3 categories based on the level of
diagnostic confidence. The 3 groups are events representing EM, SJS or TEN;
events somewhat suggestive but lacking confirmation; and events resembling
prodromal presentation but without sufficient information for diagnosis.
Cephalon has performed a similar review and in the next two slides I will review
cases from the first two groups. With respect to the third group, our review did
not support the conclusion that any of these cases should be classified as SJS
or prodrome.
We based this on the low specificity and low predictive value of reported
symptoms.
Additionally, many of the symptoms are quite common and many were not reported
concomitantly or concurrently.
First, we will review the clinical trial cases. Patient number 1 is a 7 year-old
boy who, on day 16 of treatment with a 340 mg dose, presented with symptoms
described by the investigator as erythema multiforme, Stevens-Johnson syndrome
and both FDA and Cephalon reviewers agreed that the diagnosis of Stevens-Johnson
syndrome is likely accurate, with less consensus on the possible etiology.
I am sure that this case will be discussed in more details later and, as Dr.
Raczkowski said, we have the investigator here who was treating the patient, as
well as members of our panel of dermatologists who can talk more about the case.
Patient number 2 is an 11 year-old girl reported with morbilliform rash on day
15 with treatment of a 200 mg dose of modafinil. This patient was hospitalized
and the SJS diagnosis was excluded. FDA review indicated that this was a case
representative of EM/SJS.
Cephalon's panel of independent reviewers, on the other hand, was unanimous that
the reported diagnosis of morbilliform rash is probably correct and the event
did not represent Stevens-Johnson syndrome.
Patient number 3 is a 6 year-old boy who reported rash, fever and vomiting 2
weeks after initiation of treatment. Review of the source documentation received
from the investigator indicated that this event was diagnosed as fifth disease.
Patient number 4 is an event in an 8 year-old boy described as rash on the
cheeks and blisters on the lips, and was reported as erythema multiforme. The
event occurred on day 23 of treatment with a 300 mg dose of modafinil. This case
is considered by the FDA reviewer as somewhat suggestive but not representative
of EM/SJS or TEN.
Cephalon's reviewers, on the other hand, agreed that this is unlikely erythema
multiforme, but did not agree on the alternative diagnosis. One considers this
event to be possible SJS. A second reviewer considered it to be probable
herpetic gingivostomatis and a third independent reviewer attributed to the
event as either viral etiology or SJS.
Patient number 5 is a 9 year-old boy with reported symptoms of urticaria, fever
and facial edema. This patient also had elevated transaminases. Cephalon's
review indicates that this is a possible case of hypersensitivity reaction and
it is not consistent with SJS.
In the review of postmarketing reports both FDA and Cephalon concluded that
there were 4 reports of serious skin reactions, 1 SJS/EM and 3 SJS reports.
Of the 12 suggestive but not confirmed cases on the FDA list, Cephalon has
identified 8 reports considered suggestive of possible hypersensitivity but not
indicative of EM, SJS or TEN spectrum. The other 4 cases were also not
considered suggestive of SJS.
In the Phase 3 placebo-controlled trials the incidence of rashes coded by the
COSTART coding system was 4 percent in the modafinil treatment group and 2
percent in placebo.
As we all know, the preferred term "rash" in the COSTART coding system does not
include many terms that could be considered non- urticarial rash. Therefore,
Cephalon undertook an additional analysis to ascertain the incidence of
non-urticarial rash. In collaboration with 2 external dermatology experts, we
defined a category of non-urticarial rash which included all adverse events
indicative of rash, excluding urticaria and related reactions.
Using this definition, cases of non-urticarial rash in the pediatric ADHD
studies, as well as in the pediatric studies for excessive sleepiness and in all
adult studies with modafinil were identified and frequency tables were
constructed.
Additionally, all reported adverse events of urticaria, hypersensitivity
reactions and all allergic reasons in the pediatric ADHD studies were reviewed
for possible underlying causality and prior medical history.
Based on the described methodology, we calculated the incidence of
non-urticarial rash across treatment groups in controlled pediatric ADHD trials
and in all pediatric patients. This table presents the incidence in the
placebo-controlled trials.
We also present the incidence of those described as severe and those leading to
treatment withdrawal. The overall incidence of rash was higher in the modafinil
treatment groups, with few being described as severe or leading to treatment
discontinuation.
In the ongoing open-label study in ADHD initiated after the supplemental NDA
submission a total of 303 additional newly exposed patients entered the study,
with 188 receiving modafinil for at least 4 weeks.
Presented on this slide is the observed incidence of non- urticarial rash in
that study. As in the previous slide, we also present the incidence of events
described as severe or those leading to discontinuation.
As seen on this slide, the reported incidence is somewhat lower compared to the
modafinil group in the controlled studies. One patient reported a severe rash on
day 10 and discontinued the study on day 13 due to this rash which was described
by the investigator as rash.
The overall incidence of non-urticarial rash reported in the controlled
pediatric studies for excessive sleepiness was similar between modafinil
treatment groups and placebo. These are much smaller studies Additionally, the
observed incidence was lower compared to ADHD pediatric studies.
Only one event was reported as severe for events described by the investigator
as fifth disease. No events led to discontinuation or were serious by regulatory
definition.
The observed imbalance in incidence of non-urticarial rash in the controlled
ADHD pediatric studies prompted further evaluation for possible association with
treatment. We approached this in 3 ways.
We evaluated the relationship between rash and dose; relationship between rash
and modafinil plasma exposure; and, finally, we evaluated the relationship
between rash and modafinil sulfone exposure, one of the metabolites known to be
present in higher concentrations in children.
With respect to relationship of non-urticarial rash and dose, we conducted a
case-control analysis where patients with rash were matched with controls based
on the study protocol, time in the study to event and weight. Based on this
analysis, we did not find statistical evidence for association between rash and
modafinil dose.
A second analysis looked at the modafinil plasma exposure by comparing area
under the curve between patients reporting non- urticarial rash, in the far left
box on the slide, controls, in the middle box, and overall patient population in
Phase 3 studies, in the far right box.
Areas under the curve were calculated based on sparse sampling data from the
Phase 3 trials and PK modeling. As presented on this slide, no difference was
apparent between the 3 groups.
An assessment of the relationship between non-urticarial rash and exposure to
modafinil sulfone was also conducted. Here we graphically depict the
distribution of modafinil sulfone concentrations in patients developing rash --
small red boxes at the bottom, and in patients not developing rash -- blue
boxes.
On the Y axis the number of patients is depicted and different modafinil sulfone
concentration ranges are depicted on the X axis.
We observed that the distribution of sulfone concentrations in patients with
rash appears to closely mimic the distribution of sulfone concentrations in the
full population of treated patients in placebo-controlled studies.
We conclude, therefore, that there appears to be no correlation between
non-urticarial rashes and systemic exposure to modafinil sulfone. One additional
piece of information is that 2 cases in question had modafinil sulfone
concentration of less than 6 mcg/ml.
We have also examined the adverse events database from the controlled ADHD
pediatric studies for COSTART preferred terms indicative of urticaria,
hypersensitivity reactions or allergies.
This slide presents a tabular summary of the reviewed preferred terms and
associated medical history reported prior to treatment initiation.
One can easily see from the table that the vast majority of these events was
reported in patients with prior history of seasonal allergies or asthma.
Psychiatric adverse events related to ADHD treatment have enjoyed special
interest in the recent months, culminating in some important discussions as
recently as yesterday.
In response to the request from the Division issued to all ADHD drug
manufacturers, Cephalon has performed a full analysis of psychiatric events from
all pediatric studies and from our pharmacovigilance database as per
prespecified methodology.
In addition, we have reviewed serious adverse events occurring after the last
safety update cutoff in October, 2005, covering the period through February 1,
2006. The results will be presented in the next several slides.
GOODMAN: Excuse me just a moment, I want to ask a question of clarification on
the previous metabolite levels that you showed. What was the relationship
between the timing of obtaining the sulfone metabolite level and the dosing?
Obviously, there can be a lot of noise contributed by relationship between time
of assay and dose.
STANKOVIC: We obtained the values for concentrations of modafinil sulfone
closest to the event for those patients that reported a rash.
GOODMAN: But it might not have been the same relationship to the time the dose
was actually taken. Right?
STANKOVIC: That is right, yes. That is correct.
A brief introduction on methodology of the psychiatric evaluation, all adverse
events reported in the ADHD and excessive sleepiness pediatric programs were
subject to a review by a string search for COSTART preferred terms of
investigator verbatim terms indicative of psychiatric events.
Once identified, all events are classified in the following groups, psychotic
events including mania, suicidal ideation and behavior, aggressive and violent
behavior and miscellaneous psychiatric events that were serious by regulatory
definition.
A similar string search approach was employed in the review of our
psychovigilance reports. Event terms and narratives from the ongoing pediatric
studies for serious adverse events were reviewed in order to identify
psychiatric events as well.
We present here psychiatric adverse events from the ADHD pediatric program. Just
a quick note, this table includes both events that occurred during treatment as
well as those that occurred 48 hours following last dose of modafinil. As I will
be discussing these cases, we put them together.
This is somewhat different than the methodology applied in the tabulations
presented yesterday.
In the controlled studies all psychotic events, as well as all events of
suicidal ideation or behavior were reported in modafinil treatment groups.
Reports of aggression or violent behavior were relatively balanced between
treatment groups, with a slight higher proportion of these events occurring in
placebo. Additionally, no serious miscellaneous events were reported in either
group. When the smaller pediatric program in excessive sleepiness was examined,
no psychotic or suicidal events were found. Obviously, even few events or a
psychotic or suicidal nature are a great concern so we will review them in more
detail.
A total of 5 patients reported psychotic symptoms while on modafinil treatment,
all within 48 hours post last dose. Three of these events were relatively short
in duration and why patients continued modafinil in one case or following
withdrawal of the drug in two cases.
One additional case, described as psychotic disorder aggravated, was also
relatively short in duration but did require hospitalization and led to
withdrawal from study.
This case, also in the narrative, we learned reported as suicidal verbalization
but it is included in this table in the psychotic disorders. The fifth case was
an interesting case of reported ideas of reference that apparently did not
require any specific treatment -- yes, sir?
GOODMAN: We have a question.
PINE: I want to understand both of these cases because the last two cases don't
really make sense to me and I am wondering if you could go into them in a little
detail, really the last case more than the second to the last one.
When it says psychotic disorder aggravated, that implies to me that there was
either a pre-existing psychotic disorder or some other factor that was
contributing and it sounds concerning that the child was hospitalized. So, that
is one question.
The second question is that this is a case of ideas of referential control
which, again, sounds somewhat concerning and the event lasted ten months, which
is also somewhat concerning if those are really ideas of referential control,
but the action taken was to continue with modafinil.
So, that doesn't make any sense to me. I wondered if you could explain those
situations.
STANKOVIC: Yes, I can talk a bit about those cases additionally. The psychotic
disorder aggravated is an 8 year-old boy with ADHD.
He presented with severe psychosis beginning on day 19 of the open-label study.
He was hospitalized and at the time of hospitalization we learned that there was
a prior history of a psychotic disorder that was not reported at the time of the
entry to the study.
The second case is a very interesting case to us as well. Unfortunately, we do
not have quite a clarification of continuing modafinil treatment in ten months
of continued ideas of reference. We don't have any additional details. It is
interesting and somewhat confusing but that is what happened. The investigator
continued treatment for an additional 10 months.
PINE: Just to make a comment about that, I mean, not only does that raise
questions about this case but it raises questions about the nature of the data
in general because it just wouldn't make sense that somebody would see something
like this, and idea of reference, that would be ongoing for ten months but not
feel the need to take any treatment.
Anyway, I guess it speaks for itself.
STANKOVIC: We have here a similar presentation for the 5 patients reporting
adverse events classified as suicidal ideation or behavior.
The first 3 patients experienced brief episodes of suicidal ideation, described
as suicidal statement. In 1 patient this happened on 2 occasions.
None of these events required either treatment for the event or study drug
discontinuation. One patient verbalized a suicidal threat which was resolved
after study drug was discontinued.
One case, however, is a case of aggressive behavior reported initially as normal
behavior.
The case narrative described suicidal behavior in a 6 year-old girl with a
psychiatric history and possible family history. The event occurred 2 days
following the last dose of study medication and required hospitalization and
prolonged treatment.
Between the last safety update in November, 2005 and February, 2006 4 serious
adverse events indicative of suicidality of psychotic symptoms were reported in
the ongoing pediatric studies. These include both ADHD studies and ongoing
pediatric studies in excessive sleepiness.
Three patients reported events that were classified as suicidal events, ideation
or gesture. In 2 of these cases no treatment intervention was required and the
patients continued in the study. Treatment was withdrawn for 1 patient.
One additional patient reported paranoid reaction following 16 days of
treatment. The event lasted 5 days and the study drug was withdrawn.
In the request from the Division for analysis of psychiatric adverse events, we
have been asked to review postmarketing reports received during the period
January, 2000 to June, 2005.
We estimate that for this particular period the total pediatric exposure
approximates 24,700 patient-treatment years. A total of 7 psychiatric reports
were received during this period. These are the events reported. The events were
reported in a wide ranges of ages, as you can see, from 6 to 17 years, and
across both genders.
Four events involved psychotic symptoms. One event was reported as a suicide
attempt. However, in this case modafinil was not taken prior to the event but
was only taken as a part of the cocktail of drugs used in the multi-drug
overdose.
The 2 remaining cases are events of aggressive symptoms and violent behavior.
You may wonder at this time how does the safety profile of modafinil observed in
pediatric ADHD studies compare to other programs in children.
We have one additional program, smaller, completed as a part of the pediatric
retail request in narcolepsy and obstructive sleep apnea for excessive
sleepiness. I will review here the general safety profile observed during the
pediatric development program in this indication.
Overall, a similar safety profile was observed in the small patient population;
a similar AE profile, effects in vital signs or laboratory parameters were
observed. Notably, no adverse effects on weight were observed during the
short-term trials in this patient population.
Lower incidence of non-urticarial rash was observed compared to ADHD studies,
and no events led to discontinuation or were serious in nature.
One serious adverse event from the pediatric studies in excessive sleepiness
requires discussion as it was mentioned as a point of concern in the FDA
clinical review as a possible case of Reye's syndrome.
The clinical picture in a 6 year-old boy was that of a non- specific viral
syndrome -- nausea, vomiting, pharyngitis, followed 3-4 days later by a change
in mental status characterized by somnolence, delirium, hallucinations and
seizures.
The patient had elevated serum ammonia but not transaminases.
The case was reviewed at Cephalon's request by two external consultants, one
pediatric neurologist and one pediatrician. The consensus opinion was that the
most likely diagnosis was viral encephalitis or inborn error of metabolism.
Urea cycle disorder was mentioned. Reye's syndrome was considered unlikely
because of normal LFTs.
According to the FDA briefing package, the FDA consultant also concluded that
this case is not drug related.
Some of the postmarketing information has been reviewed earlier as part of the
discussion on skin and psychiatric reactions. Here we will review the profile of
the reported events through our pharmacovigilance system from the perspective of
different system organ classes.
First, review of estimated postmarketing exposure, we estimate that as of
February, 2006 total postmarketing exposure to modafinil was 780,000
patient-treatment years. This includes worldwide exposure for the period since
drug approval in the first country in 1999.
As it appears, based on the prescription data market research that we have, 4
percent of these exposures included individuals less than 18 years of age so we
estimate that the overall pediatric exposure is about 30,000 patient-years.
Based on some information that we have available, the estimated median duration
of treatment with Provigil in the market is approximately 3 months.
So, using those numbers, one can estimate exposure to modafinil to be higher
than a million, up to 3 million adults and in excess of 100,000 children.
Presented on this graph are comparative profiles of postmarketing adverse drug
reactions reported for adult patients, in blue rectangles, and pediatric
patients, in orange.
The total number of reported adverse drug reactions in a particular system organ
class is presented on the Y axis while different system organ classes are
presented on the X axis. We had a total of 105 adverse drug reaction reports for
all pediatric patients.
As you can see, although it is a little hard on this slide, the two profiles
appear largely similar across different organ systems. It should be noted,
however, that the we do not have reliable information on how the two populations
relate with respect to underlying indications for which the drug is prescribed
or doses used.
Based on the postmarketing reports, the Provigil label is continuously reviewed
and updated as deemed necessary. This slide is a reminder of 3 label changes
initiated by Cephalon within the past 3 years.
As you can see, some of the safety events observed in the pediatric ADHD program
are fairly consistent with the postmarketing experience that resulted in label
changes.
I have reviewed a considerable amount of safety information and will try in the
next two slides to briefly summarize the main points. We believe that it is fair
to say that modafinil is generally well tolerated at doses studied.
Not unusual for ADHD medication, the most frequently reported adverse events
were insomnia, headache and anorexia. These events were seldom severe and few
led to treatment discontinuation. Likewise, few significant laboratory
abnormalities were observed. No effects on mean systolic blood pressure,
diastolic blood pressure, pulse or QTc interval were observed in the controlled
trials.
Beyond initial weight loss, there were no consistent adverse effects on growth
observed over 12-month treatment with modafinil. We did observe events of
suicidal ideation and psychotic events in the ADHD pediatric patients treated
with modafinil.
These events were short in duration in general and did not require additional
treatment in many cases.
We believe that there is one case of probable Stevens-Johnson syndrome reported
in the pediatric clinical program so far at this point, at an exposure of 1622
patients. This case resolved without any adverse sequelae.
As I mentioned, I am sure that there will be more discussion of this case and we
will hear from the investigator and consultants on this.
In the next presentation Dr. Lesley Russell will review...
GOODMAN: Before you go to that presentation, Dr. Rappley?
RAPPLEY: I have two questions; the first, in the 30,000 children that you expect
were exposed in the postmarketing period, do you expect that most of them
received the 200 mg dose?
STANKOVIC: As I said, it is very difficult to know exactly what dose was
prescribed and for what indication it was prescribed so I cannot comment on
that. I don't really know. As Dr. Temple mentioned earlier, one can assume a
variety of things. Whether it was 200 mg or higher, we don't know.
RAPPLEY: And, in your study 310 it was cited for not obtaining hematologic
values, and one of the sites was with 21 patients. In looking at your table on
slide 76 which describes neutrophilia, to what extent did those missed samples
affect your data? How many samples were missed?
STANKOVIC: I can't give you the exact number; I don't know it off the top of my
head, but I think that the number of analytes may be 390 or maybe 20 or 30
patients that don't have all of the analytes, but I am not positive about that.
I can find you that number.
RAPPLEY: Thank you.
GOODMAN: Dr. Leon?
LEON: I would like clarification on the case control analysis you did. In the
sponsor book it is on page 64-65. You very briefly made reference to your
analyses...
STANKOVIC: Yes. LEON: ... in your slides, that you found no risk of a variety of
dosing factors for the rash. It was a dependent variable. It was a case control
where you had 39 cases and 3 times that number, 117, controls apparently matched
on 3 variables. I have some questions.
First of all, it looks like you entered about 14 variables that were very highly
correlated simultaneously. I mean, that is what it says here.
The effects were measures of dose entered at one time.
RAPPLEY: Will you show us the document you are referring to? Is it this one?
LEON: Yes. Sponsor's book page 64-65. I mean, this is being used as evidence of
no association when the analyses were not conducted in the way that I believe an
association would be detected.
So, my first question has to do with entering all those variables
simultaneously, very highly correlated measures of dosing.
My second question has to do with what is the statistical power you would have
with this sample size? You would have statistical power to detect what effect?
The sample size is only 39 versus 117.
Would that be an odds ratio of maybe 2 or 2.5? You could miss some pretty
substantial associations.
Third, did the analyses account for the clustering of these sets of 4 who were
matched? In what way did it account for it?
KINGSBURY: Let me address these one at a time. First of all, let me inform you
that we did not use all 14 variables at a time. This was just different
approaches to explore those and they were done one at a time. OK?
First of all, let me describe the matched control analysis that we did. There
were 39 cases.
We found 3 matched controls, as described in the briefing document. As already
indicated they were matched by the study they came from; by the weight stratum
they were in; and also by having been in the study at least as long as the time
taken for the event to take place.
So, in that set, using each of those 14 variables one at a time, we looked at
the distribution of whatever the dose was in quartiles and tried to ascertain
whether there was a relationship, but understanding the limited power. This is
more of an exploratory analysis...
LEON: What was the way that you accounted for the clustering of these quartets
of case controls there? What was the analysis?
KINGSBURY: I am sorry? LEON: Well, you have groups of people, as you would in a
paired T-test if you had diads, and you have sets of 4 people who are matched on
these criteria that you just described, and I want to know what is the
statistical analysis that was used to account for this clustering, the
correlation among these sets, these quartets.
KINGSBURY: We did essentially a conditional logistic regression in which we
defined this stratum as the case. We identified each case and the corresponding
matched controls.
Then we looked at the odds ratios of each of the various increasing quartiles
relative to the fist quartile just to get a sense -- I mean, this was very much
a descriptive statistical approach to see if there was any evidence of a
consistent dose response. We did not find that.
LEON: So, you acknowledge limited power. You have power here with 150 subjects
total to detect what size odds ratio? Just so you can let us know the magnitude
that might have been missed there.
KINGSBURY: Because it was not an a priori designed analysis, we did not focus on
that issue. We actually did not test anything; we were just obtaining confidence
intervals because that is all we felt would be appropriate.
As I mentioned before, although the confidence intervals overlapped 1, the odds
ratios extended from 0.09 to a little over 2.
LEON: But when you are looking to see if confidence intervals are overlapping 1,
then you are doing tests, exactly the same as looking at p values. You are
getting more information as well about the magnitude of the change and about the
variability of that change, that association.
KINGSBURY: We don't claim to have shown no association. All the conclusion we
are making is that -- by the way, consistent with the limitation in the numbers
that we have no compelling evidence of an association, we did an additional
analysis based on the randomized clinical trial data, and from that analysis we
found an odds ratio of 1.4 with a confidence interval extending from 0.678 to
3.094.
Going back to the case control analysis...
GOODMAN: Thank you very much. Let's go on to our next speaker.
Thank you.
STANKOVIC: The next speaker is Dr. Lesley Russell.
RUSSELL: Thank you, Dr. Stankovic.
We have presented a lot of information this morning regarding the efficacy and
safety profile of modafinil in the treatment of ADHD.
Following your deliberations, you will be asked to answer two questions, the
first being has modafinil been shown to be effective for the treatment of ADHD
in children and adolescents?
We believe that the answer to this first question is yes. In the 3 pivotal
studies consistent benefit of treatment with modafinil was seen in all 3
studies, with these effects observed by the teacher, the parent and the treating
physician across different rating scales and instruments, and with effects being
observed both at home and at school.
You are also going to be asked today whether modafinil has been shown to be
acceptably safe for the treatment of ADHD in children and adolescents.
In the Phase 3 clinical program modafinil was generally well tolerated. The most
common adverse events reported, insomnia and anorexia, were generally mild to
moderate in severity and rarely a cause for treatment discontinuation. No
adverse signals were observed in the Phase 3 program with respect to pulse,
blood pressure or growth.
We were asked in the approvable letter to provide more information on 3 cases of
liver transaminase elevations.
As outlined in our response to the approvable letter and presented here today,
in 2 of these cases the transaminase elevations were resolving on continued
treatment with modafinil with, in 1 case, ALT values returning to normal whilst
continuing treatment.
In the third case the transaminase levels were returning to normal on
discontinuation of treatment. We do not believe that an adverse signal with
respect to liver function has been observed.
Concerns have been raised over the reporting of psychiatric adverse events. As
you are aware, these events were fully discussed yesterday at the Pediatric
Advisory Committee for all ADHD products.
Although no consensus was reached on how to label aggression, psychosis, mania
and suicidality, Cephalon has proposed language in the warning section of the
label which we believe provides appropriate information regarding these events
seen in our clinical program.
Concerns have also been raised over the reporting of serious skin reactions, and
in the approvable letter we were asked to provide you with more information on 3
cases of interest seen in the clinical trials and 4 cases reported in adults in
the postmarketing setting.
As suggested by FDA, these cases were reviewed by experts in the field and there
appeared to be general concurrence reached by these reviews and Dr. Porres, from
the FDA, with respect to the first case, the 7 year-old boy with possible SJS.
But there does appear to be some diversity of opinion regarding the other 2
clinical trial cases.
This seems to be in keeping with the diagnostic and etiologic uncertainty
surrounding the diagnosis of these types of skin reactions. However, we
acknowledge that an association with modafinil cannot fully be excluded. In all
3 of these cases, however, the events did abate following discontinuation of
drug and no adverse sequelae occurred.
In assessing the risk for SJS and reviewing the totality of the data in the
clinical trials and postmarketing database for both adults and children as
reviewed, we believe that the risk for SJS is low. However, we have proposed
language to be included in the warning section of the label.
Based on your deliberations today, we will be happy to modify this as
appropriate in order to provide patients and health care providers with adequate
information concerning these events.
Lastly, modafinil is not a new chemical entity and to date there have been
780,000 patient-years of exposure which, when looking at actual patients
exposed, may equate to approximately 3 million exposures since introduction of
the drug in France, in 1994.
Pharmacovigilance is undertaken to assess risks associated with modafinil usage
and, as you have heard today, this has led to 3 labeling changes, one regarding
the incidence of severe skin reactions. Cephalon is committed to improving these
risk assessments further by undertaking a more structured case ascertainment
with respect to skin adverse events.
So, in conclusion, we believe we have shown you today that modafinil is an
effective treatment for ADHD with an acceptable safety profile, with the
benefits of treatment outweighing its risks.
Thank you for your attention.
GOODMAN: Thank you. May I suggest that your team stay at the podium to address
some questions? I am going to assume that most of the committee members are
going to have questions for you.
If we start to run out of time, we are going to have more opportunity to ask
those questions later this afternoon.
Let me start off with what may be the easier of the two questions we are asked
to vote on today, the one regarding efficacy. From the FDA standpoint and what I
read, they were satisfied with the efficacy data. I certainly feel satisfied
from what I have seen.
Yet, before we move on to the harder question of evaluating issues of safety, it
is very important to have the context in mind of the benefit.
So, I want to give you an opportunity to answer, from your perspective, where
you see this medication fitting in; where is it going to add value or options in
the marketplace? Is it going to be advantages in the area of efficacy,
tolerability?
I wonder if you could just expand on those issues to give a little bit of a
framework to think about the benefits of this medication.
RUSSELL: Well, as you heard from Dr. Biederman with the MTS study, despite
treatment with drugs that are considered to be very effective -- and we
certainly don't doubt that -- there does remain a group of patients that still
either cannot tolerate drugs or don't respond to them.
We saw in our program that, although maybe not considered refractory, patients
who had failed on a prior stimulant therapy did appear to benefit from the drug.
We also saw that if you are stimulant naive you respond slightly better to the
drug.
So, we see this as a viable treatment alternative to other drugs that are
obviously commonly used and considered to be effective agents. However, I would
like to have a treating physician in the field come up and maybe give you that
from his perspective.
So, if I could ask Dr. Biederman?
GOODMAN: Sure, go ahead.
BIEDERMAN: I think that in clinical practice we need alternative treatments to
treat our patients. The idea that the most efficacious treatment treats all our
patients is not true to life. So, clinicians in practice need to have options to
allow us to better serve the people that consult with us.
The issue of adverse effects is a statistical issue. That means that even if
side effects are similar within a class of drugs, some patients clearly tolerate
one versus another even if on average they have a similar spectrum of adverse
effects.
So, patients that have poor tolerability may benefit from a drug that may have
on average similar issues but may be better tolerated for them.
Finally, the issue of scheduling -- I think that even though many of the new
generation stimulants that are available today are clearly less of an issue for
diversion and abuse, many clinicians and many families do not want their
children to be on a Schedule II drug.
So, I think that this gives an option for clinicians to use a lesser scheduled
drug in cases where they choose not to use a scheduled compound.
GOODMAN: Joe, before you step down, has it been your impression so far that
there is less abuse potential, less potential for diversion as, say, compared to
stimulants?
BIEDERMAN: Yes. I am not an expert on abuse and we have here a colleague that
specializes in that. The abuse and diversion -- first of all, let me comment on
abuse and diversion. There are different publics that use these drugs
recreationally and therapeutically.
Our battles in clinical practice are to encourage our patients to remain in
treatment. There is a very severe problem of non-adherence to these treatments.
So, it is not something that our patients look forward to taking.
The attraction of the stimulants is when the tablet can be crushed and snorted
for an IV-like experience. It is the parenteral intake that produces the
euphoria, not the oral intake.
So, this drug is not snortable, injectable, and so on and so forth, so it is not
a drug that the addict community on the street would pay a high price for to get
it.
But maybe we can get some of our colleagues that are here with better expertise
than mine on diversion and abuse to give a perspective.
RUSSELL: Does that answer your question?
GOODMAN: I would like to hear a little more on that issue.
RUSSELL: Dr. Dackis?
DACKIS: With regard to the abuse potential of modafinil, I think it is important
to note that it is chemically unrelated to central stimulants and has a very
weak effect on the dopamine transporter so that it is extremely unlikely to
increase dopamine levels, except in very high dosages.
There have also been a number of studies in humans to assess what the subjective
effects of this agent are and these studies, which have been conducted by
Jasinski demonstrate that in males there is no effect of modafinil.
There was a smaller study in females that did show some stimulant effects using
these various rating scales. Two other studies, again, showed that there was not
a significant high; that the subjects were not willing to pay money for
modafinil, et cetera.
In addition, animal studies, looking at things like self- administration and
condition-place preference showed very weak stimulant-like effect of this agent.
So, there is some reinforcing quality but it is very, very weak.
GOODMAN: I thought monkey studies showed preference.
DACKIS: Yes, that is correct. Gold and Balster's study did show that monkeys,
trained to self-administer cocaine, if given modafinil would continue to
self-administer large doses of this agent, as they would with other compounds
like ephedrine. So, large doses are required to continue to self-administer.
GOODMAN: Thank you.
Dr. Temple?
TEMPLE: I am sympathetic to the idea that drugs with different pharmacology may
have different usefulness, but I want to address the question of whether they
have documented the ability of this drug to work in people who are resistant to
stimulant drugs, and the answer is that they have not.
There is a perfectly simple, never done kind of study design to do that. You
take people who fail on whatever it is you want to test and then you randomize
back to that drug and to the new drug. It is a perfectly simple study.
That is how clozapine came to the market because we wouldn't have approved
clozapine unless it worked in failures because of the 1.5 percent
agranulocytosis. That study could be done. You might even think about whether it
is something that ought to be done, but it has not been done.
The mere fact that people given a second drug after failing the first respond to
it tells you nothing at all. We have many examples where drugs don't
particularly work in non-responders to other therapy but the second time around
the people do better.
So, I just want to make it clear they have not shown that. It might be true. It
is plausible even but it hasn't been shown.
PINE: Can I ask a question about that? Of course, there have been other
medications that have been discussed over the last couple of years for new
indications for ADHD and I am sure that that issue came up.
I think that those studies have not been done and what was the thinking and
discussion around that?
TEMPLE: Well, they are almost never done. We don't usually have a reason to say,
for example, only use this drug in people who have failed on other therapy, if
one thought that was an appropriate thing because I am not saying you should or
not -- you are going to get to that.
I am just making the point that they have not documented in a rigorous way that
the drug would actually work in those people. You might think that there is a
little evidence that it does, and you might think the pharmacology difference
suggests that it might, all of which I agree with but that hasn't been studied
and it can be studied, and it never is studied.
PINE: For what it is worth, my take on it would be that that would only be one
of the potential uses of the medicine clinically, and it seems like some of the
other issues are, you know, kind of bigger in terms of thinking about the
medicine as opposed to, you know, is it primarily for people who don't respond
to stimulants.
REESE: We are going to get to everyone's questions. First we are going to have
Dr. Bronstein and then we will have Dr. Wang.
Thank you.
BRONSTEIN: My question is a fairly straightforward, easy one. On slide 93, in
the Phase 3 study you have one person who had a severe event and withdrew from
the study. What kind of rash was this? RUSSELL: Unfortunately, the only
description on the case report form, which reflects the source documents, is
just a verbatim of rash so I am unable to describe it further for you.
BRONSTEIN: We can assume though that it was severe.
RUSSELL: It certainly led to discontinuation of the drug. That is all the
information I can give you.
BRONSTEIN: Thank you.
REESE: Ms. Dokken?
DOKKEN: Yes, I apologize, I thought we were supposed to hold our questions until
the end so my question really goes back to slides 30 and 31 and this issue of
the 40 percent who are non-responders or had intolerable side effects.
I am wondering whether anyone can sort of unpack, you know, how many people are
in which category because it seems to me that what we have been hearing is that
one of the marketing messages for modafinil will be that it is an alternative.
If it is an alternative and we are talking about whatever percentage of that 40
percent are ones who suffered "intolerable" side effects, certainly this
particular drug -- and those of us who were fortunate or unfortunate enough to
be present yesterday, you know, the side effects are present in almost all.
Then that leads me to the worry about the next step which is, you know, if it
were approved how is it marketed and what are the messages because probably it
was the Pediatric Advisory Committee that has seen, you know, other situations
where something is marketed as being free of something else, suggesting that
there are no risks and to say that because it is a non-stimulant it has no risk
would be a concern for me.
TEMPLE: Drug advertising reports to me so I have to worry about this. We are
fairly careful about making claims when you don't have a direct comparison and
there aren't any direct comparisons.
However, if one is scheduled at a different place, or something like that, that
is true and they would be allowed to claim that.
There are some cases in which the difference in certain side effects is so
obvious -- like it never happens with this and it happens all the time -- where
we might allow something like that.
But we are very careful about comparisons in the absence of actual comparative
data across study comparisons and treat it with suspicion.
REESE: Dr. Pfeffer?
PFEFFER: Thank you. I am not questioning the efficacy but I have some questions
on slides 52, 53 and 54, please. Maybe you can help us understand the
longitudinal process of the three studies.
For example, it looks as if in slide 52 I guess efficacy was being demonstrated
by week 5.
Then in slide 53 and 54 it seems that it was earlier, although on slide 53 at
week 5 there was perhaps less of that. I don't know if that is due to dropouts
and then resumption.
So, my question is on the early phase of these, week 3 and even week 2 on slide
54, what were the general doses that the children were on at that point in time?
Then, if you can tell us what happened in week 5, on slide 53?
Finally, if you could tell us a little bit about when were blood tests taken in
the process of the study and when did the side effects emerge, especially skin
reactions, et cetera? I am trying to link the time course with the doses and the
longitudinal course.
RUSSELL: In study 10, which is the slide up here, this is the fixed dose study
so that by the second week patients would have been titrated to that target
dose. That would have occurred by day 7 for those randomized to 340 and day 9
respectively.
PFEFFER: I thought I understood that but my concern is if, in slide 53 and 54,
you see earlier efficacy is that at the target dose or less than the target
dose?
RUSSELL: In this study, which is the fixed dose study, they would have been at
target dose.
Could you go back to the previous slide for 311, please? This is one of the
flexible dose titration studies. So, in the earlier weeks they would have still
been titrating up.
PFEFFER: Do you know approximately the average doses at the early phase?
RUSSELL: Probably around 255 mg by the second week and up to the 340 mg by the
fourth week.
PFEFFER: And on slide 54 it is similar. Is that right?
RUSSELL: Slide 54, which I think is study 310, is where they titrated up more
quickly so they would have been at target dose by day 7 and 9 respectively.
REESE: Dr. Armenteros and then Dr. Malone?
ARMENTEROS: Just to follow-up a little bit on the dosing question, I understand
the model that you used to dose the two groups of children, you know, below 30
kg and above. Now, most of the children that got into the study were above 30
kg, like 68 percent that you mention here.
Now, when you presented data on efficacy there wasn't a differential response
between these two groups by weight. The reason that I ask that question is that
we already know from your previous studies that at lower doses you do get
response for daytime sleepiness, and so forth.
So, I don't know if we may be missing perhaps different points in dosing at
which these kids may respond. Because at the end of the trial I come out with a
very fuzzy impression of what the actual dosing should be and I hope I can get a
better understanding.
RUSSELL: First let me answer the excessive sleepiness programs first because
what we do find is a very different pharmacodynamic response when we are
treating excessive sleepiness than when we are treating ADHD.
So, in the excessive sleepiness programs and the pediatric narcolepsy, although
we looked at doses of 100 mg through 400 mg, doses of 400 mg were clearly
efficacious in that model.
Then we did some PK/PD work and the target exposure needed for an effect in
narcolepsy is substantially lower than the target plasma exposure associated
with effect in ADHD -- so very different pharmacodynamic response which I don't
think I can explain, but it is very different.
In terms of looking at the doses and how did they respond to efficacy, what we
did was to look at the different quartiles of dosing and in the third and fourth
dosing quartiles, which are the higher dose groups, you see numerically a
slightly higher response but it is only a point or two.
So, I would say that the dose response, with all the caveats because we were
titrating to a target dose, is flat in the doses that we looked at here.
REESE: Dr. Malone?
MALONE: I have two questions. One is on efficacy. The stimulants wear off every
day by the end of the day. Is that true for this drug? I am just wondering if it
is like the stimulants, that you have to dose it every day; you dose it in the
morning and then it wears off by the evening.
RUSSELL: The only data we have with respect to that is actually in the 2-week
withdrawal period where the patients who had received modafinil during the
double-blind treatment period were randomized to either stay on modafinil or
were randomized to receive placebo.
What we see is not an immediate return to baseline in symptoms but a more
gradual return towards baseline and their symptoms.
So, based on the limitations of that data which I acknowledge here, there
doesn't appear to be a sort of complete rebound effect.
REESE: Dr. Bigby?
BIGBY: I have a question about the ADHD rating scale. If you gave this test to a
group of normal kids who don't have ADHD, what would their score be?
RUSSELL: The average for a 10 year-old boy I think is 18.8, and the children
going into our study had an average of around 37.
So, they were clearly much higher than what would be considered to be normative
for a 10 year-old boy, which was the average population in our study.
It does differ a little bit based on whether you are a boy or a girl or your
age, but that appears to be the average for a 10 year-old boy.
GOODMAN: Dr. Temple?
TEMPLE: In one of the studies you actually did a withdrawal phase but I believe
the data weren't shown.
RUSSELL: That is right.
TEMPLE: You must have a slide of it.
That would answer the question of how soon it wears off.
RUSSELL: If I could have the slide, please?
This is over the 2-week withdrawal period.
You can see on the right-hand side that the placebo at the end of the 7-week
period and the end of the 9-week period obviously stays the same. In the
modafinil group there is a point difference, but for those who were on modafinil
and then got changed to placebo you can see that there is a beginning of
deterioration of their symptoms over that 2-week period.
It is not huge but there is a deterioration and it looks like they are returning
towards baseline. But there doesn't appear to be a sort of instantaneous effect.
TEMPLE: And you don't have it day by day or anything like that?
RUSSELL: Unfortunately, we don't.
REESE: Dr. Malone, your second question and then Dr. Rappley.
MALONE: It was really I guess partly answered. It had to do with the abuse
potential for modafinil. I think, from the reading, it did say that it can cause
euphoria and that animals would work for this drug.
If that is true, I just have a question why would a stimulant be a Class II and
this a Class IV? How do they decide that?
GOODMAN: Dr. Temple or Dr. Laughren?
I have a very similar question about the classification. Currently this drug is
classified Schedule IV compared to the stimulants which are Schedule II. Could
you just explain that distinction?
It would be in the context of a quick follow-up I was going to do and ask
sponsor how they would best characterize or classify their compound.
LAUGHREN: Actually, FDA doesn't decide that classification. The decision is made
by the Drug Enforcement Administration. They do an 8-factor analysis. I haven't
looked at that.
Maybe the company could respond to, you know, how it is that the DEA arrived at
a Class IV rather than a Class II.
TEMPLE: There is a very sharp distinction between the level of control. I think
we are about to hear about that. II is, you know, locked cabinets and all the
rest; IV is much less.
GOODMAN: Yes, please, could we hear about that?
RUSSELL: The difference between a Schedule II and a Schedule IV, is that what
you are asking?
LAUGHREN: How it got a Schedule IV rather than a Schedule II.
RUSSELL: I wasn't with the organization at the time of the original scheduling.
Perhaps I could ask Dr. Vaught, who was here, to explain how that happened.
VAUGHT: Good morning. My name is Dr. Jeff Vaught, executive vice president for
research and development for Cephalon.
I would like to very briefly just go over the aspects of scheduling which,
certainly the agency knows as well as I do, has to do not only with the physical
chemical characteristics of the compound but also testing that is done in human
beings to suggest that there is a reinforcing property.
So, if we look at the overall physical chemical activity of modafinil, it has
very, very low water solubility which is incompatible with intravenous
injection. It is very unstable at high temperature, therefore, it is
incompatible with smoking.
Importantly, it is structurally unrelated to other agents that are known to be
abused. While it does have a very, very weak -- and it is really the only
neurochemical effect that we have been able to demonstrate in blood receptor
binding assays, et cetera -- with dopamine.
It doesn't appear to cause elevations of dopamine of nucleus accumbens, which is
markedly related to drugs of abuse, as well, it has not releasing properties as
do other Schedule II stimulants.
There is also lack of activation, as I mentioned, of reward centers, and really
the results, as Dr. Dackis described to you, from preclinical studies suggest
that if there is a signal it is very, very weak. Now, all this is theoretical
because that is all nonclinical data. Perhaps more importantly and something
that we undertook at Cephalon spontaneously, is a postmarketing surveillance,
starting in 1999 with the Haight Ashbury group.
The Haight Ashbury group monitors a variety of areas worldwide where drugs may
be diverted to, including rave scenes, medical professionals, et cetera.
Now that we have had six years we still have reporting on this. There have been
limited to no reports of euphoric effects. There are no reports of reinforcing
effects.
There has been a very large increase since the drug has been approved for
wakefulness for mainstream publicity regarding the use of modafinil, including
in The New Yorker magazine, college newspapers, et cetera, and across the
Internet every now and then we will see postings of potential use but nothing
that is consistent.
In fact, the Haight Ashbury concludes after evaluating this for the last six or
seven years that if there is abuse potential for modafinil at all, it is very,
very low.
So, all of this is consistent with what is seen as an agent with low abuse
potential.
We now have considerably more experience with the substance than we did five or
six years ago when we were getting approval and we thought that was consistent
with the regulatory standards for Schedule IV.
GOODMAN: Thank you. Apart from how DEA will classify your drug, how would you
internally classify it? Would you say it is a stimulant or is it distinct based
upon its mechanism of action, which I understand is unknown.
Although I know at one time it was thought to be mediated through orexin
receptors, I guess that is not as firmly established at this point.
The reason I ask is not just a semantic question but whether it gets counted or
considered a stimulant may have labeling implications. As revealed by
discussions yesterday, for example, Strattera, should that be considered a
stimulant and, if so, should it have certain warnings attached to it that go
with the rest of the class of stimulants?
So, I would just like the sponsor's perspective on whether you would classify
this medication as a stimulant or not.
VAUGHT: We approach this from a couple of levels. One is the preclinical data
that we have, as well as the clinical information. In direct answer to your
question, I would not classify it as a traditional sympathomimetic stimulant.
It is a CNS activating agent and we have all been taught, prior to the
introduction of modafinil, that, in fact, most of our CNS activators are
psychostimulants.
Nonclinically, modafinil has a profile of wake-promoting activity that, unlike
the classical stimulants -- its wake-promoting activities are not blocked by
haloperidol which has been characteristic of wake, if you will.
As far as the orexin component that is involved, we have been able to
demonstrate it has no interaction with the orexin system because in knock-out
animals, as well as human beings and dogs it is highly effective. When we move
to human beings, we similarly don't see the typical types of profile that one
sees with the stimulant population.
If we include this with methylphenidate and amphetamines this includes
sympathomimetic-like effects as well as generalized excitation reinforcing
properties, euphoric effects, et cetera.
So, overall the pharmacology would suggest that if we want to classify it as CNS
activating agent it is certainly a non-traditional agent.
GOODMAN: Would you say that it has less peripheral -- if you look at the
relationship between CNS, there is relatively more CNS to peripheral activation?
VAUGHT: Yes.
GOODMAN: That was my last question.
REESE: Dr. Rappley?
RAPPLEY: My question goes back to the safety area and pharmacodynamics. Dr.
Mannheim noted that we don't have information about steady state for the sulfone
metabolite. We know it accumulates to a much greater extent in children but we
don't know quite when that steady state is achieved and I wonder if you have
more information about that.
RUSSELL: The sulfone metabolite appears to reach steady state at about 2 weeks
and then it actually plateaus thereafter.
REESE: Dr. Wang?
WANG: I have one more housekeeping question about efficacy. Are these effect
sizes and response rates -- I guess this is either for the sponsor or maybe our
pediatric colleagues -- are these response rates comparable to what is seen with
other treatments for ADHD or is there some differential response here?
RUSSELL: Dr. Biederman?
BIEDERMAN: I believe that the computed effect size is about 0.7, very similar to
the effect size of Strattera; lower than the effect sizes of the stimulants that
are about 0.9. So, it is lower than the stimulants but potent enough to treat
ADHD. WANG: Then this is actually a question for the FDA. The sponsor is already
proposing warning language and I am curious what are the potential actions you
can take. I mean, bolded warning; black box warning? Are those the same thing?
Are there other intermediate warning language actions you can take? Because the
sponsor is already proposing potential language.
ANDREASON: I am sorry, I missed the first part of your question.
WANG: Firstly, I should know this but is there a difference between bolded
warning language and a black box warning? And, are there intermediates between
them and what other options are there?
ANDREASON: Yes, they are different.
Which adverse event are we talking about here?
WANG: They are already proposing language for, it sounds like, psychiatric
adverse events and also for skin rash.
LAUGHREN: Well, there is a difference between bolded language and unbolded
language in warnings. I mean, sometimes if we want to give particular emphasis
to something we will bold it.
That is different than a box. A box goes as the first thing in labeling and it
is surrounded by a box. So, that is very different than just bolding language in
warnings. So, there is a continuum.
TEMPLE: In the context of the CNS warnings, you need to think about it in the
setting of the consideration of all of the drugs that went on yesterday, and so
on. The skin is their own baby.
So, if we were very worried about it we could put it in a box. Usually you put
things in a box when you want to be very sure that the doctor absolutely,
positively considers this before prescribing it.
There are other things you can do.
Ziprasidone, because of the QT prolongation, says you really think should think
about using other drugs before you do this. You can go further, you can say this
is absolutely only for people who fail other therapy.
Sometimes we do that even if we don't know for sure, as I said earlier, that it
absolutely works in people who failed other therapy. You know, because of its
different properties, you assume there might be a population that responds that
way. There are a variety of things you can do to try to direct therapy.
We like to say we don't practice medicine but we do sometimes try to influence
the way a drug is used if we are worried about its safety. The black box is the
loudest statement. There is at least a perception that it affects use because it
scares people.
That is why some people like it and some people don't like it. Bolding is more
prominent than non-bolding, and so on. REESE: Dr. Leon?
LEON: Dr. Biederman, I would like to clarify what you said about the Strattera
effect relative to what we saw in this trial. It is my understanding that the
Strattera effect size was about 0.80 and in these data it was 0.56.
So, this is quite a bit smaller. It is still a minor effect size but it is not
as large as was seen in the Strattera trial.
BIEDERMAN: To my knowledge, and I don't remember those numbers by memory, but I
think between 0.6 to 0.7 is the effect size of modafinil.
The company may have that information better than me. I understand as well that
the effect size of Strattera on average is very much similar at about 0.7.
In the meta-analysis of non-stimulants that Dr. Faraone did a relatively short
time ago, that is shared by other non-stimulants as well, like tricyclics and
things of that type, on the order of magnitude of 0.7, a low effect size of
stimulants at about 0.9.
REESE: Dr. Pine?
PINE: I would like to go to slide number 89. I guess the thing that I am
struggling with most, and I think a lot of people might be, is the dermatologic
issue.
On the one hand, I don't want to start a fight but, on the other hand, I guess I
am struggling a little bit with some of the inconsistencies in terms of the way
three of the cases on slide 89 are being discussed.
So, I guess what I want to do is point out what I see as the inconsistencies and
then maybe hear from Dr. Bigby about do I have it right; do I not have it right;
and then maybe also try to clarify some of those inconsistencies.
So, the way that I heard it is that case number 1 or patient number 1 everybody
agrees had Stevens-Johnson but there is disagreement about the etiology, I
heard, which confuses me a little bit because I don't understand what the
etiology possibly could have been except for the medicine or except for the
modafinil. So, I would like to hear discussion about that.
For patient number 4, at least what I heard was that Dr. Bigby did think it was
Stevens-Johnson and I heard that two out of the three experts at Cephalon
thought it was at least possible Stevens-Johnson.
So, at least in the way I am thinking about it, I would think of those as two at
least likely cases.
Then, for patient number 5 I am a little blurry in terms of the magnitude of
concern as a non-dermatological clinician. If I see a possibly suggestive
hypersensitivity reaction or whatever Dr. Bigby classified it as, is that
equally concerning, or slightly less concerning, or how much less concerning
than Stevens-Johnson?
So, do we have three cases where everybody would agree that these are concerning
dermatologic issues? Do we have one case? Do we have two that are somewhat
concerning and a third that is suggestive? You know, can we get some agreement
on that?
REESE: Dr. Bigby?
BIGBY: What I would say is that case number 62338 is a case of Stevens-Johnson
syndrome and, based on the information that is provided, I would say it is drug
related.
PINE: What about the other two? For case 18004 would you also say that? And,
what is the disagreement?
BIGBY: I would say that that case is more likely to be due to something else
other than a drug. So, I don't actually count that as a drug-related case. What
was the third one?
PINE: The third one was case 056003.
You said fever, urticaria, swollen eyes, vomiting, increased ALT/AST and the
Cephalon review said possibly suggestive of a hypersensitivity reaction -- I
guess level of clinical concern in terms of a serious adverse effect related to
the medicine.
BIGBY: You are going to have to give me a little time for that one.
PINE: OK. Dr. Goodman is whispering in my ear that he wants to know what made
you conclude on case number 18004 that it was not medication related.
BIGBY: For that case it is just not so clear to me what the diagnosis is. I
mean, it is hard in sort of spottedly reported case reports to figure things out
and I just am not convinced that that is a drug rash at all.
PINE: Then I guess the last question, when I asked you before about your level
of concern you seemed fairly clear that there is, quote, a signal here in terms
of dermatologic risk. Based on what you just said, my conclusion would be that
you are basing it on this one confirmed case out of 923.
BIGBY: Plus, there is a signal for exanthems. Those aren't serious reactions but
there is also a signal of exanthems occurring with the drug.
PINE: But I also understood you to say that there is not necessarily a
relationship between exanthems and incidence of Stevens- Johnson.
BIGBY: This is correct.
PINE: So, again, I guess what I am hearing is that it is really the one case out
of the 923. BIGBY: I think that that is a good summary of how I feel about it.
RAPPLEY: But there are also the four cases in adults. Is that correct?
PINE: I think those were in adults.
RAPPLEY: That is right, in adults.
PINE: And it was consistent with the base rate. When we looked at the
patient-years exposure it was consistent with the base rate of Stevens-Johnson
syndrome, the four adults.
REESE: Dr. Robinson?
ROBINSON: Could we go to slide 112?
I just want to clarify a few things because in Dr. Andreason's presentation it
said that we were finding some dermatologic signal within the clinical trials
but not in the postmarketing, and I just want to clarify a few things on this
slide.
In the pediatric subgroup you didn't find a signal for rash in the
postmarketing. Is that correct?
RUSSELL: Certainly, in the postmarketing setting in children we have had no
reports of any serious skin reactions. That would be correct.
ROBINSON: OK. Then, one of the questions about that is, is that because there is
none or is it that you are unable to detect that?
So, that is why I would like to ask a question about the psychiatric signal that
you do have in the pediatric subgroup because in the clinical trials it seemed
that there is some signal about suicide and psychosis, and in the postmarketing
data for pediatrics were you picking up that signal?
RUSSELL: In the postmarketing data we saw seven cases that Dr. Stankovic
highlighted for you.
ROBINSON: That was in pediatrics?
RUSSELL: That was in pediatrics, yes.
ROBINSON: And it was which ones?
Psychosis or suicide?
RUSSELL: If I remember right, there were three psychosis, one suicidal ideation.
Perhaps you can clarify?
STANKOVIC: There were four cases of psychotic symptoms. There were two cases of
aggression and violent behavior and there was one case of a suicide attempt.
That was the patient that overdosed and used modafinil as one of the cocktail
drugs but it was not modafinil prior to the event.
RUSSELL: Thank you for clarifying.
ROBINSON: Thank you.
REESE: Dr. Temple?
TEMPLE: Back to derm., I think it would be helpful to be clear on what the
appropriate denominator is because there seems to be one case everybody agrees
on. This 933 number that has been used includes some very short exposures.
Dr. Bigby can tell us what kind of exposure is enough, but let's say we wanted
to say how many of those 933 or some of the people from the other studies had,
say, at least two weeks or whatever the right amount is. That would help.
Maybe it doesn't matter whether it is one out of 900 or one out of 600 but it
would be good to have a number. So, how many people who were on it long enough
to have had a nasty skin reaction actually were there for that one to be the
numerator for?
BIGBY: That is a very good question. You know, I think that the best data
available about the window of exposure where TEN/SJS is going to occur comes
from that study that I cited. It was sort of a consensus panel in three
countries, and the majority of cases occur within the first one to four weeks.
It is probably one to three weeks. And, if you sort of include in your
denominator patients that have been on it steadily for months and months and
months you actually probably come up with a lower rate than the actual because
the time that you are going to get it in is in that first month.
REESE: We can have the response and then Dr. Armenteros.
RUSSELL: I can get Dr. Shear to come up and comment on these cases with respect
to etiology and all the other aspects we have been discussing.
SHEAR: Thank you very much.
From a dermatologic point of view from somebody who has been doing this for 20
years, first of all, I would like to thank Dr. Bigby for his excellent
presentation because I agree with what he said and this is an area that has been
really messy over the years and you can see the confusion that led us here.
So, I would really focus on that one case of Stevens-Johnson syndrome. Going
through that case extensively -- the panel went through it but I also went
through it with the panel again, with Amy Paller who was the leader of the panel
-- to try and figure out exactly what was going on with that case and how we
could best characterize it.
I think we see enough to call it either Stevens-Johnson syndrome or maybe
erythema multiforme major. You could then argue about which it is, and does it
really matter since both of those can be viral induced?
Speaking with the investigator and looking through the case records, there were
clear viral-looking lesions that suggested Coxsackie very highly in the pharynx
prior to the patient getting this.
The clinical course was very compatible with a viral-induced either erythema
multiforme major or Stevens-Johnson syndrome because actually the patient was
not that sick and was able to continue going to school and continue with other
activities.
Part of the problem was getting the full history, and much of it was
retrospective and there was a language barrier, but the patient wasn't sick
enough to be admitted to hospital or really to be seen very carefully during the
actual event.
But still, piecing it together, I would certainly put viral etiology well within
the mix. I don't know what percent I would give it but, you know, drug is in
there and virus is in there so it is not a completely clear case of either
Stevens-Johnson syndrome nor is it a completely clear case that it was drug
induced.
GOODMAN: Dr. Bigby, would you concur?
BIGBY: I think the patient had SJS.
PINE: But the suggestion is that it could potentially have been Coxsackie virus
induced SJS, which would be a very different thing. Again, I mean I get the
impression that you do not think that that is likely.
BIGBY: You know, it is really impossible, never having seen a patient, to do
this. I don't think you should call things EM if the patient doesn't have
typical targets. There is no description -- the data is inadequate to be very
dogmatic or firm about this.
I mean, I would say that none of the dermatologists involved here would go out
and have a big fight about what this case is because the description is just not
good enough.
SHEAR: Yes, I should mention that in one of the papers it did describe target
lesions.
So, that was helpful but, again, there are all these bits and pieces in trying
to look at the source documents. From the source all the way to the narrative,
you get different bits and pieces.
Some are quite extensive. The MedWatch report has different data, but piecing it
all together, there is uncertainty but it is in that EM major and
Stevens-Johnson spectrum that overlap, if you will. GOODMAN: Hold your
questions. We are going to break for lunch and come back at one o'clock. We will
have the public hearing component at that time.
(RECESS)
GOODMAN: We are going to begin the afternoon proceedings. I am going to ask Dr.
Pine to read the description of the process for the benefit of the individuals
who are presenting at the public hearing segment of today's proceedings.
PINE: Both the Food and Drug Administration and the public believe in a
transparent process for information gathering and decision-making.
To ensure such transparency at the open public hearing session of the advisory
committee meeting, the FDA believes that it is important to understand the
context of an individual's presentation.
For this reason, the FDA encourages you, the open public hearing speaker, at the
beginning of your written or oral statement to advise the committee of any
financial relationship that you may have with any company or any group that is
likely to be impacted by the topic of this meeting.
For example, this financial information may include a company's or a group's
payment of your travel, lodging or other expenses in connection with your
attendance at the meeting. Likewise, FDA encourages you at the beginning of your
statement to advise the committee if you do not have any such financial
relationships.
If you choose not to address this issue of financial relationships at the
beginning of your statement, it will not preclude you from speaking.
REESE: We will have the first speaker, who will have five minutes and when there
is one minute remaining we will let you know your time.
RAVENEL: Dr. Ravenel. As a pediatrician with 36 years experience -- by the way,
I have no financial disclosure; no connections; no funding. I am here
independently as a private practitioner.
With 36 years combined experience in academic and private practice with a heavy
emphasis on behavioral pediatrics, I want to share some concerns with the
committee concerning the pending new indication for Cephalon's modafinil, to be
marketed as Sparlon.
My concerns include the potential for abuse and diversion, as well as data
questioning its effectiveness for ADHD, along with counterbalancing risk of
adverse effects.
Although being promoted as a drug with low potential for abuse, a substantial
risk is actually suggested by the following: One, the FDA posted a warning
letter on January 14, 2002 which compared the abuse potential of modafinil with
that of methylphenidate in an inpatient study of individuals experienced with
drugs of abuse.
Quote: Results from this clinical trial demonstrated that modafinil produced
psychoactive and euphoric effects and feelings consistent with other scheduled
CNS stimulants (methylphenidate).
Number two, an Internet drug information database source states, quote:
Modafinil may be habit forming. You should discuss the abuse and dependence
potential of modafinil with your doctor.
Number three, as reported in the New York Times, the United States Olympic
Committee includes modafinil in a list of banned stimulants and raises the
spectra of widespread diversion and even more problem with, quote, lifestyle and
cognitive enhancement and recreational use as has already been seen with
traditional stimulants.
Several psychiatrists and other professionals with experience with substance
abuse by teenagers and young adults have warned that off-label use of this drug
is, quote, staggering already, and warned that modafinil is very likely to
become the next popular drug for its perceived cognitive enhancement or other
perceived benefits enabling users to remain awake and alert for prolonged
periods.
Marketing claims for the drug's effectiveness for ADHD appear to be exaggerated.
A recent study in the Journal of Pediatrics of the American Academy of
Pediatrics proclaims that at the final visit 48 percent of the modafinil-treated
subjects were rated as much or very much improved compared to 17 percent of
placebo subjects.
One can see that 52 percent of subjects were not improved significantly. This
compares to 75-85 percent comparable improvement on traditional stimulants.
Insomnia was reported in 29 percent of the treated subjects, and it is
noteworthy that drug tolerability was evaluated only by spontaneously reported
adverse events.
This can be expected to minimize adverse events significantly below their actual
occurrence.
The New York Times article quotes experts as being concerned that manipulating
natural sleep by reducing it may have serious consequences such as chronic sleep
depravation damages health, immune system and is associated with life span. All
of these references are provided in my speech.
The aforementioned FDA warning letter to Cephalon pointed out that the putative
mechanism of action being claimed by the company was misleading, noting that the
PI states that, quote: The precise mechanisms of action through which modafinil
promotes wakefulness is unknown, period.
In summary, claims for potential effectiveness are exaggerated and the risks of
adverse events are minimized for a drug which has been shown to have a potential
for abuse and for recreational use that far exceeds even that for traditional
stimulants. Approval at this time for ADHD is premature considering the emerging
controversy and public awareness of issues of adverse events, diversion and
abuse related to stimulants.
It is ironic that this very phenomenon is being used by those promoting
modafinil for ADHD.
That is...
REESE: One minute.
RAVENEL: ... looking at the problems with the stimulants. The FDA would be
better served by exercising caution and by opening the door to even more of the
same criticisms that have emerged recently about stimulant drugs.
Thank you for your consideration.
GOODMAN: Thank you.
REESE: We will have speaker number two.
JACKSON: If you could hold on putting up the first slide, I might do those
towards the end.
Thank you.
My name is Dr. Grace Jackson. I am here independently as a private practice
psychiatrist from eastern North Carolina. I am here today to actually begin by
correcting some of the misinformation which has been disseminated to committee
members over the past 48 hours.
The first point I would like to make is about some of the concerns I have as a
doctor and who has actually worked in the prison system and as a former Naval
physician.
One of the first things I would like to point out is that I think that the
precautions which should be described are basically the elephants that nobody
seems to be looking at in the room. I would like to talk about some of those
elephants.
The first elephant has to do with the fact that stimulants rewire the brain.
This is what Harvard University and McLean Hospital clinicians have referred to
as neuronal imprinting.
Basically, what this means is that we shouldn't be focusing just upon the
potential for current diversion or current recreational abuse, but we should be
looking at the fact that these drugs are altering the plasticity of the brain in
children and adolescents in a way which increases the likelihood of future
chemical dependencies, particularly to nicotine and to cocaine.
I would like to direct your attention to the papers by Nadine Lambert at the
University of California Berkeley, papers published by Russell Berkeley in which
statistical manipulations have been used to try to conceal this correlation, and
also a recent publication from the University of Michigan which has demonstrated
the same kinds of findings, that people who are arriving on college campuses who
have received stimulants in middle school, high school or college have a 3- 7
times higher likelihood of taking prescription stimulants illicitly, and a
higher rate of actually using cocaine in the past year.
The second elephant that I would like to talk about which we haven't really been
hearing enough about, I don't believe, is the effects of stimulants on growth
suppression.
While it used to be the case that doctors took seriously the growth curve, it
seems that this is now something which is casually dismissed.
I believe it is time for the FDA and physicians to begin seriously considering
the suppression of growth not only on the long bones of the legs and the arms,
but also potential impact on the skull which continues development through
adolescence and particularly the growth effects upon the brain, a point to which
I will return in a few moments.
The third elephant I would like to talk about is the fact that no one yet here,
at the FDA or at these hearings in the past two days, has discussed the effects
of stimulants on cortical blood flow, specifically frontal cortex, parenteral
cortex and temporal cortex.
I believe that if you will actually pay attention to the medical literature
there is a real vascular effect which actually deserves a black box warning, at
the least, so that physicians and family members are aware of the fact that
these stimulants have the potential to shrink the cortex, especially the frontal
cortex, and if they are not doing that, at the very least, they are not
benefiting children who, some practitioners believe, begin life with smaller
brain volumes initially.
The next point I would like to make is that we hear so much about the FDA
needing to balance the risks and the benefits of drugs. Well, I would like to
just point out the fact that I have heard numerous references to the MTA study
in the past two days. Fourteen-month outcomes have been emphasized repeatedly.
I would like to just say something that was misrepresented yesterday and again
today. If you will actually go into a paper which was in the Archives of General
Psychiatry in 1999, called "Mediators and Moderators of the Outcomes of the MTA
Study," you will find about two sentences in that whole article where they
actually have done a subgroup analysis of the children who began that study in
an unmedicated condition and who remained in an unmedicated condition.
Those children actually had superior numerical improvements compared to the
children who began unmedicated and were placed on stimulants. While that finding
was not standardly significant, that may have been an effect of the study being
under-powered.
Even more important though is the fact that in the Pediatrics journal, in the
year 2004, 24-month outcomes were published for the MTA study. The findings at
that point demonstrated that the effects of medication deteriorated; that the
trajectories for symptomatic improvement reversed; and, in fact, the benefits of
behavioral therapy -- a modality that consisted mostly of one 8-week summer camp
-- actually had enduring effects.
So, I would like to suggest that this implies that a lot of the treatments that
we are hearing so much about as being so necessary are, in fact, futile when one
carries out the studies to a long enough duration of time.
Finally, I would like to return to the misinformation which continues to
surround the classification of medications that we keep hearing as they are not
really stimulants; they are just central nervous system activators...
REESE: One minute.
JACKSON: I would like to suggest to the committee that they need to talk to the
World Health Organization. Stimulants are classified not on the basis of
potential addictiveness; they are classified as stimulants on their potential to
be CNS activators.
Actually, the World Health Organization classifies drugs on the basis of three
properties: One, chemical structure. You ignore the fact that atomoxatine is a
chemical derivative of phenylpropanolamine, a chemical structure which was
removed from the market by the FDA in 2000 because it caused hemorrhagic stroke.
I would like to point out the fact that the World Health Organization also
classifies stimulants on the basis of pharmacological properties, none of which
require dopamine re-uptake inhibition to meet the criteria of being a stimulant,
and I would like to see that everybody drinking coffee here to recognize the
fact that caffeine, which is an adenosine-2 antagonist, is not something that
you would classify by Dr. Andreason's standards as a stimulant. Yet, I think
Starbucks would say something else.
Finally, I would like to say...
REESE: Time.
JACKSON: Thanks.
GOODMAN: Thank you very much.
BAUGHMAN: I am Fred Baughman, a neurologist. I have discovered and described a
handful of real neurological and genetic diseases.
I am speaking on the chemical imbalance lie as it applies to modafinil and other
ADHD drugs.
If one goes to a physician or takes a child or parent to a physician, if there
is a gross microscopic or chemical abnormality a disease is present. If there
are no abnormalities no physician should say that there is a disease. In
psychiatry there are no physical abnormalities, which means there are no actual
diseases and here we speak of the risk side of the risk-benefit equation.
Psychiatric drugs appeared in the '50s.
Psychiatry and big PhRMA married and gave birth to the chemical imbalance lie.
At a 1970 congressional hearing the chemical imbalance strategy was already in
place. Lippman, of the FDA, argued hyperkinesis is a medical syndrome.
In 1994 Leber, of the FDA, in a letter to me confessed no pathophysiology has
been delineated. At the 1998 consensus conference William Kerry concluded ADHD
appears to be a set of normal behaviors.
At the consensus conference James Swanson reviewed anatomic MRI research,
concluding ADHD subjects have on average 10 percent atrophy.
I challenged Dr. Swanson, saying why didn't you mention that virtually all of
the ADHD subjects were on stimulant therapy? The research had proven 14 times
over that the drugs, not the fictitious disease ADHD, had caused the brain
atrophy.
Caught in this lie, the consensus conference panel confessed, quote: We do not
have an independent valid test for ADHD. There are no data to indicate that ADHD
is a brain malfunction. Unlike real epidemics, once psychiatric diseases are
found not to exist, the epidemics flourish nonetheless.
In 2002 Castellanos published the one and only MRI study of an ADHD untreated
group but, inexplicably, they failed to use matched controls, voiding the study.
So, I would hope that this study is not referenced as the proof that ADHD is an
actual disease.
While the FDA's Goodman acknowledged that claims that SSRIs correct serotonin
and imbalance go too far, he had the gall to suggest, quote, this is reasonable
shorthand for expressing that this is a chemical or brain-based problem. Saying
any psychiatric diagnosis is a brain-based problem and that medications are
normalizing the function is an absolute lie.
There is nothing more despicable than a physician or physicians who knowingly
tell normal patients that they are diseased for profit...
REESE: One minute.
BAUGHMAN: ... yet, this has become standard practice throughout medicine and
FDA, APA, AMA, AACP, AAP, AANCNS, AAFP. The right to informed consent
universally abrogated must be restored. You are mandating the medical treatment
of ADHD. Where is the proof that ADHD is a disease?
Give us that reference, that citation right now, please. Give us the reference
citation to the test that demonstrates an objective abnormality child by child,
please.
REESE: Calling for speaker number four. HANSON: Good afternoon. My name is Ben
Hanson. I am from Traverse City, Michigan. In the interest of full disclosure, I
suppose I should mention a few things.
In March, 2000 I was appointed to the Michigan Department of Community Health
Recipient Rights Advisory Committee, a state watchdog panel that meets in
Lansing. I received no compensation for serving on this committee, other than
mileage for travel expenses.
Also, I am the Michigan contact person for Mind Freedom International, a
non-profit organization which advocates for the rights of individuals
stigmatized by psychiatric labels. This is a volunteer position for which I
receive no compensation.
I am also a proud member of the International Center for the Study of Psychiatry
and Psychology, icspp.org, and I was one of the principal organizers of
yesterday's ICSPP press conference here, in the Hilton.
It is possible I may be reimbursed for some of my travel expenses by ICSPP but
to date I have not received one dime of compensation from ICSPP, which is fine.
I am happy to do this work for free. Finally, I have been contracted on a
part-time basis by another non-profit organization, the Law Project for
Psychiatric Rights, psychrights.org, founded by Alaska's attorney Jim Godstein.
To date, I have received a total of not over $1000 for various services like
updating the mailing list, working on the web page, et cetera.
I want to make it clear that I am speaking on my own behalf today. I am not
speaking for anyone else, including these organizations I just mentioned. I am
here before you as a private citizen, a taxpayer of the U.S. I want to say a few
words about the drug Sparlon, also known as Provigil, also known as modafinil.
My interest in this drug began a few years ago when I learned that modafinil had
been approved for treatment of a new disease called shift work sleep disorder.
This interested me personally because for nine years, from 1995 through 2003, I
worked for the Michigan Department of Natural Resources as a ranger in a state
park located in northern Michigan.
I worked the night shift, from 7:00 p.m. until 4:00 a.m. five nights a week.
Basically, my job was to walk around in the woods after dark, which I loved
because I love the outdoors. It was a dream job except for those hours and I
never got used to it.
I can testify to the fatigue, to the irritability, to the general clumsiness and
inattentiveness which is caused by working those late night hours, especially
that last hour from 3:00 a.m. to 4:00 a.m.
The rangers call it the "dead hour," the dead of night when the whole world
except you seems to be asleep, nothing stirred, not even the crickets, not even
the mosquitoes.
I can testify to this mental dullness. In fact, I would say if you work those
hours and you don't grow a little groggy and a little clumsy, the only reason I
can think is that you are probably on some kind of drug. I believe consenting
adults should have the right to take any drug they wish but I condemn the FDA
for endorsing a fictitious disease, created most likely by some pharmaceutical
marketing department as a way to sell more drugs.
What is next, FDA? Are you going to approve jet lag as an official disease?
Perhaps it is only a coincidence but I understand the formulary patent on
modafinil expires this month, March, 2006 -- a minor inconvenience to Cephalon
and its stockholders.
But one way around that problem would be to change the name of the drug, call it
Sparlon and approve it for the treatment of ADHD, which is a larger market than
shift work sleep disorder anyway. Isn't that what Eli Lilly did when Prozac's
patent was about to expire? They changed the color of the pill from green to
pink.
They changed the name to Sarafem and they marketed it for another invented
disease, PMDD, and the FDA approved that. No problem.
I flew down here from Michigan...
REESE: One minute.
HANSON: ... because I couldn't believe -- I can't believe that you people are
really going to approve this pep pill, which reportedly allows people to get by
on two hours of sleep a night, for children diagnosed with ADHD. If you do this
I want to be here to see you do it with my own eyes. Thank you for this
opportunity to express my opinion.
GOODMAN: Thank you. At this point I would like to invite our committee members
to ask questions of both the FDA and the sponsor. At a time when I think it is
probably the appropriate moment we will put the questions up on the screen, but
before we do that let's have more free-ranging questions, including some that
may have been carried over during lunchtime.
I remember that a few people didn't get an opportunity to ask their questions.
REESE: Dr. Armenteros?
ARMENTEROS: Yes, a question to the sponsor pertaining to the most common side
effect in the list, which is insomnia, could you tell us a little bit more?
For example, does this start happening in the very beginning? Do kids get used
to it? Does it change during the time of treatment under observation? And, does
it have anything to do with dosing?
RUSSELL: In the main, the insomnia appears to start with treatment initiation,
and the highest incidence of first reports of insomnia occurred during the first
two weeks of treatment and then it does appear to taper off.
As Dr. Stankovic mentioned, I think we had seven withdrawals from the drug
because of insomnia. So, there appear to be people who either learn to get used
to the insomnia or habituate to it, as with many of the other drugs that I think
have this as a side effect.
I am sorry, I know there was a third part to the question but I have forgotten
it.
ARMENTEROS: Yes, what is the relationship to the dose?
RUSSELL: We did look at the doses and there doesn't appear to be a major
difference with the doses of 340 mg or 425 mg.
REESE: Dr. Mehta?
MEHTA: Actually, it is just a comment on Dr. Temple's earlier remark. All the
studies are two-week or longer. There is only one study in 24 subjects which is
a single dose.
So, the denominator should be somewhere around 920 or something like that.
GOODMAN: I have a question for the sponsor about the pharmacokinetics. If you
took two children, same age, and one was being administered 400 mg modafinil,
the other 200 mg modafinil obviously the plasma levels would be higher in the
one that is receiving the 400 mg, but would the levels of the metabolite be
proportionate or disproportionate to those levels as well? You may have covered
that and I may have missed it.
RUSSELL: Yes is the answer.
GOODMAN: They would be proportional?
RUSSELL: Yes.
GOODMAN: In a linear fashion?
RUSSELL: Yes.
GOODMAN: Thank you.
REESE: Dr. Leon?
LEON: Could the sponsor please show us a slide of the weekly retention rates? I
notice there is a big difference between the LOCF results and the endpoint and I
am curious to see how those retention rates look, and if there are differences.
I know maybe about 50 percent more people dropped out of placebo than active
medication.
RUSSELL: The biggest time of dropout was between weeks three and five. This
largely may have had something to do with the design of the protocol that did
allow patients who were going to come off for an adverse event to roll over into
the open-label program at that time.
The reason for that allowance was based on a lot of input from investigators who
found that it would be difficult to keep children on a placebo for that length
of time. So, there was a dropout between week three and week five.
LEON: Do you have a slide that shows the weekly retention rates? Could we see
that, please?
RUSSELL: I am looking at my colleagues and they don't seem to have it.
LEON: I didn't see it in the materials. Is it in the book maybe? It is pretty
important when we are trying to draw inferences about efficacy.
RUSSELL: I think in your briefing document there are by week numbers.
LEON: I didn't see it. Maybe you could tell us what pages to look on.
RUSSELL: Let me try and find the page. If you look at figure 4 on page 31 of the
briefing document, there are the numbers for the CGI that are actually the
numbers -- sorry, they are not; I am misleading you. I am afraid we don't have
it.
REESE: Dr. Wells?
WELLS: I have a question about the source of the postmarketing adverse events
that were reported, a question to the sponsor. These postmarketing events, do
these come from all of the postmarketing studies, all events from all studies?
Also, do they include voluntary reports from practitioners in a more
naturalistic setting?
RUSSELL: I am sorry, could you repeat the question?
WELLS: The question is about the source of the postmarketing reports of adverse
events. Where do these comes from? Presumably postmarketing studies are included
of the drug used in other indications. Would it also include voluntary reports
of practitioners...
RUSSELL: Yes, it would. The spontaneous reports would be reports from health
care providers, consumers. Any study that we undertake we include in our
clinical trials information.
WELLS: So, it is data from studies as well as voluntary reports from
practitioners?
RUSSELL: In the postmarketing it doesn't include the studies; it includes the
voluntary reports.
WELLS: Just the voluntary reports? RUSSELL: If I could clarify the previous
question, on figure 3 on page 29 of the briefing document there are numbers at
the bottom of each of the graphs.
REESE: Dr. Pine?
PINE: I guess two issues, and one of them I think maybe we will just come back
to. That is the issue that Dr. Leon just raised about the sample sizes for each
week on page 25 efficacy data.
I realize you don't have it now but, you know, I think a few of us are a little
concerned about differential attrition in terms of the efficacy data and it
would be very helpful to see those data but, again, I know that you don't have
that right now but maybe if you could get them and give them to us sometime in
the next half hour or so.
The second issue is a question on psychosis. I guess there are really two things
that -- yes, that slide, right there. If you could just give us the Ns in each
group at each data point.
RUSSELL: This is the ADHD rating scale. Actually, the numbers are here the
teachers versions so you can see that there are dropouts as the weeks go by.
PINE: Yes, they are very small.
RUSSELL: They are pretty small. I am afraid I can't see those from here.
PINE: You can barely make them out in the document but you can see them; they
are there.
But the issue of psychosis, there was an extensive discussion about this
yesterday, for people who weren't here and I don't know that we need to repeat
the whole discussion. I guess I would just like to raise two issues.
One is that I seem to recall on one of the slides from yesterday that there was
a hint -- and I can't remember which event it was, that one of the adverse
psychiatric events looked to be more prevalent in modafinil or Sparlon relative
to the other agents.
If somebody from the FDA could either point that out or bring it up, that would
be helpful. Then I have one other point about that.
GOODMAN: Which event was it?
Dr. Mosholder would know. Do you remember?
MOSHOLDER: Andy Mosholder, Office of Drug Safety at FDA. For the suicidal event
category there were four events in my analysis of modafinil, zero on placebo. I
wonder if that is the one. For psychosis there were two and none on placebo.
Those are just the double-blind. PINE: And I guess my take on it is that I don't
feel any differently looking at the data here for this compound than I felt
about the broader discussion yesterday, on the one hand.
On the other hand, I think it is important, particularly for people who weren't
here yesterday, to know that similar concerns that were raised in general for
other compounds should also be acknowledged or discussed here.
I guess the last thing to say is that the quality of the adverse event reports
in general always concerns me. But I guess on slide 102, case number 312592271
with 10 months of ideas of reference concerns me. I realize it is one case and I
don't think we should make too much out of it, on the one hand.
On the other hand, in terms of discussing the medication I do think that we need
to at least bring up the point again that there needs to be some acknowledgement
that these are potentially concerning adverse events.
GOODMAN: As long as you are on that subject, Dr. Pine, it reminds me that in the
review of the correspondence between the FDA and the sponsor there was a
description of one case that seemed to be misclassified or mis-coded.
It was an individual who was said to have had a personality change or
personality disorder and, in fact, they had a noose around their neck. Could
somebody from either the sponsor or the FDA side clarify?
Obviously, if you read a case like that it harkens back to early concerns we had
about previous problems in appropriate reporting of those kinds of AEs.
RUSSELL: Yes, I can comment on this case. This was a six year- old girl who
after two days of discontinuing the drug -- she stopped the drug on day 91 and
then on day 93 engaged in what her mother calls bizarre behavior but there was
some suicide intent by putting a rope around her neck.
The patient was hospitalized. The inpatient assessment says that the patient had
major separation anxiety and admitted to trying to hurt herself with grave
references to suicide. This was a girl who had a history of mood swings and a
family history including maternal depression and a suicide attempt.
So, that is that case which was originally thought by the investigator to be
abnormal behavior but, as you saw today, we included it on the slide with the
suicidal cases.
REESE: Dr. Bigby?
BIGBY: I have a question about response of the placebo group. You have a figure
that was in the CD that you sent and it was a summary slide for the three
studies looking at the ADHD rating scale school version for all three studies. I
think it went out to eight weeks, and it is really striking how much the placebo
curve drops down.
Also, if you can find and put that slide up -- I don't know if you have that
slide, it has the numbers of people still in the study at the various time
points.
So, I have two questions. The first one is for anybody who knows about ADHD
trials. Is this kind of effect in the placebo group sort of universally seen in
ADHD trials?
RUSSELL: Dr. Biederman?
BIEDERMAN: I am not sure whether I know what you are asking, but placebo
response in ADHD is on the order of magnitude of 30 percent on average in the
literature. You are asking if this placebo effect is typical of other studies of
ADHD.
It is pretty much within that range.
BIGBY: Then, the second question I think sort of goes back to the question about
numbers of dropouts. Now, at each of these time points you have listed the
number of patients in the treated and the control group. For the control group
you start out with 210 and by the time you get to the seventh week there are 71.
So, basically two-thirds have dropped out. Is the score with the bracket at each
one of those time points just the people still in the trial, in which case the
same would be true for the treatment group and it is sort of a per-protocol
trial and not an intent-to-treat trial.
RUSSELL: Depicted on these figures is the by week analysis so those are the
patients that are actually in the study at that particular time.
The endpoint is the last observation carried forward analysis so all values are
included in the endpoint analysis.
REESE: Dr. Wang?
WANG: Yes, I want to explore some more this differential in effect size between
modafinil and other ADHD treatments. Particularly, you mentioned Strattera. What
I am interested in is the clinical significance of that decrement.
Is this decrement of clinical significance? Is it of a size where it would
warrant making modafinil a second-line treatment? I think it will have some
bearing on how desirable we think it is to warn about the safety issues.
RUSSELL: The overall effect size across all three studies was 0.69.
WANG: I am talking about the differential between the effect size in your
pivotal trials and what is known about the effect sizes for other ADHD
treatments and what is the clinical significance of the difference. PINE: Can I
ask a question about that 0.69? That is a Cohen's D for the difference in active
versus placebo? Is that what that difference is?
RUSSELL: Dr. Kingsbury, can you comment?
PINE: You know, typically most people go by Cohen's D criteria so stimulants
have Cohen's D effect of somewhere in the low 1s, 1 to 1.2.
Strattera I think is frequently quoted as 0.7 to 0.8. So, if it is 0.7, if that
is a Cohen's D for the difference in the change of active that accounts for
placebo and that would be a reasonable effect size. But I would like to hear if
that really is the effect size they are quoting.
KINGSBURY: Specifically calculated as the difference in treatment effect divided
by the pooled estimate of the standard error.
PINE: The pool of the placebo?
KINGSBURY: The placebo.
PINE: So, that is a reasonable effect. It is not huge but it is within the realm
of an effective agent.
WANG: Would you say it is getting to the point where this would be a second-line
treatment?
PINE: I would not say that.
Clinically, based on an effect size of 0.69, I would not say that that would
make it a second-line agent necessarily. It is clearly less than what you would
expect in stimulants but I would think about it similarly as I would about
atamoxatine.
LAUGHREN: I think if you are going to be comparing effect sizes for different
drugs you ought to be looking at it in the same trial because it varies a lot
from trial to trial. It is going to depend on the sample size and on the placebo
response.
So, I think it is really hazardous to compare effect sizes, whatever measure you
are using, whether it is Cohen's D or anything else, to cross-study comparisons.
PINE: On the other hand, since we all know of multi-drug trials where people
obviously are grappling a little bit with the efficacy data I think we have to
say something about, you know, in the universe of studies of ADHD, is this in
the realm of a reasonable treatment or not. Again, I would agree; I wouldn't
quibble with what you said.
WANG: And I am not arguing. I am just trying to kind of qualitatively understand
whether if there is a warning, whatever shape or form it takes, and it drives
down use or effectively turns modafinil into a second-line treatment, is that a
terrible thing? Is it a good thing? Is it neutral? That is what I am trying to
kind of understand.
REESE: Dr. Rappley?
RAPPLEY: I want to go back to the skin issue so if anybody else wants to talk
about the effect -- keep going? OK.
I would like to ask Dr. Bigby if he might have some insight about how we might
think about the spontaneous reports of Stevens-Johnson syndrome and how that
compares to the actual incidence.
BIGBY: Actually, that is a very good question. Neil actually did a study in
Canada where he ascertained cases of TEN, and he can give you the details of the
study, and compared it to the spontaneous reporting system they have in Canada.
I think that it is vastly under-reported.
I looked at that paper last week and I think it was 10 percent or less than the
cases that he found that had actually been reported. I think the same is true
for other researchers that have looked at reporting of TEN vis-a-vis drug usage
in an attempt to try to determine rates of reactions.
SHEAR: That is correct. We tried to look at patients with TEN and contacted burn
units across the country to see patients who were coming in versus what was
actually reported to Health Canada through the spontaneous reporting system, and
we came up with a number of around 10 percent that were actually reported.
So, we realized it wasn't necessarily the burn doctors but probably hospital
pharmacists who were reporting it or other health care professionals but still
it was about a 10 percent reporting rate.
REESE: Dr. Pfeffer?
PFEFFER: Again a clarification, Dr. Bigby. Maybe you can help us. You said that
the Stevens-Johnson was dose related.
BIGBY: No, no.
PFEFFER: Then if you could clarify a little bit more about the onset of this
type of skin problem.
BIGBY: I mean, I think SJS and TEN are idiosyncratic hypersensitivity reactions.
I tend to shy away from talking about mechanism because I don't think anybody
really knows what the mechanism is.
Developing the disorder I think is not dose related but the point I was trying
to make about the dose perhaps being a factor is that I am aware of at least two
studies that have shown that the patient prognosis is better if the drug is
identified and stopped, and it has mostly to do with the half-life of the drug
and the body's ability to clear the drug.
I think that if you start with a greater concentration it will take you longer
to have undetectable levels and it might affect prognosis. I don't think it has
anything to do with the incidence.
PFEFFER: One other question about the syndrome, if a child develops this on a
medication such as modafinil, would that child be at increased risk in the
future for the syndrome?
In other words, would the exposure to this particular drug increase the risk or
would that not be an issue?
BIGBY: Increase the risk if they were exposed to any drug?
PFEFFER: Either any drug or whatever causes the syndrome, yes. Does it lead to
sensitization?
BIGBY: Well, the only definite thing that i can tell you is that if they got the
same drug again it might be that they would have the same reaction.
Whether it identifies them as someone who is more likely than the general
population to do develop TEN to other drugs, particularly drugs that are known
to be associated with TEN, I can't answer that question although there is some
suggestion, not entirely convincing, that that might be the case.
But it is not clear to me that the exposure to the drug and the fact that they
developed the TEN as the cause of that identifies them as someone who has that
potential.
So, I don't know if I am answering your question.
I think that a patient that develops TEN to a drug -- there is some evidence
that they are more likely to develop that type of reaction to drugs.
But I think probably they were that way before the exposure.
Actually, again, this is a subject that Neil has done more work on than anyone I
know. I mean, I think it would be useful for you to hear his comment on it as
well.
SHEAR: Thanks, Michael. It is a difficult question because you are not going to
get enough data ever to really do that, especially if a child has had TEN.
For every drug they get in the future the parents ask can this drug cause TEN,
it is no longer a hypothetical possibility and if the answer is yes, but don't
worry that couldn't possibly happen in a billion years, you know they are not
going to get the drug. So, you are not going to collect that data.
What we did show was that among the aromatic anticonvulsants there was a risk of
cross-reactivity and that is even hard to explain structurally. We don't know
why that is but we showed in vitro and in vivo that it does seem to exist. But
otherwise, usually people who have had Stevens-Johnson don't get it again.
REESE: Dr. Malone? MALONE: I know you said that dose probably was not related to
Stevens-Johnson but I guess it is a similar question, is there any mechanism
that will explain why a group of children getting 340 mg of the drug might have
a higher rate of Stevens-Johnson than those being treated for daytime sleepiness
getting 200 mg or less?
BIGBY: The only thing I can do is repeat I don't think the development of TEN,
as far as anyone knows, is a dose-dependent phenomenon.
GOODMAN: I think you are being appropriately cautious but there is the other
factor we discussed of the sulfone metabolite.
Although there is no proven relationship, there is certainly a suggestion based
upon other compounds that have been associated with Stevens-Johnson that have
that sulfone group.
So, is it at least conceivable or plausible that the higher levels of that
metabolite could pose a greater risk for development of Stevens-Johnson
syndrome?
BIGBY: Is it conceivable? Yes. But, I mean, I think the threshold for whatever
it is that is the mechanism for developing TEN is exceeded by all of the doses
that you are talking about here.
I mean, yes, what you said is hypothetically true. The problem is I don't have
any evidence to say that it is or isn't.
VAUGHT: Mr. Chairman, if I could address that for you, please?
REESE: You may.
VAUGHT: Thank you. What I would like to do is just perhaps orient the panel a
bit.
Because of the inference of the sulfone to agents that have been directly
associated with the occurrence of SJS -- I am not going to do a chemistry
lecture today but on the right-hand side of the slide is the modafinil sulfone.
With the structural characteristics there is, in fact, a similarity across two
agents that have been directly related to SJS. Obviously with the sulfa drugs
and the aryl-sulfonamide valdecoxib, the only similarity is the sulfone group.
I think what you will notice is -- and I agree with Dr. Bigby that while the
mechanism is not well-known, in general with the sulfa drugs the amine group
becomes activated and it is believed to be one part of the overall syndrome that
is created, as well as the fact of the close association of the sulfone group to
the aromatic ring.
Valdecoxib is similar to this in that it has a sulfonamide group again
associated with the phenyl group. While this is not a conclusive relationship,
there seems to be a very broad preponderance of this type of structural feature
being associated and directly related to SJS. We can see that with the modafinil
sulfone moiety this is structurally simply not similar to these agents.
MANNHEIM: We have a similar slide I would like to show.
CAVANAUGH: We also looked and I have to say I am very impressed with the level
of discussion today from everybody. When Dr. Mannheim asked me about
Stevens-Johnson and I heard that there was a sulfone, I said, well, you know,
sulfonamide, as you know, is classically thought of and it is in the labeling.
Sulfonamides in general are labeled as 0.1 to less than 1 percent. You can again
see the sulfone here with the amine, and that is the sulfonamide; this is
sulfanilamide and you can see it here and, again, sulfamethoxazole.
As you pointed out, there is some similarity with the sulfone but the amine is
separated by two carbons and there is also a ketone here. If you look at
sulfacetamide, and here you see a 3D structure rendering so you can see it a
little clearer with the two oxygens, two carbons separated, a third oxygen and
then the nitrogen which is going to be withdrawing electrons.
If you look at sulfacetamide, the difference is that instead of the nitrogen
being on this side, it is basically substituting for this carbon.
So, this is a sulfonamide but it has a third oxygen, it is a third atom away.
The interesting thing about sulfacetamide is that it has been reported to cause
Stevens-Johnson, at least in the labeling, at 3 percent -- I believe it is in
the labeling; it might be in other places -- and that is an eye drop.
You know, people have died with even the first dose of eye drop where they have
a history of sensitivities to sulfonamide.
So, you know, this whole issue of is it the sulfone, isn't it, I think what you
have been hearing is that it is very, very muddy. We don't know. You have heard
factual information and we don't know. The same with the dose. It is too small
numbers. We don't know. It is plausible.
Is there cross-reactivity? Maybe yes, maybe no; we don't know. So, these are
some of the issues that we have been struggling with and I am glad the committee
is dealing with them.
Let's see, was there any other point I wanted to make? The only thing that I
wanted to point out is, you know, we have been talking about Stevens-Johnson and
there has been talk about other hypersensitivity reactions, and I went through
the various cases of rash and you heard earlier about the PK and the exposures
not being any different, and that is about what you would expect. But a lot of
those rashes also were just general rashes.
When you look at cases that could be possible hypersensitivity, you have several
cases of allergic reactions. You have the vesiculobullous possible SJS. You have
increased LFTs. One of them was a hypersensitivity. You don't have anything up
here in the teens but it also could be due to the numbers.
But in general the percentage for possible hypersensitivity is kind of
consistent.
These are the individual cases and you can see the combination of symptoms. Here
is an allergic reaction. Here is an allergic reaction with nothing else.
Here is an allergic reaction with a rash. Here is the increased LFTs with eczema
and that is the individual -- oh, I am sorry, here is the increased LFTs with
edema and urticaria and that is the individual who was 17-fold higher.
You also have hives, fever, whatever. So, there is some evidence of additional
hypersensitivity. We are just arguing about numbers at this point in time.
GOODMAN: That is helpful. Thank you very much. I have a more global question for
anybody on the FDA side about the safety data. Is the FDA in general satisfied
that there is sufficient long-term safety data at the doses being used for the
pediatric population?
We have focused a lot on the acute trials, individual areas of concern, but just
in terms of a kind of more panoramic view do we have sufficient long-term safety
data at this point for this dose in this population?
LAUGHREN: I think I remember from the earlier slide that we now have about 240
patients greater than six months. Is that right? That is about as much as we
usually have.
Again, this is not a new compound. If there were some adverse event that we
thought was related that had a long latency we might be more worried about it. I
think the event that we are most concerned about here is one that probably has a
short latency.
GOODMAN: That satisfies me. I would like to turn to the questions, if we could
have those projected. There are two questions for which we must take a vote.
The first question is has modafinil been shown to be effective for the treatment
of ADHD in children and adolescents?
Number two, has modafinil been shown to be acceptably safe in the treatment of
attention deficit hyperactivity disorder in children and adolescents?
When we get to number two I would like to break that down in the following way,
starting first with dermatological issues because those have been the most
salient features; then with cardiac, growth and psychiatric. Let's begin with
the first question pertaining to efficacy.
I think I already shared my view earlier and that has not changed, that I am
satisfied that there is sufficient efficacy data as we have heard.
You know, we don't have a direct head-to-head comparison with an active
comparator. That is unfortunate but it is not an atypical situation.
When we have looked at the effect sizes, I think most of the experts in the room
said it is probably not quite at the level of the stimulants. It is probably
closer to the range of Strattera, yet it is still quite effective and has
certain features that I think would make it a valuable addition to the
armamentarium.
I just shared my opinion but I want us to have a discussion and hear from around
the room, from all of you, regarding the efficacy question. Anybody can
volunteer.
REESE: Dr. Wang?
WANG: I would just second that one caveat about the comparative efficacy. I
think it would be useful to have additional data just to understand where in the
armamentarium this would fall. That is number one.
Number two, another big area of a question mark is the dose. I think it is
unfortunate and it would be helpful if there were more data to suggest whether
you have fathomed the lower bound of the dosing range because, as Dr. Bigby
said, maybe the development of these skin rashes isn't necessarily dose
dependent but the prognosis may be dose related.
So, getting kids on the smallest dose possible would be optimal. I don't know if
this is additional trials but some way to understand if a lower dose might be
useful.
REESE: Dr. Pfeffer?
PFEFFER: I share that idea and concern and I asked the question previously. It
seems that trial 309 was a fixed dose and is the dose that was proposed, which
was the higher doses.
Trial 311 was a flexible dose and it looked to me, in slide 53, that there was
demonstrated efficacy early on and I am assuming it is at a lower dose.
Then, on slide 54, while it was a flexible dose we heard that it was a very
rapid increase of dose early on. So, there wasn't enough sense in that trial if
a lower dose might also have been effective.
So, while I think there is definitely demonstration of efficacy, the efficacy is
demonstrated on the high dose and the question about would a lower dose serve
the purpose is not answered clearly.
REESE: Dr. Temple?
TEMPLE: Well, I think it would be helpful if, maybe with another look, you took
a look at the Phase 2 study that led to the conclusion that you need the high
dose, number one. I mean, we press people for dose-response data all the time
but apparently we were satisfied that that had ruled out usefulness of lower
doses.
The other thing to do is look at the average dose or maybe even dose groups in
the titration studies to see whether, while the dose is still quite low, there
is some separation.
I mean, that wasn't the planned analysis but the company may have that. Early on
there is not much separation so at least for the earliest part of the titration
you really don't see much. Then at either three weeks, four weeks, five weeks
you do, but we don't know the doses or the average doses or the subsets of
dosing by that time.
So, perhaps one could look at that and see if we have an answer already.
REESE: Dr. Armenteros?
ARMENTEROS: That is fine, but it could also be an artifact of the time lag
between administration of the drug and response.
TEMPLE: I totally agree. If you didn't see something you wouldn't really know
whether a lower dose might -- but it was the Phase 2 study that I think is what
convinced the Division that the dose-finding was sufficient. So, I think if you
don't think that is adequate we need to know why.
REESE: Dr. Pine?
PINE: I guess just briefly to second some of the statements, it looks at least
to me fairly clear that there are not a lot of questions about efficacy. It
sounds like the data have been reviewed a few times.
Just in looking at the three studies, on the face of it there can be a
reasonably strong case made for efficacy here, and I don't know that I have a
big need to discuss it much further although I would be happy to hear other
people's thoughts.
REESE: Dr. Rappley?
RAPPLEY: Speaking from the point of view of a clinician, I would say that this
is a medication that looks to be somewhat less effective than the other options
available to me to treat attention deficit hyperactivity disorder, and it has
the common side effects, common and mild side effects that are very similar to
the other agents.
So, it would probably be perhaps a fourth or even a fifth line of medication
that I might turn to in order to treat a child who was not responding to the
other medications.
GOODMAN: I wondered if you would revise that positioning of the medication if
you had a sense of abuse potential, diversion potential. We can talk about that
a little bit more today, but I have heard a variety of different views on this.
It would appear that the abuse potential is less than with some of the
stimulants but it is certainly true we often don't find out about abuse
potential until a medication becomes widely available in a particular
population.
So, I was just wondering if you might revise that if you felt that the abuse or
diversion potential was less.
RAPPLEY: Well, I would like to answer that in two ways. One is that we have
heard that one reason a physician might want to use this is so that the
physician would not have to deal with controlled substances. I don't like that
argument.
That is not about what is best for my patient in terms of their condition and
their treatment. That is about a system that makes it difficult for me to
deliver care effectively.
So, I would rather educate my families that this is not a narcotic and it is
controlled for some legitimate reasons and it is the best set of medications I
can use and, therefore, I will work with that. So, I don't see that as
persuasive.
The other suggestion that it would be less likely to be abused as an agent
itself, I think that might be attractive to me if, in fact, I was looking at a
family where I thought abuse by other family members or my patient was possible,
which is not an unusual case for my practice.
But I have other agents in the classification of stimulants that I could turn to
for that purpose.
GOODMAN: Other comments on the issue of efficacy before we take a formal vote?
Dr. Temple?
TEMPLE: I am actually embarrassed to have to ask this, but outside of maybe
psychiatry this Cohen's D is not widely used. Could somebody dilate on that a
little bit? To divide effect size by some kind of measure of variance seems to
give you something that doesn't have tangibility.
PINE: It is not dividing the effect size. Maybe Andy can talk more about this.
It is dividing the mean. So, it is a difference in means divided by pooled
standard deviation.
It kind of goes back to the in the social sciences, in a widely cited book in
the mid '80s, about statistical power for that particular metric, which was the
difference in means divided by the pooled standard deviation in the two groups.
Standards were kind of put forth that were somewhat arbitrary at the time, in
the mid '80s, for a small, medium and large effect. And, there are standard
deviation units so up to 0.3 was a small difference; from 0.3 to 0.8 was medium;
and above 0.8 was large. Then, what has happened over the last 15 years,
particularly among pediatric psychopharmacologists but also adult
psychopharmacologists, is that those standards have been applied and they tend
to fit in terms of how people think about medications clinically.
Typically, medications that physicians tend to think about as powerful tend to
have large standardized differences or a difference in standard deviation of
approximately one unit between an active treatment and an inactive treatment.
Similarly, medium treatments tend to follow in the 0.5 to the 0.8 range.
TEMPLE: It sounds, for example, like making your study larger makes your effect
size look bigger.
PINE: No, it will not.
TEMPLE: Won't decrease the standard deviation?
PINE: No, it will not do that. In fact, one of the nice things about the Cohen's
D is that it is independent of sample size.
TEMPLE: We will talk off-line.
GOODMAN: Other comments before we call the vote?
(NO RESPONSE)
In that case, we are voting on the first question on efficacy. We have three
options, yes, no or abstain. Let's start with Dr. Mehta.
Although officially his vote doesn't count, in my mind his non- vote is
extremely persuasive.
MEHTA: On this drug it is not an issue but I think it is a pleasure not to be
able to vote on most of the drugs! I think there is clear and persistent
evidence of efficacy so efficacy-wise I don't think I have an issue.
MALONE: I don't have any issue with efficacy either. I think that all the
studies were positive and overall it looks effective.
REESE: Ms. Dokken?
DOKKEN: Yes on efficacy.
REESE: Could you say your name before you give your vote? Thanks.
WELLS: Barbara Wells, yes.
ARMENTEROS: Dr. Armenteros, yes.
PFEFFER: Dr. Cynthia Pfeffer, yes.
ROBINSON: Delbert Robinson, yes.
LEON: Andrew Leon, yes.
PINE: Danny Pine, yes.
GOODMAN: Wayne Goodman, yes.
BRONSTEIN: Jean Bronstein, yes.
WANG: Phil Wang, yes with those two caveats earlier.
RAPPLEY: Marsha Rappley, yes.
BIGBY: Michael Bigby, and if you really want my opinion about the efficacy of a
psychiatric drug, yes.
(LAUGHTER)
GOODMAN: Do you want to recap for us Cicely?
REESE: Well, "the yes" have it. It is unanimous.
GOODMAN: Let's turn to question number two, which is a bit more thorny...
BIGBY: Could I ask a question?
GOODMAN: Who has a question?
BIGBY: Me. Is there a definition for acceptably safe?
GOODMAN: It is the same that you would use in dermatology!
(LAUGHTER)
REESE: Dr. Temple?
TEMPLE: Well, this goes back to the law and various elaborations of it. What the
law asks is that safety be assessed by all tests reasonably applicable -- a very
broad standard that you could drive any sort of truck through; and that it show
the drug to be safe for its effective use, which has generally been interpreted
to mean that the benefits appear to outweigh the risks.
But it goes on to make it clear that something can be unacceptable either
because it shows something bad or because you haven't done enough. We have
elaborated on that in various risk management things but it is always the same
-- have you done what you need to do or enough of what you need to do?
A judgment call obviously. And, can you conclude that in light of what it does
that is good for you, you have acceptable risk? That is what it always means.
GOODMAN: As we return to this question, I would like to break it down to
different categories. Let's start with the dermatological issues first.
I wonder if I could turn to you, Dr. Bigby, to offer your opinion on whether you
think this drug is reasonably safe in this population, given what we have heard
today about possible dermatological complications?
BIGBY: I think that the drug should be put in the context of other currently
available, marketed and highly used drugs where over time it has become clear
that they are associated with the development of severe adverse skin reactions,
such as TEN and SJS, and I think that this drug will find itself among that
group.
PINE: Can I ask you a question about that? I actually found, and I don't know
what the number of the slide is from Dr. Andreason -- I found the slide that
gives the labeling of Lamictal interesting and relevant and I wondered if you
might comment on that.
For Lamictal it says Stevens-Johnson syndrome -- it gives 8/1000, that is what
it gives in children. It is page 8, on the bottom. Because I do think your
comment about placing it in the context of other medications is very helpful and
lamotrigine is a medication that there is some familiarity with and I wondered
if you might comment on the comparison.
It has a black box below age 15, lamotrigine. Is that right? I think that is
right. That is my recollection, anyway.
BIGBY: You know, the problem that I think you are going to have is that you are
going to have a difficult time coming up with and agreeing on a number, but I do
think that the drug should be labeled as one where people should be aware that
it could be associated with SJS/TEN.
Actually, I am quite surprised at the 8/1000 number because you are pretty close
to one percent. You know, that is a pretty high rate for TEN. So, I don't know,
I mean, I have a hard time believing that the number is really that high. Is it
really that high?
PINE: I don't know. I am just looking at what Dr. Andreason...
GOODMAN: The numbers have come down over time. Is that correct?
ANDREASON: Well, it is hard to say.
If you look at the prospective registry study that was done, there was one death
of Stevens-Johnson syndrome in that prospective registry with 1983.
So, the idea that it is more common in children than in adults is fairly well
accepted. I think that the numbers are reasonable from what we know.
I think they are reasonable estimates.
GOODMAN: It was placed in a black box and even though over time it would appear
that the incidence is lower for lamotrigine it has maintained its black box
position. Is that correct?
ANDREASON: I am not aware that the numbers have actually been documented to come
down.
TEMPLE: But if you had one death in a thousand people you wouldn't remove the
black box.
That is an impressive number for most drugs.
GOODMAN: Dr. Bigby, I have a follow-up question too. I agree with your position
but I just want to clarify the basis of it.
It seems like it is largely on one case, one case in which you have fair degree
of suspicion or confidence that there is a bona fide case of Stevens-Johnson
syndrome and, given the denominator, that was enough for you to be concerned. Is
that fair?
BIGBY: Yes.
GOODMAN: And there was some exanthem as well.
BIGBY: That is fair. I mean, that is a fair statement of my position.
GOODMAN: Let me just follow up then.
There is this disconnect that we have all talked about -- the real concern here
is the extrapolation to large numbers and there is the disconnect with the
postmarketing surveillance. But it would seem to me that that could in part be
explained by dosing.
I think I understand that dosing may not determine the incidence but it may have
played a role in the persistence of the problem.
So, we don't know whether the sulfone metabolite is relevant or not,
nevertheless, we don't have a lot of postmarketing data in that age range at
that dose and that could, indeed, explain the lower than expected rate in that
population, in my mind at least.
I just want to see others' reflection on that position.
BIGBY: Can I just make a comment?
You know, I have been involved in quite a few of these discussions about
incidence of side effects postmarketing, and one of the things that is really
striking about postmarketing studies is that unless they are very rigorous they
don't detect much.
So, when you are relying on spontaneous reports I think that you are going to
miss a lot of the cases that were, in fact, cases and it is striking how poor,
in terms of pickup of adverse reactions, postmarketing studies are unless they
are really done with some sort of design in mind.
TEMPLE: Obviously a problem is that nobody can answer the question of what the
degree of under-reporting is and it is estimated widely.
However, there is a lot of reason to think it is less bad when events occur that
are likely to be drug related. So, for example, we have been pretty good at
picking up acute hepatic necrosis in cases like that because when that happens
the drug is highly suspect.
When we approved a drug that was a major 3A4 inhibitor we got cases of
rhabdommyolysis because it inhibited the metabolism of a couple of statins. We
get cases very rapidly.
Now, I don't know whether we got them all but these kinds of things you probably
do better than things that happen regularly in the background -- seizures,
things like that -- where why would a person decide that the drug did it.
So, it is not that discouraging for things that are obvious and that deepens the
mystery to me because, you know, the fact that the dose is about half what you
would recommend now, that doesn't make it seem like there shouldn't be any
cases.
I mean, that is why it is here, because we find it a little surprising that
there are no cases and yet there was one.
CAVANAUGH: In terms of your question, Dr. Andreason showed a slide where he
estimated about 11,000 children 6-12 years old who were probably getting
modafinil from the postmarketing experience. If you take that 1/900, that is
just about 0.1 percent. So, if you take 0.1 percent of 11,000, that would be
about 10 cases.
Now, it is commonly quoted that reporting rates are about 10 percent. That is
based upon drugs where they may have been on the market a while but, all of a
sudden, somebody publishes an article with a case-control series and then
everybody else starts reporting it.
In that case, after people are, you know, kind of all reporting cases, that is
where you get the 10 percent. You know, if you even took 10 percent of 11 cases
or 10 cases you might expect one case to be reported.
Now, yesterday you heard that psychosis and aggression was about one percent
consistently with the various drugs used for ADHD. Back in June, we also
discussed this with Concerta specifically and you have about 1.25 million kids
on Concerta and we know now that it is about one percent in terms of psychosis.
Yet, you were dealing six months ago -- say, one percent out of 1.25 million is
1250 and yet you were only dealing with -- I can't remember the number but maybe
30 cases. So, it was less than one-half of one percent that was the reporting
rate.
BRONSTEIN: My question is to the FDA.
What kind of requirement does manufacture of Lamictal have for postmarketing
studies and reporting of incidence?
ANDREASON: I am not sure what the requirements are. Right now, they have already
completed the registry study. That is in labeling.
There is already a black box. I think that the risk has been capped. I am not
sure exactly what more one would want. It is also noted in the black box that it
is only approved in children for Lennox Gasteau even though it is approved for
other things in adults. I think that is about all we could expect.
BRONSTEIN: Thank you.
REESE: Dr. Laughren?
LAUGHREN: I want to come back to the point that Dr. Cavanaugh was making. I
think there is a real problem in knowing what the extent of under-reporting is
and it probably varies so much depending on what the event is.
With something like psychosis, especially depending on how you define it and if
you are defining it just as hallucinations, a lot of those probably aren't going
to get reported because it is a fairly common event in the background.
Something like Stevens-Johnson, which is an extremely unusual event, a very
alarming event, is probably much more likely to get reported.
But the truth is we don't know what the extent of under-reporting is so you have
to factor that into this. It is hard to know what it means that you don't have
any reports among roughly 35,000 kids who have been exposed to it postmarketing
but it is a disconnect and you just have to figure that in, in your overall
deliberations on this matter.
REESE: Dr. Mehta?
MEHTA: I think it is just a comment to Dr. Cavanaugh too, essentially
reiterating what Dr. Laughren said. I can't believe that 90 percent of the
Stevens-Johnson syndrome which occurs in patients, either in Europe or in this
country, is not reported.
ANDREASON: Also, those numbers on exposure are unique patients between the years
2002 and 2005 only in the United States.
REESE: Dr. Temple?
TEMPLE: This is right at the heart of all this. If you really believe the one
case is likely to be drug related you are talking about a rate with a point
estimate of something like 1/1000 and a lower bound that is a lot worse than
that.
That is one problem.
One question is how reassured to be by the fact that the pediatric use in the
outpatient setting hasn't produced any, and I guess if you follow what Dr.
Cavanaugh said you shouldn't take any reassurance from that at all because
people report so poorly.
My own view is that I take a little bit of reassurance but it is very hard to
know. But that is what is at the nub of this.
Just to make it obvious in case it isn't from the questions, the things you can
do is try to manage that risk, taking some estimate of it, or ask for more data.
That is the question. That is what question two is about.
PINE: I guess thinking out loud a little bit, and in many ways my comments are
similar to what Dr. Temple just said, I think if you listen to anybody who knows
about dermatologic issues and who has talked about it today there is clearly a
concern among everybody I think -- you know, the sponsor's dermatologist was
concerned; Dr. Bigby is clearly concerned.
I guess the thing I am struggling with is, you know, what is the level of
concern. I think the other thing we would say, and I think everybody would agree
with this and Dr. Bigby himself said this, that we really do not have enough
data clearly to specify what the level of concern would be because there is this
one case out of 923 but, when pushed, I totally agree with what you said, that
you haven't examined the patient.
So, I guess what it brings things down to and it makes me somewhat uncomfortable
is that there is a lot of judgment call going on here for a potentially
incredibly important decision.
I just feel somewhat uneasy with that because, you know, you miss it either way
and you could screw up big time. I don't know if that says we need to get more
data. I don't know what that says but it just seems to me that we are stuck in a
way.
GOODMAN: Let me take it from there.
So, I think the real question I would like to discuss now about this issue among
the committee is whether it warrants a black box for that concern about
Stevens-Johnson syndrome.
I think that is really what you are alluding to there, Danny. We have efficacy.
We have agreed upon that. We have already voted it. We have concerns about
Stevens-Johnson but we have only one case that we can really hang our hat on. We
don't have the postmarketing yet.
It might be appropriate use for a black box given that it is something that will
alert the prescriber and the patient to recognize it early. I think it is that
early recognition that could make a difference in terms of outcome.
I am not emphatic about it. I think that there might be other ways of addressing
the warning without it being put in a black box because we have so little data
at this point. Perhaps the highlighting would be a step below that. There is no
question I think at this point that it should be included among the warnings.
So, it is really a matter of does it wind up in a box or is it highlighted.
Those are probably the two choices in my mind.
Dr. Temple, help us. TEMPLE: Well, I would say, not to try to preempt the
discussion, it at least gets a black box.
PINE: Why do you say that?
TEMPLE: That is the least because the only data we have says the rate is
something like 1/1000. It is life-threatening. Everybody has to know about this
and we don't know the rate. It could be 1/300; it could be worse.
I have discussed this with Tom and I am virtually certain that would be what we
would do.
There are two other things to do though that you need to think about and address
for us.
One is whether it should be in some form or another recommended as not
first-line therapy or think about other things first. There are various levels
of subtlety in how to do it.
We also are going to ask you whether we should ask for more data before we say
yes. But maybe you think we are just wacky about the black box. That is all
right, feel free to tell us.
GOODMAN: Dr. Wang?
WANG: I think there are several lines of argument that all point towards at
least a black box. I mean, Lamictal sets the standard. If you are willing to put
a black box for one Stevens-Johnson death out of 2000, here our best estimate is
about 1/1000.
The fact that, you know, with Lamictal the case was a fatal one doesn't really
hold much weight. I mean, there are black box warnings for suicidality even
though none of the cases were fatal. So, the fact that this one case didn't die
is just fortunate I think.
GOODMAN: I am sorry to interrupt, but the big difference there is we also didn't
have efficacy, or at least very much efficacy.
WANG: Granted. I think this whole issue of should this, on efficacy grounds, be
a second-line treatment again pushes you. There appears to be less of a downside
in putting something like a black box because if that de facto has the effect of
causing it to be used second after failing a stimulant, then maybe that is, on
efficacy grounds, also justified.
TEMPLE: I have to say we would be very uncomfortable without a direct comparison
asserting -- I mean, even though everybody loves this measurement and
everything, we would be very uncomfortable asserting that it is second line
because it is not as good, without direct comparisons.
You can come back and say why don't you ask for direct comparisons all the time.
That is another story.
REESE: Dr. Rappley? RAPPLEY: Have we rendered an opinion about whether or not
this is acceptably safe? I think in some ways we have taken a jump here and
talked about what kind of labeling.
Also, something you said made me think the black box label, or whatever warning
is on the label is not related to efficacy and that is not a risk-benefit
judgment. That is just a statement of risk. Am I correct?
PINE: The way it was discussed yesterday, and it would be nice to hear that
again, in what makes a black box it was a risk-benefit consideration and
efficacy does go into the consideration, at least the way it was discussed
yesterday.
RAPPLEY: So, approval for use in children I see as weighed risk and benefit.
TEMPLE: The decision to include a box has something to do with what the drug is
for. If there were only one treatment for this and it was considered urgent to
treat it, I don't know whether you would put a black box in. We don't box most
anti-cancer drugs, but they are all lethal in one degree or another, because
that is an expected part of the deal.
So, what it is for and what it does has at least something to do with it. So,
there are several other classes of drugs that work; you have choices; and here
is one particular liability.
But feel free to tell me I am all wet.
GOODMAN: Let me stay with Dr. Rappley's comment. I didn't mean to short-circuit
the discussion. I was offering my opinion but you are welcome to express the
opinion if you feel, based upon the dermatological issues, it is not reasonably
safe.
RAPPLEY: The way I am thinking about this is I understand that there is a
particular metabolism of this medication in children and we have one case of
Stevens-Johnson, perhaps 1/1000.
We have plausibility that this medication can be linked to this serious
condition.
My understanding of under-reporting is that it is significantly under-reported
and it is more likely to be common and I am reflecting comments from Dr. Bigby
that we will find it associated in the future, and my faith in postmarketing
studies is somewhat small.
So, given those things, I think that children are at risk for serious side
effects with this medication and, if you ask me to do the cost benefit analysis,
I think it is not adequately balanced by what we have to offer in bringing this
to treatment of children for ADHD.
GOODMAN: I would like to hear if others would share that point of view.
REESE: Dr. Malone? MALONE: I think I partly share that point of view. I don't
think it is safe enough to recommend it as a first-line treatment, especially
when we have a number of effective, well-known first-line treatments -- with the
data that we have right now.
It may turn out that this isn't going to be an issue but I think with the data
that we have now it is hard to recommend as a first-line treatment something
that could have such a dangerous side effect.
REESE: Dr. Laughren?
LAUGHREN: I just want to come back to a point that Dr. Temple was making earlier
about what acceptably safe means. Part of what is inherent in that concept is
having enough information to make a judgment about safety so I really want to
make sure that you consider the full range of options.
You might, looking at what you have, decide that you don't have enough
information to make a judgment about safety but if you are going down that path,
then tell us what more information you would like to see. But I just want to
make sure you consider the full range of options other than, you know, black
boxes and whatever.
REESE: Dr. Bigby and then Dr. Robinson.
BIGBY: I actually enjoyed the comment at the end of the table here because I
don't know if you figured this out but I like to try to make things simple. You
know, thinking about it that way does actually make it simpler.
The statement about we don't have enough information to say that it is safe, I
would actually say it the other way and that is that we have reason to worry but
we don't actually have enough data to say it is not safe.
REESE: Dr. Leon?
LEON: Well, I am concerned about a couple of comments I have heard in the last
10 or 15 minutes. Dr. Pine said right now it is just a judgment. Without putting
words in his mouth, I think we are basing this without enough data.
Dr. Bigby is predicting that once this is used widely we will see more
Stevens-Johnson; Dr. Temple is saying we need more data and suggesting we should
look at more data. I don't feel comfortable saying it is safe until we have more
data.
There is at least one ongoing study. When are those results going to be in?
There are 303 children, if I am correct, being followed right now. It is
certainly worth waiting for them, and that is still a very small number.
BIGBY: But those children aren't going to help you with the issue that you have.
LEON: That is a good point, yes. But in my opinion we just have inadequate data.
In the first 1000 there was a case. Is the next 1000 going to have 20 cases or
zero cases? I don't think we can guess yet.
REESE: Dr. Robinson?
ROBINSON: Actually, it is interesting, what Andy is saying. I guess my question
is, OK, we have 1/1000, how many more kids do we have to do to where we really
say the estimate really changed dramatically, either going down or going up,
that would be clinically meaningful either down or up?
Are we talking about having another 1000 kids? Another 10,000 kids?
Because we are dealing with what seems to be a rare event with all drugs. So,
that is the question.
It is always good to say we would like more data but is that in the actual realm
of doability?
LAUGHREN: Actually, you can figure out how many patients you need to follow to
cap the risk at whatever level you want to be comfortable with. We have this
rule of 3 which, you know, estimates the upper bound of the confidence interval
for the finding of no cases.
For example, if you wanted to be comfortable with a level of 1/1000 you would
have to follow 3000 for whatever period of time was of interest. If you found no
cases, that would cap the risk at 1/1000.
So, you can use that method to calculate how many patients you would have to
look at, at the doses of interest and for the time period of interest, with the
finding of no events that would cap the risk.
Now, if you wanted to cap the risk at somewhere near the background rate, that
is not a doable experiment but you could at least figure out, say, with 3000
that the risk is no greater than 1/1000 if you found no cases.
REESE: Dr. Pine?
PINE: I guess two things. I want to bring up one point that we haven't spent
much time talking about, and that is kind of the need for more treatments in
ADHD.
You know, the important thing to remember is, yes, clearly stimulants are
effective. No question, and they are good treatments and there are other
treatments around.
Again, no question. But even when medications are effective the amount of
improvement that you get even when treatments work well is often not necessarily
what you want, and there are not nearly enough treatments available for kids
with ADHD. You know, I think it is hard to say where this is going to fit in and
I would totally second what Dr. Temple said, you know, to base a decision on
limited use on efficacy would not be a good thing to do because it is a yes/no
question.
The medication clearly works. And, I am uneasy about withholding treatment that
could be potentially efficacious given the availability of treatments, such as
they are, for ADHD.
So, that is the first thing. I don't think we have spent enough time recognizing
that fact, that there are clearly needs for other treatments. Number one.
Number two, thinking about that on the one hand, with capping the risk on the
other hand, just personally, off the top of my head, I would be much more
comfortable if we could cap the risk at 1/1000.
I would feel much more comfortable about making a statement or decision or
conclusion about whatever the word -- what is the word, relatively safe? --
acceptably safe.
If I knew that a good estimate of the risk was 1/1000 I would feel a lot better.
If you are saying that 3000 cases treated for two weeks openly and we see no
cases would answer that question, I would feel a heck of a lot better.
TEMPLE: That is our rule of 3, and I am sure Dr. Leon can explain why it is not
quite right but it has been considered close enough.
Just another way to look at this, suppose you thought that the risk could be as
great as 1/500 -- I mean, the data we have now has a confidence interval and it
probably goes down to 1/300 or something like that, where would you be
comfortable? You just said 1/1000 properly labeled and everybody knowing it
would probably be OK.
But I think it is important to discuss that.
PINE: One in 950.
REESE: Dr. Pfeffer?
PFEFFER: I think there are several other considerations. I certainly agree that
if we can enlarge our treatment spectrum for this disorder it would be
wonderful.
But I also think that we in a way have concern about the potential risks in this
case without sufficient data, and I am thinking also about what happens in the
real world once a drug is approved.
Many of the children with this disorder are treated with multiple medications,
unfortunately, and I would wonder about what drugs might have potential for
cross-reactivity that might increase the risk for these children. And, I tend to
think that we have a disorder that is severe, there is no doubt. We have
carefully tried to develop approaches to treat these children and perhaps a
careful approach is to ask for more data and to sort of place that in abeyance
for the time being until we can answer this question with a little bit more
assuredness.
It just raises a new issue because we did talk about some medications, one of
which I think is commonly used, which could have cross-reactivity.
GOODMAN: Let me clarify. We have 1/1000 and there was an estimate of -- what was
it? -- 5 percent of cases of Stevens-Johnson lead to mortality?
BIGBY: Yes.
GOODMAN: Let's start with that just as a figure. How many open cases would you
need to treat, for what period of time, in order to gather those data with some
degree of confidence?
TEMPLE: I don't think you could imagine getting good mortality data...
GOODMAN: No, I am not talking about mortality data.
TEMPLE: Well, to take a simple task, as Tom said, if you wanted reasonable
reassurance that it was not greater than 1/1000, if you had data on 3000 people
and no cases that would provide that. I mean, the tension we have had is here is
this one case in 1000.
Here are 30,000 people treated, no cases. Is this just some wild, weird fluke or
is that close to the true rate? You might even decide -- I mean, you did say
even if that is the true rate, that might be OK.
Maybe you would make it second line or do something else. That might be OK. But
at the moment, one of the reasons this was brought to you is we don't know what
the rate is. We don't have enough data to know what the rate is and it could be
rather high or maybe it is really low and this is just a fluke and that is our
uncertainty.
PINE: Speaking only for myself, that is what I would want to know and I would be
comfortable with that, but until I know that it is going to be hard for me to
make a decision.
REESE: Dr. Rappley?
RAPPLEY: I could ask it another way.
Is anybody comfortable with the amount of data that we currently have? Then we
could move to discussing what additional data we need if there is further
discussion on that. I don't mean to push.
GOODMAN: No, that is good.
TEMPLE: Just one thing, as you discuss that I think it is important to think of
enough data for everybody, enough data for a fairly scary statement that says
this is only for people who haven't responded well to other things, not that we
have data on that but, I mean, there are a number of things to think about as
you discuss this.
PINE: Again, related to the discussion we have had I don't think the questions
are really about efficacy or what the niche is going to be so, personally, I
would care less about who receives the medication in terms of what narrow type
of condition they have, and I would be more concerned with capping the risk
estimate.
Based on what Dr. Bigby said, it seems to me 3000 patients treated for a month
openly would be what you would want to do.
GOODMAN: We are not finished with this obviously. I would like to move on to
some of the other concerns we have and see if we can go through a list and
perhaps even identify where we think that this medication might have some
advantage, some possible niche.
In terms of cardiac issues, those were discussed at some length yesterday. I
think in the context of stimulants it was decided that an individual who had
known structural cardiac abnormalities should not be prescribed a stimulant.
Would we be having similar concerns about this agent? In the data that I have
seen there wasn't very much evidence for increases in cardiac parameters such as
heart rate or blood pressure and, therefore, would it be in that context perhaps
a safer alternative?
REESE: Dr. Andreason?
ANDREASON: I just wanted to add that in the Provigil labeling already it warns
against using modafinil in patients with hypertrophy and bicuspid aortic valve.
GOODMAN: So, you would already put it in the same category with the stimulants?
ANDREASON: Well, it kind of already is. It is already in labeling. Unless you
felt that the data that was presented should remove that.
GOODMAN: I don't see anyone saying yes.
REESE: Could you come to the microphone and state your name? Thank you.
HERSKOWITZ: Norman Herskowitz, medical officer in DMP. In the labeling, as I
recall, it really discusses the limitation -- I think this is the initial
studies -- to issues of mitral valve stenosis and regurge type of syndromes, but
not to any other sorts of cardiac history.
So, that is just for information sake.
ANDREASON: I am pulling up that labeling for you; I am not as fast as I thought
I would be. HERSKOWITZ: It mentions some very subtle changes in blood pressure,
but extremely subtle. In the adult studies there seemed to be a pattern of
increase in anti-hypertensive use although no changes in mean blood pressure.
ANDREASON: I have it. This is under cardiovascular system in the Provigil
labeling. It says in clinical studies of Provigil signs and symptoms, including
chest pain, palpitations, dyspnea and transient ischemic T-wave changes on ECG
were observed in three subjects in association with mitral valve prolapse or
left ventricular hypertrophy.
It is recommended that Provigil tablets not be used in patients with a history
of left ventricular hypertrophy or in patients with mitral valve prolapse who
have experienced the mitral valve prolapse syndrome in previously receiving CNS
stimulants.
Such signs may include but are not limited to ischemic ECG changes, chest pain
or arrhythmia.
GOODMAN: And that is at a lower dose than is being proposed.
ANDREASON: Correct.
REESE: Dr. Rappley?
RAPPLEY: The discussion yesterday from Dr. John Moore who is a pediatric
cardiologist on the Pediatric Advisory Committee and, Deborah, add to this if
you can, we talked about how the increases in blood pressure and pulse were
perhaps not clinically significant for children but statistically significant
and, yet, the concern persists because of the idiopathic hypertrophic subaortic
stenosis being a condition that really cannot be detected in the population
until the serious adverse event occurs, and that it is plausible that increasing
sympathetic tone could contribute to that in the same way that running track or
becoming dehydrated does.
GOODMAN: After Dr. Pine makes a comment I would like to take a ten-minute break
before we come back for further discussion and vote on the second question. I
need a few minutes to deliberate.
Dr. Pine?
PINE: I guess with a lot of these secondary adverse effects -- the cardiac
effects, the psychiatric sequelae, the growth effects -- for some of the same
reasons that people were uncomfortable making statements about comparative
efficacy, I would be uncomfortable making statements about comparative adversity
unless there have been head-to- head trials, which there haven't been.
You know, my take from looking at all the other data, besides the dermatologic
data, I am slightly concerned with the psychiatric adverse effects, no more
concerned here than the discussions yesterday, and I just think it is probably
not fair, given the data, to make statements that this is better or not better
than any other agent unless they have been compared head-to-head. I think it is,
you know, is it safe enough or not for all of these secondary issues and, again,
in my mind it seems safe enough, whatever that means.
GOODMAN: I would agree. Let's take a 10-minute break.
(RECESS)
GOODMAN: It seems to me that a lot is hinging on one case and I still haven't
decided which way I want to go based upon that pivot point.
So, let me just go back to that case for a moment.
First I would like to hear from Dr. Bigby. I think I have already heard, but I
need him to repeat, that there was definitely a case of SJS but I would like to
hear again his opinion on the association between the drug and that case of
Stevens-Johnson syndrome.
BIGBY: My opinion about that reported case is that it is probably a case of
Stevens-Johnson syndrome related to the drug. Now, that doesn't mean that it is
definitely related to the drug. And, I think that the difficulty would be for
anybody to say with any certainty that it is not drug related.
But, you know, am I absolutely certain that it was due to the drug? No. But I
wouldn't want to be put in the position to argue that it is not drug related.
That is the problem we have.
GOODMAN: I understand that the investigator who treated that subject is here.
Could that person identify himself or herself?
Would you mind coming forward and just describing your impressions of the case?
REESE: Could you please be sure to identify yourself, sir?
BELNOR: I am Samuel Belnor, a pediatric neurologist and I was the principal
investigator on this case that was a 7 year-old Asian boy who is perhaps the
most compelling case for Stevens-Johnson.
My impression on this patient -- and then I will go into detail, but my
impression was that the most likely diagnosis was erythema multiforme, possibly
Stevens-Johnson. The most likely etiology was a viral infection, possibly drug
related.
The patient had shown improvement in the clinical symptoms of ADHD after one
week on drug and was seen on the 14th day. On the 14th day the patient presented
with fever of 101.9, a sore throat and feeling bad.
I was out of town but the sub-investigator, a pediatrician, saw the patient. The
mother complained of two lesions on the leg which she thought were possibly a
brown spider bite but there was no rash.
The next day the sub-investigator put the patient on amoxicillin and did a rapid
screen for strep. which was negative.
The throat, he felt, looked like a viral throat infection. There was no
exudative pharyngitis but papules in the throat. The patient was seen the next
day by a pediatric group locally.
The pediatric group saw typical lesions of Coxsackie B virus in the posterior
pharynx and diagnosed this patient as having a Coxsackie B virus infection.
The rash was over most of the areas of the body but it was more marked on the
face and extremities.
Also, they felt that the two lesions on the legs were the target lesions of
erythema multiforme.
The patient did not develop any apparent -- there were no lesions in the mouth
at that time and no mucous membrane involvement.
About six days later -- I apologize, we have a real lack of data because the
mother did not bring the patient back to us until four weeks after the rash
developed, in spite of being called on numerous occasions. She had a single
family business and was the only employee and would not bring him back.
He went to school many of these days. We told the family the day of the rash to
stop the drug. The teacher recommended, on day 23, that she felt that he should
go back on the drug because his behavior was much worse and the mother gave him
one dose of the drug and nothing really changed much except that she felt that
he was maybe pealing more and did not give any more.
No one saw the lesions in the mouth, other than the mother, and she thought that
there were lesions in the mouth because he would not eat well.
No physician see mucosal involvement. He did complain of burning when he
urinated, which is a possibility.
The patient really felt quite good during this four-week period from the onset
of the rash until we saw him next. He went to school about half the time. The
mother was really unconcerned.
When I saw him four weeks after the rash onset I saw no lesions in the mouth.
There was no evidence of any previous lesions in the mouth. He was happy; no
stress. And, his skin was pealing.
There was no evidence of any dermal involvement other than just some pealing of
the skin, mainly on the extremities. There were no lesions in the posterior
pharynx of the Coxsackie B virus.
If we had seen the patient earlier we obviously would have done a skin biopsy.
We did a RAS test later to modafinil and to amoxicillin -- of course, it is of
limited value, but it did not show any positive reaction.
GOODMAN: I would like comments on what you have just heard from either Dr.
Rappley or Dr. Bigby. Does that help one way or the other in the diagnosis?
BIGBY: Given the description, I don't think that anybody can say that that was
not a case of SJS. You know, it would be nice to know if the patient had typical
targets or not but I don't think you are going to get that described in this
case.
RAPPLEY: I guess for me it is the degree of uncertainty that we have at every
point; it is sort of the added uncertainty that makes me uneasy; that makes me
unwilling to say that it is just fine, let's go forward and treat everybody.
GOODMAN: Can you repeat that?
RAPPLEY: It is the degree of uncertainty that we have that makes it difficult
for me to say that it is fine or perfectly acceptable to proceed with just
having people make sure they report rashes.
GOODMAN: Dr. Pine?
PINE: I want to go back to the statement Dr. Temple made. You obviously seemed
very taken with this when you said it is at least going to get a black box and
we moved away from you fairly quickly. Could you just spell out your thinking,
what made you react that way?
I mean, I think it is more than just this one case or maybe it is just this one
case but I would like to hear that.
TEMPLE: Well, it goes without saying that I have no credible, sensible view
about whether this is a bona fide case or not. I am listening to people who do
though.
So, what we are seeing is that in something like 1000 people, but perhaps when
you look at exposure it may be 700 or 800, you have one case that is at least
statistically compatible with rates that are high enough to be worrisome, you
know, down to one in a few hundred and up to whatever, and a condition that is
very scary and is life- threatening.
So, it all turns on believing the case. I mean, if this was dismissable I
wouldn't have said that but everything I have heard up to now, both internally
and even from the company, says that this is a plausible case.
So, when your best estimates of something very worrisome are in the neighborhood
of 1/1000, you know, of it was agranulocytosis or something we are accustomed to
taking full note of those. That is really all I meant.
PINE: Yes, that is helpful. Thanks.
GOODMAN: Dr. Mehta? MEHTA: Actually, I have two questions of the investigator.
One is was the patient hospitalized? And, what surface area of the body was
affected by Stevens-Johnson syndrome?
BELNOR: I am sorry, will you repeat the first question?
MEHTA: Was the patient hospitalized?
BELNOR: No. Although most of the areas of the body were involved, the total
surface area of the body involved, according to the mother's history and the
pediatrician that saw him and our examination when he came back, was less than
10 percent.
MEHTA: Can I ask Dr. Bigby a question?
GOODMAN: Sure, go ahead, Dr. Mehta.
MEHTA: What percentage of Stevens-Johnson syndrome patients would be
hospitalized?
BIGBY: Excellent question to which I do not know the answer.
GOODMAN: Ms. Bronstein?
BRONSTEIN: I think there is another signal we can't forget and that is the adult
population on the low dose having three cases in a little over a million, which
is two cases more in a million than the general population on the same drug.
So, you know, even if there is some question there is also some other linking
stuff, at least in my mind.
GOODMAN: Dr. Laughren?
LAUGHREN: Could we get some clarity, maybe from Dr. Bigby, on what the
background rate of Stevens-Johnson is? Then, what the reporting rate is in this
experience with this drug in adults?
BIGBY: If you look at sort of population-based studies the estimate is one case
in a million or 500,000.
If you look at the case-control study that was done in Germany, Italy and France
where they sort of specifically tried to identify all of the cases over a period
of time and they took detailed drug histories from the patients and they limited
the definition to SJS and TEN the way I defined it in my talk, it was in the
order of 1/100,000 to 1/400,000.
LAUGHREN: So, it sounds like it varies anywhere from 1/100,000 to 1/million. Do
we have clarity on what the reporting rate is for those three or four cases in
adults? Maybe the company would know that.
CIVIL: Yes, for the person taking the transcript, my name is Rich Civil,
C-I-V-I-L. Our reporting rate for events coded as SJS and TEN, the number of
cases we have has been discussed. There are five. Each of them can be looked at
individually and, indeed, the discussions up to this point have already excluded
largely from consideration one of the cases, that being the patient with
subarachnoid hemorrhage who developed the cutaneous skin reaction in association
with the apparent initiation of treatment we phenytoin and phenobarbital.
Subtracting that case out, we have four cases in approximately 750,000 adult
patient-treatment years of exposure.
Given the described hazard profile which suggests a greater risk in the first
four weeks perhaps, we recognize that a better denominator for that exposure
would be patients rather than patient- treatment years.
Based on what we have estimated as an average treatment duration of
approximately 2.5 months on average in the postmarketing environment, we would
then calculate that the 750,000 patient- treatment years translate to the rough
equivalent, based on IMS estimates and survey data, of approximately three
million patients treated.
LAUGHREN: So, the reporting rate with that denominator is roughly one per
million. So, there you have it. I mean, you have a reporting rate of one in a
million; background rate somewhat less than that.
TEMPLE: Well, that doesn't take in the under-reporting.
LAUGHREN: Right, but we usually compare reporting rates to background rate,
understanding that there is under-reporting. We generally take some comfort if
the reporting rate is well below the estimated background rate.
PINE: I guess my question is what is the downside of capping it at 1/1000 by
studying 3000 more patients? As far as I can hear, the only downside is that we
are going to delay putting the treatment on the market for six months or a year,
which seems like a risk worth taking if we really want to be sure that, you
know, 1/1000 is really the risk of Stevens-Johnson.
I mean, that seems like a fairly fair trade, you know, to be sure that the rate
is really no higher than 1/1000 and we delay approving a treatment for however
long that takes, six months or a year.
LAUGHREN: That is precisely what we are asking the committee.
TEMPLE: Right, and people have to weigh the cost of the delay and the
consequences of not doing that.
MALONE: Most of the talk has focused on the one Stevens-Johnson. What about the
other case? I didn't quite understand the case where there was urticaria. Was
that thought to be drug related or a signal of anything else related to serious
skin reactions?
BIGBY: I think that that case is less than 50 percent likely to be drug related.
GOODMAN: If this were a new molecular entity with no prior marketing experience
and I was presented with these data, with the degree of uncertainty that we are
all facing, I would say we needed additional data, for sure.
And, I think one of the reasons that I have been on the fence in the last hour
or so is because it is an agent that has been out there for a long period of
time.
But, given the fact that it is at a higher dose and it is going to be given to a
population that metabolizes it differently, perhaps I should be taking it more
as if it were new rather than a different indication for the same compound in
the same population.
So, I would have to say I am leaning at this point to recommend additional
safety testing.
I don't feel, as I re-read this question, that modafinil has been shown to be
acceptably safe given the doubts that we have in our minds. If it turns out to
be 2/1000 I think we would all regret the decision to go forward. I don't want
to do that experiment in the postmarketing arena.
I think, that said, if we are to recommend the studies -- hopefully, the FDA
would be the ones to really design this -- that we don't set the bar too high. I
don't want to be disingenuous. I think that this is a drug that we all agree is
efficacious. There may be certain advantages over existing compounds.
Some of those are yet to be proven. I would like to see an opportunity for the
company to come back with those additional data that would give us an extra
degree of assurance that this case was a fluke, and that could exactly be what
it was.
LAUGHREN: I think it is important to be clear about what level of comfort we
could gather from the study that I proposed earlier. The most you would be able
to do is to cap the risk at 1/1000.
So, even if you did that and you were comfortable with that as a cap, I think
the drug would still have fairly strong labeling. I just want to be clear about
that. It is not going to make the problem go away.
PINE: Related to that, there probably would be some discussion about, you know,
let's say you could do a larger study and cap the risk even lower. You know,
maybe people would want to do that. There could be some discussion about that.
I think that is probably going a little far based on the data we have right now.
I think the question is, is it safe enough or not and that is kind of what we
are debating.
GOODMAN: Dr. Wang?
WANG: I am a little bit less sanguine. You feel that with a study of another
1000 patients maybe you will cap it at 1/2000. It quantitatively gives you
reassurance; it won't qualitatively necessarily give you maybe the reassurance
we are looking for.
One thing in favor of additional studies is an active comparator, a study that
actually could maybe sort out sort of where in the armamentarium this might fit
in.
GOODMAN: Dr. Bigby?
BIGBY: Somebody has to clarify to me then what is the black box labeling for
Lamictal.
If they have a rate of 8/1000 in children what does the label say?
ANDREASON: Let me put it up.
PINE: The other thing to remember about the labeling for Lamictal is that it is
for Lennox Gasteau syndrome so it is a different disorder fundamentally.
TEMPLE: And for which I believe there is no other treatment.
PINE: There is no other treatment, that is right.
TEMPLE: It makes a difference. I am confident if there were no other treatment
here our discussion would be different.
ANDREASON: Here is the lamotrigine black box, or at least the part that has the
data and the warning up front. This is for Lennox Gasteau in kids and then
adjunctive therapy for epilepsy in adults and bipolar in adults.
GOODMAN: Dr. Temple?
TEMPLE: Well, I am sure you are going to want people to discuss what you just
said but I just want to throw one other thing into the mix, and that is, suppose
the company did a study showing definitively the way I want it shown that it
really did work in people who failed on other therapy -- a properly designed
study, not that hard to do if it really does work in that setting, would that
make any difference in all this?
GOODMAN: It would make a difference.
It would definitely wind up with a black box.
PINE: I don't think it is an either/or though. I would want to cap the risk.
TEMPLE: Well, that is what I am asking. What you have just been discussing is
capping the risk before it gains approval for this use. What I am asking is if,
before doing that, they knew that it unequivocally works in people who failed on
other therapy would that make you want to make it available even before you
capped the risk, with an appropriate box, or not? PINE: You know, that is a
theoretical debate. I would have to see how well does it work; does it really
beat a stimulant head-to- head; who are these people...
TEMPLE: That is the test. It would have to beat the drug they supposedly failed
on, presumably a stimulant, in a randomized trial and it would have to beat it.
PINE: That would be great. I mean, I can't tell you that I would definitely say
forget about the risk if you show me that, but it definitely changes the
discussion we are having right now quite appreciably.
GOODMAN: I would echo Dr. Wang's point earlier that not having the comparative
data I think is a weakness of this application.
PINE: But, personally, I don't think you have to have that. I mean, I think if
it worked just the way it does work and you knew that the risk was 1/1000, again
just speaking for myself, I would be comfortable with that.
TEMPLE: No, I just meant whether you could truncate further characterization of
the risk if you knew that thing about it. Maybe that is such a hard study nobody
is even interested but you don't know until you ask.
GOODMAN: Dr. Bigby, has your question been answered?
BIGBY: Yes.
REESE: Dr. Malone?
MALONE: If you did such a study, then would the label reflect that it was
approved for the treatment of patients who failed other treatments or would it
not include that in the label?
TEMPLE: Excellent question. With clozapine where we had those data the labeling
said you should have failed on other therapy because the 1.5 percent rate of
agranulocytosis was considered unacceptable in a first-line population.
So, if there were no further characterization of risk you might very well say
that it is for people who failed other therapy, and maybe you wouldn't have to
wait for the further characterization of risk.
If the risk were then further characterized and everybody was comfortable, maybe
then we would feel it could just be thrown into the mix and they would have this
particular piece of information.
MALONE: How well do post-approval registries help resolve a question like this
because it won't be that easily resolved? And, how would you do that?
TEMPLE: Yes, that is a hard question.
There are probably people better able to answer.
The most successful registries are ones where you are controlling distribution
so, for example, the clozapine registry, in my view, is a huge success because
you can't get the drug without going to the right pharmacies and your name goes
in it, and one of the purposes of it is to keep people who have already gotten
agranulocytosis from ever getting the drug again and, as near as we can tell, it
has been very, very successful and there have been analyses, but that is because
you have to sign up to get the drug.
Registries ordinarily in many other cases are voluntary and whether people stick
to them or not is uncertain, and they have varying degrees of success. We would
have to get some people who know more about it than I do to answer that though.
MALONE: Currently, with stimulants you almost have to see a patient fairly
regularly because you have to keep writing the prescription.
Could a registry be developed by requiring a script from a doctor? At least they
could ask if they had a rash.
TEMPLE: Well, any system that limits distribution -- first of all, it is very
difficult if the drug is already available in another form.
Second, they are a lot of trouble. I mean, we do those things for drugs we are
really worried about.
There is one being set up for Accutane that is more rigorous than before;
thalidomide -- I mean, those are the things we are talking about. You don't do
them lightly because there is actually some evidence that they interfere with
use.
We have distribution system for a drug called dofetilide that is used to
maintain normal sinus rhythm and a study, I guess out of Duke, showed that
people are using solatol or quinidine instead. Well, that was not what we had in
mind. So, you have to fit it into the system and it has to work out.
GOODMAN: Dr. Malone, by this line of questioning, are you suggesting that our
target would be to vote in favor of the compound but to put in place a rigorous
registry program to monitor for rashes, particularly Stevens-Johnson?
MALONE: No, I wasn't trying to suggest that. I don't think it is going to be
easy to answer how often a rare event occurs if you do more patients.
So, I think in the end you are going to have to have a longer way of answering
that question. I wasn't trying to suggest that you would approve it and then
handle it that way.
GOODMAN: Any members of the committee that would like to argue in favor of this
being shown acceptably safe, and we are focusing on the dermatological
complications? (NO RESPONSE)
I would like to give a representative of the company a chance to argue that
point before we take a vote.
RUSSELL: I would just like to ask Neil Shear to give his opinion on the risk of
Stevens-Johnson.
SHEAR: Well, I guess I can perhaps add strength to your difficulty. The question
of this single case is exactly the way I would have explained it, that there was
a single case that was sort of convincing.
It didn't meet a definition of Stevens-Johnson because the body surface area of
epidermal detachment was not high enough. It would probably meet a definition of
erythema multiforme major, and it probably is post viral.
The other issue you can look at is it is not 1/1000 because it was 10/10,000 --
it was one and that one could easily be zero and that one could be two. So, in
terms of it perhaps being a fluke, I think there is some strength to that
argument.
Then trying to do the balance that you are talking about, I think, you know, you
have raised various possibilities. I don't feel it is up to me to tell you what
to do on that. But keeping track of reactions has been done before for other
drugs.
I would also say that because of its already accumulated experience, the
pediatric dose notwithstanding, this is not Lamictal. This is not a drug that
had started right from the beginning -- Lamictal, when it was started in England
out of Burroughs Wellcome, was causing problems immediately and continued to
cause issues.
Now, some of those are probably over-ascertainment because people were jumping
on the bandwagon in terms of diagnosis but, still, it is a drug that has a very
different risk and I think that has been managed over the years, actually many
years now.
Here is a drug that was on the market. It is not a new chemical entity but is
being used in a broader population in children so you have the balance there.
What I have seen so far has not convinced me. I think where I would differ from
Dr. Bigby is that I don't feel that I can absolutely -- and I don't think he
said absolutely, but I don't know if I can really confidently say that there are
going to be cases of Stevens- Johnson/TEN with this.
I just don't see that based on the exposures we have but that is, again, just
personal after looking at many of these drugs for many years. If you look at
dilantin, if you look at sulfonamide, they were recognized in the '30s. When
they first came on the market it was clear that these drugs were causing these
kinds of problems right away. I do want to make one more comment since I have
the microphone for a second, the sulfonamide allergy story -- for the severe
reactions to sulfonamide it is the aromatic amine at the end of the molecule and
not the sulfonamide moiety that is considered to be responsible.
There is certainly no evidence to the contrary and the only evidence that exists
on a metabolic basis is that the aromatic amine is hydrolyzed to a hydroxylamine
which goes on to become a nitroso, which is a P450 pathway through 2C19, and
that is what appears to lead in vivo and in vivo to toxicity.
PINE: I would like to ask you a question about your statement about where you
would disagree with Dr. Bigby. How confidently would you assert that you doubt
that we would see additional cases? I understand that you said that there is not
a lot of evidence to support that.
SHEAR: Well, I guess what I would do is look at the cases that exist. What is
real?
What am I comfortable with? We do see that there are some cases in the adult
literature. It is hard to tell but, you know, we do have some numbers that are
low, like background, and they are in the 1/100,000 to 1/million type of range.
Though adults don't usually get Stevens-Johnson syndrome that often, we do see
it. We do see people come in; they have no drug and they get a real
Stevens-Johnson syndrome.
So, that is probably out there. The pediatric exposures of at least 30,000
children -- Dr. Andreason showed the numbers for people who were getting the
drug through various programs, and they had none in 30,000 exposures.
Again, if this case was rock-solid Stevens-Johnson, which it doesn't appear to
really be by the usual case definitions that we use nowadays, but if it is
erythema multiforme major, which is something that kids do get and something
that suggests viral from what we heard about the case, the more you dig into
this the more I am getting more comfortable that it isn't.
And, until I had a chance to actually talk to the investigator I don't think I
would have been saying this, but looking at it in its totality and trying to
balance it against the other known hard-core data, that is what makes me more
comfortable and I think I have had that information maybe hours longer than Dr.
Bigby, but not much more, and I think you do get more comfortable, and we sat
down as a group of experts to talk about it and we did become more and more
comfortable where that probably fit.
REESE: Dr. Bigby?
BIGBY: Do you have a response to the question that was asked about what
percentage of patients with Stevens-Johnson syndrome get admitted to the
hospital? SHEAR: Yes, your answer was a good answer; it is a good question. I
mean, we do sometimes see people who come in who we think have Stevens-Johnson
admitted to the emergency departments, but I would say that if they actually had
some real epidermal detachment they would be admitted not only to hospital but
probably to a burn unit.
I mean, we are talking about some pretty sick people and if you see a kid with
truly Stevens-Johnson syndrome, well, you are not going to send them home.
Unless you want to, you know, not only potentially kill the child but end your
career, you are not going to do that. This is a serious event and it is easy to
recognized. This is not a subtle diagnosis really.
I mean, these people have mucosal blistering that is not only horribly painful
but is hemorrhagic, and that is not what we saw in this case and, again, we have
not seen any reports in the larger pediatric population or the postmarketing
surveillance.
GOODMAN: Further discussion?
Dr. Mehta?
MEHTA: I have worked in the drug industry for about 40 years and I must say that
I have worked with a lot of different drugs and I have seen during clinical
studies about 20 patients with toxic epidermal necrolysis or Stevens-Johnson.
I don't recall a single patient not being hospitalized. Every single patient is
hospitalized. It is such a serious disease because mortality now is about 5-15
percent. Ten or 20 years ago it used to be 50 percent. So, every patient was
hospitalized.
GOODMAN: Dr. Rappley, do you have a comment?
RAPPLEY: All day we have dealt with the uncertainty before us but now we hear a
lot of confidence that it is not Stevens-Johnson. I, myself, am not changing my
view on this.
GOODMAN: Dr. Temple?
TEMPLE: Well, let me offer a suggestion or a question. My assumption is that to
the extent confidence that this case really represented Stevens-Johnson, you
would be more comfortable with going directly to approval perhaps with language
in the labeling, and I don't think we are going to be able to fully do that
here.
So, let us tell you -- you know, we might telephone you or something, but we
will look more at this. We have experts around even though none of us personally
knows about it.
If the case starts to look very weak, that is going to change things and i think
we understand what you think about that.
But if the case stays reasonable strong, not 100 percent but reasonably strong
then I think we have heard your advice.
GOODMAN: I find that acceptable. I would like to call the vote on the question
based upon what we know now.
RAPPLEY: Will you clarify what it is that we are voting on?
GOODMAN: Has modafinil been shown to be acceptably safe in the treatment of
attention deficit hyperactivity disorder in children and adolescents?
You have a comment, Dr. Andreason?
ANDREASON: Yes, Dr. Luke had a question about the case report versus the report
given by the investigator.
LUKE: Yes, in the original written case report it stated that it covered the
entire body. It was described very differently from how the investigator
describes it today.
I think that contributed somewhat to the relative uncertainty that we are now
hearing within the last half hour or so.
So, the question is what is the real story, was it the written report provided
by the sponsor or is it the investigator's testimony given now at today's
meeting?
BELNOR: I don't think we have changed the story. The implication was that it was
on all areas of the body but it didn't cover every area of the body completely.
It was less than 10 percent of the total body surface area. It was on the trunk,
the face, the extremities and the back.
LUKE: So, you are saying the pealing is less than 10 percent but perhaps the
rash itself...
BELNOR: No, the rash. The rash was around 10 percent by the history that we
obtained from the pediatrician.
LUKE: Oh, so it is by history. You did not yourself observe this?
BELNOR: No, the peeling looked like it was obviously less than 10 percent when
we saw the patient.
LUKE: So, then there is still some doubt. It is really hard for a dermatologist,
and I know other dermatologists in the room can attest to it, to make an
assessment from hearing a story, especially if it is not carefully written up.
Photographs are often helpful and biopsies are helpful but, again, it is lack of
information that adds to uncertainty.
GOODMAN: Let's go ahead with the vote. I am going to start with Dr. Bigby.
BIGBY: So, is this a yes or no answer? GOODMAN: Or abstain.
BIGBY: I would say yes, it is acceptably safe.
GOODMAN: And explain your reason.
BIGBY: You know, I think that this is an instance where we are being asked to
make a decision on the basis of a single case that is probable but not definite.
I mean, I have concern that when the drug is more widely used over a longer
period of time you are going to see cases of SJS but you see that with lots of
other drugs that are already marketed.
GOODMAN: Before I go on with the vote, I actually expected a different response
and I am assuming others did too. So, maybe there is room for further
discussion, given the opinion you just rendered, before we go on with the vote.
Does that change anybody's mind around the table?
BRONSTEIN: I have one question of the investigator. It was my impression that
you did not see this patient yourself until four weeks after the very final time
the mom brought the child in. Is that correct?
BELNOR: The mother refused to bring the child back in from the second visit
until the last visit.
BRONSTEIN: My question is when did you lay eyes on the patient.
BELNOR: I saw the patient at the first visit.
BRONSTEIN: Before the rash?
BELNOR: Before the rash.
BRONSTEIN: And did you see the patient on the last visit?
BELNOR: Yes.
BRONSTEIN: But not when the rash was in its fullest...
BELNOR: No, none of the investigators saw the patient when the rash was present.
We told the referring doctor to stop the medicine and send the patient to us for
a biopsy.
BRONSTEIN: And who did the write-up of the patient that was received?
BELNOR: I did.
BRONSTEIN: The first write-up that was received to the company?
BELNOR: I did most of the write-ups.
I don't know. There are a lot of errors in the history. BRONSTEIN: Thank you.
GOODMAN: Do you have any further comments?
BRONSTEIN: I am left with a lot of questions and a lot of lack of confidence,
and I feel like erring on the side of conservatism, either longer testing or
saying no but as the consumer representative I feel like the public needs to be
protected and we have a lot of questions here.
As a working mom, I really can relate to this mom not bringing the kid in; I did
it myself. And, I don't know that you are going to get good anecdotal reporting.
I also don't have a lot of confidence in non-dermatologists reading rashes. So,
that is where I am with all this.
GOODMAN: Dr. Wells?
WELLS: While it may be true that the case for lack of safety has not been made,
it is also true that the case for safety has not been sufficiently made, and I
think that is what we have to have in order to make a statement that it is
adequately safe and I am not there.
GOODMAN: Dr. Pfeffer?
PFEFFER: Am I voting or making a comment?
GOODMAN: You are just making a comment.
PFEFFER: I wanted to ask, I just began to remember, isn't it true, Dr. Bigby,
that this problem, Stevens-Johnson for example, doesn't always appear on the
entire body simultaneously?
Isn't there a course that goes from head to foot?
So, I was wondering about this case. How frequently did the pediatrician see the
child once the rash occurred?
BIGBY: So, Stevens-Johnson does normally evolve over a period of several days,
and it is true that it is not full-blown at its onset.
People can continue to get lesions over several days. I would say in the
majority of cases you start getting new areas of involvement after about a week
or so.
GOODMAN: Dr. Robinson?
ROBINSON: Well, I think it is very striking that the one case that we are
debating about came in the context of somebody who was in a controlled trial.
Even in a controlled trial, which wasn't designed to look at this issue, we are
in the situation where experts can debate back and forth, and I think that says
that if we approve the drug and say there is going to be postmarketing we would
not get data that was really usable because even in a controlled trial we are
debating. I think that argues for us getting a study design to look at this
specifically so if somebody has a suspected case of it the proper information is
obtained, like photographs and expert dermatologic consultation so that we can
actually say what is an estimate.
It is just striking that even in this sort of controlled trial we are not
getting the information we need and I think that argues for a specific study.
GOODMAN: Dr. Armenteros?
ARMENTEROS: I also have a concern that I am not so sure that even a controlled
trial moving forward from this point would still resolve our doubts. I am
concerned about that.
GOODMAN: Dr. Andreason?
ANDREASON: I suppose for something that is as rare as Stevens- Johnson or, say,
something like acute liver failure you don't even need a controlled because the
historical control is so rare that if you pick up a case in an open-label trial
of, say, 3000 patients that is significant.
So, that would be an acceptable design to look at something like this.
GOODMAN: Let's start with the vote again, and this time I will begin with
myself. I am going to vote no. I have been persuaded by my colleagues around the
table and my comfort level is not sufficient that this has been shown to be
acceptably safe.
I don't know what to make exactly of that one case and, frankly, I don't think
we are ever going to be sure. It certainly raises a sufficient number of doubts
about a serious adverse event that should not have occurred even at the rate of
1/1000 or less that we saw in this trial.
Perhaps the other factor that has led to my decision is the absence of other
strong, convincing reasons to consider this drug having advantages in other
areas of safety or tolerability or efficacy so I am not willing to find the risk
acceptable of going forward without additional data that would rest some of my
concerns about the dermatological reactions.
Now we can go back to Dr. Bigby.
BIGBY: I voted.
RAPPLEY: I do not think it is acceptably safe and I think you all have
articulated my feelings.
WANG: I think it is just unknown.
Can I abstain until we have more information? I mean, it could be everything
from this things shouldn't be approvable if this is a real signal to there is no
warning needed at all if this isn't the case. We don't even know what to make of
this case. There is no temporal or inter-rater reliability even within this
meeting.
GOODMAN: Dr. Laughren?
LAUGHREN: Actually, I don't understand an abstention in this situation. I mean,
we are asking you if you feel there is not enough information to make a
judgment, then I think the answer would be no.
WANG: No, OK. It is no, we don't have enough information.
BRONSTEIN: My vote is no unless more information is obtained.
PINE: I guess I will make two statements. I found Dr. Temple's statement about
you will look into it and, the more doubtful this diagnosis becomes, everything
changes, and I would agree with that.
You know, just sitting here today it has to be obvious to anybody that knows
nothing about Stevens-Johnson syndrome that there is a reasonable suspicion.
I think everybody would agree with that, that there is a reasonable suspicion
that this was a case of Stevens-Johnson syndrome related to the medication
exposure. So, that is the first thing.
The second thing is that I really don't think it is that big a deal to cap the
risk at 1/1000. So, I am going to vote no and what I would recommend is a study
of 3000 patients that is not an efficacy study, that is simply designed to make
sure that there is not a single case of Stevens-Johnson syndrome, you know,
treated for a month.
LEON: I will vote no, based on the data we have seen that modafinil has not been
shown to be acceptably safe for children and adolescents with ADHD.
ROBINSON: I am voting no because I think that we do need a study specifically
designed to at least get a good estimate of what the rate is, and especially in
a therapeutic area where modafinil hasn't shown a specific efficacy that is
greater than with the already available agents.
PFEFFER: I am voting no also. I think that we need more information which I
think will be extremely helpful in guiding not only the clinician but enhancing
perhaps compliance of patients.
My feeling is that if this were approved now, regardless of how the clinician
might feel or try to explain it, I think the compliance of parents for the
children would not be as good perhaps than if there were a clearer view of the
risks where they could make a more informed decision. I think we need more data
and I think that it is worth that wait.
ARMENTEROS: Well, based on the confusion that I have been exposed to through the
whole day, I am going to vote no and I am hoping that given this ADHD diagnosis
we can identify readily and do studies to bring on the data.
We are not talking about a condition that is rare so we should be able to move
ahead at a later stage with much more clear information that in everyone's mind
will be better at that stage.
WELLS: Barbara Wells, and I will vote no. I don't believe the case for safety
has been adequately made and, in addition, I don't believe we were convinced
that it is more effective than available treatments and perhaps not as effective
as available treatments.
We also have reason to at least suspect that the incidence of even the common
side effects is higher with this drug than with available treatments.
DOKKEN: Deborah Dokken, I also vote no on the question of safety. I mean, the
uncertainty about all of this today has been almost painful and on those grounds
I think we do need more information before we can put it out for the public.
MALONE: I vote no also. I think that the potential population who would get the
drug is fairly big, especially considering the safety risks that we have been
talking about today and the apparent lack of any safety advantages for this
drug.
MEHTA: I know I cannot vote but if I were to vote I feel like the California
voter in the presidential elections where my vote doesn't count because it has
already been decided.
Anyway, let me make a couple of comments. One is that I am not convinced that
this is a patient with Stevens-Johnson syndrome. I have heard enough discussions
and I have been faced with and reviewed patients like that. I am not a
dermatologist but still I do not believe that this is a case very clearly.
Secondly, the case for the dose relationship, that a higher dose will lead to a
higher incidence of Stevens-Johnson syndrome certainly has not been made. If
that is the case, then one should use as a denominator something like 3 million
patients.
So, we have about four or five patients with Stevens-Johnson syndrome in an
exposure of 3 million people, which is no different than anything else.
So, from my point of view, if I had to vote I would have voted differently with
a lot of strictures about how to get more data to make sure that the real
incidence is not more than what we already see.
GOODMAN: Could you give us the tally?
REESE: Yes. There is one yes and 12 no. Going back to question one, it was 12
yes.
Dr. Andreason?
ANDREASON: Just for note-taking, I heard some discussion that a risk cap at
1/1000 would be something that you would like to know about. Did you want to
talk about that or make a vote on that?
PINE: Again, I would emphasize that really the question of efficacy is not on
the table here, that we have been convinced of efficacy and I can imagine that a
fair amount of time and energy and patients experiences have already been
invested in doing that.
I would not want to reinvent the wheel there. I think the main thing would be to
know definitively what the risk is from a ballpark sampling.
Again, just speaking for myself, if we were to see open-label treatment, treated
by pediatricians who are seeing patients regularly, that there was not a single
case that would raise any dermatological concerns about Stevens-Johnson syndrome
in 1000 cases, then I would vote yes.
REESE: Dr. Rappley?
RAPPLEY: I would support that, and I think it is clear that the medication is
efficacious and the comparison studies can be done postmarketing and I would be
happy with that.
GOODMAN: What I am about to say is not necessarily a criticism of this
particular sponsor but I think there is a lesson in here about the need for
better assessment of these dermatological adverse experiences, and I think a lot
of these issues would have been settled and perhaps even the outcome would have
been different if we had better documentation that would have allowed our
dermatological colleagues to make a more definitive conclusion.
So, I think we are dealing with some fuzzy information but, given that this
wasn't a compelling enough story here, both on the efficacy side and on the
safety side, to reach a comfort level by which this committee could endorse this
compound moving forward to market.
So, I think we did err on the side of consumer protection and I would hope
sincerely that the company would find the means by which it could gather the
additional data to collect the necessary safety data and the outcome could be
different under those circumstances.
I want to thank everybody for attending for the long day, and most of all for
putting up with my scratchy voice. Thank you.
LAUGHREN: And I want to thank the committee again for a heroic effort in helping
us with our job. Thank you.
END
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PR Newswire US
March 23, 2006 Thursday 10:36 PM GMT
FDA Advisory Committee Recommends Against Approval of SPARLON(TM) for Attention
Deficit/Hyperactivity Disorder in Children and Adolescents;
Cephalon 2006 Basic Adjusted Income Per Common Share Guidance Remains Unchanged
LENGTH: 978 words
DATELINE: FRAZER, Pa. March 23
FRAZER, Pa., March 23 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
today announced that the U.S. Food and Drug Administration's (FDA)
Psychopharmacologic Drugs Advisory Committee voted not to recommend FDA approval
of SPARLON(TM) (modafinil) Tablets [C-IV], the company's investigational
medication for the treatment of attention- deficit/hyperactivity disorder (ADHD)
in children and adolescents. The committee voted unanimously that SPARLON is
effective for its intended use but recommended that the company collect
additional data to support the safety of the drug in children and adolescents
with ADHD.
"We are obviously disappointed with the recommendation of the advisory
committee. We will continue our discussions with the FDA to determine the next
steps in the review of this drug application," said Dr. Paul Blake, Executive
Vice President, Worldwide Medical and Regulatory Operations.
The company's previously issued 2006 basic adjusted income per common share
guidance of $3.80-$4.00 remains unchanged. In light of the advisory committee's
recommendation, the company is reducing its 2006 sales guidance by $100 million
to $1.45-1.50 billion; consistent with this reduction, guidance for CNS
franchise sales also is reduced by $100 million to $665-715 million.
The advisory committee's recommendation will be considered by the FDA in its
review of the Supplemental New Drug Application that Cephalon submitted for
SPARLON, a proprietary dosage form of modafinil, in December 2004. The FDA is
not bound by the committee's recommendation, but takes its advice into
consideration when reviewing investigational drugs seeking approval. Cephalon
received an approvable letter from the FDA with respect to SPARLON in October
2005.
Cephalon has scheduled a conference call with investors to discuss the outcome
of the committee meeting at 6 p.m. EST on March 23, 2006. The conference call
may be accessed by dialing 1-913-981-4901. The conference call ID number is
8645966.
SPARLON
SPARLON is a new formulation and proprietary dosage strength of modafinil, the
active ingredient in PROVIGIL(R) (modafinil) Tablets [C-IV], which is approved
for the treatment of adults with excessive sleepiness associated with
narcolepsy, obstructive sleep apnea/hypopnea syndrome and shift work sleep
disorder. SPARLON is chemically distinct from currently approved therapies and
if approved, would provide a unique option for ADHD treatment. PROVIGIL is not
approved to treat ADHD and is available only in 100 mg and 200 mg strengths.
SPARLON should not be used in combination with PROVIGIL(R) or any other
medications that contain modafinil.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products in
four core therapeutic areas: central nervous system, pain, oncology and
addiction. Cephalon currently employs approximately 3,000 people in the United
States and Europe. U.S. sites include the company's headquarters in Frazer,
Pennsylvania, and offices, laboratories or manufacturing facilities in West
Chester, Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis,
Minnesota. Cephalon's European headquarters are located in Maisons-Alfort,
France.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) Tablets, ACTIQ(R) (oral
transmucosal fentanyl citrate) [C-II], and TRISENOX(R) (arsenic trioxide)
injection, and numerous products internationally. Full prescribing information
on its U.S. products is available at http://www.cephalon.com/ or by calling
1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results, including the results of the SPARLON clinical trials;
prospects for final regulatory approval of SPARLON, including the impact of the
advisory committee's recommendation on the FDA's decision whether to approve the
sNDA for SPARLON; manufacturing development and capabilities; market prospects
for its products, particularly with respect to SPARLON sales and earnings
guidance; and other statements regarding matters that are not historical facts.
You may identify some of these forward-looking statements by the use of words in
the statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Jenifer Antonacci, +1-610-563-6018,
jantonac@cephalon.com , or Investors: Robert (Chip) Merritt, +1-610-738-6376,
cmerritt@cephalon.com , both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
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411 of 998 DOCUMENTS
Associated Press Worldstream
March 23, 2006 Thursday 11:25 PM GMT
Narcolepsy drug needs more study as possible ADHD treatment, federal advisers
say
BYLINE: By ANDREW BRIDGES, Associated Press Writer
SECTION: INTERNATIONAL NEWS
LENGTH: 358 words
DATELINE: WASHINGTON
The narcolepsy drug modafinil should not be approved as a treatment for
attention deficit hyperactivity disorder in children until more is learned about
a possible link to a serious skin disease, federal advisers said Thursday.
A Food and Drug Administration advisory committee voted 12-1 against
recommending modafinil as safe for children with ADHD. Earlier Thursday, the
psychopharmacologic drugs panel agreed unanimously that the modafinil works in
treating ADHD.
The FDA is not required to follow the recommendations of its advisory committees
but usually does.
The committee recommended that Cephalon Inc. undertake a 3,000-patient trial to
determine what risk modafinil may pose for Stevens-Johnson Syndrome. Drug
reactions cause nearly all cases of the sometimes fatal skin disease, which can
produce widespread blistering and rashes, according to The Merck Manual.
The FDA's drug chief, Dr. Robert Temple, said one out of roughly 900 children
involved in earlier studies of the drug developed the disease.
Temple and Cephalon spokeswoman Jenifer Antonacci said the agency and company
would discuss the committee's recommendation. The company does not see a "clear
link" between its drug and the skin disease, Antonacci said.
In December 1998, the FDA originally approved modafinil, under the brand name
Provigil, to treat adults with sleepiness associated with narcolepsy. The
company has proposed calling a higher-dose version of the pill Sparlon when used
to treat ADHD.
Other drugs already approved by the FDA for ADHD include Ritalin, Strattera and
Adderall.
A different advisory committee recommended on Wednesday that the FDA add
warnings to the labels of those and other ADHD drugs on the market alerting
doctors and parents to the possible risk of hallucinations in the more than 3
million children receiving the popular medications.
Narcolepsy is marked by recurring episodes of daytime sleep, lasting from a few
seconds to an hour. The disease can be merely inconvenient to some people, but
disabling and dangerous to others who may fall asleep while driving or operating
machinery.
On the Net:
Food and Drug Administration: http://www.fda.gov
LOAD-DATE: March 24, 2006
LANGUAGE: ENGLISH
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Theflyonthewall.com
This content is provided to LexisNexis by Comtex News Network, Inc.
March 22, 2006 Wednesday 9:32 AM Eastern Time
CEPH: Hot Stocks
LENGTH: 246 words
09:32 EDT Cephalon-CEPH gets brief on New Drug Application for Sparlon - Today
the Psychopharmacologic Drugs Advisory Committee, or PDAC, posted on the FDA
website a briefing document with respect to Cephalon's (CEPH) New Drug
Application for Sparlon (modafinil) for the treatment of ADHD in children and
adolescents. The briefing document, which will be reviewed by the PDAC at its
meeting tomorrow, details the chronology of events leading up to the issuance by
the FDA of an approvable letter for Sparlon. In September of 2006, the original
clinical review of the NDA was completed by Glenn Mannheim, M.D., in the
Division of Psychiatric Products of the FDA. In this review Dr. Mannheim
concluded that modafinil should not be approved for ADHD. On October 12, 2005,
Paul J. Andreason, M.D., the Acting Deputy Director of the DPP recommended an
approvable action for modafinil for ADHD. On October 19, 2005, Thomas P.
Laughren, M.D., the Director of the DPP recommended an approvable action for
modafinil for ADHD. On October 20, 2005, the FDA issued an approvable letter to
Cephalon for Sparlon, along with a proposal for labeling. Cephalon has a
conference call scheduled for tomorrow at 6:00 p.m. EST to discuss the results
of tomorrow's PDAC meeting.
As of Saturday, 03-18-2006 23:59, the latest Comtex SmarTrend(SM) Alert, an
automated pattern recognition system, indicated a DOWNTREND on 03-16-2006 for
CEPH @ $74.59. (C) 2006 Comtex News Network, Inc. All rights reserved.
LOAD-DATE: March 23, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Web Publication
Copyright 2006 Comtex News Network, Inc.
All Rights Reserved
Copyright 2006 TheFlyOnTheWall.com
413 of 998 DOCUMENTS
MarketWatch
March 16, 2006 Thursday 11:53 AM EST
Cephalon drops on FDA documents about new ADHD drug
BYLINE: Val Brickates Kennedy
LENGTH: 137 words
BOSTON (MarketWatch) -- Shares of Cephalon (ceph) dropped 5% to $74.24 Thursday
morning following reports that FDA briefing documents released earlier this week
indicate its proposed drug to treat attention deficit hyperactivity disorder
(ADHD), Sparlon, triggered suicidal and aggressive behavior in a small number of
users during a clinical trial. Sparlon, also known as modafinil, is slated to be
reviewed by an FDA advisory panel on March 23. Another FDA panel will be
discussing the safety of several leading ADHD drugs on March 22. The FDA
generally follows the recommendations of its advisory panels. Modafinil is
already marketed for the treatment of narcolepsy under the name Provigil.
©1997-2002 MarketWatch.com, Inc. All rights reserved. See details at
http://custom.marketwatch.com/custom/docs/useragreement.asp.
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414 of 998 DOCUMENTS
The Sunday Times (London)
March 12, 2006
Say goodbye to sleep
BYLINE: Graham Lawton
SECTION: FEATURES; Style; Pg. 44
LENGTH: 1511 words
And hello to 24-hour living. Graham Lawton reports on a new wave of drugs that
could help us stay awake for days and get a whole night's kip in just two hours
Between a hectic work schedule and a thriving social life, Yves (not his real
name), a 31-year-old software developer from Seattle, often doesn't have time
for a full night's sleep, so he swallows something to make sure he doesn't need
one.
"If I take a dose just before I go to bed, I can wake up after 4 or 5 hours and
feel refreshed," he says.
Yves is talking about modafinil, a stimulant that, since its launch seven years
ago, has acquired a near-mythical reputation for wiring you awake without the
jitters, euphoria and eventual crash that come after caffeine or amphetamines.
Yves has been popping modafinil on and off for three years, and says: "I'm more
organised and more motivated, and it means I can go out partying on a Friday
night and still go skiing early on Saturday morning."
Modafinil is just the first in a wave of new drugs that will enable us to
structure sleep to suit our lifestyles. "In 10 to 20 years, we'll be able to
pharmacologically turn off sleep," says Professor Russell Foster, a circadian
biologist at Imperial College London. Foster envisages a world where it is
possible, or even routine, for people to be active 22 hours a day and sleep for
two.
If that sounds unlikely, think about what is already here. Modafinil has made it
possible to have 48 hours of continuous wakefulness with few, if any, ill
effects.
New classes of sleeping pills are on the horizon that promise to deliver sleep
that is deeper and more refreshing than the real thing. Further down the line
are even more radical interventions: wakefulness promoters that can safely
abolish sleep for several days at a stretch, and sleeping pills that deliver
what feels like eight hours' sleep in half the time.
To some degree, we are already adept at controlling sleep. Most people in
full-time work deprive themselves of sleep during the week and catch up at the
weekend. We often augment our sleep-suppressing powers with caffeine, nicotine
or illegal stimulants such as cocaine and amphetamines. We are also dependent on
substances that help us to sleep. The vast majority of sleeping pills known as
hypnotics -are simply "knockout drops" that put you in a state almost like
sleep, but without its full restorative properties. With their addictive nature,
the drugs we use to keep us awake, such as coffee and amphetamines, are even
worse.
These sleeping and waking aids are driving ever more people into what Foster
calls the "stimulant-sedative loop", where they need nightly help getting to
sleep and daily help staying awake.
Modafinil has changed the rules of the game. The drug is what is known as a
eugeroic, meaning "good arousal" in Greek. It delivers natural-feeling alertness
and wakefulness, without the powerful physical and mental jolt that earlier
stimulants delivered. Perhaps the most remarkable thing about modafinil is that
users don't seem to have to pay back any "sleep debt". Normally, if you stayed
awake for 48 hours straight, you would have to sleep for about 16 hours to catch
up. Modafinil somehow allows you to catch up with only eight hours or so.
So how does modafinil work? Like other stimulant drugs, it prevents nerve cells
from reabsorbing, and so reduces the effect of, the excitatory neurotransmitter
dopamine once they release it into the brain. The difference is that it does so
without producing the addictive highs and painful crashes associated with most
stimulants. A number of independent studies suggest that this might be because
it also interferes with the reuptake of another neurotransmitter, noradrenaline.
However it works, modafinil is proving hugely successful. Sales in 2005 reached
about $575m (£ 330m). Cephalon, its maker, insists that the drug is for treating
"medical" sleepiness caused by diseases such as narcolepsy and sleep apnoea -it
is prescription-only. But it is clear that modafinil is becoming a lifestyle
drug for people such as Yves who want off-the-peg wakefulness.
All the indications are that modafinil is safe. In fact, it is hard to find
anyone with a bad word to say about it, except that there may be unseen problems
down the line, as the drug becomes more widely used. In the long run, it is
possible that casual users might have to keep upping their dose to get the same
effect. Neil Stanley, head of sleep research at the Human Psychopharmacology
Research Unit at the University of Surrey, has similar worries. "Is it a
potential drug of abuse?
Will it get street value?" he asks. "We'll see."
Cephalon does not seem to be worried, and modafinil's success has spurred it to
develop a successor, armodafinil. And the results of an experiment with a drug
called CX717 suggest that Cephalon won't have the field to itself for ever.
CX717 belongs to a class of drugs called ampakines, which ramp up brain activity
by enhancing the action of its main excitatory neurotransmitter, glutamate.
Cortex, the maker of CX717, originally saw the drug as a cognitive booster for
people with Alzheimer's, but it is its potential to counter the effects of sleep
deprivation that is attracting the most attention. Later this year, the Defense
Advanced Research Projects Agency (Darpa), the research arm of the US Department
of Defense, will put CX717 through its paces as a wakefulness promoter for
combat. It hopes that the drug will counteract sleep deprivation. "The early
signs are that people function better, their brain is a little more hyped. But
we haven't tested sleepiness directly," says Roger Stoll, chief executive of
Cortex.
It is easy to see why Darpa is interested. Soldiers on special operations
sometimes have to be awake, alert and active for 72 hours at a stretch, with
only minimal rest. That is like starting work on Monday morning and not stopping
until Thursday.
The military isn't just interested in wakefulness. It also has a keen interest
in the other side of the coin. John Caldwell of the US Air Force Research
Laboratory has spent most of his career testing the effects of stimulants and
sleep aids on pilots, and he has become aware that there is a quiet revolution
going on in sleep medicine. "There's a new idea out there," he says. "Drugs that
change sleep architecture (the different brain states that make up a full
night's sleep)."
In the past, says Caldwell, sleeping pills have generally suppressed the deepest
and most restorative "slow-wave" sleep in favour of shallower sleep. Now,
though, there are two new drugs in the offing (Merck's gaboxadol and Arena
Pharmaceuticals' APD125) that significantly increase the amount of slow wave
sleep. To Caldwell, these drugs hold out the promise of a power nap par
excellence. "Maybe you can make a short period of sleep more restorative by
filling it with slow-wave sleep," he says.
Much like modafinil, gaboxadol and APD125 are the start of something bigger. For
more than 35 years, sleeping pills have been a one-trick pony. If you wanted to
send someone to the land of nod, there was only one way of doing so -targeting
the neurotransmitter gamma-aminobutyric acid (gaba), which is the brain's
all-purpose dimmer switch. Manipulating the gaba system is a sure-fire way of
putting people to sleep, but it has its problems. The brain adapts to the drugs,
which means that most cannot be taken for more than a few days without losing
their potency, the groggy effects linger into the morning and many are
addictive. Last year, the first non-gaba sleeping pill (rozerem, made by the
Japanese firm Takeda) came onto the market, and there are at least three other
new classes of hypnotic that don't go near the gaba system.
According to Stanley, there is even more scope for improvement: "We are not that
far away from having drugs that put you to sleep for a certain length of time."
He predicts there could soon be tablets combining a hypnotic with an antidote or
wakefulness promoter designed to give you a sleep that lasts for a precise
number of hours. "A four-, five-or six-hour pill."
We seem to be moving inescapably towards a society where sleep and wakefulness
are available, if not on demand, then at least on request. Many sleep
researchers have nagging worries about the long-term impact of millions of us
using drugs to override the natural sleep-wake cycle. Stanley believes that
drugs such as modafinil and CX717 will tempt people to overdose on wakefulness
at the expense of sleep. Others point out that there are likely to be hidden
health costs to overriding natural sleep-wake cycles. Still, even the doubters
admit that we are too far down the road of the 24-hour society to turn back. For
millions of people, good sleep and productive wakefulness are already elusive,
night work or nightlife a reality, and the "stimulant-sedative" loop all too
familiar. As Jeffrey Vaught, the president of research at Cephalon, says: "We're
already there, so why not make it as clean and safe as possible?" 1 The full
version of this article appeared in New Scientist magazine
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Pediatric News
March 2006
Modafinil Offers New ADHD Option
BYLINE: Heidi Splete
SECTION: Pg. 32 Vol. 40 No. 3 ISSN: 0031-398X
LENGTH: 355 words
Modafinil film-coated tablets significantly improved the clinical symptoms of
attention-deficit hyperactivity disorder in children and adolescents aged 6-17
years, according to a new study by Dr. Joseph Biederman of Massachusetts General
Hospital in Boston and his colleagues.
Modafinil, an agent generally prescribed to promote wakefulness in patients
with narcolepsy, has been shown to activate the cortex alone. It lacks the
widespread nervous system stimulation that occurs in medications typically
prescribed for ADHD in children and adolescents.
In the randomized, double-blind trial conducted by Dr. Biederman and his
colleagues, 164 children received a flexible dose of modafinil in tablet form,
and 82 children received a placebo. The children began with one 85-mg tablet for
the first 2 days; the dose was titrated to 170 mg on days 3-7, 255 mg on days
8-14, 340 mg on days 15-21, and 425 mg on day 22 (Pediatrics 2005;116:777-84).
The dose varied with the patient's tolerance, and the maximum daily dose was
425 mg. The children were evaluated at baseline and at 1, 2, 3, 5, 7, and 9
weeks after starting treatment.
After 9 weeks, 48% of patients in the modafinil group were deemed responders,
compared with 17% of those in the placebo group. Overall, patients in the
modafinil group demonstrated significant improvement in symptoms, including
oppositional behavior, cognitive problems/inattention, hyperactivity, and the
ADHD index on the Conners' Parent Rating Scale Revised, Short Form, compared
with those in the placebo group.
Modafinil (Provigil) also was well tolerated. Only five of the patients in
the treatment group (3%) and three in the placebo group (4%) discontinued the
study because of adverse events. Most adverse events were mild to moderate, and
the only reported severe events were insomnia in one modafinil patient, erythema
multiforme in another modafinil patient, and headache in one placebo patient.
Given modafinil's safety profile and its low potential of abuse, the drug may
offer clinicians a new option for treating ADHD in children and adolescents, the
investigators said.
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Reuters Health Medical News
February 22, 2006 Wednesday 9:00 PM EST
Modafinil safe and effective for attention-deficit/hyperactivity disorder
SECTION: CLINICAL
LENGTH: 329 words
DATELINE: NEW YORK
A new formulation of modafinil (film-coated tablets) improves symptoms of
attention-deficit/hyperactivity disorder (ADHD) in children and adolescents, and
is well tolerated, according to a report in the January Journal of Clinical
Psychiatry.
Modafinil differs from central nervous system stimulants, the authors explain,
and it may reduce the symptoms of ADHD in the same way that it improves
wakefulness -- by selectively activating the cortex without generalized CNS
effects.
Dr. James M. Swanson from the University of California at Irvine and colleagues
assessed the efficacy and tolerability of modafinil in a 7-week
placebo-controlled study of 190 children and adolescents with ADHD, which was
followed by a 2-week evaluation after abrupt discontinuation of modafinil.
Modafinil-treated patients showed significant improvements in the ADHD Rating
Scale-IV School Version and Home Version scores, the results indicate, and
significantly more patients were rated by the investigators as "much improved"
or "very much improved" on a clinical global impression scale.
"These findings suggest consistent therapeutic effects of modafinil at school
and home during weekdays, evenings, and weekends as evaluated by clinicians,
teachers, and parents," the investigators write.
After abrupt discontinuation of modafinil, there were no adverse physical or
emotional effects, the researchers note, and there were no symptoms of
withdrawal or rebound of symptoms of ADHD.
Patients tolerated modafinil well, the report indicates, but insomnia and
decreased appetite were reported significantly more often with modafinil than
with placebo.
"Treatment of children with ADHD with modafinil was effective across the full
spectrum of symptoms of ADHD, including inattention, hyperactivity, and
impulsivity," Dr. Swanson and colleagues conclude. "These findings suggest that
modafinil may provide a novel therapeutic option for the management of ADHD in
pediatric and adolescent patients."
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The Express
February 18, 2006 Saturday
U.K. 1st Edition
Who needs eight hours a night? Sleeping is for wimps;
LEADER
BYLINE: David Robson
SECTION: LEADER; 12
LENGTH: 1494 words
THERE they were, tucked away just inside the entrance to my local London
underground station, tensed, like greyhounds in the traps, just waiting for
their moment.
Click the digital clock hit 8.59.58 they edge their way out 8.59.59 they
push their way through the crowd to the gates 9.00.00 they press their senior
citizens' travel passes down hard on the electronic pad and the gates do not
open.
"Seek assistance, " the machine says.
Seek assistance? Seek assistance! There were three of them, two men and a woman,
all in their late 60s or 70s and they didn't want assistance, they wanted their
rights;
and they weren't seeking, they were screaming.
"Look, it's 15 seconds past nine and the machine isn't letting us through it's
disgusting." "Disgraceful!" "What's going on?" The "assistance", a bloke in
royal blue uniform, was visibly shocked. He'd started to stammer some excuse
when the machines kicked in and the three were let through, seething. It was
9.00.50. What had we seen? Was it just bog standard Age Rage, the new British
disease that makes it unsafe for younger people to walk the streets during
daylight hours, or something altogether more complicated?
The travel passes Londoners can claim when they reach 60 give free travel on bus
and Tube. They are called Freedom Passes but, as you might expect in Blair's
Britain, freedom is far from unconfined.
The passes do not work between 4.30 and 9am.
Yes, you may think, Nanny Statism at its worst - it punishes law abiding
over-60s who favour all-night hip hop clubs and 24-hour drinking joints.
And then, you may think, older people aren't around much between 4.30 and 9am
anyway - which would just show how little you know.
NIGHT shift workers apart, I would wager that the majority of people awake in
Britain in the small hours are either under 25 or over 60. Those in between
spend lives of eight-hour-anight somnolence. But for many people, as they get
older, all-night sleep becomes a thing of the past. A four o'clock wake-up is
quite normal.
"Gosh, " they think. "Four twenty. I'll just take a leak [as you do] and then
I'll catch a night bus over to Jennifer's place for a drink oh, damn it all, my
bus pass won't work." Come to think of it, perhaps it's part of the Government's
campaign for lifelong learning.
What can you do when you wake up in the middle of the night? Well you can read,
or watch TV. What TV can you watch? Educational TV, that's what. True, in these
digital days, there's always porn and programmes about the fabulous lifestyle of
Paris Hilton to be had at any time of day or night but, late on, there's so much
that is "improving".
The BBC Learning Zone - chaps with beards, homeknitted sweaters and oldfashioned
glasses explaining the rudiments of astrophysics;
nice young women sauntering round shops in Madrid improving your language skills
(en que planta estan los zapatos? - which floor are the shoes on? ; me resulta
demasiado caro - it's too expensive for me). In the small hours, even football
is educational:
the Albanian second division, the Guatamalan junior cup.
You see places and hear names you never even knew existed.
Then at 7am, when UKTV History kicks in, you hear about the likes of Sir George
Cayley, the Yorkshireman who may or may not have invented the aeroplane, or you
can consider whether there was, or could have been, a roof on the Colosseum in
Rome.
It's only when you know what goes on in the small hours among ageing people of
non-sleeping disposition that you understand how a 45second delay on getting
your Freedom Pass to work might cause hyperventilation, or violence. That wasn't
just Age Rage; that was an explosion from the OU - the Overeducated Undead.
Apologies to those poor souls who feel their lives are blighted by insomnia but
I reckon "a good night's sleep" is vastly overrated.
"Three score years and 10 is such a stingy ration of time when there is so much
time around, " said the great science fiction writer Brian Aldiss.
"Perhaps that's why some of us are insomniacs; night is so precious that it
would be pusillanimous to sleep all through it. A 'bad night' is not always a
bad thing." Brian Aldiss has now passed four score years and I think he's right.
As James Thurber wrote: "Early to rise and early to bed/Makes a man healthy,
wealthy and dead." As far as I can see, there is only one real virtue in
sleeping long - when you're sleeping you can't be eating. That apart, it's good
to have more time to get on with things (needless to say it is nature's cruel
joke that old age, when we may have fewer things to get on with, is the age when
we are likely to sleep least).
People who really have to "get on with things" develop different sleep
strategies from the rest of us.
Napoleon, reportedly, rarely got a good night's sleep and took naps during the
day. He is believed to have suffered from apnoea (a condition that involves
heavy snoring) which makes it seem likely that his "not tonight Josephine" was
less frequent than her "not tonight Napoleon".
LEONARDO da Vinci was said to be a polyphasic sleeper - in other words he
catnapped 15 minutes at a time, every two hours. (Here is his hitherto unseen
diary from 1505-6: woke up got on with painting Mona Lisa's nose had a nap
moved on to the mouth had a nap started on her smile had a nap couldn't
remember whether she was supposed to be smiling or not had a nap decided on a
compromise had a nap finished her off had a nap slipped out for a cappuccino
with Michelangelo).
Ellen MacArthur obviously couldn't take extended kip during the 72 days of her
roundthe-world race. She averaged 5.5 hours a day broken up into 10 naps. In the
1994 race, a French sailor fell asleep and ran aground on the south western
coast of Australia. In 1990 Desmond Hampton allowed Sir Francis Chichester's
Gypsy Moth V to smash into rocks while he slept.
MacArthur had the assistance of Claudio Stampi of the Chronobiology Research
Institute in Boston, Massachusetts, who monitored and designed her sleep
patterns.
The advantage of short polyphasic naps in her circumstances are pretty obvious.
One is that it is the early stages of sleep that are most important in
recuperation - so 10 early stages are the way to do it; the other is that
lengthy slumbers are not appropriate when you've got a busy trimaran to run.
Though we talk about "beauty sleep" it is not proven that shortage of sleep has
any real physical effect on us. The brain needs rest but the body can get by
without it.
Recently there has been much talk, including in this week's New Scientist
magazine, about the drug modafinil, which may well prove able to cut our need
for sleep down to no more than a couple of hours a day. Millions have lived like
that with amphetamines, which leave you a) wired and jittery, and b) addicted.
Amphetamines may keep you awake but they don't do a lot for your judgment and
disposition.
MODAFINIL seems a quite different proposition. The American military took an
interest in it early:
American pilots flying bombladen B-2 stealth planes from Missouri to Afghanistan
were prone to errors and slow response time. But not those using modafinil. In
2004 American woman sprinter Kelli White tested positive for modafinil, an
illegal drug in athletics; she was stripped of her world 100m and 200m titles
and banned for two years. Her training partner, British sprinter Dwain Chambers,
also tested positive for the drug - his suspension from the sport has just
ended. The excuse for using modafinil in White's case, and others, was
"narcolepsy".
"It is a little odd to find an epidemic of narcolepsy among top athletes, " said
the head of the International Amateur Athletics Association's drugs commission.
Modafinil was developed to combat narcolepsy, an affliction which makes people
drift into sleep at random times but its broader role is giving users several
extra hours a day of top performance, healthy wakeful time.
Just as technologically-developed man strives to conquer the natural elements,
he also dreams of taking control of time, so that he can choose how much or
little time he sleeps and live to tell the tale (without babbling and
dribbling). At the 2004 European Championships England, captained by David
Beckham (who rarely dribbles), had a sleep consultant in the party. Their
mattresses were modified to give better slumbers. That same year artist Sam
Taylor Wood made a video of Beckham sleeping. He did it beautifully. It lasts 67
minutes - with modafinil that would be half a day's worth.
But does that appeal to you - 22 hours of wakefulness and possible workfulness?
Obviously sleep, if we can live happily without it, is nothing but a waste of
time. On the other hand, with increasingly long lives we may have time to waste.
Say what you will about sleep, it is at least environmentally friendly and it
keeps death off the roads (unless you happen to be driving). And if every
over-60 in Britain was awake 22 hours a day, I would not like to answer for the
consequences.
LOAD-DATE: February 19, 2006
LANGUAGE: ENGLISH
GRAPHIC: WAKE UP CALL : But how much sleep do we need to feel refreshed in the
morning?
PUBLICATION-TYPE: Newspaper
Copyright 2006 EXPRESS NEWSPAPERS
All Rights Reserved
418 of 998 DOCUMENTS
New Scientist
February 18, 2006
Get up and go;
A new wave of drugs will make it a breeze to go days without sleep, and give you
a good night's shut-eye in two hours. Are you ready for 24-hour living, asks
Graham Lawton
BYLINE: Graham Lawton
SECTION: FEATURES; Cover Story; Pg. 34
LENGTH: 3312 words
SO MUCH to do, so little time. Between a hectic work schedule and a thriving
social life, Yves (not his real name), a 31- year-old software developer from
Seattle, often doesn't have time for a full night's sleep. So he swallows
something to make sure he doesn't need one. "If I take a dose just before I go
to bed, I can wake up after 4 or 5 hours and feel refreshed," he says. "The
alarm goes off and I'm like, let's go!"
Yves is talking about modafinil, a stimulant that since its launch seven years
ago has acquired a near-mythical reputation for wiring you awake without the
jitters, euphoria and eventual crash that come after caffeine or amphetamines.
Yves has been popping modafinil on and off for the past three years and says it
is "tremendously useful". "I find I can be very productive at work," he says.
"I'm more organised and more motivated. And it means I can go out partying on a
Friday night and still go skiing early on Saturday morning."
Modafinil is just the first of a wave of new lifestyle drugs that promise to do
for sleep what the contraceptive pill did for sex - unshackle it from nature.
Since time immemorial, humans have structured their lives around sleep. In the
near future, we will, for the first time, be able to significantly structure the
way we sleep to suit our lifestyles.
"The more we understand about the body's 24-hour clock the more we will be able
to override it," says Russell Foster, a circadian biologist at Imperial College
London. "In 10 to 20 years we'll be able to pharmacologically turn sleep off.
Mimicking sleep will take longer, but I can see it happening." Foster envisages
a world where it's possible, or even routine, for people to be active for 22
hours a day and sleep for two. It is not a world that everyone likes the sound
of. "I think that would be the most hideous thing to happen to society," says
Neil Stanley, head of sleep research at the Human Psychopharmacology Research
Unit in the University of Surrey, UK. But most sleep researchers agree that it
is inevitable.
If that sounds unlikely, think about what is already here. Modafinil has made it
possible to have 48 hours of continuous wakefulness with few, if any, ill
effects. New classes of sleeping pills are on the horizon that promise to
deliver sleep that is deeper and more refreshing than the real thing. Further
down the line are even more radical interventions - wakefulness promoters that
can safely abolish sleep for several days at a stretch, and sleeping pills that
deliver what feels like 8 hours of sleep in half the time. Nor is it all about
drugs: one research team even talks about developing a wearable electrical
device that can wake your brain up at the flick of a switch.
To some degree, we are already adept at controlling sleep. Most people in
full-time work deprive themselves of sleep during the week, deliberately or
otherwise, and catch up at the weekend. We often augment our sleep-suppressing
powers with caffeine, nicotine or illegal stimulants such as cocaine and
amphetamines. We are also highly dependent on substances that help us sleep.
According to some estimates, 75 per cent of adults suffer at least one symptom
of a sleep problem a few nights a week or more. In 1998, a team from the Henry
Ford Health Sciences Research Institute in Detroit, Michigan, published a study
revealing that 13 per cent of adult Americans had used alcohol to help them get
to sleep in the previous year, and 18 per cent had used sleeping pills (Sleep ,
vol 21, p 178).
Despite the enormous resources that we pour into getting good sleep and
wakefulness when we want them, most of the drugs at our disposal are crude
instruments at best. The vast majority of sleeping pills - known in the business
as hypnotics - are simply "knockout drops" that put you in a state almost like
sleep but without its full restorative properties. "Hypnotic-induced sleep is
better than no sleep, but it isn't natural sleep," says Stanley. With their
addictive nature, the drugs we use to keep us awake, such as coffee and
amphetamines, are even worse. In combination with our clock-watching lifestyles,
these sleep and wake aids are driving ever more people into what Foster calls
the "stimulant-sedative loop" where they need nightly help getting to sleep and
daily help staying awake.
Modafinil has changed the rules of the game. The drug is what's known as a
eugeroic, meaning "good arousal" in Greek. It delivers natural-feeling alertness
and wakefulness without the powerful physical and mental jolt that earlier
stimulants delivered. "There are no amphetamine-like feelings," says Yves. And
as Yves' way of taking it shows, being on modafinil doesn't stop you from
falling asleep if you want to.
In fact, its effects are so subtle that many users say they don't notice
anything at all - until they need to. "I wouldn't say it makes me feel more
alert or less sleepy. It's just that thoughts of tiredness don't occur to me,"
says Yves. "If there's a job at hand that I should be doing, I'm focused, but if
I'm watching a movie or something, there is no effect."
People who take modafinil for medical reasons usually take just enough of the
drug in the morning to see them through the day, but it also seems to be able to
deliver sustained wakefulness - for a couple of days at least. "The military has
tested sequential dosing," says Jeffrey Vaught, president of R&D at Cephalon,
modafinil's Pennsylvania-based manufacturer. "It works for 48 hours or so, but
eventually you need to sleep."
Perhaps the most remarkable thing about modafinil is that users don't seem to
have to pay back any "sleep debt". Normally, if you stayed awake for 48 hours
straight you would have to sleep for about 16 hours to catch up. Modafinil
somehow allows you to catch up with only 8 hours or so. Well before Cephalon
took an interest in the drug, French researchers discovered this effect in cats
back in the early 1990s (Brain Research , vol 591, p 319), and it has since been
found to apply to humans too.
So how does modafinil work? "No one really knows," admits Vaught. He says that
Cephalon thinks it understands the drug, but is keeping the details under wraps.
What is clear is that, like other stimulant drugs, modafinil prevents nerve
cells from reabsorbing the excitatory neurotransmitter dopamine once they
release it into the brain. The difference is that it somehow does so without
producing the addictive highs and painful crashes associated with most
stimulants. A number of independent studies suggest that this might be because
it also interferes with the reuptake of another neurotransmitter, noradrenalin.
However it works, modafinil is proving hugely successful. Since it hit the
market in 1998, sales have been climbing steadily - from $25 million in 1999 to
around $575 million in 2005. Cephalon insists that the drug is for treating
"medical" sleepiness caused by diseases such as narcolepsy and sleep apnoea.
Even so, it's clear that modafinil is becoming a lifestyle drug for people like
Yves who want off-the-peg wakefulness. "At first I got it from a friend, and
then I got diagnosed as a narcoleptic online," says Yves.
All the indications are that modafinil is extremely safe. The drug can have side
effects, most commonly headaches, but up to now there have been no severe
reactions, says Vaught. In fact, it is hard to find anyone with a bad word to
say about modafinil, except that there may be unseen problems down the line as
the drug becomes more widely used. "I think it's unlikely that there can be an
arousal drug with no consequences," says Foster. In the long run, it is possible
that casual users might have to keep upping their dose to get the same effect.
Stanley has similar worries. "Is it a potential drug of abuse?" he asks. "Will
it get street value? We'll see."
Cephalon does not seem to be worried. Modafinil's success has spurred it to
develop a successor, armodafinil. The company is also developing other eugeroics
- one experimental drug called CEP-16795 switches off the H3 histamine receptor,
which appears to be one of the molecular switches that controls the sleep-wake
cycle. However, Vaught claims that the original will be a tough act to follow. "
Modafinil is very effective and very safe," he says. "How do you beat it?"
There are ideas as to how. Last year, Sam Deadwyler of Wake Forest University in
Winston-Salem, North Carolina, reported the results of an experiment with a drug
called CX717. The findings suggest that modafinil won't have the field to itself
forever.
Deadwyler kept 11 rhesus monkeys awake for 36 hours, throughout which they
performed short-term memory and general alertness tests (Public Library of
Sciences Biology , vol 3, p 299). At that level of sleep deprivation, a monkey's
performance would normally drop to the point where it could barely function at
all, but Deadwyler found that CX717 had remarkable restorative powers. Monkeys
on the drug were doing better after 36 hours of continual wakefulness than
undrugged monkeys after normal sleep. When Deadwyler imaged their brains with
functional magnetic resonance imaging, (fMRI), he found that the drug maintained
normal activity even in severely sleep-deprived individuals. The results build
on those of an earlier, small-scale trial on 16 men that found CX717 could
largely reverse the cognitive decline that comes with 24 hours of sleep
deprivation (New Scientist , 14 May 2005, p 6).
Soldiers get high
CX717 belongs to a class of drugs called ampakines, which subtly ramp up brain
activity by enhancing the action of its main excitatory neurotransmitter,
glutamate. Cortex Pharmaceuticals of Irvine, California, which developed CX717,
originally saw the drug as a cognitive booster for people with Alzheimer's, but
it is its potential to counter the effects of sleep deprivation that is
attracting the most attention.
Later this year, the Defense Advanced Research Projects Agency (DARPA), based in
Arlington, Virginia, will put CX717 through its paces as a wakefulness promoter
for combat. In an experiment designed to mimic the harsh demands of special ops,
investigators will push 48 volunteers to the limit - four consecutive nights of
hard work with only 4 hours of recovery sleep in between. "They'll go from being
tired to exhausted to crashing," says Roger Stoll, Cortex's chief executive. For
some of them, however, the ordeal will be softened by regular doses of CX717.
DARPA hopes the drug will counteract the sleep deprivation.
The trial should help answer some outstanding questions about CX717's potential.
"We don't know yet if it eliminates feelings of sleepiness," says Stoll. "The
early signs are that people function better, their brain is a little more hyped.
But we haven't tested sleepiness directly." As with modafinil, the evidence
suggests that people struggle to tell if they're on the drug or not, and that
hasn't turned out to be much of a problem for modafinil.
Whatever the outcome of the DARPA trial, CX717 won't be the last word on
eugeroics. Stoll says Cortex has similar but more powerful molecules up its
sleeve. Thought they are being developed mainly as memory enhancers, some may
turn out to be powerful wakefulness promoters too. Industry giants
GlaxoSmithKline and Eli Lilly have ampakine programmes of their own, and at
least one other company, Arena Pharmaceuticals of San Diego, California, has
declared an interest in wakefulness promoters, though it hasn't released any
details of its research.
When and if those drugs come through, the US military is sure to be interested.
DARPA is one of the most active players in the drive to conquer sleep, setting
up and funding much of the basic research on wakefulness. The army and air force
have research programmes too.
It's easy to see why DARPA is interested. "We make the assumption that soldiers
are going to be sleep-deprived," says DARPA neuroscientist Amy Kruse, who runs
the agency's sleep-deprivation research programme. "We want to know what we can
do to bring them back up to the level they would be at if they had a good
night's sleep."
When DARPA talks about sleep deprivation, it really means it. Soldiers on
special ops sometimes have to be awake, alert and active for 72 hours at a
stretch with only minimal rest. That's like starting work on Monday morning and
not stopping until Thursday. "Three days, that's when they really start
hurting," says Kruse.
The military has a long history of using caffeine and amphetamines to get its
people through. It has now added modafinil to the list, and is clearly
interested in CX717. And Kruse says she is confident that there is lots of room
for further improvement.
Last year, a DARPA-funded team led by Giulio Tononi at the University of
Wisconsin Madison discovered a strain of fruit flies that gets by on just a
third the normal amount of sleep. The "minisleep" mutant carries a change to a
single gene, encoding a protein involved in potassium transport across cell
membranes. Intriguingly, defects in potassium channels are associated with
reduced sleep in humans, particularly in the autoimmune disease Morvan's
syndrome, one symptom of which is chronic sleeplessness. What that suggests,
says Kruse, is that new drugs designed to latch onto potassium channels in the
brain could radically alter the need for sleep. There are also likely to be
other molecular targets in the brain just waiting to be exploited, she says.
DARPA is meanwhile pursuing other strategies to conquer sleep deprivation. At
Yaakov Stern's lab at Columbia University in New York, DARPA-funded
neuroscientists have used fMRI to image the brains of sleep-deprived people, to
find out which regions are affected when you are very tired. Then they used a
transcranial magnetic stimulation (TMS) machine - routinely used to switch
localised brain regions on and off - to switch off those areas and see if that
reversed the effects.
"This is all proof of concept," says Stern. "It's hard to imagine a sleep
deprived pilot using TMS," not least because the machines are too bulky to fit
in a cockpit. "The next step is to apply TMS before or during sleep deprivation
to see if it blunts the effect. That has more of a shot at a lasting effect."
Stern says his team is also looking into a new technique called DC brain
polarisation, which has similar brain-boosting effects to TMS but uses DC
current instead of magnetism. The beauty of this "poor man's TMS" is that the
equipment is significantly smaller and cheaper - it could even be incorporated
into headgear that gives you a jolt of wakefulness at the flick of a switch. And
then there's always neurofeedback - training people to activate the brain
regions that get hit by sleep deprivation, effectively willing themselves awake.
The military isn't just interested in wakefulness. It also has a keen interest
in the other side of the coin. John Caldwell works at the US Air Force Research
Laboratory in San Antonio, Texas. He has spent most of his career testing the
effects of stimulants, including modafinil, on pilots. "I'm the guy who puts
sleep-deprived pilots in a plane, gives them drugs and says, did it work?" he
says. He has also done a handful of studies on sleep aids - testing the best way
to help night pilots sleep well during the day, for example. In recent months
Caldwell has become aware that there is a quiet revolution going on in sleep
medicine. "There's a new idea out there," he says. "Drugs that change sleep
architecture."
Sleep researchers have known for over 50 years that sleep isn't merely a lengthy
period of unconsciousness, but consists of several different brain states . How
those states are put together to build a full night's sleep is called sleep
architecture.
Catching the slow waves
In the past, says Caldwell, sleeping pills were designed not to mess with sleep
architecture, although they generally do, suppressing the deepest and most
restorative "slow-wave" sleep in favour of shallower stage 2 sleep. Now, though,
modifying sleep architecture is seen as the way forward. There are two new drugs
in the offing that significantly increase the amount of slow-wave sleep. One of
them, gaboxadol, made by Merck, is in phase III clinical trials and could be on
the market next year. To Caldwell these drugs hold out the promise of a power
nap par excellence. "Maybe you can make a short period of sleep more restorative
by filling it with up with slow-wave sleep," he says.
Much like modafinil, gaboxadol and the other slow-wave sleep promoter - Arena
Pharmaceuticals' APD125, currently in phase II - are the start of something
bigger. For more than 35 years, sleeping pills have been a one-trick pony. If
you wanted to send someone to the land of nod, there was only one way of doing
so - targeting the neurotransmitter GABA, which is the brain's all-purpose
dimmer switch. Old-fashioned hypnotics such as barbiturates and benzodiazepines
work by making neurons more sensitive to the soporific effects of GABA. It's
also why alcohol makes you sleepy. Even the newer, cleaner sleeping pills, such
as the market leader Ambien, work through the GABA system.
Manipulating the GABA system is a sure-fire way of putting people to sleep, but
it has its problems. One is that the brain adapts to the drugs, which means that
most cannot be taken for more than a few days without losing their potency. The
effects often linger well into the morning, making people feel groggy and hung
over. Many are also addictive.
What's more, sleep quality has rarely been considered. "In the past we would
take a hypnotic and say, does it put you to sleep?," says Stanley. "That's a
pretty inexact way of dealing with it. In that respect, alcohol is a good
hypnotic." Now, however, there is a recognition that there is much more to sleep
than the GABA system. Last year the first non-GABA sleeping pill came onto the
market - the first new class of hypnotic for 35 years. Rozerem, made by Japanese
firm Takeda, mimics the effects of the sleep-promoting hormone melatonin. Nor is
it the only one. There are at least three other new classes of hypnotic that
don't go anywhere near the GABA system. And though gaboxadol works through GABA,
it hits a type of receptor that has never been targeted by drugs before.
According to Stanley, there is even more scope for improvement. "It is possible
that pharmaceuticals will allow you a condensed dose of sleep," he says, "and we
are not that far away from having drugs that put you to sleep for a certain
length of time." He predicts you could soon have tablet combining a hypnotic
with an antidote or wakefulness promoter designed to give you a precise number
of hours' sleep. "A 4, 5 or 6-hour pill."
We seem to be moving inescapably towards a society where sleep and wakefulness
are available if not on demand then at least on request. It's not surprising,
then, that many sleep researchers have nagging worries about the long-term
impact of millions of us using drugs to override the natural sleep-wake cycle.
Stanley believes that drugs like modafinil and CX717 will tempt people to
overdose on wakefulness at the expense of sleep. "Being awake is seen to be
attractive," he says. "It's not cool to be asleep." Foster has similar worries.
"It seems like that technology will help us cope with 24/7, but is coping really
living?" he asks. Others point out that there are likely to be hidden health
costs to overriding our natural sleep-wake cycles. "Pharmaceuticals cannot
substitute for normal sleep," says Vaught.
Still, even the doubters admit that to all intents and purposes we are already
too far down the road of the 24-hour society to turn back. For millions of
people, good sleep and productive wakefulness are already elusive, night work or
nightlife a reality, and the "stimulant-sedative" loop all too familiar. As
Vaught puts it, "We're already there." So why not make it as clean and safe as
possible?
LOAD-DATE: February 18, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
Copyright 2006 Reed Business Information, UK, a division of Reed Elsevier Inc.
All Rights Reserved
419 of 998 DOCUMENTS
The International Herald Tribune
February 6, 2006 Monday
Biker waits for a dream ruling;
CYCLING
BYLINE: Sam Abt
SECTION: SPORT; Pg. 18
LENGTH: 700 words
DATELINE: PARIS
They say there's no rest for the weary, and the woeful proof of that is Franck
Bouyer, so weary, so very weary, and so far from restful.
Partly it's physical. Bouyer is the French bicycle racer who is as well known
for a few small but sweet victories as for the fact that he has narcolepsy, a
disorder that is marked by recurring, unpredictable episodes of sleep during
normal waking hours and disturbed sleep at night. He was diagnosed with this
genetic disease late in 2003.
''Still the same at night sleep a little, wake up, stay up, back to sleep a
while, wake up,'' Bouyer, who will be 32 in March, said in a phone interview
last week from the Etoile de Besseges race in the south of France.
''During the day, though, everything's fine,'' he added. During the day is when
he takes his medicine.
But the use of the medicine, called modafinil, is the reason he is weary
psychologically. Because of modafinil, Bouyer has appeared in court lately as
often as Perry Mason.
His latest testimony was given in January, half a year after he thought he had
been cleared to use the medicine while he competed in races. In August, the
World Anti-Doping Agency ruled that modafinil did not enhance his performance
illegally and that he could take it while competing.
That decision was a reversal, since the agency had ruled five months earlier in
a court case that the medication was banned.
Pierre-Yves Mathe, the doctor for Bouyer's Bouygues Telecom team, was shocked by
the first decision. He pointed out that a French doctor had refused to issue
Bouyer's racing license unless he was using the drug. Without it, the doctor
felt, the rider was too prone to falling asleep and causing crashes.
''We're caught between two contradictions,'' Mathe said. ''On the one hand, he
won't get his license to race unless he takes the drug; on the other, he can't
race if he takes the drug.''
Bouyer was puzzled, too. ''They're talking about enhanced performances,'' he
said, ''but what they don't take into account is that, without my medicine, I
wake up at 3 o'clock in the night because my sleep is so disturbed. What
consequences does that have on my performance?
''They allow racers who have failed three drug tests to continue, but they shove
aside somebody who's really sick.''
Then, on appeal, the World Anti-Doping Agency cleared him, and Bouyer began
racing again.
''I didn't have any good results,'' he said on the phone, ''because it was so
late in the season to begin. But I worked very hard this winter, did a lot of
training and was ready to go this month except that it didn't turn out to be
that simple.''
In what his lawyer, Philippe Senmartin, characterized as a turf war, the
International Cycling Union, which governs the sport, took exception to the
decision by the World Anti-Doping Agency and brought suit in the Court of
Arbitration for Sport in Switzerland. Modafinil remains banned by the cycling
union, which often chafes at the anti-doping agency's jurisdiction.
Back onto the witness stand went Bouyer last month.
Without his medication, he has testified, he can doze off at any moment, even on
the open road amid a pack of other riders. Let that occur, and the result can be
a mass crash.
It has not happened that way yet, he says, but he has fallen asleep while
training alone near his home in southwestern France.
''One time I found myself in the courtyard of a farm, woken up by a barking dog
without knowing how I got there,'' Bouyer has said.
Similarly, a photograph of him at the Bouygues Telecom team's presentation of
its riders last year showed him sitting in a chair with his eyes closed, deep in
the sandman's embrace while his praises were being sung onstage.
He was having no such problems in the Etoile de Besseges, he noted on the phone,
since he was back on his medication. ''With it,'' he said, ''I can continue my
career. Without it ... '' He left the sentence incomplete.
''We expect a decision in four to six weeks,'' he continued. ''It's a long time
to wait, but meanwhile I'm racing.
''All these court appearances, meetings with my lawyer, waiting for decisions
they wear you out,'' he said, with a yawn. ''Both sides have experts, and they
don't agree.'' Another yawn. ''It's exhausting.''
LOAD-DATE: February 6, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2006 International Herald Tribune
All Rights Reserved
420 of 998 DOCUMENTS
US Fed News
February 6, 2006 Monday 7:00 AM EST
French Inventors Develop Modafinil Polymorphic Forms
BYLINE: US Fed News
LENGTH: 188 words
DATELINE: Alexandria, Va.
ALEXANDRIA, Va., Feb. 6 -- Véronique Broquaire of Noisy le Onaud, France,
Ludovic Broquaire of Bagnois en Foret, France, Laurent Courvoisier of
Laigneville, France, Armand Frydman of Verrieres-le-Buisson, France, Gerard
Coquerel of Boos, France, and Franck Mallet of Blangy sur Bresle, France, have
developed modafinil polymorphic forms of modafinil racemate, methods of
preparation thereof, pharmaceutical compositions and methods of therapeutic
treatment involving modafinil polymorphic forms, the U.S. Patent & Trademark
Office announced.
The inventors were issued U.S. Patent No. 6,992,219 on Jan. 31.
The patent has been assigned to Cephalon France, Maisons-Alfort, France.
The original application was filed on Aug. 7, 2003, and is available at:
http://patft.uspto.gov/netacgi/nph-Parser?Sect1=PTO2&Sect2=HITOFF&u=/netahtml/se
arch-adv.htm&r=1568&f=G&l=50&d=PTXT&s1=ISYMD-20060131&p=32&OS=ISD/01/31/2006&RS=
ISD/01/31/2006.
For more information about US Fed News federal patent awards please contact:
Myron Struck, Managing Editor/US Bureau, US Fed News, Direct: 703/866-4708,
Cell: 703/304-1897, Myron@targetednews.com.
LOAD-DATE: February 7, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 HT Media Ltd.
All Rights Reserved
421 of 998 DOCUMENTS
Cancer Drug News
Pharmaceuticals
February 2, 2006
Barr/Cephalon enter agreements regarding settlement of Actiq and Provigil patent
litigations
LENGTH: 684 words
Barr Laboratories has entered into agreements to settle its pending patent
infringement disputes in the US related to Cephalon 's Actiq (oral transmucosal
fentanyl citrate) [C-II] and Provigil ( modafinil ) Tablets [C-IV] products. The
companies have entered into a supplemental licence agreement (SLA) related to
Actiq, which supplements the licence Cephalon previously granted Barr, pursuant
to an FTC Order, in mid-2004. The existing licence grants Barr a non-exclusive
right to sell a generic version of Actiq, which is indicated for the management
of breakthrough cancer pain in patients with malignancies who are already
receiving and who are tolerant to opioid therapy for their underlying persistent
cancer pain, effective on the earlier of final approval of Cephalon's fentanyl
effervescent buccal tablet or 3rd February 2007, if Cephalon receives a
paediatric extension for Actiq (or 5th September 2006, if Cephalon does not
receive the extension). The SLA ensures that Barr will be allowed to enter the
market no later than 6th December 2006, two months earlier than the 6th February
2007 date. The SLA will go into effect only if the existing licence is not
otherwise effective on 6th December 2006, and will remain in effect until the
existing licence becomes effective. During the term of the supplemental licence,
Barr will have an exclusive royalty-bearing right to market and sell a generic
version of Actiq in the US, and Cephalon will not market or sell, nor shall it
license or authorise a third party to market or sell, a generic version of
Actiq.
The SLA will cease to be effective when the existing licence agreement becomes
effective. After that date, Barr's rights will be controlled by the terms of the
existing licence. In connection with the modafinil settlement, Cephalon will
grant Barr a non-exclusive royalty-bearing right to market and sell a generic
version of Provigil, which is indicated for the treatment of excessive
sleepiness associated with shift-work sleep disorder, in the US. Barr's licence
will become effective in October 2011, unless Cephalon obtains a paediatric
extension for Provigil, which would permit entry by Barr in April 2012. An
earlier entry by Barr may occur based upon the entry of another generic version
of Provigil. Barr and Cephalon have also agreed to a series of business
arrangements related to modafinil. Specifically, Barr has agreed to grant to
Cephalon a non-exclusive licence, effective immediately, to certain of its
worldwide intellectual property rights related to modafinil in exchange for an
up-front payment. Cephalon has also agreed to purchase certain existing and
in-process inventory of the active pharmaceutical ingredient, modafinil. The
terms of the agreements are confidential and are subject to review by the FTC.
Financial terms were not disclosed. The parties will promptly file a dismissal
with the US District Courts for the Districts of New Jersey and Delaware that
will conclude pending litigation between the parties regarding Provigil and
Actiq, respectively. This settlement and the previously-announced settlements
with Teva Pharmaceutical Industries and its affiliate, Ranbaxy Laboratories ,
and Mylan Pharmaceuticals resolve the Provigil litigation with all four firms
that Cephalon understands were the first to submit ANDAs with Paragraph IV
certifications to the FDA. As such, Teva, Ranbaxy, Mylan and Barr would be
granted the 180-day exclusivity provided by the provisions of the Federal Food,
Drug, and Cosmetic Act. The separate, ongoing Provigil patent litigation between
Cephalon and Carlsbad Technology , pending in the US District Court in New
Jersey, is unaffected by these settlements. The lawsuit against Carlsbad claims
infringement of Cephalon's US Patent No. RE37,516, which covers pharmaceutical
compositions and methods of treatment with the form of modafinil contained in
Provigil. This patent expires on 6th October 2014 and may be extended by six
months (to 6th April 2015), upon acceptance by the FDA of the paediatric study
data that was submitted by the company on 21st December 2005.
LOAD-DATE: February 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
422 of 998 DOCUMENTS
PR Newswire US
February 2, 2006 Thursday 12:33 AM GMT
Barr Announces Agreements with Cephalon, Inc. Regarding Settlement of ACTIQ(R)
and PROVIGIL(R) Patent Litigations
LENGTH: 1166 words
DATELINE: WOODCLIFF LAKE, N.J. Feb. 1
WOODCLIFF LAKE, N.J., Feb. 1 /PRNewswire-FirstCall/ -- Barr Pharmaceuticals,
Inc. (NYSE:BRL) today announced that its subsidiary, Barr Laboratories, Inc.,
and Cephalon, Inc. have entered into agreements to settle its pending patent
infringement disputes in the United States related to Cephalon's ACTIQ(R) (oral
transmucosal fentanyl citrate) [C-II] and PROVIGIL(R) (modafinil) Tablets [C-IV]
products.
"We are pleased that these agreements allow both parties to resolve pending
patent litigation in a way that ensures that Barr can launch generic fentanyl at
least 90 days prior to the expiration of any pediatric exclusivity period
Cephalon might obtain on ACTIQ and can launch generic modafinil prior to patent
expiry," said Bruce L. Downey, Barr's Chairman and Chief Executive Officer.
Barr and Cephalon have entered into a Supplemental License Agreement related to
ACTIQ, which supplements the license Cephalon previously granted Barr, pursuant
to a Federal Trade Commission Order, in mid-2004. The existing license grants
Barr a non-exclusive right to sell a generic version of ACTIQ effective on the
earlier of final approval of Cephalon's fentanyl effervescent buccal tablet
(FEBT) or February 3, 2007, if Cephalon receives a pediatric extension for ACTIQ
(or September 5, 2006, if Cephalon does not receive the extension). The
Supplemental License Agreement ensures that Barr will be allowed to enter the
market no later than December 6, 2006 - two months earlier than the February 6,
2007 date.
The Supplemental License Agreement will go into effect only if the existing
license is not otherwise effective on December 6, 2006 and will remain in effect
until the existing license becomes effective. During the term of the
Supplemental License, Barr will have an exclusive royalty-bearing right to
market and sell a generic version of ACTIQ in the United States, and Cephalon
will not market or sell, nor shall it license or authorize a third party to
market or sell, a generic version of ACTIQ. The Supplemental License Agreement
will cease to be effective when the existing license agreement becomes
effective. After that date, Barr's rights will be controlled by the terms of
the existing license.
In connection with the modafinil settlement, Cephalon will grant Barr a
non-exclusive royalty-bearing right to market and sell a generic version of
PROVIGIL in the United States. Barr's license will become effective in October
2011, unless Cephalon obtains a pediatric extension for PROVIGIL which would
permit entry by Barr in April 2012. An earlier entry by Barr may occur based
upon the entry of another generic version of PROVIGIL.
Barr and Cephalon also agreed to a series of business arrangements related to
modafinil. Specifically, Barr has agreed to grant to Cephalon a non- exclusive
license, effective immediately, to certain of its worldwide intellectual
property rights related to modafinil in exchange for an upfront payment.
The terms of the agreements are confidential, and are subject to review by the
Federal Trade Commission. Financial terms were not disclosed.
The parties will promptly file a dismissal with the United States District
Courts for the Districts of New Jersey and Delaware that will conclude pending
litigation between the parties regarding PROVIGIL and ACTIQ, respectively.
About Barr Pharmaceuticals, Inc.
Barr Pharmaceuticals, Inc. is a holding company whose principal subsidiaries,
Barr Laboratories, Inc. and Duramed Pharmaceuticals, Inc., develop, manufacture
and market generic and proprietary pharmaceuticals.
Forward-Looking Statements
Except for the historical information contained herein, the statements made in
this press release constitute forward-looking statements within the meaning of
Section 27A of the Securities Act of 1933 and Section 21E of the Securities
Exchange Act of 1934. Forward-looking statements can be identified by their use
of words such as "expects," "plans," "projects," "will," "may," "anticipates,"
"believes," "should," "intends," "estimates" and other words of similar meaning.
Because such statements inherently involve risks and uncertainties that cannot
be predicted or quantified, actual results may differ materially from those
expressed or implied by such forward-looking statements depending upon a number
of factors affecting the Company's business. These factors include, among
others: the difficulty in predicting the timing and outcome of legal
proceedings, including patent-related matters such as patent challenge
settlements and patent infringement cases; the outcome of litigation arising
from challenging the validity or non- infringement of patents covering our
products; the difficulty of predicting the timing of FDA approvals; court and
FDA decisions on exclusivity periods; the ability of competitors to extend
exclusivity periods for their products; our ability to complete product
development activities in the timeframes and for the costs we expect; market and
customer acceptance and demand for our pharmaceutical products; our dependence
on revenues from significant customers; reimbursement policies of third party
payors; our dependence on revenues from significant products; the use of
estimates in the preparation of our financial statements; the impact of
competitive products and pricing on products, including the launch of authorized
generics; the ability to launch new products in the timeframes we expect; the
availability of raw materials; the availability of any product we purchase and
sell as a distributor; the regulatory environment; our exposure to product
liability and other lawsuits and contingencies; the increasing cost of insurance
and the availability of product liability insurance coverage; our timely and
successful completion of strategic initiatives, including integrating companies
and products we acquire and implementing our new enterprise resource planning
system; fluctuations in operating results, including the effects on such results
from spending for research and development, sales and marketing activities and
patent challenge activities; the inherent uncertainty associated with financial
projections; changes in generally accepted accounting principles; and other
risks detailed from time-to-time in our filings with the Securities and Exchange
Commission, including in our Annual Report on Form 10-K for the fiscal year
ended June 30, 2005.
The forward-looking statements contained in this press release speak only as of
the date the statement was made. The Company undertakes no obligation (nor does
it intend) to publicly update or revise any forward-looking statements, whether
as a result of new information, future events or otherwise, except to the extent
required under applicable law.
First Call Analyst:
FCMN Contact: apeden@barrlabs.com
CONTACT: Carol A. Cox, +1-201-930-3720, ccox@barrlabs.com
Web site: http://www.barrlabs.com/
Company News On-Call: http://www.prnewswire.com/comp/089750.html
SOURCE Barr Pharmaceuticals, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: February 2, 2006
LANGUAGE: ENGLISH
NOTES: NOTE TO EDITORS: Barr Pharmaceuticals, Inc. news releases are available
free of charge through PR Newswire's News On-Call site at
http://www.prnewswire.com/comp/089750.html. Barr news releases and corporate
information are also available on Barr's website (www.barrlabs.com). For
complete indications, warnings and contraindications, contact Barr Laboratories'
Product Information Department at 1-800-Barr Lab. All trademarks referenced
herein are the property of their respective owners.
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
423 of 998 DOCUMENTS
Clinical Psychiatry News
February 2006
Narcolepsy Drug Is Safe, Effective for ADHD
BYLINE: Michele G. Sullivan, Mid-Atlantic Bureau
SECTION: Pg. 34 Vol. 34 No. 2 ISSN: 0270-6644
LENGTH: 408 words
TORONTO - Modafinil is safe and effective in treating pediatric
attention-deficit hyperactivity disorder, decreasing symptom scores twice as
much as placebo, according to two posters presented at the joint annual meeting
of the American Academy of Child and Adolescent Psychiatry and the Canadian
Academy of Child and Adolescent Psychiatry.
The posters, sponsored by Cephalon Inc., concluded that children tolerated
the film-coated tablets well in dosages of up to 425 mg/day. Insomnia, headache,
and decreased appetite were the most commonly reported adverse events. Those
adverse events typically occurred during the first 2 weeks of therapy and
decreased thereafter, said Dr. Christopher Kratochvil of the University of
Nebraska.
The posters analyzed three multicenter, double-blind studies that included a
total of 633 children aged 6-17 years. Two of the studies were identical 9-week
flexible-dosing trials. The third was a 7-week fixed-dose placebo-controlled
study (340 or 425 mg/day), followed by a 2-week period in which half the
modafinil group was switched to placebo without tapering while the other half
continued modafinil treatment.
Adverse events were more common in the active group than the placebo group
and included insomnia (27% vs. 4%), headache (20% vs. 13%), and decreased
appetite (16% vs. 3%).
The adverse events were all classified as mild to moderate. They peaked in
the first 2 weeks of treatment and subsequently subsided. No apparent
association was found between adverse events and dosage.
There were no significant changes in heart rate or blood pressure between the
groups, and the abrupt discontinuation of the drug did not lead to acute
withdrawal symptoms or rebound effects.
The drug effectively reduced the symptoms of ADHD, especially hyperactivity
and inattention, reported Dr. Joseph Biederman of Massachusetts General
Hospital. The effects were consistent whether assessed by physician, parent, or
teacher.
Physicians assessed almost 50% of the active groups as much improved at the
end of treatment, compared with 20% of the placebo group.
Parents and teachers rated symptom improvement of those in the active group
at about twice that of the placebo group in all areas: oppositional behavior,
inattention, and hyperactivity.
Symptom improvement differed significantly from placebo at week 2 of
treatment and continued to diverge throughout the course of all three studies.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2006 Elsevier Inc., International Medical News Group
All Rights Reserved
424 of 998 DOCUMENTS
PR Newswire US
February 1, 2006 Wednesday 10:50 PM GMT
Cephalon, Inc. Announces Agreements With Barr Laboratories, Inc. Regarding
Settlement of PROVIGIL(R) and ACTIQ(R) Patent Litigations
LENGTH: 1280 words
DATELINE: FRAZER, Pa. Feb. 1
FRAZER, Pa., Feb. 1 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that it has entered into agreements with Barr Laboratories, Inc.
to settle its pending patent infringement disputes in the United States related
to PROVIGIL(R) (modafinil) Tablets [C-IV] and ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II].
"This is a transformational event for Cephalon," said Frank Baldino, Jr.,
Chairman and Chief Executive Officer. "Continued PROVIGIL sales provide a new
foundation for further accelerating Cephalon's growth over the next several
years."
In connection with the settlements, Cephalon will grant Barr a non- exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL in the
United States. Barr's license will become effective in October 2011, unless
Cephalon obtains a pediatric extension for PROVIGIL which would permit entry by
Barr in April 2012. An earlier entry by Barr may occur based upon the entry of
another generic version of PROVIGIL.
"While we remain confident in the strength of the PROVIGIL patent, we believe
that with these settlements we have struck an appropriate balance between
protecting our intellectual property rights and providing more certainty to our
business through at least 2011," said John E. Osborn, Senior Vice President and
General Counsel.
Cephalon and Barr also agreed to a series of business arrangements related to
modafinil. Specifically, Barr has agreed to grant to Cephalon a non- exclusive
license, effective immediately, to certain of its worldwide intellectual
property rights related to modafinil in exchange for an upfront payment.
Cephalon also has agreed to purchase certain existing and in-process inventory
of the active pharmaceutical ingredient modafinil.
With respect to ACTIQ, Cephalon will grant Barr an exclusive royalty- bearing
right to market and sell a generic version of ACTIQ in the United States,
effective on December 6, 2006. Barr will pay specified royalties on net profits
of its generic ACTIQ product for the period December 6, 2006 through February 3,
2007, subject to certain limitations. Under an agreement entered into with Barr
in mid-2004 in connection with the company's acquisition of CIMA LABS and
pursuant to a Federal Trade Commission order, Cephalon granted Barr a
non-exclusive, royalty-free license to sell a generic version of ACTIQ effective
on the earlier of final approval of Cephalon's fentanyl effervescent buccal
tablet (FEBT) or February 3, 2007, if Cephalon receives a pediatric extension
for ACTIQ (or September 5, 2006, if Cephalon does not receive the extension).
The terms of the agreements are confidential, and are subject to review by the
Federal Trade Commission. Financial terms were not disclosed.
The parties will promptly file a dismissal with the United States District
Courts for the Districts of New Jersey and Delaware that will conclude pending
litigation between the parties regarding PROVIGIL and ACTIQ, respectively. This
settlement and the previously announced settlements with Teva Pharmaceutical
Industries Ltd. and its affiliate, Ranbaxy Laboratories Limited, and Mylan
Pharmaceuticals Inc. resolve the PROVIGIL litigation with all four firms that
Cephalon understands were the first to submit abbreviated new drug applications
(ANDAs) with Paragraph IV certifications to the Food and Drug Administration.
As such, Teva, Ranbaxy, Mylan and Barr would be granted the 180-day exclusivity
provided by the provisions of the Federal Food, Drug, and Cosmetic Act. The
separate, ongoing PROVIGIL patent litigation between Cephalon and Carlsbad
Technology, Inc., pending in the U.S. District Court in New Jersey, is
unaffected by these settlements. The lawsuit against Carlsbad claims
infringement of Cephalon's U.S. Patent No. RE37,516, which covers pharmaceutical
compositions and methods of treatment with the form of modafinil contained in
PROVIGIL. This patent expires in October 6, 2014 and may be extended by six
months (to April 6, 2015) upon acceptance by the FDA of the pediatric study data
submitted by the company on December 21, 2005.
As previously announced, Cephalon will reissue 2006 guidance when it releases
its fourth quarter and full year 2005 financial results on February 14, 2006 to
reflect the recent settlements of the PROVIGIL and ACTIQ patent infringement
suits, the closing of the Zeneus acquisition, the current timeline for
commercial launch of SPARLON, and the impact of the recent rise in the company's
stock price on the number of shares included in the income per share
calculation. The company expects to report a modest increase in 2006 guidance
when issued.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon currently
employs approximately 2,600 people in the United States and Europe. U.S. sites
include the company's headquarters in Frazer, Pennsylvania, and offices,
laboratories or manufacturing facilities in West Chester, Pennsylvania, Salt
Lake City, Utah, and suburban Minneapolis, Minnesota.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ and TRISENOX(R) (arsenic
trioxide) injection, and more than 20 products internationally. Full prescribing
information for all U.S. products is available at http://www.cephalon.com/ or
by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding the settlement of this litigation, including
whether the Federal Trade Commission will approve the terms of such settlement;
anticipated scientific progress on its research programs; development of
potential pharmaceutical products; interpretation of clinical results; prospects
for regulatory approval; manufacturing development and capabilities; market
prospects for its products; sales and earnings guidance; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
First Call Analyst: Robert S. Merritt
FCMN Contact:
CONTACT: Media, Robert Grupp, +1-610-738-6402, or rgrupp@cephalon.com ,
or Investors, Chip Merritt, +1-610-738-6376, or cmerritt@cephalon.com , both of
Cephalon, Inc.
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: February 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
425 of 998 DOCUMENTS
PR Newswire US
February 1, 2006 Wednesday 10:28 PM GMT
Cephalon, Inc. Provides Update on Regulatory Status of NUVIGIL(TM);
Company Anticipates Launch of Product in Mid-2006
LENGTH: 848 words
DATELINE: FRAZER, Pa. Feb. 1
FRAZER, Pa., Feb. 1 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that the United States Food and Drug Administration (FDA) has
extended the action date for its review of the New Drug Application (NDA) for
NUVIGIL(TM) (armodafinil) Tablets [C-IV] to improve wakefulness in patients
suffering from excessive sleepiness associated with narcolepsy, shift work sleep
disorder (SWSD) and obstructive sleep apnea/hypopnea syndrome (OSA/HS) to April
30, 2006.
"We will continue to work closely with the FDA to assist them in completing
their review of our application in a timely manner and do not anticipate any
further delays beyond the April 30 action date," said Dr. Paul Blake, Executive
Vice President, Worldwide Medical and Regulatory Operations. "As pioneers in the
development of wake promoting agents, we are excited about the opportunity to
bring NUVIGIL to market in the middle of this year."
A NDA for NUVIGIL was filed with the FDA on March 31, 2005. The original action
date under the Prescription Drug User Fee Act (PDUFA) for the NUVIGIL NDA was
January 31, 2006. At the FDA's request, the company submitted additional
information to FDA in October 2005. The FDA has informed the company that this
submission has been classified as a major amendment to the NDA, which enables
the FDA to extend the action date by 90 days to provide the agency time for a
full review of the submission.
About NUVIGIL
NUVIGIL is a single-isomer formulation of modafinil, the active pharmaceutical
ingredient contained in PROVIGIL(R) (modafinil) Tablets [C-IV]. The NDA is based
on positive results of four double-blind, randomized, placebo-controlled studies
in patients with excessive sleepiness associated with either narcolepsy, SWSD or
OSA/HS. In these studies, NUVIGIL was generally well tolerated, with a safety
profile consistent with that observed in studies of PROVIGIL. The most common
adverse effects observed included headache, nausea, dizziness, insomnia and
anxiety.
About Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon currently
employs approximately 2,600 people in the United States and Europe. U.S. sites
include the company's headquarters in Frazer, Pennsylvania, and offices,
laboratories or manufacturing facilities in West Chester, Pennsylvania, Salt
Lake City, Utah, and suburban Minneapolis, Minnesota.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling
1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs; development of potential pharmaceutical products; interpretation of
clinical results, particularly with respect to the NUVIGIL Phase 3 trials;
prospects for and timing of regulatory approval of NUVIGIL; anticipated product
launch date and potential benefits of NUVIGIL; manufacturing development and
capabilities; market prospects for its products; sales and earnings guidance;
and other statements regarding matters that are not historical facts. You may
identify some of these forward-looking statements by the use of words in the
statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
First Call Analyst: Robert S. Merritt
FCMN Contact:
CONTACT: Media: Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com ,
or Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com ,
both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: February 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 PR Newswire Association LLC.
All Rights Reserved.
426 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
January 26, 2006
Cephalon provides update on regulatory status of Sparlon
LENGTH: 249 words
Cephalon has reported that it does not expect final action from the FDA on its
pending NDA for Sparlon ( modafinil ) Tablets [C-IV] for the treatment of
attention deficit hyperactivity disorder (ADHD) in children and adolescents
until after the completion of several FDA advisory committee meetings. The first
two panels, scheduled for 9th February and 22nd March 2006, will consider safety
and risk-management issues associated with products in the class of
currently-approved ADHD treatments.
Since Sparlon is not an approved drug, it will not be discussed at these
meetings. A separate advisory panel to review Sparlon has been scheduled for
23rd March 2006. On 20th October 2005, the FDA issued an approvable letter with
respect to Cephalon's NDA for Sparlon; the company now expects to launch the
product during the second quarter of 2006. As a result of recent settlements of
three patent infringement suits related to Provigil (modafinil) Tablets [C-IV],
the closing of the acquisition of Zeneus Holdings, the parent company of Zeneus
Pharma , the current timeline for commercial launch of Sparlon and the impact of
the recent rise in the company's stock price on the number of shares included in
the income per share calculation, Cephalon has determined that its
previously-issued 2006 sales and diluted adjusted income per share guidance is
outdated. The company will reissue 2006 guidance when it releases its fourth
quarter and full-year 2005 financial results on 14th February 2006.
LOAD-DATE: January 30, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
427 of 998 DOCUMENTS
World Generic Markets
Pharmaceuticals
January 16, 2006
Cephalon reaches modafinil litigation settlements with Teva, Ranbaxy and Mylan
LENGTH: 390 words
Cephalon has announced it has reached agreements with Teva Pharmaceutical
Industries , Ranbaxy Laboratories and Mylan Pharmaceuticals to settle their
respective pending patent infringement litigation cases over Cephalon's
modafinil product, Provigil . In the case with Teva, the agreement settles
disputes in both the United States and the United Kingdom. In the settlements
with all three companies, Cephalon will grant the two non-exclusive
royalty-bearing rights to market and sell generic modafinil in the United
States. This will become effective for both companies in October 2011, assuming
no paediatric exclusivity periods for Provigil, in which case the date would be
set back by six months to April 2012. Interestingly, Provigil has two patents
listed against it in the FDA's Orange Book, but neither expires in October 2011.
The first expires on 22nd May 2007, and the second on 6th October 2014. However,
earlier entry by either Ranbaxy, Mylan or Teva could occur if another generic
version of the drug enters the market.
In Teva's case, the two firms have agreed to comparable terms for the licence
effective date, which would generally allow for entry in October 2012. Cephalon
has also agreed a series of business arrangements related to modafinil with the
two firms. Specifically, both Teva and Ranbaxy have agreed to grant Cephalon a
non-exclusive licence, effective immediately, to certain of their worldwide
intellectual property rights related to modafinil in exchange for milestone
payments. Cephalon has also agreed to enter into arrangements related to the
manufacture and supply of the modafinil active ingredient with the two
companies. The specific terms of the agreements are confidential, but are
subject to review by the Federal Trade Commission. In both cases, financial
terms have not been disclosed. With the agreements, the parties will file
dismissals with prejudice with the US District Court for the District of New
Jersey which will conclude all pending litigation between the firms regarding
modafinil. The lawsuits in both cases relate to Cephalon's patent which expires
in 2014 and covers pharmaceutical compositions and methods of treatment with the
form of modafinil contained in Provigil. With regard to Teva, the parties will
also file a dismissal with the UK High Court of Justice, Chancery Division.
LOAD-DATE: January 18, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
428 of 998 DOCUMENTS
Family Practice News
January 15, 2006
Modafinil Safe and Effective for Pediatric ADHD
BYLINE: Michele G. Sullivan, Mid-Atlantic Bureau
SECTION: Pg. 57 Vol. 36 No. 2 ISSN: 0300-7073
LENGTH: 346 words
TORONTO - Modafinil is safe and effective in treating pediatric
attention-deficit hyperactivity disorder. Symptom scores were twice as high as
placebo, according to two posters presented at the joint annual meeting of the
American Academy of Child and Adolescent Psychiatry and the Canadian Academy of
Child and Adolescent Psychiatry.
The posters, sponsored by Cephalon Inc., concluded that children tolerated
the film-coated tablets well in dosages of up to 425 mg/day. Insomnia, headache,
and decreased appetite were the most commonly reported adverse events. Those
adverse events typically occurred during the first 2 weeks of therapy and
decreased thereafter, said Dr. Christopher Kratochvil of the University of
Nebraska.
The posters analyzed three multicenter, double-blind studies that included a
total of 633 children aged 6-17 years. Two studies were identical 9-week
flexible-dosing trials. The third was a 7-week, fixed-dose, placebo-controlled
study (340 or 425 mg/day), followed by a 2-week period in which half the
modafinil group was switched to placebo without tapering while the other half
continued modafinil treatment.
Adverse events were more common in the active group than the placebo group
and included insomnia (27% vs. 4%), headache (20% vs. 13%), and decreased
appetite (16% vs. 3%).
The adverse events were all classified as mild to moderate. They peaked in
the first 2 weeks of treatment and subsequently subsided. No apparent
association was found between adverse events and dosage.
There were no significant changes in heart rate or blood pressure between the
groups, and the abrupt discontinuation of the drug did not lead to acute
withdrawal symptoms or rebound effects.
The drug effectively reduced the symptoms of ADHD, especially hyperactivity
and inattention, reported Dr. Joseph Biederman of Massachusetts General
Hospital. Effects were consistent whether assessed by physician, parent, or
teacher. Physicians assessed almost 50% of the active groups as much improved at
the end of treatment, vs. 20% of the placebo group.
LOAD-DATE: July 31, 2009
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PUBLICATION-TYPE: Newspaper
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Copyright 2006 Elsevier Inc., International Medical News Group
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429 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
January 11, 2006
Cephalon/Mylan enter agreement to settle Provigil patent litigation
LENGTH: 341 words
Cephalon has entered into an agreement with Mylan Pharmaceuticals to settle its
pending patent infringement dispute in the US related to Provigil ( modafinil )
Tablets [C-IV]. In connection with the settlement, Cephalon will grant Mylan a
non-exclusive royalty-bearing right to market and sell a generic version of
Provigil in the US. Mylan's licence will become effective in October 2011,
unless Cephalon obtains a paediatric extension for Provigil, which would permit
entry by Mylan in April 2012. An earlier entry by Mylan may occur based upon the
entry of another generic version of Provigil. The terms of the agreement are
confidential and are subject to review by the US FTC.
Financial terms were not disclosed. The parties will promptly file a dismissal
with prejudice with the US District Court for the District of New Jersey that
will conclude all pending litigation between the parties regarding Provigil.
This settlement and the previously-announced settlements with Teva
Pharmaceutical Industries and its affiliate, and Ranbaxy Laboratories , do not
affect the status of the ongoing Provigil patent litigations between Cephalon
and certain other generic companies that are pending in the US District Court in
New Jersey. These lawsuits claim infringement of Cephalon's US Patent No.
RE37,516 (the '516 Patent), which covers pharmaceutical compositions and methods
of treatment with the form of modafinil contained in Provigil. The '516 patent
expires on 6th October 2014 and may be extended by six months (to 6th April
2015) upon submission of paediatric study data that are acceptable to the FDA.
In January 2004, the FDA approved Provigil as the first and only medication to
treat excessive sleepiness associated with shift-work sleep disorder. The
medication is believed to work selectively through the sleep-wake centres to
activate the cortex of the brain. The exact mechanism of action of Provigil is
not known, however, it promotes wakefulness without causing the generalised
stimulation of the brain associated with CNS stimulants.
LOAD-DATE: January 12, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
430 of 998 DOCUMENTS
IPS-Inter Press Service
January 9, 2006, Monday
FRANCE: SOLDIERS SAY UNTESTED GULF WAR DRUG MADE THEM SICK
BYLINE: By Julio Godoy
LENGTH: 788 words
DATELINE: PARIS, January 9 2006
The French army administered a drug to its soldiers during the first Gulf War in
1991 without informing them of the risks, according to evidence presented at a
judicial inquiry.
The drug, Modafinil, kept the soldiers awake for days, according to documents
presented before a judicial inquiry into the Gulf War syndrome. The inquiry was
launched by the public prosecution office in June 2002 to establish
responsibility for illnesses suffered by French soldiers in Iraq.
The drug was administered to some 1,000 French soldiers who participated in the
war against Iraq.
"I and many comrades were given the drug every eight hours under orders from our
commanders," Yannick Morvan, a veteran of the 1991 Iraq campaign, told IPS. "I
am ready to give my life defending France, but that does not mean that I am
ready to be used as guinea pig against my will."
Other veterans say the commanders never spelled out what kind of drug the
soldiers were being given.
The army decided to test Modafinil in Operation Dauphin in June 1990, two years
before the drug was due for authorized distribution, according to evidence
presented at the inquiry. In an internal note in January 1991, military
authorities said the drug could only be used "outside national territory" and
only with the "utmost discretion."
The French army violated national and international rules on testing drugs that
say that no test can be carried out without written consent of those taking the
drugs, critics say.
The drug contributed to several conditions that are seen as a part of Gulf War
syndrome.
Gulf War syndrome was first identified by the U.S. Centers for Disease Control
and Prevention in 1994 after thousands of troops returning from Iraq complained
of numerous unexplained symptoms.
It is defined as having a set of symptoms that continue for more than six
months, such as fatigue, mood and cognitive symptoms such as loss of sleep or
memory, concentration disturbances, headaches and depression, and
musculoskeletal pain.
The French army denies any wrongdoing. The Defense Ministry says use of
Modafinil could in no way be described as a test.
Daniel Gautier, who served as head of the military medical department in the
early 1990s, said at a hearing that "on the war field, military medical
personnel wrongly believed that they were carrying out a therapeutic test."
Maurice Schmitt, who was commander-in-chief of the armed forces between 1987 and
1991, told a parliamentary inquiry commission in November 2000 that he had not
given specific authorization to test Modafinil. "I just left open the
possibility to test it, if the need to do it became evident," he said.
Both officers spoke of administration of the drug as a test.
Several hundred French soldiers have lodged complaints against the army alleging
they are suffering from Gulf War syndrome as a result of being given illegal
drugs or due to exposure depleted uranium or to chemical weapons such as the
nerve gas Sarin.
The soldiers have created an association, Avigolfe (short for Association of the
military and civilian victims of the Gulf War), which claims that at least 31
veterans of the Iraq campaign have died as a result of contamination from
illegal drugs or weapons.
The Avigolfe campaign led to the present judicial inquiry. A finding is expected
in June, sources close to prosecutor Marie-Odille-Bertella Geoffroy told IPS.
Guy Paris, legal counselor for Avigolfe, says soldiers still in service are
reluctant to talk about their health difficulties for fear they could be
expelled from the army.
"Many soldiers wait until they have 15 years of service to get access to full
pension before they present their pleas," Paris told IPS.
Similar inquiries have been going on in the United States and in Britain for
years.
According to the U.S. Research Advisory Committee on Gulf War Veterans'
Illnesses, an estimated 100,000 Gulf War veterans, or about one in seven
soldiers who were deployed in Iraq in 1991, suffer war-related health problems.
The committee was set up by the U.S. Congress in 1998 to "make recommendations
to the (U.S.) Secretary of Veterans Affairs on government research relating to
the health consequences of military service in the Southwest Asia theatre of
operations" during the Gulf War of 1991.
In a report released in October 2004, the committee concluded that "a
substantial proportion of Gulf War veterans are ill with multi-symptom
conditions probably linked to the exposure to chemical weapons and neurotoxins."
The report said possible sources include Sarin from an Iraqi weapons depot blown
up by U.S. forces in 1991, and also pyridostigmine bromide, a drug given to the
troops to protect them against nerve gas.
LOAD-DATE: January 19, 2006
LANGUAGE: ENGLISH
Copyright 2006 IPS-Inter Press Service/Global Information Network
431 of 998 DOCUMENTS
World Generic Markets
Pharmaceuticals
January 9, 2006
Cephalon reaches modafinil litigation settlements with Teva and Ranbaxy
LENGTH: 385 words
Cephalon has announced it has reached agreements with both Teva Pharmaceutical
Industries and Ranbaxy Laboratories to settle their respective pending patent
infringement litigation cases over Cephalon's modafinil product, Provigil . In
the case with Teva, the agreement settles disputes in both the United States and
the United Kingdom. In the settlements with both companies, Cephalon will grant
the two non-exclusive royalty-bearing rights to market and sell generic
modafinil in the United States. This will become effective for both companies in
October 2011, assuming no paediatric exclusivity periods for Provigil, in which
case the date would be set back by six months to April 2012. Interestingly,
Provigil has two patents listed against it in the FDA's Orange Book, but neither
expires in October 2011. The first expires on 22nd May 2007, and the second on
6th October 2014. However, earlier entry by either Ranbaxy or Teva could occur
if another generic version of the drug enters the market.
In Teva's case, the two firms have agreed to comparable terms for the licence
effective date, which would generally allow for entry in October 2012. Cephalon
has also agreed a series of business arrangements related to modafinil with the
two firms. Specifically, both Teva and Ranbaxy have agreed to grant Cephalon a
non-exclusive licence, effective immediately, to certain of their worldwide
intellectual property rights related to modafinil in exchange for milestone
payments. Cephalon has also agreed to enter into arrangements related to the
manufacture and supply of the modafinil active ingredient with the two
companies. The specific terms of the agreements are confidential, but are
subject to review by the Federal Trade Commission. In both cases, financial
terms have not been disclosed. With the agreements, the parties will file
dismissals with prejudice with the US District Court for the District of New
Jersey which will conclude all pending litigation between the firms regarding
modafinil. The lawsuits in both cases relate to Cephalon's patent which expires
in 2014 and covers pharmaceutical compositions and methods of treatment with the
form of modafinil contained in Provigil. With regard to Teva, the parties will
also file a dismissal with the UK High Court of Justice, Chancery Division.
LOAD-DATE: January 12, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
432 of 998 DOCUMENTS
Reuters Health Medical News
January 6, 2006 Friday 9:00 PM EST
Modafinil unlikely to perk up Parkinson's patients during the day
SECTION: CLINICAL
LENGTH: 248 words
DATELINE: NEW YORK
Modafinil (Provigil), a wake-promoting agent approved for use in narcolepsy,
does not appear to promote wakefulness in patients with Parkinson's
disease-related excessive daytime somnolence, according to results of a 4-week
double-blind, placebo-controlled study.
The etiology of excessive daytime sleepiness, which often complicates PD, is
"probably multifactorial but is probably exacerbated by dopaminergic
medications," Houston-based researchers note in the December issue of the
Journal of Neurology, Neurosurgery and Psychiatry.
Dr. William G. Ondo from Baylor College of Medicine and colleagues tested the
efficacy of modafinil (200 or 400 mg per day) against placebo in 40 PD patients
with excessive daytime somnolence.
According to the team, modafinil failed to significantly relieve daytime
sleepiness on any of the tests used, including the Epworth Sleepiness Scale, the
Multiple Sleep Latency Test, and the Fatigue Severity Scale. Hamilton Depression
Scale scores were also unchanged with modafinil.
"The drug, however, was very well tolerated and has an immediate effect, and
individual patients did benefit from taking it," Dr. Ondo and colleagues note.
"Since the etiology of excessive sleepiness is multifactorial, modafinil may be
considered on an individual basis," they conclude.
Dr. Ondo's group also points out in their report that modafinil was associated
with significant improvement in PD-related daytime sleepiness in two smaller
controlled trials of shorter duration.
LOAD-DATE: March 4, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2006 Reuters Health
All Rights Reserved
433 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
January 3, 2006
Ranbaxy enters agreement with Cephalon regarding settlement of Provigil patent
litigation
LENGTH: 420 words
Ranbaxy Laboratories has entered into an agreement with Cephalon to settle the
companies' pending patent infringement dispute in the US related to Provigil (
modafinil ) Tablets [C-IV]. In connection with the settlement, Cephalon will
grant Ranbaxy a non-exclusive royalty-bearing right to market and sell a generic
version of Provigil in the US. Ranbaxy's licence will become effective in
October 2011, in the absence of a paediatric extension for Provigil, which would
delay the entry date by six months (to April 2012). An earlier entry by Ranbaxy
may occur based upon the entry of another generic version of Provigil. The
companies have also agreed to a series of business arrangements related to
modafinil.
Specifically, Ranbaxy has agreed to grant to Cephalon a non-exclusive licence,
effective immediately, to certain of its worldwide intellectual property rights
related to modafinil in exchange for milestone payments. Cephalon has also
agreed to enter into certain arrangements with Ranbaxy related to the latter's
supply of the active pharmaceutical ingredient, modafinil. The terms of the
agreement are confidential and are subject to review by the FTC. Financial terms
were not disclosed. The parties will promptly file a dismissal with prejudice
with the US District Court for the District of New Jersey that will conclude all
pending litigation between the parties regarding Provigil. This settlement and
the previously-announced settlements with Teva Pharmaceutical Industries and
Teva Pharmaceuticals USA do not affect the status of the ongoing Provigil patent
litigations between Cephalon and certain other generic companies that are
pending in the US District Court in New Jersey. These lawsuits claim
infringement of Cephalon's US Patent No. RE37, 516 (the '516 Patent), which
covers pharmaceutical compositions and methods of treatment with the form of
modafinil contained in Provigil. The '516 Patent expires on 6th October 2014,
and may be extended by six months (to 6th April 2015) upon the submission of
paediatric study data that are acceptable to the FDA. In January 2004, the FDA
approved Provigil as the first and only medication to treat excessive sleepiness
associated with shift-work sleep disorder. The medication is believed to work
selectively through the sleep-wake centres to activate the cortex of the brain.
The exact mechanism of action of Provigil is not known, however, it promotes
wakefulness without causing the generalised stimulation of the brain associated
with CNS stimulants.
LOAD-DATE: January 9, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2006 ESPICOM Business Intelligence Ltd.
All Rights Reserved
434 of 998 DOCUMENTS
Clinical Psychiatry News
January 2006
Clinical Capsules
BYLINE: Heidi Splete
SECTION: Pg. 44 Vol. 34 No. 1 ISSN: 0270-6644
LENGTH: 802 words
Ethnicity and Depression in Teen Girls
Depression scores among white girls and young women decrease over time, but
the scores tend to hold steady among their African American counterparts,
reported Debra L. Franko, Ph.D., of Northeastern University, Boston, and her
associates.
Depression scores among white girls and young women tend to start off higher,
and that might play a role in the findings.
Previous comparisons of depression scores in African American and white girls
have shown either mixed results or higher scores among white girls at younger
ages.
The investigators conducted an age-matched study of 2,221 girls and young
women aged 16-22 years, including 1,146 African Americans and 1,075 whites. The
girls, participants in the 10-year longitudinal National Growth and Health
Study, were asked to complete a packet of questionnaires, including the Center
for Epidemiological Studies of Depression scale (CES-D) (J. Adolesc. Health
2005;37:526-9).
Adolescent depression was defined as a score of at least 24 on the CES-D.
Overall, as they got older, the percentage of white girls who met the
criteria for depression fell, and the percentage of African American girls who
met the criteria remained fairly steady. Specifically, 21% of 483 white
16-year-olds scored 24 or higher, compared with 14% of 332 white 22-year-olds.
Among African Americans, 14% of 469 16-year-olds scored 24 or higher, compared
with 15% of 452 22-year-olds.
The researchers noted that age-specific risk factors-such as body
dissatisfaction subsequent to pubertal development-are more common among white
girls and could partly account for the results. Other factors, such as access to
and use of mental health care, also could explain some of the differences.
Modafinil for ADHD
Modafinil film-coated tablets significantly improved clinical symptoms of
attention-deficit hyperactivity disorder in children and adolescents aged 6-17
years, said Dr. Joseph Biederman of Massachusetts General Hospital in Boston and
his colleagues.
Modafinil, an agent generally prescribed to promote wakefulness in patients
with narcolepsy, has been shown to activate the cortex alone.
In the randomized, double-blind trial conducted by Dr. Biederman and his
colleagues, 164 children received a flexible dose of modafinil in tablet form,
and 82 children received a placebo. The children began with one 85-mg tablet for
the first 2 days; the dose was titrated to 170 mg on days 3-7, 255 mg on days
8-14, 340 mg on days 15-21, and 425 mg on day 22 (Pediatrics 2005;116:777-84).
After 9 weeks, 48% of patients in the modafinil group were deemed responders,
compared with 17% of those in the placebo group. Overall, patients in the
modafinil group demonstrated significant improvement in symptoms, including
oppositional behavior, cognitive problems/inattention, hyperactivity, and the
ADHD index on the Conners' Parent Rating Scale Revised, Short Form, compared
with those in the placebo group.
Modafinil (Provigil) also was well tolerated. Only five of the patients in
the treatment group (3%) and three in the placebo group (4%) discontinued the
study because of adverse events. Given modafinil's safety profile and its low
potential of abuse, the drug may offer clinicians a new option for treating ADHD
in children and adolescents, the investigators said.
Teens' Perception of Body Weight
Many young teens from disadvantaged backgrounds do not perceive obesity as
unacceptable, and despite common perceptions, not all of them are striving for
thinness, reported Wendy Wills of the Centre for Research in Primary and
Community Care, University of Hertfordshire, Hatfield, England.
In a qualitative study in eastern Scotland of 36 economically disadvantaged
13- to 14-year-olds, half of the subjects were either overweight (body mass
index greater than 25 kg/m2) or obese (BMI greater than 30). The subjects were
evenly split among boys and girls (Soc. Sci. Med. 2006;62:396-406).
The overweight and obese teens had complex views of their weight and body
size. Three-quarters of them talked positively about their weight, body size, or
parts of their bodies, or expressed comfort with their bodies. A minority who
were comfortable with their bodies also reported dissatisfaction with some parts
of their bodies, and about half of these subjects wanted to lose weight or had
already tried.
Half of the overweight and obese teens had tried to lose weight (as had three
in the normal-weight group). These teens experienced an "emotional high" when
they lost weight, and a deterioration in well-being when they failed. Only a
minority of the subjects cited the health benefits of weight loss, even after
expressing a desire to lose weight. Most of the subjects said that family and
friends did not need to lose weight and should not feel pressured to do so.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2006 Elsevier Inc., International Medical News Group
All Rights Reserved
435 of 998 DOCUMENTS
Clinical Psychiatry News
January 2006
Sadness Alters Tx for Depression-Related Fatigue
BYLINE: Sherry Boschert, San Francisco Bureau
SECTION: Pg. 59 Vol. 34 No. 1 ISSN: 0270-6644
LENGTH: 649 words
SAN DIEGO - When choosing a therapy for physical fatigue in patients being
treated for depression, it is important to consider the presence or absence of
residual sadness, Dr. Stephen C. Ellen said at a psychopharmacology congress
sponsored by the Neuroscience Education Institute.
Two strategies exist for treating patients on antidepressants who complain
that activities make them feel more physically tired, winded, or older than they
felt before depression set in, despite getting help for the depression. Both
bupropion and stimulants will boost dopamine and norepinephrine in the cortex,
striatum, and spinal cord. Modafinil will boost histamine in the cortex, he
said.
Dr. Ellen is a speaker for GlaxoSmithKline, which makes Wellbutrin
(bupropion). He also serves as a consultant and speaker for Cephalon Inc., which
makes Provigil (modafinil).
If the patient's antidepressant therapy has virtually eliminated the sadness
and mood issues, choose modafinil or methylphenidate (for example, Ritalin) or
another stimulant to treat the residual physical fatigue. If some sadness still
remains, however, bupropion may boost antidepressant effects and reduce fatigue,
said Dr. Ellen of the University of Massachusetts, Worcester.
Modafinil or stimulants work much better at "waking somebody up" from
residual symptoms of depression than does bupropion, he said. Bupropion "is
brightening, but I don't think it is particularly wake promoting."
Physical fatigue is common in patients with depression or obstructive sleep
apnea, and the two problems overlap. One in six depressed people has obstructive
sleep apnea, and one in five people with obstructive sleep apnea is depressed,
he noted. A 2003 study of 60 patients found that the more severe the depression
in a patient with sleep apnea, the greater the level of fatigue.
In patients with both depression and obstructive sleep apnea, the fatigue
usually derives from the depression. "So if you're still getting words that
sound like fatigue" after treatment, consider switching to a stronger
antidepressant or increasing the dose, Dr. Ellen advised.
Bupropion is widely used to treat fatigue in patients with depression but it
"takes a while to kick in," typically 4-6 weeks, he said. Some reports suggest
that bupropion may be less likely than other antidepressants to destabilize a
patient with bipolar disorder, but other reports suggest that the risk is no
different with bupropion.
A case series of 42 patients treated for depression with selective serotonin
reuptake inhibitors found that energy levels stayed the same or improved in
patients who received adjuvant bupropion but worsened in nearly half of patients
who remained on monotherapy, Dr. Ellen said.
Stimulants are not commonly used to treat fatigue in depressed patients, but
they can quickly provide a boost in alertness with short-term use. Most studies
of stimulants for fatigue focus on patients with HIV or AIDS. There are no
controlled trials of stimulants for fatigue associated with depression, "but
that shouldn't throw you off, because there's not a single controlled study of
[bupropion for this indication] either, and we use that like crazy," he said.
Stimulants, however, can cause cardiovascular or CNS side effects and have a
high risk for abuse with long-term use. Patients may develop psychological or
physical dependence on them, and tolerance to the drug develops rapidly, Dr.
Ellen said.
Adding modafinil to antidepressant therapy appears to significantly reduce
patients' fatigue scores if the drug is given in proper doses. The best effects
are seen with 100-200 mg/day. Less benefit comes from a dosage of 300 mg/day,
and a dosage of 400 mg/day can increase fatigue, he said.
Modafinil's effects on fatigue in depression appear to be independent of
mood, and the onset of action usually is immediate, he noted.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2006 Elsevier Inc., International Medical News Group
All Rights Reserved
436 of 998 DOCUMENTS
Neurology Alert
January 1, 2006
Does Modafinil Improve Daytime Somnolence in Parkinson's Disease?
LENGTH: 828 words
Does Modafinil Improve Daytime Somnolence in Parkinson's Disease?
Abstracts & Commentary
By Claire Henchcliffe, MD, DPhil, Assistant Professor, Department of Neurology,
Weill Medical College, Cornell University. Dr. Henchcliffe is on the speaker's
bureau for GlaxoSmithKline, Teva/Eisai, and Boehringer Ingelheim.
Synopsis: Modafinil failed to significantly improve EDS in PD compared with
placebo.
Source: Ondo WG, et al. Modafinil for Daytime Somnolence in Parkinson's Disease:
Double Blind, Placebo Controlled Parallel Trial. J Neurol Neurosurg Psychiatry.
2005;76:1636-1639.
This 4-week, double blind, placebo controlled, parallel group trial randomized
40 subjects with Parkinson's disease (PD) and an Epworth Sleepiness Scale (ESS)
score > 10, to either modafinil (200-400 mg daily, 20 patients) or placebo (20
patients). Patients with undefined serious medical conditions, as well as those
diagnosed with sleep apnea and narcolepsy, were excluded. Of the 40 subjects, 37
completed the study (modafinil 19 patients, placebo 18 patients). ESS score
provided the primary measure of efficacy, and secondary end points included the
Fatigue Severity Scale, Hamilton Depression Scale, the multiple sleep latency
test (MSLT), and the Unified Parkinson's Disease Rating Scale (UPDRS). Baseline
mean ESS was 15.8 3.0 for modafinil and 15.9 3.5 for placebo treated patients,
and the 2 groups were balanced for age (mean, 64.8 11.3 years), gender, duration
of PD (mean, 6.8 5.0 years), daily dopaminergic dose, motor fluctuations, and
UPDRS activities of daily living and motor scores. Subjects were given one
tablet of modafinil (100 mg) or corresponding placebo upon waking and at lunch.
After one week, modafinil was increased to 2 tables (200 mg) upon waking and at
lunch. After another week, the ESS was administered by telephone. If patients
experienced an adverse event at higher doses, they were allowed to decrease the
total dose of modafinil to 200 mg daily. The final assessment was performed 4
weeks after the first visit. Modafinil was well tolerated, with only 1 patient
electing to return to 200 mg daily because of anxiety and nausea. At 4 weeks,
subjects on modafinil showed a non-significant improvement in ESS compared to
controls (2.7 vs 1.5 points, P = 0.28). There was a non-significant decrease in
MSLT (3.59 vs 3.28 minutes, P = 0.14), and no significant difference in any
other secondary end point.
Commentary
Excessive daytime somnolence (EDS) affects up to approximately 50% of PD
patients. It likely has multiple causes, and is associated with advanced PD,
long disease duration, male gender, and the use of dopaminergic agents.
Furthermore it has been linked to catechol-O-methyltransferase (COMT) genotype,
as well as low levels of orexin-A/hypocretin-1 in ventricular cerebrospinal
fluid. EDS interferes with social interactions and driving and, thus, may lead
to social isolation. Polysomnographic testing is helpful in selected patients to
exclude secondary causes of EDS. Treatment of EDS is difficult: use of
stimulants, such as methylphenidate, has led to inconsistent results, and side
effects are often limiting. Modafinil is a wake-promoting agent that is
FDA-approved for narcolepsy, sleep apnea, and shift work sleep disorder. Its
mechanism of action is not understood, and it is widely used off-label for a
variety of conditions associated with impaired wakefulness or fatigue, including
multiple sclerosis and traumatic brain injury.
Results of this study by Ondo and colleagues failed to support the positive
findings of 2 previous smaller randomized crossover studies.1,2 Should we
therefore abandon modafinil in treating PD-associated EDS? In our practice,
there are clearly PD patients with EDS who respond to modafinil. However, there
are no established criteria as to which patient will respond to the drug, and
response may depend upon etiology of EDS in each individual. Conflicting study
results regarding modafinil use most likely reflect our poor understanding of
variability in pathophysiology of PD-associated EDS, as well as small sample
sizes, use of subjective measurement scales, and referral bias. Modafinil is
currently not recommended in those with angina, left ventricular hypertrophy,
and other cardiac conditions. However, all studies of modafinil in PD have found
that in these selected patient groups derived from an elderly population,
modafinil is well-tolerated. Until larger studies are completed in PD, similar
to those performed for narcolepsy, modafinil is worth considering to alleviate
the debilitating symptoms of EDS for selected PD patients.
References
1. Hogl B, et al. Modafinil for the Treatment of Daytime Sleepiness in
Parkinson's Disease: A Double-Blind, Randomized, Crossover, Placebo-Controlled
Polygraphic Trial. Sleep. 2002;25:905-909.
2. Adler CH, et al. Randomized Trial of Modafinil for Treating Subjective
Daytime Sleepiness in Patients with Parkinson's Disease. Mov Disord.
2003;18:287-293.
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BioWorld Insight
December 26, 2005
Biotech - Big Pharma Collaborations: Modified And Terminated Agreements, Oct.
19-Dec. 22, 2005
LENGTH: 789 words
I. MODIFIED
AGREEMENTS
Biotech Co.* Pharma Co. Change from Terms/Details
(Country; Symbol) (Country) original agreement (Date)
Actelion Ltd. UCB Pharma They replaced Actelion assumes
(Switzerland; (Belgium) existing license full
SWX:ATLN) deal covering the responsibility for
Gaucher's disease the pre-UCB
product Zavesca obligations on
manufacturing and
supply, and
clinical
development; UCB
gets an up-front
payment in return
for a single-
digit royalty rate
on future sales
(11/17)
Cambridge Abbott They reached an CAT gets $255M,
Antibody Laboratories agreement which it will pay
Technology plc regarding to its licensors;
(UK; CATG) royalties payable it also gets five
to CAT under a annual payments of
licence agreement up $9.375M; CAT's
covering Humira royalty payments
were reduced to
2.688% of sales
from 5.1% (10/26)
Cephalon Inc. Ranbaxy They settled Ranbaxy got a
(CEPH) Laboratories Ltd. patent nonexclusive,
(India) infringement royalty-bearing
dispute in the right to market a
U.S. related to generic version of
Provigil ( the product
modafinil) starting in 2011;
they also entered
a series of
business
arrangements
related to
modafinil (12/22)
Cephalon Inc. Teva They settled Teva got a
(CEPH) Pharmaceutical patent nonexclusive,
Industries Ltd. infringement royalty-bearing
(Israel) disputes in the right to market a
U.S. and UK generic version of
related to the product
Provigil ( starting in 2011;
modafinil) they also entered
a series of
business
arrangements
related to
modafinil (12/9)
CuraGen Corp. Bayer They revised terms CuraGen exercised
(CRGN) Pharmaceuticals of deal in its right to
Corp. metabolic revert to a tiered
disorders relating royalty structure
to development of on any sales and
BAY 76-7171 no longer will
(formerly CT052) contribute to
development costs
of the drug
(12/20)
Depomed Inc. Biovail Corp. They resolved a Under the new deal
(DEPO) (Canada) dispute regarding Depomed has rights
a license to the product in
agreement on the the U.S.; Biovail
metformin-based relinquished its
diabetes product option to develop
Glumetza metformin
combination
products; Depomed
withdrew legal
action following
the agreement
(12/13)
Enzon Sanofi-Aventis They amended Enzon will pay a
Pharmaceuticals Group (France) license agreement single-digit
Inc. (ENZN) covering the royalty rate on
leukemia drug annual sales that
Oncospar exceed $25M; it
had been paying
25% on all sales;
Sanofi gets an
up-front cash
payment of $35M
(10/31)
Genetic Applera Corp. The companies Terms were not
Technologies Ltd. settled a patent disclosed but do
(Australia; GENE) dispute initiated include a license
by Gene to the non-coding
Technologies in patents from
2003 Genetic
Technologies
(12/12)
Gilead Sciences F. Hoffmann-La They resolved a Gilead gets $62.5M
Inc. (GILD) Roche Ltd. dispute related to in adjusted
(Switzerland) their 1996 deal royalties, and
covering the will get sales
influenza drug royalties from 14%
Tamiflu to 22%; Gilead
also gets certain
co-promotion
options in the
U.S.; the deal
ends arbitration
proceedings
(11/16)
Savient Barr They settled Barr paid Savient
Pharmaceuticals Pharmaceuticals patent litigation $13.75M, of which
Inc. (SVNTE) Inc. and NV regarding Barr's about $2.8M will
Organon (the generic version of be passed on to
Netherlands) Mircette, an oral the inventor
contraceptive (12/2)
product
II. TERMINATED
AGREEMENTS
Aphton Corp. Sanofi Pasteur They ended a deal Aphton regained
(APHT) (France) from 1997 to rights to the
develop Aphton's G17DT immunogen,
immunotherapy which is being
compound Insegia developed for
cancers, and
intends to find a
new partner (11/9)
Avalon Sanofi-Aventis They ended The agreement
Pharmaceuticals Group (France) December 2003 expired as a
Inc. (AVRX) collaboration result of Sanofi's
using molecular decision not to
cytogenetics to advance targets
identify and from the
validate oncology collaboration
targets (12/21)
Arqule Inc. Pfizer Inc. Pfizer is ending The deal, started
(ARQL) deal under which in 2001, will end
Arqule has been May 22, 2006;
producing Arqule expects to
synthetic chemical receive $19.8M in
compounds for connection with
Pfizer the termination
notification
(12/6)
Discovery Pfizer Inc. The companies Discovery has
Partners terminated received about
International discussions $92M from the
Inc. (DPII) regarding a chemistry deal
potential new deal from 2002 to 2005;
to replace Discovery will
existing one about reduce its
to expire combinatorial
chemistry
operations as a
result (11/29)
Notes:
# The information
in the chart does
not cover
agreements between
biotech companies
or agricultural
agreements.
* Private
companies are
indicated with an
asterisk.
Unless otherwise
noted, stock
symbols listed are
on the Nasdaq
market.
SWX = Swiss Stock
Exchange.
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438 of 998 DOCUMENTS
Hindustan Times
December 23, 2005 Friday 8:25 AM EST
RANBAXY ANNOUNCES AGREEMENT WITH CEPHALON REGARDING SETTLEMENT OF PROVIGIL
PATENT LITIGATION
BYLINE: Hindustan Times
LENGTH: 343 words
DATELINE: GURGAON, India
GURGAON, India, Dec. 23 -- Ranbaxy Laboratories Limited issued the following
press release:
Ranbaxy Laboratories Limited (Ranbaxy) announced that it has entered into an
agreement with Cephalon Inc., (Nasdaq: CEPH) to settle their pending patent
infringement dispute in the United States related to PROVIGIL (modafinil)
Tablets [C-IV].
In connection with the settlement, Cephalon will grant Ranbaxy a non-exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL in the
United States. Ranbaxy's license will become effective in October 2011 absence
of a pediatric extension for PROVIGIL, which would delay the entry date by six
months (to April 2012). An earlier entry by Ranbaxy may occur based upon the
entry of another generic version of PROVIGIL.
The companies also agreed to a series of business arrangements related to
modafinil. Specifically, Ranbaxy has agreed to grant to Cephalon a non-exclusive
license, effective immediately, to certain of its worldwide intellectual
property rights related to modafinil in exchange for milestone payments.
Cephalon also has agreed to enter into certain arrangements with Ranbaxy related
to Ranbaxy's supply of the active pharmaceutical ingredient modafinil.
The terms of the agreement are confidential, and are subject to review by the US
Federal Trade Commission. Financial terms were not disclosed.
The parties promptly will file a dismissal with prejudice with the United States
District Court for the District of New Jersey that will conclude all pending
litigation between the parties regarding PROVIGIL. These lawsuits claim
infringement of Cephalon's US Patent No. RE37, 516 ("the '516 Patent") which
covers pharmaceutical compositions and methods of treatment with the form of
modafinil contained in PROVIGIL. The '516 Patent expires in October 6, 2014 and
may be extended by six months (to April 6, 2015) upon submission of pediatric
study data that is acceptable to the US Food and Drug Administration.
Edited press releases are provided through HT Syndication, New Delhi.
LOAD-DATE: December 24, 2005
LANGUAGE: ENGLISH
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Indo-Asian News Service
December 23, 2005 Friday 1:54 PM EST
Cephalon, Ranbaxy settle patent suit
BYLINE: Indo-Asian News Service
LENGTH: 323 words
DATELINE: New Delhi
New Delhi, Dec 23 -- India's pharma major Ranbaxy Laboratories Limited has
reached a settlement with Cephalon on its US patent covering the formulation of
modafinil contained in Provigil, a treatment for daytime sleepiness associated
with narcolepsy.
Under the out of court settlement, Ranbaxy would be receiving a milestone
payment or royalty on the intellectual property right beginning 2006. It would
also supply active pharmaceutical ingredient (API) modafinil to Cephalon for an
undisclosed amount.
The new business arrangement worked out by the companies follows a similar
settlement with Teva Pharamceuticals on the modafinil patent earlier this month.
With this, Cephalon has arrived at a mutually beneficial business deal with two
of four generic drug makers against which it had filed patent suits at the US
District Court in New Jersey for alleged violation of its patent for modafinil.
Cephalon claims its patent for Provigil does not expire until 2014. The other
two generic drug companies are Mylan Pharmaceutical Inc and Barr Laboratories
Inc.
Cephalon has agreed to "grant Ranbaxy a non-exclusive royalty-bearing right to
market and sell a generic version of Provigil in the US. Ranbaxy's license will
become effective in October 2011 in the absence of a paediatric extension for
Provigil, which would delay the entry date by six months (to April, 2012)",
Ranbaxy said in a statement Friday.
"An earlier entry by Ranbaxy may occur based upon the entry of another generic
version of Provigil," the official statement said.
"The terms of the agreement are confidential, and are subject to review by the
US Federal Trade Commission." The financial terms were not disclosed.
The parties will file a dismissal with prejudice with the US District Court in
New Jersey to conclude all pending litigation between the parties regarding
Provigil.
Published by HT Syndication with permission from Indo-Asian News Service.
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The Press Trust of India
December 23, 2005 Friday
Ranbaxy settles patent case with Cephalon for Provigil
SECTION: NATIONWIDE INTERNATIONAL NEWS
LENGTH: 237 words
DATELINE: New Delhi Dec 23
Close on the heels of a US district court ruling against its patent challenge of
Pfizer's Lipitor, Ranbaxy Laboratories Ltd today said it had entered into an out
of court settlement with Cephalon Inc for the patent infringement dispute in the
US related to psychostimulant Provigil (modafinil) tablets.
As per the settlement, Cephalon will grant the Ranbaxy a non-exclusive
royalty-bearing right to market and sell a generic version of Provigil in the
US, a company statement said.
The company's license will become effective in October 2011 in the absence of a
pediatric extension for Provigil, which would delay the entry date by six months
(to April, 2012), it added.
Ranbaxy said an earlier entry might occur based upon the entry of another
generic version of Provigil.
The two companies have agreed to a series of business arrangements related to
modafinil.
Ranbaxy has a greed to grant to Cephalon an immediate non-exclusive license to
certain of its worldwide intellectual property rights related to modafinil in
exchange for milestone payments.
Cephalon also has agreed to enter into certain arrangements with Ranbaxy
regardign supply of the active pharmaceutical ingredient modafinil, it added.
The two parties would promptly file for dismissal of their litigation in the US
District Court of New Jersey, it said, adding, however, the out of court
settlement would be subject to the approval of US Federal Trade Commission.
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MarketWatch
December 22, 2005 Thursday 12:24 PM EST
Cephalon inks deal w/ Ranbaxy Labs to settle patent dispute
BYLINE: Katherine Hunt
LENGTH: 194 words
SAN FRANCISCO (MarketWatch) -- Cephalon Inc. (ceph) said Thursday it has entered
into an agreement with Ranbaxy Laboratories Ltd. (rbxlf) to settle its patent
infringement dispute related to modafinil, a wake-promoting agent marketed under
the brand name Provigil. Financial terms weren't disclosed.
Under the agreement, Cephalon will grant Ranbaxy a non-exclusive royalty-bearing
right to market and sell a generic version of Provigil in the United States.
Ranbaxy's license will become effective in October 2011 in the absence of a
pediatric extension for Provigil, which would delay the entry date by six
months, the Frazer, Pa.-based biopharmaceutical company said. Additionally,
Ranbaxy has agreed to grant to Cephalon a non-exclusive license, effective
immediately, to certain of its worldwide intellectual property rights related to
modafinil in exchange for milestone payments. Cephalon also has agreed to enter
into certain arrangements with Ranbaxy related to Ranbaxy's supply of the active
pharmaceutical ingredient modafinil.
©1997-2002 MarketWatch.com, Inc. All rights reserved. See details at
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PR Newswire
December 22, 2005 Thursday 5:01 PM GMT
Ranbaxy Laboratories Limited Announces an Agreement With Cephalon Regarding
Settlement of PROVIGIL(R) Patent Litigation;
Parties Also Agree to Business Arrangements Related to Modafinil
LENGTH: 504 words
DATELINE: PRINCETON, N.J. Dec. 22
Ranbaxy Laboratories Limited (Ranbaxy) announced today that it has entered into
an agreement with Cephalon, Inc.(NASDAQ:CEPH)to settle their pending patent
infringement dispute in the United States related to PROVIGIL(R) (modafinil)
Tablets [C-IV].
In connection with the settlement, Cephalon will grant Ranbaxy a non-exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL in the
United States. Ranbaxy's license will become effective in October 2011 absence
of a pediatric extension for PROVIGIL, which would delay the entry date by six
months (to April, 2012). An earlier entry by Ranbaxy may occur based upon the
entry of another generic version of PROVIGIL.
The companies also agreed to a series of business arrangements related to
modafinil. Specifically, Ranbaxy has agreed to grant to Cephalon a non-exclusive
license, effective immediately, to certain of its worldwide intellectual
property rights related to modafinil in exchange for milestone payments.
Cephalon also has agreed to enter into certain arrangements with Ranbaxy related
to Ranbaxy's supply of the active pharmaceutical ingredient modafinil.
The terms of the agreement are confidential, and are subject to review by the
U.S. Federal Trade Commission. Financial terms were not disclosed.
The parties promptly will file a dismissal with prejudice with the United States
District Court for the District of New Jersey that will conclude all pending
litigation between the parties regarding PROVIGIL. These lawsuits claim
infringement of Cephalon's U.S. Patent No. RE37, 516 ("the '516 Patent") which
covers pharmaceutical compositions and methods of treatment with the form of
modafinil contained in PROVIGIL. The '516 Patent expires in October 6, 2014 and
may be extended by six months (to April 6, 2015) upon submission of pediatric
study data that is acceptable to the U.S. Food and Drug Administration.
Ranbaxy Laboratories Limited, headquartered in India, is an integrated, research
based, international pharmaceutical company producing a wide range of quality,
affordable generic medicines, trusted by healthcare professionals and patients
across geographies.
Ranbaxy's continued focus on R&D has resulted in several approvals in developed
markets and significant progress in New Drug Discovery Research. The Company's
foray into Novel Drug Delivery Systems has led to proprietary "platform
technologies", resulting in a number of products under development. The Company
is serving its customers in over 100 countries and has an expanding
international portfolio of affiliates, joint ventures and alliances, ground
operations in 46 countries and manufacturing operations in 7 countries.
*PROVIGIL(R) is a registered trademark of Cephalon, Inc.
CONTACT: Charles M. Caprariello, Vice President, CorporateCommunications,
Ranbaxy Inc., +1-609-720-5615; or Edwige Buteau, +1-212-994-7517, or Anuj
Baveja, +1-212-994-7552, both of RF Binder Partners Inc. forRanbaxy Inc.
Web site: http://www.ranbaxy.com/
SOURCE Ranbaxy Laboratories Limited
URL: http://www.prnewswire.com
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443 of 998 DOCUMENTS
PR Newswire
December 22, 2005 Thursday 5:00 PM GMT
Cephalon, Inc. Announces Agreement with Ranbaxy Laboratories Limited Regarding
Settlement of PROVIGIL(R) Patent Litigation;
Parties Also Agree to Business Arrangements Related to Modafinil
LENGTH: 866 words
DATELINE: FRAZER, Pa. Dec. 22
Cephalon, Inc.(NASDAQ:CEPH)announced today that it has entered into an agreement
with Ranbaxy Laboratories Limited to settle its pending patent infringement
dispute in the United States related to PROVIGIL(R) (modafinil) Tablets [C-IV].
In connection with the settlement, Cephalon will grant Ranbaxy a non- exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL in the
United States. Ranbaxy's license will become effective in October 2011 in the
absence of a pediatric extension for PROVIGIL, which would delay the entry date
by six months (to April 2012). An earlier entry by Ranbaxy may occur based upon
the entry of another generic version of PROVIGIL.
The companies also agreed to a series of business arrangements related to
modafinil. Specifically, Ranbaxy has agreed to grant to Cephalon a non-
exclusive license, effective immediately, to certain of its worldwide
intellectual property rights related to modafinil in exchange for milestone
payments. Cephalon also has agreed to enter into certain arrangements with
Ranbaxy related to Ranbaxy's supply of the active pharmaceutical ingredient
modafinil.
The terms of the agreement are confidential, and are subject to review by the
U.S. Federal Trade Commission. Financial terms were not disclosed.
The parties will promptly file a dismissal with prejudice with the United States
District Court for the District of New Jersey that will conclude all pending
litigation between the parties regarding PROVIGIL. This settlement and the
previously announced settlements with Teva Pharmaceutical Industries Ltd. and
Teva Pharmaceuticals USA, Inc. do not affect the status of the ongoing PROVIGIL
patent litigations between Cephalon and certain other generic companies that are
pending in the U.S. District Court in New Jersey. These lawsuits claim
infringement of Cephalon's U.S. Patent No. RE37,516 ("the '516 Patent") which
covers pharmaceutical compositions and methods of treatment with the form of
modafinil contained in PROVIGIL. The '516 patent expires in October 6, 2014 and
may be extended by six months (to April 6, 2015) upon submission of pediatric
study data that is acceptable to the U.S. Food and Drug Administration.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon currently
employs approximately 2,600 people in the United States and Europe. U.S. sites
include the company's headquarters in Frazer, Pennsylvania, and offices,
laboratories or manufacturing facilities in West Chester, Pennsylvania, Salt
Lake City, Utah, and suburban Minneapolis, Minnesota.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection, and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding the settlement of this litigation, including
whether the Federal Trade Commission will approve the terms of such settlement,
anticipated scientific progress on its research programs; development of
potential pharmaceutical products; interpretation of clinical results; prospects
for regulatory approval; manufacturing development and capabilities; market
prospects for its products; sales and earnings guidance; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
CONTACT: Media: Robert Grupp, +1-610-738-6402, rgrupp@cephalon.com ;
orInvestors: Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com , both
ofCephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
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LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved.
444 of 998 DOCUMENTS
Internal Medicine News
December 15, 2005
Data Back Broader Narcolepsy Indication for Sodium Oxybate
BYLINE: Bruce Jancin, Denver Bureau
SECTION: Pg. 23 Vol. 38 No. 24 ISSN: 1097-8690
LENGTH: 752 words
DENVER - Sodium oxybate (Xyrem) is effective not only for cataplexy-its only
approved indication at present-but also for the other primary symptoms of
narcolepsy, investigators reported at the annual meeting of the Associated
Professional Sleep Societies.
Based on data from two randomized clinical trials presented at the meeting,
the drug's manufacturer, Orphan Medical Inc., has submitted a supplemental New
Drug Application to the Food and Drug Administration. If approval is granted,
sodium oxybate's expanded indication would make it the first drug approved for
treatment of all the primary symptoms of narcolepsy: excessive daytime
sleepiness; fragmented sleep; and cataplexy, the sudden, brief loss of muscle
tone frequently experienced by narcoleptics during periods of emotional
intensity such as surprise, laughter, or anger.
Terri E. Weaver, Ph.D., noted that in the last few years, quality of life
issues in patients with incurable chronic illnesses have drawn greater
regulatory and clinical attention. And the quality of life impact of narcolepsy,
she stressed, is profound: In one study, the impact was rated greater than
living with Parkinson's disease.
"Individuals with narcolepsy are struggling to complete their activities of
daily living," said Dr. Weaver of the University of Pennsylvania, Philadelphia.
She presented the first-ever study of sodium oxybate's quality of life impact in
narcoleptic patients. The double-blind, placebo-controlled, 8-week trial
involved 228 patients randomized to receive either placebo or 4.5 g, 6 g, or 9 g
sodium oxybate per night in two equally divided doses at bedtime and from 21/2
to 4 hours later.
Quality of life was assessed with the Functional Outcomes of Sleep
Questionnaire administered at baseline, 4 weeks, and 8 weeks. Patients assigned
to 4.5 g/night showed no quality of life gains. But those who received 6 g or 9
g had significant improvement in four of the five domains measured: general
productivity, vigilance, social outcome, and activity level. The only domain in
which they didn't fare significantly better than placebo was the intimacy/sexual
relationships subscale.
The benefit was greater with the 9-g dose. "The effect size was clinically
meaningful and quite large," she noted.
The potential for improved quality of life needs to be presented to patients
in the context of the possible treatment disadvantages so they can make an
informed decision. Patients on sodium oxybate experience a deep sleep and
increased arousal threshold. They may not hear a smoke alarm, a late-night
telephone call, or a child's cry.
"Individuals who have children at home have to weigh the benefit of having a
good night's sleep and being able to function and take care of those children
during the day. We all know daytime sleepiness and some of the other effects of
narcolepsy can be hazardous, too, in terms of caring for young ones," Dr. Weaver
said.
Jed E. Black, M.D., presented another phase III trial, this one designed to
assess the relative efficacy of sodium oxybate when taken as monotherapy or with
modafinil (Provigil), a widely used wakefulness-promoting agent approved for
treatment of the excessive daytime sleepiness component of narcolepsy.
The double-blind, 230-patient trial began with all participants on 200-600
mg/day of modafinil. They were then randomized to receive modafinil plus
placebo, modafinil plus sodium oxybate, placebo plus sodium oxybate, or double
placebos. The sodium oxybate dose was 6 g/night for the first 4 weeks and 9 g
thereafter. Monotherapy with either drug appeared equally effective for the
primary study end point, reduction in excessive daytime sleepiness. The
improvement was greater with the 9-g dose of sodium oxybate than with the 6-g
dose.
But combination therapy was most effective of all, not only in terms of
reduced daytime sleepiness but also consolidation of fragmented sleep and
enhanced slow-wave sleep, said Dr. Black of Stanford (Calif.) University. Side
effects that occurred more often with sodium oxybate than placebo included
nausea, dizziness, headache, sleepiness, and bedwetting.
Prior to its 2002 approval as a tightly controlled schedule-III drug for
cataplexy, sodium oxybate was available as [#x3b3]-hydroxybutyrate in health
food stores. During that era it was abused as a recreational drug and implicated
as a "date rape" drug.
Both randomized trials were sponsored by Orphan Medical. Dr. Weaver serves as
a consultant to the company.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
445 of 998 DOCUMENTS
Generic Line
December 14, 2005
Teva, Cephalon Reach Agreement to End Provigil Patent Dispute
SECTION: Vol. 22, No. 24
LENGTH: 522 words
Teva Pharmaceutical and Cephalon have agreed to settle patent infringement suits
in the U.S. and the UK over Cephalon's narcolepsy drug Provigil.
The settlement could remove one near-term generic threat to Provigil (modafinil)
and its extended-release follow-on -- set to hit the market in early 2006 -- as
well as removing a potential threat to another modafinil formulation Cephalon
plans to market for pediatric attention-deficit/hyperactivity disorder (ADHD).
However, three other generic firms -- Mylan Laboratories, Ranbaxy Laboratories
and Barr Laboratories -- are still poised to market generic Provigil when
Cephalon's orphan drug status expires, which will happen in late December or
next June, depending on whether Cephalon receives a pediatric patent extension.
"The opportunity presented itself and we pursued it," Cephalon spokesman Robert
Grupp told Generic Line. "Investors don't like uncertainty. It made sense to
settle this and remove one element of uncertainty."
Under the agreement, Teva and biopharmaceutical firm Cephalon will file
dismissals with prejudice with the U.S. District Court for the District of New
Jersey as well as the Chancery Division of the UK's High Court of Justice. Teva
will pay Cephalon a royalty for the non-exclusive right to market and sell a
generic version of Provigil, and Teva will manufacture modafinil for Cephalon.
Cephalon, meanwhile, will pay Teva a royalty on Provigil sales. Financial terms
of the deal were not disclosed.
Cephalon sued Teva and three other generic firms in March 2003 after they filed
to market generic Provigil (Generic Line, April 9, 2003, Page 3).
Teva will be able to start selling generic Provigil for the U.S. market in
October 2011 and in Europe by October 2012 -- three years before Provigil's
composition patents for those areas expire. However, Teva could launch generic
Provigil earlier if another generic firm launches a version of the drug.
Provigil was Cephalon's top-selling drug in 2004, generating sales of $439.7
million, and the FDA is poised to approve Nuvigil (armodafinil), an
extended-release version of the drug, in January 2006.
Provigil has also been shown to improve wakefulness, performance and attention
level in patients with shift work sleep disorder.
Meanwhile, Cephalon has also received an approvable letter from the FDA to
market modafinil in a new formulation and dosage for pediatric ADHD in children
ages 6 to 17. Cephalon will market Sparlon with the help of Johnson & Johnson's
McNeil Consumer & Specialty Pharmaceuticals unit, which signed a co-promotion
agreement with Cephalon in August. Once launched, Sparlon could see even greater
commercial success since Eli Lilly in September warned that its ADHD drug
Strattera may increase the risk of suicidal thoughts in adolescents and
children.
Grupp said Cephalon still plans to pursue litigation against Mylan, Ranbaxy and
Barr. No trial date has been set yet for those cases, which have been
consolidated in the New Jersey district court, Grupp said. -- Dar Haddix
(mailto:dhaddix@fdanews.comtarget=_blank)
Release date: Dec. 14, 2005
LOAD-DATE: December 13, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
446 of 998 DOCUMENTS
FDAnews Drug Daily Bulletin
December 13, 2005
TEVA, CEPHALON REACH AGREEMENT TO END PATENT DISPUTE
SECTION: Vol. 2, No. 242
LENGTH: 517 words
Teva Pharmaceutical and Cephalon have agreed to settle patent infringement suits
in the U.S. and the UK over Cephalon's narcolepsy drug Provigil. Under the
agreement, Teva and biopharmaceutical firm Cephalon will file dismissals with
prejudice with the U.S. District Court for the District of New Jersey as well as
the Chancery Division of the UK's High Court of Justice. Cephalon sued Teva and
three other generic firms in March 2003 after they filed to market generic
Provigil. The settlement could remove one near-term generic threat to Provigil
(modafinil) and its extended-release follow-on, set to hit the market in early
2006, as well as a potential threat to Cephalon's forthcoming modafinil-based
drug intended as a treatment for pediatric attention-deficit/hyperactivity
disorder (ADHD) in children ages 6 to 17. With its mild side effects, the ADHD
drug now has even more commercial potential since Eli Lilly in September warned
that its ADHD drug Strattera may increase the risk of suicidal thoughts in
adolescents and children. "The opportunity presented itself and we pursued it,"
Cephalon spokesman Robert Grupp told FDAnews. "Investors don't like uncertainty.
It made sense to settle this and remove one element of uncertainty." However,
three other generic firms -- Mylan Laboratories, Ranbaxy Laboratories and Barr
Laboratories -- are still poised to market generic Provigil when Cephalon's
orphan drug status expires, which will happen in late December or next June,
depending on whether Cephalon receives a pediatric patent extension. Under the
agreement, Teva will be able to start selling generic Provigil for the U.S.
market in October 2011 and in Europe by October 2012 -- three years before
Provigil's composition patents for those areas expire. However, Teva could
launch generic Provigil earlier if another generic firm launches a version of
the drug. Provigil was Cephalon's top-selling drug in 2004, generating sales of
$439.7 million, and the FDA is poised to approve Nuvigil (armodafinil), an
extended-release version of the drug, in January 2006. Provigil has also been
shown to improve wakefulness, performance and attention level in patients with
shift work sleep disorder. Meanwhile, Cephalon has also received an approvable
letter from the FDA to market modafinil in a new formulation and dosage for the
treatment of pediatric ADHD. Cephalon will market Sparlon with the help of
Johnson & Johnson's McNeil Consumer & Specialty Pharmaceuticals unit, which
signed a co-promotion agreement with Cephalon in August. Under the settlement,
Teva will pay Cephalon a royalty for the non-exclusive right to market and sell
a generic version of Provigil, and Teva will manufacture modafinil for Cephalon.
Cephalon meanwhile will pay Teva a royalty on Provigil sales. Financial terms of
the deal were not disclosed. Grupp said Cephalon still plans to pursue
litigation against Mylan, Ranbaxy and Barr. No trial date has been set yet for
those cases, which have been consolidated in the New Jersey district court,
Grupp said.
Release date: Dec. 13, 2005
LOAD-DATE: December 12, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
447 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
December 12, 2005
Teva and Cephalon settle pending Provigil patent infringement dispute
LENGTH: 394 words
Teva Pharmaceutical Industries has entered into an agreement with Cephalon to
settle their pending patent infringement disputes in the US and the UK related
to Provigil ( modafinil ) Tablets C-IV. Provigil is indicated for the treatment
of excessive sleepiness associated with disorders of sleep and wakefulness in
adults. In connection with the settlement, Cephalon will grant Teva a
non-exclusive royalty-bearing right to market and sell a generic version of the
drug.
Teva's licence in the US will become effective in October 2011, without a
paediatric extension for Provigil, which would delay the entry date by six
months (to April 2012). Outside of the US, the parties agreed to comparable
terms for the licence effective date, which generally allow for entry in October
2012. An earlier entry by Teva in any of the territories may occur based upon
the entry of another generic version of the drug. The companies also agreed to a
series of business arrangements related to modafinil. Specifically, Teva has
agreed to grant to Cephalon a non-exclusive licence, effective immediately, to
its worldwide intellectual property rights related to the manufacture,
development and formulation of modafinil in exchange for royalty payments.
Cephalon has also agreed to enter into certain arrangements with Teva related to
the latter's manufacture and supply of the active pharmaceutical ingredient,
modafinil. The terms of the agreement are confidential and are subject to review
by the US Federal Trade Commission. Financial terms were not disclosed. The
parties will promptly file dismissals with prejudice with the US District Court
for the District of New Jersey and the UK High Court of Justice, Chancery
Division, which will conclude all pending litigations between the parties
regarding Provigil. Cephalon's US Patent No. RE37,516 expires on 6th October
2014 and may be extended by six months (to 6th April 2015) upon the submission
of paediatric study data that are acceptable to the FDA. This settlement does
not affect the status of the ongoing Provigil patent litigations between
Cephalon and certain other generic companies that are pending in the US District
Court in New Jersey. These lawsuits claim infringement of Cephalon's US '516
patent, which covers pharmaceutical compositions and methods of treatment with
the form of modafinil contained in Provigil.
LOAD-DATE: December 14, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
448 of 998 DOCUMENTS
Drug Industry Daily
December 12, 2005
Teva, Cephalon Reach Agreement to End Provigil Patent Dispute
SECTION: Vol. 4, No. 241
LENGTH: 527 words
Teva Pharmaceutical and Cephalon have agreed to settle patent infringement suits
in the U.S. and the UK over Cephalon's narcolepsy drug Provigil. Under the
agreement, Teva and biopharmaceutical firm Cephalon will file dismissals with
prejudice with the U.S. District Court for the District of New Jersey as well as
the Chancery Division of the UK's High Court of Justice. Cephalon sued Teva and
three other generic firms in March 2003 after they filed to market generic
Provigil.
The settlement could remove one near-term generic threat to Provigil (modafinil)
and its extended-release follow-on, set to hit the market in early 2006, as well
as a potential threat to Cephalon's forthcoming modafinil-based drug intended as
a treatment for pediatric attention-deficit/hyperactivity disorder (ADHD) in
children ages 6 to 17. With its mild side effects, the ADHD drug now has even
more commercial potential since Eli Lilly in September warned that its ADHD drug
Strattera may increase the risk of suicidal thoughts in adolescents and
children.
"The opportunity presented itself and we pursued it," Cephalon spokesman Robert
Grupp told DID. "Investors don't like uncertainty. It made sense to settle this
and remove one element of uncertainty."
However, three other generic firms -- Mylan Laboratories, Ranbaxy Laboratories
and Barr Laboratories -- are still poised to market generic Provigil when
Cephalon's orphan drug status expires, which will happen in late December or
next June, depending on whether Cephalon receives a pediatric patent extension.
Under the agreement, Teva will be able to start selling generic Provigil for the
U.S. market in October 2011 and in Europe by October 2012 -- three years before
Provigil's composition patents for those areas expire. However, Teva could
launch generic Provigil earlier if another generic firm launches a version of
the drug.
Provigil was Cephalon's top-selling drug in 2004, generating sales of $439.7
million, and the FDA is poised to approve Nuvigil (armodafinil), an
extended-release version of the drug, in January 2006.
Provigil has also been shown to improve wakefulness, performance and attention
level in patients with shift work sleep disorder (DID, Aug. 8, Page 3).
Meanwhile, Cephalon has also received an approvable letter from the FDA to
market modafinil in a new formulation and dosage for the treatment of pediatric
ADHD. Cephalon will market Sparlon with the help of Johnson & Johnson's McNeil
Consumer & Specialty Pharmaceuticals unit, which signed a co-promotion agreement
with Cephalon in August (DID, Oct. 24, Page 3).
Under the settlement, Teva will pay Cephalon a royalty for the non-exclusive
right to market and sell a generic version of Provigil, and Teva will
manufacture modafinil for Cephalon. Cephalon meanwhile will pay Teva a royalty
on Provigil sales. Financial terms of the deal were not disclosed.
Grupp said Cephalon still plans to pursue litigation against Mylan, Ranbaxy and
Barr. No trial date has been set yet for those cases, which have been
consolidated in the New Jersey district court, Grupp said. -- Dar Haddix
Release date: Dec. 12, 2005
LOAD-DATE: December 9, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
449 of 998 DOCUMENTS
Globes [online] - Israel's Business Arena
December 11, 2005 Sunday
Teva and Cephanol settle dispute over Provigil;
Teva will be able to sell a generic version of wakefulness drug Provigil in
October 2011.
BYLINE: Globes correspondent
LENGTH: 268 words
Teva Pharmaceutical Industries Ltd. (Nasdaq: TEVA ; TASE: TEVA) and Teva
Pharmaceuticals USA, Inc. have entered into an agreement with Cephalon, Inc.
(Nasdaq: CEPH) to settle their pending patent infringement disputes in the US
and the UK over Provigil (modafinil) tablets.
Provigil is a mood-brightening and memory-enhancing psychostimulant which
enhances wakefulness and vigilance.
Cephalon will grant Teva a non-exclusive royalty-bearing right to market and
sell a generic version of Provigil. Teva's license in the US will become
effective in October 2011 absent a pediatric extension for Provigil, which would
delay the entry date by six months (to April 2012). Outside the US, the parties
agreed to comparable terms for the license effective date, which generally allow
for entry in October 2012. An earlier entry by Teva in any of the territories
may occur based upon the entry of another generic version of Provigil.
The companies also agreed to a series of business arrangements related to
modafinil. Teva has agreed to grant to Cephalon a non-exclusive license,
effective immediately, to its worldwide intellectual property rights related to
the manufacture, development and formulation of modafinil in exchange for
royalty payments. Cephalon has also agreed to enter into certain arrangements
with Teva related to Teva's manufacture and supply of the active pharmaceutical
ingredient modafinil.
The terms of the agreement are subject to review by the US Federal Trade
Commission.
Financial terms were not disclosed.
Published by Globes [online], Israel business news - www.globes.co.il - on
December 11, 2005
LOAD-DATE: December 11, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2005 Globes Publisher Itonut (1983) Ltd.
All Rights Reserved
450 of 998 DOCUMENTS
Business Wire
December 9, 2005 Friday 1:45 PM GMT
Teva Announces Agreement with Cephalon Regarding Settlement of PROVIGIL(R)
Patent Litigation; Parties Also Agree to Business Arrangements Related to
Modafinil
LENGTH: 895 words
DATELINE: JERUSALEM Dec. 9, 2005
Teva Pharmaceutical Industries Ltd. (Nasdaq: TEVA) and Teva Pharmaceuticals USA,
Inc. announced today that they have entered into an agreement with Cephalon,
Inc. (Nasdaq: CEPH) to settle their pending patent infringement disputes in the
United States and the United Kingdom related to PROVIGIL(R) (modafinil) Tablets
(C-IV).
In connection with the settlement, Cephalon will grant Teva a non-exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL. Teva's
license in the United States will become effective in October 2011 absent a
pediatric extension for PROVIGIL, which would delay the entry date by six months
(to April 2012). Outside the United States, the parties agreed to comparable
terms for the license effective date, which generally allow for entry in October
2012. An earlier entry by Teva in any of the territories may occur based upon
the entry of another generic version of PROVIGIL.
The companies also agreed to a series of business arrangements related to
modafinil. Specifically, Teva has agreed to grant to Cephalon a non-exclusive
license, effective immediately, to its worldwide intellectual property rights
related to the manufacture, development and formulation of modafinil in exchange
for royalty payments. Cephalon has also agreed to enter into certain
arrangements with Teva related to Teva's manufacture and supply of the active
pharmaceutical ingredient modafinil.
The terms of the agreement are confidential, and are subject to review by the
U.S. Federal Trade Commission. Financial terms were not disclosed.
The parties will promptly file dismissals with prejudice with the United States
District Court for the District of New Jersey and United Kingdom High Court of
Justice, Chancery Division, which will conclude all pending litigations between
the parties regarding PROVIGIL. Cephalon's U.S. Patent No. RE37,516 expires in
October 6, 2014 and may be extended by six months (to April 6, 2015) upon
submission of pediatric study data that is acceptable to the U.S. Food and Drug
Administration.
Teva Pharmaceutical Industries Ltd., headquartered in Israel, is among the top
20 pharmaceutical companies and among the largest generic pharmaceutical
companies in the world. The company develops, manufactures and markets generic
and innovative human pharmaceuticals and active pharmaceutical ingredients.
Close to 90% of Teva's sales are in North America and Europe.
Safe Harbor Statement under the U. S. Private Securities Litigation Reform Act
of 1995: This release contains forward-looking statements, which express the
current beliefs and expectations of management. Such statements are based on
management's current beliefs and expectations and involve a number of known and
unknown risks and uncertainties that could cause Teva's future results,
performance or achievements to differ significantly from the results,
performance or achievements expressed or implied by such forward-looking
statements. Important factors that could cause or contribute to such differences
include whether and when the proposed acquisition of IVAX Corporation will be
consummated and the terms of any conditions imposed in connection with such
closing, the terms and conditions of the financing utilized by Teva for the IVAX
acquisition, Teva's ability to rapidly integrate IVAX's operations and achieve
expected synergies, Teva's ability to successfully develop and commercialize
additional pharmaceutical products, the introduction of competitive generic
products, the impact of competition from brand-name companies that sell or
license their own generic products under generic trade dress and at generic
prices (so called "authorized generics") or seek to delay the introduction of
generic products, regulatory changes that may prevent Teva from exploiting
exclusivity periods, potential liability for sales of generic products prior to
a final court decision, including that relating to the generic versions of
Neurontin(R) and Allegra(R), the effects of competition on Copaxone(R) sales,
the impact of pharmaceutical industry regulation and pending legislation that
could affect the pharmaceutical industry, the difficulty of predicting U.S. Food
and Drug Administration, European Medicines Association and other regulatory
authority approvals, the regulatory environment and changes in the health
policies and structure of various countries, Teva's ability to successfully
identify, consummate and integrate acquisitions, exposure to product liability
claims, dependence on patent and other protections for innovative products,
significant operations outside the United States that may be adversely affected
by terrorism or major hostilities, fluctuations in currency, exchange and
interest rates, operating results and other factors that are discussed in Teva's
Annual Report on Form 20-F and its other filings with the U.S. Securities and
Exchange Commission. Forward-looking statements speak only as of the date on
which they are made and the Company undertakes no obligation to update publicly
or revise any forward-looking statement, whether as a result of new information,
future developments or otherwise.
CONTACT: Teva Pharmaceutical Industries Ltd. Dan Suesskind, (011) 972-2-589-2840
or Teva North America George Barrett, (215) 591-3030 or Investor Relations:
Liraz Kalif, (011) 972-3-926-7554 or Kevin Mannix, (215) 591-8912
URL: http://www.businesswire.com
LOAD-DATE: December 10, 2005
LANGUAGE: ENGLISH
DISTRIBUTION: Pharmaceutical Writers; Business Editors
PUBLICATION-TYPE: Newswire
Copyright 2005 Business Wire, Inc.
451 of 998 DOCUMENTS
PR Newswire
December 9, 2005 Friday 1:45 PM GMT
Cephalon, Inc. Announces Agreement with Teva Pharmaceutical Industries Ltd.
Regarding Settlement of PROVIGIL(R) Patent Litigation;
Parties Also Agree to Business Arrangements Related to Modafinil
LENGTH: 902 words
DATELINE: FRAZER, Pa. Dec. 9
Cephalon, Inc.(NASDAQ:CEPH)announced today that it has entered into an agreement
with Teva Pharmaceutical Industries Ltd.(NASDAQ:TEVA)and Teva Pharmaceuticals
USA, Inc. to settle its pending patent infringement disputes in the United
States and the United Kingdom related to PROVIGIL(R) (modafinil) Tablets [C-IV].
In connection with the settlement, Cephalon will grant Teva a non- exclusive
royalty-bearing right to market and sell a generic version of PROVIGIL. Teva's
license in the United States will become effective in October 2011 absent a
pediatric extension for PROVIGIL, which would delay the entry date by six months
(to April 2012). Outside the United States, the parties agreed to comparable
terms for the license effective date, which generally allow for entry in October
2012. An earlier entry by Teva in any of the territories may occur based upon
the entry of another generic version of PROVIGIL.
The companies also agreed to a series of business arrangements related to
modafinil. Specifically, Teva has agreed to grant to Cephalon a non-exclusive
license, effective immediately, to its worldwide intellectual property rights
related to the manufacture, development and formulation of modafinil in exchange
for royalty payments. Cephalon has also agreed to enter into certain
arrangements with Teva related to Teva's manufacture and supply of the active
pharmaceutical ingredient modafinil.
The terms of the agreement are confidential, and are subject to review by the
U.S. Federal Trade Commission. Financial terms were not disclosed.
The parties will promptly file dismissals with prejudice with the United States
District Court for the District of New Jersey and United Kingdom High Court of
Justice, Chancery Division, which will conclude all pending litigations between
the parties regarding PROVIGIL.
This settlement does not affect the status of the ongoing PROVIGIL patent
litigations between Cephalon and certain other generic companies that are
pending in the U.S. District Court in New Jersey. These lawsuits claim
infringement of Cephalon's U.S. Patent No. RE37,516 ("the '516 Patent") which
covers pharmaceutical compositions and methods of treatment with the form of
modafinil contained in PROVIGIL. The '516 patent expires in October 6, 2014 and
may be extended by six months (to April 6, 2015) upon submission of pediatric
study data that is acceptable to the U.S. Food and Drug Administration.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon currently
employs approximately 2,500 people in the United States and Europe. U.S. sites
include the company's headquarters in Frazer, Pennsylvania, and offices,
laboratories or manufacturing facilities in West Chester, Pennsylvania, Salt
Lake City, Utah, and suburban Minneapolis, Minnesota.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection, and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding the settlement of this litigation, including
whether the Federal Trade Commission will approve the terms of such settlement,
anticipated scientific progress on its research programs; development of
potential pharmaceutical products; interpretation of clinical results; prospects
for regulatory approval; manufacturing development and capabilities; market
prospects for its products; sales and earnings guidance; and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
CONTACT: Media: Robert Grupp, +1-610-738-6402, rgrupp@cephalon.com ,
orInvestors: Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com , both
ofCephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: November 29, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 PR Newswire Association LLC.
All Rights Reserved.
452 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
December 6, 2005
Sparlon significantly improves ADHD symptoms in children and adolescents
LENGTH: 394 words
Results of a clinical study evaluating Sparlon ( modafinil ) Tablets (C-IV) for
the treatment of attention-deficit hyperactivity disorder (ADHD) in children and
adolescents have been published in the December issue of Pediatrics
(2005;116:e777-e784). In the study, modafinil significantly improved the
symptoms associated with ADHD as reported by physicians, parents and teachers,
and was generally well tolerated. The published trial is one of three pivotal
studies of Sparlon for the treatment of ADHD in children and adolescents. The
nine-week, double-blind, flexible-dose study included 248 children and
adolescents with ADHD (ages six to 17 years) who were randomised to either
once-daily Sparlon or placebo.
The primary endpoint was the teacher/physician-completed ADHD Rating Scale-IV
(ADHD-RS-IV) School Version total score. Symptom improvement was also rated
using a variety of other scales, including evaluations by parents. In the study,
patients treated with Sparlon showed significantly greater improvement than with
placebo in the core symptoms of ADHD at school and home (both p<0.0001). By the
end of the study, 48 per cent of Sparlon-treated patients were rated by
physicians as "much" or "very much" improved compared with 17 per cent of
patients who received placebo (p<0.0001). In the study, the drug was generally
well tolerated and discontinuation rates due to adverse events (AEs) were not
significantly different from placebo. The most common AEs associated with
Sparlon were generally mild-to-moderate in nature and included insomnia,
headache and decreased appetite. Sparlon, marketed by Cephalon , is a new dosage
form of modafinil, the active ingredient in the company's Provigil Tablets
(C-IV), which is approved for the treatment of adults with excessive sleepiness
associated with narcolepsy, obstructive sleep apnoea/hypopnoea syndrome and
shift work sleep disorder. Provigil is not approved to treat ADHD. In August
2005, Cephalon announced an agreement with McNeil Consumer & Specialty
Pharmaceuticals Division of McNeil-PPC ( Johnson & Johnson ) to co-promote
Sparlon. Cephalon has submitted data to the FDA requesting approval to market
Sparlon for the treatment of ADHD in children and adolescents. The FDA has not
yet determined that the drug is safe and effective. If approved, Sparlon is
expected to be available in early 2006.
LOAD-DATE: December 9, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
453 of 998 DOCUMENTS
PR Newswire
December 5, 2005 Monday 12:15 PM GMT
Pediatrics Publishes Pivotal Study Showing SPARLON(TM) Significantly Improves
ADHD Symptoms in Children and Adolescents
LENGTH: 1008 words
DATELINE: FRAZER, Pa. Dec. 5
Cephalon, Inc.(NASDAQ:CEPH)today announced that results of a clinical study
evaluating SPARLON(TM) (modafinil) Tablets [C-IV] for the treatment of
attention- deficit/hyperactivity disorder (ADHD) in children and adolescents
have been published in this month's issue of Pediatrics, the peer-reviewed
journal of the American Academy of Pediatrics. In the study, SPARLON
significantly improved the symptoms associated with ADHD as reported by
physicians, parents and teachers, and was generally well tolerated.
"In this study, children and adolescents treated with once-daily SPARLON showed
improvement in ADHD symptoms, including inattention, impulsivity, and
hyperactivity, both at school and at home," said Joseph Biederman, M.D., chief,
Department of Pediatric Psychopharmacology, Massachusetts General Hospital,
professor of Psychiatry at Harvard Medical School, and a lead investigator in
the trial. "SPARLON also was associated with a favorable side effect profile."
About the Study
The published study is one of three pivotal studies of SPARLON for the treatment
of ADHD in children and adolescents. The nine-week, double-blind, flexible-dose
study included 248 children and adolescents with ADHD (ages six to 17 years) who
were randomized to either once-daily SPARLON or placebo. The primary endpoint
was the teacher/physician-completed ADHD Rating Scale-IV (ADHD-RS-IV) School
Version total score. Symptom improvement also was rated using a variety of other
scales, including evaluations by parents.
In the study, patients treated with SPARLON showed significantly greater
improvement than with placebo in the core symptoms of ADHD at school and home
(both p<0.0001). By the end of the study, 48 percent of patients treated with
SPARLON were rated by physicians as "much" or "very much" improved compared with
17 percent of patients who received placebo (p<0.0001).
In the study, SPARLON was generally well tolerated and discontinuation rates due
to adverse events were not significantly different from placebo. The most common
adverse events associated with SPARLON were generally mild to moderate in nature
and included insomnia, headache and decreased appetite.
SPARLON
SPARLON is a new dosage form of modafinil, the active ingredient in PROVIGIL(R)
(modafinil) Tablets [C-IV], which is approved for the treatment of adults with
excessive sleepiness associated with narcolepsy, obstructive sleep
apnea/hypopnea syndrome and shift work sleep disorder. PROVIGIL is not approved
to treat ADHD. Cephalon has submitted data to the FDA requesting approval to
market SPARLON for the treatment of ADHD in children and adolescents. The FDA
has not yet determined that SPARLON is safe and effective. If approved, SPARLON
is expected to be available in early 2006.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 2,500 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, Pennsylvania,
and offices, laboratories or manufacturing facilities in West Chester,
Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis, Minnesota.
Cephalon's European headquarters are located in Maisons-Alfort, France and other
European offices are located in Guildford, England, and Martinsried, Germany.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, including the results of the SPARLON clinical trials,
prospects for final regulatory approval of SPARLON, including the anticipated
timetable for the launch of the product, manufacturing development and
capabilities, market prospects for its products, particularly with respect to
SPARLON sales and earnings guidance, and other statements regarding matters that
are not historical facts. You may identify some of these forward-looking
statements by the use of words in the statements such as "anticipate,"
"estimate," "expect," "project," "intend," "plan," "believe" or other words and
terms of similar meaning. Cephalon's performance and financial results could
differ materially from those reflected in these forward-looking statements due
to general financial, economic, regulatory and political conditions affecting
the biotechnology and pharmaceutical industries as well as more specific risks
and uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media, Jenifer Antonacci of Cephalon, +1-610-738-6674,
jantonac@cephalon.com , or Kerry Dixon, +1-720-216-0011, or kdixon@gcigroup.com
, for Cephalon, or Investors, Robert (Chip) Merritt ofCephalon, +1-610-738-6376,
cmerritt@cephalon.com
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: November 29, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 PR Newswire Association LLC.
All Rights Reserved.
454 of 998 DOCUMENTS
The Evening Standard (London)
November 28, 2005 Monday
Spend money on buses, not Kiley
SECTION: A MERGE; Pg. 43
LENGTH: 1151 words
FURTHER to the outrage at Bob Kiley's "golden farewell", I support people being
remunerated if they deserve it. The more pressing issue is that while TfL
managers are being richly rewarded, the employees on whom commuters most rely
are being given a rough deal (25 November).
Bus travel requires good, dedicated drivers, yet increasingly passengers are
complaining about poor service and bumpy rides. Little wonder as since
privatisation, drivers have been denied access to the London Transport
Superannuation Fund and have little incentive to stay put. Bus companies'
pension policies are little better than savings schemes.
Buses are the transport of the future, because they are an effective use of
existing infrastructure. Yet the different bus companies in London have
different internal layout and design; if you ask a Metroline employee when the
next Stagecoach bus is coming they can't tell you and are not allowed to due to
commercial confidentiality.
In New York, Kiley famously came to an accommodation with the subway unions and
in London he fought against Tube privatisation.
Will his successor have more success in restoring some sense to our bus system?
Nick Warner, N4.
YOU report that there are 30,245 people who have applied for compensation for
injuries sustained on London streets since 2000. The real figure may be
significantly worse, depending on how many claims are still "in process", and
the details provided seem to exclude Transport for London's highways, (24
November) My experience suggests the failure of transport contract management as
much as the compensation culture may lie behind this situation. Since my
retirement as Camden's chief engineer, it has become clear that no one from the
council has been properly monitoring repairs that contractors are paid Pounds
1.2 million a year in advance to carry out.
Over the past year, I have publicised 350 photographs of unfixed repairs but the
council has still not apparently addressed these problems.
This is also an issue in other boroughs - in Enfield, there is a pothole that
has not been fixed for eight months.
Meanwhile, Transport for London has told me that it has no specifications for
controlling the storage of materials and equipment on its roads, which present
major hazards, especially at night.
Bob Kiley's successor should lead a campaign for "zero tolerance" of highway
defects and the attitudes that allow them to pass.
Dugald Gonsal, NW3.
Don't mess with medicine
FURTHER to your feature: The Genius Pill: would you be an idiot to take it?
(22 November) in which the prescription-only drug modafinil was purchased over
the internet and taken by three Evening Standard journalists, we wish to
emphasise as licence holders of Provigil (modafinil) in the UK that the drug
should only be used under the guidance of a doctor.
Modafinil is indicated for the treatment of excessive sleepiness and is not a
"cognitive-enhancing drug". Any attempts to demonstrate the medication is
"memory-enhancing" or "mind-sharpening" are therefore ill-founded at best.
We agree with Alice Hart-Davis's remark that "there's nothing clever about
taking drugs without a prescription", and hope your readers take on board Dr
Ebrahim's comment that "these medications shouldn't be used for purposes for
which they are not licensed".
Dr Alan McDougall, medical director, Cephalon UK Ltd.
Kids are great sometimes
I HAVE great sympathy for Liz Jones, who is dreading Christmas because of the
contempt she is held in as a childless woman (22 November).
I chose a partnership without children but have goddaughters and nephews to take
on trips and buy presents for, and I can't understand the "me" generation who
aren't happy unless you spoil their children as much as they do.
Jones should practise tough love and inform any friends who tell her what their
children "want" for Christmas that they'll get nothing at all.
I pay my taxes, but do I get a handout or special treatment for not having
children? I am sick of seeing family offers on posters and adverts, and yet when
I choose to attend something I would consider an adult event I can guarantee my
shins will be battered by a passing pram.
Don't get me wrong - I love children, but I don't think they should take over
everybody's life.
Geoff Askey, Harrow.
LIZ Jones's candid tales of her neuroses make me smile, but she really must try
to understand the true concept of what it is to have children.
What does she mean when she describes having kids as making a "lifestyle
choice"?
Does she think it's like deciding whether to buy another cat and give it a
cashmere blanket for Christmas?
I hope she shows more tolerance of other people's children when they're grown up
and attending to her myriad needs.
Ania Zawisza, W12.
Clarkson's so rude, they'll love him in the US YOU speculate whether Jeremy
Clarkson's nonappearance at the international Emmys in the US, at which he won
an award, was to do with his track record of faux pas or because he had
something better to do (21 November).
Surely the reality is much more disturbing - that he is preparing to break into
America and understands that this is the sort of uncouth and superior behaviour
expected of a US star. Certainly his personality and the Top Gear programme
would go down a storm there - without irony.
Perhaps Clarkson sees a gap in the market for a man of his style, after the
extent to which Graham Norton has been praised by American critics as a master
of comedy.
I trust that Clarkson's friend AA Gill will be able to take him down a peg.
George Brooks, W12.
Kids are great sometimes
I HAVE great sympathy for Liz Jones, who is dreading Christmas because of the
contempt she is held in as a childless woman (22 November).
I chose a partnership without children but have goddaughters and nephews to take
on trips and buy presents for, and I can't understand the "me" generation who
aren't happy unless you spoil their children as much as they do.
Jones should practise tough love and inform any friends who tell her what their
children "want" for Christmas that they'll get nothing at all.
I pay my taxes, but do I get a handout or special treatment for not having
children? I am sick of seeing family offers on posters and adverts, and yet when
I choose to attend something I would consider an adult event I can guarantee my
shins will be battered by a passing pram.
Don't get me wrong - I love children, but I don't think they should take over
everybody's life.
Geoff Askey, Harrow.
LIZ Jones's candid tales of her neuroses make me smile, but she really must try
to understand the true concept of what it is to have children.
What does she mean when she describes having kids as making a "lifestyle
choice"?
Does she think it's like deciding whether to buy another cat and give it a
cashmere blanket for Christmas?
I hope she shows more tolerance of other people's children when they're grown up
and attending to her myriad needs.
Ania Zawisza, W12.
LOAD-DATE: November 28, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2005 Associated Newspapers Ltd.
All Rights Reserved
455 of 998 DOCUMENTS
The Evening Standard (London)
November 22, 2005 Tuesday
The Genius Pill: would y you be an idiot to take it?;
It's said to give you extra brainpower and is the smart new drug in the US. Now
it's available on the internet. But does it work?
BYLINE: ALICE HART-DAVIS
SECTION: A SPR; Pg. 32
LENGTH: 862 words
AT 2.45am, I send two emails then sit back and rub my eyes. They're burning with
fatigue, which isn't surprising since I've been awake since 5.30am the previous
day. What is astonishing, though, is that my brain feels as sharp as it did
midmorning.
I have achieved this spectacular lucidity by obtaining over the internet a
prescription drug that might easily become a lifestyle aid among London's
professional elite. Yet, as we all know, nothing is ever simple with drugs - and
there are serious questions to be answered. There is no such thing as a free
lunch.
Modafinil is a "cognitive-enhancement" drug licensed in Britain and the US for
the treatment of narcolepsy (a rare disorder in which patients fall asleep
during the day) but is fast becoming the pep pill of choice for anyone who needs
their brain to be working in overdrive or wants to stay up all night and still
be functional the next day.
Made by pharmaceutical company Cephalon and variously branded as Provigil or
Modavigil, it can keep a person awake and alert for up to 90 hours without
either the highs or jitters that amphetamines or caffeine would induce. It is
huge in the States (American Vogue devoted four pages to it this month) with
sales doubling from a million in 2002 to two million last year. Its properties
are also highly regarded by the military; French soldiers use modafinil and the
British MoD has bought more than 24,000 tablets since 1998.
It is not precisely known how modafinil - otherwise known as
2-diphenylmethyl)sulfinyl]acetamide - works, though it appears to act on the
central nervous system, slowing the release of GABA, a sleep-promoting amino
acid, in the brain. It is a crystalline powder described as a "psychostimulant",
but there is no "high", making it unlikely to become a street drug, and it's
slow to act, taking a couple of hours to kick in.
Dr Irshaad Ebrahim, medical director of the London Sleep Centre, describes the
drug as highly effective in combating narcolepsy. He also uses it for other
sleep disorders and knows it is used by US Air Force pilots in Iraq to raise
alertness. "It has been proven not to be addictive in clinical trials, which
differentiates it from amphetamines," he says.
"But there are two problems associated with its use. A significant number of
people who take it get headaches, though these usually disappear within a couple
of weeks of daily use. There are also some cardiovascular effects, which are
potentially dangerous in high doses (some narcoleptics need 10 100mg pills a
day); raised blood pressure and abnormal heart rhythms." There are other listed
side effects, too, including nausea, diarrhoea, dry mouth, loss of appetite,
sore throat, dizziness and nervous feelings.
So how do those willing to take the risk get hold of the drug? Some doctors, it
is said, have been surprised at how many young professionals visiting their
clinics claim to have previously undiagnosed narcolepsy, but no doctor of my
acquaintanc e would contemplate prescribing a medicine I obviously didn't need.
"I could be struck of f for doing that," said one.
Finally, I order it off the internet, which is disturbingly easy. For Pounds
49.11, Inhousepharmacy. co. uk sent me 30 pills, no questions asked, which
showed up eight days later, postmarked Vanuatu, an island in the South Pacific.
Dr Ebrahim is appalled.
"These medications shouldn't be used for purposes for which they are not
licensed," he says.
I take one 100mg pill, half the normal dose, first thing in the morning.
After a while I feel anxious. The feeling gets worse and I can't settle at my
desk.
Gradually a sense of purpose comes on and I need to get on with my work. I make
calls, work through the post, write emails. But I find I am frequently typing
gibberish and have to edit the words carefully.
My husband tells me I'm gabbling when I talk.
And though I'm working hard, I'm not prioritising. By lunchtime, I haven't
dispatched any of the three pieces waiting to be written, nor done my bit
organising the school bazaar.
Yet I feel keyed up and I know it's not caffeine or adrenaline doing it.
At least there's no hint of the crushing fatigue that usually sets in for an
hour after lunch and of all the possible side effects listed for the medication,
I can only tick dry mouth, nervousness and loss of appetite.
The afternoon is calmer. The anxiety goes, replaced with a clear, tense focus. I
organise the children and cook dinner for friends. I daren't drink, worried
about the effect of alcohol when combined with modafinil. I'm not hungry,
either, and everything tastes a bit odd. When they go, I return to my desk. I
normally work at night, but not past midnight. Tonight, however, it's easy.
By 3am, I go to bed. One occasional modafinil user I spoke to warned me I might
need sleeping pills, but I drop off instantly and am astonished to find, when my
small son wakes me three hours later, that I feel fine. I feel awake and alert
all day.
It may be billed as a "clever pill", but I'm well aware that there's nothing
clever about taking taking drugs without a prescription. The thing is, though,
this pill worked for me.
Would I take it again? I'm afraid it's only a question of when.
LOAD-DATE: November 22, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2005 Associated Newspapers Ltd.
All Rights Reserved
456 of 998 DOCUMENTS
Family Practice News
November 1, 2005
Caffeine, Medications Treat Excessive Sleepiness
BYLINE: Sherry Boschert, San Francisco Bureau
SECTION: Pg. 74 Vol. 35 No. 21 ISSN: 0300-7073
LENGTH: 641 words
SAN DIEGO - All three main treatments for problem sleepiness can perk
patients up, but they differ in cost and side effects, Milton Erman, M.D., said
at a psychopharmacology congress sponsored by the Neuroscience Education
Institute.
Caffeine is the cheapest, most accessible, and most widely used stimulant.
The two other treatment options are prescription medications, which are more
expensive: modafinil or CNS stimulants (most commonly amphetamines or
methylphenidate).
Tolerance to caffeine develops rapidly, however, and there's a moderate risk
for dependence. Stopping a daily caffeine habit too quickly can trigger a
"caffeine headache." Side effects from regularly drinking caffeine include
nervousness, irritability, insomnia, and GI problems, said Dr. Erman of the
University of California, San Diego.
"Many of my insomniac patients tell me proudly that they aren't using
caffeine" to indicate that caffeine can't be blamed for their insomnia, he said.
Ironically, a good cup of caffeine in the morning may be just what they need.
"The problem with many of these insomniac patients is that they can't get going,
get functioning in the morning," he explained. Limited use of caffeine in the
morning may help them function better.
Use of CNS stimulants also leads to tolerance, and they have a high potential
for dependence. Side effects from use include nervousness, headaches, insomnia,
anorexia, GI problems, and mood changes. General CNS stimulants such as
amphetamines have a high risk of abuse and hyperactivity because of their broad
mechanism of action.
One experimental study of sleep deprivation that compared amphetamines with
modafinil treatment to maintain wakefulness suggested that the two drugs are
equally potent. In real life, however, "I think amphetamines are more potent,"
he said. Patients with narcolepsy who have used amphetamines in the past often
aren't satisfied with the effects of modafinil.
Modafinil works more specifically on wakefulness circuits and has fewer side
effects than other stimulants. Tolerance is not an issue-it maintains most of
its efficacy over time-and use of the drug does not lead to dependence. Side
effects include headache, nausea, dry mouth, insomnia, and hyperactivity.
The risk of headache relates to the dosing of modafinil. In early research on
the drug, headache appeared primarily in patients who titrated up to a dose of
400 mg/day by the third day. In subsequent research that gave patients 7-9 days
to titrate up to 400 mg/day, headache was much less of a problem, Dr. Erman
said.
"Modafinil works quite well, particularly if we're not talking about the most
severely hypersomnolent patients," such as narcoleptics who have become
accustomed to taking stimulants, he said.
Dr. Erman is a speaker and consultant for, and has received research funding
from, the company that makes modafinil, Cephalon Inc. Modafinil is approved to
treat sleepiness from shift work, narcolepsy, and sleep apnea.
The most common cause of problem sleepiness is sleep apnea, which occurs in
perhaps 10% of the population, he said. Restless leg syndrome can interrupt
sleep and lead to daytime sleepiness. Narcolepsy is fairly uncommon. Insomnia
can cause excessive sleepiness, but more often, insomniac patients are
hypervigilant. "If anything, they are more alert" than they want to be, he said.
Secondary causes of sleepiness include chronic pain and any medical condition
that causes pain or discomfort, which may interrupt sleep. Medications used to
alleviate pain also can lead to daytime sleepiness because they affect breathing
during sleep and increase the risk for sleep apnea.
Check to see if patients who complain of sleepiness are taking drugs that may
cause sedation or that disrupt sleep, Dr. Erman added, and consider alternative
therapies.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
457 of 998 DOCUMENTS
Internal Medicine News
November 1, 2005
Treatments for Excess Sleepiness Compared
BYLINE: Sherry Boschert, San Francisco Bureau
SECTION: Pg. 36 Vol. 38 No. 21 ISSN: 1097-8690
LENGTH: 656 words
SAN DIEGO - All three main treatments for problem sleepiness-caffeine,
modafinil, and central nervous system stimulants-can perk patients up, but they
differ in cost and side effects, Milton Erman, M.D., said at a
psychopharmacology congress sponsored by the Neuroscience Education Institute.
Caffeine is the cheapest, most accessible, and most widely used stimulant.
The two other treatment options are prescription medications, which are more
expensive: modafinil or CNS stimulants (most commonly amphetamines or
methylphenidate).
Tolerance to caffeine develops rapidly, however, and there's a moderate risk
for dependence. Stopping a daily caffeine habit too quickly can trigger a
"caffeine headache." Side effects from regularly drinking caffeine include
nervousness, irritability, insomnia, and GI problems, said Dr. Erman of the
University of California, San Diego. "Many of my insomniac patients tell me
proudly that they aren't using caffeine" to indicate that caffeine can't be
blamed for their insomnia, he said.
Ironically, a good cup of caffeine in the morning may be just what they need.
"The problem with many of these insomniac patients is that they can't get going,
get functioning in the morning," he explained. Limited use of caffeine in the
morning may help them function better.
Use of CNS stimulants also leads to tolerance, and they have a high potential
for dependence. Side effects from use include nervousness, headaches, insomnia,
anorexia, GI problems, and mood changes. General CNS stimulants such as
amphetamines have a high risk of abuse and hyperactivity because of their broad
mechanism of action.
One experimental study of sleep deprivation that compared amphetamines with
modafinil treatment to maintain wakefulness suggested that the two drugs are
equally potent. In real life, however, "I think amphetamines are more potent,"
he said.
Modafinil works more specifically on wakefulness circuits and has fewer side
effects than other stimulants. Tolerance is not an issue, and use does not lead
to dependence. Side effects include headache, nausea, dry mouth, insomnia, and
hyperactivity.
The risk of headache relates to the dosing of modafinil. In early research on
the drug, headache appeared primarily in patients who titrated up to a dose of
400 mg/day by the third day. In subsequent research that gave patients 7-9 days
to titrate up to 400 mg/day, headache was much less of a problem, Dr. Erman
said.
"Modafinil works quite well, particularly if we're not talking about the most
severely hypersomnolent patients," such as narcoleptics who have become
accustomed to taking stimulants, he said.
Dr. Erman is a speaker and consultant for, and has received research funding
from, the company that makes modafinil, Cephalon Inc. Modafinil is approved to
treat sleepiness from shift work, narcolepsy, and sleep apnea.
The most common cause of problem sleepiness is sleep apnea, which occurs in
perhaps 10% of the population, he said. Restless leg syndrome can interrupt
sleep and lead to daytime sleepiness. Narcolepsy is fairly uncommon. Insomnia
can cause excessive sleepiness, but more often, insomniac patients are
hypervigilant. "If anything, they are more alert" than they want to be, he said.
Secondary causes of sleepiness include any medical condition that causes pain
or discomfort, which may interrupt sleep. Pain medications also can lead to
daytime sleepiness as they affect breathing during sleep and increase the risk
for sleep apnea.
Check to see if patients who complain of sleepiness are taking drugs that
cause sedation or disrupt sleep, Dr. Erman added, and consider alternative
therapies.
Lifestyle issues, such as graveyard shift work, also contribute to excessive
sleepiness. The pace of U.S. culture commonly leads to chronic sleep deprivation
that affects daytime function. "As a society, we really haven't dealt with
this," he said.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
458 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
October 24, 2005
Cephalon receives approvable letter for Sparlon
LENGTH: 306 words
Cephalon has received an approvable letter from the FDA to market Sparlon (
modafinil ) Tablets (C-IV) for the treatment of attention deficit hyperactivity
disorder (ADHD) in children and adolescents ages six through 17 years. The
company submitted an sNDA to the FDA in December 2004. Cephalon expects to
launch Sparlon, a proprietary dosage form of modafinil, in early 2006, subject
to final FDA approval.
In August 2005, Cephalon announced an agreement with McNeil Consumer & Specialty
Pharmaceuticals Division of McNeil-PPC ( Johnson & Johnson ) to co-promote
Sparlon. Cephalon also presented, for the first time, results of integrated
analyses of efficacy and safety data from its three pivotal trials evaluating
Sparlon for the treatment of ADHD in children and adolescents at a major medical
meeting of child and adolescent psychiatrists in Toronto, Canada. The three
Phase III studies, in which more than 600 children and adolescents (ages six
through 17 years) with ADHD were randomised to treatment with Sparlon or
placebo, included two identically-designed, nine-week, flexible-dosage studies
and one seven-week, fixed-dosage study. Patients treated with Sparlon
experienced significant improvement compared to placebo as early as the first
week, with continued improvement during titration and dose maintenance. In the
trials, Sparlon was generally well tolerated and discontinuation rates due to
adverse events were not significantly different from placebo. The most common
adverse events associated with Sparlon were generally mild-to-moderate in nature
and included insomnia, headache and decreased appetite. Insomnia and decreased
appetite generally occurred upon initiation of treatment and often resolved with
continued treatment. Data from these three trials were submitted to the FDA for
evaluation as part of the sNDA.
LOAD-DATE: November 4, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
459 of 998 DOCUMENTS
PR Newswire US
October 21, 2005 Friday 11:30 AM GMT
Cephalon Receives Approvable Letter for SPARLON(TM) for the Treatment of ADHD in
Children and Adolescents;
SPARLON Pivotal Data Presented at Major Child and Adolescent Psychiatry Meeting
LENGTH: 1006 words
DATELINE: FRAZER, Pa. Oct. 21
FRAZER, Pa., Oct. 21 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
today announced that it has received an approvable letter from the U.S. Food and
Drug Administration (FDA) to market SPARLON(TM) (modafinil) Tablets [C-IV] for
the treatment of attention-deficit/hyperactivity disorder (ADHD) in children and
adolescents ages six through 17. The company submitted a supplemental new drug
application (sNDA) to FDA in December 2004.
"SPARLON is distinct from all currently available ADHD therapies," said Dr. Paul
Blake, Executive Vice President, Worldwide Medical and Regulatory Operations.
"We are excited to offer physicians and families a potential new option in the
treatment of ADHD and are working closely with the FDA to obtain final
approval."
Cephalon expects to launch SPARLON, a proprietary dosage form of modafinil, in
early 2006 subject to final FDA approval. In August 2005, Cephalon announced an
agreement with McNeil Consumer & Specialty Pharmaceuticals Division of
McNeil-PPC, Inc. to co-promote SPARLON.
Cephalon also presented for the first time results of integrated analyses of
efficacy and safety data from its three pivotal trials evaluating SPARLON
Tablets [C-IV] for the treatment of attention-deficit/hyperactivity disorder
(ADHD) in children and adolescents at a major medical meeting of child and
adolescent psychiatrists in Toronto. The three Phase 3 studies in which more
than 600 children and adolescents (ages six through 17) with ADHD were
randomized to treatment with SPARLON or placebo included two identically
designed nine-week, flexible-dosage studies and one seven-week, fixed-dosage
study. Patients treated with SPARLON experienced significant improvement
compared to placebo as early as the first week, with continued improvement
during titration and dose maintenance.
In the clinical trials, SPARLON was generally well tolerated and discontinuation
rates due to adverse events were not significantly different from placebo. The
most common adverse events associated with SPARLON were generally mild to
moderate in nature and included insomnia, headache and decreased appetite.
Insomnia and decreased appetite generally occurred upon initiation of treatment
and often resolved with continued treatment.
Data from these three trials were submitted to the FDA for evaluation as part of
the sNDA.
SPARLON
SPARLON is a new formulation and proprietary dosage strength of modafinil, the
active ingredient in PROVIGIL(R) (modafinil) Tablets [C-IV], which is approved
for the treatment of adults with excessive sleepiness associated with
narcolepsy, obstructive sleep apnea/hypopnea syndrome and shift work sleep
disorder. PROVIGIL is not approved to treat ADHD and is available only in 100 mg
and 200 mg strengths. If approved, SPARLON is expected to be available in early
2006.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 2,300 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, Pennsylvania,
and offices, laboratories or manufacturing facilities in West Chester,
Pennsylvania, Salt Lake City, Utah, and suburban Minneapolis, Minnesota.
Cephalon's European headquarters are located in Maisons-Alfort, France and other
European offices are located in Guildford, England, and Martinsried, Germany.
The company currently markets four proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling
1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, including the results of the SPARLON clinical trials,
prospects for final regulatory approval of SPARLON, including the anticipated
timetable for the launch of the product, manufacturing development and
capabilities, market prospects for its products, particularly with respect to
SPARLON sales and earnings guidance, and other statements regarding matters that
are not historical facts. You may identify some of these forward-looking
statements by the use of words in the statements such as "anticipate,"
"estimate," "expect," "project," "intend," "plan," "believe" or other words and
terms of similar meaning. Cephalon's performance and financial results could
differ materially from those reflected in these forward-looking statements due
to general financial, economic, regulatory and political conditions affecting
the biotechnology and pharmaceutical industries as well as more specific risks
and uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Jenifer Antonacci, +1-610-563-6018,
jantonac@cephalon.com , or Investors: Robert (Chip) Merritt, +1-610-738-6376,
cmerritt@cephalon.com , both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: December 7, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 PR Newswire Association LLC.
All Rights Reserved.
460 of 998 DOCUMENTS
Clinical Psychiatry News
October 2005
Data Back Broader Indication for Sodium Oxybate;
Trial results lead Xyrem maker to seek approval of drug for narcolepsy symptoms
beyond cataplexy.
BYLINE: Bruce Jancin, Denver Bureau
SECTION: Pg. 61 Vol. 33 No. 10 ISSN: 0270-6644
LENGTH: 781 words
DENVER - Sodium oxybate (Xyrem) is effective not only for cataplexy-its only
approved indication at present-but also for the other primary symptoms of
narcolepsy, investigators reported at the annual meeting of the Associated
Professional Sleep Societies.
Based on data from two randomized clinical trials presented at the meeting,
the drug's manufacturer, Orphan Medical Inc., has submitted a supplemental New
Drug Application to the Food and Drug Administration. If approval is granted,
sodium oxybate's expanded indication would make it the first drug approved for
treatment of all the primary symptoms of narcolepsy: excessive daytime
sleepiness; fragmented sleep; and cataplexy, the sudden, brief loss of muscle
tone frequently experienced by narcoleptics during periods of emotional
intensity such as surprise, laughter, or anger.
Terri E. Weaver, Ph.D., noted that in the last few years, quality of life
issues in patients with incurable chronic illnesses have drawn greater
regulatory and clinical attention. And the quality of life impact of narcolepsy,
she stressed, is profound: In one study, the impact was rated greater than
living with Parkinson's disease.
"Individuals with narcolepsy are struggling to complete their activities of
daily living," said Dr. Weaver of the University of Pennsylvania, Philadelphia.
She presented the first-ever study of sodium oxybate's quality of life impact in
narcoleptic patients. The double-blind, placebo-controlled, 8-week trial
involved 228 patients randomized to receive either placebo or 4.5 g, 6 g, or 9 g
of sodium oxybate per night in two equally divided doses at bedtime and from
21/2 to 4 hours later.
Quality of life was assessed with the Functional Outcomes of Sleep
Questionnaire administered at baseline, 4 weeks, and 8 weeks. Patients assigned
to 4.5 g/night showed no quality of life gains. But those who received 6 g or 9
g experienced significant improvement in four of the five domains measured by
this instrument: general productivity, vigilance, social outcome, and activity
level. The only domain in which they didn't fare significantly better than
placebo was the intimacy/sexual relationships subscale.
The benefit was greater with the 9-g dose. "The effect size was clinically
meaningful and quite large," she noted.
The potential for improved quality of life needs to be presented to patients
in the context of the possible treatment disadvantages so they can make an
informed decision. Patients on sodium oxybate experience a deep sleep and
increased arousal threshold. They may not hear a smoke alarm, a late-night
telephone call, or a child's cry. "Individuals who have children at home have to
weigh the benefit of having a good night's sleep and being able to function and
take care of those children during the day. We all know daytime sleepiness and
some of the other effects of narcolepsy can be hazardous, too, in terms of
caring for young ones," Dr. Weaver said.
Jed E. Black, M.D., presented another phase III trial, this one designed to
assess the relative efficacy of sodium oxybate when taken as monotherapy or with
modafinil (Provigil), a widely used wakefulness-promoting agent approved for
treatment of the excessive daytime sleepiness component of narcolepsy. The
double-blind, 230-patient trial began with all participants on 200-600 mg/day of
modafinil. They were then randomized to receive modafinil plus placebo,
modafinil plus sodium oxybate, placebo plus sodium oxybate, or double placebos.
The sodium oxybate dose was 6 g/night for the first 4 weeks and 9 g thereafter.
Monotherapy with sodium oxybate or modafinil appeared to be equally effective
in terms of the primary study end point, reduction in excessive daytime
sleepiness as measured by the Maintenance of Wakefulness Test, the Epworth
Sleepiness Scale, and patient self-report. The improvement was greater with the
9-g dose of sodium oxybate than with the 6-g dose. But combination therapy was
most effective of all, not only in terms of reduced daytime sleepiness but also
consolidation of fragmented sleep and enhanced slow-wave sleep, said Dr. Black
of Stanford (Calif.) University. Side effects that occurred more often with
sodium oxybate than placebo in the trials included nausea, dizziness, headache,
sleepiness, and bedwetting.
Prior to its 2002 approval as a tightly controlled schedule-III drug for
cataplexy, sodium oxybate was available as [#x3b3]-hydroxybutyrate in health
food stores. During that era it was abused as a recreational drug and implicated
as a "date rape" drug.
Both randomized trials were sponsored by Orphan Medical. Dr. Weaver serves as
a consultant to the company.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
461 of 998 DOCUMENTS
Family Practice News
October 1, 2005
No Withdrawal Syndrome Seen With Modafinil for ADHD
BYLINE: Damian Mcnamara, Miami Bureau
SECTION: Pg. 61 Vol. 35 No. 19 ISSN: 0300-7073
LENGTH: 386 words
BOCA RATON, FLA. - Children and adolescents with attention-deficit
hyperactivity disorder did not experience withdrawal or discontinuation syndrome
after abrupt cessation of modafinil film-coated tablets in a phase III,
double-blind, multicenter trial.
Researchers also found efficacy as early as 1 week in this 9-week study of 6-
to 17-year-olds with attention-deficit hyperactivity disorder (ADHD). The Food
and Drug Administration has approved modafinil (Provigil) for treatment of
narcolepsy and is currently reviewing a special pediatric formulation for ADHD.
"This is not surprising. Modafinil is a medication that improves vigilance
and alertness and could improve similar symptoms in ADHD," Joseph Biederman,
M.D., said in an interview at his poster presentation during a meeting of the
New Clinical Drug Evaluation Unit sponsored by the National Institute of Mental
Health.
Dr. Biederman and his associates compared efficacy using the school and home
versions of the ADHD Rating Scale-IV, the Clinical Global Impression of
Improvement (CGI-I) scores, and adverse event reporting by 125 patients taking
the pediatric formulation of modafinil and 64 taking a placebo.
The modafinil group had significantly improved school rating total scores,
compared with those of the placebo group at 1 week, an effect that was
maintained through week 7. The final 2 weeks of the study was a washout phase.
Mean reduction from baseline was 17 points with modafinil versus 8 points with
placebo. Significant reductions in home rating total scores also were observed
with modafinil at all visits, according to Dr. Biederman, chief of the joint
program in pediatric psychopharmacology, Massachusetts General Hospital, Boston.
A significantly greater percentage of modafinil patients was rated as "much"
or "very much" improved on the CGI-I (49%) than were placebo patients (25%).
Modafinil was abruptly discontinued in 37 patients. Abrupt cessation was not
associated with symptom rebound, and no evidence of withdrawal or
discontinuation syndrome was seen.
This and other phase III study results were submitted to the FDA in December
2004. "I don't see any reason why they wouldn't approve it," said Dr. Biederman,
who reported no affiliation with Cephalon Inc., the manufacturer and sponsor of
the study.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
462 of 998 DOCUMENTS
NIDA Notes
October 2005
Modafinil Improves Behavioral Therapy Results In Cocaine Addiction;
Research Findings
BYLINE: Patrick Zickler, NIDA NOTES Staff Writer
SECTION: NIDA NOTES - Vol. 20, No. 3
LENGTH: 722 words
NIDA-supported researchers evaluating modafinil's potential to enhance
behavioral treatment for cocaine addiction have reported a second successful
clinical efficacy trial. The new results affirm and extend the promising
findings of the earlier, smaller, and less stringent "open label" trial, and
they set the stage for large-scale multisite trials that could definitively
establish the medication's usefulness.
Dr. Charles Dackis and colleagues at the University of Pennsylvania Treatment
Research Center recruited 62 individuals (44 male, 18 female; mean age, 44.5
years) for their double-blind study. All had come to the Center seeking
treatment for cocaine addiction, had ingested at least $200 worth of cocaine in
the 30 days prior to presenting for treatment, and met the cocaine-dependence
criteria of the Diagnostic and Statistical Manual of Mental Disorders, 4th
Edition (DSM-IV). The patients agreed to visit the clinic twice a week for
individual sessions of cognitive-behavioral therapy (CBT) and provide urine
samples 3 times a week for the 8-week course of the study. Once each week, the
clinic staff dispensed a week's supply of pills, either modafinil in daily doses
of four 100 mg pills (30 patients) or an equal number of identical-looking
placebo pills (32 patients).
[Table Omitted]
Throughout the study, modafinil-treated patients gave fewer cocaine-positive
urine samples than the placebo group. "More impressive, though, is the fact that
more than twice as many modafinil patients as placebo patients (33 percent
compared with 13 percent) were able to attain abstinence for 3 weeks or more, "
Dr. Dackis says. "Maintaining abstinence for a prolonged period during treatment
is an important clinical threshold. Cocaine is a binge drug, and it is common in
outpatient treatment for a patient to go 4 or 5 days without using, relapse,
then have another clean week. The long continuous abstinence we saw with
modafinil is a strong and encouraging signal that this medication can help
patients avoid relapse during the critical first weeks of treatment." Both
groups of patients attended the same average number of CBT sessions, he adds,
further supporting the likelihood that modafinil was the factor accounting for
reduced cocaine abuse in those who received it.
Modafinil, a medication currently used to treat narcolepsy, enhances levels of
glutamate, a chemical that influences the activity of cells throughout the
brain. Animal research has shown that repeated exposure to cocaine depletes
glutamate levels in brain regions associated with development of dependence and
addiction, and that increasing glutamate concentrations will block reinstatement
of cocaine self-administration in rats--a model of relapse to drug abuse in
humans (see ", " NIDA NOTES , Vol. 19, No. 3).
Modafinil's modulation of glutamate transmission may account for a striking
effect reported by patients: "The mechanism for this isn't clear, but some
patients receiving modafinil told us that if they did use cocaine it did not
produce the irresistible urge to use more, which they had always felt before, "
Dr. Dackis says. "Some of the patients told me they had flushed cocaine away. In
25 years of treating addiction, no one ever told me they threw away cocaine."
"The body of research suggesting that modafinil is effective in treating cocaine
addiction is growing, " says Dr. Ivan Montoya of NIDA's Division of
Pharmacotherapies and Medical Consequences of Drug Abuse. "Animal research
supports the assumption that modafinil reverses the cocaine-induced
neurochemical disruptions of glutamate and of dopamine-containing neurons in the
brain's reward centers. Clinically, modafinil has effects that are opposite to
the symptoms of cocaine withdrawal, which usually include oversleeping,
depression, poor concentration, and craving."
Dr. Dackis and his colleagues are now planning the next test for modafinil: a
multisite clinical trial that will include more than 650 participants. The study
will evaluate modafinil's efficacy in doses of 200 mg and 400 mg per day in
combination with CBT, and results may be available by mid-2006, Dr. Montoya
says.
Source
* Dackis, C.A., et al. A double-blind, placebo-controlled trial of modafinil for
cocaine dependence. Neuropsychopharmacology 30(1): 205-211, 2005. []
Volume 20, Number 3 (October 2005)
LOAD-DATE: January 2, 2006
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Report
Copyright 2005 Federal Information and News Dispatch, Inc.
463 of 998 DOCUMENTS
World Markets Analysis
September 23, 2005
Cephalon's Modafinil Approved for New Indication in Germany
BYLINE: Mitra Thompson
SECTION: IN BRIEF
LENGTH: 229 words
U.S. pharmaceutical company Cephalon has seen its narcolepsy drug modafinil
approved for a new indication by the Federal Institute for Drugs and Devices in
Germany, where it will now be marketed for moderate-to-severe chronic shift-work
sleep disorder in patients with excessive sleepiness who work night shifts. The
company has not speculated on how much extra revenue it expects to earn via the
extended indication - modafinil has been sold as a regular narcolepsy treatment
in Germany since 1998 under the brand name Vigil - however, Germany is only the
third European country to approve modafinil for this particular sleep disorder.
Significance: Sales of modafinil, sold elsewhere as Provigil, leapt 51%
year-on-year during 2004, amounting to US$439.7 million, or 43% of total company
revenue. A new indication in Germany will be welcomed by Cephalon, despite the
relatively limited market size of the indication. Generic competition for
modafinil has been biting at Cephalon's heels over the past year, with Mylan,
Barr (both U.S.), and Dr Reddy's (India) securing preliminary approval for their
versions from the U.S. FDA, although Swiss generics firm Sandoz agreed in May to
postpone its plans for a generic copy of Provigil until a key Cephalon patent
expires in 2014 (see United States: 3 May 2005: Cephalon Relief as Sandoz Makes
Provigil U-Turn).
LOAD-DATE: September 23, 2005
LANGUAGE: ENGLISH
Copyright 2005 World Markets Research Limited;
All Rights Reserved
464 of 998 DOCUMENTS
Internal Medicine Alert
September 15, 2005
Pharmacology Watch
LENGTH: 1423 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 + 0.4 vs 0.3 +
0.3 minutes, respectively; P = 0.002). More patients also had improvement in
their clinical symptoms based on multiple objective tests and patients diaries
(74% vs 36%, respectively; P < 0.001). Patients taking modafinil also had
reduction in frequency and duration of lapses in attention during nighttime
testing of performance, and proportionally fewer patients reported having had
accidents or near accidents while commuting home (both P < 0.001). These
benefits, however, were mild, and patients treated with modafinil continued to
have excessive sleepiness and impaired performance at night. The authors
conclude that modafinil 200 mg at the beginning of a shift may improve
shift-worker's performance as compared to placebo, although the benefit is
modest (Czeisler CA, et al. Modafinil for Excessive Sleepiness Associated with
Shift-Work Disorder. N Engl J Med. 2005;353:476-486). An accompanying editorial
urges caution when interpreting these results and suggests "the current study
does not adequately assess the clinical value of this particular drug in
shift-work sleep disorder, nor does it justify writing more prescriptions for
modafinil." The authors do note that up to 20% of workers in industrialized
nations are shift-workers and calls for "further scientific studies to address
in a cohesive manner the serious health and safety issues that surround us by
virtue of us having become, to a large extent, a shift-working society" (Basner
RC. Shift-Work Sleep Disorder--The Glass is More Than Half Empty. N Engl J Med.
2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
465 of 998 DOCUMENTS
Clinical Cardiology Alert
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High-risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
466 of 998 DOCUMENTS
Clinical Oncology Alert
September 1, 2005
Pharmacology Watch
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
467 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
September 1, 2005
McNeil/Cephalon to co-promote modafinil for ADHD
LENGTH: 327 words
McNeil Consumer & Specialty Pharmaceuticals ( Johnson & Johnson ) has entered
into an agreement with Cephalon to co-promote the attention-deficit
hyperactivity disorder (ADHD) drug, modafinil . Under the terms agreed, McNeil
will promote modafinil upon approval in the US primarily to paediatric
specialists, whilst Cephalon will promote the product to psychiatrists,
neurologists, primary care physicians and other appropriate healthcare
professionals.
The co-promotion agreement will run for up to three years following the date of
commercial launch of modafinil. Cephalon will pay McNeil commission fees,
calculated as a percentage of annual net sales of modafinil during the term of
the agreement, retaining all responsibility for the development, manufacture,
distribution and sale of the product. The companies also plan to form a joint
commercial committee to manage the promotion of modafinil. The proprietary
dosage form of modafinil, named Attenace by Cephalon, is awaiting FDA approval
for the treatment of ADHD in children and adolescents. Cephalon submitted an
sNDA in December 2004 and anticipates a response on the PDUFA date of 20th
October 2005. Data from earlier trials in children and adolescents with ADHD led
to the development of modafinil as small, film-coated tablets in unique dosage
strengths. The new tablets will be available in 85, 170, 255, 340 and 425mg
strengths, and will allow for tailored dosing with a single tablet for children
and adolescents. The active ingredient in modafinil is currently available as
Provigil Tablets [C-IV] in 100 and 200mg strengths. Provigil is indicated for
the treatment of excessive sleepiness associated with narcolepsy, obstructive
sleep apnoea/hypopnoea syndrome and shift work sleep disorder. The most
frequently reported adverse events in clinical trials with Provigil were
headache, nausea, nervousness, stuffy nose, diarrhoea, back pain, anxiety,
trouble sleeping, dizziness and upset stomach.
LOAD-DATE: September 1, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
468 of 998 DOCUMENTS
Critical Care Alert
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
469 of 998 DOCUMENTS
Infectious Disease Alert
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
470 of 998 DOCUMENTS
Neurology Alert
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High-risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
471 of 998 DOCUMENTS
OB/GYN Clinical Alert
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ~ 0.4 vs 0.3 ~ 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
472 of 998 DOCUMENTS
Pharma Marketletter
September 1, 2005
McNeil to co-promote modafinil for ADHD with Cephalon
LENGTH: 159 words
McNeil Consumer & Specialty Pharmaceuticals, a subsidiary of Johnson & Johnson,
has entered into an agreement with Cephalon to co-promote modafinil.
This proprietary dosage form of modafinil is awaiting US Food and Drug
Administration approval for the treatment of attention-deficit hyperactivity
disorder in children and adolescents. Cephalon submitted a supplemental New Drug
Application for the compound to the FDA in December 2004 and anticipates a
response on October 20.
Upon approval in the USA, more than 300 McNeil sales representatives who
currently sell the ADHD product Concerta (methylphenidate HCl) C-II
extended-release tablets will promote modafinil, primarily to pediatric
specialists. Cephalon will use its existing central nervous system specialty
sales force of approximately 400 detailmen to promote modafinil to
psychiatrists, neurologists, primary care physicians and other appropriate
health care professionals.
LOAD-DATE: September 1, 2005
LANGUAGE: ENGLISH
Copyright 2005 Marketletter Publications Ltd.
473 of 998 DOCUMENTS
Primary Care Reports
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1422 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High-risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 + 0.4 vs 0.3 +
0.3 minutes, respectively; P = 0.002). More patients also had improvement in
their clinical symptoms based on multiple objective tests and patients diaries
(74% vs 36%, respectively; P < 0.001). Patients taking modafinil also had
reduction in frequency and duration of lapses in attention during nighttime
testing of performance, and proportionally fewer patients reported having had
accidents or near accidents while commuting home (both P < 0.001). These
benefits, however, were mild, and patients treated with modafinil continued to
have excessive sleepiness and impaired performance at night. The authors
conclude that modafinil 200 mg at the beginning of a shift may improve
shift-worker's performance as compared to placebo, although the benefit is
modest (Czeisler CA, et al. Modafinil for Excessive Sleepiness Associated with
Shift-Work Disorder. N Engl J Med. 2005;353:476-486). An accompanying editorial
urges caution when interpreting these results and suggests "the current study
does not adequately assess the clinical value of this particular drug in
shift-work sleep disorder, nor does it justify writing more prescriptions for
modafinil." The authors do note that up to 20% of workers in industrialized
nations are shift-workers and calls for "further scientific studies to address
in a cohesive manner the serious health and safety issues that surround us by
virtue of us having become, to a large extent, a shift-working society" (Basner
RC. Shift-Work Sleep Disorder--The Glass is More Than Half Empty. N Engl J Med.
2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
474 of 998 DOCUMENTS
Travel Medicine Advisor
September 1, 2005
Pharmacology Watch: Beta-Blockers May Be Useful for Noncardiac Surgery
LENGTH: 1420 words
Beta-Blockers May Be Useful for Noncardiac Surgery
Pharmacology Watch
High risk patients benefit from perioperative beta-blockers when undergoing
major noncardiac surgery according to new study. Researchers from Tufts
University reviewed the records of 782,969 patients in 2000 and 2001 at 329
hospitals throughout the United States. Patients were graded with the Revised
Cardiac Risk Index (RCRI), which takes into account high-risk surgery, ischemic
heart disease, cerebrovascular disease, renal insufficiency, and diabetes. The
RCRI is graded on a 0-5 point scale, with 5 representing the highest risk. High
risk surgery included all intrathoracic, intraperitoneal, and superinguinal
vascular procedures. Patients with contraindications to beta blocker therapy
were excluded. Over 660,000 patients had no contraindications to beta-blockers,
and 120,338 patients received beta-blocker treatment during the first 2 hospital
days. The relationship between perioperative beta-blocker treatment and the
risk of death varied directly with cardiac risk. Patients with an RCRI of 0 or
1 were found to have no benefit from beta-blocker treatment, whereas for
patients with an RCRI of 2, 3, or 4, or more the adjusted odds ratio for death
in the hospital, were 0.88 (95% CI, 0.80, 0.80-0.98), 0.71 (95% CI, 0.63 - 0.80)
and 0.58 (95% CI, 0.50-0.67), respectively. The authors conclude that
perioperative beta-blocker therapy is associated with a reduced risk of
in-hospital death among high-risk patients undergoing major noncardiac surgery.
They also noted that there was no benefit for low risk patients (Lindenauer PK,
et al. Perioperative Beta-Blocker Therapy and Mortality After Major Noncardiac
Surgery. N Engl J Med. 2005;353:349-361). An accompanying editorial points out
that perioperative beta-blocker therapy has been somewhat controversial because
of conflicting data in recent years. The current study shows an apparent
benefit in high-risk patients, but they also look forward to the results of 2
ongoing randomized trials that will help clarify the role of beta-blockers for
low-risk and intermediate-risk patients (Poldermans D, et al. Beta-Blocker
Therapy in Noncardiac Surgery. N Engl J Med. 2005;353:412-414).
Promising New Weight Loss Drug?
More data shows that topiramate (Topamax) is associated with weight loss and, in
this latest study, may also lower blood pressure in obese, hypertensive
patients. In a study from Norway, 531 obese patients with hypertension were
randomized to placebo, topiramate 96 mg/day, or topiramate 192 mg/day. All
patients received the same diet, exercise, and behavioral modification advice.
Patients were followed for 28 weeks. Mean weight loss was 1.9% for placebo and
5.9% and 6.5% for the 96 mg and 192 mg doses, respectively (P < 0.001 for each
compared with placebo). Diastolic blood pressure was reduced 2.1, 5.5, and 6.3
mm Hg, respectively (P < 0.015 vs placebo). Systolic blood pressure was reduced
4.9, 8.6, and 9.7 mm Hg, respectively (P = NS). Paresthesia occurred in 33% of
the active treatment group. The authors conclude that topiramate produced
clinically relevant effects in reducing body weight and BP, with generally mild
to moderate adverse effects (Tonstad S, et al. Efficacy and Safety of Topiramate
in the Treatment of Obese Subjects with Essential Hypertension. Am J Cardiol.
2005;96:243-251).
Treating Shift-Work Disorder
Modafinil (Provigil) may be of some value for people with excessive sleepiness
associated with shift-work sleep disorder. Researchers from Harvard randomized
209 patients with shift-work sleep disorder to receive either 200 mg of
modafinil or placebo before the start of each shift. Modafinil resulted in
modest improvement in nighttime sleep latency (1.7 ± 0.4 vs 0.3 ± 0.3 minutes,
respectively; P = 0.002). More patients also had improvement in their clinical
symptoms based on multiple objective tests and patients diaries (74% vs 36%,
respectively; P < 0.001). Patients taking modafinil also had reduction in
frequency and duration of lapses in attention during nighttime testing of
performance, and proportionally fewer patients reported having had accidents or
near accidents while commuting home (both P < 0.001). These benefits, however,
were mild, and patients treated with modafinil continued to have excessive
sleepiness and impaired performance at night. The authors conclude that
modafinil 200 mg at the beginning of a shift may improve shift-worker's
performance as compared to placebo, although the benefit is modest (Czeisler CA,
et al. Modafinil for Excessive Sleepiness Associated with Shift-Work Disorder. N
Engl J Med. 2005;353:476-486). An accompanying editorial urges caution when
interpreting these results and suggests "the current study does not adequately
assess the clinical value of this particular drug in shift-work sleep disorder,
nor does it justify writing more prescriptions for modafinil." The authors do
note that up to 20% of workers in industrialized nations are shift-workers and
calls for "further scientific studies to address in a cohesive manner the
serious health and safety issues that surround us by virtue of us having become,
to a large extent, a shift-working society" (Basner RC. Shift-Work Sleep
Disorder--The Glass is More Than Half Empty. N Engl J Med. 2005;353:519-521).
Another Flu Vaccine Shortage?
With the flu season looming, Chiron Corp. is again having difficulty with flu
vaccine production. Last year the company found contamination at its Liverpool
production plant, a situation that cause severe shortages of vaccine in the
United States. This year, the company has discovered contamination at a German
plant and is stating that it can only provide vaccine for the US market. The
German plant was primarily the source of the Begrivac flu vaccine, which was
sold on the world market. The company is making "substantial progress" in
fixing problems at the Liverpool plant where the US vaccine is made. Meanwhile,
Acambis plc is working on a universal flu vaccine that could offer permanent
protection against all types of influenza. The company hopes to generate a
universal vaccine that would not require annual changes in formulation and would
protect against both influenza A and B including avian strains. The company,
however, states that it may require years of clinical trials before earning
approval. Fears of avian influenza pandemic have prompted the French company
Sanofi-Aventis to work on a vaccine for the avian H5N1 strain that has killed
millions of birds and 50 people in Asia. Preliminary results are promising,
however, full-scale production could take months, according to Anthony Fauci,
MD, Director of the National Institute of Allergy and Infectious Diseases.
FDA Actions
The FDA has approved the first of the new class of drugs for the treatment of
insomnia characterized by difficulty with sleep onset. Takeda Pharmaceutical's
ramelteon (Rozerem) is a selective agonist at 2 melatonin receptors in
suprachiasmatic nucleus, receptors that are thought to regulate circadian rhythm
and sleepiness. Recently marketed sleeping medications target GABA receptors
(ambien, lunesta) and, although these drugs are associated with less addiction
and sleep latency then benzodiazepines, they are still designated as Schedule IV
drugs. Ramelteon has shown no evidence of abuse or dependence potential and
will, therefore, be marketed as a unscheduled drug. It is also approved for
long-term use and has not been associated with memory impairment or impairment
of motor ability. The most common adverse events associated with ramelteon were
somnolence, fatigue and dizziness (> 2% over placebo).
Plan B, Barr Pharmaceutical's "morning-after pill" is being considered for
over-the-counter approval by the FDA. The issue has become a political hot
potato, and even briefly held up the Senate's confirmation of Lester Crawford,
MD, as Commissioner of the FDA. It is expected that decision will be made by
September.
This supplement was written by William T. Elliott, MD, FACP, Chair, Formulary
Committee, Kaiser Permanente, California Division; Assistant Clinical Professor
of Medicine, University of California-San Francisco. In order to reveal any
potential bias in this publication, we disclose that Dr. Elliott reports no
consultant, stockholder, speaker's bureau, research, or other financial
relationships with companies having ties to this field of study. Questions and
comments, call: (404) 262-5416. E-mail:
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 AHC Media LLC
All Rights Reserved
475 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
August 31, 2005
Cephalon receives approval to market modafinil for SWSD in Germany
LENGTH: 161 words
Cephalon has received authorisation from the Federal Institute for Drugs and
Devices (BfArM) to market modafinil tablets in Germany for the treatment of
moderate-to-severe chronic shift work sleep disorder (SWSD) with excessive
sleepiness in patients working night shifts, if measures of sleep hygiene have
not led to a satisfactory improvement. Marketed under the tradename Vigil ,
modafinil has been available in Germany since 1998.
Modafinil is the first and only medication in a new class of wake-promoting
agents believed to work selectively through the sleep/wake centres to activate
the cortex of the brain. The medication is currently approved in more than 20
countries and available under several brandnames, including Provigil , Alertec ,
Modiodal , Modasomil and Modavigil . In 2004, the FDA approved Provigil C-IV
Tablets for improving wakefulness in patients with excessive sleepiness
associated with obstructive sleep apnoea/hypopnoea syndrome and SWSD.
LOAD-DATE: August 31, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
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476 of 998 DOCUMENTS
Midnight Trader
This content is provided to LexisNexis by Comtex News
Network, Inc.
August 30, 2005 Tuesday
Cephalon Gets German OK to Market Modafinil for Sleep Disorder
LENGTH: 199 words
DATELINE: Boston
Cephalon (CEPH) said tonight that it has received authorization from the Federal
Institute for Drugs and Devices to market modafinil tablets in Germany for the
treatment of moderate to severe chronic shift work sleep disorder with excessive
sleepiness in patients working night shifts, if measures of sleep hygiene have
not led to a satisfactory improvement.
Marketed under the trade name VIGIL, modafinil has been available in Germany
since 1998.
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477 of 998 DOCUMENTS
PR Newswire US
August 30, 2005 Tuesday 8:30 PM GMT
Cephalon Receives Approval to Market Modafinil for Shift Work Sleep Disorder in
Germany
LENGTH: 848 words
DATELINE: FRAZER, Pa. Aug. 30
FRAZER, Pa., Aug. 30 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
announced today that the company has received authorization from the Federal
Institute for Drugs and Devices (BfArM) to market modafinil tablets in Germany
for the treatment of moderate to severe chronic shift work sleep disorder with
excessive sleepiness in patients working night shifts, if measures of sleep
hygiene have not led to a satisfactory improvement. Marketed under the trade
name VIGIL(R), modafinil has been available in Germany since 1998.
"Germany is the third European country to approve modafinil for the treatment of
shift work sleep disorder and to recognize the need to treat it. This new
indication capitalizes on the strong clinical data surrounding this medication
and allows us to improve the quality of life of the people suffering from this
debilitating disorder," said Alain Aragues, President, Cephalon Europe.
Modafinil
Modafinil is the first and only medication in a new class of wake- promoting
agents believed to work selectively through the sleep/wake centers to activate
the cortex of the brain. The medication is currently approved in more than 20
countries and available under several brand names (PROVIGIL(R), ALERTEC(R),
MODIODAL(R), MODASOMIL(R), MODAVIGIL(R) VIGIL). In 2004, the United States Food
and Drug Administration approved PROVIGIL(R) (modafinil) [C-IV] Tablets for
improving wakefulness in patients with excessive sleepiness associated with
obstructive sleep apnea/hypopnea syndrome and shift work sleep disorder (SWSD).
PROVIGIL was originally approved in 1998 for improving wakefulness in patients
with excessive sleepiness associated with narcolepsy.
About Cephalon
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon currently
employs approximately 2,300 people in the United States and Europe. U.S. sites
include the company's headquarters in Frazer, Pennsylvania, and offices,
laboratories or manufacturing facilities in Salt Lake City, Utah, and suburban
Minneapolis, Minnesota.
The company currently markets four proprietary products in the United States:
PROVIGIL(R), GABITRIL(R) (tiagabine hydrochloride), ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and TRISENOX(R) (arsenic trioxide) injection and more
than 20 products internationally. Full prescribing information for all U.S.
products is available at http://www.cephalon.com/ or by calling 1-800-896-5855
(PROVIGIL, GABITRIL, and ACTIQ) or 1-800-715-0944 (TRISENOX).
Cephalon Europe
Cephalon Europe has headquarters in Maisons-Alfort France and offices in the
United Kingdom, Germany and Switzerland employing more than 600 people. European
operations market more than 20 pharmaceutical products such as ACTIQ(R) for
cancer pain; GABITRIL(R) for seizures associated with epilepsy; modafinil under
the brand names PROVIGIL(R), MODIODAL(R) and VIGIL(R) for excessive sleepiness
associated with multiple disorders; and SPASFON(R), an antispasmodic.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
guidance, and other statements regarding matters that are not historical facts.
You may identify some of these forward-looking statements by the use of words in
the statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com ,
or Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com ,
both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: August 31, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 PR Newswire Association LLC.
All Rights Reserved.
478 of 998 DOCUMENTS
Hamilton Spectator (Ontario, Canada)
August 23, 2005 Tuesday Final Edition
It's often tough to pick up zzzzzzzs after a night's work
SOURCE: The Hamilton Spectator
SECTION: WELL-BEING; Pg. G06
LENGTH: 237 words
When people work all night and try to sleep during the day, some adjust but
others never do.
They're chronically sleepy on the job and experience daytime insomnia, a
condition known as shift work sleep disorder.
A study assigned 204 adults who worked night shifts and had been diagnosed with
shift work sleep disorder to take modafinil (Provigil) or a placebo 30 to 60
minutes before starting work each night.
After three months, 74 per cent of the modafinil group reported at least minimal
improvements, compared with 36 per cent of the placebo group.
They also had fewer attention lapses during their normal working hours, whereas
the placebo group experienced more, and they reported having fewer accidents or
near-accidents while commuting home than the others.
However, the modafinil group continued to be excessively sleepy and exhibited
nighttime performance weaknesses. Neither the drug nor the placebo worsened
daytime insomnia.
Caveats: Long-term safety and effectiveness of the drug were not tested.
The study was funded by Cephalon, which makes Provigil. Four of the 10 primary
authors work for the pharmaceutical company; the others have received
consultants' fees from it.
Find the study in the New England Journal of Medicine; abstract available online
at www.nejm.org.
Learn more about shift work and sleep problems at
www.sleepfoundation.org/sleeptionary and www.mayoclinic.com.
LOAD-DATE: August 23, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo:
TYPE: News
Copyright 2005 Metroland Media Group Ltd
479 of 998 DOCUMENTS
The Houston Chronicle
August 14, 2005, Sunday 2 STAR EDITION
Drug helping night workers stay alert, researchers find;
Study indicates medication for shift-work sleep disorder is the first in its
field
SOURCE: Newsday
BYLINE: DELTHIA RICKS
SECTION: A; Pg. 15
LENGTH: 474 words
In the first study of medicating people who work graveyard shifts, researchers
have found that an alertness drug can spur wakefulness and prevent accidents on
the drive home.
The drug, modafinil, sold as Provigil, originally was approved to treat the
uncontrollable sleepiness of narcolepsy. The study, reported in the New England
Journal of Medicine by Boston researchers, marks the first time that it has been
tested in people who must remain awake all night.
"One out of 10 people have difficulty adapting to night-shift work," said Dr.
Charles Czeisler, chief of Brigham and Women's Sleep Medicine division.
He said not just anyone who yawns on an overnight shift meets criteria for
shift-work sleep disorder, which he defines as most prevalent among people who
can't stay awake past midnight.
Czeisler said those with the condition are more likely to doze incessantly on
the job but remain awake during the day. They also are more likely to be
depressed, have cardiovascular problems and ulcers. Czeisler also defines the
group as being more prone to "accidents and near-accidents" in their commute
home.
"We live in a society in which a number of critical services are offered at
night," Czeisler said, "so it is important for some people to be awake. This
isn't exactly new to the modern world; even shepherds had to guard their flocks
because of nocturnal predators."
In the study of 209 patients, 74 percent of roughly half who got modafinil were
less likely to be sleepy at work, compared with 36 percent of those who got a
dummy pill.
Manufactured by Cephalon Inc., modafinil was approved by the Food and Drug
Administration in 1998. Cephalon also sponsored the study, which was conducted
at 28 medical centers throughout the United States.
Czeisler acknowledged that no one knows how the drug induces wakefulness, though
he adds that the medication is safe.
The drug is being studied by the Department of Defense to maintain alertness in
pilots and troops in Iraq.
Dr. Robert Basner, a sleep expert at Columbia University's College of Physicians
and Surgeons in Manhattan, said the study is not definitive.
"This is very contentious, and a lot is at stake here," he said. "I am not
taking out my pad to write more prescriptions for modafinil based on this
study."
Basner said while shift-work sleep disorder is a genuine medical condition,
doctors should not assume Czeisler's study has proven that the drug is safe for
patients with the condition.
"They've taken this one drug and given it to shift workers to determine if it
would make them less sleepy - and it did, compared to nothing, which was the
placebo. There are other stimulants that can be studied in a similar protocol."
He suggested caffeine probably would produce similar results if studied the same
way.
LOAD-DATE: August 14, 2005
LANGUAGE: ENGLISH
Copyright 2005 The Houston Chronicle Publishing Company
480 of 998 DOCUMENTS
Sunday Age (Melbourne, Australia)
August 7, 2005 Sunday
First Edition
The science of never celling yourself short
BYLINE: MARK RUSSELL
SECTION: EXTRA; Pg. 17
LENGTH: 800 words
Whether it's listening to Mozart or popping Modafinil, there are ways to retrain
your brain and enjoy greater wellbeing, writes Mark Russell.
EATING beans on toast for breakfast, an omelet and salad for lunch with a
yoghurt dessert, and fish for dinner followed by strawberries and blueberries,
is a good way to boost brain power, according to the New Scientist's list of 11
Steps to a Better Brain.
The list suggests that a high-protein diet helps to stimulate and improve the
brain, as does listening to Mozart, taking smart drugs, getting a decent night's
sleep, walking for half an hour three times a week, doing the crossword,
knitting, paying attention, memorising such things as a series of dots on a
grid, and using the power of thought to boost creativity and alter personality
traits.
Leading Australian brain experts believe this new list of ways to improve the
brain is an example of the public's increasing fascination with the science of
wellbeing.
The 11 Steps to a Better Brain involves the use of smart drugs (including
Modafinil, which keeps the brain alert for up to 90 hours); music (Mozart makes
listeners feel better); bionics (electrodes to send small currents to the
brain); mental workouts (such as mathematics tests); memory tricks; hobbies;
sleep; physical exercise; food; concentration; and neurofeedback (thought
control).
Dr Evian Gordon, founding director of the Brain Dynamics Centre at Sydney's
Westmead Hospital and chief executive of the Brain Resource Company, said it was
remarkable how many people wanted to know more about what he terms positive
psychology to increase brain power.
"Theoretically if you do activate your brain neurones in a very targeted way to,
say, improve your memory, there's no reason that your memory shouldn't improve
to some extent," Dr Gordon told The Sunday Age.
"It's a very interesting area, this notion of retraining the brain.
"When people actually see evidence that they can genuinely improve their own
brain function, it has a very significant impact on them.
"We all know we should do exercise and eat better, but when you actually see it
having an effect (on the brain), it's like lowering your own heart rate. It
really is a concrete way in which people can see they are more masters of their
own destinies than they imagined."
But while applauding efforts to improve the brain, Dr Gordon cautioned against
the use of
so-called smart drugs. He said the brain was a highly interconnected system
which was susceptible to side-effects when using smart drugs.
New Scientist claims research shows the drug Modafinil helps to keep people
awake without the side-effects that amphetamines or coffee produce while Ritalin
helps to improve concentration during exams or important negotiations.
Dr Gordon said: "There's that broad kind of concern in tinkering with the brain
. . . that we're tinkering with a system that we don't fully understand.
"The issue to me is how much is the variance explained. In other words, if I'm
going to take a drug to improve my memory, how much of a benefit is there and
how enduring is that benefit?
"It's all very well to say this is a drug that shows improvement (to the brain),
but is there a better way to do it, is there a less invasive way to do it?"
11 STEPS TO A BETTER BRAIN
- Food for thought: you are what you eat.
- Gainful employment: put your mind to work in the right way and it could bring
an impressive bonus.
- Body and mind: physical exercise can boost brain as well as brawn.
- Memory marvels: mind like a sieve? Don't worry. The difference between mere
mortals and memory champs is more method than mental capacity.
- Bionic brains: if training and tricks seem too much like hard work, some
technological short cuts can boost brain function.
- Attention-seeking: you can be smart, well-read, creative and knowledgeable,
but none of it is any use if your mind isn't on the job.
- Positive feedback: Thought control is easier than you might imagine.
- The Mozart effect: Mozart has been shown to improve mathematical and spatial
reasoning but the impact of music lessons is even more impressive. The IQ scores
of six-year-old music students were 2 to 3 points higher than their peers.
- Sleep on it: never underestimate the power of a good night's rest.
- Smart drugs: 'cognitive enhancement' drugs are already on the market.
- Nuns on a run: a study of the School Sisters of Notre Dame in Minnesota found
many of its 75- to 107-year-old inhabitants have avoided any kind of dementia or
senility. Their secrets included: the right amount of vitamin folate; verbal
ability early in life; positive emotions early in life; activities, crosswords,
knitting and exercising.
Source: New Scientist magazine, May 28, 2005, Kate Douglas, Alison George, Bob
Holmes, Graham Lawton, John McCrone, Alison Motluk, Helen Phillips.
LOAD-DATE: July 19, 2007
LANGUAGE: ENGLISH
GRAPHIC: EIGHT PHOTOS
PUBLICATION-TYPE: Newspaper
Copyright 2005 The Age Company Limited
All Rights Reserved
481 of 998 DOCUMENTS
The Pharmaceutical Journal
August 5, 2005
Modafinil for sleep disorder
BYLINE: Old_manager
LENGTH: 59 words
Modafinil is of some value in treating shift-work sleep disorder but does not
restore sleepiness to normal levels (New England Journal of Medicine
2005;353:476). In 209 patients modafinil 200mg taken before a night shift
improved symptoms of sleepiness as well as objective measures of sleep
propensity and performance compared with placebo.
LOAD-DATE: November 10, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Journal
Copyright 2005 PJ Online
All Rights Reserved
482 of 998 DOCUMENTS
UPI
August 5, 2005 Friday 1:33 PM EST
Drug may help night-shift workers
BYLINE: EVA A. SYLWESTER
LENGTH: 1145 words
DATELINE: WASHINGTON, Aug. 5
Working at night and sleeping during the day is not natural for any human body,
but some people have trouble adapting to such arrangements to the point where
their distress qualifies as a medical disorder. Now, this underdiagnosed and
difficult-to-treat condition is the subject of the first-ever clinical trial of
the promising medication modafinil.
Shift-work sleep disorder is marked by sleepiness during night-time working
hours, insomnia while trying to sleep during the day and instances of
fatigue-induced accidents and errors on the job in people whose work shifts
include more than six hours between 10 p.m. and 8 a.m. Effects include higher
rates of accidents, absenteeism, depression, ulcers and frequently missing
family and social activities.
Charles Czeisler, lead author of the study -- which appears in the Aug. 4 issue
of the New England Journal of Medicine -- told United Press International the
condition affects 5 percent to 10 percent of night-shift workers. It also is
often underdiagnosed because it is mistaken for ordinary fatigue.
Czeisler compared the difference between normal tiredness and the disorder to
the scene at tourist destinations, where some travelers walk around examining
landmarks and others slump on benches due to the effects of jet lag.
"Some people are more affected than others," he said.
David Dinges, chief of the Division of Sleep and Chronobiology at the University
of Pennsylvania in Philadelphia and a co-author of the paper, told UPI he has
been conducting another study. This one, sponsored by the National Institutes of
Health, is examining healthy people not on shift-work schedules who have spent
non-consecutive nights without sleep.
He said he found that participants who have experienced great difficulty during
their first night without sleep also had difficulty on subsequent nights without
sleep -- regardless of how much they slept in the interim. At the same time,
participants who remained relatively functional after their first sleepless
night retained that ability on other nights when they stayed up.
"This is a trait-like characteristic of people," Dinges said.
Czeisler, who is chief of sleep medicine at Brigham and Women's Hospital in
Boston and a professor of medicine at Harvard Medical School, said that in
addition to revealing a possible treatment, another notable aspect of the study
was its findings on the effects of shift-work sleep disorder.
"It revealed how sleepy this group of patients is," Czeisler said. "They're just
as sleepy as patients with narcolepsy or sleep apnea."
In the study, researchers assigned 209 shift-work sleep-disorder patients to
receive 200 milligrams of either modafinil or a placebo before the start of each
work shift. Modafinil is sold under the trade name Provigil and is manufactured
by Cephalon Inc., which provided research funds to Czeisler. The drug also is
used for narcolepsy and sleep apnea.
The study measured sleep latency and lapses of attention. Sleep latency is the
amount of time it takes a person to fall asleep given the opportunity.
Czeisler said that in the daytime, falling asleep in less than five minutes
signifies excessive sleepiness. No standards have been developed for healthy
sleep latency at night, so the sleep-latency figures collected in his study
simply served as a measure of change. The average decrease in sleep latency for
patients receiving modafinil was 1.7 minutes, compared to 0.3 minutes for the
placebo group. The difference in sleep latency was most pronounced early in the
night, around 2 a.m., and decreased toward 6 a.m.
The Psychomotor Vigilance Test was used to monitor lapses of attention. Patients
in the modafinil group experienced a median rate of 2.63 fewer lapses of
attention per 20-minute test, while patients in the placebo group experienced
3.75 more lapses of attention than they had before receiving the placebo.
Patients in Czeisler's study worked a wide variety of occupations, including
manufacturing, investment banking, police work and hospital nursing.
"Something that was common to all of them was actual or near-miss motor-vehicle
accidents driving home from work," Czeisler said.
Among the study's placebo group, 54 percent reported accidents or near accidents
during their commute home, while only 29 percent of patients receiving modafinil
reported such incidents.
Czeisler acknowledged that although modafinil is helpful, it does not enable
perfect functioning.
"It brings (patients) about a third of the way to what's normal during the
daytime, but we don't know what's normal during the night," he said. Also,
patients in the modafinil group experienced daytime insomnia at a 6-percent
higher rate than the placebo group.
Czeisler said the brain sends out a strong drive for sleep at night, and that it
is contrary to the body's circadian rhythms to work at night and sleep in the
daytime, but modern life sometimes demands the suppression of biological
directives.
"There are many essential services provided by people who do work at night, and
we live in a society that requires many round-the-clock operations," Czeisler
said.
Dinges said that with the number of U.S. shift workers at 6 million and growing,
it would be economically unfeasible to bar even people with innate difficulties
from night-shift work, even though numerous government and scientific studies
point to dangerous consequences from such activities, such as industrial
accidents and highway collisions.
"I don't know how realistic it is to suggest that people who are vulnerable
shouldn't work night shift," he said.
Other doctors suggest that more possibilities may be found for managing the
disorder.
Robert Basner, associate professor of clinical medicine at Columbia University,
wrote in the NEJM article that other researchers' findings show 600 mg doses of
caffeine can produce similar effects to modafinil in improved performance for
people who have been awake more than 40 hours, and according to Czeisler's
study, modafinil does not affect the underlying circadian rhythm.
"Neither these data nor any other published studies provide evidence to indicate
that modafinil is uniquely suited to be used as an enhancer of wakefulness and
vigilance in humans subjected to nighttime shift work," Basner wrote.
Czeisler said he did not test -- nor would he personally advocate -- the drug's
potential to keep people awake for indefinite periods of time, such as all-night
studying.
Dinges said caffeine and bright lights have been used to treat shift-work sleep
disorder for years, but they have not been tried in many experiments.
"In the experiments where they have been tried, they have limited utility," he
said. He agreed that more research needs to be done on the disorder and in
establishing standards for normal levels of nighttime alertness.
Eva Sylwester is an intern for UPI Science News. E-mail: sciencemail@upi.com
LOAD-DATE: August 6, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 U.P.I.
All Rights Reserved
483 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
August 4, 2005
Modafinil demonstrates reduced excessive sleepiness in SWSD patients
LENGTH: 401 words
The results of Cephalon 's pivotal Phase III study of Provigil ( modafinil ) in
patients with shift-work sleep disorder (SWSD) have been published in the 4th
August issue of the NEJM (2005;353:476-486). In the first ever clinical study of
SWSD, patients taking modafinil showed improvements in their wakefulness,
performance and level of attention. Cephalon has also completed a larger Phase
III study in SWSD with its second wake-promoting agent, Nuvigil ( armodafinil ),
which is currently being reviewed as part of a request for marketing approval by
the FDA. The three-month, randomised, double-blind, placebo-controlled study was
conducted at 28 centres in the US between December 2001 and September 2002. All
204 patients treated in the study were prescreened for SWSD and received
modafinil 200mg or placebo. Key results of the study showed that: modafinil
significantly improved patients' level of alertness when measured objectively,
as compared to patients treated with placebo; modafinil significantly reduced
patients' level of sleepiness when measured subjectively, as compared to
patients treated with placebo; patients treated with modafinil had a significant
reduction in the number and duration of lapses of attention during 20-minute
computerised tests conducted in a sleep laboratory, as compared to patients
treated with placebo; and a higher percentage of patients treated with modafinil
(74 per cent) were rated as improved using the physician-rated Clinical Global
Impression of Change scale, as compared to patients treated with placebo (36 per
cent). The study concluded that treatment with modafinil 200mg reduced the
extreme sleepiness that is observed in patients with SWSD and resulted in a
small but significant improvement in performance as compared with placebo.
However, according to the study authors, the residual sleepiness that was
observed in the treated patients underscores the need for the development of
interventions that are even more effective. In January 2004, the FDA approved
Provigil as the first and only medication to treat excessive sleepiness
associated with SWSD. The medication is believed to work selectively through the
sleep-wake centres to activate the cortex of the brain. The exact mechanism of
action of Provigil is not known, however, it promotes wakefulness without
causing the generalised stimulation of the brain associated with CNS stimulants.
LOAD-DATE: August 4, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
484 of 998 DOCUMENTS
The Vancouver Province (British Columbia)
August 4, 2005 Thursday
Final Edition
Pill helps night-shift workers stay awake, research shows: Increases vigilance,
wakefulness: study
BYLINE: Scripps Howard
SECTION: NEWS; Pg. A26
LENGTH: 302 words
In a 24-7 world, tens of thousands of North Americans fall victim to shift-work
sleep disorder -- they're sleepy during their night of work, but suffer from
insomnia when they try to sleep in the daytime.
A study published today shows that a drug first prescribed for narcolepsy
sufferers also offers some relief to night-shift workers.
The drug, called modafinil and sold under the brand name Provigil, extended the
length of time it took shift workers between the ages of 18 and 60 to nod off at
night from an average of about two minutes to nearly four minutes. It improved
the workers' self-reported wakefulness and vigilance in tests.
Researchers say nearly 6.5 million North Americans work at night on a permanent
or rotating basis, and some five per cent to 10 per cent suffer from the
shift-work disorder.
"Shift-work sleep disorder . . . can compromise personal safety and
significantly impact quality of life," said Dr. Charles Czeisler, chief of the
sleep-medicine division at Brigham and Women's Hospital in Boston and leader of
the study presented in The New England Journal of Medicine.
"This study demonstrates that while modafinil can significantly improve symptoms
and reduce sleep tendency during night-work hours, patients remain excessively
sleepy even after treatment for this sleep-wake disturbance," Czeisler said.
Originally intended to treat narcoleptics -- people with a rare brain disorder
that causes them to uncontrollably fall asleep -- the drug is now approved in
the U.S. for people with shift-work disorder as well as those suffering from
sleep apnea.
The drug's manufacturer, Cephalon, sponsored the new research and Czeisler is a
paid consultant to the firm.
The pills generally keep people awake with less of the jitteriness and other
side-effects seen from using caffeine or amphetamines.
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Internal Medicine News
August 1, 2005
Antinarcolepsy Drug May Improve ADHD
BYLINE: Mary Ellen Schneider, Senior Writer
SECTION: Pg. 46 Vol. 38 No. 15 ISSN: 1097-8690
LENGTH: 857 words
ATLANTA - Results from two new studies highlight a possible alternative to
stimulants for the treatment of attention-deficit hyperactivity disorder in
children and adolescents.
Two phase III studies presented at the annual meeting of the American
Psychiatric Association show that a once-daily pediatric formulation of
modafinil is well tolerated and improves attention-deficit hyperactivity
disorder (ADHD) symptoms in children and adolescents.
Modafinil is currently marketed by Cephalon under the brand name Provigil in
100-mg and 200-mg strengths. Provigil is indicated for the treatment of
excessive sleepiness associated with narcolepsy, obstructive sleep apnea,
hypopnea syndrome, and shift work sleep disorder.
The company, which funded the phase II trials, is seeking approval from the
Food and Drug Administration to market modafinil in 85-mg, 170-mg, 255-mg,
340-mg, and 425-mg strengths. If approved, the drug would be indicated for
treatment of ADHD in children and adolescents aged 6-17 years.
The company is planning to launch the drug under the brand name Attenace by
early 2006.
In one study, 189 patients with ADHD aged 6-17 years were randomized to a
7-week double-blind, fixed-dose treatment with either modafinil or placebo. This
regimen was followed by a 2-week withdrawal period in which half of the
modafinil-treated patients were placed on placebo without tapering, and half
were continued on the drug, said Joseph Biederman, M.D., the lead investigator
in the study and professor of psychiatry at Harvard University in Boston.
Modafinil was administered once daily, starting at 85 mg/day, and was rapidly
titrated over 7-9 days to dosages of either 340 mg/day for patients who weighed
less than 30 kg or 425 mg/day for patients who weighed 30 kg or more.
The results of the study were assessed using the school and home ADHD Rating
Scale-IV total score change from baseline to last treatment visit.
After 1 week, the 125 modafinil-treated patients had significantly greater
improvements in school scores, compared with the 64 placebo patients, and those
results were maintained through week 7.
On the school scale, patients on modafinil experienced a 17.2-point drop in
symptoms, compared with an 8.2-point drop for patients on placebo. Modafinil
also significantly improved total scores from parents, compared with placebo.
The side effects included insomnia and appetite decrease. Overall, the side
effects were generally mild and occurred at initiation of the treatment. There
were two serious adverse events not associated with the trial, said Dr.
Biederman, who is an advisory board member for Cephalon and receives
research/grant support from the company.
The researchers also assessed ADHD symptoms and physical/emotional response
after rapid discontinuation. During the 2-week withdrawal phase, there were no
reported symptom rebounds, no adverse events related to withdrawal, and no
physical or emotional responses.
Modafinil appears to work like a gentler stimulant, Dr. Biederman said in an
interview. The findings present possible new treatment options, he said.
Although stimulants are effective, they are not universally effective. About
30%-40% of patients are nonresponsive to stimulants, he said, and some patients
also have tolerability problems.
Stimulants also have the potential for acute deterioration and symptom
rebound if treatment is interrupted or discontinued without tapering, Dr.
Biederman said.
In the second study, researchers considered the effect of a flexible dose of
modafinil in children and adolescents.
The study included 198 patients aged 6-17 years who were started on a dose of
85 mg/day of modafinil, which was titrated over 22 days based on clinical
effectiveness. The maximum dose was 425 mg/day with once-daily dosing, said
James Swanson, Ph.D., of the University of California at Irvine Child
Development Center, who was the lead investigator.
The results were assessed using the school and home ADHD Rating Scale-IV, the
Clinical Global Impression of Improvement (CGI-I), and the Test of Variables of
Attention (TOVA).
The home score showed a mean drop of 17.6 points in symptoms for the 131
patients receiving modafinil at a mean stable dose of 361 mg/day, compared with
a 7.5-point drop in symptoms for the 67 patients on placebo. The improvement in
the total school score was also significantly greater for modafinil patients,
Dr. Swanson reported.
Modafinil was shown to significantly improve inattention and
hyperactivity/impulsivity, and there was an improvement in overall clinical
condition and in the TOVA measurements of ADHD.
The researchers focused not only on decreasing symptoms of ADHD, but on
increasing positive interaction and social skills, and they saw an increase in
positive behaviors, he said.
The side effects included insomnia, headache, and appetite problems, which
are similar to the side effects for stimulants, said Dr. Swanson, who is an
advisory board member with Cephalon, receives research/grant support from the
company, and is a member of the company's speakers' bureau.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: IMNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
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486 of 998 DOCUMENTS
Pediatric News
August 2005
Trial Finds No Withdrawal Syndrome With Modafinil
BYLINE: Damian Mcnamara, Miami Bureau
SECTION: Pg. 28 Vol. 39 No. 8 ISSN: 0031-398X
LENGTH: 388 words
BOCA RATON, FLA. - Children and adolescents with attention-deficit
hyperactivity disorder did not experience withdrawal or discontinuation syndrome
after abrupt cessation of modafinil film-coated tablets in a phase III,
double-blind, multicenter trial.
Researchers also found efficacy as early as 1 week in this 9-week study of 6-
to 17-year-olds with attention-deficit hyperactivity disorder (ADHD). The Food
and Drug Administration has approved modafinil (Provigil) for treatment of
narcolepsy and is currently reviewing a special pediatric formulation for ADHD.
"This is not surprising. Modafinil is a medication that improves vigilance
and alertness and could improve similar symptoms in ADHD," Joseph Biederman,
M.D., said in an interview at his poster presentation during a meeting of the
New Clinical Drug Evaluation Unit sponsored by the National Institute of Mental
Health.
Dr. Biederman and his associates compared efficacy using the school and home
versions of the ADHD Rating Scale-IV, the Clinical Global Impression of
Improvement (CGI-I) scores, and adverse event reporting by 125 patients taking
the pediatric formulation of modafinil and 64 taking a placebo.
The modafinil group had significantly improved school rating total scores,
compared with those of the placebo group at 1 week, an effect that was
maintained through week 7. The final 2 weeks of the study was a washout phase.
Mean reduction from baseline was 17 points with modafinil versus 8 points with
placebo. Significant reductions in home rating total scores also were observed
with modafinil at all visits, according to Dr. Biederman, chief of the joint
program in pediatric psychopharmacology, Massachusetts General Hospital, Boston.
A significantly greater percentage of patients, 49%, was rated as "much" or
"very much" improved on the CGI-I in the modafinil group vs. 25% in the placebo
group.
Modafinil was abruptly discontinued in 37 patients. Abrupt cessation was not
associated with symptom rebound, and no evidence of withdrawal or
discontinuation syndrome was seen.
This and other phase III study results were submitted to the FDA in December
2004. "I don't see any reason why they wouldn't approve it," said Dr. Biederman,
who reported no affiliation with Cephalon Inc., the manufacturer and sponsor of
the study.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: PDNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
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487 of 998 DOCUMENTS
Family Practice News
July 15, 2005
Pediatric Modafinil Eased ADHD Symptoms
BYLINE: Mary Ellen Schneider, Senior Writer
SECTION: Pg. 41 Vol. 35 No. 14 ISSN: 0300-7073
LENGTH: 850 words
ATLANTA - Results from new research point to a possible alternative to
stimulants for the treatment of attention-deficit hyperactivity disorder in
children and adolescents.
Two phase III studies presented at the annual meeting of the American
Psychiatric Association show that a once-daily pediatric formulation of
modafinil is well tolerated and improves attention-deficit hyperactivity
disorder (ADHD) symptoms in children and adolescents.
Modafinil is currently marketed by Cephalon under the brand name Provigil in
100-mg and 200-mg strengths. Provigil is indicated for the treatment of
excessive sleepiness associated with narcolepsy, obstructive sleep apnea,
hypopnea syndrome, and shift work sleep disorder.
The company, which funded the phase II trials, is seeking approval from the
Food and Drug Administration to market modafinil in 85-mg, 170-mg, 255-mg,
340-mg, and 425-mg strengths. If approved, the drug would be indicated for
treatment of ADHD in children and adolescents aged 6-17 years. The company is
planning to launch the drug under the brand name Attenace by early 2006.
In one study, 189 patients with ADHD aged 6-17 years were randomized to a
7-week double-blind, fixed-dose treatment with either modafinil or placebo. This
regimen was followed by a 2-week withdrawal period in which half of the
modafinil-treated patients were placed on placebo without tapering, and half
were continued on the drug, said Joseph Biederman, M.D., the lead investigator
in the study and professor of psychiatry at Harvard University in Boston.
Modafinil was administered once daily, starting at 85 mg/day, and was rapidly
titrated over 7-9 days to dosages of either 340 mg/day for patients who weighed
less than 30 kg or 425 mg/day for patients who weighed 30 kg or more.
The results of the study were assessed using the school and home ADHD Rating
Scale-IV total score change from baseline to last treatment visit.
After 1 week, the 125 modafinil-treated patients had significantly greater
improvements in school scores, compared with the 64 placebo patients, and those
results were maintained through week 7.
On the school scale, patients on modafinil experienced a 17.2-point drop in
symptoms, compared with an 8.2-point drop for patients on placebo. Modafinil
also significantly improved total scores from parents, compared with placebo.
The side effects included insomnia and appetite decrease. Overall, the side
effects were generally mild and occurred at initiation of the treatment. There
were two serious adverse events not associated with the trial, said Dr.
Biederman, who is an advisory board member for Cephalon and receives
research/grant support from the company.
The researchers also assessed ADHD symptoms and physical/emotional response
after rapid discontinuation. During the 2-week withdrawal phase, there were no
reported symptom rebounds, no adverse events related to withdrawal, and no
physical or emotional responses.
Modafinil appears to work like a gentler stimulant, Dr. Biederman told this
newspaper. The findings present possible new treatment options, he said.
Although stimulants are effective, they are not universally effective. About
30%-40% of patients are nonresponsive to stimulants, and some patients also have
tolerability problems.
Stimulants have the potential for acute deterioration and symptom rebound if
treatment is interrupted or discontinued without tapering, he said.
In the second study, researchers considered the effect of a flexible dose of
modafinil in children and adolescents.
The study included 198 patients aged 6-17 years who were started on a dose of
85 mg/day of modafinil, which was titrated over 22 days based on clinical
effectiveness. The maximum dose was 425 mg/day with once-daily dosing, said
James Swanson, Ph.D., of the University of California at Irvine Child
Development Center, who was the lead investigator.
The results were assessed using the school and home ADHD Rating Scale-IV, the
Clinical Global Impression of Improvement (CGI-I), and Test Variables of
Attention (TOVA).
The home score showed a mean drop of 17.6 points in symptoms for the 131
patients receiving modafinil at a mean stable dose of 361 mg/day, compared with
a 7.5-point drop in symptoms for the 67 patients on placebo. The improvement in
the total school score was also significantly greater for modafinil patients,
Dr. Swanson said.
Modafinil was shown to significantly improve inattention and
hyperactivity/impulsivity, and there was an improvement in overall clinical
condition and in the TOVA measurements of ADHD.
The researchers focused not only on decreasing symptoms of ADHD, but on
increasing positive interaction and social skills, and they saw an increase in
positive behaviors, he said.
The side effects included insomnia, headache, and appetite problems, which
are similar to the side effects for stimulants, said Dr. Swanson, who is an
advisory board member with Cephalon, receives research/grant support from the
company, and is a member of the company's speakers' bureau.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: FPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
488 of 998 DOCUMENTS
RELIGION & ETHICS NEWSWEEKLY
Prepared by Burrelle's Information Services, which takes sole responsibility for
accuracy of transcription.
July 15, 2005 Friday
SHOW: Religion & Ethics NewsWeekly 6:00 PM EST PBS
Neuroscience and brain gain
ANCHORS: BOB ABERNETHY
REPORTERS: LUCKY SEVERSON
LENGTH: 1555 words
BOB ABERNETHY, anchor:
We have a story today about some of the ways drugmakers and neuroscientists are
enhancing what human brains can do and what the implications of these
developments are. For instance, what if brain researchers someday learn to find
out what a patient is thinking? Or to predict a disabling disease? Or, right
now, what about so-called "smart pills" that improve a college student's
performance on an exam? Is it fair that only the well-off can afford them? Lucky
Severson reports from Austin, Texas.
LUCKY SEVERSON reporting:
There's no way of knowing how many college students are popping "cognitive
performance enhancers." But health-care professionals say the use of so-called
"smart pills" has been increasing dramatically over the past five years. It
comes as no surprise to Charles Brieden, an economics major at the University of
Texas in Austin.
Mr. CHARLIE BRIEDEN (University of Texas Student): I would definitely say that
most of the kids who use it at least on a, you know, semifrequent basis don't
have a prescription. You know, it--it's fairly easy to get a hold of.
SEVERSON: Unlike most students, Charlie has a prescription for the drug he
takes, called Adderall. Charlie has attention deficit disorder or ADD. Adderall
and another drug, Ritalin, are often prescribed to treat ADD, but a lot of
students use the drugs to enhance performance--that is, to help them concentrate
and focus and face the stress and tests of modern college life.
Mr. BRIEDEN: They're in demand and you know, kids--kids pay for them, you know,
from--from their friends--buy them from their friends all the time.
SEVERSON: Is it very popular amongst the students?
Mr. ALEX MALDONADO (University of Texas Student): It is very popular, very
expensive.
SEVERSON: Alex Maldonado is another University of Texas student, a freshman, who
bought one pill of Adderall to cram for an exam.
Mr. MALDONADO: I aced the test so--I mean, I was happy about it. If it wasn't
that expensive, maybe I would take it more often.
SEVERSON: There's now a relatively new memory-boosting drug known as modafinil
or Provigil that appears, so far, to be an even more effective enhancer with
virtually no side effects. But it can cost as much as $200 for 30 pills.
Dr. JUDY ILLES (Stanford University): What does it mean to have a college
student who can't even afford an expensive drug like modafinil--for example, to
stay up all night--and vs. somebody who is able to have as much modafinil as
they wish?
SEVERSON: Judy Illes is a neuroethicist at Stanford University, and she worries
that these powerful new drugs could create an unfair advantage for kids who can
afford them.
Dr. ILLES: What does that mean for opportunities to individuals and
disenfranchised populations and so forth? So there's a host of very complex
issues that come into play there.
SEVERSON: This new science that allows us to enhance, even to alter who we are,
promises advances that seemed decades away only a few years ago. Now it's here.
Problem is, for every advance, there will be a trade-off.
Dr. Paul Root Wolpe is a professor of psychiatry at the University of
Pennsylvania.
Dr. PAUL ROOT WOLPE (University of Pennsylvania): There's an enormous amount of
talk about genetics right now. But, in fact, I really think that it's
neuroscience that's the cutting edge of the ethical issues that we have in our
society. The challenges of neuroscience are happening right now. We can do
things now that were science fiction just a short time ago.
Unidentified Man: Those signals go out through the chip.
SEVERSON: For instance, this FDA-approved, privately funded clinical trial that
could give Matthew Nagel's brain the means to move objects.
Mr. MATTHEW NAGEL: I am going to open the first e-mail, which has congrats. It
says, `You are doing a great job.'
SEVERSON: Matthew has been a paraplegic since a car accident four years ago. The
object here is to enable him to operate a computer by his thoughts, with the aid
of a tiny electrode chip implanted in his brain.
Mr. NAGEL: Now I am going to close the hand.
SEVERSON: John Donoghue is chairman of neuroscience at Brown University and
founder of Cyberkinetics, Inc.
Dr. JOHN DONOGHUE (Cyberkinetics, Inc.): These kinds of devices kick off a whole
new age of neurotechnology developments in which we can create medical devices
that can cure a whole host of diseases.
Mr. NAGEL: I can't put it into words. It's just, I--I use my brain. I just
thought it. I said, `Cursor go up to the top right.' And it did, and now I can
control it all over the screen. It will give me a sense of independence.
SEVERSON: Stanford law Professor Hank Greely says the chip adds something to the
human dimension that wasn't there before.
Professor HANK GREELY (Stanford University): When we get into people talking
about various implants to either put new sensory--you give humans new senses or
allow humans by thinking to control devices externally, that becomes a little
more troubling. To a lot of people, the idea that somehow we're transcending
what we're supposed to be as humans.
SEVERSON: In the popular thriller "The Manchurian Candidate," a brain implant
prompts a man to become an assassin. That scenario is no longer science fiction.
Scientists say the technology to modify our personality or memory is barely
around the bend.
Mr. MICHAEL GAZZANIGA (Dartmouth College): There are things happening with
incredible speed.
SEVERSON: Michael Gazzaniga is director of neuroscience at Dartmouth College.
Mr. GAZZANIGA: Two years ago--I would say, three years ago, no one would imagine
that in a brain-imaging environment, you could begin to understand how people go
about doing moral reasoning. And that is now happening.
SEVERSON: Gazzaniga is author of "The Ethical Brain." He thinks our brains are
all wired with similar moral circuitry--at least those of us considered normal.
Mr. GAZZANIGA: We don't kill. We don't like incest. We don't like cheaters. The
guess is that there's something, probably some moral spark, that's in us. Some
moral compass is guiding us through all this social behavior.
SEVERSON: That would mean that a secular person may have the same moral values
as a religious one. It's a controversial conclusion.
Mr. GAZZANIGA: I'm not antireligious in any way, shape or form. It's none of my
business how you got to your--your set of moral values. I think what's happening
is, though, we're going to find out that everybody in the room basically has
their brain built in such a way that they tend to respond in a particular moral
way, because of the way their brain is built.
SEVERSON: It's all possible because of magnetic resonance imaging, MRI, that is
becoming so sophisticated neuroscientists are able to identify what kinds of
thoughts and emotions stimulate certain parts of the brain.
Dr. ROOT WOLPE: We can do things now, such as looking at brain images, and
predict what a person had just been looking at or what they had just been
thinking about.
SEVERSON: Professor Greely says a potential negative side of the neuroscience
revolution is the ability to predict someone's physical or mental illness.
Prof. GREELY: If your insurer can figure out well in advance that you're going
to have Parkinson's disease or Alzheimer's disease, then that could be pretty
significant in terms of whether you can get long-term care insurance.
SEVERSON: And there's more. Until now, our thoughts were our own.
Dr. ROOT WOLPE: We may actually be able to breach that barrier and ex--extract
directly from your brain information that before we could only get by you
choosing to tell it to us. That's very, very new. And it raises profound
questions about privacy.
SEVERSON: There are many troubling questions that have profound implications,
some ethical, some physical. The smart pills, for example, so popular on campus,
it's too early to tell if they have dangerous side effects.
Mr. GAZZANIGA: The safety and efficacy of these drugs is simply not known. The
possible side effects, in terms of real damage to the nervous system, hasn't
even begun to be worked out.
Mr. BRIEDEN: I had my first, you know, bout with depression. Like, last--last
semester I actually, like, started freaking out. Because I was taking it, I was
taking it too frequently, and it was, you know, you can start to get, you know,
schized out.
SEVERSON: Ultimately, the bigger question, in the view of Professor Wolpe, is
the question of values.
Dr. ROOT WOLPE: Do we want to say that some path to self-improvement is ennobled
by the struggle? Or are we OK with the idea that there's a quicker path to
enlightenment?
SEVERSON: The answer is not entirely clear. Take Fiorella Vargas, a George
Washington University graduate. She survived college without the help of
cognitive enhancers.
Ms. FIORELLA VARGAS: It is very--it's very stressful. So, but you deal with it.
And you get beyond it. And then you are proud once graduation day comes.
SEVERSON: Charlie, on the other hand, wouldn't think twice.
Mr. BRIEDEN: Any way you can get a leg up in life, you know, any way you can get
an advantage, you know, whatever it may be, you know, I'd say go for it.
SEVERSON: The question that can't be answered yet is whether smart pills and
brain technology actually enhance us or prevent us from discovering and
developing who we really are.
For RELIGION & ETHICS NEWSWEEKLY, I'm Lucky Severson in Washington.
LOAD-DATE: July 18, 2005
LANGUAGE: ENGLISH
DOCUMENT-TYPE: Profile
PUBLICATION-TYPE: Transcript
Copyright 2005 WNET-TV.
All Rights Reserved
489 of 998 DOCUMENTS
Clinical Psychiatry News
July 2005
Antinarcolepsy Drug May Improve ADHD;
Modafinil could prove an alternative to stimulants for addressing symptoms,
phase III studies show.
BYLINE: Mary Ellen Schneider, Senior Writer
SECTION: Pg. 38 Vol. 33 No. 7 ISSN: 0270-6644
LENGTH: 856 words
ATLANTA - Results from new research point to a possible alternative to
stimulants for the treatment of attention-deficit hyperactivity disorder in
children and adolescents.
Two phase III studies presented at the annual meeting of the American
Psychiatric Association show that a once-daily pediatric formulation of
modafinil is well tolerated and improves attention-deficit hyperactivity
disorder (ADHD) symptoms in children and adolescents.
Modafinil is currently marketed by Cephalon under the brand name Provigil in
100-mg and 200-mg strengths. Provigil is indicated for the treatment of
excessive sleepiness associated with narcolepsy, obstructive sleep apnea,
hypopnea syndrome, and shift work sleep disorder.
The company, which funded the phase II trials, is seeking approval from the
Food and Drug Administration to market modafinil in 85-mg, 170-mg, 255-mg,
340-mg, and 425-mg strengths. If approved, the drug would be indicated for
treatment of ADHD in children and adolescents aged 6-17 years.
The company is planning to launch the drug under the brand name Attenace by
early 2006.
In one study, 189 patients with ADHD aged 6-17 years were randomized to a
7-week double-blind, fixed-dose treatment with either modafinil or placebo. This
protocol was followed by a 2-week withdrawal period in which half of the
modafinil-treated patients were placed on placebo without tapering, and half
were continued on the drug, said Joseph Biederman, M.D., the lead investigator
in the study and professor of psychiatry at Harvard University in Boston.
Modafinil was administered once daily, starting at 85 mg/day, and was rapidly
titrated over 7-9 days to dosages of either 340 mg/day for patients who weighed
less than 30 kg or 425 mg/day for patients who weighed 30 kg or more.
The results of the study were assessed using the school and home ADHD Rating
Scale-IV total score change from baseline to last treatment visit.
After 1 week, the 125 modafinil-treated patients had significantly greater
improvements in school scores, compared with the 64 placebo patients, and those
results were maintained through week 7.
On the school scale, patients on modafinil experienced a 17.2-point drop in
symptoms, compared with an 8.2-point drop for patients on placebo. Modafinil
also significantly improved total scores from parents, compared with placebo.
The side effects included insomnia and appetite decrease. Overall, the side
effects were generally mild and occurred at initiation of the treatment. There
were two serious adverse events not associated with the trial, said Dr.
Biederman, who is an advisory board member for Cephalon and receives
research/grant support from the company.
The researchers also assessed ADHD symptoms and physical/emotional response
after rapid discontinuation. During the 2-week withdrawal phase there were no
reported symptom rebounds, no adverse events related to withdrawal, and no
physical or emotional responses.
Modafinil appears to work like a gentler stimulant, Dr. Biederman said in an
interview.
The findings present possible new treatment options, he said. Although
stimulants are effective, they are not universally effective. About 30%-40% of
patients are nonresponsive to stimulants, he said, and some patients also have
tolerability problems.
Stimulants also have the potential for acute deterioration and symptom
rebound if treatment is interrupted or discontinued without tapering, Dr.
Biederman said.
In the second study, researchers considered the effect of a flexible dose of
modafinil in children and adolescents.
The study included 198 patients aged 6-17 years who were started on a dose of
85 mg/day of modafinil, which was titrated over 22 days based on clinical
effectiveness. The maximum dose was 425 mg/day with once-daily dosing, said
James Swanson, Ph.D., of the University of California at Irvine Child
Development Center, who was the lead investigator.
The results were assessed using the school and home ADHD Rating Scale-IV, the
Clinical Global Impression of Improvement (CGI-I), and Test Variables of
Attention (TOVA).
The home score showed a mean drop of 17.6 points in symptoms for the 131
patients receiving modafinil at a mean stable dose of 361 mg/day, compared with
a 7.5-point drop in symptoms for the 67 patients on placebo. The improvement in
the total school score was also significantly greater for modafinil patients,
Dr. Swanson reported.
Modafinil was shown to significantly improve inattention and
hyperactivity/impulsivity, and there was an improvement in overall clinical
condition and in the TOVA measurements of ADHD.
The researchers focused not only on decreasing symptoms of ADHD, but on
increasing positive interaction and social skills, and they saw an increase in
positive behaviors, he said.
The side effects included insomnia, headache, and appetite problems, which
are similar to the side effects for stimulants, said Dr. Swanson, who is an
advisory board member with Cephalon, receives research/grant support from the
company, and is a member of the company's speakers' bureau.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
490 of 998 DOCUMENTS
Pediatric News
July 2005
Pediatric Modafinil Shows Results in ADHD
BYLINE: Mary Ellen Schneider, Senior Writer
SECTION: Pgs. 28-29 Vol. 39 No. 7 ISSN: 0031-398X
LENGTH: 864 words
ATLANTA - Results from new research point to a possible alternative to
stimulants for the treatment of attention-deficit hyperactivity disorder in
children and adolescents.
Two phase III studies presented at the annual meeting of the American
Psychiatric Association show that a once-daily pediatric formulation of
modafinil is well tolerated and improves attention-deficit hyperactivity
disorder (ADHD) symptoms in children and adolescents.
Modafinil is currently marketed by Cephalon under the brand name Provigil in
100-mg and 200-mg strengths.
Provigil is indicated for the treatment of excessive sleepiness associated
with narcolepsy, obstructive sleep apnea, hypopnea syndrome, and shift work
sleep disorder.
The company, which funded the phase II trials, is seeking approval from the
Food and Drug Administration to market modafinil in 85-mg, 170-mg, 255-mg,
340-mg, and 425-mg strengths. If approved, the drug would be indicated for
treatment of ADHD in children and adolescents aged 6-17 years.
The company is planning to launch the drug under the brand name Attenace by
early 2006.
In one study, 189 patients with ADHD aged 6-17 years were randomized to a
7-week double-blind, fixed-dose treatment with either modafinil or placebo. This
regime was followed by a 2-week withdrawal period in which half of the modafinil
-treated patients were placed on placebo without tapering, and half were
continued on the drug, said Joseph Biederman, M.D., the lead investigator in the
study and professor of psychiatry at Harvard University in Boston.
Modafinil was administered once daily, starting at 85 mg/day, and was rapidly
titrated over 7-9 days to dosages of either 340 mg/day for patients who weighed
less than 30 kg or 425 mg/day for patients who weighed 30 kg or more.
The results of the study were assessed using the school and home ADHD Rating
Scale-IV total score change from baseline to last treatment visit.
After 1 week, the 125 modafinil-treated patients had significantly greater
improvements in school scores, compared with the 64 placebo patients, and those
results were maintained through week 7.
On the school scale, patients on modafinil experienced a 17.2-point drop in
symptoms, compared with an 8.2-point drop for patients who were on placebo.
Modafinil also significantly improved total scores from parents, compared with
placebo.
The side effects included insomnia and appetite decrease. Overall, the side
effects were generally mild and occurred at initiation of the treatment. There
were two serious adverse events not associated with the trial, said Dr.
Biederman, who is an advisory board member for Cephalon and receives
research/grant support from the company.
The researchers also assessed ADHD symptoms and physical/emotional response
after rapid discontinuation. During the 2-week withdrawal phase, there were no
reported symptom rebounds, no adverse events related to withdrawal, and no
physical or emotional responses.
Modafinil appears to work like a gentler stimulant, Dr. Biederman said in an
interview. The findings present possible new treatment options, he said.
Although stimulants are effective, they are not universally effective.
About 30%-40% of patients are nonresponsive to stimulants, he said, and some
patients also have tolerability problems.
Stimulants also have the potential for acute deterioration and symptom
rebound if treatment is interrupted or discontinued without tapering, Dr.
Biederman said.
In the second study, the researchers considered the effect of a flexible dose
of modafinil in children and adolescents.
The study included 198 patients aged 6-17 years who were started on a dose of
85 mg/day of modafinil, which was titrated over 22 days based on clinical
effectiveness. The maximum dose was 425 mg/day with once-daily dosing, said
James Swanson, Ph.D., of the University of California at Irvine Child
Development Center, who was the lead investigator.
The results were assessed using the school and home ADHD Rating Scale-IV, the
Clinical Global Impression of Improvement (CGI-I), and the Test of Variables of
Attention (TOVA).
The home score showed a mean drop of 17.6 points in symptoms for the 131
patients receiving modafinil at a mean stable dose of 361 mg/day, compared with
a 7.5-point drop in symptoms for the 67 patients on placebo.
The improvement in the total school score was also significantly greater for
modafinil patients, Dr. Swanson reported.
The researchers said Modafinil was shown to significantly improve inattention
and hyperactivity/impulsivity, and there was an improvement in overall clinical
condition and in the TOVA measurements of ADHD.
The researchers focused not only on decreasing symptoms of ADHD, but on
increasing positive interaction and social skills, and they saw an increase in
positive behaviors, he said.
The side effects included insomnia, headache, and appetite problems, which
are similar to the side effects for stimulants, said Dr. Swanson, who is an
advisory board member with Cephalon, receives research/grant support from the
company, and is a member of the company's speakers' bureau.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: PDNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
491 of 998 DOCUMENTS
The Herald (Glasgow)
June 14, 2005
Doping drug rejected by NHS over cost
BYLINE: CALUM MacDONALD
SECTION: NEWS; Pg. 4
LENGTH: 168 words
A DRUG which has been at the centre of a number of doping scandals involving
athletes has been rejected for use by the NHS in Scotland because it is not
cost-effective.
The Scottish Medicines Consortium (SMC) has advised NHS boards not to prescribe
Provigil, a brand name for the generic modafinil drug, to patients suffering
from excessive sleepiness associated with shift work sleep disorder or
obstructive sleep apnoea, the complete absence of breathing for more than 10
seconds during sleep.
Despite trials showing that modafinil did bring about a modest improvement in
sleepiness and quality of life, the SMC decided the therapy was not
cost-effective.
Modafinil is a moodbrightening and memoryenhancing psychostimulant which
enhances wakefulness and vigilance.
Kelli White, the American sprinter, received a two-year ban for using modafinil
and was stripped of her 100m and 200m gold medals won in Paris in 2003.
It was claimed at the time that she used the drug for treating narcolepsy, the
sleeping disorder.
LOAD-DATE: June 17, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: NEWSPAPER
JOURNAL-CODE: GHERLD
Copyright 2005 Newsquest Media Group
All rights reserved
492 of 998 DOCUMENTS
New Scientist
May 28, 2005
11 steps to a better brain;
It doesn't matter how brainy you are or how much education you've had - you can
still improve and expand your mind. Boosting your mental faculties doesn't have
to mean studying hard or becoming a reclusive bookworm. There are lots of
tricks, techniques and habits as well as changes to your lifestyle, diet and
behaviour that can help you flex your grey matter and get the best out of your
brain cells. Follow New Scientist's guide to getting smarter, and maximise your
brain's potential
BYLINE: Kate Douglas, Alison George, Bob Holmes, Graham Lawton, John McCrone,
Alison Motluk, Helen Phillips
SECTION: FEATURES; Pg. 28
LENGTH: 4542 words
Smart drugs
Does getting old have to mean worsening memory, slower reactions and fuzzy
thinking?
AROUND the age of 40, honest folks may already admit to noticing changes in
their mental abilities. This is the beginning of a gradual decline that in all
too many of us will culminate in full-blown dementia. If it were possible
somehow to reverse it, slow it or mask it, wouldn't you?
A few drugs that might do the job, known as "cognitive enhancement", are already
on the market, and a few dozen others are on the way. Perhaps the best-known is
modafinil. Licensed to treat narcolepsy, the condition that causes people to
suddenly fall asleep, it has notable effects in healthy people too. Modafinil
can keep a person awake and alert for 90 hours straight, with none of the
jitteriness and bad concentration that amphetamines or even coffee seem to
produce.
In fact, with the help of modafinil, sleep-deprived people can perform even
better than their well-rested, unmedicated selves. The forfeited rest doesn't
even need to be made good. Military research is finding that people can stay
awake for 40 hours, sleep the normal 8 hours, and then pull a few more
all-nighters with no ill effects. It's an open secret that many, perhaps most,
prescriptions for modafinil are written not for people who suffer from
narcolepsy, but for those who simply want to stay awake. Similarly, many people
are using Ritalin not because they suffer from attention deficit or any other
disorder, but because they want superior concentration during exams or
heavy-duty negotiations.
The pharmaceutical pipeline is clogged with promising compounds - drugs that act
on the nicotinic receptors that smokers have long exploited, drugs that work on
the cannabinoid system to block pot-smoking-type effects. Some drugs have also
been specially designed to augment memory. Many of these look genuinely
plausible: they seem to work, and without any major side effects.
So why aren't we all on cognitive enhancers already? "We need to be careful what
we wish for," says Daniele Piomelli at the University of California at Irvine.
He is studying the body's cannabinoid system with a view to making memories less
emotionally charged in people suffering from post-traumatic stress disorder.
Tinkering with memory may have unwanted effects, he warns. "Ultimately we may
end up remembering things we don't want to."
Gary Lynch, also at UC Irvine, voices a similar concern. He is the inventor of
ampakines, a class of drugs that changes the rules about how a memory is encoded
and how strong a memory trace is - the essence of learning (see New Scientist ,
14 May, p 6). But maybe the rules have already been optimised by evolution, he
suggests. What looks to be an improvement could have hidden downsides.
Still, the opportunity may be too tempting to pass up. The drug acts only in the
brain, claims Lynch. It has a short half-life of hours. Ampakines have been
shown to restore function to severely sleep-deprived monkeys that would
otherwise perform poorly. Preliminary studies in humans are just as exciting.
You could make an elderly person perform like a much younger person, he says.
And who doesn't wish for that?
Food for thought
You are what you eat, and that includes your brain. So what is the ultimate
mastermind diet?
YOUR brain is the greediest organ in your body, with some quite specific dietary
requirements. So it is hardly surprising that what you eat can affect how you
think. If you believe the dietary supplement industry, you could become the next
Einstein just by popping the right combination of pills. Look closer, however,
and it isn't that simple. The savvy consumer should take talk of brain-boosting
diets with a pinch of low-sodium salt. But if it is possible to eat your way to
genius, it must surely be worth a try.
First, go to the top of the class by eating breakfast. The brain is best fuelled
by a steady supply of glucose, and many studies have shown that skipping
breakfast reduces people's performance at school and at work.
But it isn't simply a matter of getting some calories down. According to
research published in 2003, kids breakfasting on fizzy drinks and sugary snacks
performed at the level of an average 70-year-old in tests of memory and
attention. Beans on toast is a far better combination, as Barbara Stewart from
the University of Ulster, UK, discovered. Toast alone boosted children's scores
on a variety of cognitive tests, but when the tests got tougher, the breakfast
with the high-protein beans worked best. Beans are also a good source of fibre,
and other research has shown a link between a high-fibre diet and improved
cognition. If you can't stomach beans before midday, wholemeal toast with
Marmite makes a great alternative. The yeast extract is packed with B vitamins,
whose brain-boosting powers have been demonstrated in many studies.
A smart choice for lunch is omelette and salad. Eggs are rich in choline, which
your body uses to produce the neurotransmitter acetylcholine. Researchers at
Boston University found that when healthy young adults were given the drug
scopolamine, which blocks acetylcholine receptors in the brain, it significantly
reduced their ability to remember word pairs. Low levels of acetylcholine are
also associated with Alzheimer's disease, and some studies suggest that boosting
dietary intake may slow age-related memory loss.
A salad packed full of antioxidants, including beta-carotene and vitamins C and
E, should also help keep an ageing brain in tip-top condition by helping to mop
up damaging free radicals. Dwight Tapp and colleagues from the University of
California at Irvine found that a diet high in antioxidants improved the
cognitive skills of 39 ageing beagles - proving that you can teach an old dog
new tricks.
Round off lunch with a yogurt dessert, and you should be alert and ready to face
the stresses of the afternoon. That's because yogurt contains the amino acid
tyrosine, needed for the production of the neurotransmitters dopamine and
noradrenalin, among others. Studies by the US military indicate that tyrosine
becomes depleted when we are under stress and that supplementing your intake can
improve alertness and memory.
Don't forget to snaffle a snack mid-afternoon, to maintain your glucose levels.
Just make sure you avoid junk food, and especially highly processed goodies such
as cakes, pastries and biscuits, which contain trans-fatty acids. These not only
pile on the pounds, but are implicated in a slew of serious mental disorders,
from dyslexia and ADHD (attention deficit hyperactivity disorder) to autism.
Hard evidence for this is still thin on the ground, but last year researchers at
the annual Society for Neuroscience meeting in San Diego, California, reported
that rats and mice raised on the rodent equivalent of junk food struggled to
find their way around a maze, and took longer to remember solutions to problems
they had already solved.
It seems that some of the damage may be mediated through triglyceride, a
cholesterol-like substance found at high levels in rodents fed on trans-fats.
When the researchers gave these rats a drug to bring triglyceride levels down
again, the animals' performance on the memory tasks improved.
Brains are around 60 per cent fat, so if trans-fats clog up the system, what
should you eat to keep it well oiled? Evidence is mounting in favour of omega-3
fatty acids, in particular docosahexaenoic acid or DHA. In other words, your
granny was right: fish is the best brain food. Not only will it feed and
lubricate a developing brain, DHA also seems to help stave off dementia. Studies
published last year reveal that older mice from a strain genetically altered to
develop Alzheimer's had 70 per cent less of the amyloid plaques associated with
the disease when fed on a high-DHA diet.
Finally, you could do worse than finish off your evening meal with strawberries
and blueberries. Rats fed on these fruits have shown improved coordination,
concentration and short-term memory. And even if they don't work such wonders in
people, they still taste fantastic. So what have you got to lose?
The Mozart effect
Music may tune up your thinking, but you can't just crank up the volume and
expect to become a genius
A DECADE ago Frances Rauscher, a psychologist now at the University of Wisconsin
at Oshkosh, and her colleagues made waves with the discovery that listening to
Mozart improved people's mathematical and spatial reasoning. Even rats ran mazes
faster and more accurately after hearing Mozart than after white noise or music
by the minimalist composer Philip Glass. Last year, Rauscher reported that, for
rats at least, a Mozart piano sonata seems to stimulate activity in three genes
involved in nerve-cell signalling in the brain.
This sounds like the most harmonious way to tune up your mental faculties. But
before you grab the CDs, hear this note of caution. Not everyone who has looked
for the Mozart effect has found it. What's more, even its proponents tend to
think that music boosts brain power simply because it makes listeners feel
better - relaxed and stimulated at the same time - and that a comparable
stimulus might do just as well. In fact, one study found that listening to a
story gave a similar performance boost.
There is, however, one way in which music really does make you smarter, though
unfortunately it requires a bit more effort than just selecting something mellow
on your iPod. Music lessons are the key. Six-year-old children who were given
music lessons, as opposed to drama lessons or no extra instruction, got a 2 to
3-point boost in IQ scores compared with the others. Similarly, Rauscher found
that after two years of music lessons, pre-school children scored better on
spatial reasoning tests than those who took computer lessons.
Maybe music lessons exercise a range of mental skills, with their requirement
for delicate and precise finger movements, and listening for pitch and rhythm,
all combined with an emotional dimension. Nobody knows for sure. Neither do they
know whether adults can get the same mental boost as young children. But,
surely, it can't hurt to try.
Bionic brains
If training and tricks seem too much like hard work, some technological short
cuts can boost brain function
Gainful employment
Put your mind to work in the right way and it could repay you with an impressive
bonus
UNTIL recently, a person's IQ - a measure of all kinds of mental problem-solving
abilities, including spatial skills, memory and verbal reasoning - was thought
to be a fixed commodity largely determined by genetics. But recent hints suggest
that a very basic brain function called working memory might underlie our
general intelligence, opening up the intriguing possibility that if you improve
your working memory, you could boost your IQ too.
Working memory is the brain's short-term information storage system. It's a
workbench for solving mental problems. For example if you calculate 73 ? 6 + 7,
your working memory will store the intermediate steps necessary to work out the
answer. And the amount of information that the working memory can hold is
strongly related to general intelligence.
A team led by Torkel Klingberg at the Karolinska Institute in Stockholm, Sweden,
has found signs that the neural systems that underlie working memory may grow in
response to training. Using functional magnetic resonance imaging (fMRI) brain
scans, they measured the brain activity of adults before and after a
working-memory training programme, which involved tasks such as memorising the
positions of a series of dots on a grid. After five weeks of training, their
brain activity had increased in the regions associated with this type of memory
(Nature Neuroscience , vol 7, p 75).
Perhaps more significantly, when the group studied children who had completed
these types of mental workouts, they saw improvement in a range of cognitive
abilities not related to the training, and a leap in IQ test scores of 8 per
cent (Journal of the American Academy of Child and Adolescent Psychiatry , vol
44, p 177). It's early days yet, but Klingberg thinks working-memory training
could be a key to unlocking brain power. "Genetics determines a lot and so does
the early gestation period," he says. "On top of that, there is a few per cent -
we don't know how much - that can be improved by training."
Memory marvels
Mind like a sieve? Don't worry. The difference between mere mortals and memory
champs is more method than mental capacity
AN AUDITORIUM is filled with 600 people. As they file out, they each tell you
their name. An hour later, you are asked to recall them all. Can you do it? Most
of us would balk at the idea. But in truth we're probably all up to the task. It
just needs a little technique and dedication.
First, learn a trick from the "mnemonists" who routinely memorise strings of
thousands of digits, entire epic poems, or hundreds of unrelated words. When
Eleanor Maguire from University College London and her colleagues studied eight
front runners in the annual World Memory Championships they did not find any
evidence that these people have particularly high IQs or differently configured
brains. But, while memorising, these people did show activity in three brain
regions that become active during movements and navigation tasks but are not
normally active during simple memory tests.
This may be connected to the fact that seven of them used a strategy in which
they place items to be remembered along a visualised route (Nature Neuroscience
, vol 6, p 90). To remember the sequence of an entire pack of playing cards for
example, the champions assign each card an identity, perhaps an object or
person, and as they flick through the cards they can make up a story based on a
sequence of interactions between these characters and objects at sites along a
well-trodden route.
Actors use a related technique: they attach emotional meaning to what they say.
We always remember highly emotional moments better than less emotionally loaded
ones. Professional actors also seem to link words with movement, remembering
action-accompanied lines significantly better than those delivered while static,
even months after a show has closed.
Helga Noice, a psychologist from Elmhurst College in Illinois, and Tony Noice,
an actor, who together discovered this effect, found that non-thesps can benefit
by adopting a similar technique. Students who paired their words with previously
learned actions could reproduce 38 per cent of them after just 5 minutes,
whereas rote learners only managed 14 per cent. The Noices believe that having
two mental representations gives you a better shot at remembering what you are
supposed to say.
Strategy is important in everyday life too, says Barry Gordon from Johns Hopkins
University in Baltimore, Maryland. Simple things like always putting your car
keys in the same place, writing things down to get them off your mind, or just
deciding to pay attention, can make a big difference to how much information you
retain. And if names are your downfall, try making some mental associations.
Just remember to keep the derogatory ones to yourself.
Sleep on it
Never underestimate the power of a good night's rest
SKIMPING on sleep does awful things to your brain. Planning, problem-solving,
learning, concentration,working memory and alertness all take a hit. IQ scores
tumble. "If you have been awake for 21 hours straight, your abilities are
equivalent to someone who is legally drunk," says Sean Drummond from the
University of California, San Diego. And you don't need to pull an all-nighter
to suffer the effects: two or three late nights and early mornings on the trot
have the same effect.
Luckily, it's reversible - and more. If you let someone who isn't sleep-deprived
have an extra hour or two of shut-eye, they perform much better than normal on
tasks requiring sustained attention, such taking an exam. And being able to
concentrate harder has knock-on benefits for overall mental performance.
"Attention is the base of a mental pyramid," says Drummond. "If you boost that,
you can't help boosting everything above it."
These are not the only benefits of a decent night's sleep. Sleep is when your
brain processes new memories, practises and hones new skills - and even solves
problems. Say you're trying to master a new video game. Instead of grinding away
into the small hours, you would be better off playing for a couple of hours,
then going to bed. While you are asleep your brain will reactivate the circuits
it was using as you learned the game, rehearse them, and then shunt the new
memories into long-term storage. When you wake up, hey presto! You will be a
better player. The same applies to other skills such as playing the piano,
driving a car and, some researchers claim, memorising facts and figures. Even
taking a nap after training can help, says Carlyle Smith of Trent University in
Peterborough, Ontario.
There is also some evidence that sleep can help produce moments of
problem-solving insight. The famous story about the Russian chemist Dmitri
Mendeleev suddenly "getting" the periodic table in a dream after a day spent
struggling with the problem is probably true. It seems that sleep somehow allows
the brain to juggle new memories to produce flashes of creative insight. So if
you want to have a eureka moment, stop racking your brains and get your head
down.
Body and mind
Physical exercise can boost brain as well as brawn
IT'S a dream come true for those who hate studying. Simply walking sedately for
half an hour three times a week can improve abilities such as learning,
concentration and abstract reasoning by 15 per cent. The effects are
particularly noticeable in older people. Senior citizens who walk regularly
perform better on memory tests than their sedentary peers. What's more, over
several years their scores on a variety of cognitive tests show far less decline
than those of non-walkers. Every extra mile a week has measurable benefits.
It's not only oldies who benefit, however. Angela Balding from the University of
Exeter, UK, has found that schoolchildren who exercise three or four times a
week get higher than average exam grades at age 10 or 11. The effect is
strongest in boys, and while Balding admits that the link may not be causal, she
suggests that aerobic exercise may boost mental powers by getting extra oxygen
to your energy-guzzling brain.
There's another reason why your brain loves physical exercise: it promotes the
growth of new brain cells. Until recently, received wisdom had it that we are
born with a full complement of neurons and produce no new ones during our
lifetime. Fred Gage from the Salk Institute in La Jolla, California, busted that
myth in 2000 when he showed that even adults can grow new brain cells. He also
found that exercise is one of the best ways to achieve this.
In mice, at least, the brain-building effects of exercise are strongest in the
hippocampus, which is involved with learning and memory. This also happens to be
the brain region that is damaged by elevated levels of the stress hormone
cortisol. So if you are feeling frazzled, do your brain a favour and go for a
run.
Even more gentle exercise, such as yoga, can do wonders for your brain. Last
year, researchers at the University of California, Los Angeles, reported results
from a pilot study in which they considered the mood-altering ability of
different yoga poses. Comparing back bends, forward bends and standing poses,
they concluded that the best way to get a mental lift is to bend over backwards.
And the effect works both ways. Just as physical exercise can boost the brain,
mental exercise can boost the body. In 2001, researchers at the Cleveland Clinic
Foundation in Ohio asked volunteers to spend just 15 minutes a day thinking
about exercising their biceps. After 12 weeks, their arms were 13 per cent
stronger.
Nuns on a run
If you don't want senility to interfere with your old age, perhaps you should
seek some sisterly guidance
THE convent of the School Sisters of Notre Dame on Good Counsel Hill in Mankato,
Minnesota, might seem an unusual place for a pioneering brain-science
experiment. But a study of its 75 to 107-year-old inhabitants is revealing more
about keeping the brain alive and healthy than perhaps any other to date. The
"Nun study" is a unique collaboration between 678 Catholic sisters recruited in
1991 and Alzheimer's expert David Snowdon of the Sanders-Brown Center on Aging
and the University of Kentucky in Lexington.
The sisters' miraculous longevity - the group boasts seven centenarians and many
others well on their way - is surely in no small part attributable to their
impeccable lifestyle. They do not drink or smoke, they live quietly and
communally, they are spiritual and calm and they eat healthily and in
moderation. Nevertheless, small differences between individual nuns could reveal
the key to a healthy mind in later life.
Some of the nuns have suffered from Alzheimer's disease, but many have avoided
any kind of dementia or senility. They include Sister Matthia, who was mentally
fit and active from her birth in 1894 to the day she died peacefully in her
sleep, aged 104. She was happy and productive, knitting mittens for the poor
every day until the end of her life. A post-mortem of Sister Matthia's brain
revealed no signs of excessive ageing. But in some other, remarkable cases,
Snowdon has found sisters who showed no outwards signs of senility in life, yet
had brains that looked as if they were ravaged by dementia.
How did Sister Matthia and the others cheat time? Snowdon's study, which
includes an annual barrage of mental agility tests and detailed medical exams,
has found several common denominators. The right amount of vitamin folate is
one. Verbal ability early in life is another, as are positive emotions early in
life, which were revealed by Snowdon's analysis of the personal autobiographical
essays each woman wrote in her 20s as she took her vows. Activities, crosswords,
knitting and exercising also helped to prevent senility, showing that the old
adage "use it or lose it" is pertinent. And spirituality, or the positive
attitude that comes from it, can't be overlooked. But individual differences
also matter. To avoid dementia, your general health may be vital: metabolic
problems, small strokes and head injuries seem to be common triggers of
Alzheimer's dementia.
Obviously, you don't have to become a nun to stay mentally agile. We can all
aspire to these kinds of improvements. As one of the sisters put it, "Think no
evil, do no evil, hear no evil, and you will never write a best-selling novel."
Attention seeking
You can be smart, well-read, creative and knowledgeable, but none of it is any
use if your mind isn't on the job
PAYING attention is a complex mental process, an interplay of zooming in on
detail and stepping back to survey the big picture. So unfortunately there is no
single remedy to enhance your concentration. But there are a few ways to improve
it.
The first is to raise your arousal levels. The brain's attentional state is
controlled by the neurotransmitters dopamine and noradrenalin. Dopamine
encourages a persistent, goal-centred state of mind whereas noradrenalin
produces an outward-looking, vigilant state. So not surprisingly, anything that
raises dopamine levels can boost your powers of concentration.
One way to do this is with drugs such as amphetamines and the ADHD drug
methylphenidate, better known as Ritalin. Caffeine also works. But if you prefer
the drug-free approach, the best strategy is to sleep well, eat foods packed
with slow-release sugars, and take lots of exercise. It also helps if you are
trying to focus on something that you find interesting.
The second step is to cut down on distractions. Workplace studies have found
that it takes up to 15 minutes to regain a deep state of concentration after a
distraction such as a phone call. Just a few such interruptions and half the day
is wasted.
Music can help as long as you listen to something familiar and soothing that
serves primarily to drown out background noise. Psychologists also recommend
that you avoid working near potential diversions, such as the fridge.
There are mental drills to deal with distractions. College counsellors routinely
teach students to recognise when their thoughts are wandering, and catch
themselves by saying "Stop! Be here now!" It sounds corny but can develop into a
valuable habit. As any Zen meditator will tell you, concentration is as much a
skill to be lovingly cultivated as it is a physiochemical state of the brain.
Positive feedback
Thought control is easier than you might imagine
IT SOUNDS a bit New Age, but there is a mysterious method of thought control you
can learn that seems to boost brain power. No one quite knows how it works, and
it is hard to describe exactly how to do it: it's not relaxation or
concentration as such, more a state of mind. It's called neurofeedback. And it
is slowly gaining scientific credibility.
Neurofeedback grew out of biofeedback therapy, popular in the 1960s. It works by
showing people a real-time measure of some seemingly uncontrollable aspect of
their physiology - heart rate, say - and encouraging them to try and change it.
Astonishingly, many patients found that they could, though only rarely could
they describe how they did it.
More recently, this technique has been applied to the brain - specifically to
brain wave activity measured by an electroencephalogram, or EEG. The first
attempts were aimed at boosting the size of the alpha wave, which crescendos
when we are calm and focused. In one experiment, researchers linked the speed of
a car in a computer game to the size of the alpha wave. They then asked subjects
to make the car go faster using only their minds. Many managed to do so, and
seemed to become more alert and focused as a result.
This early success encouraged others, and neurofeedback soon became a popular
alternative therapy for ADHD. There is now good scientific evidence that it
works, as well as some success in treating epilepsy, depression, tinnitus,
anxiety, stroke and brain injuries.
And to keep up with the times, some experimenters have used brain scanners in
place of EEGs. Scanners can allow people to see and control activity of specific
parts of the brain. A team at Stanford University in California showed that
people could learn to control pain by watching the activity of their pain
centres (New Scientist , 1 May 2004, p 9).
But what about outside the clinic? Will neuro feedback ever allow ordinary
people to boost their brain function? Possibly. John Gruzelier of Imperial
College London has shown that it can improve medical students' memory and make
them feel calmer before exams. He has also shown that it can improve musicians'
and dancers' technique, and is testing it out on opera singers and surgeons.
Neils Birbaumer from the University of Tübingen in Germany wants to see whether
neurofeedback can help psychopathic criminals control their impulsiveness. And
there are hints that the method could boost creativity, enhance our orgasms,
give shy people more confidence, lift low moods, alter the balance between left
and right brain activity, and alter personality traits. All this by the power of
thought.
LOAD-DATE: May 31, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
Copyright 2005 Reed Business Information, UK, a division of Reed Elsevier Inc.
All Rights Reserved
493 of 998 DOCUMENTS
The Guardian (London) - Final Edition
May 19, 2005
Drugs in sport: I was like a drugs guinea pig, says banned sprinter
BYLINE: Duncan Mackay
SECTION: Guardian Sport Pages, Pg. 32
LENGTH: 553 words
Kelli White, the former training partner of Britain's banned sprinter Dwain
Chambers, has claimed she was treated like a "guinea pig" as she experimented
with a cocktail of banned substances.
The American told the World Anti-Doping Agency at a hearing in Montreal that she
was asked to try out a range of performance-enhancing drugs, including the
designer anabolic steroid tetrahydrogestrinone (THG), the blood-boosting hormone
erythropoietin (EPO) and the stimulant modafinil, without ever being warned of
the potential side effects.
"I was offered a lot of things and asked to test them to see if I responded
better to certain products," she said. "I was like a guinea pig. I tried a lot
of stimulants and modafinil suited me perfectly. The same for THG, which helped
put on muscle very quickly."
White tested positive for modafinil at the 2003 world championships in Paris and
was stripped of the gold medals she had won in the 100 and 200 metres. She was
later implicated in the steroid investigation into the Bay Area Laboratory
Co-Operative and was banned for two years after she admitted using banned drugs.
Her former coach, the Ukrainian-born Remi Korchemny who also trained Chambers,
is among four men facing federal charges in the Balco case.
After her positive test, White claimed she had used modafinil to treat the
sleeping disorder narcolepsy. She told Wada that was a cover story devised by
Balco's founder and owner Victor Conte and a doctor, Brian Goldman.
"I never suffered from narcolepsy," she said. "I never even knew the word
existed until a few hours after the announcement of my positive test."
White passed 17 drugs tests after starting the programme in March 2003 but
suffered physically. "My menstrual cycle was completely disturbed. I had acne
and my voice changed incredibly. And probably the worst thing was my blood
pressure shot up. It took a long time to stabilise."
Meanwhile, revelations by some of Australia's top sportsmen that they have been
using caffeine tablets to boost their performance has led Wada to threaten to
put the substance back on its banned list. Caffeine in high dosages was removed
from its list in January 2004 because there was no scientific evidence that it
helped athletes.
The Australian men's hockey team experimented with caffeine tablets during the
Olympics in Athens and after winning the gold medal for the first time reported
that their endurance had improved.
Wada issued its warning yesterday after Australia's rugby union captain George
Gregan became the latest figure to admit he had taken caffeine pills, which are
said to contain the equivalent of 12 cups of coffee. The undisputed world
super-lightweight boxing champion Kostya Tszyu, who is due to fight Manchester's
Ricky Hatton, is another Australian who has admitted experimenting with caffeine
tablets.
"The interesting thing," said Dick Pound, the chairman of Wada, "is that the
(Australian Institute of Sport) says it is performance-enhancing, has research
to back up its claims and recommends how it should be taken. Having heard this,
(we) will take another look at it."
A recent UK Sport survey revealed that 36% of sportsmen and women in the UK have
used supplements that contain caffeine. That rose to 50% among rugby league
players.
LOAD-DATE: May 19, 2005
LANGUAGE: ENGLISH
Copyright 2005 Guardian Newspapers Limited
494 of 998 DOCUMENTS
The Record (Kitchener-Waterloo, Ontario)
May 19, 2005 Thursday Final Edition
'Treated me like guinea pig'; After admitting she used banned substances,
sprinter says she was asked to try other enhancers
SOURCE: Associated Press
SECTION: SPORTS; Pg. C7
LENGTH: 453 words
DATELINE: PARIS
American sprinter Kelli White, serving a two-year suspension after admitting she
used banned substances, says she was treated like a "guinea pig" to try out
doping products.
White testified about her drug use to the World Anti-Doping Agency executive
committee in Montreal on Monday.
The French sports daily L'Equipe, which said it was the only news organization
inside the hearing, published a transcript yesterday.
White said she was asked to try out various performance-enhancing drugs,
including the designer steroid THG, endurance-boosting hormone EPO and stimulant
modafinil. She said she was never warned of potential side effects.
"I was offered a lot of things and asked to test them to see if I responded
better to certain products," she was quoted as saying.
"I was like a guinea pig. I tried a lot of stimulants and modafinil suited me
perfectly. The same for THG, which helped put on muscle very quickly."
White tested positive for modafinil at the 2003 world championships in Paris and
was stripped of her gold medals in the 100 and 200 metres.
White was later implicated in the steroid investigation into the Bay Area
Laboratory Co-Operative. She acknowledged her use of the drugs when the U.S.
Anti-Doping Agency confronted her with evidence it had gathered against her.
White was suspended for two years in 2004 and is cooperating with the U.S.
agency. Her former coach, Remi Korchemny, is among four men indicted on federal
charges in the Bay Area Laboratory case.
After testing positive at the worlds, White claimed she had used modafinil to
treat the sleeping disorder narcolepsy. She told the world agency that was a
cover story devised by Bay Area Laboratory founder Victor Conte and a doctor,
Brian Goldman.
"I never suffered from narcolepsy," she said. "I never even knew the word
existed until a few hours after the announcement of my positive test."
White's allegation about the cover story was reported in February by the San
Francisco Chronicle. Goldman, who was an associate of Conte, hasn't been charged
in the Bay Area Laboratory case. White told the world agency panel that she took
a cocktail of drugs -- including THG, EPO, a masking agent and a mix of
stimulants -- starting in March 2003 for at least four months, and said the
results were "incredible."
White said she passed 17 doping tests in 2003 before the world championships.
"The tests didn't worry me," she said. "I was calm."
But White said she suffered physical effects from the drugs.
"My menstrual cycle was completely disturbed," she said. "I had acne and my
voice changed incredibly. And probably the worst thing was my blood pressure
shot up. It took a long time to stabilize."
LOAD-DATE: May 24, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo: ASSOCIATED PRESS; Kelli White suffered many side effects from
doping products, including high blood pressure that "took a long time to
stabilize."
TYPE: NEWS
Copyright 2005 Metroland Media Group Ltd
495 of 998 DOCUMENTS
Associated Press Worldstream
May 18, 2005 Wednesday
White treated like a 'guinea pig' as she tested doping products
SECTION: SPORTS
LENGTH: 520 words
DATELINE: PARIS
American sprinter Kelli White, serving a two-year suspension after admitting she
used banned substances, says she was treated like a "guinea pig" to try out
doping products.
White testified about her drug use to the World Anti-Doping Agency executive
committee in Montreal on Monday.
The French sports daily L'Equipe, which said it was the only news organization
inside the hearing, published a transcript Wednesday.
White said she was asked to try out various performance-enhancing drugs,
including the designer steroid THG, endurance-boosting hormone EPO and stimulant
modafinil. She said she was never warned of potential side effects.
"I was offered a lot of things and asked to test them to see if I responded
better to certain products," she was quoted as saying.
"I was like a guinea pig. I tried a lot of stimulants and modafinil suited me
perfectly. The same for THG, which helped put on muscle very quickly."
White tested positive for modafinil at the 2003 world championships in Paris and
was stripped of her gold medals in the 100 and 200 meters.
White was later implicated in the steroid investigation into the Bay Area
Laboratory Co-Operative. She acknowledged her use of the drugs when the U.S.
Anti-Doping Agency confronted her with evidence it had gathered against her.
White was suspended for two years in 2004 and is cooperating with USADA. Her
former coach, Remi Korchemny, is among four men indicted on federal charges in
the BALCO case.
After testing positive at the worlds, White claimed she had used modafinil to
treat the sleeping disorder narcolepsy. She told WADA that was a cover story
devised by BALCO founder Victor Conte and a doctor, Brian Goldman.
"I never suffered from narcolepsy," she said. "I never even knew the word
existed until a few hours after the announcement of my positive test."
White's allegation about the cover story was reported in February by the San
Francisco Chronicle. Goldman, who was an associate of Conte, hasn't been charged
in the BALCO case.
White told the WADA panel that she took a cocktail of drugs - including THG,
EPO, a masking agent and a mix of stimulants - starting in March 2003 for at
least four months, and said the results were "incredible."
White said she passed 17 doping tests in 2003 before the world championships.
"The tests didn't worry me," she said. "I was calm."
But White said she suffered physical effects from the drugs.
"My menstrual cycle was completely disturbed," she said. "I had acne and my
voice changed incredibly. And probably the worst thing was my blood pressure
shot up. It took a long time to stabilize."
White said she's concerned that other athletes are still looking for an illegal
edge.
"The worst thing is that many athletes continue to talk to me about doping and
want to know how to acquire these substances," she said. "It's troubling.
"The fight against doping must be increased and the angles of attack must be
increased," White added. "Other athletes are ready to talk and a lot of things
are still going on today. Let's not forget the trainers, because they advise the
athletes."
LOAD-DATE: May 19, 2005
LANGUAGE: ENGLISH
Copyright 2005 Associated Press
All Rights Reserved
496 of 998 DOCUMENTS
Generic Line
May 18, 2005
Sandoz Drops Patent Challenge Against Cephalon's Provigil
SECTION: Vol. 22, No. 10
LENGTH: 165 words
Cephalon has dodged a patent challenge against its top-selling drug Provigil,
which was recently targeted by an abbreviated new drug application (ANDA) filed
by Sandoz.
Cephalon said May 2 that Sandoz, the generic division of Novartis
Pharmaceuticals, no longer intends to challenge Cephalon's U.S. particle-size
Provigil (modafinil) patent. Instead, Sandoz plans to convert its ANDA for
modafinil from a Paragraph IV certification to a Paragraph III certification,
Cephalon said.
The effect of this conversion is that Sandoz will certify to the FDA that it
does not intend to market a generic form of modafinil until Cephalon's patent on
the drug expires in 2014, Cephalon said. In turn, Cephalon has agreed to drop
its patent infringement lawsuit against Sandoz.
Sandoz officials were not available to comment before press time. Provigil, a
treatment for narcolepsy, was Cephalon's top-selling drug in 2004, generating
sales of $439.7 million.
Release date: May 18, 2005
LOAD-DATE: May 17, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
497 of 998 DOCUMENTS
FDAnews Drug Daily Bulletin
May 12, 2005
Cephalon's Provigil Avoids Patent Challenge From Sandoz
SECTION: Vol. 2, No. 94
LENGTH: 153 words
Cephalon has dodged a patent challenge against its top-selling drug Provigil,
which was recently targeted by an abbreviated new drug application (ANDA) filed
by Sandoz.
Cephalon said that Sandoz, the generic division of Novartis Pharmaceuticals, no
longer intends to challenge Cephalon's U.S. particle-size Provigil (modafinil)
patent. Instead, Sandoz plans to convert its ANDA for modafinil from a Paragraph
IV certification to a Paragraph III certification, Cephalon said.
The effect of this conversion is that Sandoz will certify to the FDA that it
does not intend to market a generic form of modafinil until Cephalon's patent on
the drug expires in 2014, Cephalon said. In turn, Cephalon has agreed to drop
its patent infringement lawsuit against Sandoz.
Provigil, a treatment for narcolepsy, was Cephalon's top-selling drug in 2004,
generating sales of $439.7 million.
Release date: May 12, 2005
LOAD-DATE: May 11, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
498 of 998 DOCUMENTS
World Generic Markets
Pharmaceuticals
May 10, 2005
Cephalon reports modafinil and tiagabine challenge updates
LENGTH: 237 words
Cephalon has been notified that Sandoz will no longer challenge Cephalon's US
particle-size modafinil patent; modafinil is the generic form of Cephalon's
Provigil tables. Instead, Sandoz will convert its ANDA for the drug from a
Paragraph IV certification to a Paragraph III certification; this will mean
Sandoz will not intend to market a generic version of the drug until the
applicable patent listed in the Orange Book has expired.
This will happen on 6th October 2014. Consequently, Cephalon noted it will no
longer be necessary for it to continue to pursue its patent infringement
litigation against Sandoz. Separately, Cephalon reported that the ANDA filing
for a generic version of its tiagabine hydrochloride product, Gabitril , that
was posted on the FDA's website in April does not challenge the composition of
matter patent covering the drug. Cephalon added that Gabitril is protected by
four patents listed in the Orange Book, including a composition of matter
patent. The four patents expire on 30th September 2011, 24th March 2012, 29th
April 2016 and 10th June 2017. Cephalon also noted that Sun Pharmaceutical
Industries has filed an ANDA which targets the other three patents. However,
this ANDA also does not contain a Paragraph IV certification for the composition
of matter patent. Consequently, Cephalon noted Sun is not seeking to market a
generic version of the drug until after this patent expires in 2011.
LOAD-DATE: May 11, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
499 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
May 3, 2005
Cephalon updates on patent litigation for Provigil and Gabitril
LENGTH: 278 words
Sandoz ( Novartis ) has notified Cephalon that it will no longer challenge
Cephalon's US particle-size modafinil patent. Instead, Sandoz intends to convert
its ANDA for approval of a generic equivalent of modafinil, the active
ingredient in Provigil Tablets C-IV, from a Paragraph IV certification to a
Paragraph III certification.
Provigil is indicated for the treatment of excessive sleepiness associated with
disorders of sleep and wakefulness in adults. The effect of this conversion is
that Sandoz will certify to the FDA that it does not intend to market a generic
form of modafinil until the applicable patent for the drug (listed in the Orange
Book) has expired in 2014. Therefore, it will no longer be necessary for
Cephalon to continue to pursue its patent infringement litigation against
Sandoz. Separately, Cephalon has learned that the ANDA filing against Gabitril (
tiagabine ) Tablets that was posted last month on the FDA website does not
challenge the composition of matter patent covering the currently approved
product. Gabitril is indicated as adjunctive therapy for partial seizures in
adults and children 12 years and older. The product is protected by four Orange
Book-listed patents, including a composition of matter patent claiming the
active drug substance. Cephalon recently received notification from Sun
Pharmaceutical Industries that its ANDA is targeting the three other Cephalon
patents covering Gabitril. However, the filing does not include a Paragraph IV
certification with respect to the composition of matter patent. As such, Sun is
not seeking to market a generic form of Gabitril until after the expiration of
this patent in 2011.
LOAD-DATE: May 5, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
500 of 998 DOCUMENTS
Drug Industry Daily
May 3, 2005
Sandoz Drops Patent Challenge Against Cephalon's Provigil
SECTION: Vol. 4, No. 87
LENGTH: 166 words
Cephalon has dodged a patent challenge against its top-selling drug Provigil,
which was recently targeted by an abbreviated new drug application (ANDA) filed
by Sandoz.
Cephalon said May 2 that Sandoz, the generic division of Novartis
Pharmaceuticals, no longer intends to challenge Cephalon's U.S. particle-size
Provigil (modafinil) patent. Instead, Sandoz plans to convert its ANDA for
modafinil from a Paragraph IV certification to a Paragraph III certification,
Cephalon said.
The effect of this conversion is that Sandoz will certify to the FDA that it
does not intend to market a generic form of modafinil until Cephalon's patent on
the drug expires in 2014, Cephalon said. In turn, Cephalon has agreed to drop
its patent infringement lawsuit against Sandoz.
Sandoz officials were not available to comment before press time. Provigil, a
treatment for narcolepsy, was Cephalon's top-selling drug in 2004, generating
sales of $439.7 million. -- MN
Release date: May 3, 2005
LOAD-DATE: May 2, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
501 of 998 DOCUMENTS
World Markets Analysis
May 03, 2005
Cephalon Relief as Sandoz Makes Provigil U-Turn
BYLINE: Simon King
SECTION: IN BRIEF
LENGTH: 207 words
Executives at US pharma company Cephalon have breathed a collective sigh of
relief after Swiss-based Novartis's unit Sandoz confirmed it would not be
launching a generic version of the narcolepsy drug Provigil (modafinil). Sandoz
announced that it would end its bid to challenge Cephalon's patent on Provigil
and does not intend to market a generic version of modafinil until at least
2014, when a key patent on the compound expires.
Significance: In response, Cephalon has announced that legal action against
Sandoz has been dropped. Generics-driven loss for Provigil sales would be a
major setback for Cephalon, given the recent performance of the drug (see United
States: 16 February 2005: Sleeping Disorder Drug Drives Revenue Surge for
Cephalon). The US company is not out of the woods yet, however, with three
generic versions of modafinil manufactured by Mylan, Barr (both US) and Dr
Reddy's (India) having already secured preliminary approval with the FDA (see
United States: 11 February 2005: FDA Tentatively Clears Mylan's Generic
Modafinil). The impact of Sandoz's U-turn is therefore somewhat limited,
although it does perhaps suggest that patent protection for Provigil will be
hard to overcome in the legal arena.
LOAD-DATE: May 03, 2005
LANGUAGE: ENGLISH
Copyright 2005 World Markets Research Limited;
All Rights Reserved
502 of 998 DOCUMENTS
Knobias.com
This content is provided to LexisNexis by Comtex News
Network, Inc.
May 2, 2005 Monday
CEPH: Provides Update on Patent Litigation Matters
LENGTH: 131 words
DATELINE: Ridgeland, MS
Cephalon, Inc. (CEPH) reported that Sandoz, Inc. has notified Cephalon that it
will no longer challenge Cephalon's U.S. particle-size modafinil patent.
Instead, Sandoz said it intends to convert its abbreviated new drug application
(ANDA) for approval of a generic equivalent of modafinil, the active ingredient
contained in PROVIGIL(R) Tablets [C-IV], from a paragraph IV certification to a
paragraph III certification. The effect of this conversion is that Sandoz will
certify to the FDA that it does not intend to market a generic form of modafinil
until the applicable patent for modafinil listed in the Orange Book has expired
in 2014. Therefore, it will no longer be necessary for Cephalon to continue to
pursue its patent infringement litigation against Sandoz.
LOAD-DATE: May 3, 2005
LANGUAGE: ENGLISH
Copyright 2005 Comtex News Network, Inc.
All Rights Reserved
Copyright 2005 Knobias.com, LLC, All rights reserved
503 of 998 DOCUMENTS
MarketWatch
May 2, 2005 Monday
Cephalon: Sandoz will not challenge modafinil patent
BYLINE: Heather Wilson
LENGTH: 69 words
SAN FRANCISCO (MarketWatch) -- Cephalon Inc. (ceph) said Monday that Sandoz Inc.
has notified the company that it will not challenge Cephalon's patent on
modafinil. Sandoz will convert its abbreviated new drug application for a
generic version of modafinil to a paragraph III certification, thereby ending
the patent dispute between the two companies, Cephalon said. Modafinil is the
active ingredient in Provigil.
LOAD-DATE: May 3, 2005
LANGUAGE: ENGLISH
Copyright 2005 MarketWatch.com Inc., All Rights Reserved
504 of 998 DOCUMENTS
PR Newswire US
May 2, 2005 Monday 02:10 PM GMT
Cephalon, Inc. Provides Update on Patent Litigation Matters;
Sandoz, Inc. to Drop Challenge to PROVIGIL(R) Patent; GABITRIL(R) Composition of
Matter Patent Not Targeted by Recent Filing
LENGTH: 826 words
DATELINE: FRAZER, Pa. May 2
FRAZER, Pa., May 2 /PRNewswire-FirstCall/ -- Cephalon, Inc. (NASDAQ:CEPH)
reported today that Sandoz, Inc. has notified Cephalon that it will no longer
challenge Cephalon's U.S. particle-size modafinil patent. Instead, Sandoz said
it intends to convert its abbreviated new drug application (ANDA) for approval
of a generic equivalent of modafinil, the active ingredient contained in
PROVIGIL(R) Tablets [C-IV], from a paragraph IV certification to a paragraph III
certification.
The effect of this conversion is that Sandoz will certify to the U.S. Food and
Drug Administration (FDA) that it does not intend to market a generic form of
modafinil until the applicable patent for modafinil listed in the Orange Book
has expired in 2014. Therefore, it will no longer be necessary for Cephalon to
continue to pursue its patent infringement litigation against Sandoz.
Separately, Cephalon has learned that the ANDA filing against GABITRIL(R)
(tiagabine hydrochloride) Tablets that was posted last month on the FDA website
does not challenge the composition of matter patent covering the currently
approved product. GABITRIL is protected by four Orange Book-listed patents,
including a composition of matter patent claiming the active drug substance
contained in GABITRIL.
Cephalon recently received notification from SUN Pharmaceutical Industries
Limited that its ANDA is targeting the three other Cephalon patents covering
GABITRIL. However, the filing does not include a paragraph IV certification
with respect to the composition of matter patent. As such, SUN is not seeking
to market a generic form of GABITRIL until after the expiration of this patent
in 2011.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 2,400 people in the United States and
Europe. U.S. sites include the company's headquarters in Frazer, PA, and
offices, laboratories or manufacturing facilities in West Chester, PA, Salt Lake
City, UT, and suburban Minneapolis, MN. Cephalon's major European offices are
located in Guildford, England, Martinsried, Germany, and Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL and ACTIQ(R) (oral transmucosal fentanyl citrate) [C-II] and
more than 20 products internationally. Further information about Cephalon and
full prescribing information on its U.S. products is available at
http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding Sandoz's intent to convert its ANDA filing to a
Paragraph III filing and the need to continue the patent infringement lawsuit
against Sandoz, SUN Pharmaceuticals Paragraph IV certification with respect to
three of the four GABITRIL patents and any decision by them to not seek to
market a generic form of GABITRIL prior to 2011, anticipated scientific progress
on its research programs, development of potential pharmaceutical products,
interpretation of clinical results, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission.
Given these risks and uncertainties, any or all of these forward-looking
statements may prove to be incorrect. Therefore, you should not rely on any such
factors or forward-looking statements. Furthermore, Cephalon does not intend to
update publicly any forward-looking statement, except as required by law. The
Private Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Investor Contact: Chip Merritt, +1-610-738-6376 or
cmerritt@cephalon.com , or Media Contact: Robert W. Grupp, +1-610-738-6402 or
rgrupp@cephalon.com , both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: May 3, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 PR Newswire Association LLC.
All Rights Reserved.
505 of 998 DOCUMENTS
The Pharmaceutical Journal
April 29, 2005
Modafinil fails to improve fatigue
BYLINE: Old_manager
LENGTH: 308 words
Modafinil, a drug used to treat daytime sleepiness, does not appear to improve
fatigue in patients with multiple sclerosis, a trial has revealed. Aspirin, on
the other hand, may reduce the severity of this symptom.
French researchers examined the effects of modafinil in 115 patients
with relapsing remitting or progressive MS who were also suffering from
chronic fatigue. They found that the drug was no better than placebo at
relieving self-reported fatigue symptoms. After 35 days of treatment,
both had improved mean scores on a modified fatigue impact scale (63.1±9.3
to 52.3±18.5 for modafinil vs 63.3±10 to 49.2±16.6 for placebo).
Although the researchers conclude that no benefit was detected for modafinil,
they say that an unpublished post hoc analysis did reveal an effect related
to sleepiness. "Among patients with excessive daytime sleepiness,
modafinil tended to provide more benefit than placebo on the physical
component of fatigue," they say (Neurology2005;64:1139).
In a second study (ibid, p1267), researchers observed an improvement in
patient scores during treatment with aspirin (1,300mg daily) compared
with placebo (P=0.043). Patients were treated with both aspirin and placebo
in the cross-over trial. Among the 26 patients who completed both phases,
10 (38.5 per cent) preferred aspirin whereas only one (3.9 per cent)
preferred placebo (P=0.012).
An accompanying editorial warns that the apparent benefit of aspirin and
the lack of benefit of modafinil may be related to their effects on
other MS symptoms. "It is not clear that patients adequately distinguish
effects of fatigue from motor impairment, cognitive impairment and other
symptoms," the authors argue (ibid, p1111).
LOAD-DATE: November 10, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Journal
Copyright 2005 PJ Online
All Rights Reserved
506 of 998 DOCUMENTS
Reuters Health Medical News
April 22, 2005 Friday 9:00 PM EST
Modafinil ineffective in treating MS fatigue, but aspirin might help
SECTION: CLINICAL
LENGTH: 361 words
DATELINE: NEW YORK
The narcolepsy drug modafinil (Provigil, Cephalon) does not affect fatigue
experienced by patients with multiple sclerosis (MS), results of a double-blind
controlled trial suggest. However, a separate study found that aspirin may be of
some benefit. Both studies appeared in the April 12th issue of Neurology.
In the first study, Dr. Bruno Stankoff, at Hopital de la Salpetriere in Paris
and members of the French Modafinil Study Group note that two small pilot
studies recently showed a positive impact of modafinil on MS fatigue.
To further investigate, the group randomly assigned 56 patients scoring 45 or
more on the Modified Fatigue Impact Scale (MFIS) to modafinil, maximum 400
mg/day, and 59 to placebo.
Both groups experienced decreased fatigue during the 35-day trial, but change in
scores on the MFIS, Fatigue Impact Scale, and Epworth Sleepiness Scale did not
differ significantly between groups.
In the second paper, Dr. Dean M. Wingerchuk and colleagues point out that some
MS patients using aspirin for other purposes report reduced fatigue.
In the randomized crossover trial, 30 patients with MS and fatigue took either
aspirin 650 mg twice daily or placebo for 6 weeks, separated by a 2-week washout
period.
Mean score on the MFIS was lower during aspirin treatment (38.1 versus 42.5, p =
0.043), and there was a trend toward aspirin benefit on a 10-point visual analog
scale (5.9 versus 5.4, p = 0.076). However, response did not differ
significantly on the Fatigue Severity Scale or MS-Specific Fatigue Scale.
The researchers suggest that aspirin's ability to inhibit cyclooxygenase and
block prostaglandin E2 production "could modulate hypothalamic output, thereby
affecting neuroendocrine and autonomic responses important in fatigue
perception."
Commenting on such trials in a related editorial, Drs. Steven R. Schwid of the
University of Rochester, New York and T. Jock Murray of Dalhousie University in
Halifax, Nova Scotia observe that "until we make progress in distinguishing
fatigue from other MS symptoms, in identifying its mechanisms and in measuring
it accurately, we will not make substantial progress in treating this disabling
symptom."
LOAD-DATE: March 4, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 Reuters Health
All Rights Reserved
507 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
April 19, 2005
Alfresa files for approval to manufacture modafinil in Japan
LENGTH: 111 words
Alfresa Pharma ( Alfresa Holdings ) has filed an application for approval to
manufacture modafinil for the treatment of narcolepsy with the Japanese Ministry
of Health, Labour and Welfare.
In June 1998, the company obtained an exclusive right to develop, manufacture
and market modafinil in Japan from Cephalon . Since January 2000, when modafinil
was designated as an orphan drug by the Ministry, Alfresa has conducted clinical
trials and observed positive results. The company aims to expand indications for
modafinil not only for narcolepsy, but also for childhood attention deficit
hyperactivity disorder. Currently, modafinil is approved in 33 countries
worldwide.
LOAD-DATE: April 21, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2005 ESPICOM Business Intelligence Ltd.
All Rights Reserved
508 of 998 DOCUMENTS
JCNN
April 18, 2005 Monday
Alfresa Pharma Files Manufacturing Approval for Modafinil for Narcolepsy
BYLINE: Aki Tsukioka; Staff Writer, newsroom@japancorp.net
LENGTH: 118 words
DATELINE: Tokyo, Japan
Alfresa Holdings [TSE: 2784] announced on April 15 that its wholly owned
subsidiary Alfresa Pharma has filed an application for approval to manufacture
modafinil for the treatment of to the Ministry of Health, Labor and Welfare.
In June 1998, the company obtained an exclusive right to develop, manufacture
and market modafinil in Japan from US pharmaceutical Cephalon.
Since January 2000 when modafinil was designated as an orphan drug by the
ministry, Alfresa Pharma has conducted clinical trials and seen positive
results.
The company aims to expand indications for modafinil not only for narcolepsy but
also for childhood ADHD. Currently, Modafinil is approved in 33 countries
worldwide.
LOAD-DATE: April 19, 2005
LANGUAGE: ENGLISH
Copyright 2005 Japan Corporate News Network.
All Rights Reserved.
509 of 998 DOCUMENTS
M2 Presswire
April 1, 2005
US Financial Network: Sanofi Pasteur's new polio vaccine licensed and Cephalon
files new drug application for NUVIGIL
LENGTH: 509 words
M2 PRESSWIRE-APRIL 1, 2005-US Financial Network: Sanofi Pasteur's new polio
vaccine licensed and Cephalon files new drug application for NUVIGIL ©1994-2005
M2 COMMUNICATIONS LTD
City of Industry, CA - Biotechnology industry news provided by Financial News
USA (OTC: FNWU). Sanofi Pasteur (NYSE:SNY), the vaccines business of the
sanofi-aventis group, has received a license from the Agence Francaise de
Securite Sanitaire des Produits de Sante (AFSSAPS) for a new polio vaccine,
which is the first new vaccine developed to fight that disease in decades. The
new vaccine - Monovalent Oral Polio Vaccine 1 or MOPV1 - will be used first in
Egypt as a critical part of a new World Health Organization's strategy to end
polio transmission by the end of this year. StemCells, Inc. (NASDAQ: STEM)
announced recent, positive progress towards its goal of initiating Phase I
clinical testing of its proprietary neural cell therapy product - HuCNS-SC - in
Batten disease.
Cephalon, Inc. (Nasdaq: CEPH) announced Thursday that it has filed a New Drug
Application (NDA) with the U.S. Food and Drug Administration seeking approval to
market NUVIGIL(TM) (armodafinil) Tablets [C-IV] to improve wakefulness in
patients suffering from excessive sleepiness associated with narcolepsy, shift
work sleep disorder (SWSD) and obstructive sleep apnea/hypopnea syndrome
(OSA/HS). NUVIGIL is a single-isomer formulation of modafinil, the active
pharmaceutical ingredient contained in PROVIGIL (modafinil) Tablets [C-IV]. U.S.
BioDefense (OTCBB: UBDEE) Files for Stem Cell Research Center of Excellence with
National Institutes of Health with Research Collaborators from Los Alamos, CHOC,
UCLA, and UCI and Liver Regeneration Technology from UCL Biomedica University
College London.
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LANGUAGE: ENGLISH
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Xinhua General News Service
March 19, 2005 Saturday 10:00 PM EST
CAS rejects cyclist's appeal to use banned drug
SECTION: WORLD NEWS; Sports
LENGTH: 157 words
DATELINE: GENEVA
The Court of Arbitration for Sport has refused French cyclist Franck Bouyer to
use banned drug treating his sleep disorder, the court decided Friday.
Bouyer suffers from narcolepsy which causes bouts of sudden sleep and has not
cycled competitively since last May.
But the Bouygues Telecom rider had not received clearance by the sport's world
governing body International Cycling Union (UCI) or the World Anti-Doping
Agency to use the medicine which contains Modafinil.
Bouyer then decided to take up the issue with CAS but CAS said he had not
managed to prove the use of the medicine would not improve his performance and
it was up to him to show that.
CAS added in their statement that Bouyer did have the possibility of making a
new request to the UCI to use the drug by which time more information on its
effect on sports performance might have been obtained.
Modafinil is on cycling's banned list of drugs.
LOAD-DATE: March 19, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 Xinhua News Agency
511 of 998 DOCUMENTS
Agence France Presse -- English
March 18, 2005 Friday 4:33 PM GMT
CAS refuse cyclist's request to use drug against sleep disorder
LENGTH: 165 words
DATELINE: GENEVA March 18
French cyclist Franck Bouyer, who suffers from narcolepsy where the sufferer
falls asleep suddenly, had his request to take a drug to treat it turned down by
the Court of Arbitration for Sport here on Friday.
As Bouyer had not received clearance by the sport's world governing body UCI
(International Cycling Union) or the World Anti-Doping Agency to use the
medicine which contains Modafinil, he decided to take up the issue with CAS.
However CAS said the Bouygues Telecom rider had not managed to prove the use of
the medicine would not improve his performance and it was up to him to show
that.
CAS added in their statement that Bouyer did have the possibility of making a
new request to the UCI to use the drug by which time more information on its
effect on sports performance might have been obtained.
Bouyer, who has not cycled competitively since last May, suffers from bouts of
sudden sleep and Modafinil is needed to treat it but it is on cycling's banned
list of drugs.
avz/mo/jd05
LOAD-DATE: March 19, 2005
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2005 Agence France Presse
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512 of 998 DOCUMENTS
Associated Press Worldstream
March 18, 2005 Friday
Court rejects French cyclist's appeal to use banned stimulant
SECTION: SPORTS
LENGTH: 350 words
DATELINE: LAUSANNE, Switzerland
The Court of Arbitration for Sport turned down French cyclist Franck Bouyer's
request to be allowed the therapeutic use of banned stimulant modafinil.
The court backed the International Cycling Union and the World Anti-Doping
Agency, who had already denied Bouyer's request.
Bouyer, who has not raced since the end of May 2004, wanted to be allowed
modafinil to alleviate a condition that causes sudden faintness and
uncontrollable drowsiness. He said it can occur when he is riding.
He turned to the court after his case was rejected by the other bodies.
The case was handed to a panel of three experts and the hearing held March 4 in
Lausanne, with Bouyer, his council, and representatives from the UCI and WADA
attending.
The court noted that, according to WADA and UCI rules, one of the conditions in
awarding permission to use a banned substance for therapeutic use is that it
does not enhance performance outside that of the athlete returning to normal
health following treatment of a proven pathological condition.
The jury concluded that Bouyer had failed to prove that modafinil would not
enhance his performance.
The panel told Bouyer that he could renew his request to UCI for special
dispensation if he came up with any new evidence.
Witness testimony said it was difficult to regulate modafinil dosage to prevent
performance enhancement, and that there is no reliable method to do so.
U.S. sprinter Kelli White, who won two gold medals at the world championships in
2003, tested positive for the drug later the same year.
She claimed she took the prescription stimulant because she suffered from
narcolepsy, but later admitted to taking illegal performance-enhancing drugs
after the USADA confronted her with evidence that she used undetectable
steroids.
She was banned for two years - missing the Athens Olympics - and was stripped of
every medal she'd won the past four years.
The United States was also stripped of its 1,600-meter relay gold medal from the
2003 worlds after Calvin Harrison was found guilty of using modafinil at the
June 2003 U.S. championships.
LOAD-DATE: March 19, 2005
LANGUAGE: ENGLISH
Copyright 2005 Associated Press
All Rights Reserved
513 of 998 DOCUMENTS
Scotland on Sunday
February 27, 2005, Sunday
MOD'S SECRET PEP PILL TO KEEP FORCES AWAKE
BYLINE: Brian Brady Westminster Editor
SECTION: Pg. 13
LENGTH: 712 words
SOLDIERS and aircrews will be dosed up with "pep pills" to help them stay alert
for longer under controversial plans being developed by the Ministry of Defence,
confidential papers have revealed.
A secret MoD report obtained by Scotland on Sunday has laid bare the project to
test whether the drug modafinil could be used to reduce the amount of sleep
needed by servicemen and women on active duty.
The covert supply of stimulants to fighting forces has become a controversial
subject in recent years, particularly after it emerged that two United States
F-16 pilots - Major Harry Schmidt and Major William Umbach - who killed four
Canadians in a "friendly fire" incident in Afghanistan in April 2003, had taken
an amphetamine issued by their superiors.
Defence chiefs have spent more than GBP 50,000 on modafinil allegedly to treat
conditions including the sleep disorder narcolepsy.
However, the secret report, obtained by Scotland on Sunday under the Freedom of
Information Act, shows that the MoD has ploughed hundreds of thousands of pounds
into researching whether they should follow the lead of forces including the
French Foreign Legion and start using the drug to keep military personnel
vigilant for up to 60 hours at a time.
A GBP 300,000 investigation completed last year has effectively given the green
light to start using the drug, marketed as 'Provigil', after it found a single
dose helped people stay alert for more than 18 hours with limited side -effects.
Following problems with the amphetamine Dexedrine, attention has switched to
modafinil, which has vastly improved alertness in patients with narcolepsy,
shift-work sleep disorder and sleep apnoea, and with few apparent side -effects.
But it has already been banned as a performance-enhancing drug by athletics
governing bodies, and been implicated in the BALCO doping scandal in which Kelli
White is one of a number of top US athletes accused of using modafinil to propel
her to championship-winning performances.
The report into stimulant drugs, presented to MoD chiefs by the Defence
Evaluation Research Agency (Dera) six years ago, said the Canadians and the
French had found that "during a period of 64 hours' continuous work, modafinil
improved performance in a manner similar to amphetamine, and led to fewer side
-effects".
However, later studies warned that the drug could lead to "over-confidence",
cause motion-sickness, vertigo and dizziness in air-crews, and therefore the
Americans preferred to stick to amphetamine-based stimulants.
Nevertheless, the MoD agreed to spend almost GBP 300,000 on research into the
use of "hypnotics and stimulants", including modafinil. Key documents relating
to the lengthy research programme explicitly state that its purpose was to test
the drug for use in combat situations. One of the reports focusing on air
operations, compiled by the defence agency QinetiQ, states:
"In recent years there has been much interest in the stimulant modafinil, which
is reported to have beneficial effects on performance during prolonged periods
of wakefulness extending from 24 to 60 hours."
The findings, presented to the MoD last summer and delivered to a high-level
conference in the autumn, suggest that the side-effects can be manageable as
long as the dose is restricted. Defence chiefs and ministers are now discussing
whether to issue the drug on a routine basis to service personnel on operational
duty.
When it emerged last summer that the department had bought 24,000 Provigil pills
since 1998, with a particularly large order delivered before the campaign in
Iraq, the MoD maintained that the drug was purely for medical purposes.
MoD surgeon-general, Vice Admiral Ian Jenkins, said: "The MoD does not use
Provigil for performance-enhancing purposes or to alleviate the effects of sleep
deprivation on operations or in training.
"Provigil may only be prescribed by medical officers within the Defence Medical
Services for legitimate clinical reasons, in the same manner as it would be used
by the NHS."
An MoD spokeswoman insisted that the armed forces did not issue stimulants to
servicemen and women. She said: "Our current policy is that we don't provide
stimulants."
LOAD-DATE: February 28, 2005
LANGUAGE: ENGLISH
PUB-TYPE: PAPER
Copyright 2005 The Scotsman Publications Ltd.
514 of 998 DOCUMENTS
Generic Line
February 23, 2005
Briefs
SECTION: Vol. 22, No. 4
LENGTH: 639 words
FDA Approves Mylan's Generic Celexa
The FDA has granted final approval for Mylan Laboratories' abbreviated new drug
application for citalopram hydrobromide tablets, the generic version of Forest
Laboratories' antidepressant Celexa. The product will be available in 10-, 20-
and 40-mg doses.
Sanofi-Aventis to Market Eloxatin
The FDA has granted marketing approval to sanofi-aventis' aqueous solution
formulation of its colorectal cancer drug Eloxatin. Eloxatin injection is
expected to be more convenient for doctors and nurses than the original
Eloxatin, as it takes fewer steps to administer, sanofi-aventis said. Eloxatin
in combination with infusional 5-FU/LV has been approved in the U.S. for
treatment of advanced carcinoma of the colon or rectum since January 9, 2004.
Eloxatin first received European approval in France for second-line treatment of
metastatic colorectal cancer in April 1996.
Tentative Approval for Mylan's Modafinil
The FDA had granted tentative approval to Mylan Laboratories' abbreviated new
drug application for 100- and 200-mg modafinil tablets. Modafinil tablets are
the generic version of Cephalon's Provigil tablets, indicated to treat excessive
tiredness associated with sleep disorders resulting from narcolepsy, shift work
sleep disorder or obstructive sleep apnea/hypopnea syndrome. The agency issued
Mylan tentative approval for its product because Provigil is covered by patents
that do not expire until 2007 and 2014. Cephalon said it expects Provigil sales
of up to $450 million in 2004 and up to $600 million in 2005.
FDA Approves Chewable Amoxicillin
The FDA has granted final approval to Teva Pharmaceutical's abbreviated new drug
application for amoxicillin/clavulante potassium chewable tablets USP in 200
mg/28.5 mg and 400 mg/57 mg doses. The company is expecting to ship the product,
which is the generic equivalent of GlaxoSmithKline's antibiotic Augmentin
chewable tablets, immediately. Augmentin is used to treat bacterial infections
of the ears, lungs, sinuses, skin and urinary tract. Total annual brand and
generic sales of the product are approximately $21 million.
Teva Moving Ahead on Levofloxacin
Teva Pharmaceutical has received tentative approval from the FDA for its
abbreviated new drug application for levofloxacin injection 5 mg/mL in 250
mg/bag and 500 mg/bag doses and levofloxacin injection 25 mg/mL in 20 mL and 30
mL vials. Levofloxacin injection is the generic equivalent of Ortho McNeil's
antibacterial agent Levaquin. Final approval for the product will depend on
resolution of ongoing patent litigation, Teva said. Total annual sales of the
brand product are approximately $220 million.
Dr. Reddy's Starts Ireland Trial
Indian drugmaker Dr. Reddy's has initiated a Phase I clinical trial in Belfast,
Ireland, to test its cardiovascular drug candidate, RUS 3108, in humans. The
company is developing the drug to treat atherosclerosis, a major cause of heart
attacks and strokes. Currently there is no treatment on the market to directly
treat this disorder. The drug uses a protein called perlecan to affect multiple
pathways involved in the disease such as inflammation, proliferation and
thrombosis. The study marks the first time Dr. Reddy's has conducted a trial in
Europe.
Spectrum Challenging Imitrex Patent
Spectrum Pharmaceuticals is challenging GlaxoSmithKline's (GSK) patent on
Imitrex injection 6mg/0.5mL. Spectrum said it believes GSK' s patent on Imitrex
(sumatriptan succinate), which is set to expire Feb. 6, 2009, is invalid.
Spectrum submitted an abbreviated new drug application containing a Paragraph IV
certification for a generic Imitrex injection product with the FDA in October
2004, and received notification of acceptance with Paragraph IV certification in
January 2005.
Release date: Feb. 23, 2005
LOAD-DATE: February 22, 2005
LANGUAGE: ENGLISH
Copyright 2005 Washington Business Information, Inc., All Rights Reserved
515 of 998 DOCUMENTS
The San Francisco Chronicle
FEBRUARY 21, 2005, MONDAY, FINAL EDITION
Sprinters say doctor helped get their drugs;
Bay Area psychiatrist says he did sporadic consulting for Conte
SOURCE: Chronicle Staff Writer
BYLINE: Seth Rosenfeld
SECTION: NEWS; Pg. A1
LENGTH: 1522 words
Two champion athletes who have admitted obtaining illegal steroids from BALCO,
the Bay Area firm at the center of the nation's largest sports-doping case, have
claimed a local doctor played a role in their use of banned
performance-enhancing substances.
In an interview with The Chronicle, world class sprinter Kelli White said Dr.
Brian Goldman publicly stated he had diagnosed her with a sleeping disorder in
an effort to justify her use of a banned stimulant that he made available to
her. White said that she had no sleeping disorder, and that Goldman's statements
were part of a false story devised by BALCO head Victor Conte.
In sworn testimony, world champion sprinter Tim Montgomery said Goldman wrote a
prescription for him under a false name so it would not be traceable.
Both athletes said they had never met Goldman at the time.
During several telephone conversations with The Chronicle, Goldman declined to
discuss White. He denied Montgomery's account. "There's just no story here,"
said Goldman. "I don't have anything to hide at all."
Goldman, 50, was an associate of Conte, who ran the Bay Area Laboratory
Co-Operative, or BALCO. Conte and three other men were indicted in U.S. District
Court in San Francisco on steroid conspiracy charges. They have pleaded not
guilty.
Goldman, a psychiatrist, has not been charged. He has said he was medical
director of BALCO in 1984, when the firm focused on holistic health, but since
then has done only on-and-off consulting with Conte.
Goldman specializes in treating adults and children with autistic-spectrum
disorders and other behavioral problems. He works at the Amen Clinic in
Fairfield and at Diablo Behavioral Healthcare center in Danville, where clinical
director William Shryer called him a "top-flight" doctor.
The U.S. attorney's office declined to comment on Goldman in regard to the BALCO
case. Robert Holley, Conte's lawyer, also declined to comment.
The case of Kelli White, the Union City sprinter, began to unfold in August
2003, when she tested positive for modafinil after winning gold medals in the
100- and 200-meter sprints during the World Track and Field Championships in
Paris.
At a news conference the night her test result became public, she said she took
the drug for a sleeping disorder called narcolepsy.
"I have never taken any substance to enhance my performance," she said on Aug.
30, 2003. "Close members of my family have been under doctor's care for the
condition of narcolepsy for years. I, too, have been diagnosed with this
condition by my physician, Dr. Brian Goldman. He prescribed the drug Provigil
(which contains modafinil) for this condition ...."
In a "To whom it may concern" letter dated the same day, Goldman said White "has
been consulting with our clinic since the beginning of the year.
"Kelli has had excessive daytime somnolence, particularly in the afternoon and
worsening toward the late afternoon and evening. Kelli has complained of falling
asleep while talking on the telephone ... .
"Per my instruction, Kelli was provided with one or two sample bottles of
modafinil (Provigil), by my staff," Goldman said in the letter. "I have
recommended that her nutritional regime include the prescription medication,
modafinil (Provigil) ...."
He said he did not believe modafinil had been banned in her sport.
The same day, Goldman told the Washington Post that he gave her two sample
bottles of the drug after diagnosing her as suffering from narcolepsy during a
consultation in the Bay Area.
In a Sept. 3, 2003, letter to the International Association of Athletics
Federations, the governing body for world track and field, Goldman said:
"Modafinil was prescribed for her and I believe was taken by her in the spirit
of allowing her to feel as normal as the other athletes, who do not have a sleep
disorder, to level the playing field, and not to seek any untoward advantage."
Goldman later gave copies of his letters to The Chronicle, and told the
newspaper that Conte had referred White to him because he is a "local narcolepsy
expert."
But White's story about narcolepsy began to unravel.
In late 2003, she testified before the federal grand jury investigating BALCO,
and some of the evidence from that case was turned over to the U.S. Anti-Doping
Agency. She then admitted to USADA officials that she did not have narcolepsy
and had taken modafinil and other banned drugs to gain a competitive advantage.
USADA in May 2004 suspended White from competition for two years. She received
the minimum punishment after acknowledging her mistakes and agreeing to help
USADA fight doping.
In a December interview with several reporters, which USADA helped arrange,
White took responsibility for her doping and said she deeply regretted cheating.
White confirmed that she did not have a sleeping disorder and admitted that
modafinil helped her compete.
In response to questions from a Chronicle reporter, White said Goldman's
statements were part of a story concocted by Conte.
According to White, within hours of testing positive for modafinil in Paris, she
phoned Conte, who told her to issue the false statement saying she took the drug
for narcolepsy. "It sounded good. It was a story that Victor (Conte) told me to
use," she said.
Soon after that, she said, Goldman called and helped make up the story for the
press conference.
"I was contacted by Dr. Goldman, and that's how the story came about," she said.
"And that was my first time ever meeting, or speaking, to Dr. Goldman."
But though White said Goldman helped her with the cover story, she added that
she was unsure how much he knew about her situation.
"I'm not sure exactly what Victor told Dr. Goldman," she said. "But I don't
think he fully knew what was going on... I think he was really oblivious. I
don't think he knew."
White's New Jersey lawyer, Jerrold Colton, who was present at the interview,
emphasized that White took responsibility for her drug use, and commented about
Goldman in response to reporters' questions.
Contacted last month, Goldman declined to comment on White's account and his
prior statements about her. He referred The Chronicle to a former assistant who
said White had been seen by Goldman at the Amen Clinic, but could not recall
whether it was before or after she tested positive for modafinil.
Montgomery, who holds the world record for the 100-meter sprint, testified about
Goldman during his Nov. 6, 2003, appearance before the grand jury investigating
BALCO.
The sprinter said that Conte had given him a steroid called "the clear," and
that Goldman wrote him a prescription under a false name for Clomid, which
helped boost testosterone production.
Assistant U.S. Attorney Jeff Nedrow later asked: "Who was the person he (Conte)
got to get prescriptions -- what did Mr. Conte tell you about that?"
Montgomery: "Dr. Goldman."
Nedrow asked: "To your knowledge, did Dr. Goldman actually legitimately consult
with athletes in developing treatments for them for diseases and stuff like
that?"
Montgomery said that "Dr. Goldman was a guy that he (Conte) would talk to on the
telephone and (Conte would) tell him what was going on with the athlete. And he
(Goldman) would -- he would give a suggestion on what they should do, what they
should not do. And if it was a prescription that needed to be written out, he
would make it out."
Montgomery said he knew of these activities because in March 2001 he visited
Conte at BALCO and Conte "told me how the whole operation was running."
Montgomery said he was present when Conte spoke with Goldman on the phone. "Yes,
I was. That's how I got the Clomid."
In a June 25, 2004, interview, Goldman disputed Montgomery's testimony.
"Everything is a lie," he told The Chronicle. "I don't think I've ever
prescribed Clomid. The fact is, I've never spoken to him, never spoken to anyone
about him, have nothing to do with his treatment, and I would not OK any
non-physician to write prescriptions."
Montgomery's lawyers declined to comment.
In October 2003, Prentice Steffen, a San Francisco physician and bicycle racing
coach, asked the California Medical Board to examine Goldman's conduct after
reading news reports that he had been medical director of BALCO.
The board told Steffen in a letter that it had closed the case on Jan. 9, 2004,
for lack of evidence.
"The Medical Board of California ... has concluded its review of your complaint
alleging that Dr. Goldman is involved in the BALCO doping case," the letter
said. "It was determined that the board does not have sufficient evidence to
proceed."
In a separate inquiry, the state Department of Health Services last month
decided not to fine Goldman for BALCO's alleged violations of laboratory
regulations.
The department agreed with Goldman's assertion that his name had been forged on
records listing him as medical director of BALCO between 1989 and 2003.
Chronicle staff writers Gwen Knapp, Mark Fainaru-Wada and Lance Williams
contributed to this report.E-mail Seth Rosenfeld at srosenfeld@sfchronicle.com.
LOAD-DATE: February 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: PHOTO (3), (1) Sprinters Kelli White (left) / Paul Sakuma / Associated
Press 2003, (2) and Tim Montgomery say Dr. Brian Goldman helped them obtain
performance-enhancing substances. White says Goldman provided her with
modafinil, while Montgomery says Goldman wrote a prescription for a drug that
boosts testosterone. / Michel Euler / Associated Press 2002, (3)Victor Conte
Copyright 2005 The Chronicle Publishing Co.
516 of 998 DOCUMENTS
World Markets Analysis
February 11, 2005
FDA Tentatively Clears Mylan's Generic Modafinil
BYLINE: Henry Dummett
SECTION: IN BRIEF
LENGTH: 185 words
The US FDA has granted tentative approval for a generic version of modafinil in
100mg and 200mg tablet form, submitted by US drug-maker Mylan Pharmaceuticals.
Modafinil is marketed by Cephalon (US), under the Provigil brand, and is used to
treat narcolepsy; it is the only FDA approved drug for excessive sleepiness
associated with obstructive sleep apnea/hypopnea syndrome and shift-work sleep
disorder. The efficacy of Cephalon against attention deficit hyperactivity
disorder (ADHD) is currently being assessed..
Significance: The onset of generic competition would cause greater damage to
Cephalon's top line than it would benefit the marketer of a generic version.
Provigil is one of only three products marketed by Cephalon, and is a major
growth-driver for the company. During the first nine months of 2004, the drug
garnered US$276.1m on the US market, an year-on-year increase of 48%. Mylan will
find itself in a competitive market when formal FDA approval is issued, with
Barr (US) and Ranbaxy (India) having already secured preliminary FDA clearance
for generic versions of the drug.
LOAD-DATE: February 11, 2005
LANGUAGE: ENGLISH
Copyright 2005 World Markets Research Limited;
All Rights Reserved
517 of 998 DOCUMENTS
MarketWatch
February 10, 2005 Thursday
CORRECT: Mylan modafinil tablets get tentative FDA OK
BYLINE: Heather Wilson
LENGTH: 71 words
SAN FRANCISCO (MarketWatch) -- Mylan Laboratories (myl) said Thursday that its
modafinil tablets have received tentative approval from the U.S. Food and Drug
Administration. Modafinil is used to treat sleep disorders such as narcolepsy
and sleep apnea/hypopnea syndrome. The Pittsburgh-based pharmaceutical company
said the drug is a generic version of Cephalon's (ceph) Provigil. (Corrects
spelling of Cephalon and Provigil.)
LOAD-DATE: February 11, 2005
LANGUAGE: ENGLISH
Copyright 2005 MarketWatch.com Inc., All Rights Reserved
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PR Newswire US
February 10, 2005 Thursday
Mylan Receives Tentative Approval for Modafinil Tablets
LENGTH: 153 words
DATELINE: PITTSBURGH Feb. 10
PITTSBURGH, Feb. 10 /PRNewswire-FirstCall/ -- Mylan Laboratories Inc.
(NYSE:MYL) today announced that the U.S. Food and Drug Administration has
granted tentative approval for Mylan Pharmaceuticals Inc.'s Abbreviated New Drug
Application for Modafinil Tablets, 100 mg and 200 mg.
Modafinil Tablets are the generic version of Cephalon Inc.'s Provigil(R)
Tablets.
Mylan Laboratories Inc. is a leading pharmaceutical company with four
subsidiaries, Mylan Pharmaceuticals Inc., Mylan Technologies Inc., UDL
Laboratories Inc. and Mylan Bertek Pharmaceuticals Inc., that develop, license,
manufacture, market and distribute an extensive line of generic and proprietary
products.
For more information about Mylan, visit http://www.mylan.com/ .
CONTACT: Media, Heather Bresch, +1-724-514-1800, or Investors, Kris
King, +1-724-514-1800, both of Mylan Laboratories Inc.
Web site: http://www.mylan.com/
SOURCE Mylan Laboratories Inc.
URL: http://www.prnewswire.com
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Clinical Psychiatry News
February 2005
Modafinil Still Effective for Sleep Apnea After 17 Weeks of Therapy
BYLINE: Nicholas Mulcahy, Contributing Writer
SECTION: Pg. 60 Vol. 33 No. 2 ISSN: 0270-6644
LENGTH: 440 words
PHILADELPHIA - Modafinil in patients with obstructive sleep apnea and
excessive daytime sleepiness despite positive airway pressure therapy was
effective in improving wakefulness for at least 17 weeks in a small study
presented at the annual meeting of the Associated Professional Sleep Societies.
Previous studies of the wakefulness drug and obstructive sleep apnea (OSA)
had been limited to 12 weeks, Juan Moralejo, M.D., reported.
"In our study population, modafinil was more likely to be effective in the
elderly and those with high Epworth Sleepiness Scale scores at the time of
diagnosis" of daytime sleepiness, said Dr. Moralejo, a pulmonary medicine fellow
at Graduate Hospital, Philadelphia.
The study sample consisted of 22 patients (13 males and 9 females), mean age
53.9 years. Of the 18 patients receiving "conventional treatment," 9 were using
continuous positive airway pressure, 8 were using bilevel positive airway
pressure, and 1 was using a dental device. At the time of the survey, four
patients were not using any conventional treatment for OSA.
The mean Epworth Sleepiness Scale score was 15.9 at diagnosis, 13.6 after
treatment with conventional modalities, and 8.9 after treatment with modafinil
(Provigil). A lower Epworth score is indicative of improved wakefulness, and
reduction of 4 points is considered a response to treatment. No statistical
difference was found between the Epworth scores before and after conventional
treatment, but the change after modafinil treatment was significant, Dr.
Moralejo said.
The improvement in Epworth Sleepiness Scale score was similar whether
patients were on modafinil for more than or less than 12 weeks. The average
duration of treatment was 17 weeks (range 1-40).
On univariate analysis, factors associated with response to modafinil were
higher Epworth Sleepiness Scale score at diagnosis, higher Epworth score while
on conventional therapy, and male gender, said Dr. Moralejo, who has no
affiliation with Cephalon, maker of Provigil. But on multivariate analysis, a
high Epworth score at diagnosis of OSA and increasing age correlated best with
response to modafinil.
The average dosage of modafinil was 227.3 mg once daily (range 100-800). No
significant side effects were documented.
Epworth Sleepiness Scale scores at the diagnosis of OSA and after treatment
with conventional modalities were obtained from the patients' records. A
telephone survey was conducted and included questions about patients'
demographics, modafinil treatment, and type of ongoing conventional treatment
for OSA as well as patient compliance with this treatment.
LOAD-DATE: July 31, 2009
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520 of 998 DOCUMENTS
Pharma Company Insight
Pharmaceuticals
January 19, 2005
Orphan Medical submits Xyrem sNDA
LENGTH: 703 words
Orphan Medical has submitted an sNDA to the FDA for Xyrem ( sodium oxybate )
oral solution. Xyrem is currently marketed as the only approved treatment for
cataplexy, a sudden loss of muscle tone that is a debilitating symptom of
narcolepsy. The sNDA is expected to expand the product's label to encompass
improvement in the other primary symptoms of narcolepsy, specifically the
reduction of excessive daytime sleepiness (EDS) and the improvement in
fragmented night-time sleep. There is no medication currently approved to treat
all of the primary symptoms of narcolepsy. EDS has been treated with stimulant
medications and disrupted night-time sleep by sedative-hypnotic medications. The
sNDA includes two Phase IIIb trials with EDS as the primary efficacy measure, as
well as positive data relating to the treatment of other components of
narcolepsy. The FDA user fee (PDUFA) deadline is ten months from the date the
FDA receives the sNDA submission. The first Phase IIIb trial, SXB-15, generated
strong positive data across both primary and secondary endpoints. The trial
evaluated improvement in the EDS of patients with narcolepsy when a dose of 4.5,
6.0 or 9.0g of Xyrem was added to unchanged stimulant therapy. The trial results
demonstrated dose-related improvement in the Epworth Sleepiness Scale (ESS)
scores, statistically significant at the 6 and 9g daily doses. At the 9g dose,
Xyrem produced statistically significant improvement in the Maintenance of
Wakefulness Test (MWT), an established objective measure of EDS. Treatment of
sleep continuity and structure was significantly improved at the 6 and 9g doses,
with reductions in subjectively and objectively measured awakenings after sleep
onset, and a marked increase in delta sleep, thought to be the restorative
period of sleep.
Daytime functionality was assessed using the validated Functional Outcome of
Sleep Questionnaire (FOSQ). The FOSQ outcomes demonstrated dose-related
improvements in four of the five factorial assessments, as well as significant
improvement in the global score at the 6 and 9g dose levels. This double-blind,
placebo-controlled, randomised trial assessed 228 patients over an eight-week
treatment period in 40 sleep centres in North America and eight in Europe. The
second trial, EXCEEDS (Evaluation of Xyrem to Check Efficacy in Excessive
Daytime Sleepiness), was designed to evaluate the improvement of EDS associated
with narcolepsy when Xyrem is used alone or with Cephalon 's Provigil (
modafinil ), a wakefulness-promoting agent approved for the treatment of EDS.
The primary endpoint of the trial was EDS as measured by the objective MWT. The
secondary endpoint also measured EDS using the ESS. The trial demonstrated that
Xyrem monotherapy is effective in the treatment of EDS associated with
narcolepsy using both measures. The combined use of Xyrem and modafinil showed a
greater response than either agent alone. EXCEEDS was a double-blind,
double-dummy, placebo-controlled, parallel-group, multi-centre randomised study.
In both trials, the safety profile is consistent with that of previous Xyrem
trials and commercial use. The most commonly-reported dose-related adverse
events (AEs) occurring in more than 5 per cent of patients across all controlled
trials were nausea, dizziness, headache, vomiting, somnolence and enuresis. No
significant new or unexpected AEs were seen in the SXB-15 trial. Occurring
infrequently, but more often at the 9g dose, were disorientation, sleepwalking
and enuresis. These side effects occurred at reduced rates in the expanded
safety dataset of the sNDA. The safety profile of Xyrem in the EXCEEDS trial was
consistent with other previous controlled clinical trials. The side effect of
nausea occurred more often for groups receiving Xyrem and both Xyrem and
modafinil together, as did vomiting which had a markedly lower incidence.
Headache was a common symptom in the EXCEEDS trial, including placebo, but
dizziness and tremor were more common in the group on both drugs, as was
anxiety. The incidence of sleep walking and enuresis, previously reported as
associated with Xyrem, showed a very low incidence in this study that was not
significantly different between groups.
LOAD-DATE: January 19, 2005
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PUBLICATION-TYPE: Newsletter
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521 of 998 DOCUMENTS
The Independent (London)
January 18, 2005, Tuesday
HEALTH: MESSING WITH OUR MINDS;
WANT TO IMPROVE YOUR MENTAL ABILITY, BOOST CONCENTRATION AND EVEN
BYLINE: JEREMY LAURANCE
SECTION: First Edition; FEATURES; Pg. 8
LENGTH: 1481 words
HIGHLIGHT:
Science fiction or future fact? Jim Carrey erases unhappy memories in Eternal
Sunshine of the Spotless Mind'
To err is human. But for the pilot of a commercial airliner, it is unacceptable.
As holidaymakers jet off on winter breaks or plan next summer's long-haul
adventure, the one thing that they will demand above all is safety. Airlines
have spent millions devising elaborate systems to guarantee maximum safety.
Pilot error can never be ruled out, but researchers now believe that it might be
reduced - by careful tweaking of brain chemistry. Drugs are becoming available
that increase alertness and improve concentration. Should all pilots take them?
This question has begun to tax scientists in the US involved in the development
of so-called "smart" drugs - chemical enhancements for the mind. A range of
compounds are being tested - some are already available and being traded over
the internet - that may change not only the way we perform, but what we think of
as "normal" performance.
The drugs being examined have applications far beyond air travel. Three areas
that are attracting attention are movement and endurance, attention and
learning, and moods. Medicines such as anabolic steroids can already make people
stronger, swifter and more enduring. Though life-giving to victims of muscle
disorders, they are widely abused in sport. Long- distance lorry drivers and Air
Force pilots have used amphetamines to ward off drowsiness. Generations of
students have sustained themselves through exams with over-the-counter caffeine
tablets. But the new "cognitive enhancers" may offer more powerful, better
targeted and longer lasting improvements in mental acuity. And some are already
being tested on human volunteers.
One such drug is donepezil, a cholinesterase inhibitor developed for the
treatment of dementia. This drug slows the progress of Alzheimer's disease and
is being used as a treatment for age-associated memory impairment. But what is
causing excitement among researchers is the possibility that donepezil may boost
highly skilled performance, where concentration and alertness are prerequisites.
A study published in the journal Neurology found that commercial pilots who took
5mg of donepezil for one month performed better than pilots on a placebo when
asked to fly a Cessna 172 on a flight simulator. There was a marked difference
between the groups when dealing with emergencies.
Modafinil, a drug used to treat the sleep disorder narcolepsy, has also been
tested on pilots. A trial reported in the Psychopharmacology journal found that
it boosted the performance of helicopter pilots flying on simulators who had
been deprived of sleep.
Anyone who has gone two nights without sleep will know what it is like to suffer
from extreme tiredness. Nothing can defeat the desire to sleep. Nothing except,
apparently, modafinil. While commercial pilots have strict rules governing
flying time and rest periods, fighter pilots may be called to action at a
moment's notice. Modafinil is under investigation by the military for its
ability to keep pilots and other members of the armed forces awake for long
periods without the "rebound" effect associated with stimulants such as
amphetamines.
Barbara Sahakian, Professor of Neuropsychology at the University of Cambridge,
who tested modafinil in a series of experiments on volunteers found that they
showed greater concentration, faster learning and increased mental agility. "It
may be the first real smart drug," she says. "A lot of people will probably take
modafinil. I suspect they do already."
"If people can gain a millimetre, they'll want to take it," says Jerome
Yesavage, director of Stanford University's Ageing Clinical Research Center, and
an author of the donepezil study. That view was backed by Judy Illes, a
psychologist at Stanford's Centre for Biomedical Ethics. Mind-enhancing medicine
could become as "ordinary as a cup of coffee", she says.
If drugs such as donepezil and modafinil were proved to raise performance, and
hence safety, the implications could be far-reaching. Airline executives might
require pilots to take the drugs, or offer financial incentives for doing so.
They might market their airline as the one whose pilots took the
safety-enhancing drug. Would people pay more to fly on such an airline?
The question is raised in a review of the new science, dubbed "cosmetic
neurology", by Dr Anjan Chatterjee, a neurologist at the University of
Pennsylvania. As the rich turn to cosmetic surgery to refine what nature gave
them, cosmetic neurology offers a different kind of personal improvement. It is
the "nip and tuck" for the mind. The conventional aids of caffeine, alcohol and
tobacco are already used to boost mood and performance, and neurologists argue
that the use of other drugs is a logical extension of this self-medication.
Writing in Annals of Neurology, Dr Chatterjee says that amphetamine drugs that
help stroke patients who have suffered partial paralysis to relearn motor skills
might assist healthy individuals to learn to swim or play the piano. A new class
of drugs called ampakines are being investigated as memory enhancers, and have
already been shown to boost recall in early studies in humans.
Trials of the heart drug propranolol, a beta-blocker, have shown that it can
neutralise emotionally charged memories so that they do not cause distress when
recalled. In one experiment, reported in Biological Psychiatry, patients injured
in accidents were given propranolol in the A&E department and were found to
suffer fewer post-traumatic stress disorder symptoms when assessed one month
later.
The new science is creating problems for neurologists, who are used to treating
the sick, not enhancing the healthy. Dr Chatterjee writes: "One plausible
scenario is that neurologists will become quality-of-life consultants. Following
the model of financial consultants, we could offer a menu of options with the
likely outcomes and risks." The advent of cosmetic neurology is inevitable, he
says, and warns: "Prospecting for better brains may be the new gold rush."
Signs that it has already arrived can be seen on college campuses in the US.
Faced with the pressure of exams and essay deadlines, students have been
abandoning the traditional crutches of coffee and cigarettes for Ritalin, a
stimulant best known as a treatment for hyperactive children. It has found a
ready black market among students who are desperate to succeed. Users say that
it helps them to concentrate.
Anecdotal reports from drug agencies in Britain suggest that the problem is just
emerging here. It has already spread to Canada and Australia, and university
authorities have been warned to be vigilant. The search for a short cut in
learning has worried teachers. But doctors have confirmed the potential benefits
of the drugs, unwittingly encouraging the trend. For example, Eric
Heiligenstein, the director of clinical psychiatry at Wisconsin University,
says: "Caffeine is fine. This Ritalin is better. Students are able to accumulate
more information in a shorter time. They minimise fatigue and help maintain a
high performance level." A study of 2,200 students at an unnamed university in
North America, published in Pharmacotherapy last year, found that 66 of them (3
per cent) admitted abusing Ritalin in the previous year. "Illicit use of
prescription-only stimulants on college campuses is a potentially serious public
health issue," it said.
If "natural" performance or responses can be boosted in these areas, it may
challenge our concept of what it is to be human. In one view, medicine should be
about healing the sick, not turning people into gods. But the boundary between
therapy and enhancement can be hard to define. Short people can be treated with
growth hormone - but is that cosmetic or therapeutic? In an ageing society,
treatments to boost attention, learning and memory will be increasingly relevant
- but should they be applied to people who are healthy but merely old?
In the field of athletics, drug use is rife but it is referred to disparagingly
as "doping". The underlying assumption is that boosting performance without
doing the work is cheating and undermines human endeavour. Yet no one feels the
same way about putting up with a headache or indigestion. We reach for tablets
without hesitation. The ethical dilemma may prove to be academic, however, if
the drugs now being tested fail to deliver on performance, or their side-effects
prove to be troublesome.
A memory drug might cause subjects to remember too much detail, cluttering the
mind, for example. Martha Farah, a psychologist at the University of
Pennsylvania, says: "The brain was designed by evolution over millennia to be
well adapted because of the lives we lead. We are better served by being able to
focus on the essential information than being able to remember every little
detail. We meddle with these designs at our peril."
LOAD-DATE: January 18, 2005
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522 of 998 DOCUMENTS
Philadelphia Inquirer
January 12, 2005, Wednesday
Drug may help addicts kick cocaine
BYLINE: By Stacey Burling
SECTION: DOMESTIC NEWS
LENGTH: 654 words
PHILADELPHIA _ After decades of failed attempts to find a drug that helps
addicts kick cocaine, researchers at the University of Pennsylvania say they
have finally found a medication that looks promising _ a drug currently approved
to treat sleepiness.
Addicts who took modafinil _ used to treat narcolepsy and help pilots and
night-shift workers stay alert _ were about twice as likely to avoid cocaine in
a given week as those who received a placebo pill, according to a small Penn
study published this month in the Journal of Neuropsychopharmacology.
Patients taking the medicine, marketed as Provigil, were also nearly three times
as likely as unmedicated counterparts to stay off cocaine for a three-week
stretch _ 33 percent vs. 13 percent, said Charles Dackis, chief of psychiatry at
Penn's Medical Center-Presbyterian and lead investigator of the 62-patient
study.
The National Institute on Drug Abuse funded the Penn study and is paying for
three longer, larger studies as well.
The institute is also funding similar studies of three other medicines:
baclofen, which is used to treat spastic disorders; topiramate, an
anti-convulsant; and disulfiram or Antabuse. Ultimately, the medicines may be
targeted at specific subgroups within the nation's 1.5 million cocaine users,
said Frank Vocci, director of the division of pharmacotherapies and medical
consequences of drug abuse.
Modafinil, he said, has qualities that could "propel it to the top." Addicts
don't mind its side effects and like its "alerting effect." It may also reduce
impulsiveness, a key factor in addiction.
Given the high percentage of addicts in the study who still used cocaine, the
drug clearly is not a cure for cocaine addiction, which is notoriously difficult
to treat. But it may be an important, early step toward better drug therapies,
said Robert Malcolm, a Medical University of South Carolina psychiatrist who
heads another of the modafinil studies. "Is this drug a home run?" he asked.
"No. Maybe it's a single or at best a double."
Nonetheless, he and Dackis said modafinil is the most promising drug they have
seen for cocaine addiction in 20 years.
Dackis said researchers had tried as many as a 100 drugs against cocaine during
that time with no success.
Modafinil, made by Cephalon Inc. of West Chester, Pa., earned $300 million in
2003 and has projected sales of $410 million for 2004. The company is awaiting
word on its request to market the drug for attention deficit hyperactivity
disorder.
Dackis believes that modafinil helps restore function to the brain's pleasure
center, which is thrown chemically off balance by long-term cocaine use. Addicts
often say they don't "feel right" without cocaine. "You're craving something
that will make you feel better," he said.
Modafinil, he added, "does promote a sense of well being but not euphoria and
certainly not the rush of euphoria you experience with cocaine." One of his
previous studies showed that the drug blunted the cocaine euphoria. The
government lists modafinil as having mild potential for abuse. Dackis said he
saw no evidence that modafanil is addictive.
A middle-aged man who participated in the Penn study believes the drug helped
him go 14 weeks without cocaine, an unusually long time for him during 15 years
of addiction.
"I had more energy to stay focused on things I had to do on my job, things I had
to do at home, at church," he said. "I didn't have time to sneak off into North
Philly and get lost."
The man, a professional with a college degree who asked that his name not be
used, said he stopped taking the medicine when the study ended. He used cocaine
again last week. Now, he has asked his primary-care doctor to prescribe
modafinil for him. He also plans to go back into therapy. "I guess I need that
crutch," he said.
___
Visit Philadelphia Online, the Inquirer's World Wide Web site, at
http://www.philly.com/
LOAD-DATE: January 12, 2005
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Knight Ridder/Tribune News Service
Copyright 2005 The Philadelphia Inquirer
523 of 998 DOCUMENTS
UPI
January 12, 2005 Wednesday 12:01 AM EST
Drug shows promise for cocaine addiction
LENGTH: 188 words
DATELINE: PHILADELPHIA, Jan. 12
U.S. researchers said a medication used to treat the sleep disorder narcolepsy
also has shown promise for treating cocaine addiction.
Cocaine addicts who were given the drug, known as Modafinil, were more likely to
abstain from using cocaine than addicts who received an inactive placebo, said
researchers from the University of Pennsylvania Medical Center, who reported the
finding in the January issue of Journal of Neuropsychopharmacology.
If the finding is confirmed, Modafinil could become the first medication for
treating cocaine addiction, they said. Cocaine addiction affects thousands of
people around the globe and can disrupt the lives of not only addicts but also
their loved ones.
In the study, researchers treated 30 cocaine addicts with Modafinil and gave 32
others a placebo for eight weeks. The Modafinil-treated addicts were more likely
to go for long periods without using cocaine, as confirmed by cocaine-negative
urine samples.
The researchers also noted Modafinil did not appear to cause any serious side
effects and none of the addicts dropped out of the study due to adverse
reactions to the medication.
LOAD-DATE: January 12, 2005
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PUBLICATION-TYPE: Newswire
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524 of 998 DOCUMENTS
The Philadelphia Inquirer
JANUARY 11, 2005 Tuesday CITY-D EDITION
Drug offers cocaine addicts hope;
Modafinil boosts alertness and may curb impulsiveness, a Penn study shows.
BYLINE: Stacey Burling INQUIRER STAFF WRITER
SECTION: NATIONAL; Pg. A04
LENGTH: 651 words
After decades of failed attempts to find a drug that helps addicts kick cocaine,
researchers at the University of Pennsylvania say they have finally found a
medication that looks promising - a drug currently approved to treat sleepiness.
Addicts who took modafinil - used to treat narcolepsy and help pilots and
night-shift workers stay alert - were about twice as likely to avoid cocaine in
a given week as those who received a placebo pill, according to a small Penn
study published this month in the Journal of Neuropsychopharmacology.
Patients taking the medicine, marketed as Provigil, were also nearly three times
as likely as unmedicated counterparts to stay off cocaine for a three-week
stretch - 33 percent vs. 13 percent, said Charles Dackis, chief of psychiatry at
Penn's Medical Center-Presbyterian and lead investigator of the 62-patient
study.
The National Institute on Drug Abuse funded the Penn study and is paying for
three longer, larger studies as well.
The institute is also funding similar studies of three other medicines:
baclofen, which is used to treat spastic disorders; topiramate, an
anti-convulsant; and disulfiram or Antabuse. Ultimately, the medicines may be
targeted at specific subgroups within the nation's 1.5 million cocaine users,
said Frank Vocci, director of the division of pharmacotherapies and medical
consequences of drug abuse.
Modafinil, he said, has qualities that could "propel it to the top." Addicts
don't mind its side effects and like its "alerting effect." It may also reduce
impulsiveness, a key factor in addiction.
Given the high percentage of addicts in the study who still used cocaine, the
drug clearly is not a cure for cocaine addiction, which is notoriously difficult
to treat. But it may be an important, early step toward better drug therapies,
said Robert Malcolm, a Medical University of South Carolina psychiatrist who
heads another of the modafinil studies. "Is this drug a home run?" he asked.
"No. Maybe it's a single or at best a double."
Nonetheless, he and Dackis said modafinil is the most promising drug they have
seen for cocaine addiction in 20 years.
Dackis said researchers had tried as many as a 100 drugs against cocaine during
that time with no success.
Modafinil, made by Cephalon Inc. of West Chester, earned $300 million in 2003
and has projected sales of $410 million for 2004. The company is awaiting word
on its request to market the drug for attention deficit hyperactivity disorder.
Dackis believes that modafinil helps restore function to the brain's pleasure
center, which is thrown chemically off balance by long-term cocaine use. Addicts
often say they don't "feel right" without cocaine. "You're craving something
that will make you feel better," he said.
Modafinil, he added, "does promote a sense of well being but not euphoria and
certainly not the rush of euphoria you experience with cocaine." One of his
previous studies showed that the drug blunted the cocaine euphoria. The
government lists modafinil as having mild potential for abuse. Dackis said he
saw no evidence that modafanil is addictive.
A middle-aged man who participated in the Penn study believes the drug helped
him go 14 weeks without cocaine, an unusually long time for him during 15 years
of addiction.
"I had more energy to stay focused on things I had to do on my job, things I had
to do at home, at church," he said. "I didn't have time to sneak off into North
Philly and get lost."
The man, a professional with a college degree who asked that his name not be
used, said he stopped taking the medicine when the study ended. He used cocaine
again last week. Now, he has asked his primary-care doctor to prescribe
modafinil for him. He also plans to go back into therapy. "I guess I need that
crutch," he said.
Contact staff writer Stacey Burling at 215-854-4944 or sburling@phillynews.com.
LOAD-DATE: September 6, 2005
LANGUAGE: ENGLISH
Copyright 2005 Philadelphia Newspapers, LLC
All Rights Reserved
525 of 998 DOCUMENTS
Clinical Psychiatry News
January 2005
Modafinil Dose Higher in Narcolepsy Than Apnea
BYLINE: Nicholas Mulcahy, Contributing Writer
SECTION: Pg. 65 Vol. 33 No. 1 ISSN: 0270-6644
LENGTH: 617 words
PHILADELPHIA - The median dose of modafinil was 300 mg for patients with
obstructive sleep apnea and 400 mg for patients with narcolepsy in long-term
open-label extensions of placebo-controlled trials, , Jonathan Schwartz, M.D.,
said at the annual meeting of the Associated Professional Sleep Societies.
The labeling for modafinil (Provigil) calls for a dosage of 200 mg/day to
improve wakefulness in patients with excessive sleepiness associated with either
condition.
"Modafinil dosing was flexible-between 200 and 400 mg/day-based on the
investigators' impressions of clinical efficacy and tolerability [during the
open-label extensions]. The dose was slightly higher in patients with
narcolepsy, which may be attributable to the underlying differences in severity
of excessive sleepiness between the two conditions," said Dr. Schwartz, a
pulmonologist in Oklahoma City.
The open-label extensions involved two double-blind, placebo-controlled
trials of modafinil in patients with narcolepsy and one in patients with nasal
continuous positive airway pressure (nCPAP)-treated obstructive sleep apnea
(OSA).
In the narcolepsy studies, 84% of 478 patients were titrated to a modafinil
dose greater than 200 mg, with 50% at 400 mg, 34% at 300 mg, and 16% at 200 mg.
In the OSA study, 76% of the 266 patients were titrated to a modafinil dose
greater than 200 mg, with 43% at 300 mg, 33% at 400 mg, and 24% at 200 mg.
Modafinil was well tolerated in both populations at all doses, Dr. Schwartz
said. Adverse events were similar in the two patient populations.
Treatment duration was 40 weeks for both narcolepsy studies and 12 months for
the OSA study.
Baseline excessive sleepiness was assessed by mean score on the Epworth
Sleepiness Scale (ESS); the score was significantly higher in the narcolepsy
patients than in the OSA population (17.4 vs. 14.5, respectively; P< .001).
"Narcolepsy and obstructive sleep apnea are both frequently associated with
excessive sleepiness, but patients with narcolepsy are usually sleepier than
nCPAP-treated patients with OSA," said Dr. Schwartz.
In OSA, modafinil is indicated as an adjunct to standard treatments for the
underlying obstruction in patients who continue to experience residual excessive
sleepiness, despite treatment of the underlying obstruction, he added.
At least 20% of OSA patients are still sleepy despite nCPAP therapy, he said.
The mean change in ESS scores from baseline to final clinic visit in the
study populations was virtually identical-about 4.25 points-for the narcolepsy
and OSA patients, said Dr. Schwartz. In other words, there was a similar
efficacy (mean reduction in sleepiness), despite the difference in the mean
dose.
The mean body mass index was significantly lower in the narcolepsy group
(28.8 kg/m2) than in the OSA patients (36.2 kg/m2). Despite having significantly
lower body mass indexes than OSA patients, patients with narcolepsy were
titrated to higher modafinil doses to achieve clinical improvement, Dr. Schwartz
observed.
The mean age for the narcolepsy patients was 42 years; the OSA patients' mean
age was 50 years. Of the narcolepsy patients, 46% were male, as were 77% of the
OSA patients.
Overall, 84% of patients in the studies completed the specified treatment
period, but completion rates were higher in the 40-week narcolepsy studies (95%)
than in the single 12-month OSA study (66%).
Clinic visits for both narcolepsy studies were scheduled at baseline and
after 1, 2, 6, 8, 16, 24, and 40 weeks.
Clinic visits for the OSA study were scheduled at baseline and at 3, 6, 9,
and 12 months.
The study was funded by Cephalon Inc., the maker of modafinil.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
JOURNAL-CODE: CPNEWS
Copyright 2005 Elsevier Inc., International Medical News Group
All Rights Reserved
526 of 998 DOCUMENTS
Clinical Neurology News
January 2005
Narcolepsy Requires Higher Modafinil Dose
BYLINE: Nicholas Mulcahy, Contributing Writer
SECTION: Pg. 24 Vol. 1 No. 1 ISSN: 1553-3212
LENGTH: 637 words
PHILADELPHIA - The median therapeutic dose of modafinil was 300 mg for
patients with obstructive sleep apnea and 400 mg for patients with narcolepsy in
long-term open-label extensions of placebo-controlled trials, Dr. , Jonathan
Schwartz said at the annual meeting of the Associated Professional Sleep
Societies.
The labeling for modafinil (Provigil) calls for a dosage of 200 mg/day to
improve wakefulness in patients with excessive sleepiness associated with either
condition. "Modafinil dosing was flexible-between 200 and 400 mg/day-based on
the investigators' impressions of clinical efficacy and tolerability [during the
open-label extensions]. The dose was slightly higher in patients with
narcolepsy, which may be attributable to the underlying differences in severity
of excessive sleepiness between the two conditions," said Dr. Schwartz, a
pulmonologist in Oklahoma City.
The open-label extensions involved two double-blind, placebo-controlled
trials of modafinil in patients with narcolepsy and one in patients with nasal
continuous positive airway pressure (nCPAP)-treated obstructive sleep apnea
(OSA).
In the narcolepsy studies, 84% of 478 patients were titrated to a modafinil
dose greater than 200 mg, with 50% at 400 mg, 34% at 300 mg, and 16% at 200 mg.
In the OSA study, 76% of the 266 patients were titrated to a modafinil dose
greater than 200 mg, with 43% at 300 mg, 33% at 400 mg, and 24% at 200 mg.
Modafinil was well tolerated in both populations at all doses, Dr. Schwartz
said. Adverse events were similar in the two patient populations. Treatment
duration was 40 weeks for both narcolepsy studies and 12 months for the OSA
study.
Baseline excessive sleepiness was assessed by mean score on the Epworth
Sleepiness Scale (ESS); the score was significantly higher in the narcolepsy
patients than in the OSA population (17.4 vs. 14.5, respectively; P < .001).
"Narcolepsy and obstructive sleep apnea are both frequently associated with
excessive sleepiness, but patients with narcolepsy are usually sleepier than
nCPAP-treated patients with OSA," said Dr. Schwartz.
In OSA, modafinil is indicated as an adjunct to standard treatments for the
underlying obstruction in patients who continue to experience residual excessive
sleepiness, despite treatment of the underlying obstruction, he added.
At least 20% of OSA patients are still sleepy despite nCPAP therapy, he said.
The mean change in ESS scores from baseline to final clinic visit in the
study populations was virtually identical-about 4.25 points-for the narcolepsy
and OSA patients, said Dr. Schwartz. In other words, there was a similar
efficacy (mean reduction in sleepiness), despite the difference in the mean
dose.
The mean body mass index was significantly lower in the narcolepsy group
(28.8 kg/m2) than in the OSA patients (36.2 kg/m2). Despite having significantly
lower body mass index than OSA patients, patients with narcolepsy were titrated
to higher modafinil doses to achieve clinical improvement, Dr. Schwartz
observed.
The mean age for the narcolepsy patients was 42 years; the OSA patients' mean
age was 50 years. Of the narcolepsy patients, 46% were male, as were 77% of the
OSA patients.
Overall, 84% of patients in the studies completed the specified treatment
period, but completion rates were higher in the 40-week narcolepsy studies (95%)
than in the single 12-month OSA study (66%).
Clinic visits for both narcolepsy studies were scheduled at baseline and
after 1, 2, 6, 8, 16, 24, and 40 weeks.
Clinic visits for the OSA study were scheduled at baseline and at 3, 6, 9,
and 12 months.
The study included patients who withdrew after two evaluations if their
withdrawal was not due to adverse events.
The study was funded by Cephalon Inc., the maker of modafinil.
LOAD-DATE: July 31, 2009
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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527 of 998 DOCUMENTS
PR Newswire US
December 21, 2004 Tuesday
Cephalon Files Application for Marketing Approval of New Modafinil Formulation
for the Treatment of Children and Adolescents with
Attention-Deficit/Hyperactivity Disorder;
Accelerated Submission Date Based on Highly Significant Results From Three
Studies of New Once-Daily Doses
LENGTH: 1284 words
DATELINE: WEST CHESTER, Pa. Dec. 21
WEST CHESTER, Pa., Dec. 21 /PRNewswire-FirstCall/ -- Cephalon, Inc.
(NASDAQ:CEPH) today announced that it has filed a supplemental new drug
application (sNDA) with the U.S. Food and Drug Administration (FDA) requesting
marketing approval of ATTENACE(TM) (modafinil) Tablets [C-IV], a new proprietary
dosage form of modafinil for the treatment of attention- deficit/hyperactivity
disorder (ADHD) in children and adolescents between the ages of six and 17.
In August 2004, Cephalon announced results from three multi-center clinical
trials that showed that ATTENACE 340 mg and 425 mg tablets significantly improve
symptoms of ADHD in children and adolescents. Based upon the strength of the
study results, the company accelerated the filing of its application with the
FDA from the first quarter of 2005 to the fourth quarter of 2004. The company is
targeting a launch of ATTENACE by early 2006.
"Physicians and parents continue to seek treatment for children and adolescents
with ADHD that provides a balanced efficacy and tolerability profile. In our
phase 3 trials, we were encouraged that ATTENACE improved the symptoms of many
children and adolescents with ADHD to levels within the range considered normal
for those without ADHD, as measured by the ADHD rating scales used in our
studies. There was a low discontinuation rate due to adverse events in these
studies as well," said Paul Blake, MB, FRCP, Senior Vice President of Clinical
Research and Regulatory Affairs.
"The consistency of the effectiveness of ATTENACE to treat the full range of
ADHD symptoms uniformly across the three studies allows us to present what we
believe is a strong submission package to FDA," Dr. Blake added.
Frank Baldino Jr., Ph.D., Chairman and CEO, said, "We are enthusiastic about the
data from our clinical trials and the potential for ATTENACE, once approved, to
capture a substantial portion of the ADHD market. We expect that ATTENACE will
provide another exceptional growth opportunity for Cephalon."
About the Clinical Trials
In three nine-week, double-blind, placebo-controlled studies, more than 600
children and adolescents between the ages of six and 17 with ADHD were
randomized to either placebo or ATTENACE. The primary endpoint in all studies
was the teacher-completed school version of the ADHD Rating Scale IV. All of
the ATTENACE-treated groups showed a highly statistically significant
improvement on the ADHD rating scale compared to placebo (p<0.0001). ATTENACE
was generally well tolerated, with a safety profile consistent with that
observed in other studies of modafinil. The most common adverse events observed
in the phase 3 trials with children and adolescents with ADHD included mild
transient insomnia, headache and loss of appetite. The complete Phase 3 study
data are expected to be presented at major medical meetings in 2005.
ATTENACE
Data from earlier clinical trials in children and adolescents with ADHD led to
the development of ATTENACE as small, film-coated tablets in unique dosage
strengths. The new tablets will be available in 85 mg, 170 mg, 255 mg, 340 mg,
and 425 mg strengths and will allow for tailored dosing with a single tablet for
children and adolescents with ADHD. The active ingredient in ATTENACE, modafinil
, is currently available as PROVIGIL(R) (modafinil) Tablets [C-IV] in 100 mg and
200 mg strengths. PROVIGIL is indicated for the treatment of excessive
sleepiness associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome
(OSAHS) and shift work sleep disorder. The most frequently reported adverse
events in clinical trials with PROVIGIL were headache, nausea, nervousness,
stuffy nose, diarrhea, back pain, anxiety, trouble sleeping, dizziness and upset
stomach.
Attention-Deficit/Hyperactivity Disorder
According to the National Institutes of Mental Health, ADHD is one of the most
common psychiatric disorders among children, affecting three to five percent of
American children. The most common ADHD behaviors fall into three categories:
inattention, hyperactivity, and impulsivity. A diagnosis of ADHD is generally
made when these behaviors become excessive, long-term, and pervasive. Studies
have shown that children with ADHD have higher medical costs than children
without ADHD due to the risk of accidents and injury resulting from inattention,
impulsivity and hyperactivity.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 2,100 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah,
and suburban Minneapolis, Minnesota. Cephalon's European offices are located in
Guildford, England, Martinsried, Germany, and Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) [C-II] and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, including the results of the three multi-center clinical
trials of ATTENACE, prospects for regulatory approval of ATTENACE, including the
strength of the Company's submission package to FDA and the anticipated
timetable for the launch of the product, manufacturing development and
capabilities, market prospects for its products, particularly with respect to
the potential for the Company to capture a substantial portion of the ADHD
marketplace with ATTENACE and the growth opportunity provided by the product,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward- looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
CONTACT: Media: Jenifer Antonacci, +1-610-738-6674,
jantonac@cephalon.com ; or Investors: Robert (Chip) Merritt, +1-610-738-6376,
cmerritt@cephalon.com , both of Cephalon
Web site: http://www.cephalon.com/
Company News On-Call: http://www.prnewswire.com/comp/134563.html
SOURCE Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: December 22, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association LLC.
All Rights Reserved.
528 of 998 DOCUMENTS
The San Francisco Chronicle
DECEMBER 11, 2004, SATURDAY, FINAL EDITION
Collins slapped with 8-year ban;
Sprinter, 33, faces end of her career
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. D1
LENGTH: 834 words
If Michelle Collins were a Major League Baseball player, she would have received
a slap on the wrist for using banned performance-enhancing drugs.
Instead, she's a track and field athlete. She was clobbered by the iron fist of
her sport's anti-doping organization.
Collins, a sprinter from Raleigh, N.C., became the first athlete from the BALCO
investigation to be suspended based on non-analytical evidence, meaning a lack
of a positive drug test, when the U.S. Anti-Doping Agency on Friday banned her
from competition for eight years.
Collins is the 13th track and field athlete with BALCO ties to receive sanctions
for doping offenses.
USADA has also charged sprinters Chryste Gaines and Tim Montgomery with doping
offenses based on non-analytical evidence. Their arbitration hearings are
scheduled for next year.
At 33, the suspension is tantamount to a lifetime ban for Collins, once a
training partner of Marion Jones. She has one avenue of appeal left, should she
decide to take it, with the international Court of Arbitration for Sport.
"I've never heard of anyone getting eight years," said Collins' attorney, Brian
Getz of San Francisco. "We are disappointed with the (decision) and are studying
it as we consider our options."
A three-person panel of the American Arbitration Association/North American CAS
ruled that "USADA has proved, beyond a reasonable doubt, that Collins took EPO,
the testosterone/epitestosterone cream, and THG."
The panel, comprised of two lawyers and a judge, concluded that because Collins
used a variety of illegal drugs for several years and attempted to cover up her
doping through substances designed to avoid detection in urine tests, her ban
should be double what other BALCO athletes received.
"I think they (the panelists) said she never admitted to her guilt, didn't agree
to cooperate and because of that it amounted to a cover-up," said Travis Tygart,
legal counsel for USADA. "(It) will keep her out of coaching until she's 41."
Sprinter Alvin Harrison admitted to using a variety of illegal drugs and was
banned for four years. Middle-distance runner Regina Jacobs tested positive for
THG ("the clear") and received four years. Neither athlete agreed to cooperate
with USADA's investigation, thus the four years.
Sprinter Kelli White, conversely, admitted to using a regimen of banned drugs
from BALCO, agreed to cooperate with investigators and was given a two-year
sanction.
White, in fact, was one of four witnesses called by USADA to provide testimony
in Collins' hearing, which was held Nov. 17-18 in San Francisco, based on her
involvement with BALCO and subsequent admission of guilt to doping charges.
"Kelli White, when she was first confronted with the evidence, denied
everything," Getz said. "She's doing it to benefit herself because she wants to
race again."
The other witnesses were Dr. Larry Bowers, USADA's managing director; Dr.
Michael Sawka, an expert on blood doping; and Dr. Richard Clark, a pharmacology
expert with the company GlaxoSmithKline.
Sawka examined several of Collins' blood tests and concluded her elevated red
blood cell levels could only be the result of the endurance-boosting agent EPO.
Even when fortified by transfusions of their own red blood cells, U.S. military
personnel training at high altitude did not have as high a percentage as
Collins, Sawka testified.
Clark testified that Collins' extreme fluctuations in testosterone levels could
be explained by her use of BALCO's testosterone cream -- which she admitted to
in e-mail exchanges with Conte.
All of Collins' competitive results since Feb. 1, 2002, are nullified as a
result of the ban. Her biggest accomplishments were winning U.S. and World
Indoor championships at 200 meters in 2003. Allyson Felix is thus the U.S.
indoor champ for 2003 while Muriel Hurtis of France claims the retroactive World
Indoor title for that year.
------------------------------------------------------
The BALCO bunch
Here are the track and field athletes affiliated with BALCO who have received
sanctions for doping offenses, with their events, suspensions and the substances
they were penalized for using:
Dwain Chambers* (100) -- Life (THG); Michelle Collins (200, 400) -- 8 years
(EPO, THG, testosterone cream); Alvin Harrison (400) -- 4 years (EPO, THG,
testosterone cream, insulin, modafinil); Regina Jacobs (1,500) -- 4 years (THG)
Calvin Harrison (400) -- 2 years (modafinil); John McEwen (hammer) -- 2 years
(THG, modafinil); Melissa Price (hammer) -- 2 years (THG); Kevin Toth (shot put)
-- 2 years (THG); Kelli White (100, 200) -- 2 years (EPO, THG, modafinil)
All received public warnings for use of modafinil: Chryste Gaines (100, 200);
Sandra Glover (400 hurdles); Chris Phillips (110 hurdles); Eric Thomas (400
hurdles)
Note: Further doping cases pending -- Gaines, Tim Montgomery
*British citizen. Banned for life from Olympics by his federationE-mail John
Crumpacker at jcrumpacker@sfchronicle.com.
LOAD-DATE: December 11, 2004
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, Michelle Collins never tested positive for banned substances. /
Thomas Kienzle / Associated Press
TYPE: RELATED STORY ATTACHED
Copyright 2004 The Chronicle Publishing Co.
529 of 998 DOCUMENTS
Pittsburgh Post-Gazette (Pennsylvania)
November 29, 2004 Monday
SOONER EDITION
U.S. STRIPPED OF GOLD MEDAL
BYLINE: From local and wire dispatches
SECTION: SPORTS; MORNING BRIEFING; Pg. E-7
LENGTH: 616 words
The United States was stripped of its 1,600-meter relay gold medal from the 2003
world championships because of Calvin Harrison's second doping violation.
The gold instead goes to France, with Jamaica getting the silver and the Bahamas
the bronze, the world governing body of track and field said.
Harrison was found guilty of using the stimulant modafinil at the U.S.
championships in June 2003. He had contended that modafinil wasn't specifically
mentioned on the official list of banned substances at the time.
Ten years earlier, Harrison tested positive for the stimulant pseudoephedrine
during the 1993 U.S. junior indoor championships and served a three-month ban.
More running
Gunder Hagg, who set the mile world record in 1945 and held it until Roger
Bannister broke the four-minute barrier, died at 85 after a long illness.
Hagg died Saturday at a nursing home and spent his last years in a wheelchair,
sports writer and friend Ulf R. Johansson said.
Hagg broke 15 world marks in middle distance running and set no less than 10
world marks during three months in 1942. That year, the Swede also was the first
to run 5,000 meters in under 14 minutes.
He is survived by wife, Daisy, and son Gunder Hagg, Jr.
Tennis
This week's U.S.-Spain Davis Cup final in Seville, Spain, is expected to break
the attendance record for a sanctioned tennis match.
The temporary clay court set up in Seville's Olympic Stadium has been configured
to seat 26,600. The existing mark was set in 1954 in Sydney, Australia, when
25,578 watched the United States defeat Australia in the Davis Cup final.
Volleyball
The Penn State women's team has been selected to the NCAA tournament field for
the 24th year in a row. The fourth-ranked and second-seeded Lions (27-2) will
face American University (24-6) Friday in the first round. Pitt (21-10) also
made the 64-team field and will take on Ohio (28-2) Friday in Columbus.
Skiing
Bode Miller became the first man to open a World Cup season with three victories
in three disciplines, winning a super-giant slalom in Lake Louise, Alberta,
ahead of Hermann Maier.
Miller's first career Super G win came one day after his first World Cup
downhill victory. He also won the season-opening giant slalom in Soelden,
Austria, and is just the fourth skier to win World Cup races in all five
disciplines in his career (slalom and combined are the others).
* Finland's Tanja Poutiainen won for the second time in three races at Aspen
Mountain, beating Italy's Manuela Moelgg by more than a second in a World Cup
slalom in Aspen, Colo. American Kristina Koznick was third.
* Finland's Janne Ahonen won his second consecutive World Cup ski jump on a
large hill before his home fans in Kuusamo. Austria's Thomas Morgenstern was
second and the Czech Republic's Jakub Janda third.
Swimming
South Africa's Ryk Neethling and Australia's Libby Lenton each won a fifth event
at a World Cup short-course swim meet in Melbourne, Australia.
Lenton took the 200 freestyle in 1 minute, 56.98 seconds to edge countrywoman
Shayne Reese. Lenton won the 50- and 100-meter freestyle and 50 and 100
butterfly events on the opening two nights.
Neethling added the 50-meter freestyle to the 100 and 200 freestyle, 50
butterfly and 100 individual medley.
Neethling and Lenton shared swimmer of the meet honors.
Speed skating
Apolo Anton Ohno won two races and teamed with Hyo-Jung Kim to give the United
States a sweep in the 1,000-meter event at the World Cup short-track tournament
in Madison, Wis.
Ohno won the 1,000 meters in 1:26.914 then captured the 3,000-meter event in
5:13.504. Ohno increased his World Cup medal count this season to 13. He also
took gold in the 1,500 meters and silver in the 500 meters this weekend.
LOAD-DATE: October 20, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 P.G. Publishing Co.
530 of 998 DOCUMENTS
Edmonton Journal (Alberta)
October 20, 2004 Wednesday
Final Edition
U.S. runner accepts ban for steroid use: Alvin Harrison was BALCO client
BYLINE: San Jose Mercury News
SECTION: SPORTS; Pg. D5
LENGTH: 369 words
DATELINE: SAN JOSE, Calif.
SAN JOSE, Calif. - In another victory for the U.S. Anti-Doping Agency's effort
to clean up track and field, Olympic runner Alvin Harrison accepted a four-year
suspension Tuesday for drug violations stemming from the BALCO Laboratories
case.
Harrison, 30, became the second athlete connected to BALCO to admit to using
performance-enhancing drugs after being presented with evidence from the
criminal case. Sprinter Kelli White accepted a two-year ban in May.
"It was time for him to speak out," said Harrison's lawyer, Robert Harris of
Durham, N.C.
Harrison, who won gold medals as part of the 1996 and 2000 U.S. 1,600-metre
relay teams, could not be reached. He and his twin, Calvin Harrison, denied in
July that they took illegal drugs. The brothers railed against the anti-doping
agency for trying to ban Alvin without a positive test.
Calvin Harrison is serving a two-year suspension after testing positive for
modafinil, his second flunked drug screen.
Alvin Harrison admitted to using THG, testosterone cream, insulin,
erythropoietin (EPO), the human growth hormone and modafinil -- the catalogue of
drugs connected to BALCO. Harrison's admission came because he wants to move on,
his lawyer said.
Harris said the 400-metre runner took the drugs only after the 2000 Olympics and
that his accomplishments should not be diminished because of it.
"He wants to show how this is being done and even forced on athletes," Harris
said, adding that the runner might write a book as well as try to play
professional football.
The anti-doping agency used evidence based in large part on material subpoenaed
by the Senate Commerce Committee and then handed to drug testers.
Travis Tygart, USADA's legal director, said Harrison's admission validated the
anti-doping agency's pursuit of athletes based on BALCO evidence, which included
calendars of drug schedules. Three cases based on similar evidence -- involving
Tim Montgomery, Chryste Gaines and Michelle Collins -- are scheduled before the
Court of Arbitration for Sport next month in San Francisco.
Alvin Harrison and his Sydney relay teammates face the possibility of losing
their gold medals because runner Jerome Young tested positive for steroids a
year before the 2000 Games.
LOAD-DATE: October 20, 2004
LANGUAGE: ENGLISH
DOCUMENT-TYPE: Sports
PUBLICATION-TYPE: Newspaper
Copyright 2004 CanWest Interactive, a division of CanWest Global Communications
Corp.
All Rights Reserved
531 of 998 DOCUMENTS
Reuters Health Medical News
October 15, 2004 Friday 9:00 PM EST
Modafinil added to SSRIs alleviates sedation
SECTION: CLINICAL
LENGTH: 280 words
DATELINE: NEW YORK
Excessive sleepiness and fatigue related to therapy with serotonergic
antidepressants can be alleviated with adjunctive use of modafinil, according to
a report in the September issue of the Journal of Clinical Psychiatry.
Dr. Thomas L. Schwartz and colleagues at the New York Upstate Medical University
in Syracuse, New York enrolled 20 adults in a 3-week, open label study to
determine the effect of modafinil, given once daily, on sedation related to
serotonergic drugs. All patients had major depressive disorder, but all reported
that sedation, fatigue, and low energy had developed only after they began to
take selective serotonin reuptake inhibitors.
In the 16 patients who completed the study, the addition of modafinil
"significantly improved overall depressive symptoms, as shown by reductions in
mean Hamilton Rating Scale for Depression total scores," the researchers report.
Also, the investigators found, modafinil therapy was associated with improved
subjective impressions of wakefulness and reduced fatigue.
By their final study visit, the study participants had improvements in their
overall health status and health-related quality of life, as shown by their
significantly improved mean total scores on the Medical Outcomes Study
Short-Form 12-Item Health Survey, and by improved physical health and mental
health subscores.
"Generalization of these findings is limited by the open-label nature of [the
study], exclusion of a control group, and selective entry criteria for study
participants," the investigators admit. Still, they conclude, "These positive
findings, as well as the effects of adjunctive modafinil on responder rates,
warrant further systematic study."
LOAD-DATE: March 4, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2004 Reuters Health
All Rights Reserved
532 of 998 DOCUMENTS
Business Wire
September 14, 2004 Tuesday
Orphan Medical Announces Positive Xyrem Clinical Results in Second Excessive
Daytime Sleepiness Trial -- Trial Supports Use of Xyrem as Monotherapy for
Narcolepsy
LENGTH: 1159 words
DATELINE: MINNEAPOLIS, Sept. 14, 2004
BODY: Orphan Medical, Inc. (Nasdaq:ORPH) announced positive results from a Phase
III (b) trial designed to evaluate the improvement of excessive daytime
sleepiness (EDS) associated with narcolepsy when Xyrem(R) (sodium oxybate) oral
solution is used alone or with modafinil (Provigil(R)), a wakefulness promoting
agent approved for the treatment of EDS. The primary endpoint of the trial was
EDS as measured by the objective Maintenance of Wakefulness Test (MWT). The
secondary endpoint also measured EDS using the Epworth Sleepiness Score. The
trial demonstrated that Xyrem monotherapy is effective in the treatment of EDS
associated with narcolepsy as measured by objective response in the MWT. The
combined use of Xyrem and modafinil showed a greater response than either agent
alone. EXCEEDS (Evaluation of Xyrem to Check Efficacy in Excessive Daytime
Sleepiness) was a double-blind, placebo-controlled, parallel group multi-center
randomized study.
This data follows the June announcement of positive clinical results from the
Company's SXB-15 trial which evaluated the benefits of Xyrem in EDS associated
with narcolepsy where the use of Xyrem was incremental to the use of stimulants
or wakefulness-promoting drugs. In that trial, adding Xyrem resulted in
statistically significant improvement in EDS as measured by The Epworth
Sleepiness Score (ESS), the Clinical Global Impression of Change (CGIc) and the
MWT.
Bill Houghton, M.D., Orphan Medical Chief Medical & Scientific Officer, said,
"Together, these two trials now demonstrate that Xyrem can be proposed as
first-line therapy in narcolepsy, since Xyrem data has been produced to show
efficacy in treating the symptoms of EDS, cataplexy and fragmented nighttime
sleep."
John H. Bullion, Orphan Medical Chief Executive Officer, stated, "The results of
EXCEEDS further support our belief that Xyrem represents the foundation for the
treatment of narcolepsy. We intend to file a Supplemental New Drug Application
(sNDA) incorporating the results of both EDS trials with the U.S. Food and Drug
Administration (FDA) by the end of the year. The sNDA timing will position the
Company for an FDA decision in 2005 that could allow us to expand the use of
Xyrem to all of narcolepsy."
Narcolepsy is a chronic, debilitating neurological disease characterized by
symptoms of excessive daytime sleepiness, cataplexy (sudden loss of muscle tone)
and fragmented nighttime sleep. Excessive daytime sleepiness is experienced by
all narcolepsy patients and is usually treated with stimulants during the day to
help keep patients awake. Xyrem is currently the only approved medication for
the treatment of cataplexy.
Trial Results
The trial was conducted in narcoleptic patients with established EDS for which
they were treated with modafinil at doses of 200-600 mg daily. After meeting
entry criteria, and following two weeks of blinded randomized treatment with
modafinil and Xyrem placebo, they were randomized to four evenly distributed
groups in the trial with one group receiving active Xyrem only, another with
active modafinil alone, a third group with both active medications, and a final
group receiving both Xyrem and modafinil placebo. As expected, the group
receiving both active medications saw the greatest mean change of 2.7 minutes
from baseline while maintained in blinded fashion on unchanged dose of modafinil
. It is not yet known if the two products are additive or synergistic in their
benefit. The Xyrem, modafinil and combined drug treatment groups were highly
statistically significant compared to the placebo group. Changes in the Epworth
Sleepiness Score (ESS) were also measured and those results further support the
MWT data.
The safety profile seen in this study was consistent with other controlled
clinical trials, with a relatively uniform distribution across all groups. The
side effect of nausea occurred more often for groups receiving Xyrem and both
Xyrem and modafinil together, as did vomiting which had a markedly lower rate of
incidence. Headache was a common symptom in all groups, including placebo, but
dizziness and tremor were more common in the group on both drugs, as was
anxiety. The incidence of sleep walking and enuresis, previously reported in our
studies as associated with Xyrem showed a very low incidence in this study that
was not significantly different between groups.
Background Information
Narcolepsy is a chronic, debilitating neurological disease. Cataplexy, a sudden
loss of muscle tone, is usually triggered by strong emotions such as laughter,
anger, or surprise. As such, patients often selectively isolate themselves from
interaction with others resulting in a dramatic effect on a patient's quality of
life. Narcolepsy afflicts approximately 100,000 to 140,000 Americans with about
50,000 to 75,000 patients receiving some form of treatment for their symptoms.
An estimated sixty to ninety percent of those with narcolepsy suffer from
cataplexy. All patients with narcolepsy suffer from excessive daytime
sleepiness.
Orphan Medical acquires, develops, and markets pharmaceuticals of high medical
value for inadequately treated and uncommon CNS diseases treated by specialist
physicians. The lead product for the company is Xyrem, which is the first and
only approved treatment for cataplexy associated with narcolepsy. Xyrem has now
been assessed as a treatment for the full range of narcolepsy symptoms including
excessive daytime sleepiness. Orphan Medical's pipeline includes development
stage products for fibromyalgia and pain. Orphan Medical's Internet Web site
address is www.orphan.com.
The information in this press release contains forward-looking statements within
the meaning of the Private Securities Litigation Reform Act of 1995. In some
cases, you can identify forward looking statements by terminology such as
"expects," "anticipates," "intends," "may," "should," "plans," "believes,"
"seeks," "estimates," "could," "would" or the negative of such terms or other
comparable terminology. Such forward-looking statements are based upon current
expectations and beliefs and involve numerous risks and uncertainties, both
known and unknown, that could cause actual events or results to differ
materially from these forward-looking statements. A number of factors could
cause actual results to differ materially from the Company's assumptions and
expectations. These are set forth in the cautionary statements included in
Orphan Medical's most recent Form 10-Q or Form 10-K filed with the Securities
and Exchange Commission. (These documents can be accessed through the Orphan
Medical Web site at http://www.orphan.com). All forward-looking statements are
qualified by, and should be considered in conjunction with, such cautionary
statements.
CONTACT: Orphan Medical, Inc.
Tim McGrath, 952-513-6900
or
David Folkens, 952-513-6994
URL: http://www.businesswire.com
LOAD-DATE: September 15, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: Health/Medical Writers; Business Editors
Copyright 2004 Business Wire, Inc.
533 of 998 DOCUMENTS
The New Atlantis
Summer 2004
Doping for Seconds SUBTITLE: The Shadow of Drugs on American Athletics
BYLINE: The Editors of The New Atlantis
SECTION: Pg. 124-125 No. 6
LENGTH: 739 words
With the return of the Summer Olympics, the world of athletics is once again
focusing its attention on allegations, investigations, and confessions of drug
use -- especially in light of doping scandals throughout the sports world over
the last year.
In August 2003, track and field fans watched Kelli White become the first
American and third woman in history to clinch both the 100- and 200-meter
sprints at the world championships in Paris. But not long after she was awarded
two gold medals, it was announced that she had tested positive for the stimulant
modafinil, used to treat narcolepsy. White admitted to taking modafinil for a
sleep disorder, and claimed she hadn't reported it to proper authorities because
it was not on the official list of banned substances. But soon after, three
other American track and field athletes tested positive for modafinil, and
international drug-testing officials suggested they were not the only guilty
Americans.
In the fall of 2003, the U.S. Anti-Doping Agency conducted a raid of the Bay
Area Laboratory Co-Operative (BALCO), a company suspected of serving an
underground market for steroids and designer drugs. Investigators discovered
correspondence between Kelli White and Victor Conte, Jr., founder of BALCO,
which linked White to a number of designer drugs -- which work by producing the
same result as a banned substance, but sneak past drug screeners due to slightly
different molecular structures. White was linked to such drugs dating back to
2000. In exchange for her cooperation and confession, White escaped lifetime
banishment from her sport -- but she will sit out the next two years of track
and field competition (including this year's Olympics), and all her placements
and medals between 2000 and 2004 were annulled.
The Kelli White drug investigations also implicated several other runners, as
well as numerous athletes from other sports. Craig Masback, chief executive of
the U.S. Track and Field Team, declared that "the situation in which we find
ourselves is not a track and field problem, or even a baseball problem; it is an
American problem." He pointed out that "more than four percent of American high
school seniors" say they have used steroids in the last year.
This figure is backed up by recent studies showing that steroid use decreased
slightly among the overall population of U.S. high school students, but usage
increased among student athletes. While steroids and supplements are used by
young athletes to build muscle, other performance-enhancing drugs -- like asthma
medications -- are increasingly used by young athletes to improve their lung
capacity. The studies show that most teenage boys are aware that steroids can
lead to impotence, and that the side effects of other performance-enhancing
drugs include nausea, diarrhea, and vomiting. Perhaps most alarming is that the
number of students who have a moral or ethical problem with the use of steroids
is declining -- even though drug education and prevention programs are at an
all-time high.
At a recent Senate hearing on steroid use by adolescent athletes, one of the
witnesses was Don Hooten of Plano, Texas, whose high school son suffered from
severe depression due to withdrawal from steroids and eventually killed himself.
Thanks to the Internet, Mr. Hooten said, "all our kids need is a credit card
number or a money order and they can have hard-core prescription anabolic
steroids delivered right to their doorstep." An anonymous college football
player testified about the "competitive edge" that steroids give athletes trying
to keep up with their peers.
Sports doping was deemed important enough by President Bush to earn a mention in
his 2004 State of the Union address: "The use of performance-enhancing drugs
like steroids in baseball, football, and other sports is dangerous, and it sends
the wrong message -- that there are shortcuts to accomplishment, and that
performance is more important than character."
Surely Tori Edwards, a sprinter who competed against Kelli White, would agree
with this sentiment. Upon hearing that White's medals were being annulled, she
said: "I am disappointed, because she took something from me.... The honor of
winning that race, crossing the finish line first, throwing my hands up in the
air and having my family seeing me on the podium.... Even if they send me a gold
medal in the mail, it's not going to be the same. It's a moment I'll never get
back."
LOAD-DATE: November 4, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Magazine
Copyright 2004 Ethics and Public Policy Center
All Rights Reserved
534 of 998 DOCUMENTS
CNS Drug News
Pharmaceuticals
August 20, 2004
Cephalon obtains positive results with new modafinil formulation for younger
ADHD patients
LENGTH: 335 words
Cephalon
has released results from three multi-centre trials showing that new proprietary
once-daily dosage forms of
Provigil
C-IV tablets (
modafinil
) significantly improved symptoms of attention deficit hyperactivity disorder
(ADHD) in children and adolescents. Based upon the study results, the company
plans to accelerate the filing of its application with the FDA from the first
quarter of 2005 to the fourth quarter of 2004.
In three nine-week, double-blind, placebo-controlled studies, 600 children and
adolescents between the ages of six and 17 years with ADHD were randomised to
either placebo or an optimised new dosage form of modafinil. The primary
endpoint in all studies was the teacher-completed school version of the ADHD
Rating Scale IV. All of the modafinil-treated groups showed a highly
statistically significant improvement on the primary endpoint compared to
placebo (p<0.0001). Modafinil was generally well tolerated and the most common
side effects observed in these studies were consistent with those observed in
other studies of this compound and included insomnia, headache and loss of
appetite. The complete Phase III study data are expected to be presented at
major medical meetings over the next 12 months.
Cephalon focused its clinical efforts on identifying optimal doses of modafinil
for these studies because children metabolise the drug in a different way to
adults. The resulting dosage strengths of 340 and 425mg produced robust symptom
improvement in children and adolescents with ADHD in these studies. The company
was encouraged by the robust effects of modafinil on both the inattentive and
hyperactive symptoms of the disorder.
Modafinil is currently available in 100 and 200mg strengths and is indicated for
the treatment of excessive sleepiness associated with narcolepsy, obstructive
sleep apnoea and shift work sleep disorder. Modafinil for the treatment of
children and adolescents with ADHD will be manufactured as smaller, film-coated
tablets in unique dosage strengths.
LOAD-DATE: August 25, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2004 ESPICOM Business Intelligence Ltd.
All Rights Reserved
535 of 998 DOCUMENTS
Knobias.com
This content is provided to LexisNexis by Comtex News
Network, Inc.
August 19, 2004 Thursday
CEPH: Positive Trial Results of Modafinil in ADHD
LENGTH: 109 words
DATELINE: Ridgeland, MS
Cephalon, Inc. (CEPH) announced results from three multi-center clinical trials,
which show that new proprietary once-daily dosage forms of modafinil
significantly improve symptoms of Attention Deficit Hyperactivity Disorder
(ADHD) in children and adolescents. The primary endpoint in all studies was the
teacher-completed school version of the ADHD Rating Scale IV. All of the
modafinil treated groups showed a highly statistically significant improvement
on the primary endpoint compared to placebo. The company plans to accelerate the
filing of its application with the FDA from the first quarter of 2005 to the
fourth quarter of 2004.
LOAD-DATE: August 20, 2004
LANGUAGE: ENGLISH
Copyright 2004 Comtex News Network, Inc.
All Rights Reserved
Copyright 2004 Knobias.com, LLC, All rights reserved
536 of 998 DOCUMENTS
PR Newswire
August 19, 2004 Thursday
Cephalon Announces Positive Results with a New Modafinil Formulation for the
Treatment of Children with Attention Deficit Hyperactivity Disorder;
Results with New Pediatric Doses Were Highly Significant in All Three Studies;
Regulatory Filing Accelerated to Late 2004
SECTION: FINANCIAL NEWS
LENGTH: 1096 words
DATELINE: WEST CHESTER, Pa. Aug. 19
Cephalon, Inc. (Nasdaq: CEPH) today announced results from three multi-center
clinical trials, which show that new proprietary once-daily dosage forms of
modafinil significantly improve symptoms of Attention Deficit Hyperactivity
Disorder (ADHD) in children and adolescents.
In three nine-week, double-blind, placebo-controlled studies, 600 children and
adolescents between the ages of six and 17 with ADHD were randomized to either
placebo or an optimized new proprietary dosage form of modafinil. The primary
endpoint in all studies was the teacher-completed school version of the ADHD
Rating Scale IV. All of the modafinil treated groups showed a highly
statistically significant improvement on the primary endpoint compared to
placebo (p<0.0001). Modafinil was generally well tolerated, and the most common
side effects observed in these studies were consistent with those observed in
other studies of this compound and included insomnia, headache and loss of
appetite. The complete Phase III study data are expected to be presented at
major medical meetings over the next 12 months.
"Because children metabolize modafinil differently from adults, our clinical
efforts focused on identification of optimal doses of modafinil for these
studies," said Dr. Paul Blake, MB, FRCP, Senior Vice President of Clinical
Research and Regulatory Affairs at Cephalon. "The result was the development of
proprietary dosage strengths of 340 and 425 milligrams, which in these Phase III
studies demonstrated robust symptom improvement in children and adolescents with
ADHD. The most encouraging aspects of these results were the strength and
consistency of the effects of modafinil across the three studies and the robust
effects of modafinil on both the inattentive and hyperactive symptoms of ADHD."
Based upon the demonstrated strength of the study results, the company plans
to accelerate the filing of its application with the Food and Drug
Administration from the first quarter of 2005 to the fourth quarter of 2004.
Frank Baldino Jr., Ph.D., Chairman and CEO of Cephalon, said, "We are excited
about these data and the promise they hold for the ADHD community. We expect
this product, once approved, to command a substantial presence in this large and
growing market that today exceeds several billion dollars. With its excellent
clinical profile and strong intellectual property protection for use in ADHD, we
anticipate this product will be an important contributor to Cephalon's revenue
growth for many years to come."
Modafinil
Modafinil (PROVIGIL(R) C-IV Tablets) is currently available in 100 and 200
milligrams and is indicated for the treatment of excessive sleepiness associated
with narcolepsy, obstructive sleep apnea and shift work sleep disorder.
Modafinil for the treatment of children and adolescents with ADHD will be
manufactured as smaller, film-coated tablets in unique dosage strengths.
Attention Deficit Hyperactivity Disorder
According to the National Institutes of Mental Health, ADHD is one of the most
common psychiatric disorders among children, affecting three to five percent of
American children. ADHD is associated with dysfunction in the prefrontal cortex
area of the brain. The most common ADHD behaviors fall into three categories:
inattention, hyperactivity, and impulsivity. A diagnosis of ADHD is generally
made when these behaviors become excessive, long-term, and pervasive.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs more than 2,000 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah
and Eden Prairie, Minnesota. Cephalon's major European offices are located in
Guildford, England, Martinsried, Germany, and Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at http://www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, including the results of the three multi- center clinical
trials of modafinil in ADHD, prospects for regulatory approval of modafinil for
ADHD and the anticipated timetable for filing a marketing application for the
use of modafinil in ADHD, manufacturing development and capabilities, market
prospects for its products, particularly with respect to the Company's ability
to effectively compete in the ADHD marketplace with modafinil, sales and
earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
SOURCE Cephalon, Inc.
CONTACT: Media: Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com, or
Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com, both
of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: August 20, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association, Inc.
537 of 998 DOCUMENTS
Agence France Presse -- English -- English
August 11, 2004 Wednesday
US athletes who have tested positive for drugs
SECTION: Sports
LENGTH: 255 words
DATELINE: ATHENS, Aug 11
Following the two-year suspension handed down to sprinter Torri Edwards on
Wednesday, here is a list of athletes from the United States who have tested
positive for banned substances since last August's world championships in Paris:
BANNED
Kelli White (100 metres/200m): two years (steroids and erythropoietin/EPO)
Regina Jacobs (middle distance): four years (tetrahydrogestrinone/THG)
Calvin Harrison (400m): two years (Modafinil)
Torri Edwards (100m/200m): two years (nikethamide, pending Court of Arbitration
for Sport appeal)
Kevin Toth (shot putt): two years (tetrahydrogestrinone/THG and Modafinil)
Melissa Price (hammer): two years (tetrahydrogestrinone/THG)
John McEwen (hammer): two years (tetrahydrogestrinone/THG)
CASES UNDER INVESTIGATION
Jerome Young (400m): life suspension (erythropoietin/EPO)
Larry Wade (110m hurdles): (norandrosterone)
Mickey Grimes (100m/200m): (norandrosterone)
WARNINGS (WITHOUT BAN)
Chryste Gaines (100m/200m): Modafinil)
Sandra Glover (400m hurdles): (Modafinil)
Eric Thomas (400m hurdles): (Modafinil)
Tim Rusan (triple jump): (marijuana)
Bernard Williams (100m/200m): (marijuana)
Note:
Erythropoietin (EPO) is used to boost endurance.
Tetrahydrogestrinone (THG) is a previously undetectable anabolic steroid which
came to light last year when a sample was sent anonymously to the US Anti-Doping
Agency.
Norandrosterone is a steroid.
Modafinil is a stimulant.
Nikethamide is a stimulant.
sg/gj04
Oly-2004-Athletics-USA-doping-list
LOAD-DATE: August 12, 2004
LANGUAGE: ENGLISH
Copyright 2004 Agence France Presse
538 of 998 DOCUMENTS
PNG Post-Courier
August 4, 2004 Wednesday
US sprinter gets 2-year suspension for doping
SECTION: SPORT; Pg. 40
LENGTH: 462 words
RALEIGH, North Carolina: American sprinter Calvin Harrison has been suspended
for two years for a second doping violation and will be ineligible for the
Athens Olympics, the US Anti-Doping Agency (USADA) said yesterday.
The ruling could also cost the United States its 2003 world 4x400 metres relay
gold medal since Harrison, according to the decision, was ineligible to compete
at the time.
In a similar case last month, the International Association of Athletics
Federations (IAAF) recommended that the International Olympic Committee (IOC)
strip the US 4x400 metres relay team of its Sydney Olympics gold medal because
another sprinter, Jerome Young, was ineligible following a 1999 positive doping
test.
Harrison ran on US 4x400 metres relay teams at both the 2000 Games and 2003
world championships.
He tested positive for the banned stimulant modafinil at the 2003 US national
championships, the USADA said in a statement.
Harrison s first doping offence occurred at the 1993 US junior national
championships, which also involved a prohibited stimulant.
He had been named to the preliminary 4x400 metres relay pool for Athens after
finishing fifth in the individual event at last month s Olympic trials.
Harrison s lawyer, Edward Williams said he did not know whether his client would
appeal the decision, made by a three-member panel of the American Arbitration
Association (AAA)/North American Court of Arbitration for Sport (CAS).
He s disappointed, particularly about the fact that the arbitrators didn t
essentially nullify the repercussions of the first offence, which dealt with
pseudoephedrine, which is no longer on the (banned) list... It was then but is
not now, Williams said in a telephone interview from New York. Williams also
said Harrison s due process was denied in the 1993 hearing process.
The lawyer also expressed disappointment that the hearing panel did not accept
the testimony of his expert witness, a pharmacologist once employed by the
manufacturer of modafinil, that the drug was not a stimulant.
USADA officials said modafinil was prohibited at the time of the test because it
is related to the classes of substances banned under IAAF rules.
Harrison admitted in an October 2003 telephone interview with Reuters that he
tested positive for modafinil at the nationals. He said a coach in California
had given him this pill and he had taken it.
He (the coach) emphasised that it was not on the banned substance list and
assured me that it was not an illegal substance, Harrison said.
The doping agency said Harrison would lose all competitive results and winnings
from June 21, 2003, the date of his positive test for modafinil, including his
second place finish in the 400m at the 2003 US championships.
LOAD-DATE: August 4, 2004
LANGUAGE: ENGLISH
JOURNAL-CODE: PTC
Copyright 2004 Nationwide News Pty Limited
539 of 998 DOCUMENTS
The Associated Press
August 3, 2004, Tuesday, BC cycle
Harrison ineligible for Athens Games, U.S. could forfeit more medals
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 541 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. Olympic team and likely forcing the United
States to forfeit a relay gold medal in the world championships.
The U.S. Anti-Doping Agency said Monday that Harrison was found guilty of using
the stimulant modafinil at the U.S. track and field championships in June 2003.
The case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results.
Harrison also tested positive for the stimulant pseudoephedrine during the 1993
U.S. junior indoor championships and served a three-month suspension. As a
repeat offender, he got the two-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that because modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - now on the
banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team in the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been selected to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal in the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 4, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2004 Associated Press
All Rights Reserved
540 of 998 DOCUMENTS
The Associated Press State & Local Wire
August 3, 2004, Tuesday, BC cycle
Harrison ruled ineligible for Athens Games
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 547 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. Olympic team and likely forcing the United
States to forfeit a relay gold medal in the world championships.
The U.S. Anti-Doping Agency, which is based in Colorado Springs, said Monday
that Harrison was found guilty of using the stimulant modafinil at the U.S.
track and field championships in June 2003.
The case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results.
Harrison also tested positive for the stimulant pseudoephedrine during the 1993
U.S. junior indoor championships and served a three-month suspension. As a
repeat offender, he got the two-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that because modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - now on the
banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team in the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been selected to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal in the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 4, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2004 Associated Press
All Rights Reserved
541 of 998 DOCUMENTS
Associated Press Online
August 3, 2004 Tuesday
Harrison Ineligible for Athens Olympics
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 552 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. team for the Athens Olympics and likely
forcing the United States to forfeit a relay gold medal from last year's world
championships.
The U.S. Anti-Doping Agency said Monday that Harrison was found guilty of using
the stimulant modafinil at the U.S. track and field championships in June 2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the 8-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he got the 2-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - which is now
on the banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team at the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young had failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 4, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
542 of 998 DOCUMENTS
Ottawa Citizen
August 3, 2004 Tuesday Final Edition
American sprinter ineligible for Athens: Harrison doping violation could cost
U.S. world relay gold
SOURCE: The Associated Press
BYLINE: Rob Gloster
SECTION: Sports; Pg. C12
LENGTH: 475 words
DATELINE: ATHENS
ATHENS - Calvin Harrison has been suspended for two years for a second doping
violation, knocking the sprinter off the U.S. team for the Athens Olympics and
likely forcing the United States to forfeit a relay gold medal from last year's
world championships.
The U.S. Anti-Doping Agency said Monday that Harrison was found guilty of using
the stimulant modafinil at the U.S. track and field championships in June 2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the eight-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he received a two-year ban.
Harrison's lawyer, Ed Williams, said yesterday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil -- which is now
on the banned list -- was prohibited in 2003 because it was chemically related
to stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-metre gold medal relay team at the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test -- two months
before the world championships -- will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medallist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: The Associated Press; Calvin Harrison tested positive for
the prohibited stimulant modafinil at the USA Outdoor Track & Field
Championships at Stanford, California on June 21, 2003.
TYPE: Sports
Copyright 2004 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
543 of 998 DOCUMENTS
The San Francisco Chronicle
AUGUST 3, 2004, TUESDAY, FINAL EDITION
His run has ended;
Calvin Harrison given 2-year ban by USADA
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. D1
LENGTH: 807 words
Olympic gold-medal relay runner Calvin Harrison lost his spot on the 2004 U.S.
team Monday and was suspended for two years because he tested positive for the
stimulant modafinil, 11 years after testing positive for a substance no longer
on the banned list.
In the vast quagmire that is sports doping, two positive tests for stimulants
equals one positive test for steroids. That is, a two-year ban from competition.
Harrison had been named to the pool of runners for the 4x400m relay; he and his
twin brother Alvin ran on the gold-medal-winning relay team at the Sydney
Olympic Games in 2000.
Following a hearing before a three-person panel of the American Arbitration
Association, the U.S. Anti-Doping Agency announced a two-year ban for Harrison,
30, of Salinas, effective July 26.
Harrison tested positive for modafinil, a prescription medicine used to treat
sleep disorders such as narcolepsy and also attention deficit disorder, on June
21, 2003, at the U.S. outdoor track and field championships at Stanford. He was
one of seven athletes to test positive for the substance at the U.S. nationals.
That modafinil test, combined with a 1993 positive test for pseudoephedrine,
resulted in the two-year ban. USADA noted, pointedly, that Harrison "loses all
competitive results and winnings" from the date of the positive test. Harrison
won a gold medal on the 4x400 relay at last year's World Championships; relay
teams split $80,000 for gold medals.
"He's just disappointed that the panel did not recognize he did not receive due
process in 1993," said Harrison's attorney, Edward Williams. "What it means is
they rejected my argument that the first offense from 1993 should be a nullity."
Edwards said Harrison did not receive a hearing after his positive '93 test for
pseudoephedrine at the U.S. Junior Championships. The 1978 Amateur Sports Act
guarantees athletes the right to a hearing in doping cases.
"(U.S.) track and field's rules back then provided that as soon as you tested
positive on the 'B' sample, you were automatically suspended before any hearing
... which is contrary to the Sports Act," Williams said.
Pseudoephedrine since has been taken off the banned list because of its common
usage in cold medications. It is listed by USADA under "examples of permitted
medications -- 2004."
Calvin Harrison was named to the relay pool for Athens based on his fifth-place
finish in the 400 meters at last month's Olympics track and field trials. The
runners who finished behind him, Andrew Rock, Kelly Willie and Jerry Harris,
probably will move into consideration for the relay.
Harrison attended North Salinas High School and lives now in Raleigh, N.C. He is
coached by Trevor Graham, who has had seven of his athletes test positive for
banned substances. The Chronicle reported that sprinter Tim Montgomery testified
before a federal grand jury investigating the BALCO case that Graham gave
steroids to some of his athletes.
Alvin and Calvin Harrison testified before the grand jury in San Francisco last
fall.
The Harrison brothers did not have an easy upbringing and their athletic careers
have been checkered. They moved from Orlando to Salinas when their father found
work on the Monterey Bay Aquarium project. They were homeless for a time and
lived in their car around the time they enrolled in, and later dropped out of,
Hartnell College.
Their careers peaked in 2000 when they both made the Olympics team and ran on
the relay. Alvin also won a silver medal in the 400 meters when he finished
behind Michael Johnson. The brothers are credited with writing an inspirational
book titled "Go to Your Destiny" and they appeared on the "Oprah Winfrey Show"
after the Olympics.
Now Calvin is suspended and Alvin is under investigation by USADA for a
suspected doping violation, although his case has not been resolved and he
remains eligible for competition. Alvin Harrison did not advance to the final of
the 400 at the Olympics trials and is not a member of the Olympics team.
Meanwhile, the makers of modafinil, under the trade name Provigil, say it is not
a stimulant in the common sense of the word in that it does not have
amphetamine-like qualities "like hyper-arousal and irritability," said Dr.
Jeffry Vaught, president of research and development for Cephalon, Inc., the
West Chester, Pa., company that makes Provigil.
"There's no reason why anyone who is healthy should be prescribed any
prescription-based product. That would include modafinil," Vaught said. "Am I
surprised they're taking modafinil? I suppose so."
In addition to Calvin Harrison, other track and field athletes who tested
positive for modafinil in 2003 were Kelli White, Chryste Gaines, John McEwen,
Eric Thomas, Chris Phillips and Sandra Glover.E-mail John Crumpacker at
jcrumpacker@sfchronicle.com.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, Calvin Harrison / Vincent Laforet / New York Times
Copyright 2004 The Chronicle Publishing Co.
544 of 998 DOCUMENTS
The Associated Press
August 2, 2004, Monday, BC cycle
Harrison ineligible for Athens Games, U.S. could forfeit more medals
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 555 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. team for the Athens Olympics and likely
forcing the United States to forfeit a relay gold medal from last year's world
championships.
The U.S. Anti-Doping Agency said Monday that Harrison was found guilty of using
the stimulant modafinil at the U.S. track and field championships in June 2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the 8-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he got the 2-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - which is now
on the banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team at the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young had failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photo NY154
Copyright 2004 Associated Press
All Rights Reserved
545 of 998 DOCUMENTS
The Associated Press State & Local Wire
August 2, 2004, Monday, BC cycle
Harrison ineligible for Athens Games, U.S. could forfeit more medals
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 561 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. team for the Athens Olympics and likely
forcing the United States to forfeit a relay gold medal from last year's world
championships.
The U.S. Anti-Doping Agency, based in Colorado Springs, Colo., said Monday that
Harrison was found guilty of using the stimulant modafinil at the U.S. track and
field championships in June 2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the 8-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he got the 2-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - which is now
on the banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team at the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young had failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photo NY154
Copyright 2004 Associated Press
All Rights Reserved
546 of 998 DOCUMENTS
Associated Press Online
August 2, 2004 Monday
Harrison Ineligible for Athens Olympics
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 552 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. team for the Athens Olympics and likely
forcing the United States to forfeit a relay gold medal from last year's world
championships.
The U.S. Anti-Doping Agency said Monday that Harrison was found guilty of using
the stimulant modafinil at the U.S. track and field championships in June 2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the 8-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he got the 2-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - which is now
on the banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team at the Sydney Olympics
that already faces loss of its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could face loss of its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The International
Association of Athletics Federations will decide whether to strip the U.S. squad
of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young had failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
547 of 998 DOCUMENTS
Associated Press Worldstream
August 2, 2004 Monday
Harrison ineligible for Athens Games, U.S. could forfeit more medals
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 544 words
DATELINE: ATHENS, Greece
Calvin Harrison has been suspended for two years for a second doping violation,
knocking the sprinter off the U.S. team for the Athens Olympics and likely
forcing the United States to forfeit a relay gold medal from last year's world
championships.
The U.S. Anti-Doping Agency said on Monday that Harrison was found guilty of
using the stimulant modafinil at the U.S. track and field championships in June
2003.
His case was heard last week by a three-member arbitration panel, which rejected
Harrison's appeal of the test results. Harrison did not attend the 8-hour
arbitration hearing.
Harrison also tested positive for the stimulant pseudoephedrine at the 1993 U.S.
junior indoor championships and served a three-month suspension. As a repeat
offender, he got the 2-year ban.
Harrison's lawyer, Ed Williams, said Monday he was not sure whether he will
appeal the ruling to the Swiss-based Court of Arbitration for Sport.
Williams said he was disappointed the arbitrators did not accept his argument
that the 1993 suspension should have been nullified because athletes were not
accorded adequate due process at that time.
He also argued unsuccessfully before the panel that since modafinil was not
specifically named on the banned substance list in 2003, that Harrison would
have had no way of knowing it was prohibited.
USADA's director of legal affairs, Travis Tygart, said modafinil - which is now
on the banned list - was prohibited in 2003 because it was chemically related to
stimulants named on the list of banned substances.
"Modafinil is a banned substance and is a stimulant. You can only get it in the
U.S. by prescription. It is classified by the federal government as a central
nervous system stimulant," Tygart said in a telephone interview.
"Athletes are generally warned not to take drugs when they compete, and they
should be held accountable when they do so."
Harrison, part of the 1,600-meter gold medal relay team at the Sydney Olympics
that already faces losing its medals because of a positive drug test by Jerome
Young, had been named to the U.S. squad for Athens as part of the relay pool.
He also was on the 1,600 relay team that won a gold medal at the 2003 world
championships in Paris, and that squad now could lose its medals.
All of Harrison's results from the time of the positive drug test - two months
before the world championships - will be nullified. The IAAF will decide whether
to strip the U.S. squad of its gold and award it to silver medalist France.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Young.
Harrison's twin brother, Alvin, faces a lifetime ban after being charged by
USADA with steroid use. His case is awaiting arbitration.
The 2000 Sydney relay gold medals could be forfeited because Young had failed a
steroid test in 1999.
The Court of Arbitration for Sport ruled in late June that Young should be
stripped of his relay medal, and the IAAF has recommended that the entire team -
including Michael Johnson - be stripped of its medals.
A final decision rests with the International Olympic Committee, which is
expected to rule days before the Athens Games and is expected to endorse the
IAAF recommendation.
LOAD-DATE: August 3, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
548 of 998 DOCUMENTS
The Times (London)
July 27, 2004, Tuesday
Seize the daytime
BYLINE: Jerome Burne
SECTION: Features; Times2; 8
LENGTH: 588 words
A CONTROVERSIAL NEW DRUG HAS SOUNDED A WAKE-UP CALL FOR NARCOLEPTICS, SAYS
JEROME BURNE
AS A TEENAGER, Brendan Maguire had to be careful not to laugh. If he did, he
could fall to the floor in a deep sleep. He spent most of his days in bed
because he always felt sleepy.
Maguire has narcolepsy and his life was transformed two years ago by a new drug,
Provigil, that allows him to live an almost normal life. "Now I can do a 12 hour
shift at a call centre," he says.
The only remedies for overwhelming sleepiness used to be coffee, cigarettes or
amphetamines -all linked with unpleasant side-effects such as jitteriness. What
seems to distinguish Provigil is that it is precisely targeted. It keeps the
user awake for about six hours then allows them to sleep normally, with no
comedown.
In the US, it is largely used for non-medical reasons -to sustain a party or
business lifestyle without apparent penalties. In the UK, however, it was
tightly regulated until a few months ago. Last year only 17,000 prescriptions
were written for the treatment of narcolepsy and an insomnia disorder known as
sleep apnoea.
Now it can be prescribed for any chronic condition that involves "excessive
daytime sleepiness", such as Parkinson's disease or multiple sclerosis. "Studies
show it's safe, effective and well tolerated," says Dr Paul Reading, a
neurologist who runs the sleep clinic in Newcastle where Maguire is treated. The
drug is also used for "chronic shiftworker sleep disorder", a condition that
isn't recognised medically in the UK but is regularly diagnosed in the US and
usually involves older people who keep falling asleep on the job.
"Until now GPs would normally either suggest you get a different job or
prescribe barbiturates to take in the day," says Reading. "Giving Provigil,
which is associated with far fewer problems, seems to make more sense. But it
shouldn't be given to people who are just overworked or overdoing it."
Provigil is controversial because, like Viagra, it blurs the line between
treating a medical condition and a lifestyle choice. "We don't know the
long-term effects of using drugs to stay awake longer," says Professor Jim
Horne, of the Sleep Research Centre at Loughborough University. "What we do know
is that there are powerful mechanisms for sleep and no natural ways to override
them, so it's potentially a dangerous thing to do."
If the promise of research is fulfilled, Provigil may event-ually have a wider
range of targets, including attention deficit hyperactivity disorder and weight
loss; it may also be used to boost antidepressants.
Scientists still don't know exactly how the drug, known generically as modafinil
, works. The consensus seems to be that it targets the hypo-thalamus -an area of
the brain also involved in regulating other body systems such as sex and
appetite -in a precise way. Unlike the general state of arousal produced by
other stimulants, modafinil seems only to target neurones involved in
wakefulness.
That still allows a number of other applications. A study at the University of
Pennsylvania found that both modafinil and amphetamine reduced appetite but
that, unlike amphetamine, modafinil didn't raise heart rate and blood pressure.
American psychiatrists are increasingly prescribing modafinil to boost the
effectiveness of antidepressants.
Fans of the drug claim that it not only keeps them painlessly awake but also
makes them more focused and effective at work, and there is research to support
this.
LOAD-DATE: July 27, 2004
LANGUAGE: ENGLISH
Copyright 2004 Times Newspapers Limited
549 of 998 DOCUMENTS
Chemist & Druggist
July 10, 2004
DTB: little proof for new modafinil uses
SECTION: Pg. 22
LENGTH: 294 words
Use of modafinil, the non-amphetamine wake promoter, may prevent the underlying
cause of excessive sleepiness from being treated. There is also little proof for
its newly approved uses, claims the Drug and Therapeutics Bulletin.
Extending the drug's use to include shift work sleep disorder and obstructive
sleep apnoea could mean the underlying cause of excessive sleepiness is
overlooked or not addressed, says the DTB. Evidence for modafinil's benefit for
these patients is "limited or unconvincing".
The drug may also reduce the use of continuous positive airway (CPAP) therapy in
patients with obstructive sleep apnoea, says DTB. Although modafinil is
effective in patients with narcolepsy, no head to head studies of modafinil and
dexamphetamine have been carried out, DTB says.
DTB acting editor Ike Iheanacho said: "The broader licensing of modafinil is of
concern; there is little compelling evidence to justify this potentially
indiscriminate use and the drug may increasingly be used as an unsatisfactory
alternative to addressing whatever's causing the sleepiness."
Dr John Shneerson, Papworth Hospital's Respiratory Support and Sleep Centre
director, said: "In addition to its first-line use in narcolepsy, modafinil has
been shown to relieve persisting excessive sleepiness in obstructive sleep
apnoea patients despite CPAP treatment. Long-term data appears to show no
clinically relevant reduction in CPAP compliance amongst patients taking
modafinil for this reason.
"Unfortunately, excessive sleepiness is frequently under-diagnosed in the UK and
its impact is underestimated. It is always important to identify and treat any
underlying cause."
For more information: Drug and Therapeutics Bulletin 2004; 42: 52-6
LOAD-DATE: July 13, 2004
LANGUAGE: English
PUB-TYPE: Magazine
Copyright 2004 CMP Information Ltd
550 of 998 DOCUMENTS
American Health Line
June 30, 2004 Wednesday
SLEEP: NEW YORK TIMES EXAMINES USE OF MODAFINIL
SECTION: TRENDS & TIMELINES
LENGTH: 345 words
The New York Times on Tuesday looked at how modafinil, a
drug that "revs up the central nervous system without the
jitteriness of caffeine or the addiction and euphoria of
amphetamines" and keeps people "awake for hours or even days,"
is being prescribed. The Cephalon drug, which is marketed as
Provigil, was approved in 1998 as a narcolepsy treatment, and
FDA this year broadened its approved uses to include obstructive
sleep apnea and sleeping problems caused by shift work. Sales
have been "skyrocketing," but "[n]o one knows exactly how" the
drug works, according to the Times. Global sales in 2003
exceeded $290 million. About 90% of modafinil prescriptions are
for off-label uses, including as a treatment for attention
deficit hyperactivity disorder, depression, fatigue and
drowsiness caused by other medications, according to Cephalon
officials. The drug is also being tested as an appetite
suppressant and a cocaine addiction treatment. However, some
scientists worry that modafinil might be dangerous because
taking it could mask underlying causes of fatigue, such as
diabetes and sleep apnea. The drug "might also pose a more
subtle danger: to the countless Americans in search of an extra
edge, modafinil could be a cure for sleep," and losing sleep
over an extended period of time can have long-term
cardiovascular and neurological effects, according to the Times.
Dr. Neil Kavey, director of the Sleep Disorders Center at
Columbia Presbyterian Medical Center, said, "[I]ncreasing mounds
of data sho[w] that sleep is a restorative, protective health
process [that] ... affects performance, blood pressure, heart
rate, insulin, various hormone secretions." He added, "No
matter what medications come out that make sleep seem like a
waste of time, we know that the sleep-deprived state is a bad
one to be in." Studies have shown that sleep deprivation
weakens the immune system, increases the likelihood of illness
and is associated with a shorter life span (O'Connor, New York
Times, 6/29).
LOAD-DATE: June 30, 2004
LANGUAGE: ENGLISH
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551 of 998 DOCUMENTS
The New York Times
June 29, 2004 Tuesday
Late Edition - Final
Wakefulness Finds a Powerful Ally
BYLINE: By ANAHAD O'CONNOR
SECTION: Section F; Column 2; Health & Fitness; Pg. 1
LENGTH: 2250 words
Laurie Coots, a marketing executive who flies to meetings in other countries
twice a week, spent years trying to conquer sleepless nights and chronic jet
lag. But nothing worked, she says, and every day was a struggle to stay awake.
''It was debilitating,'' said Ms. Coots, 46, who is from Los Angeles. ''I
couldn't give an effective presentation because I was always shaky and nervous
from being amped up on caffeine and stimulants.''
Then she found modafinil, a small white pill that revs up the central nervous
system without the jitteriness of caffeine or the addiction and euphoria of
amphetamines.
''Without it my life would not be possible,'' she said.
Since 1998, modafinil, made by Cephalon and sold under the brand name Provigil,
has quietly altered the lives of millions of people. No one knows exactly how it
works, but sales of the drug are skyrocketing.
People who take it say it keeps them awake for hours or even days. It has been
described as a nap in the form of a pill, making most users feel refreshed and
alert but still able to go to bed when they are ready. And because its side
effects are rarely worse than a mild headache or slight nausea, experts fear
that it has rapidly become a tempting pick-me-up to a nation that battles sleep
with more than 100 million cups of coffee a day.
Few numbers are available, but experts say that as modafinil grows more widely
available, it is becoming a fixture among college students, long-haul truckers,
computer programmers and others determined to burn the midnight oil. Some worry
that an array of common disorders, like diabetes and sleep apnea, will go
undiagnosed if doctors dole out Provigil instead of seeking the underlying
diseases that cause fatigue.
In a culture of 24-hour stores, graveyard shifts and coffee shops on every
corner, modafinil might also pose a more subtle danger: to the countless
Americans in search of an extra edge, modafinil could be a cure for sleep.
''This drug enables us to be that much more workaholic and that much more
obsessed with accomplishments and productivity, and I think our society is
already extreme along those lines,'' said Dr. Martha J. Farah, director of the
Center for Cognitive Neuroscience at the University of Pennsylvania. ''The
natural checks on that tendency, like needing to go to bed, are being rolled
back by modafinil.''
To the extent that modafinil becomes the latest lifestyle drug, as ubiquitous as
Viagra, scientists warn that cutting back on sleep, even by one hour a night,
can have long-term neurological and cardiovascular effects that are only now
being recognized.
''It's almost fortuitous that at the same time that this drug has come out, we
have increasing mounds of data showing that sleep is a restorative, protective
health process,'' said Dr. Neil B. Kavey, director of the Sleep Disorders Center
at Columbia Presbyterian Medical Center. ''It affects performance, blood
pressure, heart rate, insulin, various hormone secretions. No matter what
medications come out that make sleep seem like a waste of time, we know that the
sleep-deprived state is a bad one to be in.''
Discovered by French researchers in the late 1970's, modafinil went on the
market in the United States in 1998 as a treatment for narcolepsy, a severe
sleep disorder. Earlier this year, the Food and Drug Administration broadened
its approved uses to include obstructive sleep apnea, a narrowing or blockage of
the airways, and sleeping problems caused by shift work. An effort by Cephalon
to have the drug approved for a third indication, excessive sleepiness from any
cause, was rejected.
But the three conditions modafinil is approved to treat make up only a fraction
of its total uses. According to Cephalon, based in West Chester, Pa., 90 percent
of all prescriptions for the drug are for ''off-label'' uses, including fatigue,
depression, attention deficit hyperactivity disorder, and sleepiness caused by
other prescription medications.
In the last year, six American track and field athletes have tested positive for
the substance, which is on the United States Olympic Committee's list of banned
stimulants. One group of scientists is testing its effectiveness as an appetite
suppressant in people who are overweight. And a government-financed study found
that it blunts the high produced by cocaine, making it a promising treatment for
addiction.
''The off-label use of this drug is staggering,'' said Dr. Eric Heiligenstein, a
psychiatrist at the University of Wisconsin who studies substance abuse by
teenagers.
''This is a very clean drug that affects all the things that help people with
their cognitive functioning,'' he said. ''The main barrier to more widespread
use is that it's expensive, which will change as more insurance companies start
to cover it.''
For doctors, modafinil's biggest lure is its safety profile. It was used in
France for several years without reports of major problems before reaching the
United States. In clinical trials, only about 1 percent of people complained of
side effects, including nausea, mild headache and nervousness.
But scientists point out that as with any drug, more serious side effects could
appear as modafinil is used more widely.
''I'm not aware of any terrible outcomes, but I don't think there have been
enough long-term studies of modafinil to rule out all dangers,'' said Dr. Jerome
M. Siegel, chief of neurobiology research at the Veterans Affairs Greater Los
Angeles Healthcare System.
Total worldwide sales of Provigil soared above $290 million in 2003, up from
$207 million in 2002. Marc Goodman, a pharmaceutical analyst at Morgan Stanley,
expects that figure to reach $409 million this year. More than 90 percent of
that revenue, he said, will come from sales in the United States alone.
''If you look back before the drug was launched, no one would ever have believed
it would be this big,'' Mr. Goodman said. ''Everyone viewed narcolepsy as the
market and didn't appreciate the benign side-effect profile and how that would
play into off-label uses.''
Between 2002 and 2003, Provigil's share of the stimulants market grew by 39
percent, according to IMS Health, a company that tracks the pharmaceutical
industry.
In the near future, modafinil could find its way into even more medicine
cabinets. Mr. Goodman said it was likely that Cephalon's patent for the compound
would be challenged by several drug companies seeking to market generic
versions. If they succeed, it would increase the availability of modafinil and
almost certainly drive down the price of a monthly supply, which is now $120 or
more.
Cephalon is working on Provigil's successor, a longer lasting version the
company calls Nuvigil. It also hopes to win approval for modafinil as a
treatment for children with attention deficit disorder, the most commonly
diagnosed behavioral disorder of childhood. Some experts think this would open
the door to the drug becoming even more of a household name.
Of all the questions surrounding modafinil, perhaps the most intriguing is how
it works. After more than two decades of research, scientists are still trying
to figure out just how it manipulates the brain.
''It is amazing that this drug has become so widely used without any real
understanding of the basic science behind it,'' Dr. Siegel said.
Researchers know that modafinil is distinctly different from conventional
stimulants, which ramp up arousal and set off a flurry of activity throughout
the brain. Such stimulants, like cocaine and amphetamines, for example, produce
wakefulness but also produce a high and can lead to dependence. Modafinil
appears to steer clear of those side effects by aiming at specific structures
and chemicals.
One neurotransmitter that is thought to be involved is dopamine, which mediates
the reward pathways in the brain, producing euphoria, pleasure and addiction.
Cocaine and amphetamines cause a surge in dopamine levels, while modafinil's
effects are much weaker. A study of animals lacking a protein that helps process
dopamine found that they did not respond to modafinil.
Dr. Thomas Scammell, an associate professor of neurology at Harvard's medical
school who was involved in preclinical trials of the drug, believes that
modafinil may home in on a single poorly understood dopamine circuit that is
specific for wakefulness, while amphetamines and other stimulants activate all
three of the brain's dopamine pathways, including those involved in addiction
and locomotor activity. That selectivity, he said, might be crucial in
modafinil's lack of unwanted side effects.
''I think it is a subtle enough drug that it doesn't just activate everything,''
he said.
Modafinil's impact on the brain is so subtle that brain scans of people who have
taken it hardly register any change in activity at all. Give them amphetamine or
a drug for Parkinson's disease, Dr. Scammell said, and ''the changes in brain
function are spectacular,'' but give them modafinil, and they show little more
than ordinary wakefulness.
Most scientists suspect that at least three other transmitters are involved. One
of them, histamine, is responsible for the sleep-inducing effects of many cold
and allergy medications. In a study last month, Dr. Siegel, who is also a
professor of psychiatry and biobehavioral sciences at the University of
California at Los Angeles, found that histamine in the brain helps control
consciousness.
In the rapid-eye-movement stage of sleep, lower levels of norepinephrine and
serotonin keep the body still, producing the characteristically slack muscle
tone of sleep. Lower levels of histamine, however, specifically reduce
consciousness and awareness. In studies on animals last year, Japanese
researchers found that modafinil releases histamine. French researchers this
year found that it elevates levels of norepinephrine. And a smaller number of
scientists suspect minor involvement by orexin, a substance that is severely
depleted in narcoleptics.
Several researchers, including Dr. Siegel, have proposed a unified theory
suggesting that all these chemicals are necessary for modafinil to take effect.
''Many things have to work together to achieve alertness,'' he said. ''Modafinil
might activate dopamine, which then activates norepinephrine, which then
activates histamine, for example. But we still want to know where the initial
action is.''
Scientists think that the chain of reactions set off by modafinil leads to the
hypothalamus, a small structure embedded in the forebrain that controls the
body's hormones and regulatory functions. One part of the hypothalamus, known as
the ventrolateral preoptic nucleus, appears to act as the body's sleep
generator. When it is active, it produces a chemical, GABA, that inhibits the
firing of cells involved in wakefulness and arousal. Scientists suspect that by
increasing norepinephrine levels, modafinil may block the region from promoting
sleep.
Just next door, in the posterior hypothalamus, are bundles of thousands of
neurons that produce histamine. Damage to this region, scientists have found,
causes excessive sleepiness. Dr. Rod Hughes, senior director of scientific
communications for Cephalon, thinks the histamine center may generate
wakefulness, counteracting the effects of its sleep-inducing neighbor. Modafinil
might increase output in this region, coaxing a tired body into switching on its
natural alertness system.
Some scientists say that regularly manipulating this system to skimp on sleep
could have dire consequences. Studies have shown that chronic sleep deprivation
damages health, weakening the immune system and increasing the likelihood of
illness. It is also associated with a shorter life span.
But other experts counter that Americans will continue to cut back on sleep,
whether they have modafinil or not. The toll of this deprivation has been
visible for years on the nation's highways, where impaired judgment from
sleepiness is blamed for about 100,000 accidents a year. Lack of sleep is also
believed to have played a role in the space shuttle Challenger disaster, the
nuclear meltdown at Chernobyl and the Exxon Valdez oil spill.
''In terms of error rate, 18 hours of no sleep, which many of us regularly do,
is equivalent to a blood alcohol level of about .05,'' said Dr. Ronald Chervin,
who was involved in clinical trials of modafinil and is the director of the
University of Michigan sleep disorders center. ''Twenty-one hours of no sleep is
equivalent to a blood alcohol level of .08, which is illegal in many states.''
If someone is falling asleep on the highway, and has no other option than
driving to work, Dr. Chervin said, ''I think many sleep experts would give that
patient modafinil, and I think many do.''
Dr. Farah, at the Center for Cognitive Neuroscience, is more concerned about the
people who are taking modafinil simply so they can get ahead at work or finish a
term paper. As it becomes more and more popular to use it for those reasons, she
said, people might feel they have to take it just to seem as if they are
performing normally.
''It would be a shame for a generation of young adults to come of age believing
that the only way they can take on a challenging project is with some kind of
pharmacological help,'' she said. ''It's quite possible that modafinil will be
the next Ritalin on campus, something that kids go off to college with. If it is
widely used for A.D.H.D., then it will probably end up being readily available
to the undergraduate masses.''
URL: http://www.nytimes.com
LOAD-DATE: June 29, 2004
LANGUAGE: ENGLISH
GRAPHIC: Photo: ''I don't think there have been enough long-term studies of
modafinil to rule out all dangers,'' Dr. Jerome M. Siegel said. (Photo by
Stephanie Diani for The New York Times)(pg. F6)
(Illustration by Frank Ippolito)(pg. F1)Chart/Diagram: ''The Brain, Awake and
Asleep''Scientists do not know exactly how modafinil works. But they are finding
out more about the brain chemistry of sleep and waking.CORTEXControls
coordination of movement, organization and planning among other things.THALAMUSA
relay between the cortex and the rest of the brain.HYPOTHALAMUSControls
regulatory functions and hormones.FOR WAKEFULNESSClusters of brain cells, or
neurons, send signals (neurotransmitters) to activate the cortex.FOR LIGHT AND
DEEP SLEEPOther clusters of neurons send signals that turn off the neurons that
are active during wakefulness.THE DETAILS: WAKEFULNESSFour neurotransmitters --
istamine, dopamine, serotonin and norepinephrine -- are thought to work
together to activate the cortex. A fifth, acetylcholine, activates the thalamus
and cortex.NON-DREAMING SLEEPPart of the hypothalamus produces a
neurotransmitter called GABA (gamma amino-butyric acid), which silences the
brain cells that are active during wakefulness.DREAMING SLEEP (RAPID EYE
MOVEMENT)Cells in the medial medulla are activated, inhibiting the motor neurons
up and down the spinal cord and paralyzing nearly all muscles in the
body.(Sources by Dr. Thomas Scammell and Rodrigo Espaa, Harvard Medical School
and Beth Israel Deaconess Medical Center)(pg. F1)
PUBLICATION-TYPE: Newspaper
Copyright 2004 The New York Times Company
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The Guardian (London) - Final Edition
June 9, 2004
Athletics: American sprinters fear ban
BYLINE: James Hammond
SECTION: Guardian Sport Pages, Pg. 34
LENGTH: 471 words
Tim Montgomery and Chryste Gaines came under threat of suspension from the
Olympics yesterday as the Balco scandal continued to spread its shadow over US
sprinting.
Montgomery, the world 100 metres record holder, has received a letter from the
US Anti-Doping Agency alleging that he used banned substances. And Chryste
Gaines, a member of the 1996 Olympic 4x100m gold medal-winning team, was last
night charged with a doping violation.
"Tim Montgomery has not done anything wrong and we intend to fight any attempt
to prevent Tim from running in the Olympics," his lawyer Cristina Arguedas said
last night.
"The evidence that we have been shown by Usada and that we are still reviewing
is inconclusive and internally inconsistent. It is fundamentally unfair to try
and take away (an) athlete's reputation, his work and his dreams based on meagre
information, flimsy documents and a flawed process."
Gaines's lawyer Cameron A Myler said: "We have received a letter from Usada.
(It) has charged Chryste with a doping violation based on documents obtained in
the Balco investigation."
Gaines was one of the athletes coached by Remi Korchemny, who also coached
Britain's European and 100 metres record holder Dwain Chambers. Korchemny has
been charged along with three other men with being involved in a conspiracy to
supply banned drugs to elite athletes. He has pleaded not guilty.
Also charged is Victor Conte, the founder of Balco, which allegedly supplied
Chambers with the designer steroid tetrahydrogestrinone (THG). Chambers tested
positive last August and was this year handed a two-year suspension.
It was announced last October that Gaines had tested positive for modafinil,
which is used to treat narcolepsy. Modafinil had not been on the International
Association of Ath- letics Federations' banned list of drugs although it was
proscribed after the world championships in August. Gaines had tested positive
in June, at the US Championships. Modafinil can be used as a masking agent for
steroids.
Her fellow sprinter Kelli White and the hurdler Chris Phillips, who both trained
with Korchemny, also tested positive for modafinil. Korchemny denied giving
modafinil to Gaines. In May White, the world champion at 100m and 200m, became
the first athlete in history to be banned for a doping offence without having
tested positive.
Montgomery is the partner of the triple Olympic champion Marion Jones, who has
also been linked with Balco. A representative for Jones told the New York Times
that she had not received any letter from Usada.
Jones competed in the long jump at the Golden Spike meeting in Ostrava last
night but failed to break seven metres. She is returning from a year off after
giving birth to Montgomery's son last year.
Bekele breaks world record, page 29
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LANGUAGE: ENGLISH
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The Washington Post
May 20, 2004 Thursday
Final Edition
USADA Bans White for 2 Years;
Evidence Seized in Raid on BALCO Is Used to Prove Track Star's Steroid Use
BYLINE: Amy Shipley, Washington Post Staff Writer
SECTION: Sports; D01
LENGTH: 1044 words
U.S. sprinter Kelli White, the winner of two gold medals at last year's world
track and field championships, accepted a two-year ban for taking a host of
performance-enhancing drugs including undetectable steroids, the U.S.
Anti-Doping Agency announced yesterday.
The case is significant not only because it will keep one of the sport's top
stars out of the 2004 Olympic Games, but also because USADA for the first time
used evidence seized in a federal raid of the Bay Area Laboratory Co-Operative
(BALCO) last fall in building its case and exacting punishment. The penalty
includes the nullification of all of White's results since late 2000, when she
began taking drugs.
"In doing this, I have not only cheated myself, but also my family, friends and
sport," White said in a statement released by her attorney, Jerrold D. Colton of
Voorhees, N.J. "I am sorry for the poor choices I have made."
White, 27, said that she expected charges to be brought against others by USADA,
but she did not elaborate. USADA agreed to the two-year ban in exchange for
White's cooperation in its continuing investigation, which also entitles her to
apply for early reinstatement to the world track and field governing body (IAAF)
in accordance with the organization's bylaws. Colton said White would apply for
early reinstatement. Colton also said he expected USADA to seek four-year bans
against others caught up in the BALCO scandal.
Yesterday's disclosure illuminated White's success in masking the use of
sophisticated and powerful drugs for more than two years despite frequent
unannounced drug-testing, raising questions about the pervasiveness of
performance-enhancing drug use in track and field and other sports.
White received the minimum ban for a host of violations that had not previously
been publicly known, which included taking multiple designer steroids and the
blood-boosting drug erythropoietin (EPO), along with the stimulant modafinil.
Last year, White tested positive for modafinil, which is considered a relatively
minor drug compared with steroids and EPO. She never failed a drug test for any
other performance-enhancing drug.
BALCO is at the center of a federal steroid investigation that has thus far
resulted in the indictments of four men, including BALCO founder Victor Conte
Jr. and White's coach, Remi Korchemny, on steroid distribution charges.
Colton said USADA confronted White last Tuesday with incriminating information
from the BALCO files, which had been turned over to USADA by the Senate Commerce
Committee about 10 days ago. The files consist of thousands of pages of
documents obtained in the raid of the lab, including drug schedules with White's
name on them, according to a source. Before the Tuesday meeting, Colton said,
White was aware only of the positive tests for modafinil and had been talking
with USADA only about that matter.
"When USADA received the documents [from the Senate], the conversation changed,"
Colton said. "USADA said they thought we might be interested in reviewing those
materials and having discussions with them."
White's two-year suspension, first reported by the San Jose Mercury News, began
Monday. All of her results since Dec. 15, 2000, the date she began using
performance-enhancing drugs, have been nullified -- including the double gold
medals she won at last year's U.S. championships and world championships in the
100 and 200 meters.
The disqualifications mean that U.S. sprinter Torri Edwards becomes the world
champion in the 100 meters and the U.S. champion in the 100 and 200. Edwards
finished second to White in all three races, and she won the bronze in the 200
final at the world championships.
In New York on Monday, Edwards, who toiled in White's shadow all season, said
she would be bitter if it turned out that White used performance-enhancing
drugs.
"I am disappointed, because she took something away from me," Edwards said. "The
honor of winning that race, crossing the finish line first, throwing my hands up
in the air and having my family seeing me on the podium. . . . Even if they send
me a gold medal in the mail, it's not going to be the same. It's a moment I'll
never get back."
White's agent, Robert Wagner, said he had been unaware White had taken anything
other than modafinil.
"The modafinil is one thing," Wagner said by cell phone from Germany. Steroids
"is another thing, and EPO on top of that -- this is crazy."
With Marion Jones taking time off to have a child, White emerged last year as
the biggest female star in the sport and was considered a threat to Jones's
dominance this season. Like White, Jones also has connections to BALCO and two
Bay Area newspapers reported she received steroids from Conte. But Jones's
lawyer, Joe Burton, said in a statement yesterday that Jones had not been
contacted by USADA and did not expect to be contacted.
At a news conference in New York on Sunday, Jones said she had never taken
performance-enhancing drugs and would sue if USADA tried to ban her from the
Olympics without solid evidence.
It is unclear to what extent White plans to cooperate with USADA. She said she
wanted to help in "cleaning up the sport" but declined to discuss other athletes
in the statement. Colton said he and White believed she would have been subject
to a four-year ban -- and no hope of reinstatement -- if she did not cooperate
because of the compelling nature of the evidence in USADA's possession.
Colton also said White was motivated by a desire to tell the truth. At last
year's world championships, she denied in front of dozens of reporters taking
any performance-enhancing drugs and claimed she took modafinil to combat the
sleep disorder narcolepsy.
"I have had a very difficult time since winning the world championships last
August," White said in the statement. "I have had to continue to train while
knowing I had acted improperly. With my suspension, I now have some time to
evaluate my life, the choices I have made and the direction in which I would
like it to go."
Said USADA CEO Terry Madden in a statement: "Ms. White has made mistakes, but I
admire her courage in acknowledging these mistakes and accepting responsibility
for them. It is not easy to admit you have done wrong and then stand up to do
something about it."
LOAD-DATE: May 20, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 The Washington Post
554 of 998 DOCUMENTS
The San Francisco Chronicle
APRIL 30, 2004, FRIDAY, FINAL EDITION
DRUGS AND SPORTS;
Agency issues first bans;
USADA suspends Price, McEwen 2 years for steroids
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. D1
LENGTH: 756 words
Hammer throwers Melissa Price and John McEwen were the first U.S. athletes to be
suspended for positive tests of the designer steroid THG when the U.S.
Anti-Doping Agency announced two-year bans from competition for the pair
Thursday.
Price, 24, and McEwen, 30, both tested positive for THG last June at the U.S.
national track and field championships at Stanford and are not eligible to
compete until April 2006. McEwen also tested positive for the stimulant
modafinil.
"This decision confirms the tremendous work of all those who believe in
drug-free sport," said Terry Madden, executive director of USADA. "Today is a
great day for those athletes who want to compete on a level playing field."
Howard Jacobs, the attorney for Price and McEwen, said, "I talked to both of
them briefly today. They're both disappointed but they realized this was a
distinct possibility."
Two other American athletes who tested positive for THG last year await rulings
from USADA after their appeals are heard by arbitrators from the North American
Court of Arbitration for Sport. They are shot-putter Kevin Toth and middle
distance runner Regina Jacobs of Oakland, no relation to Howard Jacobs.
At 40, Jacobs' career likely would be over if she's suspended for two years. A
year ago she became the oldest woman to establish a world record when she ran
the indoor 1,500 meters in 3:59.98. Toth, 36, previously announced his
retirement from the sport; he unleashed a world-leading mark of 74 feet, 4 1/2
inches two months before his positive THG test in 2003.
U.S. anti-doping officials allege the THG came from BALCO, the Burlingame
laboratory of Victor Conte, who, along with three other men, was indicted on
federal charges of money laundering and distributing steroids and other banned
substances to elite athletes.
Sprinter Dwain Chambers of Great Britain, a client of Conte's, tested positive
for THG last summer and has been suspended for two years by his federation.
Chambers' competitive results from last August were thrown out Thursday by
track's world governing body, the IAAF.
In rejecting the appeals of Price and McEwen, the arbitration panel concluded
that, "The use of such a powerful anabolic steroid could be for no other purpose
than to enhance an athlete's performance in violation of the spirit and absolute
proscription of the IAAF doping rules."
Attorney Jacobs said he did not know if either athlete plans to return to
competition once the suspensions are up in 2006.
"Certainly they're young enough to do it," he said. "I know a lot of athletes'
initial response is they're not going to compete, but they are competitive
athletes. I've had athletes return from two-year suspensions and do phenomenally
well."
The suspensions of Price and McEwen come less than a week after The Chronicle
reported that investigators were told that a number of elite track athletes,
including sprinters Marion Jones and Tim Montgomery, received steroids from
Conte's Bay Area Laboratory Co-Operative.
In addition to the adjudication for Jacobs and Toth, still to be resolved are
the appeals of sprinters Kelli White of Union City and Calvin Harrison of
Salinas, both of whom tested positive last year for modafinil.
It is believed that Jacobs, Toth and White will have their appeals heard
sometime in May.
All told, 10 American track and field athletes tested positive for banned drugs
in the watershed summer of 2003, according to USADA. Seven came up positive for
modafinil and four for THG, with McEwen testing positive for both substances.
Modafinil use does not carry a ban from competition, which is why four athletes
recently accepted relatively mild sanctions for what is considered a stimulant
of the central nervous system.
Stanford graduate Chryste Gaines, a sprinter, and hurdlers Sandra Glover, Eric
Thomas and Chris Phillips received public warnings and were disqualified from
the competitions where their positive tests occurred in 2003 (the World
Championships for Phillips, U.S. nationals for Gaines, Glover and Thomas).
White and Harrison chose to file appeals with the North American arbitration
court because their consequences are greater.
White won the 100- and 200-meter dashes at last summer's World Championships in
Paris and would have earned $120,000 in prize money had she not tested positive
for modafinil.
Harrison tested positive for a stimulant in 1993. A second positive test for a
stimulant, in this case modafinil, could result in a two-year ban from
competition.
LOAD-DATE: April 30, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Chronicle Publishing Co.
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Hamilton Spectator (Ontario, Canada)
April 21, 2004 Wednesday Final Edition
Sports Notebook
SOURCE: Spectator wire services
SECTION: SPORTS; Pg. SP10
LENGTH: 1085 words
Hasek, Jagr and '98 Czech team subject of opera tribute
PRAGUE The Olympic champion Czech Republic hockey team is getting a curtain
call.
Dominik Hasek, Jaromir Jagr and the rest of the 1998 gold-medal winning hockey
team are the subjects of a new opera that re-enacts their victory at the Nagano
Olympics.
"Nagano," billed as "an opera in three periods and one overtime," is the first
Czech opera about a sports event.
Characters include Hasek, Jagr, Robert Reichel and Martin Rucinsky as well as
Vaclav Havel, the former anti-communist dissident turned Czech president.
The opera, based on a script written by Jaroslav Dusek, follows the final stages
of the Czech team's Olympic run and the celebrations afterward, during which a
chorus of fans yell Hasek is God and Hasek for president.
The Czechs defeated the United States and Canada before beating arch-rival
Russia to win their first Olympic title.
U.S. track and field athletes receive 'public warnings'
COLORADO SPRINGS, COLO. Four U.S. track and field athletes received public
warnings for using the stimulant modafinil, but they can compete at the Athens
Olympics and other events this year.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas tested
positive for modafinil at the U.S. championships in June. Hurdler Chris Phillips
tested positive at the world championships in August.
Thomas was stripped of his national championship in the 400-metre hurdles.
Last year modafinil was considered a minor stimulant that warranted only a
disqualification.
This year modafinil is classified as a serious stimulant by the World
Anti-Doping Agency and carries a two-year ban.
Sprint champion Kelli White is contesting her positive tests for modafinil at
the U.S. and world championships.
Spaniard Corretja sends defending champion home
MONTE CARLO Two-time defending champion Juan Carlos Ferrero was upset by fellow
Spaniard Alex Corretja in the first round of the Monte Carlo Masters yesterday.
Ferrero, the reigning French Open champion, lost 6-2, 6-3 in a match that lasted
just a little more than an hour.
Corretja broke Ferrero in his first service game and took leads of 3-0 in the
first set and 5-2 in the second.
In other first-round matches, former U.S. Open champions Lleyton Hewitt of
Australia and Marat Safin of Russia both rallied from a set down to win. Hewitt
beat Frenchman Julien Benneteau 3-6, 6-3, 6-4, while Safin got past Olivier
Rochus of France 4-6, 6-3, 6-3.
Organization and purse of Opens will improve for tennis fans
The U.S. Open Series will include 10 North American tennis tournaments -- six
men's and four women's -- leading up to the U.S. Open.
Players finishing in the top three in the new series will receive bonus money at
the U.S. Open in 2004 and 2005. The top male and female player in the series
will have 50 per cent added to their Open winnings in 2004, while their Open
take will be doubled in 2005.
Stacey Allaster, tournament director for this year's Tennis Masters Series in
Toronto, said the objective is to "try to create a more consistent platform for
fans to follow our sport."
She said the Canadian events will benefit from greater television coverage in
the U.S., making them more attractive to sponsors.
This year's series begins with the men's event in Los Angeles and the women's
tournament at Stanford, Calif., both the week of July 12-18.
Pipe-swinging attack leads to lifetime ban for boxer
MEXICO CITY A 17-year-old amateur Mexican boxer has been banned from the sport
for life after he was accused of attacking a fellow athlete with a metal pipe at
the national Olympic training centre, according to the national amateur boxing
federation.
Jorge Alfonso Montoya, 17, allegedly attacked Jose Andres Romero, 20, early
Monday in a dormitory. Romero's cheek bone was broken. Both had been preparing
for youth tournaments.
Amateur boxing officials said Montoya was apparently angry over a scuffle the
two had a week earlier.
Clarett tries another legal hip swivel to get into NFL draft
COLUMBUS, OHIO Maurice Clarett filed an emergency appeal with the U.S. Supreme
Court yesterday to try to force his way into this weekend's NFL draft.
Clarett's lawyer, Alan Milstein, asked for a stay of a decision by the 2nd U.S.
Circuit Court of Appeals preventing the former Ohio State tailback from entering
the draft.
Monday's decision put on hold a lower-court ruling that said the NFL can't force
players to wait three years after high school before turning pro.
Report says Old Trafford a target for terrorist bombing
MANCHESTER, ENGLAND Manchester United dismissed speculation yesterday that the
club's 67,000-seat Old Trafford stadium was a target for al-Qaeda terrorists.
British media reported that seven people arrested in anti-terrorist raids in the
Manchester area Monday were planning suicide bomb attacks at the soccer team's
high-profile Premier League game against Liverpool on Saturday.
Quoting unidentified police sources, the Sun tabloid said the suspected
terrorists had bought tickets for the game and planned to sit at various points
around the sold-out stadium before detonating bombs.
Police declined to comment on the reports.
"We're not getting involved in speculation," a Greater Manchester Police
spokeswoman said on condition of anonymity.
United spokesman Phil Townsend said the club had received no specific warnings
from police.
He said no special security arrangements were made for last night's game against
Charlton or Saturday's match against Liverpool.
Keane back in Irish lineup for friendly with Poland
DUBLIN Almost two years after walking out on the team at the World Cup, Roy
Keane was back on the Ireland squad Tuesday for a friendly against Poland.
The Manchester United star missed the 2002 World Cup in Korea and Japan after he
had a blazing argument with coach Mick McCarthy over the team's preparations and
training facilities.
He flew home while the team played on without him and reached the second round.
With McCarthy in charge, Keane refused to return to the Ireland fold. But he
announced last week that he was willing to play for the team under McCarthy's
successor, Brian Kerr.
Kerr named the vastly experienced but volatile midfielder in his squad to go to
Poznan for a friendly April 28.
That likely will upset Manchester United manager Sir Alex Ferguson, who believed
his injury-prone star would only play in World Cup qualifying games.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
GRAPHIC: Photo: Ian Hodgson, Reuters; A police officer on horseback stands guard
outside Manchester United's Old Trafford stadium after reports 10 terrorist
suspects had tickets to yesterday's game.
TYPE: Brief
Copyright 2004 Metroland Media Group Ltd
556 of 998 DOCUMENTS
National Post (Canada)
April 21, 2004 Wednesday National Edition
Track and Field: Modafinil warning issued
SOURCE: National Post news services
SECTION: Sports; Pg. S7
LENGTH: 65 words
Four U.S. track and field athletes received public warnings for using the
stimulant modafinil, but they can compete at the Athens Olympics and other
events this year. Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric
Thomas tested positive for modafinil at the U.S. championships in June. Another
hurdler, Chris Phillips, tested positive at the world championships in August.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
TYPE: Sports; Brief
Copyright 2004 National Post, All Rights Reserved
557 of 998 DOCUMENTS
The New York Post
April 21, 2004 Wednesday
THE SPORTS BLOTTER
SECTION: Sports+Late City Final; Pg. 83
LENGTH: 180 words
DROPPED: Prosecutors dropped assault charges against former heavyweight boxing
champion Joe Frazier yesterday after the alleged victim refused to testify.
Frazier was arrested after a domestic dispute in February and charged with
assaulting the mother of his 12-year-old son.
The case was scheduled to go to trial in Philadelphia yesterday, but prosecutors
said there was no way to move forward without testimony from the woman.
The alleged victim maintained all along that she would not cooperate.
STRIPPED: The U.S. Anti-Doping Agency stripped Eric Thomas of his national
400-meter hurdles title and reprimanded sprinter Chryste Gaines and hurdlers
Sandra Glover and Christopher Phillips for using the banned stimulant modafinil,
which was found in their systems following major competitions last year. They
remain eligible for the Summer Olympics in Athens.
Starting this year, athletes who test positive for modafinil will automatically
be banned from competition for two years.
ACQUITTED: Former Olympic boxer Tim Austin was acquitted of charges he raped a
16-year-old girl.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 N.Y.P. Holdings, Inc.
All Rights Reserved
558 of 998 DOCUMENTS
San Jose Mercury News (California)
April 21, 2004 Wednesday MORNING FINAL EDITION
DRUG REPRIMANDS HANDED OUT;
GAINES, THREE HURDLERS ACCEPT PENALTIES FOR POSITIVE TESTS
BYLINE: PETE CAREY, Mercury News
SECTION: SPORTS; Pg. 4D
LENGTH: 459 words
Four U.S. track athletes who tested positive for the mild stimulant modafinil
last year have accepted public warnings that leave them eligible to compete at
the Athens Olympics and any other event.
Sprinter Chryste Gaines and hurdlers Sandra Glover, Eric Thomas and Christopher
Phillips tested positive in 2003 for the drug, which is prescribed for sleep
disorders.
The sanction was announced by the U.S. Anti-Doping Agency. The athletes will
lose their results for the competitions at which they tested positive.
Gaines, Glover and Thomas failed their drug tests at the U.S. outdoor track and
field championships last summer at Stanford. Thomas loses a first-place finish
in the 400-meter hurdles, Glover a third in the 400 hurdles and Gaines a fifth
in the 100 dash.
Phillips loses a fifth-place finish in the 110 hurdles at the IAAF world
championships.
Sprinter Kelli White is still in the anti-doping agency's adjudication process
and probably will contest the finding before a panel of arbitrators. The Union
City athlete has continued to compete.
"I don't know how her case will be handled," said White's agent, Robert Wagner.
"I am sure they will make a right and fair decision. Let's leave it up to them."
White -- who says she took modafinil as treatment for narcolepsy -- could lose
gold medals in the 100 and 200 meters and $120,000 in prize money. She and
Gaines are coached by Remi Korchemny, one of four men indicted on charges of
distributing prescription drugs and illegal steroids to athletes through
Burlingame-based Balco Laboratories.
Calvin Harrison tested positive for modafinil at the U.S. track championships.
Because he tested positive once before for a stimulant found in cold medicines,
he faces a possible two-year ban from competition. His lawyers are in federal
court trying to expand the pool of arbitrators that could hear his case.
By accepting sanctions, the four athletes have put the issue behind them. Had
they contested the sanction, there was a small risk of a two-year sanction
depending on how USADA argued the case in arbitration, said Cameron Myler, the
lawyer for Gaines, Glover and Thomas.
The athletes decided they couldn't take that risk, Myler said.
Modafinil was not named on the IAAF's list of banned substances and is being
treated as a substance related to others on its list. Myler said her clients
didn't know it was banned.
Under the new World Anti-Doping Agency Code, which was adopted by the IAAF on
March 1, the penalty for a positive test for modafinil is a two-year ban from
competition. The athletes received only a public warning because the violations
took place last year, when the old IAAF rules called for only a public warning
for a first offense.
LOAD-DATE: August 24, 2005
LANGUAGE: ENGLISH
Copyright 2004 San Jose Mercury News
All Rights Reserved
559 of 998 DOCUMENTS
The Washington Post
April 21, 2004 Wednesday
Final Edition
Athletes Are Warned About Modafinil, but Can Compete
SECTION: Sports; D02
LENGTH: 232 words
Four U.S. track and field athletes received public warnings for using the
stimulant modafinil, but they can compete at the Athens Olympics and other
events this year.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas tested
positive for modafinil at the U.S. championships in June.
Another hurdler, Chris Phillips, tested positive at the world championships in
August.
Thomas was stripped of his national championship in the 400-meter hurdles.
The U.S. Anti-Doping Agency announced yesterday that all four accepted their
sanctions, including a public warning and forfeiting results from the event
where they tested positive.
In 2003, modafinil was considered a minor stimulant that warranted only a
disqualification. Starting this year, modafinil is classified as a serious
stimulant on the World Anti-Doping Agency banned list and carries a two-year
ban.
Sprint champion Kelli White is still contesting her positive tests for modafinil
at the U.S. and world championships. White, who could lose world titles in the
100 and 200, said she was prescribed modafinil for a sleeping disorder.
White and Gaines are coached by Remi Korchemny, who was charged in February with
distributing performance- enhancing drugs in the Bay Area Laboratory
Co-Operative case. Phillips said Korchemny gave him a modafinil pill for jet lag
at the world championships.
-- From News Services
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 The Washington Post
560 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
April 21, 2004, Wednesday
Athletes warned for using stimulant
SECTION: WORLD NEWS; SPORTS
LENGTH: 131 words
DATELINE: WASHINGTON, April 20
Four U.S. track and field athletes had been warned by the U.S. Anti-Doping
Agency Tuesday for using the stimulant modafinil, but still could compete in the
Athens Olympic Games this summer.
Eric Thomas, U.S. 400-meter hurdles champion, was tested positive for modafinil
at the U.S. championships last June, along with sprinter Chryste Gaines and
hurdler Sandra Glover.
Another hurdler, Chris Phillips, tested positive at the world championships in
August.
The four were striped of all their results at the competitions at which they
tested positive, but remain eligible for the Olympics.
Modafinil, the stimulant that Kelli White used at the world championships, is
classified as a serious stimulant on the World Anti-Doping Agency banned list
and carries a two-year ban.
LOAD-DATE: April 22, 2004
LANGUAGE: ENGLISH
COPYRIGHT 2004 XINHUA NEWS AGENCY
561 of 998 DOCUMENTS
The Associated Press
April 20, 2004, Tuesday, BC cycle
Four athletes get warning for stimulant use
SECTION: Sports News
LENGTH: 252 words
DATELINE: COLORADO SPRINGS, Colo.
Four U.S. track and field athletes received public warnings for using the
stimulant modafinil, but they can compete at the Athens Olympics and other
events this year.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas tested
positive for modafinil at the U.S. championships in June. Another hurdler, Chris
Phillips, tested positive at the world championships in August.
Thomas was stripped of his national championship in the 400-meter hurdles.
The U.S. Anti-Doping Agency announced Tuesday that all four accepted their
sanctions, including a public warning and forfeiting results from the event
where they tested positive.
In 2003, modafinil was considered a minor stimulant that warranted only a
disqualification. Starting this year, modafinil is classified as a serious
stimulant on the World Anti-Doping Agency banned list and carries a two-year
ban.
Sprint champion Kelli White is still contesting her positive tests for modafinil
at the U.S. and world championships. She expects an arbitration hearing next
month.
White, who could lose world titles in the 100 and 200, said she was prescribed
modafinil for a sleeping disorder.
White and Gaines are coached by Remi Korchemny, one of four men charged in
February with distributing performance-enhancing drugs. Phillips said Korchemny
gave him a modafinil pill at the world championships to help him overcome jet
lag.
Korchemny and his three co-defendants, including Barry Bonds' personal trainer,
pleaded innocent.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
562 of 998 DOCUMENTS
Associated Press Online
April 20, 2004 Tuesday
4 Athletes Get Warning for Stimulant Use
SECTION: SPORTS
LENGTH: 251 words
DATELINE: COLORADO SPRINGS, Colo.
Four U.S. track and field athletes received public warnings for using the
stimulant modafinil, but they can compete at the Athens Olympics and other
events this year.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas tested
positive for modafinil at the U.S. championships in June. Another hurdler, Chris
Phillips, tested positive at the world championships in August.
Thomas was stripped of his national championship in the 400-meter hurdles.
The U.S. Anti-Doping Agency announced Tuesday that all four accepted their
sanctions, including a public warning and forfeiting results from the event
where they tested positive.
In 2003, modafinil was considered a minor stimulant that warranted only a
disqualification. Starting this year, modafinil is classified as a serious
stimulant on the World Anti-Doping Agency banned list and carries a two-year
ban.
Sprint champion Kelli White is still contesting her positive tests for modafinil
at the U.S. and world championships. She expects an arbitration hearing next
month.
White, who could lose world titles in the 100 and 200, said she was prescribed
modafinil for a sleeping disorder.
White and Gaines are coached by Remi Korchemny, one of four men charged in
February with distributing performance-enhancing drugs. Phillips said Korchemny
gave him a modafinil pill at the world championships to help him overcome jet
lag.
Korchemny and his three co-defendants, including Barry Bonds' personal trainer,
pleaded innocent.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
563 of 998 DOCUMENTS
Associated Press Worldstream
April 20, 2004 Tuesday
Four athletes get warning for stimulant use
SECTION: SPORTS
LENGTH: 254 words
DATELINE: COLORADO SPRINGS, Colorado
Four U.S. track and field athletes received public warnings for using the
stimulant modafinil, but they can compete at the Athens Olympics and other
events this year.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas tested
positive for modafinil at the U.S. championships in June. Another hurdler, Chris
Phillips, tested positive at the world championships in August.
Thomas was stripped of his national championship in the 400-meter hurdles.
The U.S. Anti-Doping Agency announced on Tuesday that all four accepted their
sanctions, including a public warning and forfeiting results from the event
where they tested positive.
In 2003, modafinil was considered a minor stimulant that warranted only a
disqualification. Starting this year, modafinil is classified as a serious
stimulant on the World Anti-Doping Agency banned list and carries a two-year
ban.
Sprint champion Kelli White is still contesting her positive tests for modafinil
at the U.S. and world championships. She expects an arbitration hearing next
month.
White, who could lose world titles in the 100 and 200, said she was prescribed
modafinil for a sleeping disorder.
White and Gaines are coached by Remi Korchemny, one of four men charged in
February with distributing performance-enhancing drugs. Phillips said Korchemny
gave him a modafinil pill at the world championships to help him overcome jet
lag.
Korchemny and his three co-defendants, including baseball slugger Barry Bonds'
personal trainer, pleaded innocent.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
564 of 998 DOCUMENTS
The Associated Press State & Local Wire
These materials may not be republished without the express
written consent of The Associated Press
April 20, 2004, Tuesday, BC cycle
Four track athletes get public warning for stimulant use
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 326 words
Four U.S. track and field athletes have received public warnings for using the
stimulant modafinil during 2003 competitions, but all remain eligible for this
summer's Athens Olympics and other events.
Sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas all tested
positive for modafinil at the U.S. championships last June. Another hurdler,
Chris Phillips, tested positive at the world championships in August.
The U.S. Anti-Doping Agency said Tuesday all four had accepted their sanctions,
which includes a public warning and the forfeiture of all results from the
competition at which they tested positive. As a result, Thomas loses his U.S.
championship in the 400-meter hurdles.
At the time of their positive tests, modafinil was considered a minor stimulant
warranting only a disqualification. Starting this year, modafinil is classified
as a serious stimulant on the World Anti-Doping Agency banned list and carries a
two-year ban.
Sprint champion Kelli White is still contesting her positive tests for modafinil
at both the U.S. and world championships, and expects to have an arbitration
hearing next month.
White, who faces the loss of world championship gold medals in the 100 and 200
meters, said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
White and Gaines are coached by Remi Korchemny, one of four men charged in
February with distributing performance-enhancing drugs to professional athletes.
Phillips said Korchemny gave him a modafinil pill at the world championships to
help him overcome jet lag.
Korchemny and his three co-defendants - Bay Area Laboratory Co-Operative founder
Victor Conte, BALCO vice president James Valente and Greg Anderson, the personal
trainer for baseball slugger Barry Bonds - have pleaded innocent to all charges
in the drug distribution case.
LOAD-DATE: April 21, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
565 of 998 DOCUMENTS
Espicom Business Intelligence
April 14, 2004
Cephalon receives broad label for Provigil in UK
LENGTH: 161 words
Cephalon has received marketing approval in the UK to expand the label of
Provigil (modafinil) tablets [C-IV] to include the treatment of excessive
sleepiness in patients with chronic pathological conditions, including
narcolepsy, obstructive sleep apnoea/hypopnoea syndrome and moderate-to-severe
chronic shift work sleep disorder. Cephalon is planning to launch the new
indication later in April and the company anticipates additional approvals for
expanded indications for modafinil in Europe during 2004.
Modafinil is the first in a new class of wake-promoting agents believed to work
through the sleep-wake centres to activate the cortex of the brain. The
medication currently is approved in more than 20 countries under several
brandnames. Provigil was originally approved in the UK in 1998 for the treatment
of narcolepsy, and in 2002, for the treatment of excessive daytime sleepiness
associated with obstructive sleep apnoea/hypopnoea syndrome.
LOAD-DATE: April 15, 2004
LANGUAGE: ENGLISH
Copyright 2004 ESPICOM Business Intelligence Ltd.
566 of 998 DOCUMENTS
PR Newswire
April 13, 2004 Tuesday
Cephalon Receives Broad Label for PROVIGIL in the United Kingdom
SECTION: FINANCIAL NEWS
LENGTH: 797 words
DATELINE: WEST CHESTER, Pa. April 13
Cephalon, Inc. (Nasdaq: CEPH) announced that it has received marketing approval
in the United Kingdom to expand the label of PROVIGIL(R) (modafinil) Tablets
$(C-IV$) to include the treatment of excessive sleepiness in patients with
chronic pathological conditions, including narcolepsy, obstructive sleep
apnea/hypopnea syndrome and moderate to severe chronic shift work sleep
disorder. Cephalon UK Limited is planning to launch the new indication later
this month.
"This UK approval and the recent U.S. approval are significant milestones in our
global regulatory strategy," said Dr. Paul Blake, MB, FRCP, Senior Vice
President of Clinical Research and Regulatory Affairs at Cephalon. "We
anticipate additional approvals for expanded indications for modafinil in Europe
this year."
John Dawson, Vice President, Pharmaceutical Operations Europe, added: "This
broader indication offers us a tremendous opportunity to address the unmet needs
of many patients with excessive sleepiness and to accelerate our already strong
sales growth in the European market."
PROVIGIL
PROVIGIL is the first in a new class of wake-promoting agents believed to work
through the sleep-wake centers to activate the cortex of the brain. The
medication currently is approved in more than 20 countries under several brand
names. PROVIGIL initially was approved in the United Kingdom in 1998 for the
treatment of narcolepsy, and in 2002, for the treatment of excessive daytime
sleepiness associated with obstructive sleep apnea/hypopnea syndrome.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs more than 1,600 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England,
Martinsried, Germany, and Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at www.cephalon.com or by calling 1-800-896-5855.
Cephalon UK Limited has headquarters in Guildford and markets drugs to treat a
number of central nervous system disorders. In collaboration with Novartis
Pharma AG, Cephalon UK markets Tegretol(R) (carbamazepine), Ritalin(R)
(methylphenidate), Anafranil(R) (clomipramine) and Lioresal(R) (baclofen). Also
included in this collaboration is PROVIGIL for the UK and Ireland. In addition,
Cephalon UK markets GABITRIL(R) and ACTIQ(R) in the UK and Ireland.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
guidance, and other statements regarding matters that are not historical facts.
You may identify some of these forward-looking statements by the use of words in
the statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
SOURCE Cephalon, Inc.
CONTACT: Media: Sheryl Williams, +1-610-738-6493, swilliam@cephalon.com, or
Investors: Robert (Chip) Merritt, +1-610-738-6376, cmerritt@cephalon.com, both
of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: April 14, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association, Inc.
567 of 998 DOCUMENTS
Agence France Presse -- English -- English
April 8, 2004 Thursday
White to appear at doping hearing in May: IAAF
SECTION: Sports
LENGTH: 146 words
DATELINE: PARIS, April 8
American sprinter Kelli White could be called to appear "around May 18th" at a
hearing for her positive dope test for modafinil in June of last year, the
athletics world ruling body IAAF said Thursday.
According to an IAAF spokesperson, the United States Anti-Doping Agency (USADA)
plans to convene all American athletes who are concerned with positive dope
tests for the banned substances modafinil or THG (tetrahydrogestrinone) between
"mid-April and May 25".
White, along with six other athletes, tested positive for modafinil during the
American national championships in June 2003.
White's agent, Robert Wagner, said he has no news about the date of her hearing
but said White - who won the 100 and 200 metre titles in Paris at last year's
world championships - could return to competition at Mexico on May 22.
ep/cyb/jd/dj04
Athletics-USA-White-doping
LOAD-DATE: April 9, 2004
LANGUAGE: ENGLISH
Copyright 2004 Agence France Presse
568 of 998 DOCUMENTS
Pharma Marketletter
March 18, 2004
Cephalon's Provigil shows promise in schizophrenia
LENGTH: 131 words
Researchers from the department of Psychiatry at the University of Cambridge,
UK, have shown that Cephalon's narcolepsy drug Provigil (modafinil) may produce
cognitive enhancement in schizophrenia patients. The study found that, after
taking a tablet of modafinil, subjects performed significantly better at memory
tests involving short-term memory and, importantly, showed improved mental
flexibility, a core deficit normally oberved in patients with schizophrenia,
noted the scientists. However, they also point out that these results need to be
confirmed in long-term studies with modafinil. The agent is currently approved
in more than 20 countries, including the USA, for the treatment of excessive
daytime sleepiness associated with narcolepsy (Marketletters passim).
LOAD-DATE: March 18, 2004
LANGUAGE: ENGLISH
Copyright 2004 Marketletter Publications Ltd.
569 of 998 DOCUMENTS
World Markets Analysis
February 26, 2004
Ranbaxy Receives Tentative FDA Approval for Modafinil Tablets
BYLINE: Sacha Baggili
SECTION: IN BRIEF
LENGTH: 204 words
India's Ranbaxy Laboratories has announced tentative approval from the US Food
and Drug Administration (FDA) for a generic version of US company Cephalon's
Provigil (modafinil), a treatment for the improvement of wakefulness in people
with excessive daytime sleepiness associated with narcolepsy. Asia Pulse reports
that the Indian firm's modafinil tablets will be made available to pharmacies
throughout the US once final approval has been granted. Sales and marketing of
the product will be backed by the generic company's wholly-owned US subsidiary
Ranbaxy Pharmaceutical Inc.
Significance: This tentative approval comes just a few weeks after Barr
Laboratories (US) received a similar FDA nod for generic modafinil in 100mg and
200mg strengths. According to Asia Pulse, the total market value for modafinil
tablets is estimated at around US$297m. As with Barr's provisional approval, a
transition to full approval is contingent on the outcome of litigation currently
pending over the branded drug's patent status; however, the case is not due to
be heard before January 2005. Despite this, Ranbaxy's early move on this drug
illustrates the company's increasingly raised profile on the US generics market.
LOAD-DATE: February 26, 2004
LANGUAGE: ENGLISH
Copyright 2004 World Markets Research Limited;
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Asia Pulse
February 23, 2004 Monday
INDIA'S RANBAXY LABS GETS USFDA APPROVAL FOR MODAFINIL
SECTION: Northern Territory Regional
LENGTH: 116 words
DATELINE: NEW DELHI, Feb 23
Ranbaxy Laboratories (BSE:RANB) on Monday said it has received tentative
approval from US Food and Drug Administration to manufacture and market
Modafinil tablets, a generic of Cepahalon's Provigil.
Sales and marketing of the product will be supported by Ranbaxy Pharmaceutical
Inc, a wholly-owned subsidiary of Ranbaxy Laboratories, and will be made
available to all pharmacy outlets located throughout the US after final approval
is granted by USFDA, a company statement said here.
Modafinil is indicated to improve wakefulness in patients with excessive daytime
sleepiness associated with narcolepsy.
Total market for Modafinil tablets is estimated at US$297 million.
(PTI)
LOAD-DATE: February 24, 2004
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Espicom Business Intelligence
February 23, 2004
Ranbaxy granted tentative FDA approval for modafinil
LENGTH: 88 words
On 8th February, Ranbaxy Laboratories received tentative FDA approval to
manufacture and market modafinil tablets in 100 and 200mg strengths. Currently
marketed by Cephalon as Provigil, modafinil is indicated to improve wakefulness
in patients with excessive daytime sleepiness associated with narcolepsy.
Ranbaxy's product will be made available to all pharmacy outlets located
throughout the US, including chain and independent pharmacies, wholesalers and
generic distributors, at the time final FDA approval is granted.
LOAD-DATE: February 24, 2004
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The Press Trust of India
February 23, 2004 Monday
Ranbaxy Labs gets tentative USFDA approval for Modafinil
SECTION: Nationwide International News
LENGTH: 122 words
DATELINE: New Delhi, Feb 23
Ranbaxy Laboratories, one of the major pharmaceutical companies in India, on
Monday said it has received tentative approval from US Food and Drug
Administration to manufacture and market Modafinil tablets, a generic of
Cepahalon's Provigil.
Sales and marketing of the product will be supported by Ranbaxy Pharmaceutical
Inc, a wholly-owned subsidiary of Ranbaxy Laboratories, and will be made
available to all pharmacy outlets located throughout the US after final approval
is granted by USFDA, a company release said here.
Modafinil is indicated to improve wakefulness in patients with excessive daytime
sleepiness associated with narcolepsy.
Total market for Modafinil tablets is estimated at 297 million dollar.
LOAD-DATE: February 23, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Press Trust of India
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PR Newswire
February 20, 2004 Friday
Ranbaxy is Granted Tentative Approval for the Manufacturing and Marketing of
Modafinil
SECTION: FINANCIAL NEWS
LENGTH: 396 words
DATELINE: JACKSONVILLE, Fla. Feb. 20
Ranbaxy Pharmaceuticals Inc. (RPI), a wholly owned subsidiary of Ranbaxy
Laboratories Limited (RLL), announced today that RLL has received tentative
approval from the U.S. Food and Drug Administration, Office of Generic Drugs, to
manufacture and market Modafinil Tablets in 100 mg and 200 mg strengths. Total
market sales for Provigil(R) (Modafinil) tablets were $297 million (IMS - MAT:
December 2003).
Modafinil is indicated to improve wakefulness in patients with excessive daytime
sleepiness associated with narcolepsy.
Sales and marketing for this product will be supported by the Ranbaxy
Pharmaceuticals Inc. Sales and Marketing Team. Product will be made available to
all pharmacy outlets located throughout the U.S. including chain and independent
pharmacies, wholesalers, and generic distributors at the time final approval is
granted by the U.S. FDA.
"When approved, this product will provide a CNS product to RPI's expanding
product portfolio, along with our commitment to bring affordable generic
alternatives to the U.S. healthcare system," according to Jim Meehan, Vice
President of Sales and Marketing for RPI.
Ranbaxy Pharmaceuticals Inc. ("RPI") based in Jacksonville, Florida, is the
wholly owned subsidiary of Ranbaxy Laboratories Limited ("RLL"), India's largest
pharmaceutical company. RPI is engaged in the sale and distribution of generic
and branded prescription products in the U.S. healthcare system.
Ranbaxy Laboratories Limited, India's largest pharmaceutical company,
manufactures and markets branded generic pharmaceuticals and Active
Pharmaceutical Ingredients. Ranbaxy's continued focus on R&D has resulted in
several approvals in developed markets and significant progress in New Drug
Discovery Research.Ranbaxy's foray into Novel Drug Delivery Systems has led to
proprietary "platform technologies" resulting in a number of products under
development. The Company is selling its products in over 70 countries and has an
expanding international portfolio of affiliates, joint ventures and alliances,
ground operations in 34 countries and manufacturing operations in 7 countries.
* Provigil(R) is a registered trademark of Cephalon
SOURCE Ranbaxy Pharmaceuticals Inc.
CONTACT: Charles M. Caprariello, Vice President, Business Development, Ranbaxy
Pharmaceuticals Inc., +1-609-720-5615; Janine Lang of RF Binder Partners,
+1-212-994-7525, for Ranbaxy
URL: http://www.prnewswire.com
LOAD-DATE: February 21, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association, Inc.
574 of 998 DOCUMENTS
The Age (Melbourne, Australia)
February 18, 2004 Wednesday
National Edition
Email link to White drugs scandal;
DRUGS IN SPORT
BYLINE: Jacquelin Magnay
SECTION: SPORT; Pg. 19
LENGTH: 435 words
Sydney
Balco laboratory president Victor Conte knew several months before world sprint
champion Kelli White tested positive to the stimulant modafinil that the drug
was on the banned list for sports.
White is facing the loss of her two Paris world championship medals and being
stripped of the 100 metres and 200 metres titles because of a positive test to
modafinil, a drug she claims was used to treat the medical condition narcolepsy.
But on June 8, 2003, two months before White tested positive, an unnamed
international track and field coach sent Conte an email warning him of the new
anti-doping list, which specified modafinil, and suggesting that unknown numbers
of athletes had been using an old, but specially made, designer steroid.
White's coach is Remi Korchemny, who along with Conte and two others has been
charged in the United States with distribution of illegal drugs.
The unnamed coach wrote in the email: "As you can see at the stimulant list,
modafinil is on it!!! Of course after (US drug tester Don) Catlin's norbolethone
detection this AAS is also included. I guess the party is over."
US federal agent Jeff Novitzky said the steroid norbolethone was first
synthesised in 1966 and is not marketed by a pharmaceutical company, leading him
to conclude that the steroid had been manufactured by an unauthorised source.
Only one competitor has been caught using norbolethone.
Balco is at the centre of the steroid tetrahydragestrinone (THG) and it is
believed it manufactured several other undetectable steroids.
The email raises questions as to why White, who is linked to Conte through
Korchemny, was not told about the developments. Another of Korchemny's
sprinters, Chryste Gaines, has also tested positive to modafinil.
At the time of the world championships, modafinil was classified a minor
stimulant, but it now attracts a two-year ban.
The email also indicates that Conte had an inside informant, tipping him off
about drug-testing developments.
In August 2002, he wrote to an international track and field coach: "I need for
you to advise xxx to discontinue using the clear (a code word for steroids). I
recently found out that . . . xxx, xxx and xxx sent a sample of the clear to the
IOC testers on an anonymous basis.
"I will be getting more information shortly regarding exactly when they will be
testing for it . . . We might also want to somehow get this information to the
coach for the Greek athletes xxx and xxx so that nobody tests positive."
Meanwhile, officials have confirmed that US shot putter Kevin Toth tested
positive for THG and modafinil at the 2003 US championships in June.
LOAD-DATE: June 18, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 The Age Company Limited
All Rights Reserved
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The Age (Melbourne, Australia)
February 18, 2004 Wednesday
Late Edition
Email link to White drugs scandal;
DRUGS IN SPORT
BYLINE: Jacquelin Magnay
SECTION: SPORT; Pg. 19
LENGTH: 438 words
Sydney
Balco laboratory president Victor Conte knew several months before world sprint
champion Kelli White tested positive to the stimulant modafinil that the drug
was on the banned list for sports.
White is facing the loss of her two Paris world championship medals and being
stripped of the 100 metres and 200 metres titles because of a positive test to
modafinil, a drug she claims was used to treat the medical condition narcolepsy.
But on June 8, 2003, two months before White tested positive, an unnamed
international track-and-field coach sent Conte an email warning him of the new
anti-doping list, which specified modafinil, and suggesting that unknown numbers
of athletes had been using an old, but specially made, designer steroid.
White's coach is Remi Korchemny, who along with Conte and two others has been
charged in the United States with distribution of illegal drugs.
The coach wrote in the email: "As you can see at the stimulant list, modafinil
is on it!!! Of course after (US drug tester Don) Catlin's norbolethone detection
this AAS is also included. I guess the party is over."
US federal agent Jeff Novitzky said the steroid norbolethone was first
synthesised in 1966 and is not marketed by a pharmaceutical company, leading him
to conclude that the steroid had been manufactured by an unauthorised source.
Only one competitor has been caught using norbolethone.
Balco is at the centre of the steroid tetrahydragestrinone (THG) and it is
believed it manufactured several other undetectable steroids.
Another of Korchemny's sprinters, Chryste Gaines, has also tested positive to
modafinil.
At the time of the world championships, modafinil was classified a minor
stimulant, but it now attracts a two-year ban.
The email also indicates that Conte had an inside informant, tipping him off
about drug-testing developments.
In August 2002, he wrote to an international track-and-field coach: "I need for
you to advise xxx to discontinue using the clear (a code word for steroids). I
recently found out that . . . xxx, xxx and xxx sent a sample of the clear to the
IOC testers on an anonymous basis.
"I will be getting more information shortly regarding exactly when they will be
testing for it . . . We might also want to somehow get this information to the
coach for the Greek athletes xxx and xxx so that nobody tests positive."
· Cricket could lose its Federal Government funding and elite development
programs if it failed to comply with a world standard anti-doping code by
January, a senate committee was told yesterday. Cricket is currently receiving
$900,000 over three years from the Australian Sports Commission.
LOAD-DATE: June 18, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
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Sydney Morning Herald (Australia)
February 18, 2004 Wednesday
Late Edition
Why White should have known;
DRUGS IN SPORT
BYLINE: Jacquelin Magnay
SECTION: SPORT; Pg. 34
LENGTH: 446 words
BALCO laboratory president Victor Conte knew several months before world sprint
champion Kelli White tested positive to the stimulant Modafinil that the drug
was on the banned list.
White is facing the loss of her Paris world championship gold medals for the 100
metres and 200m because of a positive test to Modafinil, which she claims she
used to treat narcolepsy .
But on June 8, 2003, two months before White tested positive, an unnamed
international track and field coach sent Conte an email warning him of the new
anti-doping list, which specified Modafinil, and suggesting that unknown numbers
of athletes had been using an old but specially made designer steroid.
White's coach is Remi Korchemny, who with Conte and two others has been charged
in the US with distribution of illegal drugs including steroids, growth hormone
and erythropoietin .
The unnamed coach wrote in the email: "As you can see at the stimulant list
Modafinil is on it!!! Of course after [US drug tester Don] Catlin's Norbolethone
detection this AAS is also included. I guess the party is over."
Federal agent Jeff Novitzky said the steroid norbolethone was first synthesised
in 1966 but not marketed by a pharmaceutical company, leading him to the
conclusion that it had been manufactured by a clandestine, unauthorised source.
Only one athlete, a female cyclist, has been caught using norbolethone. BALCO is
accused of manufacturing another steroid, tetrahydrogestrinone (THG) and it is
believed it made several other undetectable designer steroids.
The email raises questions as to why White, linked to Conte through Korchemny,
was not told about the list. Another of Korchemny's sprinters, Chryste Gaines ,
also tested positive to Modafinil.
At the time of the world championships Modafinil was classified a minor
stimulant, but it now attracts a two-year ban.
The email correspondence also indicates that Conte had an inside informant,
tipping him off about drug testing developments.
In August 2002 he wrote to an international coach: "I need for you to advise
[name deleted] to discontinue using the clear [a code word for steroids]. I
recently found out that [three names deleted] sent a sample of the clear to the
IOC testers on an anonymous basis. This is very unfortunate.
"We might also want to somehow get this information to the coach for the Greek
athletes [two names deleted] so that nobody tests positive."
Officials have confirmed that US shot putter Kevin Toth tested positive for THG
and Modafinil at the 2003 US championships in late June. Toth says he will now
retire, but continues to dispute the results. Europe's fastest man, Dwain
Chambers, will have his THG drugs hearing on Friday.
LOAD-DATE: July 17, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2004 John Fairfax Publications Pty Ltd
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577 of 998 DOCUMENTS
The Associated Press
February 16, 2004, Monday, BC cycle
USOC: Shot putter Kevin Toth tested positive for THG, modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 494 words
American shot put champion Kevin Toth tested positive for the newly discovered
steroid THG and the stimulant modafinil at the U.S. championships and faces a
two-year suspension, the U.S. Olympic Committee announced Monday.
Toth is one of four athletes who flunked THG tests during the meet last June at
Stanford. The others were middle-distance runner Regina Jacobs, hammer thrower
John McEwen and hammer thrower Melissa Price. Jacobs and Price also won titles
at that national meet.
The 36-year-old Toth, of Hudson, Ohio, shocked the track and field world with a
throw of 74 feet, 4 1/2 inches at the Kansas Relays in April - the best
performance in the world in 13 years. His winning throw at the national
championships was 69-7 1/2.
The USOC said Toth also tested positive for THG during an out-of-competition
test on July 27, 2003, a month after winning his first U.S. title.
Toth is disputing the THG test results through the U.S. Anti-Doping Agency's
arbitration process, as are McEwen and Price. Jacobs has gone outside the USADA
process, filing an arbitration claim with the American Arbitration Association.
All four face two-year bans if the positive tests are upheld. Final decisions on
their cases are expected this spring.
European 100-meter champion sprinter Dwain Chambers also tested positive last
year for THG and faces a two-year ban.
THG was unveiled when a track coach sent a syringe with the substance to the
USADA last summer. That coach said the substance came from Victor Conte, founder
of the Bay Area Laboratory Co-Operative, a nutritional supplements lab in
Burlingame, Calif.
Conte was one of four men named in a 42-count indictment last week that charges
they participated in a steroid-distribution ring that provided drugs to dozens
of top athletes. All four men pleaded innocent on Friday. Conte has said he was
not the source of the syringe provided to the USADA.
Toth was one of dozens of athletes who appeared before a grand jury probing
BALCO last fall.
In addition to the four U.S. athletes who tested positive for THG at the
national championships, the USOC has announced in recent months that several
athletes tested positive for modafinil at that meet.
Those athletes include Kelli White, whose positive test for modafinil at the
world championships means she likely will be forced to forfeit her 100- and
200-meter gold medals. Another is Calvin Harrison, whose flunked test could
affect several U.S. teammates.
It is a second drug violation for Harrison, who also tested positive for the
stimulant pseudoephedrine at the 1993 U.S. junior indoor championships and
served a three-month suspension. As a repeat offender, he would face a two-year
ban.
That means Harrison should not have been eligible for last summer's world
championships, at which he ran the opening leg on the winning U.S. 1,600-meter
relay team. And that means the U.S. squad could lose its gold medal from that
relay.
LOAD-DATE: February 17, 2004
LANGUAGE: ENGLISH
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578 of 998 DOCUMENTS
The Associated Press
February 16, 2004, Monday, BC cycle
USOC: Toth tested positive for THG, modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 437 words
American shot put champion Kevin Toth tested positive for the steroid THG and
the stimulant modafinil at the 2003 national championships and could be
suspended for two years, the U.S. Olympic Committee announced Monday.
Toth is one of four athletes who flunked THG tests during the U.S. championships
in June. The others, announced earlier, were Regina Jacobs, John McEwen and
Melissa Price.
Jacobs and Price also were national champions.
All four face two-year bans if the positive tests are upheld. Final decisions on
their cases are expected this spring.
Later Monday, agent John Nubani announced Toth was retiring, though he still
plans to go through with the appeals process.
Toth stunned the track and field world with a throw of 74 feet, 4 1/2 inches at
the Kansas Relays in April - the best performance in the world in 13 years. His
winning throw at the national championships was 69-7 1/2.
The USOC said Toth also tested positive for THG during an out-of-competition
test in July.
Toth, McEwen and Price are disputing the THG test results through the U.S.
Anti-Doping Agency's arbitration process. Jacobs instead filed a claim with the
American Arbitration Association.
"We're contesting the charges, and the case will proceed through the USADA
process," said Toth's attorney, Howard Jacobs, no relation to Regina.
European 100-meter champion Dwain Chambers also tested positive last year for
THG and faces a two-year ban. He will appear before a UK Athletics disciplinary
panel Thursday.
Toth was one of dozens of athletes who appeared before a grand jury probing a
nutritional supplements lab.
The lab's founder and Barry Bonds' personal trainer were among four people
indicted last week on charges they participated in a steroid-distribution ring
that provided drugs to top athletes. All four pleaded innocent Friday.
The USOC has announced in recent months that several athletes tested positive
for modafinil at the U.S. championships, including Kelli White and Calvin
Harrison.
White's positive test for modafinil at the world championships means she
probably will lose 100- and 200-meter gold medals.
Harrison's flunked test could affect several U.S. teammates. He also tested
positive for the stimulant pseudoephedrine at the 1993 U.S. junior indoor
championships and served a three-month suspension. As a repeat offender, he
would face a two-year ban.
That means Harrison should not have been eligible for last summer's world
championships, at which he ran the opening leg on the U.S. 1,600 relay team.
That means the relay team members could lose their gold medals.
LOAD-DATE: February 17, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photos CAPS104-105
Copyright 2004 Associated Press
All Rights Reserved
579 of 998 DOCUMENTS
The Associated Press State & Local Wire
February 16, 2004, Monday, BC cycle
USOC: Toth tested positive for THG, modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 437 words
American shot put champion Kevin Toth tested positive for the steroid THG and
the stimulant modafinil at the 2003 national championships and could be
suspended for two years, the U.S. Olympic Committee announced Monday.
Toth is one of four athletes who flunked THG tests during the U.S. championships
in June. The others, announced earlier, were Regina Jacobs, John McEwen and
Melissa Price.
Jacobs and Price also were national champions.
All four face two-year bans if the positive tests are upheld. Final decisions on
their cases are expected this spring.
Later Monday, agent John Nubani announced Toth was retiring, though he still
plans to go through with the appeals process.
Toth stunned the track and field world with a throw of 74 feet, 4 1/2 inches at
the Kansas Relays in April - the best performance in the world in 13 years. His
winning throw at the national championships was 69-7 1/2.
The USOC said Toth also tested positive for THG during an out-of-competition
test in July.
Toth, McEwen and Price are disputing the THG test results through the U.S.
Anti-Doping Agency's arbitration process. Jacobs instead filed a claim with the
American Arbitration Association.
"We're contesting the charges, and the case will proceed through the USADA
process," said Toth's attorney, Howard Jacobs, no relation to Regina.
European 100-meter champion Dwain Chambers also tested positive last year for
THG and faces a two-year ban. He will appear before a UK Athletics disciplinary
panel Thursday.
Toth was one of dozens of athletes who appeared before a grand jury probing a
nutritional supplements lab.
The lab's founder and Barry Bonds' personal trainer were among four people
indicted last week on charges they participated in a steroid-distribution ring
that provided drugs to top athletes. All four pleaded innocent Friday.
The USOC has announced in recent months that several athletes tested positive
for modafinil at the U.S. championships, including Kelli White and Calvin
Harrison.
White's positive test for modafinil at the world championships means she
probably will lose 100- and 200-meter gold medals.
Harrison's flunked test could affect several U.S. teammates. He also tested
positive for the stimulant pseudoephedrine at the 1993 U.S. junior indoor
championships and served a three-month suspension. As a repeat offender, he
would face a two-year ban.
That means Harrison should not have been eligible for last summer's world
championships, at which he ran the opening leg on the U.S. 1,600 relay team.
That means the relay team members could lose their gold medals.
LOAD-DATE: February 17, 2004
LANGUAGE: ENGLISH
GRAPHIC: AP Photos CAPS104-105
Copyright 2004 Associated Press
All Rights Reserved
580 of 998 DOCUMENTS
Associated Press Worldstream
February 16, 2004 Monday
USOC: Toth tested positive for THG, modafinil
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 438 words
DATELINE: SAN FRANCISCO
American shot put champion Kevin Toth tested positive for the steroid THG and
the stimulant modafinil at the 2003 national championships and could be
suspended for two years, the U.S. Olympic Committee said.
Toth is one of four athletes who flunked THG tests during the U.S. championships
in June. The others, announced earlier, were Regina Jacobs, John McEwen and
Melissa Price.
Jacobs and Price also were national champions.
All four face two-year bans if the positive tests are upheld. Final decisions on
their cases are expected this spring.
Later Monday, agent John Nubani announced Toth was retiring, though he still
plans to go through with the appeals process.
Toth stunned the athletics world with a throw of 22.67 meters (74 feet, 4 1/2
inches) at the Kansas Relays in April - the best performance in the world in 13
years. His winning throw at the national championships was 21.22 meters (69-7
1/2).
The USOC said Toth also tested positive for THG during an out-of-competition
test in July.
Toth, McEwen and Price are disputing the THG test results through the U.S.
Anti-Doping Agency's arbitration process. Jacobs instead filed a claim with the
American Arbitration Association.
"We're contesting the charges, and the case will proceed through the USADA
process," said Toth's attorney, Howard Jacobs, no relation to Regina.
European 100-meter champion Dwain Chambers also tested positive last year for
THG and faces a two-year ban. He will appear before a UK Athletics disciplinary
panel Thursday.
Toth was one of dozens of athletes who appeared before a grand jury probing a
nutritional supplements lab.
The lab's founder and Barry Bonds' personal trainer were among four people
indicted last week on charges they participated in a steroid-distribution ring
that provided drugs to top athletes. All four pleaded innocent Friday.
The USOC has announced in recent months that several athletes tested positive
for modafinil at the U.S. championships, including Kelli White and Calvin
Harrison.
White's positive test for modafinil at the world championships means she
probably will lose 100- and 200-meter gold medals.
Harrison's flunked test could affect several U.S. teammates. He also tested
positive for the stimulant pseudoephedrine at the 1993 U.S. junior indoor
championships and served a three-month suspension. As a repeat offender, he
would face a two-year ban.
That means Harrison should not have been eligible for last summer's world
championships, at which he ran the opening leg on the United States 4x400 relay
team. That means the relay team members could lose their gold medals.
LOAD-DATE: February 17, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
581 of 998 DOCUMENTS
The San Francisco Chronicle
FEBRUARY 13, 2004, FRIDAY, FINAL EDITION
Drugs involved in BALCO case
BYLINE: Keay Davidson
SECTION: NEWS; Pg. A23
LENGTH: 938 words
Here is a look at some of the performance-enhancing drugs named in Thursday's
indictment of BALCO founder Victor Conte and others for alleged involvement in a
widespread drug distribution ring:
-- Erythropoietin, or EPO
Commercially sold as Epogen, erythropoietin (EPO) improves the ability of red
blood cells to transport oxygen. It is a favorite of some athletes in endurance
sports.
Erythropoietin is a hormone naturally produced by the kidneys and liver. When
oxygen levels are abnormally low, the kidneys respond by manufacturing
erythropoietin, which stimulates the bone marrow into producing more red blood
cells. Erythropoietin also spurs the production of hemoglobin, the
oxygen-carrying molecule within red blood cells.
Doctors can spot kidney disease, bone marrow disease and illegal use of Epogen
by testing a patient's blood levels of erythropoietin. The drug's legitimate
uses include treating anemia, a deficiency in the body's ability to transport
oxygen.
-- Human growth hormone, or HGH
Human growth hormone's legitimate medical uses include treatment of children
diagnosed as pituitary dwarfs, although even these legal uses can have dangerous
side effects, according to the U.S. Food and Drug Administration.
In theory, HGH builds muscle mass. However, some scientists have questioned
whether human growth hormone builds muscle mass enough to benefit athletes. Some
studies suggest that the muscles of athletes who take the hormone don't grow
bigger than those in a control group given a placebo.
Researchers have long struggled to develop techniques for identifying human
growth hormone in athletes' blood or urine. A new diagnostic technique will most
likely be available in time for this year's Athens Olympics.
-- Modafinil
A mild stimulant, modafinil is typically prescribed as a treatment for
narcolepsy and other sleep disorders. It is marketed under the name Provigil.
Some organizers of athletic competitions seem to view modafinil more benignly
than they do other drugs. Several U.S. track and field athletes have recently
tested positive for modafinil, such as double World Champion Kelli White.
But in November, in an interview with The Chronicle, Dick Pound, chair of the
World Anti-Doping Agency, spoke caustically of the drug's users. "It is a
stimulant," he stressed. "You look at the excuse given -- narcolepsy? Please. So
(the athlete) wouldn't fall asleep in the starting blocks in the 100 meters? Oh,
please.
"You live by the sword, you die by the sword. How would you feel if your
daughter got beat by Kelli White by a hundredth of a second?"
-- Testosterone cream
In males, the natural production of the hormone testosterone surges at puberty.
It tends to decline with age, especially after age 50. The hormone is
responsible for development of primary and secondary male physical
characteristics, including genitalia, fat distribution, and muscle and bone
mass.
Testosterone can give athletes an edge by helping them trim body fat and build
up muscles. It can be injected, applied as a patch to the skin, or rubbed as a
cream onto the arms and torso. Cream applications are considerably less
effective than injections.
-- Tetrahydrogestrinone, or THG
THG is a designer steroid whose effects are probably similar to related classes
of anabolic steroids.
THG users become bigger and stronger, but it has side effects: Men become more
feminine, and women become more masculine. It will make women grow hair on their
face and make men more bald. A man's testicles will shrink and his breasts grow,
while a woman's breasts will get smaller.
For now, routine tests for detecting anabolic steroids are blind to THG.
However, Dr. Don Catlin, director of the UCLA Olympic Analytical Laboratory in
Los Angeles, and other researchers are developing ways to detect THG in
athletes' urine.
--------------------------------------
STEROID PRIMER
The sports doping scandal playing out before a federal grand jury in San
Francisco focuses on elite athletes' use of performance-enhancing drugs,
particularly a previously undetectable anabolic steroid called THG. Athletes use
such steroids to get bigger, stronger and faster, but health experts say there
is a risk to users.
HOW STEROIDS WORK
Blood carries steroid to muscle
Steroid is drawn toward muscle cell's wall and attaches to a receptor
Steroid enters cell nucleus, interacts with chromosomes
Nucleus sends out information to increase protein production, which strengthens
muscle.
WAYS OF TAKING STEROIDS
Oral steroids
Pill or liquid taken daily
Steroid is absorbed by stomach
Steroids travel to liver and enter the blood stream
Injectable steroids
last longer than oral and are injected into thigh or buttocks
Dose enters blood for several days
Blood carries steroid into body
Other methods: Inhaler and skin patch
SIDE EFFECTS
-- Men:
Shrinking of testicles
Reduced sperm count
Impotence
Hair loss
Enlarged breasts
-- Women:
Facial hair appears
Voice deepens
Breasts shrink
Menstruation disrupted
Male-pattern baldness
-- Both sexes:
Acne
High blood pressure
Increased cholesterol level
Jaundice
Aggressiveness
Weight gain
Blood clots
Increased body hair
HEALTH RISKS
Heart disease
Caused by the increase in cholesterol
Liver damage
Principal site for oral input of steroids. Makes liver vulnerable to damage and
tumors
Tendon ruptures
Muscle tissue strengthens faster than tendons, elevating the risk for damage
Sources: Associated Press; Bantam Medical Dictionary; Chronicle research
LOAD-DATE: February 13, 2004
LANGUAGE: ENGLISH
GRAPHIC: GRAPHIC, John Blanchard / The Chronicle
Copyright 2004 The Chronicle Publishing Co.
582 of 998 DOCUMENTS
FD (Fair Disclosure) Wire
February 12, 2004 Thursday
Event Brief of Q4 2003 Cephalon, Inc. Earnings Conference Call - Final
LENGTH: 6224 words
CORPORATE PARTICIPANTS
. Robert Grupp, Cephalon, Inc., VP, Corporation Communications . Frank Baldino,
Cephalon, Inc., Chairman & CEO . Kevin Buchi, Cephalon, Inc., SVP & CFO . Robert
Roche, Cephalon, Inc., SVP, Pharmaceutical Operations . Paul Blake, Cephalon,
Inc., SVP, Clinical Research and Regulatory Affairs . John Osborn, Cephalon,
Inc., SVP, General Counsel and Secretary
OVERVIEW
CEPH reported 2003 sales of $685.3m and an adjusted EPS of $1.54. The co.
secured an expanded US label for Provigil to treat apnea, shift work sleep
disorder and narcolepsy. EPS guidance for 2004 is expected to be $2.00 per
share, up 30% over 2003. Q&A Focus: new indication for Provigil, GM,
international sales, CEP-1347, tax rate, Actiq, Gabatril and product sales.
FINANCIAL DATA
A. Key Data From Call 1. Total Revenues 2003: $714.8m, up 41% over 2002. 2.
Product sales 2003: $685.3m, up 47% over 2002. 3. SG&A 2003: $252m. 4. R&D 2003:
$170.3m, or 24% of revenues. 5. Cash balance as of Dec. 31: $1.2b.
PRESENTATION SUMMARY
S1. Business Overview (F.B.) 1. 4Q03 and 2003 Results: 1. 2003 was the most
profitable year ever. 2. Total prescriptions and sales for Provigil, Actiq and
Gabitril reached record levels. 3. 2003 Sales: $685.3m. 4. EPS: adjusted diluted
net income per share was $1.54, surpassing co. guidance. 5. Provigil sales: grew
at compound annual rate of over 40% over the last three years. 1. Gabitril was
60%, Actiq was 110% in same period. 2. European operations: 1. Expanded Provigil
with a sleep apnea indication in UK, Germany and Ireland. 2. These expanded
labels drove ex-US Provigil sales, up by 60% over 2002. 3. Clinical Research in
2003: 1. Secured an expanded US label for Provigil to treat apnea, shift work
sleep disorder and narcolepsy. 1. Provigil is the first drug for these
disorders. 2. ADHD: 1. Results from a 248-patient study of ADH in children were
reported at American Psychiatric Association's annual meeting in May. 1.
Reported statistically significant results with one daily dose of Provigil. 2.
Investigated Gabitril for the treatment of anxiety, insomnia, and neuropathic
pain. 1. Goal was to demonstrate effectiveness in one of these disorders; it may
be effective in treating all three. 3. Doubled total number of publications for
marketed products. 4. Received FDA approval for a new Actiq formulation. 1.
World-wide production is being carried out at Salt Lake City facility. 4. 2004
Outlook: 1. Expect strong year. 2. Expanded sales force will call on approx.
double the number of doctors in 2003. 3. Will move beyond specialty physician
universe. 4. Clinical Research: 1. Will conduct numerous registrations studies
in several areas. 5. Pipeline: 1. Neurogenerative disease: Cep-1347 inhibits
cell-signaling pathways. 1. Will complete enrollment for an 800-patient clinical
trial evaluating Cep 1347 for treatment of Parkinson's disease. 1. This has the
potential to be the first drug to mitigate the death of neurons in Parkinson's
disease. 2. Publications concerning this drug are authored by co. and by other
academic labs, such as NIH. 6. Other programs: 1. Label expansions for existing
products: 1. Modafinil study for ADHD application is underway. 2. Should be
completed by mid-year, with data available by year end. 2. R-modafinil: 1.
Enrolling patients in three clinical trials for R-modafinil for the treatment
narcolepsy and obstructive sleep apnea. 1. This formulation has longer duration
of action than Provigil . 2. With approval, it will be a once-a-day wakeness
medicine. 3. Will also study potential drug interaction. 2. Studying the role of
R-modafinil in improving cognitive function. 1. Several publications have
addressed the positive affects of R-modafinil on cognition. 2. Collaborating
with a UK co. to study R-modafinil 's affects on attention, information
processing, working and long-term memory. 3. Goal is to support submission of an
NDA at end of 2004. 3. Gabitril Development: 1. Could potentially treat anxiety,
insomnia and neuropathic pain. 2. Two large 200+ patient studies in generalized
anxiety disorder and post-traumatic stress disorder should be completed in 2Q04.
3. Pending positive results, will begin a larger clinical program in 2H04 to
evaluate Gabitril for one of these anxiety states. 4. It may be effective for
insomnia and neuropathic pain. 1. Co. will evaluate these applications as well,
starting with insomnia patients in 2004. 2. An earlier study showed it decreases
wake after sleep onset and increased slow-wave sleep. 4. Co. expects the
combined impact of its R&D program will transform the co. 1. ADHD, R-modafinil,
sugarfree Actiq, Gabitril anxiety and Gabitril insomnia represent a significant
increase over the previous level of R&D. 1. 2003: 1200 patients were enrolled in
clinical programs. 2. 2004: approx. 3000 patients are expected to be enrolled.
3. In 2004 the topline data will become available to the investment community.
5. Believe that beginning 2006, the co. will achieve even more significant
growth. 7. Cima Labs Transaction: 1. Complying with Federal Trade Commission's
request for more information. 2. Co. believes it will get FTC clearance to close
the transaction. 3. The HSR process makes it difficult to predict the timing of
the closing.
S2. Financial Overview (K.B.) 1. 4Q03 and 2003: 1. Total Revenues 2003: $714.8m,
up 41% over 2002. 2. Product sales 2003: $685.3m, up 47% over 2002. 3. Sales by
product: 1. Provigil: $290.5m. 2. Actiq: $237.5m. 3. Gabitril: $63.7m. 4. Other
European product sales: $93.6m. 4. Prescription metrics: 1. Provigil 2003: 1.4m
prescriptions filled in US, up 31% over 2002. 2. Provigil 4Q03: 398,000, more
than 30,000 a week. 3. Actiq 2003: 326,000 in 2003, up 76% over 2002. 4. Actiq
4Q03: 97,000, more than 7400 per week. 5. Gabitril 2003: 680,000, up 53% over
2002. 6. Gabitril 4Q03: 196,000, more than 15,000 per week. 7. Physicians are
exploring new uses for Gabitril, including anxiety, insomnia and neuropathic
pain. 8. US channel inventory levels: flat. 5. SG&A 2003: $252m, reflecting
investment and enhanced marketing. 6. R&D 2003: $170.3m or 24% of revenues. 1.
Drivers: Research on Cep-1347 for Parkinson's disease, Modafinil for ADHD, R-
modafinil for excessive sleepiness, and Gabitril for anxiety, insomnia and
neuropathic pain. 7. Fully diluted GAAP EPS in 2003: $1.44. 8. Retired the
balance of 5.25% convertible debt and a portion of 3.875% debt. 1. Total cash
outlays: $192m. 2. These early retirements resulted in pre-tax charges of $9.8m.
3. Excluding these 3Q03 charges, the adjusted fully diluted 2003 EPS is $1.54
vs. guidance of $1.52. 9. Cash balance as of Dec. 31: $1.2b. 2. 2004 Guidance:
1. Reiterating 2004 guidance. 2. Total product sales: expected $900-950m in
sales. 1. Provigil sales: expected $375-425m. 2. Actiq sales: expected
$325-375m. 3. Gabitril sales: expected $80-90m. 4. Other product sales: expected
$80-90m. 3. SG&A: expected $320-330m. 4. R&D: expected $250-270m. 5. EPS:
expected $2.00 per share, up 30% over the $1.54 in 2003. 3. 1Q04 guidance: 1.
Product sales: expected $210-215m. 2. Diluted EPS: $0.28 per share, up 33% over
$0.21 YoverY. 3. This does not include impact of the pending CIMA transaction.
4. Expect increased sales throughout 2004 and flat expenses, resulting in
greater EPS as the year progresses. 5. Will no longer provide sales guidance for
individual products. 1. With comparable margins for the three products, the
product sales mix in any qtr. is not relevant to profitability.
QUESTION AND ANSWER SUMMARY
Q1. (Cory Davis, JP Morgan) My question is on the new indication for Provigil
and if we're trying to gauge when you might see an uptake in the growth rate for
Provigil as a function of the new roll-out. The question would be, how many
times does the sales rep have to hit a new doctor before they write one
prescription and how long is that period of time, a month, couple of months or
weeks?
A. (Kevin Buchi) Well Cory, I'm going to pass that question over to Bob Roche
who built and reconstructed the sales force to address that very issue. So Bob,
won't you answer Cory's question.
A. (Robert Roche) We are really excited about the prospects that the new label
has for Provigil and we expect to see a positive evolution for the product
throughout 2004 and very importantly, beyond that as well. We've already seen
good growth in the first month of the year, we're about 30 percent over where we
were last year and that's right in line with our expectations for 2004. And now
we've got this big new sales organization in the field actually operating today.
We're about three or four months ahead of where we were last year at this point
in time and I'm very confident that we're going to be seeing the positive
affects of that as well as of our marketing operations right throughout the rest
of 2004 and beyond.
Q2. (Cory Davis, JP Morgan) And I'll ask Kevin a question on the gross margin, I
know you gave pretty detailed guidance for '04 but always want a little bit
more. Directionally is it going to be - should it be up or down over this
quarter?
A. (Kevin Buchi) I think the expectation here, Cory, is it's going to be
relatively flat.
Q3. (Cory Davis, JP Moran) And last question, can you just break out the
international sales on all three products for the quarter?
A. (Kevin Buchi) Sure, I'd be happy to. For the fourth quarter, Provigil sales
U.S. 78 million dollars. Provigil sales international 7.4. Actiq sales U.S. 71.9
million dollars, international 1.3. Gabitril U.S. 18 million dollars,
international 1.2. And of course the other is all international, 24.7. That
should give you total U.S. 167.9, total international 34.6.
Q4. (Cory Davis, JP Morgan) If there's any thoughts that you guys have on the
Lundbeck/Gaboxadol deal with Merck and any parallels that that product may have
to Gabitril in insomnia?
A. (Kevin Buchi) Well, first of all, I think it's a good deal between Lundbeck
and Mercks, I'm happy for them. Gaboxadol is a different kind of compound, just
to remind you that that's a directing acting agonist on the GABA-A receptor.
It's nice to know that other people believe that the GABA [indiscernible] is a
great target for pharmaceutical development so I think that deal underscores
that concept. There's other GABA agonists that have been developed over the
years, as you might remember way back when when the GABA-B agonist, Baclophin
[phonetic] was developed. We like the more of a modulatory approach to the GABA
ergics system. If you look back in the history at the benzodiazaphines and older
drugs that have been very successful in that category and today looking at the
Ambiens and Neurontins and that category, of course, Gabatril are real
modulators of the GABA ergic system and not direct acting agonists and we're
very comfortable with that approach, given the history and given what we've seen
in our clinical data.
Q5. (Matt Geller, CIBC WorldMarkets) Frank, could you talk a little bit about
what you've seen thus far with Armadaphin patients. A little bit about - go into
a little more detail about what kind of safety and efficacy benefits maybe
you've seen already. And also can you talk a little bit about your strategy for
switching people over from Provigil to Armadaphenol [phonetic] and why you think
it will be successful
A. (Frank Baldino) I'm going to hand this over to Paul Blake to answer the
specific data questions now. But just to remind you that I did show data at the
JP Morgan conference that I think was picked up by the analysts, Cory did a
great job of reporting on the data that he saw, this Pharmacokinetic data,
there's Efficacy's data and I'll pass it over to Paul Blake to give you some
more details.
A. (Paul Blake) The big difference that we're looking to see in the Phase III
program that's underway now, that we've seen in the earlier work, is in duration
of effect. As you may recall, Provigil is arrasinate and the bulk of the dose
interval is due to the RIsomer, giving the RIsomer alone with SES we will see a
longer duration of wakefulness. We've seen that in general and we've seen it
specifically in sleep deprived people. A very similar side effect profile to
Provigil, as you would expect, and the other different that we're going to look
to explore is the potential for different drug interaction patent, hopefully
with a lesser effect and a lower number of specific instances in the warning
section of the new label that we're going to write.
A. (Frank Baldino) The other question you asked, Matt, was about the switching
program for patients from Provigil to Armadaphenol when that does get approved,
and I'll ask Bob to talk about what his thoughts in that program at this very
early stage.
A. (Robert Roche) And it is indeed an early stage but the plan, Matt, as I know
you're aware, is that we will be able to bring the RIsomer, Armadaphenol to the
marketplace probably by the end of next year or early 2006 at the latest. And
with the benefits that Paul has just described, I'm quite confident and our
market research indicates that there will be a real tendency on the physician's
part and on payer's parts as well to move towards the new product. Now this all
has to be borne out in the clinical development program and through the
regulatory process but we're very confident that we can get patients onto
Armadaphenol from Provigil when we choose to do so.
A. (Frank Baldino) Just to remind you Matt, that the - there is no competition
out there for Provigil. One thing to remember is all the switches we have data
on that have been successful are in the context of a lot of competitve products.
The most recent example that's been very, very well done by Forest with their
[indiscernible] selexa. Remember, they've done a really great job with that.
They also did it in the context of seven competitive agents and a generic Prozac
that's on the market today. We have a little bit of an advantage in our
switching program, is that we are the only manufacture of Provigil out there, we
have the only wakefulness promotor in the world and we certainly don't intend to
compete against ourself in this process. So I hope that helps your thinking
along those lines.
Q6. (David Buck, Buckingham Research) The first question is for Paul Blake on
CEP1347 since Frank made a point of highlighting it. Can you give us a refresher
on the protocol in this study that you're expecting to complete enrollment this
year and again what the milestones are in that study and what's the duration of
that study will be? And just a couple of housekeeping questions for Kevin, could
you give us the interest to add back for the convert and can you give us a sense
of sales force size right now and are we - do we have all the additions that we
were planning?
A. (Frank Baldino) Let's start with Paul answering your first question because
you can always come back with some others.
A. (Paul Blake) David, 1347 is being developed as a neuro protective agent in
the treatment of patients who have early symptoms of Parkinson's Disease. And
the primary end point is a delay in the need for the physician to institute
dopamenergic therapy for that patient. We're looking to get 800 patients
through to two years of therapy and we're using 64 sights in the U.S. and Canada
with the help of the Parkinson's study group who are the leading experts in this
area in consortia type studies in Parkinson's Disease. We've agreed to this
protocol with the FDA and we've agreed it with their Canadian equivalents and
this a North American, not just a U.S. study. Each patient has a chance to be
randomized to one of three active doses that they take twice a day or placebo.
Between screening and randomization, they're all flown to an imaging center in
New Haven, Connecticut associated with Yale University and they're all imaged in
the same unit on the same machinery by the same team for spect - measurement of
their dopamenergic transporter activity. As I said at randomization and at two
years or if possible at any point if that occurs earlier. We're coming close to
recruiting the 800th patient in the first half of this year. We have a planned
interim analysis when 200 patients get to one year of treatment which will be
around the turn of the first and second quarter next year. And if all remains
well then, as we expect and the science still in this blinded study are good, we
should finish that up two years after the 800th patient goes in which will be in
the first half of 2006. Does that answer the - this 1347 question for you?
Q7. (David Buck, Buckingham Research) Yes, it does. And just a couple of
housekeeping for Kevin, just the interest add back and on sales force are we at
the 500 level and can you give us some sense of timing of sales and promotional
spending for the year?
A. (Frank Baldino) Yeah, let's get the interest add back from Kevin and then
I'll pass you over to Bob for the sales force answer.
A. (Kevin Buchi) The interest add back for the fourth quarter was 2.3 million
dollars, which can easily add back to the full year was 8.4 million.
Q8. (David Buck, Buckingham Research) And would that be constant into the first
quarter?
A. (Frank Baldino) It should be, yeah. And Bob?
A. (Bob Roche) Yeah, and - we are at full capacity in the sales force. Right now
we have all the territories filled, managerial slots filled and are going into
our national sales meeting in the next couple of weeks, after which the actual
launch of the new expanded label will take place.
Q9. (David Buck, Buckingham Research) And timing of expenses throughout the
year?
A. (Bob Roche) I would expect that expenses are going to be relatively flat
throughout the year, David.
Q10. (Mike King, Bank of America Security) I was wondering, Bob Roche, could you
talk about what kind of prelaunch activities you're doing now with sales force
training, CME programs and the like of that to get aggressive about marketing
the new label?
A. (Robert Roche) We have really jacked up the Provigil promotional expense
number for 2004 to reflect the terrific opportunity the new label provides us.
And we actually began the process of market sensitization and working with
primary care physicians the middle of last year and then began a process which
had primary care docs meeting with psychiatrists, learning about the product and
so forth through medical education kind of peer-to-peer influencing strategy
sessions that have now been going on for over six months. The premarketing of
the product from a marketing perspective has also been going on for quite some
time. But as we've just received approval for the new label and just now
finalizing all the promotional materials which of course have to be prereviewed
and so forth and advertising campaign and that sort of thing, that will all be
coming together and being pushed out along with the sales force launch of the
product in early March.
Q11. (Mike King, Bank of America Security) Early March, okay. And so the first
meeting where we should see some new material - marketing materials and such
would be what, APA?
A. (Robert Roche) Yes, whichever is first, the APA or the APSS or ANA and I'm
not quite sure which is which, I can check that for you.
A. (Frank Baldino) Mike, I think it's usually the ANA meeting end of April and
then rolling into the psychiatric meetings in May and then the fleet meetings
later in June.
Q12. (Mike King, Bank of America Security) And then just a quick finance
question, the shelf that you announced recently, what's the purpose of that?
A. (Kevin Buchi) We have no current intentions to issue any additional
securities, Mike, as you know a shelf just gives you the flexibility in the
event that you need to raise monies, that it gives you the ability to go and do
it quickly. And that would principly from our perspective be around, as you can
imagine transactions where we're still aggressively looking for additional
products to add to our portfolio, additional companies that have products, those
types of things.
Q13. (Mike King, Bank of America) But more for product acquisition as opposed to
taking out higher coupon debt?
A. (Kevin Buchi) Well, as you know, the two and a half percent debt is callable
at par at the end of this year, that is a potential use of it for sure.
A. (Frank Baldino) But for the record, Mike, to repeat what Kevin initially
said, we have no plans to issue any securities at the moment.
Q14. (Eric Schmidt, SG Cowan) Kevin, looking for a little bit of help on the tax
rate for '04, directionally?
A. (Kevin Buchi) I think we're expecting at this point in time the tax rate for
'04 to be about 36 percent, which would be consistent with the '03 tax rate.
Q15. (Eric Schmidt, SG Cowan) And then Bob, I know you've taken great pains not
to cause any sales force disruption as you've gone through this expansion
period. Any feedback from the sales force in that regard? Scripts have been a
little bit sluggish on Actiq over the last couple of months.
A. (Bob Roche) Yeah, well we aboslutely have done everything in our power to
minimize any sales force disruption but when you implement a change of this
magnitude, you're always going to get something. I think the important message
is that whatever we would have anticipated is already behind us or we expect
that it's behind us. We really began this sales force build out in September of
last year and trained and put into the field about 150 new sales reps at the end
of December. We've just fielded another 50 new people in the last couple of
weeks so if there is any disruption to the process, I'm really confident that
it's behind us and we're moving forward very, very positively.
Q16. (Mark Goodman, Morgan Stanley) Bob, could you talk a little bit about Actiq
and just the different patient populations that we're treating now? Like how
many patients were treated with Actiq this year? How many new patients are you
seeing and the new patient populations that it's moving into? And then Frank,
can you just maybe talk about the Cima deal just a little bit. I mean is there
anything incremental that you can help us with to better understand what's
happening there?
A. (Kevin Baldino) I'm going to answer the question first so Bob can get his -
he can dig out some of the numbers that you were asking for. I think you're -
is your question why we didn't do, Mark, or....
Q17. (Mark Goodman, Morgan Stanley) No, no, no, of course not. No, I know
exactly why you did it. I'm just saying like from the FTC's perspective, like
what - have you learned anything new that you can help us with just to better
understand what they're thinking right now?
A. (Kevin Baldino) Yeah, I wish I could tell you that the - we are hot and heavy
in discussions with the FTC on these major issues. But I think fundamentally FTC
takes time. The timing of our filing wasn't necessarily prudent because it was
during the Christmas holidays and they couldn't even get any meetings together
there. So there's been some of that kind of delay and they really haven't
brought any substantive issues to the floor. We hope to get an audience with
them in the near term that would help this out. Now on the phone with us, he
couldn't be with us today, is John Osborn. Maybe John could provide some color
for you Mark, he's much more closely aligned with this process than I am. But
John, are you there?
A. (John Osborn) I mean I don't think there's anything that's particularly
unusual about this, it's - we made our filing, it was as Frank said, in the
midst of a holiday period. We have had some preliminary discussions with the FTC
and we've been providing documents as you do when you go through this process. I
think it - it's not parciularly surprising to see that they've wanted to take a
bit of time in looking at this, they're always interested in pharmaceutical
industry acquisition. And there's a relationship between OS and Actiq that's
been commented upon. But having said that, I think it's going reasonably well.
We've had frequent contact with them and we're pretty confident that, although
as Frank said earlier, you can never predict the precise timing of it, we're
pretty confident that we're moving in the right direction that we are answering
the concerns that they have and that we're going to get clearance and be able to
move forward with the deal.
A. (Kevin Baldino) Mark, your question about Actiq, do you want to repeat that
just so the audience will remember what it was?
Q18. (Mark Goodman, Morgan Stanley) Yeah, I mean basically Bob, I'm just trying
to understand how many patients have been taking Actiq now? How many new
patients came in during this past year? What types of patients are they? Just so
I can understand, are we broadening it to new populations and just try to
understand what's going on in Actiq.
A. (Bob Roche) Yeah, I mean Actiq is really a remarkable asset and it surprises
even us I think by how well it continues to do quarter after quarter, year after
year. We grew prescriptions, Mark, in 2003 by over 75 percent to well over
325,000. Now this would probably translate to somewhere around 30 to 40,000,
maybe a little more patients than that treated during the course of the year. So
you can figure that that's probably 75 percent greater than what we treated in
the year 2002. So we're really making terrific progress there. On average, at
the beginning of 2003 around 2,500 physicians per month were writing
prescriptions for Actiq. By the end of the year that was over 4,000. So really
significant growth in the prescriber base and what they're using it for is a mix
of cancer pain and non-malignant pain. We're getting additional useage because
of Fentonal is really a well understood pain fighting utility and in a wide
variety of areas and we're now beginning to explore these a little more
systematically from a clinical perspective as well. Does that - did that answer
the question more or less?
Q19. (Mark Goodman, Morgan Stanley) Yes.
Q20. (Louis Webb, WR Hambreck) Yes, a question for Frank. Assuming a late 2005
approval of Armadaphenal, you would agree that the original formulation would be
phased out over a period of a few months. And the second part would be is there
any reason that you'd continue to market the original?
A. (Frank Baldino) Well, the second part of your question is about marketing the
original, don't forget we did sell the Racmid [phonetic] in Europe which is a
different environment, as you well know, so we'll continue to do that. Also the
Racmid will be used in the new proprietary formulation that we're selling to
patients with - the doctors for the indication with ADHD provided that approval
is there at that time. So yes, we'll be selling it in that context. But
regarding the switch to the R, we're going to switch this as fast as practicably
possible. And again, we're not going to compete against ourselves and it's a
pretty straight-forward approach we're going to use to do this, nothing out of
the ordinary. You slow down the manufacture of one and put the other one in
place and go forward with it and make sure all of the elements of the supply
chain know what's going on and they're properly informed of the process and
educated as to the process as we continue. I don't know if that answers your
question?
Q21. (Louis Webb, WR Hambreck) Yes, that's clear, thanks.
Q22. (Jim Birchnell, Lehman Brothers) Just a maintenance question to start with,
I just want to see if we should expect the same EPS distribution relative
quarter by quarter that we had in '03 and '04?
A. (Paul Blake) Yes, I would. That's certainly the path that we set with the
first quarter guidance, yes.
Q23. (Jim Birchnell, Lehman Brothers) And then I think you mentioned that we
should expect expenses to be flat throughout the year but I know in the past
we've had front end weighted expenses for SG&A around conferences, front end
weighted. Is there a change there or shall we expect the same distribution there
as well?
A. (Paul Blake) No, I think overall I'd expect expenses to be fairly flat
throughout the year, you may see some front end weighting of the SG&A and some
back end weighting of the R&D. But I think generally it's going to be - overall
I would expect it to be relatively flat.
Q24. (Jim Birchnell, Lehman Brothers) And then just looking at product sales
going into the first quarter, it seems like sequentially, I mean it's relatively
flat, four to five percent sequential growth. Is that just territory realingment
or is there a seasonal aspect that we tend to see in the first quarter?
A. (Frank Baldino) Bob, do you want to answer that question?
A. (Bob Roche) You're talking about growth from December into January, Jim?
Q25. (Jim Birchnell, Lehman Brothers) Just from fourth quarter '03 to first
quarter '04, it seems like we're growing sequentially four percent or so and
that seems a little flatish versus what we've seen previously.
A. (Bob Roche) Well don't forget, I mean the only data that exists thus far for
first quarter '04 are a couple of - well, four weekly prescription numbers from
IMS. And as I mentioned earlier, it means those numbers are well up on where we
were last year and right within our expectations. Q4 '03 grew for Provigil,
about six percent on Q3 '03, for Gabatril it grew about 11 percent on Q3 '03,
and for Actiq it grew - the prescription numbers grew by about seven percent. So
I mean I - if we can generate that kind of sequential quarter on quarter growth
and we certainly believe that we will do that and probably more, then we're
certainly making the numbers that we've put forward for you guys today.
A. (Frank Baldino) But clearly there's certainly a - you have to consider some
impact of the sales force realignment and all of that and I think the good news,
after our experience last year, that in our calculus for the guidance we
provided and our calculus for the expectations that we have for the quarter, we
figured - we factored that in.
Q26. (Jim Birchnell, Lehman Brothers) And then just one final question with
perhaps some evolving focus on Gabatril. Do you have a sense of what the
distribution of scripts are in terms of whether you're getting business right
now from GAD and how much versus use in epilepsy and other indications? And
could we expect data like that as the year progresss?
A. (Frank Baldino) We are happy to share that kind of data with you, Jim. The
most recent data set that I have in front of me today is from September of 2003
for Gabatril where we're expecting the fourth quarter data to come in any day.
But where we are at the end of 200 - and September '03, and it probably isn't
going to change a whole lot was neuropathic pain was about 17 percent of the
total Gabitril prescribing activity, up from about 11 percent in the same period
of 2002, so September of 2002. Anxiety, depression and other psychiatric
disorders made up well over 60 percent of the total Gabatril prescribing by
September '03 and that was up from about 50 percent in 2002. Epilepsy was around
15 percent of total Gabitril prescribing, up from - pardon me, down from around
30 percent in the previous year.
A. (Bob Roche) I mean clearly we're following the positions of Utility
[phonetic] here. I mean they are the ones who pointed us in the direction of
anxiety and that's why the trials are going on. So it's not surpising
distribution is as it is.
Q27. (Steve Slaughter, UBS) Frank, I'd just be interested in what you thought of
the label now that the final approved text is out for the expanded label on
Provigil. Anything in there that was a surprise and I guess one specific
question, the comment on the label that prescribers should be aware that
patients may not acknowledge sleepiness or drowsiness unless directly questioned
about drowsiness or sleepiness, which kind of begs the question not short term
but maybe intermediate term or perhaps with the R, is there a DTC opportunity
with an expanded label for this product or the follow on?
A. (Frank Baldino) Well Steve, first of all regarding the label and I'll have
Paul comment specifically on your question and I'll answer the other part of
your question so it gives him time to think about the answer for you. But we're
pretty excited about this label. I mean being first in this category in the
United States is a big deal, it allows us to continue to develop the franchise
as we expected to and we've got just about everything we need to in the label to
have a big impact on this product in this patient population. Regarding - Paul,
do you have a specific answer to his question on that one - in the label about
sleepiness?
A. (Paul Blake) Yes, I think that's a very pragmatic and realistic statement
that you could apply to many drugs and many diseases, that most people sadly are
not cured completely in every instance by every drug. And while people may feel
better, it's a reasonable public health caution just to make sure they check and
say am I completely normalized or do I still need to be careful. So I think it's
something that's reasonable and logical that we're very comfortable with. In
terms of are we surprised by anything in the label, I think given the
negotiation period and review period and comments that we've had, in the end we
weren't surprised at all. If we look back through the whole process, we might
say we're a little surprised that the broadest label wasn't granted given that
was something we were encouraged to seek by the agency rather than the specific
one but we're very happy with the way its come out and I think it's supported by
the data wonderfully.
Q28. (Steve Slaughter, UBS) And Paul, thank you for that. I'm just wondering
maybe a question for Bob, is there an opportunity for direct to consumer
advertising? If patients aren't necessarily highlighting for a physician then
sleepiness or drowsiness if they experience for example in shift work
situations, is there a targeted way to heighten the awareness in the patient's
eyes with some type of DTC down the road?
A. (Bob Roche) I think somewhere down the road, Steve, there may absolutely be.
We do not - we don't have that in our immediate plans, what we're doing for the
first six to nine months of this at least is going out there and making sure
that physicians understand the importance of sleepiness in their patient
populations because not a great deal of time and effort is being put on sleep
issues per se, in med school or thereafter and so there's a lot of education
that has to happen with the docs before we would consider going to the patients.
But there's enough opportunity here I think for us to certainly consider doing
both at some point in time.
A. (Frank Baldino) Yeah, I think Steve, the message we get from the major
players, a lesson learned from the majors out there, is that you don't want to
go too early with DTC and you, being a guy who was in the field selling your
products know this more than anybody, you don't want to DTC ad out there before
the doctors really understand the drug, what they're prescribing, what its
limitations are because they don't like to be surprised, like any other
profession doesn't like to be surprised. And especially when you have first in
class drug, the first label ever for these indications. So we're - it will be
something we pursue going forward once we increase the base of understanding
amongst the largest group of prescribers, the general practitioner going
forward.
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LOAD-DATE: February 27, 2004
LANGUAGE: ENGLISH
Transcript 021204so.765
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583 of 998 DOCUMENTS
The San Francisco Chronicle
FEBRUARY 8, 2004, SUNDAY, FINAL EDITION
LETTERS TO THE GREEN
SECTION: SPORTS; Pg. B2; LETTERS TO THE GREEN
LENGTH: 538 words
Korchemny responds to USATF story
Editor -- On Saturday, Jan. 31, The Chronicle published an article entitled
"USATF removes local coach" that contained some misinformation. The article
stated that Remi Korchemny "gave the stimulant modafinil to some of the athletes
he coaches, including Kelli White and Chryste Gaines."
That is incorrect information and I would like to set the record straight. First
of all, modafinil has not been scientifically determined to be a stimulant.
In fact, many credible scientists at major universities, including Stanford,
have published that modafinil is a non-stimulant. Furthermore, there is
absolutely zero scientific evidence suggesting that modafinil enhances athletic
performance. Modafinil is approved for narcolepsy and recently for shift
workers, plus it is commonly recommended by physicians for off-label purposes
including jet-lag and excess daytime sleepiness.
Secondly, I have not ever, at any time, given modafinil to either Kelli White or
Chryste Gaines. I have nothing to do with either of their pending modafinil
cases involving USADA. Modafinil was not even listed as a "prohibited substance"
by USADA, USATF, IAAF or WADA at the times the samples were collected from the
athletes involved in the modafinil controversy.
In the meantime, no one should forget that guilt or innocence can only be
determined after due process, and there has been no due process, as of yet.
REMI KORCHEMNY
Via e-mail
--------------------------------
No hiring freeze
Editor -- I applaud the Washington Redskins after reading that coach Joe Gibbs
and owner Daniel Snyder have made 21 coaching hires. The Redskins and the NFL
have made a significant impact reducing the nation's unemployed ranks. This is
certain fuel for George Bush's re-election. I hope these jobs will not be
outsourced to India or China.
DONALD G. PETER
San Mateo
--------------------------------
The next one
Editor -- I suspect the next halftime entertainment package will include the Del
Courtney Orchestra with vocal performances from Steve Lawrence and Eydie Gorme.
RON FELL
San Francisco
--------------------------------
Azinger fan
Editor -- Paul Azinger was right to spurn the AT&T out of loyalty to his amateur
partner, ("Azinger decries Pebble," Feb. 3) but he was wrong when he said, "My
being there isn't going to sell one ticket." I won't be buying one, nor will a
sizable cadre I joined to follow him in the Arizona desert last weekend. The man
has serious fans.
Ollie Nutt must indeed be daft to alienate not only a popular player but a past
champion who has done more than his share for the tournament.
Will I buy a ticket? No way. Watch the broadcast? Probably not. And AT&T? I'm
taking my cell-phone number and hitting the highway. It won't make one bit of
difference to their big bottom line, but I'll sleep better at night, as I'm sure
Azinger does.
NANCY SCHLESINGER
Carlsbad (San Diego County)
Address correspondence to Letters to the Green, Chronicle Sports Department, 901
Mission Street, S.F., CA 94103. E-mail: letterstogreen@sfchronicle.com. Fax:
415-543-3754. Letters may be edited for brevity/clarity; include hometown and
daytime phone number.
LOAD-DATE: February 8, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Chronicle Publishing Co.
584 of 998 DOCUMENTS
San Jose Mercury News (California)
February 1, 2004 Sunday MORNING FINAL EDITION
SPRINT COACH KORCHEMNY DISMISSED FROM WORLD TEAM;
COACH DENIES PROVIDING ATHLETES BANNED DRUGS, HAS NOT BEEN SANCTIONED
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 2C
LENGTH: 577 words
USA Track & Field officials dismissed Remi Korchemny of Castro Valley from
coaching the world indoor championship team because he admitted giving a drug to
an athlete.
The action signals a new era in drug testing as coaches, trainers and physicians
could face more scrutiny if athletes they help test positive for banned
substances.
Stephanie Hightower, chair of the women's track and field committee, said
Saturday that the group didn't want negative publicity regarding drugs to
overshadow the athletes at the March championships in Budapest, Hungary. She
said they were acting in the best interests of the sport, although Korchemny,
72, has not been sanctioned or called before a hearing panel.
"A lot of people were uncomfortable sending someone on a national team with this
kind of cloud over their head," Hightower said, referencing the ongoing federal
grand jury investigation in San Francisco of Balco and its owner, Victor Conte
Jr.
Korchemny said he has sent athletes to Conte's Burlingame laboratory to test for
nutritional purposes. The renowned sprint coach denied Saturday giving athletes
banned drugs.
Korchemny gave hurdler Chris Phillips the sleep disorder medication modafinil
during last summer's world championships because it wasn't on the banned list of
the international track and field federation. Korchemny, who did not coach
Phillips, has maintained that the medication is not performance enhancing and
was used to combat jet lag.
Officials announced that six athletes last summer tested positive for modafinil,
which was banned under the "related substances" clause in the rules. The
athletes would receive only a disqualification from the meet in which they took
the drug test if they lose pending arbitration hearings.
But the World Anti-Doping Agency last week classified modafinil as a stimulant
that warrants a two-year ban in the future. Hightower acknowledged that
Korchemny is caught in a bigger battle involving USA Track & Field.
The group is particularly sensitive to questions about drugs because
international officials have harshly criticized it over the handling of the
Jerome Young case.
Young, a 400-meter sprinter, tested positive for the steroid nandrolone in1999
but was cleared by USA Track & Field and went on to win a gold medal at the
Sydney Games.
The International Association of Athletics Federations is going to the Court of
Arbitration for Sport this year to try the case again. Furthermore, the revised
IAAF drug code, which goes into effect this spring, says anyone helping athletes
cheat could be sanctioned by losing credentials to meets.
Hightower said the IAAF was refusing to give Korchemny a credential for the
indoor championships. Korchemny could be the test case for the new rule. He is
being singled out because two of his athletes -- sprint stars Kelli White of
Union City and Chryste Gaines of Lithonia, Ga. -- were among those testing
positive for modafinil last summer.
Now the question is whether the new rules will affect other coaches whose
athletes have tested positive in the past. For example, John Smith of Los
Angeles has had three sprinters penalized for taking stimulants -- Ato Boldon,
Mickey Grimes and Inger Miller.
Smith is the head coach of the men's 2005 outdoor world championship team.
Marion Jones' former coach, Trevor Graham, has had at least six athletes with
positive drug tests, including Young and Olympic sprinter Dennis Mitchell.
LOAD-DATE: August 22, 2005
LANGUAGE: ENGLISH
Copyright 2004 San Jose Mercury News
All Rights Reserved
585 of 998 DOCUMENTS
The San Francisco Chronicle
JANUARY 31, 2004, SATURDAY, FINAL EDITION
Correction Appended
USATF removes local coach;
Korchemny not going to Indoors
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. C2
LENGTH: 434 words
Track coach Remi Korchemny of Castro Valley was removed Friday from his position
as a coach of the U.S. team for the World Indoor Championships in March because
he gave the stimulant modafinil to some of the athletes he coaches, including
sprinters Kelli White and Chryste Gaines.
"I don't care," the 71-year-old Korchemny said. "I did not elect myself (to the
U.S. team) and I did not reject myself. ... It's a very symbolic job. It's not
important in the life of a person. You volunteer your time. They don't need you?
It's their problem."
Korchemny was informed of the decision in a letter from Bill Roe, president of
USA Track & Field. USATF will send a team to the World Indoor Championships
March 5-7 in Budapest, Hungary.
In removing Korchemny from the coaching staff, Roe said the IAAF, track and
field's world governing body, would not issue him a credential and in any event,
his presence in Budapest would send a wrong message.
Having Korchemny on the U.S. staff would be a "futile endeavor," Roe said. "The
IAAF said publicly and confirmed to us privately they would not credential Remi
as a U.S. coach. And we wouldn't want someone on the staff who would be more of
a focus than the athletes."
Although not on the list of banned substances by name, modafinil is considered a
mild stimulant by the U.S. Anti-Doping Agency. The World Anti-Doping Agency on
Thursday announced that from now on a positive test for modafinil would result
in a two-year ban from competition.
White, Gaines and four others tested positive for modafinil last summer, when
sanctions included a public warning and disqualification from the event where
the test occurred.
It is yet another spin-off from the ongoing federal investigation into Victor
Conte, whose Burlingame laboratory was raided by the Internal Revenue Service
and the Food and Drug Administration in September. U.S. anti-doping officials
claim the designer steroid THG came from the Conte-owned Bay Area Laboratory
Co-Operative.
Korchemny was introduced to Conte by NFL linebacker Bill Romanowski, then of the
Denver Broncos.
"It did not hurt when they decided not to take me," Korchemny said. "I can
travel where I want and I can buy my own ticket."
Korchemny said he is the victim of a "double standard" in U.S. track and field
in that other prominent coaches were not singled out when some of their athletes
tested positive for banned substances.
"Other coaches have athletes who have had violations," he said. "There's issues
more important than Remi Korchemny."E-mail John Crumpacker at
jcrumpacker@sfchronicle.com.
LOAD-DATE: February 4, 2004
LANGUAGE: ENGLISH
CORRECTION-DATE: February 3, 2004
CORRECTION: A story in Saturday's Sporting Green misstated the reason USA Track
and Field gave for removing Remi Korchemny as a coach of the U.S. track team in
the World Indoor Championships. The organization said it had removed Korchemny
because of his association with athletes who tested positive for the drug
modafinil. Korchemny denies he provided banned stimulants to athletes.
(02/03/04, P. A2)
Copyright 2004 The Chronicle Publishing Co.
586 of 998 DOCUMENTS
The San Francisco Chronicle
JANUARY 30, 2004, FRIDAY, FINAL EDITION
2-year ban for using modafinil
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. C2
LENGTH: 424 words
The federal grand jury investigating possible sports doping and money laundering
by Burlingame laboratory owner Victor Conte and personal trainer Greg Anderson
met Thursday but apparently did not hear witness testimony in the case.
Nevertheless, fallout from the ongoing probe continued to be felt around the
sporting world.
In Lausanne, Switzerland, headquarters of the International Olympic Committee,
the World Anti-Doping Agency announced that henceforth, positive tests for the
stimulant modafinil will result in two-year bans from competition.
Current sanctions call for a public warning and disqualification from the
competition where the test occurred.
Several clients of Conte's tested positive for modafinil, including world-class
sprinters Kelli White and Chryste Gaines. Six track and field athletes came up
positive for the putative narcolepsy medication last year but they will not be
subjected to retroactive sanctions.
White received modafinil in a prescription from Bay Area psychiatrist Dr. Brian
Goldman, who said the Union City sprinter was referred to him by Conte.
In another development Thursday in Lausanne, WADA said a test for human growth
hormone will likely be available in time for the Athens Olympics in August. If
not, blood samples from athletes will be stored and examined later when a
reliable test is available and retroactive sanctions will be imposed on
cheaters.
Human growth hormone, or hGH, works like an anabolic steroid in building
strength and aiding in recovery time. Until now, it has gone undetected in urine
screening.
In 1999, the wife of Raiders linebacker Bill Romanowski told investigators in a
Colorado prescription drug-fraud case that her husband obtained hGH from Conte's
Bay Area Laboratory Co-Operative and injected it in his knee.
"We've never been so close to having a test in our hands," said Olivier Rabin,
science director for WADA. "There will be new substances detected in Athens,
there's no question about that. We hope hGH is one of them. But we don't want to
tell the athletes when it's coming."
In New York, the attorney for Gaines said the former Stanford sprinter and
two-time Olympian is now the first alternate to get a lane for the 60-meter dash
in next week's Millrose Games indoor track meet. Skip Stolley, the Millrose meet
director, initially said Gaines had not been invited because her modafinil
-inspired role in the Conte saga would be a focal point of the competition.
The Associated Press and Reuters contributed to this report.
LOAD-DATE: January 30, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Chronicle Publishing Co.
587 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
January 30, 2004, Friday
Athletes faces two-year ban for testing positive for modafinil
SECTION: WORLD NEWS; SPORTS
LENGTH: 138 words
GENEVA, Jan. 29 (Xinhua) -- Athletes testing positive for modafinil, the
subtance double American sprint champion Kelli White took at last year's world
championships in Paris, will be banned for two years from competition.
World Anti-Doping Agency (WADA) officials told a one-day media symposium in
Lausanne, Switzerland on Thursday that modafinil was considered a serious drug
on the banned list which came into application at the beginning of this month.
White tested positive for modafinil after winning the 100 meters title in Paris
last August. She later said she was being treated for a sleeping disorder.
At the time the International Association of Athletics Federation (IAAF) said it
regarded modafinil as a related substance to minor stimulants, which meant the
only sanction was the loss of her medal.
LOAD-DATE: January 31, 2004
LANGUAGE: ENGLISH
COPYRIGHT 2004 XINHUA NEWS AGENCY
588 of 998 DOCUMENTS
Associated Press Worldstream
January 29, 2004 Thursday
Doping agency set to test for human growth hormone in Athens
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 768 words
DATELINE: LAUSANNE, Switzerland
Athletes using human growth hormone be warned: The drug police will be waiting
to catch you at the Olympics next summer.
A test for the previously undetectable drug - considered one of the most widely
used banned substances in sports - is all but finalized and likely to be
introduced at the Athens Games, World Anti-Doping Agency officials said
Thursday.
And, even if the test isn't quite ready for Athens, officials will be able to
retest samples later to punish cheaters retroactively.
"We've never been so close to having a test in our hands," said Olivier Rabin,
WADA's science director.
Human growth hormone, or hGH, works like an anabolic steroid, building muscle
mass and helping athletes recover faster from hard training.
Although hGH has been around for decades, standard doping controls haven't been
able to distinguish between the naturally produced hormone and the synthetic
version used by cheaters.
Attempts to devise a test for hGH have dragged on for years, with a number of
projects stalled by a lack of funding.
Rabin said WADA was now in the final phase of validating two hGH tests developed
by scientists in Britain and Germany. Both involve blood, not urine, tests.
"We are doing everything we can to bring it in as quickly as possible," Rabin
said in an interview during a WADA symposium.
WADA, however, will not announce when or if the test is ready, preferring to
keep the drug cheats guessing. Rabin said WADA could also have new tests for
blood-based oxygen carriers, illegal blood transfusions, insulin and new
steroids.
"There will be new substances detected in Athens, there's no question about
that," Rabin said. "We hope hGH is one of them. But we don't want to tell the
athletes when it's coming. They know it's prohibited. The day we catch one or
several athletes, then it will be revealed to the world that the test has been
validated."
Rabin stressed that if a test is not used in Athens, it will be put into
practice shortly after the Olympics. The Athens samples will be stored and
reanalyzed for hGH once the test is finalized, he said.
Retesting of drug samples took place in several sports last year following the
unmasking of the designer steroid THG, the drug at the center of a major
U.S.-based scandal.
Rabin said WADA had evidence that at least one other designer steroid - devised
specifically to avoid detection - was in circulation in the sports world.
"We are tracking some of these substances," he said. "We are asking labs if they
see any unusual readings to keep the samples and retest them to identify any
unique pattern."
Meanwhile, WADA officials said Kelli White and five other U.S. athletes who
tested positive last year for the stimulant modafinil were fortunate to have
escaped without two-year bans.
White tested positive at the World Championships in Paris, claiming she used
modafinil for treatment of the sleep disorder narcolepsy. She faces being
stripped of her gold medals in the 100 and 200 meters.
The International Association of Athletics Federations ruled at the time that
modafinil was a "minor" stimulant and warranted a public warning and
disqualification from the event but not a ban.
WADA's list of banned substances, which went into effect on Jan. 1, classifies
modafinil in the group of stimulants carrying a two-year ban.
WADA medical director Alain Garnier said medical research has shown that
modafinil can enhance performance by stimulating the reflex action of the
muscles, particularly useful in sprint events.
Others who tested positive for modafinil were sprinters Calvin Harrison and
Chryste Gaines and hurdlers Chris Phillips, Sandra Glover and Eric Thomas.
The cases are being handled by the U.S. Anti-Doping Agency.
Despite WADA's ruling on modafinil, agency and IAAF officials said the athletes
would likely be judged by the rules in place at the time.
"If Kelli White was to test positive today, she would get two years," IAAF
spokesman Nick Davies said. "But I can't see how she could be banned for last
year's test."
Also Thursday, basketball's world governing body became the 24th summer Olympic
federation to adopt WADA's anti-doping code, which sets out uniform rules and
sanctions cutting across all sports and countries.
Under the accord, NBA players eligible for Olympic teams will be subjected to
out-of-competition drug tests before Athens just like athletes in other sports.
Soccer, cycling, volleyball and badminton are the four sports yet to formally
enact the code, but WADA director general David Howman said he expects all to
sign up as required before Athens.
LOAD-DATE: January 30, 2004
LANGUAGE: ENGLISH
Copyright 2004 Associated Press
All Rights Reserved
589 of 998 DOCUMENTS
PR Newswire
January 28, 2004 Wednesday
Cephalon, Inc. Selects Cognitive Drug Research's Computerized Cognitive Function
Assessment System for Pivotal Phase III Clinical Trials for The R-isomer of
Modafinil
SECTION: FINANCIAL NEWS
LENGTH: 614 words
DATELINE: READING, England Jan. 28
Cognitive Drug Research, Ltd. (CDR) announced today that Cephalon, Inc., of West
Chester Pennsylvania, has selected Cognitive Drug Research's, Computerized
Cognitive Function Assessment System (CDRSystem) for inclusion in four Phase III
clinical trials of the R- isomer of modafinil. The CDRSystem is being used to
assess the degree to which the R-isomer of modafinil effects cognitive function
in the treatment of excessive sleepiness associated with narcolepsy, obstructive
sleep apnea/hypopnea syndrome (OSAHS) and chronic shift work sleep disorder
(SWSD).
The CDRSystem is a sensitive computer based cognitive assessment tool that has
been specifically developed to definitively assess both enhancement and
impairment in the four major aspects of cognitive functioning: attention,
working memory, episodic secondary memory and motor control.
"The decision to use Cognitive Drug Research was based on the sensitivity and
validity of their computerized tests as well as their proven ability to provide
cognitive function testing in a large multi-national clinical program," said Dr.
Paul Blake, Senior Vice President, Clinical Research and Regulatory Affairs, at
Cephalon.
The CDRSystem is being used in this Phase III program to assess R-modafinil's
affect on attention, working memory, and episodic secondary memory. The program
with R-modafinil consists of 2 twelve-week clinical trials in patients with
OSA/HS, one in patients with narcolepsy and one planned in patients with chronic
shift work sleep disorder. These randomized, double-blind, placebo-controlled
clinical trials are expected to include over 800 patients with trials being
conducted concurrently at sites in the United States, Europe, Canada, Russia and
Australia.
"We are delighted to be working with Cephalon on these important trials and
I congratulate Cephalon for their forward thinking in taking the time to study
how the R-isomer of modafinil may lessen cognitive impairment" said Professor
Keith Wesnes, CDR's founder. "Cephalon's decision reconfirms our strategy of
creating computerized clinical research tools that meet the emerging needs of
pharmaceutical researchers and the belief that our system delivers real business
value in Phase III programs."
About Cognitive Drug Research, Ltd.
Founded in 1986, Cognitive Drug Research Ltd. (CDR) is the world's leading
provider of innovative cognitive function assessment technology and services to
the pharmaceutical industry. CDR combines innovative technology and validated
psychometric tests to definitively measure the effects of pharmaceuticals on the
mental efficiency of volunteers and patients in clinical trials.
CDR has experience assessing cognitive function in areas including cancer,
depression, pain, epilepsy, age related cognitive decline, schizophrenia, sleep
disorders, diabetes, stroke and hypertension. CDR also has extensive experience
in dementia with international studies involving Alzheimer's Disease,
Parkinson's Disease with Dementia, Vascular Dementia and Dementia with Lewy
Bodies.
CDR is a privately held company with headquarters in the Goring-on-Thames, U.K
and sales offices in New Jersey, U.S. CDR has established a significant record
of achievement with methods that have been used in over 500 studies and has been
proven through wide spread independent scientific validation. It is also
documented in accordance with FDA 21 Code of Federal Regulations part 11.
Additional information about CDR can be found by visiting the company's website
on www.cdr.org.uk.
SOURCE Cognitive Drug Research, Ltd.
CONTACT: U.S. - Roman Kruchowy, roman@cdr.us.com, U.K - Paula Stubbs,
paulas@cdr.org.uk, both of Cognitive Drug Research, Ltd.
URL: http://www.prnewswire.com
LOAD-DATE: January 29, 2004
LANGUAGE: ENGLISH
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PR Newswire Europe
January 28, 2004 Wednesday
Cephalon, Inc. Selects Cognitive Drug Research's Computerised Cognitive Function
Assessment System for Pivotal Phase III Clinical Trials for The R-isomer of
Modafinil
LENGTH: 620 words
READING, England, January 28 /PRNewswire/ -- Cognitive Drug Research, Ltd. [CDR]
announced today that Cephalon, Inc ., of West Chester Pennsylvania, has selected
Cognitive Drug Research's, Computerized Cognitive Function Assessment System
[CDRSystem] for inclusion in four Phase III clinical trials of the R- isomer of
modafinil. The CDRSystem is being used to assess the degree to which the
R-isomer of modafinil effects cognitive function in the treatment of excessive
sleepiness associated with narcolepsy, obstructive sleep apnea/hypopnea syndrome
[OSAHS] and chronic shift work sleep disorder [SWSD].
The CDRSystem is a sensitive computer based cognitive assessment tool that has
been specifically developed to definitively assess both enhancement and
impairment in the four major aspects of cognitive functioning: attention,
working memory, episodic secondary memory and motor control.
"The decision to use Cognitive Drug Research was based on the sensitivity and
validity of their computerised tests as well as their proven ability to provide
cognitive function testing in a large multi- national clinical program," said
Dr. Paul Blake, Senior Vice President, Clinical Research and Regulatory Affairs,
at Cephalon.
The CDRSystem is being used in this Phase III program to assess R- modafinil's
affect on attention, working memory, and episodic secondary memory. The program
with R-modafinil consists of 2 twelve-week clinical trials in patients with
OSA/HS, one in patients with narcolepsy and one planned in patients with chronic
shift work sleep disorder. These randomised, double-blind, placebo-controlled
clinical trials are expected to include over 800 patients with trials being
conducted concurrently at sites in the United States, Europe, Canada, Russia and
Australia.
"We are delighted to be working with Cephalon on these important trials and I
congratulate Cephalon for their forward thinking in taking the time to study how
the R-isomer of modafinil may lessen cognitive impairment" said Professor Keith
Wesnes, CDR's founder. "Cephalon's decision reconfirms our strategy of creating
computerised clinical research tools that meet the emerging needs of
pharmaceutical researchers and the belief that our system delivers real business
value in Phase III programs."
About Cognitive Drug Research, Ltd.
Founded in 1986, Cognitive Drug Research Ltd. [CDR] is the world's leading
provider of innovative cognitive function assessment technology and services to
the pharmaceutical industry. CDR combines innovative technology and validated
psychometric tests to definitively measure the effects of pharmaceuticals on the
mental efficiency of volunteers and patients in clinical trials.
CDR has experience assessing cognitive function in areas including cancer,
depression, pain, epilepsy, age related cognitive decline, schizophrenia, sleep
disorders, diabetes, stroke and hypertension. CDR also has extensive experience
in dementia with international studies involving Alzheimer's Disease,
Parkinson's Disease with Dementia, Vascular Dementia and Dementia with Lewy
Bodies.
CDR is a privately held company with headquarters in the Goring-on- Thames, U.K
and sales offices in New Jersey, U.S. CDR has established a significant record
of achievement with methods that have been used in over 500 studies and has been
proven through wide spread independent scientific validation. It is also
documented in accordance with FDA 21 Code of Federal Regulations part 11.
Additional information about CDR can be found by visiting the company's website
on www.cdr.org.uk.
Web site: http://www.cdr.org.ukCognitive Drug Research, Ltd.
CONTACT:
CONTACT: U.S. - Roman Kruchowy, roman@cdr.us.com, U.K - Paula Stubbs,
paulas@cdr.org.uk, both of Cognitive Drug Research, Ltd. FCMN Contact:
roman@CDR.us.com
LOAD-DATE: January 29, 2004
LANGUAGE: ENGLISH
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591 of 998 DOCUMENTS
San Jose Mercury News (California)
January 24, 2004 Saturday MORNING FINAL EDITION
GAINES' LAWYERS SET A DEADLINE;
DECISION ON ENTRY MUST BE BY MONDAY
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 2D
LENGTH: 402 words
Chryste Gaines' lawyers have given U.S. track officials until Monday to pave the
way for the Olympic sprinter to compete at the Verizon Millrose Games in New
York.
Gaines' attorney, Cameron Myler, would not say Friday what action is planned if
Millrose officials refuse to allow the athlete to enter the 60-meter race at the
Feb. 6 meet in Madison Square Garden. Myler said a meeting with officials from
USA Track & Field and the U.S. Olympic Committee failed to resolve the dispute.
"We're trying to come up with ways to get the result that we want," Myler said.
Gaines, a former Stanford sprinter who ranked second in the world last year, is
being banished by meet organizers because of a pending drug case involving the
sleep-disorder-medication modafinil.
Her lawyers say this is unfair because Gaines, 33, of Lithonia, Ga., is eligible
under International Association of Athletics Federations rules. Even if she were
to lose her case in an upcoming arbitration hearing, Gaines would remain
eligible because the punishment for modafinil is solely disqualification from
the meet at which the athlete tested positive. That occurred in June, at the
U.S. championships at Stanford, when the drug was not named on the IAAF banned
list.
Gaines and five others who tested positive for modafinil are being prosecuted
under the "related substance" clause of the drug code. Lawyers for many of the
athletes say they will argue that modafinil is not a stimulant and has no
performance-enhancing qualities.
Although Gaines' drug case is minor, she and others have been banned from some
indoor meets this season. Myler is focusing on the Millrose Games, where sprint
star Marion Jones is planning to mark her return after taking last year off to
have a son.
Myler said USA Track & Field's chief executive, Craig Masback, agreed totry to
help Gaines' cause. But track officials say they cannot tell organizers who to
invite, or which events they should hold, at individual meets -- even those that
the group sanctions. The Millrose Games is one of four meets that will make up
USA Track & Field's Indoor Golden Spike Tour this winter. Gaines has entered a
non-paying 60 meters at one of those meets, the Tyson Foods Invitational on Feb.
14.
Myler filed a complaint with the USOC this week, alleging that USA Track & Field
has failed to protect athletes' rights as stated in the USOC constitution.
LOAD-DATE: August 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo;
PHOTO: Gaines
Eligible, but drug test has brought some meet bans
Copyright 2004 San Jose Mercury News
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592 of 998 DOCUMENTS
San Jose Mercury News (California)
January 23, 2004 Friday MORNING FINAL EDITION
GAINES FILES A COMPLAINT IN EFFORT TO RACE;
EVENTS BARRING HER BECAUSE OF DRUG TEST
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 6D
LENGTH: 643 words
A lawyer for Chryste Gaines has filed a complaint with the U.S. Olympic
Committee this week in an effort to force track and field officials to open
their events to the former Stanford sprinter.
In what Olympic experts say is the first case of its kind, the complaint alleges
that USA Track & Field, the sport's national governing body, has an obligation
to ensure that eligible athletes are not excluded from events it sanctions.
Gaines, 33, of Lithonia, Ga., tested positive for modafinil, a sleep-disorder
medication, last June. According to track officials, athletes who test positive
for modafinil face disqualification from the event where the test occurred but
no further sanctions.
However, Gaines was not invited to the prestigious Verizon Millrose Games in New
York next month because of the test. She also is being barred from a meet in
Stuttgart, Germany, and on Thursday, organizers of the Athens indoor meet told
her she is not welcome even though she is eligible for this summer's Olympics
there.
Gaines' attorney, Cameron Myler, alleges that meet organizers' actions are
preventing the sprinter from qualifying for next month's indoor national
championships in Boston. A spokeswoman for USA Track & Field, Jill Geer, said
Thursday that if Gaines files a waiver she would be allowed to run the 60 meters
at the championships. She added that USA Track & Field has no control over the
meets, which are invitationals and are part of its Indoor Golden Spike Tour.
The parties are scheduled to discuss the situation today. Myler said she would
decide afterward whether to file for arbitration.
"We're still hoping to gain entrance into the Millrose Games," Myler said. "It
is about Chryste being denied the opportunity to compete."
Gaines, a two-time Olympian who is training in Miami, asked that her lawyer
discuss the case. Myler said that Gaines hopes to qualify for the world indoor
championships in March in Budapest, Hungary.
The complaint alleges that USA Track & Field has responsibilities under federal
and USOC regulations to make sure the rights of its athletes are protected.
It claims Gaines is being blocked because of publicity over a minor drug case.
Modafinil is not on the banned list provided by the International Association of
Athletics Federations, track and field's worldwide governing body, but Gaines
and five other track athletes, including training partner Kelli White of Union
City, are being prosecuted under a related-substanceclause in the guidelines.
Officials must prove the medication is a stimulant beyond a reasonable doubt,
and sleep-disorder experts have questioned that claim.
Myler wrote in the complaint that modafinil is not related to any substances
included on the prohibited list.
Gaines' case has received extra attention because the modafinil positives have
been linked to nine others involving THG, a previously undetected steroid. U.S.
Anti-Doping Agency officials have alleged that a Burlingame nutrition company,
Balco Laboratories, is the likely source of the steroid.
An ongoing federal grand jury investigation in San Francisco, involving
testimony from scores of athletes from baseball, football and Olympic sports,
has kept the case in the news. That led Skip Stolley of the Millrose Games to
deny Gaines a chance to run. He said he did not want attention from the drug
case to distract from his meet, but he happily signed on sprint star Marion
Jones, who was one of the biggest names to testify before the grand jury.
Art Huff of the Tyson Foods Invitational in Fayetteville, Ark., does not want to
decide who is eligible: "Who am I to say no?" he asked.
Huff recently added the women's 60 meters, but it is a race without prize money.
Gaines, Torri Edwards and Inger Miller have asked for lanes, turning it into one
of the winter's premier sprint races.
LOAD-DATE: August 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo;
PHOTO: LIONEL CIRONNEAU -- ASSOCIATED PRESS
Chryste Gaines says USA Track & Field must ensure that eligible athletes can
race in its events.
Copyright 2004 San Jose Mercury News
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San Jose Mercury News (California)
January 22, 2004 Thursday MORNING FINAL EDITION
GAINES IS BANNED FROM GERMAN MEET
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 4D
LENGTH: 439 words
The director of a track and field meet to be held in Germany this month decided
Wednesday to ban Chryste Gaines from his event, the latest move against the
Olympic sprinter who tested positive for a stimulant last summer but is eligible
to compete.
Fredy Schafer said he did not invite Gaines, the world's second-ranked female
sprinter, or hurdler Chris Phillips to the Jan. 31 meet in Stuttgart because of
their positive tests for modafinil, the controversial sleep-disorder medication.
Athletes who test positive for modafinil face disqualification from the event in
which they tested positive but no further sanctions. Schafer's action
underscores how track and field is struggling to be fair at a time when its
image is suffering over drugs.
"This is a difficult thing in Germany with the main sponsors, because they don't
want track being involved in doping," Schafer said. "We want to be onthe safe
side."
While Gaines and Phillips await hearings with the U.S. Anti-Doping Agency, some
officials are worried that athletes are being unfairly ostracized because of the
federal grand jury investigation of Balco Laboratories, the Burlingame
nutritional-supplement company that has been linked with the designer steroid
THG.
"It's very disturbing to us people are being judged before the process," said
Bill Roe, president of USA Track & Field, the sport's national governing body.
Roe said of Gaines' situation: "They want to make sure we are tough on doping,
but here is a specific instance that it has not worked."
Gaines, a former Stanford sprinter who is among six athletes who tested positive
for modafinil, also has been banned from next month's Verizon Millrose Games in
New York. USA Track & Field recently addressed the fairness issue with American
promoters, who have control of their events.
"The only thing in our power is to guarantee to Chryste that she will not have
to worry about gaining entry into our national championships," Roe said.
Gaines declined to talk, but her agent, Renaldo Nehemiah, said, "We are the most
dysfunctional, functioning body in professional sports."
Nehemiah said he sent a memo to European meet promoters and leaders of the
International Athletics Federations Association, track and field's worldwide
governing body, asking them to clarify their positions.
"Chryste is being a scapegoat for maybe some other kind of issue," said
Nehemiah, a former world-class hurdler and San Francisco 49er.
Nehemiah said Gaines might run the 60 meters at the Tyson Indoor meet in
Arkansas next month, but added she could also be banished from a meet in
Birmingham, England.
LOAD-DATE: August 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo;
PHOTO: Gaines
U.S. sprinter tested positive for modafinil but is eligible
Copyright 2004 San Jose Mercury News
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The San Francisco Chronicle
JANUARY 21, 2004, WEDNESDAY, FINAL EDITION
Jacobs won't be at youth clinic
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. C8
LENGTH: 546 words
The organizer of a prestigious track and field clinic in Union City has decided
against inviting Olympic runner Regina Jacobs to next month's event at James
Logan High School because of her recent positive test for the designer steroid
THG.
Logan track coach Lee Webb, who annually lines up a who's-who of current and
retired track stars for his youth clinic, said he did not want the attention
Jacobs would bring to the Feb. 14 event.
"I don't want that to be the focus of the whole thing," Webb said. "We've
already had plenty of attention."
That was in reference to Remi Korchemny, a Castro Valley coach who volunteers
his time working with high school athletes at Logan. Korchemny, who coaches
several athletes who have tested positive for the stimulant modafinil and one
for THG, said he will not be at the clinic.
For next month's clinic, Webb has invited such track stars of the past as Tommie
Smith, John Carlos, Dick Fosbury, Mac Wilkins, Andre Phillips, Tom Petranoff,
Charlie Greene and Jim Hines. Jacobs, world-record holder for the women's indoor
1,500 meters, would have worked with middle- and long-distance runners.
Jacobs, 40, of Oakland, is in the process of appealing her positive test for THG
from last June's U.S. Championships at Stanford, where she won the 1,500. Her
appeal will be heard by the American Arbitration Association. If unsuccessful,
she could be banned from competition for two years.
Through her attorney, Edward G. Williams of New York, Jacobs is seeking to
broaden the pool of potential arbitrators for what will be a three-person panel.
Jacobs could not be reached for comment.
Korchemny, who said he provided modafinil to some of his athletes to combat the
effects of jet leg, said he has not been called to testify before the federal
grand jury in San Francisco investigating Victor Conte, owner of a nutritional
supplement laboratory in Burlingame.
The grand jury is expected to reconvene Thursday at the federal building.
Korchemny said he is currently in Florida working with sprinter Chryste Gaines,
a two-time Olympian who tested positive for modafinil at the U.S. Championships.
The sanctions for modafinil use include a public warning and disqualification
from the event where the test occurred.
Gaines remains eligible for all competition, including the Olympic Games, but
because of the furor over the investigation into Conte and his lab, she was not
invited to run in next month's Millrose Games in New York.
"It's just a warning," Korchemny said. "Why should professional athletes suffer
loss of income? Unfortunately, the Millrose director, he has double standards
for athletes. People dealing with BALCO (Conte's lab) are not going to run in
his meet."
Gaines testified before the grand jury in San Francisco, as did fellow sprinters
Marion Jones and Tim Montgomery. Jones was invited to run in the Millrose Games.
"Both of them were subpoenaed," Korchemny said. "They are also clients of BALCO.
Why can they run? People are afraid to ask the meet director why he has double
standards."
Millrose director Skip Stolley said he did not invite Gaines because he did not
want the focus of the meet to be on a continuing drug story.E-mail John
Crumpacker at jcrumpacker@sfchronicle.com.
LOAD-DATE: January 21, 2004
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, Regina Jacobs is the world-record holder for the women's indoor
1,500 meters. / Carlos Avila Gonzalez / The Chronicle
Copyright 2004 The Chronicle Publishing Co.
595 of 998 DOCUMENTS
Edmonton Journal (Alberta)
January 18, 2004 Sunday Final Edition
A life without ZZZZZs: Doze of reality: Eager to try a new prescription drug
that lets you stave off sleep for up to 40 hours? Here's a wake-up call: get
used to disrupted routines and lonely nights
SOURCE: Sunday Telegraph
BYLINE: Julia Llewellyn Smith
SECTION: Sunday Reader; Pg. D9
LENGTH: 1477 words
DATELINE: LONDON
LONDON - It's 4 a.m., I've been up for 20 hours, but I don't feel tired. I'm not
at a wild party, nor rocking a wailing infant, nor am I lying miserably in bed
cursing my insomnia.
I am sitting at my desk paying my bills on the Internet as if it were
mid-afternoon. I put some washing in the machine, then paint my toenails. I look
at the clock: 4:45 a.m. I haven't yawned once.
The reason for my alertness is 200 milligrams of modafinil, a new prescription
drug that staves off sleep for hours on end. (In Canada, it has been available
since 1999 under the name Alertec.)
Unlike the drugs we've traditionally used to keep us going, modafinil appears to
have few side-effects. While coffee drinkers shake and amphetamine-users jabber
aggressively, on modafinil I feel calm, focused -- and able to work all night.
According to Leon Kreitzman, author of The 24-Hour Society, drugs like modafinil
will transform society.
"Modafinil belongs to a new class of awakening drugs known as eugeroics, which
are unravelling the mechanisms of sleepiness. Once you've done that you will end
up in a world where the need to sleep is optional. I would say that will happen
within the next quarter of a century."
When I tell my friends about Kreitzman's vision, they react in unison. "But I
love sleep," they protest. "A world without it would be horrible." A moment
later, they ask: "Where did you say you got those pills? Could I have one?"
But at what price? Round-the-clock supermarkets, 24-hour television, electric
lighting, demanding bosses all make it harder and harder to get the eight hours'
rest most of us need to function properly. Last month, the research group Demos
pointed out that too many crucial decisions, such as the one that launched the
Challenger space shuttle, are made by people handling complex data after days of
sleep deprivation.
Already, the armed forces are committed to modafinil, having used it to help
British and American troops "power on" to Baghdad: marching for 40 hours,
sleeping for eight, and repeating the pattern without noticeable ill-effect.
If it works for the military, who else could it help? New mothers, long-distance
truck drivers, hospital interns? The truth is we'd love to burn the candle at
both ends: we just need to find the wax.
Modafinil was developed in France a decade ago as an aid for narcoleptics --
people who fall asleep uncontrollably. Henry Nicholls, 30, a London-based
science writer with narcolepsy, has been using the drug for two years to control
his condition, thought to affect 2,500 people in Britain.
"For me, it works amazingly well," he says. "No one knows what the long-term
effects of taking it daily will be, but I'm happy to be a guinea pig.
"Before, I used to worry that I'd never be able to hold down a normal job,
because when the sleepiness took over there really was nothing I could do. Now I
am able to function like anyone else. "
Nicholls needs a prescription for his supply. It is, however, easy to bypass the
system, because the drug is available to anyone with a credit card and a
computer. It takes me two clicks on the Internet to find a site that offers to
send me 30 tablets for about $175. The pills arrive six days later.
DRUG'S DEVELOPERS NOT SURE EXACTLY HOW IT WORKS
I call Ian Davison, of Cephalon, which makes modafinil in Britain and in the
U.S. under the name ProVigil, and is developing even more powerful versions. "We
are not 100-per-cent sure how ProVigil works," he says. "We know it has an
effect on the hypothalamus region of the brain, which controls our sleep-wake
generating sites, whereas amphetamines control the completely separate
dopaminergic side.
"Both sides stimulate the cerebral cortex, which keeps people awake, but the
dopaminergic also stimulates the heart rate and blood pressure. When the
amphetamines wear off there is a crash, while with modafinil people just go back
to their normal rhythm of sleep-wake."
Davison stresses modafinil is intended solely for narcoleptics: "You really
should only take a medicine for what it's prescribed for. In any case, you're
wrong to think you will get to a situation where you won't sleep at all. In the
end, the overwhelming drive to sleep will come whether you use modafinil or
not."
He is backed up by Dr. Irshaad Ebrahim of the London Sleep Centre. Sleep, he
points out, helps the brain store memories and recuperate from work, and helps
the body build its immune system. "If you use a drug to overcome that, you will
deprive yourself of those things."
There are no feelings of euphoria associated with modafinil, so it is unlikely
to become fashionable; sleep experts certainly hope it won't. Nonetheless, when
I swallow my first one I am surprised to feel absolutely nothing.
I've started slowly with a 100 milligram dose -- half the recommended amount --
to avoid potential nausea and headaches, the most common side-effects. As usual,
I've crawled out of bed reluctantly at 8 a.m., after too-late a night and with a
mountain of tasks ahead of me.
My day passes well: I feel sharp, moderately energetic but certainly not like
superwoman. But as the hours wear on, I notice what doesn't happen: no yawning,
no intense yearning for a 2 p.m. nap. Instead I steadily work through my to-do
list.
It's in the evening that things get interesting: I go out to dinner with
friends. We stay until after midnight. Normally I'd be flagging, but now I sit
and talk cheerfully as if it were mid-morning (it may help I'm not drinking,
since Cephalon has not yet tested the effects of mixing alcohol with modafinil).
I get home and rather than dive into bed as I usually do, I watch some TV and
read for half an hour. I turn the light out at about 2 a.m., worried that I
won't sleep at all, but in fact I crash out at once.
Astonishingly, I'm awake before 7 a.m., at least two hours earlier than I
usually would after such a late night, and instantly want to jump out of bed and
get going. I pop another pill and look forward to enjoying another busy day and
a late night. I'm thrilled.
It's time to push my boundaries. I am going to a party in a pub. Just before I
go out I take a 200-milligram dose. At the party I am surrounded by
thirtysomethings who, shattered after a long week, can't conceal their yawns.
Yet I don't glance once at my watch.
My friends are disappointed that I'm not grinding my teeth or acting "wired." I
explain that I'm not taking amphetamines.
One by one, as they start calling taxis, I am still there talking animatedly
(but not maniacally) and having fun. I'm surprised to feel my legs shake
slightly -- a symptom of exhaustion. I realize modafinil may stop you from
feeling sleepy but you still feel tired. My limbs grow heavier, but that doesn't
stop the wakefulness. If wake-up drugs catch on, "tiredness" and "sleepiness"
will have to be separated: a hard concept to grasp.
I go home around 1:30 a.m., where again I feel no desire to sleep. At the same
time, when it's cold and dark the prospect of a cosy bed is very appealing. Why
would I want to work all night when I could be snuggled under a duvet?
I can't resist climbing under the covers, but instead of turning off the light,
I read. After an hour, I remember I need to check my tax bill. I might as well
do it now. Having done so, there seems no particular reason -- tradition apart
-- to go back to bed. It's 3 a.m. There's an article I have to finish, a letter
I need to write. I really should do some washing. Why not do it now?
I MAY NOT BE SLEEPY, BUT I AM BONE-WEARY
Yet although it's satisfying to power through my work, it's unpleasant. It's
tiredness versus sleepiness again: I am awake enough to function efficiently but
plowing through the backlog is still physically wearying.
The loneliness is miserable. I feel as if I'm the only person in the world. Yes,
I could go out and find an all-night supermarket, but it's freezing outside and
I might get mugged. I end up behaving like insomniacs everywhere and I go
online, surfing wildly and sending silly e-mails to feel connected to humanity.
I'm starting to understand how sleep gives a fundamental pattern to your life.
Without that break, time stretches ahead of you dauntingly like a desert. I
worry what would happen if wake-up drugs were widely available. If your biggest
rival at work was taking them, would you really be able to resist? Would people
who slept be seen as losers?
By 6 a.m. I have had a bath and breakfast. I can't wait for the rest of the
world to wake up. As soon as the newspaper shop opens at 7 a.m., I'm out of the
house, desperate for human contact.
I realize now how much more bushy-tailed I was on modafinil days. I hated my
sleepless night because it felt so unnatural, but I still think modafinil could
be the perfect response to a broken night, an urgent deadline or jet lag.
LOAD-DATE: January 18, 2004
LANGUAGE: ENGLISH
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TYPE: News
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CanWest Global Communications Corp.
All Rights Reserved
596 of 998 DOCUMENTS
The San Francisco Chronicle
JANUARY 17, 2004, SATURDAY, FINAL EDITION
Track organizers are wary;
Wait-and-see attitude on positive-testing athletes
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. C2; OLYMPIC BEAT
LENGTH: 825 words
Organizers of several outdoor track and field meets scheduled for the spring
said they will take a wait-and-see approach toward inviting athletes caught up
in the ongoing doping scandal emanating from Victor Conte's nutritional
supplement lab in Burlingame.
The meet director for the Feb. 6 Millrose Games in New York said he did not
invite sprinter Chryste Gaines, who tested positive for the mild stimulant
modafinil, because he wanted the meet to focus on performance -- not
performance-enhancing drugs. Gaines also will not compete in an indoor meet Jan.
31 in Boston.
A positive test for modafinil does not call for a ban from competition, unlike
steroids, and Gaines and others who used the stimulant are subject only to a
public warning and a disqualification from competition where the test occurred.
Gaines and fellow sprinter and modafinil positive Kelli White, recovering from a
knee injury, remain eligible for all domestic and international competition,
including the Olympic Games.
"We're going to be real careful with regards to modafinil," said Gregg Miller,
meet director for the May 8 Tom Moore Modesto Relays. "It's something I want to
look at and consider the individual athletes. I want to protect the integrity of
the events because I don't want to invite someone who may be suspended. That
would have ramifications for everybody."
In recent years the Modesto meet has featured sprinter Dwain Chambers of Great
Britain and American shot putter Kevin Toth -- both of whom tested positive for
THG and face two-year bans from competition.
"It's really a shame," Miller said of Chambers. "Maybe I'm nave. I'd like to
think he's one person who didn't realize what was going on. I really consider
him a good guy."
U.S. anti-doping officials alleged the THG came from Conte's lab in Burlingame,
prompting Miller to say, "Overall, he's really hurt our sport. Not just our
sport, but a lot of others. We're going to be careful."
Asked whether he would invite Gaines, White or any of the other four athletes
who tested positive for modafinil to the prestigious Prefontaine Classic June 19
in Eugene, Ore., meet director Tom Jordan said, "I guess you could say it would
be a case-by-case decision. Certainly I can understand the motivation of the
indoor meet directors. You don't want the focus to be on that."
Nancy Ditz, executive director of the Grand Prix II meet at Stanford on June 6,
said, "We'll wait and see how the adjudication process goes. There's a lot more
to learn until we make a blanket judgment."
Ditz is sensitive to the many facets of the BALCO story because Stanford's Cobb
Track & Angell Field is Ground Zero, the place in June where an anonymous coach
sent to U.S. anti-doping officials a syringe loaded with what was determined to
be the designer steroid THG.
"You don't want to diminish the caliber of the meet by including people who are
deemed to have had an unfair advantage," said Ditz, a Stanford graduate and 1988
Olympian in the marathon. "I wouldn't make a step until I talked to USA Track &
Field. We in no way condone people trying to get an unfair advantage."
Meanwhile, the man who coaches Gaines and White, Remi Korchemny of Castro
Valley, could be banned by U.S. track officials from coaching the U.S. team at
the World Indoor Championships in March in Budapest, Hungary. USATF is
considering sanctioning coaches, doctors and trainers of athletes who test
positive for banned substances. Korchemny maintains modafinil is not a
performance-enhancing drug.
Paddlers coming to Oakland: The Olympic trials in flatwater canoe and kayak will
be held April 15-18 at Lake Merritt in Oakland, site of the U.S. national
championships last August. Because of the job done by the host Lake Merritt
Rowing Club, the canoe and kayak federation chose to return for its trials.
"That event came off so well, the governing body decided they would award us the
Olympic trials," said Scott Whitney of the local organizing committee.
Twelve finals will be held over the three days at the lake, starting with two
that will send the winners directly to the Athens Olympics without having to go
through further competition at a Pan Am qualifying event in Brazil in June.
Winners of the men's and women's K1 500-meter races (kayak singles) on April 15
will be able to call themselves Olympians after paddling across the finish line.
Other events to be contested include men's and women's kayak pairs at 500 and
1,000 meters, men's and women's kayak fours and canoe singles and pairs at 500
and 1,000.
The world at large: Superstar Marion Jones, returning to competition after
giving birth to a son in June, will contest the long jump indoors for the first
time in her career Feb. 20 in Birmingham, England. She'll also run the 60-meter
dash. Jones and her boyfriend, Tim Montgomery, currently are training in the
Cayman Islands.E-mail John Crumpacker at jcrumpacker@sfchronicle.com.
LOAD-DATE: January 17, 2004
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, Chryste Gaines was not invited to the Millrose Games due to a
positive test for modafinil. / Michael Probst / Associated Press
Copyright 2004 The Chronicle Publishing Co.
597 of 998 DOCUMENTS
Espicom Business Intelligence
January 14, 2004
Cephalon begins Phase III trials for the R-isomer of modafinil
LENGTH: 215 words
Cephalon has released data from its earlier clinical trials with R-modafinil and
information about the Phase III programme for the compound that the company
initiated in December 2003. R-modafinil, a single-isomer of the active
pharmaceutical ingredient contained in Provigil (modafinil) Tablets, is
initially being developed for the treatment of excessive sleepiness associated
with narcolepsy and obstructive sleep apnoea/hypopnoea syndrome (OSA/HS).
The efficacy portion of the Phase III programme with R-modafinil consists of two
12-week clinical trials in patients with OSA/HS and one in patients with
narcolepsy. These randomised, double-blind, placebo-controlled trials are
expected to include approximately 800 patients. The primary outcome measures of
the trials are the Maintenance of Wakefulness Test and the CGI of
Change-Clinician. The trials are being conducted concurrently at sites in the
US, Europe, Canada and Australia.
The company remains on schedule to complete the OSA/HS programme, and expects to
file an NDA for R-modafinil with the FDA in the fourth quarter of 2004. In
addition, the company will commence a study of R-modafinil in patients with
shift work sleep disorder in early 2004 and intends to file an sNDA for that
additional indication as well.
LOAD-DATE: January 14, 2004
LANGUAGE: ENGLISH
Copyright 2004 ESPICOM Business Intelligence Ltd.
598 of 998 DOCUMENTS
Knobias.com
This content is provided to LexisNexis by Comtex News
Network, Inc.
January 13, 2004 Tuesday
CEPH Launches Phase III Study of R-modafinil
LENGTH: 100 words
DATELINE: Ridgeland, MS
Cephalon, Inc. (CEPH) announced data from its clinical trials with R-modafinil
and information about the Phase III clinical program for the compound. R-
modafinil, a single-isomer of the active pharmaceutical ingredient contained in
PROVIGIL(R) (modafinil) Tablets [C-IV], is initially being developed for the
treatment of excessive sleepiness associated with narcolepsy and obstructive
sleep apnea/hypopnea syndrome. The efficacy portion of the Phase III program
with R-modafinil consists of 2 twelve-week clinical trials in patients with
OSA/HS syndrome and one in patients with narcolepsy.
LOAD-DATE: January 14, 2004
LANGUAGE: ENGLISH
Copyright 2004 Comtex News Network, Inc.
All Rights Reserved
Copyright 2004 Knobias.com, LLC, All rights reserved.
599 of 998 DOCUMENTS
PR Newswire
January 13, 2004 Tuesday
Cephalon, Inc. Initiates Phase III Clinical Trials for the R-isomer of Modafinil
;
Clinical Program Remains on Schedule
SECTION: FINANCIAL NEWS
LENGTH: 857 words
DATELINE: WEST CHESTER, Pa. Jan. 13
Cephalon, Inc. (Nasdaq: CEPH) announced today, at the JP Morgan Healthcare
Conference, data from its earlier clinical trials with R-modafinil and
information about the Phase III clinical program for the compound that the
company initiated in December 2003. R-modafinil, a single-isomer of the active
pharmaceutical ingredient contained in PROVIGIL(R) (modafinil) Tablets $(C-IV$),
is initially being developed for the treatment of excessive sleepiness
associated with narcolepsy and obstructive sleep apnea/hypopnea syndrome
(OSA/HS).
The efficacy portion of the Phase III program with R-modafinil consists of 2
twelve-week clinical trials in patients with OSA/HS and one in patients with
narcolepsy. These randomized, double-blind, placebo-controlled clinical trials
are expected to include approximately 800 patients. The primary outcome measures
of the trials are the Maintenance of Wakefulness Test (MWT) and the Clinical
Global Impression of Change-Clinician (CGI-C). The trials are being conducted
concurrently at sites in the United States, Europe, Canada and Australia.
The company remains on schedule to complete the OSA/HS program, and expects to
file a New Drug Application (NDA) for R-modafinil with the U.S. Food and Drug
Administration in the fourth quarter of 2004. In addition, the company will
commence a study of R-modafinil in patients with Shift Work Sleep Disorder in
early 2004 and intends to file a supplemental New Drug Application (sNDA) for
that additional indication as well.
"The decision to move forward with this Phase III program was based on earlier
placebo-controlled clinical trials that demonstrated that R-modafinil maintained
wakefulness and had a longer duration of effect than does PROVIGIL," said Dr.
Paul Blake, Senior Vice President, Clinical Research and Regulatory Affairs, at
Cephalon.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,600 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England,
Martinsried, Germany, and Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Full
prescribing information on its U.S. products is available at www.cephalon.com or
by calling 1-800-896-5855.
Cephalon is a leader in optimizing a data-driven approach to developing new
drugs and in expanding the therapeutic potential of existing products.
Cephalon's research pipeline is focused on the identification of novel molecules
that affect cell survival and death. Additional information about Cephalon and
its subsidiaries can be obtained by visiting the company's website at
http://www.cephalon.com.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs including clinical trials of R-modafinil, the duration of effect for R-
modafinil, timing of the completion of trials and the filing of the NDA,
development of potential pharmaceutical products, interpretation of clinical
results, prospects for regulatory approval, manufacturing development and
capabilities, market prospects for its products, sales and earnings projections,
and other statements regarding matters that are not historical facts. You may
identify some of these forward-looking statements by the use of words in the
statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties such
as those set forth below and in its reports on Form 8-K, 10-Q and 10-K filed
with the U.S. Securities and Exchange Commission. Given these risks and
uncertainties, any or all of these forward-looking statements may prove to be
incorrect. Therefore, you should not rely on any such factors or forward-looking
statements. Furthermore, Cephalon does not intend to update publicly any
forward-lookingstatement, except as required by law. The Private Securities
Litigation Reform Act of 1995 permits this discussion.
SOURCE Cephalon, Inc.
CONTACT: Investor - Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com, or
Media - Robert Grupp, +1-610-738-6402, rgrupp@cephalon.com, both for Cephalon,
Inc.
URL: http://www.prnewswire.com
LOAD-DATE: January 14, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association, Inc.
600 of 998 DOCUMENTS
San Jose Mercury News
January 12, 2004, Monday
Track might ban coach from world indoor meet
BYLINE: By Elliott Almond
SECTION: SPORTS
LENGTH: 795 words
SAN JOSE, Calif. _ U.S. track officials might banish Remi Korchemny from
coaching the American team at the world indoor championships in March because of
his connection to a Burlingame nutrition company under grand jury investigation.
A ranking USA Track & Field official, Stephanie Hightower, said the group is
exploring the legality of excluding the Castro Valley coach because he worked
with Victor Conte Jr., president of Balco Laboratories. Conte is the target of a
money-and-drug investigation involving athletes from baseball, football, boxing
and Olympic sports.
"We don't have any regulations for this," said Hightower, chair of the women's
track committee. "We haven't had to deal with this kind of stuff before."
Three of Korchemny's sprinters _ Kelli White of Union City, Chryste Gaines of
Georgia and Dwain Chambers of England _ had positive drug tests last summer.
White and Gaines had taken modafinil, a sleep-disorder medication that Olympic
drug officials classify as a mild stimulant.
"It bothers me that people continue to attack us," Korchemny said. "I know that
I don't feel I have committed any crime because I strongly believe modafinil is
not something that makes athletes perform better."
Chambers tested positive for THG, the newly discovered steroid at the center of
a growing international scandal. Korchemny said he never gave THG to Chambers,
who faces a suspension from UK Athletics.
The scandal has continued to fuel criticism that USA Track defies worldwide drug
standards, and some in the organization worry about Korchemny's presence during
the championships in Budapest, Hungary.
"The feeling is that his going would be a manifestation that the United States
is not serious about drugs," said Brooks Johnson, director of high performance
at the U.S. Olympic Training Center in Chula Vista.
Johnson said he doesn't endorse sanctions without giving the coach a hearing.
Korchemny, one of the indoor team's three assistants, has not been subpoenaed by
the grand jury nor charged with any wrongdoing.
A handful of track athletes tested positive for modafinil or
tetrahydrogestrinone, which at the time were not on the International
Association of Athletics Federation's banned list. Officials from the U.S.
Anti-Doping Agency said Conte was the source of THG, a previously undetectable
steroid for which four Raiders players, four American track athletes and
Chambers have tested positive.
Athletes who test positive for modafinil face disqualification from the event in
which they tested positive but no further sanctions. White, Gaines and four
other track athletes tested positive for the medication, which they say doesn't
help them run faster. A physician said he gave White the medication to combat
narcolepsy.
Many of the athletes who tested positive are connected to the ZMA Track Club,
which Korchemny started with Conte in 2001. But Korchemny coaches only three of
those implicated.
Another who was caught with modafinil, Chris Phillips of Arkansas, received the
drug from Korchemny at the world championships in Paris. But Korchemny does not
coach Phillips, who placed fifth in the 110-meter hurdles in Paris.
Korchemny accused USA Track of a double standard against him. For instance, no
one has suggested that John Smith of the HSI team in Los Angeles face similar
treatment, although three of his athletes _ Inger Miller, Ato Bolden and Mickey
Grimes _ have tested positive for mild stimulants since 1999. Smith, a 1972
Olympian, is men's coach of the 2005 world championship team.
Another coach to escape scrutiny is Trevor Graham, who is based in Raleigh, N.C.
A handful of his athletes have tested positive, including 400 runner Jerome
Young, who Olympic officials say was allowed to compete in Sydney although the
Americans knew he had tested positive for a steroid in 1999.
Agent Emanuel Hudson, Smith's business partner, said it is unfair to compare the
positives of the HSI athletes with those in the Balco case. For example, he said
Grimes took a cold medication at the Pan American Games last summer, whereas the
rash of modafinil cases seems concentrated in one group.
"It sounds very suspicious when you have a new substance that hadn't been on the
circuit and all of a sudden shows up and shows up with those associated with one
another," said Hudson, a bitter rival of the ZMA team.
But Korchemny, a former Soviet coach, said he learned about modafinil from
European coaches a year before the scandal _ in 2002. He said the drug was to
help fight his fatigue from traveling to meets around the world, not to give to
athletes.
___
(c) 2004, San Jose Mercury News (San Jose, Calif.).
Visit MercuryNews.com, the World Wide Web site of the Mercury News, at
http://www.mercurynews.com.
LOAD-DATE: January 12, 2004
LANGUAGE: ENGLISH
KR-ACC-NO: K3371
JOURNAL-CODE: SJ
Copyright 2004 Knight Ridder/Tribune News Service
Knight Ridder/Tribune News Service
601 of 998 DOCUMENTS
San Jose Mercury News (California)
January 12, 2004 Monday MORNING FINAL EDITION
USA TRACK MIGHT BAN COACH FROM WORLD INDOOR MEET;
OFFICIALS LEERY OF TIES WITH BALCO
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 4D
LENGTH: 768 words
U.S. track officials might banish Remi Korchemny from coaching the American team
at the world indoor championships in March because of his connection to a
Burlingame nutrition company under grand jury investigation.
A ranking USA Track & Field official, Stephanie Hightower, said the group is
exploring the legality of excluding the Castro Valley coach because heworked
with Victor Conte Jr., president of Balco Laboratories. Conte is the target of a
money-and-drug investigation involving athletes from baseball, football, boxing
and Olympic sports.
"We don't have any regulations for this," said Hightower, chair of the women's
track committee. "We haven't had to deal with this kind of stuff before."
Three of Korchemny's sprinters -- Kelli White of Union City, Chryste Gaines of
Georgia and Dwain Chambers of England -- had positive drug tests last summer.
White and Gaines had taken modafinil, a sleep-disorder medication that Olympic
drug officials classify as a mild stimulant.
"It bothers me that people continue to attack us," Korchemny said. "I know that
I don't feel I have committed any crime because I strongly believe modafinil is
not something that makes athletes perform better."
Chambers tested positive for THG, the newly discovered steroid at the center of
a growing international scandal. Korchemny said he never gave THG to Chambers,
who faces a suspension from UK Athletics.
The scandal has continued to fuel criticism that USA Track defies worldwide drug
standards, and some in the organization worry about Korchemny's presence during
the championships in Budapest, Hungary.
"The feeling is that his going would be a manifestation that the United States
is not serious about drugs," said Brooks Johnson, director of high performance
at the U.S. Olympic Training Center in Chula Vista.
Johnson said he doesn't endorse sanctions without giving the coach a hearing.
Korchemny, one of the indoor team's three assistants, has not been subpoenaed by
the grand jury nor charged with any wrongdoing.
A handful of track athletes tested positive for modafinil or
tetrahydrogestrinone, which at the time were not on the International
Association of Athletics Federation's banned list. Officials from the U.S.
Anti-Doping Agency said Conte was the source of THG, a previously undetectable
steroid for which four Raiders players, four American track athletes and
Chambers have tested positive.
Athletes who test positive for modafinil face disqualification from the event in
which they tested positive but no further sanctions. White, Gaines and four
other track athletes tested positive for the medication, which they say doesn't
help them run faster. A physician said he gave White the medication to combat
narcolepsy.
Many of the athletes who tested positive are connected to the ZMA Track Club,
which Korchemny started with Conte in 2001. But Korchemny coaches only three of
those implicated.
Another who was caught with modafinil, Chris Phillips of Arkansas, received the
drug from Korchemny at the world championships in Paris. But Korchemny does not
coach Phillips, who placed fifth in the 110-meter hurdles in Paris.
Korchemny accused USA Track of a double standard against him. For instance, no
one has suggested that John Smith of the HSI team in Los Angeles face similar
treatment, although three of his athletes -- Inger Miller, Ato Bolden and Mickey
Grimes -- have tested positive for mild stimulants since 1999. Smith, a 1972
Olympian, is men's coach of the 2005 world championship team.
Another coach to escape scrutiny is Trevor Graham, who is based in Raleigh, N.C.
A handful of his athletes have tested positive, including 400 runner Jerome
Young, who Olympic officials say was allowed to compete in Sydney although the
Americans knew he had tested positive for a steroid in 1999.
Agent Emanuel Hudson, Smith's business partner, said it is unfair to compare the
positives of the HSI athletes with those in the Balco case. For example, he said
Grimes took a cold medication at the Pan American Games last summer, whereas the
rash of modafinil cases seems concentrated in one group.
"It sounds very suspicious when you have a new substance that hadn't been on the
circuit and all of a sudden shows up and shows up with those associated with one
another," said Hudson, a bitter rival of the ZMA team.
But Korchemny, a former Soviet coach, said he learned about modafinil from
European coaches a year before the scandal -- in 2002. He said the drug was to
help fight his fatigue from traveling to meets around the world, not to give to
athletes.
LOAD-DATE: August 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo;
PHOTO: JIM GENSHEIMER -- MERCURY NEWS
Remi Korchemny has not been charged with wrongdoing and says: "It bothers me
that people continue to attack us."
Copyright 2004 San Jose Mercury News
All Rights Reserved
602 of 998 DOCUMENTS
SUNDAY TELEGRAPH(LONDON)
January 11, 2004, Sunday
This 'stay-awake' drug is far from safe
SECTION: Pg. 22
LENGTH: 223 words
Your article "The 44 hour day" (Review, January 4) gives the impression that
Modafinil is a drug without significant side effects that can be used, as
required, to stay awake. Nothing could be further from the truth. Modafinil is a
prescription-only medicine for the debilitating condition of narcolepsy. Your
reporter attempts to reassure us that Modafinil is "non-addictive and
non-carcinogenic" and mentions none of the dangers associated with taking it.
She even gives the website address for readers to order the drug.
The British National Formulary states that the side effects of Modafinil are
anorexia, abdominal pain, headache, personality disorder, CNS stimulation,
excitation, euphoria, nervousness, dry mouth, palpitations, tachycardia,
hypertension, tremor, gastro-intestinal disturbances, rashes, pruritis and liver
disorders. It also states that dependence cannot be ruled out and that it should
be used with caution.
The availability of prescription-only medication over the internet is a matter
of great concern and about which the medical profession in this country is
trying to educate the public. This prominent article, giving such an unbalanced
view, will contribute to this growing and dangerous problem.
(Dr) Angus Ross MRCP
Barnard Castle, County Durham
[PS]Features: [ES]
Letter to the Editor:
LOAD-DATE: January 11, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Telegraph Group Limited
603 of 998 DOCUMENTS
World Markets Analysis
January 09, 2004
FDA Gives Barr Tentative Backing for Excessive Sleeping Generic
BYLINE: Henry Dummett
SECTION: IN BRIEF
LENGTH: 159 words
Barr Laboratories - a subsidiary of Barr Pharmaceuticals - has obtained
tentative FDA approval for a generic version of Cephalon's Provigil (modafinil)
in 100mg and 200mg strengths. When formally cleared for sale, the drug will be
indicated for use in improving wakefulness in patients suffering from excessive
daytime sleepiness associated with narcolepsy.
Significance: According to IMS Health data, modafinil tablets achieved sales
valued at US$289m in the 12 months ending November 2003. It will be some time,
however, before Barr is able to seize some of the market through its generic
version. Full approval is contingent on the outcome of litigation pending over
the drug's patent status. The case is not due to be heard before January 2005.
Barr initiated a legal challenge against two patents held by Cephalon over
modafinil in February 2003, which provoked Cephalon into filing a patent
infringement suit against Barr in response.
LOAD-DATE: January 09, 2004
LANGUAGE: ENGLISH
Copyright 2004 World Markets Research Limited;
All Rights Reserved
604 of 998 DOCUMENTS
PR Newswire
January 8, 2004 Thursday
Barr Receives Tentative Approval for Modafinil Tablets, 100 mg and 200 mg
SECTION: FINANCIAL NEWS
LENGTH: 738 words
DATELINE: WOODCLIFF LAKE, N.J. Jan. 8
Barr Pharmaceuticals, Inc. (NYSE: BRL) today announced that its wholly-owned
subsidiary, Barr Laboratories, Inc., has received tentative approval from the
U.S. Food and Drug Administration (FDA) for its generic version of Cephalon's
Provigil(R) Tablets (Modafinil Tablets), 100 mg and 200 mg. The Company is
currently litigating whether its products infringe a patent held by Cephalon. A
trial in the U.S. District Court of New Jersey is currently scheduled for
January 2005.
Barr's tentatively approved Modafinil Tablets is indicated to improve
wakefulness in patients with excessive daytime sleepiness associated with
narcolepsy. Modafinil Tablets had annual sales of approximately $289 million,
based on IMS data for the twelve months ended November 2003.
Barr filed an Abbreviated New Drug Application (ANDA) for Modafinil Tablets, 100
mg and 200 mg, with the FDA on December 24, 2002, and received notification of
the application's acceptance for filing in early February 2003. Following
receipt of notice from FDA, Barr notified Cephalon on February 20, 2003 of
Barr's challenge to the two patents that Cephalon had listed in the Orange Book
in connection with Provigil(R). On March 28, 2003, Cephalon filed suit against
four generic pharmaceutical companies, including Barr, for alleged infringement
of one of two listed Cephalon patents in U.S. District Court for the District of
New Jersey.
A tentative approval reflects FDA's preliminary determination that a generic
product satisfies the substantive requirements for approval, subject to the
expiration of all statutorily imposed non-approval periods. A tentative approval
does not allow the applicant to market the generic drug product.
Barr Pharmaceuticals, Inc. and its subsidiaries are engaged in the development,
manufacture and marketing of generic and proprietary pharmaceuticals.
Forward-Looking Statements
The following press release contains a number of forward-looking statements. To
the extent that any statements made in this press release contain information
that is not historical, these statements are essentially forward-looking.
Forward-looking statements can be identified by their use of words such as
"expects," "plans," "will," "may," "anticipates," "believes," "should,"
"intends," "estimates" and other words of similar meaning. These statements are
subject to risks and uncertainties that cannot be predicted or quantified and,
consequently, actual results may differ materially from those expressed or
implied by such forward-looking statements. Such risks and uncertainties
include: the difficulty in predicting the timing and outcome of legal
proceedings, including patent-related matters such as patent challenge
settlements and patent infringement cases; the difficulty of predicting the
timing of U.S. Food and Drug Administration, or FDA, approvals; court and FDA
decisions on exclusivity periods; the ability of competitors to extend
exclusivity periods for their products; the success of our product development
activities; market and customer acceptance and demand for our pharmaceutical
products; our dependence on revenues from significant customers; reimbursement
policies of third party payors; our dependence on revenues from significant
products; the use of estimates in the preparation of our financial statements;
the impact of competitive products and pricing; the ability to develop and
launch new products on a timely basis; the availability of raw materials; the
availability of any product we purchase and sell as a distributor; our mix of
product sales between manufactured products, which typically have higher
margins, and distributed products; the regulatory environment; our exposure to
product liability and other lawsuits and contingencies; the increasing cost of
insurance and the availability of product liability insurance coverage; our
timely and successful completion of strategic initiatives, including integrating
companies and products we acquire and implementing new enterprise resource
planning systems; fluctuations in operating results, including the effects on
such results from spending for research and development, sales and marketing
activities and patent challenge activities; and other risks detailed from time
to time in our filings with the Securities and Exchange Commission.
SOURCE Barr Pharmaceuticals, Inc.
CONTACT: Carol A. Cox of Barr Pharmaceuticals, Inc., +1-201-930-3720,
ccox@barrlabs.com
URL: http://www.prnewswire.com
LOAD-DATE: January 9, 2004
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2004 PR Newswire Association, Inc.
605 of 998 DOCUMENTS
San Jose Mercury News
January 8, 2004, Thursday
Sprinter White out for indoor season
BYLINE: By Elliott Almond
SECTION: SPORTS
LENGTH: 636 words
SAN JOSE, Calif. _ World champion sprinter Kelli White has not trained for four
months because of a knee injury that could hinder preparations for the 2004
Summer Olympics.
Coach Remi Korchemny told the San Jose Mercury News that White, of Union City,
Calif., had knee surgery last month to correct a bone-tissue problem and will
not compete during the upcoming indoor season. White left Thursday to stay with
fiance Boris Henry, a javelin thrower in Germany, where she plans to continue
treatment. She did not respond to an e-mail request for an interview.
"Nobody knows what is wrong with her knee," Korchemny said. "It is very hard to
say what the diagnosis is."
If the problem persists, it could affect White's ability to prepare for the U.S.
Olympic trials in Sacramento in July and the Summer Games in Athens in August.
White, 26, became the first American woman to sweep the sprint races at a world
championships when she won the 100 meters and 200 titles in Paris last year. But
since the August meet, she has been ensnarled in a drug scandal involving a
Burlingame nutrition company and its owner, Victor Conte Jr.
White tested positive for the controversial medication modafinil, which
drug-testing officials classify as a mild stimulant. A physician formerly
connected to Conte's Balco laboratories said he gave White samples of the
medication to combat narcolepsy, which she suffers along with her mother.
White faces the loss of her gold medals in Paris, as well as $120,000 in prize
money. She also tested positive for the drug at the U.S. nationals in Stanford
in June and faces the loss of her American titles as well.
Modafinil was not on a banned list last summer, but officials are using a clause
in the drug code _ "related substances" _ to prosecute athletes caught with the
medication. The World Anti-Doping Agency, which sets the standards for Olympic
drug testing, added the medication to its banned list last week.
Korchemny maintains White did nothing wrong because the medication was not on
the list when she took it, and points out many sleeping disorder researchers say
modafinil is not a stimulant. It is an argument expected to be decided in
hearings with the U.S. Anti-Doping Agency, the group adjudicating the American
cases.
Others who tested positive for modafinil were sprinter Chryste Gaines; hurdlers
Sandra Glover, Chris Phillips and Eric Thomas; and hammer thrower John McEwen,
who also was found with the designer steroid THG. The modafinil cases could lead
to disqualification from the event in which the athletes participated.
While White's case continues to shadow her, Korchemny has other concerns. "I
mostly worry about Kelli's knee," he said.
Korchemny, who also coaches Gaines, estimated that White would be ready to walk
on a track in a few weeks. She is able to complete drills in a swimming pool but
cannot lift weights, he said.
"It is the kind of injury you cannot overload," Korchemny added.
The coach said physicians suggested White's tissue problems are related to an
allergy to milk products. Korchemny said skipping the indoor season would not
jeopardize White's chances for spring and summer if she recovers in time to
begin training.
The knee problem is the latest injury to beset White, a former James Logan High
star. She returned from a tendon tear in 2002, an injury so severe that
Korchemny wondered whether she would walk again. Last spring a painful foot
injury almost forced White to quit.
Instead, she blossomed to become the world's top-ranked sprinter and had hopes
of challenging defending Olympic champion Marion Jones, who took last year off
to have a son.
___
(c) 2004, San Jose Mercury News (San Jose, Calif.).
Visit MercuryNews.com, the World Wide Web site of the Mercury News, at
http://www.mercurynews.com.
LOAD-DATE: January 8, 2004
LANGUAGE: ENGLISH
KR-ACC-NO: K1289
JOURNAL-CODE: SJ
Copyright 2004 Knight Ridder/Tribune News Service
Knight Ridder/Tribune News Service
606 of 998 DOCUMENTS
San Jose Mercury News (California)
January 8, 2004 Thursday MORNING FINAL EDITION
KNEE INJURY COULD THREATEN KELLI WHITE'S OLYMPIC DREAM
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 1D
LENGTH: 606 words
World champion sprinter Kelli White has not trained for four months because of a
knee injury that could hinder preparations for the 2004 Summer Olympics.
Coach Remi Korchemny told the Mercury News that White, of Union City, had knee
surgery last month to correct a bone-tissue problem and will not compete during
the upcoming indoor season. White left today to stay with fiance Boris Henry, a
javelin thrower in Germany, where she plans to continue treatment. She did not
respond to an e-mail request for an interview.
"Nobody knows what is wrong with her knee," Korchemny said. "It is very hard to
say what the diagnosis is."
If the problem persists, it could affect White's ability to prepare for the U.S.
Olympic trials in Sacramento in July and the Summer Games in Athens in August.
White, 26, became the first American woman to sweep the sprint races at a world
championships when she won the 100 meters and 200 titles in Paris last year. But
since the August meet, she has been ensnarled in a drug scandal involving a
Burlingame nutrition company and its owner, Victor Conte Jr.
White tested positive for the controversial medication modafinil, which
drug-testing officials classify as a mild stimulant. A physician formerly
connected to Conte's Balco laboratories said he gave White samples of the
medication to combat narcolepsy, which she suffers along with her mother.
White faces the loss of her gold medals in Paris, as well as $120,000 in prize
money. She also tested positive for the drug at the U.S. nationals in Stanford
in June and faces the loss of her American titles as well.
Modafinil was not on a banned list last summer, but officials are using a clause
in the drug code -- "related substances" -- to prosecute athletes caught with
the medication. The World Anti-Doping Agency, which sets the standards for
Olympic drug testing, added the medication to its banned list last week.
Korchemny maintains White did nothing wrong because the medication was not on
the list when she took it, and points out many sleeping disorder researchers say
modafinil is not a stimulant. It is an argument expected to be decided in
hearings with the U.S. Anti-Doping Agency, the group adjudicating the American
cases.
Others who tested positive for modafinil were sprinter Chryste Gaines; hurdlers
Sandra Glover, Chris Phillips and Eric Thomas; and hammer thrower John McEwen,
who also was found with the designer steroid THG. The modafinil cases could lead
to disqualification from the event in which the athletes participated.
While White's case continues to shadow her, Korchemny has other concerns. "I
mostly worry about Kelli's knee," he said.
Korchemny, who also coaches Gaines, estimated that White would be ready to walk
on a track in a few weeks. She is able to complete drills in a swimming pool but
cannot lift weights, he said.
"It is the kind of injury you cannot overload," Korchemny added.
The coach said physicians suggested White's tissue problems are related to an
allergy to milk products. Korchemny said skipping the indoor season wouldnot
jeopardize White's chances for spring and summer if she recovers in time to
begin training.
The knee problem is the latest injury to beset White, a former James Logan High
star. She returned from a tendon tear in 2002, an injury so severe that
Korchemny wondered whether she would walk again. Last spring a painful foot
injury almost forced White to quit.
Instead, she blossomed to become the world's top-ranked sprinter and had hopes
of challenging defending Olympic champion Marion Jones, who took last year off
to have a son.
LOAD-DATE: August 21, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo;
PHOTO: White
Sprinter from Union City had surgery last month
Copyright 2004 San Jose Mercury News
All Rights Reserved
607 of 998 DOCUMENTS
The Vancouver Sun (British Columbia)
January 5, 2004 Monday Final Edition
Prescription drug keeps you going without feeling tired: Modafinil appears to
offer alertness without side-effects, but doctors remain cautious
SOURCE: The Sunday Telegraph
BYLINE: Julia Llewellyn Smith
SECTION: News; Pg. D8
LENGTH: 811 words
DATELINE: LONDON
LONDON -- It's 4 a.m., I've been up for 20 hours, but I don't feel tired.
The reason for my alertness is 200 milligrams of modafinil, a new prescription
drug that staves off sleep for hours on end. Unlike the drugs we've
traditionally used to keep us going, modafinil appears to have few, if any, side
effects. While coffee-drinkers shake and amphetamine-users jabber aggressively,
on modafinil I feel calm, focused -- and able to work all night.
According to Leon Kreitzman, author of The 24-Hour Society, drugs like modafinil
will transform society.
"Modafinil belongs to a new class of awakening drugs known as eugeroics, which
are unravelling the mechanisms of sleepiness. Once you've done that you will end
up in a world where the need to sleep is optional. I would say that will happen
within the next quarter of a century."
As Kreitzman points out to me, "The idea of a world without sleep may sound too
bizarre to contemplate, but that doesn't mean it won't be acceptable to future
generations."
He adds, "We spend one-third of our lives asleep. If we eliminated that, we'd
have another 25 years to do things."
But at what price? Round-the-clock supermarkets, 24-hour television, electric
lighting, and demanding bosses all make it harder to get the eight hours rest
most of us need to function properly.
Last month, the research group Demos even declared Britain's creativity and
productivity was at risk because the average British person has accumulated a
"sleep deficit" of 25 to 30 hours. It pointed out that too many crucial
decisions, such as the one that launched the Challenger space shuttle, are made
by people handling complex data after days of sleep deprivation.
Already, the armed forces are committed to the drug, having used it to help
British and U.S. troops "power on" to Baghdad: marching for 40 hours, sleeping
for eight, and repeating the pattern without noticeable ill-effect. In previous
conflicts, armies stoked up on amphetamines, but these made soldiers jumpy and
caused terrible "crashes" of fatigue and depression when they were withdrawn.
Worse, such drugs were thought to be responsible for some fatal lapses in
judgment, such as the recent "friendly fire" killing of four Canadian soldiers
in Afghanistan. By contrast, helicopter pilots given modafinil were shown to be
more alert, energetic and confident than those who were not.
If it works for the military, who else could it help? New mothers, long-distance
truck drivers?
Modafinil, which was developed in France a decade ago, was approved in 1998 as
an aid for narcoleptics -- people who fall asleep uncontrollably. Anyone who
wants to get the drug from a pharmacist in Britain needs a prescription. It is,
however, easy to bypass the system, for the drug is readily available to anyone
with a credit card and a computer. Studies in the U.S. show that while only
150,000 Americans are narcoleptics, 250,000 are using modafinil.
It takes me two clicks on the Internet to find the aurapharm.com site, which
will send me 30 tablets for about $175 Cdn. The pills arrive six days later.
I call Ian Davison, of Cephalon, which manufactures modafinil in the U.S. under
the name ProVigil, and is developing even more powerful versions. "We are not
100 per cent sure how ProVigil works," he says. "We know it has an effect on the
hypothalamus region of the brain, which controls our sleep-wake generating
sites, whereas amphetamines control the completely separate dopaminergic side.
"Both sides stimulate the cerebral cortex, which keeps people awake, but the
dopaminergic also stimulates the heart rate and blood pressure. When the
amphetamines wear off there is a crash, while with modafinil people just go back
to their normal rhythm of sleep-wake."
A couple of years ago the U.S. Food and Drug Administration admonished Cephalon
for "over-reaching" its marketing of ProVigil. Davison stresses that modafinil
is intended solely for narcoleptics: "We think we are responsible in how we
market and portray the drug. We certainly don't condone its use 'off-label.' You
really should only take a medicine for what it's prescribed for. In any case,
you're wrong to think you will get to a situation where you won't sleep at all.
In the end, the overwhelming drive to sleep will come whether you use modafinil
or not."
He is backed up by Dr. Irshaad Ebrahim of the London Sleep Centre. "Modafinil is
very effective, and occasionally I prescribe it to insomniacs who can't function
during the day. But to see it as a panacea for all is ridiculous. I would always
try to promote a good night's sleep through natural methods like diet and
exercise." Sleep, he points out, helps the brain store memories and recuperate
from work, and helps the body build its immune system. "If you use a drug to
overcome that, you will deprive yourself of those things."
LOAD-DATE: January 5, 2004
LANGUAGE: ENGLISH
TYPE: Business
Copyright 2004 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
608 of 998 DOCUMENTS
SUNDAY TELEGRAPH(LONDON)
January 04, 2004, Sunday
The 44-Hour Day
BYLINE: BY JULIA LLEWELLYN SMITH
SECTION: Pg. 01
LENGTH: 2328 words
It's 4am, I've been up for 20 hours, but I don't feel tired. I'm not at a wild
party, nor rocking a wailing infant, nor am I lying miserably in bed cursing my
insomnia. I am sitting at my desk paying my bills on the internet as if it were
mid-afternoon. There is none of the usual roar of traffic from outside, just my
keyboard tapping into eerie silence. I call friends in Australia - where it's
mid-afternoon and they're very surprised to hear from me. I put some washing in
the machine, then paint my toenails. I look at the clock: 4.45am. I haven't
yawned once.
The reason for my alertness is 200mg of modafinil, a new prescription drug that
staves off sleep for hours on end. Unlike the drugs we've traditionally used to
keep us going, modafinil appears to have few, if any, side effects. While
coffee-drinkers shake and amphetamine-users jabber aggressively, on modafinil I
feel calm, focused - and able to work all night.
According to Leon Kreitzman, author of The 24-Hour Society, drugs like modafinil
(pronounced modafinil) will transform society. "Modafinil belongs to a new class
of awakening drugs known as eugeroics, which are unravelling the mechanisms of
sleepiness. Once you've done that you will end up in a world where the need to
sleep is optional. I would say that will happen within the next quarter of a
century."
When I tell my friends about Kreitzman's vision, they react in unison. "But I
love sleep," they protest. "A world without it would be horrible." A moment
later, they ask: "Where did you say you got those pills? Could I have one?"
As Kreitzman points out to me, "The idea of a world without sleep may sound too
bizarre to contemplate, but that doesn't mean it won't be acceptable to future
generations. After all, I am talking to you from a mobile phone in a car and 20
years ago we couldn't contemplate that. We spend one-third of our lives asleep.
If we eliminated that we'd have another 25 years to do things."
But at what price? Round-the-clock supermarkets, 24-hour television, electric
lighting, demanding bosses all make it harder and harder to get the eight hours
rest most of us need to function properly. Last month, the research group Demos
even declared the nation's creativity and productivity was at risk because the
average British person has accumulated a "sleep deficit" of 25 to 30 hours. It
pointed out that too many crucial decisions, such as the one that launched the
Challenger space shuttle, are made by people handling complex data after days of
sleep deprivation, and it urged the Government to promote "sleep days" for
bleary-eyed employees to catch up on their rest.
There has been no official response to this report, but it's worth noting that
when Tony Blair was admitted to hospital in October with an irregular heartbeat,
his condition was blamed on too little sleep (he rarely gets more than six
hours) and too much caffeine. Recently, an aide to Lady Thatcher revealed that
the former Prime Minister's famed ability to get by on a mere four hours was
achieved with the help of vitamin B12 injections.
These days, modafinil enables ordinary mortals to imitate her. Already, the
armed forces are committed to the drug, having used it to help British and
American troops "power on" to Baghdad: marching for 40 hours, sleeping for
eight, and repeating the pattern without noticeable ill-effect. In previous
conflicts, armies stoked up on amphetamines, but these made soldiers jumpy and
caused terrible "crashes" of fatigue and depression when they were withdrawn.
Worse, such drugs were thought to be responsible for some fatal lapses in
judgment, such as the recent "friendly fire" killing of four Canadian soldiers
in Afghanistan. By contrast, helicopter pilots given modafinil were shown to be
more alert, energetic and confident than those who were not.
If it works for the military, who else could it help? New mothers, long-distance
lorry drivers, junior doctors, the holiday motorist hell-bent on reaching the
Cote d'Azur in one unbroken drive? Or City traders working 14-hour days, who
resent spending most of the remaining 10 asleep? Or perhaps the contestants in
Shattered, Channel 4's barbaric new game show which starts tonight, who have to
stay awake for a week to win? Recently six American athletes were banned from
competition after it was discovered that they were dosing themselves with the
drug. The truth is that we would love to burn the candle at both ends: we just
need to find the wax.
Modafinil, which was developed in France a decade ago, was approved here and in
America in 1998 as an aid for narcoleptics - people who fall asleep
uncontrollably. Henry Nicholls, 30, a London-based science writer with
narcolepsy, has been using the drug for two years to control his condition,
thought to affect 2,500 people in Britain. "For me, it works amazingly well," he
says. "No one knows what the long-term effects of taking it daily will be, but
I'm happy to be a guinea-pig.
"Before, I used to worry that I'd never be able to hold down a normal job,
because when the sleepiness took over there really was nothing I could do. Now I
am able to function like anyone else. I take a 100mg dose in the morning and in
the evening I go to sleep like anyone else. Conversely, if I forget to take it,
the symptoms come back almost immediately."
Nicholls, like anyone who wants to get the drug from a pharmacist in this
country, needs a prescription for his supply. It is, however, easy to by-pass
the system, for the drug is readily available to anyone with a credit card and a
computer. Studies in the US show that while only 150,000 Americans are
narcoleptics, 250,000 are using modafinil.
It takes me two clicks on the internet to find the aurapharm.com site, which
will send me 30 tablets for 125 ( pounds 87). The pills arrive six days later in
a tiny blister packet, like aspirin. The instructions are in Turkish - although
words like kardiosvaskuuler and depresyon jump out at me. Alarmed, I go on-line
again to find the English instructions and read that the drugs are non-addictive
and non-carcinogenic. More clicking reveals that the drug seems to slow the
release of an amino-acid called GABA, a sleep-promoter in the brain, and may
also help release histamines that promote wakefulness.
I call Ian Davison, of Cephalon, which manufactures modafinil here and in the US
under the name ProVigil, and is developing even more powerful versions. "We are
not 100 per cent sure how ProVigil works," he says. "We know it has an effect on
the hypothalamus region of the brain, which controls our sleep-wake generating
sites, whereas amphetamines control the completely separate dopaminergic side.
"Both sides stimulate the cerebral cortex, which keeps people awake, but the
dopaminergic also stimulates the heart rate and blood pressure. When the
amphetamines wear off there is a crash, while with modafinil people just go back
to their normal rhythm of sleep-wake."
A couple of years ago the US Food and Drug Administration admonished Cephalon
for "over-reaching" its marketing of ProVigil. Davison stresses that modafinil
is intended solely for narcoleptics: "We think we are responsible in how we
market and portray the drug. We certainly don't condone its use 'off-label'. You
really should only take a medicine for what it's prescribed for. In any case,
you're wrong to think you will get to a situation where you won't sleep at all.
In the end, the overwhelming drive to sleep will come whether you use modafinil
or not."
He is backed up by Dr Irshaad Ebrahim of the London Sleep Centre. "Modafinil is
very effective, and occasionally I prescribe it to insomniacs who can't function
during the day. But to see it as a panacea for all is ridiculous. I would always
try to promote a good night's sleep through natural methods like diet and
exercise." Sleep, he points out, helps the brain store memories and recuperate
from work, and helps the body build its immune system. "If you use a drug to
overcome that, you will deprive yourself of those things."
There are no feelings of euphoria associated with modafinil, so it is unlikely
to become fashionable; sleep experts certainly hope it won't. None the less,
when I swallow my first one I am surprised to feel absolutely nothing. I've
started slowly with a 100mg dose - half the recommended amount - to avoid
potential nausea and headaches, the most common side effects. As usual, I've
crawled out of bed reluctantly at 8am, after too-late a night and with a
mountain of tasks ahead of me. My day passes well: I feel sharp, moderately
energetic but certainly not like superwoman. But as the hours wear on, I notice
what doesn't happen: no yawning, no intense yearning for a 2pm nap. Instead I
steadily work through my to-do list.
It's in the evening that things get interesting: I go out to dinner with
friends. We stay until after midnight. Normally I would be flagging, but now I
sit and talk cheerfully as if it were mid-morning (it may help that I'm not
drinking, since Cephalon has not yet tested the effects of mixing alcohol with
modafinil).
I get home and rather than dive into bed as I usually do, I watch some
television and read for half an hour. I turn the light out at about 2am, worried
that I won't sleep at all, but in fact I crash out at once. Astonishingly, I'm
awake before 7am, at least two hours earlier than I usually would after such a
late night, and instantly want to jump out of bed and get going. I pop another
pill and look forward to enjoying another busy day and a late night. I'm
thrilled.
It's time to push my boundaries. I
am going to a party in a pub. Just before I go out I take a 200mg dose. At the
party I am surrounded by thirty-somethings who, shattered after a long week,
can't conceal their yawns. Yet I don't glance once at my watch.
My friends are disappointed that I am not grinding my teeth or acting "wired". I
explain again and again that I am not taking amphetamines. They study my face
for signs of drug-abuse but find nothing. A few accuse me of taking a placebo.
But as, one-by-one, they start calling taxis, I am still there talking
animatedly (but not manically) and having fun. I'm surprised to feel my legs
shake slightly - a symptom of exhaustion. I realise modafinil may stop you from
feeling sleepy but you still feel tired. My limbs grow heavier, but that doesn't
stop the wakefulness. If wake-up drugs catch on, "tiredness" and "sleepiness"
will have to be separated: a hard concept to grasp.
I go home around 1.30am, where again I feel no desire to sleep. At the same
time, when it's cold and dark the prospect of a cosy bed is very appealing. Why
would I want to work all night when I could be snuggled under a duvet? I can't
resist climbing under the covers, but instead of turning off the light, I read.
After an hour, I remember I need to check my tax bill. I might as well do it
now. Having done so, there seems no particular reason - tradition apart - to go
back to bed. It's 3am. There's an article I have to finish, a letter I need to
write. I really should do some washing. Why not do it now?
Yet although it's satisfying to power through my work, it's unpleasant. It's
tiredness versus sleepiness again: I am awake enough to function efficiently but
ploughing through the backlog is still physically wearying. I need a break, and
turn on the television: only BBC News 24. I curse myself for not having cable
and return to the keyboard. The loneliness is miserable. I feel as if I'm the
only person in the world. Yes, I could go out and find an all-night supermarket,
but it's freezing outside and I might get mugged. I end up behaving like
insomniacs everywhere and I go on-line, surfing wildly and sending silly e-mails
in order to feel connected to humanity.
I am beginning to understand how sleep gives a fundamental pattern to your life.
Without that break, time stretches ahead of you dauntingly like a desert. I
worry about what would happen if wake-up drugs were widely available. If your
biggest rival at work was taking them, would you really be able to resist? Would
people who slept be seen as losers? Will this be the 21st-century version of
Eve's apple?
By 6am I have had a bath and breakfast. I can't wait for the rest of the world
to wake up. As soon as the paper shop opens at 7am, I'm out of the house,
desperate for human contact. I bump into a neighbour. "I can tell you've been up
all night, you look terrible," he says. Modafinil works, yes, but you need to
invest heavily in under-eye concealer.
I've now been 24 hours without sleep. The rest of the day isn't much fun,
although I get through it. There's a family brunch, followed by more long hours
on-line organising a complicated trip to Australia. By now, the gulf between
fatigue and sleepiness is even more apparent. I still feel no urge to put my
head down, but I am just as irritable and subdued as I always am without a
decent night's sleep. If I were a pilot, I wouldn't want to fly a mission right
now.
After a meal, I cheer up considerably. (The most important thing is to remember
to eat - if you are going to stay awake for double the normal amount of time,
you'll need double the amount of fuel.) I try to nap during the day, but can't.
I go to bed at 11pm and don't fall asleep until gone 2am. Modafinil has given me
well over 40 hours on the trot - as promised.
As I write this, the following morning, I have a nasty cold - I suspect the
effect of no sleep on my immune system. I don't feel as if I've missed a night's
sleep, but by mid-afternoon I'm yawning as I normally would.
I realise now how much more bushy-tailed I was on modafinil days. I hated my
sleepless night because it felt so unnatural, but I still think modafinil could
be the perfect response to a broken night, an urgent deadline or jet-lag. And
no, I will not share the rest of my tablets with my friends. If they want to get
ahead, they can get their own.
LOAD-DATE: January 4, 2004
LANGUAGE: ENGLISH
Copyright 2004 The Telegraph Group Limited
609 of 998 DOCUMENTS
Aberdeen Evening Express
January 2, 2004
US track stars test positive
SECTION: Sport; Soccer; Scots1/2/3; Pg. 38
LENGTH: 301 words
Athletics: Sprint champion Kelli White is one of six American athletes to have
tested positive for the stimulant modafinil, the US Olympic Committee confirmed.
She tested positive at the USA Track and Field Championships in June, which was
the qualifying event for American athletes for the World Championships in Paris.
The 26-year-old White went on to win the 100 and 200 metre gold medals at the
Paris competition two months later, and also tested positive there.
Fellow sprinter Chryste Gaines and hurdlers Sandra Glover, Chris Phillips and
Eric Thomas had modafinil in their system, while hammer thrower John McEwen
produced a positive sample for both modafinil and tetrahydrogestrinone (THG).
football: Chelsea are 4/1 favourites for the FA Cup with bookmaker William Hill,
who also offer 6/1 Arsenal, Manchester United; 7 Liverpool; 14 Middlesbrough,
Newcastle; 16 Everton, Tottenham; 20 Blackburn, Fulham, Portsmouth; 25
Manchester City.
Champs out to impress HOCKEY: Dundee Wanderers men's team is the only Scottish
side to be competing in this weekend's Coaching Solutions Indoor Invitational
Tournament at centres in Kidderminster and Birmingham.
As reigning Scottish Indoor champions, Wanderers are expected to get to the
quarter-finals, but will need to qualify from Pool B by finishing ahead of
Stourport, Kingston upon Hull and Swansea.
The tournament is being played over January 3 and 4.
Cove Lottery FOOTBALL: Numbers drawn at Cove Rangers Lottery were: 3, 8, 9, 16,
22, 25. There were no winners.
Consolation £10 winners were: D Boyd, c/o McIntosh Donalds; Ernie Hay, c/o Cove
Rangers; Jim Gillespie, c/o Three Lums.
Next week's prize is £1,400 using 1-25.
Alickie quiz ANSWERS: 1 Sir Clive Woodward; 2 Hibernian; 3 Sydney; 4 Romania; 5
Gregor Townsend.
LOAD-DATE: January 3, 2004
LANGUAGE: English
Copyright 2004 Aberdeen Evening Express
610 of 998 DOCUMENTS
Akron Beacon Journal (Ohio)
January 1, 2004 Thursday 1 STAR EDITION
U.S. ATHLETES FLUNK DRUG TEST;
WHITE, NORTH CANTON'S MCEWEN AND FIVE OTHERS ARE APPEALING THE RESULTS
BYLINE: From staff and wire reports
SECTION: SPORTS; Pg. C3
LENGTH: 302 words
Sprint champion Kelli White and six other American athletes flunked drug tests
this summer, according to a report issued by the U.S. Olympic Committee.
White and five other track and field athletes tested positive for the banned
stimulant modafinil.
Hammer thrower John McEwen of North Canton tested positive for modafinil and the
newly discovered steroid THG.
Cyclist Adham Sbeih tested positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
samples from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing the test results, the USOC said in a news
release from its base in Colorado Springs, Colo. Any suspensions or other
penalties would come only after appeals.
U.S. shot put champion Kevin Toth of Hudson, who reportedly tested positive for
THG, said Wednesday he is still awaiting word from his lawyer about his status.
"We're still in a wait-and-see mode," Toth said.
McEwen and Toth both have a goal of competing in the U.S. Track and Field Trials
to make the 2004 Olympics Games next August in Athens, Greece.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, 400-meter runner Sandra Glover, McEwen, and hurdler
Eric Thomas of Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the world championships.
McEwen's attorney, Howard Jacobs, said McEwen would consider working with the
International Association of Athletics Federations, which floated an offer of
leniency for drug cheaters who provide valuable information about doping.
No such offer has yet been made by the IAAF, Jacobs said in an interview with
the Associated Press.
LOAD-DATE: August 24, 2005
LANGUAGE: ENGLISH
NOTES: 2004 Olympics
Copyright 2004 Akron Beacon Journal
All Rights Reserved
611 of 998 DOCUMENTS
The Australian
January 1, 2004 Thursday All-round Country Edition
White among seven US athletes to fail tests
SOURCE: AFP
SECTION: SPORT; Pg. 22
LENGTH: 422 words
* Drugs
DUAL sprint world champion Kelli White tested positive for the banned substance
modafinil in June, two months before returning another positive sample at the
world titles, the US Olympic Committee announced yesterday.
White was the biggest name among the seven leading US athletes to fail drug
tests during the northern summer.
Also testing positive for modafinil at the national titles were former US
champion sprinter Chryste Gaines, four-time national champion 400metre hurdler
Sandra Glover, reigning US 400m hurdles champion Eric Thomas and hammer thrower
John McEwen.
Hurdler Chris Phillips tested positive for modafinil at the 2003 world
championships in Paris in August.
Cyclist Adham Sbeih became the first American to test positive for the hormone
EPO at the US championships in August, the USOC said.
McEwen also tested positive for the new designer steroid tetrahydrogestrinone,
or THG.
All seven plan to appeal.
Modafinil use results in disqualification at the event at which a positive test
has occurred but no suspension. THG use can lead to a two-year ban.
US Anti-Doping Agency spokesman Rich Wanninger said yesterday's announcement was
made after samples taken from the athletes went through a series of confirmation
tests and a 30-day review.
White won the 100m-200m double at the world championships, where she also tested
positive to modafinil.
She could lose her two gold medals and $US120,000 ($160,650) prizemoney from the
world titles after testing positive for modafinil, a stimulant which is used to
treat narcolepsy.
White is one of 40 athletes who have been subpoenaed to testify into a federal
government investigation of a San Francisco lab, BALCO, which has been linked to
THG.
White's doctor, Brian Goldman, is BALCO's former medical director.
Gaines, 33, won the US 100m championship in 2001 but is running faster now than
ever before. She set her best time of 10.86sec in the 100m at the season-ending
World Athletics Finals in Monaco in 2003.
Glover, 34, is a four-time US 400m hurdle champion and won the silver medal at
the world titles behind Sydney's Jana Pittman last year.
The 31-year-old Phillips finished fourth at the national titles last year and
fifth at the world titles in the 110m hurdles.
Thomas is the reigning US champion in the 400m hurdles and won silver medals at
the Pan American Games in 2003 and 1999.
McEwen, 29, placed second at the 2003 US championships at Stanford in the hammer
throw with a toss of 72.96m.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: AUS
Copyright 2004 Nationwide News Pty Limited
612 of 998 DOCUMENTS
The Australian
January 1, 2004 Thursday All-round Metro Edition
White among seven in US to fail tests
SOURCE: AFP
SECTION: SPORT; Pg. 22
LENGTH: 373 words
* Drugs
DUAL sprint world champion Kelli White tested positive for the banned substance
modafinil in June, two months before returning another positive sample at the
world titles, the US Olympic Committee announced yesterday.
Also testing positive for modafinil at the national titles were former US
champion sprinter Chryste Gaines, four-time national champion 400metre hurdler
Sandra Glover, reigning US 400m hurdles champion Eric Thomas and hammer thrower
John McEwen.
Hurdler Chris Phillips tested positive for modafinil at the 2003 world
championships in Paris in August.
Cyclist Adham Sbeih became the first American to test positive for the hormone
EPO at the US championships in August, the USOC said.
McEwen also tested positive for the new designer steroid tetrahydrogestrinone,
or THG.
All seven plan to appeal.
US Anti-Doping Agency spokesman Rich Wanninger said yesterday's announcement was
made after samples taken from the athletes went through a series of confirmation
tests and a 30-day review.
White won the 100m-200m double at the world championships, where she also tested
positive to modafinil.
She could lose her two gold medals and $US120,000 ($160,650) prizemoney from the
world titles after testing positive for modafinil, a stimulant.
White is one of 40 athletes who have been subpoenaed to testify into a federal
government investigation of a San Francisco lab, BALCO, which has been linked to
THG.
White's doctor, Brian Goldman, is BALCO's former medical director.
Gaines, 33, won the US 100m championship in 2001 but is running faster now than
ever before. She set her best time of 10.86sec in the 100m at the season-ending
World Athletics Finals in Monaco in 2003.
Glover, 34, is a four-time US 400m hurdle champion and won the silver medal at
the world titles behind Sydney's Jana Pittman last year.
The 31-year-old Phillips finished fourth at the national titles last year and
fifth at the world titles in the 110m hurdles.
Thomas is the reigning US champion in the 400m hurdles and won silver medals at
the Pan American Games in 2003 and 1999.
McEwen, 29, placed second at the 2003 US championships at Stanford in the hammer
throw with a toss of 72.96m.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: AUS
Copyright 2004 Nationwide News Pty Limited
613 of 998 DOCUMENTS
Courier Mail (Queensland, Australia)
January 1, 2004 Thursday
Top US athletes fail tests for drugs
SECTION: SPORT; Pg. 32
LENGTH: 391 words
DUAL sprint world champion Kelli White tested positive for the banned substance
modafinil in June, two months before returning another positive sample at the
world titles, the United States Olympic Committee announced in Colorado
yesterday.
White was the biggest name among seven leading US athletes to fail drug tests
during the northern hemisphere summer.
Also testing positive for modafinil at the nationals were former US champion
sprinter Chryste Gaines, four-time national champion 400m hurdler Sandra Glover,
reigning US 400m hurdles champion Eric Thomas and hammer thrower John McEwen.
Hurdler Chris Phillips tested positive for modafinil at the Paris world
championships in August.
Cyclist Adham Sbeih became the first American to test positive for the hormone
EPO at the US cycling championships in August, the USOC said.
McEwen also tested positive for the new designer steroid tetrahydrogestrinone,
or THG.
The seven Americans all plan to appeal.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension, while THG use can lead to a two-year ban.
White, who won the 100m-200m double at the world championships where she also
tested positive to modafinil, is the most prominent name to fail the drug tests.
She is one of 40 athletes who have been subpoenaed to testify into a federal
government probe of a San Francisco-area lab, BALCO, that has been linked to
THG.
She could lose her two gold medals and $US120,000 ($A160,650) in prizemoney from
the world titles after testing positive for modafinil, a stimulant used to treat
narcolepsy.
White's doctor Brian Goldman is BALCO's former medical director.
Gaines won the US 100m championship in 2001 but is running faster now than she
ever has. She set a personal best of 10.86sec in the 100m at the World Athletics
Finals in Monaco in 2003.
Glover, 34, is a four-time US 400m hurdle champion and won the silver medal at
the worlds in Paris this year.
The 31-year-old Phillips finished fourth at the nationals this year and fifth at
the worlds in the 110m hurdles.
Thomas is the reigning US champion in the 400m hurdles and won silver medals at
the Pan American Games in 2003 and 1999.
McEwen, 29, placed second at the 2003 US championships in Stanford in the hammer
throw with a toss of 72.96m.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: CML
Copyright 2004 Nationwide News Pty Limited
614 of 998 DOCUMENTS
Geelong Advertiser (Regional Daily)
January 1, 2004 Thursday
Stars fail drug tests
SOURCE: AFP
SECTION: SPORT; Pg. 46
LENGTH: 390 words
DUAL sprint world champion Kelli White tested positive for the banned substance
Modafinil in June, two months before returning another positive sample at the
world titles, the United States Olympic Committee has announced.
White was the biggest name among the seven leading US athletes to fail drug
tests during the northern hemisphere summer.
Also testing positive for Modafinil at the nationals were former US champion
sprinter Chryste Gaines; four-time national champion 400m hurdler Sandra Glover;
reigning US 400m hurdles champion Eric Thomas and hammer thrower John McEwen.
Hurdler Chris Phillips tested positive for Modafinil at the 2003 Paris world
championships in August.
Cyclist Adham Sbeih became the first American to test positive for the hormone
EPO at the US cycling championships in August, the USOC said.
McEwen also tested positive for the new designer steroid tetrahydrogestrinone,
or THG.
The seven Americans all plan to appeal.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension.
THG use can lead to a two-year ban.
The announcement was made after samples went through a series of confirmation
tests and a 30-day review.
White, who won the 100m-200m double at the world championships where she also
tested positive to Modafinil, is the most prominent name to fail the drug tests.
Her first positive sample was returned at the national track and field
championships in June.
White is one of 40 athletes who have been subpoenaed to testify into a US
government probe of a San Francisco-area lab, BALCO, that has been linked to
THG.
She could lose her two gold medals and $160,650 in prizemoney from the world
titles after testing positive for Modafinil, a stimulant used to treat
narcolepsy.
Gaines won the US 100m championship in 2001. She set a personal best of 10.86
seconds in the 100m at the World Athletics Finals in 2003.
Glover, 34, is a four-time US 400m hurdle champion and won silver at the worlds
in Paris this year.
The 31-year-old Phillips finished fourth at the nationals this year and fifth at
the worlds in the 110m hurdles.
Thomas is the reigning US champion in the 400m hurdles and won silver at the Pan
American Games in 2003 and 1999.
McEwen, 29, was second at the 2003 US championships in the hammer throw.
LOAD-DATE: January 2, 2004
LANGUAGE: ENGLISH
JOURNAL-CODE: GAT
Copyright 2004 Nationwide News Pty Limited
All Rights Reserved
615 of 998 DOCUMENTS
The Sun
January 1, 2004
TRACK ACE KELLI FAILS TEST NO2
BYLINE: Harry Talbot
SECTION: ATHLETICS
LENGTH: 243 words
THE world's fastest woman Kelli White has tested positive for drugs again.
White, 26, won the 100 and 200 metre titles at the athletics World Championships
in August -but subsequently tested positive for the banned stimulant modafinil.
She currently faces the loss of both her world championship gold medals.
Now the US Olympic committee have revealed White is one of seven athletes who
failed drugs tests last summer -in her case for the same substance, modafinil.
The other six athletes implicated are hammer thrower John McEwen, cyclist Adham
Sbeih, sprinter Chryste Gaines and hurdlers Sandra Glover, Eric Thomas and Chris
Phillips.
White won both 100m and 200m events at the US championships -where she tested
positive -and qualified for the World Championships in Paris in the process.
Steroid
She is coached by Remy Korchemny, who also guides British sprinter Dwain
Chambers.
Chambers currently faces a two-year ban for using the newly-discovered steroid
THG.
At the time of her positive test for modafinil in August, White said she was
taking it to combat a sleep disorder.
This claim was ridiculed by international track officials after word emerged of
other athletes using the banned stimulant.
All seven athletes who failed tests last summer are challenging the results.
If modafinil use is proved, it results in disqualification at the event at which
a positive test occurred -but no suspension.
LOAD-DATE: January 2, 2004
LANGUAGE: English
PUB-TYPE: Newspaper
Copyright 2004 NEWS GROUP NEWSPAPERS LTD
616 of 998 DOCUMENTS
Agence France Presse -- English
December 31, 2003 Wednesday
Seven leading US athletes failed drug tests: USOC
SECTION: Sports
LENGTH: 482 words
DATELINE: COLORADO SPRINGS, Colorado, Dec 30
Seven leading US athletes, including American sprint champion Kelli White,
failed drug tests this summer, the United States Olympic Committee announced on
Tuesday.
White tested positive for the banned substance Modafinil at the June United
States Track and Field Championships in Stanford, California, the USOC revealed.
Also testing positive for Modafinil at the nationals were former US champion
sprinter Chryste Gaines; four-time national champion hurdler Sandra Glover;
reigning US hurdles champion Eric Thomas and hammer thrower John McEwen.
Hurdler Chris Phillips tested positive for Modafinil at the 2003 Paris World
Championships in August, the USOC said in a news release.
Cyclist Adham Sbeih tested positive for the hormone EPO at the US cycling
championships in August.
McEwen also tested positive for the new designer steroid tetrahydrogestrinone,
or THG.
The seven Americans all plan to appeal, the USOC said.
Rich Wanninger, spokesman for the US Anti-Doping Agency, said Tuesday's
announcement was made after samples taken from the athletes went through a
series of confirmation tests and a 30-day review.
Wanninger downplayed the significance of Tuesday's announcement but others have
said the number of positive tests this summer is unprecedented for American
athletes.
"It is not our announcement," said Wanninger.
White, the reigning world and US champion in both the 100 and 200 metres, is the
most prominent name to fail the drug tests. The USOC said she also tested
positive for Modafinil at the worlds.
The 26-year-old White ran a personal best time of 10.85secs to capture the world
100m title. She also won 100m races in Brussells, Los Angeles and Portland,
Oregon in 2003.
White is one of 40 athletes who has been subpoenaed to testify into a federal
government probe of a San Francisco-area lab, BALCO, that has been linked to
THG.
White could lose her two gold medals and 120,000 dollars in prize money from the
world titles after testing positive for Modafinil, a stimulant used to treat
narcolepsy,
White's doctor Brian Goldman is BALCO's former medical director.
Gaines won the US 100m championship in 2001 but is running faster now than she
ever has.
She set a personal best of 10.86secs in the 100m at the World Athletics Finals
in Monaco in 2003. The 33-year-old Gaines also ran a 10.88 this year in
Brussells.
Glover, 34, is a four-time US 400m hurdle champion and won the silver medal at
the worlds in Paris this year.
The 31-year-old Phillips finished fourth at the nationals this year and fifth at
the worlds in the 110-metre hurdles.
Thomas is the reigning US champion in the 400m hurdles and won silver medals at
the Pan American Games in 2003 and 1999.
McEwen, 29, placed second at the 2003 US championships in Stanford in the hammer
throw with a toss of 72.96 metres.
gph03
Athletics-USA-doping
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Agence France Presse
617 of 998 DOCUMENTS
The Associated Press
December 31, 2003, Wednesday, BC cycle
White's agent wants case settled quickly
SECTION: Sports News
LENGTH: 251 words
DATELINE: LONDON
Kelli White's agent wants the sprint champion's drug case settled quickly,
saying it is hurting her financially and damaging her reputation.
White and six other American athletes tested positive for banned substances, the
U.S. Olympic Committee said Tuesday following a review by the U.S. Anti-Doping
Agency.
White faces the loss of two world championship gold medals because of use of the
stimulant modafinil. The USOC said White also tested positive for modafinil at
the national championships in June, when she swept the 100 and 200 meters.
Modafinil, considered a minor stimulant, carries a public warning and
disqualification from the event where the test took place, but no ban.
All seven athletes are challenging the results, the USOC said from its Colorado
headquarters. Any penalties would come only after arbitration.
White's agent, Robert Wagner, said the sprinter is awaiting a final decision
from the USADA.
"If they don't make a decision, we have to find a court because it's hurting us,
financially, reputationwise, everything," he said Wednesday by telephone from
Austria.
White said she was prescribed modafinil for a sleeping disorder - a claim
dismissed by international track officials after word emerged of other athletes
using the substance.
Wagner wants the matter decided before this summer's Athens Olympics.
"This USOC announcement won't do them any good," he said. "We tried to follow
the rules. Can we get a position from someone so we can move forward?"
LOAD-DATE: January 1, 2004
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
618 of 998 DOCUMENTS
Associated Press Online
December 31, 2003 Wednesday
White's Agent Wants Case Settled Quickly
SECTION: SPORTS
LENGTH: 250 words
DATELINE: LONDON
Kelli White's agent wants the sprint champion's drug case settled quickly,
saying it is hurting her financially and damaging her reputation. White and six
other American athletes tested positive for banned substances, the U.S. Olympic
Committee said Tuesday following a review by the U.S. Anti-Doping Agency.
White faces the loss of two world championship gold medals because of use of the
stimulant modafinil. The USOC said White also tested positive for modafinil at
the national championships in June, when she swept the 100 and 200 meters.
Modafinil, considered a minor stimulant, carries a public warning and
disqualification from the event where the test took place, but no ban.
All seven athletes are challenging the results, the USOC said from its Colorado
headquarters. Any penalties would come only after arbitration.
White's agent, Robert Wagner, said the sprinter is awaiting a final decision
from the USADA.
"If they don't make a decision, we have to find a court because it's hurting us,
financially, reputationwise, everything," he said Wednesday by telephone from
Austria.
White said she was prescribed modafinil for a sleeping disorder - a claim
dismissed by international track officials after word emerged of other athletes
using the substance.
Wagner wants the matter decided before this summer's Athens Olympics.
"This USOC announcement won't do them any good," he said. "We tried to follow
the rules. Can we get a position from someone so we can move forward?"
LOAD-DATE: January 1, 2004
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
619 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 31, 2003, Wednesday, BC cycle
White's agent wants case settled quickly
SECTION: Sports News
LENGTH: 256 words
DATELINE: LONDON
Kelli White's agent wants the sprint champion's drug case settled quickly,
saying it is hurting her financially and damaging her reputation.
White and six other American athletes tested positive for banned substances, the
U.S. Olympic Committee said Tuesday following a review by the U.S. Anti-Doping
Agency.
White, of Union City, Calif., faces the loss of two world championship gold
medals because of use of the stimulant modafinil. The USOC said White also
tested positive for modafinil at the national championships in June, when she
swept the 100 and 200 meters. Modafinil, considered a minor stimulant, carries a
public warning and disqualification from the event where the test took place,
but no ban.
All seven athletes are challenging the results, the USOC said from its Colorado
headquarters. Any penalties would come only after arbitration.
White's agent, Robert Wagner, said the sprinter is awaiting a final decision
from the USADA.
"If they don't make a decision, we have to find a court because it's hurting us,
financially, reputation-wise, everything," he said Wednesday by telephone from
Austria.
White said she was prescribed modafinil for a sleeping disorder - a claim
dismissed by international track officials after word emerged of other athletes
using the substance.
Wagner wants the matter decided before this summer's Athens Olympics.
"This USOC announcement won't do them any good," he said. "We tried to follow
the rules. Can we get a position from someone so we can move forward?"
LOAD-DATE: January 1, 2004
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
620 of 998 DOCUMENTS
Birmingham Evening Mail
December 31, 2003, Wednesday
ATHLETICS: WHITE FAILS DRUGS TEST
SECTION: SPORT; Pg. 40
LENGTH: 119 words
Sprint champion Kelli White is one of six American athletes to have tested
positive for the stimulant modafinil.
White was one of two athletes to provide two positive urine samples.
Her first was taken at the USA Track and Field Championships in June, the
qualifying event for American athletes for the World Championships in Paris.
The 26-year-old White went on to win the 100 and 200 metre gold medals at the
Paris competition two months later, and also tested positive there.
Fellow sprinter Chryste Gaines and hurdlers Sandra Glover, Chris Phillips and
Eric Thomas had modafinil in their system, while hammer thrower John McEwen
produced a positive sample for both modafinil and THG.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
PUB-TYPE: PAPER
Copyright 2003 Midland Independent Newspapers plc
621 of 998 DOCUMENTS
Bristol Evening Post
December 31, 2003
Seven Us Stars Test Positive
SECTION: Sport; Athletics; Athletes; Pg. 46
LENGTH: 159 words
Sprint champion Kelli White is just one of seven American athletes to have
tested positive for the stimulant modafinil, the US Olympic Committee confirmed.
White's first positive urine sample was taken at the USA Track and Field
Championships in June, which was the qualifying event for American athletes for
the World Championships in Paris.
The 26-year-old went on to win the 100 and 200 metre gold medals at the Paris
competition two months later, and also tested positive there.
Fellow sprinter Chryste Gaines and hurdlers Sandra Glover, Chris Phillips and
Eric Thomas had modafinil in their system, while hammer thrower John McEwen
produced a positive sample for both modafinil and tetrahydrogestrinone (THG).
Meanwhile, a sample provided by cyclist Adham Sbeih at the US National
Championships has shown up the endurance-boosting EPO.
All seven dispute the findings and will now argue their case to the US
AntiDoping Agency.
LOAD-DATE: January 1, 2004 3112BRISEP211seven
LANGUAGE: English
PUB-TYPE: News
Copyright 2003 Bristol United Press
622 of 998 DOCUMENTS
Calgary Herald (Alberta, Canada)
December 31, 2003 Wednesday Final Edition
Women's sprint champ fails test
SOURCE: The Associated Press
BYLINE: Rob Gloster
SECTION: Sports; Pg. E2
LENGTH: 449 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
metres.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes -- including McEwen and Chambers -- have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports -- including baseball sluggers Barry Bonds and Jason Giambi
-- appeared before the panel.
McEwen's lawyer, Howard Jacobs, said the hammer thrower would consider working
with the International Association of Athletics Federations, which floated an
offer of leniency for drug cheaters who provide valuable information about
doping.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: Herald Archive, Associated Press; Kelli White has tested
positive for banned stimulant modafinil.
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
623 of 998 DOCUMENTS
THE DAILY TELEGRAPH(LONDON)
December 31, 2003, Wednesday
US reveal failed tests
BYLINE: By Tom Knight
SECTION: Pg. 08
LENGTH: 460 words
THE extent of the doping problem facing officials in the United States was
outlined yesterday when the sprinter Kelli White was named among seven American
athletes who failed drug tests during the year.
In addition to those seven, three other so-far unnamed US athletes are facing
disciplinary hearings after testing positive for the new designer steroid, THG.
White tested positive for the banned stimulant modafinil as did her fellow
sprinter, Chryste Gaines, the 400 metres hurdlers Sandra Glover and Eric Thomas,
the 110m hurdler Chris Phillips and hammer thrower John McEwen, who was also
among the four Americans reported to have failed tests for THG. Urine samples
provided by the cyclist, Adham Sbeih, were found to contain the blood-boosting
hormone, EPO.
All seven athletes, who were listed by the US Olympic Committee, are appealing
against their test results and, to the continued frustration of the World
Anti-Doping Agency, none of the cases have been resolved.
White tested positive for modafinil on two occasions during the summer. The
first time was at the World Championships in Paris, where she became the first
woman to win the 100m and 200m sprint double. She claimed that she had been
prescribed the drug to combat narcolepsy and did not know that it was a banned
substance. She said she was careful about doping issues but, while she listed
other medication on the form she handed to drug testing officials in Paris, she
did not include the drug that contained modafinil. Speaking during the World
Championships, she said: "Because I took it so early in the day, I never thought
to mention it. After a competition, it is quite hard to remember everything you
have taken in the day."
The French dope testers have long thought that the drug in the White case was
being used by athletes seeking a way round the system. For their part, the
International Association of Athletics Federations insisted that modafinil was
classified as a stimulant and carried the punishment of instant disqualification
and a public warning.
White's positive test in Paris means she faces being stripped of her two gold
medals. Her case was not helped by the fact that she was also found to have
tested positive for modafinil at the US Championships in June, a result which
means she should not have even been included in the American team for Paris.
Gaines, Glover, McEwen and Thomas were also found to have modafinil in their
system when the urine samples collected at the national championships were
revisited in the wake of the THG scandal.
Phillips, meanwhile, tested positive for modafinil at the World Championships,
where he claimed he was given the drug by his coach to combat jet-lag and
fatigue.
[PS]Sport: [ES]
Rugby Union:
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LANGUAGE: ENGLISH
Copyright 2003 Telegraph Group Limited
624 of 998 DOCUMENTS
Edmonton Journal (Alberta)
December 31, 2003 Wednesday Final Edition
Seven American athletes flunked tests: USOC
SOURCE: The Associated Press
SECTION: Sports; Pg. D1
LENGTH: 401 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release.
Any suspensions or other penalties would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday White also tested positive for modafinil at
the national championships in June, when she swept the 100 and 200 metres.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban.
- - -
EPHEDRA UPDATE
Steve Bechler's parents welcomed the U.S. government's ban on ephedra, saying it
should save lives and ensure their son did not die in vain.
The Baltimore Orioles pitcher's heat stroke in February was linked to the herbal
weight-loss supplement, which has also been blamed for more than 150 other
deaths.
"In one aspect, I feel that it's not enough, because it won't bring Steve back,"
Bechler's mother, Pat, said from Medford, Ore. "But it will help and protect
other people."
While the NFL, NCAA and International Olympic Committee have banned ephedra,
Major League Baseball has not.
Steve Bechler, 23, died during spring training in Fort Lauderdale, Fla.
The medical examiner said ephedra contributed to heat stroke.
The Associated Press
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: The Associated Press, File; Kelli White: Not a banner
year.
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
625 of 998 DOCUMENTS
Facts on File World News Digest
December 31, 2003
Sports;
Bonds Testifies in Drug Probe; Other Developments
SECTION: Pg. 1098A1
LENGTH: 851 words
Left fielder Barry Bonds, who played for the San Francisco Giants of Major
League Baseball (MLB), December 4 testified before a federal grand jury in San
Francisco, California that was investigating Bay Area Laboratory Cooperative
(BALCO), a nutritional supplement company in Burlingame, California. The grand
jury was investigating alleged tax evasion by the company, which listed several
high-profile athletes, including Bonds, among its clients. It was also looking
into accusations that BALCO had provided banned performance-enhancing drugs to
its clients. The probe had been prompted in part by the recent discovery of
tetrahydrogestrinone (THG), an anabolic steroid previously unknown to drug
testers. [See 2003 Sports: Bonds, Rodriguez Win Baseball MVPs; Other
Developments; 2003 U.S. Anti-Doping Agency Finds New 'Designer' Steroid; Several
Athletes Test Positive; Other Developments]
The grand jury was reportedly focusing on Victor Conte Jr., the president of
BALCO who was said to have been Bonds's nutritionist since 2000, and Greg
Anderson, Bonds's personal trainer since the late 1990s. Bonds's appearance
before the grand jury did not necessarily mean that he had been implicated in
any wrongdoing. Bonds, the reigning National League most valuable player, had
repeatedly denied using performance-enhancing drugs. Proceedings of the grand
jury were closed to the public.
Several other athletes December 11 testified before the grand jury. Those
athletes included New York Yankees first baseman Jason Giambi; MLB outfielder
Gary Sheffield, a free agent; center Barret Robbins and linebacker Bill
Romanowski, who played for the Oakland Raiders of the National Football League;
and boxer Shane Mosley. [See 2003 U.S. Anti-Doping Agency Finds New 'Designer'
Steroid; Several Athletes Test Positive; Other Developments; 2003 Buccaneers
Rout Raiders to Win Super Bowl XXXVII; Tampa Bay Defense Dominates]
U.S. Announces Positive Tests
The U.S. Olympic Committee (USOC) December 30 announced that seven U.S.
athletes had tested positive for banned substances earlier in 2003. (Some of the
athletes had already been publicly identified.) The USOC said that sprinters
Kelli White and Chryste Gaines, hurdlers Sandra Glover and Eric Thomas, and
hammer thrower John McEwen had tested positive for modafinil, a stimulant used
to treat narcolepsy, a sleep disorder, at the U.S. Track and Field Championships
in June. The USOC said that McEwen had also tested positive for THG. The USOC
said that hurdler Chris Phillips had tested positive for modafinil at the World
Track and Field Championships in August. The USOC also revealed that cyclist
Adham Sbeih had tested positive for the banned drug erythropoietin, or EPO,
which improved endurance. [See 2003 U.S. Anti-Doping Agency Finds New 'Designer'
Steroid; Several Athletes Test Positive; Other Developments; 2001 Armstrong Wins
Third Straight Tour de France; American Rider Joins Cycling's Elite]
The USOC officially revealed the athletes' identities after two of their urine
tests had been found to contain the banned substances, and after a 30-day review
period. Since modafinil was not officially banned by the International
Association of Athletics Federations (IAAF), track and field's world governing
body, but was considered a related substance, the athletes who tested positive
faced disqualification only from the event at which the tests were taken.
Athletes who tested positive for THG faced a two-year ban. [See below]
The IAAF November 22 had said that two athletes tested positive for THG at the
sport's world championships in August, but did not identify the athletes.
U.S. Ruling on Sprinter Questioned
International Olympic Committee (IOC) President Jacques Rogge December 1 said
that U.S. officials had failed to satisfactorily explain why U.S. sprinter
Jerome Young had been cleared to participate in the 2000 Summer Olympics. Young
in 1999 had tested positive for anabolic steroids, but had been cleared on
appeal by USA Track and Field, the sport's U.S. governing body. Young had won a
gold medal at the 2000 Olympics for the U.S. team's gold medal-winning
performance in the 4x400-meter relay. (Young did not participate in the final
race, but was awarded one of a total of six gold medals for having competed in
an earlier round.) The U.S.'s handling of Young's case had been widely
criticized by international Olympic, athletics and antidoping officials. [See
2000 2000 Summer Olympics: Medalists; 2000 Summer Olympics Conclude in Sydney,
Australia; U.S. First in Medals]
The USOC September 25 for the first time had confirmed that Young failed the
1999 test, and that he had not been disciplined under the rules applicable at
the time. The IOC September 30 initiated disciplinary proceedings that could
result in the relay team being stripped of its gold medals.
USA Track and Field December 7 voted to impose a lifetime ban on athletes who
tested positive for steroids. However, the ban, which was stricter than
penalties imposed by the IAAF, would not take effect until the two governing
bodies resolved several legal issues.
LOAD-DATE: June 24, 2004
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 Facts on File, Inc.
626 of 998 DOCUMENTS
Guelph Mercury (Ontario, Canada)
December 31, 2003 Wednesday Final Edition
U.S. star, six others failed tests
SOURCE: Associated Press
SECTION: SPORTS; Pg. B4
LENGTH: 289 words
DATELINE: COLORADO SPRINGS, COLO.
Champion sprinter Kelli White and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced Tuesday.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih tested positive
for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she also swept the 100 and
200 metres.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, hurdler Sandra Glover, McEwen, and hurdler Eric Thomas.
Hurdler Chris Phillips tested positive for modafinil at the world championships.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
Sbeih tested positive for EPO at the U.S. Cycling Federation's Elite Track
National Championships in August.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
TYPE: NEWS
Copyright 2003 Metroland Media Group Ltd
627 of 998 DOCUMENTS
Hamilton Spectator (Ontario, Canada)
December 31, 2003 Wednesday Final Edition
Seven failed drug tests; U.S. Olympic Committee releases names of athletes
SOURCE: The Associated Press
BYLINE: Rob Gloster
SECTION: SPORTS; Pg. SP16
LENGTH: 235 words
Champion sprinter Kelli White and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced yesterday.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih tested positive
for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency. All seven athletes are appealing their test
results, the USOC said in a news release from its base in Colorado Springs,
Colo. Any suspensions or other penalties would come only after appeals.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said yesterday that White also tested positive for
modafinil at the national championships in June, when she also swept the 100 and
200 metres.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, 400-metre runner Sandra Glover, McEwen, and hurdler
Eric Thomas.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: White
TYPE: News
Copyright 2003 Metroland Media Group Ltd
628 of 998 DOCUMENTS
The Houston Chronicle
December 31, 2003, Wednesday 3 STAR EDITION
Seven test positive for banned drugs;
Appeals coming from White, others
SOURCE: Houston Chronicle News Services
SECTION: SPORTS; Pg. 3
LENGTH: 515 words
DATELINE: COLORADO SPRINGS, Colo.
COLORADO SPRINGS, Colo. - Capping a year of sports drug scandals, the U.S.
Olympic Committee announced Tuesday that sprint champion Kelli White and six
other American athletes tested positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover of Sugar Land and Eric Thomas
of Houston. Glover, 35, once ran for Stephen F. Austin and UH; Thomas, 30, was
on the track teams at Abliene Christian and Blinn.
Another hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill to help him overcome jet lag.
At least five track and field athletes - including McEwen and Chambers - have
tested positive for THG.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports - including baseball sluggers Barry Bonds and Jason Giambi
- appeared before the panel.
Donovan leads soccer picks - Landon Donovan, star of the U.S. team at the 2002
World Cup, was among 25 players selected for the national Under-23 training camp
leading to Olympic qualifying.
Coach Glenn Myernick also chose DaMarcus Beasley, another member of the American
team that went to the World Cup quarterfinals. Myernick will choose 20 players
after the U-23 squad trains in Carson, Calif., for two weeks, and that team will
play in the Olympic qualifying tournament in Guadalajara, Mexico from Feb. 2-12.
The U.S. training camp roster includes Jose Burciaga Jr. of Duncanville and
Ricky Lewis of Spring.
LOAD-DATE: January 8, 2004
LANGUAGE: ENGLISH
GRAPHIC: Mugs: 1. John McEwen; 2. Kelli White
Copyright 2003 The Houston Chronicle Publishing Company
629 of 998 DOCUMENTS
The Mirror
December 31, 2003, Wednesday
ATHLETICS: WHITE FAILS DRUGS TEST
SECTION: SPORT; Pg. 52
LENGTH: 119 words
SPRINT champion Kelli White is one of six US athletes to have tested positive
for the stimulant modafinil, the US Olympic Committee confirmed.
White was one of two athletes to provide two positive urine samples.
Her first was taken at the qualifying event for the world championships and the
second at the Paris championships themselves where White won 100 and 200m gold.
Fellow sprinter Chryste Gaines and hurdlers Sandra Glover, Chris Phillips and
Eric Thomas had modafinil in their system, while hammer thrower John McEwen
produced a positive sample for modafinil and tetrahydrogestrinone (THG).
The athletes dispute the findings and will argue their case with the US
Anti-Doping Agency.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 MGN Ltd.
630 of 998 DOCUMENTS
The New York Post
December 31, 2003, Wednesday
THE SPORTS BLOTTER
SECTION: All Editions; Pg. 069
LENGTH: 234 words
STEROID SCANDAL: Capping a year of sports drug scandals, the U.S. Olympic
Committee announced yesterday that sprint champion Kelli White and six other
American athletes tested positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
All seven are challenging their test results, the USOC said.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said that White also tested positive for modafinil at
the national championships in June.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
PLAYER SHOT: South Florida safety Johnnie Jones was shot twice during a
nightclub dispute in his hometown of Sarasota but was released from the hospital
one day later.
Jones, 21, was shot in the neck and shoulder and pistol-whipped around 1:15
Christmas morning at the Town Hall Bar. Police arrested Antonio T. Puente, 19,
and charged him with aggravated battery with a firearm.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 N.Y.P. Holdings, Inc. All rights reserved.
631 of 998 DOCUMENTS
The Record (Kitchener-Waterloo, Ontario)
December 31, 2003 Wednesday Final Edition
Seven American athletes revealed as drug cheats; Sprinter Kelli White faces loss
of two gold medals from world championships
SOURCE: Associated Press
SECTION: SPORTS; Pg. C6
LENGTH: 461 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
yesterday that sprint champion Kelli White and six other American athletes
tested positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from Colorado Springs, Colo. Any suspensions or other penalties would come only
after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said yesterday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes -- including McEwen and Chambers -- have
tested positive for THG, and a source who requested anonymity has told
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports -- including baseball sluggers Barry Bonds and Jason Giambi
-- appeared before the panel.
McEwen's lawyer, Howard Jacobs, said the hammer thrower would consider working
with the International Association of Athletics Federations, which floated an
offer of leniency for drug cheaters who provide valuable information about
doping. Jacobs said yesterday that no such offer has yet been made by the IAAF.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
TYPE: NEWS
Copyright 2003 Metroland Media Group Ltd
632 of 998 DOCUMENTS
Saint Paul Pioneer Press (Minnesota)
December 31, 2003 Wednesday CITY EDITION
WHITE AMONG SEVEN FROM U.S. TO FAIL DRUG TESTS
SECTION: SPORTS; QUICK HITS; Pg. D2
LENGTH: 973 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
BASEBALL
Rose might say he bet on baseball in book
A new autobiography of Pete Rose, "My Prison Without Bars'" is scheduled to hit
bookstores Jan. 8 amid widespread expectations that Rose will use the book to
admit publicly for the first time that he bet on baseball while managing the
Cincinnati Reds.
Rose was barred from baseball in August 1989 for illegally betting on sports
events, although not specifically on baseball. Ever since then, he has denied
that he bet on baseball, despite significant evidence to the contrary. But there
have been increasing hints over the past year that Rose, who has the most base
hits in major league history, now understood he would have to make such an
admission to win reinstatement to baseball and entry to the Hall of Fame, and
that he was prepared to do so.
-- Right-handed pitcher Jason Johnson, who pitched the five previous seasons
with Baltimore, agreed to a $7 million, two-year contract with the Detroit
Tigers. Johnson, 30, was 10-10 with a 4.18 earned-run average in 189 2/3 innings
last season. His victories matched a career high, set in 2001.
-- Free-agent right-handed pitcher Mike DeJean agreed to a one-year contract
with the Orioles. The contract is contingent on the right-hander passing a
physical exam next week. DeJean went 5-8 with 19 saves and a 4.68 ERA in 76
games with the Milwaukee Brewers and St. Louis Cardinals last season.
-- A major safety switch was missing from an escalator when it malfunctioned at
Coors Field last summer, injuring dozens of baseball fans, Denver city
inspectors said. Inspectors said the switch would have prevented the escalator
from hurtling out of control July 2.
MISCELLANEOUS
CART sale nears court approval
The Championship Auto Racing Teams racing series could win court approval of its
proposed sale to a group of team owners by Jan. 28 under a plan approved by a
bankruptcy judge in Indianapolis.
U.S. District Judge Frank Otte's approval of CART's proposed sales procedures
came two weeks after the series filed for Chapter 11 bankruptcy protection as
part of an agreement with the series' buyers, Open Wheel Racing Series LLC.
-- Former NASCAR rookie of the year Dick Brooks was in a plane crash, the
Federal Aviation Administration said. The exact nature of Brooks' injuries were
not immediately known. Brooks, 61, was taxiing a plane down the runway at his
farm in Woodruff, S.C., on Sunday when a wheel caught in the grass and turned
the plane over, a Spartanburg, S.C., newspaper reported.
-- Brian Kelly was hired as football coach at Central Michigan. Kelly, who led
Grand Valley State to the past two Division II championships, replaces Mike
DeBord. Central Michigan finished 3-9 this season, and DeBord's four-year record
at the school was 12-34.
-- Nebraska receiver Grant Mulkey was arrested and charged with marijuana
possession following the Cornhuskers' 17-3 victory over Michigan State in the
Alamo Bowl in San Antonio on Monday.
-- Landon Donovan, star of the U.S. team at the 2002 World Cup, was among 25
players selected for the national Under-23 training camp leading to Olympic
qualifying. Coach Glenn Myernick will choose 20 players after the U-23 squad
trains in Carson, Calif., for two weeks, and that team will play in the Olympic
qualifying tournament in Guadalajara, Mexico from Feb. 2-12.
WINTER SPORTS
Werner's two goals lead U.S. victory
Stephen Werner of the University of Massachusetts scored two goals, including
the winner, as the United States beat Sweden 4-3 at the world junior hockey
championships in Helsinki, Finland. The United States remained undefeated in the
under-20 tournament and plays Russia today. The winner of that game will top
Group A and get a bye into the tournament semifinals on Saturday.
-- Ronny Ackermann of Germany swept to his fifth World Cup Nordic combined
victory of the season in Oberhof, Germany. Ackermann finished 53.6 seconds ahead
of Austria's Felix Gottwald, last year's winner, with American Todd Lodwick
third, 1:06.6 behind.
LOAD-DATE: August 19, 2005
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: ASSOCIATED PRESS FILE PHOTO
Sprinter Kelli White was among seven American athletes identified Tuesday by the
U.S. Olympic Committee as having failed drug tests last summer.
Copyright 2003 Saint Paul Pioneer Press
All Rights Reserved
633 of 998 DOCUMENTS
The San Francisco Chronicle
DECEMBER 31, 2003, WEDNESDAY, FINAL EDITION
7 U.S. athletes fail drug tests;
Some tied to lab in Bay Area probed in doping scandal
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: NEWS; Pg. A1
LENGTH: 1268 words
Union City sprinter Kelli White and Stanford graduate Chryste Gaines were among
seven athletes who tested positive for banned substances last summer, according
to an announcement Tuesday by the United States Olympic Committee after tests
confirmed the presence of the drugs in backup samples.
Whether or not seven positive tests is indicative of "intentional doping of the
worst sort" as the U.S. Anti-Doping Agency claimed in October, the USOC released
the names of six track and field athletes and a cyclist who tested positive in a
new era of heightened awareness of doping in sport.
Tuesday's announcement by the USOC furthers claims by international sports
officials that U.S. athletes are as guilty of doping offenses as athletes from
other countries that are easy targets of speculation, namely China, the former
East Germany and other old Soviet-bloc nations.
It is also the latest development in an ongoing story that began last summer
with the discovery of THG, a previously unknown designer steroid said to have
come from a Burlingame laboratory and been used by athletes in track and field
and pro football to gain strength and speed. Victor Conte, owner of Bay Area
Laboratory Co-operative, is the subject of a continuing federal grand jury
investigation into his business practices.
In keeping with its policy, the USOC announced the names of the athletes 30 days
after a review by USADA confirmed their "B" samples showed the presence of
banned substances detected earlier in "A" samples.
The track athletes are White, Gaines of Lithonia, Ga., hammer thrower John
McEwen of Ashland, Ohio, and hurdlers Sandra Glover of Sugarland, Texas, Chris
Phillips of Little Rock, Ark., and Eric Thomas of Houston. The cyclist is Adham
Sbeih of Sacramento.
White, Gaines, Glover, Thomas and Phillips tested positive for the mild
stimulant modafinil, a medication normally prescribed for treatment of sleep
disorders like narcolepsy. McEwen tested positive for modafinil and the designer
steroid THG, which USADA said came from Conte's lab in Burlingame. Sbeih tested
positive for erythropoietin, or EPO, a banned substance that boosts the
oxygen-carrying capacity of red blood cells and is used by athletes in endurance
sports.
BALCO was raided by the Internal Revenue Service, the Food and Drug
Administration and the San Mateo County Narcotics Task Force on Sept. 3.
Investigators found bottles indicating they contained steroids, human growth
hormone and testosterone.
Grand jury probe
White and Gaines were two of at least 27 athletes known to have testified before
a federal grand jury in San Francisco investigating Conte and personal trainer
Greg Anderson, who serves as the weight trainer for Giants star Barry Bonds.
In an announcement in October, U.S. anti-doping officials said the discovery of
the designer steroid THG indicated "intentional doping of the worst sort" and
said the case could lead to the biggest doping scandal in U.S. sports history.
The man who made that announcement, USADA chief executive Terry Madden, was not
available for comment on Tuesday.
Earlier reports indicated four U.S. athletes had tested positive for THG,
including shot putter Kevin Toth of Hudson, Ohio, and middle distance runner
Regina Jacobs of Oakland. Toth and Jacobs are both clients of Conte and BALCO.
But McEwen was the only athlete named Tuesday as testing positive for THG.
Further announcements on THG positives are expected the last two weeks of
January.
According to USADA -- an independent agency in Colorado Springs, Colo.,
responsible for drug testing and adjudication for Olympic sports in the United
States -- all seven athletes named Tuesday plan to challenge the results of
their tests.
They have two avenues of appeal: the North American Court of Arbitration for
Sport in New York and the International Court of Arbitration for Sport. CAS is
regarded as the Supreme Court for sports disputes, the last stop in the appeals
process.
If athletes take their cases to the North American CAS and lose, they can then
appeal to the International CAS, based in Lausanne, Switzerland, whose ruling is
binding. An appeal directly to the International CAS leaves an athlete without
further recourse.
To date, 14 athletes who tested positive for illegal performance-enhancing drugs
appealed. Of those, three athletes with steroid positives took their appeals to
the International CAS and received varying rulings: Swimmer Kicker Vencill's
sanction was reduced from four years to two; bobsledder Pavle Jovanovic had his
ban increased from nine months to two years; and boxer Joseph Pastorello's
sanction was upheld at 18 months.
2 gold medals at stake
White, who stands to lose two gold medals and $120,000 in prize money if her
appeal is rejected, came up positive for the substance June 30 at the U.S.
national track and field championships at Stanford and again in August at the
World Championships in Paris.
White, 26, a James Logan High School and University of Tennessee graduate, won
world championship titles in the 100- and 200-meter sprints and ran 2003
world-best times in both races.
Modafinil is considered a mild stimulant, and an athlete testing positive is not
subject to a ban from competition, only a disqualification from the competition
where the test occurred. The steroid THG, on the other hand, could result in a
two-year suspension for a positive sample.
At the time of her positive test for modafinil in August, White said she was
taking the medication to combat narcolepsy, which she said runs in her family.
"I still believe modafinil is not a stimulant," said Remi Korchemny of Castro
Valley, who coaches White, Gaines and Phillips.
Korchemny's athletes have received services from Conte, the lab owner under
investigation. Korchemny and Conte were introduced by Oakland Raiders linebacker
Bill Romanowski, and the coach remains a supporter of the embattled lab owner.
"They did not do anything wrong," Korchemny said of his athletes. "They did not
take anything to enhance their performance. Why should they be convicted of
something that is not a crime?"
Ridicule from other coaches
Korchemny may be a lone voice crying in the wilderness. That modafinil is a
benign substance is a charge ridiculed by other coaches and anti-doping
officials in light of how many athletes have tested positive for it.
"It is a stimulant," Dick Pound, head of the World Anti-Doping Agency in
Montreal, said in an interview with The Chronicle. "You look at the excuse given
-- narcolepsy? Please. So she wouldn't fall asleep in the starting blocks of the
100 meters? Oh, please."
Like White, Phillips tested positive for modafinil at the World Championships.
Korchemny questioned why White had tested positive for modafinil after her
victory in the 100 meters at August's World Championship and not after the 200
meters several days later.
"Kelli was negative for (modafinil) for the 200. Why did she take it for the 100
and not the 200?" her coach wondered. "I don't believe it is a stimulant; it is
just a medication to relieve symptoms of some kind of problem."
Gaines, Glover, McEwen and Thomas turned in positive samples for modafinil at
the U.S. nationals at Stanford.
It was at that competition that an anonymous "high profile" track coach sent a
syringe containing an unknown substance to U.S. anti-doping officials in what
was the starting point in the current fevered campaign against doping in sport.
The syringe was later found to contain THG.
E-mail John Crumpacker at jcrumpacker@sfchronicle.com.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: (1) Kelli White is a worldchampion sprinter from Union City., (2)
Chryste Gaines is an Olympic gold medal sprinter., (3) John McEwenis a hammer
thrower fromAshland, Ohio., (4) Sandra Glover is a hurdler from Sugarland,
Texas., (5) Chris Phillips is a hurdler fromLittle Rock, Ark. (6) Eric Thomas, a
Houston athlete, also runs the hurdles.
Copyright 2003 The Chronicle Publishing Co.
634 of 998 DOCUMENTS
San Jose Mercury News (California)
December 31, 2003 Wednesday MORNING FINAL EDITION
USOC TO PROCEED WITH CASE AGAINST ATHLETES;
WHITE, GAINES AMONG SEVEN PEOPLE TARGETED
JACOBS ARGUES SHE TOOK NO BANNED SUBSTANCE
BYLINE: ELLIOTT ALMOND AND PETE CAREY, Mercury News
SECTION: SPORTS; Pg. 1D
LENGTH: 904 words
U.S. Olympic officials announced Tuesday that there was sufficient evidence to
proceed against seven athletes, including East Bay sprinters Kelli White and
Chryste Gaines, for using performance-enhancing drugs.
In response, athletes and their representatives criticized the country's Olympic
drug-testing system, suggesting for the first time how they will defend
themselves. All but one of these cases involves the mild stimulant modafinil, a
sleeping disorder medication.
The announcement signaled the next phase of a drug scandal that first surfaced
in September with the federal investigation of a Burlingame nutrition company,
Balco Laboratories, and that has brought dozens of athletes from baseball,
football and Olympic sports before a grand jury in San Francisco.
In November, the International Association of Athletics Federations announced
that four athletes tested positive for a new designer steroid, THG, at the USA
Outdoor Track and Field Championships at Stanford in June.
One of those four, three-time Olympian Regina Jacobs of Oakland, spoke up for
the first time Tuesday in a statement saying she had filed for arbitration
although a review panel had not decided on her case yet.
Suggesting the defense that athletes accused of taking THG may take, shesaid USA
Track & Field and the U.S. Anti-Doping Agency "seek to deny me the opportunity
to compete in the upcoming Olympics on the grounds that something I have never
heard of, and which was not on any list of banned substances," should be
considered "somehow 'related' to something" on track's list of banned
substances.
Jacobs, a former Stanford star, said the Anti-Doping Agency had refused to
provide documents showing what THG is and had denied an expert she had retained
a "meaningful opportunity" to observe the urine test that was positive for the
substance.
Howard Jacobs, a lawyer for the three others who tested positive for THG, or
tetrahydrogestrinone -- John McEwen, Kevin Toth and a yet unnamed athlete --
also questioned the validity of the test developed this summer by Don Catlin,
head of the UCLA Olympic drug laboratory, to detect THG.
"They still have to prove, ultimately, that it is an anabolic steroid," Jacobs
said, adding that USADA officials have not shown the test has had a scientific
peer review.
He said, "They have to prove it was legally just to retest all these samples"
from the national meet, which took place before Catlin had identified THG, and
from the world championships, which took place before the existence of THG was
announced. "It is one thing to say it is obviously a steroid but it is another
thing to prove it legally."
USADA officials declined to comment because of the pending cases.
In addition to White and Gaines, the others named Tuesday were 400-meter runner
Sandra Glover of Texas, hammer thrower McEwen of Ohio, hurdlers Chris Phillips
of Arkansas and Eric Thomas of Texas, and cyclist Adham Sbieh of Citrus Grove.
Olympic officials said the track athletes had tested positive for modafinil, a
sleep-disorder drug, and the cyclist for the blood-boosting EPO.
Neither THG nor modafinil is on the list of banned substances maintained by the
IAAF, track's governing body. The cases are proceeding because the mild
stimulant falls under the "related substances" clause in the drug code.
The owner of Balco Laboratories, Victor Conte Jr., has been identified by
anti-doping officials as the source of THG.
Jacobs said he did not know why officials failed to announce the THG case of
Toth, a leading shot putter, Tuesday.
Even before federal officials searched Balco in September, White tested positive
for modafinil in August at the World Championships in Paris, where she had
become the first American woman to win both the 100 meters and 200 meters.
White, a James Logan High graduate, has repeatedly denied using the drug to aid
performance. A doctor connected to Balco said he gave her the medication because
White suffers from narcolepsy. White's mother, a one-time Olympic runner from
Jamaica, also suffers from the illness, she said.
Those who tested positive for modafinil have the same concern with the drug
testers as those who tested positive for THG. They are questioning how they can
be punished for a drug that was not on any banned list, and also lacks proof
that it aids performance, something sleeping experts question.
The questions surfacing could help frame the debate for the future of drug
testing as sports officials worldwide try to develop a standard practice to
include all sports.
Thomas, from Houston, said Tuesday that he did not take modafinil to circumvent
the system.
"Not at all," he said. "I took it to be alert. It is just a pill that helps you
be focused and alert."
Cameron Myler, a New York lawyer who represents Thomas, Gaines and Glover, said
her athletes, all of whom tested positive for modafinil, also are seeking
arbitration.
"As you probably know, USADA uses the rules of the international federation,"
said Myler, a four-time Olympian. "Modafinil has never been on a banned list of
the IAAF. The only way USADA could prevail on this is if they could show that
modafinil is 'chemically or pharmacologically related to' something on the
banned list."
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban.
LOAD-DATE: August 19, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photos (2);
PHOTO: Gaines
PHOTO: White
Copyright 2003 San Jose Mercury News
All Rights Reserved
635 of 998 DOCUMENTS
THE SEATTLE POST-INTELLIGENCER
December 31, 2003, Wednesday FINAL
ROSE MAY ADMIT HE BET ON BASEBALL
SECTION: SPORTS, Pg. D12
LENGTH: 901 words
BASEBALL
A new autobiography of Pete Rose is scheduled to hit bookstores next week amid
widespread expectations Rose will use the book to admit publicly for the first
time that he bet on baseball while managing the Cincinnati Reds, the New York
Times reported.
The book, "My Prison Without Bars," has a huge first printing, 500,000 copies,
and is being handled in top-secret fashion by the publisher, Rodale Press, which
has embargoed the book until Jan. 8, when Rose will conduct a series of
interviews with reporters about the book's contents.
Rose was barred from baseball in August 1989 for illegally betting on sports
events, although not specifically on baseball. Ever since then, he has denied
that he bet on baseball, despite significant evidence to the contrary. But there
have been increasing hints over the past year that Rose, who has the most base
hits in major league history, understood he would have to make such an admission
to win reinstatement to baseball and entry to the Hall of Fame, and that he was
prepared to do so.
In fact, a major league official said yesterday, Rose made such an admission
when he met with Commissioner Bud Selig in Milwaukee on Nov. 25, 2002.
The official, who said he was aware of what was discussed at the meeting, said
Rose was asked by Selig if he had bet on baseball and that he replied that he
did.
The official said Selig responded to Rose's admission by noting that every
clubhouse in baseball had a sign stating that gambling on baseball was
prohibited and proceeded to ask Rose why he had so blatantly ignored the
warnings.
Three days after he was gunned down at a bar, former Mariner Ivan Calderon was
buried yesterday as dozens of relatives and friends recalled his intense love of
baseball. Police said two men shot Calderon multiple times in the head and back
Saturday evening in the Puerto Rican town of Loiza, where the 41-year-old lived.
Detectives have ruled out robbery and are investigating revenge as a possible
motive.
Calderon sometimes loaned money to people and in retirement worked as a
bondsman, police said. The former slugger played with the Mariners, White Sox,
Expos and Red Sox during his 10-year Major League Baseball career, which ended
in 1993. New York Yankees center fielder Bernie Williams visited Calderon's
family at their home yesterday, and Yankees outfielder Ruben Sierra attended a
wake Monday.
Right-hander Jason Johnson signed a two-year, $7 million free-agent contract
with the Detroit Tigers.
Right-hander Mike DeJean agreed to a one-year contract with the Baltimore
Orioles.
Chris Speier was hired by the Oakland Athletics as bench coach to replace Terry
Francona, who left to become the manager of the Boston Red Sox.
TRACK AND FIELD
White, others test positive
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
sprint champion Kelli White and six other American athletes tested positive for
banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
ETC.
Donovan joins U.S. Olympic team
Landon Donovan, star of the U.S. team at the 2002 World Cup, was among 25
players selected for the national Under-23 training camp leading to Olympic
qualifying.
Coach Glenn Myernick also chose DaMarcus Beasley, another member of the American
team that went to the World Cup quarterfinals. Myernick will choose 20 players
after the U-23 squad trains in Carson, Calif., for two weeks. That team will
play in the Olympic qualifying tournament in Guadalajara, Mexico, from Feb.
2-12.
The roster includes another veteran of the 2000 Under-23 squad, forward Conor
Casey, who will be making his first appearance with the team since the Olympics.
The CART racing series could win court approval of its proposed sale to a group
of team owners by Jan. 28 under a plan a bankruptcy judge approved. U.S.
District Judge Frank J. Otte's approval of CART's proposed sales procedures came
two weeks after the series filed for Chapter 11 bankruptcy protection as part of
an agreement with the series' buyers, Open Wheel Racing Series LLC.
Stephen Werner of the University of Massachusetts scored two goals, including
the winner, as the United States beat Sweden 4-3 at the world junior hockey
championships in Helsinki, Finland. The United States remained undefeated in the
under-20 tournament and plays Russia today. The winner of that game will top
Group A and get a bye into the tournament semifinals Saturday.
LOAD-DATE: January 1, 2004
LANGUAGE: ENGLISH
NOTES: WORLD
Copyright 2003 Seattle Post-Intelligencer
636 of 998 DOCUMENTS
St. Petersburg Times (Florida)
December 31, 2003 Wednesday 0 South Pinellas Edition
USOC lists 7 who tested positive for banned substances
SOURCE: Compiled from Wire Reports
SECTION: SPORTS; Pg. 9C
LENGTH: 560 words
Capping a year of drug scandals, the U.S. Olympic Committee announced Tuesday
that sprint champion Kelli White and six other Americans tested positive for
banned substances.
White and five other track and field athletes tested positive for the stimulant
modafinil. Hammer thrower John McEwen also tested positive for the newly
discovered steroid THG, and cyclist Adham Sbeih became the first U.S. athlete to
test positive for the endurance-boosting hormone EPO.
The USOC announced the results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging the results, the USOC said. Any suspensions or other
penalties would come only after arbitration.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said she also tested positive for the drug at the
national championships in June, when she swept the 100 and 200 meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national championships were sprinter
Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another hurdler,
Chris Phillips, tested positive for modafinil at the world championships.
MOTORSPORTS
CART sale moves ahead
The CART racing series could win court approval of its proposed sale to a group
of team owners by Jan. 28 under a bankruptcy plan approved by U.S. District
Judge Frank J. Otte in Indianapolis. Otte overruled objections to the sales
procedures and scheduled Jan. 23 as the deadline for alternative bids for CART's
assets. If any such bids emerge, they could be considered during an auction Jan.
28. Without any qualifying bids, Otte could approve the sale to Open Wheel
Racing Series LLC that day.
OBITUARY: Rina Andretti, mother of retired auto racing great Mario Andretti,
died in Bethlehem, Pa., at age 90.
BASEBALL
Missing switch mystery
A major safety switch was missing from an escalator when it malfunctioned at
Coors Field on July 2, hurtling out of control and injuring dozens of fans,
Denver city inspectors said. The device was there when the escalator was
originally certified, and contractors said they inspected it in March.
CALDERON BURIAL: Former major-leaguer Ivan Calderon was buried in Loiza, Puerto
Rico, three days after he was shot multiple times in the back at a Loiza bar.
TIGERS: Right-hander Jason Johnson, who pitched the past five seasons for
Baltimore, agreed to a $7-million, two-year contract.
ET CETERA
SOCCER: Florida State sophomore Leah Gallegos has been named a College Sports
Television second-team All-American. FSU freshmen Julia Schnugg and India
Trotter are training with the U.S. Under-19 National Team in Carson, Calif.
HOCKEY: Stephen Werner scored two goals, including the winner, as the United
States beat Sweden 4-3 at the world junior championships in Helsinki. The
Americans play Russia today for a bye into the semifinals.
BIATHLON: Jacob Beste of St. Cloud, Minn., won the men's 12.5-kilometer pursuit
and Rachel Steer of Anchorage won the women's 10K pursuit at the national
championships in Lake Placid, N.Y.
- Compiled from Times wires.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
SERIES: IN BRIEF
TYPE: DIGEST
Copyright 2003 Times Publishing Company
637 of 998 DOCUMENTS
Times Colonist (Victoria, British Columbia)
December 31, 2003 Wednesday Final Edition
Sprint star White on U.S. drug-cheat list
SOURCE: The Associated Press
SECTION: Sports; Pg. C12
LENGTH: 388 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
metres.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes -- including McEwen and Chambers -- have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
638 of 998 DOCUMENTS
Topeka Capital-Journal (Kansas)
December 31, 2003, Wednesday
Briefly in sports
BYLINE: Capital-Journal
Pg. D4
LENGTH: 1078 words
General: Seven U.S. athletes
test positive for banned steroids
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder --- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant. Also testing positive for modafinil at the national
track championships were sprinter Chryste Gaines and hurdlers Sandra Glover and
Eric Thomas. Another hurdler, Chris Phillips, tested positive for modafinil at
the world championships.
THE KANSAS TICKET OFFICE has a limited number of tickets available for the
Villanova game on Friday, KU officials announced Tuesday. Game time is 7 p.m. in
Allen Fieldhouse.
The tickets, which were returned by Villanova, cost $30 each. They can be
purchased in person at the Fieldhouse ticket office, by calling 1-800-34-HAWKS,
or (785) 864-3141, or online at www.kustore.com.
HAYDEN will play a varsity basketball doubleheader starting at 1 p.m. Friday at
Wamego. The starting times have been changed so they won't conflict with that
night's Fiesta Bowl. Varsity girls will start at 1 p.m., followed by the varsity
boys about 2:30 p.m.
WICHITA STATE has announced its 2004 Pizza Hut Shocker Sports Hall of Fame
inductees. They are two-time all-Missouri Valley Conference basketball player
Greg Carney, two-time NCAA tennis qualifier and All-American Phil Cooper,
two-time All-America second baseman Jim Thomas and All-America pitcher Shane
Dennis.
The induction will be at halftime of the WSU-Indiana State game at 7:05 p.m. on
Jan. 17. A reception and dinner is set for 6:30 p.m. on Jan. 16 at the Charles
Koch Arena Champions Club.
KANSAS BASEBALL COACH Ritch Price will be a featured speaker at the 2004
American Baseball Coaches Association national clinic from Friday through Monday
in San Antonio, Texas. The second-year Kansas coach will talk on "Zone Double
Play Feeds and Pivots" on Sunday, speaking to an estimated 4,000 coaches from
around the country.
MLB: Malfunction discovered
in Coors Field escalator incident
A major safety switch was missing from an escalator when it malfunctioned at
Coors Field this summer, injuring dozens of baseball fans, city inspectors said
Tuesday.
City inspectors said the switch would have prevented the escalator from hurtling
out of control July 2.
The device was there when the escalator was originally certified, and
contractors said they inspected it in March, according to Julius Zsako,
spokesman for the city Community Planning and Development Office.
''We don't know when it was removed,'' Zsako said.
Escalators at Coors Field are maintained by Kone Inc., which disuputed the
inspectors' finding. The company previously issued a report that blamed the
accident on overcrowding and a misconnected wire, and said Tuesday that tests
left ''no doubt'' that the misconnected wire was to blame.
JASON JOHNSON likes the changes going on in Detroit, so he decided to join the
Tigers. The right-hander who pitched the five previous seasons with Baltimore
agreed to a $7 million, two-year contract with the Tigers on Tuesday.
Football: Tice will return
next season as Vikings coach
Minnesota Vikings owner Red McCombs' silence led many people, including Mike
Tice himself, to believe he was about to fire the head coach. But after waiting
two days, McCombs said Tice would return next season and wondered what all the
fuss was about.
A relieved Tice began his offseason planning in earnest while continuing to
commiserate with his assistants over what could've been. McCombs, on a
conference call Tuesday, insisted he never had thoughts of replacing Tice --- or
anyone else on staff.
A 3-7 finish by the Vikings, including an unfathomable fourth-quarter failure in
an 18-17 defeat at Arizona on Sunday that kept them out of the playoffs,
prompted speculation Tice could be fired. Not so, said McCombs from his San
Antonio office, a day after staying suspiciously mum on the subject.
''I don't know where all the smoke is coming from,'' said the owner, who more
than once this season voiced his confidence in Tice's performance. ''It's not
coming from me.''
TENNESSEE coach Phillip Fulmer was given a one-year contract extension and a
$140,000 raise Tuesday, three days before the Volunteers play Clemson in the
Peach Bowl. The agreement keeps Fulmer at Tennessee through the 2010 season and
raises his salary to $1,789,500, up from $1.65 million this year. Fulmer ranks
second in wins among active Division I-A coaches with at least five years
experience. He has a 113-27 record for an .807 winning percentage.
NEW YORK JETS coach Herman Edwards shook up his staff Tuesday by firing
defensive coordinator Ted Cottrell and three assistants. Edwards said the Jets
needed to go a different direction after finishing 28th against the run and 21st
in yards allowed this season, when the team finished 6-10.
TENNESSEE TITANS quarterback Steve McNair tossed a few balls and took some snaps
in a 90-minute walk through Tuesday, and coach Jeff Fisher said McNair will
practice Wednesday.
That would be McNair's first practice in three weeks. A strained right calf and
sprained left ankle that also has a cracked bone spur had kept him off the field
and out of two of the past three games. Both injuries are significantly
improved, according to Fisher.
From staff and wire reports
LOAD-DATE: January 6, 2004
LANGUAGE: ENGLISH
Copyright 2003 The Topeka Capital-Journal
639 of 998 DOCUMENTS
The Vancouver Sun (British Columbia)
December 31, 2003 Wednesday Final Edition
Kelli White, six others test positive for drugs
SOURCE: Associated Press; Canadian Press
SECTION: Sports; In Brief; Pg. E5
LENGTH: 136 words
DATELINE: COLORADO SPRINGS
COLORADO SPRINGS -- Capping a year of sports drug scandals, the U.S. Olympic
Committee announced Tuesday that sprint champion Kelli White and six other
American athletes tested positive for banned substances. White and five other
track and field athletes tested positive for the banned stimulant modafinil.
Hammer thrower John McEwen tested positive for modafinil and the newly
discovered steroid THG, and cyclist Adham Sbeih became the first U.S. athlete to
test positive for the endurance-boosting hormone EPO. Also testing positive for
modafinil at the national track championships were sprinter Chryste Gaines and
hurdlers Sandra Glover and Eric Thomas. Another hurdler, Chris Phillips, tested
positive for modafinil at the world championships. All seven are challenging
their test results, the USOC said.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
TYPE: Brief; Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
640 of 998 DOCUMENTS
The Vancouver Province (British Columbia)
December 31, 2003 Wednesday FINAL C Edition
White among 7 to test positive
SOURCE: The Associated Press
SECTION: Sports; Pg. A37
LENGTH: 115 words
The U.S. Olympic Committee announced Tuesday that sprint champion Kelli White
and six other American athletes tested positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
All seven are challenging their test results. White said she was prescribed
modafinil for a sleeping disorder -- a claim ridiculed by international track
officials after word emerged of other athletes using the banned stimulant.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: The Associated Press; Kelli White plans to appeal her
positive test result.
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
641 of 998 DOCUMENTS
The Vancouver Province (British Columbia)
December 31, 2003 Wednesday Final Edition
Top sprinter among seven U.S. athletes to fail drug test: Kelli White had taken
banned stimulant modafinil
SOURCE: News Services
SECTION: Sports; Pg. A37
LENGTH: 291 words
The U.S. Olympic Committee announced Tuesday that sprint champion Kelli White
and six other American athletes tested positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
All seven are challenging their test results. White said she was prescribed
modafinil for a sleeping disorder -- a claim ridiculed by international track
officials after word emerged of other athletes using the banned stimulant.
Coulthard Nears Finish
Long-serving McLaren Formula One driver David Coulthard looks set to be dropped
from the team at the end of the upcoming season according to the BBC on Tuesday.
The 32-year-old has had a disappointing two seasons being outshone by teammate
Kimi Raikkonen last campaign when the Finn was second behind Michael Schumacher
while the Scot was only seventh.
EPHEDRA BAN WELCOMED
Steve Bechler's parents welcomed the U.S. federal government's ban on ephedra,
saying it should save lives and ensure their son did not die in vain.
The Baltimore Orioles pitcher's heatstroke in February was linked to the herbal
weight-loss supplement, which also has been blamed for more than 150 other
deaths.
"In one aspect, I feel that it's not enough, because it won't bring Steve back,"
Bechler's mother, Pat, said. "But it will help and protect other people."
DEJEAN AN ORIOLE
Free-agent pitcher Mike DeJean agreed Monday to a one-year contract with the
Baltimore Orioles, contingent on the right-hander passing a physical exam next
week.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: The Associated Press; Kelli White plans to appeal her
positive test result.
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
642 of 998 DOCUMENTS
The Washington Post
December 31, 2003 Wednesday
Final Edition
USOC Formally Announces Flunked Tests
SECTION: Sports; D02
LENGTH: 432 words
Sprint champion Kelli White and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced yesterday.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih tested positive
for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests. All
seven athletes are appealing their test results. Any suspensions or other
penalties would come only after appeals.
White said she was prescribed modafinil for a sleeping disorder -- a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, hurdler Sandra Glover, McEwen, and hurdler Eric Thomas.
Hurdler Chris Phillips tested positive for modafinil at the world championships.
* SOCCER: Landon Donovan, star of the U.S. team at the 2002 World Cup, was
among 25 players selected for the under-23 national training camp leading to
Olympic qualifying.
Coach Glenn Myernick also chose DaMarcus Beasley, another member of the American
team that went to the World Cup quarterfinals, as well as five D.C. United
players -- Doug Warren, Bobby Convey, Alecko Eskandarian, David Stokes and Brian
Carroll.
* WINTER SPORTS: Ronny Ackermann of Germany swept to his fifth World Cup Nordic
combined victory .
Ackermann finished 53.6 seconds ahead of Austria's Felix Gottwald, with American
Todd Lodwick third, 1:06.6 behind, in Oberhof, Germany. . . .
Jacob Beste and Rachel Steer won pursuit events at the U.S. biathlon
championships in Lake Placid, N.Y.
* HOCKEY: Stephen Werner of the University of Massachusetts scored two goals,
including the game-winner, as the United States defeated Sweden, 4-3, at the
world junior hockey championship in Helsinki. The United States remained
undefeated in the under-20 tournament.
* AUTO RACING: The CART racing series could win court approval of its proposed
sale to a group of team owners by Jan. 28 under a plan an Indianapolis
bankruptcy judge approved.
U.S. District Judge Frank J. Otte's approval of CART's proposed sales procedures
came two weeks after the series filed for Chapter 11 bankruptcy protection as
part of an agreement with the series' buyers, Open Wheel Racing Series LLC.
-- From News Services
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
643 of 998 DOCUMENTS
The Associated Press
December 30, 2003, Tuesday, BC cycle
USOC releases names of athletes with positive drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 382 words
Sprint champion Kelli White was among seven American athletes - six in track and
field and one in cycling - identified Tuesday by the U.S. Olympic Committee as
having flunked drug tests this summer.
White and five others tested positive for the banned stimulant modafinil. Hammer
thrower John McEwen tested positive for modafinil and the newly discovered
steroid THG, and cyclist Adham Sbeih tested positive for the endurance-boosting
hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release from its base in Colorado Springs, Colo., and any suspensions or other
sanctions would come only after those appeals are exhausted.
White, of Union City, Calif., already faces the loss of her two gold medals at
the World Championships because of modafinil use. The USOC said Tuesday that
White also tested positive for modafinil at the U.S. track and field
championships at Stanford, Calif., in June - where she also swept the 100 and
200 meter titles.
By winning at the national meet in June, White qualified for the world meet in
August in France. She has claimed she was prescribed modafinil for the sleep
disorder narcopelsy - a claim that has been ridiculed by international track
officials since word emerged of other athletes using the banned stimulant.
Also testing positive for modafinil at the U.S. track and field championships
were sprinter Chryste Gaines, of Lithonia, Ga.; 400-meter runner Sandra Glover
of Sugarland, Texas; McEwen, of Ashland, Ohio, and hurdler Eric Thomas of
Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the World Championships.
Sbeih of Sacramento, Calif., tested positive for EPO at the U.S. Cycling
Federation's Elite Track National Champonships at Trexlertown, Pa., in August.
Modafinil use results in disqualification at the event at which a positive test
has occurred. THG use could lead to a two-year ban for McEwen.
At least three other U.S. track and field athletes tested positive for THG this
summer, and their cases are still being considered by USADA.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
644 of 998 DOCUMENTS
The Associated Press
December 30, 2003, Tuesday, BC cycle
World-champion sprinter among seven athletes to fail drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Domestic News
LENGTH: 215 words
A world-champion sprinter and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced Tuesday.
The Olympic Committee announced the results after banned substances were found
in two urine tests from each of the athletes, and following a 30-day review of
the tests by the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said. Any
suspensions or other penalties would come only after appeals.
The athletes include sprint champion Kelli White, who tested positive for the
banned stimulant modafinil along with five other track and field athletes. A
hammer thrower tested positive for modafinil and the newly discovered steroid
THG, and a cyclist tested positive for the endurance-boosting hormone EPO.
White twice tested positive for modafinil during the summer. Officials
previously disclosed that she tested positive at the world championships in
August.
On Tuesday, the USOC said White also tested positive for modafinil at the
national championships in June. White won the 100 and 200 meters at both events.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
645 of 998 DOCUMENTS
The Associated Press
December 30, 2003, Tuesday, BC cycle
White among seven athletes to fail drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 407 words
Sprint champion Kelli White and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced Tuesday.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih tested positive
for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release from its base in Colorado Springs, Colo. Any suspensions or other
penalties would come only after appeals.
White, of Union City, Calif., already faces the loss of two world championship
gold medals because of modafinil use. The USOC said Tuesday that White also
tested positive for modafinil at the national championships in June, when she
also swept the 100 and 200 meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, hurdler Sandra Glover, McEwen, and hurdler Eric Thomas
of Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the world championships.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
Sbeih of Sacramento, Calif., tested positive for EPO at the U.S. Cycling
Federation's Elite Track National Championships in August. Sbeih faces up to a
two-year ban.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban.
McEwen's attorney, Howard Jacobs, said McEwen would consider working with the
International Association of Athletics Federations, which floated an offer of
leniency for drug cheaters who provide valuable information about doping.
No such offer has yet been made by the IAAF, Jacobs said in an interview with
The Associated Press.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
646 of 998 DOCUMENTS
The Associated Press
December 30, 2003, Tuesday, BC cycle
White among seven U.S. athletes to fail drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 462 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes - including McEwen and Chambers - have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports - including baseball sluggers Barry Bonds and Jason Giambi
- appeared before the panel.
McEwen's attorney, Howard Jacobs, said the hammer thrower would consider working
with the International Association of Athletics Federations, which floated an
offer of leniency for drug cheaters who provide valuable information about
doping. Jacobs said Tuesday that no such offer has yet been made by the IAAF.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
647 of 998 DOCUMENTS
Associated Press Worldstream
December 30, 2003 Tuesday
White among seven United States athletes to fail drug tests
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 453 words
DATELINE: SAN FRANCISCO
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
that sprint champion Kelli White and six other American athletes tested positive
for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said Tuesday in a news
release from its base in Colorado Springs, Colorado. Any suspensions or other
penalties would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes - including McEwen and Chambers - have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports - including baseball sluggers Barry Bonds and Jason Giambi
- appeared before the panel.
McEwen's attorney, Howard Jacobs, said the hammer thrower would consider working
with the IAAF, which floated an offer of leniency for drug cheaters who provide
valuable information about doping. Jacobs said Tuesday that no such offer has
yet been made by the IAAF.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
648 of 998 DOCUMENTS
Associated Press Online
December 30, 2003 Tuesday
Names of Drug-Positive Athletes Released
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 460 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes - including McEwen and Chambers - have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports - including baseball sluggers Barry Bonds and Jason Giambi
- appeared before the panel.
McEwen's attorney, Howard Jacobs, said the hammer thrower would consider working
with the International Association of Athletics Federations, which floated an
offer of leniency for drug cheaters who provide valuable information about
doping. Jacobs said Tuesday that no such offer has yet been made by the IAAF.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
649 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 30, 2003, Tuesday, BC cycle
USOC releases names of athletes with positive drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 382 words
Sprint champion Kelli White was among seven American athletes - six in track and
field and one in cycling - identified Tuesday by the U.S. Olympic Committee as
having flunked drug tests this summer.
White and five others tested positive for the banned stimulant modafinil. Hammer
thrower John McEwen tested positive for modafinil and the newly discovered
steroid THG, and cyclist Adham Sbeih tested positive for the endurance-boosting
hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release from its base in Colorado Springs, Colo., and any suspensions or other
sanctions would come only after those appeals are exhausted.
White, of Union City, Calif., already faces the loss of her two gold medals at
the World Championships because of modafinil use. The USOC said Tuesday that
White also tested positive for modafinil at the U.S. track and field
championships at Stanford, Calif., in June - where she also swept the 100 and
200 meter titles.
By winning at the national meet in June, White qualified for the world meet in
August in France. She has claimed she was prescribed modafinil for the sleep
disorder narcopelsy - a claim that has been ridiculed by international track
officials since word emerged of other athletes using the banned stimulant.
Also testing positive for modafinil at the U.S. track and field championships
were sprinter Chryste Gaines, of Lithonia, Ga.; 400-meter runner Sandra Glover
of Sugarland, Texas; McEwen, of Ashland, Ohio, and hurdler Eric Thomas of
Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the World Championships.
Sbeih of Sacramento, Calif., tested positive for EPO at the U.S. Cycling
Federation's Elite Track National Champonships at Trexlertown, Pa., in August.
Modafinil use results in disqualification at the event at which a positive test
has occurred. THG use could lead to a two-year ban for McEwen.
At least three other U.S. track and field athletes tested positive for THG this
summer, and their cases are still being considered by USADA.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
650 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 30, 2003, Tuesday, BC cycle
Two Texans among athletes USOC says had positive drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 382 words
Sprint champion Kelli White was among seven American athletes - six in track and
field and one in cycling - identified Tuesday by the U.S. Olympic Committee as
having flunked drug tests this summer.
White and five others tested positive for the banned stimulant modafinil. Hammer
thrower John McEwen tested positive for modafinil and the newly discovered
steroid THG, and cyclist Adham Sbeih tested positive for the endurance-boosting
hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release from its base in Colorado Springs, Colo., and any suspensions or other
sanctions would come only after those appeals are exhausted.
White, of Union City, Calif., already faces the loss of her two gold medals at
the World Championships because of modafinil use. The USOC said Tuesday that
White also tested positive for modafinil at the U.S. track and field
championships at Stanford, Calif., in June - where she also swept the 100 and
200 meter titles.
By winning at the national meet in June, White qualified for the world meet in
August in France. She has claimed she was prescribed modafinil for the sleep
disorder narcopelsy - a claim that has been ridiculed by international track
officials since word emerged of other athletes using the banned stimulant.
Also testing positive for modafinil at the U.S. track and field championships
were sprinter Chryste Gaines, of Lithonia, Ga.; 400-meter runner Sandra Glover
of Sugarland, Texas; McEwen, of Ashland, Ohio, and hurdler Eric Thomas of
Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the World Championships.
Sbeih of Sacramento, Calif., tested positive for EPO at the U.S. Cycling
Federation's Elite Track National Championships at Trexlertown, Pa., in August.
Modafinil use results in disqualification at the event at which a positive test
has occurred. THG use could lead to a two-year ban for McEwen.
At least three other U.S. track and field athletes tested positive for THG this
summer, and their cases are still being considered by USADA.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
651 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 30, 2003, Tuesday, BC cycle
White among seven athletes to fail drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 407 words
Sprint champion Kelli White and six other American athletes flunked drug tests
this summer, the U.S. Olympic Committee announced Tuesday.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih tested positive
for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each of the athletes, and following a 30-day review of the tests by
the U.S. Anti-Doping Agency.
All seven athletes are appealing their test results, the USOC said in a news
release from its base in Colorado Springs, Colo. Any suspensions or other
penalties would come only after appeals.
White, of Union City, Calif., already faces the loss of two world championship
gold medals because of modafinil use. The USOC said Tuesday that White also
tested positive for modafinil at the national championships in June, when she
also swept the 100 and 200 meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines, hurdler Sandra Glover, McEwen, and hurdler Eric Thomas
of Houston.
Hurdler Chris Phillips of Little Rock, Ark., tested positive for modafinil at
the world championships.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
Sbeih of Sacramento, Calif., tested positive for EPO at the U.S. Cycling
Federation's Elite Track National Championships in August. Sbeih faces up to a
two-year ban.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban.
McEwen's attorney, Howard Jacobs, said McEwen would consider working with the
International Association of Athletics Federations, which floated an offer of
leniency for drug cheaters who provide valuable information about doping.
No such offer has yet been made by the IAAF, Jacobs said in an interview with
The Associated Press.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
652 of 998 DOCUMENTS
The Associated Press State & Local Wire
December 30, 2003, Tuesday, BC cycle
White among seven U.S. athletes to fail drug tests
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 462 words
Capping a year of sports drug scandals, the U.S. Olympic Committee announced
Tuesday that sprint champion Kelli White and six other American athletes tested
positive for banned substances.
White and five other track and field athletes tested positive for the banned
stimulant modafinil. Hammer thrower John McEwen tested positive for modafinil
and the newly discovered steroid THG, and cyclist Adham Sbeih became the first
U.S. athlete to test positive for the endurance-boosting hormone EPO.
The USOC announced the test results after the substances were found in two urine
tests from each athlete, and following a review by the U.S. Anti-Doping Agency.
All seven are challenging their test results, the USOC said in a news release
from its base in Colorado Springs, Colo. Any suspensions or other penalties
would come only after an arbitration process.
White already faces the loss of two world championship gold medals because of
modafinil use. The USOC said Tuesday that White also tested positive for
modafinil at the national championships in June, when she swept the 100 and 200
meters.
White said she was prescribed modafinil for a sleeping disorder - a claim
ridiculed by international track officials after word emerged of other athletes
using the banned stimulant.
Also testing positive for modafinil at the national track championships were
sprinter Chryste Gaines and hurdlers Sandra Glover and Eric Thomas. Another
hurdler, Chris Phillips, tested positive for modafinil at the world
championships.
Modafinil use results in disqualification at the event at which a positive test
has occurred, but no suspension. THG use can lead to a two-year ban. Sbeih, who
tested positive for EPO at the national cycling championships in August, faces
up to a two-year ban.
White and Gaines are coached by Remy Korchemny, who also coaches British
sprinter Dwain Chambers, now facing a two-year suspension for THG. Phillips said
Korchemny gave him a modafinil pill at the world championships to help him
overcome jet lag.
At least five track and field athletes - including McEwen and Chambers - have
tested positive for THG, and a source who requested anonymity has told The
Associated Press that four Oakland Raiders also flunked THG tests.
The discovery of THG led to a grand jury probe in San Francisco. Athletes from
at least five sports - including baseball sluggers Barry Bonds and Jason Giambi
- appeared before the panel.
McEwen's attorney, Howard Jacobs, said the hammer thrower would consider working
with the International Association of Athletics Federations, which floated an
offer of leniency for drug cheaters who provide valuable information about
doping. Jacobs said Tuesday that no such offer has yet been made by the IAAF.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
653 of 998 DOCUMENTS
Voice of America News
December 30, 2003
USOC Announces Sprint Champ Kelli White Failed Doping Test
SECTION: SPORTS
LENGTH: 213 words
Filed: 20:41 UTC
The USOC announced Tuesday that White, sprinter Chryste Gaines, hurdlers Sandra
Glover, Chris Phillips and Eric Thomas, and hammer-thrower John McEwen tested
positive for the banned stimulant modafinil at either the U.S. or World
Athletics Championships.
John McEwen also tested positive for the newly discovered steroid THG, while
cyclist Adham Sbeih tested positive for the endurance-boosting hormone EPO.
The USOC announced the results after the substances were found in two urine
tests from each of the athletes following a 30-day review of the tests by the
U.S. Anti-Doping Agency. All seven athletes will appeal their test results, and
any suspensions or other sanctions would come only after those appeals are
exhausted.
White already faces the loss of her two gold medals at the World Championships
because of modafinil use. The USOC said Tuesday that White also tested positive
for modafinil at the U.S. track and field championships in June, where she swept
the 100- and 200-meter titles.
White has claimed she was prescribed modafinil for the sleep disorder
narcolepsy. At least three other U.S. track and field athletes tested positive
for THG this summer, and their cases are still being considered by the U.S.
Anti-Doping Agency.
LOAD-DATE: December 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Federal Information and News Dispatch, Inc.
654 of 998 DOCUMENTS
Edmonton Journal (Alberta)
December 29, 2003 Monday Final Edition
Stay-awake drugs high in demand: Despite society's chronic lack of sleep
SOURCE: Ottawa Citizen; CanWest News Service
BYLINE: Sharon Kirkey
SECTION: Body & Health; Pg. B13
LENGTH: 808 words
DATELINE: OTTAWA
OTTAWA - Psychologist Stanley Coren finds a particular lunacy to our
determination to squeeze more minutes out of every day, when science shows not
getting enough sleep is putting people at risk.
Humans have been hardwired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia. "Generally, we're about two hours sleep-deprived
every night."
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night, or less.
But what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks at inappropriate times.
But now, the U.S. Food and Drug Administration has given preliminary blessing to
expanded uses of the drug to treat excessive daytime sleepiness in shift workers
as well as for sleep apnea, a condition that causes people to stop breathing at
night. Official approval, which is expected soon, will mean Cephalon can start
promoting the drug not just to sleep doctors but to family doctors. The company
is gearing up to deploy an "expanded sales force" early next year.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors can't even agree whether "shift
work sleep disorder" is a true medical illness, and there's evidence people are
taking Modafinil for conditions not sanctioned by government regulators.
In the U.S. alone, some 250,000 people are using Modafinil, even though only
150,000 Americans are estimated to have narcolepsy. Canadian prescriptions have
nearly doubled since 2001. Nearly 28,000 prescriptions were dispensed in
Canadian drugstores during the 12 months ending October 2003, compared to 14,648
in 2001, according to Health Canada.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for Modafinil, says Cornell University psychologist and sleep
expert James Maas.
"There is this notion that if you sleep a lot, you're lazy and useless," Coren
says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it's little wonder we've become a nation
"of walking zombies," says Maas. Millions try to catch up by oversleeping on
holidays and weekends, but our sleep debts just keep accruing, week after week.
Studies have found that people who sleep six hours or less a night have an
increased risk of high blood pressure, heart attacks and stroke.
Just one bad night's sleep can have a dramatic effect on memory, alertness,
concentration and judgment, and chronic sleep deprivation can lead to
depression.
More worrisome, "when we're really sleep deprived, at some point in time we
start to micro-sleep," says Coren. "No matter what we're doing, our brain goes
into a sleep state, and it can remain there anywhere from 10 seconds to a
minute.
"Now suppose that you're tooling down the road in your car at 50 kilometres an
hour and you have one of these small little micro-sleeps, and it's the 10-second
kind. What that means is that your car will travel more than the length of a
football field while you're asleep."
Still, Coren worries about using drugs to manipulate the body's need for sleep.
"Obviously if you have an individual who is in jeopardy of losing his livelihood
if he can't adapt to shift work, you might consider it."
But given the huge number of people in the world who work odd hours, from
nurses, firefighters, and factory workers to pilots and 911 operators, "we could
be talking about a large number of individuals who are going to start to muck up
their sleep chemistry."
And no matter how safe drugs that beat back sleep become, they will always bump
up against the fact that the brain will always find a way to sleep, no matter
what we're doing. That, the experts say, is enough to lose sleep over.
LOAD-DATE: December 29, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
655 of 998 DOCUMENTS
Windsor Star (Ontario)
December 24, 2003 Wednesday Final Edition
'Wake-promoting' drugs a hot untapped market;
Polls say one out of three Canadians getting six hours of sleep or less
SOURCE: CanWest News Service
BYLINE: Sharon Kirkey CanWest News Service
SECTION: NEWS; Pg. C1
LENGTH: 666 words
DATELINE: Ottawa
Psychologist Stanley Coren finds a particular lunacy in our determination to
squeeze more minutes out of every day, when all the science shows not getting
enough sleep makes people, as he puts it, clumsy, stupid, unhappy and dead.
Humans have been hardwired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia. "Generally speaking, we're about two hours
sleep-deprived every night."
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night, or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks in the middle of a conversation, sitting in the
drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, or so-called "shift work sleep disorder," as well as for sleep
apnea, a condition that causes people to stop breathing for a minute or longer
up to 100 times a night.
Official approval, which is expected soon, will mean Cephalon can start
promoting the drug not just to sleep doctors and other specialists, but to the
real wellspring for drug sales: family doctors. The company is already gearing
up to deploy an "expanded sales force" early next year.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors can't even agree whether "shift
work sleep disorder" is a true medical illness and there's already evidence
people are getting modafinil "off label," meaning for conditions that haven't
been sanctioned by government regulators.
In the U.S. alone, some 250,000 people are using modafinil, even though only
150,000 Americans are estimated to have narcolepsy. Canadian prescriptions have
nearly doubled since 2001. Nearly 28,000 prescriptions were dispensed in
Canadian drugstores during the 12 months ending October 2003, compared to 14,648
in 2001, according to IMS Health Canada.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for modafinil, says Cornell University psychologist and sleep
expert James Maas.
ATHLETE'S STIMULANT DU JOUR?
Some reports suggest the drug has become the stimulant du jour among track and
field athletes. U.S. sprinter Kelli White tested positive for the drug at the
world championships in Paris earlier this year. She says she was taking it to
treat her narcolepsy. Chris Phillips, another U.S. athlete, also tested positive
for modafinil at the same Paris meet, prompting anti-doping officials to muse
about the oddly high number of athletes with narcolepsy.
But the potential for abuse isn't limited to the playing field. Some fear the
pressure for employees to drug themselves to meet employers' demands may be
huge. After all, sleep is seen as a luxury, not a need, Coren says.
LOAD-DATE: December 24, 2003
LANGUAGE: ENGLISH
GRAPHIC: Kelli White
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
656 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
December 24, 2003, Wednesday
YEARENDER-Athletics-Modafinil, THG rock track and field
SECTION: WORLD NEWS; SPORTS
LENGTH: 822 words
By Sportswriter Pan Yi
BEIJING, Dec. 24 (Xinhua) -- Modafinil, a medical stimulant which can prevent a
person from sleepiness, and THG, a newly- detected steroid, have become the two
most eye-catching things in this year's world track and field arena which has
seen tougher anti-doping hands of IAAF and dim performances by top stars.
Attention was drawn to the doping as many top names emerged on the black list.
British sprinter Dwain Chambers, the European 100 meters champion and record
holder, tested positive for the designer anabolic steroid tetrahydrogestrinone
(THG) and is facing a two-year ban and return of the men's 4x100m relay silver
medal gained at the Paris World Championships in August.
Chambers' training partner American Kelli White, who claimed the titles of
women's 100m and 200m in Paris, tested positive for modafinil. Also on the
modafinil list were American sprinter Chryste Gaines, a member of the victorious
women's 4x100m relay team in the 1996 Atlanta Olympics, hurdler Chris Phillips,
who finished sixth in men's 110m hurdles in Paris, and American 400m runner
Calvin Harrison, the Olympic and world gold medallist and a member of the
American team who won the gold medal in the 4x400m relay in Paris.
Obviously, the United States, the world athletics powerhouse, has become the
most serious doping-hit area where three shinning stars, middle-distance runner
Regina Jacobs, shot put champion Kevin Toth and hammer thrower John McEwan, have
also tested positive for THG this year.
Coincidentally, Gaines, White, Phillips, Chambers all train with Ukrainian-born
coach Remi Korchemny who is under scrutiny for doping abuse. Moreover, White,
Chambers, Harrison and Phillips are all clients of a California lab that sells
nutritional supplements but is suspected by the U.S. federal grand jury of
developing THG.
THG is a new kind of anabolic steroids which are synthetic versions of the male
hormone testosterone. Athletes use them illegally to bulk up muscle and enhance
performance.
U.S. drug authorities first learned about THG this summer after an unidentified
coach gave them a syringe containing it. THG apparently was designed
specifically (molecule structure changed) to be undetectable by the standard
test given to athletes.
Modafinil, which is marketed under the name Provigil, was not officially banned
until after the world championships in August but it qualified as a banned
substance because of a broad clause in the anti-doping rules prohibiting
substances closely related to banned drugs.
As so many athletes were suddenly testing positive for Modafinil, doping experts
suspected that they were also taking THG. It is possible they believe that
modafinil would act as a masking agent in case laboratories could test for THG.
Facing the two new foes of the sport and such an embarrassing situation, the
International Association of Athletics Federations (IAAF) took prompt moves and
used iron hands to purify the arena. It has decided to retest all urine samples
(about 400) from Paris World Championships. Any positive findings would lead to
retroactive disqualification, including stripping of any medals, and two-year
bans.
"The emergence of this new steroid is a matter of great concern and we are
taking all steps that we can to investigate how widespread its use has been,"
IAAF president Lamine Diack said in October.
The IAAF also requested the United States, which is at the heart of the doping
scandals, to make extensive and intensive investigation into the doping cases.
In the war against THG, the IAAF needs the concrete assistance from the United
States, the only country having the effective methods to check THG.
The United States, which is often blamed for shielding its suspected athletes,
has paid great attention to the new situation now. It has identified THG as
illegal, put manufacturers on notice that the government will crack down on
anyone caught selling it.
The U.S. Food and Drug Administration also warned consumers that the use of
anything containing THG may risk their health. The U.S. anti-doping agency has
retested the samples from the U.S. Championships, and those found guilty have
been punished.
Partly because of the IAAF anti-doping punches, there were lack of astonishing
performances in the world arena this year, especially made by those star
athletes. At the Paris World Championships, the highest-level gathering this
year, the mark of the champion from the most eye-catching men's 100m was only
10.07 seconds, which was the poorest one in high-level competitions in 20 years.
However, the IAAF anti-doping determination has won support from most of the
world. People rather want to see no-shinning but real results than shinning but
fake ones. Fair play is unshakable norm of sports forever. At the 2004 Olympic
Games, people from all over the world are eager to see brilliant and cheat-free
performances.
LOAD-DATE: December 25, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
657 of 998 DOCUMENTS
Edmonton Journal (Alberta)
December 23, 2003 Tuesday Final Edition
Cutting back on sleep at your peril: Illness, accidents result from fatigue
SOURCE: CanWest News Service
BYLINE: Sharon Kirkey
SECTION: News; Pg. A1
LENGTH: 784 words
DATELINE: OTTAWA
OTTAWA - Psychologist Stanley Coren finds a particular lunacy in our
determination to squeeze more minutes out of every day, when all the science
shows not getting enough sleep makes people, as he puts it, clumsy, stupid,
unhappy and dead.
Humans have been hard-wired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia.
"Generally speaking, we're about two hours sleep-deprived every night."
Some polls suggest one out of every three Canadians is managing on just six
hours of sleep a night, or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks in the middle of a conversation, sitting in the
drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, or so-called "shift work sleep disorder," as well as for sleep
apnea, a condition that causes people to stop breathing for a minute or longer
up to 100 times a night. Official approval, which is expected soon, will mean
Cephalon can start promoting the drug not just to sleep doctors and other
specialists, but to the real wellspring for drug sales: family doctors. The
company is already gearing up to deploy an "expanded sales force" early next
year.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors can't even agree whether "shift
work sleep disorder" is a true medical illness, and there's already evidence
people are getting modafinil "off label," meaning for conditions that haven't
been sanctioned by government regulators.
In the U.S. alone, some 250,000 people are using modafinil, even though only
150,000 Americans are estimated to have narcolepsy. Canadian prescriptions have
nearly doubled since 2001.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for modafinil, says Cornell University sleep expert James Maas.
"There is this notion somehow or another that if you sleep a lot, you're lazy
and useless," Coren says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it's little wonder we've become a nation
"of walking zombies," says Maas.
Studies have found that people who sleep six hours or less a night have an
increased risk of high blood pressure, heart attacks and stroke. Just one bad
night's sleep can have a dramatic effect on memory, alertness, concentration and
judgment, and chronic sleep deprivation can lead to anxiety and depression.
More worrisome, "when we're really sleep deprived, at some point in time we
start to micro sleep," says Coren. "No matter what we're doing, our brain goes
into a sleep state, and it can remain there anywhere from 10 seconds to a
minute."
"Now suppose that you're tooling down the road in your car at 50 kilometres an
hour and you have one of these small little micro sleeps, and it's the 10-second
kind. What that means is that your car will travel more than the length of a
football field while you're asleep."
In fact, Coren's team has found that traffic accidents in Canada jump seven per
cent on the Monday after the switch to daylight time and people lose an hour's
worth of sleep.
Still, Coren worries about using drugs to manipulate the body's need for sleep.
"Obviously if you have an individual who is in jeopardy of losing his livelihood
if he can't adapt to shift work, you might consider it."
LOAD-DATE: December 23, 2003
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: Ottawa Citizen, Canwest News, File; Drowsy drivers are
one symptom of a sleep-deprived society.
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
658 of 998 DOCUMENTS
The Gazette (Montreal, Quebec)
December 23, 2003 Tuesday Final Edition
Drugs mean you can forfeit 40 winks: Humans have been hardwired to require nine,
even 10 hours of sleep a night. But what if you could get a good night's sleep
in a pill?
SOURCE: CanWest News Service
BYLINE: SHARON KIRKEY
SECTION: News; Pg. A4
LENGTH: 799 words
DATELINE: OTTAWA
Psychologist Stanley Coren finds a particular lunacy in our determination to
squeeze more minutes out of every day, when most research suggests not getting
enough sleep makes people, as he puts it, clumsy, stupid, unhappy and dead.
Humans have been hardwired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia. "Generally speaking, we're about two hours
sleep-deprived every night."
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night, or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks in the middle of a conversation, sitting in the
drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, as well as for sleep apnea, a condition that causes people to
stop breathing for a minute or longer up to 100 times a night.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous.
People have always searched for ways to get by on less sleep. Coffee has become
the second-most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for modafinil, says Cornell University psychologist and sleep
expert James Maas.
Some reports suggest the drug has become the stimulant du jour among track and
field athletes. U.S. sprinter Kelli White tested positive for the drug at the
world championships in Paris this year. She says she was taking it to treat her
narcolepsy. Chris Phillips, another U.S. athlete, also tested positive for
modafinil at the same Paris meet, prompting anti-doping officials to muse about
the oddly high number of athletes with narcolepsy.
But the potential for abuse isn't limited to the playing field. Some fear the
pressure for employees to drug themselves to meet employers' demands may be
huge. After all, sleep is seen as a luxury, not a need, Coren says. A Microsoft
executive once sniffed sleep is "nonproductive downtime."
"There is this notion somehow or another that if you sleep a lot, you're lazy
and useless," Coren says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it's little wonder we've become a nation
"of walking zombies," Maas says.
Millions try to catch up by oversleeping on holidays and weekends, but our sleep
debts just keep accruing, week after week.
Studies have found people who sleep six hours or less a night have an increased
risk of high blood pressure, heart attacks and stroke. Just one bad night's
sleep can have a dramatic effect on memory, alertness, concentration and
judgment, and chronic sleep deprivation can lead to anxiety and depression.
More worrisome, "when we're really sleep deprived, at some point in time we
start to micro sleep," Coren says. "No matter what we're doing, our brain goes
into a sleep state, and it can remain there anywhere from 10 seconds to a
minute."
In fact, Coren's team has found traffic accidents in Canada jump seven per cent
on the Monday after the switch to daylight savings time and people lose an
hour's worth of sleep.
Still, Coren worries about using drugs to manipulate the body's need for sleep.
"We could be talking about a large number of individuals who are going to start
to muck up their sleep chemistry," he says, considering the high number of
people who work night shifts.
And no matter how safe drugs that beat back sleep become, they will always bump
up against the fact that the brain will always find a way to sleep, no matter
what we're doing.
That, the experts say, is enough to lose sleep over.
LOAD-DATE: December 23, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: THE GAZETTE; Modafinil has become the stimulant du jour for some
athletes.
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
659 of 998 DOCUMENTS
National Post (Canada)
December 23, 2003 Tuesday National Edition
Giving sleep a rest: A drug narcoleptics take to stay awake is being promoted
for a sleep-deprived public
SOURCE: CanWest News Service
BYLINE: Sharon Kirkey
SECTION: News; Pg. A17
LENGTH: 1270 words
Psychologist Stanley Coren finds a particular lunacy in our determination to
squeeze more minutes out of every day, when all the science shows not getting
enough sleep makes people, as he puts it, clumsy, stupid, unhappy and dead.
Humans have been hardwired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia. "Generally speaking, we're about two hours
sleep-deprived every night."
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night, or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: modafinil (sold as Alertec in Canada and Provigil
in the United States) has been available since 1999 for the treatment of
narcolepsy, a devastating disorder that affects one out of every 3,000 people
and causes uncontrollable sleep attacks in the middle of a conversation, sitting
in the drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, or so-called "shift work sleep disorder," as well as for sleep
apnea, a condition that causes people to stop breathing for a minute or longer
up to 100 times a night. Official approval, which is expected soon, will mean
the manufacturer, Cephalon, can start promoting the drug not just to sleep
doctors and other specialists, but to the real wellspring for drug sales: family
doctors. The company is gearing up to deploy an expanded sales force early next
year.
Meanwhile, Massachusetts-based Hypnion Inc. has wake-alertness compounds in the
queue that it claims are superior to modafinil. Researchers in Ottawa are about
to start testing a new chemical cousin of modafinil. And a Canadian
military-sponsored research facility in Toronto has been testing modafinil in
soldiers under different simulated field conditions of "sustained wakefulness."
According to Wired Magazine, "continuous alertness could be available over the
counter" within 10 years. "These drugs will do for sleep disorders what Prozac
did for depression," Dale Edgar, co-founder of Hypnion, told the magazine.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors cannot even agree whether "shift
work sleep disorder" is a true medical illness, and there is already evidence
people are getting modafinil "off label," meaning for conditions that have not
been sanctioned by government regulators.
In the United States alone, some 250,000 people are using modafinil, even though
only 150,000 Americans are estimated to have narcolepsy. Canadian prescriptions
have nearly doubled since 2001. Nearly 28,000 prescriptions were dispensed in
Canadian drugstores during the 12 months ending October, 2003, compared to
14,648 in 2001, according to IMS Health Canada.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions" for modafinil, says Cornell University psychologist and sleep
expert James Maas.
"There is this notion somehow or another that if you sleep a lot, you're lazy
and useless," Coren says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it is little wonder we have become a
nation "of walking zombies," says Maas. Millions try to catch up by oversleeping
on holidays and weekends, but our sleep debts just keep accruing, week after
week.
Children, too, are being increasingly sleep starved, a phenomenon Maas partly
pins on parents "who don't know diddly about sleep and sleep requirements" in
school-aged children.
Old diaries and letters suggest that people were logging about nine hours a
night before 1913. Then Thomas Edison invented the light bulb.
"Part of the reason he did was that he really felt people were using darkness as
an excuse not to work and he wanted to increase our productivity," says Coren,
author of the book Sleep Thieves. "I don't know whether we're more productive,
but we're certainly more tired."
Scientist do not really know why humans need sleep, although most believe it
plays a fundamental role in regulating the genes in the brain that are involved
in numerous cellular functions. Deprive rats of sleep long enough and they will
die, usually within two weeks. Researchers also know that sleep occurs
throughout the animal kingdom, right down to the smallest complex animals, such
as fruit flies.
Shortened sleep can lead to reduced brain levels of leptin, the hormone that
controls appetite. Get too little sleep, Maas says, and the brain signals us to
eat complex carbohydrates, starches and sugars. U.S. researchers recently
discovered that "short sleepers" produce more cytokines, molecules that normally
fight germs and other invaders. "Except there are no germs, you just slept too
little, but they have to attack something, so they start to eat the arterial
walls," Maas says.
Studies have found that people who sleep six hours or less a night have an
increased risk of high blood pressure, heart attacks and stroke. Just one bad
night's sleep can have a dramatic effect on memory, alertness, concentration and
judgment, and chronic sleep deprivation can lead to anxiety and depression.
More worrisome, "when we're really sleep deprived, at some point in time we
start to micro sleep," Coren says. "No matter what we're doing, our brain goes
into a sleep state, and it can remain there anywhere from 10 seconds to a
minute."
"Now suppose that you're tooling down the road in your car at 50 kilometres an
hour and you have one of these small little micro sleeps, and it's the 10-second
kind. What that means is that your car will travel more than the length of a
football field while you're asleep."
In fact, Coren's team has found that traffic accidents in Canada jump 7% on the
Monday after the switch to daylight savings time and people lose an hour's
sleep.
Still, Coren worries about using drugs to manipulate the body's need for sleep.
"Obviously if you have an individual who is in jeopardy of losing his livelihood
if he can't adapt to shift work, you might consider it."
But given the huge number of people in the world who work odd hours, from
nurses, firefighters and factory workers to pilots and 911 operators, "we could
be talking about a large number of individuals who are going to start to muck up
their sleep chemistry."
And no matter how safe drugs that beat back sleep become, they will always bump
up against the fact that the brain will always find a way to sleep, no matter
what we're doing.
That, the experts say, is enough to lose sleep over.
LOAD-DATE: December 23, 2003
LANGUAGE: ENGLISH
GRAPHIC: Black & White Photo: Carlo Allegri, National Post; Researchers say few
people get the sleep their bodies require. One solution would be to remove the
need for rest.
TYPE: News
Copyright 2003 National Post, All Rights Reserved
660 of 998 DOCUMENTS
Ottawa Citizen
December 23, 2003 Tuesday Final Edition
Sleep-deprived Canadians make enticing market for alertness drugs
SOURCE: The Ottawa Citizen
BYLINE: Sharon Kirkey
SECTION: News; Pg. A1
LENGTH: 1523 words
Psychologist Stanley Coren finds a particular lunacy in our determination to
squeeze more minutes out of every day, when all the science shows not getting
enough sleep makes people, as he puts it, clumsy, stupid, unhappy and dead.
Humans have been hardwired through evolution to require nine, even 10, hours of
sleep a night, but the average North American is getting more like seven, says
Mr. Coren, director of the Human Neuropsychology and Perception Laboratory at
the University of British Columbia. "Generally speaking, we're about two hours
sleep-deprived every night."
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks in the middle of a conversation, sitting in the
drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, or so-called "shift work sleep disorder," as well as for sleep
apnea, a condition that causes people to stop breathing for a minute or longer
up to 100 times a night. Official approval, which is expected soon, will mean
Cephalon can start promoting the drug not just to sleep doctors and other
specialists, but to the real wellspring for drug sales: family doctors. The
company is already gearing up to deploy an "expanded sales force" early next
year.
Meanwhile, Massachusetts-based Hypnion Inc. has wake-alertness compounds in the
queue that it claims are superior to modafinil. Researchers in Ottawa are about
to start testing a new chemical cousin of modafinil. And a Canadian
military-sponsored research facility in Toronto has been testing modafinil in
soldiers under different simulated field conditions of "sustained wakefulness."
According to Wired magazine, "continuous alertness could be available over the
counter" within 10 years. "These drugs will do for sleep disorders what Prozac
did for depression," Dale Edgar, cofounder of Hypnion, told the magazine.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors can't even agree whether "shift
work sleep disorder" is a true medical illness, and there's already evidence
people are getting modafinil "off-label," meaning for conditions that haven't
been sanctioned by government regulators.
In the U.S. alone, some 250,000 people are using modafinil, even though only
150,000 Americans are estimated to have narcolepsy. Canadian prescriptions have
nearly doubled since 2001. Nearly 28,000 prescriptions were dispensed in
Canadian drugstores during the 12 months ending October 2003, compared to 14,648
in 2001, according to IMS Health Canada.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for modafinil, says Cornell University psychologist and sleep
expert James Maas.
Some reports suggest the drug has become the stimulant du jour among track and
field athletes. U.S. sprinter Kelli White tested positive for the drug at the
world championships in Paris earlier this year. She says she was taking it to
treat her narcolepsy. Chris Phillips, another U.S. athlete, also tested positive
for modafinil at the same Paris meet, prompting anti-doping officials to muse
about the oddly high number of athletes with narcolepsy.
But the potential for abuse isn't limited to the playing field. Some fear the
pressure for employees to drug themselves to meet employers' demands may be
huge. After all, sleep is seen as a luxury, not a need, Mr. Coren says. A
Microsoft executive once sniffed that sleep is "nonproductive downtime."
"There is this notion somehow or another that if you sleep a lot, you're lazy
and useless," Mr. Coren says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it's little wonder we've become a nation
"of walking zombies," says Mr. Maas. Millions try to catch up by oversleeping on
holidays and weekends, but our sleep debts just keep accruing, week after week.
Children too are being increasingly sleep starved, a phenomenon Mr. Maas partly
pins on parents "who don't know diddly about sleep and sleep requirements" in
school-aged children.
Old diaries and letters suggest that people were logging about nine hours a
night before 1913. Then Thomas Edison invented the light bulb.
"Part of the reason he did was that he really felt people were using darkness as
an excuse not to work and he wanted to increase our productivity," says Mr.
Coren, author of the book Sleep Thieves. "I don't know whether we're more
productive, but we're certainly more tired."
Scientist don't really know why humans need sleep, although most believe it
plays a fundamental role in regulating the genes in the brain that are involved
in numerous cellular functions. Deprive rats of sleep long enough and they will
die, usually within two weeks. Researchers also know that sleep occurs
throughout the animal kingdom, right down to the smallest complex animals, such
as fruit flies.
Shortened sleep can lead to reduced brain levels of leptin, the hormone that
controls appetite. Get too little sleep, Mr. Maas says, and the brain signals us
to eat complex carbohydrates, starches and sugars. U.S. researchers recently
discovered that "short sleepers" produce more cytokines, molecules that normally
fight germs and other invaders. "Except there are no germs, you just slept too
little, but they have to attack something so they start to eat the arterial
walls," Mr. Maas says.
Studies have found that people who sleep six hours or less a night have an
increased risk of high blood pressure, heart attacks and stroke. Just one bad
night's sleep can have a dramatic effect on memory, alertness, concentration and
judgment, and chronic sleep deprivation can lead to anxiety and depression.
More worrisome, "when we're really sleep-deprived, at some point in time we
start to microsleep," says Mr. Coren. "No matter what we're doing, our brain
goes into a sleep state, and it can remain there anywhere from 10 seconds to a
minute."
"Now suppose that you're tooling down the road in your car at 50 kilometres an
hour and you have one of these small little microsleeps, and it's the 10-second
kind. What that means is that your car will travel more than the length of a
football field while you're asleep."
In fact, Mr. Coren's team has found that traffic accidents in Canada jump seven
per cent on the Monday after the switch to daylight savings time, when people
lose an hour's worth of sleep.
Modafinil, for its part, appears safer than traditional stimulants at conquering
sleepiness. Researchers at the Ottawa Hospital have found more complaints of
nausea and nervousness in patients taking 400 mg of modafinil a day versus those
on a placebo, though the side-effects disappeared after a week. Some studies
have shown a significant increase in "pounding, pulsating" headaches, reports
Ottawa sleep expert Dr. Roger Broughton, usually also during the first several
days of treatment. "But the rates of side-effects are really quite low."
The drug doesn't cause the hangover effects amphetamines do, and you can't get
high from it. There is also a lower risk of abuse. (It can, however, interfere
with some forms of birth control.)
Still, Mr. Coren worries about using drugs to manipulate the body's need for
sleep.
"Obviously, if you have an individual who is in jeopardy of losing his
livelihood if he can't adapt to shift work, you might consider it."
But given the huge number of people in the world who work odd hours, from
nurses, firefighters, and factory workers to pilots and 911 operators, "we could
be talking about a large number of individuals who are going to start to muck up
their sleep chemistry."
And no matter how safe drugs that beat back sleep become, they will always bump
up against the fact that the brain will always find a way to sleep, no matter
what we're doing.
That, the experts say, is enough to lose sleep over.
LOAD-DATE: December 23, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
661 of 998 DOCUMENTS
The Vancouver Sun (British Columbia)
December 23, 2003 Tuesday Final Edition
Take this pill, stay awake all day and all night, too: Go 40 hours without sleep
with no side effects
SOURCE: CanWest News Services
BYLINE: Sharon Kirkey
SECTION: News; Pg. A1
LENGTH: 1520 words
DATELINE: OTTAWA
OTTAWA -- Psychologist Stanley Coren finds a particular lunacy in our
determination to squeeze more minutes out of every day, when all the science
shows not getting enough sleep makes people, as he puts it, clumsy, stupid,
unhappy and dead.
Humans have been hardwired through evolution to require nine, even 10 hours of
sleep a night, but the average North American is getting more like seven, says
Coren, director of the Human Neuropsychology and Perception Laboratory at the
University of British Columbia.
"Generally speaking, we're about two hours sleep-deprived every night," he says.
Some polls suggest one out of every three Canadians is managing just six hours
of sleep a night, or less.
But, what if you could get the equivalent of a good night's sleep in a pill, a
drug that would keep you awake for 40 hours or more with little, if any, of the
jitteriness, agitation, anxiety and insomnia associated with other brain
stimulants, including caffeine?
"Wake-promoting" agents have become one of the hottest fields of drug research,
with a vast, mostly untapped market potentially worth billions. The patient
population for "sleep therapeutics" is bigger than that for depression.
One such drug is already here: Modafinil (sold as Alertec in Canada and Provigil
in the U.S.) has been available since 1999 for the treatment of narcolepsy, a
devastating disorder that affects one out of every 3,000 people and causes
uncontrollable sleep attacks in the middle of a conversation, sitting in the
drive-through at McDonald's or any other inappropriate time.
But now, the U.S. Food and Drug Administration has given its preliminary
blessing for expanded uses of the drug to treat excessive daytime sleepiness in
shift workers, or so-called "shift work sleep disorder," as well as for sleep
apnea, a condition that causes people to stop breathing for a minute or longer
up to 100 times a night. Official approval, which is expected soon, will mean
Cephalon can start promoting the drug not just to sleep doctors and other
specialists, but also to the real wellspring for drug sales: family doctors. The
company is already gearing up to deploy an "expanded sales force" early next
year.
Meanwhile, Massachusetts-based Hypnion Inc. has wake-alertness compounds in the
queue that it claims are superior to modafinil. Researchers in Ottawa are about
to start testing a new chemical cousin of modafinil. And a Canadian
military-sponsored research facility in Toronto has been testing modafinil in
soldiers under different simulated field conditions of "sustained wakefulness."
According to Wired Magazine, "continuous alertness could be available over the
counter" within 10 years. "These drugs will do for sleep disorders what Prozac
did for depression," Dale Edgar, cofounder of Hypnion, told the magazine.
But the prospect of people swallowing pills to postpone sleep has some critics
nervous. When is sleepiness a sickness? Doctors can't even agree whether "shift
work sleep disorder" is a true medical illness, and there's already evidence
people are getting modafinil "off label," meaning for conditions that haven't
been sanctioned by government regulators.
In the U.S. alone, some 250,000 people are using modafinil, even though only
150,000 Americans are estimated to have narcolepsy. Canadian prescriptions have
nearly doubled since 2001. Nearly 28,000 prescriptions were dispensed in
Canadian drugstores during the 12 months ending October 2003, compared with
14,648 in 2001, according to IMS Health Canada.
People have always searched for ways to get by on less sleep. Coffee has become
the second most commonly traded commodity in the world, next to oil. But now
athletes and CEOs and college students "and everyone who wants to stay wide
awake all day long under minimal sleep are asking their physicians for
prescriptions," for modafinil, says Cornell University psychologist and sleep
expert James Maas.
Some reports suggest the drug has become the stimulant du jour among track and
field athletes. U.S. sprinter Kelli White tested positive for the drug at the
world championships in Paris earlier this year. She says she was taking it to
treat her narcolepsy. Chris Phillips, another U.S. athlete, also tested positive
for modafinil at the same Paris meet, prompting anti-doping officials to muse
about the oddly high number of athletes with narcolepsy.
But the potential for abuse isn't limited to the playing field. Some fear the
pressure for employees to drug themselves to meet employers' demands may be
huge. After all, sleep is seen as a luxury, not a need, Coren says. A Microsoft
executive once sniffed that sleep is "nonproductive downtime."
"There is this notion somehow or another that if you sleep a lot, you're lazy
and useless," Coren says.
Add that to our frenetic lives, the growing numbers of harried, dual-income
families trying to cope with the demands of work and home, the seductive
all-night allure of the Internet, and it's little wonder we've become a nation
"of walking zombies," says Maas. Millions try to catch up by oversleeping on
holidays and weekends, but our sleep debts just keep accruing, week after week.
Children too are being increasingly sleep starved, a phenomenon Maas partly pins
on parents "who don't know diddly about sleep and sleep requirements" in
school-aged children.
Old diaries and letters suggest that people were logging about nine hours a
night before 1913. Then Thomas Edison invented the light bulb.
"Part of the reason he did was that he really felt people were using darkness as
an excuse not to work and he wanted to increase our productivity," says Coren,
author of the book Sleep Thieves. "I don't know whether we're more productive,
but we're certainly more tired."
Scientists don't really know why humans need sleep, although most believe it
plays a fundamental role in regulating the genes in the brain that are involved
in numerous cellular functions. Deprive rats of sleep long enough and they will
die, usually within two weeks. Researchers also know that sleep occurs
throughout the animal kingdom, right down to the smallest complex animals, such
as fruit flies.
Shortened sleep can lead to reduced brain levels of leptin, the hormone that
controls appetite. Get too little sleep, Maas says, and the brain signals us to
eat complex carbohydrates, starches and sugars. U.S. researchers recently
discovered that "short sleepers" produce more cytokines, molecules that normally
fight germs and other invaders. "Except there are no germs, you just slept too
little, but they have to attack something so they start to eat the arterial
walls," Maas says.
Studies have found that people who sleep six hours or less a night have an
increased risk of high blood pressure, heart attacks and stroke. Just one bad
night's sleep can have a dramatic effect on memory, alertness, concentration and
judgment, and chronic sleep deprivation can lead to anxiety and depression.
More worrisome, "when we're really sleep deprived, at some point in time we
start to micro sleep," says Coren. "No matter what we're doing, our brain goes
into a sleep state, and it can remain there anywhere from 10 seconds to a
minute."
"Now suppose that you're tooling down the road in your car at 50 kilometres an
hour and you have one of these small little micro sleeps, and it's the 10-second
kind. What that means is that your car will travel more than the length of a
football field while you're asleep."
In fact, Coren's team has found that traffic accidents in Canada jump seven per
cent on the Monday after the switch to daylight savings time and people lose an
hour's worth of sleep.
Modafinil, for its part, appears safer than traditional stimulants at conquering
sleepiness. Researchers at the Ottawa Hospital have found more complaints of
nausea and nervousness in patients taking 400 mg of modafinil a day versus those
on a placebo, though the side effects disappeared after a week. Some studies
have shown a significant increase in "pounding, pulsating" headaches, reports
Ottawa sleep expert Dr. Roger Broughton, usually also during the first several
days of treatment. "But the rates of side effects are really quite low."
The drug doesn't cause the hangover effects amphetamines do, and you can't get
high from it. There is also a lower risk of abuse. (It can, however, interfere
with some forms of birth control.)
Still, Coren worries about using drugs to manipulate the body's need for sleep.
"Obviously if you have an individual who is in jeopardy of losing his livelihood
if he can't adapt to shift work, you might consider it."
But given the huge number of people in the world who work odd hours, from
nurses, firefighters, and factory workers to pilots and 911 operators, "we could
be talking about a large number of individuals who are going to start to muck up
their sleep chemistry."
And no matter how safe drugs that beat back sleep become, they will always bump
up against the fact that the brain will always find a way to sleep, no matter
what we're doing.
That, the experts say, is enough to lose sleep over.
LOAD-DATE: December 23, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
662 of 998 DOCUMENTS
The Leader-Post (Regina, Saskatchewan)
November 22, 2003 Saturday Final Edition
New drug fools the brain into being alert
SOURCE: Special to The Leader-Post
BYLINE: Ed Willett
SECTION: Weekender; Science; Pg. G3
LENGTH: 524 words
There were lots of bleary-eyed people around Regina this week, following the
Grey Cup revelry. But then, there are always lots of bleary-eyed people around,
since very few of us get enough sleep.
So wouldn't it be great if you could just take a pill and feel alert?
I'm not talking about amphetamines, but about eugeroics (the name means "good
arousal"), a new class of drugs which currently has only two members, adrafinil
and its successor, modafinil, developed in France and available in Canada since
1999 as Alertec. Currently approved only for narcolepsy it's beginning to find
its way into the hands of other people who need to stay awake, from soldiers to
stockbrokers.
Eugeroics differ significantly from amphetamines. Amphetamines stimulate the
entire central nervous system, essentially by fooling the brain into thinking
it's being threatened. They raise your pulse rate, give you jolts of adrenaline,
interfere with normal sleep, and can be addictive. You also have to to take
larger and larger doses to get the same effect until, inevitably, you crash.
Modafinil, on the other hand, somehow (the precise mechanism isn't known)
targets a part of the hypothalamus called the suprachiasmatic nuclei. In the
late 1980s, researchers discovered this part of the brain controls wakefulness,
quite separately from the mechanism that makes us feel sleepy. Modafinil keeps
the wakefulness centre active long after it would normally have shut down. As a
result, the rest of the brain thinks it's well-rested, even when it's not.
Modafinil doesn't produce the "wired" sensation of amphetamines or caffeine. It
also doesn't interfere with normal sleep -- you can take it, stay alert until
bedtime, then go to sleep as usual. Modafinil also shows no signs of being
addictive and only rarely causes minor side effects like headache and nausea.
So will it be available over-the-counter? Not in the short term.
Side-effects from long-term use might still crop up. As well, experts worry
people would use it to avoid sleep to the point that their health would suffer
-- besides keeping us mentally alert, sleep helps regulate our hormonal and
immune systems. There is also concern about unknown interactions with other
drugs.
However, tests are underway for its use to help sufferers of chronic fatigue
syndrome and sleep apnea, multiple sclerosis, and depression. It's being tested
on Chicago shift workers who find themselves too sleepy to work in the middle of
the night. And it's apparently already in use, in a limited and somewhat
unofficial fashion, by the U.S. forces in Iraq.
More effective drugs, both to help people stay awake and to help them fall
asleep more quickly and sleep better are now under development.
We may eventually be able to schedule sleep when we want it, and avoid it when
it's inconvenient. What that means to society, no one can yet say. For now, at
least, the age-old solution to drowsiness remains the best: take a nap.
- Edward Willett is a Regina freelance writer. E-mail comments or questions to
edward@edwardwillett.com. Read a longer version of this column online at
www.edwardwillett.com
LOAD-DATE: November 22, 2003
LANGUAGE: ENGLISH
TYPE: Column
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
663 of 998 DOCUMENTS
The Daily Telegraph (Sydney, Australia)
November 20, 2003 Thursday
Hot on the trail of the THG cheats
SOURCE: MATP
BYLINE: MIKE HURST
SECTION: SPORTTABLE; Pg. 73
LENGTH: 1222 words
SEPARATE investigations into seemingly unrelated drug busts for designer
anabolic steroids appear to be converging as America finally responds to calls
to get tougher on sports doping.
A US grand jury has called many high-profile sports champions, including 100m
world record-holder Tim Montgomery and fellow Sydney Olympic sprint gold
medallist Marion Jones, to testify under oath at an inquiry into the use of
tetrahydrogestrinone (THG) -- a body-building steroid previously unidentified by
drug testers.
There is no suggestion Montgomery or Jones used or supplied THG or any other
drug.
The grand jury is also questioning witnesses about the endurance-enhancing drug
EPO, HGH (human growth hormone) and other anabolic agents.
Another investigation by the US Attorney's Office in the Central District of
Illinois has been running since March this year when track cyclist Tammy Thomas
became the first person known to have failed a test for the obscure anabolic
steroid Norbolethone.
Thomas, 33, won a sprint silver medal at the 2001 world championships in
Antwerp, Belgium.
She has received a life ban from USA Cycling.
US anti-doping officials believe prominent dietary supplement designer, Patrick
Arnold, may have made Norbolethone.
Arnold is said to be the first chemist outside of the former East Germany to
make androstenedione, a legal steroid in the US where it is used in food
supplements. He is also credited with inventing 1-testosterone, another steroid
legal used in US supplements.
Arnold and Thomas deny knowing each other.
Also known as Genabol, powerfully acting Norbolethone was designed in 1964 at
Wyeth Laboratories in Philadelphia and studied until 1972 when the company
decided not to trade the product.
Nothing was heard in public about Norbolethone until in 2001 Canadian athletics
coach Charlie Francis wrote: "In a review of the negative tests after the Sydney
Olympics, the drug testers saw a suspicious compound on many of their tests and
began to investigate. Some months later they identified the compound as Genabol
[also called Norbolethone].
"By the time a test was developed, the word was out and the athletes moved on to
newer products." One of those newer products may have been the fore-runner to
THG, which appears to have been this year's most favoured model.
Five track and field athletes have so far tested positive to THG. They include
Europe's top sprinter Dwain Chambers of England and Americans Regina Jacobs
(1500m, 5000m), Kevin Toth (shot put) and John McEwen (hammer throw).
The identity of a fifth athlete who competed at the recent world championships
in Paris has not been made public.
The fifth athlete is understood to be a low-profile thrower, possibly an
American male hammer thrower.
Another investigation into the use of a stimulant, Modafinil, has been running
concurrent with the THG inquiry and there appears to be some overlapping.
Kelli White, the world 100m and 200m champion, claims after she was busted in
the Paris championships in August that she took Modafinil to treat narcolepsy,
which is a sleep-disorder.
White's training partner, Chryste Gaines, also tested positive for Modafinil.
Fellow Americans, the Paris world championship 400m hurdles silver medallist
Sandra Glover, Eric Thomas, Calvin Harrison and Chris Phillips were also caught
for Modafinil. They dispensed with the narcolepsy excuse.
The common denominator between most of these athletes is 71-year-old Remy
Korchemny, a famous coach of the Soviet Union's 1972 Munich Olympic sprint
double winner Valeriy Borzov.
He is now based at Berkeley, California, where he coaches White, Gaines and
Chambers.
Korchemny admits giving Modafinil to Phillips. He also coaches Harrison's twin
brother Alvin, both of whom won Olympic 4x400m relay gold medals in Sydney.
The Daily Telegraph has been told by a source close to the grand jury
proceedings that an as yet unnamed but high-profile athlete has talked under
immunity of receiving THG and using it on assurances that it could not be found.
She did not fail a test for THG.
She allegedly nominated Victor Conte as having provided her with THG and gave
Conte a $US10,000 bonus out of her winnings at the end of the European season.
Conte denies being the source of THG.
CONTE and Korchemny formed a track club called ZMA, short for Zinc-Magnesium,
two common minerals Conte developed into a sports formula to reap a small
fortune.
Arnold and Conte know each other, but deny doing business with each other.
Conte is the owner of the Bay Area Laboratory Co-Operative (BALCO). Conte does
not have a college degree or professional background in health or science, but
runs a lucrative nutritional and testing business near San Francisco airport.
BALCO was raided on September 3 by agents from the San Mateo County Narcotics
Task Force and Internal Revenue Service (taxation) authorities who confiscated
numerous boxes of files.
This followed the case-breaking delivery in mid-June, allegedly by an anonymous
whistleblower athletics coach, of a syringe containing a "designer" steroid to
the United States Anti Doping Agency.
USADA claims to have passed the syringe to the UCLA Olympic Analytical
Laboratory where the lab chief of 21 years, Don Catlin, a molecular
pharmacologist and endocrinologist, drew together a team of chemists who
"reverse engineered" the substance and identified it as THG.
THE STORY SO FAR
* United States Anti-Doping Agency (USADA) claim to receive a syringe containing
a "designer steroid" from an anonymous athletics coach in mid-June.
* UCLA Olympic lab sleuths "reverse engineer" the mystery compound and named it
THG (tetrahydrogestrinone).
* Europe's top sprinter Dwain Chambers returns positive result for THG from test
taken on August 1 * New world sprint double champion Kelli White tests positive
for stimulant Modafinil on August 30 in Paris.
* Narcotics agents and IRS raid the California sports food supplements
laboratory, BALCO, on September 3.
* USADA reveals existence of THG on October 16.
* Worldwide investigation involving re-testing of samples across the globe and
from athletics and swimming world championships and winter olympics * American
grand jury convened to investigate doping in US sport.
THE ATHLETES
* Positive to Modafinil Americans: Kelli White (world champion 100m, 200m),
Chryste Gaines (world's second fastest 100m runner), Calvin Harrison (world
champion 4x400m), Chris Phillips (world finalist 110m hurdles), Sandra Glover
(world 400m hurdles silver medallist), Eric Thomas (world championships
semi-finalist).
* Positive to THG Britain's Dwain Chambers (Goodwill Games and European
Championships 100m winner), and Americans Regina Jacobs (at 39, set world record
indoor 1500m this year), Kevin Toth (this year threw longest shot put mark since
1990), John McEwen (runner-up hammer throw at US titles).
WHAT NEXT
* WADA to expand influence into communist China, specifically targeting the
Thinker Chemical lab in Hangzhou.
* Revelations about other designer drugs, dating back to 1984 LA Olympics *
Increased funding to develop tests for HGH (human growth hormone) * Legal
challenges by athletes busted in re-testing Legal challenges to the EPO
(erythropoietin) test.
Resurgence of the drug culture
LOAD-DATE: November 19, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: DTM
Copyright 2003 Nationwide News Pty Limited
664 of 998 DOCUMENTS
The Times (London)
November 13, 2003, Thursday
White's second positive serves only to muddy waters
BYLINE: Peter Nichols
SECTION: Sport; 42
LENGTH: 590 words
KELLI WHITE could miss out on the Olympic Games next year after recording a
second positive drugs test. The United States sprinter's 100 metres and 200
metres world titles were already under threat after the sample given after the
100 metres final in Paris three months ago showed evidence of Modafinil, a drug
variously described as a "mild stimulant" and a "wake-promoter".
The second positive, also for Modafinil, has come after the re-examination by
the US Anti-Doping Agency (Usada) of samples taken at the US Track and Field
Championships at Stanford, California, in June.
The rules of the International Association of Athletics Federations (IAAF) state
that the penalty for a first offence is a warning and disqualification from the
championships in question; for a second offence, the penalty is a two-year ban.
Should the IAAF apply the letter of the law, White will lose not just her world
titles, but be banned until 2005.
If, that is, Modafinil is definitively identified as a banned substance. When
the story broke in Paris in August, Arne Lundqvist, chairman of the IAAF Medical
Commission, stated that he had no doubt that Modafinil was a banned substance,
even though it was not on either the IAAF list nor that of the World Anti Doping
Authority (Wada).
Yet when questioned as to which group it fell into or which of the drugs on the
list it related to, Lundqvist was unable to answer. Even though the drug could
not be properly classified, the US team, for fear of being disqualified later,
withdrew White from the 4 x 100 metres relay team.
The IAAF subsequently determined that Modafinil was a "mild stimulant" and fell
within the category of substances similar to those listed. However, while the
definition given by the Wada list is a distinctly loose one, stating that any
"related substances" are banned, the IAAF list is much more precise, listing 36
examples and adding substances that are "pharmacologically or chemically
related".
Within a fortnight of the World Championships, Robert Wagner, White's agent,
handed a 25-page statement to Lundqvist which argued that Modafinil could not be
considered a banned substance.
Later that month, Cephalon, the worldwide manufacturers of the drug, sent a
submission to Dick Pound, chief executive of Wada. Paul Blake, senior
vice-president of Cephalon, argued that Modafinil was not a stimulant, but a
"wake-promoter" and could not be related to any stimulant on the list. "It is a
separate pharmacological entity," Blake said.
Olivier Rabin, the science director of Wada, accepted that Modafinil was not
related chemically to any of the drugs on the list and could only be classified
as pharmacologically related because there was some evidence that it "stimulated
the central nervous system". Rabin agreed that Wada's information on the drug
was minimal. "It is not the typical profile of a stimulant...the full mechanism
of this substance remains unknown," he said, adding that the final decision may
be made in the US Courts.
Usada must determine not whether White was seeking to claim an advantage -
Modafinil has been used in sailing and rallying to promote wakefulness -but
whether a doping offence has been committed. The Usada Anti-Doping Review Board
should reach a decision soon but, having ordered the wholesale retesting of
samples, it may have argued itself into a corner.
Should it decide that no offence has been committed, the case reverts back to
the IAAF, which could itself decide to take further action.
LOAD-DATE: November 13, 2003
LANGUAGE: ENGLISH
Copyright 2003 Times Newspapers Limited
665 of 998 DOCUMENTS
The Sun Herald (Sydney, Australia)
November 9, 2003 Sunday
Late Edition
Drug crisis tai nts all: Fortune;
ATHLETICS
BYLINE: JAMES MacSMITH
SECTION: SPORT; Pg. 106
LENGTH: 348 words
ONE of Australia's leading coaches says he is worried about the future of
athletics and the reputations of its star performers, if the drugs crisis
continues to gain momentum.
Peter Fortune, best known as Cathy Freeman's former coach, said if the spate of
positive tests to designer steroid tetrahydrogestrinone and banned stimulant
modafinil grew, an increasingly sceptical public might consider coaches and
athletes guilty
of doping simply because they were involved in the sport.
Five world-class athletes have tested positive to using THG, and six top runners
have been caught taking modafinil.
"I'm not necessarily surprised at the extent of it [the doping] as much as it
does seem to be confined to a group or an area," Fortune said.
"One of the interesting things is that it's come about through jealousy [a coach
anonymously sending in a sample of THG to drug testing authorities in the US].
"It's disturbing and very negative for the sport. And it shows the extent that
some people are prepared to go to cheat."
Fortune said one of the good things to take out of the crisis was that the US
appeared to be getting serious in the fight against doping in track and field.
"It seems that at last authorities in the US are taking a much stronger
approach, where they have been a bit soft before, and that can only be good for
the sport," he said.
Athletics has been plunged into its biggest drugs crisis since Ben Johnson
tested positive to a steroid at the 1988 Olympic Games.
It began when THG was detected in the urine samples of athletes including
British sprinter Dwain Chambers. Others, including Sandra Glover, who finished
second in the 400-metres hurdles at the world championships in August, and
double world sprint champion Kelli White, tested positive to modafinil.
Fortune warned that clean athletes and coaches might be unfairly grouped with
those guilty of using, or promoting the use of performance-enhancing substances.
But the responsibility for drug use rested with athletes. "They shouldn't be
taking anything unless they know exactly what it is and where it came from," he
said.
LOAD-DATE: June 20, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 John Fairfax Publications Pty Ltd
All Rights Reserved
666 of 998 DOCUMENTS
The San Francisco Chronicle
NOVEMBER 4, 2003, TUESDAY, FINAL EDITION
PROFILE;
Remi Korchemny;
Caught in a tempest
SOURCE: Chronicle Staff Writer
BYLINE: John Crumpacker
SECTION: SPORTS; Pg. C1
LENGTH: 1822 words
If Remi Korchemny isn't quite in the eye of the storm, he's close enough to find
himself swept up in a widening sports-doping scandal. For more than three
decades, the Ukrainian-born Korchemny built a reputation as an astute and
analytical track and field coach, specializing in the sprints and hurdles.
His runners include some of the world's fastest men and women, as well as some
Union City teenagers who dream of becoming elite athletes themselves.
But now, at age71, this man -- whose father was executed by a Stalinist firing
squad and whose mother was imprisoned when he was a boy -- is being drawn toward
the center of an international sports-drug scandal that involves his clients and
a Burlingame laboratory.
Dwain Chambers, Great Britain's fastest man, said Korchemny sent him to Victor
Conte, the owner of the Bay Area Laboratory Co-Operative (BALCO), for
nutritional supplements last year. Now, Chambers said through his lawyer that he
tested positive for THG, the newly discovered designer steroid that the U.S.
Anti-Doping Agency (USADA) says came from BALCO.
Kelli White, the Union City champion sprinter who has worked with Korchemny
since her pre-teen years, tested positive for the stimulant modafinil during the
World Championships in Paris last August. Dr. Brian Goldman, once BALCO's
medical director, said he prescribed the drug for White to counter symptoms of
narcolepsy.
White is among the scores of top athletes subpoenaed to testify before a federal
grand jury in San Francisco that is investigating Conte and BALCO.
USADA said when it retested urine samples of athletes who competed in the June
U.S. Track and Field Championships at Stanford -- looking for THG -- it also
discovered several competitors who tested positive for modafinil.
Hurdler Chris Phillips, who coaches himself, reportedly told the International
Association of Athletics Federations after he tested positive for using
modafinil at the Stanford meet that he got the drug from Korchemny. The
Washington Post quoted the coach as saying he'd given Phillips one pill -- for
sleeping problems, not to make him run faster.
Olympic relay gold medalist and Stanford grad Chryste Gaines, another sprinter
coached by Korchemny, also tested positive for modafinil at Stanford. So did
Olympic gold-medal relay winner Calvin Harrison of Salinas, another Korchemny
client.
Korchemny denies giving any of his athletes a drug to enhance performance, but
colleagues in the world of track and field say his reputation is being tarnished
by the scandal.
Reputation will take hit
"He's going to be the collateral damage for this whole thing, that's for sure,"
said track coach Randy Huntington, who works at the U.S. Olympic Training Center
in Chula Vista (San Diego County). "I feel bad for Remi. He probably feels he
was doing something OK. The athletes will suffer from it and he'll suffer from
it."
Korchemny, standing alongside the track at James Logan High School in Union
City, where he volunteers to work with prep sprinters and hurdlers, agreed.
"Yes, it is going to affect my reputation as a coach," he said in an interview
with The Chronicle. "People think my success is not a result of my work, but a
stimulant. My success is a result of my hard work and knowledge."
It's knowledge gleaned from nearly a half-century of working with sprinters,
starting in his native Ukraine, where an early pupil was the schoolboy Valery
Borzov, who would win gold medals in the 100- and 200-meter dashes for the
Soviet Union at the 1972 Munich Olympics. All told, Korchemny has coached three
athletes who went on to win eight Olympic medals, including Gaines in 1996 and
2000 and Harrison in 2000.
Arrived in '75
Korchemny came to the United States in 1975, following brief stays in Israel and
Italy, after being allowed to leave the former Soviet Union. Having a Jewish
mother (who spent four years -- 1937-41 -- in a work camp) facilitated his
departure. His father, a suspected dissident, was executed by a Stalinist firing
squad in 1937 in a dockside labor dispute when Remi was 5.
"Too many stories," Korchemny said with a sigh. "The most important thing was to
get to the free world. The most difficult thing was to establish yourself in
another country, with a new culture."
Korchemny's interest in sprinting sprung from need. After his father was
executed and his mother sent to a work camp, young Remi went to live with
grandparents. With money and food in short supply, he took to racing boys at his
school for bread and sandwiches. Lose, and he'd have to carry the winner on his
shoulders in front of the school.
"I never lost," he said in a 2002 interview in American Track & Field magazine.
Eventually, Korchemny became a very good sprinter, running 100 meters in 10.4
seconds. He became an even better coach. Korchemny molded the early career of
fellow Ukrainian Borzov.
Borzov was regarded as a technically perfect sprinter, at least in part because
of the coaching he received as a teenager from Korchemny. Korchemny unfailingly
points out that he was not Borzov's personal coach when he won at Munich in
1972.
Korchemny "is one of the best," Huntington said. "He's taught many coaches in
this country a lot about sprint mechanics and hurdle mechanics. ... This is like
everyone's grandfather: gentle, sweet, caring. To see him go through this hurts
a lot of us."
BALCO link unclear
Korchemny's link to BALCO and Conte and the sports-doping scandal swirling
around them is not entirely clear, but the fact of the link is as evident as the
floppy hat the coach wore to shade the sun on a recent afternoon at James Logan
High.
Above the hat's brim are stitched the letters ZMA. It's a promotion for Conte's
signature product, a zinc magnesium supplement that athletes from the Giants'
Barry Bonds to Raiders linebacker Bill Romanowski swear by.
Korchemny remains a supporter of Conte and his nutritional supplement products,
despite the controversy. The coach and Conte reportedly formed the ZMA Track
Club several years ago, featuring clients of BALCO.
"It's just a company that makes the supplement, Korchemny said. "It (the track
club) doesn't exist as an organization. Somebody made it up. It's much easier to
call USA Track & Field (and ask) if they have registered ZMA as a club."
There was a ZMA Track Club registered with USA Track & Field in 2001, but it is
no longer in existence, according to that organization's records.
As for Conte, Korchemny said: "I still believe in what he's doing. I still
believe he provides excellent services for people. Not just good -- excellent. I
still use his product. I still recommend to people to use ZMA."
Korchemny says he learned of Conte "three or four years ago" from a professional
football player he was training. Though he would not say who the player was,
Korchemny did work with Romanowski when he was with the Denver Broncos.
Romanowski got some of his supplements from Conte at BALCO and recommended the
lab to other athletes.
Chambers, the champion sprinter from Great Britain who said Korchemny sent him
to BALCO, seemed to blame Conte after testing positive for the steroid THG.
"Dwain had never heard of this substance and he immediately challenged Mr. Conte
on this finding and was categorically assured that all the supplements he had
been given were within the rules of the International Association of Athletics
Federations (IAAF)," Chambers' British lawyer, Graham Shear, said. "In his eight
years in international athletics, he has never been tempted to succumb to
illegal methods of enhancing a performance."
Korchemny, who said he introduced Chambers to Conte last year, said his client
doesn't know where the THG in his system came from "and I don't know where it
came from."
Athletes caught using a steroid such as THG can be banned from competition for
two years. Use of modafinil, the stimulant for which some of Korchemny's other
clients tested positive, results in a public warning and disqualification from
the competition in which the athlete tested positive.
Korchemny told The Chronicle he never gave or recommended modafinil to an
athlete to make the athlete run faster.
'No scientific evidence'
"It doesn't improve their performance," he said. "There's no scientific evidence
or proof it improves performance. As a stimulant, it's very mild. It's not on
the list of prohibited substances. There's no evidence that this substance can
change athletic performance.
"They found it only affects your sleeping. When you travel a lot and don't have
a whole night's sleep and have to practice the next day, you feel sleepy. I
don't feel anyone did anything wrong with this substance."
Noting that two other stimulants, caffeine and over-the-counter cold medications
such as Sudafed, recently were removed from the list of banned substances,
Korchemny said, ruefully, "Better to have a cup of coffee than one modafinil."
Huntington and another coach, former Stanford head man Brooks Johnson, both said
Korchemny told them he gave his athletes modafinil to combat the effects of
plane travel.
"He told me he only gave it to the kids to beat jet lag," said Johnson, now
director of the U.S. Olympic Training Center. "It had nothing to do with
performance ..."
Skirting culpability
However, standing on Logan High's rubberized track in the meager shade of a
baking afternoon, Korchemny skirted the issue of culpability. "I did not make a
statement that I gave it to them," he said. "I don't know where it came from."
White, for one, said earlier the modafinil was prescribed to her by her doctor,
Goldman, of Walnut Creek, to counteract the effects of narcolepsy, which she
said runs in her family.
The modafinil findings have brought stress and accusations to Korchemny at an
age when he should be enjoying the tag end of his long career in coaching. He
has many supporters in the sport of track and field who said they don't want to
see the man's reputation tarnished by one act for which he might bear some
responsibility.
"He was a fantastic coach and the kids loved him," Johnson said of Korchemny's
time (1983-87) on his staff at Stanford. "He really earned their trust because
he was basically selfless. Remi was the most modest, non-ego-driven person of
any magnitude in the sport I've seen."
With accusations flying about him, Korchemny appears to seek pleasure, as well
as refuge, from the storm by volunteering as a coach at Logan High, not far from
his home in Castro Valley. One of his young charges, Logan junior Kevin
Craddock, is among the best prep hurdlers in the country and could develop into
an elite competitor one day.
"I enjoy my life," Korchemny said. "I enjoy working with kids. I enjoy passing
my knowledge to the younger generation. My nature is as a teacher. I love to
teach."
E-mail John Crumpacker at jcrumpacker@sfchronicle.com.
LOAD-DATE: November 4, 2003
LANGUAGE: ENGLISH
GRAPHIC: PHOTO (4), (1) These days, Remi Korchemny spends time as a volunteer
track coach at James Logan High in Union City. / Kurt Rogers / The Chronicle,
(2) Sprinters Kelli White (front) and Dwain Chambers both have connections with
Korchemny. / Darryl Bush / The Chronicle, (3) Athletes on the track team at
Logan High chat with Remi Korchemny (with hat), who is a volunteer coach at the
Union City school. / Kurt Rogers / The Chronicle, (4) Valery Borzov, a student
of Korchemny's, won the 100- and 200-meter dashes at the 1972 Olympics. /
Associated Press 1972
Copyright 2003 The Chronicle Publishing Co.
667 of 998 DOCUMENTS
Sunday Times (South Africa)
November 2, 2003
Dwain's coach takes heat as list of drugs cheats grows
BYLINE: DAVID MILLER
SECTION: Sport; Pg. 3
LENGTH: 593 words
Dwain's coach takes heat as list of drugs cheats grows
TOM KNIGHT and
THE focus in the escalating American doping scandal shifted to Dwain Chambers's
coach, Remi Korchemny, this week, as yet another of his athletes was reported to
have tested positive for a banned substance.
According to the Washington Post, American sprinter Chryste Gaines is the latest
athlete to have tested positive for modafinil, a stimulant.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Korchemny could become the first coach to face sanctions -
possibly a life ban - in a doping case.
It is understood modafinil was found in Gaines's urine sample at the US
Championships in June. The samples were recently retested when the US
Anti-Doping Agency uncovered the existence of a new, designer steroid called
tetrahydrogestrinone, or THG.
Gaines, 33, who won the 100m at the World Athletics Finals in Monte Carlo, would
be the fourth athlete connected to Korchemny to have failed a drugs test.
Chambers has tested positive for THG and Americans Kelli White, Chris Phillips
and Calvin Harrison for modafinil, a drug banned by the IAAF because it is
categorised as being related to the family of stimulants.
Phillips and Harrison said they were given modafinil by Korchemny. Phillips, who
along with White tested positive at the world championships, told the IAAF that
he was given the drug just before his 110m hurdles semifinal.
Gyulai said: "If what Phillips said is true, we will investigate, because it is
unacceptable for coaches to encourage athletes to take prohibited substances."
Robert Wagner, Phillips's agent, said: "Everybody is taking something to be
alert and awake. I've seen sprinters drink lots of coffee because it makes you
sharper."
Korchemny remained defiant. He said: "Modafinil is the same as aspirin or coffee
- big deal. It was not on the list of banned substances."
* Countries that fail to help fund the World Anti-Doping Agency (Wada) will not
have their national anthem played if they win gold at next year's Olympic Games
in Athens.
In addition, they will not be able to display their national flag at the opening
and closing ceremonies, and their officials will not be given accreditation to
attend any Olympic event or function. They will also lose out on funding for
coaches.
Wada are hoping the potential embarrassment of such sanctions will force into
line those governments which have yet to pay their subscription to the agency.
Dick Pound, chairman of Wada, is determined his organisation should be properly
funded in order to tackle the growing problem of drugs in sport.
"We are prepared to take the gloves off," warned Pound, who was in London this
week for an informal meeting with sports minister Richard Caborn.
However, the threat will alarm leading athletes, according to Stephanie Cook,
who won gold for Britain in the women's modern pentathlon at the 2000 Olympics
in Sydney.
"Watching the flag being raised and hearing the music is what it's all about,"
Cook said. "To not have that because your country has not contributed to
fighting the drugs problem would be like not recognising what you've achieved."
According to Pound, the main offenders are from Central/South America and Africa
- the latter including Senegal, the country of Lamine Diack, president of the
IAAF. Funding by governments is arranged on a continental basis - Europe 47.5%,
America 29%, Asia 20% and Africa 0.5%.
© The Telegraph, London
LOAD-DATE: November 5, 2003
LANGUAGE: ENGLISH
PUB-TYPE: Paper
Copyright 2003 Times Media Limited
668 of 998 DOCUMENTS
The Washington Times
November 2, 2003, Sunday, Final Edition
More athletes use anti-sleep drug
BYLINE: By Steve Nearman, THE WASHINGTON TIMES
SECTION: SPORTS; WEEKEND ATHLETE: RUNNING; Pg. C13
LENGTH: 761 words
Has track and field in America become so boring that even its athletes need to
take modafinil to keep from falling asleep during competition?
Just wait until they start busting track and field writers for taking the
stimulant.
Three U.S. athletes have tested positive for the eugeroic drug, which in medical
terms simply means "good arousal." More positive tests may follow.
The drug's revelation hit the track circuit shortly after the Track & Field
World Championships in Paris in late August.
World 100/200 double champ Kelli White was the first athlete exposed, saying she
took modafinil on prescription from her physician to combat narcolepsy. The
International Association of Athletics Federations charged her with a doping
offense.
True, modafinil, a k a provigil, is used to improve wakefulness in people with
excessive daytime sleepiness associated with narcolepsy.
But now we have two other U.S. athletes who competed at the worlds - Chris
Phillips who finished fifth in the 110-meter hurdles and Calvin Harrison who ran
the opening leg of the gold-medal 1,600-meter relay - who admitted they took
modafinil.
While modafinil was not on the banned substance list at the time of the world
championships, caffeine and amphetamines were. Just recently, caffeine was taken
off the list.
An interesting question came out of research conducted in 1991 by T.J. Lyons and
J. French for the U.S. Air Force School of Aerospace Human Systems Division at
Brooks Air Force Base in Texas:
"The development of modafinil brings to light a crucial social question. What
would be the impediment for its use, if a compound such as modafinil is more
like caffeine than amphetamine in terms of safety, and yet, as effective as the
amphetamines?"
Marine Corps magic - No performance in the 28-year history of the Marine Corps
Marathon was as dominating as Heather Hanscom's triumph this year.
The 25-year-old Alexandria resident's margin of victory last weekend was 20
minutes and 47 seconds over runner-up Lindsey Gannon. The next largest win,
including both the men's and women's 28 races, was approximately six minutes,
according to historian George Banker.
Only Olga Markova of Russia had a faster winning time for women at Marine Corps,
covering the 1990 course 59 ticks faster than Hanscom did a week ago.
Even more significant for Hanscom, in her marathon debut, is that she qualified
with an "A" standard for the U.S. Women's Olympic Trials in St. Louis on April
3. Her time has her ranked in the top 20 of nearly 125 American women to qualify
thus far for the trials.
That "A" standard - a time of 2:39:59 or faster - will get her travel expenses
to the trials paid by the race organizers. And this is just the beginning for
Hanscom.
The Marine Corps win launched Markova's career. She traveled from Russia as an
unknown, had lodging arranged with a couple living on Capitol Hill and went on
to triumphs at Boston in 1992 and 1993.
The Marine Corps Marathon also spring-boarded a career in the marathon for 1987
titlist Mary Robertson. The then-Richmond resident's 2:44 qualified her for the
1988 U.S. Women's Olympic marathon trials.
Today, she is Mary Wittenberg, executive vice president and chief operating
officer of the New York Road Runners Club, organizers of today's New York City
Marathon.
Olympic marathon trials fever - When the Chicago Marathon had a few last-minute
cancellations, a chunk of money was freed up. So organizers offered cash
incentives of $2,500 and $3,500 to each U.S. athlete running a "B" or an "A"
Olympic trials qualifying standard.
The marathon paid out $115,000 to 39 U.S. marathoners in its Oct. 12 event.
There were 21 men, including area runners Edmund Burke of Burtonsville and Nick
Gramsky of McLean, as well as 18 women. There goes your amateur status, boys.
Today for the first time at New York, organizers have hired U.S. marathon
record-holder Deena Kastor [formerly Drossin] to pace, for at least 25
kilometers, a group of approximately six American women to break the 2:40
Olympic trials "A" standard. Meanwhile, 2003 USA Marathon champion Sara Wells
will lead a large group of athletes toward the 2:48 "B" standard.
+++++
EVENTS
* Ivymount School 5K Race for Excellence - Today, 8 a.m., Potomac, Md.
Information: 301/871-0400.
* Halloween Young Run - Today, 9 a.m., Rockville. Ages 12-and-under run
quarter-, half- or full mile. Information: 301/353-0200.
* United We Stand 5K - Saturday, 1 p.m., Bon Air Park, Arlington.
LOAD-DATE: November 3, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Washington Times LLC
All Rights Reserved
669 of 998 DOCUMENTS
Contra Costa Times
October 31, 2003 Friday FINAL EDITION
ATHLETES WARY OF GROCERY LIST OF BANNED DRUGS;
OVERSIGHTS OCCUR FROM THE VOLUMINOUS EDUCATIONAL INFORMATION AVAILABLE
BYLINE: ANN TATKO, TIMES STAFF WRITER
SECTION: SPORTS; Pg. B06
LENGTH: 697 words
Three years ago, a simple case of bronchitis wasn't so simple for Cal grad Jason
Han.
As a member of the U.S. Taekwondo team, Han hesitated before taking an
antibiotic prescribed by his doctor. Antibiotics were listed as acceptable
medication under the International Olympic Committee's guidelines for prohibited
substances, but Han decided to check with a national team trainer, just to be
safe.
This cautious approach is how most aspiring Olympic athletes live because of the
IOC's lengthy list of performance-enhancing drugs and costly ramifications of
taking one, even accidentally.
Recently, five track and field athletes tested positive for a previously
undetected designer steroid, tetrahydrogestrinone, also known as THG. Three of
them have denied knowingly taking any banned substance.
In a separate case, six track athletes reportedly tested positive for modafinil,
a stimulant used to treat sleep disorders. Those athletes include former El
Sobrante resident Kelli White and ex-Stanford star Chryste Gaines.
White said she didn't know modafinil was a banned substance when her doctor
prescribed it for narcolepsy, a sleep disorder that runs in her family. At the
time, modafinil was included on the IOC list as a "related substance," making it
a prohibited mild stimulant.
She failed a drug test at the world track and field championships in August and
may lose the gold medals she won in the 100- and 200-meter races.
"I've never taken any performance enhancing drugs and I certainly didn't believe
I was taking one (at worlds)," she said. "I was on the medicine all summer and
never tested positive once."
Ignorance rarely passes as a defense when athletes fail drug tests these days
because educational information is so readily available, said Terry Madden,
chief executive officer of the U.S. Anti-Doping Agency.
In the United States, Madden's agency handles dispersing such information and
drug testing athletes from the country's 39 Olympic sport organizations. USADA
provides athletes with a 37-page guidebook listing more than 100 banned generic
stimulants and anabolic agents. It also operates a toll-free drug reference
phone line to answer athletes' questions.
But having information doesn't make it necessarily easy to assimilate.
"Generic drugs go by so many different (pharmaceutical) names; you may think
it's safe to take a medicine that's actually prohibited," Han said. "That's why
I always double check. I don't want to jeopardize my career because of an
oversight."
Oversights could occur easily considering the amount of information athletes are
expected to know.
USADA provides "wallet cards," via its Web site, that list a condensed version
of some allowed medications and prohibited substances. The cards completely fill
two letter-size pages with small type, and even then, not all drugs are
included.
Also, some permissible medications include warnings that they are allowed only
in certain forms, such as decongestants only in nasal sprays, or that some may
contain prohibited substances, such as in certain cold medicines.
"It's like reading through a warranty for something you buy - a lot of
mind-numbing fine print," said skier Daron Rahlves, a native of Clayton and
former world champion. "But you have to do it, because even one inadvertent
slip-up could cost you everything."
Rahlves witnessed just such an example at the 2002 Olympics in Salt Lake City,
where Great Britain's Alain Baxter won his country's first Olympic alpine skiing
medal with a bronze in slalom. He later lost that medal when he tested positive
for methamphetamine because of a Vicks inhaler he used.
In some cases, perhaps even White's, an athlete could avoid failing a drug test
by seeking permission to take a banned prescription medication. If an athlete
needs it because of a diagnosed condition, he can fill out a medical
notification form and wait for approval from USADA.
"Filling out paperwork and drug testing may be inconvenient, but it's how the
system works," said biathlete Rachel Steer, a USADA athlete ambassador.
"Everyone wants fair competition, and this is the best system we have to
accomplish that."
LOAD-DATE: November 10, 2005
LANGUAGE: ENGLISH
Copyright 2003 Contra Costa Times
All Rights Reserved
670 of 998 DOCUMENTS
THE DAILY TELEGRAPH(LONDON)
October 31, 2003, Friday
US gold still under threat
BYLINE: By Scott Purchase
SECTION: Pg. 06
LENGTH: 410 words
THE United States could lose the 4 x 400 metre relay gold medal from this
summer's World Championships due to a second drug violation by Calvin Harrison,
the sport's top anti-doping official said yesterday.
Harrison confirmed last week that he tested positive for the stimulant modafinil
at the United States track championships at Stanford in June.
Under international rules the penalty for stimulants is a public warning and
disqualification from the event where the test took place, but no ban.
The International Association of Athletics Federations had said that, despite
the positive test in June, Harrison remained eligible for the World
Championships in Paris in August, but Arne Ljungqvist, head of the IAAF medical
commission, pointed to an earlier offence.
Ljungqvist confirmed that Harrison tested positive for the stimulant
pseudoephedrine at the 1993 US junior indoor championships and served a
three-month suspension.
This second offence at Stanford in June should have attracted a two-year ban,
and Harrison should not have been eligible for the World Championships,
according to Ljungqvist. The athlete could be retroactively disqualified.
Harrison, who finished sixth in the individual 400 metres, ran the opening leg
in the relay final in Paris. The other runners were Tyree Washington, Derrick
Brew and Jerome Young. It was Young who failed a doping test in 1999.
Ljungqvist said Harrison's case must first be investigated by the US Anti-Doping
Agency. USADA have not announced the names of athletes who tested positive for
modafinil or the designer steroid THG, pending the analysis of backup 'B'
samples.
Under IAAF rules the American relay team face being stripped of the gold medal
if Harrison is found guilty of the second doping offence by USADA and the ruling
is upheld through appeal.
Ljungqvist said: "That is our interpretation, but it will be a matter for the
legal people to debate. It's a little tricky because he was properly entered. At
the time it was not know he was had an earlier test for modafinil."
If the United States team lose the relay medal, the French team - anchored by
Marc Raquil - would move up to the gold.
USADA retested urine samples from the US championships after the UCLA doping
control laboratory devised a test for previously undetectable THG.
Six Americans have been identified as testing positive for modafinil, which is
prescribed for narcolepsy.
[PS]Sport: [ES]
Yachting:
LOAD-DATE: October 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Telegraph Group Limited
671 of 998 DOCUMENTS
The Age (Melbourne, Australia)
October 30, 2003 Thursday
Late Edition
Pittman rival tests positive
BYLINE: Jacquelin Magnay, Len Johnson
SECTION: SPORT; Pg. 16
LENGTH: 445 words
One of Jana Pittman's main rivals in the 400 metres hurdles, American champion
Sandra Glover, has tested positive to the banned stimulant modafinil.
The 34-year-old athlete, who calls herself the "grandma" of the track, was named
by the Los Angeles Times as testing positive to the drug during re-testing of
the US Track and Field trial samples for the steroid THG.
Glover is the latest big name athlete to have been caught in the biggest drugs
scandal since Ben Johnson was stripped of his 100 metres gold medal in 1988.
Her fast finishing burst at the Paris world championships in August snared her
the silver medal to relegate the world-record holder Yuliya Pechonkina into
third place, as Sydneysider Pittman triumphed.
In the last event of the season, the world grand prix final, Glover won the 400
metres hurdles in the absence of Pittman and Pechonkina.
Glover is likely to face the loss of her US trial title but she will be able to
keep the world championships silver medal under IAAF rules. But the humiliation
will not sit easily with Glover, a primary school teacher, and she might retire.
Sprinters Chryste Gaines and Kelli White, another 400 metres hurdler Eric
Thomas, 400 runner Calvin Harrison and 110 hurdler Chris Phillips have already
tested positive to modafinil.
Doctors say modafinil is taken to regulate sleeping patterns but bodybuilders
believe it also promotes the production of growth hormone in the body.
World governing body, the IAAF, has said it will punish any coaches directly
connected to the spate of positive tests for modafinil.
Meanwhile, a key element of the defence mounted by the coach and the nutritional
supplement company linked to the designer steroid scandal has been knocked out
with the declaration by the US Food and Drug Administration that the drug
involved is potentially harmful and not a nutritional supplement.
A statement in Washington said the FDA had completed an analysis of THG and
determined it is "an unapproved new drug," which makes its use for any reason
illegal in the US.
"Rather, it is a purely synthetic `designer' steroid derived by simple chemical
modification from another anabolic steroid that is explicitly banned by the US
Anti-Doping Agency," the statement said.
THG is also a banned substance in Australia. The Therapeutic Goods
Administration said yesterday it fell under the Schedule Eight, Customs
(Prohibited Imports) regulations entry for "anabolic or androgenic substances".
It appears unlikely that any Australian-based athlete will be found to have used
THG. The Customs Department has confirmed that there has been no commercial
importation of Balco products into Australia in the past five years.
LOAD-DATE: June 18, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Age Company Limited
All Rights Reserved
672 of 998 DOCUMENTS
Associated Press Worldstream
October 30, 2003 Thursday
Harrison had previous doping offense; US could lose world relay gold
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 687 words
DATELINE: LONDON
The United States could lose its 1,600-meter relay gold medal from this summer's
World Championships due to a second drug violation by Calvin Harrison, the
sport's top anti-doping official said Thursday.
Harrison confirmed last week that he tested positive for the stimulant modafinil
at the U.S. track championships at Stanford in June.
Under international rules, the penalty for stimulants is a public warning and
disqualification from the event where the test took place - but no ban.
The International Association of Athletics Federations had said that, despite
the positive test in June, Harrison remained eligible for the World
Championships in Paris in August.
But IAAF medical commission chief Arne Ljungqvist told The Associated Press on
Thursday that he has since confirmed that Harrison tested positive for the
stimulant pseudoephedrine at the 1993 U.S. junior indoor championships and
served a three-month suspension.
Jill Geer, spokeswoman of USA Track & Field, confirmed the 1993 positive.
"This would be a second offense," Ljungqvist said in a phone interview. "The
second offense for a mild stimulant would be a two-year ban."
In that case, Harrison should not have been eligible for the world meet and he
could be retroactively disqualified, Ljungqvist said.
Harrison ran the opening leg in the relay final in Paris. The other runners were
Tyree Washington, Derrick Brew and Jerome Young, who is engulfed in controversy
over a failed doping test in 1999.
Harrison also finished sixth in the individual 400-meter final in Paris.
Ljungqvist said Harrison's case must first be investigated by the U.S.
Anti-Doping Agency. USADA has not announced the names of athletes who tested
positive for modafinil or the designer steroid THG, pending the analysis of
backup B samples.
Under IAAF rules, the U.S. relay team faces being stripped of the gold medal if
Harrison is found guilty of the second doping offense by USADA and the ruling is
upheld through the appeals process.
"That is our interpretation but it will be a matter for the legal people to
debate," Ljungqvist said. "It's a little tricky because he was properly entered.
At the time it was not know he was had an earlier test for modafinil."
If the U.S. team loses the relay medal, the French team - anchored by Marc
Raquil - would move up to the gold.
USADA retested urine samples from the U.S. championships after the UCLA doping
control laboratory devised a test for previously undetectable THG.
Six Americans have been identified as testing positive for modafinil, which is
prescribed for treatment of the sleeping disorder narcolepsy.
Harrison and Young were both members of the winning U.S. 1,600 relay squad at
the 2000 Sydney Olympics. The team was anchored by Michael Johnson.
Young tested positive for the steroid nandrolone in 1999, but was exonerated on
appeal by USA Track & Field officials.
The IOC and IAAF are investigating whether Young was improperly cleared and
should have been ineligible for the Olympics. The probe could lead to the team
being stripped of the gold.
Young, who won golds in the 400 meters and 1,600 relay at the Paris
championships, said he never committed a doping offense.
In a column in Thursday's Daily Telegraph, Johnson said he can't see how he
could lose one of his five Olympic gold medals because of the positive tests of
Young and Harrison.
"The only way the medals could be taken away now, since neither athlete tested
positive during the games, is if one of them were to admit having taken
performance enhancing drugs during the games," he said.
"Personally I don't like the rules and think they should be changed. But as they
stand now I don't think Young should be targeted, and his medals threatened, for
a positive test four years ago for which he was exonerated."
World Anti-Doping Agency chairman Dick Pound scoffed at Johnson's position.
"He's trying to keep his medal," he told the AP. "There was clearly a very goofy
internal process ... The worst thing is USA Track & Field knew it and still put
(Young) in the event and put Michael Johnson at risk as well."
LOAD-DATE: October 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
673 of 998 DOCUMENTS
The Daily Telegraph (Sydney, Australia)
October 30, 2003 Thursday
Athletes' mentors to face punishment
SOURCE: MATP
BYLINE: STEPHEN WILSON
SECTION: SPORT; Pg. 61
LENGTH: 323 words
THE International Association of Athletics Federation plans to punish any
coaches directly connected to the spate of positive tests among US athletes for
the stimulant modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Some were coached by Ukrainian-born coach Remi Korchemny, who is based in the
San Francisco area.
IAAF general secretary Istvan Gyulai said yesterday that coaches involved in
drug cases should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offence
themselves," he said.
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more US athletes were cited in newspaper reports yesterday for positive
modafinil tests.
The Washington Post reported that 1996 Olympic 4x100m gold medallist Chryste
Gaines tested positive at the US championships in Stanford in July.
The Los Angeles Times also cited Gaines along with hurdlers Sandra Glover and
Eric Thomas.
Glover is a four-time US 400m hurdles champion and won silver at the World
Championships in Paris in August. Thomas is the US men's 400m hurdles champion.
Olympic and world relay gold medallist Calvin Harrison had already confirmed he
has tested positive for modafinil, while Kelli White -- who won gold in both
100m and 200m in Paris -- and hurdler Chris Phillips tested positive at the
world championships.
White could be stripped of her medals.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified it as a "minor
stimulant".
It has now been placed by name on the World Anti-Doping Agency's banned list.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: DTM
Copyright 2003 Nationwide News Pty Limited
674 of 998 DOCUMENTS
Sydney Morning Herald (Australia)
October 30, 2003 Thursday
Late Edition
Pittman rival shows positive to vogue drug in mass retesting of US track team;
ATHLETICS
BYLINE: Jacquelin Magnay, AP for the last two paragraphs only.
SECTION: SPORT; Pg. 38
LENGTH: 607 words
One of Jana Pittman's key rivals in the 400-metre hurdles, the American champion
Sandra Glover , has tested positive to the banned stimulant modafinil .
The 34-year-old, who calls herself the "grandma" of the track, was named by the
Los Angeles Times as having tested positive during mass retesting of the US
track-and-field trial drug samples for the other vogue steroid drug
tetrahydrogestrinone (THG).
The religious Glover is the latest big-name athlete to have been caught in the
biggest drugs scandal since Ben Johnson in 1988.
Her fast-finishing burst at the Paris world championships in August snared her
the silver medal to relegate world-record-holder Yuliya Pechonkina to third
place, as Sydneysider Pittman triumphed.
And in the last event of the season, the world grand prix final, Glover won the
400m hurdles as Pittman partied and Pechonkina was sick with bronchitis.
Glover is likely to face the loss of her US trial title but she will be able to
keep the world championships silver medal because under current IAAF rules the
modafinil sanction involves the stripping of results from the competition in
which the stimulant was found, as well as a public warning.
But the humiliation will not sit easily with Glover, a primary school teacher.
She may elect to retire.
Glover's US colleague Kelli White is battling to keep her two sprint gold medals
from the world championships because she tested positive to modafinil at that
Paris competition.
Those caught taking modafinil now include sprinter Chryste Gaines , another 400m
hurdler Eric Thomas , 400m runner Calvin Harrison , 110m hurdler Chris Phillips
, Glover and White.
Doctors say modafinil is taken to regulate sleeping patterns but bodybuilders
believe it also promotes the production of growth hormone in the body.
Meanwhile, the US Food and Drug Administration yesterday banned the sale and use
of THG, to which British sprinter Dwain Chambers ; hammer-thrower John McEwen;
shot-putter Kevin Toth ; distance-runner Regina Jacobs and another unnamed US
athlete have
tested positive in the past fortnight after retesting of stored urine samples.
The drug administration ruled the drug was not a dietary supplement, but a
synthetic designer steroid and warned its use may pose considerable risk to
health.
The administration's associate commissioner, John Taylor, told US Congress that
THG was derived from gestrinone . Gestrinone is often used in Europe to treat
endometriosis, an extremely painful condition where part of the womb grows into
the abdomen.
Taylor also said THG was chemically linked to the veterinary steroid trenbolone
, which is favoured by US cattle ranchers to beef up the size of their cows.
The classification of THG as a controlled substance similar to that of morphine,
runs contrary to the claims by the man accused of supplying THG to athletes,
BALCO president Victor Conte , that it was a dietary supplement.
Conte is facing a US grand jury over tax fraud and dozens of his clients,
including high-profile athlete Marion Jones and baseballers Barry Bonds and
Jason Giambi have been subpoenaed to appear.
In a news release, the administration said it was working with other federal law
enforcement agencies to aggressively engage, enforce, and prosecute those firms
or individuals who manufacture, distribute or market THG.
* Phoenix: Olympic sprint champion Gail Devers , 37, will return to competition
next season hoping to show young athletes and fans there can be success without
performance-enhancing drugs, AP reports.
In a telephone interview from Japan, Devers said she was motivated to come back
by the recent controversy over the designer steroid THG.
LOAD-DATE: July 17, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 John Fairfax Publications Pty Ltd
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The Times (London)
October 30, 2003, Thursday
White's case strengthened by claims of drugs company
BYLINE: Peter Nichols
SECTION: Sport; 50
LENGTH: 394 words
KELLI WHITE, who tested positive for the stimulant modafinil at the World
Championships in August, has been given hope in her battle to retain the 100 and
200 metres titles that she won in Paris. Speaking to The Times, Dr Paul Blake, a
senior vice-president of Cephalon, the company that manufactures the drug, has
cast serious doubt on the claims of the IAAF that it could be regarded as a
banned substance at the time of the World Championships.
Modafinil was not identified by name on the list of banned stimulants and the
disqualification of White hinges on the fact that the drug falls into the
catch-all category of "chemically and pharmacologically related compounds".
However, Blake insists that modafinil is not related to the stimulants on the
list. "It is clearly a very different chemical, having a different
pharmacological structure. It is a separate pharmacological entity," he said.
Modafinil was developed more than 20 years ago in France at Lafon Laboratories,
a company that is now part of the Cephalon group. Company literature describes
modafinil as a "wake promoter" rather than a stimulant and states that the drug
belongs to its own class, which it has called Eugeroics, of which there is just
one other related drug, also manufactured by Cephalon.
The Food and Drug Administration first ratified modafinil's limited use in the
United States in 1998 and recently a more extended approval has been given for
the drug, which is generally used to treat sleeping disorders.
Blake expressed surprise that, when the positive test for the drug surfaced in
Paris, the IAAF did not contact the company immediately. "We eventually
contacted WADA (the World Anti-Doping Agency) after it had gone on their lists
and asked if we could present a submission," Blake said. That review of the
status of the drug has yet to take place, but Blake's comments will provide
ammunition for White, whose hearing is expected soon, although the US
Anti-Doping Agency (USADA) would not give a date.
If the USADA cannot classify modafinil in the "related compounds" grouping and
it will be all too aware of the threat of legal action if there are any doubts -
then White would keep both the 100 metres and 200 metres titles that she won in
Paris and also collect $ 120,000 (about £70,000) in prize-money that has so far
been withheld.
LOAD-DATE: October 30, 2003
LANGUAGE: ENGLISH
Copyright 2003 Times Newspapers Limited
676 of 998 DOCUMENTS
USA TODAY
October 30, 2003, Thursday, FINAL EDITION
Athletes reported with positive tests
SECTION: SPORTS; Pg. 16C
LENGTH: 129 words
There have been a rash of positive drug tests recently for the previously
undetectable steroid THG and the stimulant modafinil. Athletes are entitled to
appeals. The THG penalty is a two-year ban from competition. Modafinil carries a
penalty of disqualification for the meet in which the athlete was tested but no
further competition ban. Athletes identified as testing positive:
THG
1. Regina Jacobs, USA, middle-distance runner
2. Kevin Toth, USA, shot put
3. John McEwen, USA, hammer thrower
4. Dwain Chambers, Britain, sprinter
Modafinil
1. Kelli White, USA, sprinter
2. Chris Phillips, USA, hurdler
3. Calvin Harrison, USA, sprinter
4. Sandra Glover, USA, hurdler
5. Eric Thomas, USA, hurdler
6. Chryste Gaines, USA, sprinter
LOAD-DATE: October 30, 2003
LANGUAGE: ENGLISH
Copyright 2003 Gannett Company, Inc.
677 of 998 DOCUMENTS
The Advertiser
October 29, 2003 Wednesday
IAAF wakes up to drug pattern
BYLINE: By STEPHEN WILSON in London
SECTION: SPORT; Pg. 102
LENGTH: 324 words
TWO drugs under scrutiny in sports - modafinil and THG - are part of a pattern
of doping abuse in the United States, according to Arne Ljungqvist, the IAAF's
medical commission chief.
Evidence suggests a link between Modafinil - the drug sprinter Kelli White says
she took for a sleep disorder - and Tetrahydrogestrinone, or THG, a previously
undetectable designer steroid that has turned up in the samples of several track
and field athletes.
"What emerges now is a pattern," Ljungqvist said.
"People have taken THG for obvious reasons - it's been designed with the intent
not to be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them." The Washington Post, citing unidentified
international sources with knowledge of the results, reported on its Web site
Monday night that American sprinter Chryste Gaines tested positive for modafinil
at the US track and field championships in July. Calvin Harrison, an Olympic and
world relay gold medallist, also tested positive for the stimulant this past
summer, a source close to a US doping investigation said.
Harrison, still awaiting the result of his backup B sample, was tested at the US
national championships in June at Stanford, California. Modafinil first came to
prominence in August when White tested positive for the drug at the world
championships in Paris. She stands to be stripped of her 100m and 200m titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offence and submitted her case to U.S. authorities for
disciplinary action.
Referring to White's narcolepsy defence, Ljungqvist said: "It comes into a
different sort of light when it becomes known that modafinil has been taken by a
number of athletes."
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: ADV
Copyright 2003 Nationwide News Pty Limited
678 of 998 DOCUMENTS
DAILY MAIL (London)
October 29, 2003
Narcolepsy drug used by seven, say IAAF
BYLINE: NEIL WILSON
SECTION: ED_2ND; Pg. 77
LENGTH: 301 words
SEVEN athletes have recently tested positive for the new stimulant modafinil,
the head of the International Association of Athletics Federations, Istvan
Gyulai, revealed yesterday. 'We have been informed about the number, it's a
maximum of seven, but I can't name them,' he said.
Modafinil, normally used to treat narcolepsy, does not appear on the IAAF's
banned list but is closely related to other drugs that do.
One of the seven is the US sprinter Chryste Gaines, 33, the Washington Post
claimed yesterday. Gaines is coached by Remi Korchemny, the Ukrainian who also
numbers Kelli White, winner of the 100m and 200m titles at this year's World
Championships, and Britain's 100metres European champion Dwain Chambers in his
stable of athletes. Chambers tested positive for the designer steroid THG in
August, while White stands to lose her sprint titles after also showing positive
for modafinil in the summer.
Meanwhile, one of the athletes subpoenaed to testify before the U.S.
federal grand jury investigating the California laboratory BALCO, which
allegedly manufactured THG, is suing the American scientist who unmasked it.
Tammy Thomas, a former world track cycling record holder before she was banned
for life last year, has accused Dr Don Catlin and his Los Angeles university
laboratory of unethical conduct in identifying her in its published research, a
federal offence. What makes Thomas of interest to prosecutors may be Catlin's
claim that the steroid he caught her using on two occasions, norbolethone, could
have come from an illicit laboratory, possibly BALCO. Yesterday, the US Food and
Drug Administration declared THG illegal.
It is not a dietary supplement, they say, but a designeer steroid which could
have serious effects on longterm health.
END
LOAD-DATE: October 30, 2003
LANGUAGE: English
PUB-TYPE: Paper
Copyright 2003 Associated Newspapers Ltd.
679 of 998 DOCUMENTS
THE DAILY TELEGRAPH(LONDON)
October 29, 2003, Wednesday
Chambers coach in new link
BYLINE: By Tom Knight
SECTION: Pg. 05
LENGTH: 325 words
THE focus in the escalating American doping scandal shifted to Dwain Chambers's
coach, Remi Korchemny, yesterday, as yet another of his athletes was reported to
have tested positive for a banned substance.
According to the Washington Post the American sprinter Chryste Gaines is the
latest athlete to have tested positive for the stimulant, modafinil.
Istvan Gyulai, general- secretary of the International Association of Athletics
Federations, said Korchemny could become the first coach to face sanctions -
possibly a life ban - in a doping case.
It is understood modafinil was found in the urine sample provided by Gaines at
the US Championships in June. The samples collected at those championships were
recently re-tested when the US Anti-Doping Agency uncovered the existence of a
new, designer steroid called tetrahydrogestrinone, or THG.
Gaines, 33, who enjoyed a late run of form during the season to win the 100
metres at the World Athletics Finals in Monte Carlo, would be the fourth athlete
connected to Korchemny to have failed a drugs test.
Chambers has tested positive for THG and the Americans Kelli White, Chris
Phillips and Calvin Harrison for modafinil, a drug banned by the IAAF because it
is categorised as being related to the family of stimulants.
Phillips and Harrison said they were given modafinil by Korchemny. Phillips, who
along with White tested positive at the World Championships, told the IAAF that
he was given the drug just before his 110m hurdles semi-final.
Korchemny remained defiant. He said: "Modafinil is the same as aspirin or coffee
- big deal. It was not on the list of banned substances."
In a later development, the Los Angeles Times reported that two other American
athletes had tested positive for modafinil - Sandra Glover, a four-time US
champion in the 400m hurdles and runner-up in August at the World Championships
in Paris, and Eric Thomas, the reigning US 400m hurdles champion.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Telegraph Group Limited
680 of 998 DOCUMENTS
Edmonton Journal (Alberta)
October 29, 2003 Wednesday Final Edition
IAAF threatens to nab drug-pushing coaches
SOURCE: The Associated Press
SECTION: Sports; Pg. D4 /
LENGTH: 422 words
DATELINE: LONDON
LONDON - Track and field's world governing body plans to punish any coaches
directly connected to the spate of positive tests among U.S. athletes for the
stimulant modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Tuesday that any coaches or trainers involved in the use of
modafinil should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offence
themselves," he said. "This has to be investigated. We cannot just turn a blind
eye to this."
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more U.S. athletes were cited in newspaper reports Tuesday for positive
modafinil tests.
The Washington Post reported that sprinter Chryste Gaines -- a relay gold
medallist at the 1996 Olympics --tested positive at the U.S. championships in
Stanford, Calif., in July.
The Los Angeles Times said hurdlers Sandra Glover and Eric Thomas also tested
positive for the drug.
Calvin Harrison, an Olympic and world relay gold medallist, had previously
confirmed he tested positive for modafinil at the U.S. meet.
Sprinter Kelli White and hurdler Chris Phillips tested positive at the World
Championships. White, who said she took modafinil for narcolepsy, risks losing
her gold medals from the 100 and 200 metres.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified as a "minor
stimulant."
Gyulai stressed that modafinil should not be viewed in the same light as the
designer steroid THG, which has turned up in the samples of several track and
field athletes. The sanction for steroids is a two-year ban.
"THG was invented, produced and masterminded to cheat," Gyulai said. "There is a
major difference with modafinil. The athletes may have thought this is not
forbidden. They should have checked more carefully."
DEVERS RETURNS
- Olympic champion sprinter Gail Devers will return to competition next season,
hoping to show young athletes and track fans that there can be success without
performance-enhancing drugs.
- Devers says she was motivated to come back by the recent controversy over THG.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
681 of 998 DOCUMENTS
The Guardian - Final Edition
October 29, 2003
Football: Chambers coach under scrutiny
BYLINE: Vivek Chaudhary
SECTION: Guardian Sport Pages, Pg. 34
LENGTH: 678 words
Track and field's world governing body, the International Association of
Athletics Federations (IAAF), yesterday announced plans to punish any coaches
directly connected to the spate of positive tests among US athletes for the
stimulant modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, the IAAF's general secretary, said that any coaches or trainers
involved in the use of modafinil would face sanctions. iIf it is proved that
they incite or promote the use of drugs or substances which are not permitted,
they are considered to have committed a doping offence themselves,i he said.
The announcement came on the day that the American sprinter Chryste Gaines
became the fourth athlete trained by the Ukrainian-borncoach Remi Korchemny to
test positive for banned drugs.
The IAAF confirmed that Gaines had tested positive for modafinil and that it
would launch an investigation into the links between Korchemny, who also coaches
Britain's Dwain Chambers, and the positive drugs tests of some of his athletes.
Gaines, 33, was a
member of the victorious women's 4x100 metres relay team in the 1996 Atlanta
Olympics.
Gaines, her fellow sprinter Kelli White and the hurdler Chris Phillips, who all
train with Korchemny, have all tested positive for modafinil.
Chambers has tested positive for the designer steroid tetrahydrogestrinone
(THG).
Gyulai revealed that up to seven athletes had tested positive for modafinil. iOf
course modafinil is a concern for us. We have been informed about the number (of
positive tests). It's a maximum of seven but I can't name them.i
He said that the links between the athletes and Korchemny was a matter of
concern.
iIf it's proven that this coach was offering anything that is not a permissible
substance to athletes, that is the biggest concern to the IAAF.i
White, Gaines and Chambers train frequently with Korchemny in the San Francisco
area. Phillips coaches himself, but he told the IAAF
that Korchemny gave him a modafinil pill before the 110 metres hurdles
semi-finals in the world championships in Paris because he was having trouble
sleeping.
Korchemny told the Washington Post yesterday that he gave Phillips the modafinil
to help him sleep and not to improve his performance. He denied giving modafinil
to Gaines and said that he did not know how she had tested positive.
Modafinil, which is marketed under the name Provigil, was not officially banned
until after the world championships in August but drug-testingofficials said
that it qualified as a banned substance because of a broad clause in the
antidoping rules prohibiting substances closely related to banned drugs.
Referring to the White and Phillips cases, Korchemny said: iI had in my package
one pill because Kelli took only one pill. I'm sorry I did it . . . but it was
not prohibited (under anti-doping rules) . . . I was
100% sure everything was legal.i
Commenting on Gaines's positive test, he said: iI don't know anything about her
case. She is my student, but I don't know anything about her. I didn't give her
modafinil.i
White's agent Robert Wagner, who also represents Phillips, claimed that there
was a grey area in the use of modafinil that had left manyathletes confused.
Wagner said: iAthletes travel a lot; they come from different time zones. They
can't just drink five or six cups of coffee so they need to find something
similar that's not on the banned list. Modafinil was not on the banned list; it
is still not on the banned list.i
After the positive test of Chambers' A sample, his lawyer Graham Shear claimed
that Korchemny made all the arrangements for his nutritional supplements and
that he had no idea he was taking a
banned steroid when he consumed THG.
Three Americans, the middle-distance runner Regina Jacobs, the US shot put
champion Kevin Toth and the hammer thrower John McEwan, have also tested
positive for THG this year.
LOAD-DATE: October 30, 2003
LANGUAGE: ENGLISH
Copyright 2003 Guardian Newspapers Limited
682 of 998 DOCUMENTS
The Guardian - Final Edition
October 29, 2003
Football: Drugs coaches to face charges
BYLINE: Vivek Chaudhary
SECTION: Guardian Sport Pages, Pg. 34
LENGTH: 420 words
The International Association of Athletics Federations (IAAF) yesterday
announced plans to punish any coaches directly connected to the spate of
positive tests among US athletes for the stimulant modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, the IAAF's general secretary, said that any coaches or trainers
involved in the use of modafinil would face sanctions. "If it is proved that
they incite or promote the use of drugs or substances which are not permitted,
they are considered to have committed a doping offence themselves," he said.
The announcement came on the day that the American sprinter Chryste Gaines
became the fourth athlete trained by the Ukrainian-born coach Remi Korchemny to
test positive for banned drugs.
The IAAF confirmed that Gaines, 33, had tested positive for modafinil and that
it would launch an investigation into the links between Korchemny, who also
coaches Britain's Dwain Chambers, and the positive tests of some of his
athletes.
Gaines, her fellow sprinter Kelli White and the hurdler Chris Phillips, who all
train with Korchemny, have all tested positive for modafinil. Chambers has
tested positive for the designer steroid tetrahydrogestrinone (THG).
Gyulai said: "We have been informed about the number (of positive tests for
madafinil). It's a maximum of seven but I can't name them."
White, Gaines and Chambers train with Korchemny in the San Francisco area.
Phillips coaches himself, but he told the IAAF that Korchemny gave him a
modafinil pill before the 110 metres hurdles semi- finals in the world
championships in Paris because he was having trouble sleeping.
Korchemny denied giving modafinil to Gaines and said that he did not know how
she had tested positive. "She is my student, but I don't know anything about
her. I didn't give her modafinil." Referring to the White and Phillips cases, he
said: "I had in my package one pill because Kelli took only one pill. I'm sorry
I did it . . . but it was not prohibited (under anti-doping rules) . . . I was
100% sure everything was legal."
White's agent Robert Wagner, who also represents Phillips, said: "Athletes
travel a lot; they come from different time zones. They can't just drink five or
six cups of coffee so they need to find something similar that's not on the
banned list. Modafinil was not on the banned list; it is still not on the banned
list."
LOAD-DATE: October 30, 2003
LANGUAGE: ENGLISH
Copyright 2003 Guardian Newspapers Limited
683 of 998 DOCUMENTS
The Herald (Glasgow)
October 29, 2003
Fresh scare for Chambers;Steroid 'a health risk' warns US food and drug
administration
BYLINE: Doug Gillon
SECTION: Pg. 32
LENGTH: 494 words
THE American Food and Drug Administration yesterday said that users of an
anabolic steroid specifically designed to evade detection face a health risk.
This is a new concern for the British sprinter Dwain Chambers, who faces a ban
despite claims that he took the drug unwittingly.
Since development of a test for the previously undetectable substance,
competitors are running scared as their stored urine samples await re
-examination.
The US authority has classified tetrahydrogestrinone (THG) as an illegal drug,
and not a dietary supplement. As such it poses serious health risks to users,
said the FDA associate commissioner John Taylor.
He said THG would require clearance to be sold in the US. Consequently its use
there is illegal. Side effects of steroid-use include tumours, liver damage,
heart disease, anxiety and rage.
Little is known about the specific effects of THG, as it is so new, but Taylor
added that it is likely to pose similar risks.
The European 100 metres champion, Chambers, the world No.1 shot-putter Kevin
Toth, the world indoor 1500m record-holder Regina Jacobs, and the US hammer No.2
John McEwan have been named as having tested positive for THG.
The world athletics body expect more to be identified. Their general secretary,
Istvan Gyulai, confirmed yesterday that up to seven athletes have tested
positive for the stimulant Modafinil, but declined to name them. However a US
newspaper yesterday identified the sprinter Chryste Gaines as being among them.
Gaines, who was a member of the gold medal 4 x 100m US relay squad at the 1996
Olympics and 2001 world championships, was also in their quartet in Paris at the
world event in August.
The favourites were beaten into second by France after Kelli White was withdrawn
from the US team. White is likely to forfeit world 100 and 200m gold, having
given a sample which showed she used the same stimulant. She, Gaines, and
Chambers worked with the same coach, Remi Korchemny, as did the sprint hurdler
Chris Phillips, who was fifth in the Paris final. He, too, has tested positive
for Modafinil.
White said that she and her mother use Modafinil to treat a sleeping disorder
called narcolepsy, but the condition seems to have reached epidemic proportions
in athletics.
Professor Arne Ljungqvist, head of the medical commision at the International
Association of Athletics Federations, said evidence suggests a link between
modafinil and THG. "It's a pattern I've seen before, where drugs have become
popular and we find them."
White's defence of a family condition seems compromised. As Ljungqvist said: "It
comes into a different sort of light when it becomes known that modafinil has
been taken by a number of athletes."
l The French Sports Ministry are to screen 10,200 promising young athletes for
drugs next year. This will be in addition to the 7300 already tested on national
teams. The UK does some 6000 tests annually.
LOAD-DATE: October 29, 2003
LANGUAGE: English
GRAPHIC: WAKE-UP CALL: Chryste Gaines is lastest champion to test positive for
stimulant. Picture: Getty Images
PUB-TYPE: Paper
Copyright 2003 Scottish Media Newspapers Limited
684 of 998 DOCUMENTS
The San Francisco Chronicle
OCTOBER 29, 2003, WEDNESDAY, FINAL EDITION
FDA outlaws designer steroid;
Burlingame firm allegedly the source of controversial drug
SOURCE: Chronicle Staff Writer
BYLINE: Mark Fainaru-Wada
SECTION: NEWS; Pg. A10
LENGTH: 548 words
The designer steroid linked by Olympic drug-testing officials to a Burlingame
supplement lab being investigated by a federal grand jury is illegal, the Food
and Drug Administration announced Tuesday.
The FDA issued a statement saying it had determined that tetrahydrogestrinone
(THG) is an unapproved drug, and the agency said it is working with other
federal agencies to "aggressively engage, enforce and prosecute those firms or
individuals who manufacture, distribute or market THG."
Two weeks ago, the U.S. Anti-Doping Agency (USADA), a nonprofit that oversees
drug testing of Olympic sports, announced the discovery of THG as part of a
doping scandal and named Victor Conte and the Bay Area Laboratory Co-Operative
(BALCO) as the source of the drug.
Conte has denied in repeated e-mails to The Chronicle and other media outlets
that he is the source of the substance, and he also has questioned whether it is
anabolic in nature. Anabolic steroids stimulate muscle development.
That question is moot to the FDA, which said in its statement that unapproved
new drugs can't be marketed without undergoing the agency's approval process.
Because that has not been done with THG, an FDA spokesperson said anyone
marketing or providing the drug would be in violation of the Food, Drug and
Cosmetic Act.
The FDA said that although THG might be marketed by some as a dietary
supplement, it is, indeed, a "designer" steroid that is "closely and
structurally related" to gestrinone and trenbolone, two synthetic anabolic
steroids.
Conte and his company have been thrust into the middle of what has become an
international doping scandal, details of which continue to trickle out daily.
More athletes were reported to have tested positive for the stimulant modafinil,
which had previously showed up in a test of Union City sprinter and BALCO client
Kelli White at the World Championships in Paris this summer. White's doctor,
Brian Goldman, once a BALCO medical director, said she used the drug to combat
narcolepsy.
When the USADA announced its news about THG, it also said re-testing of samples
from the U.S. National Track and Field Championships at Stanford revealed
several other athletes testing positive for modafinil.
The Washington Post and Los Angeles Times, citing sources, said BALCO client and
U.S. sprinter Chryste Gaines had tested positive for the substance, and the
Times also named hurdlers Eric Thomas and Sandra Glover. Salinas sprinter Calvin
Harrison and U.S. hurdler Chris Phillips also have been identified as having
tested positive for modafinil.
Also Tuesday, the Associated Press reported that track's international governing
body would pursue punishment of coaches as well as athletes directly connected
to use of prohibited substances. The organization's medical commission chief,
Arne Ljungqvist, was quoted as saying the revelations about THG and modafinil
were part of a "pattern" of abuse in the United States.
Several other sports associations have announced additional testing since USADA
first discussed THG publicly. Swimming's world governing body said Tuesday it
would retest hundreds of urine samples from this summer's world championships
for the designer steroid.E-mail Mark Fainaru-Wada at
mfainaru-wada@sfchronicle.com
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Chronicle Publishing Co.
685 of 998 DOCUMENTS
San Jose Mercury News (California)
October 29, 2003 Wednesday MORNING FINAL EDITION
POSITIVE DRUG TESTS REVEALED;
BAY AREA TRACK COACH HAS TIES TO SOME WHO USED STIMULANT
BYLINE: PETE CAREY, Mercury News
SECTION: SPORTS; Pg. 2D
LENGTH: 615 words
A secondary track and field drug scandal involving the use of the narcolepsy
drug modafinil grew Tuesday with disclosures that a half-dozen top athletes have
tested positive for it.
The agent for the American 110-meter hurdler Chris Phillips said Phillips told
the International Association of Athletics Federations that he was given a
modafinil tablet by Castro Valley track coach Remi Korchemny, who assured him it
was not a banned substance.
Also Tuesday, the Food and Drug Administration declared that the designer
steroid THG, or tetrahydrogestrinone, is an unapproved new drug and cannot
legally be marketed. A representative said the FDA would "prosecute those firms
or individuals who manufacture, distribute or market THG."
THG is a steroid derivative identified this summer after someone anonymously
mailed a used syringe to the U.S. Anti-Doping Agency, saying it came from
nutritionist Victor Conte Jr. and his Burlingame company, Balco Laboratories.
Several athletes with ties to Conte have since tested positive for THG.
Modafinil is not a steroid, but a treatment for sleep disorders approved in
1998. The continuing positive tests are an indication that athletes were telling
one another that there were benefits from taking it.
Four of the athletes reported to have tested positive for modafinil are linked
to Korchemny through his coaching, consulting or a track club he helped found --
Phillips; Union City sprinter Kelli White; sprinter Chryste Gaines, and Salinas
native Calvin Harrison.
The Los Angeles Times, citing "sources familiar with the inquiry," reported that
four-time U.S. Outdoor champion Sandra Glover and 400-meter hurdles champion
Eric Thomas also tested positive.
A leading authority on sprint events, Korchemny has also used Balco products
with his athletes. The coach couldn't be reached for comment Tuesday, but he has
repeatedly told the Mercury News he does not provide performance-enhancing drugs
to his athletes.
A longtime friend, Bill Alston, said he spoke to Korchemny recently and "he
sounds really depressed. He's really hurting."
"He's so adamant against drugs," Alston said. "He just fumes when he thinks
about that. To have him in that position, it just doesn't fit."
Sold under the brand name Provigil, modafinil is used in treating narcolepsy but
has several "off label" uses, from treating multiple sclerosis symptoms to
keeping soldiers alert in battle.
Track federations have classified modafinil as a mild stimulant. An athlete
found using it at a meet would be disqualified and would forfeit any medals.
White won two gold medals in August at the world championships in Paris and then
tested positive. She said the drug was prescribed for narcolepsy by Balco's
former medical director.
Sports organizations say modafinil is performance-enhancing, while sleep experts
doubt that.
Even if it has only a small positive effect, said Dr. Gary Wadler, a New York
University School of Medicine professor and sports doping expert, "it could be
the difference between a gold and a silver medal, or a silver and bronze."
Robert Wagner, the agent for Phillips, White and Glover, told the Associated
Press his athletes were taking the drug all summer. None of them thought it was
a prohibited substance, he said.
"When Americans come to Europe, they take it to get over the jet lag," he said.
"It's not a stimulant. It wasn't on the list."
Also Tuesday, the world governing organization for swimming said it would retest
athletes' urine samples from the world championships in July for THG. David
Howman, director general of the World Anti-Doping Agency, said this could prompt
other sports to do the same.
LOAD-DATE: August 17, 2005
LANGUAGE: ENGLISH
Copyright 2003 San Jose Mercury News
All Rights Reserved
686 of 998 DOCUMENTS
Sydney Morning Herald (Australia)
October 29, 2003 Wednesday
Early Edition
US star and Chinese the latest to test positive;
DRUGS IN SPORT
BYLINE: Jacquelin Magnay
SECTION: SPORT; Pg. 38
LENGTH: 402 words
The drip-feed of athletes testing positive to banned drugs continues, the latest
being US sprinter Chryste Gaines , ranked No.3 in the world in the 100 metres.
Gaines tested positive to the same modafinil stimulant that has jeopardised the
two world championship gold medals won by her San Francisco training partner,
Kelli White .
But the biggest surprise is the news of positive drug tests to erythropoietin
(EPO) in China, which has so far escaped the ignominy of tetrahydrogestrinone
(THG) or modafinil.
Chinese runners Zheng Yongji and Li Huiquan were expelled from the fifth Chinese
City Games at the weekend after testing positive for the blood boosting hormone.
So quickly is the drugs issue moving that EPO, which has been around for nearly
20 years but testing for which has been refined only in the past three years,
seems rather passe.
Zheng Yongji finished second in qualification for the men's 3000m steeplechase,
while Li Huiquan won the men's 800m qualification. Chinese authorities have
promised that the cases will be investigated promptly.
But it is Gaines's test result that has confirmed the strong links between those
caught in the latest drugs scandal, the coach Remi Korchemny , his San Francisco
training group and the vitamin and supplement company BALCO.
The IAAF medical commission chairman Arne Ljungqvist said there might be six to
eight modafinil cases being processed at the moment, damaging White's defence
that she had a genuine medical excuse. He said the drug was the latest
fashionable stimulant among athletes.
"It's a little odd to find an epidemic of narcolepsy in top athletes," he said.
Gaines has made no comment about how modafinil came to be in her urine sample
taken at the July US track and field trials.
"She is my student, but I don't know anything about her," Korchemny told The
Washington Post. "I didn't give her modafinil."
White reckoned she took the substance to treat narcolepsy after it was
prescribed by Brian Goldman, a doctor who used to be BALCO's medical director.
White has trained under Korchemny for the past three years, and last season
European champion sprinter Dwain Chambers joined the squad. Chambers is one of
four top athletes to have tested positive to THG. Chambers was introduced to
BALCO by Korchemny.
The IAAF officials have started their own investigations and are likely to
impose a sanction on Korchemny within their rules, but seldom applied.
LOAD-DATE: July 17, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 John Fairfax Publications Pty Ltd
All Rights Reserved
687 of 998 DOCUMENTS
Sydney Morning Herald (Australia)
October 29, 2003 Wednesday
Late Edition
US star and Chinese the latest to fall;
DRUGS IN SPORT
BYLINE: Jacquelin Magnay
SECTION: SPORT; Pg. 38
LENGTH: 395 words
The drip-feed of athletes testing positive to banned drugs continues, the latest
being US sprinter Chryste Gaines , ranked No.3 in the world in the 100 metres.
Gaines tested positive to the same modafinil stimulant that has jeopardised the
two world championship gold medals won by her San Francisco training partner,
Kelli White .
But the biggest surprise is the news of positive drug tests to erythropoietin
(EPO) in China, which has so far escaped the ignominy of tetrahydrogestrinone
(THG) or modafinil.
Chinese runners Zheng Yongji and Li Huiquan were expelled from the fifth Chinese
City Games at the weekend after testing positive for the blood boosting hormone.
So quickly is the drugs issue moving that EPO, which has been around for nearly
20 years but testing for which has been refined only in the past three years,
seems rather passe.
Zheng Yongji finished second in qualification for the men's 3000m steeplechase,
while Li Huiquan won the men's 800m qualification. Chinese authorities have
promised that the cases will be investigated promptly.
But it is Gaines's test result that has confirmed the strong links between those
caught in the latest drugs scandal, the coach Remi Korchemny , his San Francisco
training group and the vitamin and supplement company BALCO.
The IAAF medical commission chairman Arne Ljungqvist said there might be six to
eight modafinil cases being processed at the moment, damaging White's defence
that she had a genuine medical excuse. He said the drug was the latest
fashionable stimulant among athletes. "It's a little odd to find an epidemic of
narcolepsy in top athletes," he said.
Gaines has made no comment about how modafinil came to be in her urine sample
taken at the July US track and field trials.
"She is my student, but I don't know anything about her," Korchemny told The
Washington Post. "I didn't give her modafinil."
White reckoned she took the substance to treat narcolepsy after it was
prescribed by Brian Goldman, a doctor who used to be BALCO's medical director.
White has trained under Korchemny for the past three years, and last season
European champion sprinter Dwain Chambers joined the squad. Chambers is one of
four top athletes to have tested positive to THG. Chambers was introduced to
BALCO by Korchemny.
The IAAF officials have started their own investigations and are likely to
impose a sanction on Korchemny.
LOAD-DATE: July 17, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 John Fairfax Publications Pty Ltd
All Rights Reserved
688 of 998 DOCUMENTS
Tampa Tribune (Florida)
October 29, 2003, Wednesday, FINAL EDITION
FDA Classifies Steroid THG As An Illegal Drug
BYLINE: A Tribune staff, wire report; BILL WARD, TRIBUNE WIRES
SECTION: SPORTS, Pg. 2
LENGTH: 561 words
WASHINGTON - The newly detected steroid that is casting a shadow on Olympic and
professional sports is an illegal drug that may pose considerable health risks,
the government warned Tuesday.
THG has been sold in the guise of a dietary supplement when it is in fact a drug
that lacks federal permission for sale in this country, the Food and Drug
Administration said. It is a drug derived from another steroid long banned in
athletics, the agency said.
The FDA's official designation of THG as illegal, which had been anticipated
since the scandal about the previously undetectable steroid emerged, puts
manufacturers on notice that the government will crack down on anyone caught
selling it.
It also is the strongest warning yet that using THG is risky. Anabolic steroids
can have dangerous side effects, including liver damage, heart disease, anxiety
and rage. While little is known about THG's specific effects because it is new,
its close chemical similarity to other well-known steroids means it poses the
same risks, FDA Associate Commissioner John Taylor said.
"The greatest importance is preventing exposure and trying to nip this in the
bud," he said.
U.S. drug authorities first learned about THG, or tetrahydrogestrinone, this
summer after an unidentified coach gave them a syringe containing it. THG
apparently was designed specifically to be undetectable by the standard test
given to athletes.
Now armed with a test, sports organizations are scrambling to re-examine
athletes and to decide what penalties to impose for THG use. Four U.S. track and
field athletes have tested positive for THG, and Europe's top sprinter has
admitted taking it in nutritional supplements that he says he thought were
allowed.
Anabolic steroids are synthetic versions of the male hormone testosterone. Some
are approved by FDA for prescription-only sale to treat certain diseases;
athletes use them illegally to bulk up muscle and enhance performance.
ATHLETES TEST POSITIVE: The Washington Post reported that U.S. sprinter Chryste
Gaines, the 2001 U.S. champion at 100 meters and a two-time Olympic medalist in
the 4x100 relay, tested positive for the banned stimulant modafinil.
Quoting "international officials with knowledge of the results," the Post said
Gaines tested positive for modafinil, which is often used to treat the sleep
disorder narcolepsy, at the U.S. Track and Field Championships in July. Gaines
is the fourth athlete connected to Ukrainian-born coach Remi Korchemny to test
positive for banned drugs this summer. International Association of Athletics
Federations General Secretary Istvan Gyulai called the matter a "concern" and
said the IAAF planned to conduct an investigation.
"This has to be investigated," he said. "We cannot just turn a blind eye to
this."
Gaines, 100/200 world champion Kelli White and seven-time NCAA All-America
hurdler Chris Phillips - all with ties to Korchemny - have tested positive for
modafinil. Another of Korchemny's athletes, former European 100 champion Dwain
Chambers of England, tested positive for THG.
Meanwhile, The Los Angeles Times, citing unnamed sources, said hurdlers Sandra
Glover and Eric Thomas also tested positive for modafinil.
Calvin Harrison, an Olympic and world relay gold medalist, had previously
confirmed he tested positive for modafinil at the U.S. meet.
LOAD-DATE: October 30, 2003
LANGUAGE: ENGLISH
NOTES: TRACK AND FIELD
Copyright 2003 The Tribune Co. Publishes The Tampa Tribune
689 of 998 DOCUMENTS
The Toronto Star
October 29, 2003 Wednesday Ontario Edition
Narcolepsy outbreak among top athletes?
BYLINE: Randy Starkman, Toronto Star
SECTION: SPORTS; Pg. C07
LENGTH: 504 words
HIGHLIGHT:
Four U.S. runners test positive for new drug All of them 'can't have a sleep
problem'
Narcolepsy is a disease affecting about one in every 2,000 Americans, but there
appears to be an epidemic among top U.S. track athletes. At least four of them
have now tested positive for a drug created to treat the sleep disorder.
Modafinil first came to prominence in sports when double gold medallist Kelli
White of the U.S. tested positive for it in August at the world track and field
championships in Paris.
White, who stands to lose her gold medals from the women's 100 and 200 metres,
claimed she was using the medication to treat narcolepsy, which is characterized
by sudden and uncontrollable episodes of deep sleep.
But top anti-doping officials say the rash of positive tests - sprinter Chryste
Gaines is the fourth American reported to have tested positive for it -
demonstrates that athletes are using modafinil as a stimulant. Track officials
say there have been as many as seven positive tests for the drug.
"All the athletes can't be narcoleptic and have a sleep problem," said Dr.
Christiane Ayotte of the IOC-accredited testing laboratory in Montreal. "This is
enough now. They thought they had a stimulant that was not detectable and was
not being tested by the lab."
Ayotte said the first positive modafinil finding was made in the Paris lab
during the world championships because of pressure applied by the French
government to test for such substances. Modafinil was not officially listed as a
banned substance, but is considered a "like substance" in the banned stimulant
category.
Dr. Leonid Kayumov, professor of psychiatry at the University of Toronto and
director of the sleep disorders clinic at Toronto Western Hospital, said
modafinil has proved to be a good treatment for narcolepsy because it has fewer
side effects than previously used medications.
He said it would likely improve motor skills and motor reaction if taken by a
healthy athlete.
"It has an alerting effect, a boosting of energy," Kayumov said. "It has a life
of about 10 hours and then it would be eliminated from the bloodstream. It's
very disconcerting that people in sport would take this. It's inappropriate."
Kayumov also finds it hard to believe someone could be narcoleptic and a
world-class athlete. "It's (the disease) incompatible with sport," he said.
Modafinil is a controlled substance both here and in the U.S. and illegal to
distribute without a prescription. Under present rules, a positive test calls
for disqualification from the event but no additional ban, meaning the athletes
can compete at next year's Athens Olympics.
The four reported positives for the drug include Alvin Harrison, an Olympic and
world gold medallist in the men's 4x400-metre relay, and Chris Phillips, who
tested positive after finishing fifth in the men's 110-metre hurdles at Paris.
White, Gaines and Phillips are coached by 71-year-old Ukrainian Remy Korchemney,
who is associated with Victor Conte, owner of Balco Laboratories, which is the
subject of a U.S. federal grand jury investigation.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Toronto Star Newspapers, Ltd.
690 of 998 DOCUMENTS
USA TODAY
October 29, 2003, Wednesday, FINAL EDITION
Developments come quick in drug issue
BYLINE: Dick Patrick
SECTION: SPORTS; Pg. 10C
LENGTH: 424 words
The drugs in sport issue continued on different fronts Tuesday.
In a Senate Commerce Committee hearing, chairman John McCain (R-Ariz.) was
disturbed over a statistic cited in a hearing on a bill seeking to reclassify
the popular steroid precursor androstenedione, which is banned by the Olympics,
the NFL and NCAA but is available over the counter in the USA.
The CEO of the U.S. Anti-Doping Agency, Terry Madden, reported a study of 624
dietary supplements determined that 41% of the products by U.S. companies
contained either a steroid precursor or banned substance not disclosed on the
label. "It's very worrisome to athletes," Madden told McCain.
Meanwhile, the list of U.S. track athletes with positive drug tests grew.
Sprinter Chryste Gaines and 400-meter hurdlers Sandra Glover and Eric Thomas
have tested positive for the stimulant modafinil, according to the Los Angeles
Times and Washington Post.
The penalty for modafinil calls for disqualification from the meet in which the
violation occurs but carries no further competition ban. If Glover and Thomas
don't win appeals, they'll lose titles won at June's USA Track & Field
Championships.
U.S. sprinter Calvin Harrison has acknowledged a positive test for modafinil,
and officials from the international track federation (IAAF) have indicated
there could be six to eight U.S. positives from re-evaluations of drug tests at
the U.S. championships.
In August's world track and field championships, sprinter Kelli White and
hurdler Chris Phillips, both Americans, tested positive for modafinil. White,
who says it was prescribed for the sleep disorder narcolepsy, faces loss of her
100- and 200-meter titles.
There are connections between some of the modafinil-positive athletes, including
White, and the man being investigated by a federal grand jury for his activities
at BALCO Laboratories.
USADA has linked BALCO owner Victor Conte to the designer steroid THG,
undetectable until recently when it resulted in at least five positive tests,
four from Americans. Conte denies he's the source of THG and also contends THG
is not a steroid.
The search for THG keeps expanding. The world swimming federation (FINA) plans
to retest hundreds of urine samples from July's world championships. The IAAF
and the NFL already said they would retest.
Another link is Remi Korchemny, who coaches White, Gaines, THG-positive British
sprinter Dwain Chambers and Phillips. The IAAF has revived talk of suspending
coaches found to promote drug use.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, B/W, 2000 photo by Jack Gruber, USA TODAY; Troubling trend:
Hurdler Eric Thomas and two other U.S. athletes are the latest to test positive
for modafinil, a stimulant. The penalty for using modafinil does not include
suspension.
Copyright 2003 Gannett Company, Inc.
691 of 998 DOCUMENTS
Agence France Presse -- English
October 28, 2003 Tuesday
Reports say Gaines among US modafinil dope positives
SECTION: Sports
LENGTH: 525 words
DATELINE: LOS ANGELES, Oct 28
Olympic gold medal winner Chryste Gaines is among three athletes who tested
positive for the banned stimulant modafinil at June's United States athletics
championship, according to US newspaper reports.
The Los Angeles Times and Washington Post, both citing unnamed sources, reported
Tuesday that Gaines, a member of the triumphant US 4x100m relay at the 1996
Olympics, failed a doping test at the US meet.
Sandra Glover, a four-time US champion in the 400m hurdles and runner-up in
August at the World Championship in Paris, and Eric Thomas, the reigning US 400
hurdles champion, also tested positive at the US meet, the Times reported.
At least six US athletes are believed to have tested positive for modafinil,
with 2000 Olympic triumphant US 4x400 relay member Calvin Harrison admitting a
positive test for a substance, used to combat the sleep disorder narcolepsy.
A drug scandal has swirled around US athletics since United States Anti-Doping
Agency chief executive Terry Madden disclosed that a designer steroid,
tetrahydrogestrinone (THG), was being taken by US athletes.
Madden linked the previously undectable substance to BALCO Labs, a nutritional
supplement firm near San Francisco run by Victor Conte, who has denied
wrongdoing.
Harrison's positive test for modafinil touched off yet another firestorm over
modafinil a key figure being Ukranian-born coach Remi Korchemny, also living in
the San Francisco area.
Gaines became the fourth athlete with ties to Korchemny to test positive for
banned drugs this summer, following US sprinter Kelli White, hurdler Chris
Phillips and British sprinter Dwain Chambers, the Post reported.
"If it is proven that this coach was offering anything that is not a permissible
substance to athletes, that is the biggest concern to the IAAF," Istvan Gyulai,
general secretary for the world governing body, told the Post.
Chambers, Gaines and White train with Korchemny.
Robert Wagner, the agent for Phillips and White, told the Post that Korchemny
gave Phillips a modafinil pill before the 110m semi-finals at the world
championships in Paris because he was having trouble sleeping.
Korchemny told the Post he gave Phillips modafinil and White also.
"I'm sorry I did it ... but it was not prohibited," Korchemny told the Post. "I
was 100 percent sure everything was legal."
Korchemny said he knew nothing about Chambers' arrangements with BALCO for
supplements and that he did not give Gaines modafinil, adding, "She is my
student, but I don't know anything about her."
Modafinil was not banned until after the world championships but comes under
anti-doping jurisdictions, drug-test officials told the Post, because of rule
provisions regarding substances closely related to banned drugs.
"They were all under the impression modafinil was OK," Wagner told the Post.
US athletics officials say four Americans would join Chambers with positive
doping tests for THG.
Various US newspaper accounts have identified three of them as middle-distance
runner Regina Jacobs, US shot put champion Kevin Toth and hammer thrower John
McEwan.
js/ea03
Athletics-USA-doping
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Agence France Presse
692 of 998 DOCUMENTS
Alameda Times-Star (Alameda, CA)
October 28, 2003 Tuesday
Hot Gordon grabs second win in row
BYLINE: WIRE REPORTS
SECTION: SPORTS NEWS & COLUMNS
LENGTH: 809 words
Jeff Gordon is back to his old winning ways, holding off a challenge from Tony
Stewart on Monday at Atlanta Motor Speedway to earn his second straight victory.
The Bass Pro Shops MBNA 500, halted by rain Sunday after just 39 of 325 laps,
was completed Monday under a caution after pole-winner Ryan Newman was sent
spinning into the wall with a tap on the rear bumper by Dale Earnhardt Jr. four
laps from the end.
Gordon had gone 22 races without a win before taking the checkered flag Oct.19
at Martinsville. The four-time Winston Cup champion now has three wins this
season and 64 in his career.
"Never count us out," Gordon said. "I know we haven't won a lot this year, but
we're strong finishers."
The two latest wins followed four straight fifth-place finishes and have helped
Gordon move to fifth in the season points, only 38 points behind third-place
Kevin Harvick.
On Monday, Gordon passed six-time Atlanta winner Bobby Labonte for the lead on
lap 277 and stayed out front the rest of the way to earn his second victory in
as many weeks.
Jimmie Johnson, who finished second to his car owner and Hendrick Motorsports
teammate at Martinsville, was third. He was followed by Bill Elliott and
Labonte, who faded after the final pit stops.
Series leader Matt Kenseth, who came into the race with a 240-point lead over
Harvick, finished 11th. Earnhardt's sixth-place finish Monday, combined with a
20th-place run by Harvick, moved Earnhardt to second in the points race.
TRACK AND FIELD
Two drugs under scrutiny in sports -- modafinil and THG -- are part of a pattern
of doping abuse in the United States, a top track and field executive said.
Arne Ljungqvist, the IAAF's medical commission chief, said the evidence suggests
a link between the substances.
Modafinil is the drug sprinter Kelli White of Union City says she took for a
sleep disorder. Tetrahydrogestrinone, or THG, is a previously undetectable
designer steroid that has turned up in the samples of several track and field
athletes.
The Washington Post, citing unidentified international sources with knowledge of
the results, reported on its Web site Monday night that former Stanford sprinter
Chryste Gaines tested positive for modafinil at the U.S. track and field
championships in July.
"What emerges now is a pattern," Ljungqvist told The Associated Press by phone
from Sweden. "People have taken THG for obvious reasons -- it's been designed
with the intent not to be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
FOOTBALL
Florida State moved to the top of the one-loss crowd. The Seminoles are third in
the new Bowl Championship Series standings, trailing only unbeaten Oklahoma and
Miami in the race to play for the national championship.
Southern California, third in both the AP and coaches polls, is fourth in the
BCS standings, followed by Georgia and Ohio State.
Georgia cornerback Decory Bryant had neck surgery Sunday morning that will end
his season and leaves his NFL future in doubt, the seventh starter or top backup
lost to a season-ending injury for the Bulldogs this season.
SOCCER
Mia Hamm, Joy Fawcett and Shannon Boxx, all World Cup all-stars, were selected
to the U.S. team that will play Mexico on Sunday at the Cotton Bowl.
U.S. coach April Heinrichs chose 19 players as the national team wraps up a 2003
season in which it has a 16-2-4 record and finished third at the World Cup.
Among the others chosen by Heinrichs were defender Brandi Chastain, goalkeepers
Brianna Scurry and Siri Mullinix; defender Danielle Slaton of Santa Clara;
midfielder Tiffany Roberts of San Ramon and Aly Wagner from Santa Clara.
Mexico's popular Chivas team and Major League Soccer reached an agreement in
principal for the Gudalajara-based team to acquire an expansion franchise.
Chivas, one of Mexico's most popular clubs, probably won't operate the team
until 2005.
MLS and Chivas officials are leaning toward putting the team in San Diego.
TENNIS
Albert Costa of Spain defeated Mariano Zabaleta of Argentina 6-7 [4], 6-4, 7-5
to reach the second round of the Paris Masters.
BOXING
Former lightweight champion Paul Spadafora was arraigned in Pittsburgh on Monday
on charges of attempted homicide and aggravated assault for allegedly shooting
his girlfriend after an argument over flat tires.
HOCKEY
Marc Savard and Jeff Cowan scored 24 seconds apart in the third period, and
Savard scored again with 15 seconds left in overtime as the Atlanta Thrashers
rallied for a 3-2 victory over host Toronto.
John LeClair had a goal and an assist in his first game of the season, and
Robert Esche earned his sixth career shutout, leading Philadelphia to a 5-0 win
over visiting Montreal.
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
Copyright 2003 MediaNews Group, Inc. and ANG Newspapers
693 of 998 DOCUMENTS
The Associated Press
October 28, 2003, Tuesday, BC cycle
AP Interview: Top track official sees pattern of doping abuse
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 575 words
DATELINE: LONDON
Two drugs under scrutiny in sports - modafinil and THG - are part of a pattern
of doping abuse in the United States, a top track and field executive said
Monday.
Arne Ljungqvist, the IAAF's medical commission chief, said the evidence suggests
a link between the substances.
Modafinil is the drug sprinter Kelli White says she took for a sleep disorder.
Tetrahydrogestrinone, or THG, is a previously undetectable designer steroid that
has turned up in the samples of several track and field athletes.
"What emerges now is a pattern," Ljungqvist told The Associated Press by phone
from Sweden. "People have taken THG for obvious reasons - it's been designed
with the intent not to be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
The Washington Post, citing unidentified international sources, reported Tuesday
that American sprinter Chryste Gaines tested positive for modafinil at the U.S.
track and field championships in July.
The Los Angeles Times also cited Gaines along with hurdlers Sandra Glover and
Eric Thomas as testing positive for modafinil. The Times based its report on
unidentified sources.
Calvin Harrison, an Olympic and world relay gold medalist, also tested positive
for the stimulant this past summer, a source close to a U.S. doping
investigation, told the AP on Saturday on condition of anonymity.
Harrison, still awaiting the result of his backup B sample, was tested at the
U.S. national championships in June at Stanford, Calif.
Modafinil first came to prominence in August when White tested positive for the
drug at the world championships in Paris. She stands to be stripped of her
100-meter and 200 titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offense and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in the 110 hurdles at
the worlds, also tested positive for modafinil at the Paris meet. Harrison ran
the opening leg of the 1,600 relay at the worlds.
Ljungqvist said the IAAF's penalty for modafinil is a public warning and
disqualification from the competition where the test took place - but no ban.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip, devised a test for THG. While retesting, U.S.
officials discovered several positives for modafinil.
Ljungqvist said the IAAF had been "directly or indirectly" informed of six to
eight modafinil cases.
Referring to White's narcolepsy defense, he said: "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test - a case
that could cost the United States an Olympic relay gold medal. Ljungqvist set a
deadline of Nov. 21 for USATF to comply.
Young tested positive for the steroid nandrolone but was cleared on appeal by
USATF officials. He went on to win a 1,600 relay gold medal at the 2000
Olympics.
USATF officials have declined to provide the information, citing confidentiality
rules at the time.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
694 of 998 DOCUMENTS
The Associated Press
October 28, 2003, Tuesday, BC cycle
IAAF to go after coaches in modafinil cases
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 613 words
DATELINE: LONDON
Track and field's world governing body plans to punish any coaches directly
connected to the spate of positive tests among U.S. athletes for the stimulant
modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Tuesday that any coaches or trainers involved in the use of
modafinil should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offense
themselves," he told The Associated Press in a telephone interview.
"This has to be investigated," Gyulai added. "We cannot just turn a blind eye to
this."
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more U.S. athletes were cited in newspaper reports Tuesday for positive
modafinil tests.
The Washington Post, citing unidentified sources, reported that sprinter Chryste
Gaines - a relay gold medalist at the 1996 Olympics -tested positive at the U.S.
championships in Stanford, Calif., in July.
The Los Angeles Times, citing unnamed sources, said hurdlers Sandra Glover and
Eric Thomas also tested positive for the drug.
Calvin Harrison, an Olympic and world relay gold medalist, had previously
confirmed he tested positive for modafinil at the U.S. meet.
Sprinter Kelli White and hurdler Chris Phillips tested positive at the World
Championships. White, who said she took modafinil for narcolepsy, risks losing
her gold medals from the 100 and 200 meters.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified as a "minor
stimulant." It has since been placed by name on the World Anti-Doping Agency's
banned list.
Gyulai said it's possible the athletes all believed modafinil wasn't prohibited.
"This is an option, but it has been determined that it is a stimulant and was a
stimulant at the time as well," he said. "It's up to USA Track & Field to take
the necessary action."
The IAAF's penalty for use of minor stimulants is a public warning and
disqualification from the event where the test took place - but no ban.
Some of the athletes have been coached by Ukrainian-born coach Remi Korchemny,
who is based in the San Francisco area. He did not return repeated messages left
by the AP this week.
Robert Wagner, the agent for White, Phillips and Glover, said Phillips told the
IAAF that Korchemny gave him a modafinil tablet at the worlds because he was
having trouble sleeping.
"None of these athletes thought this was a prohibited substance, they were
taking it all summer," Wagner told the AP by telephone from Austria. "It's like
melatonin. When Americans come to Europe, they take it to get over the jet lag.
It's not a stimulant. It wasn't on the list."
Gyulai stressed that modafinil should not be viewed in the same light as the
designer steroid THG, which has turned up in the samples of several track and
field athletes. The sanction for steroids is a two-year ban.
"THG was invented, produced and masterminded to cheat," Gyulai said. "There is a
major difference with modafinil. The athletes may have thought this is not
forbidden. They should have checked more carefully."
Gyulai said he had read or heard reports of a total of seven modafinil cases,
but stressed the IAAF had received no official notification of the tests or
names involved.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
695 of 998 DOCUMENTS
Associated Press Worldstream
October 28, 2003 Tuesday
IAAF to go after coaches in modafinil cases
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 710 words
DATELINE: LONDON
Track and field's world governing body plans to punish any coaches directly
connected to the spate of positive tests among U.S. athletes for the stimulant
modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Some of the athletes have been coached by Ukrainian-born coach Remi Korchemny,
who is based in the San Francisco area.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Tuesday that any coaches or trainers involved in the use of
modafinil should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offense
themselves," he told The Associated Press in a telephone interview.
"This has to be investigated," Gyulai added. "We cannot just turn a blind eye to
this."
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more U.S. athletes were cited in newspaper reports Tuesday for positive
modafinil tests.
The Washington Post, citing unidentified international sources, reported that
sprinter Chryste Gaines - a relay gold medalist at the 1996 Olympics -tested
positive at the U.S. championships in Stanford in July.
The Los Angeles Times also cited Gaines along with hurdlers Sandra Glover and
Eric Thomas. The Times based its report on unidentified sources.
Glover is a four-time U.S. champ in the 400 hurdles and won the silver medal at
the World Championships in Paris in August. Thomas is the U.S. men's 400 hurdles
champion. He did not win a medal in Paris.
Calvin Harrison, an Olympic and world relay gold medalist, had previously
confirmed that he tested positive for modafinil at the U.S. meet.
Sprinter Kelli White and hurdler Chris Phillips tested positive at the World
Championships. White, who said she took modafinil for narcolepsy, risks losing
her gold medals from the 100 and 200 meters.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified as a "minor
stimulant." It has since been placed by name on the World Anti-Doping Agency's
banned list.
Gyulai said it's possible the athletes all believed modafinil wasn't prohibited.
"This is an option, but it has been determined that it is a stimulant and was a
stimulant at the time as well," he said. "It's up to USA Track & Field to take
the necessary action."
The IAAF's penalty for use of minor stimulants is a public warning and
disqualification from the event where the test took place - but no ban.
Gyulai reiterated the IAAF's position that athletes who tested positive for
modafinil at the U.S. championships remained eligible for the world meet.
Robert Wagner, the agent for White, Phillips and Glover, said Phillips told the
IAAF that Korchemny gave him a modafinil tablet at the worlds because he was
having trouble sleeping.
"None of these athletes thought this was a prohibited substance, they were
taking it all summer," Wagner told the AP by telephone from Austria. "It's like
melatonin. When Americans come to Europe, they take it to get over the jet lag.
It's not a stimulant. It wasn't on the list. Why weren't all the labs testing
for it?"
Gyulai stressed that modafinil should not be viewed in the same light as the
designer steroid THG, which has turned up in the samples of several track and
field athletes. The sanction for steroids is a two-year ban.
Urine samples from the U.S. championships were retested after the UCLA doping
control laboratory, acting on a tip, devised a test for THG. While retesting,
U.S. officials discovered several modafinil cases as well as four THG positives.
"THG was invented, produced and masterminded to cheat," Gyulai said. "There is a
major difference with modafinil. The athletes may have thought this is not
forbidden. They should have checked more carefully."
Gyulai said he had read or heard reports of a total of seven modafinil cases,
but stressed the IAAF had received no official notification of the tests or
names involved.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
696 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 28, 2003, Tuesday, BC cycle
IAAF to go after coaches in modafinil cases
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 613 words
DATELINE: LONDON
Track and field's world governing body plans to punish any coaches directly
connected to the spate of positive tests among U.S. athletes for the stimulant
modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Tuesday that any coaches or trainers involved in the use of
modafinil should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offense
themselves," he told The Associated Press in a telephone interview.
"This has to be investigated," Gyulai added. "We cannot just turn a blind eye to
this."
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more U.S. athletes were cited in newspaper reports Tuesday for positive
modafinil tests.
The Washington Post, citing unidentified sources, reported that sprinter Chryste
Gaines - a relay gold medalist at the 1996 Olympics - tested positive at the
U.S. championships in Stanford, Calif., in July.
The Los Angeles Times, citing unnamed sources, said hurdlers Sandra Glover and
Eric Thomas also tested positive for the drug.
Calvin Harrison, an Olympic and world relay gold medalist, had previously
confirmed he tested positive for modafinil at the U.S. meet.
Sprinter Kelli White and hurdler Chris Phillips tested positive at the World
Championships. White, who said she took modafinil for narcolepsy, risks losing
her gold medals from the 100 and 200 meters.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified as a "minor
stimulant." It has since been placed by name on the World Anti-Doping Agency's
banned list.
Gyulai said it's possible the athletes all believed modafinil wasn't prohibited.
"This is an option, but it has been determined that it is a stimulant and was a
stimulant at the time as well," he said. "It's up to USA Track & Field to take
the necessary action."
The IAAF's penalty for use of minor stimulants is a public warning and
disqualification from the event where the test took place - but no ban.
Some of the athletes have been coached by Ukrainian-born coach Remi Korchemny,
who is based in Castro Valley, Calif. He did not return repeated messages left
by the AP this week.
Robert Wagner, the agent for White, Phillips and Glover, said Phillips told the
IAAF that Korchemny gave him a modafinil tablet at the worlds because he was
having trouble sleeping.
"None of these athletes thought this was a prohibited substance, they were
taking it all summer," Wagner told the AP by telephone from Austria. "It's like
melatonin. When Americans come to Europe, they take it to get over the jet lag.
It's not a stimulant. It wasn't on the list."
Gyulai stressed that modafinil should not be viewed in the same light as the
designer steroid THG, which has turned up in the samples of several track and
field athletes. The sanction for steroids is a two-year ban.
"THG was invented, produced and masterminded to cheat," Gyulai said. "There is a
major difference with modafinil. The athletes may have thought this is not
forbidden. They should have checked more carefully."
Gyulai said he had read or heard reports of a total of seven modafinil cases,
but stressed the IAAF had received no official notification of the tests or
names involved.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
697 of 998 DOCUMENTS
Associated Press Online
October 28, 2003 Tuesday
AP Interview: Track Head Discusses Doping
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 610 words
DATELINE: LONDON
Track and field's world governing body plans to punish any coaches directly
connected to the spate of positive tests among U.S. athletes for the stimulant
modafinil.
Six Americans have been identified as testing positive for the substance, which
is prescribed for treatment of the sleeping disorder narcolepsy.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said Tuesday that any coaches or trainers involved in the use of
modafinil should face sanctions.
"If it proved that they incite or promote the use of drugs or substances which
are not permitted, they are considered to have committed a doping offense
themselves," he told The Associated Press in a telephone interview.
"This has to be investigated," Gyulai added. "We cannot just turn a blind eye to
this."
IAAF rules do not specify penalties for non-athletes in doping cases. But Gyulai
said the IAAF could consider banning a coach or refusing accreditation for major
events.
Three more U.S. athletes were cited in newspaper reports Tuesday for positive
modafinil tests.
The Washington Post, citing unidentified sources, reported that sprinter Chryste
Gaines - a relay gold medalist at the 1996 Olympics -tested positive at the U.S.
championships in Stanford, Calif., in July.
The Los Angeles Times, citing unnamed sources, said hurdlers Sandra Glover and
Eric Thomas also tested positive for the drug.
Calvin Harrison, an Olympic and world relay gold medalist, had previously
confirmed he tested positive for modafinil at the U.S. meet.
Sprinter Kelli White and hurdler Chris Phillips tested positive at the World
Championships. White, who said she took modafinil for narcolepsy, risks losing
her gold medals from the 100 and 200 meters.
Modafinil wasn't named on the sport's banned drug list, but the IAAF said it
fell under the category of related substances and classified as a "minor
stimulant." It has since been placed by name on the World Anti-Doping Agency's
banned list.
Gyulai said it's possible the athletes all believed modafinil wasn't prohibited.
"This is an option, but it has been determined that it is a stimulant and was a
stimulant at the time as well," he said. "It's up to USA Track & Field to take
the necessary action."
The IAAF's penalty for use of minor stimulants is a public warning and
disqualification from the event where the test took place - but no ban.
Some of the athletes have been coached by Ukrainian-born coach Remi Korchemny,
who is based in the San Francisco area. He did not return repeated messages left
by the AP this week.
Robert Wagner, the agent for White, Phillips and Glover, said Phillips told the
IAAF that Korchemny gave him a modafinil tablet at the worlds because he was
having trouble sleeping.
"None of these athletes thought this was a prohibited substance, they were
taking it all summer," Wagner told the AP by telephone from Austria. "It's like
melatonin. When Americans come to Europe, they take it to get over the jet lag.
It's not a stimulant. It wasn't on the list."
Gyulai stressed that modafinil should not be viewed in the same light as the
designer steroid THG, which has turned up in the samples of several track and
field athletes. The sanction for steroids is a two-year ban.
"THG was invented, produced and masterminded to cheat," Gyulai said. "There is a
major difference with modafinil. The athletes may have thought this is not
forbidden. They should have checked more carefully."
Gyulai said he had read or heard reports of a total of seven modafinil cases,
but stressed the IAAF had received no official notification of the tests or
names involved.
LOAD-DATE: October 29, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
698 of 998 DOCUMENTS
Calgary Herald (Alberta, Canada)
October 28, 2003 Tuesday Final Edition
Track official detects pattern in doping tests
SOURCE: The Associated Press
SECTION: Sports; Pg. F4
LENGTH: 167 words
DATELINE: LONDON
Two drugs under scrutiny in sports -- modafinil and THG -- are part of a pattern
of doping abuse in the United States, a top track and field executive said
Monday.
Arne Ljungqvist, the IAAF's medical commission chief, said the evidence suggests
a link between the substances.
Modafinil is the drug sprinter Kelli White says she took for a sleep disorder.
Tetrahydrogestrinone, or THG, is a previously undetectable designer steroid that
has turned up in the samples of several track and field athletes.
"What emerges now is a pattern," Ljungqvist said via phone from Sweden. "People
have taken THG for obvious reasons -- it's been designed with the intent not to
be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
Ljungqvist spoke after 400-metre runner Calvin Harrison became the latest
athlete identified as having tested positive for modafinil.
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
699 of 998 DOCUMENTS
Edmonton Journal (Alberta)
October 28, 2003 Tuesday Final Edition
Narcolepsy the new excuse for drug use among athletes: Narcolepsy drug has ties
with designer steroid
SOURCE: The Associated Press
SECTION: Sports; Pg. D4
LENGTH: 417 words
DATELINE: LONDON
LONDON - Two drugs under scrutiny in sports -- modafinil and THG -- are part of
a pattern of doping abuse in the United States, a top track and field executive
said Monday.
Arne Ljungqvist, medical commission chief of track and field's governing body,
said the evidence suggests a link between the substances.
Modafinil is the drug sprinter Kelli White says she took for a sleep disorder.
Tetrahydrogestrinone, or THG, is a previously undetectable designer steroid that
has turned up in the samples of several track and field athletes.
"What emerges now is a pattern," Ljungqvist said via phone from Sweden. "People
have taken THG for obvious reasons -- it's been designed with the intent not to
be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
Ljungqvist spoke after 400-metre runner Calvin Harrison became the latest
athlete identified as having tested positive for modafinil.
Harrison, an Olympic and world relay gold medallist, tested positive for
modafinil this past summer, according to an anonymous source.
Harrison, still awaiting the result of his backup B sample, was tested at the
U.S. national championships in June at Stanford, Calif.
Modafinil first came to prominence in August when White tested positive for the
drug at the World Championships in Paris. She stands to be stripped of her 100-
and 200-metre titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offence and submitted her case to U.S. authorities for
disciplinary action.
The drug has become the "fashionable" stimulant of choice among certain American
athletes, track and field's top anti-doping official said Monday.
"It's a little odd to find an epidemic of narcolepsy in top athletes," said
Ljungqvist. "The disorder of narcolepsy is not that frequent."
Another U.S. athlete, Chris Phillips, who finished fifth in the 110-metre
hurdles at the Worlds, also tested positive for modafinil at the Paris meet.
Ljungqvist said the IAAF's penalty for modafinil is a public warning and
disqualification from the competition where the test took place -- but no ban.
Referring to White's narcolepsy defence, he said: "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
700 of 998 DOCUMENTS
Hamilton Spectator (Ontario, Canada)
October 28, 2003 Tuesday Final Edition
Drug use ridiculed; Claims modafinil taken to combat narcolepsy
SOURCE: The Canadian Press
BYLINE: Stephen Wilson
SECTION: SPORTS; Pg. SP09
LENGTH: 487 words
DATELINE: LONDON
Modafinil, the drug which sprinter Kelli White claims she took for a sleep
disorder, has become the "fashionable" stimulant of choice among certain
American athletes, track and field's top anti-doping official said yesterday.
"It's a little odd to find an epidemic of narcolepsy in top athletes," said Arne
Ljungqvist, medical commission chief of track and field's governing body. "The
disorder of narcolepsy is not that frequent."
Ljungqvist spoke after 400-metre runner Calvin Harrison became the latest
athlete identified as having tested positive for the drug.
In an interview with The Associated Press, Ljungqvist said a spate of positive
tests for modafinil suggests the substance is part of a pattern of doping abuse
in the United States along with the designer steroid THG.
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test -- a case
which could cost the U.S. an Olympic relay gold medal. Ljungqvist set a deadline
of Nov. 21 for the U.S. association to comply.
Harrison, an Olympic and world relay gold medallist, tested positive for
modafinil last summer, a source told the AP on Saturday.
Harrison, still awaiting the result of his backup B sample, was tested at the
U.S. national championships in June at Stanford. Modafinil first came to
prominence in August when White tested positive for the drug at the world
championships in Paris.
She stands to be stripped of her 100-metre and 200-metre titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offence and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in 110-metre hurdles at
the worlds, also tested positive for modafinil at the Paris meet.
Harrison ran the opening leg of the 1,600-relay at the world championships.
Ljungqvist disputed reports that Harrison's relay gold could be stripped because
of his positive test in June. He said IAAF's penalty for modafinil is a public
warning and disqualification from the competition where the test took place --
but no ban.
"He was eligible in our rules for the world championships," Ljungqvist said.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip-off, devised a test for the previously unknown and
undetectable steroid tetrahydrogestrinone, or THG.
While retesting for THG, U.S. officials discovered several positives for
modafinil.Ljungqvist said the IAAF had been "directly or indirectly" informed of
between six and eight modafinil cases.
Referring to White's narcolepsy defence, he said, "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: Paul Sakuma, the Associated Press; Victor Conte has been accused
of supplying athletes a new designer drug that's rocked track and field world.
TYPE: News
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701 of 998 DOCUMENTS
The Independent (London)
October 28, 2003, Tuesday
ATHLETICS: MODAFINIL IS DRUG OF CHOICE, SAYS IAAF CHIEF
BYLINE: MIKE ROWBOTTOM
SECTION: SPORT; Pg. 26
LENGTH: 419 words
MODAFINIL, THE drug which the world 100 metres champion, Kelli White, claims she
took for a sleep disorder, has become the "fashionable" stimulant of choice
among certain American athletes, the sport's top anti- doping official said
yesterday.
"It's a little odd to find an epidemic of narcolepsy in top athletes," Arne
Ljungqvist, the head of the International Association of Athletics Federations'
medical commission, said. "The disorder of narcolepsy is not that frequent."
Ljungqvist was speaking after the American 400m runner Calvin Harrison became
the latest athlete identified as having tested positive for the substance,
although Harrison's comments about his case appeared to make it clear that the
stimulant had not been recommended to him for any other reason than to keep him,
in his own words, "up".
The Olympic and world gold medallist, who has trained with Dwain Chambers in the
group supervised by the Ukrainian coach, Remy Korchemny, confirmed he had tested
positive for modafinil at this summer's American Championships.
"I did have modafinil in my system," Harrison said. He added that he was given
the substance by a coach in California, stressing that he had never been given
an illegal substance by his current coach, Trevor Graham.
"He the coach in California had given me this pill and I had taken it. He told
me it was not a steroid and that it would just keep you up' so you wouldn't be
so fatigued," Harrison said. "He emphasised that it was not on the banned
substance list and assured me that it was not an illegal substance."
Ljungqvist said a spate of positive tests for modafinil suggests the substance
is part of a pattern of doping abuse in the United States along with the
designer steroid THG.
Chambers, who tested positive for THG at an out-of-competition sampling on 1
August, will find out within the next fortnight whether his test is confirmed
through an analysis of the B sample.
Three other US athletes have now been named as testing positive for THG but
await B sample test results: Kevin Toth, the world's leading shot putter this
year; Regina Jacobs, the 39-year-old who broke the world indoor 1500m record
this year before beating Kelly Holmes to gold at the World Indoor Championships
in Birmingham; and the hammer thrower John McEwen. Two other US athletes who
have tested positive for THG have yet to be named.
Ljungqvist said the IAAF had been "directly or indirectly" informed of between
six and eight modafinil cases.
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Times Colonist (Victoria, British Columbia)
October 28, 2003 Tuesday Final Edition
Anti-doping officials focus on modafinil
SOURCE: Associated Press
SECTION: Sports; Pg. C2
LENGTH: 566 words
DATELINE: LONDON
LONDON (AP) -- Modafinil, the drug which sprinter Kelli White claims she took
for a sleep disorder, has become the "fashionable" stimulant of choice among
certain American athletes, track and field's top anti-doping official said
Monday.
"It's a little odd to find an epidemic of narcolepsy in top athletes," said Arne
Ljungqvist, medical commission chief of track and field's governing body. "The
disorder of narcolepsy is not that frequent."
Ljungqvist spoke after 400-metre runner Calvin Harrison became the latest
athlete identified as having tested positive for the drug.
In an interview with The Associated Press, Ljungqvist said a spate of positive
tests for modafinil suggests the substance is part of a pattern of doping abuse
in the United States along with the designer steroid THG.
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test -- a case
which could cost the U.S. an Olympic relay gold medal. Ljungqvist set a deadline
of Nov. 21 for the U.S. association to comply.
Harrison, an Olympic and world relay gold medallist, tested positive for
modafinil last summer, a source told the AP on Saturday. Harrison, still
awaiting the result of his backup B sample, was tested at the U.S. national
championships in June at Stanford.
Modafinil first came to prominence in August when White tested positive for the
drug at the world championships in Paris. She stands to be stripped of her
100-metre and 200-metre titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offence and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in the 110-metre
hurdles at the worlds, also tested positive for modafinil at the Paris meet.
Harrison ran the opening leg of the 1,600-relay at the world championships.
Ljungqvist disputed reports that Harrison's relay gold could be stripped because
of his positive test in June. He said the IAAF's penalty for modafinil is a
public warning and disqualification from the competition where the test took
place -- but no ban.
"He was eligible in our rules for the world championships," Ljungqvist said.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip-off, devised a test for the previously unknown and
undetectable steroid tetrahydrogestrinone, or THG. While retesting for THG, U.S.
officials discovered several positives for modafinil.
Ljungqvist said the IAAF had been "directly or indirectly" informed of between
six and eight modafinil cases.
Referring to White's narcolepsy defence, he said, "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
Ljungqvist, who is also head of the IOC's medical commission, said the evidence
suggests a link between THG and modafinil.
"What emerges now is a pattern," he said by phone from Sweden. "People have
taken THG for obvious reasons -- it's been designed with the intent not to be
discovered. And modafinil seems to have become a fashionable stimulant among
certain athletes as well. It's a pattern I've seen before, where drugs have
become popular and we find them."
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LANGUAGE: ENGLISH
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
703 of 998 DOCUMENTS
The Times (London)
October 28, 2003, Tuesday
Harrison to keep medal despite his positive test
BYLINE: Peter Nichols
SECTION: Sport; 42
LENGTH: 246 words
CALVIN HARRISON, the United States 400 metres runner who has admitted taking the
stimulant modafinil, will not be stripped of his World Championships relay gold
medal, according to Arne Ljungqvist, the head of the International Association
of Athletics Federations (IAAF) Medical Commission. "He was eligible in our
rules for the World Championships," Ljungqvist said.
Ljungqvist was citing the rule that, for stimulants in modafinil's class, the
athlete is disqualified from the competition only where the positive test has
taken place and receives a public warning. Since Harrison's positive came from
the re-test of samples taken at the US trials in California in June, IAAF
sanctions, according to Ljungqvist's interpretation, allow him to be
disqualified only from that championship.
Representatives of the US Anti-Doping Agency that re-tested the samples would
make no comment yesterday, but the ruling effectively undermines the re-analysis
of samples for stimulants in the modafinil class because, in many cases, the
only retrospective sanction available is a public warning. Nor will it seem like
justice to Kelli White, the American who tested positive for modafinil at the
World Championships in Paris. The ruling does allow White to be stripped of the
100 and 200 metres titles.
To date, three athletes have tested positive for the drug: Harrison, White and
Chris Phillips, who was fifth in the 110 metres hurdles in Paris.
Debate, page 35
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The Washington Post
October 28, 2003 Tuesday
Final Edition
Gaines Took Banned Drug;
She Is 4th Athlete Tied to Korchemny
BYLINE: Amy Shipley, Washington Post Staff Writer
SECTION: Sports; D01
LENGTH: 901 words
U.S. sprinter Chryste Gaines, who trains with Ukrainian-born coach Remi
Korchemny, tested positive for modafinil, a stimulant used to treat narcolepsy,
at the U.S. Track and Field Championships in July, according to international
officials with knowledge of the results.
Gaines is the fourth athlete connected to Korchemny to test positive for banned
drugs this summer. International Association of Athletics Federations General
Secretary Istvan Gyulai called the matter a "concern" and said the IAAF planned
to conduct an investigation.
Gaines, fellow sprinter Kelli White and hurdler Chris Phillips, all U.S.
athletes with ties to Korchemny, have tested positive for modafinil, a
prescription drug said to promote wakefulness that is commonly used to treat
sleep disorders. Another of Korchemny's athletes, British sprinter Dwain
Chambers, tested positive for the designer steroid tetrahydrogestrinone (THG).
"If it is proven that this coach was offering anything that is not a permissible
substance to athletes, that is the biggest concern to the IAAF," Gyulai said
yesterday.
The developments are the latest in a drug scandal that has enveloped track and
field since U.S. Anti-Doping Agency CEO Terry Madden publicly identified THG
about 10 days ago, saying the steroid was part of a "conspiracy" among coaches,
chemists and athletes to defraud the American public.
IAAF rules permit -- but do not define -- sanctions against anyone who assists
or incites a doping offense, Gyulai said.
White, Gaines and Chambers train frequently with Korchemny in the San Francisco
area. Phillips coaches himself, but he told the IAAF Korchemny gave him a
modafinil pill before the 110-meter hurdle semifinals at the August world
championships in Paris because he was having trouble sleeping, his agent Robert
Wagner said yesterday. Phillips finished fifth in the final.
Korchemny told The Post that he gave Phillips the modafinil, but only to resolve
his sleeping problem, not for performance enhancement. He said he had one pill
available because White had taken only one of the two she had at the world
championships.
Because modafinil is a Schedule IV controlled substance, it is illegal to
distribute it without a prescription in the United States.
"I had in my package one pill because Kelli took only one pill," Korchemny said.
"I'm sorry I did it . . . but it was not prohibited [under anti-doping rules]. .
. . I was 100 percent sure everything was legal."
Korchemny said he did not give modafinil to Gaines. He said he did not know she
had tested positive until informed by a reporter.
"I don't know anything about her [case]," Korchemny said. "She is my student,
but I don't know anything about her. I didn't give her" modafinil.
Gaines and her agent, Renaldo Nehemiah, have not returned repeated phone
messages in the last week.
Modafinil, marketed under the name Provigil, was not officially banned until
after the world championships, but drug-testing officials said it qualified as a
banned drug because of a broad clause in the anti-doping rules prohibiting
substances closely related to banned drugs.
Wagner, who also represents White, said it was "ridiculous" that the IAAF would
punish athletes for using substances not specifically banned. He said Phillips
and White had no idea they were consuming prohibited substances.
"The explanation Chris gave the IAAF was that Remi gave him a tablet in Paris
because he had problems sleeping," Wagner said. " . . . Everybody is taking
something to be alert and awake. . . . Some people drink five or six cups of
coffee, others people take modafinil. They were all under the impression
modafinil was okay."
Chambers's lawyer, Graham Shear, alleged in a statement that Korchemny made all
arrangements for Chambers's nutritional supplements through Bay Area Laboratory
Co-Operative (BALCO) and that Chambers had no idea that he was taking a banned
steroid when he consumed THG.
Korchemny said last week that Chambers made his own supplement arrangements with
BALCO and that he had never heard of THG before the positive tests were revealed
about 10 days ago.
After White tested positive for modafinil at the world championships, she said
she took the stimulant to treat the sleep disorder narcolepsy. She said a sample
of Provigil was given to her by her physician, Brian Goldman.
She told The Post she was informed by the USADA that she also tested positive
for the substance at the U.S. championships. If White is found guilty of a
doping offense, she is subject to losing the four gold medals she won at both
championships.
USADA officials allege that BALCO is the source of the designer steroid THG, for
which Chambers, middle-distance runner Regina Jacobs, U.S. shot put champion
Kevin Toth and hammer thrower John McEwan have tested positive this summer.
McEwan's positive was first reported by the Chicago Tribune. One unidentified
U.S. track and field athlete has also tested positive for THG.
BALCO is also the subject of a federal grand jury investigation. Noted BALCO
clients including Barry Bonds, Jason Giambi, White and Toth have been subpoenaed
to appear before the grand jury.
USADA officials said several U.S. athletes tested positive for modafinil this
summer, but declined to release their names. The positives were uncovered during
re-testing of some 350 samples from the U.S. championships and about 200
additional out-of-competition tests.
LOAD-DATE: October 28, 2003
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PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
705 of 998 DOCUMENTS
The Associated Press
October 27, 2003, Monday, BC cycle
AP Interview: Top track official sees pattern of doping abuse
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 534 words
DATELINE: LONDON
Two drugs under scrutiny in sports - modafinil and THG - are part of a pattern
of doping abuse in the United States, a top track and field executive said
Monday.
Arne Ljungqvist, the IAAF's medical commission chief, said the evidence suggests
a link between the substances.
Modafinil is the drug sprinter Kelli White says she took for a sleep disorder.
Tetrahydrogestrinone, or THG, is a previously undetectable designer steroid that
has turned up in the samples of several track and field athletes.
"What emerges now is a pattern," Ljungqvist told The Associated Press by phone
from Sweden. "People have taken THG for obvious reasons - it's been designed
with the intent not to be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
Ljungqvist spoke after 400-meter runner Calvin Harrison became the latest
athlete identified as having tested positive for modafinil.
Harrison, an Olympic and world relay gold medalist, tested positive for
modafinil this past summer, a source close to a U.S. doping investigation, told
the AP on Saturday on condition of anonymity.
Harrison, still awaiting the result of his backup B sample, was tested at the
U.S. national championships in June at Stanford, Calif.
Modafinil first came to prominence in August when White tested positive for the
drug at the world championships in Paris. She stands to be stripped of her
100-meter and 200-meter titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offense and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in the 110-meter
hurdles at the worlds, also tested positive for modafinil at the Paris meet.
Harrison ran the opening leg of the 1,600-relay at the worlds.
Ljungqvist said the IAAF's penalty for modafinil is a public warning and
disqualification from the competition where the test took place - but no ban.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip, devised a test for THG. While retesting, U.S.
officials discovered several positives for modafinil.
Ljungqvist said the IAAF had been "directly or indirectly" informed of six to
eight modafinil cases.
Referring to White's narcolepsy defense, he said: "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test - a case
that could cost the United States an Olympic relay gold medal. Ljungqvist set a
deadline of Nov. 21 for USATF to comply.
Young tested positive for the steroid nandrolone but was cleared on appeal by
USATF officials. He went on to win a 1,600-meter relay gold medal at the 2000
Olympics.
USATF officials have declined to provide the information, citing confidentiality
rules at the time.
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LANGUAGE: ENGLISH
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All Rights Reserved
706 of 998 DOCUMENTS
Associated Press Worldstream
October 27, 2003 Monday
AP Interview: IAAF official scoffs at 'narcolepsy epidemic'
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 736 words
DATELINE: LONDON
Modafinil, the drug which sprinter Kelli White claims she took for a sleep
disorder, has become the "fashionable" stimulant of choice among certain
American athletes, the sport's top anti-doping official said Monday.
"It's a little odd to find an epidemic of narcolepsy in top athletes," said Arne
Ljungqvist, medical commission chief of track and field's governing body. "The
disorder of narcolepsy is not that frequent."
Ljungqvist spoke after 400-meter runner Calvin Harrison became the latest
athlete identified as having tested positive for the drug.
In an interview with The Associated Press, Ljungqvist said a spate of positive
tests for modafinil suggests the substance is part of a pattern of doping abuse
in the United States along with the designer steroid THG.
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test - a case
which could cost the United States an Olympic relay gold medal. Ljungqvist set a
deadline of Nov. 21 for USATF to comply.
Harrison, an Olympic and world relay gold medalist, tested positive for
modafinil last summer, a source told the AP on Saturday. Harrison, still
awaiting the result of his backup B sample, was tested at the U.S. national
championships in June at Stanford.
Modafinil first came to prominence in August when White tested positive for the
drug at the World Championships in Paris. She stands to be stripped of her
100-meter and 200-meter titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offense and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in the 110-meter
hurdles at the worlds, also tested positive for modafinil at the Paris meet.
Harrison ran the opening leg of the 1,600-relay at the World Championships.
Ljungqvist disputed reports that Harrison's relay gold could be stripped because
of his positive test in June. He said the IAAF's penalty for modafinil is a
public warning and disqualification from the competition where the test took
place - but no ban.
"He was eligible in our rules for the World Championships," Ljungqvist said.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip-off, devised a test for the previously unknown and
undetectable steroid tetrahydrogestrinone, or THG.
While retesting for THG, U.S. officials discovered several positives for
modafinil.
Ljungqvist said the IAAF had been "directly or indirectly" informed of between
six and eight modafinil cases.
Referring to White's narcolepsy defense, he said, "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
Ljungqvist, who is also head of the IOC's medical commission, said the evidence
suggests a link between THG and modafinil.
"What emerges now is a pattern," he said by phone from Sweden. "People have
taken THG for obvious reasons - it's been designed with the intent not to be
discovered. And modafinil seems to have become a fashionable stimulant among
certain athletes as well. It's a pattern I've seen before, where drugs have
become popular and we find them."
Meanwhile, Ljungqvist said the IAAF has sent a second letter to USATF requesting
explanation for Young's exoneration in 1999.
Young tested positive for the steroid nandrolone, but was cleared on appeal by
USATF officials and went on to win a 1,600-meter relay gold medal at the 2000
Sydney Olympics.
The International Olympic Committee started disciplinary proceedings last month
which could result in Young and the rest of the team losing the gold medal.
USATF officials have declined to provide the information, citing confidentiality
rules in place at the time and an arbitration court ruling upholding their right
not to disclose details of 13 positive cases from 1996-2000.
Ljungqvist said the IAAF had received some documents from the USOC but "one
crucial piece" was still missing - a witness statement upon which the USATF
appeals board based its decision to clear Young.
The IAAF must have the information before the Nov. 21-23 meeting of its
decision-making Council in Berlin or else "we will have a big new problem,"
Ljungqvist said.
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LANGUAGE: ENGLISH
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All Rights Reserved
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Associated Press Online
October 27, 2003 Monday
AP Interview: Track Chief Discusses Doping
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 531 words
DATELINE: LONDON
Two drugs under scrutiny in sports - modafinil and THG - are part of a pattern
of doping abuse in the United States, a top track and field executive said
Monday.
Arne Ljungqvist, the IAAF's medical commission chief, said the evidence suggests
a link between the substances.
Modafinil is the drug sprinter Kelli White says she took for a sleep disorder.
Tetrahydrogestrinone, or THG, is a previously undetectable designer steroid that
has turned up in the samples of several track and field athletes.
"What emerges now is a pattern," Ljungqvist told The Associated Press by phone
from Sweden. "People have taken THG for obvious reasons - it's been designed
with the intent not to be discovered.
"And modafinil seems to have become a fashionable stimulant among certain
athletes as well. It's a pattern I've seen before, where drugs have become
popular and we find them."
Ljungqvist spoke after 400-meter runner Calvin Harrison became the latest
athlete identified as having tested positive for modafinil.
Harrison, an Olympic and world relay gold medalist, tested positive for
modafinil this past summer, a source close to a U.S. doping investigation, told
the AP on Saturday on condition of anonymity.
Harrison, still awaiting the result of his backup B sample, was tested at the
U.S. national championships in June at Stanford, Calif.
Modafinil first came to prominence in August when White tested positive for the
drug at the world championships in Paris. She stands to be stripped of her
100-meter and 200-meter titles.
White said she took modafinil on prescription from her personal doctor to combat
narcolepsy. The International Association of Athletics Federations charged her
with a doping offense and submitted her case to U.S. authorities for
disciplinary action.
Another U.S. athlete, Chris Phillips, who finished fifth in the 110-meter
hurdles at the worlds, also tested positive for modafinil at the Paris meet.
Harrison ran the opening leg of the 1,600-relay at the worlds.
Ljungqvist said the IAAF's penalty for modafinil is a public warning and
disqualification from the competition where the test took place - but no ban.
Samples from the U.S. championships were retested after the UCLA doping control
laboratory, acting on a tip, devised a test for THG. While retesting, U.S.
officials discovered several positives for modafinil.
Ljungqvist said the IAAF had been "directly or indirectly" informed of six to
eight modafinil cases.
Referring to White's narcolepsy defense, he said: "It comes into a different
sort of light when it becomes known that modafinil has been taken by a number of
athletes."
On another drug issue, Ljungqvist said USA Track & Field still has not provided
the required documents on Jerome Young's 1999 positive steroid test - a case
that could cost the United States an Olympic relay gold medal. Ljungqvist set a
deadline of Nov. 21 for USATF to comply.
Young tested positive for the steroid nandrolone but was cleared on appeal by
USATF officials. He went on to win a 1,600-meter relay gold medal at the 2000
Olympics.
USATF officials have declined to provide the information, citing confidentiality
rules at the time.
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LANGUAGE: ENGLISH
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All Rights Reserved
708 of 998 DOCUMENTS
The Australian
October 27, 2003 Monday All-round Country Edition
Stimulant cloud over Harrison
SOURCE: Reuters, The Times
SECTION: SPORT-BIOG- CALVIN HARRISON; Pg. 24
LENGTH: 538 words
* Drugs
IN the latest in a series of scandals to rock athletics, Olympic 4x400m relay
gold medallist Calvin Harrison admitted yesterday he had tested positive for the
banned stimulant modafinil.
Harrison's positive test comes in the wake of revelations that four US athletes
and Britain's European 100m champion Dwain Chambers had tested positive to the
previously undetectable designer steroid tetrahydrogestrinone.
Dozens of other athletes, including Marion Jones and Tim Montgomery, have been
engulfed in the THG scandal through their links to Victor Conte, the head of the
company that has been identified as the drug's source.
"Yes, I tested positive for modafinil at the (US) nationals," Harrison said. "I
was notified that they (the US Anti-Doping Agency) had tested my A sample and
that they would test my B sample, which they probably have by now.
"I did have modafinil in my system. However, I am not in the least advocating
the taking of any illegal substances because I strongly believe in fair play."
Harrison, 29, is alleged to be one of up to 12 athletes who have tested positive
for the stimulant in re-tests from the meeting in Stanford, California. He said
he was given the substance by a coach in California.
But the athlete stressed he had never been given an illegal substance by his
current coach, Trevor Graham.
"He (the coach in California) had given me this pill and I had taken it,"
Harrison said. "He told me it was not a steroid and that it would just keep you
up so you wouldn't be so fatigued.
"He emphasised that it was not on the banned substance list and assured me that
it was not an illegal substance."
Modafinil is the same stimulant to which double world sprint champion Kelli
White of the US tested positive at the world championships in Paris in August.
While not specified by name on the banned list at the time, modafinil was
covered under the stimulants category of "related substances", the International
Association of Athletics Federations said.
Modafinil has since been added to the list. White, who is also a client of
Conte, owner of the Bay Area Laboratory Co-operative (BALCO), has said she was
prescribed the drug for a sleeping disorder.
Her case is under review by the US Anti-Doping Agency. If she is found to have
committed a doping offence, she could lose her Paris gold medals.
Harrison's positive, if confirmed by the testing of his B urine sample, could
also put in jeopardy the 4x400m relay gold medal the US won at the world
championships, as he ran the opening leg.
He was also a member of the victorious 2000 Olympics 4x400m relay team, who
could have their gold medal taken away because Jerome Young ran in the early
rounds after failing a 1999 doping test.
The International Olympic Committee has called for an investigation into why
Young was allowed to run.
The four US athletes to have tested positive to THG include US shot put champion
Kevin Toth, world indoor 1500m champion Regina Jacobs and US hammer thrower John
McEwen. The fourth athlete is yet to be identified.
A group of 40 athletes and sports stars have been subpoenaed to give evidence to
a US federal grand jury investigation into BALCO's finances.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: AUS
Copyright 2003 Nationwide News Pty Limited
709 of 998 DOCUMENTS
The Daily Telegraph (Sydney, Australia)
October 27, 2003 Monday
Now US Olympic gold sprinter tests positive
SOURCE: MATP
BYLINE: GENE CHERRY
SECTION: SPORT-BIOG- CALVIN HARRISON; Pg. 29
LENGTH: 290 words
AMERICAN sprinter Calvin Harrison has tested positive for banned stimulant
modafinil, he revealed yesterday.
"I tested positive for modafinil at the [US] nationals," the US Sydney Olympics
4x400m relay gold medallist said.
"I was notified [the US Anti-Doping Agency] had tested my A sample and that they
would test my B sample." Harrison's modafinil positive is the latest in a
series of drug shocks that have rocked track and field and could leave next
year's Athens Olympics missing a host of big names.
It follows the discovery of the previously undetectable designer steroid THG, or
tetrahydrogestrinone.
American officials say four US athletes have tested positive for THG, as has
Britain's 100m star Dwain Chambers.
"I did have modafinil in my system," Harrison said.
"However, I am not advocating the taking of any illegal substances because I
strongly believe in fair play." Harrison said he was given the substance by a
former coach in California.
"He had given me this pill and I had taken it. He told me it was not a steroid
and would just keep you 'up' so you wouldn't be so fatigued.
"He emphasised that it was not on the banned substance list and assured me that
it was not an illegal substance." Modafinil is the stimulant for which US
double world sprint champion Kelli White tested positive at the world
championships in Paris in August.
It is not specifically named on the banned list, but the International
Association of Athletics Federations (IAAF) has said it falls into the category
of "related substances".
If Harrison's positive test is confirmed, the US could be stripped of its 4x400
metres relay gold medal at this year's world championships, where he ran the
opening leg.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: DTM
Copyright 2003 Nationwide News Pty Limited
710 of 998 DOCUMENTS
Gold Coast Bulletin (Australia)
October 27, 2003 Monday
Positive test for US star
SECTION: SPORT; Pg. 33
LENGTH: 249 words
Athletics
US Olympic 4x400m relay gold medallist Calvin Harrison has tested positive for
the banned stimulant modafinil.
"Yes, I tested positive for modafinil at the (US) nationals," said Harrison.
"I was notified they (the US Anti-Doping Agency) had tested my A sample and
they would test my B sample, which they probably have by now."
Harrison's modafinil positive is the latest in a series of positive tests
which have rocked track and field on both sides of the Atlantic and could leave
next year's Athens Olympics missing a host of banned big-name athletes.
It also follows the discovery of the previously undetectable designer steroid
tetrahydrogestrinone THG.
Four US athletes have tested positive for the steroid, American officials
have said, as has Britain's European 100m champion Dwain Chambers, who said
through his lawyer if he did take the drug it was unwittingly.
"I did have modafinil in my system," said Harrison.
"However, I am not in the least advocating the taking of any illegal
substances because I strongly believe in fair play."
Harrison said he was given the substance by a coach in California.
But the athlete stressed he had never been given an illegal substance by his
current coach, Trevor Graham.
"He (the coach in California) had given me this pill and I had taken it. He
told me it was not a steroid and it would just keep you 'up' so you wouldn't be
so fatigued," said Harrison.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: GCB
Copyright 2003 Nationwide News Pty Limited
711 of 998 DOCUMENTS
The Guardian - Final Edition
October 27, 2003
Athletics: Harrison blames controversial coach for positive test
BYLINE: Duncan Mackay
SECTION: Guardian Sport Pages, Pg. 26
LENGTH: 402 words
The Olympic and world gold medallist Calvin Harrison, an occasional training
partner of Britain's Dwain Chambers, has admitted he is the latest top American
athlete to have tested positive for banned performance-enhancing drugs.
Harrison has confirmed that he has failed a test for modafinil, the stimulant
prescribed to treat narcolepsy.
Sources close to the case claim that Harrison has alleged he was given the
banned substance by Remi Korchemny, the San Francisco-based coach whom Chambers
was working under when he tested positive for the banned designer anabolic
steroid tetrahydrogestrinone (THG).
Harrison's positive test is the latest in a series of positive tests that have
rocked the sport on both sides of the Atlantic and could leave next year's
Athens Olympic Games missing a number of banned big-name athletes.
"I did have modafinil in my system," Harrison said. "However, I am not in the
least advocating the taking of any illegal substances because I strongly believe
in fair play."
Modafinil is the drug that has put Kelli White's 100 and 200m titles from the
world championships at risk. Like Harrison, White claims she took modafinil for
narcolepsy. Korchemny is her coach.
Harrison said a coach in California gave him the substance. But he stressed he
had never been given an illegal substance by his current coach, Trevor Graham,
who has previously worked with the world's leading female and male sprinters
Marion Jones and Tim Montgomery.
"He (the coach in California) had given me this pill and I had taken it. He told
me it was not a steroid and that it would just keep you 'up' so you wouldn't be
so fatigued," said Harrison. "He emphasised that it was not on the banned
substance list and assured me it was not an illegal substance."
Harrison, who rose to prominence in track and field with his twin brother Alvin
in the late 1990s, was a member of the American team who won the 4x400 metres
relay in the 2000 Sydney Olympics and the world championships in Paris.
His positive test came to light after 350 samples from the US championships in
Stanford in June were retested after American anti-doping officials were given a
used syringe by an unidentified track coach containing the previously
undetectable THG.
Sources have warned that more major names from America may come out this week as
having tested positive for THG and modafinil.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
Copyright 2003 Guardian Newspapers Limited
712 of 998 DOCUMENTS
Illawarra Mercury (Australia)
October 27, 2003 Monday
Late Edition
US sprinter admits positive test
SECTION: SPORT MONDAY; Pg. 37
LENGTH: 175 words
RALEIGH, North Carolina.- US Olympic 4x400m relay gold medallist Calvin Harrison
has tested positive for the banned stimulant modafinil.
"Yes, I tested positive for modafinil at the (US) nationals," Harrison said in a
telephone interview from his North Carolina home.
"I was notified that they (the US Anti-Doping Agency) had tested my A sample and
that they would test my B sample, which they probably have by now."
Harrison's modafinil positive is the latest in a series of positive tests which
have rocked track and field on both sides of the Atlantic and could leave next
year's Athens Olympics missing a host of banned big-name athletes.
It also follows the discovery of the previously undetectable designer steroid
tetrahydrogestrinone THG.
Four US athletes have tested positive for the steroid, American officials have
said, as has Britain's European 100m champion Dwain Chambers.
"I did have modafinil in my system," Harrison said.
"However, I am not in the least advocating the taking of any illegal substances
because I strongly believe in fair play."
LOAD-DATE: June 19, 2007
LANGUAGE: ENGLISH
GRAPHIC: Illus: CALVIN HARRISON
PUBLICATION-TYPE: Newspaper
Copyright 2003 Illawarra Newspapers Holdings Pty Ltd
All Rights Reserved
713 of 998 DOCUMENTS
The Straits Times (Singapore)
Champion tests positive
October 27, 2003 Monday
RALEIGH (North Carolina) - Calvin Harrison has tested positive for the banned
stimulant modafinil, the US Olympic and world 4x400 metres relay gold medallist
told Reuters on Saturday.
'Yes, I tested positive for modafinil at the US nationals,' he said in a
telephone interview.
He said he was notified that the US Anti-Doping Agency had tested his A sample
and that they would test his B sample.
This is the latest in a series of positive drugs tests which have rocked track
and field on both sides of the Atlantic. It also follows the discovery of the
previously undetectable designer steroid tetrahydrogestrinone THG.
Harrison said he was given the substance by a coach - 'who emphasised it was not
on the banned substance list' - in California.
But the runner stressed he had never been given an illegal substance by current
coach Trevor Graham.
Modafinil is the same stimulant that American double world sprint champion Kelli
White tested positive for at the World Championships in Paris last August.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of 'related substances'.
Harrison's positive, if confirmed by the testing of his B urine sample, could
put in jeopardy the 4x400m gold won in Paris, as he ran the opening leg.
SECTION: WHATS IN; Sports
LENGTH: 216 words
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
Copyright 2003 Singapore Press Holdings Limited
714 of 998 DOCUMENTS
The Times (London)
October 27, 2003, Monday
Harrison a sample of things to come
SECTION: Sport; 35
LENGTH: 263 words
THE positive test for modafinil that has shown up on the re-tested sample of
Calvin Harrison, the United States 400 metres runner, could be the first of
many.
Harrison's sample was just one of about 350 taken at the US Trials at Stanford
in June, all of which are being re-tested.
The re-testing programme was initiated by the US Anti-Drug Agency after the
development of new protocols to identify tetrahydrogestrinone (THG), the
designer steroid. But there was no test for modafinil, so that procedure was
added. Modafinil came to light in athletics circles only at the World
Championships in Paris in August, when Kelli White, the US sprinter and winner
of the 100 metres and 200 metres, tested positive for the drug. White, like
Harrison and Dwain Chambers, the British sprinter, has been advised by Remi
Korchemny, the coach with links to the Bay Area Laboratory Co-operative (Balco),
at present the subject of a Grand Jury investigation in San Francisco.
White claimed that she was prescribed the drug for a sleeping disorder, but even
if her story is accepted, the sprinter still stands to lose both titles.
Harrison also won gold in Paris, leading off the US relay team in the 4 x 400m
final, and, if his positive test is confirmed, he and his team-mates stand to be
disqualified.
Harrison, 29 was also part of the gold-medal winning US relay squad at the 2000
Olympic Games, and that medal could be lost if the International Olympic
Committee decides that Jerome Young, who failed a drugs test in 1999, should not
have been allowed to compete.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
Copyright 2003 Times Newspapers Limited
715 of 998 DOCUMENTS
Townsville Bulletin/Townsville Sun (Australia)
October 27, 2003 Monday
Harrison positive
SECTION: SPORT; Pg. 18
LENGTH: 185 words
RALEIGH, North Carolina -- Calvin Harrison has tested positive for the banned
stimulant modafinil, the US Olympic 4x400m relay gold medallist said yesterday.
"Yes, I tested positive for modafinil at the (US) nationals," Harrison said.
"I was notified that they (the US Anti-Doping Agency) had tested my A sample and
that they would test my B sample, which they probably have by now."
Harrison's result is the latest in a series of positive tests which have rocked
track and field on both sides of the Atlantic and could leave next year's Athens
Olympics missing a host of banned big-name athletes.
It also follows the discovery of the previously undetectable designer steroid
tetrahydrogestrinone THG.
Four US athletes have tested positive for the steroid, American officials have
said, as has Britain's European 100m champion Dwain Chambers, who said through
his lawyer that if he did take the drug it was unwittingly.
"I did have modafinil in my system," Harrison said.
"However, I am not in the least advocating the taking of any illegal substances
because I strongly believe in fair play."
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: BUL
Copyright 2003 Nationwide News Pty Limited
716 of 998 DOCUMENTS
Associated Press Worldstream
October 26, 2003 Sunday
Correction Appended
Source: Relay gold medalist flunked test for modafinil
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 410 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said
Saturday, speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, California.
Harrison finished second in the 400 meters at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
CORRECTION-DATE: October 28, 2003 Tuesday
CORRECTION: In an Oct. 25 story about runner Calvin Harrison testing positive
for the stimulant modafinil, The Associated Press reported erroneously that
Harrison could face a two-year suspension and miss the 2004 Athens Olympics.
The penalty for modafinil use is disqualification from the competition where
the test took place, not a two-year ban.
Copyright 2003 Associated Press
All Rights Reserved
717 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 26, 2003, Sunday, BC cycle
Correction Appended
Source: Relay gold medalist flunked test for modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 421 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison, who graduated from North Salinas High School in 1993, finished second
in the 400 meters at that meet, making the U.S. team for the world championships
and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
CORRECTION-DATE: October 28, 2003, Tuesday
CORRECTION:
In an Oct. 25 story about runner Calvin Harrison testing positive for the
stimulant modafinil, The Associated Press reported erroneously that Harrison
could face a two-year suspension and miss the 2004 Athens Olympics.
The penalty for modafinil use is disqualification from the competition where the
test took place, not a two-year ban.
718 of 998 DOCUMENTS
Associated Press Online
October 26, 2003 Sunday
Correction Appended
Source: Runner Harrison Flunked Drug Test
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 410 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison finished second in the 400 meters at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
CORRECTION-DATE: October 28, 2003 Tuesday
CORRECTION: In an Oct. 25 story about runner Calvin Harrison testing positive
for the stimulant modafinil, The Associated Press reported erroneously that
Harrison could face a two-year suspension and miss the 2004 Athens Olympics.
The penalty for modafinil use is disqualification from the competition where the
test took place, not a two-year ban.
Copyright 2003 Associated Press
All Rights Reserved
719 of 998 DOCUMENTS
Calgary Herald (Alberta, Canada)
October 26, 2003 Sunday Final Edition
Olympic champion Harrison fails drug test
SOURCE: The Associated Press
SECTION: Sports; Pg. B2
LENGTH: 428 words
Olympic and world relay gold medallist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 4x400-metre relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison finished second in the 400 metres at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison.
Korchemny is the coach of British sprinter Dwain Chambers, the only athlete to
publicly announce he tested positive for THG.
Meanwhile, the National Football League is rechecking players' drug tests to
look for the newly identified steroid THG.
The USADA received a used syringe containing the designer steroid from an
anonymous coach and then began retesting samples of track and field athletes.
NFL spokesman Greg Aiello said Saturday "as soon as the report came out about
THG, we said we would be testing for it and we are."
That includes previously taken urine samples that were tested by the NFL for
other drugs.
An NFL player testing positive for steroids receives a four-game suspension for
the first offence.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
720 of 998 DOCUMENTS
San Jose Mercury News (California)
October 26, 2003 Sunday MORNING FINAL EDITION
DRUG SCANDAL INVOLVES SALINAS' CALVIN HARRISON
BYLINE: MARK EMMONS, Mercury News
SECTION: FRONT; Pg. 27A
LENGTH: 220 words
Another prominent track-and-field name has surfaced in the sport's "other" drug
scandal. U.S. Olympic 4x400-meter relay gold medalist Calvin Harrison reportedly
has tested positive for the banned stimulant modafinil. The positive test came
from a drug test conducted during the summer, sources told Reuters.
Harrison becomes the third American to test for modafinil. Union City sprinter
Kelli White, who tested positive in August, risks losing two gold medals she won
at the World Championships in Paris. White, who trains with East Bay coach Remi
Korchemny, claims that she was given the drug to combat the sleeping disorder
narcolepsy. American hurdler Chris Phillips, who uses Korchemny as a consultant,
also tested positive.
Harrison, according the various track Web sites, has been a member of ZMA Track
Club -- which was formed by Korchemny and Victor Conte, the nutritionist and
owner the Burlingame laboratory that is currently under investigation as the
possible source of a new designer steroid. Calvin Harrison and his twin brother
Alvin both were track stars at North Salinas High.
The positive test, if confirmed by a second sample, could put in jeopardy the
United States' 4x400 gold medal at the World Championships because Calvin
Harrison ran the opening leg on the Americans' winning team.
LOAD-DATE: August 17, 2005
LANGUAGE: ENGLISH
NOTES: RELATED STORY, PAGE 1A
GRAPHIC: Photo;
PHOTO: KAREN T. BORCHERS -- MERCURY NEWS ARCHIVES
Calvin Harrison reportedly tested positive for the banned stimulant modafinil
this summer.
Copyright 2003 San Jose Mercury News
All Rights Reserved
721 of 998 DOCUMENTS
The Times Union (Albany, NY)
October 26, 2003 Sunday THREE STAR EDITION
Tests find new stimulant
BYLINE: Combined Wire Services
SECTION: SPORTS, Pg. C2
LENGTH: 506 words
Sprinter Calvin Harrison, a gold medalist in the relays at the Sydney Olympic
Games, tested positive this summer for the stimulant modafinil, sources told the
Los Angeles Times, adding that at least half a dozen U.S. athletes might have
tested positive for the same stimulant.
The positive testing for modafinil showed up when the U.S. Anti-Doping Agency
reviewed tests taken at the U.S. national track championships at Stanford in
June and after the agency learned of a new designer steroid,
tetrahydrogestrinone, or THG.
Modafinil was recently added to the list of banned performance-enhancing
substances.
Track's worldwide governing body, the International Assn. of Athletics
Federations, has said it plans to retest about 400 samples from the world
championships in August in Paris for THG.
FIGURE SKATING Tanith Belbin and Benjamin Agosto became the first U.S. ice
dance team to take a Grand Prix event in six years when they won Skate America
in Reading, Pa. Belbin and Agosto, ranked seventh in the world, easily won the
free dance with a rousing performance to "West Side Story." They edged Ukraine's
Elena Grushina and Ruslan Goncharov, who won the compulsories.
Belbin and Agosto finished with 212.08 points. Grushina and Goncharov were at
197.66.
TRIATHLON
Rasmus Henning of Denmark won the triathlon World Cup by 0.03 seconds in
Vouliagmeni, Greece, when Cedric Fleureton of France stumbled at the finish of
the 10-kilometer run. Michellie Jones of Australia won the women's division of
the competition, which served as an Olympic test event.
Henning, who edged Cedric Fleureton of France in a photo finish, completed the
1.5-kilometer swim, 40-kilometer cycle and the closing run in 1 hour, 52
minutes, 41.93 seconds. Among the women, Jones, the Olympic silver medalist,
beat Britain's Jodie Swallow by 1.30 seconds, finishing in 2:06:47.02.
TENNIS
Top-seeded Andy Roddick was knocked off by David Nalbandian 7-5, 7-5 in the
semifinals of the Swiss Indoors in Basel. It was a rematch from the U.S. Open
semifinals, where Roddick overcame a two-set deficit and a match point to win en
route to his first Grand Slam title. Nalbandian will play Guillermo Coria in an
all-Argentine final today. Coria eliminated Ivan Ljubicic 6-4, 6-4. Kim
Clijsters overwhelmed 16-year-old Maria Sharapova 6-0, 6-3 in the SEAT Open
semifinals in Luxembourg. Clijsters, who will regain the No. 1 ranking next
week, will play Chanda Rubin in the final. SKIING Martina Ertl of Germany
opened the World Cup ski season by winning a giant slalom in Soelden, Austria,
for her first victory in three years. She had a two-run time of 2 minutes, 31.86
seconds in recording her 14th World Cup victory. Veikko Hakulinen, a Finnish
cross-country skier who won three Olympic gold medals, died after being hit by a
car in Helsinki, police said. He was 78. Hakulinen's victories began with the
50-kilometer race at the 1952 Oslo Olympics. In all, he won three golds, three
silvers and one bronze at Olympics.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Hearst Corporation
722 of 998 DOCUMENTS
The Washington Post
October 26, 2003 Sunday
Final Edition
U.S.'s Harrison Tests Positive for Stimulant
BYLINE: From News Services
SECTION: Sports; E02
LENGTH: 574 words
Calvin Harrison has tested positive for the banned stimulant modafinil, the U.S.
Olympic 4x400-meter relay gold medalist told Reuters yesterday.
"Yes, I tested positive for modafinil at the [U.S.] nationals," Harrison said in
a telephone interview. "I was notified that they [the U.S. Anti-Doping Agency]
had tested my A sample and that they would test my B sample, which they probably
have by now."
Harrison's modafinil positive test is the latest in a series of positive tests
that have rocked track and field on both sides of the Atlantic and could leave
next year's Athens Olympics missing a number of banned big-name athletes.
It also follows the discovery of the previously undetectable designer steroid
tetrahydrogestrinone (THG).
"I did have modafinil in my system," Harrison said. "However, I am not in the
least advocating the taking of any illegal substances because I strongly believe
in fair play."
Skiing
Martina Ertl of Germany opened the World Cup season by winning a giant slalom in
Soelden, Austria, her first victory in three years.
"This is absolutely sensational," Ertl said. "I've been waiting so long."
She had a two-run time of 2 minutes 31.86 seconds in recording her 14th World
Cup victory.
Anja Paerson of Sweden, the World Cup champion and reigning world championship
gold medalist, was second in 2:32.06. Maria Jose Rienda Contreras was third in
2:32.25, giving Spain its first top-three finish since Carolina Ruiz Castillo in
2000.
Sarah Schleper of the United States was seventh in 2:34.30.
"I'm psyched," Schleper said. "The atmosphere on our team is getting better and
better."
Teammate Kirsten Clark was 23rd and Caroline Lalive was 28th.
Ertl's last World Cup victory was a giant slalom on the same site in October
2000. She has struggled since a series of knee injuries in that season.
The German was third in the 2002 Olympic combined event, which adds the downhill
and slalom times.
"It's been two years that I've been injury-free, but it has been a long road
back to the top," Ertl said. "I am lucky that I am a person who has a lot of
energy and determination and I really wanted to fight."
Schleper was tied for 13th after the first run, then rose to seventh after
posting the fifth-fastest second run.
"I'm believing more and more in myself," she said.
The men's World Cup season opens today with a giant slalom. . . .
In Duesseldorf, Germany, Sweden's Peter Larsson and Italy's Gabriela Paruzzi won
the opening races of the World Cup cross-country season.
Larsson was first in the one-kilometer sprint for the second straight year.
Martin Koukal of the Czech Republic was second, followed by Thobias Fredriksson
of Sweden. Swedish men captured five of the top eight places.
Among the women, Russians Olena Sidko and Yevgenia Chachina were second and
third. German biathlon star Uschi Disl was a surprising fourth.
Tennis
David Nalbandian upset top-seeded Andy Roddick, 7-5, 7-5, in the semifinals of
the Swiss Indoors in Basel.
It was a rematch from the U.S. Open semifinals, in which Roddick overcame a
two-set deficit and a match point to win en route to his first Grand Slam title.
Nalbandian will play Guillermo Coria in an all-Argentine final today. Coria
eliminated Ivan Ljubicic, 6-4, 6-4. Both finalists are playing in their first
tournament since the U.S. Open, having taken time off because of injuries.
Nalbandian beat Roddick with impressive returns and passing shots.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
723 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
October 26, 2003, Sunday
American Harrison tests positive for stimulant
SECTION: WORLD NEWS; SPORTS
LENGTH: 216 words
WASHINGTON, Oct. 25 (Xinhua) -- American Calvin Harrison, winning member of the
U.S. Olympic 4x400 meters relay team, has tested positive for stimulant
modafinil, sources close to the anti-doping program said on Saturday.
Harrison's A sample tested positive this summer, but he ran the opening leg on
the US 4x400m winning team at the world championships in Paris last August.
If his positive is confirmed by the B sample, the United States might be
stripped of its world and Olympic titles in the 4x400m relay as Jerome Young
also ran in the early Olympic rounds of relay after failing a 1999 doping test.
World 100 and 200m woman champion Kelli White also tested positive for the same
stimulant at the world championships, and her case is under review by the U.S.
Anti-Doping Agency.
Harrison's modafinil positive is the latest in the doping scandal that has
rocked the track and field world, followed the discovery of designer steroid
tetrahydrogestrinone (THG).
Four positives for THG and a number for the stimulant modafinil were found at
the re-testing of urine samples from the U.S. championships in June, the
sources said.
Britain's European 100m champion Dwain Chambers, and US world indoor 1,500m
record holder Regina Jacobs also tested positive for the THG.
LOAD-DATE: October 27, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
724 of 998 DOCUMENTS
The Associated Press
October 25, 2003, Saturday, BC cycle
Correction Appended
Source: Relay gold medalist flunked test for modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 412 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison finished second in the 400 meters at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
CORRECTION-DATE: October 28, 2003, Tuesday
CORRECTION: In an Oct. 25 story about runner Calvin Harrison testing positive
for the stimulant modafinil, The Associated Press reported erroneously that
Harrison could face a two-year suspension and miss the 2004 Athens Olympics.
The penalty for modafinil use is disqualification from the competition where the
test took place, not a two-year ban.
Copyright 2003 Associated Press
All Rights Reserved
725 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 25, 2003, Saturday, BC cycle
Correction Appended
Source: Relay gold medalist flunked test for modafinil
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 412 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison finished second in the 400 meters at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
CORRECTION-DATE: October 28, 2003, Tuesday
CORRECTION:
In an Oct. 25 story about runner Calvin Harrison testing positive for the
stimulant modafinil, The Associated Press reported erroneously that Harrison
could face a two-year suspension and miss the 2004 Athens Olympics.
The penalty for modafinil use is disqualification from the competition where the
test took place, not a two-year ban.
726 of 998 DOCUMENTS
Associated Press Online
October 25, 2003 Saturday
Source: Runner Harrison Flunked Drug Test
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 410 words
DATELINE: SAN FRANCISCO
Olympic and world relay gold medalist Calvin Harrison tested positive for a
banned stimulant, a source told The Associated Press on Saturday.
Harrison, a member of the winning U.S. 1,600-meter relay team at the 2000
Olympics and this summer's world championships, tested positive for the
stimulant modafinil, a source close to a U.S. anti-doping investigation said,
speaking on the condition of anonymity.
The Los Angeles Times reported Saturday that Harrison's flunked drug test was
believed to be from a urine sample taken at the U.S. track and field
championships in June at Stanford, Calif.
Harrison finished second in the 400 meters at that meet, making the U.S. team
for the world championships and qualifying for a spot on the relay squad.
Harrison, who rose to prominence in track and field with his twin brother,
Alvin, in the late 1990s, could not immediately be reached for comment.
Some 350 samples from the Stanford meet were retested after U.S. anti-doping
officials were given a used syringe by an unidentified track coach containing a
substance that turned out to be the previously undetectable designer steroid
THG.
While retesting for THG, officials discovered several positive tests for
modafinil, U.S. Anti-Doping Agency chief executive Terry Madden said last week.
The names of those athletes have not been released by the USADA.
Harrison tested positive on his "A" sample, but results of his "B" sample were
not yet available, the source said.
If confirmed as a positive test, Harrison could face a two-year suspension and
miss the 2004 Athens Olympics.
Modafinil is the same drug that has put Kelli White's 100 and 200 titles from
the world championships at risk. White claims she took modafinil for the sleep
disorder narcolepsy.
White is coached by Remi Korchemny, who has also worked with Harrison. Korchemny
is the coach of British sprinter Dwain Chambers, the only athlete to publicly
announce he tested positive for THG.
Harrison ran the first leg of the 1,600 relay at the world championships. The
anchor leg was run by Jerome Young, who is engulfed in controversy because of a
failed doping test in 1999.
At the 2000 Olympics, Harrison ran the third leg of the winning U.S. 1,600 squad
that was anchored by Michael Johnson. Young ran in the preliminary and semifinal
rounds for that squad, just weeks after being cleared by U.S. officials in a
process now under scrutiny by international sports authorities.
LOAD-DATE: October 26, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
727 of 998 DOCUMENTS
CTV Television, Inc.
23:00:00 - 23:30:00 Eastern Time
SHOW: CTV NEWS
October 25, 2003, Saturday
New pill makes weary persons alert
ANCHOR: SANDIE RINALDO
LENGTH: 478 words
SANDIE RINALDO: Sunday at 2:00 a.m., much of the country says
good-bye to daylight saving time. Most of us will set our clocks back an hour
and it seems many could use the extra sleep. A poll commissioned by the
Better Sleep Council of Canada says more than one-third of us gets less than
six hours of sleep a night. Soon, there will be a pill on the US market that
could
help the weary stay alert. But as CTV's Genevieve Beauchemin shows us,
Canadian experts warn it is not for everyone.
GENEVIEVE BEAUCHEMIN [Reporter]: For twenty-three years, nurse Inge
Decastris has helped moms deliver their babies day and night.
INGE DECASTRIS [St. Mary's Hospital Nurse]: During the night, around three
o'clock, you're ready, your eyes start to droop if you're not really busy and
active.
BEAUCHEMIN: But a pill promises to perk up the sleep deprived. The US Food
and Drug Administration and Health Canada approved Modafinil for the
treatment of narcolepsy in the late 1990s. Now the United States is set to
approve it for wider use, including for shift workers desperate to stay alert.
And
that has caused controversy over whether that should happen in Canada too.
Dr. Ross Pigeau studied Modafinil's effects for the Department of National
Defence. He kept soldiers up for 64 hours, gave them the drug and tested their
performance.
DR. ROSS PIGEAU [Defence Research and Development Canada]: Modafinil
would be, from my research, a good alternative to, for instance, amphetamine.
BEAUCHEMIN: Amphetamines and other stimulants including coffee cause
side effects, including jitteriness and heart palpitations. Modafinil doesn't.
But
experts warn it is not a magic pill. They fear expanding its use could lead to
abuse. But it may be a licence for many to try to do more on less sleep. Sleep
depravity leads to increased risk of diabetes, heart problems and shorter
lifespans.
DR. DIANE BOIVIN [Sleep Expert]: The only real treatment for sleep
deprivation is sleep itself.
BEAUCHEMIN: Dr. Diane Boivin researched shift workers' sleep troubles. She
says the Modafinil is a good drug that could help emergency workers who need
to work nights, but few others.
BOIVIN: There is a choice of society to be made, and we should try to limit as
much as possible this twenty-four hour society because it's still not normal to
work nights.
BEAUCHEMIN: The company that sells Modafinil in Canada says it has not
started the process of having it approved for any other use than in the
treatment of narcolepsy. The Canadian Sleep Society says it hopes there will
be further studies into the drug's long-term effects before that happens.
Genevieve Beauchemin, CTV News, Montreal.
RINALDO: Thank you for joining us here at CTV News this Saturday. Good
night. Enjoy that extra hour. I'm Sandie Rinaldo. We'll see you tomorrow.
LOAD-DATE: November 3, 2003
LANGUAGE: ENGLISH
Copyright 2003 CTV Television, Inc.
728 of 998 DOCUMENTS
San Jose Mercury News (California)
October 19, 2003 Sunday MORNING FINAL EDITION
STEROID FLAP OVERSHADOWS ANOTHER DRUG;
MANY ATHLETES TEST POSITIVE FOR MILD STIMULANT MODAFINIL
BYLINE: MARK EMMONS AND PETE CAREY, Mercury News
SECTION: FRONT; Pg. 25A
LENGTH: 1095 words
When sprinter Kelli White tested positive for a mild stimulant called modafinil
at the World Championships in Paris in August, she had an explanation. She told
officials that she suffers from narcolepsy and that her doctor prescribed the
drug to combat her excessive fatigue.
But now that extensive laboratory sleuthing by the U.S. Anti-Doping Agency has
found several other American track athletes, so far unnamed, who tested positive
for modafinil this summer, one of two conclusions can be drawn:
* There is an epidemic of sleep disorders among the U.S. track elite.
* At least some athletes believe the drug enhances performance.
Thursday, the anti-doping agency said it was "fairly certain" that Balco
Laboratories of Burlingame was the source of a sample of a previously unknown
"designer" steroid, tetrahydrogestrinone, for which several athletes at the
national championships at Stanford University tested positive. Balco and its
president, Victor Conte Jr., also are targets of a federal grand jury that has
subpoenaed dozens of athletes to testify.
Another drug
But almost lost in the steroid controversy is the anti-doping agency's
announcement Thursday that track athletes may be using another banned drug to
aid them on the track: modafinil.
Asked Thursday if modafinil improves performance, the agency's chief executive,
Terry Madden, said bluntly: "Absolutely."
Yet sleep experts who prescribe the drug to patients sharply disagree.
"If I was an athlete, I sure wouldn't pick modafinil," said Dr. Thomas Scammell
of Beth Israel Deaconess Medical Center in Boston.
White, of Union City, is facing the loss of two gold medals and $120,000 that
she won in Paris. She denies that she took modafinil, sold under the brand name
Provigil, to give her an extra boost.
Last week European newspapers reported that a second U.S. athlete, hurdler Chris
White, also tested positive for modafinil. He finished sixth in the 110-meter
hurdles in Paris.
Sprinter's defense
White says she didn't know the International Association of Athletics
Federations considered modafinil a "related substance" to other stimulants on
the official banned list. But she also didn't disclose, on a form that all
athletes must complete listing the medications they are ingesting, that she was
taking Provigil.
Dr. Brian Goldman, an East Bay physician who at one time was Balco's medical
director, said he prescribed the drug for White when she showed symptoms of
narcolepsy, including fatigue and depression, before the World Championships.
Goldman said White's mother and maternal aunt also have the ailment.
Sleep experts respond
Goldman said that he had "no idea" athletes were using the drug when he gave
White some samples of Provigil. He believes White, at least, had a legitimate
reason to take it. He also remains convinced that the drug doesn't do anything
to improve athletic performance.
But he does note that because athletes may have been convinced that it would
help them, a "placebo effect" could have helped their performance.
"Athletes are very prone to a placebo effect," Goldman said. "So maybe they
believe it works, so it does."
But several sleep disorder experts say they don't understand how international
sports organizations can consider modafinil a substance that would make track
athletes faster. They say it does not act like a traditional stimulant, a main
reason prescriptions for it have grown sharply in recent years.
"I don't know what their issue is," said Joyce A. Walsleben, director at the New
York University School of Medicine's Sleep Disorders Center. "It's not a
stimulant as we know the word stimulant.
"It is a wake promoter, working in the area of the brain that wakes people up.
It does not stimulate the cardiovascular system or muscle system as amphetamines
do."
Dr. James Wyatt of Chicago's Rush University Medical Center said, "It is
actually one of the less potent medications available. That's one of the reasons
why it is preferred by sleep disorder specialists."
A representative for Cephalon, the West Chester, Pa., company that makes
Provigil, said reports of athletes using the drug are mystifying.
"We heard Kelli White had narcolepsy, so it wasn't surprising that she was
taking Provigil, because that's the standard of care for excessive sleep,"
Sheryl Williams said. "The whole situation with the IAAF is something that we
weren't expecting and prepared for because we make a pharmaceutical product for
sick people."
Other uses
Although the Food and Drug Administration approved Provigil in 1998 for
narcolepsy treatment, Williams said only about 20 percent of prescriptions
concern sleep disorders. She said it also is used to treat fatigue associated
with multiple sclerosis, depression, Parkinson's disease and chronic fatigue
syndrome, among other conditions.
In fact, physicians have found plenty of "off-label" uses for Provigil. People
who need to stay awake for long periods of time, such as truck drivers, use it.
The U.S. military is testing Provigil on pilots.
Dr. Frank Baldino, Cephalon's chief executive, recently told Fortune magazine
that some of the off-label uses of Provigil make him slightly uncomfortable. "In
some sense, physicians are way ahead of us," he said.
The question is whether athletes think they're way ahead, too.
When the anti-doping agency began its steroid investigation, it re-examined 350
urine samples taken at the USA Outdoor Track & Field Championships at Stanford
University and took 200 additional out-of-competition samples from athletes in
track and other Olympic sports.
'Really frustrating'
While the stunning news was the discovery of the designer steroid in some
samples, the agency said "several" positive tests for modafinil also were found.
Those who test positive for steroids risk a minimum two-year ban from
competition. The penalty for using modafinil is disqualification from the meet
where an athlete tested positive.
Goldman said that whether other athletes were taking it to gain an advantage,
White was taking it legitimately.
Contacted last week at her East Bay home, White sounded weary. She has been
subpoenaed to testify before a grand jury in the federal investigation of Balco.
She adamantly denied being one of the athletes who tested positive for THG.
"I've already got enough stuff to deal with," White said, referring to the
modafinil case.
Then, after a deep sigh, she added: "This is really frustrating and it's
probably going to get even more frustrating over the next few weeks."
LOAD-DATE: August 17, 2005
LANGUAGE: ENGLISH
NOTES: RELATED STORY: page 1A.
Copyright 2003 San Jose Mercury News
All Rights Reserved
729 of 998 DOCUMENTS
SUNDAY TELEGRAPH(LONDON)
October 19, 2003, Sunday
Doping scandal could cost White more gold Simon Hart reports on the gathering
drugs scandal which has been sparked by the detection of a new steroid
BYLINE: by Simon Hart
SECTION: Pg. 16
LENGTH: 624 words
KELLI WHITE, the American sprint star who faces being stripped of the two gold
medals she won at the World Championships in Paris after failing a drug test,
could also lose the two golds she won at this summer's US Championships after
testing positive for the same banned substance.
White has admitted that the urine sample she gave at the US Championships in
Palo Alto, California, in June has revealed traces of modafinil - the same drug
that was discovered in the sample taken two months later after her 100 metres
triumph in Paris. The American claims the drug was prescribed for an hereditary
sleeping disorder but admits she failed to notify the anti-doping authorities in
advance because she had no idea it was a banned drug.
The reason that the earlier drug test failure has only recently come to light is
because at the time of the US Championships the US Anti-Doping Agency (USADA)
did not test for modafinil. However, all 350 samples provided at the
championships have recently been re-examined following an anonymous tip-off that
a new, hitherto undetectable anabolic called tetrahydrogestrinone, or THG, was
being widely abused. Tests for modafinil were also carried out as part of the
investigation.
White faces a disciplinary hearing in the United States which is likely to
result in the loss of the two gold medals she won in Paris in the 100m and 200m,
and she expects the US Championships case to be dealt with at the same time.
However, her claims that the drug, a mild stimulant, was used to treat a
narcolepsy condition have been thrown into doubt by the revelation that several
more modafinil 'positives' have been detected among other samples. Unless
sleeping disorders are rife among American athletes, the likelihood seems to be
that it is being used as a performance enhancer.
White, who insists she has not tested positive for THG, has also confirmed that
she is one of 40 American sports stars who have been subpoenaed to give evidence
to a Federal Grand Jury in San Francisco investigating the activities of the Bay
Area Laboratory Cooperative (BALCO) in California, a company producing
nutritional supplements that has been named as the source of THG, a so-called
"designer" or artificially produced steroid that was previously unknown to
drug-testers. USADA were alerted to the drug by a tip-off in May but have only
recently discovered a reliable test to detect it.
Up to 20 stars are said to have tested positive for the steroid in what could be
one of the biggest doping scandals in history, though anti-doping officials are
refusing to reveal their identities until tests on second 'B' samples have been
carried out.
The only athlete to have been named is American shot put champion Kevin Toth,
one of dozens of sportsmen mentioned on BALCO's website. His agent, John Nubani,
has confirmed THG was part of his supplement package but said his client had no
idea it was a banned anabolic steroid.
USADA have confirmed that 100 out-of-competition samples were also being
re-analysed as part of the THG investigation, though it is unclear whether any
foreign athletes are involved.
The THG scandal, which anti-doping officials in America have described as an
"international doping conspiracy", is threatening to bring down the country's
governing body of athletics, USA Track and Field.
Yesterday, the US Olympic Committee gave athletics officials one month to regain
control of their sport or face being wound up following a series of
controversies including Jon Drummond's histrionics against a false start in
Paris and the revelation that world 400m champion Jerome Young was cleared to
compete at the Sydney Olympics despite testing positive for nandrolone in 1999.
[PS]Sport: [ES]
GOLF:
LOAD-DATE: October 19, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Telegraph Group Limited
730 of 998 DOCUMENTS
The Washington Post
October 18, 2003 Saturday
Final Edition
White Says She Passed THG Test;
But Sprinter Flunked 2nd Modafinil Screening
BYLINE: Amy Shipley, Washington Post Staff Writer
SECTION: Sports; D01
LENGTH: 920 words
U.S. sprinter Kelli White said yesterday she is not among the handful of U.S.
track and field athletes who have tested positive for the newly discovered
anabolic steroid tetrahydrogestrinone (THG), but she acknowledged flunking a
second drug test for the stimulant modafinil at the U.S. Track and Field
Championships this summer, a development that could cost her the two gold medals
she won there.
Meantime, NFL spokesman Greg Aiello said yesterday that the league plans to
include THG on its banned list and will begin testing for the drug shortly. He
added that league officials would consider retroactive testing, which officials
of the U.S. Anti-Doping Agency undertook this summer after discovering the new
steroid. USADA officials announced Thursday that several track and field
athletes had tested positive in retroactive testing for THG.
White, notified of the second positive test for modafinil in recent days, is
already facing a public warning and the loss of the two gold medals she won at
the August world championships as a result of her first positive test for
modafinil. White emerged this summer as the top female sprinter in the world in
the absence of five-time Olympic medalist Marion Jones.
White, who said she took modafinil to treat narcolepsy, said she expected the
two cases to be adjudicated together this fall. USADA officials, who are
handling the case, declined to comment.
White also said she has been subpoenaed to appear before a federal grand jury
looking into activities at the Bay Area Laboratory Co-Operative (BALCO), a
nutrition company run by Victor Conte that USADA officials alleged Thursday was
the source of the new steroid.
USADA CEO Terry Madden said he believed THG was distributed by Conte and BALCO
as part of an international conspiracy to beat standard drug tests. He declined
to name the athletes who flunked drug tests, but called it the biggest anabolic
steroid bust in sports history.
U.S. shot put champion Kevin Toth is among those who have tested positive,
according to several sources with knowledge of the investigation.
John Nubani, Toth's agent, said yesterday Toth likely was unaware that THG was
an anabolic steroid because it was not on the International Olympic Committee's
list of banned substances and had never -- until now -- triggered a positive
test. Toth, who finished fourth at the world championships, has used nutrition
products from Conte and has credited him for helping turn his career around.
Toth is among the dozens of athletes mentioned in BALCO's Web site.
Nubani said Toth, 35, of Hudson, Ohio, had never tested positive for any other
substance during his career. He won his first U.S. indoor and outdoor titles
this year.
"All I know is what he told me: He said part of his supplement package included
whatever this is," Nubani said, referring to the THG. "I don't know if he
ingested it, took shots, drops, or what . . . . I don't think he was aware of it
[being a steroid] . . . . Guys are always looking for a better edge, better
vitamins."
Toth, who Nubani said also has been summoned to appear before the grand jury,
did not return calls seeking comment.
Conte denied Thursday being the source of the drug in an e-mail sent to a number
of news outlets, saying the charges against him were motivated by politics and
jealousy. In other e-mails yesterday, he said it was "outrageous" for
anti-doping officials to describe THG as a powerful anabolic steroid.
"USADA is really making a scientific stretch by suggesting that [THG] is closely
related to an anabolic steroid. . . . " Conte wrote in one e-mail, adding in
another that, "my understanding from what I have been told by experts in this
field, is that a very small alteration in the molecular structure of an anabolic
steroid can cause it to become totally ineffective. THG may not even reach the
androgen receptor at all and there may be absolutely no anabolic effects."
Also yesterday, the executive committee of the U.S. Olympic Committee met for
more than four hours in Cleveland to discuss the latest drug testing scandal
involving track and field athletes.
"The United States Olympic Committee has to take the responsibility and
leadership to solve this problem because we are not satisfied with the action
that has been taken to date by USA Track and Field," USOC acting president Bill
Martin said in a news conference afterward. "This is a problem rooted in both
perception and reality, and it is a problem related to doping, athlete conduct
and the credibility of the sport."
Martin appointed a three-person panel to work with USA Track & Field on a plan,
to be submitted by Nov. 17 to the USOC, detailing how it will deal with doping
issues, athlete conduct and restoring the credibility within USATF.
Later, in a news conference of his own, USATF chief executive officer Craig
Masback said "we welcome ideas from the USOC or anyone on how we can be better
at doing what we're doing, on how we can have a higher profile on these issues
and how we can play a more positive role on this issue.
"What the developments of the last few days tell us is there's a problem out
there. That there is a small number of people, perhaps in pockets around the
country, that seem to be under the influence of some gurus who say they can help
people get away with something. That they are preying on athletes and they are
taking advantage of people who are weak, and who are willing to listen to such
arguments."
Staff writer Thomas Heath contributed to this report from Cleveland.
LOAD-DATE: October 18, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
731 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 17, 2003, Friday, BC cycle
U.S. Anti-Doping Agency says it has uncovered steroid conspiracy
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 850 words
DATELINE: SAN FRANCISCO
The U.S. Anti-Doping Agency has uncovered a widespread drug conspiracy involving
coaches, chemists and several track athletes who tested positive for a
previously undetectable steroid and now face suspensions that could bar them
from the 2004 Athens Olympics.
USADA chief executive officer Terry Madden said Thursday that the U.S. athletes
had tested positive for the steroid, known as tetrahydrogestrinone, or THG. He
said the ongoing inquiry began in June with an anonymous tip and has expanded to
include U.S. professional sports.
"I know of no other drug bust that is larger than this involving the number of
athletes involved," said Madden, who refused to reveal the names or genders of
the athletes, or to be more specific about how many had tested positive.
Olympic athletes face drug tests at major competitions, as well as random
testing between events. Their samples are divided in two and stored for future
reference.
The athletes whose "A" samples revealed THG have been notified and will now have
their "B" samples tested. If those also are positive, a review process will
begin. Appeals could last for months. Track athletes found to have used steroids
would face two-year bans.
"What we have uncovered appears to be intentional doping of the worst sort,"
Madden said in a conference call from USADA headquarters in Colorado Springs,
Colo. "This is a far cry from athletes accidentally testing positive as a result
of taking contaminated nutritional supplements.
"Rather, this is a conspiracy involving chemists, coaches and certain athletes
using what they developed to be 'undetectable' designer steroids to defraud
their fellow competitors and the American and world public who pay to attend
sports events."
THG has a chemical structure similar to the banned anabolic steroids gestrinome
and trenbolone, Madden said. Though THG is not specifically named as a banned
substance in world track, it would be considered a related substance outlawed
under the sport's doping rules.
Madden said the USADA received a call from a man in early June claiming to be a
track coach and naming athletes whom he claimed were using an undetectable
designer steroid. He then sent the agency, by overnight courier, a used syringe
containing some of the substance, Madden said.
The anti-doping laboratory at UCLA run by Don Catlin determined that the syringe
contained THG, leading the USADA to retest 350 urine samples taken from athletes
at the U.S. track and field championships in late June at Stanford, as well as
100 samples from random out-of-competition tests.
Madden said USADA contacted federal authorities with the findings. He wouldn't
say how many of the samples tested positive for THG.
Madden said the anonymous tipster identified the source of the THG as Victor
Conte, founder of BALCO laboratory of Burlingame. Madden would not say whether
he had independent proof the substance came from Conte or BALCO.
"Everything that the coach has identified to us up to this time is true. We are
fairly certain this substance came from Victor Conte and BALCO labs," said
Madden, refusing to provide more specifics about what made him so certain.
In an e-mail sent to The Associated Press and other news organizations Thursday,
Conte denied BALCO was the source of the substance.
"In my opinion, this is about jealous competitive coaches and athletes that all
have a history of promoting and using performance enhancing agents being
'completely hypocritical' in their actions," Conte wrote.
Madden said he had not spoken with Conte.
BALCO, which supplies nutritional guidance and supplements to athletes ranging
from Barry Bonds to Bill Romanowski to Marion Jones, was the subject of a visit
last month by agents from the Internal Revenue Service and a San Mateo County
narcotics task force.
No arrests were made, and IRS spokesman Mark Lessler said at the time he could
not comment on the purpose of the unannounced visit.
Sprinter Kelli White, whose failed drug test for the stimulant modafinil at this
summer's track and field World Championships could cost her a pair of sprint
gold medals, also is associated with BALCO. Her case is being considered by
USADA.
White was prescribed modafinil by Dr. Brian Goldman, a psychiatrist who worked
with Conte for nearly 20 years. White's coach, Remi Korchemny, joined with Conte
to form a track club.
As part of the retesting of the 350 samples from the U.S. track championships,
Madden said, officials discovered several positive tests for modafinil - which
White claims she was taking for the sleep disorder narcolepsy.
"Information we gathered showed athletes were using modafinil as a stimulant,"
Madden said. He said there's no chemical link between modafinil and THG.
Dick Pound, chairman of the World Anti-Doping Agency, applauded USADA's work in
a statement released at WADA headquarters in Montreal.
"This is a serious warning for cheaters," Pound said. "It shows that supposedly
undetectable substances can be detected as new tests are developed."
On the Net:
www.usantidoping.org
LOAD-DATE: October 18, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
732 of 998 DOCUMENTS
The Orange County Register (California)
October 17, 2003 Friday
Designer steroid exposed;
Widespread use of THG among track and field athletes is uncovered.
BYLINE: By SCOTT M. REID , The Orange County Register
SECTION: SPORTS
LENGTH: 480 words
The U.S. Anti-Doping Agency said Thursday it has uncovered a widespread doping
ring involving U.S. and international track and field athletes, coaches and a
prominent Bay area laboratory.
``Several'' track athletes tested positive for tetrahydrogestrinone, or THG, a
previously undetectable steroid, said Terry Madden, chief executive director of
the anti-doping agency, but he refused to name the athletes or say how many
tested positive.
Madden said the names might not be made public until the completion of an
appeals process in December.
Athletes who test positive for anabolic steroids face two-year suspensions that
would keep them out of the 2004 Olympic Games in Athens.
``I know of no other drug bust that is larger than this,'' Madden said.
``This is a far cry from athletes accidentally testing positive as a result of
taking contaminated nutritional supplements,'' Madden said.
``Rather, this is a conspiracy involving chemists, coaches and certain athletes
using what they developed to be `undetectable' designer steroids to defraud
their fellow competitors and the American and world public who pay to attend
sports events.''
The first break in the case came in early June, Madden said, when an anonymous
source describing himself as a ``top-flight track coach,'' contacted the
anti-doping agency. Madden said Thursday agency officials still do not know the
source's identity.
The source provided a syringe containing a designer steroid, undetectable by
previous drug tests, Madden said. According to the source, the steroid came from
Victor Conte of the BALCO Laboratory in Burlingame, Madden said.
Conte and BALCO have supplied supplements and nutritional consultation to
slugger Barry Bonds, sprinter Marion Jones and a number of NFL stars.
Citing the potentially illegal activity by a distributor of a controlled
substance, the agency contacted the Department of Justice, Madden said.
The IRS raided BALCO facilities last month. The IRS also searched the offices of
Bonds' personal trainer.
The UCLA drug lab was able to come up with a test to detect TGH in mid-June. The
anti-doping agency re-tested 350 in-competition samples tests from the 2003 U.S.
Track & Field Championships. The organization also ordered 100
out-of-competition drug tests of U.S. track athletes and another 100 tests of
athletes in other Olympic sports.
Madden also said the agency found a number of positive test results for
modafinil, a stimulant.
Sprinter Kelli White tested positive for modafinil after winning two gold medal
at the World Championships in August. White was prescribed modafinil by Dr.
Brian Goldman, a psychiatrist who has worked with Conte for nearly 20 years.
The athletes have recently been notified of their positive test results, Madden
said. If the initial result is confirmed by a second lab test, the athlete will
be considered positive and face suspension.
sreid@ocregister.com
LOAD-DATE: October 28, 2003
LANGUAGE: ENGLISH
DOCUMENT-TYPE: Story
PUBLICATION-TYPE: Newspaper
Copyright 2003 Orange County Register
733 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 16, 2003, Thursday, BC cycle
U.S. Anti-Doping Agency says it has uncovered steroid conspiracy; Byline: 1/8 By
ROB GLOSTER
BYLINE: AP Sports Writer
SECTION: Sports News
LENGTH: 775 words
DATELINE: SAN FRANCISCO
The U.S. Anti-Doping Agency has uncovered a widespread drug conspiracy involving
coaches, chemists and several track athletes who tested positive for a
previously undetectable steroid and now face suspensions that could bar them
from the 2004 Athens Olympics.
USADA chief executive officer Terry Madden said Thursday that both American and
international athletes had tested positive for the steroid, known as
tetrahydrogestrinone, or THG. He said the ongoing inquiry began with an
anonymous tip and has expanded to include U.S. professional sports.
"I know of no other drug bust that is larger than this involving the number of
athletes involved," said Madden, who refused to reveal the names, genders or
nationalities of the athletes, or to be more specific about how many had tested
positive.
Olympic athletes face drug tests at major competitions, as well as random
testing between events. Their samples are divided in two and stored for future
reference.
The athletes whose "A" samples revealed THG have been notified and will now have
their "B" samples tested. If those also are positive, a review process will
begin. Appeals could last for months. Track athletes found to have used steroids
would face two-year bans.
"What we have uncovered appears to be intentional doping of the worst sort,"
Madden said in a conference call from USADA headquarters in Colorado Springs,
Colo. "This is a far cry from athletes accidentally testing positive as a result
of taking contaminated nutritional supplements.
"Rather, this is a conspiracy involving chemists, coaches and certain athletes
using what they developed to be 'undetectable' designer steroids to defraud
their fellow competitors and the American and world public who pay to attend
sports events."
THG has a chemical structure similar to the banned anabolic steroids gestrinome
and trenbolone, Madden said. Though THG is not specifically named as a banned
substance in world track, it would be considered a related substance outlawed
under the sport's doping rules.
Madden said the USADA received a call from a man in early June claiming to be a
track coach and naming athletes whom he claimed were using an undetectable
designer steroid. He then sent the agency, by overnight courier, a used syringe
containing some of the substance, Madden said.
The anti-doping laboratory at UCLA run by Don Catlin determined that the syringe
contained THG, leading the USADA to retest 350 urine samples taken from athletes
at the U.S. track and field championships in late June at Stanford, as well as
100 samples from random out-of-competition tests.
Madden said USADA contacted federal authorities with the findings. He wouldn't
say how many of the samples tested positive for THG.
Madden said the anonymous tipster identified the source of the THG as Victor
Conte, founder of BALCO laboratory of Burlingame. Madden would not say whether
he had independent proof the substance came from Conte or BALCO.
"Everything that the coach has identified to us up to this time is true. We are
fairly certain this substance came from Victor Conte and BALCO labs," said
Madden, refusing to provide more specifics about what made him so certain.
Madden said he had not spoken with Conte, and Conte did not immediately respond
Thursday to an e-mail inquiry from The Associated Press. A message left by phone
at BALCO went unanswered.
BALCO, which supplies nutritional guidance and supplements to athletes ranging
from Barry Bonds to Bill Romanowski to Marion Jones, was the subject of
enforcement action last month by the Internal Revenue Service and a San Mateo
County narcotics task force.
No arrests were made, and IRS spokesman Mark Lessler said he could not comment
on the purpose of the unannounced visit to BALCO.
Sprinter Kelli White, whose failed drug test for the stimulant modafinil at this
summer's track and field World Championships could cost her a pair of sprint
gold medals, also is associated with Conte. Her case currently is being
considered by USADA.
White was prescribed modafinil by Dr. Brian Goldman, a psychiatrist who has
worked with Conte for nearly 20 years. And White's coach, Remi Korchemny, joined
with Conte to form a track club.
As part of the retesting of the 350 samples from the U.S. track championships,
Madden said, officials discovered several positives for modafinil - which White
claims she was taking for the sleep disorder narcolepsy.
"Information we gathered showed athletes were using modafinil as a stimulant,"
Madden said. He said there's no chemical link between modafinil and THG.
On the Net:
www.usantidoping.org
LOAD-DATE: October 17, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
734 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 16, 2003, Thursday, BC cycle
U.S. Anti-Doping Agency says it has uncovered steroid conspiracy
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 868 words
DATELINE: SAN FRANCISCO
The U.S. Anti-Doping Agency has uncovered a widespread drug conspiracy involving
coaches, chemists and several track athletes who tested positive for a
previously undetectable steroid and now face suspensions that could bar them
from the 2004 Athens Olympics.
USADA chief executive officer Terry Madden said Thursday that the U.S. athletes
had tested positive for the steroid, known as tetrahydrogestrinone, or THG. He
said the ongoing inquiry began in June with an anonymous tip and has expanded to
include U.S. professional sports.
"I know of no other drug bust that is larger than this involving the number of
athletes involved," said Madden, who refused to reveal the names or genders of
the athletes, or to be more specific about how many had tested positive.
Olympic athletes face drug tests at major competitions, as well as random
testing between events. Their samples are divided in two and stored for future
reference.
The athletes whose "A" samples revealed THG have been notified and will now have
their "B" samples tested. If those also are positive, a review process will
begin. Appeals could last for months. Track athletes found to have used steroids
would face two-year bans.
"What we have uncovered appears to be intentional doping of the worst sort,"
Madden said in a conference call from USADA headquarters in Colorado Springs,
Colo. "This is a far cry from athletes accidentally testing positive as a result
of taking contaminated nutritional supplements.
"Rather, this is a conspiracy involving chemists, coaches and certain athletes
using what they developed to be 'undetectable' designer steroids to defraud
their fellow competitors and the American and world public who pay to attend
sports events."
THG has a chemical structure similar to the banned anabolic steroids gestrinome
and trenbolone, Madden said. Though THG is not specifically named as a banned
substance in world track, it would be considered a related substance outlawed
under the sport's doping rules.
Madden said the USADA received a call from a man in early June claiming to be a
track coach and naming athletes whom he claimed were using an undetectable
designer steroid. He then sent the agency, by overnight courier, a used syringe
containing some of the substance, Madden said.
The anti-doping laboratory at UCLA run by Don Catlin determined that the syringe
contained THG, leading the USADA to retest 350 urine samples taken from athletes
at the U.S. track and field championships in late June at Stanford, as well as
100 samples from random out-of-competition tests.
Madden said USADA contacted federal authorities with the findings. He wouldn't
say how many of the samples tested positive for THG.
Madden said the anonymous tipster identified the source of the THG as Victor
Conte, founder of BALCO laboratory of Burlingame. Madden would not say whether
he had independent proof the substance came from Conte or BALCO.
"Everything that the coach has identified to us up to this time is true. We are
fairly certain this substance came from Victor Conte and BALCO labs," said
Madden, refusing to provide more specifics about what made him so certain.
In e-mails to several newspapers Thursday, Conte denied BALCO was the source of
the substance.
"In my opinion, this is about jealous competitive coaches and athletes that all
have a history of promoting and using performance enhancing agents being
'completely hypocritical' in their actions," Conte said.
Madden said he had not spoken with Conte, and Conte did not immediately respond
Thursday to an e-mail inquiry from The Associated Press. A message left by phone
at BALCO went unanswered.
BALCO, which supplies nutritional guidance and supplements to athletes ranging
from Barry Bonds to Bill Romanowski to Marion Jones, was the subject of a visit
last month by agents from the Internal Revenue Service and a San Mateo County
narcotics task force.
No arrests were made, and IRS spokesman Mark Lessler said at the time he could
not comment on the purpose of the unannounced visit.
Sprinter Kelli White, whose failed drug test for the stimulant modafinil at this
summer's track and field World Championships could cost her a pair of sprint
gold medals, also is associated with BALCO. Her case is being considered by
USADA.
White was prescribed modafinil by Dr. Brian Goldman, a psychiatrist who worked
with Conte for nearly 20 years. White's coach, Remi Korchemny, joined with Conte
to form a track club.
As part of the retesting of the 350 samples from the U.S. track championships,
Madden said, officials discovered several positive tests for modafinil - which
White claims she was taking for the sleep disorder narcolepsy.
"Information we gathered showed athletes were using modafinil as a stimulant,"
Madden said. He said there's no chemical link between modafinil and THG.
Dick Pound, chairman of the World Anti-Doping Agency, applauded USADA's work in
a statement released at WADA headquarters in Montreal.
"This is a serious warning for cheaters," Pound said. "It shows that supposedly
undetectable substances can be detected as new tests are developed."
On the Net:
www.usantidoping.org
LOAD-DATE: October 17, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
735 of 998 DOCUMENTS
Edmonton Journal (Alberta)
October 10, 2003 Friday Final Edition
White's second test shows stimulant: IAAF leaves it up to USA Track & Field to
decide next move
SOURCE: The Associated Press
SECTION: Sports; Pg. D5
LENGTH: 316 words
DATELINE: PARIS
PARIS - A second drug test indicates U.S. sprinter Kelli White used a stimulant
during the world championships this summer when she won two gold medals, track's
world governing body said Thursday.
The results confirmed an earlier test that found modafinil, a medication used to
treat a sleep disorder, in White's urine, according to Nick Davies, a spokesman
for the International Association of Athletics Federations.
The latest test was conducted on a second sample taken from White during the
August meet, but not tested until now.
U.S. officials must now decide whether the case constitutes a doping offence.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said.
White will lose her 100- and 200-metre gold medals if U.S. officials determine
she committed a doping offence.
USA Track & Field spokeswoman Jill Geer wouldn't comment Thursday other than to
say the results from the second test weren't surprising.
"Remember, Kelli said the day the story broke that she was taking modafinil, so
she's never said it wasn't in her system," she said.
After she tested positive for modafinil at the championships in France, White
said she used the medication for a sleep disorder and didn't know it contained
banned substances.
The IAAF said modafinil was covered under the category of "related substances."
If White is stripped of her medals, Torri Edwards of the United States would be
awarded the 100 gold medal while Zhanna Block of Ukraine would take the silver
and Chandra Sturrup of Bahamas the bronze.
The new 200 champion would be Russia's Anastaiya Kapachinskaya.
Edwards would take the silver and France's Muriel Hurtis the bronze.
Also Thursday, the IAAF said a second sample from American 110-metre hurdler
Chris Phillips, who finished fifth at the worlds, also tested positive for
modafinil.
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: The Associated Press, File; U.S. sprinter Kelli White
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
736 of 998 DOCUMENTS
Espicom Business Intelligence
October 10, 2003
Modafinil approved for expanded use in Germany and Republic of Ireland
LENGTH: 275 words
Cephalon has received authorisation from the Federal Institute for Drugs and
Devices and the Irish Medicines Board to market modafinil tablets in Germany and
the Republic of Ireland, respectively, for the treatment of excessive daytime
sleepiness associated with obstructive sleep apnoea/hypopnoea syndrome (OSA/HS).
Both approvals include the adjunctive use of modafinil in patients who are
receiving adequate treatment for their OSA/HS with standard therapy continuous
positive airway pressure (CPAP). Modafinil is marketed under the trade name,
Vigil, in Germany and as Provigil in Ireland.
Modafinil is the first in a new class of wake-promoting agents believed to work
selectively through the sleep/wake centres to activate the cortex of the brain.
The drug is currently approved in more than 20 countries for the treatment of
excessive daytime sleepiness associated with narcolepsy.
In December of 2002, Provigil was approved to treat excessive daytime sleepiness
in patients with OSA/HS in the UK.
On 25th September 2003, the Peripheral and Central Nervous System Advisory
Committee of the FDA recommended to expand the label for Provigil beyond its
current indication for excessive daytime sleepiness associated with narcolepsy.
The FDA is expected to determine the precise language of the modified label for
Provigil by year-end.
In controlled clinical trials, modafinil has been found to be generally well
tolerated with a low incidence of adverse events relative to placebo. The most
commonly observed adverse events associated with the use of modafinil were
headache, infection, nausea, nervousness, anxiety and insomnia.
LOAD-DATE: October 13, 2003
LANGUAGE: ENGLISH
Copyright 2003 ESPICOM Business Intelligence Ltd.
737 of 998 DOCUMENTS
Philadelphia Daily News
OCTOBER 10, 2003 Friday 4STAR EDITION
Kelli White's positive test confirmed
BYLINE: Daily News Wire Services
SECTION: SPORTS; Pg. 126
LENGTH: 288 words
A second drug test indicates U.S. sprinter Kelli White used a stimulant during
the World Championships this summer, when she won two gold medals, track's world
governing body said yesterday in Paris.
The results confirmed an earlier test that found modafinil, a medication used to
treat a sleep disorder, in White's urine, said Nick Davies, a spokesman for the
International Association of Athletics Federations.
The latest test was conducted on a second sample taken from White during the
August meet, but not tested until now.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said. White will lose her 100- and
200-meter gold medals if U.S. officials determine she committed a doping
offense.
After she tested positive for modafinil at the championships in France, White
said she used the medication for a sleep disorder and didn't know it contained
banned substances.
The IAAF said modafinil was covered under the category of "related substances."
Olympics
* About 1,200 employees at the Olympic Village in Athens staged a 24-hour
strike, a day after a construction worker was killed after being hit by a
vehicle.
* Olympic skating champion Alexei Yagudin applied for an alcohol education
program that would clear his record of a drunken driving charge. Yagudin, 23,
was pulled over Aug. 31 while driving in a Hartford, Conn., suburb.
Sport Stops
* Scott Verplank shot a second-round 62 to tie Steve Flesch for the lead at the
Las Vegas Invitational.
* South Carolina basketball center Rolando Howell pleaded no contest to
domestic-violence charges and was ordered to pay a $50 fine and complete a
counseling program. *
LOAD-DATE: August 17, 2005
LANGUAGE: ENGLISH
Copyright 2003 Philadelphia Newspapers, LLC
All Rights Reserved
738 of 998 DOCUMENTS
The Associated Press
October 9, 2003, Thursday, BC cycle
Second drug test shows U.S. sprinter Kelli White used a stimulant, IAAF says
BYLINE: By ANGELA DOLAND, Associated Press Writer
SECTION: Sports News
LENGTH: 316 words
DATELINE: PARIS
A second drug test indicates U.S. sprinter Kelli White used a stimulant during
the World Championships this summer, when she won two gold medals, track's world
governing body said Thursday.
The results confirmed an earlier test that found modafinil, a medication used to
treat a sleep disorder, in White's urine, according to Nick Davies, a spokesman
for the International Association of Athletics Federations.
The latest test was conducted on a second sample taken from White during the
August meet, but not tested until now.
U.S. officials must now decide whether the case constitutes a doping offense.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said. White will lose her 100 and
200 meter gold medals if U.S. officials determine she committed a doping
offense.
USA Track & Field spokeswoman Jill Geer wouldn't comment Thursday other than to
say the results from the second test weren't surprising.
"Remember, Kelli said the day the story broke that she was taking modafinil, so
she's never said it wasn't in her system," she said.
After she tested positive for modafinil at the championships in France, White
said she used the medication for a sleep disorder and didn't know it contained
banned substances.
The IAAF said modafinil was covered under the category of "related substances."
If White is stripped of her medals, Torri Edwards of the United States would be
awarded the 100 gold medal while Zhanna Block of Ukraine would take the silver
and Chandra Sturrup of Bahamas the bronze.
The new 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would
take the silver and France's Muriel Hurtis the bronze.
Also Thursday, the IAAF said a second sample from American 110-meter hurdler
Chris Phillips, who finished fifth at the worlds, also tested positive for
modafinil.
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
739 of 998 DOCUMENTS
Associated Press Worldstream
October 9, 2003 Thursday
URGENT Second drug test shows U.S. sprinter Kelli White used a stimulant at
world championships
BYLINE: ANGELA DOLAND; Associated Press Writer
SECTION: SPORTS
LENGTH: 278 words
DATELINE: PARIS
A second urine sample showed that U.S. sprinter Kelli White used a stimulant
during the August world championships, where she won two gold medals, the IAAF
said Thursday.
The results of a B Sample confirmed an earlier test that indicated White had
ingested modafinil, a medication used to treat a sleep disorder, said Nick
Davies, spokesman for the International Association of Athletics Federations.
L'Equipe newspaper reported that the second test was done earlier in the week.
U.S. officials must now decide whether the case constitutes a doping offense.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said. White will lose both her 100
and 200 meter gold medals if U.S. officials determine she committed a doping
offense.
After she tested positive for modafinil at the world championships in France,
White said she used the medication for a sleep disorder and didn't know it
contained banned substances because it didn't appear on the list.
The IAAF said modafinil was covered under the category of "related substances."
It rejected White's explanation.
If White is stripped of her medals, Torri Edwards of the United States would be
awarded the 100 gold medal while Zhanna Block of Ukraine would take the silver
and Chandra Sturrup of Bahamas the bronze.
In the possible shake-up, the new 200 champion would be Russia's Anastaiya
Kapachinskaya. Edwards would take the silver and France's Muriel Hurtis the
bronze.
The IAAF spokesman also said a B Sample from American 110-meter hurdler Chris
Phillips, who finished fifth at the worlds, also tested positive for modafinil.
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
740 of 998 DOCUMENTS
The Associated Press State & Local Wire
October 9, 2003, Thursday, BC cycle
Second drug test shows Kelli White used stimulant, IAAF says
BYLINE: By ANGELA DOLAND, Associated Press Writer
SECTION: Sports News
LENGTH: 328 words
DATELINE: PARIS
A second drug test indicates U.S. sprinter Kelli White used a stimulant during
the World Championships this summer, when she won two gold medals, track's world
governing body said Thursday.
The results confirmed an earlier test that found modafinil, a medication used to
treat a sleep disorder, in White's urine, according to Nick Davies, a spokesman
for the International Association of Athletics Federations.
The latest test was conducted on a second sample taken from White during the
August meet, but not tested until now. White grew up in Oakland, Calif., and now
lives nearby in Union City.
U.S. officials must now decide whether the case constitutes a doping offense.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said. White will lose her 100 and
200 meter gold medals if U.S. officials determine she committed a doping
offense.
USA Track & Field spokeswoman Jill Geer wouldn't comment Thursday other than to
say the results from the second test weren't surprising.
"Remember, Kelli said the day the story broke that she was taking modafinil, so
she's never said it wasn't in her system," she said.
After she tested positive for modafinil at the championships in France, White
said she used the medication for a sleep disorder and didn't know it contained
banned substances.
The IAAF said modafinil was covered under the category of "related substances."
If White is stripped of her medals, Torri Edwards of the United States would be
awarded the 100 gold medal while Zhanna Block of Ukraine would take the silver
and Chandra Sturrup of Bahamas the bronze.
The new 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would
take the silver and France's Muriel Hurtis the bronze.
Also Thursday, the IAAF said a second sample from American 110-meter hurdler
Chris Phillips, who finished fifth at the worlds, also tested positive for
modafinil.
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
741 of 998 DOCUMENTS
Associated Press Online
October 9, 2003 Thursday
IAAF: 2nd Test Shows White Used Stimulant
BYLINE: ANGELA DOLAND; Associated Press Writer
SECTION: SPORTS
LENGTH: 314 words
DATELINE: PARIS
A second drug test indicates U.S. sprinter Kelli White used a stimulant during
the World Championships this summer, when she won two gold medals, track's world
governing body said Thursday.
The results confirmed an earlier test that found modafinil, a medication used to
treat a sleep disorder, in White's urine, according to Nick Davies, a spokesman
for the International Association of Athletics Federations.
The latest test was conducted on a second sample taken from White during the
August meet, but not tested until now.
U.S. officials must now decide whether the case constitutes a doping offense.
The results go to USA Track & Field officials, who are expected to refer the
case to the U.S. Anti-Doping Agency, Davies said. White will lose her 100 and
200 meter gold medals if U.S. officials determine she committed a doping
offense.
USA Track & Field spokeswoman Jill Geer wouldn't comment Thursday other than to
say the results from the second test weren't surprising.
"Remember, Kelli said the day the story broke that she was taking modafinil, so
she's never said it wasn't in her system," she said.
After she tested positive for modafinil at the championships in France, White
said she used the medication for a sleep disorder and didn't know it contained
banned substances.
The IAAF said modafinil was covered under the category of "related substances."
If White is stripped of her medals, Torri Edwards of the United States would be
awarded the 100 gold medal while Zhanna Block of Ukraine would take the silver
and Chandra Sturrup of Bahamas the bronze.
The new 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would
take the silver and France's Muriel Hurtis the bronze.
Also Thursday, the IAAF said a second sample from American 110-meter hurdler
Chris Phillips, who finished fifth at the worlds, also tested positive for
modafinil.
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
742 of 998 DOCUMENTS
Midnight Trader
This content is provided to LexisNexis by Comtex News
Network, Inc.
October 9, 2003 Thursday
Cephalon Gets German, Irish Oks for Expanded Use of Modafinil Sleep Disorder
Drug
LENGTH: 107 words
DATELINE: Boston
Cephalon (CEPH) said today the company has received authorization from the
Federal Institute for Drugs and Devices and the Irish Medicines Board to market
modafinil tablets in Germany and the Republic of Ireland, respectively, for the
treatment of excessive daytime sleepiness associated with obstructive sleep
apnea/hypopnea syndrome.
Both approvals include the adjunctive use of modafinil in patients who are
receiving adequate treatment for their OSA/HS with standard therapy continuous
positive airway pressure.
Stock should see continued movement into the after-hours.
http://www.midnighttrader.com
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LANGUAGE: ENGLISH
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Copyright 2003 MidnightTrader.com. All rights reserved.
Unauthorized reproduction is strictly prohibited.
743 of 998 DOCUMENTS
PR Newswire
October 9, 2003 Thursday
Cephalon Receives Approval for Expanded Use of Modafinil in Germany and the
Republic of Ireland
SECTION: FINANCIAL NEWS
LENGTH: 984 words
Market Authorization Received for the Treatment of Excessive Daytime
Sleepiness Associated with Obstructive Sleep Apnea/Hypopnea Syndrome
WEST CHESTER, Pa., Oct. 9 /PRNewswire-FirstCall/ -- Cephalon, Inc. (Nasdaq:
CEPH) announced today that the company has received authorization from the
Federal Institute for Drugs and Devices (BfArM) and the Irish Medicines Board
(IMB) to market modafinil tablets in Germany and the Republic of Ireland,
respectively, for the treatment of excessive daytime sleepiness associated with
obstructive sleep apnea/hypopnea syndrome (OSA/HS). Both approvals include the
adjunctive use of modafinil in patients who are receiving adequate treatment for
their OSA/HS with standard therapy continuous positive airway pressure (CPAP).
Modafinil is marketed under the trade name VIGIL(R) in Germany and under the
trade name PROVIGIL(R) in Ireland.
"Modafinil is an important component of our European business, and these
approvals and our label expansion strategy will contribute to our growing
presence in the European market," said John Dawson, Vice President,
Pharmaceutical Operations Europe.
Modafinil
Modafinil is the first in a new class of wake-promoting agents believed to work
selectively through the sleep/wake centers to activate the cortex of the brain.
The drug is currently approved in more than 20 countries for the treatment of
excessive daytime sleepiness associated with narcolepsy.
In December of 2002, PROVIGIL was approved to treat excessive daytime sleepiness
in patients with obstructive sleep apnea/hypopnea syndrome in the UK.
On September 25, 2003, the Peripheral and Central Nervous System Advisory
Committee of the U.S. Food and Drug Administration recommended to expand the
label for PROVIGIL (modafinil) $(C-IV$) beyond its current indication for
excessive daytime sleepiness associated with narcolepsy. The FDA is expected to
determine the precise language of the modified label for PROVIGIL by year-end.
In controlled clinical trials, modafinil has been found to be generally well
tolerated with a low incidence of adverse events relative to placebo. The most
commonly observed adverse events associated with the use of modafinil were
headache, infection, nausea, nervousness, anxiety and insomnia.
Obstructive Sleep Apnea/Hypopnea Syndrome
Obstructive sleep apnea/hypopnea syndrome is a serious and potentially
life-threatening sleep disorder affecting four percent of middle-aged men and
two percent of middle-aged women. Individuals with obstructive sleep
apnea/hypopnea syndrome experience frequent awakenings throughout the night as a
result of blockage of the airway during sleep. This disruption of sleep leads to
excessive daytime sleepiness causing many people to doze off repeatedly
throughout the day -- at their jobs and at home.
The most commonly used standard treatment is continuous positive airway pressure
(CPAP). A nasal CPAP device can prevent airway closure while in use and
therefore is used to treat the underlying disorder. Despite treatment of the
underlying disorder, many patients continue to experience residual excessive
sleepiness and may be candidates for modafinil.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,400 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England,
Martinsried, Germany, and at Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding the timing of FDA action on Cephalon's sNDA, the
opportunity created by an expanded PROVIGIL label, anticipated scientific
progress on its research programs, development of potential pharmaceutical
products, interpretation of clinical results, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
SOURCE Cephalon, Inc.
CONTACT: Media: Robert Grupp, +1-610-738-6402, rgrupp@cephalon.com; or Investor:
Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com, both of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2003 PR Newswire Association, Inc.
744 of 998 DOCUMENTS
PR Newswire Europe
October 9, 2003 Thursday
Cephalon receives approval for expanded use of Modafinil in Germany and the
Republic of Ireland
LENGTH: 1018 words
- Market authorization received for the treatment of excessive daytime
sleepiness associated with obstructive sleep Apnea/Hypopnea Syndrome
Cephalon, Inc. announced today that the company has received authorization from
the Federal Institute for Drugs and Devices [BfArM] and the Irish Medicines
Board [IMB] to market modafinil tablets in Germany and the Republic of Ireland,
respectively, for the treatment of excessive daytime sleepiness associated with
obstructive sleep apnea/hypopnea syndrome [OSA/HS]. Both approvals include the
adjunctive use of modafinil in patients who are receiving adequate treatment for
their OSA/HS with standard therapy continuous positive airway pressure [CPAP].
Modafinil is marketed under the trade name VIGIL[R] in Germany and under the
trade name PROVIGIL[R] in Ireland.
"Modafinil is an important component of our European business, and these
approvals and our label expansion strategy will contribute to our growing
presence in the European market," said John Dawson, Vice President,
Pharmaceutical Operations Europe.
Modafinil
Modafinil is the first in a new class of wake-promoting agents believed to work
selectively through the sleep/wake centers to activate the cortex of the brain.
The drug is currently approved in more than 20 countries for the treatment of
excessive daytime sleepiness associated with narcolepsy.
In December of 2002, PROVIGIL was approved to treat excessive daytime sleepiness
in patients with obstructive sleep apnea/hypopnea syndrome in the UK.
On September 25, 2003, the Peripheral and Central Nervous System Advisory
Committee of the U.S. Food and Drug Administration recommended to expand the
label for PROVIGIL [modafinil] [C-IV] beyond its current indication for
excessive daytime sleepiness associated with narcolepsy. The FDA is expected to
determine the precise language of the modified label for PROVIGIL by year-end.
In controlled clinical trials, modafinil has been found to be generally well
tolerated with a low incidence of adverse events relative to placebo. The most
commonly observed adverse events associated with the use of modafinil were
headache, infection, nausea, nervousness, anxiety and insomnia.
Obstructive Sleep Apnea/Hypopnea Syndrome
Obstructive sleep apnea/hypopnea syndrome is a serious and potentially
life-threatening sleep disorder affecting four percent of middle-aged men and
two percent of middle-aged women. Individuals with obstructive sleep
apnea/hypopnea syndrome experience frequent awakenings throughout the night as a
result of blockage of the airway during sleep. This disruption of sleep leads to
excessive daytime sleepiness causing many people to doze off repeatedly
throughout the day -- at their jobs and at home.
The most commonly used standard treatment is continuous positive airway pressure
[CPAP]. A nasal CPAP device can prevent airway closure while in use and
therefore is used to treat the underlying disorder. Despite treatment of the
underlying disorder, many patients continue to experience residual excessive
sleepiness and may be candidates for modafinil.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,400 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England,
Martinsried, Germany, and at Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL[R] [tiagabine hydrochloride] and ACTIQ[R] [oral transmucosal
fentanyl citrate] [C-II] and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at http://www.cephalon.com/ or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding the timing of FDA action on Cephalon's sNDA, the
opportunity created by an expanded PROVIGIL label, anticipated scientific
progress on its research programs, development of potential pharmaceutical
products, interpretation of clinical results, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
Web site: http://www.cephalon.com/Cephalon
CONTACT:
Media: Robert Grupp, +1-610-738-6402, rgrupp@cephalon.com; or Investor: Chip
Merritt, +1-610-738-6376, cmerritt@cephalon.com, both of Cephalon/ First Call
Analyst: Robert S. Merritt/ Company News On-Call:
http://www.prnewswire.com/comp/134563.html
LOAD-DATE: October 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 PR Newswire Europe Limited
745 of 998 DOCUMENTS
The Independent (London)
October 4, 2003, Saturday
SPORT LETTERS: HEALTHY CASE
BYLINE: HANS NAERT
SECTION: SPORT; Pg. 9
LENGTH: 150 words
Sir: It would be an unacceptable mistake to disqualify Kelli White as the world
champion in the 100 and 200 metres dash. The IAAF wants that because they found
Modafinil in her urine after the 100m. Modafinil is not, however, on the list of
banned products. The IAAF's statement that it is a "light stimulant" and a
"related product" is extremely vague and subjective.
Modafinil is a kind of anti-sleeping pill, the best medicine to fight the
symptoms of narcolepsy, a disease from which White suffers. Narcolepsy is a form
of brain damage that makes her fall asleep without being tired.
White needs Modafinil for her health, not to run faster. This makes it a
medicine, not a doping product. She is clearly a victim of false accusations.
She should take legal action against the IAAF. An athlete doesn't have to accept
this kind of treatment.
HANS NAERT
Berchem, Netherlands
LOAD-DATE: October 6, 2003
LANGUAGE: ENGLISH
Copyright 2003 Independent Print Ltd
746 of 998 DOCUMENTS
Agence France Presse -- English
September 24, 2003 Wednesday
Anti-doping body place 'Kelli White drug' on banned list
SECTION: Sports
LENGTH: 392 words
DATELINE: MONTREAL, Sept 23
The World Anti-Doping Agency (WADA) added Modafinil, the stimulant which may
cost American sprinter Kelli White her two world sprint titles, to its list of
banned substances here on Tuesday.
Caffeine and pseudoephedrine were however taken off the list, which will be
published on WADA's website on October 1.
"Changes to the list this year include the removal of caffeine and
pseudoephedrine. Some substances, such as modafinil, have been added," said a
statement after the final day of the global anti-drugs body's Executive
Committee.
Modafinil, known in the United States by the brand name Provigil, was found in
White's urine sample after her 100 metres victory at last month's World
Championships in Paris.
White claimed she took the drug to combat narcolepsy, or extreme tiredness, but
the International Association of Athletics Federations rejected her explanation
and passed the case on to the US Anti-Doping Agency (USADA).
Although White is likely to lose her titles, she will not be banned because
Modafinil was not on the banned list although it was considered related to drugs
that were. By adding it to the list, WADA will hope to eliminate a troublesome
grey area.
WADA said it had examined a number of reprisals for countries who fail to pay
their fees to the Agency, which has collected less than 63 percent of dues owned
for 2003.
Major contributors such as the United States and Italy are among those late in
paying up.
In a statement, WADA said it was considering "removing members from the
Executive Committee or Board whose countries or regions have not paid their
dues. It will also be recommended to the Board that no laboratory receive
accreditation or re-accreditation from WADA until the country in which the lab
is situated has met its financial commitments to the Agency."
It said WADA would ask for support from the International Olympic Committee on
the matter.
WADA President Dick Pound said he still hoped the World Anti-Doping Code would
be adopted by all sports federations in time for next year's Athens Olympics.
"The speed with which governments and sports organizations are adopting the Code
is very encouraging," Pound said in a statement. "I believe we are well on our
way to implementation of the Code by the sports world prior to Athens".
pjl/gj
Sport-doping-WADA-Athletics
LOAD-DATE: September 24, 2003
LANGUAGE: ENGLISH
Copyright 2003 Agence France Presse
747 of 998 DOCUMENTS
Contra Costa Times
September 24, 2003 Wednesday FINAL EDITION
WHITE PONDERING HANGING UP SPIKES
BYLINE: ANN TATKO, TIMES COLUMNIST
SECTION: SPORTS; Pg. B03
LENGTH: 782 words
SPRINTER KELLI WHITE said next season likely will be her last as a track
athlete.
Since testing positive for a stimulant at the world championships last month,
White said, she has struggled to deal with physical and emotional strain.
She intimated before last week's Moscow Challenge that retirement may come
sooner rather than later. She said Tuesday by phone that sooner probably means
after next summer's Olympics.
"What I'm going through now has forced me to re-evaluate how much longer I want
to be in this sport," White, 26, said. "I have other options. I'd like to start
a few businesses, and a family, eventually. This situation has been very
difficult and I'm not sure if (competing) is worth it any more."
White, a former El Sobrante resident, tested positive for modafinil after
winning the 100-meter world title Aug. 24. White said she was prescribed
modafinil for a sleeping disorder. She no longer takes the medication, she said,
which has led to her feeling weak and tired.
Although she wasn't suspended from competition, White may lose the two gold
medals she won at the championships. The U.S. Anti-Doping Agency is reviewing
her case.
On Tuesday in Montreal, a two-day meeting of the World Anti-Doping Agency
executive committee made modafinil a banned stimulant for the first time. (At
the same time, the committee removed caffeine and pseudoephedrine, an ingredient
in over-the-counter cold remedies such as Sudafed, from the list of banned
substances for international sports.)
White said she was hit hardest by the boos she has received from fans at three
meets since worlds.
"I know next year will be difficult, too," she said. "But I intend to stick it
out. After that, it probably will be time to move on."
SILVER ALL AROUND: M.J. McColgan of Danville and David Bueche of Concord won
silver medals at last week's National Special Olympics Golf Championships in
Port St. Lucie, Fla.
McColgan competed in the level 3 tournament - an 18-hole Ryder Cup format - with
his father, Mike. He shot a three-day total of 270 to finish second by five
strokes behind Mike and John Higgs of Michigan.
McColgan also won silver last year. He bettered his score this year by seven
strokes.
Competing at level 5, in an 18-hole individual stroke play, Bueche seemed headed
for gold after shooting 36 on the front nine. He finished the day at 81, two
strokes behind winner Kevin Erickson of Wisconsin.
The championship was open to 158 of the nation's top golfers who have some form
of disability.
HAWAIIAN DEBUT: Brent Descalopoulis, 35, of Pleasanton will join about 1,500
competitors at next month's Ironman World Championships in Kailua Kona, Hawaii.
Descalopoulis, an air traffic controller, is making his first trip to the world
championships, which will be held Oct. 18.
The ironman triathlon features a 2.4-mile swim, 112-mile bike ride and 26.2-mile
marathon. Athletes have 17 hours to complete the competition.
ONE DOWN: Logan Tom of Stanford helped the U.S. women's volleyball team secure a
spot in the first Olympic qualifier.
Team USA defeated three-time defending Olympic champion Cuba at the NORCECA Zone
Championship in Santo Domingo, Dominican Republic, last week. Tom scored 12
points in the match.
Both teams advance to the World Cup, to be held Nov. 1 to 15 in Japan. The top
three finishers at the World Cup earn a berth to next summer's Olympics.
ROSTER SELECTIONS: USA Baseball officials will announce today the 32 players who
will attend next week's USA team trials in Phoenix. They will make the
announcement live on MLB.com Radio at 9 a.m. The trials will determine the
25-man roster for an Olympic qualifying event that begins Oct. 30 in Panama.
College and minor-league baseball players are eligible to compete, but
major-league players are not.
Montreal Expos manager Frank Robinson will manage the U.S. national team, USA
Baseball announced.
QUICK HITS: Sayaka Matsumoto of Richmond failed to place at the World Judo
Championships in Osaka, Japan, last week. Competing at 48 kilograms, Matsumoto
lost to eventual silver medalist Frederick Jossinet of France in the first round
and to Danieska Carrion of Cuba in the first repechage (a second-chance match.)
n Former Cal star Holly McPeak and Elaine Youngs lost in a first-round playoff
at the women's U.S. Grand Slam beach volleyball tournament last week in Los
Angeles. McPeak and Youngs won their three pool play matches before falling
22-20, 21-17 to Tian Jia and Wang Fei of China in the first round.
The PGA, USA Volleyball, U.S. Judo, U.S. Sailing and USA Baseball contributed
information for this article. Contact Ann Tatko at atatko@cctimes.com.
LOAD-DATE: November 10, 2005
LANGUAGE: ENGLISH
Copyright 2003 Contra Costa Times
All Rights Reserved
748 of 998 DOCUMENTS
The New York Times
September 24, 2003 Wednesday
Late Edition - Final
Sports Briefing
SECTION: Section D; Column 1; Sports Desk; Pg. 7
LENGTH: 830 words
INTERNATIONAL SPORTS
Caffeine and a Cold Medication No Longer Banned; Modafinil Is
Caffeine and pseudoephedrine, an ingredient in over-the-counter cold remedies
like Sudafed, were removed from the list of banned substances for international
sports.
The World Anti-Doping Agency said yesterday in Montreal that it wanted to
prevent the suspensions of athletes who took common cold remedies or drank cola
or coffee.
A two-day meeting of W.A.D.A.'s executive committee also made modafinil a banned
stimulant for the first time. That is the medication that could cost the
American sprinter Kelli White two gold medals from the world championships last
month.
Last week, Arne Ljungqvist, the head of W.A.D.A.'s medical research committee,
said the list would be changed to reflect changing times. The agency has set a
deadline of Oct. 1 for final ratification of the list, which would take effect
globally Jan. 1. The list applies to all sports and all countries covered by
W.A.D.A.'s global anti-doping code. It would be in force for next year's Athens
Olympics. (AP)
SWIMMING
Champion's Suspension Reduced
The Olympic freestyle champion Claudia Poll's suspension for testing positive
for a banned steroid was cut to two years, allowing her to compete next year in
the Athens Games.
FINA, swimming's world governing body, said yesterday in Geneva that Poll, a
30-year-old Costa Rican swimmer, was benefiting from its new doping code,
applied retroactively.
Poll, the 200-meter freestyle champion at the 1996 Atlanta Games, tested
positive for the banned steroid norandrosterone in an out-of-competition test in
2002 and was suspended for four years.
FINA also said that the Greek swimmer Vasileios Demetis, barred for life after
testing positive for norandrosterone and lidocaine two years ago, would also be
allowed to return to competition because of the new rule, adopted Sept. 11. (AP)
FIGURE SKATING
Yagudin and Slutskaya Pull Out
The Olympic champion Aleksei Yagudin and the 2002 world champion Irina
Slutskaya withdrew yesterday from next week's International Figure Skating
Classic at Madison Square Garden.
Yagudin, a four-time world champion from Russia attempting to come back from a
severe hip injury that sidelined him last season, is still not fully fit. Scott
Smith of the United States will replace Yagudin. Smith won the silver medal at
the Nebelhorn Trophy earlier this month in the first event tested under the
International Skating Union's new judging system.
Slutskaya withdrew with an illness. The American Jennifer Kirk will replace
Slutskaya. (AP)
COLLEGE FOOTBALL
F.S.U.'s Rix Is Ticketed Again
Florida State quarterback Chris Rix was ticketed again yesterday for a parking
violation, this time for leaving his vehicle in a spot reserved for patients at
the university's regional rehabilitation center in Tallahassee.
Rix was ticketed last week for parking in a handicapped-only spot and was fined
$100. Yesterday's offense was reported by a student who took several photos of
Rix's vehicle, university officials said.
Team officials imposed a punishment of extra running drills against Rix this
week in response to the handicapped-spot ticket. More team-imposed penalties
against Rix are possible, Coach Bobby Bowden said yesterday. Rix refused to
comment. (AP)
PRO BASKETBALL
Lobo Retires from W.N.B.A.
Rebecca Lobo retired yesterday after a career in which she led Connecticut to
its first N.C.A.A. basketball championship and helped launch the W.N.B.A. Lobo,
30, who spent last season with the Connecticut Sun, was plagued by knee injuries
during her seven years in the W.N.B.A.
"While I still love playing the game, in my heart, I know it's time to move on
to a new phase of my life," the 6-foot-4 Lobo said.
Lobo led UConn to the national championship in 1995, when the team went 35-0.
She was one of the W.N.B.A.'s original players in 1997, assigned to the Liberty.
She spent the first five years of her pro career in New York, missing almost two
full seasons because of knee injuries. Lobo averaged 6.7 points and 4.1 rebounds
in 121 W.N.B.A. games. (AP)
Shaw Retiring From Lakers
Los Angeles Lakers guard Brian Shaw, 37, is retiring after 14 N.B.A. seasons to
join the team's front office. He won three N.B.A. titles in four seasons with
the Lakers, and averaged 6.9 points in 943 N.B.A. games with seven teams. (AP)
Coles Returns to Heat
The free-agent point guard Bimbo Coles returned to the team where he started
his career, signing with the Miami Heat yesterday.
The 6-foot-2 Coles, a 13-year N.B.A. veteran, played for Cleveland and Boston
last season and averaged 4.4 points. (AP)
SOCCER
New Owner for M.L.S.'s Rapids
Stan Kroenke, owner of basketball's Denver Nuggets and hockey's Colorado
Avalanche, bought Major League Soccer's Colorado Rapids and plans to build them
a soccer-only stadium.
Kroenke purchased the Rapids from Phil Anschutz, who still owns 5 of the
league's 10 teams. Financial terms of the sale were not disclosed. (Bloomberg
News)
URL: http://www.nytimes.com
LOAD-DATE: September 24, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The New York Times Company
749 of 998 DOCUMENTS
Associated Press Worldstream
September 12, 2003 Friday
IAAF confirms White's entry in sprints at Final
SECTION: SPORTS
LENGTH: 250 words
DATELINE: MONTE CARLO, Monaco
American sprinter Kelli White, under investigation for testing positive for a
minor stimulant at the Paris worlds, will attempt a sprint double at the
inaugural World Athletics Final this weekend, the sport's governing body said
Friday.
White was originally only entered in the 100 meters in Monaco.
"Kelli White is scheduled to run in both 100 and 200 meters," IAAF spokesman
Nick Davis told The Associated Press by telephone.
White tested positive for modafinil after winning the 100 meters at the World
Championships on August 24, and four days later won the 200 meters. She set
personal best times in both races.
Because modafinil is considered a minor stimulant, the IAAF did not suspend
White. She won the 100 meters at a Golden League meeting in Brussels on
September 5.
But the IAAF rejected a doctor's report explaining why she needed to take
modafinil. White had claimed she used it to treat a sleep-related disorder
called narcolepsy.
The IAAF has now asked U.S. track officials to begin disciplinary measures
against her. If found guilty of doping, White will be stripped of both her world
championship gold medals.
White is now scheduled to compete in Saturday's 200 meters and in the 100 on
Sunday. She joins some 30 world champions and 250 other athletes competing in
the event.
The World Athletics Final is the last event of the season before the male and
female World Athletes of the Year are crowned. Points gained over the weekend
count toward the overall rankings.
LOAD-DATE: September 13, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
750 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
September 12, 2003, Friday
White says she will fight to maintain two gold medals
SECTION: WORLD NEWS; SPORTS
LENGTH: 174 words
LONDON, Sept. 12 (Xinhua) -- American double world sprint champion Kelli White,
who tested positive for modafinil at the Paris world championships, said on
Friday she would fight to keep her gold medals.
The International Association of Athletics Federations(IAAF) said early this
week that it did not accept White's explanation for her positive test for
modafinil and had referred the matter to the U.S. anti-doping agency.
White, who tested positive after winning the 100 meters on August 24, said she
took the prescribed medication to combat narcolepsy. A second test after the 200
final was clean.
If she is found guilty of a doping offence then she would be disqualified and
forced to give up both her gold medals.
"No way. No way. I'm still going to fight to keep the medals," White told CNN on
Friday. "I still think there is a chance that I will be able to keep my medals.
Modafinil is not yet on the IAAF's banned list, therefore, White is still able
to compete at this weekend's IAAF Grand Prix Final in Monaco.
LOAD-DATE: September 13, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
751 of 998 DOCUMENTS
Herald Sun (Melbourne, Australia)
September 11, 2003 Thursday
IAAF rejects White's drug defence
SOURCE: REUTERS
SECTION: SPORT; Pg. 60
LENGTH: 281 words
THE International Association of Athletics Federations has rejected double world
sprint champion Kelli White's explanation of why she tested positive for the
stimulant modafinil at the world championships in Paris last month.
IAAF spokesman Nick Davies said her explanation had not been accepted and, in
accordance with the normal disciplinary procedures, her case had been referred
to the US anti-doping agency for a hearing.
White, the first American to win the 100m-200m sprint double, has not been
suspended pending her hearing and can run at this weekend's inaugural World
Athletics Final at Monaco's Stade Louis II. However, if she was found guilty of
a doping offence she would be stripped of the individual gold medals she won in
Paris.
The 26-year-old White tested positive for modafinil, which is not on the IAAF
banned list, after winning the 100m final on August 24. A urine sample taken
after she won the 200m four days later was clean.
The sprinter said at the time that she had been prescribed modafinil to combat
narcolepsy, or sleepiness, and had not sought exemption or entered it on her
doping control form because it was not on the banned list.
The IAAF said last week that modafinil, which is related to prohibited drugs,
will be classified as a weaker stimulant and placed on the World Anti-Doping
Agency's banned list next year.
White has until September 29 to ask for the B sample to be examined, which she
is expected to do, and the US anti-doping agency then has up to three months to
hear her case.
If the IAAF does not then agree with the result of that hearing it can take the
case to the Court of Arbitration for Sport in Switzerland.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: DHS
Copyright 2003 Nationwide News Pty Limited
752 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 10, 2003, Wednesday, BC cycle
IAAF rules Kelli White guilty of doping offense
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 622 words
DATELINE: LONDON
Track and field's governing body wants American sprinter Kelli White stripped of
her two gold medals from the World Championships. Now it's up to U.S.
anti-doping officials.
The International Association of Athletics Federations ruled Tuesday that White
committed a doping offense when she tested positive for a stimulant and should
lose her world titles in the 100 and 200 meters.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of Tuesday
afternoon. Once that information is received, Wanninger said, the agency will
begin a review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "Our experts
have determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200. White would
also lose the $120,000 in prize money she won at the worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds. She is to run in the Grand Prix final in Monaco
this weekend and a meet in Moscow on Sept. 20.
LOAD-DATE: September 11, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
753 of 998 DOCUMENTS
Birmingham Post
September 10, 2003, Wednesday
ATHLETICS: WHITE FACING US DRUG HEARING
SECTION: SPORT; Pg. 24
LENGTH: 300 words
The International Association of Athletics Federations (IAAF) has rejected
double world sprint champion Kelli White's explanation of why she tested
positive for a stimulant at the world championships.
'The IAAF has received the athlete's explanation for testing positive for
modafinil at the world championships in Paris last month,' IAAF spokesman Nick
Davies said yesterday.
'Following careful examination, the explanation has not been accepted.
'The matter has now be referred to the United States anti-doping agency for a
hearing.'
White (pictured), the first American to win the 100-200 metres sprint double,
has not been suspended pending her hearing before the US antidoping agency and
can therefore run at this weekend's inaugural World Athletics Final at Monaco's
Stade Louis II.
However, if she is found guilty of a doping offence, White would be stripped of
the individual gold medals she won in Paris last month.
'The IAAF has already announced that if it is confirmed after the hearing that
the athlete has committed a doping offence, the sanction under IAAF rules will
be a public warning and disqualification from the competition,' said Davies.
The 26-year-old White tested positive for modafinil, which is not at present on
the IAAF banned list, after winning the 100m final on August 24. A urine sample
taken after she won the 200 four days later was found to be clean.
The sprinter said at the time that she had been prescribed modafinil to combat
narcolepsy sleepiness and had not sought exemption, or entered it on her doping
control form, because it was not on the banned list.
The IAAF said last week that modafinil is now to be classified as a weaker
stimulant and will be placed on the World Anti-Doping Agency's banned list next
year.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
PUB-TYPE: PAPER
Copyright 2003 Midland Independent Newspapers plc
754 of 998 DOCUMENTS
Birmingham Post
September 10, 2003, Wednesday
ATHLETICS: WHITE FACING US DRUG HEARING
SECTION: SPORT; Pg. 24
LENGTH: 300 words
The International Association of Athletics Federations (IAAF) has rejected
double world sprint champion Kelli White's explanation of why she tested
positive for a stimulant at the world championships.
'The IAAF has received the athlete's explanation for testing positive for
modafinil at the world championships in Paris last month,' IAAF spokesman Nick
Davies said yesterday.
'Following careful examination, the explanation has not been accepted.
'The matter has now be referred to the United States anti-doping agency for a
hearing.'
White (pictured), the first American to win the 100-200 metres sprint double,
has not been suspended pending her hearing before the US antidoping agency and
can therefore run at this weekend's inaugural World Athletics Final at Monaco's
Stade Louis II.
However, if she is found guilty of a doping offence, White would be stripped of
the individual gold medals she won in Paris last month.
'The IAAF has already announced that if it is confirmed after the hearing that
the athlete has committed a doping offence, the sanction under IAAF rules will
be a public warning and disqualification from the competition,' said Davies.
The 26-year-old White tested positive for modafinil, which is not at present on
the IAAF banned list, after winning the 100m final on August 24. A urine sample
taken after she won the 200 four days later was found to be clean.
The sprinter said at the time that she had been prescribed modafinil to combat
narcolepsy sleepiness and had not sought exemption, or entered it on her doping
control form, because it was not on the banned list.
The IAAF said last week that modafinil is now to be classified as a weaker
stimulant and will be placed on the World Anti-Doping Agency's banned list next
year.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
PUB-TYPE: PAPER
Copyright 2003 Midland Independent Newspapers plc
755 of 998 DOCUMENTS
Contra Costa Times
September 10, 2003 Wednesday FINAL EDITION
SPRINTER WHITE SUFFERS SETBACK;
IAAF RULES THE WORLD CHAMPION IS GUILTY OF A DOPING VIOLATION
BYLINE: ANN TATKO, TIMES STAFF WRITER
SECTION: SPORTS; Pg. B01
LENGTH: 563 words
Track and field's governing body on Tuesday found sprinter Kelli White guilty of
a doping violation, but she plans to fight any disciplinary action that results
in the loss of her gold medals from the world championships.
The International Association of Athletics Federation ruled White committed a
doping offense when she tested positive for a stimulant after her 100-meter
victory at last month's meet in Paris. Four days later, she passed a drug test
after winning the 200.
The case now moves to the U.S. Anti-Doping Agency to determine what disciplinary
action should be taken.
Rich Wanninger, a spokesman for the USADA, said the IAAF had not turned the case
over to his organization as of Tuesday afternoon. Once the information is
received, USADA will hold a hearing that could last several months, Wanninger
said by phone from Colorado Springs, Colo.
Cases such as these usually end with an athlete receiving a public warning and
disqualification from the entire championships.
That would cost White both of her gold medals.
"I'm very disappointed by the finding," White said by phone Tuesday from Monte
Carlo, Monaco. "I have never taken any performance-enhancing drug. (The IAAF
officials) have called my reputation into question. Of course, I am going to
fight that."
White, a former El Sobrante resident, said her doctor prescribed the stimulant,
modafinil, for a sleeping disorder. Although not on the banned list of drugs,
modafinil is classified as a "related substance."
Because the drug was not on the banned list, White said she didn't seek a
medical waiver or list taking the medication on doping control forms, as
required, at the world championships.
IAAF general secretary Istvan Gyulai said that was not a viable excuse.
"Her explanation was rejected," Gyulai said by phone Tuesday from IAAF
headquarters in Monaco. "Athletes must take responsibility for knowing the rules
and following them. Our experts have determined this medication is a
performance-enhancing stimulant; therefore, it is a doping violation."
Understanding what results in a doping violation, however, is complex
considering the number of banned drugs and related substances. The USADA
provides a list that covers more than 50 pages.
White's doctor, Brian Goldman, argued that modafinil has no
performance-enhancing value but added that he should have checked the drug more
thoroughly against the list provided by the USADA.
White said she also shares some of the responsibility.
"I realize in hindsight that I should have done some things differently," she
said. "But I didn't win the medals because I took (modafinil). I've won races
all year without once testing positive."
White avoided the harshest discipline when the IAAF last week ruled modafinil is
a light stimulant as opposed to strong stimulant, which would have resulted in a
two-year suspension from competition.
An appeal is expected regardless of how the USADA's hearing concludes.
White said she will not give up her medals -- and the $120,000 prize money she
won because of them -- without a fight.
Should the USADA decide she can keep the medals, Gyulai said, IAAF officials
will send the case to the Court of Arbitration for Sport in Lausanne,
Switzerland. That court has the final ruling in all doping violation cases.
The Associated Press contributed to this story.
LOAD-DATE: November 10, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo 1, Kelli White mug. Photo 2, Kelli White. (Yves Logghe, AP)
Copyright 2003 Contra Costa Times
All Rights Reserved
756 of 998 DOCUMENTS
Deseret Morning News (Salt Lake City)
September 10, 2003, Wednesday
U.S. sprinter accused of doping
BYLINE: Associated Press
SECTION: SPORTS; Pg. D06
LENGTH: 406 words
U.S. sprinter Kelli White committed a doping offense at the World Championships
and should be stripped of her two gold medals, track and field's governing body
ruled Tuesday.
The International Association of Athletics Federations sent White's case to U.S.
track officials for disciplinary action.
A final ruling could take months.
White should be disqualified and stripped of the medals she won in the 100 and
200 meters last month in France, IAAF general secretary Istvan Gyulai said. A
final ruling could take months.
The U.S. Anti-Doping Agency must schedule a hearing with White. If it decides
not to disqualify White and remove the medals, the IAAF would take the case to
the Court of Arbitration for Sport in Lausanne, Switzerland.
White, the first American woman to sweep the two sprints at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for the
sleep disorder narcolepsy.
"The explanation has been studied and turned down," Gyulai told The Associated
Press. "Our experts have determined the stimulant is performance-enhancing."
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she did not
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required, or apply for a medical exemption to use the
product.
White has vowed to fight to keep her medals.
The IAAF ruled Sept. 4 that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil -- sold in the United States under the brand name Provigil -- been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White passed a drug test after the 200, the IAAF considers one positive
test enough for disqualification from the entire championships.
Under track and field rules, athletes are considered guilty of a doping
violation if banned substances are found in their bodies, regardless of the
circumstances.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Deseret News Publishing Co.
757 of 998 DOCUMENTS
Edmonton Journal (Alberta)
September 10, 2003 Wednesday Final Edition
IAAF wants White stripped of her medals but leaves it up to U.S. Anti-Doping
Agency to take action
SOURCE: The Associated Press
BYLINE: Stephen Wilson
SECTION: Sports; Pg. D1
LENGTH: 621 words
DATELINE: LONDON
LONDON - Track and field's governing body wants American sprinter Kelli White
stripped of her two gold medals from the World Championships.
Now it's up to U.S. anti-doping officials.
The International Association of Athletics Federations ruled Tuesday that White
committed a doping offence when she tested positive for a stimulant and should
lose her world titles in the 100 and 200 metres.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of Tuesday
afternoon. Once that information is received, Wanninger said, the agency will
begin a review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said.
"Our experts have determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance.
However, she did not declare modafinil on her doping control form as required or
apply for a medical exemption to use the product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil -- sold in the United States under the brand name Provigil -- been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200.
White would also lose the $120,000 US in prize money she won at the Worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds.
She is to run in the Grand Prix final in Monaco this weekend and a meet in
Moscow on Sept. 20.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: The Associated Press, File; American sprinter Kelli White
TYPE: Sports
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
758 of 998 DOCUMENTS
The Guardian (London)
September 10, 2003
Athletics: Drug plea by White rejected
BYLINE: Michael Phillips
SECTION: Guardian Sport Pages, Pg. 27
LENGTH: 202 words
Kelli White, the American double world champion who tested positive for the
stimulant modafinil, has had her letter of explanation rejected by the
International Association of Athletics Federations. The case has been passed on
to her governing body, USA Track and Field, and it will be dealt with by the
American anti-doping agency.
If the sprinter is found guilty she will lose the gold medals she won in the
100m and 200m in last month's World Championships in Paris and the Dollars
120,000 (pounds 76,000) prize money she would have received because she will be
disqualified from the competition.
White claimed she took modafinil to combat the sleeping disorder narcolepsy and
insisted she did not declare it to the IAAF because it was not on the list of
banned substances. She tested positive after the 100m.
The IAAF has since announced that because modafinil is a minor stimulant she
will incur a public warning and disqualification but no ban if found guilty of
the offence.
On Friday White won the 100m in the Golden League meeting in Brussels and this
weekend she is due to compete in the World Athletics Final in Monte Carlo where,
ironically, the IAAF has its headquarters.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Guardian Newspapers Limited
759 of 998 DOCUMENTS
Hamilton Spectator (Ontario, Canada)
September 10, 2003 Wednesday Final Edition
White will lose golds for using stimulant
SOURCE: The Associated Press
SECTION: SPORTS; Pg. E03
LENGTH: 457 words
DATELINE: LONDON
Track and field's governing body wants American sprinter Kelli White stripped of
her two gold medals from the World Championships.
Now it's up to U.S. anti-doping officials.
The International Association of Athletics Federations ruled yesterday that
White committed a doping offence when she tested positive for a stimulant and
should lose her world titles in the 100 and 200 metres.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of yesterday
afternoon. Once that information is received, he said, the agency will begin a
review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until yesterday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "Our experts
have determined the stimulant is performance-enhancing."
White was unavailable for comment. She said last week she will fight to keep her
medals. "Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance.
However, she did not declare modafinil on her doping control form as required or
apply for a medical exemption to use the product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification.
The decision allowed White to continue competing.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 Metroland Media Group Ltd
760 of 998 DOCUMENTS
The Independent (London)
September 10, 2003, Wednesday
ATHLETICS: WHITE TO LOSE PARIS MEDALS AS POSITIVE DRUG TEST CONFIRMED
BYLINE: MIKE ROWBOTTOM
SECTION: SPORT; Pg. 26
LENGTH: 379 words
KELLI WHITE'S doping infraction at the recent World Championships in Paris was
confirmed yesterday by the sport's international governing body, which intends
to disqualify her retrospectively and strip her of the 100 and 200 metres gold
medals she won in Paris. She also stands to lose the $ 120,000 (pounds 75,000)
prize money she picked up.
After examining details of the 26-year-old American's case, the International
Association of Athletics Federations found her guilty of taking a minor
stimulant. A final ruling could take weeks or months, however, as the case now
goes to the US Anti-Doping Agency, which must schedule a hearing with White. If
the US body decides not to disqualify White and remove the medals, the IAAF
would take the case to the Court of Arbitration for Sport in Lausanne.
White, the first American woman to win both sprints at a World Championships,
tested positive for modafinil after winning the 100m gold on 24 August. She
passed a drug test after winning the 200m four days later. The IAAF gave White
until yesterday to produce medical documents explaining her use of modafinil.
She said she took the medication on prescription from her personal doctor for
the sleep disorder narcolepsy.
"The explanation has been studied and turned down," Istvan Gyulai, the IAAF
secretary, said. "The IAAF has reached the conclusion she has committed a doping
offence. Our experts have determined the stimulant is performance- enhancing."
Modafinil is not named on the sport's list of banned drugs, but the IAAF says it
falls under the category of "related substances".
White denied taking the medication to enhance performance and said she had "no
idea" it contained a banned substance. However, she did not declare the
substance on her doping control form as required or apply for a medical
exemption to use the product.
The IAAF ruled last week that modafinil was a minor stimulant, similar to
ephedrine, and carried a penalty of a public warning and disqualification. The
decision allowed White to continue competing. Had modafinil - sold in the United
States under the brand name Provigil - been classified as a stronger stimulant,
White also would have faced a two-year ban and ineligibility for the 2004 Athens
Olympics.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Independent Print Ltd
761 of 998 DOCUMENTS
The New York Times
September 10, 2003 Wednesday
Late Edition - Final
Sprinter Likely to Lose Medals
SECTION: Section D; Column 5; Sports Desk; Pg. 4
LENGTH: 256 words
Track and field's world governing body has rejected the sprinter Kelli White's
explanation for taking a stimulant, recommending that she be stripped of the
gold medals she won at 100 and 200 meters at the recent world championships in
Paris.
The International Association of Athletics Federations, which governs the sport,
said yesterday it believed that White should receive a public warning for the
use of the stimulant modafinil, which means she faces disqualification from the
world championships.
In addition to losing her medals, she stands to forfeit $160,000 in prize money,
but she will not be barred from competition.
White will be granted a hearing before the United States Anti-Doping Agency,
which will rule on the case. No date for the hearing has been set. If White and
the I.A.A.F. accept the eventual ruling by the agency, the case will be closed.
If either side disagrees, the final arbiter will be the Court of Arbitration for
Sport in Switzerland.
White said she took modafinil to combat the fatigue and sleep-inducing affects
of narcolepsy. She failed to notify the I.A.A.F. that she was using the
stimulant, however, and she did not obtain a waiver. She said she did not know
the substance was banned. Modafinil is not listed among prohibited
performance-enhancing drugs, but is considered a related substance. "The
explanation has been studied and turned down," Istvan Gyulai, general secretary
of the I.A.A.F., told The Associated Press. "Our experts have determined the
stimulant is performance-enhancing."
URL: http://www.nytimes.com
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The New York Times Company
762 of 998 DOCUMENTS
San Jose Mercury News (California)
September 10, 2003 Wednesday MORNING FINAL EDITION
IAAF: WHITE SHOULD BE STRIPPED OF GOLD MEDALS;
RECOMMENDATION SETS OFF DEBATE
BYLINE: ELLIOTT ALMOND, Mercury News
SECTION: SPORTS; Pg. 1D
LENGTH: 913 words
In what could spark a protracted debate about doping and sports, track and field
officials ruled Tuesday that Kelli White of Union City should be stripped of her
world championship gold medals for failing a drug test.
The worldwide governing body for track and field rejected White's arguments that
the sleeping disorder medication in question -- modafinil -- had no performance
benefit.
The International Association of Athletics Federations will send the case to the
U.S. Anti-Doping Agency, which oversees drug testing for Olympians. A hearing
has not been scheduled but White has vowed to fight to keep the medals she won
in the 100 meters and 200 meters in France last month. It could take months
before it is resolved.
The latest episode in Olympic drug testing could have larger ramifications in
the complicated world of pharmacology and sports. Olympic leaders are trying to
curtail drug abuse at the same time White's supporters are challenging the
foundations used to exact punishment.
In documents provided to the Mercury News, physicians representing White
questioned the IAAF's definition of a banned substance.
"Essentially, we support the IAAF's strict enforcement of its rules, but those
of us who consult to the athletes would like to know prospectively what is on
the 'prohibited substances list,' and not be told retroactively," child
psychiatrist Brian Goldman wrote in a Sept. 2 letter to the IAAF.
Goldman, a volunteer consultant with Bay Area Laboratories Cooperative, which
works with world-class athletes, including White, said he gave the sprinter
medication for narcolepsy. He said some Internet information calling modafinil a
psycho-stimulant is incorrect. The company that makes the drug also said bad
information about modafinil was being distributed.
"If anyone says getting someone out of bed is enhancing performance, that would
be an interesting debate," said Sheryl Williams of Cephalon, the firm that
manufactures the medication.
The IAAF ruled that modafinil is a minor stimulant although it is not included
on its banned list. It comes under the category of "related substances." The
IAAF rejected White's claims because the group's experts determined the
stimulant is performance-enhancing, Secretary General Istvan Gyulai told the
Associated Press.
White's supporters say the IAAF has no basis for its ruling, which would cost
the sprinter at least $120,000 in prize money.
"They are not defining what is performance-enhancing," said Robert Picker, a
Concord psychiatrist who also sent the IAAF a letter on White's behalf. "What is
their argument? They are not providing one iota of evidence to show that this
drug is performance-enhancing."
Larry Bowers of the U.S. Anti-Doping Agency said the performance benefits of
modafinil were unclear. Although the drug did not have the properties of
amphetamines, Bowers said it could benefit an athlete by changing the perception
of fatigue.
"One could argue in a 100-meter or 200-meter race it might not be that
beneficial -- or it might be," he said last month.
Picker wrote to the IAAF: "In Ms. White's case, the only advantage it might give
her is not falling asleep at an inappropriate time and missing the bus to the
stadium. This is a case of the IAAF simply not keeping up to date on the science
involved."
White's case likely is headed for the Court of Arbitration for Sport (CAS), a
Swiss body of jurists that makes binding decisions about Olympic disputes. IAAF
officials said they would appeal the case to the court if U.S. officials reject
their recommendations. White seems likely to ask for a CAS ruling should she
lose her medals.
Goldman, who works at the Amen Clinics in Fairfield, said he gave White two
samples of the medication to see if it would help with her sleeping problem. She
took the drug on an as-needed basis.
"Kelli has complained of falling asleep while talking on the telephone, even if
it's during an interesting conversation," Goldman wrote in another
correspondence.
White's mother, Debra Byfield, and her aunt also suffer from the disorder, the
family said. Byfield, a 1972 Olympic runner for Jamaica, said her mother
exhibited similar symptoms.
White said she took the drug the morning of the 100-meter competition Aug. 24
because she felt "drained" in France. But after the race she did not list it on
a doping control form, a requirement almost every world-class athlete
understands. Even if she had included it, officials say she needed a medical
waiver to take the medication.
Olympic athletes face a catch-all phrase known as 'strict liability' when it
comes to what they ingest. They are responsible for any substance they take and
cannot claim ignorance if it turns up positive.
White, who is in Europe, could not be reached. But Byfield said the worst part
is the stigma of being viewed a drug cheat. "What it does, it erases the hard
work that she put in," Byfield said.
Although not related, White's situation has come at the same time as a raid on
Bay Area Laboratories Cooperative, a dietary supplement company in Burlingame.
Federal and San Mateo county authorities refuse to say why their agents searched
the firm of Victor Conte, and the home of Greg Anderson, Barry Bonds' personal
trainer. But Olympic drug testers are helping with the investigation, which is
ongoing.
White is one of the many elite athletes working with Conte, who professes to
help performers through natural means.
LOAD-DATE: August 16, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photos (2), Diagram;
DIAGRAM: T.G. TSO -- MERCURY NEWS
THE ANATOMY OF A DRUG CASE
Source: U.S. Anti-Doping Agency, Mercury News reporting
PHOTO: ANJA NIEDRINGHAUS -- ASSOCIATED PRESS
Kelli White wins the 200 at the world championships -- one of the gold medals in
dispute.
PHOTO: MICHEL EULER -- ASSOCIATED PRESS
Kelli White's case moves to the U.S. Anti-Doping Agency, which oversees drug
testing.
Copyright 2003 San Jose Mercury News
All Rights Reserved
763 of 998 DOCUMENTS
The Times (London)
September 10, 2003, Wednesday
White likely to lose tarnished gold medals after IAAF ruling
BYLINE: David Powell, Athletics Correspondent and John Goodbody
SECTION: Sport; 39
LENGTH: 448 words
THE sport's world governing body yesterday rejected the evidence from Kelli
White in defence of her failed drugs test at the World Championships in Paris
two weeks ago and insisted she be stripped of her two gold medals and $ 120,000
(about Pounds 76,000) in prize-money. White tested positive for a mild stimulant
after winning the women's 100 metres but returned a negative sample after her
200 metres victory.
White, from the United States, remains eligible to compete because the category
of drug carries only a warning. The International Association of Athletics
Federations (IAAF) will now expect White's national federation, USA Track &
Field (USATF), to confirm her punishment. Should it fail to do so, the case will
be decided by the Court of Arbitration for Sport.
After criticism of its handling of drugs cases up to the 2000 Olympics, USATF
agreed to delegate such matters to the United States Anti-Doping Agency, whose
first step will be to arrange a hearing with White, 26.
White said in Paris that she had taken the drug, modafinil, on prescription from
her doctor to counter narcolepsy, a condition that ran in her family, but,
having failed either to declare it on her drug-testing form or seek an
exemption, her defence is weak.
Already back in competition, having won the 100 metres at the Golden League
meeting in Brussels on Friday, White said that she would fight to keep her
medals and winnings. "Whatever I have to do to keep them, I will do," she said.
She stands to lose her 200 metres rewards, as well as those from the 100 metres,
because, under IAAF rules, an athlete is disqualified from the meeting in which
the offence was committed.
Although not named on the banned list, modafinil falls into the "related
substances" category, carrying the same penalty as specified drugs. Cephalon,
the manufacturer of Provigil, by which modafinil is sold under licence, said
that it had not "systematically evaluated" its effect on athletes, but Istvan
Gyulai, the IAAF secretary, said: "Our experts have determined (it) is
performance-enhancing."
Even before the White case, the World Anti-Doping Agency had asked for modafinil
to be added to the banned list from next year.
Torri Edwards, White's compatriot, who was second in the 100 metres, and
Anastasiya Kapachinskaya, from Russia, runner-up in the 200 metres, may have to
wait months before the process is exhausted if they are to be crowned champions.
Should White's punishment be confirmed, she will lose not only her prize-money
and medals but the chance of a lucrative match-up with Marion Jones, the Olympic
champion who missed the World Championships after giving birth.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Times Newspapers Limited
764 of 998 DOCUMENTS
Tulsa World (Oklahoma)
September 10, 2003 Wednesday Final Home Edition
Sports FYI: White ruled guilty
BYLINE: Staff Reports
SECTION: SPORTS; General Sports; Pg. B2
LENGTH: 1092 words
Last month Kelli White became the first American woman to sweep the 100- and
200-meter dashes at the World Championships. White committed a doping offense at
the worlds and the IAAF has recommended she be stripped of her medals. ANJA
NIEDRINGHAUS / Associated Press file
TRACK
U.S. sprinter Kelli White committed a doping offense at the World Championships
and should be stripped of her two gold medals, the sport's governing body ruled
at Monte Carlo, Monaco, Tuesday. The International Association of Athletics
Federations sent White's case to U.S. officials for disciplinary action.
White should be disqualified and stripped of the medals she won in the 100 and
200 meters last month in France, IAAF general secretary Istvan Gyulai said. A
final ruling could take months.
The U.S. Anti-Doping Agency must schedule a hearing with White. If it decides
not to disqualify White and remove the medals, the IAAF would take the case to
the Court of Arbitration for Sport in Lausanne, Switzerland.
White, the first American woman to sweep the two sprints at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for the
sleep disorder narcolepsy. Modafinil is not on the sport's list of banned drugs,
but the IAAF says it falls under the category of "related substances."
White denied taking the medication to enhance performance and said she did not
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required, or apply for a medical exemption to use the
product. White has vowed to fight to keep her medals.
The IAAF ruled Sept. 4 that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil -- sold in the United States under the brand name Provigil -- been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
TENNIS
Roddick leads U.S. team: U.S. Open champion Andy Roddick will lead an American
Davis Cup team that plays at Slovakia this month in a World Group playoff.
Roddick is joined by Mardy Fish, James Blake, Brian Vahaly and twins Bob and
Mike Bryan. The nominations by the U.S. Tennis Association and captain Patrick
McEnroe were submitted to the International Tennis Federation.
GOLF
Cowgirls ranked No. 4: Golfweek Magazine has ranked Oklahoma State fourth in its
preseason women's collegiate poll. Duke was ranked No. 1, followed by UCLA
(second) and Ohio State (third). Sophomore Karin Sjodin and junior Annie Thurman
were named preseason first-team All-Americans. AUTO RACING
Lowe's keeps All-Star race: NASCAR's annual all-star race will remain at Lowe's
Motor Speedway in Charlotte, N.C., next season as part of the 36-race, Nextel
Cup schedule released. The Nextel All-Star Challenge will be run May 22 at
Lowe's, marking the 18th consecutive year the all-star event will be run at the
Concord track.
The Southern 500 at Darlington will now be run on Nov. 14 and be the penultimate
race in the Nextel Cup Series title chase. The switch was all part of NASCAR's
"Realignment 2004 and Beyond" plan, designed to move races out of the crowded
Southeastern market and into large cities.
California Speedway will run its traditional spring event on May 2. Its second
race will be Sept. 5, under the lights.
The only other change involved the order of the spring races at Talladega
Superspeedway and Martinsville Speedway. They will switch their order from the
previous year's schedule, with Martinsville being run April 18 and Talladega on
April 25. HORSE RACING
Jockey suspended: A jockey at Great Lakes Downs in Fruitport Township, Mich.,
has been suspended after allegations he used an electrical "buzzer" to influence
a race he won. A buzzer is a hand-held, battery-operated device that emits an
electric shock when pressed against the horse.
Jeffrey H. Faul declined to testify at a hearing before track stewards. The
stewards will consider the evidence and decide what action to take against Faul,
said Dominic Perrone, spokesman for the Michigan Office of Racing Commissioner.
Faul denies he cheated in the race, said his agent, Ron Salmon.
The state suspended Faul indefinitely pending a decision by the stewards. The
suspension decision was made after track stewards ruled there was credible
evidence of cheating.
The accusations stem from an Aug. 24 claiming race at the Muskegon County track
near Muskegon. Faul ran aboard Run for You and was among the leaders before
making a move at the top of the stretch, The Muskegon Chronicle reported. HOCKEY
Oilers add two: The Tulsa Oilers have signed defenseman Jordon Flodell and
forward/defenseman Rob Meanchoff.
Flodell is returing for his second season with the Oilers. Meanchoff is a
rookie, who recently finished his college career after four years with the
University of Ottawa. TENNIS
OSU players ranked: Oklahoma State has two individuals ranked in the ITA Top 75
for the first time in coach James Wadley's 32-year tenure. Mark Van Elden and
Yevgen Bondarchuk are ranked Nos. 32 and 55, respectively, in the preseason
rankings. Van Elden and Bondarchuck went 14-5 and 14-8 last year as the Cowboys'
Nos. 1 and 2 singles players. SOCCER
Zapata earns honor: Oral Roberts' Hector Zapata was named Mid-Continent
Conference Defensive Player of the Week. He posted his ninth career shutout at
Drake in a scoreless tie.
The host Bulldogs outshot the Golden Eagles 20-7 while Zapata made six saves.
Zapata lowered his goals-allowed average to 0.62 by posting his second
consecutive shutout. He has allowed only two goals in 290 minutes of work.
BASKETBALL
No confidence in Sloan: Baylor's faculty senate passed a "no confidence" motion
for embattled President Robert Sloan.
The 26-6 vote of no confidence came after the faculty senate met for more than
three hours.
Joe Cox, the faculty senate chairman, said the motion cites the "deeply
polarized and relationally paralyzed Baylor community" under Sloan's presidency.
The senate, which has no actual authority over Sloan's employment, will forward
its recommendation for his ouster to Baylor's 36-member board of regents, which
opens a two-day meeting Thursday.
LOAD-DATE: September 11, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Tulsa World
765 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
September 10, 2003, Wednesday
White's explanation for positive doping test rejected
SECTION: WORLD NEWS; SPORTS
LENGTH: 231 words
LONDON, Sept. 9 (Xinhua) -- The reason given by American Kelli White, who won
women's 100m/200m titles at the Paris athletic worlds in August, for positive
test for modafinil was rejected by the International Association of Athletics
Federations (IAAF) on Tuesday.
"Following careful examination the explanation has not been accepted," IAAF
spokesman Nick Davies said.
The 26-year-old White tested positive for modafinil, which is not at present on
the IAAF banned list, after winning the 100 meters final on August 24. A urine
sample taken after she won the 200m four days later was found to be clean.
The sprinter said at the time that she had been prescribed modafinil to combat
narcolepsy, or sleepiness, and had not sought exemption or entered it on her
doping control form because it was not on the banned list.
The IAAF said last week that modafinil is now to be classified as a weaker
stimulant and will be placed on the World Anti-Doping Agency's banned list next
year.
"In accordance with the normal disciplinary procedures under our rules the
matter has now be referred to the U.S. anti-doping agency for a hearing on a
date to be agreed with the athlete."
White has not been suspended pending her hearing before the U.S. anti-doping
agency and can therefore run at this weekend's inaugural World Athletics Final
at Monaco's Stade Louis II.
LOAD-DATE: September 11, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
766 of 998 DOCUMENTS
The Associated Press
September 9, 2003, Tuesday, BC cycle
U.S. sprinter Kelli White guilty of doping offense
SECTION: International News; Sports News
LENGTH: 402 words
DATELINE: MONTE CARLO, Monaco
U.S. sprinter Kelli White committed a doping offense at the World Championships
and should be stripped of her two gold medals, track and field's governing body
ruled Tuesday.
The International Association of Athletics Federations sent White's case to U.S.
track officials for disciplinary action.
White should be disqualified and stripped of the medals she won in the 100 and
200 meters last month in France, IAAF general secretary Istvan Gyulai said. A
final ruling could take months.
The U.S. Anti-Doping Agency must schedule a hearing with White. If it decides
not to disqualify White and remove the medals, the IAAF would take the case to
the Court of Arbitration for Sport in Lausanne, Switzerland.
White, the first American woman to sweep the two sprints at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for the
sleep disorder narcolepsy.
"The explanation has been studied and turned down," Gyulai told The Associated
Press. "Our experts have determined the stimulant is performance-enhancing."
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she did not
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required, or apply for a medical exemption to use the
product.
White has vowed to fight to keep her medals.
The IAAF ruled Sept. 4 that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White passed a drug test after the 200, the IAAF considers one positive
test enough for disqualification from the entire championships.
Under track and field rules, athletes are considered guilty of a doping
violation if banned substances are found in their bodies, regardless of the
circumstances.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
767 of 998 DOCUMENTS
The Associated Press
September 9, 2003, Tuesday, BC cycle
IAAF rules Kelli White guilty of doping offense
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 622 words
DATELINE: LONDON
Track and field's governing body wants American sprinter Kelli White stripped of
her two gold medals from the World Championships. Now it's up to U.S.
anti-doping officials.
The International Association of Athletics Federations ruled Tuesday that White
committed a doping offense when she tested positive for a stimulant and should
lose her world titles in the 100 and 200 meters.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of Tuesday
afternoon. Once that information is received, Wanninger said, the agency will
begin a review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "Our experts
have determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200. White would
also lose the $120,000 in prize money she won at the worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds. She is to run in the Grand Prix final in Monaco
this weekend and a meet in Moscow on Sept. 20.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
768 of 998 DOCUMENTS
Associated Press Worldstream
September 9, 2003 Tuesday
URGENT IAAF rules Kelli White guilty of doping offense
SECTION: SPORTS
LENGTH: 595 words
DATELINE: MONTE CARLO, Monaco
U.S. sprinter Kelli White committed a doping offense when she failed a drug test
at the World Championships and should lose her two gold medals, track's world
governing body said Tuesday.
The International Association of Athletics Federations found White guilty of a
doping infraction and sent her case to U.S. officials for disciplinary action.
IAAF general secretary Istvan Gyulai said White should be disqualified and
stripped of the gold medals she won in the 100 and 200 meters at last month's
World Championships in the Paris suburb of Saint-Denis.
A final ruling could take weeks or months.
The matter now goes to the U.S. Anti-Doping Agency, which must schedule a
hearing with White. If the U.S. body decides not to disqualify White and remove
the medals, the IAAF would take the case to the Court of Arbitration for Sport
in Lausanne, Switzerland.
White, the first American woman to sweep the two sprint events at a World
Championships, tested positive for modafinil after winning the 100 on Aug. 24.
She passed a drug test after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of modafinil. She said she took the medication on prescription from her
personal doctor for the sleep disorder narcolepsy.
"The explanation has been studied and turned down," Gyulai told The Associated
Press. "The IAAF has reached the conclusion she has committed a doping offense.
Our experts have determined the stimulant is performance-enhancing."
Modafinil is not named on the sport's list of banned drugs, but the IAAF says it
falls under the category of "related substances."
White denied taking the medication to enhance performance and said she had "no
idea" it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and ineligibility for the 2004 Athens Olympics.
The IAAF said a decision to strip White's medals was not automatic.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai said. "This can only happen after she has
been given a hearing by her national federation."
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200.
In addition, White would also lose the US$120,000 in prize money she won at the
worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds, leading a 1-2-3 American sweep ahead of Chryste
Gaines and Edwards.
White is due to run in the Grand Prix final in Monaco this weekend and an
invitatational meet in Moscow on Sept. 20.
White said last week she will fight to keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
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Associated Press Worldstream
September 9, 2003 Tuesday
IAAF rules Kelli White guilty of doping offense
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 601 words
DATELINE: LONDON
Track and field's governing body says American sprinter Kelli White should be
stripped of her two gold medals from the World Championships. Now it's up to
U.S. anti-doping officials to comply.
The International Association of Athletics Federations ruled Tuesday that White
committed a doping offense when she tested positive for a stimulant and should
lose her world titles in the 100 and 200 meters.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
The process could take weeks or months.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the two sprint events at the worlds,
tested positive for modafinil after winning the 100 on Aug. 24. She passed a
drug test after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "The IAAF has
reached the conclusion she has committed a doping offense. Our experts have
determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200.
In addition, White would also lose the US$120,000 in prize money she won at the
worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds. She is to run in the Grand Prix final in Monaco
this weekend and an invitational meet in Moscow on Sept. 20.
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All Rights Reserved
770 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 9, 2003, Tuesday, BC cycle
IAAF rules Californian Kelli White guilty of doping offense
SECTION: Sports News
LENGTH: 550 words
DATELINE: MONTE CARLO, Monaco
U.S. sprinter Kelli White committed a doping offense at the World Championships
and should be stripped of her two gold medals, track and field's governing body
ruled Tuesday.
The International Association of Athletics Federations sent White's case to U.S.
track officials for disciplinary action.
White, who lives in Union City, Calif., should be disqualified and stripped of
the medals she won in the 100 and 200 meters last month in France, IAAF general
secretary Istvan Gyulai said. A final ruling could take months.
The U.S. Anti-Doping Agency must schedule a hearing with White. If it decides
not to disqualify White and remove the medals, the IAAF would take the case to
the Court of Arbitration for Sport in Lausanne, Switzerland.
White, the first American woman to sweep the two sprints at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for the
sleep disorder narcolepsy.
"The explanation has been studied and turned down," Gyulai told The Associated
Press. "Our experts have determined the stimulant is performance-enhancing."
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she did not
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
White said last week she will fight to keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
The IAAF said a decision to strip White's medals was not automatic.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai said. "This can only happen after she has
been given a hearing by her national federation."
Although White passed a drug test after the 200, the IAAF considers one positive
test enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200. In
addition, White would lose the $120,000 in prize money she won at the worlds.
Under track and field rules, athletes are considered guilty of a doping
violation if banned substances are found in their bodies, regardless of the
circumstances.
White competed at the Golden League meet in Brussels, Belgium, on Friday and won
the 100 in 10.87 seconds, leading an American sweep of the top three spots.
White is to run in the Grand Prix final in Monaco this weekend and a meet in
Moscow on Sept. 20.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
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771 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 9, 2003, Tuesday, BC cycle
IAAF rules Kelli White guilty of doping offense
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 629 words
DATELINE: LONDON
Track and field's governing body wants American sprinter Kelli White stripped of
her two gold medals from the World Championships. Now it's up to U.S.
anti-doping officials.
The International Association of Athletics Federations ruled Tuesday that White,
a former University of Tennessee sprinter, committed a doping offense when she
tested positive for a stimulant and should lose her world titles in the 100 and
200 meters.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of Tuesday
afternoon. Once that information is received, Wanninger said, the agency will
begin a review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "Our experts
have determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200. White would
also lose the $120,000 in prize money she won at the worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds. She is to run in the Grand Prix final in Monaco
this weekend and a meet in Moscow on Sept. 20.
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LANGUAGE: ENGLISH
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All Rights Reserved
772 of 998 DOCUMENTS
Associated Press Online
September 9, 2003 Tuesday
IAAF Finds Kelli White Guilty of Doping
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 618 words
DATELINE: LONDON
Track and field's governing body wants American sprinter Kelli White stripped of
her two gold medals from the World Championships. Now it's up to U.S.
anti-doping officials. The International Association of Athletics Federations
ruled Tuesday that White committed a doping offense when she tested positive for
a stimulant and should lose her world titles in the 100 and 200 meters.
The IAAF rejected White's explanation that she took the stimulant for a sleep
disorder and sent the case to the U.S. Anti-Doping Agency for a hearing and
disciplinary action.
Rich Wanninger, a spokesman for the U.S. Anti-Doping Agency, said his
organization had not received any information from the IAAF as of Tuesday
afternoon. Once that information is received, Wanninger said, the agency will
begin a review process that could last months.
The IAAF made clear it expects U.S. authorities to remove White's medals.
"The proper sanction under IAAF rules will be a public warning and
disqualification from the competition concerned," IAAF general secretary Istvan
Gyulai said.
If the IAAF isn't satisfied with the U.S. action, the international body would
take the case to the Court of Arbitration for Sport in Lausanne, Switzerland.
"She is disqualified only at the end of the procedure because further legal
issues need to be exhausted," Gyulai told The Associated Press by phone from
IAAF headquarters in Monaco. "This can only happen after she has been given a
hearing by her national federation."
White, the first American woman to sweep the sprint events at the worlds, tested
positive for modafinil after winning the 100 on Aug. 24. She passed a drug test
after winning the 200 four days later.
The IAAF gave White until Tuesday to produce medical documents explaining her
use of the drug. She said her personal doctor prescribed the medication for
narcolepsy.
"The explanation has been studied and turned down," Gyulai said. "Our experts
have determined the stimulant is performance-enhancing."
White was unavailable for comment Tuesday. She said last week she will fight to
keep her medals.
"Whatever I have to do to keep them, I will do that," she said.
Modafinil is not on the sport's list of banned drugs, but the IAAF says it falls
under the category of "related substances."
White denied taking the medication to enhance performance and said she didn't
know it contained a banned substance. However, she did not declare modafinil on
her doping control form as required or apply for a medical exemption to use the
product.
The IAAF ruled last Wednesday that modafinil was a minor stimulant, similar to
ephedrine, and carries a penalty of a public warning and disqualification. The
decision allowed White to continue competing.
Had modafinil - sold in the United States under the brand name Provigil - been
classified as a stronger stimulant, White also would have faced a two-year ban
and been ineligible for the 2004 Athens Olympics.
Although White tested clean after the 200, the IAAF considers one positive test
enough for disqualification from the entire championships.
If White loses the medals, the golds would go to fellow American sprinter Torri
Edwards in the 100 and Russia's Anastasiya Kapachinskaya in the 200. White would
also lose the $120,000 in prize money she won at the worlds.
Under the sport's policy of strict liability, athletes are considered guilty of
a doping violation if banned substances are found in their bodies, regardless of
the circumstances.
White competed at the Golden League meet in Brussels, Belgium, last Friday and
won the 100 in 10.87 seconds. She is to run in the Grand Prix final in Monaco
this weekend and a meet in Moscow on Sept. 20.
LOAD-DATE: September 10, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
773 of 998 DOCUMENTS
CNN.com
September 9, 2003 Tuesday
White's drugs explanation rejected
SECTION: SPORT
LENGTH: 295 words
DATELINE: LONDON, England
Athletics chiefs have rejected double sprint champion Kelli White's explanation
of why she tested positive at the world championships.
"The IAAF has received the athlete's explanation for testing positive for
(stimulant) modafinil...in Paris last month," IAAF spokesman Nick Davies said on
Tuesday.
And he confirmed: "Following careful examination the explanation has not been
accepted."
Davies added: "In accordance with the normal disciplinary procedures under our
rules the matter has now be referred to the U.S. anti-doping agency for a
hearing on a date to be agreed with the athlete."
White, the first American to win the 100-200 sprint double, has not been
suspended pending her hearing before the U.S. anti-doping agency and can
therefore run at this weekend's inaugural World Athletics Final in Monaco.
However, if she is found guilty of a doping offence White would be stripped of
the individual gold medals she won in Paris last month.
"The IAAF has already announced that if it is confirmed after the hearing that
the athlete has committed a doping offence, the sanction under IAAF rules will
be a public warning and disqualification from the competition," said Davies.
The 26-year-old tested positive for modafinil, which is not at present on the
IAAF banned list, after winning the 100m final on August 24. A urine sample
taken after she won the 200 four days later was found to be clean.
White said at the time she had been prescribed modafinil to combat narcolepsy,
or sleepiness, and had not sought exemption or entered it on her doping control
form because it was not on the banned list.
The IAAF said last week that modafinil is now to be classified as a weaker
stimulant and will be placed on the World Anti-Doping Agency's banned list next
year.
LOAD-DATE: September 26, 2003
LANGUAGE: ENGLISH
Copyright 2003 Cable News Network
All Rights Reserved
774 of 998 DOCUMENTS
The Washington Post
September 7, 2003 Sunday
Final Edition
Testing Positive for Sprinting
SECTION: EDITORIAL; Pg. B06
LENGTH: 217 words
If Kelli White has narcolepsy, it is unlikely that she could compete in sports
without treatment, particularly at a world-class level ["Double Gold Medalist
Tests Positive," Sports, Aug. 31]. Untreated, narcolepsy is an incapacitating
disability whose effects have been found to be as severe as multiple sclerosis
on quality-of-life assessment scales.
Does treatment with modafinil provide a competitive edge?
Based on the evidence, probably not more than someone else drinking several cups
of coffee. Just as people become tolerant of coffee, a person with narcolepsy
would have to consume ever greater amounts of modafinil to get any boosting
effect.
Modafinil is not an amphetamine and is not classified as one by the Drug
Enforcement Administration or the Food and Drug Administration. It has not been
shown to improve strength, speed or other athletic characteristics -- just to
keep people awake and alert enough to function.
Rather than condemn Ms. White, we should applaud her motivation for overcoming
symptoms that make training difficult. She is competing overseas against the
world's best -- and she is winning -- not because she is taking a medication
that helps her stay awake but because she is a great athlete.
RICHARD L. GELULA
Executive Director
National Sleep Foundation
Washington
LOAD-DATE: September 7, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
775 of 998 DOCUMENTS
The Herald (Glasgow)
September 5, 2003
IAAF give White Brussels go-ahead
BYLINE: Doug Gillon
SECTION: Pg. 40
LENGTH: 299 words
THE stimulant which double world sprint champion Kelli White took in Paris is
considered good enough to fight a war, yet those battling against drugs deem it
minor, and have cleared her to run tonight in the Brussels grand prix.
International Association of Athletics Federations experts ruled that modafinil,
which White used to treat a sleeping disorder, was "in the category of weaker
stimulants" and well short of amphetamine strength which would have brought a
two-year suspension.
As a consequence the American has received a reprimand, though her medals still
seem likely to be forfeited. The decision of the IAAF panel to downgrade
modafinil seems strange.
Professor Michel Jouvet, an authority on sleep, stated at a defence conference
in Paris: "Modafinil could keep an army on its feet and fighting for three days
and nights with no major side effects."
It was used in the Falklands by UK forces, and the Foreign Legion during the
Gulf War. The US Aerospace Medical Association reports it as being "as effective
as the amphetamines", and the US Air Force Human Systems Division says it is "an
ideal replacement for amphetamine in short-term operations".
White said she "thoroughly researched" the drug, yet a US pharmacology industry
data-base, quoting modafinil literature, warns: "Athletes should be aware one of
the main ingredients of this product would produce a positive result in anti
-doping tests." It is also listed as a banned stimulant by the International
Tennis Federation.
White is fighting to keep
her medals and endorsements.
US Track and Field is due to report by Monday and the case then goes to the US
Anti-
Doping Agency. If the IAAF is unhappy with the outcome, they will refer the case
to the Court of Arbitration for Sport.
LOAD-DATE: September 05, 2003
LANGUAGE: English
PUB-TYPE: Paper
Copyright 2003 Scottish Media Newspapers Limited
776 of 998 DOCUMENTS
THE DAILY TELEGRAPH(LONDON)
September 04, 2003, Thursday
No ban but White may lose medals
BYLINE: By Mark Hodgkinson
SECTION: Pg. 08
LENGTH: 273 words
KELLI WHITE, the American sprinter who had feared a two-year ban covering next
year's Olympic Games in Athens, learned yesterday that she would not be
suspended from competition after testing positive for a stimulant.
However, the 26-year-old Californian, who was the first woman to do the sprint
double at a World Championships since 1991, will almost certainly be stripped of
the 100 metres and 200m gold medals from Paris.
She is now expected to feature at tomorrow's Golden League meeting in Brussels
following the announcement by the International Association of Athletic
Federations that the offence does not merit suspension.
Traces of modafinil - a white, crystalline powder used by soldiers and pilots to
stay alert - were found in White's sample after her 100m gold.
Had it been classed as a harder stimulant, the penalty would have been
disqualification and a two-year ban. However, expert medical advice confirmed
that modafinil is a weak stimulant, for which the sanction is disqualification
and a public warning.
White continues to protest her innocence. She claims that she uses the drug to
combat narcolepsy, a condition which causes extreme tiredness. She had "no idea"
that her medication contained an illegal substance. Modafinil, though not named
on the banned list, falls under the "related substances" clause.
The IAAF extended the deadline until Monday for a doctor's report explaining why
White needed to take the drug. Istvan Gyulai, the general secretary of the IAAF,
said. "Unless the medical explanation casts new light on the matter, she will
lose both her medals."
[PS]Sport: [ES]
Hockey:
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Telegraph Group Limited
777 of 998 DOCUMENTS
The Daily Telegraph (Sydney, Australia)
September 4, 2003 Thursday
White could lose medals
SOURCE: MATP
BYLINE: JEROME PUGMIRE
SECTION: SPORT-BIOG- KELLI WHITE; Pg. 73
LENGTH: 315 words
AMERICAN sprinter Kelli White will not be suspended from future track meets but
is still in danger of losing the two gold medals she won at the world
championships after testing positive for a minor stimulant.
White tested positive for the stimulant modafinil after her victory in the 100
metres on August 24.
White said she used the prescription drug for a sleep disorder.
The penalty for taking a minor stimulant such as modafinil is disqualification
from the tournament where the athlete tested positive -- meaning White could
lose the golds she clinched in the 100m and 200m races.
Although White passed a drug test after winning the 200m on August 28, the fact
that she tested positive once means she could lose both medals.
IAAF General-Secretary Istvan Gyulai said from Monaco that his organisation
would decide on Monday whether White lost her medals.
The IAAF extended the deadline until then for a doctor's report explaining why
White needed to take modafinil.
The 26-year-old track star said she needed the drug to treat narcolepsy.
"Kelli White and the US federation tried to explain to us that she was ordered
by her doctor to take modafinil, so the IAAF will wait to hear the medical
explanation," Gyulai said.
"Unless the medical explanation casts new light on the matter she will lose both
her medals -- as this is the sanction," he said.
Whatever the outcome, he said, White is cleared to race immediately. She had
intended to compete in the Golden League track meet in Brussels on Friday and
the Grand Prix final in Monaco on September 13 and 14.
White, the first American woman to win both sprints at a world championships,
will also be able to participate in next year's Athens Olympics.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
JOURNAL-CODE: DTM
Copyright 2003 Nationwide News Pty Limited
778 of 998 DOCUMENTS
The Guardian (London)
September 4, 2003
There's one rule for Americans and another for the rest of us
BYLINE: Solomon Wariso
SECTION: Guardian Sport Pages, Pg. 33
LENGTH: 784 words
The news that Kelli White of the United States failed a drug test at the world
championships was greeted with knowing looks from certain quarters, not just
from the world's press but from the spectators, such was her margin of victory
in the 100 metres final. Modafinil, the drug found in her system, was allegedly
used to combat the narcolepsy she says is inherent in her family. If so she is
the fastest narcoleptic I have ever seen.
But the decision not to ban her but instead issue her a warning and strip her of
her medals and prize money illustrates what a grey area the issue of drugs in
sport has become. In 1994 I had been competing quite a lot on the grand prix
circuit as a 200m runner. Feeling partic ularly run down for a couple of days,
and with a big meeting in front of a home crowd in Gateshead looming, I came
across a herbal supplement called Up Your Gas that purported to help alleviate
tiredness. Flicking quickly through the ingredients, the only thing that looked
unfamiliar alongside the likes of cayenne pepper and kola nut was "ma huang".
Having never heard of it, I thought nothing of it and took a couple of tablets
an hour before the race.
That was at a time before the internet was widely used, when athletes were not
as paranoid about herbal supplements as they are today. As we are now all too
aware of, thanks to my case, ma huang is the plant from which ephedrine is
derived.
Nowadays every dodgy chemical or herb on the market is only a search engine away
from having its entire history and chemical makeup uncovered. That is why there
is perhaps more than meets the eye to Kelli White's story. By logging on and
tapping modafinil into a search engine, you can see warnings that the substance
is not to be used if you compete in events where drug testing is likely.
The IAAF's decision to strip her of her medals and publicly warn her means it
has decided modafinil is probably in the same chemical family as ephedrine and
pseudo-ephedrine. One only receives a ban for ephedrine now for a second and
third offence. By placing modafinil in that category, the IAAF may have
sidestepped a bullet. It allows it to legitimately avoid banning White. If it
couldn't do that, and decided not to ban her, athletes who have been banned in
the past for other offences might have had grounds to contest those decisions.
It could also be that, with White being an American, the IAAF knows that months
of litigation were sure to follow if it tried to ban her. Only lawyers would
have benefited then.
During my hearing the head of the panel of judges, the late Sir Arthur Gold,
told me that, regardless of how the substance got into my body, it was my
responsibility. He may not have actually come out and said it, but I and my team
got the distinct impression that, once you go into a drugs hearing, you are
guilty until proven innocent.
Ever since Butch Reynolds disputed the results of his positive readings back in
the early 90s and won a Dollars 20m settlement in the US Supreme Court against
the IAAF - a sum he never received because the IAAF doesn't fall under the
Supreme Court's jurisdiction - there has been the feeling in athletics that USA
Track and Field has been reluctant to ban its athletes for fear of being
bankrupted.
When word broke that there were several US athletes competing in the Sydney
Olympics who had failed drug tests, people weren't surprised. Jerome Young, a
man I competed against several times as a 400m runner in 98 and 99, was last
week exposed as having won a gold medal there and the International Olympic
Committee is now demanding hard answers from the USOC. But the US administration
has form in turning a blind eye - it emerged recently that many American
athletes in the 1988 Seoul Olympics had failed drugs tests a few months before
their trials.
Marion Jones herself had an irregular drug test result at the age of 15 and
hired Johnny Cochrane, a family friend, to defend her against the charge.
To this roll call you can add the name of Dennis Mitchell, whose massive
readings of testosterone were put down to a night of heavy boozing and sex. His
federation cleared him to compete until he was slapped down and banned by the
IAAF. And these are just the ones we know about.
Kelli White was also banned from France last year after banned corticosteroids
were found in her urine sample, so failing drug tests is not new to her.
It should therefore be no surprise that athletes the world over look at the
Americans with distrust and suspicion, because it seems that it is one rule for
them, another for the rest of us.
Solomon Wariso is a former British international at 200m and 400m
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Guardian Newspapers Limited
779 of 998 DOCUMENTS
Liverpool Daily Echo
September 4, 2003, Thursday
ATHLETICS: WHITE CLEAR
BYLINE: DAVID MARTIN
SECTION: SPORT; Pg. 63
LENGTH: 412 words
KELLI WHITE, accused of a doping violation after winning the 100 metres gold
medal in last week's World Championships, will return to action in Friday's
Golden League meeting in Brussels.
The International Association of Athletic Federations (IAAF) announced her
clearance after deciding the offence did not merit suspension, and manager
Robert Wagner confirmed she will compete in Belgium.
"Kelli will definitely be taking part," said Wagner. "She knows she needs to get
back into action as quickly as possible and is looking forward to her first race
since this unfortunate incident."
The American athlete's urine sample tested positive for a related drugs
substance called modafinil following her 100m victory on August 24.
Later in the week,after completing the sprint double by winning the 200m,White's
test sample proved negative.
The world's governing body made their decision after expert medical advice
confirmed modafinil belonged to the minor ephredine family of drugs.
IAAF spokesman Nick Davies said: "The IAAF have obtained the necessary expert
opinion on the stimulant modafinil and decided to class it in the category of
weaker stimulants. "Under IAAF rules the eventual sanction for a doping offence
for this substance would be a public warning and disqualification from the
competition which means White could be stripped of her two gold medals.
"Kelli White will now have the opportunity of a hearing in the United States
before any decision can be taken as to whether a doping offence has been
committed under our rules."
If modafinil had been classed as an amphetamine, White would already have been
stripped of her two gold medals and suspended for two years.
The American, who claimed the substance is used under prescription by her
doctor,failed to list it on her control doping form before the championships
began.
Wilfried Meert, promoter for the Brussels event which is the last Golden League
meeting of the year, said: "Of course Kelli White will be welcome at our
meeting. We must be seen to support our athletes."
He added: "The IAAF should have kept to its own rules which clearly said that
the substance which White has been in trouble for is not on their banned list.
"They should have understood that and not be drawn into the conflict which has
occurred since then.
"Saying that it is a related substance when the athlete understood it was not on
the list of banned ones isn't right."
LOAD-DATE: September 5, 2003
LANGUAGE: ENGLISH
GRAPHIC: BACK ON TRACK: Kelli White is due to make a quick return to action in
Brussels tomorrow
TYPE: Newspaper
Copyright 2003 The Liverpool Daily Post & Echo Ltd
780 of 998 DOCUMENTS
The New York Times
September 4, 2003 Thursday
Late Edition - Final
TRACK AND FIELD;
White May Lose Gold, Not Shot at Olympics
BYLINE: By JERE LONGMAN
SECTION: Section D; Column 1; Sports Desk; Pg. 4
LENGTH: 654 words
The American sprinter Kelli White will not be barred from the 2004 Athens
Olympics, but she may still lose the two gold medals she won in the 100 and 200
meters at the recent world track and field championships in Paris after testing
positive for a stimulant, the sport's world governing body said yesterday.
Modafinil, the drug found in White's urine sample after the 100 meters, has been
classified as a lesser stimulant. If found to have committed a doping violation,
she would face a public warning and disqualification from the world
championships, according to the I.A.A.F., which governs track and field.
She is eligible to run immediately and is expected to compete in the 100 meters
tomorrow at a meet in Brussels.
Had modafinil been declared a strong stimulant in the class of amphetamines,
White would have faced a two-year ban from the sport, which would have precluded
her participation in the 2004 Olympics.
Her case remains in the early stages, and no doping violation has been declared.
The I.A.A.F. said that White had until Monday evening to provide documentation
that she had been taking modafinil by doctor's consent to treat the sleeping
disorder narcolepsy. White said that some members of her family have had
narcolepsy for years.
If the world governing body decides that a doping violation has occurred, it
sends the case to USA Track and Field, which then turns it over to the United
States Anti-Doping Agency. (Since October 2000, the agency has handled all
doping cases involving American track athletes because of international
suspicion that USA Track and Field is not committed to catching drug cheaters.)
The athlete is then given a hearing before the agency, which rules on the case.
If the I.A.A.F. agrees on the ruling,it will stand. If the I.A.A.F. disagrees
with the agency's ruling, the case is settled by the International Court of
Arbitration for Sport, based in Switzerland.
The I.A.A.F. made clear again yesterday that, even with a legitimate medical
reason for taking modafinil, White would have difficulty convincing the world
track body that she did not deserve a warning and the loss of her medals.
White has admitted failing to notify the I.A.A.F., as required, that she was
using modafinil and failing to get a prior exemption to use the substance.
Modafinil is not named on the official list of banned substances but is
considered a "related substance" and thus prohibited. Stimulants are banned
because they are considered to give athletes an unfair advantage in competition.
"Why on earth didn't she declare it?" Istvan Gyulai, general secretary of the
I.A.A.F., said yesterday from the federation's headquarters in Monaco. "An
athlete of her level must be aware of that."
Athletes in Olympic-related sports are supposed to be governed by what is called
strict liability, meaning they are to be held responsible if banned substances
appear in their bodies, no matter the reason.
"If this substance is there, regardless of why it is there, it gave her unfair
advantage over her rivals," Gyulai said. "Even if she had a doctor's
prescription, its presence means performance enhancement. This is what the
doping fight is about, not to have an unfair advantage."
White, 26, said she did not notify the I.A.A.F. that she was using modafinil
because it is not named on the banned-substance list. Reached by The Associated
Press yesterday in Belgium, where she is training for tomorrow's race, White
said: "I'm now pretty much getting over the whole mental shock. Whatever
happens, I do intend to fight to keep the medals. Whatever I have to do to keep
them, I will do that."
She ran the fastest times of her career in Paris: 10.85 seconds at 100 meters
and 22.05 seconds at 200 meters. If she is stripped of the gold medals, Torri
Edwards of the United States will be declared world champion at 100 meters and
Anastasiya Kapachinskaya of Russia will be declared the winner at 200 meters.
URL: http://www.nytimes.com
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: Kelli White spoke yesterday in Brussels, where she is scheduled
to compete in a 100-meter race at a meet tomorrow. (Photo by Associated Press)
PUBLICATION-TYPE: Newspaper
Copyright 2003 The New York Times Company
781 of 998 DOCUMENTS
The Times (London)
September 4, 2003, Thursday
White to race on after escaping ban for failed test
BYLINE: David Powell, Athletics Correspondent in Brussels
SECTION: Sport; 45
LENGTH: 624 words
KELLI WHITE will compete in the Golden League meeting here tomorrow after being
told yesterday that the worst punishment she will face for failing a drugs test
at the World Championships last week is a caution and the loss of her gold
medals and prize-money.
The IAAF, the sport's world governing body, has ruled that the stimulant found
in her sample falls into the mild rather than serious category. However, it is
unclear whether modafinil, the drug for which White, the United States sprinter
who won the 100 and 200 metres in Paris, tested positive, would have given her a
performance advantage.
The IAAF had been unable to categorise it immediately after she failed the test
and only after seeking expert opinion did it rule yesterday that it was not
strong enough to warrant a suspension. White responded by confirming that she
would run here, in Monaco the weekend after next and in Russia and Japan to end
her season, but she added that the experience had left her "very tired
physically and mentally". Robert Wagner, her manager, said that she had been
ready to quit for the season until she was given a sympathetic reception on a
German television chat show on Tuesday, on which she appeared with Boris Henry,
the javelin thrower who is her boyfriend.
White had said that she was taking modafinil on prescription to counter
narcolepsy and the fact that she tested negative after the 200 metres added
weight to her claim.
The IAAF insisted yesterday that she would have benefited from the drug, but
Cephalon, the manufacturer of Provigil, under which modafinil is sold under
licence, said that during pre-marketing clinical trials it had not been
"systematically evaluated in athletes or patients engaged in significant
physical exercise or activity". However, Nick Davies, the IAAF spokesman, said:
"It is considered a stimulant, so it does have a performance- enhancing effect."
The world governing body said in a statement: "Under IAAF rules, the eventual
sanction for a doping offence for this substance, if proven, would be a public
warning and disqualification from the competition. This means that Ms White
could be stripped of her gold medals in Paris in the 100 and 200 metres events."
There seems little chance of an offence not being proven because White failed to
list the substance on her doping form.
White's medals would pass to Torri Edwards, a fellow American, in the 100 metres
and to Anastasiya Kapachinskaya, from Russia, in the 200 metres, but it could be
months before the matter is resolved. The case now goes to USA Track & Field,
the governing body in the US, which in turn is guided in such matters by the US
Anti-Doping Agency.
The IAAF statement continued: "Ms White will be afforded the opportunity of a
hearing in the United States before any decision is taken on whether a doping
offence has been committed under IAAF rules. The athlete is not suspended
pending her hearing." In other words, she can start to make up some of the $
120,000 (about Pounds 76,000) in World Championships prize-money that she is
likely to lose.
Until six years ago, White would have been suspended for three months pending a
hearing, but the IAAF dropped the punishment for a mild stimulant offence,
believing it to be too harsh. The feeling was that in some cases it could
effectively rule an athlete out for a season, whereas a steroid offence,
carrying a two-year ban and a much more serious charge, deserved a significantly
greater sentence in practical terms.
Another leading athlete who has tested positive is Bernard Lagat, the World Cup
1,500 metres champion from Kenya. It was announced yesterday that Lagat had
tested positive for EPO after a race in Germany three weeks ago.
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Times Newspapers Limited
782 of 998 DOCUMENTS
USA TODAY
September 4, 2003, Thursday, FINAL EDITION
No ban for White; golds likely gone
BYLINE: Dick Patrick
SECTION: SPORTS; Pg. 9C
LENGTH: 418 words
Kelli White will have a tough time disputing a positive drug test that could
strip her of two gold medals at the recent World Track & Field Championships in
Paris.
The 100- and 200-meter winner tested positive for modafinil, which she said was
prescribed for narcolepsy, a sleep disorder that her mother and an aunt also
share. Though modafinil is not on the banned list, the international track
federation (IAAF) considers it "a related substance" and announced Wednesday its
classification as a stimulant rather than an amphetamine, sparing White a
two-year ban.
"The problem is once this substance is in her body, this already constitutes a
doping offense, pending a hearing and explanation," says Istvan Gyulai, the IAAF
general secretary. "Even if she can explain this because of a medical
prescription, that will not nullify that she was running with a
performance-enhancing substance."
Besides documentation from her physician, the White team plans to introduce
information from Cephalon, the West Chester, Pa.-based company that produces
Provigil, the U.S. form of the drug. "They say the drug is neither an
amphetamine nor a stimulant," says Robert Wagner, White's agent.
The IAAF plans to announce Monday whether White is guilty of a doping offense,
which would mean she'd lose her medals and $ 120,000 in prize money. If the IAAF
rules against her, White could continue appeals with the U.S. Anti-Drug Agency.
White is in Brussels for a 100 race Friday, though she also considered ending
her season.
"The best thing is to go to Brussels and win," Wagner says. "We're going to ask
for doping control after each race from now on."
Wagner argues the Paris lab, which analyzed the sample, should be investigated
since White's positive was leaked to the press against IAAF regulations.
Kenyan positive: Bernard Lagat, a U.S.-based Kenyan who was third in the 1,500
at the 2000 Olympics, has been announced as positive for endurance-boosting EPO.
According to his agent, James Templeton, the confirmation test has not been
conducted and Lagat denies taking the drug.
Lagat, featured in a series of Nike ads, did not compete at the recent worlds.
"He's devastated; he cried like a baby," said Lagat's coach, James Li, the cross
country coach at Arizona. "Even in a million years, it's not possible for him to
do this. This guy is just so completely against this drug thing.
"If I don't say this, no one will hear it. If I do say it, a lot of people won't
believe it."
LOAD-DATE: September 04, 2003
LANGUAGE: ENGLISH
GRAPHIC: PHOTO, B/W, Benoit Doppagne, AFP/Getty Images; Making a case: Kelli
White says she took modafinil to combat a sleep disorder. Her agent, Robert
Wagner, says the company that produced the drug says it is neither an
amphetamine nor a stimulant."
Copyright 2003 Gannett Company, Inc.
783 of 998 DOCUMENTS
The Associated Press
September 3, 2003, Wednesday, BC cycle
U.S. sprint star Kelli White not suspended but could lose golds from Worlds
BYLINE: By JEROME PUGMIRE, Associated Press Writer
SECTION: International News; Sports News
LENGTH: 628 words
DATELINE: PARIS
American sprinter Kelli White will not be suspended from future track meets
after testing positive for a minor stimulant, but could still be stripped of the
two gold medals she won at the World Championships, IAAF general secretary
Istvan Gyulai said Wednesday.
Gyulai, speaking to The Associated Press by telephone from Monaco, said the IAAF
will not decide whether White loses her medals until next Monday.
White tested positive for the stimulant modafinil after her victory in the 100
meters at the Worlds on Aug. 24. White said she used the prescription drug for a
sleep disorder.
The penalty for taking a minor stimulant such as modafinil is disqualification
from the tournament where the athlete tested positive - meaning White could lose
the golds she won in the 100 and 200 races.
Although White passed a drug test after winning the 200 on Aug. 28, the IAAF
said her positive test after the 100 could be enough to cost her both medals.
White had set personal best times in both races - 10.85 seconds in the 100
meters and 22.05 in the 200 meters.
The IAAF extended the deadline until Monday to wait for a doctor's report
explaining why White needed to take modafinil. The 26-year-old track star said
she needed the drug to treat narcolepsy.
"Kelli White and the U.S. federation tried to explain to us that she was ordered
by her doctor to take modafinil, so the IAAF will wait to hear the medical
explanation," Gyulai said.
"Unless the medical explanation casts new light on the matter she will lose both
her medals - as this is the sanction," he said.
Whatever the outcome, he said, White is cleared to race immediately. She had
planned to compete in the Golden League track meet in Brussels on Friday and the
Grand Prix final in Monaco on Sept. 13-14.
White, the first American woman to sweep both sprints at a world championships,
will also be able to participate in next year's Athens Olympics.
If White is stripped of her medals, American runner Torri Edwards will be
awarded the 100 gold medal, while Zhanna Block of Ukraine would take silver and
Bahamas runner Chandra Sturrup the bronze.
The 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would take
silver and France's Muriel Hurtis the bronze.
The overall medals table would also be altered, with America's total tally of 20
medals dropping to 18, leaving Russia as the leader with 19.
White would also lose $60,000 in prize money for each gold.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF has said.
Under IAAF rules, the penalty for use of light stimulants also includes a public
warning. For harder stimulants, such as amphetamines, the sanction is
disqualification and a two-year ban.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
Last Saturday, White acknowledged taking modafinil the morning of the 100 final.
But she denied ever taking a substance to enhance her performance, saying she
took the medication only to treat narcolepsy and had "no idea" it contained a
banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
However, an Internet search on modafinil turned up frequent warnings to athletes
that its use could result in a positive result in an anti-doping test.
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
784 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 3, 2003, Wednesday, BC cycle
U.S. sprint star Kelli White not suspended but could lose golds from Worlds
BYLINE: By JEROME PUGMIRE, Associated Press Writer
SECTION: Sports News
LENGTH: 634 words
DATELINE: PARIS
American sprinter Kelli White will not be suspended from future track meets
after testing positive for a minor stimulant, but could still be stripped of the
two gold medals she won at the World Championships, IAAF general secretary
Istvan Gyulai said Wednesday.
Gyulai, speaking to The Associated Press by telephone from Monaco, said the IAAF
will not decide whether White loses her medals until next Monday.
White tested positive for the stimulant modafinil after her victory in the 100
meters at the Worlds on Aug. 24. White said she used the prescription drug for a
sleep disorder.
The penalty for taking a minor stimulant such as modafinil is disqualification
from the tournament where the athlete tested positive - meaning White could lose
the golds she won in the 100 and 200 races.
Although White passed a drug test after winning the 200 on Aug. 28, the IAAF
said her positive test after the 100 could be enough to cost her both medals.
White had set personal best times in both races - 10.85 seconds in the 100
meters and 22.05 in the 200 meters.
The IAAF extended the deadline until Monday to wait for a doctor's report
explaining why White needed to take modafinil. The 26-year-old track star said
she needed the drug to treat narcolepsy.
"Kelli White and the U.S. federation tried to explain to us that she was ordered
by her doctor to take modafinil, so the IAAF will wait to hear the medical
explanation," Gyulai said.
"Unless the medical explanation casts new light on the matter she will lose both
her medals - as this is the sanction," he said.
Whatever the outcome, he said, White is cleared to race immediately. She had
planned to compete in the Golden League track meet in Brussels on Friday and the
Grand Prix final in Monaco on Sept. 13-14.
White, who lives in the Bay Area and was the first American woman to sweep both
sprints at a world championships, will also be able to participate in next
year's Athens Olympics.
If White is stripped of her medals, American runner Torri Edwards will be
awarded the 100 gold medal, while Zhanna Block of Ukraine would take silver and
Bahamas runner Chandra Sturrup the bronze.
The 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would take
silver and France's Muriel Hurtis the bronze.
The overall medals table would also be altered, with America's total tally of 20
medals dropping to 18, leaving Russia as the leader with 19.
White would also lose $60,000 in prize money for each gold.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF has said.
Under IAAF rules, the penalty for use of light stimulants also includes a public
warning. For harder stimulants, such as amphetamines, the sanction is
disqualification and a two-year ban.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
Last Saturday, White acknowledged taking modafinil the morning of the 100 final.
But she denied ever taking a substance to enhance her performance, saying she
took the medication only to treat narcolepsy and had "no idea" it contained a
banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
However, an Internet search on modafinil turned up frequent warnings to athletes
that its use could result in a positive result in an anti-doping test.
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
785 of 998 DOCUMENTS
The Associated Press State & Local Wire
September 3, 2003, Wednesday, BC cycle
Kelli White not suspended but could lose golds from worlds
BYLINE: By JEROME PUGMIRE, Associated Press Writer
SECTION: Sports News
LENGTH: 612 words
DATELINE: PARIS
U.S. sprinter Kelli White will not be suspended from track meets for taking a
stimulant but still could be stripped of the two gold medals she won at the
World Championships.
The IAAF will not decide whether White loses her medals until Monday, Istvan
Gyulai, general secretary of track and field's governing body, told The
Associated Press from Monaco on Wednesday.
White tested positive for the stimulant modafinil after winning the 100 meters
at the worlds on Aug. 24. White said she used the prescription drug for the
sleep disorder narcolepsy.
The penalty for taking such a minor stimulant is disqualification from the meet
where the athlete tested positive - meaning White could lose the golds she won
in the 100 and 200.
Although White passed a drug test after winning the 200 on Aug. 28, the IAAF
said her positive test after the 100 could cost her both medals. If she loses
the medals, she would be the biggest track name stripped of a gold medal at a
major championship since Ben Johnson at the 1988 Seoul Olympics.
White set personal bests in both races - 10.85 seconds in the 100 and 22.05 in
the 200.
The International Association of Athletics Federations extended the deadline
until Monday to wait for a doctor's report explaining why White needed to take
modafinil.
"Kelli White and the U.S. federation tried to explain to us that she was ordered
by her doctor to take modafinil, so the IAAF will wait to hear the medical
explanation," Gyulai said.
"Unless the medical explanation casts new light on the matter she will lose both
her medals - as this is the sanction," he said.
Whatever the outcome, he said, White is cleared to race immediately. She had
planned to compete in the Golden League track meet in Belgium on Friday and the
Grand Prix final in Monaco on Sept. 13-14.
White, of Union City in Northern California, is the first American woman to
sweep both sprints at a World Championships. She also will be able to
participate in next year's Athens Olympics.
If White is stripped of her medals, American runner Torri Edwards will be
awarded the 100 gold medal, while Zhanna Block of Ukraine would take silver and
Bahamas runner Chandra Sturrup the bronze.
The 200 champion would be Russia's Anastaiya Kapachinskaya. Edwards would take
silver and France's Muriel Hurtis the bronze.
The overall medals standings also would be altered, with America's total tally
of 20 medals dropping to 18, leaving Russia as the leader with 19. White would
also lose $60,000 in prize money for each gold.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF has said.
Under IAAF rules, the penalty for use of light stimulants also includes a public
warning. For harder stimulants, such as amphetamines, the sanction is
disqualification and a two-year ban.
Last Saturday, White acknowledged taking modafinil the morning of the 100 final.
But she denied ever taking a substance to enhance her performance, saying she
took the medication only to treat narcolepsy and had "no idea" it contained a
banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
However, an Internet search on modafinil turned up frequent warnings to athletes
that its use could result in a positive doping test.
LOAD-DATE: September 4, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
786 of 998 DOCUMENTS
Buffalo News (New York)
September 3, 2003 Wednesday, FINAL EDITION
WHITE'S CHOICE TO USE DRUG WAS DOPEY
SECTION: SPORTS, Pg.D1
LENGTH: 709 words
The fastest woman in the world can run, but she cannot hide. Her alibi was
laughable, her feigned ignorance insulting.
Kelli White cheated last week while becoming the first U.S. woman to sweep the
sprints at the World Track and Field Championships, and the consequences should
have been more severe. White warranted the maximum penalty, a two-year
suspension that would have precluded her participation in next Summer's Athens
Olympics, after testing positive for the stimulant modafinil following her
100-meter victory in Paris.
Instead, the International Association of Athletics Federations today ruled that
White won't be suspended, although her medals remain in jeopardy. The lax
decision is yet another blow to the image of a sport that long has suffered in
the arena of credibility.
White, a native of Oakland, said she was taking the prescription medication to
combat narcolepsy, which is characterized by daytime fatigue and an urge to
sleep. Makes sense. Modafinil has been used by military organizations to
invigorate weary troops.
However, White's insistence that this was all an innocent mistake, an oversight,
is undermined by the details of her argument. She claims that she and her
physician conducted extensive research on modafinil before prescribing it for
her condition. She explained that she neither sought a medical waiver nor
disclosed her usage because modafinil is not listed on the IAAF's list of banned
substances.
But White, 26, and her physician couldn't possibly have researched the effects
of modafinil and determined it inconsequential to her performance. An Associated
Press reporter covering the championships conducted a brief Internet search and
found a Web site, www.modafinil.info, that carried this warning: "Athletes
should be aware that one of the main ingredients of this pharmaceutical product
would produce a positive result in anti-doping tests."
A lengthy article on the Web site references an Aerospace Medical Association
article that concluded: "The development of modafinil brings to light a crucial
social question. What would be the impediment for its use, if a compound such as
modafinil is more like caffeine than amphetamine in terms of safety, and yet, as
effective as the amphetamines?"
That Aerospace Medical Association article was published in 1991. How could
White and her physician have thoroughly investigated the substance and concluded
it fell outside the IAAF's list of banned (and related) substances? It doesn't
wash.
The IAAF mandates disqualification and a public warning for athletes using minor
stimulants. Disqualification and a two-year ban from competition are the
penalties for use of hard-core stimulants that produce effects similar to
amphetamines. The remedy should have been apparent. White should have been dealt
a two-year suspension and be ordered to forfeit her medals.
White's rise to track prominence is a compelling story. She once was assaulted
in a knife attack two weeks after running the fastest high school 200 meters in
the country, suffering wounds that required more than 300 stitches and left a
scar surrounding her left eye. She went on to an undistinguished career at
Tennessee, emerging only within the last 18 months as a significant threat to
world speed queen Marion Jones. You'd like to believe her transgression was
merely an oversight, however the evidence weighs in to the contrary.
The world championships should be a celebration of the sport. Instead, all that
transpired in Paris pulled it deeper into the muck.
International track organizations seethed when USA Track & Field overturned on
appeal a failed steroids test, allowing an unnamed athlete to compete in the
Sydney Olympics. The Los Angeles Times last week identified the athlete as
Jerome Young, a member of the gold-medal-winning 1,600-meter relay at Sydney and
a two-time gold medalist at the worlds. The International Olympic Committee now
is calling for a detailed investigation.
The track world bristled at U.S. defiance again during the worlds when Jon
Drummond, disqualified for a false start in the 100 meters, protested by laying
on the track and delaying the competition.
Track has some growing up to do.
e-mail: bdicesare@buffnews.com
LOAD-DATE: September 5, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Buffalo News
787 of 998 DOCUMENTS
Chicago Sun-Times
September 2, 2003 Tuesday
Fun to track Team Troubled's travails
BYLINE: Carol Slezak
SECTION: SPORTS; Pg. 103
LENGTH: 942 words
HIGHLIGHT: Whether it was a crying sprinter or a positive drug test, the
American drama was compelling and disgusting.
The World Track and Field Championships are over, and I miss them. I especially
miss opening this newspaper every morning to read about the latest U.S. mishap.
Team USA? Try Team Troubled.
Then again, what's new? If only someone could figure out a way to market track
and field in the United States in non-Olympic years, it could become the new
NASCAR. I'm telling you, the travails of Team Troubled's tracksters make for
great drama. A sprinter crying in the middle of the track. Another sprinter
trying to explain her way out of a positive drug test. Even when it's
disgusting, it's compelling.
What to make of Kelli White's drug case? White won the 100 and 200 meter
sprints--yahoo!--but tested positive for the stimulant modafinil after the 100.
Just like that, White went from Marion Jones territory to Ben Johnson territory.
White said she takes the prescription drug to treat narcolepsy, a sleep
disorder. Since modafinil is not on the banned substance list, you might think
White has a good case. But it's not that simple. The subject of sprinters and
doping never is. The International Association of Athletics Federation says
modafinil is covered under its "related substances" stimulants category. In
other words, White should have known better.
At a news conference in France after her dirty test, White insisted her
conscience is clean. She denied using modafinil to improve her performance. She
said she didn't think it was necessary to notify the IAAF she was taking
modafinil because it wasn't listed as a banned substance. She said she didn't
take the drug regularly, only as needed.
White also said she and her doctor researched the drug before deciding to use it
to treat her narcolepsy. They must have neglected to do a Google search.
Mine--"doping and modafinil"--turned up a warning that one of the main
ingredients in modafinil would produce a positive result.
Just once I'd like to see a sprinter hold a news conference after a positive
drug test and say, "I knew what I was doing. I'm just sorry I got caught."
The IAAF is investigating White's case. This could take a while. The IAAF has
yet to even decide how modafinil should be classified. Is it a light stimulant
or a hard stimulant? White, 26, could face a simple disqualification and
warning. Or she could face a two-year ban. It's unlikely she'll get off without
some form of punishment.
Until White's faux pas, the best story about a woman at the World Championships
had been a heartwarming one. It was the tale of Lima Azimi, the first Afghan
woman to compete in a World Championships. Azimi's 100-meter time, 18.37
seconds, didn't advance the cause of Afghan athletes. But her mere appearance in
France advanced the cause of all Afghan women. As Azimi told the world, "It is
not important for me to win here, but it is very important for me to race here."
Amen, sister.
Now, back to the spoiled Americans. My goodness, the U.S. men are drama queens.
Jon Drummond started things off by false-starting in his 100-meter sprint. The
man-child was so incensed with the ruling he proceeded to throw a fit on the
track. He laid down on the track and wouldn't get up. He went back to the
starting line, although he knew he had been disqualified. He cried.
Drummond subsequently withdrew from the Championships altogether. Perhaps just
to make sure he didn't return anytime soon, World track officials officially
suspended him from the rest of the Championships.
Drummond's behavior wasn't even the strangest among the American men. Tim
Montgomery's was even weirder. After coming in fifth in the 100, Montgomery
disappeared. Turns out he flew home to North Carolina. But he didn't bother to
tell his coaches he was leaving. Or his teammates on the 400-meter relay team,
for that matter. Of course, Drummond was supposed to have been on the relay
team, too. As was Maurice Greene, who withdrew with an injury. And even with
three subs, Team Troubled managed to win the relay.
Maybe Montgomery left France because he missed Marion Jones, who was back home
with the couple's infant son. But that's no excuse for going AWOL. And isn't it
just wonderful that this childish behavior was on exhibit in France of all
places? No wonder the French don't like us.
There were some highlights for Team Troubled at the Worlds. The gold in the
men's 400-relay, for instance. A gold in the 200 meters for John Capel, who was
drafted by the Bears as a wide receiver in 2001. A total of 20 medals for the
United States, one more medal than runner-up Russia. Even that's subject to
change when White's doping case is resolved.
Craig Masback, the CEO of USA Track and Field, was pleased with Team USA's
performance.
'It sets us up for next year," Masback told the Associated Press. "Ultimately,
in our world, the Olympics is the big thing."
Medal counts aside, if Athens provides half the drama of these World
Championships, I'll be satisfied.
U.S. gold medalists
The U.S. led all nations with 20 medals, including 10 gold, at last week's World
Track and Field Championship in Saint-Denis, France. Double-winner Kelli White
could be stripped of her two golds after failing a drug test. The American gold
medalists:
MEN
110 hurdles--Allen Johnson.
200--John Capel.
400--Jerome Young.
4 x 100 relay--John Capel; Bernard Williams; Darvis Patton; J.J. Johnson.
4 x 400 relay--Calvin Harrison; Tyree Washington; Derrick Brew; Jerome Young.
Long jump--Dwight Phillips.
Decathlon--Tom Pappas.
WOMEN
100--Kelli White.
200--Kelli White.
4 x 400 relay--Me'Lisa Barber; Demetria Washington; Jearl Miles Clark; Sanya
Richards.
LOAD-DATE: September 10, 2003
LANGUAGE: English
GRAPHIC: Associated Press, American 400-relay team members celebrate their
victory at the World Track and Field Championships. The team included (from
left) ex-Bears draftee John Capel, Bernard Williams, Darvis Petton and J.J.
Joshua. CHART; SEE BELOW.
Copyright 2003 Chicago Sun-Times, Inc.
788 of 998 DOCUMENTS
The International Herald Tribune
September 2, 2003 Tuesday
A tale of two championships for the U.S. team ;
Athletics
BYLINE: Jere Longman
SOURCE: The New York Times
SECTION: SPORT; Pg. 16
LENGTH: 1094 words
DATELINE: PARIS:
As the World Championships ended in a rush of U.S. gold medals, Craig Masback,
the chief executive of USA Track & Field, held a news conference promising
change and summing up his mixed feeling about the previous nine days with a
quote from a novel about a different revolutionary era in Paris "It's a
Dickensian experience: best of times, worst of times," Masback said on Sunday.
He used the conference to outline a re-evaluation of the U.S. governing body for
athletics in the light of controversies in Paris regarding performance-enhancing
drugs and the histrionic behavior of the sprinter Jon Drummond, who sprawled on
the track at the Stade de France to protest a controversial false-start rule.
After a slow start in the competition, the United States won three gold medals
in relay races on Sunday. Both the 10 gold medals and the 20 medals overall led
the competition. But two of the golds remained in jeopardy after the sprint
champion Kelli White found herself embroiled in an unresolved drug case.
White's case remains under review by the International Association of Athletics
Federations, the sport's world governing body. After the 100 meters final, White
tested positive for modafinil, a stimulant that she said she had used to treat
the sleep disorder narcolepsy. Her urine test results were negative after the
later 200-meter final, USA Track and Field said on Sunday. A San Francisco Bay
Area doctor told a California newspaper that he had given White samples of the
drug to take on an as-needed basis. White said on Saturday that she had been
experiencing constant fatigue and restlessness at night because she was falling
asleep during the day.
"In Kelli's case, she could get jet lag up to 12 days," Dr. Brian Goldman, a
child psychiatrist, told The San Jose Mercury News. "You could be having a
conversation with her, and she just falls asleep." White's mother and an aunt
have severe narcolepsy, Goldman told the newspaper in an article published on
Sunday. White did not report on an IAAF doping control form that she was using
modafinil, as required, or ask for a special exemption to use it. The drug is
not on the official list of banned substances, but it is considered a "related
substance." Athletes use it at the peril of testing positive. White said she had
not reported the drug because it was not on the banned list. If a doping
violation is ruled, she faces a warning, which would also result in the loss of
her gold medals, or a two-year ban from competition. No date for a hearing or a
resolution of the case has been set, U.S. track officials said on Sunday. White
intends to run in the Golden League final in Brussels on Friday. Her eligibility
is uncertain. There was speculation on Sunday that her defense of the use of
modafinil might also include a contention that the drug is not a stimulant and
that it is not performance-enhancing. But the IAAF said it considered modafinil
a stimulant. Stimulants are prohibited because they are considered to provide an
unfair enhancement of performance. "They do not know the nature of the substance
and cannot currently identify a possible consequence, if any," White said on
Saturday. There were essentially two meets for the United States in the Stade de
France. One had some brilliant performances, including the brisk anchor leg that
J.J. Johnson ran in the 4x100-meter relay to edge Britain for the gold medal in
38.06 seconds. The United States was without Drummond, who was disqualified from
the Championships for bringing the sport into disrepute; without Maurice Greene,
the Olympic 100-meter champion, who injured a leg in Paris, and without Tim
Montgomery, the world record holder, who left after a poor performance in the
100. Still, the United States succeeded with Bernard Williams and a threesome of
200-meter specialists -- the world champion John Capel, the world runner-up
Darvis Patton and Johnson. The United States was the surprise winner in the
women's 4x400 relay, in 3 minutes 22.63 seconds, as Sanya Richards held off
Natalya Nazarova of Russia on the last leg. In the men's 400 relay, Jerome
Young, the 400-meter world champion, held off Marc Raquil of France for the gold
medal in 2:58.88.
The 20 total medals were the most by the United States since it took 25 in the
1993 World Championships in Stuttgart. But the performances were clouded by
Drummond's outburst during the 100-meter quarterfinals and by drug revelations
that included a report that Young tested positive for a steroid in 1999.
Masback said the distractions were a "call to action" for the track federation.
In October, a summit meeting of athletes, coaches and agents will be convened in
Miami to discuss a number of issues, including athlete behavior, he said. "I
don't want to say we've been dead in the water on this," he said. "We've been
proactive, but we've got to go to the next step."
The United States also needs a rules expert at each major competition, he said.
In addition, Masback called for uniform doping rules and for better education of
athletes from the United States about prohibited substances. Last month, Mickey
Grimes was given a warning and stripped of his gold medal in the 100 meters
after testing positive for a stimulant at the Pan American Games. "Whatever we
are doing is not enough," Masback said. "We've got to do more."
Masback defended the federation's actions regarding Young. The Los Angeles Times
reported that he had tested positive for the steroid nandrolone but been
exonerated on appeal and was allowed to compete in the 2000 Olympics on the
victorious 400 relay team.
The case was settled by international arbitration, and Young's name was kept
private by USA Track & Field until the newspaper revealed it. But Dick Pound,
president of the World Anti-Doping Agency, called for the relay gold medal won
in Sydney to be stripped from the U.S. team. He criticized USA Track & Field's
handling of the Young case, saying the legitimacy of the Sydney relay team had
been "shattered." The International Olympic Committee has also called for
further investigation. "I believe we have done the appropriate thing in all
circumstances," Masback said. On Sunday, he proposed an international relations
department in the federation to help improve the image of the United States
worldwide and to foster a better understanding of its rules.
These actions seemed welcomed by IAAF officials. "The U.S. federation should sit
down and figure out how not to be so unlucky in the future," Istvan Gyulai, the
general secretary of the IAAF, said.
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The Associated Press
September 1, 2003, Monday, BC cycle
White's medals still in limbo as she heads into rest of season
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 750 words
DATELINE: SAINT-DENIS, France
Kelli White heads into the rest of the European track season not knowing if
she'll get to keep her two gold medals from the World Championships.
The nine-day meet ended Sunday but the International Association of Athletics
Federations is still investigating whether the U.S. sprinter committed a doping
offense by testing positive for a stimulant after her victory in the 100 meters.
White passed a drug test after winning her second gold, in the 200 on Thursday,
IAAF general secretary Istvan Gyulai told The Associated Press. She was the
first American woman to sweep both sprints at a world championships.
Even though White tested clean after the 200, the IAAF said her positive test
after the 100 last Sunday would be enough to cost her both medals. Depending on
the severity of the offense, she could also face a two-year ban ruling her out
of next year's Athens Olympics.
The IAAF needs to clarify White's status soon because she is scheduled to run
Friday at the Golden League meet in Brussels. She also plans to compete in the
Grand Prix final in Monaco on Sept. 13-14 and an invitational meet in Moscow on
Sept. 20.
Gyulai said the IAAF was trying to determine the exact nature of modafinil, a
prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
Gyulai said the IAAF is contacting scientists around the world to determine how
to classify modafinil. He said that could take four or five days.
After that, Gyulai said, the IAAF would have three options: accept White's
explanation and consider clearing her on grounds of "exceptional circumstances";
disqualify her and give her a warning; or disqualify her and recommend a
two-year ban.
If the IAAF decides that modafinil falls into the strong category, White would
be suspended pending a hearing by USA Track & Field, Gyulai said. Her case would
then be handled by the U.S. Anti-Doping Agency, and could potentially end up
before the Court of Arbitration for Sport. That process could take months.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
"She was the star of the championships, and now she's at the center of a doping
case," former Olympic and world champion Michael Johnson wrote in his daily
column in the French sports daily L'Equipe. "It creates trouble for our sport.
It's a big cloud over these championships."
At a news conference Saturday, White acknowledged taking modafinil the morning
of the 100 final. But she denied ever taking a substance to enhance her
performance, saying she took the medication only to treat narcolepsy and had "no
idea" it contained a banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
An Internet search on modafinil turned up frequent warnings to athletes.
"Athletes should be aware that one of the main ingredients of this
pharmaceutical product would produce a positive result in anti-doping tests,"
said the Web site www.modafinil.info.
White was not the only American athlete at the championships who came under
scrutiny for drugs.
The Los Angeles Times reported that 400 champion Jerome Young tested positive
for steroids in 1999, but was cleared on appeal by U.S. track officials and
allowed to compete in the 2000 Sydney Olympics, where he won gold as a member of
the 1,600 relay team.
World Anti-Doping Agency chief Dick Pound has called for the U.S. team to be
stripped of the medal.
Young won his second gold medal of the championships Sunday night, anchoring the
U.S. 1,600 relay team to victory in the final event of the meet.
"I just didn't worry about it," Young said of the doping allegations. "I just
put it behind me and kept on going, and just basically used that as a motivation
for me."
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LANGUAGE: ENGLISH
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All Rights Reserved
790 of 998 DOCUMENTS
Associated Press Online
September 1, 2003 Monday
Kelli White's Medals Still in Limbo
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 746 words
DATELINE: SAINT-DENIS, France
Kelli White heads into the rest of the European track season not knowing if
she'll get to keep her two gold medals from the World Championships.
The nine-day meet ended Sunday but the International Association of Athletics
Federations is still investigating whether the U.S. sprinter committed a doping
offense by testing positive for a stimulant after her victory in the 100 meters.
White passed a drug test after winning her second gold, in the 200 on Thursday,
IAAF general secretary Istvan Gyulai told The Associated Press. She was the
first American woman to sweep both sprints at a world championships.
Even though White tested clean after the 200, the IAAF said her positive test
after the 100 last Sunday would be enough to cost her both medals. Depending on
the severity of the offense, she could also face a two-year ban ruling her out
of next year's Athens Olympics.
The IAAF needs to clarify White's status soon because she is scheduled to run
Friday at the Golden League meet in Brussels. She also plans to compete in the
Grand Prix final in Monaco on Sept. 13-14 and an invitational meet in Moscow on
Sept. 20.
Gyulai said the IAAF was trying to determine the exact nature of modafinil, a
prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
Gyulai said the IAAF is contacting scientists around the world to determine how
to classify modafinil. He said that could take four or five days.
After that, Gyulai said, the IAAF would have three options: accept White's
explanation and consider clearing her on grounds of "exceptional circumstances";
disqualify her and give her a warning; or disqualify her and recommend a
two-year ban.
If the IAAF decides that modafinil falls into the strong category, White would
be suspended pending a hearing by USA Track & Field, Gyulai said. Her case would
then be handled by the U.S. Anti-Doping Agency, and could potentially end up
before the Court of Arbitration for Sport. That process could take months.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
"She was the star of the championships, and now she's at the center of a doping
case," former Olympic and world champion Michael Johnson wrote in his daily
column in the French sports daily L'Equipe. "It creates trouble for our sport.
It's a big cloud over these championships."
At a news conference Saturday, White acknowledged taking modafinil the morning
of the 100 final. But she denied ever taking a substance to enhance her
performance, saying she took the medication only to treat narcolepsy and had "no
idea" it contained a banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
An Internet search on modafinil turned up frequent warnings to athletes.
"Athletes should be aware that one of the main ingredients of this
pharmaceutical product would produce a positive result in anti-doping tests,"
said the Web site www.modafinil.info.
White was not the only American athlete at the championships who came under
scrutiny for drugs.
The Los Angeles Times reported that 400 champion Jerome Young tested positive
for steroids in 1999, but was cleared on appeal by U.S. track officials and
allowed to compete in the 2000 Sydney Olympics, where he won gold as a member of
the 1,600 relay team.
World Anti-Doping Agency chief Dick Pound has called for the U.S. team to be
stripped of the medal.
Young won his second gold medal of the championships Sunday night, anchoring the
U.S. 1,600 relay team to victory in the final event of the meet.
"I just didn't worry about it," Young said of the doping allegations. "I just
put it behind me and kept on going, and just basically used that as a motivation
for me."
LOAD-DATE: September 2, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
791 of 998 DOCUMENTS
Herald Sun (Melbourne, Australia)
September 1, 2003 Monday
Why sprint ace Kelli took drug
SOURCE: AAP
BYLINE: GUY JACKSON
SECTION: SPORT; Pg. 56
LENGTH: 479 words
AMERICAN Kelli White, who risks being stripped of both her world championships
sprint titles after testing positive for a stimulant, explained yesterday why
she had taken the drug.
White, the 100m and 200m champion, said she suffered from narcolepsy, a
condition that causes extreme tiredness.
She protested her innocence after the International Association of Athletics
Federations announced it was investigating the content of the drug, Modafinil,
also known by its brand name Provigil, and wanted to hear more evidence from
White before deciding whether to strip her of her titles.
Reading from a statement, White said: "I am under suspicion of a doping
violation. The mere fact of this allegation is personally harmful and hurtful.
"I have never taken any substance to enhance my performance. Close members of my
family have been under doctor's care for the condition of narcolepsy for years.
"I too have been diagnosed with this condition by my physician. He prescribed
the drug Provigil and I have taken it in certain circumstances, including prior
to the 100m.
"I did not seek an IAAF medical exemption for this substance or note it on my
doping control form because I had no idea that Provigil contained a banned
substance."
Professor Arne Ljungqvist, the head of the IAAF medical committee, earlier
defined Modafinil as a drug taken "by people who easily lose concentration and
awareness and actually fall asleep".
He explained that although Modafinil was not on the banned list, it could be a
"related substance" and part of either the drug group known as ephedrine or
amphetamines, both of which are forbidden.
He said White's case would not be helped by the fact she failed to declare her
use of the drug.
"She did not declare the substance beforehand," Ljungqvist said. "She should
have done it and she should have asked for an exemption to use it.
"That is a problem for her when her case is later evaluated."
But White said: "As an athlete, those lists are very hard to understand. Given
that it was not on the banned list, I think it is understandable why I didn't
realise that I needed to declare it on my doping form.
"It is kind of hard to remember everything you take in the day."
After the announcement of her positive test, 26-year-old White pulled out of the
US 4 x 100m relay squad that went on to finish second to France in yesterday's
final.
Ljungqvist said in deciding White's fate, the key factor would be Modafinil's
drug category.
If it is established it is related to ephedrine, the IAAF could strip White of
her titles and issue a warning. But if the substance is established to be in the
group of amphetamines, it would lead to White losing her titles and being
suspended for two years.
Ljungqvist said it was possible to suffer from narcolepsy and still be a
high-level athlete.
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LANGUAGE: ENGLISH
JOURNAL-CODE: DHS
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The International Herald Tribune
September 1, 2003 Monday
Drug may cost White medals
BYLINE: Jere Longman
SOURCE: The New York Times
SECTION: SPORT; Pg. 14
LENGTH: 815 words
DATELINE: PARIS:
Kelli White of the United States, the women's champion at 100 and 200 meters at
the world track and field championships, has tested positive for a stimulant,
and that could cost her the gold medals she won here and could prevent her from
competing in the 2004 Olympics in Athens, the sport's world governing body said.
The International Association of Athletics Federations, the governing body, said
a urine sample provided by White showed the presence of the stimulant modafinil,
which is used to treat narcolepsy, after she won the 100 meters in 10.85
seconds, her best time, on Aug. 24.
No action had been taken against her by Saturday, when the IAAF revealed the
failed test, and the case remained under review.
[White's urine sample taken after she won the 200 meter did not test positive,
athletics sources said Sunday, Reuters reported from Paris.]
White was cleared to run the 4x100 relay Saturday, but she did not participate,
apparently not wanting to risk disqualification of the entire team. Without
White, the United States finished second to France, but the defeat was
overshadowed by the potential disruption of White's career just when it seemed
to reach its apex. She ran faster in the 100 and 200 here than she ever had.
White's case is complicated, and no doping offense has been officially declared.
But the IAAF made it clear that White would have a difficult time defending her
use of the stimulant and avoiding a penalty.
The possible sanctions range from a warning, which would still result in
disqualification from these championships and the loss of her gold medals, to a
two-year suspension, which would bar her from competing in the 2004 Olympics.
She also stands to lose $120,000 in prize money for her victories.
Modafinil, a prescription drug sold under the brand name Provigil in the United
States, is a memory-improving and mood-brightening substance used to combat
extreme sleepiness in people with narcolepsy.
White, who is 26 and lives in California, said at a news conference that she had
been taking the substance for several months to treat symptoms of narcolepsy,
which included constant fatigue and restlessness at night because she would fall
asleep during the day.
Several members of her family have been under a doctor's care for narcolepsy for
years, White said.
"The mere fact of this allegation is personally harmful and hurtful," White
said. "I have never taken any substance to enhance my performance."
Modafinil has not been placed by name on the list of performance-enhancing
substances banned by the International Olympic Committee and the World
Anti-Doping Agency. But it is considered a related substance, meaning that
athletes use it at the risk of being found guilty of doping. The European
Council has asked that it be listed by name as a banned substance beginning next
year.
White said she had not notified the IAAF on a doping control form that she was
using modafinil, believing it was unnecessary because the stimulant was not
listed as a prohibited substance. She said she took the stimulant only when
needed and had not tested positive at previous meets this summer, so she
expected no problems at the world championships.
She had contacted the IAAF and the U.S. Anti-Doping Agency while doing extensive
research about the drug and found no evidence that it was prohibited. It was
unclear whether the contact was person-to-person or by computer.
Arne Ljungqvist of Sweden, a doctor who is a top medical official in the IAAF
and the International Olympic Committee, said athletes were required to list all
medications they were taking, and White listed supplements she was using.
It is possible that even if White had a legitimate medical reason to use
modafinil, she could lose her medals or her Olympic eligibility because she did
not provide the IAAF with sufficient notice of her usage or receive a special
waiver.
"She should have done it," Ljungqvist said of the notification. "Even more, she
should have asked for a prior exemption to use it. That is a problem for her
when her case will later be evaluated."
An Internet search of modafinil turned up a prescription medication Web site
that warned, "Athletes should be aware that one of the main ingredients of this
product would produce a positive result in anti-doping tests."
Mark Gay, the general counsel of the IAAF, said the track body would investigate
whether White had a doctor's prescription for the stimulant. Before any penalty
can be assessed, the IAAF must also decide what class of stimulants modafinil
belongs to.
If modafinil is declared to be in the same performance-enhancing class as
amphetamines, White faces a two-year ban, Ljungqvist said. If it is considered
in a class of lesser stimulants like ephedrine, White would face a warning and
disqualification from the world championships, he said.
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LANGUAGE: ENGLISH
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The Irish Times
September 1, 2003
White's gold has tarnished look now
BYLINE: By IAN O'RIORDAN
SECTION: CITY EDITION; SPORT; Pg. 58
LENGTH: 324 words
As they said in L'Equipe yesterday, 'White dans la nasse' - 'White caught in the
net'.
Kelli White, America's gold medal winner of the 100 and 200 metres, left Paris
yesterday under the darkest cloud of controversy at a major championships since
Ben Johnson cheated his way to 100 metre gold at the 1988 Seoul Olympics.
It was L'Equipe who broke the story on Saturday, revealing the presence of a
known stimulant in the doping test taken after White's 100 metre victory.
The problem for White is her sample showed traces of modafinil, not officially
on the IOC list of prohibited substances, but known to be related to substances
that are.
If the IAAF follow their usual procedure the least punishment White can expect
is the loss of her two gold medals. If they come down hard she would receive a
two-year ban.
IAAF medical chief Arne Ljungqvist has talked about a "full and proper
investigation" before any action will be taken. The problem, for now, is
modafinil hasn't yet been classified as a minor stimulant, which would only see
her lose the medal, or a major stimulant, which would also see her banned.
From next year, though, it will banned outright.
White appeared at a specially arranged press conference, where she admitted
taking the drug, but denied using it to gain a competitive advantage.
Her doctor had diagnosed the sleep disorder narcolepsy "a few months ago" and so
prescribed modafinil - as he had done for several other members of her family,
she said.
She admitted taking Provigil, which contains modafinil, on the morning of the
100 metre final. White, 26, has more explaining to do; for instance, why she
didn't, as required, declare the drug.
She claims she didn't know the substance was related to anything on the banned
list. It will be several weeks before the IAAF conclude their investigation but
even then the doubts that surround her performances in Paris won't be easy to
dispel.
LOAD-DATE: September 9, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Irish Times
794 of 998 DOCUMENTS
MX (Melbourne, Australia)
September 1, 2003 Monday
Race body swift to negate sprint wins
SECTION: SPORT; Pg. 17
LENGTH: 241 words
SLEEPLESS NIGHTS
Kelli White passed a drug test after winning the 200m but still could lose her
gold medals from the World Championships.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, said yesterday the US sprinter's latest doping test was negative.
White won the 100m last Sunday and completed the double in the 200m on Thursday,
becoming the first American woman to sweep both events at a world championships.
The IAAF said that she tested positive for the stimulant modafinil after the
100m final and risked being stripped of all her championship results if found
guilty of a doping offence.
She also could face a two-year ban that would rule her out of the 2004 Athens
Olympics.
Even though White tested clean after the 200m, the IAAF said her positive 100m
test could cost her both medals.
"It doesn't change things," IAAF spokesman Nick Davies said. "It's irrelevant.
We had a positive sample after the 100 metres. If we disqualify her, we
disqualify her."
Gyulai said the IAAF was investigating the exact nature of modafinil, a
prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under
"related substances", the IAAF said.
The penalty for use of light stimulants is disqualification and a warning. For
harder stimulants, the sanction is disqualification and a two-year ban.
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The New York Times
September 1, 2003 Monday
Late Edition - Final
TRACK AND FIELD;
As Championships End, Drug Imbroglio Goes On
BYLINE: By JERE LONGMAN
SECTION: Section D; Column 1; Sports Desk; Pg. 2
LENGTH: 1120 words
DATELINE: PARIS, Aug. 31
After a slow start last week, the United States won three gold medals in relay
races today as the world track and field championships concluded at the Stade de
France. Both the 10 gold medals and the 20 medals over all led the competition.
But two of the gold medals remained in jeopardy after the sprint champion Kelli
White found herself embroiled in an unresolved drug case.
As the championships ended, the chief executive of USA Track and Field outlined
a re-evaluation of the national governing body in light of controversies here
regarding performance-enhancing drugs and the histrionic behavior of the
sprinter Jon Drummond, who lay on the track last Sunday in protest of a
controversial false-start rule.
"It's a Dickensian experience: best of times, worst of times," Craig Masback,
the chief executive of USA Track and Field, said today at a news conference.
No action was taken today in White's case, which remains under review by the
International Association of Athletics Federations, track and field's world
governing body. After the 100 meters last Sunday, White tested positive for
modafinil, a stimulant that she said she used to treat the sleep disorder
narcolepsy. Her urine test results were negative after the 200 meters, USA Track
and Field said today.
A San Francisco Bay Area doctor confirmed to a California newspaper that he had
given White samples of the drug to take on an as-needed basis. White said on
Saturday that she had been experiencing constant fatigue and restlessness at
night because she was falling asleep during the day.
"In Kelli's case, she could get jet lag up to 12 days," Dr. Brian Goldman, a
child psychiatrist, told The San Jose Mercury News. "You could be having a
conversation with her and she just falls asleep."
White's mother and an aunt have severe narcolepsy, Goldman told the newspaper in
an article published today.
White did not report on an I.A.A.F. doping control form that she was using
modafinil, as required, or ask for a special exemption to use it. The drug is
not on the official list of banned substances, but it is considered a "related
substance." Athletes use it at the peril of testing positive.
White said she did not report the drug because it was not on the banned list. If
a doping violation is ruled, she faces a warning, which would also result in the
loss of her gold medals, or a two-year ban from competition. No date for a
hearing or a resolution of the case has been set, United States track officials
said today.
White intends to run in a meet in Brussels on Friday. Her eligibility is
uncertain. There was speculation today that her defense of the use of modafinil
might also include a contention that the drug is not a stimulant and that it is
not performance enhancing.
The I.A.A.F. said it considers modafinil a stimulant, but the governing body has
not classified the drug as a serious stimulant, like amphetamines, or a lesser
stimulant, like ephedrine. Stimulants are prohibited because they are considered
to provide an unfair enhancement of performance.
"They do not know the nature of the substance and cannot currently identify a
possible consequence, if any," White said on Saturday.
There were essentially two meets here for the United States.
One had some brilliant performances, including the brisk anchor leg that J.J.
Johnson ran in the 4x100-meter relay to edge Britain for the gold medal in 38.06
seconds.
The United States was without Drummond, who was disqualified from the meet for
bringing the sport into disrepute; without Maurice Greene, the Olympic 100-meter
champion, who injured a leg here; and without Tim Montgomery, the world
record-holder, who left after a poor performance in the 100. Still, the United
States succeeded with Bernard Williams and a threesome of 200-meter specialists
-- the world champion John Capel, the world runner-up Darvis Patton and Johnson.
"Through all the adversity, all the downfalls, we stepped up to show that the
U.S. is still a strong country and always will be," Capel said.
The United States was also the surprise winner in the women's 4x400 relay, in 3
minutes 22.63 seconds, as Sanya Richards held off Natalya Nazarova of Russia on
the anchor leg. The United States did not dominate as usual in the men's 4x400
relay, but Jerome Young, the 400-meter world champion, held off a fast-closing
Marc Raquil of France for the gold medal in 2:58.88.
The 20 total medals were the most won by the United States since the 25 achieved
at the 1993 world championships in Stuttgart, Germany. But the performances were
clouded by Drummond's outburst during the 100-meter quarterfinals and by drug
revelations that included a report that Young tested positive for a steroid in
1999.
In October, a summit of athletes, coaches and agents will be convened in Miami
to discuss a number of issues, including athlete comportment, Masback said.
"I don't want to say we've been dead in the water on this," he said. "We've been
proactive, but we've got to go to the next step."
The United States also needs a rules expert at each major competition, he said.
In addition, Masback called for uniform doping rules and for better education of
athletes from the United States about prohibited substances. Earlier this month,
Mickey Grimes was given a warning and stripped of his gold medal at 100 meters
after testing positive for a stimulant at the Pan American Games.
"Whatever we are doing is not enough," Masback said. "We've got to do more."
Masback defended the federation's actions regarding Young. The Los Angeles Times
reported that he tested positive for the steroid nandrolone, was exonerated on
appeal and was allowed to compete in the 2000 Sydney Olympics on the victorious
4x400 relay team.
The case was settled by international arbitration and Young's name was kept
private by USA Track and Field until the newspaper revealed it. But Dick Pound,
president of the World Anti-Doping Agency, called for the relay gold medal won
in Sydney, Australia, to be stripped from the United States team. He criticized
USA Track and Field's handling of the Young case, saying the legitimacy of the
Sydney relay team had been "shattered."
The International Olympic Committee has also called for further investigation.
"I believe we have done the appropriate thing in all circumstances," Masback
said.
Today, he proposed an international relations department in the federation to
help improve the image of the United States worldwide and to foster a better
understanding of its rules. These actions seemed welcomed by top I.A.A.F.
officials.
"The U.S. federation should sit down and figure out how not to be so unlucky in
the future," Istvan Gyulai, the general secretary of the I.A.A.F., said.
URL: http://www.nytimes.com
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GRAPHIC: Photo: Jerome Young of the United States crossing the finish line ahead
of Marc Raquil of France to win the men's 4x400-meter relay yesterday. (Photo by
Associated Press)
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The Northern Echo
September 1, 2003
WHITE PLEADS HER CASE
SECTION: Pg. 22
LENGTH: 396 words
Kelli White, who has tested positive for a stimulant which is not listed by name
as a banned substance, insists she should be allowed to keep the 100 metres and
200 metres gold medals which she won at the World Championships.
The American tested positive for modafinil after her 100m triumph last Sunday
and the IAAF have said that she may end up having to give back her medals - even
though the substance is not on their list of banned drugs.
The IAAF said it was covered under a clause for ''related substances'' and are
looking into whether modafinil may fall under the category of ephedrine, a minor
stimulant, or a strong stimulant like amphetamines.
If it is classified as the latter, White could be facing a ban as well as being
stripped of her medals.
White defended herself vigorously at a press conference in Paris last night,
revealing that she takes the drug Provigil because she has narcolepsy.
The drug contains modafinil.
''I am under suspicion of a doping violation,'' said the 26-year-old White.
''The mere fact of this allegation is personally harmful and hurtful.
''Honestly, deep in my heart I know I'm innocent.
"I would take full responsibility but the medication is not on the banned list.
''I have never taken any substance to enhance my performance.
''Close members of my family have been under doctors' care for the condition of
narcolepsy for years.
''I, too, have been diagnosed with this condition by my physician, Dr Brian
Goldman. He prescribed the drug Provigil for this condition and I have taken it
in certain circumstances, including prior to the 100 metres.''
Explaining why she had not declared it before the championships in accordance
with IAAF rules, White said: ''I did not seek IAAF medical exemption for this
substance or note it on my doping control form, because I had no idea Provigil
contained a banned substance."
Meanwhile, hurdling great Colin Jackson has slammed drug testing procedures.
Jackson believes the lack of a clear worldwide directive and the grey area over
which drugs are legal or not is threatening to make a mockery of athletics.
Jackson said: ''What we're seeing now is a whole mess - it is not structured and
that is where the problem lies.
''What brings the whole credibility of the sport down is that there are no real
answers to anything.'
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The Vancouver Sun (British Columbia)
September 1, 2003 Monday Final Edition
White passes second test but could lose medals: Although testing drug free after
200 victory, U.S. sprinter faces possible two-year ban
SOURCE: Associated Press
SECTION: Sports; Pg. E4
LENGTH: 452 words
DATELINE: SAINT-DENIS, France
SAINT-DENIS, France -- Kelli White passed a drug test after winning the 200
metres for her second gold medal at the world track and field championships, but
her earlier positive sample following her victory in the 100 jeopardizes both
medals.
Istvan Gyulai, general secretary of the International Association of Athletics
Federations, confirmed Sunday the U.S. sprinter's latest doping test was
negative.
White won the 100 a week ago and completed the sprint double in the 200 on
Thursday, becoming the first American woman to sweep both events at a world
championships.
The IAAF said Saturday she tested positive for the stimulant modafinil after the
100 final and risked being stripped of both gold medals if found guilty of a
doping offence. She could also face a two-year suspension.
Even though White tested negative after the 200, the IAAF said her positive test
after the 100 would be enough to disqualify her from the entire championships
and cost her both medals.
"It doesn't change things," IAAF spokesman Nick Davies said. "It's irrelevant.
We had a positive sample after the 100 metres. If we disqualify her, we
disqualify her."
Gyulai said, "It would be wrong to say, 'You are doping on Sunday, and you're
out,' and then say, 'You can win the same medal Thursday at the same
championships.' I believe this is an important moral message."
Gyulai said the IAAF was continuing to investigate the exact nature of modafinil
, a prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
Gyulai said IAAF doping officials expect it could take four or five days to
determine how to classify modafinil. After that, he said, the IAAF would have
three options: Accept her explanation and consider clearing her on grounds of
"exceptional circumstances"; disqualify her and give her a warning; or
disqualify her and recommend a two-year ban.
White denied ever taking a substance to enhance her performance. She said she
took the medication only to treat narcolepsy and had "no idea" it contained a
banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form because it wasn't named on the prohibited drug list.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," she said.
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GRAPHIC: Color Photo: Kelli White
TYPE: Sports
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All Rights Reserved
798 of 998 DOCUMENTS
The Washington Post
September 1, 2003 Monday
Final Edition
White's Other Drug Test Comes Back Negative;
As U.S. Racks Up a Record 20 Medals, Sprinter Hopes to Retain Her Two
BYLINE: Amy Shipley, Washington Post Staff Writer
SECTION: SPORTS; Pg. D01
LENGTH: 1187 words
DATELINE: SAINT-DENIS, France Aug. 31
-- The United States finished the ninth World Track and Field Championships
today with its biggest medal haul in 10 years and some negative news that was
actually quite positive.
U.S. sprinter Kelli White's drug test from Thursday's 200-meter final turned up
negative, her agent disclosed today, lending credence to her claim that she took
the stimulant modafinil at this meet for medical reasons, not performance
enhancement, and giving her hope that she might be able to keep at least one of
the two gold medals she won here.
Meantime, White's physician, Brian D. Goldman, said he gave her two sample
bottles of the drug -- about six to 12 pills -- to take on an "as needed basis"
earlier this year after diagnosing the sleep disorder narcolepsy during a
consultation in the Bay Area.
"She had all the clinical indications," said Goldman, a consultant to Victor
Conte at Balco Laboratories in Burlingame, Calif., which has worked with
hundreds of star athletes including Marion Jones and Jones's ex-husband, C.J.
Hunter, who tested positive for the steroid nandrolone just before the 2000
Summer Games in Sydney.
Today's developments, however, did not extract White from what likely will be a
protracted controversy surrounding her positive test after last week's 100
final, nor did it erase the ugliness that seemed to follow the American team
throughout this meet, even as it won 20 medals (10 gold, 8 silver, 2 bronze),
more than any other country. Russia won 19; Belarus, France and Ethiopia each
claimed seven.
"It's a Dickensian experience," USA Track and Field CEO Craig Masback said
during an impromptu news conference. "It's a best-of-times, worst-of-times
week."
The championships got underway with Jon Drummond's lay-down protest of his
disqualification from the 100 quarterfinals and ended tonight with U.S. gold
medals in the men's and women's 4x400 relays and the men's 4x100. The victory in
the short relay was something of a surprise as the U.S. team had been depleted
by a thigh injury to Maurice Greene, the mid-week disappearance of Tim
Montgomery, and the banishment of Drummond for his bad behavior.
"These four guys were never supposed to be together," said John Capel about the
team that included himself, Bernard Williams, Darvis Patton and J.J. Johnson and
won in 38.06 seconds. "Through all the adversity, all of the downfalls, we
stepped up to show that the United States is still a strong country and always
will be."
The United States was strong enough to earn more medals than it had won since
the 1993 world championships, but it might not be strong enough to keep all of
them. On Saturday, White learned she could be forced to relinquish her 100 and
200 golds and banned from the sport for two years as a result of the positive
test for modafinil, a drug that the world track and field governing body (the
IAAF) is scrambling to classify.
Earlier in the week, it was revealed that American Jerome Young, the meet's 400
world champion, had tested positive for a banned steroid in 1999, but was
exonerated by a U.S. arbitration panel in time to win a relay gold medal at the
2000 Summer Games.
"We, like other U.S. institutions, have been naive about our place in the world,
our place in the world of sports," said Masback, who said he would push for the
creation of an international relations committee within USA Track and Field.
"That's really come home to me this week . . . We, as a U.S. entity operating in
an international framework, haven't been prepared to deal with that."
Drummond's display generated an international lambasting, but White's case could
have the most damning long-term implications. Though modafinil is not
specifically banned by the IAAF, the organization could levy punishment if it
determines that the drug is similar to amphetamines or ephedrine. That would be
a severe blow both to White and the United States, as she emerged this year as a
potential rival to Jones, the five-time Olympic medalist.
Goldman said he attended a conference recently in San Francisco given by
Cephalon, which markets modafinil under the brand-name Provigil, and said a
number of experts stated that modafinal gives no competitive advantage to
athletes.
"Various doctors and scientists spoke," Goldman said. "It doesn't seem to have
any value as a performance-enhancing drug."
Added Goldman, who spoke by phone from the Bay Area: "In my experience, it
doesn't help people who are normal, unlike the asthma drugs."
Goldman said White informed him that she had a family history of narcolepsy --
her mother and maternal aunt have severe cases -- and a slate of other symptoms:
trouble overcoming jetlag; the tendency to fall into deep sleeps during the day;
and problems sleeping at night. She also suffered from mild depression while in
college at Tennessee, he said.
Goldman said his colleagues at Balco researched the drug in detail and knew it
wasn't banned either by the IAAF or International Olympic Committee, so they
weren't concerned about giving her the samples.
He said he was aware that the IAAF requires medical declarations for all
prescription drugs, but he did not think a declaration necessary in this case
since she was instructed to take the drug only as needed. Her agent, Robert
Wagner, said she told him she had taken the drug before the U.S. championships
in June, a meet in Oslo and an unannounced drug test in London.
Goldman said White was referred to him through Balco, which has worked with
Montgomery, Matt Biondi, Jim Courier, John Elway, Renaldo Nehemiah and dozens of
other star athletes, according to Goldman and company literature. Conte defended
Hunter after his positive tests for nandrolone, saying the supplements he took
were contaminated.
"I'm just a doctor," Goldman said. "My job is to make people well when the
appropriate medical indications suggest something could help. We sometimes give
people samples. If it works for them, they come back to us and say they would
like a written prescription."
Wagner said he was prepared for the case to drag on for some time but said White
-- who remains eligible to compete -- intended to run this Friday at a meet in
Brussels. He said she stayed away from Stade de France today, choosing to watch
her boyfriend, Boris Henry, on television compete in the javelin final. Henry,
who competes for Germany, won the bronze.
"It is very hard to focus on my competition today because of what is happening
with my girlfriend Kelli White right now," Henry said afterward. "I just want to
go and see her now. I need to be with her now."
Notes: Morocco's Hicham El Guerrouj and Ethiopia's Kenenisa Bekele both failed
-- barely -- in their attempts to become double gold medalists. In the men's
5,000, Kenya's Eliud Kipchoge (12 minutes 52.79 seconds) barely edged El
Guerrouj (12:52.83), the 1,500 champion, in a sprint to the finish. Bekele, the
10,000 meter champion, claimed the bronze in 12:53.12. . . . Catherine Ndereba
won Kenya's only other gold medal, winning the marathon in a championship record
of 2:23.55 seconds, holding off Japan's Mizuki Noguchi, who finished in 2:24.14.
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The Associated Press
August 31, 2003, Sunday, BC cycle
IAAF: White tested negative after second gold medal
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 624 words
DATELINE: SAINT-DENIS, France
Kelli White passed a drug test after winning the 200 meters but still could lose
her two gold medals from the World Championships, track officials said Sunday.
The results from the second test were revealed one day after officials from the
International Association of Athletics Federations said White had tested
positive following her victory in the 100.
White won gold in the 100 a week ago and completed the sprint double in the 200
on Thursday, becoming the first American woman to sweep both events at a world
championships.
Even though White tested clean after the 200, the IAAF said her positive test
after the 100 would be enough to cost her both medals.
"It would be wrong to say, 'You are doping on Sunday, and you're out,' and then
say, 'You can win the same medal Thursday at the same championships,"' Istvan
Gyulai, general secretary of the IAAF, said Sunday. "I believe this is an
important moral message."
The IAAF said Saturday that White risked being stripped of all her championship
results if found guilty of a doping offense. She also could face a two-year
suspension that would rule her out of the 2004 Athens Olympics.
Gyulai said the IAAF was continuing to investigate the exact nature of modafinil
, a prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a warning. For harder stimulants, such as amphetamines, the
sanction is disqualification and a two-year ban.
Gyulai said the IAAF is trying to determine how to classify modafinil. He said
that could take four or five days.
After that, Gyulai said, the IAAF could: accept White's explanation and consider
clearing her on grounds; disqualify her and give her a warning; or, disqualify
her and recommend a two-year ban.
If the IAAF decides modafinil falls into the strong category, White would be
suspended pending a hearing by USA Track & Field, Gyulai said. Her case would
then be handled by the U.S. Anti-Doping Agency, and could potentially end up
before the Court of Arbitration for Sport - a process that could take months.
The IAAF needs to clarify White's status soon because she is scheduled to run
Friday at the Golden League meet in Brussels. She also plans to compete in the
Grand Prix final in Monaco on Sept. 13-14 and an invitational meet in Moscow on
Sept. 20.
USA Track & Field chief executive Craig Masback said he had only been notified
of White's test result from the 100, and can't take action until getting more
details from the IAAF.
At a news conference Saturday, White acknowledged taking modafinil the morning
of the 100 final. But she denied ever taking a substance to enhance her
performance, saying she took the medication to treat narcolepsy and had no idea
it contained a banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list. She said she and her doctor did extensive research on modafinil
before deciding to use it for narcolepsy, which causes sudden fatigue or
sleepiness.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
"She was the star of the championships, and now she's at the center of a doping
case," former Olympic and world champion Michael Johnson wrote in his daily
column in the French sports daily L'Equipe. "It creates trouble for our sport.
It's a big cloud over these championships."
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Associated Press Worldstream
August 31, 2003 Sunday
White's medals still in limbo as she heads into rest of season
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 749 words
DATELINE: SAINT-DENIS, France
Kelli White heads into the rest of the European track season not knowing if
she'll get to keep her two gold medals from the World Championships.
The nine-day meet ended Sunday, but the International Association of Athletics
Federations is still investigating whether the U.S. sprinter committed a doping
offense by testing positive for a stimulant after her victory in the 100 meters.
White passed a drug test after winning her second gold, in the 200 meters on
Thursday, IAAF general secretary Istvan Gyulai told The Associated Press. She
was the first American woman to sweep both sprints at a world championships.
Even though White tested clean after the 200, the IAAF said her positive test
after the 100 last Sunday would be enough to cost her both medals. Depending on
the severity of the offense, she could also face a two-year ban ruling her out
of next year's Athens Olympics.
The IAAF needs to clarify White's status soon because she is scheduled to run
Friday at the Golden League meet in Brussels. She also plans to compete in the
Grand Prix final in Monaco on Sept. 13-14 and an invitational meet in Moscow on
Sept. 20.
Gyulai said the IAAF was trying to determine the exact nature of modafinil, a
prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
Gyulai said the IAAF is contacting scientists around the world to determine how
to classify modafinil. He said that could take four or five days.
After that, Gyulai said, the IAAF would have three options: accept White's
explanation and consider clearing her on grounds of "exceptional circumstances";
disqualify her and give her a warning, or disqualify her and recommend a
two-year ban.
If the IAAF decides that modafinil falls into the strong category, White would
be suspended pending a hearing by USA Track & Field, Gyulai said. Her case would
then be handled by the U.S. Anti-Doping Agency, and could potentially end up
before the Court of Arbitration for Sport. That process could take months.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
"She was the star of the championships, and now she's at the center of a doping
case," former Olympic and world champion Michael Johnson wrote in his daily
column in the French sports daily L'Equipe. "It creates trouble for our sport.
It's a big cloud over these championships."
At a news conference Saturday, White acknowledged taking modafinil the morning
of the 100 final. But she denied ever taking a substance to enhance her
performance, saying she took the medication only to treat narcolepsy and had "no
idea" it contained a banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list.
White said she and her doctor had done extensive research on modafinil before
deciding to use it for narcolepsy, which causes sudden fatigue or sleepiness.
The drug is sold under the brand name Provigil in the United States.
An Internet search on modafinil turned up frequent warnings to athletes.
"Athletes should be aware that one of the main ingredients of this
pharmaceutical product would produce a positive result in anti-doping tests,"
said the Web site www.modafinil.info.
White was not the only American athlete at the championships who came under
scrutiny for drugs.
The Los Angeles Times reported that 400-meter champion Jerome Young tested
positive for steroids in 1999, but was cleared on appeal by U.S. officials and
allowed to compete in the 2000 Sydney Olympics, where he won gold as a member of
the 4x400-meter relay team.
World Anti-Doping Agency chief Dick Pound has called for the U.S. team to be
stripped of the medal.
Young won his second gold medal of the championships Sunday night, anchoring the
4x400-meter relay team to victory in the final event of the meet.
"I just didn't worry about it," Young said of the doping allegations. "I just
put it behind me and kept on going, and just basically used that as a motivation
for me."
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801 of 998 DOCUMENTS
Associated Press Online
August 31, 2003 Sunday
IAAF: White Tested Negative After Medal
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 621 words
DATELINE: SAINT-DENIS, France
Kelli White passed a drug test after winning the 200 meters but still could lose
her two gold medals from the World Championships, track officials said Sunday.
The results from the second test were revealed one day after officials from the
International Association of Athletics Federations said White had tested
positive following her victory in the 100.
White won gold in the 100 a week ago and completed the sprint double in the 200
on Thursday, becoming the first American woman to sweep both events at a world
championships.
Even though White tested clean after the 200, the IAAF said her positive test
after the 100 would be enough to cost her both medals.
"It would be wrong to say, 'You are doping on Sunday, and you're out,' and then
say, 'You can win the same medal Thursday at the same championships,"' Istvan
Gyulai, general secretary of the IAAF, said Sunday. "I believe this is an
important moral message."
The IAAF said Saturday that White risked being stripped of all her championship
results if found guilty of a doping offense. She also could face a two-year
suspension that would rule her out of the 2004 Athens Olympics.
Gyulai said the IAAF was continuing to investigate the exact nature of modafinil
, a prescription medication which White said she used for a sleep disorder.
While not specified by name on the banned list, modafinil is covered under the
stimulants category of "related substances," the IAAF said.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a warning. For harder stimulants, such as amphetamines, the
sanction is disqualification and a two-year ban.
Gyulai said the IAAF is trying to determine how to classify modafinil. He said
that could take four or five days.
After that, Gyulai said, the IAAF could: accept White's explanation and consider
clearing her on grounds; disqualify her and give her a warning; or, disqualify
her and recommend a two-year ban.
If the IAAF decides modafinil falls into the strong category, White would be
suspended pending a hearing by USA Track & Field, Gyulai said. Her case would
then be handled by the U.S. Anti-Doping Agency, and could potentially end up
before the Court of Arbitration for Sport - a process that could take months.
The IAAF needs to clarify White's status soon because she is scheduled to run
Friday at the Golden League meet in Brussels. She also plans to compete in the
Grand Prix final in Monaco on Sept. 13-14 and an invitational meet in Moscow on
Sept. 20.
USA Track & Field chief executive Craig Masback said he had only been notified
of White's test result from the 100, and can't take action until getting more
details from the IAAF.
At a news conference Saturday, White acknowledged taking modafinil the morning
of the 100 final. But she denied ever taking a substance to enhance her
performance, saying she took the medication to treat narcolepsy and had no idea
it contained a banned substance.
White said she didn't apply for a medical waiver or include the medication on
her doping control form as required because it wasn't named on the prohibited
drug list. She said she and her doctor did extensive research on modafinil
before deciding to use it for narcolepsy, which causes sudden fatigue or
sleepiness.
If White loses the medals, she would be the biggest track name stripped of gold
at a major championship since Ben Johnson at the 1988 Seoul Olympics.
"She was the star of the championships, and now she's at the center of a doping
case," former Olympic and world champion Michael Johnson wrote in his daily
column in the French sports daily L'Equipe. "It creates trouble for our sport.
It's a big cloud over these championships."
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Contra Costa Times
August 31, 2003 Sunday FINAL EDITION
WHITE FAILS DRUG TEST;
A DOPING VIOLATION COULD ERASE THE SPRINTER'S GOLDS AND HER PLACE IN ATHENS
BYLINE: ANN TATKO, TIMES STAFF WRITER
SECTION: SPORTS; Pg. B01
LENGTH: 721 words
Sprinter Kelli White denied knowingly taking a drug that may cost her both of
her world championship gold medals and a chance to compete at next summer's
Olympics.
The International Association of Athletics Federation revealed Saturday that
White, a former resident of El Sobrante, had tested positive for the stimulant
modafinil after winning the 100-meter world title last Sunday. Results of her
drug test from Thursday's win in the 200 are not yet known.
Modafinil is a drug that stimulates the nervous system and helps relieve fatigue
and excessive daytime sleepiness. Although not listed on the IAAF's banned
substance list, modafinil is classified as a "related compound," which means
athletes may be at risk of a doping violation if they take it.
"I know that I did nothing wrong and sought no advantage over my competitors,"
White said, reading a statement at a press conference in Saint-Denis, France,
site of the World Track and Field Championships. "I am confident that things
will work out in the end."
White said her doctor, Brian Goldman, prescribed Provigil, which contains
modafinil, because of a sleeping disorder that runs in her family.
An IAAF spokesman said the federation has handed the possible doping violation
over to USA Track and Field, which now must hold a hearing and determine what,
if any, disciplinary action should be taken.
Although the investigation continues, IAAF officials said that early findings
indicate White likely will lose the gold medals she won in the 100 and 200. The
bigger question is whether the investigation ends with a suspension, as well.
The IAAF must decide if modafinil is a "strong" or "light" stimulant. While both
result in disqualification, a light stimulant carries only a public warning,
whereas a strong stimulant results in a two-year suspension from competition.
White said she has taken the drug throughout the season, passing drug tests at
the U.S. championships at Stanford and international meets in Europe. For that
reason, she said, she didn't seek a medical waiver or list the drug on doping
control forms.
"Given that it was not on the banned list, I think it is understandable why I
didn't realize that I needed to declare it," she said.
That assumption may hurt White's chances of avoiding disciplinary action, said
IAAF vice president Arne Ljungqvist, the federation's anti-doping chief.
"She did declare other supplements she was taking, but not this particular one,"
Ljungqvist told The Associated Press. "She should have done it. Even more, she
should have asked for a prior exemption to use it. That is, of course, a problem
for her when her case will later be evaluated."
White's agent, Robert Wagner, said by phone that White may provide her medical
records to investigators to prove the medicine was prescribed.
"This is an unfortunate situation of unwittingly taking something that perhaps
she shouldn't have," he said. "Even more unfortunate, it happens for a lot of
athletes because of the complexities of what is or is not a (banned substance)."
White encountered another possible doping violation last July when meet doctors
at a competition in Saint-Denis gave her medication for a foot injury. The
medicine contained corticoid, an anti-inflammatory steroid. She received a
six-month ban from competition in France but was cleared by the IAAF.
The latest allegation of doping, however, appears more serious.
Ljungqvist said he knows of at least three past cases in which athletes used
modafinil for performance-enhancing reasons.
White said she was upset by the suggestion that she is another one of those
athletes.
"The mere fact of this allegation is personally harmful and hurtful," she said.
"I have never taken any substance to enhance my performance."
The allegation prompted White to withdraw Saturday from the U.S. women's 400
relay team, which went on to place second behind France. IAAF officials didn't
prohibit her from competing but did note that disciplinary action resulting in
disqualification could extend to the relay, too.
In addition to disqualification and suspension, White also could lose $120,000
in prize money.
IAAF officials said they expect a ruling from the USA Track and Field hearing
later this week.
The Associated Press contributed to this story.
LOAD-DATE: November 10, 2005
LANGUAGE: ENGLISH
GRAPHIC: Photo 1, KELLI WHITE'S Olympic future may hinge on the strength of a
stimulant in her sleep medication. (MICHEL EULER, AP); Photo 2, Kelli White.
(Rusty Kennedy, AP)
Copyright 2003 Contra Costa Times
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803 of 998 DOCUMENTS
The New York Times
August 31, 2003 Sunday
Late Edition - Final
TRACK AND FIELD;
U.S. Sprinter Tests Positive For Stimulant
BYLINE: By JERE LONGMAN
SECTION: Section 8; Column 5; Sports Desk; Pg. 1
LENGTH: 1000 words
DATELINE: PARIS, Aug. 30
Kelli White of the United States, the women's champion at 100 and 200 meters at
the world track and field championships, has tested positive for a stimulant,
and that could cost her the gold medals she won here and could prevent her from
competing in the 2004 Olympics in Athens, the sport's world governing body said
today.
According to the International Association of Athletics Federations, the
governing body, a urine sample provided by White showed the presence of the
stimulant modafinil, which is used to treat narcolepsy, after she won the 100
meters in 10.85 seconds, her best time, last Sunday. No action has been taken
against her while the case remains under review.
White was cleared to run the 4x100 relay today, but she did not participate,
apparently not wanting to risk disqualification of the entire team. Without
White, the United States finished second to France.
Allen Johnson of the United States won his fourth world championship in the 110
hurdles, taking the gold medal in 13.12 seconds, but his victory was
overshadowed by the potential disruption of White's career just when it seemed
to reach its apex. She ran faster in the 100 and 200 here than she ever had.
Her case is complicated, and no doping offense has been officially declared. But
the I.A.A.F. made it clear that White would have a difficult time successfully
defending her use of the stimulant and avoiding a penalty.
Possible sanctions range from a warning, which would still result in
disqualification from these championships and the loss of her gold medals, to a
two-year suspension, which would bar her from competing in the 2004 Olympics.
She also stands to lose $120,000 in prize money for her victories here.
Modafinil, a prescription drug sold under the brand name Provigil in the United
States, is a memory-improving and mood-brightening substance used to combat
extreme sleepiness in people with narcolepsy.
White, who is 26 and lives in Union City, Calif., said at a news conference that
she had been taking the substance for several months to treat the symptoms of
narcolepsy, which included constant fatigue and restlessness at night because
she fell asleep during the daytime.
"I wanted to feel normal," White said.
Several members of her family have been under a doctor's care for narcolepsy for
years, White said. She said she had been prescribed Provigil by a San
Francisco-area doctor named Brian Goldman. A doctor by that name who advises
professional and Olympic athletes in the Bay Area was located on a Web site, but
he could not be reached for comment.
"The mere fact of this allegation is personally harmful and hurtful," White
said. "I have never taken any substance to enhance my performance."
Modafinil has not been placed by name on the list of banned
performance-enhancing substances considered by the International Olympic
Committee and the World Anti-Doping Agency.
But modafinil is considered a related substance, meaning that athletes use it at
the risk of being found guilty of doping. The European Council has asked that
modafinil be listed by name as a banned substance beginning next year.
White said she did not notify the I.A.A.F. on a doping control form that she was
using modafinil, believing it was unnecessary because the stimulant is not
listed as a prohibited substance. She said she took the stimulant only on an
as-needed basis and had not tested positive at previous meets this summer, so
she expected no problems at the world championships.
She said she contacted both the I.A.A.F. and the United States Anti-Doping
Agency while doing extensive research about the drug and found no evidence that
it was prohibited. It was unclear whether the contact was person-to-person or by
computer.
Arne Ljungqvist of Sweden, a doctor who is a top medical official in both the
I.A.A.F. and the International Olympic Committee, noted that athletes were
required to list all medications they were taking. White did list supplements
that she was using, he said.
It is possible that even if White had a legitimate medical reason to use
modafinil, she could lose her medals or her Olympic eligibility because she did
not provide the I.A.A.F. with sufficient notice of her usage or receive a
special waiver.
"She should have done it," Ljungqvist said of the notification. "Even more, she
should have asked for a prior exemption to use it. That is a problem for her
when her case will later be evaluated."
An Internet search of modafinil today turned up a prescription medication Web
site that warned: "Athletes should be aware that one of the main ingredients of
this product would produce a positive result in anti-doping tests."
Mark Gay, the general counsel of the I.A.A.F., said the track body would
investigate whether White indeed did have a doctor's prescription to use the
stimulant. Before any penalty can be assessed, the I.A.A.F. must also decide
what class of stimulants modafinil belongs to.
If modafinil is declared to be in the same performance-enhancing class as
amphetamines, White faces a two-year ban, Ljungqvist said. If modafinil is
considered in a class of lesser stimulants like ephedrine, White would face a
warning and disqualification from the world championships, he said.
The International Tennis Federation classifies modafinil as a Class 2, or
lesser, prohibited substance. A first-time offense carries a three-month ban
from competition.
"We need to have this exactly clarified because we cannot jump to a wrong
judgment in such a situation," Ljungqvist said of the I.A.A.F.
Today was not White's first brush with a doping controversy. Last summer, she
tested positive for a corticosteroid at a meet in Paris and was later prohibited
from competing in France, which has strict drug laws, for six months, Reuters
reported. The ban ended in June.
A track official from the United States said that the corticosteroid was
contained in a topical cream White used to treat a foot problem. She was not
prevented from competing elsewhere, including the United States.
URL: http://www.nytimes.com
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photos: Kelli White, 26, of Union City, Calif. (Photo by Reuters)(pg.
1); Kelli White, the world champion in the 100 and 200, said she took modafinil
to treat the symptoms of narcolepsy. (Photo by Associated Press)(pg. 8)
PUBLICATION-TYPE: Newspaper
Copyright 2003 The New York Times Company
804 of 998 DOCUMENTS
The Observer
August 31, 2003
ATHLETICS: WORLD CHAMPIONSHIPS: White tests positive for stimulant
BYLINE: PETER NICHOLS IN PARIS
SECTION: Observer Sport Pages, Pg. 12
LENGTH: 495 words
KELLI WHITE, THE American sprinter who has been one of the revelations of these
championships, winning the double of 100 metres and 200 metres, has tested
positive for a stimulant, Modafinil.
In a statement issued by the sport's governing body, the IAAF, it stated that
White had claimed that she was taking the drug 'on prescription for a medical
condition', but her failure to ask for a prior exemption makes it likely that
she will lose both titles.
The test was taken after White's victory in the 100m final last Sunday and the
positive result was known on Wednesday. The news was not released by the IAAF,
but was revealed in yesterday's L'Equipe newspaper, the French sports daily.
The sample after Thursday's 200m final has not yet been analysed, but Arne
Ljungqvist, chairman of the IAAF medical commission, felt that it could also
yield a positive for the drug. 'It has a fairly short half-life of 10 to 12
hours, but it breaks down quite slowly,' said Ljungqvist.
But even if that sample were clean, White would still stand to lose both titles.
'An athlete is banned not from the event, but from the competition,' said
Ljungqvist.
Modafinil is a drug used in the treatment of narcolepsy (or sleeping sickness),
but has also been noted as a performance enhancer, including in rally-driving,
where its ability to stimulate the brain keeps the drivers alert.
The drug is not yet named in either the IAAF banned list nor that of the World
Anti-Doping Agency (Wada), but Ljungqvist was in no doubt that it would fall
into the 'related compounds' category. 'We have also made a request for
Modafinil to be named in the list for Wada,' said Ljungqvist.
As Modafinil is not pharmacologically related to amphetamines, White could
escape a two-year suspension, but she could still lose her titles, to her
team-mate Torri Edwards in the 100m and the Russian Anastasiya Kapachinskaya in
the 200m.
L'Equipe also revealed that White had previously tested positive for a
corticosteroid called triamcinolone acetonide at the Golden League meeting in
the same stadium a year ago. On that occasion, the IAAF did not consider it to
be a doping offence, but the CPLD (Le Conseil de Prevention et de Lutte contre
le Dopage in France, which polices drug use in sport), imposed a six-month ban
on White from competing in the country, as the American did not have a valid
prescription for the drug.
Once the IAAF investigation is concluded for this positive, it is down to the US
governing body (USTAF) to determine what action should be taken against the
sprinter. 'If we don't agree with what they do, we have the option to take the
case to CAS (the court of arbitration for sport),' said Ljungqvist.
The USTAF have a reputation for failing to censor their own athletes. Only four
days ago, it was revealed that 400m winner Jerome Young had tested positive in
1999, but was cleared by USTAF and allowed to compete in the Sydney Olympics.
LOAD-DATE: September 3, 2003
LANGUAGE: ENGLISH
PUB-TYPE: PAPER
Copyright 2003 Guardian Newspapers Limited
805 of 998 DOCUMENTS
St. Louis Post-Dispatch (Missouri)
August 31, 2003 Sunday Five Star Edition
SPORTS DIGEST
SECTION: SPORTS; Sports Digest Column; Pg. C7
LENGTH: 499 words
TRACK AND FIELD
American sprinter flunks drug test
Kelli White provided some of the rare highlights for an underachieving U.S. team
at the World Championships - until she flunked a drug test, putting her two
sprint gold medals at risk and depriving a favored American relay team of its
anchor.
Track's world governing body is investigating a sample from White, the only
American woman to win an event at the World Championships in Saint-Denis, France
and the only U.S. woman to win both the 100 and 200 meters at a world meet.
Now, her sprint crowns are in jeopardy. And, after White's withdrawal, the U.S.
400-meter relay team lost to France on Saturday night.
L'Equipe, a Paris sports daily, reported Saturday morning that White - the first
U.S. woman to sweep the sprints at the worlds - had tested positive for a
stimulant she later said she uses for a sleeping disorder. The IAAF later
confirmed it.
White denied ever taking drugs to enhance her performance.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," she said.
White's positive test for the stimulant modafinil came after her win Monday in
the 100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. White said that she was prescribed modafinil for narcolepsy earlier
this year, and that she and close members of her family have been diagnosed with
the disorder.
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
BOXING
Klitschko wins
Wladimir Klitschko (41-2) stopped Fabio Moli (29-3) just 97 seconds into the
first round of a heavyweight fight in Munich, Germany.
NFL
Boller tabbed to start for Ravens
Kyle Boller will start at quarterback when the Baltimore Ravens open the NFL
regular season in Pittsburgh next Sunday, winning the job from incumbent Chris
Redman.
"The physical skills are obvious; anyone that's seen the kid - even in a
practice - can recognize that," Ravens coach Brian Billick said "But his ability
to absorb the offense has been shocking to me, and I've been doing this for a
while."
* In a move that was a bit surprising, the Redskins cut former Florida
quarterback Danny Wuerffel and Gibran Hamdan, which means coach Steve Spurrier
will start the season with just Patrick Ramsey and Rob Johnson available at
quarterback.
HORSE RACING
Trotting Derby is rained out
The World Trotting Derby in Du Quoin, Ill. was rained out. Mutineer had been the
favorite to take the $550,000 event. The race was not rescheduled. The entry
fees and stakes payments totaling about $35,000 per horse were to be split by
Mutineer and the six other entrants.
LOAD-DATE: August 31, 2003
LANGUAGE: English
Copyright 2003 St. Louis Post-Dispatch, Inc.
806 of 998 DOCUMENTS
Sunday Life
August 31, 2003
Athletics: White under drugs cloud
LENGTH: 199 words
KELLI White is under threat of losing her World Championship gold medals in the
100 metres and 200m after testing positive for modafinil.
Only mitigating circumstances that the American took the medication for health
reasons, it seems, will prevent her from being punished.
White has claimed she was prescribed the substance as treatment for a medical
condition which runs in her family.
IAAF senior vice-president Dr Arne Ljungqvist says that track and field's world
governing body is not certain which family of drugs modafinil falls into.
If modafinil is categorised as ephedrine, it would be classed as a minor offence
and the American would lose her gold medals.
Should it fall into the more serious category of being an amphetamine, White
would most likely pay the ultimate penalty and receive a two-year suspension.
"It needs to be clarified where it belongs," said Ljungqvist, chairman of the
IAAF's medical commission.
The Swede added: "Modafinil is used as a medication for disorders related to
sudden loss of consciousness, and awareness and (when) you fall asleep.
"It's a known disorder which requires some sort of stimulant to keep you awake."
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LANGUAGE: ENGLISH
Copyright 2003 Belfast Telegraph Newspapers
807 of 998 DOCUMENTS
The Sunday Herald
August 31, 2003
American sprint champion White fails drug test in Paris
BYLINE: By Natasha Woods In Paris
SECTION: Pg. 1
LENGTH: 576 words
KELLI White, the biggest track star to emerge from the IAAF World Championships,
was at the centre of a doping scandal last night after it emerged she tested
positive for a stimulant after winning the 100m in Paris.
The American, who set personal bests when taking both the 100m and 200m titles,
now faces the possibility of being stripped of two gold medals. She could also
be given a two-year ban from the sport if investigations by the IAAF classify
the prescription drug she took as a 'heavy stimulant'.
White, who has inherited Marion Jones' mantle as the Queen of world sprinting,
claims the traces of modafinil found relate to a drug she takes to treat
narcolepsy, a medical condition which runs in her family.
"I have never taken any substance to enhance my performance," she said last
night. "This allegation is personally harmful and hurtful. I know I am innocent.
I worked hard for the medals I earned this week and I'm going to work very hard
to keep them."
White, who says she had been taking modafinil for three months to combat
tiredness and memory problems, failed to declare she was taking the medicine on
official forms or ask for a prior exemption to use it; both breaches of the
governing body's rules.
"That will be a problem for her when her case is later evaluated," said
Professor Arne Ljungqvist, the IAAF's senior vice-president.
Modafinil, as White rightly pointed out, is not specifically named as a banned
substance under IOC rules. But it is classed as a "related substance" which
carries the same penalties.
"The IAAF classify substances into two groups - heavy stimulants and light. It
remains to be clarified exactly where this belongs because classification
results in different sorts of punishments," explained Ljungqvist.
A light stimulant brings a public warning and disqualification from the event in
which the doping offence happened; a strong stimulant and a two-year ban is
added to the punitive measures. Therefore it's likely she will lose her medals
at least, although last summer Commonwealth Games and now world 100m champion
Kim Collins was only given a warning when he failed to declare his asthma
medication.
White was cleared to run in the final of the 4x100m relay last night as the IAAF
continue their investigations, but she withdrew.
"I don't understand, I've been on this medication for months and I've had a few
drugs tests and they have been fine, so I didn't think it would be a problem
here," she added.
It remains crass naivety that she wouldn't record it on her doping control forms
here in Paris. And there are further suspicions. Modafinil may be used to treat
disorders where concentration, awareness and consciousness are affected, but the
IAAF are investigating whether it has performance-enhancing properties.
"Modafinil has been observed as a possible substance for the purpose of
performance enhancement as a stimulant. There is an awareness around that it may
be used as a doping substance by those wanting to take that chance," said
Ljungqvist.
Once the IAAF reach their decision as to whether a doping offence has occurred
it will then be up the US track and field authorities to take action. Given the
USATF's record on doping - they failed to report 13 positive tests before the
Sydney Olympics - the IAAF reserve the right to take the case to the Court of
Arbitration in Sport if they are not satisfied with the American's action.
LOAD-DATE: September 02, 2003
LANGUAGE: English
PUB-TYPE: Paper
Copyright 2003 Scottish Media Newspapers Limited
808 of 998 DOCUMENTS
Sunday Express
August 31, 2003
DRUGS SHAME THREATENS KELLI
BYLINE: By John Wragg
SECTION: SPORT; Pg. 94
LENGTH: 193 words
WORLD champion Kelli White faces being stripped of her two sprint gold medals
after the American team were caught in another drugs sensation.
White, 25, tested positive for Modafinil after winning the 100m and the findings
of the sample she provided after her 200m win on Thursday have yet to be
announced.
She told the IAAF, athletics' world governing body, that she had taken the drug
on prescription for a medical condition that runs in the family.
But she did not disclose what she was taking before the competition, which is
against IAAF rules.
Dr Arne Ljungqvist, head of drug testing, confirmed that Modafinil is not on the
banned list but is related to substances regarded as illegal.
There is also a move to put Modafinil, which is used to avoid sleepiness and
boost concentrtaion, on the banned list for the Athens Olympics next year.
The trouble for White, who escaped another ban in France at a Golden League
meeting when she claimed she was only taking painkillers, follows the disclosure
that another American, Jerome Young, who won the 400m, was the USA athlete
believed to have taken drugs at the Sydney Olympics.
LOAD-DATE: September 1, 2003
LANGUAGE: English
PUB-TYPE: Newspaper
Copyright 2003 EXPRESS NEWSPAPERS
809 of 998 DOCUMENTS
Sunday Tribune
August 31, 2003
White may lose medals after failing drugs test;
ATHLETICS NEWS
SECTION: Pg. 1
LENGTH: 143 words
KELLI WHITE is under threat of losing her World Championship gold medals in the
100 and 200 metres after testing positive for modafinil. Only mitigating
circumstances that the American sprinter took the medication for health reasons,
it seems, will prevent her from being punished.
White has claimed she was prescribed the substance as treatment for a medical
condition which runs in her family.
IAAF senior vice-president Dr Arne Ljungqvist says that track and field's world
governing body is not certain which family of drugs modafinil falls into.
If modafinil is categorised as ephedrine, it would be classed as a minor offence
and the American would lose her gold medals.
Should it fall into the more serious category of being an amphetamine, White
would most likely pay the ultimate penalty and receive a two-year suspension.
LOAD-DATE: March 1, 2004
LANGUAGE: ENGLISH
Copyright 2003 The Sunday Tribune plc
810 of 998 DOCUMENTS
The Times Union (Albany, NY)
August 31, 2003 Sunday THREE STAR EDITION
White's medals at risk
BYLINE: Combined Wire Services
SECTION: SPORTS, Pg. C2
LENGTH: 506 words
DATELINE: SAINT-DENIS, France
Kelli White provided some rare highlights for an underachieving U.S. team at the
World Championships -- until she flunked a drug test, putting her two gold
medals at risk and depriving a favored American relay team of its anchor.
Track's world governing body is investigating a sample from White, the only
American woman to win an event at these World Championships and the only U.S.
woman to win both the 100 and 200 meters at a world meet.
After White's withdrawal, the U.S. 400-meter relay team lost to France on
Saturday night.
White said her positive drug test stemmed from prescription medicine for a sleep
disorder.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," she said. "I
have never taken any substance to enhance my performance."
White's positive test for the stimulant modafinil came after her win Monday in
the 100.
Modafinil is used to fight fatigue and sleepiness. White said she was prescribed
modafinil for narcolepsy earlier this year and that she and close members of her
family have been diagnosed with the disorder.
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China won the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber of France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters. HOCKEY Defenseman Oleg Tverdovsky is returning to Russia after
playing last season for the New Jersey Devils. He signed a two-year contract
with Avangard of the Super League.
Tverdovsky, 27, was traded to the Devils last season. He had an erratic season
that was limited by a head injury. He played 50 games and had five goals and
eight assists. UNIVERSITY GAMES Olympic and world champion swimmer Yana
Klochkova of Ukraine won her fourth gold medal and China captured 13 finals to
ensure its top spot in the standings at the World University Games in Daegu,
South Korea.
The United States, without any representatives in men's basketball or track and
field, will finish with its fewest medals at a University Games since 1989, when
it had 26 from four sports.
The United States has five golds, 13 silvers and 16 bronzes from nine sports and
the prospect of only one more medal from today's bronze-medal volleyball game
with France on the competition's final day. ROWING The United States won
gold medals Saturday in the women's coxless four and men's coxed pairs, both
non-Olympic events, at the World Rowing Championships in Milan, Italy. The
one-week competition ends today, highlighted by the men's and women's eights.
BOXING Wladimir Klitschko stopped Fabio Moli just 97 seconds into the first
round of a heavyweight fight in Munich, Germany. Klitschko (41-2) threw a left
that Moli (29-3) ducked into.
LOAD-DATE: September 3, 2003
LANGUAGE: ENGLISH
Copyright 2003 The Hearst Corporation
811 of 998 DOCUMENTS
The Washington Post
August 31, 2003 Sunday
Final Edition
What Is Modafinil?
SECTION: SPORTS; Pg. E04
LENGTH: 80 words
Modafinil is a memory-improving and mood-brightening psychostimulant. It
enhances wakefulness but is less likely than other stimulants to cause
jitteriness and anxiety.
Modafinil has been proved clinically useful in treating narcolepsy, a
neurological disorder marked by uncontrollable attacks of daytime sleepiness.
Modafinil is banned by the International Tennis Federation and carries a
three-month suspension for first-time offenders.
-- From News Services, Staff Reports
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
812 of 998 DOCUMENTS
The Washington Post
August 31, 2003 Sunday
Final Edition
Double Gold Medalist Tests Positive;
U.S. Sprinter White Says She Used Stimulant to Deal With Narcolepsy
BYLINE: Amy Shipley, Washington Post Staff Writer
SECTION: SPORTS; Pg. E01
LENGTH: 840 words
DATELINE: SAINT-DENIS, France Aug. 30
-- U.S. sprinter Kelli White might have to give up the two gold medals she won
here at the ninth World Track and Field Championships because a drug test taken
a week ago, after her victory in the 100 meters, showed the presence of a
stimulant known as modafinil.
Although modafinil is not on the Olympic movement's banned list, it could
trigger punitive action under an often-used clause in the rules that prohibits
substances related to banned drugs. Citing that clause, the IAAF -- track and
field's world governing body -- could disqualify White and rescind her gold
medals in the 100 and 200.
White's status for the 2004 Athens Olympics could be in jeopardy as well.
Depending on the nature of the stimulant, which IAAF officials say will be
determined in the coming weeks, White could face a two-year competition ban.
White today acknowledged taking the drug but denied using it for a competitive
advantage. She said her physician diagnosed narcolepsy "a few months ago" and
prescribed modafinil on an "as needed basis." She said she had taken the drug "a
few times" throughout the track season, including the morning of the 100 final.
She said other family members have been treated for narcolepsy but declined to
elaborate.
"I have never taken any substance to enhance my performance," White said,
reading from a statement. ". . . Because I know that I did nothing wrong and
sought no advantage over my competitors, I am confident that things will work
out in the end."
Though her case could take weeks to resolve, today's news was a severe blow to
White, who had emerged this season as a fierce and legitimate rival to five-time
Olympic medalist Marion Jones.
White voluntarily withdrew from tonight's 4x100 relay final, a move that likely
cost the United States the gold medal. In a major upset, Americans Angela
Williams, Chryste Gaines, Inger Miller and Torri Edwards finished second to
France. However, if White had competed and later was disqualified from the meet,
the relay team's results would have been nullified.
White said her physician, Brian Goldman of San Francisco, recently prescribed
for her the brand-name drug Provigil, which contains modafinil, at her request.
She said she asked about the substance because she was having trouble sleeping
at night, was tired all of the time and was suffering from memory loss.
"This year, I did contact my doctor about it," she said. "The reason I started
taking the medication is I wanted to feel normal. I wanted to have a regular
season this year, so I wanted to take the medication."
White said she did not declare the drug on her testing disclosure form because
she knew it was not on the banned list. She said she researched it extensively,
contacting both the U.S. Anti-Doping Agency and IAAF.
White had a drug-testing problem in France last year. At a grand prix meet in
Paris, she tested positive for corticosteroids -- commonly used painkillers that
are banned in France, but not banned by any bodies in the Olympic movement.
Though she received no penalty from any sports body, she was banned from
competition in France for six months.
Despite her troubles then, she said it did not occur to her to declare the
substance on the disclosure form, though she said she listed a number of other
substances she was taking. She also said that she occasionally forgets to
mention a substance that she takes very early in the day.
"I've been on the medication for months now," she said. "I have had a few drug
tests. They were fine. I never thought it would be a problem now."
IAAF medical chief Arne Ljungqvist said athletes are required to declare any
substances, medications or supplements they use on their drug disclosure forms.
White's case will go to USA Track and Field, which will hold a hearing and
recommend action. The IAAF, however, has ultimate jurisdiction and can impose
the penalty it chooses.
"We haven't yet found whether her explanation holds water," IAAF attorney Mark
Gay said. "It may or may not. We have to establish the facts."
Ljungqvist said White's test results from Thursday's 200 final were not yet
available.
In recent years, the IAAF and other Olympic bodies have become reluctant to
accept any excuses from athletes for drug violations of any kind. At the 2002
Winter Games in Salt Lake City, several cross-country skiers were banned for
using a substance that was not mentioned on the International Olympic
Committee's prohibited list, but that was determined to be similar to the banned
endurance-enhancing drug erythropoietin (EPO).
Ljungqvist said that if modafinil is found to be related to amphetamines, a
strong class of stimulants, White would face a possible two-year ban. If the
substance is found to be related to ephedrine, a less potent stimulant, she
would face a possible public warning, but she still would be disqualified from
this meet and forced to give up her medals.
"We need more information in this case," Ljungqvist said. "We need to know
exactly how to classify the substance. We need to evaluate her own statement."
LOAD-DATE: August 31, 2003
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PUBLICATION-TYPE: Newspaper
Copyright 2003 The Washington Post
813 of 998 DOCUMENTS
XINHUA GENERAL NEWS SERVICE
August 31, 2003, Sunday
Kelli White in trouble for taking upcoming-banned stimulant
SECTION: WORLD NEWS; SPORTS
LENGTH: 230 words
PARIS, Aug. 30 (Xinhua) -- Modafinil, a medical substance which can prevent a
person from sleepiness but will be banned for athletes from Athens Olympics, put
American female star sprinter Kelli White in trouble on Saturday.
A sample provided by White, who had been crowned in women's 100m and 200m races
at the ninth athletic worlds, tested positive for Modafinil, an IAAF statement
said here.
Modafinil can be easily got from pharmacy on prescription in the United States.
A substance similar to Modafinil had been banned for athletes years ago but was
ticked off from the list later.
The statement said, "Today we have received an explanation from the athlete to
the following effect; Ms White has been taking the substance on prescription to
treat a medical condition that runs in her family."
As both the nature of the substance and the content of her explanation require
further inquiry and investigation, the IAAF has taken the view that bearing in
mind the very serious consequences for the athlete of being suspended and being
removed form competition at this late stage, the most appropriate course of
action is to allow her to compete pending the completion of the necessary
scientific and factual investigations.
So far, the IAAF has not yet received the results of the analysis on her sample
provided after the 200m final.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
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XINHUA GENERAL NEWS SERVICE
August 31, 2003, Sunday
Modafinil not on ban list, I am innocent: White
SECTION: WORLD NEWS; SPORTS
LENGTH: 338 words
PARIS, Aug. 30 (Xinhua) -- Kelli White, the new American sprint queen who had
been crowned in 100m and 200m at the ninth athletics worlds but failing a doping
test later, said here Saturday that she was innocent as the medical substance
she took is not on the ban list.
Modafinil, a medical substance which can prevent a person from sleepiness but
will be banned for athletes at Athens Olympics, put White in trouble as it was
in a sample provided by White for doping test.
White, who was in black and without any smile on her face, told a press
conference that it was a big surprise for her when she got to know the news from
newspaper this morning.
She said she took the medicine on her personal doctor's prescription because she
wanted to be fine form and have a regular season.
Answering a question, White said," I do not take the medicine everyday." She
said she only took it for months and even before the 100m final in Paris but
nothing happened before.
Modafinil can be easily got from pharmacy on prescription in the United States.
A substance similar to Modafinil had been banned for athletes years ago but was
ticked off from the list later.
An IAAF statement issued today said, "We have received an explanation from the
athlete to the following effect; Ms White has been taking the substance on
prescription to treat a medical condition that runs in her family."
As both the nature of the substance and the content of her explanation require
further inquiry and investigation, the IAAF has taken the view that bearing in
mind the very serious consequences for the athlete of being suspended and being
removed form competition at this late stage, the most appropriate course of
action is to allow her to compete pending the completion of the necessary
scientific and factual investigations.
However, White did not appear on the track to compete for the 4x100m relay for
the American team, who had to settle in the second place in the final. The
French team took the gold.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
COPYRIGHT 2003 XINHUA NEWS AGENCY
815 of 998 DOCUMENTS
Yorkshire Post
August 31, 2003
Drugs test cloud over White's victories
SOURCE: Yorkshire Post
LENGTH: 415 words
Kelli White, who tested positive for a stimulant which is not listed by name as
a banned substance, insists she should be allowed to keep the gold medals which
she won in the 100m and 200m at the World Championships.
The American tested positive for modafinil after her 100m triumph last Sunday
and the IAAF have said that she may end up having to give back her medals - even
though the substance is not on their list of banned drugs.
The IAAF said it was covered under a clause for "related substances" and are
looking into whether modafinil may fall under the category of ephedrine, a minor
stimulant, or a strong stimulant like amphetamines.
If it is classified as the latter, White could be facing a ban as well as being
stripped of her medals.
White defended herself vigorously at a press conference in Paris on Saturday,
revealing that she takes the drug Provigil because she has narcolepsy. The drug
contains modafinil.
"I am under suspicion of a doping violation," said the 26-year-old White. "The
mere fact of this allegation is personally harmful and hurtful.
"Honestly, deep in my heart I know I'm innocent.
"I would take full responsibility but the medication is not on the banned list.
"I have never taken any substance to enhance my performance. Close members of my
family have been under doctors' care for the condition of narcolepsy for years.
"I, too, have been diagnosed with this condition by my physician, Dr Brian
Goldman. He prescribed the drug Provigil for this condition and I have taken it
in certain circumstances, including prior to the 100 metres".
Explaining why she had not declared it before the championships in accordance
with IAAF rules, White said: "I did not seek IAAF medical exemption for this
substance or note it on my doping control form, because I had no idea Provigil
contained a banned substance.
"Neither Provigil nor the substance in Provigil identified (modafinil acide) by
the IAAF, are on any lists of banned substances.
"I treat these matters very carefully. I have carefully and consistently noted
other substances used to treat injuries on my doping control form".
Hurdling great Colin Jackson has slammed drug testing procedures and believes
the lack of a clear worldwide directive and the grey area over which drugs are
legal or not is threatening to make a mockery of athletics.
He said: "What we're seeing now is a whole mess - it is not structured and that
is where the problem lies.
LOAD-DATE: June 25, 2004
Copyright 2003 Johnston Press Plc
816 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
SECTION: Sports News
LENGTH: 137 words
A brief explanation of the drug modafinil, for which double gold medalist Kelli
White tested positive at the track and field World Championships:
Modafinil is a memory-improving and mood-brightening psychostimulant. It
enhances wakefulness but is less likely than other stimulants to cause
jitteriness and anxiety.
Modafinil has been proved clinically useful in treating narcolepsy, a
neurological disorder marked by uncontrollable attacks of daytime sleepiness.
Narcolepsy affects more than 1 in 2,000 Americans. In some cases, patients
experience dreamlike hallucinations or become physically weak or paralyzed for a
few seconds.
Modafinil is marketed in the United States by Cephalon, Inc. as Provigil.
---
On the Net:
www.modafinil.com
www.provigil.com
www.cephalon.com
www.narcolepsy.com
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
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The Associated Press
August 30, 2003, Saturday, BC cycle
White scratched from 400-meter relay final
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 447 words
DATELINE: SAINT-DENIS, France
American sprinter Kelli White was scratched from the 400-meter relay final
Saturday as an investigation into a positive drug sample by the double world
champion jeopardized both her sprint gold medals.
Track's world governing body confirmed it is probing a sample from White, the
only American woman to win an event at these World Championships. She won the
100 on Sunday and became the first U.S. woman to complete a world sprint sweep
by capturing the 200 on Thursday.
White's positive drug test for the stimulant modafinil came after her win in the
100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy as well.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference that the IAAF is aware of other
cases is which modafinil has been used by athletes "for the purpose of
performance enhancement."
White could not immediately be reached for comment. USA Track and Field
officials had no comment.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a "strong"
stimulant, she also would face a two-year international ban.
Ljungqvist said he did not think the case would be resolved during the World
Championships, because it still must go through a USATF hearing.
Gyulai and Ljungvist said White told IAAF officials she has a doctor's
prescription for modafinil as a treatment for narcolepsy, a sleep disorder. She
told IAAF officials she has a history of narcolepsy in her family.
Athletes are required to declare the use of any drug for medical purposes, and
both Gyulai and Ljungqvist said White did not do that. Gyulai said she told
officials she did not see modafinil on the IAAF list of banned substances, so
she did not make a declaration.
Gyulai said it is not specifically listed as a banned drug, but is "covered by a
clause on related compounds."
"Of course it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2003 Associated Press
All Rights Reserved
818 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
White withdraws from relay final amid drug probe
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 522 words
DATELINE: SAINT-DENIS, France
Kelli White withdrew from the U.S. 400-meter relay team Saturday night as an
investigation into a positive drug test by the double world champion jeopardized
both her sprint gold medals.
Track's world governing body confirmed it is investigating a sample from White,
the only American woman to win an event at these World Championships. She won
the 100 on Sunday and became the first U.S. woman to complete a world sprint
sweep by capturing the 200 on Thursday.
On the track, Allen Johnson won his fourth world title in the 110-meter hurdles,
edging U.S. teammate Terrence Trammell by eight-hundredths of a second. Liu
Xiang of China took the bronze.
White's positive drug test for the stimulant modafinil came after her win in the
100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy as well.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference the IAAF is aware of other
cases is which modafinil has been used by athletes "for the purpose of
performance enhancement."
White could not immediately be reached for comment but set a news conference for
later in the evening. USA Track and Field officials had no comment.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a "strong"
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Ljungqvist said he did not think the case would be resolved during the World
Championships because it still must go through a USATF hearing.
Gyulai and Ljungqvist said White told IAAF officials she has a doctor's
prescription for modafinil as a treatment for narcolepsy, a sleep disorder. She
told IAAF officials she has a history of narcolepsy in her family.
Athletes are required to declare the use of any drug for medical purposes, and
Gyulai and Ljungqvist said White did not do that. Gyulai said she told officials
she did not see modafinil on the IAAF list of banned substances, so she did not
make a declaration.
Gyulai said it is not specifically listed as a banned drug but is "covered by a
clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
Other winners Saturday were Mirela Manjani of Greece in the women's javelin,
Jaouad Gharib of Morocco in the men's marathon and 18-year-old Tirunesh Dibaba
of Ethiopia in the women's 5,000 meters.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
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819 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
U.S. relay loses after Kelli White withdraws amid drug probe
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 613 words
DATELINE: SAINT-DENIS, France
The heavily favored U.S. 400-meter relay team lost to France on Saturday after
anchor and double world champion Kelli White withdrew because of a positive drug
test that jeopardizes both her sprint gold medals.
Track's world governing body said it is investigating a sample from White, the
only American woman to win an event at these World Championships. She won the
100 on Sunday and became the first U.S. woman to complete a world sprint sweep
by capturing the 200 on Thursday.
White's positive drug test for the stimulant modafinil came after her win in the
100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy as well.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference the IAAF is aware of other
cases is which modafinil has been used by athletes "for the purpose of
performance enhancement."
White could not immediately be reached for comment, but set a news conference
for later Saturday. USA Track and Field officials had no comment.
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Ljungqvist said he did not think the doping case involving White would be
resolved during the World Championships because it still must go through a USATF
hearing.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a "strong"
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Gyulai and Ljungqvist said White told IAAF officials she has a doctor's
prescription for modafinil as a treatment for narcolepsy, a sleep disorder. She
told IAAF officials she has a history of narcolepsy in her family.
Athletes are required to declare the use of any drug for medical purposes, and
Gyulai and Ljungqvist said White did not do that. Gyulai said she told officials
she did not see modafinil on the IAAF list of banned substances, so she did not
make a declaration.
Gyulai said it is not specifically listed as a banned drug but is "covered by a
clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
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All Rights Reserved
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The Associated Press
August 30, 2003, Saturday, BC cycle
White denies taking drugs to enhance performance
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 724 words
DATELINE: SAINT-DENIS, France
U.S. sprinter Kelli White said her positive drug test at the World Championships
stemmed from prescription medicine for a sleep disorder, and the double gold
medalist denied ever taking drugs to enhance her performance.
Track's world governing body is investigating a sample from White, whose gold
medals in the 100 and 200 meters are in jeopardy. She is the only American woman
to win an event at these World Championships.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," said White,
who withdrew from the U.S. 400-meter relay team. "The mere fact of this
allegation is personally harmful and hurtful. I have never taken any substance
to enhance my performance."
Without White, the heavily favored Americans lost to France in the relay final
on Saturday night.
White's positive drug test for the stimulant modafinil came after her win in the
100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference the IAAF is aware of other
cases is which modafinil has been used by athletes "for the purpose of
performance enhancement."
White said at a news conference Saturday night that she was prescribed modafinil
for narcolepsy, and that she and close members of her family have been diagnosed
with the condition. White, who was somber but composed during the news
conference, said she found out about the positive test by reading the French
sports daily L'Equipe.
White said she is confident she'll be able to keep her medals.
"Honestly, deep in my heart, I do believe so," she said. "I believe I'm
innocent, I know I'm innocent. I've worked very hard for the medals I earned
this week, and I'm going to work very hard to keep them."
Ljungqvist said he did not think the doping case involving White would be
resolved during the World Championships because it still must go through a USATF
hearing.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a "strong"
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Athletes are required to declare the use of any drug for medical purposes and
seek an exemption for its use, but White neither declared her use of modafinil
nor sought such an exemption. Since the drug is not on the IAAF's list of banned
substances, White said she saw no need to make sure a declaration.
Gyulai said modafinil is not specifically listed as a banned drug, but is
"covered by a clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2003 Associated Press
All Rights Reserved
821 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
American double gold medalist denies taking drugs to enhance performance
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: International News
LENGTH: 965 words
DATELINE: SAINT-DENIS, France
U.S. sprinter Kelli White said her positive drug test at the World Championships
stemmed from prescription medicine for a sleep disorder, and the double gold
medalist denied ever taking drugs to enhance her performance.
Track's world governing body is investigating a sample from White, whose gold
medals in the 100 and 200 meters are in jeopardy. She is the only American woman
to win an event at these World Championships, and the only U.S. woman to win
both sprints at a world meet.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," said White,
who withdrew from the U.S. 400-meter relay team. "The mere fact of this
allegation is personally harmful and hurtful. I have never taken any substance
to enhance my performance."
Without White, the heavily favored Americans lost to France in the relay final
on Saturday night.
White's positive test for the stimulant modafinil came after her win Monday in
the 100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference that the IAAF is aware of other
cases in which modafinil has been used by athletes "for the purpose of
performance enhancement."
White responded at her own news conference Saturday night, saying that she was
prescribed modafinil for narcolepsy earlier this year, and that she and close
members of her family have been diagnosed with the disorder. She said she went
to her doctor after feeling tired all the time and having trouble with her
memory.
White, who was somber but composed during the news conference, is confident
she'll be able to keep her medals.
"Honestly, deep in my heart, I do believe so," she said. "I believe I'm
innocent; I know I'm innocent. I've worked very hard for the medals I earned
this week, and I'm going to work very hard to keep them."
It's not the first time White has been involved in a disputed drug test in
France.
In July 2002, after running in a meet at Saint-Denis, White's sample turned up
traces of a corticoid - an anti-inflammatory steroid. She was suspended for six
months by France's anti-doping agency because she lacked a medical certificate,
but the IAAF cleared her.
And it was just the latest controversy for the U.S. team at the World
Championships.
The head of the World Anti-Doping Agency called for the U.S. 1,600-meter relay
team from the Sydney Olympics to return its medals after a report that Jerome
Young, a surprise winner here in the 400 meters, failed a drug test in 1999 but
was quietly cleared by U.S. officials and allowed to run in the 2000 Games.
Also, American sprinter Jon Drummond withdrew from the meet after a tantrum in
the men's 100 quarterfinals. Drummond threw a fit after being disqualified for a
false start.
Ljungqvist said he did not think White's doping case would be resolved during
the World Championships.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a stronger
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Athletes are required to declare the use of any drug for medical purposes and
seek an exemption for its use, but White neither declared her use of modafinil
nor sought such an exemption. Since the drug is not on the IAAF's list of banned
substances, White said she saw no need to make sure a declaration.
"The reason that I did not declare this on my doping control list is because I
do not take it every day. It is on an as-needed basis," she said. "Because I
took it so early in the day, I never thought to list it. After a competition,
it's kind of hard to remember everything you take during the day."
Gyulai said modafinil is not specifically listed as a banned drug, but is
"covered by a clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Arron said she was glad White withdrew from the race.
"It's good that White wasn't there," Arron said. "It would have shown a lack of
respect for us if she had run."
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
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LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2003 Associated Press
All Rights Reserved
822 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
Double gold medalist White denies taking drugs to enhance performance
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 1011 words
DATELINE: SAINT-DENIS, France
Kelli White provided some of the rare highlights for an underachieving U.S. team
at the World Championships - until she flunked a drug test, putting her two
sprint gold medals at risk and depriving a favored American relay team of its
anchor.
Track's world governing body is investigating a sample from White, the only
American woman to win an event at these World Championships and the only U.S.
woman to win both the 100 and 200 meters at a world meet.
Now, her sprint crowns are in jeopardy. And, after White's withdrawal, the U.S.
400-meter relay team lost to France on Saturday night.
It's just the latest controversy for the U.S. team at the World Championships.
American sprinter Jon Drummond withdrew from the meet after a tantrum in the
men's 100 quarterfinals. Drummond threw a fit after being disqualified for a
false start.
Then the head of the World Anti-Doping Agency called for the U.S. 1,600-meter
relay team from the Sydney Olympics to return its medals after a report that
Jerome Young, a surprise winner here in the 400 meters, failed a drug test in
1999 but was quietly cleared by U.S. officials and allowed to run in the 2000
Games.
There also have been plenty of disappointments on the track - including medal
shutouts in events Americans usually rule, such as the men's 100 and the women's
pole vault.
White said her positive drug test stemmed from prescription medicine for a sleep
disorder, and she denied ever taking drugs to enhance her performance.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," she said.
"The mere fact of this allegation is personally harmful and hurtful. I have
never taken any substance to enhance my performance."
White's positive test for the stimulant modafinil came after her win Monday in
the 100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference that the IAAF is aware of other
cases in which modafinil has been used by athletes "for the purpose of
performance enhancement."
White responded at her own news conference Saturday night, saying that she was
prescribed modafinil for narcolepsy earlier this year, and that she and close
members of her family have been diagnosed with the disorder. She said she went
to her doctor after feeling tired all the time and having trouble with her
memory.
White, who was somber but composed during the news conference, is confident
she'll be able to keep her medals.
"Honestly, deep in my heart, I do believe so," she said. "I believe I'm
innocent; I know I'm innocent. I've worked very hard for the medals I earned
this week, and I'm going to work very hard to keep them."
It's not the first time White has been involved in a disputed drug test in
France.
In July 2002, after running in a meet at Saint-Denis, White's sample turned up
traces of a corticoid - an anti-inflammatory steroid. She was suspended for six
months by France's anti-doping agency because she lacked a medical certificate,
but the IAAF cleared her.
Ljungqvist said he did not think White's doping case would be resolved during
the World Championships.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a stronger
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Athletes are required to declare the use of any drug for medical purposes and
seek an exemption for its use, but White neither declared her use of modafinil
nor sought such an exemption. Since the drug is not on the IAAF's list of banned
substances, White said she saw no need to make sure a declaration.
"The reason that I did not declare this on my doping control list is because I
do not take it every day. It is on an as-needed basis," she said. "Because I
took it so early in the day, I never thought to list it. After a competition,
it's kind of hard to remember everything you take during the day."
Gyulai said modafinil is not specifically listed as a banned drug, but is
"covered by a clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Arron said she was glad White withdrew from the race.
"It's good that White wasn't there," Arron said. "It would have shown a lack of
respect for us if she had run."
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
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LANGUAGE: ENGLISH
GRAPHIC: AP Photos
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All Rights Reserved
823 of 998 DOCUMENTS
The Associated Press
August 30, 2003, Saturday, BC cycle
White had 'no idea' medication included banned substance
BYLINE: By STEPHEN WILSON, AP Sports Writer
SECTION: Sports News
LENGTH: 719 words
DATELINE: SAINT-DENIS, France
Kelli White insists she did nothing wrong.
The American sprinter says she took medication only to treat a sleep disorder,
not to enhance her performance, and had no idea it contained a banned substance.
She says she didn't bother to apply for a medical waiver or include the
medication on her doping control form because it wasn't on the prohibited drug
list.
That was White's defense Saturday as she came under investigation for a positive
test that could cost her two gold medals from the World Championships.
"I have never taken any substance to enhance my performance," said White, who
pulled out of Saturday's 400-meter relay final. "Because I know that I did
nothing wrong and sought no advantage over my competitors, I am confident that
things will work out in the end."
Convincing world track officials of her innocence won't be easy - the rule book
and precedent aren't on her side.
The International Association of Athletics Federations said White risks being
stripped of her gold medals in the 100 and 200 meters after testing positive for
the stimulant modafinil. She also could face a two-year suspension.
Under the sport's strict policy, athletes are disqualified from an event if a
banned substance is found in their system - regardless of the circumstances.
In one of the most celebrated cases of its kind, Romanian teenage gymnast
Andreaa Raducan was stripped of the all-around gold medal at the 2000 Sydney
Olympics after testing positive for a stimulant contained in a cold pill.
Olympic officials acknowledged the measure was harsh but said they had to apply
the rules.
IAAF officials indicated the central issue in White's case was not so much
whether she should be disqualified and lose the medals but whether she also
should receive a warning or a two-year suspension.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
The IAAF said it was trying to determine the status of modafinil, which
stimulates the central nervous system. While not specified by name on the banned
list, modafinil is covered under the stimulants category of "related
substances," the IAAF said.
In recent years, athletes have been warned repeatedly to refrain from using
supplements or other substances that could trigger a positive test. They are
told to clear all medications with team doctors.
Under IAAF rules, athletes must notify the federation in advance of any products
they take for medical reasons. To apply for a medical waiver, athletes must
provide records proving they need to take a substance for therapeutic reasons.
But White insisted she didn't need to do that.
"Given that it (modafinil) was not on the banned list, I think it is
understandable why I didn't realize that I needed to declare it," White said.
"We thoroughly researched this," she added. "It wasn't on the banned list."
White said she was diagnosed with narcolepsy this year and began taking the drug
Provigil, which contains modafinil, a few months ago on the prescription of her
personal doctor, Brian Goldman.
"It has improved the condition in my day-to-day life and helped me function
normally," White said.
"I was extremely tired all the time, not sleeping well in the evening due to
sleeping in the daytime," White said. "My memory isn't very good. I needed just
to be right."
White said she had been taking the medication at the time of competitions in the
United States, London and Oslo, Norway, and passed all drug tests at the time.
"I never thought that this would be a problem now," she said.
White said she used the substance the morning of Sunday's 100-meter final. She
didn't say whether she also used the medication before Thursday's 200-meter
race.
Pressed on why she didn't list the substance on her forms, White said: "Because
it isn't a medication that I take every single day. It's on an as-needed basis,
and because I took it so early in the day I never thought to list it. After a
competition, it's kind of hard to remember everything you take during the day."
White tried to be philosophical.
"Things happen in life," she said, "and I will just have to deal with the
consequences."
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
824 of 998 DOCUMENTS
Associated Press Worldstream
August 30, 2003 Saturday
Fact box on drug at center of Kelli White case
BYLINE: The Associated Press
SECTION: SPORTS
LENGTH: 111 words
A brief explanation of the drug modafinil, for which double gold medalist Kelli
White tested positive at the World Championships:
Modafinil is a memory-improving and mood-brightening psychostimulant. It
enhances wakefulness but is less likely than other stimulants to cause
jitteriness and anxiety.
Modafinil has been proved clinically useful in treating narcolepsy, a
neurological disorder marked by uncontrollable attacks of daytime sleepiness. In
some cases, patients experience dreamlike hallucinations or become physically
weak or paralyzed for a few seconds.
On the Net:
www.modafinil.com
www.provigil.com
www.cephalon.com
www.narcolepsy.com
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
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All Rights Reserved
825 of 998 DOCUMENTS
Associated Press Worldstream
August 30, 2003 Saturday
White says she had 'no idea' medication included banned substance
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 717 words
DATELINE: SAINT-DENIS, France
Kelli White insists she did nothing wrong.
The American sprinter says she only took medication to treat a sleep disorder,
not to enhance her performance, and had no idea it contained a banned substance.
She says she didn't bother to apply for a medical waiver or include the
medication on her doping control form because it wasn't on the prohibited drug
list.
That was White's defense Saturday as she came under investigation for a positive
test that could cost her two gold medals from the World Championships.
"I have never taken any substance to enhance my performance," she said. "Because
I know that I did nothing wrong and sought no advantage over my competitors, I
am confident that things will work out in the end."
Convincing world track officials of her innocence won't be easy - the rule book
and precedent aren't on her side.
The International Association of Athletics Federations said White risks being
stripped of her gold medals in the 100 and 200 meters after testing positive for
the stimulant modafinil. She also could face a two-year suspension.
Under the sport's strict liability policy, athletes are disqualified from an
event if a banned substance is found in their system - regardless of the
circumstances.
In one of the most celebrated cases of its kind, Romanian teenage gymnast
Andreaa Raducan was stripped of the all-around gold medal at the 2000 Sydney
Olympics after testing positive for a stimulant contained in a cold pill.
Olympic officials acknowledged the measure was harsh, but said they had to apply
the rules.
IAAF officials indicated the central issue in White's case was not so much
whether she should be disqualified and lose the medals, but whether she also
should receive a warning or a two-year suspension.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
The IAAF said it was trying to determine the status of modafinil, which
stimulates the central nervous system. While not specified by name on the banned
list, modafinil is covered under the stimulants category of "related
substances," the IAAF said.
In recent years, athletes have been warned repeatedly to refrain from using
supplements or other substances which could trigger a positive test. They are
told to clear all medications with team doctors.
Under IAAF rules, athletes must notify the federation in advance of any products
they take for medical reasons. To apply for a medical waiver, athletes must
provide records proving they need to take a substance for therapeutic reasons.
But White insisted she didn't need to do that.
"Given that it (modafinil) was not on the banned list, I think it is
understandable why I didn't realize that I needed to declare it," White said.
"We thoroughly researched this," she added. "It wasn't on the banned list."
White said she was diagnosed with narcolepsy this year and began taking the drug
Provigil, which contains modafinil, a few months ago on the prescription of her
personal doctor, Brian Goldman.
"It has improved the condition in my day-to-day life and helped me function
normally," White said.
"I was extremely tired all the time, not sleeping well in the evening due to
sleeping in the daytime," White said. "My memory isn't very good. I needed just
to be right."
White said she had been taking the medication at the time of competitions in the
United States, London and Oslo, Norway, and passed all drug tests at the time.
"I never thought that this would be a problem now," she said.
White said she used the substance the morning of Sunday's 100-meter final. She
didn't say whether she also used the medication ahead of Thursday's 200-meter
race.
Pressed on why she didn't list the substance on her forms, White said, "Because
it isn't a medication that I take every single day. It's on an as-needed basis,
and because I took it so early in the day I never thought to list it. After a
competition, it's kind of hard to remember everything you take during the day."
White, who pulled out of Saturday's 400-meter relay final, tried to be
philosophical.
"Things happen in life," she said, "and I will just have to deal with the
consequences."
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
826 of 998 DOCUMENTS
The Associated Press State & Local Wire
August 30, 2003, Saturday, BC cycle
White denies taking drugs to enhance performance
BYLINE: By ROB GLOSTER, AP Sports Writer
SECTION: Sports News
LENGTH: 724 words
DATELINE: SAINT-DENIS, France
U.S. sprinter Kelli White said her positive drug test at the World Championships
stemmed from prescription medicine for a sleep disorder, and the double gold
medalist denied ever taking drugs to enhance her performance.
Track's world governing body is investigating a sample from White, whose gold
medals in the 100 and 200 meters are in jeopardy. She is the only American woman
to win an event at these World Championships.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," said White,
who withdrew from the U.S. 400-meter relay team. "The mere fact of this
allegation is personally harmful and hurtful. I have never taken any substance
to enhance my performance."
Without White, the heavily favored Americans lost to France in the relay final
on Saturday night.
White's positive drug test for the stimulant modafinil came after her win in the
100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference the IAAF is aware of other
cases is which modafinil has been used by athletes "for the purpose of
performance enhancement."
White said at a news conference Saturday night that she was prescribed modafinil
for narcolepsy, and that she and close members of her family have been diagnosed
with the condition. White, who was somber but composed during the news
conference, said she found out about the positive test by reading the French
sports daily L'Equipe.
White said she is confident she'll be able to keep her medals.
"Honestly, deep in my heart, I do believe so," she said. "I believe I'm
innocent, I know I'm innocent. I've worked very hard for the medals I earned
this week, and I'm going to work very hard to keep them."
Ljungqvist said he did not think the doping case involving White would be
resolved during the World Championships because it still must go through a USATF
hearing.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a "strong"
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Athletes are required to declare the use of any drug for medical purposes and
seek an exemption for its use, but White neither declared her use of modafinil
nor sought such an exemption. Since the drug is not on the IAAF's list of banned
substances, White said she saw no need to make sure a declaration.
Gyulai said modafinil is not specifically listed as a banned drug, but is
"covered by a clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
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LANGUAGE: ENGLISH
GRAPHIC: AP Photos
Copyright 2003 Associated Press
All Rights Reserved
827 of 998 DOCUMENTS
Associated Press Online
August 30, 2003 Saturday
Sprinter Denies Taking Drugs for Event
BYLINE: ROB GLOSTER; AP Sports Writer
SECTION: SPORTS
LENGTH: 960 words
DATELINE: SAINT-DENIS, France
U.S. sprinter Kelli White said her positive drug test at the World Championships
stemmed from prescription medicine for a sleep disorder, and the double gold
medalist denied ever taking drugs to enhance her performance.
Track's world governing body is investigating a sample from White, whose gold
medals in the 100 and 200 meters are in jeopardy. She is the only American woman
to win an event at these World Championships, and the only U.S. woman to win
both sprints at a world meet.
"Because I know that I did nothing wrong and sought no advantage over my
competitors, I am confident that things will work out in the end," said White,
who withdrew from the U.S. 400-meter relay team. "The mere fact of this
allegation is personally harmful and hurtful. I have never taken any substance
to enhance my performance."
Without White, the heavily favored Americans lost to France in the relay final
on Saturday night.
White's positive test for the stimulant modafinil came after her win Monday in
the 100. Arne Ljungqvist, vice president of the International Association of
Athletics Federations and head of that organization's anti-doping commission,
said White's 200 medal is in jeopardy, too.
Modafinil stimulates the central nervous system and is used to fight fatigue and
sleepiness. Ljungqvist said at a news conference that the IAAF is aware of other
cases in which modafinil has been used by athletes "for the purpose of
performance enhancement."
White responded at her own news conference Saturday night, saying that she was
prescribed modafinil for narcolepsy earlier this year, and that she and close
members of her family have been diagnosed with the disorder. She said she went
to her doctor after feeling tired all the time and having trouble with her
memory.
White, who was somber but composed during the news conference, is confident
she'll be able to keep her medals.
"Honestly, deep in my heart, I do believe so," she said. "I believe I'm
innocent; I know I'm innocent. I've worked very hard for the medals I earned
this week, and I'm going to work very hard to keep them."
It's not the first time White has been involved in a disputed drug test in
France.
In July 2002, after running in a meet at Saint-Denis, White's sample turned up
traces of a corticoid - an anti-inflammatory steroid. She was suspended for six
months by France's anti-doping agency because she lacked a medical certificate,
but the IAAF cleared her.
And it was just the latest controversy for the U.S. team at the World
Championships.
The head of the World Anti-Doping Agency called for the U.S. 1,600-meter relay
team from the Sydney Olympics to return its medals after a report that Jerome
Young, a surprise winner here in the 400 meters, failed a drug test in 1999 but
was quietly cleared by U.S. officials and allowed to run in the 2000 Games.
Also, American sprinter Jon Drummond withdrew from the meet after a tantrum in
the men's 100 quarterfinals. Drummond threw a fit after being disqualified for a
false start.
Ljungqvist said he did not think White's doping case would be resolved during
the World Championships.
"It is very clear that it is a stimulant, but whether it is a soft stimulant or
a strong stimulant is not clear," IAAF general secretary Istvan Gyulai told The
Associated Press. "If it ends as a doping case - at the moment all indications
are toward that direction - then she will be deprived of the gold medal."
Gyulai and Ljungqvist said if it is a "soft" stimulant, White would be
disqualified from the 100 and stripped of her medal. If it is a stronger
stimulant similar to an amphetamine, she also would face a two-year
international ban.
Athletes are required to declare the use of any drug for medical purposes and
seek an exemption for its use, but White neither declared her use of modafinil
nor sought such an exemption. Since the drug is not on the IAAF's list of banned
substances, White said she saw no need to make sure a declaration.
"The reason that I did not declare this on my doping control list is because I
do not take it every day. It is on an as-needed basis," she said. "Because I
took it so early in the day, I never thought to list it. After a competition,
it's kind of hard to remember everything you take during the day."
Gyulai said modafinil is not specifically listed as a banned drug, but is
"covered by a clause on related compounds."
"Of course, it is an embarrassing factor for her that she would neither declare
nor get prior exemption," Ljungqvist said. "She should have done it. Even more,
she should have asked for a prior exemption to use it, that is of course a
problem for her when her case will later be evaluated."
White would have anchored the relay. Instead it was Torri Edwards, who got the
baton with a lead but was passed in the final few meters by France's Christine
Arron. As the French sprinters danced to the cheers of a joyous crowd, the
dispirited Americans shook their heads.
"I felt a little bit fatigued, but I did the best I could," said Edwards, who
won silver in the 100 and bronze in the 200 and now could move up to gold and
silver if White is disqualified.
Arron said she was glad White withdrew from the race.
"It's good that White wasn't there," Arron said. "It would have shown a lack of
respect for us if she had run."
Also Saturday, Allen Johnson won his fourth world title in the 110-meter
hurdles, edging U.S. teammate Terrence Trammell by eight-hundredths of a second.
Liu Xiang of China took the bronze.
Other winners were Mirela Manjani of Greece in the women's javelin, Jaouad
Gharib of Morocco in the men's marathon, Eunice Barber won France in the women's
long jump and 18-year-old Tirunesh Dibaba of Ethiopia in the women's 5,000
meters.
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
All Rights Reserved
828 of 998 DOCUMENTS
Associated Press Online
August 30, 2003 Saturday
White Had 'no Idea' on Banned Substance
BYLINE: STEPHEN WILSON; AP Sports Writer
SECTION: SPORTS
LENGTH: 714 words
DATELINE: SAINT-DENIS, France
Kelli White insists she did nothing wrong. The American sprinter says she took
medication only to treat a sleep disorder, not to enhance her performance, and
had no idea it contained a banned substance.
She says she didn't bother to apply for a medical waiver or include the
medication on her doping control form because it wasn't on the prohibited drug
list.
That was White's defense Saturday as she came under investigation for a positive
test that could cost her two gold medals from the World Championships.
"I have never taken any substance to enhance my performance," said White, who
pulled out of Saturday's 400-meter relay final. "Because I know that I did
nothing wrong and sought no advantage over my competitors, I am confident that
things will work out in the end."
Convincing world track officials of her innocence won't be easy - the rule book
and precedent aren't on her side.
The International Association of Athletics Federations said White risks being
stripped of her gold medals in the 100 and 200 meters after testing positive for
the stimulant modafinil. She also could face a two-year suspension.
Under the sport's strict policy, athletes are disqualified from an event if a
banned substance is found in their system - regardless of the circumstances.
In one of the most celebrated cases of its kind, Romanian teenage gymnast
Andreaa Raducan was stripped of the all-around gold medal at the 2000 Sydney
Olympics after testing positive for a stimulant contained in a cold pill.
Olympic officials acknowledged the measure was harsh but said they had to apply
the rules.
IAAF officials indicated the central issue in White's case was not so much
whether she should be disqualified and lose the medals but whether she also
should receive a warning or a two-year suspension.
Under IAAF rules, the penalty for use of light stimulants, such as ephedrine, is
disqualification and a public warning. For harder stimulants, such as
amphetamines, the sanction is disqualification and a two-year ban.
The IAAF said it was trying to determine the status of modafinil, which
stimulates the central nervous system. While not specified by name on the banned
list, modafinil is covered under the stimulants category of "related
substances," the IAAF said.
In recent years, athletes have been warned repeatedly to refrain from using
supplements or other substances that could trigger a positive test. They are
told to clear all medications with team doctors.
Under IAAF rules, athletes must notify the federation in advance of any products
they take for medical reasons. To apply for a medical waiver, athletes must
provide records proving they need to take a substance for therapeutic reasons.
But White insisted she didn't need to do that.
"Given that it (modafinil) was not on the banned list, I think it is
understandable why I didn't realize that I needed to declare it," White said.
"We thoroughly researched this," she added. "It wasn't on the banned list."
White said she was diagnosed with narcolepsy this year and began taking the drug
Provigil, which contains modafinil, a few months ago on the prescription of her
personal doctor, Brian Goldman.
"It has improved the condition in my day-to-day life and helped me function
normally," White said.
"I was extremely tired all the time, not sleeping well in the evening due to
sleeping in the daytime," White said. "My memory isn't very good. I needed just
to be right."
White said she had been taking the medication at the time of competitions in the
United States, London and Oslo, Norway, and passed all drug tests at the time.
"I never thought that this would be a problem now," she said.
White said she used the substance the morning of Sunday's 100-meter final. She
didn't say whether she also used the medication before Thursday's 200-meter
race.
Pressed on why she didn't list the substance on her forms, White said: "Because
it isn't a medication that I take every single day. It's on an as-needed basis,
and because I took it so early in the day I never thought to list it. After a
competition, it's kind of hard to remember everything you take during the day."
White tried to be philosophical.
"Things happen in life," she said, "and I will just have to deal with the
consequences."
LOAD-DATE: August 31, 2003
LANGUAGE: ENGLISH
Copyright 2003 Associated Press
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829 of 998 DOCUMENTS
Facts on File World News Digest
August 23, 2003
Sports:World Track Championships Held
SECTION: Pg. 699A1
LENGTH: 995 words
The biennial World Track and Field Championships were held August 23-31 in
Paris, France. The U.S. topped the medals table, winning 20, and also garnered
the most gold medals, with 10. Russia was second in medals, with 19, and
Ethiopia, Belarus and France tied for a distant third, with seven each. However,
a doping scandal called into question whether a U.S. sprinter who had won two
events would be allowed to keep her medals.
U.S. Sprinter Tests Positive for Drug
The International Association of Athletics Federations (IAAF), track and field's
world governing body, August 30 announced that U.S. sprinter Kelli White had
tested positive for the banned stimulant modafinil. White, 26, August 24 had won
the women's 100 meters, posting a time of 10.85 seconds. She won her second gold
medal of the championships August 28, posting a time of 22.05 seconds in the 200
meters. Both times were career bests.
The IAAF said that a urine sample provided by White after her victory in the 100
meters was found to contain modafinil. White at a news conference August 30 said
she had been taking modafinil for several months to treat narcolepsy, a sleep
disorder. She said she did not notify the IAAF that she was taking the drug and
get a prior exemption to use it because it was not on the official list of
banned substances. Athletes were required to inform the IAAF of any medications
or supplements they were taking.
White's physician, Brian Goldman, August 31 confirmed that he had given White
the drug for the sleep disorder. Also August 31, USA Track & Field, the sport's
governing body in the U.S., said the results of a urine test taken after White's
win in the 200 meters were negative.
The IAAF September 3 announced that since modafinil had been classified as a
lesser stimulant, White would not be suspended for testing positive. Had
modafinil been classified as a strong stimulant, such as amphetamines, White
would have faced a two-year ban.
However, White could still be stripped of the two gold medals she won at the
world championships. The IAAF September 3 said that White had until September 8
to provide evidence that she had been taking modafinil at the direction of a
doctor for the treatment of narcolepsy. The IAAF would then determine if a
doping violation had occurred. Athletes in Olympic-related sports were held
accountable for any banned substance found in their bodies, and the IAAF said
that White could have a difficult time avoiding the loss of her medals, even if
she proved she was taking modafinil for a legitimate reason.
U.S. Sprinter Disrupts Men's 100 Heat
U.S. sprinter Jon Drummond August 24 disrupted a quarterfinal heat for the men's
100 meters when he refused to leave the track after being disqualified for a
false start. Drummond was disqualified under a new false-start rule instituted
earlier in 2003. Under the previous rule, each individual sprinter was allowed
one false start (a false start was defined as a runner leaving the blocks less
than a tenth of a second after the starter's pistol was fired), and was
disqualified from the race for a second violation. Under the new rule, the
entire field of a race was judged to have committed a false start if one
sprinter left early. Any sprinter who committed a subsequent false start was
disqualified.
In Drummond's August 24 heat, Jamaican sprinter Dwight Thomas was called for a
false start. On the restart, both Drummond and Jamaica's Asafa Powell were
disqualified for false starts: Drummond for leaving 0.052 of a second early and
Powell for leaving 0.086 of a second early. Drummond claimed that he had
flinched, setting off the computerized false-start detection equipment at the
starting blocks. Drummond complained to officials, then lay down on the track
and refused to get up for several minutes in protest of his disqualification. He
eventually left the track, only to return minutes later and stand in front of
the starting blocks, waving his arms to the crowd. Officials postponed the heat
and ran the two remaining men's 100-meter quarterfinal heats. When officials
tried to rerun the postponed heat, the crowd jeered and whistled loudly, further
delaying the race. It was eventually completed about 45 minutes after its
scheduled start.
Kim Collins of the Caribbean island nation of St. Christopher (St. Kitts) and
Nevis August 25 won the men's 100-meter final in 10.07 seconds. It was the
slowest winning time at the world championships since 1983. In every Olympics
and world championships since then, the winner of the men's 100 meters had
posted a time under 10 seconds.
Drummond August 26 withdrew from the U.S. team for the rest of the world
championships. He had been scheduled to compete with the men's 4x100-meter relay
team later in the competition. The IAAF that day disqualified him from the
championships for "bringing the sport into disrepute."
Other Highlights
In other highlights of the World Track and Field Championships:
Allen Johnson of the U.S. August 30 won the gold medal in the men's 110-meter
hurdles. It was Johnson's fourth world championship gold medal in the event.
Hicham el-Guerrouj of Morocco August 27 won his fourth consecutive world
championships gold medal in the men's 1,500 meters.
Lima Azimi August 23 became the first Afghan woman to participate in a major
international event in any sport when she ran in a first-round heat for the 100
meters. Azimi also became the first Afghan athlete, male or female, to compete
in the world track and field championships since 1983.
British triple jumper Jonathan Edwards August 22 announced that he would retire
after the world championships. Edwards, 37, had won gold in the event at the
1995 and 2001 world championships and in the 2000 Summer Olympics, and had set
two world records in 1995. Edwards, who had injured his ankle earlier in August,
competed for the final time August 25, but withdrew after finishing only two
jumps.
LOAD-DATE: September 15, 2003
LANGUAGE: ENGLISH
Copyright 2003 Facts on File, Inc.
830 of 998 DOCUMENTS
Espicom Business Intelligence
May 22, 2003
Provigil improves symptoms of ADHD in children
LENGTH: 445 words
Data from two double-blind, placebo-controlled Phase II studies presented at the
156th Annual Meeting of the American Psychiatric Association, held from 17th to
22nd May, in San Francisco, CA, show that Cephalon's Provigil (modafinil) C-IV
improves attention deficit hyperactivity disorder (ADHD) symptoms in children in
both school and home settings. These studies also showed that modafinil was well
tolerated with different dose regimens. Preclinical studies suggest that
modafinil works selectively through the sleep/wake centres to activate the
cortex of the brain.
During one four-week study, 248 children with ADHD aged six to 13 years were
randomised to receive either once- or twice-daily doses of modafinil in
different combinations of 300mg doses or placebo. Children weighing >30kg
(66lbs) could be assigned to any of the 300mg treatment groups or to a group
receiving a 400mg a day dose. In the study, 69 per cent of patients were
treatment naive, with 31 per cent having had prior stimulant treatment for their
symptoms. The primary outcome was a change from baseline in the School Version
of the ADHD Rating Scale IV, a tool for the assessment of ADHD symptoms as
completed by the patient's teacher.
The 300mg regimen of modafinil administered once daily and a split dose regimen
(200/100mg) significantly improved symptoms as measured by the teacher-rated
ADHD Rating scale (p<0.05). In addition, the 300mg once-daily dose improved
symptoms of ADHD across all other rating scales used in the study including the
parent rated home version of the ADHD rating scale and the Conner's Parent ADHD
Rating Scale.
Side effects reported in the study were mild-to-moderate with insomnia,
abdominal pain, loss of appetite, cough, fever and rhinitis reported more
frequently in the modafinil-treated groups, compared to placebo.
In a second four-week, double-blind, placebo-controlled, cross-over study, 48
children (aged six to 13 years) were randomised to receive placebo or modafinil
100, 200, or 300mg and children weighing >=30kg could be assigned to any of the
100 to 300mg treatment groups or to a group receiving 400mg once daily. The ADHD
Rating Scale-IV (home version) was the primary efficacy measurement tool. The
most significant improvements were seen in patients receiving the 300 or 400mg
dose of modafinil (p<0.05) as assessed in the home environment by the
parent-rated ADHD Rating Scale. The most common side effects observed in the
modafinil treated group as compared to placebo were abdominal pain and headache.
Based on results from these studies, Cephalon will be initiating Phase III
studies in children with ADHD later in 2003.
LOAD-DATE: May 22, 2003
LANGUAGE: ENGLISH
Copyright 2003 ESPICOM Business Intelligence Ltd.
831 of 998 DOCUMENTS
FD (Fair Disclosure) Wire
May 7, 2003 Wednesday
Event Brief of Q1 2003 Cephalon, Inc. Earnings Conference Call - Final
LENGTH: 3955 words
CORPORATE PARTICIPANTS
. Robert Grupp, Cephalon, VP, Corporate Communications . Frank Baldino, Jr.
Ph.D, Cephalon, Chairman, CEO . Kevin Buchi, Cephalon, SVP, CFO . Robert Roche,
Cephalon, SVP, Sales and Marketing . Paul Blake, Cephalon, SVP, Clinical
Research and Regulatory Affairs . John Osborne, Cephalon, SVP , Secretary, and
General Counsel
OVERVIEW
Management announced 1Q03 diluted EPS of $0.21 on total product sales of
$137.6m. 2003 guidance was reiterated for sales of $650-660m and EPS of $1.50.
Q&A Focus: patent litigation, FDA discussions and marketing programs.
FINANCIAL DATA
A. Key Data From Call 1. 1Q03 Diluted EPS = $0.21. 2. 1Q03 Total Product Sales =
$137.6m. 3. Total revenue = $144.7m. 4. Cash, cash equivalents and investments =
$546.8m. 5. Reiterating 2003 product sales guidance of $650-660m. 6. 2003 EPS
guidance = $1.50. 7. 2Q03 product sales guidance = $155m. 8. 2Q03 diluted EPS
guidance is $0.30.
PRESENTATION SUMMARY
S1. 1Q03 Performance (F.B.) 1. Reported 1Q03 Diluted EPS of $0.21. 1. Exceeded
guidance. 2. Topics on Investors' Minds. 1. Prescription trends for key
products. 1. Co. has enjoyed consistent strong sequential prescription growth Q
after Q. 2. Based on unique benefits and ability to execute strategic plan. 3.
1Q03 saw moderation of prescription growth due to disruption caused by expansion
and reorganization of sales force. 4. Added over 100 new employees to US
commercial organization. 5. Realigned every territory. 6. Inevitable disruption
was underestimated. 7. Impact was temporary. 8. Positive effects, coupled with
important marketing initiatives, will allow co. to meet guidance. 2. 8-10% of
Provigil sales come from outside US. 1. Rate of sequential prescription growth
required in US is less than 10% per quarter for rest of year. 3. Actiq Recall In
Europe. 1. Initiated precautionary recall of certain lots of Actiq in Europe. 2.
Manufactured in Salt Lake City facility, where Actiq has been manufactured for
Europe for several years. 3. Drug recalls not uncommon. 4. Have contacted
relevant regulatory authorities. 5. Salt Lake City continues to manufacture
Actiq for Europe and for US as planned later in 2Q03. 6. Not a material event.
7. All costs were included in 1Q03 results. 4. Update on Generic Modafinil
Filings. 1. Four generic companies have filed ANDAs to market generic form of
modafinil. 2. No unexpected disclosures or innovative chemistry apparent. 3. Co.
initiated patent infringement lawsuit against each company. 4. Legal process
will run its course over next several years. 5. Remain confident in strength of
patent provision and expect to prevail. 6. Co. has sound strategy to develop
follow on compounds to Provigil. 7. Provigil is first entrant into new category
of weight-promoting products. 8. Anticipate that R-Isomer of modafinil will be
next, with clinical trials beginning next month. 1. Targeting launch of this
product in late 2005. 9. Regardless of outcome of patent infringement, r-
modafinil will build upon and extend the Provigil brand.
S2. Product Detail (B.F.) 1. 2003 Is Transitional Year for Provigil. 1.
Preparing for expected approval of SNDA. 1. Filed last December seeking broader
label to treat sleep disorders. 2. Expect FDA action in 4Q. 3. Positive decision
will allow expansion of marketing message and expansion of physician universe.
4. Increase in central nervous system US sales force is complete. 5. Begun
rolling out new marketing programs to increase reach of key product messages. 6.
Clinical development programs have produced important data that will be
presented and published in 2003. 7. Will have significant presence at major
psychiatry, neurology and sleep meetings during the year. 8. Two platform
presentations at American Psychiatric Association meeting this month, discussing
positive results from clinical trial for Provigil to treat ADHD in children. 9.
Pleased with response to expanded label in UK granted in 2002. 10. Have
broadened message and increased physician call universe. 11. Result is increase
in UK sales vs. 1Q02. 12. Filed application for obstructive sleep apnea label in
France in 1Q03, and plan similar filings in Germany and Italy next month. 13.
Continue to believe there is enormous untapped potential in Provigil. 2. Actiq
Is Only Drug Approved to Treat Breakthrough Cancer Pain. 1. In 2003, sales and
marketing efforts focused on raising awareness of breakthrough cancer pain and
product's benefits. 2. Data have been presented that explore the use of Actiq to
treat breakthrough pain unrelated to cancer. 1. In March, positive data was
presented at American Academy of Pain Medicine demonstrating utility of Actiq in
treating migraine pain. 2. Similar studies were presented at the American Pain
Society meeting. 3. Migraine patients often require rescue treatment in hospital
emergency departments. 4. Data suggests Actiq may play role in outpatient
treatment of severe migraine pain. 5. Will conduct additional studies in utility
of Actiq in patients with breakthrough or episodic pain. 3. Gabitiril is Only
SGRI Available Today. 1. With understanding of mechanism, proven safety profile
and low potential for interactions, physicians prescribe for a range of clinical
disorders. 2. In 1Q03, completed two dose-ranging studies in general anxiety
disorder and naturopathic pain. 3. Data demonstrated beneficial impact on widely
accepted anxiety and pain scales. 4. Showed benefit on standard quality of sleep
measures. 5. Both studies provide important dosing information. 6. Expect to
initiate larger studies on generalized anxiety disorder and post-traumatic
stress disorder. 7. Patient feedback and clinical data point to benefit of
Gabitiril in treating overlapping symptoms of insomnia, anxiety and pain. 4.
Expect 2003 to be Best Year Ever. 1. With three substantial products in US,
expanded sales force, continuing positive clinical data and expanding European
business, positioned for excellent year. 2. Will continue to balance risk, while
driving sales and earnings growth.
S3. 1Q03 Financial Detail (K.B.) 1. Total Product Sales Were $137.6m in 1Q03. 1.
44% increase over 1Q02. 2. Total revenue was $144.7m, up 30% over prior year. 1.
Sales of Provigil were $55.8m. 2. Actiq sales were $46.2m. 3. Gabitiril sales
were $12.7m. 4. Other European product sales were $22.9m. 3. Sales growth was
modest, but EBITDA of $35.9m and EPS of $0.21 per share exceeded guidance. 1.
1Q03 results included increase in R&D and SG&A, although expenses did not rise
to level indicated in guidance. 4. Ended quarter with cash, cash equivalents and
investments of $546.8m. 1. Provide flexibility to pursue attractive strategic
opportunities. 5. Reiterating 2003 product sales guidance of $650-660m. 1.
Represents sales growth of 40% YoverY. 6. 2003 EPS guidance remains at $1.50,
including tax provision of 38%. 7. Pre-tax earnings will grow by almost 100% in
2003. 8. SEC discourages use of non-GAAP measures such as EBITDA. 1. As a
result, EBITDA guidance will no longer be provided. 9. 2Q03 product sales
guidance is $155m. 10. 2Q03 diluted EPS guidance is $0.30. 11. Expect sales to
ramp, resulting in greater EPS in 2H03. 12. 2Q03 guidance includes Provigil
sales of $65-68m, Actiq sales of $50-55m, Gabitiril sales of $15-18m and other
product sales of $21-23m.
QUESTION AND ANSWER SUMMARY
Q1. (Matt Geller, CIBC World Markets) How do you see sales picking up throughout
the year? What do you see catalyzing the increase? Can you talk about Gabitril
for insomnia and how it differs from other drugs?
A. (Robert Roche) We anticipate the ramp up we've seen in past years. We're
beginning to see it in the early stages of 2Q for all three products, and we
expect that to continue and we'll be able to reach our targets.
A. (Paul Blake) In insomnia, we start off with the expectation that an SGRI will
have an effect. We have some pre-clinical data and pilot work that encourages
us. We have a pilot study that should report in 3Q. At a meeting last week I
presented some data that showed secondary endpoints in studies of general
anxiety disorders and neuropathic pain where Gabitril worked also showed
benefits in insomnia. We're expecting a positive signal from our phase II work
looking at total sleep time, latency to persistent sleep and wake after sleep
onset.
Q2. (Eric Schmidt, SG Cowan) Can you touch on usage of cash, which went down
QoverQ, as well as inventory effects in 1Q?
A. (Kevin Buchi) The largest use of cash was a $30m investment we made into NDS
Proteomics. Other changes were in working capital areas. We saw an increase in
accounts receivable, associated with higher sales, increases in inventory.
Nothing else noteworthy. Provigil showed another slight decrease in inventories
and we ended the quarter with Provigil inventories below a month and a half.
That's wholesale and retail.
Q3. (Eric Schmidt, SG Cowan) You mentioned no innovative chemistry disclosures
in the ANDA filings. Can you educate us on that? What should we expect going
forward?
A. (Frank Baldino) For obvious reasons, we're not going to talk about our
strategy or what the findings are. Simply stated, there was a lot of concern on
the street about innovative approaches to getting around the particle size
patent. Frankly, we haven't seen that.
A. (John Osborne) As you know, different courts have different timetables. This
kind of litigation is reasonably complex, involves a fair amount of discovery
and usually takes several years. We can't be any more specific than that.
A. (Frank Baldino) I think it's fair to say that disclosure from us in this
matter will be almost non-existent.
A. (John Osborne) We're prepared to litigate this in the courts, but not by
speaking to the investment community.
Q4. (Corey Davis, JP Morgan) Do you still expect an FDA panel meeting for
Provigil's new claim? Any idea when that may be?
A. (Frank Baldino) We have not been officially informed of a panel meeting by
the FDA. We assume we'll have one, probably in the later half of the year. We're
preparing as if we'll have one later in the year. We're confident it will be
later than the June, July time frame. When we get notice, we'll inform the
street.
Q5. (Corey Davis, JP Morgan) Gabitril's revenue growth was below volume growth,
so I assume inventory dropped on that as well. The 1.5 months you gave is
different from IMS wholesale data. Where's the difference there, and what's the
chance that inventory will come down further in 2Q?
A. (Kevin Buchi) We track wholesaler and retailer data. The data you buy from
IMS is just wholesaler. The difference is material held on retail pharmacy
shelves. Gabitril is a smaller product, so we tend to see more fluctuation in
inventory levels. Sales were below underlying prescription demand, so I expect
it will be more variable given its size.
Q6. (Corey Davis, JP Morgan) Will Provigil inventories come down in 2Q?
A. (Kevin Buchi) It's really hard to tell. We've said we think inventories have
reached the bottom, but it continues to slide. I'm reluctant to say it's at the
bottom. It's hard to conceive of wholesale getting below two weeks, and it's not
a whole lot above that at this point.
Q7. (Corey Davis, JP Morgan) In the past, you've given a breakdown of Provigil
use. I'm particularly interested in ADHD and whether you're getting hurt by
Stratera, and whether that might come back.
A. (Frank Baldino) I think where our business is coming from really hasn't
changed. The largest market area has been psychiatry for the last couple of
years. As far as ADHD is concerned, the first big presentation will be this year
at the American Psychiatric Association meeting. After that, we should see some
more interest in the physician community. Right now, it's about 12-15% of our
business. Stratera has had zero impact on the small part of the market that
Provigil is dominating.
Q8. (Geraldine O'Keeffe, Fordis Bank) You mentioned a new marketing program for
Provigil. Can you expand on that?
A. (Robert Roche) The marketing programs conceived and implemented for Provigil
in 2003 are far greater in magnitude and scope than in the past. Our increase in
marketing expenditure in 2003 is about $55m higher than at any point in the
past. We've tripled our investment in Provigil marketing and marketing in
general. The programs we're pursuing are the standard promotional activities
used worldwide, but because of the nature of our products, and because the
information needs to be shared under unrestricted educational grants, that's a
huge proportion of what we're doing. We've invested heavily in continuing
medical education programs, consultancy meetings, speakers training meetings,
etc. There will be a lot of expenditure around the symposia data being rolled
out toward the middle or 3Q of this year, and the exciting new information we'll
be sharing
Q9. (Geraldine O'Keeffe, Fordis Bank) So will you be marketing in the areas you
already have approval for, or for areas you expect to get approval for?
A. (Robert Roche) We market only in the area for which we have approval. We sell
the benefits of Provigil to a wide variety of physician groups, we focus on the
features of the products, and those physicians have made the determination that
the drug can be helpful in a wide variety of patient populations.
A. (Frank Baldino) Basically, we're going to continue to invest more
aggressively in those techniques that have worked well for us in the past. We're
expecting the broader label for Provigil this year, and internally, we're
preparing for the launch into a broader market in early '04. That's when you'll
see the largest impact of Provigil growth, larger than anything we've seen to
date.
Q10. (Jim Birchenough, Lehman Brothers) Are you moving toward sleep specialists
or are you still focusing on high-prescribing psychiatrists? How many reps do
you have and how are they divided?
A. (Robert Roche) We continue to focus on the three primary physician groups
we've been working with for the past few years: sleep specialists, neurologists,
psychiatrists. That's what we're doing today. The sales expansion allows us to
interact with a greater number of physicians especially in psychiatry. That's
where the sales and marketing muscle is being allocated.
Q11. (Jim Birchenough, Lehman Brothers) There's been a seasonal use to Provigil
with a slowdown over the summer. Are you getting into markets that are less
seasonal?
A. (Robert Roche) The guidance we provided indicates strong growth in 2Q, and we
anticipate 8-10% prescription growth in 3Q and 4Q, so we're anticipating a
strong 2H.
Q12. (Jim Birchenough, Lehman Brothers) When do you expect the Surtax (phonetic)
acquisition to close? Where is your focus in terms of in-licensing other
products? How are discussions going on a Provigil partnership?
A. (Frank Baldino) Surtax is a difficult deal. We made a fair bid, the
shareholders have not tendered their shares yet. It's targeted to close or
expire at the end of May, so by then we'll know if we'll be able to capture 90%
of the company. In terms of in-licensing, we're going to continue to focus on
areas where we've established some strength. We see opportunities there and we
intend to pursue those. If the opportunity is very good, we'll go beyond that.
Regarding partnerships, we believe there are only a couple of ways to go. By
June, we need to make a strategic decision in anticipation of a broad label
approval for Provigil. We're talking to a number of companies with a lot of
potential, and we're also looking internally to see if we can do it ourselves.
That decision will be made in June, and we'll let you know when it's made. The
first priority in a partner is to find someone with the expertise and focus to
make these products much larger than they are. That's driving our discussions.
I'd rather get strong economics on the products we have today.
Q13. (Chris Juner (phonetic), T. Rowe Price) Could you repeat your comments
about the timing of the follow on isomer strategy? Could you review the
individual half-lives of both isomers as it relates to the parent compound and
whether there's a theoretical concern that it would disturb sleep?
A. (Paul Blake) The r isomer has a half life of 12-15 hours and the s isomer has
a half life of 2-3 hours. When you give Provigil you end up with the net result
of 50% of each. When we give the r isomer alone, we expect the half life to be
12-15 hours, which we think will give a nice response and should not disturb
sleep. We've done a number of studies, one of which has just been accepted for
publication, using Provigil twice daily in people who need a greater effect.
Split doses we think we'll be able to mirror without any disturbance of sleep.
We expect to confirm this in the clinical program beginning next week
Q14. (Chris Juner, T. Rowe Price) Can you go over again the timeline for the
execution of the r IND filing in this country?
A. (Paul Blake) We'll be executing the program next week and we expect to file
by the end of next year.
Q15. (Marc Goodman, Morgan Stanley) Where was Provigil inventory at the end of
the year?
A. (Kevin Buchi) A little north of 1.5.
Q16. (Marc Goodman, Morgan Stanley) How much did that hurt revenues in the
quarter?
A. (Kevin Buchi) If we dollarized the published prescription numbers, we'd come
up with a number around $52m.
Q17. (Marc Goodman, Morgan Stanley) How low do you think these guys are going to
go?
A. (Kevin Buchi) It's really hard to say. We've been consistently surprised that
inventories continue to get drawn down to these levels. Our assumption has been
that normal inventory levels would be somewhere north of where we are today.
Everyone has an incentive to manage inventories as tightly as possible. It's
just getting tighter and tighter. I don't think it can go a whole lot lower that
they are right now.
A. (Frank Baldino) The inventory information we get is the same as you get. It
happens, we track it. You can't manage that. Looking at where demand is, if you
have to have an inventory situation, I'd rather it be low than high. I think
we're in a really strong position here.
Q18. (Marc Goodman, Morgan Stanley) What about the other two products? Any
comments on April for the three products?
A. (Kevin Buchi) I don't have any comments on April for the three products. We
gave our sales guidance and you should assume we take all the data available
into account. We don't spend as much time or effort worrying about the other two
products because they tend not to be as material and the inventories have not
fluctuated as much. Our initial focus occurred in 3Q01 when we had some
wholesalers speculating on price increases. It's a schedule two substance so
it's more expensive to hold inventories so we'd expect less speculation
Q19. (Marc Goodman, Morgan Stanley) SG&A, R&D, is guidance the same as it was
before?
A. (Kevin Buchi) Yes, we believe the numbers being below guidance in 1Q was
simply timing, and we'll catch up in April.
Q20. (Felicia Reed, Adams, Harkness & Hill) For Provigil, Actiq and Gabitril,
what was the contribution for ex-US sales?
A. (Kevin Buchi) For Provigil, $6.2m, for Actiq, about $600,000, for Gabitril
about $1.3m.
Q21. (Felicia Reed, Adams, Harkness & Hill) And that was included in the other
sales line?
A. (Kevin Buchi) No, that was included in the sales line for each product.
Q22. (Michael King, Banc of America Securities) Regarding the generic filers,
one recently said they expected others to file. Do you expect others?
A. (Frank Baldino) It's hard to predict the future. We know when people file.
We've had four. In the next decade or so, people can file whenever they wish. We
don't see that happening. There's an advantage to being the first guy in, who
gets a six-month advantage over the others. Then they all pile in for whatever's
left after that.
A. (John Osborne) Perhaps more important than whether or not there is another,
the point in filing a single suit is to obtain a single ruling on our patent in
validity and scope. If someone else decides to take a shot, we would join them
in the same action. I don't know that the number will affect our position.
A. (Frank Baldino) No matter how many filings you have, they'll be wrapped in
the same suit that will go on for several years. We're operating with confidence
in our patents, but we're building the r isomer and moving on to the new
Provigil and expect to build that franchise. Our job is to ensure to the
shareholders that the follow on products continue to grow and for the new
markets we're creating, to preserve EPS growth independent of whatever decision
comes down.
Q23. (Michael King, Banc of America Securities) Are you willing to say which
court you'd like to see the patent case litigated in?
A. (John Osborne) It's public record. We've filed our action in US District
Court in New Jersey.
Q24. (Michael King, Banc of America Securities) Does your '03 guidance assume
any price increases?
A. (Kevin Buchi) I'd rather not comment on that.
Q25. (Jim Dawson, Buckingham Research) How much of the product sales guidance is
based on positive data for Provigil and Gabitril coming out this year?
A. (Kevin Buchi) None of the guidance is based on generating new data you're not
already aware of, either for the quarter or the year.
A. (Frank Baldino) Guidance is based on the performance we think we can achieve
with the marketing programs we have, with the sales messages we're delivering,
coupled with the data delivery that's already been made public at upcoming
meetings. We don't have any additional data we haven't shared with the street.
Q26. (Jim Dawson, Buckingham Research) What has your conversation been like with
the FDA on the SNDA for Provigil?
A. (Frank Baldino) We don't comment on FDA discussions. That's been our policy
for some time and we're going to stay with that.
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832 of 998 DOCUMENTS
Generic Line
April 9, 2003
CEPHALON SUES GENERIC FIRMS TO DEFEND MODAFINIL PATENT
SECTION: Vol. 20, No. 7
LENGTH: 271 words
Cephalon has filed a patent infringement lawsuit against four generic drugmakers
that seek to market an equivalent of the company's narcolepsy drug Provigil (
modafinil), the biopharmaceutical firm announced March 31.
The suit, filed in the U.S. District Court for the District of New Jersey,
alleges generic firms Teva, Mylan, Ranbaxy and Barr want to infringe the '516
patent covering the composition of Provigil, which does not expire until 2014.
According to Cephalon, the firms Teva and Mylan claimed the '516 patent is
invalid, while Ranbaxy and Barr principally claimed the patent would not be
infringed by their respective products.
"We have reviewed each of these filings in detail. We have not found anything in
them that is surprising or unanticipated," said Cephalon Senior Vice President
and General Counsel John Osborn.
Barr confirmed it had filed an abbreviated new drug application (ANDA) for
100-mg and 200-mg tablets for generic modafinil on Dec. 24, 2002, the first day
it was legally entitled to file. Provigil had sales of about $217 million for
the 12 months ending in January, Barr said. But Cephalon said it would be years
before a generic modafinil could be sold in the U.S. The FDA has granted
Provigil orphan drug exclusivity, which prevents the approval of any ANDA for a
modafinil product until at least December 2005. This period could be extended
until June 2006 if the agency grants the company a six-month extension for a
pediatric study.
Cephalon announced in February that at least one generic firm was seeking to
market generic modafinil (Generic Line, Feb. 12, Page 2).
LOAD-DATE: April 25, 2003
LANGUAGE: ENGLISH
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833 of 998 DOCUMENTS
Espicom Business Intelligence
April 1, 2003
Cephalon files patent infringement lawsuit against generic companies
LENGTH: 323 words
Cephalon has filed a lawsuit in US District Court in New Jersey against four
generic drug companies for infringement of its US Patent No. RE37516. The '516
patent covers the pharmaceutical compositions of the form of modafinil contained
in Provigil tablets (C-IV) and does not expire until 2014.
The lawsuit against Teva Pharmaceutical Industries, Mylan Pharmaceuticals,
Ranbaxy Pharmaceuticals and Barr Laboratories is based upon ANDAs filed by each
of the companies seeking FDA approval for a generic equivalent of modafinil to
be sold in the US. A company may file an ANDA requesting permission to market a
generic drug prior to expiration of a pioneer company's patent only if it
alleges that the patent either is invalid, unenforceable or would not be
infringed by the proposed generic product. In their filings, Teva and Mylan
principally claimed that Cephalon's '516 patent is invalid, and Ranbaxy and Barr
principally claimed the '516 patent would not be infringed by their respective
generic products.
Even if the lawsuit is unsuccessful and an ANDA application eventually is
approved by the FDA, it will be years before a generic equivalent modafinil
product can be sold in the US. In addition to the pharmaceutical composition
patent that protects Provigil until 2014, the drug has orphan drug exclusivity
that prevents the approval of any ANDA for a modafinil product prior to June
2006, provided the FDA grants the company a six-month extension to the December
2005 orphan drug exclusivity upon completion of a paediatric study.
Provigil was approved by the FDA for the treatment of excessive daytime
sleepiness associated with narcolepsy in December 1998 and was launched in the
US by Cephalon in February 1999. In December 2002, the company filed an sNDA
with the FDA seeking to expand its US labelling to cover the treatment of
excessive sleepiness associated with disorders of sleep and wakefulness in
adults.
LOAD-DATE: April 2, 2003
LANGUAGE: ENGLISH
Copyright 2003 ESPICOM Business Intelligence Ltd.
834 of 998 DOCUMENTS
Pharma Marketletter
March 31, 2003
Cephalon files patent suits over generic Provigil
LENGTH: 143 words
Cephalon of the USA has filed a lawsuit in the US District Court in New Jersey
against four generic drug companies for infringement of its US patent no
RE37516. The '516, which patent covers the pharmaceutical compositions of the
form of modafinil contained in Provigil (modafinil), does not expire until 2014,
according to the company.
The lawsuit against Teva Pharmaceuticals USA, Mylan Pharmaceutical, Ranbaxy
Pharmaceuticals and Barr Laboratories is based upon Abbreviated New Drug
Applications filed by each of the companies seeking US Food and Drug
Administration approval for a generic equivalent of modafinil to be sold in the
USA. In their filings, Teva and Mylan principally claimed that Cephalon's '516
patent is invalid, while Ranbaxy and Barr maintained that the patent would not
be infringed by their respective generic products.
LOAD-DATE: March 31, 2003
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835 of 998 DOCUMENTS
PR Newswire
March 31, 2003 Monday
Cephalon, Inc. Files Patent Infringement Lawsuit Against Generic Companies
SECTION: FINANCIAL NEWS
LENGTH: 952 words
DATELINE: WEST CHESTER, Pa. March 31
Cephalon, Inc. (Nasdaq: CEPH) announced today that it has filed a lawsuit in
U.S. District Court in New Jersey against four generic drug companies for
infringement of Cephalon's U.S. Patent No. RE37516. The '516 patent covers the
pharmaceutical compositions of the form of modafinil contained in PROVIGIL(R)
Tablets $(C-IV$) and does not expire until 2014.
The lawsuit against Teva Pharmaceuticals USA, Inc., Mylan Pharmaceutical Inc.,
Ranbaxy Pharmaceuticals Inc., and Barr Laboratories, Inc. is based upon
Abbreviated New Drug Applications (ANDAs) filed by each of the companies seeking
U.S. Food and Drug Administration (FDA) approval for a generic equivalent of
modafinil to be sold in the United States. A company may file an ANDA requesting
permission to market a generic drug prior to expiration of a pioneer company's
patent only if it alleges that the patent either is invalid, unenforceable, or
would not be infringed by the proposed generic product. In their filings, Teva
and Mylan principally claimed that Cephalon's '516 patent is invalid, and
Ranbaxy and Barr principally claimed the '516 patent would not be infringed by
their respective generic products.
"We have reviewed each of these filings in detail. We have not found anything in
them that is surprising or unanticipated. Our patent was approved by the United
States Patent and Trademark Office based on the results of extensive research by
Cephalon, and we continue to believe that our patent position for this product
is strong," said John E. Osborn, Senior Vice President and General Counsel of
Cephalon.
Even if the lawsuit is unsuccessful and an ANDA application eventually is
approved by the FDA, it will be years before a generic equivalent modafinil
product can be sold in the United States. In addition to the pharmaceutical
composition patent that protects PROVIGIL until 2014, the drug has orphan drug
exclusivity that prevents the approval of any ANDA for a modafinil product prior
to June 2006, provided the FDA grants the company a six-month extension to the
December 2005 orphan drug exclusivity upon completion of a pediatric study.
Also, the lawsuit triggers a stay that precludes the FDA from approving any ANDA
for up to 30 months to allow the court adequate time to resolve the infringement
lawsuit. Because this lawsuit commenced prior to the end of the New Chemical
Entity exclusivity period for PROVIGIL and within 45 days of the date of notice
by a generic company, the 30-month stay effectively begins at the expiration of
the NCE exclusivity period on December 24, 2003.
PROVIGIL was approved by the FDA for the treatment of excessive daytime
sleepiness associated with narcolepsy in December 1998 and was launched in the
United States by Cephalon in February 1999. In December 2002, the company filed
a Supplemental New Drug Application with the FDA seeking to expand its U.S.
labeling to cover the treatment of excessive sleepiness associated with
disorders of sleep and wakefulness in adults.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,300 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon also has European operations in the United Kingdom, France and Germany.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding the patent litigation, potential generic
competition, the strength of the PROVIGIL patent position, anticipated
scientific progress on its research programs, development of potential
pharmaceutical products, interpretation of clinical results, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings guidance, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties facing Cephalon such as those set forth in
its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend to update publicly any forward-looking statement, except as
required by law. The Private Securities Litigation Reform Act of 1995 permits
this discussion.
SOURCE Cephalon, Inc.
CONTACT: Robert S. (Chip) Merritt of Cephalon, +1-610-738-6376 or
cmerritt@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: April 1, 2003
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS, MEDICAL AND LEGAL AFFAIRS EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2003 PR Newswire Association, Inc.
836 of 998 DOCUMENTS
United Press International
March 26, 2003 Wednesday
Drugs, nutrition may aid soldier function
BYLINE: By STEVE MITCHELL
LENGTH: 619 words
DATELINE: WASHINGTON, March 26 (UPI)
Fatigue and sleep deprivation can take a toll quickly on soldiers in combat
conditions, such as those being experienced in Iraq, but the U.S. military is
well aware of this problem and has implemented programs to improve soldier
performance using both nutrition and drugs, experts said Wednesday.
"There is a lot of focus on performance enhancing," Janice Rosado, a civilian
physical scientist at the Natick Soldier Center's Combat Feeding Directorate in
Natick, Mass., told United Press International.
"Whatever we can do to give the war fighter an edge, we will do," said Rosado,
who is involved with research focused on developing nutritional supplements,
such as energy bars and drinks, that might improve soldier performance.
The Army "wants to give (soldiers) every edge they possibly can and if they can
find a safe, effective way of doing that through a performance-enhancing bar or
drink they would want to do that," she said.
Two products close to being in a soldier's standard gear are an energy bar known
as HooAH! (named after the famous military call) and a sports drink known as
ERGO, for Energy Rich Glucose Optimized Drink.
These products consist mainly of carbohydrates and would be included in
something called a first strike ration, Rosado said. The ration is intended to
be used "for the first few days of conflict where soldiers are on the move and
do not have time to stop and eat," she said.
"It would be carb-loaded because it would be just for a few days when you really
just need to be able to have a lot of carbs for energy," she said.
Rosado's department has done studies in conjunction with the U.S. Army Research
Institute of Environmental Medicine and found both HooAH! and ERGO increased
physical performance, such as how far soldiers could go on a march, by 17
percent compared to soldiers who did not take the supplements.
The agencies plan to do further studies to determine if the products enhance
cognitive performance, she said.
One factor that can impair cognitive performance significantly is lack of sleep,
said David Dinges, chief of the University of Pennsylvania's Division of Sleep
and Chronobiology and director of a research center for the Air Force Office of
Scientific Research focused on developing drugs that can lessen the deleterious
effects of sleep deprivation.
"Sleep deprivation impairs the brain, it impairs the ability to perform," Dinges
told UPI. "It can alter your ability to pay attention, you don't respond as
quickly ... your ability to think quickly and accurately at the same time is
slower."
This can impact soldier performance and perhaps contribute to mistakes that lead
to friendly fire incidents or other fatalities, he said.
One promising remedy may be a drug called modafinil that is approved for the
treatment of excessive sleepiness in people with narcolepsy, Dinges said. His
lab is "trying to understand whether that drug used in healthy people can
promote cognitive capability but not have negative consequences."
Dinges has conducted experiments with soldiers, in which they stayed awake for
88 hours or about 3.5 days, while taking modafinil. He could not divulge the
details of the results because the study has not yet been published. However, he
said, modafinil "looks promising."
Although modafinil might not be the final solution for improving soldier
performance under sleep deprivation conditions, Dinges said, "The potential for
finding additional medicines that are very specifically targeting areas of brain
that are involved in keeping you awake ... is very, very good."
"Over the next 10 years I think we're going to see one or two things come along"
that safely promote wakefulness, he said.
LOAD-DATE: March 27, 2003
LANGUAGE: ENGLISH
Copyright 2003 U.P.I.
837 of 998 DOCUMENTS
Times Colonist (Victoria, British Columbia)
March 24, 2003 Monday Final Edition
Doctors worry over stimulant that has no 'crash' consequence
SOURCE: CanWest News Service
BYLINE: Tom Spears
SECTION: Canada; Pg. B6
LENGTH: 1004 words
DATELINE: OTTAWA
OTTAWA - U.S. soldiers are staying awake for days and nights on end in Iraq, and
many are almost certainly benefiting from military research into pills that let
them work for 40 hours straight -- without feeling "wired" and without crashing
afterwards.
Soldiers in past wars have taken stimulants when they can't afford to fall
asleep, but these have all had side effects -- poor judgment, jumpiness and the
need for extra sleep as soon as the soldier stops popping them.
But the new stay-awake pills appear to have no side effects, at least in the
short term. They don't make people feel powerful or dizzy or happy or sexually
charged. There's no jumpiness, no wired feeling, no crashing later.
Modafinil just helps them stay awake and feel normal, though one sleep expert
says it delivers a kick like 20 cups of coffee.
U.S. military studies found that soldiers can stay awake and function alertly
for 40 hours, grab eight hours of sleep, and then stay awake for 40 more, all
without the impaired judgment of old-fashioned uppers.
That's beginning to scare some doctors, who say that modafinil, sold in Canada
as Alertec and in the U.S. as Provigil, may threaten the health of people who
abuse it.
Just as steroids help a body-builder pump iron longer, modafinil may help a
computer geek work all day and night at his screen without getting tired, but
also without a caffeine-style buzz or the side-effects of amphetamines.
Modafinil was designed to help people with narcolepsy stay awake. These people,
150,000 of them in the United States, sometimes fall asleep suddenly in the
middle of the day. Some doctors also prescribe modafinil to patients with
multiple sclerosis to help them feel less tired.
Modafinil is not addictive. But what happens when a student or an office worker
starts popping modafinil to stay awake for the next 30 or 40 hours, for the
deadline that just has to be met?
And what happens when there's another must-do job after that, and then another,
and another?
Increasingly, Americans who feel the need to stay awake, and who don't have a
serious sleep disorder, are getting "off-label" prescriptions for modafinil. In
other words, doctors are prescribing the drug for people for whom it was never
intended.
That's why there are 150,000 Americans with narcolepsy, but as many as 250,000
are getting regular prescriptions for modafinil.
The drug was first approved for use in Canada in 1999.
"I'm sure it's being used that way. I've heard about it anecdotally. You can
understand how hard it would be to study such a situation, particularly when
it's intermittent," says Dr. Tom Scammell, a sleep expert at Beth Israel
Deaconess Medical Center in Boston. "Most clinicians I talk to are really down
on that."
Less than a year ago, the U.S. supplier of the drug posted a summary of who was
taking it on their Web site, Scammell recalls. A quarter had narcolepsy, others
had multiple sclerosis, some had depression, "and then there was a large
category of 'other.'"
These include people taking the drug just because they want to stay awake, not
because they need it. While the drug itself may not be hurting them directly, he
feels that lack of sleep may be dangerous.
"In a nutshell, we do not know all of the consequences of sleep deprivation.
However, there are some consequences that are very clear. When somebody is sleep
deprived they become sluggish. Their reaction times are slower than usual. They
become clumsy. Somebody who's been sleep-deprived for just one night drives as
badly as somebody who is legally intoxicated.
"If you look at the number of cars accidents (as a rate), it's highest between 2
and 5 a.m. because people are sleepy."
People who are tired sometimes show blood-sugar levels similar to people with
diabetes.
"And there are some labs that have felt that they see differences in immune
function as well. And that certainly supports what everybody's grandmother would
tell them" i.e. that losing sleep may make you sick.
A Washington Post reporter who sat up for 30 hours on the drug happily wrote he
felt fine, adding: "Modafinil may have the power to change Washington, D.C., and
other high-powered cities."
That's where doctors fear the misuse may come from. It's not a "feel-good" drug,
but one that people may take if they're under heavy pressure to perform at work
or school.
"It's just one of these misuses, in my view, of a medical application. You could
probably get the same thing with 20 cups of coffee, but you wouldn't like it,"
says Dr. Judith Leech, a respirologist who sees patients with sleep disorders at
the Ottawa Hospital.
"Get some sleep! Don't use a pill to stay awake! Does that make good medical
sense? On the other hand, people will use it that way.
"I think sleep is a good thing. The healthy thing to do is to sleep more if
you're tired, right?
"Compared with other stimulants that have been prescribed, such as dexedrine and
ritalin, it (modafinil) doesn't work the same way so it doesn't have the same
side effects," she adds. It doesn't cause high blood pressure or feeling wired
-- all the effects that are part of the nervous system's "fight or flight"
reflex.
"On the other hand we don't really know which brain chemical it does work on.
Personally I'm not really big on stimulating people's brains with things I'm not
sure of, unless there's a medical indication."
Leech notes that soldiers have been offered drugs before to keep them awake: if
it isn't modafinil, it's something else that may in fact be worse, such as
amphetamines.
"On the other hand, what I use in somebody whose life is totally impaired by a
brain chemistry disorder is different from what I think you should use in an
army person" or other healthy people.
"It's bad to use drugs for bad reasons.
"There's a reason why we get sleepy." Sleep helps the brain store memories and
recuperate from work, and helps the body build its immune system. "And you
deprive yourself of those things if you use a stimulant to overcome it."
LOAD-DATE: March 24, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
838 of 998 DOCUMENTS
The Denver Post
March 23, 2003 Sunday 1ST EDITION
KEEPING TROOPS AWAKE, ALERT Anti-sleep drug getting unplanned use
BYLINE: Diedtra Henderson Denver Post Science Writer
SECTION: A SECTION; Pg. A-18
LENGTH: 987 words
Mere mortals might feel sleepy with just a few hours of lost shuteye, but the
armed forces expect no such weakness in fighters strapped into aircraft or
battling on the field.
The federal 'Continuous Assisted Performance' project is pursuing genetic
tinkering that would permit military pilots to fly 24-hour missions without any
sleep and without popping the amphetamine 'go' pills now the norm on lengthy
flights. And the Air Force is testing a new wonder drug that has the promise of
letting pilots remain awake and alert for up to four days without amphetamine's
side effects.
The research is happening against the backdrop of nighttime bombing missions in
Iraq and as a military court found insufficient evidence for criminal charges
against two F-16 pilots accused of killing four Canadians in a friendly fire
mishap an hour after the pilots popped 'go' pills.
The military researchers' ultimate goal: seven sleepless days for combat
troops, during which they don't lose the power to reason, react or realize the
impact of their actions.
Right now, popping a modafinil - a pill designed for people who fall deeply and
unexpectedly asleep - has the most promise.
Already an Army researcher at Alabama's Fort Rucker gave pilots modafinil.
Another group got nothing. The pilots were kept awake for 40 hours during which
they sat at flight simulators.
'When the pilots were not receiving the modafinil, they were having significant
problems staying awake - particularly when you got around that point of 3 in
the morning to noon the next day,' said researcher John Caldwell.
Instructions had to be repeated for unmedicated pilots, who also nodded off
during the simulated flight. Those pilots also flubbed basic flight
requirements: They couldn't maintain precise altitude, heading or air speed.
Modafinil 'wiped out' most of those effects, Caldwell said.
Canadian and French military forces have conducted similar research.
Caldwell's next research project using the drug, this time for the Air Force,
will do head-to-head tests comparing the effects of single doses of modafinil,
Dexedrine and caffeine tablets for military volunteers kept awake for 38 hours.
'Do you get the same amount of boost from these three doses and, if you do,
does the effect last the same?' Caldwell asked.
Popular media accounts - some using reporters who popped pills to see if they
could banish sleep - make Sheryl Williams, spokeswoman for the pharmaceutical
company Cephalon, hopping mad.
Cephalon has a pending application to expand the use of its modafinil drug,
Provigil, to medical conditions beyond narcolepsy. Williams fears that
recreational use by hard-charging civilians who want to make sleep optional
might put the FDA in a denying mood.
'We have not applied to have this drug used as a substitute for sleep, nor
would we ever do that,' Williams said. 'The biggest worry that we have is the
average American - that person who is out there reading these things, thinking
there is something out there they could take they could substitute for sleep.'
Sleep remains an uncharted frontier for science. Researchers haven't worked out
all of the whys and hows, but sleep is essential for humans and most other
animals. Deprive most living creatures of those restful, recharging hours, and
a cascade of problems begins, including memory loss, hobbled reason, impaired
judgment, reduced sexual capacity, weakened immunity - even early death.
Recent research suggests that the crux may not be the benefit of sleep but the
high cost of remaining awake.
'There seems to be a wear and tear of staying awake too long,' said Hans P.A.
Van Dongen, an assistant research professor at the University of Pennsylvania
school of medicine.
Tallying a high number of wide-
awake hours predicts almost precisely how poorly people will perform on
reaction tests. Recent work indicates that the brain builds up a certain
chemical as the body remains awake. Caffeine, as it turns out, binds to the
same receptor as that brain chemical, temporarily zapping its ability to turn
on sleep.
Still, clinical trials on how to keep troops fighting-sharp while
sleep-deprived continue at military bases.
Bomber missions, with aerial refueling, may extend 24 to 25 hours.
'In the case of a bomber, you usually have a two-person crew. You catch a
couple of hours here or there, but that's not a full, restful sleep,' said
Betty Anne Mauger, a spokeswoman for the Air Force surgeon general. 'The
overall thing we're dealing with is fatigue.'
Depending on the weight of the pilot and the individual's ground-
tested tolerance for amphetamines, a flight that long might mean popping 10
milligrams of Dexedrine every four hours.
Affidavits from experts presented in the friendly fire case suggested even such
low doses of amphetamines could contribute to muddled thinking and extreme
tunnel vision.
'Those negative effects would be enhanced by adding stress,' said Charles W.
Gittins, the attorney who represented Maj. Harry Schmidt, who dropped a
500-pound bomb on what he thought were Taliban forces.
Gittins said after the first Gulf War, an F-15C aircraft with the 58th Tactical
Fighter Squadron ran off the runway, a mishap tied by accident investigators to
the pilot's use of Dexedrine.
Air Force public affairs representatives from national headquarters, Eglin Air
Force Base - where the squadron is headquartered - and Langley Air Force Base,
which convened the investigation panel, couldn't immediately track down the
accident investigation summary.
Denver Post science writer Diedtra Henderson can be reached at
dhenderson@denverpost.com or at 303-820-1910.
LOAD-DATE: March 25, 2003
LANGUAGE: ENGLISH
GRAPHIC: PHOTO: Reuters/Russell Boyce A British pilot rests as he waits in his
Harrier GR-7 in Kuwait. The U.S. military is seeking ways to keep
sleep-deprived troops fighting-sharp.
Copyright 2003 The Denver Post
All Rights Reserved
839 of 998 DOCUMENTS
Ottawa Citizen
March 23, 2003 Sunday Final Edition
New drug may help soldiers stay awake: Doctors unsure of long-term effect
SOURCE: The Ottawa Citizen
BYLINE: Tom Spears
SECTION: News; Pg. A5
LENGTH: 831 words
U.S. soldiers are staying awake for days and nights on end in Iraq, and many are
almost certainly benefiting from military research into pills that let them work
for 40 hours straight, without feeling "wired" and without crashing afterward.
Soldiers in past wars have taken stimulants when they can't afford to fall
asleep, but these have all had side effects: poor judgment, jumpiness and the
need for extra sleep as soon as the soldier stops popping them.
But the new stay-awake pills appear to have no side effects, at least in the
short term.
U.S. military studies found that soldiers can stay awake and function alertly
for 40 hours, get eight hours of sleep, and then stay awake for 40 more, all
without the impaired judgment of old-fashioned uppers.
That's beginning to scare some doctors, who say that modafinil, sold in Canada
as Alertec and in the U.S. as Provigil, might threaten the health of people who
abuse it.
Modafinil is designed to help people with narcolepsy stay awake. These people,
150,000 of them in the United States, sometimes fall asleep suddenly in the
middle of the day. Some doctors also prescribe modafinil to patients with
multiple sclerosis to help them feel less tired.
Modafinil is not addictive. But what happens when a student or an office worker
starts popping modafinil to stay awake for the next 30 or 40 hours for a
deadline project? And what happens if the cycle continues?
Increasingly, Americans who feel the need to stay awake, and who don't have a
serious sleep disorder, are getting "off-label" prescriptions for modafinil.
That's why there are 150,000 Americans with narcolepsy, but as many as 250,000
are using modafinil. The drug was first approved for use in Canada in 1999.
"I'm sure it's being used that way. You can understand how hard it would be to
study such a situation, particularly when it's intermittent," says Dr. Tom
Scammell, a sleep expert at Beth Israel Deaconess Medical Center in Boston.
"Most clinicians I talk to are really down on that."
Less than a year ago, the U.S. supplier of the drug posted a patient summary on
its Web site, Dr. Scammell recalls, showing one-quarter had narcolepsy, while
others had multiple sclerosis and some had depression.
"And then there was a large category of 'Other.'"
These include people taking the drug just because they want to stay awake, not
because they need it. And while the drug itself might not be hurting them
directly, he believes that lack of sleep might be dangerous.
"In a nutshell, we do not know all of the consequences of sleep deprivation.
However, there are some consequences that are very clear. When somebody is sleep
deprived they become sluggish. Their reaction times are slower than usual. They
become clumsy. Somebody who's been sleep-deprived for just one night drives as
badly as somebody who is legally intoxicated.
"If you look at the number of cars accidents (as a rate) it's highest between 2
and 5 a.m. because people are sleepy."
People who are tired sometimes show blood-sugar levels similar to people with
diabetes.
A Washington Post reporter who sat up for 30 hours on the drug happily wrote he
felt fine, adding: "Modafinil may have the power to change Washington, D.C., and
other high-powered cities."
Doctors fear the that modafinil, while not a "feel-good" drug, is one that
people may take if they're under heavy pressure.
"It's just one of these misuses, in my view, of a medical application. You could
probably get the same thing with 20 cups of coffee, but you wouldn't like it,"
says Dr. Judith Leech, a respirologist who sees patients with sleep disorders at
the Ottawa Hospital. "Get some sleep! Don't use a pill to stay awake! Does that
make good medical sense?
"I think sleep is a good thing. The healthy thing to do is to sleep more if
you're tired, right?"
"Compared with other stimulants that have been prescribed, such as dexedrine and
ritalin, it (modafinil) doesn't work the same way so it doesn't have the same
side effects," she adds. It doesn't cause high blood pressure or feeling wired,
all the effects that are part of the nervous system's "fight or flight" reflex.
"On the other hand we don't really know which brain chemical it does work on.
Personally I'm not really big on stimulating people's brains with things I'm not
sure of, unless there's a medical indication."
Dr. Leech notes that soldiers have been offered drugs before to keep them awake:
if it isn't modafinil, it may be something worse, such as amphetamines.
"On the other hand, what I use in somebody whose life is totally impaired by a
brain chemistry disorder is different from what I think you should use in an
army person" or other healthy people.
"It's bad to use drugs for bad reasons. There's a reason why we get sleepy."
Sleep helps the brain store memories and recuperate from work, and helps the
body build its immune system. "And you deprive yourself of those things if you
use a stimulant to overcome it."
LOAD-DATE: March 23, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: Oleg Popov, Reuters; U.S. soldiers, shown here removing an
injured prisoner near Basra, can't always sleep when they should. Modafinil
would allow them function well for up to 40 hours without 'crashing' afterwards.
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
840 of 998 DOCUMENTS
Slate Magazine
March 7, 2003, Friday
Wake Up, Little Susie
BYLINE: David Plotz
SECTION: superman
LENGTH: 1592 words
On most days, my accumulated sleep deficit and post-lunch stupor gang up on me
around 2 p.m., and I begin my slow fade. My eyes droop. Saliva dribbles onto my
sweater. If I were trying to write this sentence at 2 p.m. on a normal day, it
would read something like: If I were tryyyyyyyyyyyyyyy
But today, I am bright-eyed and bushy-tailed, a chatty Kathy with my
officemates, eager to spend all afternoon banging on the keyboard. (I normally
prefer chewing my fingers off to writing.) I am not exactly wired, but I'm more
alert, more focused, more Plotz-like. Today I am my own Superman, dosed on 100
milligrams of modafinil.
Every year, we need the same amount of sleep, and every year we get less. Since
the invention of artificial illumination, sleep has been a bear market. There
are many reasons we catch fewer Z's: Round-the-clock workplaces, longer
commutes, brighter lights, 24-hour Krispy Kreme stores, the Home Shopping
Network "the list goes on. According to University of Pennsylvania professor of
psychology David Dinges, Americans probably sleep about six and a half to seven
hours per night, compared to the more than eight hours our bodies want.
We have learned to cope with a regular sleep deficit, but we pay a price (and
not just $4.05 for the venti latte). Studies by Dinges and military scientists
have proved that performance deteriorates when you sleep less than eight hours.
People who rest seven or six or five hours a night may not feel tired, but their
thinking and dexterity are suffering. We medicate ourselves with caffeine, a
drug that raises alertness but at a cost of jitteriness, irregular heartbeat,
and addiction. Folks who really need to stay awake dope themselves with
amphetamines "stimulants that can ward off sleep for days but cause terrible
crashes when they wear off. (And we don't know what long-term damage they
cause.)
The military is enthralledwith the possibility of doing away with shut-eye. The
supersecret Defense Advanced Research Projects Agency is investigating drugs
that would keep soldiers awake for a week. The Air Force prescribes go pills
"small doses of the amphetamine Dexedrine "to pep up long-haul pilots. (But
hopped-up pilots may be dangerous: The American pilots who accidentally bombed
and killed Canadian soldiers last spring were taking go pills.)
Avoiding sleep for a week might be necessary in an extreme situation like war,
but the run-of-the-mill, office-working, wannabe Superman requires something
different. We don't want a pill that will keep us Exceling and Power Pointing
for three days straight. We just want something that makes us feel alert through
an entire normal day "a drug that makes us feel as lively for the 18-hour-day we
have to live as for the 16-hour-day we ought to live.
Hence my rendezvous with modafinil. The drug, made by Cephalon, is marketed
under the creepy, pharma-Orwellian name Provigil. The FDA approved it in 1998 to
treat narcolepsy, but it is starting to have a underground life as a pick-me-up
for the routinely sleep-deprived. The military has tested it heavily,
particularly on pilots.
The way modafinil works is not understood. It seems to slow the release of GABA,
a sleep promoter in the brain. It also may act on the histamine system, which is
connected to sleep regulation. What is clear is that modafinil differs from most
other pick-me-ups, which tend to be indiscriminate in their function.
Amphetamines like Dexedrine, for example, promote wakefulness by interfering
with uptake of the neurotransmitter dopamine, causing dopamine to flood the
brain. Dopamine, says Joyce Walsleben, director of the NYU Sleep Disorders
Center, is a broad hitter that sets the heart racing, causes twitchiness, and
makes you feel high. When the effect of such stimulants wears off, the crash is
nasty. Caffeine affects a different pathway, involving adenosine, but that, too,
spills over the brain's flood wall, making coffee drinkers jittery.
But modafinil tiptoes around dopamine, confining its activity to the particular
neurological processes connected to wakefulness. It doesn't seem to act as a
broad stimulant. (This is one reason, Walsleben says, that modafinil has not
become a street drug. Unlike cocaine or amphetamines, modafinil doesn't make you
feel high, and it acts very slowly, taking a couple of hours or more to kick
in.) Narcoleptics seem to love modafinil. (By boosting alertness throughout the
day, modafinil reduces the narcoleptic's compulsion to nod off.) Now doctors are
getting barraged by requests from regular folks who want to use it to cut down
on sleep.
The seduction of modafinil is that you can feel as peppy after six hours sleep
as you would after nine. (It may also have a more.) Doctors see modafinil as an
occasional pick-me-up. They doubt you could take the drug everyday without
consequences: Most sleep researchers agree that the longer sleep is necessary
for hormonal regulation, among other essential bodily functions. (Drugs aren't
the only way we may steal less sleep. Click to read about how we may enlist gene
therapy to help us stay awake.)
Tired of merely writing about enhancement (and tired, period), I decided to
conduct my own unscientific trial of modafinil. As the father of a 2-year-old, I
live in a constant haze of sleep deprivation. I vowed to take modafinil for a
week and see what happened. Could it transform a lazy, exhausted hack into a
brilliant Jeffrey Goldberg? Or recast a grouchy father into Superdad? I
persuaded my doctor "and no, you can't have his number "to prescribe me a week's
supply of Provigil, seven 200-milligram pills.
Here is the diary I kept.
Day 1, Monday 6:45 a.m.: Woken up by my daughter after the usual six and a half
hours.
7 a.m.: I open the bottle. The pills are monstrous. I start to chicken out. I've
never smoked pot, much less taken cocaine or amphetamines. I decide to halve the
dosage. When I cut the first pill with my pocketknife, half of it shoots off my
bureau, slides across the floor, and disappears under a dresser, no doubt to be
discovered and eaten by my daughter someday in the near future. I pop the other
100-milligram half.
10 a.m.: At the office. I've felt no rush, but alertness has snuck up on me. I
am incredibly attentive, but not on edge. I really, really feel like working, a
rare sensation.
12 p.m.: I reach for my usual lunchtime Coca-Cola, then think better of it.
Caffeine plus this sprightliness and I will be ping-ponging off the walls.
2 p.m.: This is when I usually fold. Today I am the picture of vivacity. I am
working about twice as fast as usual. I have a desperate urge to write, to make
reporting calls, to finish my expense account "activities I religiously avoid. I
find myself talking very loudly and quickly. A colleague says I am grinning like
a feral chipmunk.
6 p.m.: Annoyed to have to leave the office when there is all this lovely work
to do.
9 p.m.: Home. After dinner, I race upstairs to start working again. This is
totally out of character, especially on a Monday Night Football evening.
12 a.m.: I want the day to keep going but force myself to go to bed. I fall
asleep easily enough, but it's a weird night. I have lots of dreams, which is
unusual. All are about Getting Things Done.
Day 2, Tuesday6:30 a.m.: I wake up feeling good, cut another pill in two, and
pop a half.
9 a.m.-7 p.m.: I work like a fiend again. These have been the two most
productive days I've had in years. Idea for new Provigil ad slogan: Bosses'
Little Helper.
1 a.m.: Again I'm alert through the late evening "so alert that I infuriate my
wife by chattering at her long past her bedtime. This time, when I do conk out,
I sleep deeply.
Day 3, Wednesday7 a.m.: My one-man clinical trial starts to fall apart. Everyone
says modafinil is not addictive, but I wake up worried about how long my supply
will last. I count the pills and realize I have only five and a half left.
That's just an 11-day supply. I remember that I offered a sample to a friend
yesterday. I am annoyed "one day less for me. I start to cut up the remaining
pills, wondering if I can divide them into thirds instead of halves.
I realize that maybe I can find a different supplier. I log onto the Internet to
see if I can get modafinil on the sly. I find it cheap at the Discount Mexican
Pharmacy. I feel delighted and relieved. Then I feel terrified that I am
delighted and relieved. Discount Mexican Pharmacy?!
7:30 a.m.: I end my experiment after two days. I am acting like a lunatic. I
stash the remaining pills in a distant corner of the medicine cabinet. I calm
myself with the reminder that I have 11 more great days to look forward to.
So is modafinil a drug for future superpeople? Maybe. There are good reasons for
doubt, though. The drug is approved only for treating narcolepsy, and doctors
are not going to prescribe it like aspirin anytime soon. Though patients don't
seem to get addicted to modafinil or to build a tolerance, according to
Walsleben, the drug has been in use for only 10 years, and no one knows for
certain that it's safe over the long term. (Cephalon and other drug companies,
incidentally, are working on even more powerful wakefulness drugs, but none is
on the market yet.)
I loved taking modafinil for two days. I worked supernaturally hard and well.
But I'd be afraid to make it a habit. I'll use it again for a special occasion
"when I am late for a deadline, perhaps. In the meantime, I'll just yawn my way
through the midafternoon.
LOAD-DATE: March 13, 2003
LANGUAGE: ENGLISH
Copyright 2003 Washingtonpost.Newsweek Interactive Company,
LLC. All rights reserved
841 of 998 DOCUMENTS
Washington Drug Letter
February 17, 2003
CEPHALON PLANS VIGOROUS DEFENSE OF MODAFINIL PATENT
SECTION: Vol. 35, No. 7
LENGTH: 163 words
The first abbreviated new drug application (ANDA) for a generic version of
Cephalon's narcolepsy drug Provigil (modafinil) has been accepted by the FDA,
the biopharmaceutical firm announced.
The identity of the generic applicant was not immediately available. Cephalon
said that even if the FDA approves the ANDA, it would be years before a generic
equivalent could be sold in the U.S. The composition patent for modafinil in
Provigil does not expire until 2014, the company said.
The FDA has also granted Provigil orphan drug exclusivity, which prevents the
approval of any ANDAs for a modafinil product until at least December 2005.
"We have anticipated the possibility of a filing for some time, and we believe
that our patent position for this product is strong," said John Osborn, senior
vice president and general counsel of Cephalon. The company launched Provigil in
1999. The drug had U.S. sales of more than $200 million last year, according to
the firm.
LOAD-DATE: February 28, 2003
LANGUAGE: ENGLISH
Copyright 2003 Washington Business Information, Inc., All Rights Reserved
842 of 998 DOCUMENTS
Generic Line
February 12, 2003
CEPHALON VOWS TO DEFEND MODAFINIL ON GENERIC CHALLENGE
SECTION: Vol. 20, No. 3
LENGTH: 157 words
The FDA has accepted the first ANDA for a generic version of Cephalon's
narcolepsy drug Provigil (modafinil), the biopharmaceutical firm announced last
week.
The identity of the generic applicant was not disclosed. Cephalon said that even
if the FDA approves the ANDA, it would be years before a generic equivalent
could be sold in the U.S.
The composition patent for the modafinil ingredient does not expire until 2014,
the company said. The FDA has also granted Provigil orphan drug exclusivity,
which prevents the approval of any ANDAs for a modafinil product until at least
December 2005.
"We have anticipated the possibility of a filing for some time, and we believe
that our patent position for this product is strong," said John Osborn, senior
vice president and general counsel of Cephalon.
The company launched Provigil in 1999. The drug had U.S. sales of more than $200
million last year, according to the firm.
LOAD-DATE: February 28, 2003
LANGUAGE: ENGLISH
Copyright 2003 Washington Business Information, Inc., All Rights Reserved
843 of 998 DOCUMENTS
Espicom Business Intelligence
February 10, 2003
Cephalon learns of generic modafinil filing
LENGTH: 162 words
The FDA has accepted an ANDA for a generic form of modafinil, the active
ingredient found in Cephalon's Provigil Tablets (C-IV).
Provigil is protected in the US by a patent that does not expire until 2014 and
that covers the pharmaceutical composition of the form of modafinil contained in
Provigil. The product was also granted orphan drug exclusivity that prevents the
approval of any ANDA for a modafinil product prior to June 2006, provided the
FDA grants the company a 6-month extension to the December 2005 orphan drug
exclusivity upon completion of a paediatric study.
Provigil was approved by the FDA for the treatment of excessive daytime
sleepiness associated with narcolepsy in December 1998 and was launched in the
US by Cephalon in February 1999. In December 2002, the company filed an sNDA
with the FDA seeking to expand its US labelling to cover the treatment of
excessive sleepiness associated with disorders of sleep and wakefulness in
adults.
LOAD-DATE: February 11, 2003
LANGUAGE: ENGLISH
Copyright 2003 ESPICOM Business Intelligence Ltd.
844 of 998 DOCUMENTS
Calgary Herald (Alberta, Canada)
February 6, 2003 Thursday Final Edition
Latest 'go' pill has few side-effects
SOURCE: Ottawa Citizen
BYLINE: Joanne Laucius
SECTION: Vitality; Pg. E4
LENGTH: 422 words
DATELINE: OTTAWA
A prescription drug being touted as the next lifestyle drug can keep you up all
day and all night. And all day and all night again.
Modafinil has been proven to keep military helicopter pilots awake for almost
two days straight while still performing complex tasks.
It is being tested on soldiers, medical staff and truck drivers. There have been
predictions it may soon be used to perk up drowsy shift workers and students
cramming for exams.
Modafinil -- marketed as Provigil in the U.S. and Alertec in Canada -- has the
same effect as six cups of coffee, but it doesn't leave the user feeling
jittery.
So far, it has only been approved to treat a few sleep-related disorders,
including narcolepsy, which causes people to fall asleep suddenly.
Studies, including one conducted in Ottawa about five years ago, showed
modafinil was not addictive.
Unlike amphetamines, it didn't affect blood pressure or cause irritability,
cognitive problems or psychotic episodes. There were some side-effects,
including dizziness and headaches.
And, although it has been called a stimulant, it isn't, said neurologist Dr.
Roger Broughton, the founding president of the Canadian Sleep Society. It's a
"wake-maintaining substance."
Broughton sees potential uses for modafinil -- and truck drivers and sleepy
students aren't among them.
On the other hand, modafinil may be valuable for soldiers in combat and for
police and firefighters in civilian disaster situations.
"If it's proven that in the military vein it helps soldiers and airmen stay
awake in combat without harm or side-effects, that's a rational use," said
Broughton, who is the medical director of the Sleep Medicine Centre in Ottawa.
But, for casual use, a lot more work has to be done.
"We don't know the long-term effects of the drug. The fact that a lot of sleepy
people want this drug doesn't mean they need access."
In the U.S., there has been speculation that modafinil is being used for
unapproved purposes.
About 150,000 people have narcolepsy, but the drug's manufacturer, Cephalon,
reports 250,000 new modafinil users every three months.
Even Cephalon senior vice-president Paul Blake has said he is concerned about
the casting of the drug as an alternative to a good night's rest.
Meanwhile, Broughton says the drug has proved effective for several other uses
that have not yet received approval, including treatment for fatigue and
sleepiness in patients with attention deficit hyperactivity disorder, multiple
sclerosis and Parkinson's disease.
LOAD-DATE: February 6, 2003
LANGUAGE: ENGLISH
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
845 of 998 DOCUMENTS
PR Newswire
February 5, 2003 Wednesday
Cephalon, Inc. Learns of Generic Modafinil Filing;
Company Intends to Vigorously Defend the Product's 2014 Patent
SECTION: FINANCIAL NEWS
LENGTH: 729 words
DATELINE: WEST CHESTER, Pa. Feb. 5
Cephalon, Inc. (Nasdaq: CEPH) reported today that the U.S. Food and Drug
Administration (FDA) has accepted an abbreviated new drug application (ANDA) for
a generic form of modafinil, the active ingredient found in the company's
PROVIGIL(R) Tablets $(C-IV$).
Even if an ANDA application eventually is approved by the FDA, it will be years
before a generic equivalent modafinil product can be sold in the United States.
PROVIGIL is protected in the United States by a patent that does not expire
until 2014 and that covers the pharmaceutical composition of the form of
modafinil contained in PROVIGIL. PROVIGIL also was granted orphan drug
exclusivity that prevents the approval of any ANDA for a modafinil product prior
to June 2006, provided the FDA grants the company a six-month extension to the
December 2005 orphan drug exclusivity upon completion of a pediatric study.
"Wehave anticipated the possibility of a filing for some time, and we believe
that our patent position for this product is strong," said John E. Osborn,
Senior Vice President and General Counsel of Cephalon. "We will thoroughly
evaluate any filing when it becomes available to us, and we are prepared to
vigorously protect our intellectual property rights."
PROVIGIL was approved by the FDA for the treatment of excessive daytime
sleepiness associated with narcolepsy in December 1998 and was launched in the
United States by Cephalon in February 1999. In December 2002, the company filed
a Supplemental New Drug Application with the FDA seeking to expand its U.S.
labeling to cover the treatment of excessive sleepiness associated with
disorders of sleep and wakefulness in adults.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,500 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon also has European operations in the United Kingdom, France and Germany.
The company currently markets three proprietary products in the United States:
PROVIGIL, GABITRIL(R) (tiagabine hydrochloride) and ACTIQ(R) (oral transmucosal
fentanyl citrate) $(C-II$) and more than 20 products internationally. Further
information about Cephalon and full prescribing information on its U.S. products
is available at www.cephalon.com or by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding potential generic competition and our responses
thereto, the strength of the PROVIGIL patent position, anticipated scientific
progress on its research programs, development of potential pharmaceutical
products, interpretation of clinical results, prospects for regulatory approval,
manufacturing development and capabilities, market prospects for its products,
sales and earnings guidance, and other statements regarding matters that are not
historical facts. You may identify some of these forward-looking statements by
the use of words in the statements such as "anticipate," "estimate," "expect,"
"project," "intend," "plan," "believe" or other words and terms of similar
meaning. Cephalon's performance and financial results could differ materially
from those reflected in these forward-looking statements due to general
financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties facing Cephalon such as those set forth in its reports on Form
8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange Commission. Given
these risks and uncertainties, any or all of these forward-looking statements
may prove to be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
SOURCE Cephalon, Inc.
CONTACT: Media: Robert Grupp, +1-610-738-6402 or rgrupp@cephalon.com; or
Investors: Robert S. (Chip) Merritt, +1-610-738-6376 or cmerritt@cephalon.com,
both of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: February 6, 2003
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2003 PR Newswire Association, Inc.
846 of 998 DOCUMENTS
St. John's Telegram (Newfoundland)
January 31, 2003 Friday Final Edition
Awake, but not wired: Studies show the drug modafinil perks up the drowsy with
few side-effects
SOURCE: Southam Newspapers
BYLINE: Joanne Laucius
SECTION: Lifestyles; Pg. B6
LENGTH: 498 words
DATELINE: OTTAWA
OTTAWA - A prescription drug being touted as the next lifestyle drug can keep
you up all day and all night. And all day and all night again.
Modafinil has already been proven to keep military helicopter pilots awake for
almost two days straight while still performing complex tasks.
It is being tested on soldiers, medical staff and truck drivers. There have been
predictions it may soon be used to perk up drowsy shift workers and even
students cramming for exams.
Modafinil -- marketed as Provigil in the U.S. and Alertec in Canada -- has the
same effect as six cups of coffee, but it doesn't leave the user feeling
jittery.
So far, however, it has only been approved to treat a few sleep-related
disorders including narcolepsy, which causes people to fall asleep suddenly.
It has been used in France for about 15 years. Studies, including one conducted
in Ottawa about five years ago, showed modafinil was not addictive.
Unlike amphetamines, it didn't affect blood pressure or cause irritability,
cognitive problems or psychotic episodes. There were some side-effects,
including dizziness and headaches.
And although it has been called a stimulant, it isn't, said neurologist Dr.
Roger Broughton, the founding president of the Canadian Sleep Society. It's a
"wake-maintaining substance."
Broughton sees potential uses for modafinil -- and truck drivers and sleepy
students aren't among them.
On the other hand, modafinil may be valuable for soldiers in combat and for
police and firefighters in civilian disaster situations.
"If it's proven that in the military vein it helps soldiers and airmen stay
awake in combat without harm or side-effects, that's a rational use," said
Broughton, who is the medical director of the Sleep Medicine Centre at the
Ottawa Hospital's General campus. "You don't want pilots to be sleepy when
they're at war."
But for casual use, a lot more work has to be done.
"People just want to pop a pill," said Broughton.
"We don't know the long-term effects of the drug. The fact that a lot of sleepy
people want this drug doesn't mean they need access."
In the U.S., there has already been speculation that modafinil is being used for
unapproved purposes.
About 150,000 people have narcolepsy, but the drug's manufacturer, Cephalon,
reports 250,000 new modafinil users every three months.
Even Cephalon senior vice-president Paul Blake has said he is concerned about
the casting of the drug as an alternative to a good night's rest.
"Provigil is not a substitute for sleep," he said earlier this month.
Meanwhile, Broughton says the drug has proved effective for several other uses
that have not yet received approval, including treatment for fatigue and
sleepiness in patients with attention deficit hyperactivity disorder, multiple
sclerosis and Parkinson's disease.
As for demand outside of its approved uses, he hasn't seen it.
"It's a controlled drug -- which is controlled as much as narcotics. That's the
law for the moment."
LOAD-DATE: January 31, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: Southam News; Modafinil can keep you up for days, with no
jitters and few side-effects, but sleep specialists still say nothing beats a
good night's sleep.
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
847 of 998 DOCUMENTS
Ottawa Citizen
January 29, 2003 Wednesday Final Edition
Awake, but not wired: Studies show drug perks up the drowsy with few side
effects
SOURCE: The Ottawa Citizen
BYLINE: Joanne Laucius
SECTION: News; Pg. A12
LENGTH: 500 words
A prescription drug being touted as the next lifestyle drug can keep you up all
day and all night. And all day and all night again.
Modafinil has already been proven to keep military helicopter pilots awake for
almost two days straight while still performing complex tasks.
It is being tested on soldiers, medical staff and truck drivers. There have been
been predictions it may soon be used to perk up drowsy shift workers and even
students cramming for exams.
Modafinil -- marketed as Provigil in the U.S. and Alertec in Canada -- has the
same effect as six cups of coffee, but it doesn't leave the user feeling
jittery.
But so far, it has only been approved to treat a few sleep-related disorders
including narcolepsy, which causes people to fall asleep suddenly.
It has been used in France for about 15 years. Studies, including one conducted
in Ottawa about five years ago, showed modafinil was not addictive.
Unlike amphetamines, it didn't affect blood pressure or cause irritability,
cognitive problems or psychotic episodes. There were some side effects,
including dizziness and headaches.
And although it has been called a stimulant, it isn't, said neurologist Dr.
Roger Broughton, the founding president of the Canadian Sleep Society. It's a
"wake-maintaining substance."
Dr. Broughton sees potential uses for modafinil -- and truck drivers and sleepy
students aren't among them.
On the other hand, modafinil may be valuable for soldiers in combat and for
police and firefighters in civilian disaster situations.
"If it's proven that in the military vein it helps soldiers and airmen stay
awake in combat without harm or side effects, that's a rational use," said Dr.
Broughton, who is the medical director of the Sleep Medicine Centre at the
Ottawa Hospital's General campus. "You don't want pilots to be sleepy when
they're at war."
But for casual use, a lot more work has to be done.
"People just want to pop a pill," said Dr. Broughton.
"We don't know the long-term effects of the drug. The fact that a lot of sleepy
people want this drug doesn't mean they need access. "
In the U.S., there has already been speculation that modafinil is being used for
unapproved purposes.
About 150,000 people have narcolepsy, but the drug's manufacturer, Cephalon,
reports 250,000 new modafinil users every three months.
Even Cephalon senior vice-president Paul Blake has said he is concerned about
the casting of the drug as an alternative to a good night's rest.
"Provigil is not a substitute for sleep," he said earlier this month.
Meanwhile, Dr. Broughton says the drug has proved effective for several other
uses that have not yet received approval, including treatment for fatigue and
sleepiness in patients with attention deficit hyperactivity disorder, multiple
sclerosis and Parkinson's disease.
As for demand outside of its approved uses, he hasn't seen it.
"It's a controlled drug -- which is controlled as much as narcotics. That's the
law for the moment."
LOAD-DATE: January 29, 2003
LANGUAGE: ENGLISH
GRAPHIC: Photo: The Ottawa Citizen; Modafinil can keep you up for days, with no
jitters and few side effects, but sleep specialists still say nothing beats a
good night's sleep.
TYPE: News
Copyright 2003 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
848 of 998 DOCUMENTS
San Mateo County Times (San Mateo, CA)
January 25, 2003 Saturday
Military researching pilot fatigue
BYLINE: By John Jurgensen
SECTION: MORE HEADLINE NEWS
LENGTH: 703 words
HARTFORD COURANT
Along with the beef stew and peanut butter bundled into their rations, Persian
Gulf War soldiers had instant coffee to keep them going. Lacking hot water, many
ripped open the packets of Taster's Choice and swallowed the dry coffee
crystals.
Thousands of feet above the ground forces, where the stakes were higher, Air
Force pilots were gulping amphetamine pills issued by military physicians. The
"go pills" helped fliers stay alert during the long, grueling combat sorties.
More than a decade later, despite steady advancements in weaponry, the strategy
behind keeping soldiers awake has barely changed. Nor has it since World War II,
when amphetamines were first doled out to U.S. troops. But the ongoing trial of
two Air Force pilots involved in a friendly-fire incident in Afghanistan a
formidable adversary, but the military is challenging it with new research.
Majs. Harry Schmidt and William Umbach face court-martial for dropping a
500-pound bomb on Canadian troops last April, killing four and wounding eight.
Their defense has contended that the amphetamines they took during a 20-hour
workday impaired their judgment. The Air Force dismisses the claim, describing
the drug as a "medical tool," prescribed in small[5-milligram], controlled
doses.
A majority of fighter pilots surveyed after Desert Storm said they used
stimulants, and 61 percent of those who did said stimulants were essential to
the missions.
John Caldwell, a research psychologist at Brooks Air Force Base in San Antonio,
puts exhausted pilots through round-the-clock missions in flight simulators
while evaluating their mood, cognition and performance. Although he defends the
military's use of go pills, he acknowledges new solutions are needed for the
age-old problem of staying awake.
"Every year we extend the duration of these missions," Caldwell said, citing the
experience of B-2 bomber pilots who may spend more than 30 hours in the cockpit.
Foremost, Caldwell prescribes careful scheduling, strategic napping and sound
sleep. For that, he's helped develop a computerized tool that will help
commanders predict the alertness of personnel in various scenarios.
But when shut-eye is nonexistent, the remedies are pharmacological. Because the
Army can't drop controlled substances into ration packs, caffeine will likely
remain the drowsy GI's drug of choice. But for Air Force pilots, Dexedrine
remains the "gold standard stimulant," according to Caldwell. "Any new
alertness-enhancing compound must be compared to dextro-amphetamine to ensure
that the new product is better and not just different."
Modafinil, a drug designed to help narcoleptics stay awake, has offered the most
promise. Though its workings remain mysterious, modafinil causes wakefulness
with little disruption of sleep architecture, unlike amphetamines.
But Col. Gregory Belenky, a director of neuropsychiatry at Walter Reed Army
Institute of Research in Silver Spring, Md., doesn't think modafinil is much
better than a more historical stimulant. We compared caffeine to modafinil. In
our study, we did not see any difference.
Modafinil has less potential for abuse than amphetamines, but because physicians
must administer it, its widespread use on the battlefield presents a logistical
challenge, Belenky said.
Looking for other creative ways to overcome the limits of biology, the U.S.
Defense Advanced Research Projects Agency has sponsored studies investigating
the brain chemistry of sleepless migrating birds and the effects of magnetic
fields on neurons.
But at the Soldier Center of Excellence in Natick, Mass., researchers are
working with well-known substances to power up everyday rations. The trick, said
senior food technologist Jack Briggs, is making them taste good while achieving
the required shelf life. We need to ensure that after three years, what we want
to deliver is still there.
The results, including ERGO [a powdered drink] and HooAH [an energy bar], are
battle-ready improvements on products already on the market. They provide a
potent fuel of carbohydrates, lipids, protein and, of course, caffeine.>
Distributed by the Los Angeles Times-Washington Post News Service
LOAD-DATE: June 17, 2003
LANGUAGE: ENGLISH
Copyright 2003 MediaNews Group, Inc. and ANG Newspapers
849 of 998 DOCUMENTS
Espicom Business Intelligence
December 20, 2002
Cephalon reacquires rights to modafinil in European markets
LENGTH: 155 words
Cephalon has reacquired all rights to modafinil in Germany and Spain. Cephalon
markets modafinil in the US under the brandname Provigil. The company reacquired
rights to modafinil in Germany, Austria, Switzerland and certain countries in
Central and Eastern Europe from Merckle and in Spain from Cepa Schwarz Pharma.
Financial terms were not disclosed. Merckle and Cepa acquired marketing rights
to the drug from Laboratoire L Lafon in 1993. Cephalon acquired Lafon in 2001.
Modafinil is marketed in Europe for the treatment of excessive daytime
sleepiness associated with narcolepsy, under the brandnames Provigil in the UK,
Modiodal in France and Spain, Vigil in Germany, and Modasomil in Austria and
Switzerland. Earlier this month, Cephalon also received marketing approval in
the UK to expand the label of the product to treat excessive daytime sleepiness
in patients with obstructive sleep apnea/hypopnea syndrome.
LOAD-DATE: December 20, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
850 of 998 DOCUMENTS
PR Newswire
December 18, 2002 Wednesday
Cephalon Reacquires Rights to Modafinil in Major European Markets;
Product Rights in Additional Countries Further Strengthens Cephalon's
International Marketing Presence
SECTION: FINANCIAL NEWS
LENGTH: 876 words
DATELINE: WEST CHESTER, Pa. Dec. 18
Cephalon, Inc. (Nasdaq: CEPH), an international biopharmaceutical company,
announced that it has reacquired all rights to modafinil in Germany and Spain,
two of Europe's largest pharmaceutical markets. Cephalon markets modafinil in
the United States under the brand name PROVIGIL(R) (modafinil) tablets $(C-IV$).
The company reacquired rights to modafinil in Germany, Austria, Switzerland and
certain countries in Central and Eastern Europe from Merckle GmbH, and in Spain
from Cepa Schwarz Pharma. Financial terms of the agreements were not disclosed.
Merckle and Cepa Schwarz Pharma acquired marketing rights to the drug from
Laboratoire L. Lafon in 1993. Cephalon acquired Lafon in 2001.
"We have made tremendous progress this year in our strategy to consolidate
worldwide rights for all of our marketed products," said Frank Baldino, Jr.,
Chairman and CEO of Cephalon. "Modafinil already is an important contributor to
our European business in the United Kingdom and France. This marketing
experience, together with the product's excellent performance in the United
States, should enable us to effectively position modafinil in these additional
European markets."
Modafinil is marketed in Europe for the treatment of excessive daytime
sleepiness associated with narcolepsy, under the brand names PROVIGIL in the
United Kingdom, MODIODAL(R) in France and Spain, VIGIL(R) in Germany, and
MODASOMIL(R) in Austria and Switzerland. Earlier this month, Cephalon also
received marketing approval in the United Kingdom to expand the label of
PROVIGIL to treat excessive daytime sleepiness in patients with obstructive
sleep apnea/hypopnea syndrome.
In the past year, Cephalon has significantly expanded its international
business and now holds extensive European and Asian rights to the three products
that it markets in the United States: PROVIGIL, ACTIQ, and GABITRIL. In October,
Cephalon reacquired all rights to ACTIQ in 12 countries, principally in Europe.
In January, Cephalon acquired worldwide rights to GABITRIL (excluding Canada,
Latin America, and Japan). In December 2001, Cephalon purchased Laboratoire L.
Lafon and acquired control of worldwide rights to PROVIGIL.
PROVIGIL
PROVIGIL is the first in a new class of wake-promoting agents. While its exact
mechanism of action is not known, the drug acts selectively in areas of the
brain believed to regulate normal wakefulness. Launched in the United States in
February 1999, the drug is currently approved in more than 20 countries for the
treatment of excessive daytime sleepiness associated with narcolepsy. For full
prescribing information about PROVIGIL, please visit http://www.PROVIGIL.com.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs more than 1,200 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England,
Martinsried, Germany, and at Laboratoire L. Lafon in Maisons-Alfort, France.
Further information about Cephalon and full prescribing information on its U.S.
products is available at www.cephalon.com or by calling +1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release contains forward-looking statements. Forward-looking statements provide
Cephalon's current expectations or forecasts of future events. These may include
statements regarding anticipated scientific progress on its research programs,
development of potential pharmaceutical products, interpretation of clinical
results, prospects for regulatory approval, manufacturing development and
capabilities, market prospects for its products, including its ability to
favorably position modafinil in Europe, sales and earnings projections including
the impact of the German operations on Cephalon's business, the importance of
PROVIGIL, ACTIQ and GABITRIL and other marketed products to Cephalon's European
territories and other statements regarding matters that are not historical
facts. Cephalon's performance and financial results could differ materially from
those reflected in these forward-looking statements due to general financial,
economic, regulatory and political conditions affecting the biotechnology and
pharmaceutical industries, as well as more specific risks and uncertainties such
as those set forth below and in its reports on Form 8-K, 10-Q and 10-K filed
with the U.S. Securities and Exchange Commission. Given these risks and
uncertainties, any or all of these forward-looking statements ultimately may
prove to be incorrect. Therefore, you should not rely on any such factors or
forward- looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The U.S.
Private Securities Litigation Reform Act of 1995 permits this discussion.
MAKE YOUR OPINION COUNT - Click Here
http://tbutton.prnewswire.com/prn/11690X45175747
SOURCE Cephalon, Inc.
CONTACT: Robert W. Grupp, +1-610-738-6402 or rgrupp@cephalon.com, or Investor
Contact, Chip Merritt, +1-610-738-6376 or cmerritt@cephalon.com, both of
Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: December 19, 2002
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2002 PR Newswire Association, Inc.
851 of 998 DOCUMENTS
Health Media Group Media Watch Services
December 13, 2002
Modafinil approved for sleep apnoea
SOURCE: Doctor 12/12/02; p.6
SECTION: Health Media Group Media Watch Services
LENGTH: 66 words
Modafinil (Provigil), used to treat narcolepsy, can now be prescribed for sleep
apnoea. It is estimated that 30 per cent of sleep apnoea patients do not respond
to continuous positive airways pressure, and the use of modafinil will be of
benefit to them. Initially the drug will be prescribed by specialists as a
second-line treatment for daytime sleepiness associated with sleep apnoea.
LOAD-DATE: December 16, 2002
Copyright Health Media Ltd 2002
852 of 998 DOCUMENTS
Health Media Group Media Watch Services
December 13, 2002
Modafinil approved for sleep apnoea
SOURCE: Doctor 12/12/02; p.6
BYLINE: Health Newswire reporters
SECTION: Health Media Group Media Watch Services
LENGTH: 66 words
Modafinil (Provigil), used to treat narcolepsy, can now be prescribed for sleep
apnoea. It is estimated that 30 per cent of sleep apnoea patients do not respond
to continuous positive airways pressure, and the use of modafinil will be of
benefit to them. Initially the drug will be prescribed by specialists as a
second-line treatment for daytime sleepiness associated with sleep apnoea.
LOAD-DATE: March 31, 2003
Copyright Health Media Ltd 2002
853 of 998 DOCUMENTS
PR Newswire
December 3, 2002 Tuesday
Cephalon Receives Approval to Expand Marketing of Provigil in the United
Kingdom;
-Drug to be marketed for Obstructive Sleep Apnea Hypopnea Syndrome and
Narcolepsy -
SECTION: FINANCIAL NEWS
LENGTH: 958 words
DATELINE: WEST CHESTER, Pa. Dec. 3
Cephalon, Inc. (Nasdaq: CEPH) today announced that it has received marketing
approval from the Medicines Control Agency (MCA) in the United Kingdom to expand
the label of PROVIGIL(R) (modafinil) to treat excessive daytime sleepiness in
patients with obstructive sleep apnea/hypopnea syndrome. The 200 mg tablet of
PROVIGIL was also approved, in addition to the 100 mg dosage currently available
in this territory. Cephalon UK Limited will officially launch the new indication
at a symposium during the British Thoracic Society meeting being held December
4-6 in London.
"We are pleased that the data used to support this label expansion was accepted
by the UK regulatory authority," said Paul Blake, MB, FRCP, Senior Vice
President of Clinical Research and Regulatory Affairs at Cephalon. "Achievement
of this milestone will enable us to grow the market for modafinil in the United
Kingdom and sets the stage for regulatory submissions in other European
countries over the next year."
The UK approval is the first of two regulatory milestones that Cephalon expects
to achieve this year for PROVIGIL. Cephalon intends to file an application with
the U.S. Food and Drug Administration at year-end seeking to expand the label of
PROVIGIL to include treatment of excessive sleepiness associated with sleep
disorders beyond narcolepsy.
PROVIGIL
Modafinil is the first in a new class of wake-promoting agents and is currently
approved in more than 20 countries for the treatment of excessive daytime
sleepiness associated with narcolepsy. PROVIGIL was initially launched in the UK
in 1998 for the treatment of narcolepsy.
In controlled clinical trials, PROVIGIL has been found to be generally well
tolerated with a low incidence of adverse events relative to placebo. The most
commonly observed adverse events associated with the use of PROVIGIL were
headache, infection, nausea, nervousness, anxiety and insomnia.
Obstructive Sleep Apnea Hypopnea Syndrome
Obstructive sleep apnea/hypopnea syndrome is a serious and potentially
life-threatening sleep disorder affecting four percent of middle-aged men and
two percent of middle-aged women. Individuals with obstructive sleep apnea
hypopnea syndrome experience frequent awakenings throughout the night as a
result of blockage of the airway during sleep. This disruption of sleep leads to
excessive daytime sleepiness causing many people to doze off repeatedly
throughout the day -- at their jobs and at home.
The most commonly used standard treatment is continuous positive airway pressure
(CPAP). A nasal CPAP device can prevent airway closure while in use, but despite
this treatment many patients continue to experience residual excessive
sleepiness.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc., is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain. Cephalon employs 1,200
people in the United States and Europe. The company markets three proprietary
products in the United States and 22 products internationally. Full prescribing
information on Cephalon's US products is available by calling 1-800-896-5855.
Cephalon's biotechnology pipeline is focused on the identification of novel
molecules that affect cell survival and death. Additional information about
Cephalon and its subsidiaries can be obtained by visiting the company's Website
at http://www.cephalon.com .
Cephalon UK Limited has headquarters in Guildford and markets drugs to treat a
number of central nervous system disorders. In collaboration with Novartis,
Cephalon UK markets Tegretol(R) (carbamazepine), Ritalin(R) (methylphenidate),
Anafranil(R) (clomipramine) and Lioresal(R) (baclofen). Also included in this
collaboration is PROVIGIL (modafinil) for the UK. In addition, Cephalon UK also
markets Gabitril(R) (tiagabine monohydrate) and Actiq (R) (fentanyl -- as
citrate) in the UK and Ireland.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
projections, and other statements regarding matters that are not historical
facts. You may identify some of these forward-looking statements by the use of
words in the statements such as "anticipate," "estimate," "expect," "project,"
"intend," "plan," "believe" or other words and terms of similar meaning.
Cephalon's performance and financial results could differ materially from those
reflected in these forward-looking statements due to general financial,
economic, regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties such
as those set forth below and in its reports on Form 8-K, 10-Q and 10-K filed
with the U.S. Securities and Exchange Commission. Given these risks and
uncertainties, any or all of these forward-looking statements may prove to be
incorrect. Therefore, you should not rely on any such factors or forward-looking
statements. Furthermore, Cephalon does not intend to update publicly any
forward-looking statement, except as required by law. The Private Securities
Litigation Reform Act of 1995 permits this discussion.
MAKE YOUR OPINION COUNT - Click Here
http://tbutton.prnewswire.com/prn/11690X10888858
SOURCE Cephalon, Inc.
CONTACT: Media: Sheryl Williams +1-610-738-6493, swilliam@cephalon.com, or
Investors: Robert Chip Merritt, +1-610-738-6376, cmerritt@cephalon.com, both of
Cephalon, Inc.
URL: http://www.prnewswire.com
LOAD-DATE: December 4, 2002
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS, MEDICAL AND HEALTH EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2002 PR Newswire Association, Inc.
854 of 998 DOCUMENTS
Pharma Marketletter
November 11, 2002
Modafinil may have cognitive-enhancing effect
LENGTH: 157 words
Modafinil, the active ingredient in Cephalon's narcolapsy drug Provigil, may
have a cognition-enhancing effect, according to a study from the Department of
Psychiatry at the University of Cambridge, UK.
Data showed that modafinil appears to improve certain mental abilities, without
the common side effects noted by the use of other mental stimulants, such as
amphetamine.
Danielle Turner of the UoC took 60 healthy young men and tested them, using
touch-sensitive computer screens and easy-to-understand computer games, after
they had received either modafinil or placebo.
"In the study, the volunteers given modafinil performed significantly better in
neuropsychological tests involving short-term memory and showed less impulsive
responding and an increased tendency to reflect on the tasks they were given,"
she added.
Modafinil has also shown no evidence of addiction, one common side effect of
mental stimulants.
LOAD-DATE: November 12, 2002
LANGUAGE: ENGLISH
Copyright 2002 Marketletter Publications Ltd.
855 of 998 DOCUMENTS
Health Newswire Consumer
November 5, 2002
Sleep drug "boosts brain"
BYLINE: Deirdre Lee
SECTION: Health Newswire Consumer
LENGTH: 294 words
HIGHLIGHT: A drug normally prescribed to treat sleep disorders also boosts
certain mental abilities, a UK study suggests.
Researchers at Cambridge University found that volunteers who took a medication
called modafinil - normally prescribed for narcolepsy - showed improved ability
in planning complex problems, recalling long strings of numbers and remembering
abstract patterns.
The discovery could lead to new treatments for people with conditions such as
Attention Deficit Hyperactivity Disorder (ADHD), who suffer from selective
impairments in memory, problem solving and planning, say researchers.
The study involved 60 healthy young males who were tested using touch-sensitive
computer screens and easy-to-understand "computer games" after they had taken
either a dummy tablet (placebo) or modafinil.
Researcher Danielle Turner from the Department of Psychiatry says, "In the
study, the volunteers given modafinil performed significantly better at
neuropsychological tests involving short-term memory, and showed less impulsive
responding and an increased tendency to reflect on the tasks they were given."
Of particular importance was the discovery that modafinil seemed to make people
stop and think, say researchers. After taking it, the volunteers were
significantly better at inhibiting impulsive responding and reflecting on
problems. This could prove valuable for people with ADHD who have increased
impulsiveness, say researchers.
Encouragingly, modafinil also appeared to boost brainpower, with no evidence of
addiction and fewer side effects than mental stimulants previously prescribed,
like amphetamine.
"The next important step is to confirm these positive effects on mental
functioning (cognition) in patients," says Ms Turner. Future research will test
whether young adults with ADHD show similar improvements to the healthy
volunteers.
LOAD-DATE: January 15, 2003
Copyright Health Media Ltd 2002
856 of 998 DOCUMENTS
Health Newswire Consumer
November 5, 2002
Sleep drug "boosts brain"
BYLINE: Deirdre Lee
SECTION: Health Newswire Consumer
LENGTH: 294 words
HIGHLIGHT: A drug normally prescribed to treat sleep disorders also boosts
certain mental abilities, a UK study suggests.
Researchers at Cambridge University found that volunteers who took a medication
called modafinil - normally prescribed for narcolepsy - showed improved ability
in planning complex problems, recalling long strings of numbers and remembering
abstract patterns.
The discovery could lead to new treatments for people with conditions such as
Attention Deficit Hyperactivity Disorder (ADHD), who suffer from selective
impairments in memory, problem solving and planning, say researchers.
The study involved 60 healthy young males who were tested using touch-sensitive
computer screens and easy-to-understand "computer games" after they had taken
either a dummy tablet (placebo) or modafinil.
Researcher Danielle Turner from the Department of Psychiatry says, "In the
study, the volunteers given modafinil performed significantly better at
neuropsychological tests involving short-term memory, and showed less impulsive
responding and an increased tendency to reflect on the tasks they were given."
Of particular importance was the discovery that modafinil seemed to make people
stop and think, say researchers. After taking it, the volunteers were
significantly better at inhibiting impulsive responding and reflecting on
problems. This could prove valuable for people with ADHD who have increased
impulsiveness, say researchers.
Encouragingly, modafinil also appeared to boost brainpower, with no evidence of
addiction and fewer side effects than mental stimulants previously prescribed,
like amphetamine.
"The next important step is to confirm these positive effects on mental
functioning (cognition) in patients," says Ms Turner. Future research will test
whether young adults with ADHD show similar improvements to the healthy
volunteers.
LOAD-DATE: March 31, 2003
Copyright Health Media Ltd 2002
857 of 998 DOCUMENTS
Espicom Business Intelligence
October 24, 2002
Cephalon achieves positive results in Provigil SWSD trial
LENGTH: 195 words
Results of Cephalon's clinical study evaluating Provigil (modafinil) C-IV in
patients with shift-work sleep disorder (SWSD) showed statistical significance
on both primary endpoints of the study. The 12-week, randomised, double-blind,
placebo-controlled study included 209 patients with an international
classification of sleep disorders (ICSD)-confirmed diagnosis of SWSD randomised
to either modafinil 200mg or placebo.
Patients in the study received modafinil or placebo as a single dose given prior
to the start of their night shift. The study showed that modafinil significantly
improved wakefulness compared to placebo, as measured by the Multiple Sleep
Latency Test (MSLT), an objective measure of sleepiness (p<0.01). In addition,
patients treated with modafinil showed significant improvement in their clinical
condition as measured by the CGI-C when compared to patients treated with
placebo (p<0.0001).
Modafinil was well tolerated. The most commonly reported adverse events in this
study were consistent with those described in the current product label. The
complete study data are expected to be presented at a major medical meeting in
2003.
LOAD-DATE: October 28, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
858 of 998 DOCUMENTS
The Sunday Times (Perth, Australia)
October 6, 2002, Sunday
US drug sales a wake-up call
BYLINE: Liam Bartlett
LENGTH: 800 words
So much to do, there's plenty on the farm
I'll sleep when I'm dead
Saturday night I like to raise a little harm
I'll sleep when I'm dead.
-- Warren Zevon
THE excitable boy had it just right. Hard workers or party animals with too much
to do and not enough time to do it in have only one choice -- delay the shut-eye
until you drop.
Unfortunately, Zevon now has terminal lung cancer so his options are almost up
but for the rest of the population, another possibility is coming soon to a
pharmacy near you.
From November, the Australian company CSL will sell a drug called Modafinil. In
local chemist shops it will be marketed under the trade name Modavigil and if
the American experience is any indication it is set to change the life of a lot
more people than it was
designed for.
Modafinil has been dubbed the two-days-awake pill because it artificially shuts
off your urge to sleep for at least 40 hours.
The tablet that challenges Mother Nature was originally tested on US army
helicopter pilots, allowing them to stay up safely for almost two days while
remaining alert, focused and as capable of solving complex problems as the well
rested.
Then, after a good eight hours sleep, they can get up and do it again -- for
another 40 hours, before finally catching up on their sleep.
Researchers claim Modafinil has the potential to replace caffeine because it
works without the jitter, buzz or addictive characteristics of caffeine and
causes none of the
euphoria, crash or potential for paranoid delusion of stimulants like
amphetamines or cocaine.
However, it does have the power to change the way we work and live and judging
by its usage patterns, the social impact might already have begun.
In the US, the sales of Modafinil have doubled over the past 12 months to $150
million.
While that might not sound huge given the size of the US pharmaceuticals market
it is certainly out of kilter with the drug's official reason for being.
The US Food and Drug
Administration has approved Modafinil marketing only to narcoleptics, who fall
asleep frequently and uncontrollably.
But at best estimate there are only 125,000 to 250,000 narcoleptics in America
and yet the drug's owners are claiming that more than a million prescriptions
have been written with sales now soaring.
Similarly here in Australia the numbers people put narcoleptics around 16,000 --
hardly a huge market for CSL to bother buying the exclusive licence and shunting
them into pharmacies at a wholesale price of $87.50 for 30 tablets.
No doubt they are punting on a range of other possibilities that this drug,
designed to help the sick, might have to augment the lives of the healthy.
We've already seen this happen with Viagra, where the social ends up outweighing
the medical.
In a world of increasing competition where there never seems to be enough hours
in the day, the potential for lifestyle usage is enormous.
Think of the long distance truckies or the taxi drivers who would be tempted to
see out a 40-hour shift in one hit.
What about students cramming for exams or hospital and emergency service
personnel who are already burning the candle at both ends?
I can imagine the odd Canberra lobbyist who would love to sit on the end of a
phone for two days without blinking.
And the expression "shop-till-you-drop" could take on an alarming new dimension
come Christmas.
More seriously, perhaps the whole concept of what is a "normal" human capability
is at stake as people are tempted to control their sleep in order to be more
competitive.
One could speculate that this medicine and other modified forms that will
undoubtedly follow, could create even more demand for people to be available
around the clock.
Nobody is saying exactly how Modafinil works and its long-term effects are
largely
unknown, but researchers marvel at the way it seems to target specific regions
of the brain believed to regulate normal wakefulness.
The US FDA has already had to warn Modafinil's owners, Cephalon that their
promotional material was overreaching their approved target of narcoleptics.
But in this country there are no such conditions placed on marketing under its
inclusion on the Australian Register of Therapeutic Goods.
Other than requiring a prescription from your local doctor, the great awakening
is easy at $3 a pop, plus whatever retail margin the pharmacists decide to add.
And this could be just the start.
More drugs in the pipeline include those that attack shyness, forgetfulness and
the mental decline of ageing.
Others add muscle mass and boost the ability to learn -- at least in mice. But
even mice need their sleep. Or do they?
* Liam Bartlett hosts the Statewide Morning Program on ABC Radio.
Email: liam@your.abc.net.au
LOAD-DATE: October 5, 2002
LANGUAGE: ENGLISH
JOURNAL-CODE: SDT
Copyright 2002 Nationwide News Pty Limited
859 of 998 DOCUMENTS
Deseret News (Salt Lake City)
September 22, 2002, Sunday
Narcolepsy pill may emerge as 'lifestyle' drug of the busy
BYLINE: By Carey Goldbert The Boston Globe
SECTION: WIRE; Pg. A08
LENGTH: 1327 words
Just to see what it was like, the Cambridge computer programmer stayed awake
four straight days. He felt fine, he reported later, not jittery, nicely
focused. "Imagine," he wrote in an e-mail, "having all the time you could want
to goof off, knowing that you still have just as much time as usual to spend on
things you have to do."
On the other hand, he added, "if you lack imagination and run out of things to
do, you could end up bored real fast."
The programmer, who asked that he not be identified, has not repeated his
"little experiment," partly because of its questionable legality. To stay awake,
he borrowed a prescription drug, modafinil, that is meant for narcoleptics,
whose affliction causes excessive sleepiness.
But he appears to have plenty of company in his desire to cheat time by cheating
sleep. In the three years since the drug was introduced under the brand name
Provigil for narcolepsy, sales have skyrocketed to more than 250,000
prescriptions every three months, outstripping the needs of the nation's
estimated 150,000 narcoleptics.
Cephalon, the company that makes Provigil, says the seemingly excess
prescriptions mainly go to patients with other diseases that cause fatigue.
But the buzz about modafinil as a potential elixir for millions of "sleep when I
die" Americans has been building for months. Some predict it may become the next
Viagra or Prozac, the next "lifestyle drug."
Sleep specialists hate that idea. Though modafinil causes few side effects, they
say, and though it shows little potential for addiction, using it lightly to
deprive the body of sleep, especially long-term, is asking for trouble.
Nonetheless, talk about modafinil has been spreading, including debates online
and in print about whether such a pill could be a dream come true for the
underslept or a nightmare for a society that is already running too fast.
A Washington Post reporter who tried staying up for two days on Provigil gave it
warm reviews in the paper, writing that "Modafinil may have the power to change
Washington, D.C., and other high-powered cities."
But then, he wrote that story during a 40-hour period of modafinil-enhanced
wakefulness, so his judgment may have been affected. Modafinil is believed to
target areas of the brain responsible for maintaining wakefulness more precisely
than caffeine or other stimulants, so it does not bring on a wired feeling or
later crash, but experts say it does not completely do away with all the mental
impairment that comes with sleep deprivation.
The military, too, has added to the attention paid modafinil by reporting
publicly that it has been testing the drug as "performance enhancement" for
combatants who must stay awake for days. It turned out that they could function
well for 40 hours, sleep eight hours, and then get up and go another 40 hours
before needing rest.
For all the talk, however, it remains unclear how much Provigil is already being
used by otherwise healthy sleep-cheaters.
Since the biotech firm Cephalon introduced Provigil in early 1999, the drug's
sales have jumped to a rate of $200 million per year if current sales keep up.
Quarterly sales are up about 70 percent over last year, and prescriptions are
now running at the rate of 250,000 in a three-month period, according to IMS
Health, a health information company.
Those numbers seem particularly high given that there are only an estimated
150,000 narcoleptics in the country. And company officials have acknowledged
that perhaps only a quarter of the prescriptions are going to narcoleptics.
But they also say that they are not encouraging the use of Provigil by people
who do not need it, and they have no indication that it is being widely abused.
Rather, they believe it is being prescribed "off-label" by doctors to help
patients with a variety of sleep disorders. And they are seeking approval from
the Food and Drug Administration to broaden Provigil's label to include a wider
variety of diseases that cause fatigue.
However, there is anecdotal evidence of a nonmedical demand for Provigil. For
example, Dr. Richard J. Castriotta, a sleep expert at the University of Texas,
said that a handful of people have asked him for a Provigil prescription just to
perk them up, but he has refused them. Meanwhile, Web sites offer to sell
Provigil without a prescription.
Modafinil may be OK for pilots or emergency workers, Castriotta said, but it
would be wrong "to make that leap and say, 'Well, gosh, why can't I just sleep
three hours a night as a way of life?' We don't know enough about sleep
deprivation to be able to determine what the long-range effects might be, and
that's very, very dangerous."
He and other researchers predicted that in any case, because Provigil is a
controlled substance, and because it brings users no euphoria, it is unlikely to
be very widely abused.
But in a country where more than half the population is averaging more than
three cups of coffee per day, it does seem to have broad potential appeal --
particularly for the truckers and students and new parents and others whose
lives sometimes require all-nighters.
International Antiaging Systems, a company that has one of the offshore pharmacy
Web sites that sell modafinil, says that its modafinil sales have at least
doubled in the last year, but it would not specify the numbers involved.
A swath of studies, many sponsored by Cephalon, are underway to see if Provigil
might help patients with the fatigue caused by diseases ranging from multiple
sclerosis to attention deficit to sleep apnea to depression. Much of the initial
research shows tentative promise.
Another set of extensive studies is looking at whether modafinil will help shift
workers who have to stay awake at times when their bodies beg to sleep. Their
numbers are estimated at about 15 million.
Provigil's side effects tend to be mild, Cephalon says, with headache and nausea
the most common. It can also interact poorly with some other drugs; in
particular, it can reduce the effects of birth control pills.
The prospect of Provigil or even better "wake-enhancing" drugs gaining broad
usage deeply concerns sleep specialists like Dr. Thomas Scammell of Beth Israel
Deaconess Medical Center, a leading authority on modafinil.
"For society, it does bring up a really key question," he said. "The simplest
way to answer it is to say, 'If I could give you a pill that would take away
your hunger, does that mean you shouldn't eat?' Well, duh, you've got to eat and
you know why, because you'll waste away."
"The problem," he added, "is that the science of sleep research hasn't reached
the point that we can say, 'If you don't get enough sleep, X, Y, and Z will
happen to you."
However, a growing body of research does indicate that lack of sleep may be even
more harmful than previously thought. It may be contributing to obesity by
changing the metabolisms of the underslept and to heart disease by causing
low-grade inflammation.
But Americans are nonetheless sleeping less and working more, according to the
National Sleep Foundation. Its polls have found that Americans sleep an average
of about seven hours a night during the work week, an hour and a half less than
in 1900, and that one third of adults are so sleepy in the daytime they could be
dangerous. Federal highway officials say lack of sleep causes 100,000 crashes a
year.
To Dr. Daniel F. Kripke, a sleep expert at the University of California at San
Diego, excitement over a new drug like modafinil is neither new nor very
exciting -- not to a veteran doctor who remembers when cocaine and amphetamines
spurred similar reactions.
"I think it is a promising drug but it has only been tested a little," said Dr.
Kripke, whose own research suggests that people who sleep somewhat less than
average may live longer.
"I'm very much in favor of broader scientific testing," he said, "but I'm not in
favor of people jumping off the deep end."
LOAD-DATE: September 22, 2002
LANGUAGE: ENGLISH
Copyright 2002 The Deseret News Publishing Co.
860 of 998 DOCUMENTS
Espicom Business Intelligence
September 17, 2002
Positive results for Provigil ADHD study
LENGTH: 181 words
Cephalon has released results from an investigational, multi-centre study in 248
children aged between 6 and 13 years. The results show that Provigil (modafinil)
tablets significantly improves symptoms of attention deficit hyperactivity
disorder (ADHD) in children.
In the 4-week, randomised, double-blind, placebo-controlled, parallel design
study, children and adolescents with ADHD were assigned to 1 of 4 dose regimens
of modafinil daily or placebo. The primary efficacy endpoint measure was the
teacher-completed school version of the ADHD Rating Scale IV. All of the
modafinil-treated groups showed a reduction in symptoms of ADHD, with certain
groups reaching statistical significance compared to placebo (p<0.05). The
greatest significance was achieved in the group assigned to modafinil 300mg once
daily (p<0.01). The drug was generally well tolerated and the side effects seen
were consistent with those described in the product label, with insomnia being
the most frequent. The complete study data are expected to be presented at a
major medical meeting in 2003.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
861 of 998 DOCUMENTS
Espicom Business Intelligence
September 17, 2002
Positive results for Provigil ADHD study
LENGTH: 181 words
Cephalon has released results from an investigational, multi-centre study in 248
children aged between 6 and 13 years. The results show thatProvigil (modafinil)
tablets significantly improves symptoms of attention deficit hyperactivity
disorder (ADHD) in children.
In the 4-week, randomised, double-blind, placebo-controlled, parallel design
study, children and adolescents with ADHD were assigned to 1 of 4 dose regimens
of modafinil daily or placebo. The primary efficacy endpoint measure was the
teacher-completed school version of the ADHD Rating Scale IV. All of the
modafinil-treated groups showed a reduction in symptoms of ADHD, with certain
groups reaching statistical significance compared to placebo (p<0.05). The
greatest significance was achieved in the group assigned to modafinil 300mg once
daily (p<0.01). The drug was generally well tolerated and the side effects seen
were consistent with those described in the product label, with insomnia being
the most frequent. The complete study data are expected to be presented at a
major medical meeting in 2003.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
862 of 998 DOCUMENTS
Espicom Business Intelligence
September 2, 2002
Modafinil cleared for marketing in Australia, New Zealand and South Korea
LENGTH: 142 words
Cephalon has been granted marketing approval formodafinil in Australia, New
Zealand and South Korea. Cephalon licensees,CSL in Australia and New Zealand
andChoongwae in Korea, will market modafinil under the brandnames,Modavigil
andProvigil, respectively. Approved for the treatment of excessive daytime
sleepiness associated with narcolepsy, the launch of the products in these
markets is expected to occur within 6 months.
Cephalon markets modafinil as Provigil tablets in the US and other countries.
Modafinil is approved worldwide in >20 countries. It is the first drug in a new
class of wake-promoting agents, which improve daytime wakefulness yet preserve
the ability to sleep at night. The most common side effects associated with
Provigil in clinical trials include headache, nausea, infection, nervousness,
anxiety and insomnia.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
863 of 998 DOCUMENTS
PR Newswire
August 30, 2002 Friday
Cephalon Announces Modafinil Receives Marketing Clearance In Australia, New
Zealand and South Korea
SECTION: FINANCIAL NEWS
LENGTH: 834 words
DATELINE: WEST CHESTER, Pa. Aug. 30
Cephalon, Inc. (Nasdaq: CEPH), an international biopharmaceutical company,
announced today that regulatory authorities have granted marketing approval for
modafinil in Australia, New Zealand and the Republic of Korea. Cephalon
licensees, CSL Limited in Australia and New Zealand and Choongwae Pharma
Corporation in the Republic of Korea will market modafinil under the brand names
of MODAVIGIL(R) and PROVIGIL(R) respectively.
Approved for the treatment of excessive daytime sleepiness (EDS) associated with
narcolepsy, launch of the products in these markets is expected to occur within
six months. Worldwide, modafinil is approved in more than 20 countries.
"PROVIGIL continues to experience significant growth in the United States and
European markets, and our partnerships with CSL and Choongwae provide the
opportunity to extend this growth into the Asia/Pacific region," said Robert
Roche, Senior Vice President, Pharmaceutical Operations at Cephalon.
Cephalon markets modafinil as PROVIGIL(R) (modafinil) tablets $(C-IV$) in the
United States and other countries. PROVIGIL is the first drug in a new class of
wake-promoting agents, which improve daytime wakefulness yet preserve the
ability to sleep at night. The most common side effects associated with PROVIGIL
in clinical trials include headache, nausea, infection, nervousness, anxiety and
insomnia.
CSL Limited
CSL Limited (ASX: CSL) is Australia's largest domestic pharmaceutical company.
CSL develops, manufactures and markets biological products for human use and
markets vaccines and other prescription pharmaceuticals in Australia and New
Zealand. The prescription pharmaceuticals include antibiotics, dermatologicals
emergency products, neurological products, analgesic products, and urological
products supplied by other manufacturers.
Choongwae Pharma
Choongwae Pharma is a leading pharmaceutical company whose products include
cardiovascular and anti-cancer agents, biological products, intravenous
solutions and other healthcare products. Recognized as one of the most preferred
pharmaceutical companies in Korea by its customers, Choongwae Pharma is
committed to providing premium-quality pharmaceutical products and services.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological disorders, cancer and pain.
Cephalon currently employs approximately 1,200 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guildford, England, and at
Laboratoire L. Lafon in Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL(R) (modafinil) Tablets $(C-IV$), GABITRIL(R) (tiagabine hydrochloride)
and ACTIQ(R) (oral transmucosal fentanyl citrate) $(C-II$) and more than 20
products internationally. Further information about Cephalon and full
prescribing information on its U.S. products is available at www.cephalon.com or
by calling 1-800-896-5855.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
guidance, and other statements regarding matters that are not historical facts.
You may identify some of these forward-looking statements by the use of words in
the statements such as "anticipate," "estimate," "expect," "project," "intend,"
"plan," "believe" or other words and terms of similar meaning. Cephalon's
performance and financial results could differ materially from those reflected
in these forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties
facing Cephalon such as those set forth in its reports on Form 8-K, 10-Q and
10-K filed with the U.S. Securities and Exchange Commission. Given these risks
and uncertainties, any or all of these forward-looking statements may prove to
be incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend to update
publicly any forward-looking statement, except as required by law. The Private
Securities Litigation Reform Act of 1995 permits this discussion.
MAKE YOUR OPINION COUNT - Click Here
http://tbutton.prnewswire.com/prn/11690X71363274
SOURCE Cephalon, Inc.
CONTACT: Sheryl Williams of Cephalon, +1-610-738-6493, or cell, +1-484-432-0046,
swilliam@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: August 31, 2002
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2002 PR Newswire Association, Inc.
864 of 998 DOCUMENTS
The Jerusalem Post
August 25, 2002 Sunday
Still sick, but not as tired
BYLINE: JUDY SIEGEL-ITZKOVICH
SECTION: HEALTH; Pg. 9
LENGTH: 611 words
HIGHLIGHT: Rx FOR READERS
I am a 47-year-old woman and have suffered from relapsing-remitting multiple
sclerosis for over 10 years. I take Copaxone by injection. Fortunately, I am in
good condition and have only negligible neurological deficits My only symptom is
tiredness. I have to sleep several hours in the afternoon, and it reduces my
time for activity. It's as if the disease takes over my body and makes my brain
tired. Is there any treatment for this type of MS-induced narcolepsy that does
not have annoying side effects? S.P., Beersheba
Prof. Avinoam Reches, chairman of the Israel Neurology Society and a senior
neurologist at Hadassah-University Hospital in Jerusalem's Ein Kerem, says:
Narcolepsy in multiple sclerosis patients occurs quite often, but we don't
understand the mechanisms. The amount of rest that patients need varies. We
prescribe the drug Provigil, which is generically known as modafinil and
manufactured by the Cephalon company. It has no negative interaction with the
injectible Teva drug for MS, Copaxone, but if you take other drugs, you should
consult with your doctor.
Modafinil is given not only for sleepiness during the day in MS patients, but
also to those who sleep due to other conditions. It promotes daytime wakefulness
without affecting nighttime sleep, and has been found to be well- tolerated,
with only mild to moderate side effects in a minority of users. The pill should
be taken in the morning to help you stay awake during the day , but it is a
prescription drug, and your daily dose and schedule should be determined by your
doctor.
As a complication of flu, my husband suffered hearing loss and developed
tinnitus. A composer, singer, and lover of music, he was understandably
distraught. A few months later, loud noises like shouting or car horns began to
cause him acute pain. Three Tel Aviv-area ear specialists found no organic
reason for the pain. They could not even give a name to what he had, but we
later got a diagnosis, "hyperacusis," from an Israeli doctor on the Internet. My
husband started wearing ear plugs to block out noise (though I warned him that
this would make him only more sensitive and intolerant toward even "normal"
noise) and two years later he cannot go out of the house, or even sit in a quiet
room with a couple of people, without ear plugs.
As far as he is concerned, he has this problem under control. I worry, though,
especially as we're planning to have children, and I don't want our baby to see
ear plugs as the norm or, worse, to always have to "be quiet around Daddy."
Moreover, I find there are inconsistencies and emotional elements in his
response to noise that suggest his problem is psychological/neurological. What
can be done, and what kind of specialist deals with this condition? R.E. Tel
Aviv
Prof. Rafi Feinmesser, head of the ear, nose and throat department at the Rabin
Medical Center-Beilinson Campus in Petah Tikva, replies:
When hyperacusis occurs, it is usually due to damage to the auditory nerve. The
nervous system reacts in a compensatory way by creating increased auditory
signals, so the patient hears more noise. It is not a psychiatric problem. Your
husband subjectively hears more noise. Earplugs could help him. It's also
possible that biofeedback or auto-suggestion could improve his situation. His is
certainly an extreme case, but every ear,nose and throat specialist knows of
hyperacusis. Go to another expert for help.
Rx For Readers welcomes queries from readers. Write Rx For Readers, The
Jerusalem Post, POB 81, Jerusalem 91000, fax your question to Judy
Siegel-Itzkovich at (02) 538- 9527, or e-mail it to jusie@jpost.co.il, giving
initials, age and place of residence.
LOAD-DATE: October 4, 2011
LANGUAGE: ENGLISH
GRAPHIC: Photo: Taking a nap is great, but narcolepsy requires a pill.
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Jerusalem Post
All Rights Reserved
865 of 998 DOCUMENTS
National Post (Canada)
August 14, 2002 Wednesday National Edition
Could this be the new lifestyle drug?: Narcolepsy medicine tested for use on the
healthy but sleep-deprived
SOURCE: National Post
BYLINE: Sharon Kirkey
SECTION: Arts & Life; Pg. AL1
LENGTH: 1625 words
Patients who come to see Dr. Roger Broughton are the sort who might fall asleep
in their car waiting for the light to change. They might doze off in the middle
of a conversation or while taking a shower or walking in the mall. A strong
emotion, even laughter, can make their bodies go as slack as a rag doll.
They suffer from narcolepsy, a rare condition characterized by the overwhelming
and irresistible urge to sleep, no matter what people do to try to stay awake.
Several years ago, Dr. Broughton, a professor of neurology at the University of
Ottawa, was the lead investigator in a multi-centre Canadian trial that found a
new drug called modafinil could keep people with narcolepsy awake and alert with
less of the jitteriness, agitation and other side effects of amphetamines and
other central nervous-system stimulants.
For many people with narcolepsy, modafinil has now become "the best stimulant
they've ever been on," reports Dr. Broughton, who is also director of the Sleep
Medicine Centre at The Ottawa Hospital's General Campus.
But it's what the pill might do for everyone else that has people really
buzzing.
Researchers have begun testing the medicine's effects on shift workers,
soldiers, long-haul truck drivers and rescue workers. In one trial involving
U.S. Army helicopter pilots, modafinil kept the aviators alert and able to
perform complicated manoeuvres on flight simulators during two days and one
night without sleep.
The study was conducted to measure modafinil's effect on sleep-deprived
"normals" -- otherwise healthy volunteers required to perform demanding tasks
despite sleep loss.
If the drug can keep pilots clear-headed during two 40-hour periods of
continuous wakefulness, what might it mean for a country where at least half of
the population is suffering from sleep deprivation? Could modafinil soon become
the ultimate lifestyle drug: a pill we can pop to dodge our body's need for
sleep, a way of cramming more into our increasingly and dangerously
over-extended lives?
The Canadian distributors of modafinil (sold as Alertec in Canada, and Provigil
in the United States) insist the drug "clearly is not intended" for such
purposes. (However, the U.S. Food and Drug Administration criticized modafinil's
U.S. manufacturer, Cephalon, earlier this year, for using sales aids and journal
ads that suggested the drug is safe and effective "for anyone with daytime
sleepiness.") "While [Alertec] has an effect on alertness and there may be
applications beyond narcolepsy, I don't see it becoming a drug you go [to your
doctor] and ask for" for non-therapeutic indications, says Dan Brazier,
president of DRAXIS Pharmaceutica Inc., which holds the exclusive Canadian
licence to market and sell Alertec.
So far, the drug is only approved in Canada for the treatment of narcolepsy. But
once a drug is approved for a specific use, physicians can prescribe it for
other purposes, a common and legal practice called "off-label" prescribing.
According to The Washington Post, three-quarters of the US$150-million worth of
modafinil tablets sold in the United States last year "were swallowed by people
who didn't have narcolepsy."
In Canada, Brazier will say only that Alertec's sales are growing, though not to
the extent that they are in the U.S., where more than 700,000 prescriptions for
the drug have been written since it was approved in 1999. And, says Brazier,
based on the evidence from France, Germany and other countries where modafinil
has been available for years, there is no evidence "to suggest that
non-therapeutic use is being sought out."
But as researchers begin testing the drug on an ever-broadening array of
problems, where will doctors draw the line?
"Pharmacological developments like modafinil will pose great temptations to
society," warned David Dinges, a University of Pennsylvania sleep-deprivation
researcher, recently in the Houston Chronicle. "They'll have the potential to
satisfy our relentless desire to control time."
Some doctors in Canada have already prescribed modafinil for off-label purposes.
Dr. Jon Fleming, the co-director of the Sleep Program at University Hospital in
Vancouver, says he has, on occasion, written prescriptions for Alertec to treat
jet lag, and for shift workers who are at risk of dozing off during the drive to
or from work. But those are "one-off" situations, Dr. Fleming says.
"Like all clinical situations, you have to assess impairment, and then assess
risks and benefits," he says. "The important thing for anybody who has
sleepiness is to identify the cause. If the cause relates to lifestyle issues
and insufficient nocturnal sleep, the treatment should always be to try and
improve nocturnal sleep."
Yet studies show people just aren't spending enough time in bed, says Dr.
Fleming. The amount of sleep an individual needs is highly variable; some can
get by on six hours a night, others may need closer to 10 hours. But in general,
doctors typically recommend adults get eight hours of sleep nightly. A recent
U.S. study, however, found one-third of those surveyed were getting less than
six hours of sleep a night. Ironically, almost half of those polled said they
are sleeping less in order "to be more productive."
But sleep debts eventually catch up.
"A lot of us don't use the top 10% of our brain most of the day --we're not
called upon to do original artwork or think up a computer game -- so, if you're
doing the laundry or walking to the mailbox, you can get by fine," says Dr. Judy
Leech, a sleep physician at The Ottawa Hospital.
"But the memory, the concentration, the originality part of the brain is the
first to go when you don't have sleep. Those guys in Silicon Valley, when they
were putting bunks in their offices? It was like this big new discovery suddenly
that sleep is something people need to perform better."
No one knows sleep's exact function. "We know obviously that if you don't have
any, if you have absolutely none, probably within two or three weeks you would
become psychotic," Dr. Leech says.
But researchers believe sleep has a restorative effect on all body functions.
For example, growth hormones peak at night during sleep. So do parts of the
immune system. "You even make more bone at night," says Dr. Leech. Osteocalcin,
which increases bone turnover, is higher at night.
"So lots of things are going on and, if you sort of screw those up, I'm not
saying you won't grow, but you know how you feel lousy if you don't sleep? It
might not just be the lack of sleep, it might be because you disturbed all the
other hormones," says Dr. Leech. Studies involving shift workers have found the
sleep-deprived workers tend to get sick more frequently and are at a greater
risk for high blood pressure, weight gain and gastrointestinal problems than
workers who get more sleep.
In addition, it's during sleep that we put down memory, filing it from the
short-term to the long-term "hard drive," Dr. Leech says. "That's how come when
you practice the piano today, you play better tomorrow."
Modafinil caused a stir in the sleep research field when it was approved in the
United States and Canada several years ago. The drug was heralded as the first
new drug since 1959 to be approved for the treatment of narcolepsy. According to
the journal American Family Physician, the drug's exact mechanism is unknown,
but studies done on animals found it acts on the area of the brain that controls
wakefulness and helps regulate the body's internal biological clock. It also
appears to cause less agitation, anxiety and insomnia than Ritalin and
amphetamines, the traditional treatments for narcolepsy, "and may have less
potential for abuse": Patients report that they don't get the same high as they
do with other stimulants. Finally, it doesn't interfere with nighttime sleep, or
leave people with the hangover effects of other stay-awake pills.
"Side effect-wise," says Dr. Leech, modafinil "is pretty minimal." For example,
the drug doesn't increase blood pressure. The most common complaints are
headache. "But there still could be long-term side effects that are untoward
that we don't know of," she says.
For that reason, Dr. Leech and others maintain that the drug should be reserved
for those with a bona fide sleep disorder, or other medical problems that can
cause excessive sleepiness either due to the illness itself or the drugs used to
treat it. For example, modafinil is being tested to treat chronic daytime
fatigue in patients with multiple sclerosis, sleep apnea and Parkinson's.
Dr. Leech concedes that "In some things like shift work, where, obviously,
people don't sleep the correct number of hours, maybe [modafinil] would fit in."
As for people who have deliberately deprived themselves of sleep, Dr. Leech
would advise they need to take better control of their lives. "I think it's
pretty superficial to say, 'Oh well, I'll take Alertec to stay awake," she says.
Some basic sleep hygiene can help people get the most out of the time they do
spend in bed: Always have the same wake-up time. "People focus on the bedtime
but the main thing is the get-up time," Dr. Leech says, "because that's what
really sets your internal clock." Keep the bedroom for sex and sleep (no
television, no Internet). Avoid caffeine later in the day. Cigarettes and
alcohol are equally stimulating -- alcohol may help people fall asleep, "but as
you withdraw from it in the night, it gives you worse sleep, so you're tossing
and turning at 3 a.m.," says Dr. Leech. Keep the bedroom cool and dark.
"We all don't get enough sleep at times. It's a function of society," says Dr.
Leech. "But I'd prefer my pilot was well rested rather than had a chemical
stimulant to stay awake."
LOAD-DATE: August 14, 2002
LANGUAGE: ENGLISH
GRAPHIC: Black & White Photo: Adrian Dennis, Agence France-Presse; Researchers
have begun testing the effects of modafinil on such sleep-deprived workers as
long-haul truck drivers, soldiers and U.S. Army helicopter pilots.
TYPE: News
Copyright 2002 National Post, All Rights Reserved
866 of 998 DOCUMENTS
CBS News Transcripts
July 9, 2002 Tuesday
SHOW: The Early Show (7:00 AM ET) - CBS
Checking the efficacy of Modafinil, the drug that is supposed to help people
stay awake and alert for extended periods
ANCHORS: JANE CLAYSON
BYLINE: TRACY SMITH
LENGTH: 1020 words
JANE CLAYSON, co-host:
If you've ever wished for more hours in the day, a new drug could help turn back
the clock. Our Tracy Smith decided to see how it works so well.
Tracy, hi.
TRACY SMITH reporting:
Be careful what you wish for.
CLAYSON: I'm not sure I want to do this. I'm not sure I want to stay awake for
40 hours.
SMITH: I'm not sure whether I could.
Modafinil is a drug that's used for sleeping disorders, and it's now being
tested as a way to keep people awake safely for up to 40 hours. So does it
work? Well, as I said, it's still being tested, but with my doctor's consent, I
conducted a little test of my own.
Think of it as time in a bottle. One little pill and up to 40 straight hours
without sleep. Coffee can give you the jitters; Modafinil can keep you alert,
jitter-free, all day and all night, maybe.
'Dizziness, mental mood changes, loss of appetite, dry mouth.'
Like any drug, it may not agree with you.
'Nausea, diarrhea or headache may occur.' Those are the most common.
And the label can be confusing.
'Report promptly trouble sleeping.' Trouble sleeping? I thought that was the
whole point!
But the best way for me to see if it worked was to take one and see what
happened. On the last Monday morning in June, I got up with Julie.
Morning, Julie. All right, it is 4:30 AM. Here's to the next 40 hours.
The idea was to work a normal day and see just how long I could stay alert.
I'm excited because I'm thinking about all the things that I can do with this
extra time. Well, for me it's an extra eight or nine hours every night that I
could be doing something else.
Part of this assignment was a flight to Houston, Texas, to talk to someone who's
testing the drug on people who work the night shift.
Mr. MAX HIRSCHKOWITZ (Sleep Researcher): I don't care how good your exercise
program is or how good your nutritional program is, if you don't get enough
sleep, you feel like crap.
SMITH: And there's nothing--no drug that--at the present...
Mr. HIRSCHKOWITZ: Not at the present time.
SMITH: ...that's going to fix that.
Mr. HIRSCHKOWITZ: Not at the present time.
SMITH: Somehow, just hearing him say that made me feel like turning in. But oh,
the night was still young.
Unidentified Man: America stays up late, and I'm one of those people who serve
the people that stay up late, and I'm proud of it.
SMITH: Houston after dark is like any other big city. An army of night workers
drive the trucks, wait the tables and staff the hospitals. They have their own
ideas about staying awake without taking a pill.
Mr. LEROY BECK (Houston VA Medical Center): Trying to find something to do to
keep myself busy. That's probably the main thing, staying busy. If you can do
that, I think you can make it.
Unidentified Man: Anything that allows you to stay up for two or three days,
isn't that--that seems unnatural to me.
Mr. BECK: Don't look at the clock. You know, just keep working and working.
Unidentified Man: Now maybe if I was doing a job that required me to be really,
really alert, I might consider it, where other lives were at stake, but I serve
sandwiches.
Mr. BECK: I myself, I like coffee when I'm really sleepy.
SMITH: How much coffee?
Mr. BECK: Oh, like a ton of coffee. You know, we go through pots of coffee.
SMITH: By half past midnight, a pot of coffee sounded pretty good to me. I still
felt alert, but I was beat.
All right. So it is 1:15 AM Houston time. I was up at 3:30 AM New York time,
which would be 2:30 AM here, so carry the one--that's just about 23 hours that
I've been up now. How do I look?
Don't answer that. The truth is, I looked like I felt: exhausted. A key
feature of Modafinil is that it allows you to sleep if you want to, and by 2 AM,
I wanted to. By 3, I did.
Seriously, people shouldn't look at this as a replacement for their five cups of
coffee, for those who do drink that?
Mr. HIRSCHKOWITZ: Not at this point. Not at this point.
SMITH: Someday?
Mr. HIRSCHKOWITZ: Perhaps.
SMITH: Now it didn't work for me right away, but your experience could be
different. When the Army tested Modafinil on helicopter pilots, they were able
to stay up for days and perform in simulators almost as well as they did with a
full night's sleep.
For more about Modafinil Go to WWW.CBSNEWS.COM
CLAYSON: So I'm with the guy who says it seems unnatural. There have to be side
effects here, as well.
SMITH: The short-term side effects are nausea, headache, dizziness. I didn't
get any of those. I felt terrific. Long-term effects, they don't know yet.
This drug came out in 1998...
CLAYSON: Right.
SMITH: ...so nobody knows.
CLAYSON: So did they find out or did they tell you why it didn't work so well on
you?
SMITH: Well, the problem is when I interviewed the doctor, I still thought it
was working, and then he started talking about the placebo effect, and then I
started thinking, 'Oh, maybe--maybe I'm not really awake' and I think I crashed
after that.
CLAYSON: Right. Right. How addictive is it, is the question?
SMITH: It's not. It doesn't make you high. You feel perfectly normal, so
there's no addictive qualities, physically. Now psychologically could be
different.
CLAYSON: Right. So this is now only being prescribed to narcoleptics.
SMITH: That's right.
CLAYSON: And if you want to get a prescription...
SMITH: You can ask your doctor.
CLAYSON: ...it's not FDA-approved yet.
SMITH: No, but you can ask your doctor and they could approve it just like Botox
was prescribed before it was approved, for wrinkles.
CLAYSON: Would you do it again?
SMITH: I might if I had a crucial interview or something and I was up the night
before, might take it.
CLAYSON: And you felt OK.
SMITH: I have two extra ones here, so...
CLAYSON: Oh! Stay away. I don't want it. Tracy, it's an interesting story
though, thank you.
SMITH: No problem.
CLAYSON: And good to see you.
7:37 now. Up next, two best-selling authors who also happen to be mother and
daughter. We're back with that on THE EARLY SHOW after this.
(Announcements)
LOAD-DATE: July 9, 2002
LANGUAGE: ENGLISH
TYPE: Analysis
Copyright 2002 CBS Worldwide Inc.
All Rights Reserved
867 of 998 DOCUMENTS
CNBC News Transcripts
July 8, 2002 Monday
SHOW: Early Today (4:30 AM ET) - CNBC
Researchers debating use of drug to keep people awake longer
ANCHORS: NANETTE HANSEN
BYLINE: Dr. IAN SMITH
LENGTH: 392 words
NANETTE HANSEN, anchor:
Welcome back. I am told sleep is a basic need for everybody. We seem to do
without it on this shift, though. Seventy million Americans have trouble
sleeping. But if given the option, would you stay awake longer to get more done
if there were few side effects? NBC's Dr. Ian Smith takes a look at a
controversial drug that might help the sleep deprived stay awake.
Dr. IAN SMITH reporting:
Now a provocative question has been raised among sleep researchers about whether
a medicine being tested to treat excessive daytime sleepiness might be misused
by otherwise healthy people who just want to stay awake. The drug is modafinil,
marketed as Provigil, already approved to treat narcoleptics like Juliet Block.
Ms. JULIET BLOCK: It helps a lot, and it--it gets me through the day, like
anyone else could get through the day.
SMITH: Modafinil is different from older stimulants, which affect the central
nervous system and can leave users nauseous or jittery. Instead, it acts only on
the hypothalamus, the area of the brain which houses the sleep center. It can
keep people awake and alert for extended periods of time. That quality has even
led the military to give it to pilots on some combat missions. The company
which makes modafinil is funding studies in the hopes of getting FDA approval to
use it for other sleep disorders. Neurologist Dr. Thomas Scammel says the very
attributes that make modafinil so effective in treating sleep disorders may
invite trouble.
Dr. THOMAS SCAMMEL (Harvard Medical School): If you have a drug with minimal
side effects that can help keep people awake, there's a real temptation for
people to work longer hours, to perhaps stay up all night if this drug can
easily make that possible.
Unidentified Man: It's essential to life. It's as essential as breathing. It's
essential as the beat of your heart and there's nothing that will replace it.
No drug, no substance--not caffeine, no vitamins, no herbs. It's gotta be
sleep.
SMITH: Especially since recent studies show that sleep deprivation doesn't just
make us drowsy, but increases our risk for diabetes and hormonal imbalances. So
while these powerful medications may keep us going longer, there's no masking
the long-term effects sleeplessness can have on our bodies. Dr. Ian Smith, NBC
News, New York.
LOAD-DATE: July 8, 2002
LANGUAGE: ENGLISH
TYPE: Newscast
Copyright 2002 CNBC, Inc.
868 of 998 DOCUMENTS
NBC News Transcripts
July 7, 2002 Sunday
SHOW: NBC Nightly News (6:30 PM ET) - NBC
New medicine to help sleeplessness might be misused by people who want to stay
awake
ANCHORS: JOHN SEIGENTHALER
BYLINE: Dr. IAN SMITH
LENGTH: 509 words
JOHN SEIGENTHALER, anchor:
Now to LIFELINE and something we all need and never get enough of--sleep.
TEXT:
NIGHTLY QUESTION
PROBLEM SLEEPING?
A 50 MILLION
B 70 MILLION
C 100 MILLION
SEIGENTHALER: This week's Newsweek magazine devotes its cover to the subject and
gives us the answer to our NIGHTLY QUESTION, which is B. Seventy million
Americans have trouble sleeping. And now there is a drug that might be used to
help the sleep deprived to stay alert. Here's NBC's Dr. Ian Smith.
Dr. IAN SMITH reporting:
Twenty-first century America now working around the clock, squeezing out every
precious minute to stay awake, but at a cost.
Dr. GARY ZAMMIT (Sleep Disorders Institute, St. Lukes Roosevelt Hospital
Center): We know that people who are sleep deprived are not functioning at peak.
SMITH: Now, a provocative question has been raised among sleep researchers about
whether a medicine being tested to treat excessive daytime sleepiness might be
misused by otherwise healthy people who just want to stay awake. The drug is
modafinil, marketed as Provigil, already approved to treat narcoleptics like
Juliet Block.
Ms. JULIET BLOCK: It helps a lot, and it--it gets me through the day like anyone
else could get through the day.
SMITH: Modafinil is different from older stimulants which affect the central
nervous system and can leave users nauseous or jittery. Instead, it acts only
on the hypothalamus, the area of the brain which houses the sleep center. It
can keep people awake and alert for extended periods of time. That quality has
even led the military to give it to pilots on some combat missions. The company
which makes modafinil is funding studies in the hopes of getting FDA approval to
use it for other sleep disorders. Neurologist Dr. Thomas Gamil says the very
attributes that make modafinil so effective in treating sleep disorders may
invite trouble.
Dr. THOMAS GAMIL: If you have a drug with minimal side effects that can help
people awake, there's a real temptation for people to work longer hours, to
perhaps stay up all night if this drug can easily make that possible.
SMITH: A real concern, especially where there's an economic incentive to delay
sleep. But Cephalon, the company which makes modafinil, says there is no
evidence of misuse. While some envision a day where new medications will double
and even triple the time we stay awake, experts insist that sound sleep remains
fundamental to human biology.
Dr. ZAMMIT: It's essential to life. It's as essential as breathing. It's as
essential as the beat of your heart, and there's nothing that will replace
it--no drug, no substance, not caffeine, no vitamin, no herb. It's got to be
sleep.
SMITH: Especially since recent studies show that sleep deprivation doesn't just
make us drowsy but increases our risk for diabetes and hormonal imbalances. So
while these powerful medications may keep us going longer, there's no masking
the long-term effects sleeplessness can have on our bodies. Dr. Ian Smith, NBC
News, New York.
LOAD-DATE: July 8, 2002
LANGUAGE: ENGLISH
TYPE: Profile
Copyright 2002 National Broadcasting Co. Inc.
869 of 998 DOCUMENTS
The Washington Post
June 29, 2002 Saturday
Final Edition
A Pill to Keep You Going
SECTION: EDITORIAL; Pg. A22
LENGTH: 296 words
While Joel Garreau ["The Great Awakening," Style, June 17] adequately
characterized the appropriate and inappropriate uses of Cephalon's product,
modafinil (Provigil), we are concerned that he consumed the product while
writing his story without identifying the medical condition for which he was
prescribed the drug.
Cephalon has worked for more than nine years to develop modafinil for patients
with serious sleep disorders.
It is our expectation that clinical studies completed and currently underway
will help Cephalon and those with sleep disorders understand the implications of
potential broader use of the product for other disorders where excessive
sleepiness is a major symptom.
PAUL BLAKE
Senior Vice President
Clinical Research and Regulatory Affairs
Cephalon Inc.
West Chester, Pa.
*
I am one of the sleep researchers quoted in Joel Garreau's story, which dealt
with issues related to sleep and the medication, modafinil. As such, I wish to
clarify a few points.
My statement about unexpected toxic effects of new medications was a general
comment about the need for caution in drug development and use. It was not
intended to include modafinil. Modafinil has been tested for efficiency and
safety and has been in use long enough that it can be regarded as safe.
Specifically, modafinil was in clinical trials in France in the 1980s and in the
United States in the early 1990s.
Pharmacological induction of many days of wakefulness with little or no
intervening sleep will need careful study. I am unaware of long-term studies
even in animals.
The results of such research would be of great interest to many components of
society and, of course, to Post readers.
WILLIAM C. DEMENT
Director
Stanford Sleep Disorders
And Research Center
Palo Alto, Calif.
LOAD-DATE: June 29, 2002
LANGUAGE: ENGLISH
DOCUMENT-TYPE: LETTER
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
870 of 998 DOCUMENTS
The Washington Post
June 21, 2002 Friday
Final Edition
Staying Awake To Modafinil's Possibilities
BYLINE: Donna Britt
SECTION: METRO; DONNA BRITT; Pg. B01
LENGTH: 821 words
What would you do if you could stay awake and alert for 40-hour stretches?
Label your videos and organize your closets while the world slept? Drive
straight through from the District to Santa Fe, N.M.? (That's 31 hours' road
time, plus eight hours for bathroom and food breaks.) Start your novel? Party
till you didn't drop from exhaustion?
Prepare to find out. You've probably heard a lot less about the drug modafinil
than you have about Viagra, but I'm convinced that will change. Why?
Because Viagra addresses male sexual dysfunction, which only affects millions of
men and their partners. Modafinil shuts off human beings' urge to sleep.
Who doesn't that affect?
As someone who's been sleepy for two decades -- my eldest child is 20 -- I read
Post reporter Joel Garreau's article about the drug with excitement and dismay.
In trials on healthy people, modafinil allowed users to stay up for almost two
days while remaining nearly as focused, alert and capable of problem-solving as
the well-rested.
After eight hours of sleep, Garreau writes, users can rise and go another 40
hours. Reportedly, modafinil users don't experience the jitters or addiction --
with its euphoric ups and spiraling downs -- suffered by users of amphetamines,
cocaine and even coffee.
Considering its downside, why is caffeine the world's most widely used drug? Why
is there a Starbucks on every other corner?
Because most Americans don't get enough sleep -- two-thirds of us, according to
the National Sleep Foundation.
So why aren't people more excited about modafinil? The military may salivate at
the prospect of an ever-ready "24-hour soldier"; my friends with young children
sigh at the notion of being awake enough for occasional lovemaking.
But when I described the drug to my manicurist, she responded, "No way. Why
would anyone want to stay up 40 hours?"
"Forty hours? That's scary," echoed bakery manager Melbin Perdigon, 25. "Maybe
if you were doing a really long drive . . . "
Silver Spring artist Ellen Jacobson was leaving a video store, clutching "The
Princess Bride." Exhausted by her son's graduation, Jacobson hoped her daughter,
5, would watch "Princess" while she napped.
But pop a pill to eradicate her sleepiness? Please.
"We have life cycles for a reason," said Jacobson, a potter and painter. "If
people have that much to do, they should cut some things out and prioritize."
So she'd never consider modafinil?
Pause. "Maybe when I'm getting ready for my holiday sale. . . . But it would
seem like you'd be going against nature.
"This is not going to solve the problem of time."
Time, we long ago decided, is the Enemy. Despite our desperate battles with it,
our endless manipulations, it ticks on -- taking a toll on our bodies, minds,
careers and every relationship we find too little time to nurture.
So we worry, plan and strategize. We introduce our skin to industrial-strength
moisturizers, our bodies to energy boosters and memory enhancers, our kids to
after-after-school care and marathon TV sessions. We spend more time working
than we would like.
Forty more hours a week? We'd probably do more of what we regret doing now.
Even sleep researchers who tout modafinil wonder about its long-term effects.
Accumulated sleep deprivation is suspected of causing obesity and illness.
Still, modafinil, currently marketed to people with sleep disorders, is bound to
be sought by truck drivers, hospital interns, pilots, exam takers -- and
everybody else who pulls all-nighters.
In a world of 24-hour laundromats, diners, shopping services, TV channels and
copier stores, that means millions.
Who won't go for it? Those who, realizing that the body repairs itself during
sleep, believe that not sleeping for extended periods must be physically
harmful. But what of the soul? Is tampering with something as fundamental as
sleep . . . wrong?
Even God rested after His labors.
District pastor Allen White, who says he hates sleep because he would rather
stay awake to play the piano and pray, says modafinil reminds him of Psalm 127:
"It is vain for you to rise up early, to retire late, to eat the bread of
painful labors; for He gives to His beloved even in his sleep."
Even without our constant labor, the passage suggests, God provides.
"It means we can go to sleep and everything will be all right," says White.
"People think if they're not doing something every second, nothing will get
done. That's vanity."
That's life as many of us know it. If modafinil scares you, don't even consider
the next generation of "wake-performing" drugs. Scientists say they'll keep us
awake indefinitely -- without adding sleep debt.
Decades from now, people wary of modafinil may seem as quaint as those who once
said, "If God wanted man to fly, He'd have given him wings."
But we'll be too miserable from never getting a break from our ever-wakeful
families and co-workers to take any pleasure in it.
LOAD-DATE: June 21, 2002
LANGUAGE: ENGLISH
DOCUMENT-TYPE: COLUMN
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
871 of 998 DOCUMENTS
The Washington Post
June 21, 2002 Friday
Final Edition
Staying Awake To Modafinil's Possibilities
BYLINE: Donna Britt
SECTION: METRO; DONNA BRITT; Pg. B01
LENGTH: 821 words
What would you do if you could stay awake and alert for 40-hour stretches?
Label your videos and organize your closets while the world slept? Drive
straight through from the District to Santa Fe, N.M.? (That's 31 hours' road
time, plus eight hours for bathroom and food breaks.) Start your novel? Party
till you didn't drop from exhaustion?
Prepare to find out. You've probably heard a lot less about the drug modafinil
than you have about Viagra, but I'm convinced that will change. Why?
Because Viagra addresses male sexual dysfunction, which only affects millions of
men and their partners. Modafinil shuts off human beings' urge to sleep.
Who doesn't that affect?
As someone who's been sleepy for two decades -- my eldest child is 20 -- I read
Post reporter Joel Garreau's article about the drug with excitement and dismay.
In trials on healthy people, modafinil allowed users to stay up for almost two
days while remaining nearly as focused, alert and capable of problem-solving as
the well-rested.
After eight hours of sleep, Garreau writes, users can rise and go another 40
hours. Reportedly, modafinil users don't experience the jitters or addiction --
with its euphoric ups and spiraling downs -- suffered by users of amphetamines,
cocaine and even coffee.
Considering its downside, why is caffeine the world's most widely used drug? Why
is there a Starbucks on every other corner?
Because most Americans don't get enough sleep -- two-thirds of us, according to
the National Sleep Foundation.
So why aren't people more excited about modafinil? The military may salivate at
the prospect of an ever-ready "24-hour soldier"; my friends with young children
sigh at the notion of being awake enough for occasional lovemaking.
But when I described the drug to my manicurist, she responded, "No way. Why
would anyone want to stay up 40 hours?"
"Forty hours? That's scary," echoed bakery manager Melbin Perdigon, 25. "Maybe
if you were doing a really long drive . . . "
Silver Spring artist Ellen Jacobson was leaving a video store, clutching "The
Princess Bride." Exhausted by her son's graduation, Jacobson hoped her daughter,
5, would watch "Princess" while she napped.
But pop a pill to eradicate her sleepiness? Please.
"We have life cycles for a reason," said Jacobson, a potter and painter. "If
people have that much to do, they should cut some things out and prioritize."
So she'd never consider modafinil?
Pause. "Maybe when I'm getting ready for my holiday sale. . . . But it would
seem like you'd be going against nature.
"This is not going to solve the problem of time."
Time, we long ago decided, is the Enemy. Despite our desperate battles with it,
our endless manipulations, it ticks on -- taking a toll on our bodies, minds,
careers and every relationship we find too little time to nurture.
So we worry, plan and strategize. We introduce our skin to industrial-strength
moisturizers, our bodies to energy boosters and memory enhancers, our kids to
after-after-school care and marathon TV sessions. We spend more time working
than we would like.
Forty more hours a week? We'd probably do more of what we regret doing now.
Even sleep researchers who tout modafinil wonder about its long-term effects.
Accumulated sleep deprivation is suspected of causing obesity and illness.
Still, modafinil, currently marketed to people with sleep disorders, is bound to
be sought by truck drivers, hospital interns, pilots, exam takers -- and
everybody else who pulls all-nighters.
In a world of 24-hour laundromats, diners, shopping services, TV channels and
copier stores, that means millions.
Who won't go for it? Those who, realizing that the body repairs itself during
sleep, believe that not sleeping for extended periods must be physically
harmful. But what of the soul? Is tampering with something as fundamental as
sleep . . . wrong?
Even God rested after His labors.
District pastor Allen White, who says he hates sleep because he would rather
stay awake to play the piano and pray, says modafinil reminds him of Psalm 127:
"It is vain for you to rise up early, to retire late, to eat the bread of
painful labors; for He gives to His beloved even in his sleep."
Even without our constant labor, the passage suggests, God provides.
"It means we can go to sleep and everything will be all right," says White.
"People think if they're not doing something every second, nothing will get
done. That's vanity."
That's life as many of us know it. If modafinil scares you, don't even consider
the next generation of "wake-performing" drugs. Scientists say they'll keep us
awake indefinitely -- without adding sleep debt.
Decades from now, people wary of modafinil may seem as quaint as those who once
said, "If God wanted man to fly, He'd have given him wings."
But we'll be too miserable from never getting a break from our ever-wakeful
families and co-workers to take any pleasure in it.
LOAD-DATE: June 21, 2002
LANGUAGE: ENGLISH
DOCUMENT-TYPE: COLUMN
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
872 of 998 DOCUMENTS
Newsbytes
June 17, 2002, Monday
The Great Awakening
BYLINE: Joel Garreau; Washington Post Staff Writer
LENGTH: 4025 words
DATELINE: United States
Grubb's Pharmacy is an unassuming if not seedy two-story clapboard landmark amid
the grand brick townhouses of East Capitol Street. Not only is it one of the
busiest pharmacies in the District. But being only four blocks from the Capitol,
it is also the neighborhood provider of potions and portents to congressmen,
lobbyists, super-lawyers, Supreme Court justices, ambitious aides and all those
other classic Type A Washingtonians who think that whatever they're working on
is The Most Important Thing in the World. And of course sometimes they may be
right.
Yet Grubb's is filling only about five prescriptions a month for a drug named
modafinil. "It's nothing like Viagra. That was a national explosion," says
Edward F. Dillon, the pharmacist. "Or a drug like Propecia, for hair loss. Or
Prozac. Let me tell you. When Time magazine put that on the cover, you could
definitely see the spike."
This may be the calm before the storm, however. For modafinil may have the power
to change Washington.
What it does is shut off your urge to sleep.
"It's a standing joke among sleep doctors that nobody sleeps in New York or
Washington," says Helene Emsellem, director of the Center for Sleep and Wake
Disorders in Chevy Chase. "Except in New York they do it for pleasure, while in
Washington they do it to work."
In trials on healthy people like Army helicopter pilots, modafinil has allowed
humans to stay up safely for almost two days while remaining practically as
focused, alert, and capable of dealing with complex problems as the well-rested.
Then, after a good eight hours' sleep, they can get up and do it again -- for
another 40 hours, before finally catching up on their sleep.
Originally aimed at narcoleptics, who fall asleep frequently and uncontrollably,
modafinil works without the jitter, buzz, euphoria, crash, addictive
characteristics or potential for paranoid delusion of stimulants like
amphetamines or cocaine or even caffeine, researchers say. As with an increasing
number of the so-called superhuman, posthuman or trans-human drugs or genetic
manipulations rapidly entering our lives, modafinil thus calls into question
some fundamental underpinnings of hundreds of thousands of years of thought
regarding what are normal human capabilities.
The implications for Washington are profound.
The Defense Advanced Research Projects Agency is searching for ways to create
the "metabolically dominant soldier." Among the projects it is pursuing is the
creation of a warrior who can fight 24 hours a day, seven days straight.
"Eliminating the need for sleep while maintaining the high level of both
cognitive and physical performance of the individual will create a fundamental
change in war-fighting," says the Defense Sciences Office on its Web site. As
usual, DARPA did not comment directly for this report.
William C. Dement, director of the Stanford University Sleep Center, who is
known as "the father of sleep medicine" for his pioneering work in the '50s,
embraces the idea of modafinil use for official Washington. "If Donald Rumsfeld
had to stay awake for a long period of time, I would want him fully alert," he
says.
Francis Fukuyama of Johns Hopkins University recently published "Our Posthuman
Future: Consequences of the Biotechnology Revolution," a book that is scathingly
critical of what he sees as runaway biotech that could rob us of our very human
nature. When asked about modafinil and its effects on Washington, he responded
with a 2:50 a.m. e-mail from Europe, where he was finishing a grueling
three-week trip. "I haven't heard of this but I'm not surprised," he wrote.
"I better get some," he half-joked.
Modafinil and its follow-on technologies hold the potential for changing
society. "This could replace caffeine," says Joyce Walsleben, director of the
NYU Sleep Disorders Center.
Caffeine -- the globe's most widely used drug -- today is a bigger food additive
in dollar terms than salt. The U.S. soft drink industry alone sold 10 billion
192-ounce cases of bubbly last year, most of it caffeinated.
Modafinil's sales are still small. But it did double sales to $150 million in
only the last year, according to Cephalon, the pharmaceutical company that
markets it under the trade name Provigil.
Its potential for changing how people work and live is intriguing. In an
increasingly 24-7 world, will such medicine create even more demand for people
to be available round-the-clock? Were Robert Frost's lines from 1923 prophetic?
The woods are lovely, dark and deep.
But I have promises to keep,
And miles to go before I sleep,
And miles to go before I sleep.
Will people feel that they need to routinely control their sleep in order to be
competitive? Will unenhanced people suffer fewer promotions and raises than
their modified colleagues? Will this start an arms race over human
consciousness?
To get some hint of what such a Washington life might be like, the bulk of the
writing of this article, a task not unlike others with many moving parts --
software development or the juggling of a diplomatic flap -- was accomplished in
one 40-hour period enabled by the prescribed use of modafinil.
10 a.m. Thursday. Third hour awake. Back from working out at the gym. Gazing at
the white 200 mg. tab of modafinil. Hey, how scary can this be. It's not like
this is life's first all-nighter. This one is even legal. Ironic. Four decades
after the '60s, some of the most startling drugs are those available by
prescription. But safety first. Take the advice of the sleep docs. Cut the tab
in half. If, as sometimes happens, there is going to be a headache or nausea,
start with a low dose.
Humans have been manipulating their sleep chemistry for a long time. Caffeine is
as old as coffee in Arabia, tea in China and chocolate in the New World.
For at least as long, sleep has been seen as a universal solvent.
"Now blessing light on him that first invented this same sleep!" says Sancho
Panza in "Don Quixote." "It covers a man all over, thoughts and all, like a
cloak; 'tis meat for the hungry, drink for the thirsty, heat for the cold, and
cold for the hot. 'Tis the current coin that purchases all the pleasures of the
world cheap; and the balance that sets the king and the shepherd, the fool and
the wise man even."
The effects of medicated sleeplessness on a vast healthy population is still
unknown. "Before you start taking it for the rest of your life, find out what it
does to your heart valves or some damn thing," Dement says. "A lot of people
know the story of fen-phen or thalidomide. If you take it all the time, and try
to stay awake all the time, there's a big chance that there may be some hitherto
unknown toxic effect."
Nonetheless, modafinil (pronounced mo-DAF-i-nil) is distinguished by its
apparently precise neurological focus. Nobody knows exactly how modafinil works,
but researchers marvel at the way it seems to target very specific regions of
the brain believed to regulate normal wakefulness. It's that narrow effect that
is lacking in other stimulants, resulting in their notorious side effects.
In fact, on the wall of his office at a company named Hyperion, off Boston's
Interstate 495 near Worcester, Mass., sleep researcher Dale M. Edgar has a sign.
"It's about the sleepiness, stupid," it reads.
As with the rest of the cascade of new drugs that promise to augment human
performance, here are three groups of people who will ultimately be attracted to
new wakefulness drugs, researchers say. In this order, they are:
The sick.
The otherwise healthy with a critical need.
The rest of us.
It's the future of the third group -- the millions who, in the immortal words of
Kiss, "wanna rock and roll all nite and party every day" -- that deeply concerns
the sleep business.
The Food and Drug Administration so far has approved modafinil marketing only to
narcoleptics, as the FDA reminded Cephalon in January, when it charged that the
company's promotional materials were overreaching. Cephalon will soon submit an
application to the FDA to expand its marketing to people with other sleep
disorders, including the ones associated with sleep apnea and Parkinson's
disease.
There are only 125,000 to 250,000 narcoleptics in the United States. Cephalon
brags that hundreds of thousands of patients have taken Provigil, with over a
million prescriptions written as of 2001, and sales soaring. Nonetheless,
Cephalon spokesman Sheryl Williams says that "we are not aware of any
significant prescribing of the drug for nonmedical conditions."
What exactly is a "nonmedical condition"?
This enters the murky world of the second group -- healthy people engaged in
"mission-critical tasks for which sleepiness is not an option," as Edgar puts
it.
"Like flying a big C-17 transport plane from Charleston Air Force Base to
Afghanistan virtually nonstop," says Edgar. "That happened. There are lots of
examples in the Air Force. It's what they call susops -- sustained operations.
You really, really need something on those long flights, and not just for the
pilots. The payload specialists in back have no place to sleep, and they have to
be on the ready to deploy the load. It's hard, but it's also critical to the
success of the mission, and reducing accidents."
The crucial issue is not staying awake. It's doing so without making lethal
mistakes. The fatal decision to launch the Challenger space shuttle was made by
people handling very complex data after days of irregular work hours and
insufficient sleep, as all sleep researchers remind themselves.
Fort Rucker, Ala., is 58,000 hot and steamy acres of Southern pine and the
occasional wild magnolia. All the Army's helicopter pilots are trained there.
John Caldwell has a low, impressively equipped, sprawling brick sleep laboratory
with the Air Crew Health and Performance Division of the U.S. Army Aeromedical
Research Laboratory. His modafinil study is the one that kept awake the
helicopter pilots -- "normals without any pathological conditions," as he so
clinically puts it.
The pilots flew a simulator in which they had to respond quickly to commands --
to fly for two minutes straight and level at 3,000 feet maintaining 120 knots at
a heading of 180, for example, then perform a turn of 360 degrees over exactly
two minutes, maintaining speed and altitude. Then the pilots had to perform four
different tasks simultaneously -- watching warning lights come on and dials
deviate from normal, while monitoring the fuel levels and clearing blockages,
while holding a target constant, while responding on the radio to someone
commanding, "NGT 504, NGT 504, set communications radio to 121.5"
Caldwell expresses a sentiment volunteered by almost every sleep researcher.
"One thing I want to make clear -- when we look at compounds like modafinil or
amphetamines or caffeine, those are emergency kinds of measures, not a
replacement for sleep. It's not nice to fool with Mother Nature."
Says Stanford's Dement: "The real problem is the accumulated sleep debt, not
daily need. It's established fact that lost sleep accumulates. You quickly
become too tired to be functional." Even with a substance like modafinil that
can keep you wakeful, if you don't ultimately catch up on the sleep you missed,
bad things will happen, sleep researchers have always believed.
"Your grandmother was right. If you don't get enough sleep, you're going to get
sick," says Chevy Chase researcher Emsellem.
When you're facing a critical situation, however, it's better to have help being
alert, Caldwell firmly believes. "Combat operations are very unpredictable."
Even with a 14-hour-a-day rest schedule, "if the enemy attacks during the 14
hours off, we're going to have to respond."
"There are a lot of other medically justified scenarios," says Edgar. "Think of
emergency medical services. What happens when a building collapses? As we
unfortunately learned recently, teams work around the clock. Can you justify it
to save lives? Absolutely. Particularly if it's a hazardous situation. Somebody
needs to do the job, and if there is something that is safe, effective, and
non-habit-forming, I think the answer is yes."
Sleep research is a very young science, and the number of things it doesn't know
about substances like modafinil is daunting.
"How long can somebody stay awake and not suffer? Hard to say. The jury is still
out," says Edgar, who is on leave from Stanford. He is now ensconced in a serene
research facility sporting green glass that matches the stripes of the mallard
ducks on the pond. Inside are a sophisticated array of computers and hundreds of
mice and rats. In his small office, wraparound screens stream brain wave
activity being transmitted live from around the world over the Internet. Edgar
has taken up a new role as senior vice president for preclinical research at
Hypnion, which he describes as the world's first biotech company specifically
dedicated to solving problems of sleep-wake disorders.
"Do you function as if you were rested? The answer is you're probably better off
than if you haven't taken it, but you're not at 100 percent. Where are you?
Fifty percent on cognitive performance? Is that good enough?"
But then Edgar drops the bomb.
"The next generation of wake-performing therapeutics will be more effective.
You'll be able to stay awake for X amount of time and not add sleep debt.
Ideally, it means being able to be up all day, all night, and all the next day
and not have incremental increase in sleepiness or in sleep debt. It would be
medication that gives you an interest-free loan.
"It could change the world. A complete paradigm shift. I'm not trying to plug my
company. But we are in the forefront. We could see this being a reality,
starting to become available, in about five years."
Friday, 2 a.m., Hour 19. The effortless mental focus brought on by modafinil is
remarkable. No attention deficit here. The feeling is that you have been given a
gift of time, and it is too precious to waste.
The focus is almost more interesting than the sleep-avoidance. In fact, it makes
you wonder what it will be like to grow up in a world in which this stuff is
common. Suppose you are just getting started in a career and you're a basket of
insecurities. Suppose you could regularly produce at levels unheard of even by
today's workaholic standards simply by popping a pill. Could you resist it?
Worse yet, suppose you were competing for raises and promotions against someone
who was happy to grab whatever enhancements were available. Will it become
routine to hear "There'll be plenty of time to sleep when you're 40"?
You can't get high on modafinil. There's no euphoria to it. When they first take
it, a lot of test subjects figure they must have gotten the placebo.
On this do sleep researchers base their hope that wakefulness agents won't be
the next glam drug phenom, hyped on magazine covers and distributed with abandon
to people for whom they were never intended, under circumstances that have never
been studied.
But they know the facts. Two-thirds of all Americans don't get enough sleep,
according to the National Sleep Foundation. Sleep deprivation may be a factor in
the national epidemic of obesity. America is full of people burning the candle
at both ends, wanting to know only where they can get more wax.
"Most of them are impaired. A lot of jobs you can do almost in your sleep --
lifting boxes onto shelves in a department store," says Dement. "But I'm
frequently an expert witness in cases that involve falling asleep at the wheel.
A recent case involved a man who was working two jobs, and on the night job he
was frequently observed to fall asleep. His supervisor escorted him out the
door. He drove into an oncoming lane and killed three people."
The graveyard shift is hardly just for factory workers anymore. The world is
open 24-7 -- restaurants, health clubs, Wal-Marts, Home Depots, help desks,
stock and commodities traders, catalogue sales and overnight shippers, to
mention a few. Why do people getting off the red-eye from Los Angeles or to
London seem so ruefully proud even when they look like dog meat? The classic
hero figure of capitalism is the CEO who says he never needs more than a few
hours of sleep -- he's proud of being on the go all the time.
Washington has its own special breeds of sleep-defiers. Think of the rat
calculus of campaign strategists running the maze of late October before
Election Day. Hunched and harried, they work the phones to the Coast until 2 or
3 in the morning, while writing the candidate's talking points for the next day,
and then hitting the Eastern time zone phones at dawn. The badge of special
honor is simultaneously to be advising campaigns from Washington in the time
zones of Britain and Israel.
Friday, 4 a.m., Hour 21. When this stuff takes over, it takes over. Gently, not
violently. No apparent loss of acuity. But you have definitely kicked into a
gear you didn't know you had.
Playing computer games like FreeCell as an informal way of testing cognitive
ability. Do you dare send e-mails? Will you regret them when you return to
normal?
Speaking of rhythms, remember to eat. Got to keep up strength. Discomfort still
far less than it would have been had coffee been used to accomplish this task.
Getting awful sick of herb tea, though.
So what about the dreaded third group -- the rest of us, those who are in a
fundamentally different situation from the first two groups? We have a choice
whether to live a saner life or try to solve our problems with a pill.
"The young professional who wants to work and play and do everything, and
doesn't want to spend time sleeping?" asks University of Pennsylvania sleep
researcher David Dinges. "That's another matter."
Yes, sleep researchers grudgingly admit, there are going to be some
way-off-label users. The college students crashing on term papers. Truck
drivers. Barge operators. Airline pilots. The physician in long hours of
training. The new parent. Ever watch the White House-based television show "The
West Wing?" They never seem to go home. That is not fantasy.
"Sleepiness is everywhere," says Neil Feldman, medical director of the St.
Petersburg, Fla., Sleep Disorder Center, who is conducting a shift work study
for Cephalon. "We're a 24-hour society. We no longer live by the night/day
cycle. We live by whatever our occupation demands. Physicians on call at night.
Nuclear power plant operators. Police, firemen. Plus the world is becoming a
smaller place. Trans-meridian travel, commonly known as jet lag. There are
economic demands -- more than one job -- plus raising children.
"How many have fallen asleep at the wheel of a car? Something like 25 percent at
least momentarily once during the year. Sleep deprivation is everywhere. Our
society looks at people who sleep as less strong people. People who nap are
slugs."
Suppose a lawyer came to you and said, "I have a client on death row and the
governor has just given me three days to draft his appeal before he is
executed."
"I'd probably prescribe the drug," Feldman said. "But three pills. Not a
hundred. I can rationalize that."
"People ask me about it almost daily," says Dement. "Everybody would like to be
able to have more time to do whatever they want to do. I could stand in front of
a roomful of Stanford undergrads right now and say, 'If you feel tired, raise
your hand,' and every hand would go up."
Such a fundamental change in human nature is hardly without risks. "Emphasize
the idea that we may be playing with fire here," says Emsellem. "Who knows why
we get cancer? Chronic sleep deprivation may be a risk factor for long-term
disease. I would love to get by on five hours of sleep because I don't like to
lie in bed, leashed by a sleep requirement. I would love to be unleashed. But at
the same time, prove that it is safe. I don't need another round of winter flu,
thank you very much. Getting sick, being constitutionally exhausted."
"When you have debate on this topic," says Edgar, "on one side, people say:
'Just sleep more. Do what you have to do and the economy be damned. Get the
sleep that you need and that's that.' On the other side, people are saying: 'But
wait a minute. This is a 24-hour world. Those services have to be performed at
the highest level they can. People make mistakes.' "
How do you compete?
Edgar sighs.
"This gets into this fair and legitimate debate. Type A people in Washington go
until they drop. You don't know the ultimate consequences. The extra load on the
kidneys, liver, pancreas, endocrine functions. This could be really important."
"The final twist is that caffeine is a food additive," says Edgar. Replacing
caffeine with modafinil -- "that would be the revolutionary next step. Just as
one replaces sugar with NutraSweet. Everybody drinks soda pop with caffeine from
the age of 5 up. Yeah. You're changing the world. Yeah. I'm telling you as a
sleep scientist the kinds of things we see on the horizon. It's exciting.
Changing lives. Saving lives. That's for certain.
"Is it appropriate for college students pulling an all-nighter? No. Sleep
physiologists will all tell you the same thing. There is no true substitute for
sleep itself. We say that with conviction," Edgar says.
Suppose that will no longer be the case?
"The more far-out question is: What if we eventually had something that was
absolutely safe that could substitute for sleep?" asks Dinges. "Is that the
direction we want to go? Many would say yes. I don't know what the implications
are for our species. Probably not bad. This is pure speculation. Should humans
try to live without sleep? I don't know. We're already trying to do that."
Friday afternoon, 4 p.m., Hour 33. Tired from all this writing. But not sleepy.
Interesting to imagine a future in which those are two distinctly separate
things. The problem isn't wakefulness. The problem is cranking through three or
four days' worth of work in one burst.
Started to yawn at 8 a.m., at the bottom of circadian rhythms. Lay down for a
two-hour nap. As researchers say, this stuff doesn't prevent you from sleeping,
it just controls the desire to. Arose alert. Went back to productive work. Naps
are good, as the sleep researchers ceaselessly point out.
Glad this experiment occurred in a home office, and not downtown. Wouldn't
relish driving at this point. Don't feel impaired, but wouldn't want to test the
proposition. Have no interest in taking any more pills to further the
experiment. Looking forward to returning to the planet of the mortals with a
glass of wine and a good supper.
Wonder what this will read like after a good night's sleep? The concern is this:
One is always taught never to hand in a complicated project at the end of the
day. Read it over one last time with fresh eyes in the morning. But fresh eyes
are optional, when you don't have to sleep. Fatigue still hasn't set in. It
wouldn't be hard to hand this in and begin preparations for the next project
with a whole afternoon in front of you. What happens when fresh eyes are a
choice, not an inevitable part of the rhythms of life?
We will be asking ourselves these questions about human nature with increased
frequency as biotechnology advances and drugs originally designed for the sick
begin to augment the healthy. We have already seen this happen with Viagra. It
now sponsors network evening news shows, a development that would have boggled
scenario planners just five years ago. More drugs are in the works that attack
shyness, forgetfulness and the mental decline of aging. Others add muscle mass
and boost the ability to learn, at least in mice.
Saturday morning, 10 a.m., Hour 51, after eight hours of sleep. Would need to
have an awfully compelling reason to want to do this again. But can imagine how
others might differ. Sure was a lot of living packed into the last two days. Got
so much done that there is a whole unencumbered weekend in sight. What a
concept.
Reported By TechNews.com, http://www.TechNews.com
(20020617/WIRES /)
LOAD-DATE: June 18, 2002
LANGUAGE: ENGLISH
TYPE: news
Copyright 2002 Post-Newsweek Business Information, Inc.
873 of 998 DOCUMENTS
The Washington Post
June 17, 2002 Monday
Final Edition
The Great Awakening;
With a Pill Called Modafinil, You Can Go 40 Hours Without Sleep -- and See Into
the Future
BYLINE: Joel Garreau, Washington Post Staff Writer
SECTION: STYLE; Pg. C01
LENGTH: 3996 words
Grubb's Pharmacy is an unassuming if not seedy two-story clapboard landmark amid
the grand brick townhouses of East Capitol Street. Not only is it one of the
busiest pharmacies in the District. But being only four blocks from the Capitol,
it is also the neighborhood provider of potions and portents to congressmen,
lobbyists, super-lawyers, Supreme Court justices, ambitious aides and all those
other classic Type A Washingtonians who think that whatever they're working on
is The Most Important Thing in the World. And of course sometimes they may be
right.
Yet Grubb's is filling only about five prescriptions a month for a drug named
modafinil. "It's nothing like Viagra. That was a national explosion," says
Edward F. Dillon, the pharmacist. "Or a drug like Propecia, for hair loss. Or
Prozac. Let me tell you. When Time magazine put that on the cover, you could
definitely see the spike."
This may be the calm before the storm, however. For modafinil may have the power
to change Washington.
What it does is shut off your urge to sleep.
"It's a standing joke among sleep doctors that nobody sleeps in New York or
Washington," says Helene Emsellem, director of the Center for Sleep and Wake
Disorders in Chevy Chase. "Except in New York they do it for pleasure, while in
Washington they do it to work."
In trials on healthy people like Army helicopter pilots, modafinil has allowed
humans to stay up safely for almost two days while remaining practically as
focused, alert, and capable of dealing with complex problems as the well-rested.
Then, after a good eight hours' sleep, they can get up and do it again -- for
another 40 hours, before finally catching up on their sleep.
Originally aimed at narcoleptics, who fall asleep frequently and uncontrollably,
modafinil works without the jitter, buzz, euphoria, crash, addictive
characteristics or potential for paranoid delusion of stimulants like
amphetamines or cocaine or even caffeine, researchers say. As with an increasing
number of the so-called superhuman, posthuman or trans-human drugs or genetic
manipulations rapidly entering our lives, modafinil thus calls into question
some fundamental underpinnings of hundreds of thousands of years of thought
regarding what are normal human capabilities.
The implications for Washington are profound.
The Defense Advanced Research Projects Agency is searching for ways to create
the "metabolically dominant soldier." Among the projects it is pursuing is the
creation of a warrior who can fight 24 hours a day, seven days straight.
"Eliminating the need for sleep while maintaining the high level of both
cognitive and physical performance of the individual will create a fundamental
change in war-fighting," says the Defense Sciences Office on its Web site. As
usual, DARPA did not comment directly for this report.
William C. Dement, director of the Stanford University Sleep Center, who is
known as "the father of sleep medicine" for his pioneering work in the '50s,
embraces the idea of modafinil use for official Washington. "If Donald Rumsfeld
had to stay awake for a long period of time, I would want him fully alert," he
says.
Francis Fukuyama of Johns Hopkins University recently published "Our Posthuman
Future: Consequences of the Biotechnology Revolution," a book that is scathingly
critical of what he sees as runaway biotech that could rob us of our very human
nature. When asked about modafinil and its effects on Washington, he responded
with a 2:50 a.m. e-mail from Europe, where he was finishing a grueling
three-week trip. "I haven't heard of this but I'm not surprised," he wrote.
"I better get some," he half-joked.
Modafinil and its follow-on technologies hold the potential for changing
society. "This could replace caffeine," says Joyce Walsleben, director of the
NYU Sleep Disorders Center.
Caffeine -- the globe's most widely used drug -- today is a bigger food additive
in dollar terms than salt. The U.S. soft drink industry alone sold 10 billion
192-ounce cases of bubbly last year, most of it caffeinated.
Modafinil's sales are still small. But it did double sales to $ 150 million in
only the last year, according to Cephalon, the pharmaceutical company that
markets it under the trade name Provigil.
Its potential for changing how people work and live is intriguing. In an
increasingly 24-7 world, will such medicine create even more demand for people
to be available round-the-clock? Were Robert Frost's lines from 1923 prophetic?
The woods are lovely, dark and deep.
But I have promises to keep,
And miles to go before I sleep,
And miles to go before I sleep.
Will people feel that they need to routinely control their sleep in order to be
competitive? Will unenhanced people suffer fewer promotions and raises than
their modified colleagues? Will this start an arms race over human
consciousness?
To get some hint of what such a Washington life might be like, the bulk of the
writing of this article, a task not unlike others with many moving parts --
software development or the juggling of a diplomatic flap -- was accomplished in
one 40-hour period enabled by the prescribed use of modafinil.
10 a.m. Thursday. Third hour awake. Back from working out at the gym. Gazing at
the white 200 mg. tab of modafinil. Hey, how scary can this be. It's not like
this is life's first all-nighter. This one is even legal. Ironic. Four decades
after the '60s, some of the most startling drugs are those available by
prescription. But safety first. Take the advice of the sleep docs. Cut the tab
in half. If, as sometimes happens, there is going to be a headache or nausea,
start with a low dose.
Humans have been manipulating their sleep chemistry for a long time. Caffeine is
as old as coffee in Arabia, tea in China and chocolate in the New World.
For at least as long, sleep has been seen as a universal solvent.
"Now blessing light on him that first invented this same sleep!" says Sancho
Panza in "Don Quixote." "It covers a man all over, thoughts and all, like a
cloak; 'tis meat for the hungry, drink for the thirsty, heat for the cold, and
cold for the hot. 'Tis the current coin that purchases all the pleasures of the
world cheap; and the balance that sets the king and the shepherd, the fool and
the wise man even."
The effects of medicated sleeplessness on a vast healthy population is still
unknown. "Before you start taking it for the rest of your life, find out what it
does to your heart valves or some damn thing," Dement says. "A lot of people
know the story of fen-phen or thalidomide. If you take it all the time, and try
to stay awake all the time, there's a big chance that there may be some hitherto
unknown toxic effect."
Nonetheless, modafinil (pronounced mo-DAF-i-nil) is distinguished by its
apparently precise neurological focus. Nobody knows exactly how modafinil works,
but researchers marvel at the way it seems to target very specific regions of
the brain believed to regulate normal wakefulness. It's that narrow effect that
is lacking in other stimulants, resulting in their notorious side effects.
In fact, on the wall of his office at a company named Hyperion, off Boston's
Interstate 495 near Worcester, Mass., sleep researcher Dale M. Edgar has a sign.
"It's about the sleepiness, stupid," it reads.
As with the rest of the cascade of new drugs that promise to augment human
performance, here are three groups of people who will ultimately be attracted to
new wakefulness drugs, researchers say. In this order, they are:
* The sick.
* The otherwise healthy with a critical need.
* The rest of us.
It's the future of the third group -- the millions who, in the immortal words of
Kiss, "wanna rock and roll all nite and party every day" -- that deeply concerns
the sleep business.
The Food and Drug Administration so far has approved modafinil marketing only to
narcoleptics, as the FDA reminded Cephalon in January, when it charged that the
company's promotional materials were overreaching. Cephalon will soon submit an
application to the FDA to expand its marketing to people with other sleep
disorders, including the ones associated with sleep apnea and Parkinson's
disease.
There are only 125,000 to 250,000 narcoleptics in the United States. Cephalon
brags that hundreds of thousands of patients have taken Provigil, with over a
million prescriptions written as of 2001, and sales soaring. Nonetheless,
Cephalon spokesman Sheryl Williams says that "we are not aware of any
significant prescribing of the drug for nonmedical conditions."
What exactly is a "nonmedical condition"?
This enters the murky world of the second group -- healthy people engaged in
"mission-critical tasks for which sleepiness is not an option," as Edgar puts
it.
"Like flying a big C-17 transport plane from Charleston Air Force Base to
Afghanistan virtually nonstop," says Edgar. "That happened. There are lots of
examples in the Air Force. It's what they call susops -- sustained operations.
You really, really need something on those long flights, and not just for the
pilots. The payload specialists in back have no place to sleep, and they have to
be on the ready to deploy the load. It's hard, but it's also critical to the
success of the mission, and reducing accidents."
The crucial issue is not staying awake. It's doing so without making lethal
mistakes. The fatal decision to launch the Challenger space shuttle was made by
people handling very complex data after days of irregular work hours and
insufficient sleep, as all sleep researchers remind themselves.
Fort Rucker, Ala., is 58,000 hot and steamy acres of Southern pine and the
occasional wild magnolia. All the Army's helicopter pilots are trained there.
John Caldwell has a low, impressively equipped, sprawling brick sleep laboratory
with the Air Crew Health and Performance Division of the U.S. Army Aeromedical
Research Laboratory. His modafinil study is the one that kept awake the
helicopter pilots -- "normals without any pathological conditions," as he so
clinically puts it.
The pilots flew a simulator in which they had to respond quickly to commands --
to fly for two minutes straight and level at 3,000 feet maintaining 120 knots at
a heading of 180, for example, then perform a turn of 360 degrees over exactly
two minutes, maintaining speed and altitude. Then the pilots had to perform four
different tasks simultaneously -- watching warning lights come on and dials
deviate from normal, while monitoring the fuel levels and clearing blockages,
while holding a target constant, while responding on the radio to someone
commanding, "NGT 504, NGT 504, set communications radio to 121.5"
Caldwell expresses a sentiment volunteered by almost every sleep researcher.
"One thing I want to make clear -- when we look at compounds like modafinil or
amphetamines or caffeine, those are emergency kinds of measures, not a
replacement for sleep. It's not nice to fool with Mother Nature."
Says Stanford's Dement: "The real problem is the accumulated sleep debt, not
daily need. It's established fact that lost sleep accumulates. You quickly
become too tired to be functional." Even with a substance like modafinil that
can keep you wakeful, if you don't ultimately catch up on the sleep you missed,
bad things will happen, sleep researchers have always believed.
"Your grandmother was right. If you don't get enough sleep, you're going to get
sick," says Chevy Chase researcher Emsellem.
When you're facing a critical situation, however, it's better to have help being
alert, Caldwell firmly believes. "Combat operations are very unpredictable."
Even with a 14-hour-a-day rest schedule, "if the enemy attacks during the 14
hours off, we're going to have to respond."
"There are a lot of other medically justified scenarios," says Edgar. "Think of
emergency medical services. What happens when a building collapses? As we
unfortunately learned recently, teams work around the clock. Can you justify it
to save lives? Absolutely. Particularly if it's a hazardous situation. Somebody
needs to do the job, and if there is something that is safe, effective, and
non-habit-forming, I think the answer is yes."
Sleep research is a very young science, and the number of things it doesn't know
about substances like modafinil is daunting.
"How long can somebody stay awake and not suffer? Hard to say. The jury is still
out," says Edgar, who is on leave from Stanford. He is now ensconced in a serene
research facility sporting green glass that matches the stripes of the mallard
ducks on the pond. Inside are a sophisticated array of computers and hundreds of
mice and rats. In his small office, wraparound screens stream brain wave
activity being transmitted live from around the world over the Internet. Edgar
has taken up a new role as senior vice president for preclinical research at
Hypnion, which he describes as the world's first biotech company specifically
dedicated to solving problems of sleep-wake disorders.
"Do you function as if you were rested? The answer is you're probably better off
than if you haven't taken it, but you're not at 100 percent. Where are you?
Fifty percent on cognitive performance? Is that good enough?"
But then Edgar drops the bomb.
"The next generation of wake-performing therapeutics will be more effective.
You'll be able to stay awake for X amount of time and not add sleep debt.
Ideally, it means being able to be up all day, all night, and all the next day
and not have incremental increase in sleepiness or in sleep debt. It would be
medication that gives you an interest-free loan.
"It could change the world. A complete paradigm shift. I'm not trying to plug my
company. But we are in the forefront. We could see this being a reality,
starting to become available, in about five years."
Friday, 2 a.m., Hour 19. The effortless mental focus brought on by modafinil is
remarkable. No attention deficit here. The feeling is that you have been given a
gift of time, and it is too precious to waste.
The focus is almost more interesting than the sleep-avoidance. In fact, it makes
you wonder what it will be like to grow up in a world in which this stuff is
common. Suppose you are just getting started in a career and you're a basket of
insecurities. Suppose you could regularly produce at levels unheard of even by
today's workaholic standards simply by popping a pill. Could you resist it?
Worse yet, suppose you were competing for raises and promotions against someone
who was happy to grab whatever enhancements were available. Will it become
routine to hear "There'll be plenty of time to sleep when you're 40"?
You can't get high on modafinil. There's no euphoria to it. When they first take
it, a lot of test subjects figure they must have gotten the placebo.
On this do sleep researchers base their hope that wakefulness agents won't be
the next glam drug phenom, hyped on magazine covers and distributed with abandon
to people for whom they were never intended, under circumstances that have never
been studied.
But they know the facts. Two-thirds of all Americans don't get enough sleep,
according to the National Sleep Foundation. Sleep deprivation may be a factor in
the national epidemic of obesity. America is full of people burning the candle
at both ends, wanting to know only where they can get more wax.
"Most of them are impaired. A lot of jobs you can do almost in your sleep --
lifting boxes onto shelves in a department store," says Dement. "But I'm
frequently an expert witness in cases that involve falling asleep at the wheel.
A recent case involved a man who was working two jobs, and on the night job he
was frequently observed to fall asleep. His supervisor escorted him out the
door. He drove into an oncoming lane and killed three people."
The graveyard shift is hardly just for factory workers anymore. The world is
open 24-7 -- restaurants, health clubs, Wal-Marts, Home Depots, help desks,
stock and commodities traders, catalogue sales and overnight shippers, to
mention a few. Why do people getting off the red-eye from Los Angeles or to
London seem so ruefully proud even when they look like dog meat? The classic
hero figure of capitalism is the CEO who says he never needs more than a few
hours of sleep -- he's proud of being on the go all the time.
Washington has its own special breeds of sleep-defiers. Think of the rat
calculus of campaign strategists running the maze of late October before
Election Day. Hunched and harried, they work the phones to the Coast until 2 or
3 in the morning, while writing the candidate's talking points for the next day,
and then hitting the Eastern time zone phones at dawn. The badge of special
honor is simultaneously to be advising campaigns from Washington in the time
zones of Britain and Israel.
Friday, 4 a.m., Hour 21. When this stuff takes over, it takes over. Gently, not
violently. No apparent loss of acuity. But you have definitely kicked into a
gear you didn't know you had.
Playing computer games like FreeCell as an informal way of testing cognitive
ability. Do you dare send e-mails? Will you regret them when you return to
normal?
Speaking of rhythms, remember to eat. Got to keep up strength. Discomfort still
far less than it would have been had coffee been used to accomplish this task.
Getting awful sick of herb tea, though.
So what about the dreaded third group -- the rest of us, those who are in a
fundamentally different situation from the first two groups? We have a choice
whether to live a saner life or try to solve our problems with a pill.
"The young professional who wants to work and play and do everything, and
doesn't want to spend time sleeping?" asks University of Pennsylvania sleep
researcher David Dinges. "That's another matter."
Yes, sleep researchers grudgingly admit, there are going to be some
way-off-label users. The college students crashing on term papers. Truck
drivers. Barge operators. Airline pilots. The physician in long hours of
training. The new parent. Ever watch the White House-based television show "The
West Wing?" They never seem to go home. That is not fantasy.
"Sleepiness is everywhere," says Neil Feldman, medical director of the St.
Petersburg, Fla., Sleep Disorder Center, who is conducting a shift work study
for Cephalon. "We're a 24-hour society. We no longer live by the night/day
cycle. We live by whatever our occupation demands. Physicians on call at night.
Nuclear power plant operators. Police, firemen. Plus the world is becoming a
smaller place. Trans-meridian travel, commonly known as jet lag. There are
economic demands -- more than one job -- plus raising children.
"How many have fallen asleep at the wheel of a car? Something like 25 percent at
least momentarily once during the year. Sleep deprivation is everywhere. Our
society looks at people who sleep as less strong people. People who nap are
slugs."
Suppose a lawyer came to you and said, "I have a client on death row and the
governor has just given me three days to draft his appeal before he is
executed."
"I'd probably prescribe the drug," Feldman said. "But three pills. Not a
hundred. I can rationalize that."
"People ask me about it almost daily," says Dement. "Everybody would like to be
able to have more time to do whatever they want to do. I could stand in front of
a roomful of Stanford undergrads right now and say, 'If you feel tired, raise
your hand,' and every hand would go up."
Such a fundamental change in human nature is hardly without risks. "Emphasize
the idea that we may be playing with fire here," says Emsellem. "Who knows why
we get cancer? Chronic sleep deprivation may be a risk factor for long-term
disease. I would love to get by on five hours of sleep because I don't like to
lie in bed, leashed by a sleep requirement. I would love to be unleashed. But at
the same time, prove that it is safe. I don't need another round of winter flu,
thank you very much. Getting sick, being constitutionally exhausted."
"When you have debate on this topic," says Edgar, "on one side, people say:
'Just sleep more. Do what you have to do and the economy be damned. Get the
sleep that you need and that's that.' On the other side, people are saying: 'But
wait a minute. This is a 24-hour world. Those services have to be performed at
the highest level they can. People make mistakes.' "
How do you compete?
Edgar sighs.
"This gets into this fair and legitimate debate. Type A people in Washington go
until they drop. You don't know the ultimate consequences. The extra load on the
kidneys, liver, pancreas, endocrine functions. This could be really important."
"The final twist is that caffeine is a food additive," says Edgar. Replacing
caffeine with modafinil -- "that would be the revolutionary next step. Just as
one replaces sugar with NutraSweet. Everybody drinks soda pop with caffeine from
the age of 5 up. Yeah. You're changing the world. Yeah. I'm telling you as a
sleep scientist the kinds of things we see on the horizon. It's exciting.
Changing lives. Saving lives. That's for certain.
"Is it appropriate for college students pulling an all-nighter? No. Sleep
physiologists will all tell you the same thing. There is no true substitute for
sleep itself. We say that with conviction," Edgar says.
Suppose that will no longer be the case?
"The more far-out question is: What if we eventually had something that was
absolutely safe that could substitute for sleep?" asks Dinges. "Is that the
direction we want to go? Many would say yes. I don't know what the implications
are for our species. Probably not bad. This is pure speculation. Should humans
try to live without sleep? I don't know. We're already trying to do that."
Friday afternoon, 4 p.m., Hour 33. Tired from all this writing. But not sleepy.
Interesting to imagine a future in which those are two distinctly separate
things. The problem isn't wakefulness. The problem is cranking through three or
four days' worth of work in one burst.
Started to yawn at 8 a.m., at the bottom of circadian rhythms. Lay down for a
two-hour nap. As researchers say, this stuff doesn't prevent you from sleeping,
it just controls the desire to. Arose alert. Went back to productive work. Naps
are good, as the sleep researchers ceaselessly point out.
Glad this experiment occurred in a home office, and not downtown. Wouldn't
relish driving at this point. Don't feel impaired, but wouldn't want to test the
proposition. Have no interest in taking any more pills to further the
experiment. Looking forward to returning to the planet of the mortals with a
glass of wine and a good supper.
Wonder what this will read like after a good night's sleep? The concern is this:
One is always taught never to hand in a complicated project at the end of the
day. Read it over one last time with fresh eyes in the morning. But fresh eyes
are optional, when you don't have to sleep. Fatigue still hasn't set in. It
wouldn't be hard to hand this in and begin preparations for the next project
with a whole afternoon in front of you. What happens when fresh eyes are a
choice, not an inevitable part of the rhythms of life?
We will be asking ourselves these questions about human nature with increased
frequency as biotechnology advances and drugs originally designed for the sick
begin to augment the healthy. We have already seen this happen with Viagra. It
now sponsors network evening news shows, a development that would have boggled
scenario planners just five years ago. More drugs are in the works that attack
shyness, forgetfulness and the mental decline of aging. Others add muscle mass
and boost the ability to learn, at least in mice.
Saturday morning, 10 a.m., Hour 51, after eight hours of sleep. Would need to
have an awfully compelling reason to want to do this again. But can imagine how
others might differ. Sure was a lot of living packed into the last two days. Got
so much done that there is a whole unencumbered weekend in sight. What a
concept.
LOAD-DATE: June 17, 2002
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
874 of 998 DOCUMENTS
Edmonton Journal (Alberta)
May 20, 2002 Monday Final Edition
An assault on sleep: Canadian military researchers look for a way to keep the
troops awake: OVERCOMING THE INSTINCT TO SLEEP
SOURCE: Southam Newspapers; Ottawa Citizen
BYLINE: Tim Lougheed
SECTION: Living Well; Pg. C2
LENGTH: 840 words
DATELINE: Ottawa
Perhaps from the time the first human being had to pull an all-nighter, the
enemies of sleep have been hard at work on ways of helping us overcome this very
powerful natural instinct.
But while stimulants such as amphetamines or caffeine have become
well-established for their effectiveness, along with their various side effects,
researchers are now focusing on a new and very different drug that was developed
less than 20 years ago.
Modafinil is a synthetic compound discovered in the early 1980s by a small
family-owned French pharmaceutical firm, Lafon Laboratories.
Although its biochemical mechanism is still not fully understood, the drug was
quickly hailed as a revolutionary new treatment for narcolepsy. This chronic
condition causes people to suffer from a constant, irresistible urge to fall
asleep, yet the quality of their sleep is poor.
Conventional stimulants can help narcoleptics resolve their symptoms
temporarily, but these treatments do not address the underlying problem.
Modafinil apparently does, at least for some patients.
By managing their dosage, these individuals are able to stay awake through the
day and get a restful night's sleep, with few significant side effects.
Above all, the drug continues to remain effective, even after it has been taken
for as long as 15 years.
The unique properties of modafinil have inspired active exploration of possible
applications.
"There's a whole world of researchers that are working on this drug right now,"
says Joseph Baranski, a member of the human factors division of Defence R&D
Canada.
The Toronto-based facility is one of five federal military research
installations across Canada, and has taken a leading role in examining the
elements that enable people to perform at their best under ordinary and
extraordinary circumstances.
Not surprisingly, sleep is among the foremost of those elements. And it takes on
special significance when it comes to planning intense missions that might
require troops to remain awake and alert for several days at a time.
The U.S. military has published studies about the use of amphetamines by its
pilots flying night missions.
Over the last decade Defence R&D Canada has compared the value of amphetamines
and modafinil under simulated mission-critical conditions.
Ross Pigeau, head of the agency's human factors division, led a major study
conducted in 1994. Subjects were kept awake continuously for 64 hours, and kept
busy with a series of computer tasks lasting almost two hours at a time.
At key points, some participants were given amphetamines, some were given
modafinil, and some were given placebos, although no one knew who was getting
what.
As measured by the quality of computer work, modafinil managed to stave off a
serious drop in mental competence after almost three days. For people taking
nothing, that drop could amount to two-thirds of performance.
Modafinil kept the decrease to about half of that amount, with the added virtue
of not disturbing the quality of sleep afterward, which amphetamines can do.
"It seems that the mechanism of it is much different than amphetamines," says
Pigeau. "Amphetamine is a general nervous system stimulant. It just gooses up
the whole nervous system. Whereas modafinil apparently stops you from feeling
sleepy. It essentially inhibits the natural sleep-inducing processes of the
brain."
In fact, modafinil does not attack sleep so much as it promotes wakefulness.
Over the past few decades, scientists studying sleep have learned even more
about what it means to be awake. According to Roger Broughton, who has been in
the field for 40 years, there are in upwards of seven distinct brain centres
controlling this aspect of our consciousness. Modafinil acts on at least one of
them.
"There are multiple brain systems with different transmitters that sustain
wakefulness," says Broughton, who conducts sleep research at the Ottawa
Hospital's General campus.
"We don't really know yet their hierarchical interactions. But almost all of
them do other things as well."
He was one of the principal researchers in a definitive Canadian study,
published in 1997, which led to Health Canada's approval of modafinil in 1999.
The drug is still listed as a controlled substance, although it can be found for
sale on the Internet through mail-order drug warehouses operating out of
offshore legal havens such as Britain's Channel Islands.
Because the neurological mechanism of modafinil is still being fathomed,
researchers are highly cautious about its widespread use.
For now the prospect worries Timothy Monk, director of the human chronobiology
research program at the University of Pittsburgh Medical Centre.
"What I worry about is the issue of somebody who wants to succeed in business
and work 100-hour weeks, and the way to do that is to pop a modafinil.
"That is a cause for concern, given that we don't know the effects of only
having four hours of sleep and then avoiding the negative sleepiness with a
pill."
LOAD-DATE: May 20, 2002
LANGUAGE: ENGLISH
GRAPHIC: Photo: Southam Newspapers, Ottawa Citizen; Canadian research looks at
ways to enable people to perform at their best without sleep.
TYPE: News
Copyright 2002 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
875 of 998 DOCUMENTS
Internet Wire
May 20, 2002 Monday
Attention Science Writers: New Clinical Data In Treating Symptoms Of Depression
LENGTH: 1063 words
DATELINE: May 20, 2002; INTERNET WIRE
Depression affects more than 18 million American adults annually. Patients
experience persistent sadness, anxiousness, or emptiness along with feelings of
hopelessness, pessimism and guilt, and a loss of interest or pleasure in hobbies
and activities that they once enjoyed.
In addition, patients also suffer from equally debilitating physical symptoms,
such as fatigue and excessive daytime sleepiness (EDS). These patients also
report feeling a "lack of energy" and constant weariness, drowsiness and
exhaustion, despite the amount of sleep they receive.
Further, antidepressant medications often exacerbate fatigue and EDS, leaving
the patient feeling sleepy, sluggish, lethargic and, ultimately, hopeless about
ever being "cured" of depression. Mental health professionals have just begun
to understand the importance of managing these less noticeable, yet equally
harmful, symptoms of depression that have a tremendous impact on the patient's
recovery.
WHAT:Study results on modafinil, the latest therapeutic agent
being investigated for the management of EDS and fatigue in patients
with depression.
Abstract attached:
-- Adjunct Modafinil Rapidly Improves Fatigue and Wakefulness in
Patients with Major Depressive Disorder- Doghramji, K., et al.
-- Effect of Adjunct Modafinil on Energy and Concentration in
Depressed Patients- Menza, M.A., et al.
WHO:Study Investigators:
Karl Doghramji, M.D.
Associate Professor of Psychiatry and Human Behavior
Jefferson Medical College
Philadelphia, PA
Matthew A. Menza, M.D.
Chief of Clinical Psychopharmacology
Robert Wood Johnson Medical School
Piscataway, NJ
WHEN: Monday, May 20, 2002
11 a.m.- 12: 30 p.m. EST
Thursday, May 23, 2002
11 a.m.- 12: 30 p.m. EST
WHERE:155th Annual Meeting of the American Psychiatric Association
Philadelphia Convention Center
Level 200, Room 204 A
Please visit www.provigil.com for complete prescribing information.
--------------------------------------------------------------------------------
------------------------------------------------------------ Modafinil Rapidly
Improves Fatigue and Wakefulness in Patients With Major Depressive Disorder
Karl Doghramji, M.D., Sleep Disorders Center, Thomas Jefferson University, 1015
Walnut St, Ste 319, Philadelphia, PA 19107; Matthew Menza, M.D., Murray
Rosental, D.O., Ronald Fieve, M.D.
OBJECTIVE: and sleepiness are primary symptoms of major depressive disorder
(MDD) that often do not resolve with antidepressant therapy and may require
additional therapeutic measures. Modafinil, a novel wake-promoting agent,
improves wakefulness in patients with excessive sleepiness, and reduces fatigue
in patients with multiple sclerosis. This study evaluated the effects of
Modafinil on fatigue and sleepiness in patients with MDD.
METHOD: with partial response to antidepressants given for at least 6 weeks for
a current major depressive episode were enrolled in this -week, randomized,
double-blind, placebo-controlled, multicenter study. Patients received
Modafinil (100-400 mg/day) or placebo as adjunct treatment to ongoing
antidepressant therapy. Changes in fatigue and daytime sleepiness were
evaluated using the Fatigue Severity Scale (FSS) and Epworth Sleepiness Scale
(ESS), respectively. Adverse events were recorded.
RESULTS: 136 patients randomized, 118 (87%) completed the study. Most patients
were fatigued (82%), and half (51%) were sleepy. Modafinil rapidly improved
fatigue and daytime wakefulness, with significantly greater mean changes from
baseline than placebo in FSS scores at week 2 (p < 0.05) and ESS scores at week
1 (p < 0.01). Modafinil was well tolerated in combination with a variety of
antidepressants.
CONCLUSION: may be a useful adjunct for the management of fatigue and sleepiness
in patients who are partial responders to antidepressant therapy.
FUNDING: by Cephalon, Inc.
Literature References: 1. Menza MA, Kaufman KR, Castellanos A. Modafinil
augmentation of antidepressant treatment in depression. J Clin Psychiatry
2000;61:378-381. 2. DeBattista C, Solvason HB, Kendrick E, Schatzberg AF.
Modafinil as an adjunctive agent in the treatment of fatigue and hypersomnia
associated with major depression. In: New Research Program and Abstracts of the
154th Annual Meeting of the American Psychiatric Association; May 9, 2001; New
Orleans, LA. Abstract NR532:144
--------------------------------------------------------------------------------
------------------------------------------------------------ Use of Modafinil in
Depression
To recognize the potential benefit of Modafinil, a wake promoting medicine in
the treatment of some depressed patients
Menza MA, et al: Modafinil Augmentation of Antidepressant Treatment in
Depression. J Clin Psychiatry 2000; 61:378-381
Mitchell PB: Novel Antidepressants Not Available in the United States.
Psychopharmacology Bull 1995; 31(3): 509-519
OBJECTIVE: study is a retrospective review of the use of Modafinil, a wake
promoting agent, as an adjunct in the treatment of depression in a general
psychiatric practice.
METHODS: records of seventy-eight (N=78) depressed Caucasian outpatients who
were deemed in need of adjunctive treatment with a stimulant over a 9 months
period were reviewed. There were 49 females and 29 males. Their mean age was
44 years (+/- 14). 55 patients (71%) had previously failed or did not tolerate
other stimulants. 60 patients (77%) were diagnosed with Unipolar Depression, 13
(71%) with Bipolar Depression, and 5 with other depression diagnoses. Outcome
measures included the Visual Analog Scale (VAS), the Carroll Depression (self)
Rating Scale, the CGI-C pre and post treatment.
RESULTS: were significant improvement in the CGI-S score (p < 0.001), CDRS (p <
0.02) and VAS (p < 0.03). The mean CGI-C was 1.91 (+/- 0.94) Modafinil was well
tolerated at an average dose of 249mg/day (+/- 122mg) and a range of 100 to 800
mg/day.
CONCLUSIONS: Modafinil is a useful adjunct in the treatment of depression,
especially when stimulants are needed for help with sleepiness and fatigue, or
incomplete remission with antidepressants.
CONTACT:
Sheryl Williams
Cephalon
610-738-6493
swilliam@cephalon.com
Andrea Pelliciarri
Hill and Knowlton
212-885-0623
apellicc@hillandknowlton.com
LOAD-DATE: May 21, 2002
LANGUAGE: ENGLISH
Copyright 2002 Internet Wire, Incorporated.
All rights reserved.
876 of 998 DOCUMENTS
Ottawa Citizen
May 13, 2002 Monday Final Edition
An assault on sleep: A drug used to keep narcoleptics awake is being tested by
Canadian military researchers as a way to keep troops awake and alert for days,
reports Tim Lougheed.
SOURCE: The Ottawa Citizen
BYLINE: Tim Lougheed
SECTION: News; Pg. A12
LENGTH: 936 words
Perhaps from the time the first human being had to pull an all-nighter, the
enemies of sleep have been hard at work on ways of helping us overcome this very
powerful natural instinct. But while stimulants such as amphetamines or caffeine
have become well-established for their effectiveness, along with their various
side effects, researchers are now focusing on a new and very different drug that
was developed less than 20 years ago.
Modafinil is a synthetic compound discovered in the early 1980s by a small
family-owned French pharmaceutical firm, Lafon Laboratories. Although its
biochemical mechanism is still not fully understood, the drug was quickly hailed
as a revolutionary new treatment for narcolepsy. This chronic condition causes
people to suffer from a constant, irresistible urge to fall asleep, yet the
quality of their sleep is poor.
Conventional stimulants can help narcoleptics resolve their symptoms
temporarily, but these treatments do not address the underlying problem.
Modafinil apparently does, at least for some patients. By managing their dosage,
these individuals are able to stay awake through the day and get a restful
night's sleep, with few significant side effects. Above all, the drug continues
to remain effective, even after it has been taken for as long as 15 years.
If modafinil works such wonders in people who need to sleep all the time, could
it help the rest of us cut down the amount of sleep we must have each night? The
short answer is no, but the unique properties of modafinil have inspired active
exploration of other possible applications.
"There's a whole world of researchers that are working on this drug right now,"
says Joseph Baranski, a member of the human factors division of Defence R&D
Canada. The Toronto-based facility is one five federal military research
installations across Canada, and has taken a leading role in examining the
elements that enable people to perform at their best under ordinary and
extraordinary circumstances.
Not surprisingly, sleep is among the foremost of those elements. And it takes on
special significance when it comes to planning intense missions that might
require troops to remain awake and alert for several days at a time. The U.S.
military has published studies about the use of amphetamines by its pilots
flying night missions, who have access to the drug but are not under orders to
take it. Canada has no policy of similar sleep-fighting drug use in military
settings, but over the last decade Defence R&D Canada has compared the value of
amphetamines and modafinil under simulated mission-critical conditions.
Ross Pigeau, head of the agency's human factors division, led a major study
conducted in 1994. Subjects were kept awake continuously for 64 hours, and kept
busy with a series of computer tasks lasting almost two hours at a time. At key
points, some participants were given amphetamines, some were given modafinil,
and some were given placebos, although no one knew who was getting what.
As measured by the quality of computer work, modafinil managed to stave off a
serious drop in mental competence after almost three days. For people taking
nothing, that drop could amount to two-thirds of performance. Modafinil kept the
decrease to about half of that amount, with the added virtue of not disturbing
the quality of sleep afterward, which amphetamines can do.
"It seems that the mechanism of it is much different than amphetamines," says
Mr. Pigeau. "Amphetamine is a general nervous system stimulant. It just gooses
up the whole nervous system. Whereas modafinil apparently stops you from feeling
sleepy. It essentially inhibits the natural sleep-inducing processes of the
brain."
In fact, modafinil does not attack sleep so much as it promotes wakefulness.
Over the past few decades, scientists studying sleep have learned even more
about what it means to be awake. According to Roger Broughton, who has been in
the field for 40 years, there are in upwards of seven distinct brain centres
controlling this aspect of our consciousness. Modafinil acts on at least one of
them.
"There are multiple brain systems with different transmitters that sustain
wakefulness," says Dr. Broughton, who conducts sleep research at the Ottawa
Hospital's General campus. "We don't really know yet their hierarchical
interactions. But almost all of them do other things as well."
He was one of the principal researchers in a definitive Canadian study,
published in 1997, which led to Health Canada's approval of modafinil in 1999.
The drug is still listed as a controlled substance, although it can be found for
sale on the Internet through mail-order drug warehouses operating out of
offshore legal havens such as Britain's Channel Islands.
Because the neurological mechanism of modafinil is still being fathomed,
researchers are highly cautious about speculating as to whether it will find a
place alongside such popular and widely available stimulants as caffeine. For
now the prospect worries Timothy Monk, director of the human chronobiology
research program at the University of Pittsburgh Medical Centre.
"The potential use for modafinil is clear and to some extent proven," says Dr.
Monk, who is currently examining its use by groups like firefighters and
astronauts. "What I worry about more is the issue of somebody who wants to
succeed in business and work 100-hour weeks, and the way to do that is to pop a
modafinil. That is a cause for concern, given that we don't know the effects of
only having four hours of sleep and then avoiding the negative sleepiness with a
pill."
LOAD-DATE: May 13, 2002
LANGUAGE: ENGLISH
GRAPHIC: Colour Photo: Stephen Thorne, the canadian press; Defence R&D Canada is
examining whether modafinil, a narcolepsy drug, can be given to troops who must
perform at their best under extraordinary circumstances, even if they are
severely sleep-deprived.
TYPE: News
Copyright 2002 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
877 of 998 DOCUMENTS
Neurology Alert
May 1, 2002
CME Questions
LENGTH: 279 words
CME Questions
Regarding functional recovery after perinatal brachial plexus injury (PRPP):
a. spontaneous recovery rates are high in Grade 1 and Grade 2 injuries.
b. sensory function may recover in infants with high-grade avulsions only if
surgery is performed by age 3 months.
c. following surgery, there is substantial loss of topographic localization of
stimuli.
d. a substantial number of children report pain several years following severe
perinatal brachial plexus injury.
e. only nonoperated patients describe severe pain years after perinatal brachial
plexus injury.
In the treatment of fatigue in MS, Rammohan et al found that:
a. modafinil was well tolerated in patients.
b. 200 mg/d of modafinil significantly improves fatigue.
c. 400 mg/d did not significantly improve fatigue.
d. None of the above
e. All of the above
Electrical stimulation following nerve injury:
a. depresses BDNF levels in regenerating nerve.
b. enhances nerve growth factor (NGF) levels.
c. increases trkB mRNA expression in the injured nerve.
d. All of the above
e. None of the above
In patients with a spontaneous CSF leak, all of the following suggest an
underlying connective tissue disorder except:
a. hyperflexible joints.
b. laxity of joints
c. history of a carotid artery dissection.
d. retinal detachment at a young age.
e. mental retardation.
Microendoscopic decompressive laminotomy:
a. is the procedure of choice for lumbar spinal stenosis.
b. is associated with an increased incidence of dural tears.
c. may be as effective for spinal stenosis as unilateral open laminotomy.
d. is associated with a decreased incidence of injury to the exiting nerve
roots.
e. None of the above
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2002 AHC Media LLC
All Rights Reserved
878 of 998 DOCUMENTS
The Washington Post
April 28, 2002 Sunday
Final Edition
For Sleep-Deprived, a Dream Drug?;
Doctors Question Use of Narcolepsy Medicine to Support Lifestyle Choice
BYLINE: Shankar Vedantam, Washington Post Staff Writer
SECTION: A SECTION; Pg. A03
LENGTH: 1377 words
Merrill Mitler travels frequently, often sleeping consecutive days in different
time zones. When his body clock feels out of sync with his schedule, he swallows
a medicine that was approved to treat sleepiness associated with a rare disorder
he doesn't have.
Americans last year bought $ 150 million worth of the drug modafinil, which was
approved to treat narcolepsy, an unusual disorder that causes people to fall
asleep suddenly. Three-quarters of the pills were swallowed by people who didn't
have narcolepsy. Doctors are prescribing the drug to patients with other
disorders and, increasingly, to people with no disorder at all.
Three years after it was approved, the medicine is raising questions about how
many healthy Americans might soon want it simply to sleep less -- yet another
example of a medicine being used not to treat illness, but to support a
lifestyle choice.
Unlike amphetamines and conventional stimulants, modafinil does not give people
a jolt. Doctors believe it is not addictive and say it is generally safe, with
only occasional side effects such as headache or nausea. But no one knows what
might happen if people use the drug to do away with sleep for prolonged periods.
"The biggest questions are societal," said Thomas Scammell, a neurologist at
Harvard Medical School. "What's to keep us from working 24-7? . . . To take a
drug and try to counter this natural necessity of sleep is to defy nature. It's
like if I can give you a pill to take away your appetite -- does it mean it's
okay not to eat?"
The drug's manufacturer, Cephalon Inc. of West Chester, Pa., had promoted it as
effective for more than just narcolepsy. But after the Food and Drug
Administration charged in January that Cephalon's promotional materials were
"false, lacking in fair balance or otherwise misleading," the company promised
to limit its promotional pitches to narcolepsy. The company plans eventually to
present studies to the FDA that would expand the drug's approval for sleepiness
associated with a variety of psychiatric and neurological disorders.
Studies are also underway to test whether modafinil can help healthy truck
drivers navigate night journeys and get to their destinations safely by dawn.
The military is investigating whether modafinil can help healthy soldiers stay
awake for lengthy periods in combat. A large trial is studying the medicine's
effectiveness among shift workers.
At one site of this study, the Scripps Research Institute in San Diego,
psychologist Mitler is evaluating whether modafinil can help people fight their
normal circadian rhythms. His use of the medicine suggests he knows the result.
"Do you need a pill to treat a normal condition?" Mitler said. "There is all
sorts of precedent for that -- we take aspirin for sore muscles associated with
exercise. Muscles are supposed to hurt when they are not trained. Yet we
medicalize it in order to treat the discomfort."
"The side effects of caffeine are much more severe than the side effects of
modafinil," said Mitler, who believes that decisions about modafinil are best
left to individuals and their doctors.
Americans have long been fascinated by sleep -- or rather, with not sleeping:
Students glorify in tales of all-nighters; sleeping on the job has often been
grounds for getting fired; and the ultimate capitalist utopia is the 24-hour
workday.
A spokeswoman for Cephalon acknowledged that the company sought to expand the
market for modafinil beyond narcoleptics. Studies are showing that the medicine,
which is sold as Provigil, could help people with sleepiness associated with
depression, Parkinson's disease and other disorders, she said.
"There are so many conditions where people have pathological sleepiness where we
can help them," said the spokeswoman, Sheryl Williams. "Can we stop people from
using the product for other things? Absolutely not, but the right place to be is
in treating serious medical problems."
Once a drug is approved for one use, doctors are free to prescribe it for
others. Williams said most of the medicine's "off-label" use was in treating
psychiatric and neurological conditions. "We have not seen in our tracking data
a significant proportion of patients with nonmedical conditions," she said.
But treating sleepiness can blur the line between medical disorders and
lifestyle problems, since sleepiness is not a disorder. The shift workers in
Mitler's study, for example, are known to be at heightened risk for accidents
and to have increased medical problems associated with their irregular sleep.
But there may not be anything intrinsically wrong with them since their problems
often go away when they resume normal schedules.
Yet, doctors have classified sleep disturbances caused by the workers' lifestyle
as a disorder. The American Psychiatric Association, for instance, says,
"Circadian Rhythm Sleep Disorder" can occur when people's "circadian sleep-wake
cycle is normal" but there is a "conflict between the pattern of sleep and
wakefulness generated by the circadian system and the desired pattern of sleep
and wakefulness required by shift work."
"These individuals are impaired," Mitler said. "Whether you call it a disorder
or not is less important than the fact that they are impaired. Physicians have
found themselves in the mix simply by declaring this a treatable disorder."
Cephalon eventually would like modafinil to be recognized as a treatment for all
sleepiness associated with any disorder. But in warning the company about its
promotional materials in January, the FDA noted that "Provigil is not approved
to treat such symptoms as sleepiness, tiredness, decreased activity, lack of
energy and fatigue."
"Provigil is indicated to improve wakefulness in patients with excessive daytime
sleepiness associated with narcolepsy," the FDA wrote to a senior official at
the company Jan. 3. "Provigil is not approved for use as a daytime stimulant."
After Cephalon agreed to alter its marketing materials, the FDA considered the
matter resolved.
Notwithstanding the FDA's protests, there is every indication that modafinil is
effective in keeping healthy people awake. It may soon be common for shift
workers, soldiers and truck drivers to pop the pills before embarking on long
journeys or difficult projects.
Nancy Wesensten, a researcher at the Walter Reed Army Institute of Research in
Silver Spring, has shown that healthy people who have been kept awake for 54
hours -- more than two nights -- still function effectively when given modafinil
. The drug seems to work on other species, too: At the University of
Pennsylvania, scientist Joan Hendricks has even found that modafinil helps
sleep-deprived fruit flies perk up.
"It has a much gentler effect on promoting wakefulness" than amphetamines and
conventional stimulants, said Scammell, the Harvard neurologist. "Many people
feel comfortably awake -- they don't feel wound up, jazzed or euphoric. That's
what makes it attractive to doctors. We are always worried that amphetamines may
not be used properly. The abuse potential [of modafinil] is low."
He pointed out that the exact mechanism of modafinil is not understood. For
example, while many researchers believe that the medicine doesn't affect the
brain's dopamine system -- a neural mechanism known to underlie many addictions
-- this hasn't been conclusively demonstrated. About 1 in 10 people on modafinil
have headaches, and smaller numbers feel some nausea, he said.
Scammell, Mitler and others who study the medicine warn that talk of replacing
sleep altogether is foolish. Other chemicals have been similarly touted -- and
then found to be harmful.
"People were using [amphetamines] to stay awake for a number of days at a time
-- there were a lot of problems associated with that," said John Caldwell, a
research psychologist at the U.S. Army Aeromedical Research Lab at Fort Rucker,
Ala., who has conducted experiments to show that sleep-deprived helicopter
pilots perform better when given modafinil.
"Who knows what will happen with modafinil?" he said. "We don't know why sleep
has the restorative effect it does. Given we don't understand the nature of
sleep, I don't think it's a good idea to try to replace it with a drug of any
description."
LOAD-DATE: April 30, 2002
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
879 of 998 DOCUMENTS
San Mateo County Times (San Mateo, CA)
February 4, 2002 Monday
Colon cancer
SECTION: LIVING
LENGTH: 537 words
The question: For patients with colon cancer, is laparoscopic-assisted surgery
preferable to traditional, open-colon surgery?
Past studies of laparoscopic-assisted colectomy [LAC] have rarely focused on
patients who were being treated for cancer, have assessed only the short-term
effects of this minimally invasive technique and have involved only small
numbers of patients.
This study compared the physical and mental state of 428 patients two days, two
weeks and two months after LAC or open surgery. On average, patients who
underwent LAC stayed in the hospital almost one day less and needed less pain
medication while hospitalized than those who had open surgery. The authors
considered these benefits minimal. The two groups had similar experiences
regarding factors such as nausea, insomnia and fatigue.
Who may be affected by these findings? People with localized colon cancer.
Caveats: The researchers did not assess the patients' need for pain relief after
their discharge from the hospital. More important, this study did not compare
the survival rates of the two groups of patients. [This issue is being evaluated
using data from these and other patients, but the results will not be known for
several years.]
Bottom line: People with localized colon cancer may wish to refrain from asking
doctors for LAC until more is known about its risks and benefits. And as an
editorial accompanying the study suggests, those who nonetheless prefer LAC may
wish to consider entering a clinical trial to help establish the effectiveness
and safety of the technique.
Find this study: Jan. 16 issue of the Journal of the American Medical
Association; abstract online at http://jama.ama-assn.org/
Multiple sclerosis
The question: Can modafinil, a drug used to treat narcolepsy, alleviate the
fatigue caused by multiple sclerosis [MS]?
Past studies have shown that drugs such as amantadine [e.g., Symmetrel], which
is used to treat Parkinson's syndrome, and the stimulant pernoline [Cylert] have
only minimal effects on the fatigue often experienced by MS patients.
This study examined whether modafinil [Provigil] would be more beneficial. The
researchers compared the effects of a placebo with those of 200 and 400
milligrams of modafinil in 18 men and 54 women for nine weeks. [The participants
were not told when they were using the placebo and when they were receiving the
drug.] Most experienced significant relief from fatigue when they were taking
200 milligrams of modafinil; others benefited from the higher dose. Side effects
of the drug included mild to moderate cases of headache, nausea and anxiety.
Who may be affected by these findings? People with multiple sclerosis who
experience fatigue daily.
Caveats: Cephalon Inc., the manufacturer of Provigil, funded the study, which
was based on self-reports, which may not be accurate. Also, the long-term
effects of the drug on MS patients are not known.
Bottom line: People with multiple sclerosis may wish to consult a physician
about taking modafinil.
Find this study: February issue of the Journal of Neurology, Neurosurgery and
Psychiatry; abstract online at http://jnnp.bmjjournals.com/
-- Washington Post
LOAD-DATE: June 19, 2003
LANGUAGE: ENGLISH
Copyright 2002 MediaNews Group, Inc. and ANG Newspapers
880 of 998 DOCUMENTS
The Washington Post
January 29, 2002 Tuesday
Final Edition
MULTIPLE SCLEROSIS An anti-sle ...
SECTION: HEALTH; QUICK STUDY A WEEKLY DIGEST OF NEW RESEARCH ON MAJOR HEALTH
TOPICS; Pg. F09
LENGTH: 775 words
MULTIPLE SCLEROSIS
* THE QUESTION Can modafinil, a drug used to treat narcolepsy, alleviate the
fatigue caused by multiple sclerosis (MS)?
* PAST STUDIES have shown that drugs such as amantadine (e.g., Symmetrel), which
is used to treat Parkinson's syndrome, and the stimulant pernoline (Cylert) have
only minimal effects on the fatigue often experienced by MS patients.
* THIS STUDY examined whether modafinil (Provigil) would be more beneficial. The
researchers compared the effects of a placebo with those of 200 and 400
milligrams of modafinil in 18 men and 54 women over nine weeks. (The
participants were not told when they were using the placebo and when they were
receiving the drug.) Most experienced significant relief from fatigue when they
were taking 200 milligrams of modafinil; others benefited from the higher dose.
Side effects of the drug included mild to moderate cases of headache, nausea and
anxiety.
* WHO MAY BE AFFECTED BY THESE FINDINGS? People with multiple sclerosis who
experience fatigue daily.
* CAVEATS Cephalon Inc., the manufacturer of Provigil, funded the study, which
was based on self-reports, which may not be accurate. Also, the long-term
effects of the drug on MS patients are not known.
* BOTTOM LINE People with multiple sclerosis may wish to consult a physician
about taking modafinil.
* FIND THIS STUDY February issue of the Journal of Neurology, Neurosurgery and
Psychiatry; abstract online at http://jnnp.bmjjournals.com/.
HAY FEVER
* THE QUESTION Does the herb butterbur relieve hay fever symptoms as effectively
as do antihistamines?
* PAST STUDIES have shown that antihistamines can relieve some of the symptoms
of hay fever, such as runny nose and sneezing, but these drugs may also cause
drowsiness.
* THIS STUDY, which was double-blind, compared the effectiveness of the herbal
extract butterbur to cetirizine (Zyrtec) in relieving hay fever symptoms. The
researchers randomly assigned 125 people with hay fever to receive daily doses
of either butterbur or cetirizine. After two weeks, the people in both groups
experienced similar amounts of symptom relief.
* WHO MAY BE AFFECTED BY THESE FINDINGS? People who experience hay fever.
* CAVEATS Zeller AG of Switzerland, a manufacturer of herbal remedies, funded
the study. In addition, the long-term effects of butterbur are not known.
Finally, the results are partially based on self-reports of symptoms by the
participants.
* BOTTOM LINE People with hay fever who would like to avoid the drowsiness
caused by antihistamines may wish to consult their doctor about using butterbur.
(They should also be aware that supplies of this herb may not have guaranteed
purity and potency, and that experts advise users to be sure that the extract
has been processed to remove potentially dangerous chemicals called
pyrrolizidine alkaloids.)
* FIND THIS STUDY Jan. 19 issue of the British Medical Journal or www.bmj.com.
COLON CANCER
* THE QUESTION For patients with colon cancer, is laparoscopic-assisted surgery
preferable to traditional, open-colon surgery?
* PAST STUDIES of laparoscopic-assisted colectomy (LAC) have rarely focused on
patients who were being treated for cancer, have assessed only the short-term
effects of this minimally invasive technique and have involved only small
numbers of patients.
* THIS STUDY compared the physical and mental state of 428 patients two days,
two weeks and two months after LAC or open surgery. On average, patients who
underwent LAC stayed in the hospital almost one day less and needed less pain
medication while hospitalized than those who had open surgery. The authors
considered these benefits minimal. The two groups had similar experiences
regarding factors such as nausea, insomnia and fatigue.
* WHO MAY BE AFFECTED BY THESE FINDINGS? People with localized colon cancer.
* CAVEATS The researchers did not assess the patients' need for pain relief
after their discharge from the hospital. More important, this study did not
compare the survival rates of the two groups of patients. (This issue is being
evaluated using data from these and other patients, but the results will not be
known for several years.)
* BOTTOM LINE People with localized colon cancer may wish to refrain from asking
doctors for LAC until more is known about its risks and benefits. And as an
editorial accompanying the study suggests, those who nonetheless prefer LAC may
wish to consider entering a clinical trial to help establish the effectiveness
and safety of the technique.
* FIND THIS STUDY Jan. 16 issue of the Journal of the American Medical
Association; abstract online at http://jama.ama-assn.org/.
-- Haleh V. Samiei
LOAD-DATE: January 29, 2002
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2002 The Washington Post
881 of 998 DOCUMENTS
Espicom Business Intelligence
January 23, 2002
Modafinil approved for marketing in Mexico
LENGTH: 118 words
Cephalon's partner,
Armstrong Laboratorios (
Organizacion Bago), has received approval to sell and distribute
modafinil in Mexico. Armstrong will market modafinil under the brandname,
Modiodal. Cephalon controls worldwide rights to modafinil, marketed as
Provigil in the US and several other countries. Armstrong has successfully
executed a 6-month regulatory approval for modafinil in Mexico.
Modafinil is a wake-promoting agent currently approved in several countries for
the treatment of excessive daytime sleepiness associated with narcolepsy. The
most common side effects associated with the drug in clinical trials include
headache, nausea, infection, nervousness, anxiety and insomnia.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
882 of 998 DOCUMENTS
Reuters Health eLine News
January 23, 2002 Wednesday 9:00 PM EST
Mexico clears daytime sleepiness drug
LENGTH: 170 words
DATELINE: WASHINGTON, Jan 23
The Mexican partner of Cephalon Inc., Armstrong Laboratorios de Mexico, has
received approval to market Cephalon's daytime sleepiness treatment modafinil in
Mexico, the West Chester, Pennsylvania-based concern announced on Tuesday.
The drug is marketed under the brand name Provigil in the US and several other
countries. In Mexico, it will be sold under the trade name Modiodal. In the US,
Provigil was approved in 1998 for the treatment of a sleep disorder called
narcolepsy and launched in February 1999. People with the disorder can fall
asleep abruptly, possibly putting themselves and others in danger.
The most common side effects of the drug are headache, infection, nausea,
nervousness, anxiety and insomnia. Modafinil is not recommended for use in
individuals with certain types of heart problems.
Armstrong is a subsidiary of Organizacion Bago, one of Latin America's largest
drug distributors. Cephalon and Armstrong entered the distribution and marketing
agreement in May. Details of the deal were not disclosed.
LOAD-DATE: July 24, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2002 Reuters Health
All Rights Reserved
883 of 998 DOCUMENTS
Espicom Business Intelligence
January 22, 2002
Modafinil effective treatment for fatigue in MS
LENGTH: 363 words
Fatigue is one of the most debilitating effects of multiple sclerosis (MS).
Researchers at the Ohio State University have now carried out a study to assess
the efficacy and safety of
Cephalon's
Provigil (
modafinil) for the treatment of fatigue in MS. The data, published in the
February issue of the Journal of Neurology, Neurosurgery and Psychiatry
(2002;72:179-183), suggest that modafinal 200mg/day significantly improves
fatigue and is well tolerated in MS patients.
A total of 72 patients (74 per cent relapsing-remitting MS, 7 per cent
primary-progressive MS, 19 per cent secondary-progressive MS) were enrolled in
the 9-week, single-blind, 2-centre Phase II study. The patients were aged 18 to
65 years, and had a diagnosis of MS, a stable disability level 6 on the Kurtzke
extended disability status scale (EDSS), and a mean score >4 on the fatigue
severity scale (FSS).
Exclusion criteria included a diagnosis of narcolepsy, sleep apnoea, or
clinically significant major systemic disease and recent use of medications
affecting fatigue. All patients received placebo during weeks 1 to 2, 200mg/day
modafinil during weeks 3 to 4, 400mg/day modafinil during weeks 5 to 6, and
placebo during weeks 7 to 9. Safety was evaluated by unblinded investigators.
Efficacy was evaluated by self-rating scales, using the FSS, the modified
fatigue impact scale (MFIS), a visual analogue scale for fatigue (VAS-F) and the
Epworth sleepiness scale (ESS).
After treatment with modafinil 200mg/day for 2 weeks, a significant improvement
in fatigue versus placebo run in was demonstrated. Mean scores after treatment
with modafinil200mg/daywere: FSS, 4.7 versus 5.5 for placebo (p<0.001); MFIS,
37.7 versus 44.7 (p<0.001); and VAS-F, 5.4 versus 4.5 (p=0.003). Fatigue scores
for modafinil 400mg/daywere not significantly improved versus placebo run-in.
Mean ESS scores were significantly improved (p<0.001) with
modafinil200mg/day(7.2) and 400mg/day (7.0) versus the score at baseline (9.5).
Serious adverse events were not found at either dose. The most common adverse
events were headache, nausea and asthenia. Sixty-five patients (90 per cent)
completed the study.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2002 ESPICOM Business Intelligence Ltd.
884 of 998 DOCUMENTS
PR Newswire
January 22, 2002 Tuesday
Cephalon Announces Modafinil Receives Marketing Approval in Mexico
SECTION: FINANCIAL NEWS
LENGTH: 731 words
DATELINE: WEST CHESTER, Pa. Jan. 22
Cephalon, Inc. (Nasdaq: CEPH), an international biopharmaceutical company,
announced today that its partner, Armstrong Laboratorios de Mexico S.A.C.V., has
received approval to sell and distribute modafinil in Mexico. Armstrong will
market modafinil under the brand name, MODIODAL. Cephalon controls worldwide
rights to modafinil, marketed as PROVIGIL(R) (modafinil) tablets $(C- IV$) in
the United States and several other countries.
PROVIGIL is a unique, wake-promoting agent currently approved in several
countries for the treatment of excessive daytime sleepiness associated with
narcolepsy. The most common side effects associated with PROVIGIL in clinical
trials include headache, nausea, infection, nervousness, anxiety and insomnia.
"Armstrong has successfully executed a 6-month regulatory approval for modafinil
in Mexico," said Frank Baldino, Jr. Ph.D., chairman and CEO of Cephalon. "The
Mexican pharmaceutical market is experiencing double-digit growth, thereby
providing a dynamic environment for the introduction of modafinil."
Armstrong Laboratorios is a subsidiary of the Organizacion Bago, Latin America's
leading regional pharmaceutical company. Sales volume for Armstrong's neurology
and psychiatry products increased by 29 percent in 2000. The Mexican
pharmaceutical market is the tenth largest in the world and has been
experiencing greater percentage growth than the U.S. market.
Cephalon, Inc.
Founded in 1987, Cephalon, Inc. is an international biopharmaceutical company
dedicated to the discovery, development and marketing of innovative products to
treat sleep and neurological, disorders, cancer and pain.
Cephalon currently employs approximately 1,200 people in the United States and
Europe. U.S. sites include the company's headquarters in West Chester,
Pennsylvania, and offices and manufacturing facilities in Salt Lake City, Utah.
Cephalon's major European offices are located in Guilford, England and in
Maisons-Alfort, France.
The company currently markets three proprietary products in the United States:
PROVIGIL(R) (modafinil) tablets $(C-IV$), GABITRIL(R) (tiagabine hydrochloride)
and ACTIQ(R) (oral transmucosal fentanyl citrate) $(C-II$). Full prescribing
information on these products is available at www.cephalon.com. Cephalon markets
22 products outside the United States.
Cephalon's biotechnology pipeline is focused on the identification of novel
molecules that affect cell survival and death. Additional information about
Cephalon and its subsidiaries can be obtained by visiting the company's Web site
at http://www.cephalon.com.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
projections, and other statements regarding matters that are not historical
facts. You may identify some of these forward-looking statements by the use of
words in the statements such as "anticipate," "estimate," "expect," "project,"
"intend," "plan," "believe" or other words and terms of similar meaning.
Cephalon's performance and financial results could differ materially from those
reflected in these forward-looking statements due to general financial,
economic, regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties such
as those set forth below and in its reports on Form 8-K, 10-Q and 10-K filed
with the U.S. Securities and Exchange Commission. Given these risks and
uncertainties, any or all of these forward-looking statements may prove to be
incorrect. Therefore, you should not rely on any such factors or forward-looking
statements. Furthermore, Cephalon does not intend to update publicly any
forward-looking statement, except as required by law. The Private Securities
Litigation Reform Act of 1995 permits this discussion.
MAKE YOUR OPINION COUNT - Click Here
http://tbutton.prnewswire.com/prn/11690X53813698
SOURCE Cephalon, Inc.
CONTACT: Media: Sheryl Williams, +1-610-738-6493 or swilliams@cephalon.com; or
Investors: Robert S. (Chip) Merritt, +1-610-738-6376 or cmerritt@cephalon.com,
both of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: January 23, 2002
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
PUBLICATION-TYPE: Newswire
Copyright 2002 PR Newswire Association, Inc.
885 of 998 DOCUMENTS
CBS News Transcripts
January 15, 2002 Tuesday
SHOW: CBS Morning News (6:30 AM ET) - CBS
New drug now used for narcolepsy may someday allow people to stay awake for
extended periods without side effects
ANCHORS: SUSAN McGINNIS
BYLINE: ELIZABETH KALEDIN
LENGTH: 476 words
SUSAN McGINNIS, anchor:
Most people seem to agree there are not enough hours in the day. Well, now
scientists are developing a new drug that may someday allow us to burn the
candle at both ends and in the middle. Elizabeth Kaledin reports in this
morning's Eye on America.
ELIZABETH KALEDIN reporting:
It's 3:00 in the morning, and Home Depot is hopping. What better time to pick
up a new washing machine?
Unidentified Man #1: Can I help you?
Unidentified Man #2: Yeah. Can I get a cheeseburger...
KALEDIN: It's a 24-hour-a-day world, and despite what the clock says, the goal
of modern society, it seems, is to expand time to make the difference between
day and night obsolete. One little problem? We need to sleep.
Professor DAVID DINGES (University of Pennsylvania): We're constantly pounding
on this desire to get control of time and to use it, and sleep stands in the
way.
KALEDIN: Professor David Dinges is at the center of a growing new area of
scientific interest...
Prof. DINGES: Here, over here. There's a K-complex.
KALEDIN: ...how to achieve wakefulness 24 hours a day.
Prof. DINGES: There's growing evidence it's not good to go without sleep, and
yet that's what everybody wants to do.
KALEDIN: Dinges is studying the effects of a drug called Modafinil. Already
approved by the FDA to treat the sleep disorder narcolepsy, Modafinil can
convince the brain to be awake at any hour. Other older stimulants affect many
centers of the brain, often causing the increased heart rate and blood pressure
that lead to jitteriness, but Modafinil works only on specific neurotransmitters
in the hypothalamus that control wakefulness.
Janet Cassidy takes Modafinil twice a day to control narcolepsy and has no side
effects.
Ms. JANET CASSIDY (Narcoleptic): It's almost like you wouldn't know you'd taken
anything.
KALEDIN: Modafinil raises the possibility that we may one day be able to
eliminate the need for sleep. Imagine the benefits for shift workers, hospital
employees, brand-new parents. The American military is particularly interested.
At Ft. Rucker in Alabama, researchers are giving Modafinil to Blackhawk
helicopter pilots, who often have to fly long missions with no rest.
Mr. DAVID TALARCZYK (Pilot): Typically, you're pretty physically and mentally
drained.
KALEDIN: Pilots here who took the drug and stayed awake as long as 35 hours
performed the same as their well-rested peers.
Mr. JOHN CALDWELL (US Army Aeromedical Research Center): It's nice to be able to
do a research that's going to make our military pilots more effective.
KALEDIN: But just because we can fight sleep, should we? Scientists don't know
what the long-term health effects might be. It's a question we'll have to sleep
on--if we ever go to bed, that is. In New York, I'm Elizabeth Kaledin for Eye
on America.
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Newscast
Copyright 2002 CBS Worldwide Inc.
All Rights Reserved
886 of 998 DOCUMENTS
CBS News Transcripts
January 14, 2002 Monday
SHOW: CBS Evening News (6:30 PM ET) - CBS
New drug to help people stay awake and alert for days
ANCHORS: JOHN ROBERTS
BYLINE: ELIZABETH KALEDIN
LENGTH: 491 words
JOHN ROBERTS, anchor:
Almost everyone wishes that there were more hours in the day, and while that's
not possible, researchers may have found a way to get more out of the hours we
have: a new drug to help people stay alert for days without sleep and not feel
tired, wired or weird. CBS News medical correspondent Elizabeth Kaledin reports
tonight's wide open Eye on America.
ELIZABETH KALEDIN reporting:
It's 3:00 in the morning, and Home Depot is hopping. What better time to pick
up a new washing machine?
Unidentified Man #1: Can I help you?
Unidentified Man #2: Yeah. Can I get a cheeseburger...
KALEDIN: It's a 24-hour-a-day world, and despite what the clock says, the goal
of modern society, it seems, is to expand time to make the difference between
day and night obsolete. One little problem? We need to sleep.
Professor DAVID DINGES (University of Pennsylvania): We're constantly pounding
on this desire to get control of time and to use it, and sleep stands in the
way.
KALEDIN: Professor David Dinges is at the center of a growing, new area of
scientific interest...
Prof. DINGES: Here, over here. There's a K-complex.
KALEDIN: ...how to achieve wakefulness 24 hours a day.
Prof. DINGES: There's growing evidence it's not good to go without sleep, and
yet that's what everybody wants to do.
KALEDIN: Dinges is studying the effects of a drug called Modafinil. Already
approved by the FDA to treat the sleep disorder narcolepsy, Modafinil can
convince the brain to be awake at any hour. Other older stimulants affect many
centers of the brain, often causing the increased heart rate and blood pressure
that lead to jitteriness, but Modafinil works only on specific neurotransmitters
in the hypothalamus that control wakefulness.
Janet Cassidy takes Modafinil twice a day to control narcolepsy and has no side
effects.
Ms. JANET CASSIDY (Narcoleptic): It's almost like you wouldn't know you'd taken
anything.
KALEDIN: Modafinil raises the possibility that we may one day be able to
eliminate the need for sleep. Imagine the benefits for shift workers, hospital
employees, brand-new parents. The American military is particularly interested.
At Ft. Rucker in Alabama, researchers are giving Modafinil to Blackhawk
helicopter pilots, who often have to fly long missions with no rest.
Unidentified Pilot: Typically, you're pretty physically and mentally drained.
KALEDIN: Pilots here who took the drug and stayed awake as long as 35 hours
performed the same as their well-rested peers.
Mr. JOHN CALDWELL (US Army Aeromedical Research Center): It's nice to be able to
do a research that's going to make our military pilots more effective.
KALEDIN: But just because we can fight sleep, should we? Scientists don't know
what the long-term health effects might be. It's a question we'll have to sleep
on, if we ever go to bed, that is. In New York, I'm Elizabeth Kaledin for Eye
on America.
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Profile
Copyright 2002 CBS Worldwide Inc.
All Rights Reserved
887 of 998 DOCUMENTS
University Wire
January 14, 2002
'Alertness' pill not designed for all-night studying
BYLINE: By Shabina S. Khatri, Michigan Daily
SOURCE: U. Michigan
LENGTH: 432 words
DATELINE: Ann Arbor, Mich.
Imagine all the benefits of a caffeine pill, but without the harmful
consequences. Sound too good to be true? The reality may not be too far off.
Studies are being conducted on a drug called Modafinil, which was approved by
the Federal Drug Administration in 1998 to treat narcolepsy, a sleep disorder
characterized by uncontrollable sleepiness and frequent daytime sleep. Unlike
other stimulants, Modafinil, also known as Provigil, has been found to increase
alertness and focus in subjects without leaving them feeling wired or anxious.
Most studies of the drug have been performed on subjects mimicking the condition
of sleep-deprived shift workers, who alternately work day and night shifts. The
military has also conducted similar experiments, based on the rationale that
soldiers who sleep less can perform better.
But is the drug safe enough for healthy, non sleep-deprived individuals who are
just looking for a way to stay up at night?
Dr. Ronald Chervin, director of the University of Michigan's Sleep Disorders
Clinic, doesn't think so.
"Modafinil is not a drug that students should take to cram for a test or write a
paper," he said. "I have not seen published reports about its use for people
without chronic sleep disorders."
This lack of information involving the long-term effects of the drug on normal
individuals has led many researchers reluctant to praise Modafinil as the newest
miracle drug. In addition, Chervin said, "Modafinil does have known side
effects, perhaps the most common being headache when patients first start a
regular dose."
Dr. Naseer Ahmad, an endocrinologist at Beaumont Hospital in Royal Oak, also
agrees caution is needed. "This drug is a stimulant used to treat narcolepsy. It
keeps your brain active. If not used properly, Modafinil could cause diarrhea,
nausea and damage to the liver."
LSA junior Anna Boonin, a biopsychology and cognitive science major, admits the
idea of this magic pill is tempting but remains skeptical.
"There's a risk when you introduce anything into your body. It's nice to think,
oh I can take this pill and get all my work done and stay up all night," Boonin
said.
"But, then what about when you stop taking it? You wouldn't be able to function
normally in society," she said.
Until extensive research involving sleep deprivation in normal individuals is
conducted, Chervin does not foresee Modafinil being sold over the counter.
"This drug will not be made public and readily available through some other
mechanism than a prescription," he said.
(C) 2002 Michigan Daily via U-WIRE
LOAD-DATE: January 14, 2002
LANGUAGE: ENGLISH
Copyright 2002 Michigan Daily via U-Wire
888 of 998 DOCUMENTS
The Associated Press State & Local Wire
January 9, 2002, Wednesday, BC cycle
NEVADA FOCUS: Las Vegas shift workers often have trouble sleeping
BYLINE: By EMILY RICHMOND, Las Vegas Sun
SECTION: State and Regional
LENGTH: 872 words
DATELINE: LAS VEGAS
Alex Repp hasn't had a good night's sleep in 17 years.
As a pit boss at Harrah's hotel-casino on the Las Vegas Strip, Repp works the
casino floor from 8 p.m. to 4 a.m. and drives home through near-empty streets,
searching for rest.
At home, Repp pulls down the room-darkening shades in his bedroom, unplugs the
phone and climbs under the covers. And then he waits for sleep to come.
"I'll close my eyes and nothing happens," the 42-year-old said. "Sometimes it
takes me three hours to fall asleep, and then I'm only sleeping for two hours.
And when I wake up, I'm more tired than when I went to bed."
Repp's hope for rest lies in a new study at the Clinical Research Center of
Nevada that is trying to uncover a solution for shift-work sleep disorder. The
disorder affects Repp and thousands of other shift workers whose bodies can't
adjust to the schedule of working while others are off.
If there's an answer, researchers figure, it will be in Las Vegas, where about a
third of the work force pulls shifts outside the regular 9-to-5.
"When you think about shift workers, you think about Las Vegas," said Dr. John
Pinto, the study's lead researcher. "We have a unique opportunity to define what
happens to shift workers' sleep and how we can help."
Getting a good night's sleep is more than satisfying a mother's urging,
researchers say. Sleep problems can lead to health problems and contribute to
accidents caused by fatigue.
"A good night's sleep is a basic necessity, not a luxury," Pinto said. "When you
don't get enough sleep it takes a toll on you physically and emotionally."
Nearly two-thirds of shift workers surveyed reported difficulty sleeping, and 29
percent said at least a few days a week sleepiness interfered with work and
daily activities, according to the National Sleep Foundation. That's compared
with 17 percent of regular day workers who reported similar difficulties.
The study is trying to use a drug to simulate the effects of sleep on the brain,
giving shift-workers - who struggle after an unnatural sleep cycle - the ability
to rest.
Until recently, most sleep studies have focused on the effects of stimulants to
keep people awake. College students pulling all-nighters long ago discovered
sugar and caffeine as ways to avoid sleep, Pinto said.
There are also prescription stimulants, such as amphetamines, that can boost
wakefulness for short periods. But amphetamines, sometimes in the form of speed
or crank, have a high potential for addiction. People usually end up "crashing"
when such drugs wear off, and experience dangerous side effects such as
irregular heartbeat.
The new study will focus on the drug modafinil, currently used for the treatment
of narcolepsy. Cephalon Inc., a pharmaceutical company and the manufacturer of
modafinil, is sponsoring the Las Vegas sleep study. Modafinil is believed to
replace orexin, a recently discovered brain protein that is believed to control
sleep-wake cycles.
Unlike conventional stimulants, modafinil seems to have no effect on people who
have enough orexin.
"There's no buzz like we see with amphetamine, which means the chances of
someone abusing modafinil are reduced," Pinto said. "If you're already awake and
you take it, nothing happens."
No drug should be viewed as a replacement for sleep, said Dr. Robert Ingham, an
assistant professor at the University of Nevada School of Medicine.
The idea of replacing sleep and creating soldiers capable of fighting 24 hours a
day or factory workers who never go home isn't realistic, he said.
Modafinil could be a promising "rescue drug," helping shift workers get through
the night while they learn healthier sleep patterns, said Ingham, who is not
part of the study.
Ingham said most of his patients are insomniacs - unable to fall asleep no
matter how hard they try. Las Vegas offers special challenges to insomniacs
because there's never a shortage of places to go or things to do besides sleep,
Ingham said.
The first step toward helping people with sleep disorders is to determine how
their circadian clocks are set, Ingham said. Some people are drawn to night work
because they naturally feel more alert after dark, Ingham said. Most people are
sleepiest from midnight to 6 a.m.
"There are definitely night owls and early birds," Ingham said. "And early birds
probably shouldn't be shift workers."
Repp said he would like to switch to day shifts, but pit bosses are needed
mostly at night. Repp, who has six children ranging in age from 9 to 18, said
his work and sleep schedule contributed to his divorce and hurt his
relationships with friends and family.
"You're not around your family as much as you need to be, and when you're trying
to sleep, they're walking on pins and needles trying not to wake you up," Repp
said. "It's frustrating for them, and frustrating for me."
As a participant in the study, Repp will have to use a computerized organizer to
record what he eats, how tired he feels and how successful he is at falling, and
staying, asleep.
"I'll do anything they tell me to if it means my eyes won't feel so heavy all
the time," Repp said. "If I could just get a few hours real sleep every day, I
would be doing great."
LOAD-DATE: January 10, 2002
LANGUAGE: ENGLISH
GRAPHIC: AP Photo
Copyright 2002 Associated Press
All Rights Reserved
889 of 998 DOCUMENTS
The Houston Chronicle
January 07, 2002, Monday 3 STAR EDITION
WAKE-UP CALL;
Despite its success, anti-sleep drug raises alarm
SOURCE: Staff
BYLINE: TODD ACKERMAN, Houston Chronicle Medical Writer
SECTION: A; Pg. 1
LENGTH: 1151 words
In a world of all-night businesses and time-zone-straddling global trading, it
probably had to happen: a drug to keep you awake, alert and performing well
without the harsh effects of habit-forming amphetamines.
The drug is called Modafinil (Provigil) and, though doctors warn that it
shouldn't be used for nonmedical purposes, its success with sleep-disorder
patients and sleep-deprived military personnel is causing a buzz that the day is
coming soon when biopharmacology redefines what is meant by a good night's
sleep.
"Pharmacological developments like Modafinil will pose great temptations to
society," said David Dinges, a sleep-deprivation researcher at the University of
Pennsylvania. "They'll have the potential to satisfy our relentless desire to
control time."
Modafinil, approved by the Food and Drug Administration in 1998 for narcolepsy,
is being studied around the country to determine whether it could be a boon to
rescue workers and others who work long hours under intense conditions. A
nonaddictive stimulant that has no detectable effect on people already up and
alert, it already has been found to enhance the performance of sleep-deprived
military pilots.
The question, if it proves successful and becomes widely available, is whether
it will become the drug of choice for students cramming for exams and Type-A
individuals all too willing to sacrifice sleep for achievement.
The desire to control time has researchers around the world studying sleep and
its mechanisms. After all, people working night shifts have more health and
performance problems than people who work during the day, and in situations like
war that can mean the difference between life and death.
But most of those researchers caution that far more work needs to be done before
society starts planning for the day when one need only take a pill to go days
without sleeping or to regularly sleep just four hours a night. Too little is
known about the value of sleep and too many negative effects have been
attributed to a lack of sleep, they say.
"We haven't got to the point where we know enough about the body's internal
clock to manipulate it without fear of causing damage," said John Byrne, a
neurobiologist at the University of Texas Medical School at Houston recently
awarded a $ 1.6 million grant from the U.S. Department of Defense to design a
mathematical model of the network of genes and proteins that control the clock.
"Until then, I think the long-term ingestion of any so-called magic bullet is
likely to cause serious side effects."
Nevertheless, the clamor for Modafinil has begun. Dr. Richard Castriotta, a
UT-Houston professor and medical director of Memorial Hermann's sleep disorders
clinic, said he is receiving lots of requests for it from people without sleep
disorders, people who want it to make their busy lifestyles more manageable. (He
refuses these requests.)
Dinges said that one need only consider the growth of Starbucks to imagine how
society will react to a "wake-up drug." Calling coffee the beverage of choice in
America, he noted that many people drink it mostly because of the caffeine's
perceived stimulant effects.
Modafinil appears to work much better, researchers say. They report that study
subjects say they feel alert without experiencing a "wired" sensation when it
takes effect or a "crash" when it wears off, symptoms typically felt when using
amphetamines or lots of caffeine. It seems to have no potential for addiction
nor have users developed tolerance.
It also doesn't affect normal sleep. Users, who have gone as long as 72 hours
without sleep in tests, sleep a normal eight hours when they do retire and then
wake up without the hangover feeling many stimulants cause.
(Modafinil isn't free of side effects. In studies, it has caused mild headaches,
dizziness, nausea and other minor symptoms in fairly significant percentages.)
"Modafinil might herald a brave new world," said Timothy Monk, a University of
Pittsburgh Medical Center professor of psychiatry conducting a NASA-funded study
in which subjects on Modafinil and a placebo get 40 percent of their usual sleep
over a week's duration. "I hope not. We have knowledge and technology today such
that we could substitute vitamins for a lot of eating, but we don't do that. I
hope people value sleep as much."
Monk, who worries Modafinil could become the Viagra of wakefulness, sees a
future in which the drug is good for people with sleep and other disorders and
for emergency and night-shift workers. Although now prescribed for narcolepsy
and other sleep disorders, physicians are experimenting with it for patients
with other disorders, such as multiple sclerosis, Parkinson's disease and
depression. It has been shown to alleviate the drowsiness and fatigue that
accompany all three.
But a more widespread application may be for many of the more than 15 million
shift-work employees nationwide, those who work at night and those whose shifts
frequently rotate, such as emergency-room workers or paramedics. An estimated 70
percent of these workers suffer from sleep disorders associated with their jobs,
according to the American Academy of Sleep Medicine.
Modafinil studies on such workers have boded well. A military-funded study by
Harvard and the University of Pennsylvania looked at subjects who underwent a
28-hour period of sleep deprivation, then began a four-day period of being awake
at night and sleeping from 11 a.m. to 7 p.m. Those on Modafinil did far better
on cognitive tests involving memory skills than did their counterparts on
placebos.
The military is also funding more innovative studies, such as one recently
launched at Sea World in San Diego that focuses on dolphins, which never go
fully to sleep. In search of methods to sustain cognitive performance in people,
scientists are attempting to figure out how the animals' two cerebral
hemispheres trade off sleeping while they maintain a basic level of alertness.
Still, researchers Byrne and Castriotta say it's a big leap to go from
interesting lessons learned from animal studies and strong human showings in
controlled experiments to thinking people can "control time" over indefinite
periods. Despite our primitive knowledge of sleep, they say the existing
evidence shows serious long-term consequences among those who have tried to go
long periods without it.
"We have potent painkillers, but we only use them after diagnosing the problem
because we know pain is a warning that something is wrong," said Castriotta. "We
don't understand the reasons for sleep that well, but it's highly unlikely that
evolution designed it for anything but an important function.
"There may be a coming revolution in which we learn to sleep more efficiently,
but anyone who thinks that he or she can go for a long period of time without
sleep these days without paying a price will learn the hard way."
LOAD-DATE: January 8, 2002
LANGUAGE: ENGLISH
GRAPHIC: Photo: John Byrne, a University of Texas neurobiologist seen holding a
brain model, says "we haven't got to the point where we know enough about the
body's internal clock to manipulate it without fear of causing damage." Byrne is
studying genes and proteins that control the body's clock (p. 6); Karl Stolleis
/ Chronicle
Copyright 2002 The Houston Chronicle Publishing Company
890 of 998 DOCUMENTS
The Houston Chronicle
January 7, 2002, Monday
Despite Success, Anti-Sleep Drug Raises Alarm
BYLINE: By Todd Ackerman
LENGTH: 1177 words
In a world of all-night businesses and time-zone-straddling global trading, it
probably had to happen: a drug to keep you awake, alert and performing well
without the harsh effects of habit-forming amphetamines.
The drug is called Modafinil (Provigil) and, though doctors warn that it
shouldn't be used for nonmedical purposes, its success with sleep-disorder
patients and sleep-deprived military personnel is causing a buzz that the day is
coming soon when biopharmacology redefines what is meant by a good night's
sleep.
"Pharmacological developments like Modafinil will pose great temptations to
society," said David Dinges, a sleep-deprivation researcher at the University of
Pennsylvania. "They'll have the potential to satisfy our relentless desire to
control time."
Modafinil, approved by the Food and Drug Administration in 1998 for narcolepsy,
is being studied around the country to determine whether it could be a boon to
rescue workers and others who work long hours under intense conditions. A
nonaddictive stimulant that has no detectable effect on people already up and
alert, it already has been found to enhance the performance of sleep-deprived
military pilots.
The question, if it proves successful and becomes widely available, is whether
it will become the drug of choice for students cramming for exams and Type-A
individuals all too willing to sacrifice sleep for achievement.
The desire to control time has researchers around the world studying sleep and
its mechanisms. After all, people working night shifts have more health and
performance problems than people who work during the day, and in situations like
war that can mean the difference between life and death.
But most of those researchers caution that far more work needs to be done before
society starts planning for the day when one need only take a pill to go days
without sleeping or to regularly sleep just four hours a night. Too little is
known about the value of sleep and too many negative effects have been
attributed to a lack of sleep, they say.
"We haven't got to the point where we know enough about the body's internal
clock to manipulate it without fear of causing damage," said John Byrne, a
neurobiologist at the University of Texas Medical School at Houston recently
awarded a $ 1.6 million grant from the U.S. Department of Defense to design a
mathematical model of the network of genes and proteins that control the clock.
"Until then, I think the long-term ingestion of any so-called magic bullet is
likely to cause serious side effects."
Nevertheless, the clamor for Modafinil has begun. Dr. Richard Castriotta, a
UT-Houston professor and medical director of Memorial Hermann's sleep disorders
clinic, said he is receiving lots of requests for it from people without sleep
disorders, people who want it to make their busy lifestyles more manageable. (He
refuses these requests.)
Dinges said that one need only consider the growth of Starbucks to imagine how
society will react to a "wake-up drug." Calling coffee the beverage of choice in
America, he noted that many people drink it mostly because of the caffeine's
perceived stimulant effects.
Modafinil appears to work much better, researchers say. They report that study
subjects say they feel alert without experiencing a "wired" sensation when it
takes effect or a "crash" when it wears off, symptoms typically felt when using
amphetamines or lots of caffeine. It seems to have no potential for addiction
nor have users developed tolerance.
It also doesn't affect normal sleep. Users, who have gone as long as 72 hours
without sleep in tests, sleep a normal eight hours when they do retire and then
wake up without the hangover feeling many stimulants cause.
(Modafinil isn't free of side effects. In studies, it has caused mild headaches,
dizziness, nausea and other minor symptoms in fairly significant percentages.)
"Modafinil might herald a brave new world," said Timothy Monk, a University of
Pittsburgh Medical Center professor of psychiatry conducting a NASA-funded study
in which subjects on Modafinil and a placebo get 40 percent of their usual sleep
over a week's duration. "I hope not. We have knowledge and technology today such
that we could substitute vitamins for a lot of eating, but we don't do that. I
hope people value sleep as much."
Monk, who worries Modafinil could become the Viagra of wakefulness, sees a
future in which the drug is good for people with sleep and other disorders and
for emergency and night-shift workers. Although now prescribed for narcolepsy
and other sleep disorders, physicians are experimenting with it for patients
with other disorders, such as multiple sclerosis, Parkinson's disease and
depression. It has been shown to alleviate the drowsiness and fatigue that
accompany all three.
But a more widespread application may be for many of the more than 15 million
shift-work employees nationwide, those who work at night and those whose shifts
frequently rotate, such as emergency-room workers or paramedics. An estimated 70
percent of these workers suffer from sleep disorders associated with their jobs,
according to the American Academy of Sleep Medicine.
Modafinil studies on such workers have boded well. A military-funded study by
Harvard and the University of Pennsylvania looked at subjects who underwent a
28-hour period of sleep deprivation, then began a four-day period of being awake
at night and sleeping from 11 a.m. to 7 p.m. Those on Modafinil did far better
on cognitive tests involving memory skills than did their counterparts on
placebos.
The military is also funding more innovative studies, such as one recently
launched at Sea World in San Diego that focuses on dolphins, which never go
fully to sleep. In search of methods to sustain cognitive performance in people,
scientists are attempting to figure out how the animals' two cerebral
hemispheres trade off sleeping while they maintain a basic level of alertness.
Still, researchers Byrne and Castriotta say it's a big leap to go from
interesting lessons learned from animal studies and strong human showings in
controlled experiments to thinking people can "control time" over indefinite
periods. Despite our primitive knowledge of sleep, they say the existing
evidence shows serious long-term consequences among those who have tried to go
long periods without it.
"We have potent painkillers, but we only use them after diagnosing the problem
because we know pain is a warning that something is wrong," said Castriotta. "We
don't understand the reasons for sleep that well, but it's highly unlikely that
evolution designed it for anything but an important function.
"There may be a coming revolution in which we learn to sleep more efficiently,
but anyone who thinks that he or she can go for a long period of time without
sleep these days without paying a price will learn the hard way."
-----
To see more of the Houston Chronicle, or to subscribe to the newspaper, go to
http://www.chron.com
LOAD-DATE: January 8, 2002
LANGUAGE: ENGLISH
KR-ACC-NO: HO-SLEEP-DRUG
JOURNAL-CODE: HO
Copyright 2002 Knight Ridder/Tribune Business News
Copyright 2002 Houston Chronicle
891 of 998 DOCUMENTS
The Age (Melbourne, Australia)
December 22, 2001 Saturday
Late Edition
Amazing `alert pill' may lead to abuse
BYLINE: STEVE DOW
SECTION: NEWS; Pg. 8
LENGTH: 571 words
It's the 24-hour sleepless society. Supermarkets and factories operate around
the clock. Children are cramming more activities into their leisure time.
Round-the-clock gymnasiums are popular. The net result? We're averaging about an
hour less sleep a night than we were a decade ago. Teenagers and 20-somethings
have eschewed alcohol in favour of all-night amphetamine binges. Why cut the
night short when you can dance brightly among the shiny, happy people?
Small wonder that 40 per cent of us have sleep disorders, ranging from the
intermittent lack of sleep to the chronic. Sleep experts estimate that up to 15
per cent of people have "restless legs" in bed. They're literally running in
their dreams.
Most sleeping pills leave us groggy. How tempting it would be to pop a
"wakefulness pill" to snap us into order during the day.
Enter the new wonder drug, modafinil.
Modafinil is likely to arrive soon in Australia from Laboratoire Lafon in France
via CSL Ltd. It's a wakefulness drug unlike any other, awesomely effective in
narcoleptics - that very small group of people who fall asleep at the wrong
time.
Its brand name is Provigil. Even the connotation of the name "pro" and "vigil"
suggest that this new compound, discovered in the early 1980s but only recently
put into effect, might hold the key to understanding what it is for us to be
awake.
But federal health bureaucrats fear that the drug could be misused by shift
workers, executives and "party animals". Mostly they fear more taxpayer
hip-pocket damage in the wake of cost blow-outs on drugs such as Celebrex and
Viagra.
Modafinil, United States sleep expert David Dinges recently told The New Yorker,
is "the most tempting drug for our society to come along in decades ... It
promises to satisfy our relentless desire to control time".
The drug works on orexins, a relatively newly identified group of
neurotransmitters in the brain. It is known that a deficiency of orexins causes
narcolepsy.
Unlike traditional stimulants, which work on the central nervous system to
release the chemical dopamine to suppress sleep, modafinil takes a novel
approach. It stimulates adrenaline sensors in the brain to promote wakefulness.
It peaks at 40 minutes to an hour, but remains effective for six to eight hours.
It has few side-effects: no heart palpitations, no rush, no hyperactivity, and,
in most cases, it promotes much less over-confidence than do amphetamines.
But this creates a potential for abuse.
Doctors treating children for attention deficit hyperactivity disorder (ADHD)
with the amphetamine Ritalin are showing a big interest in modafinil. The
Australian and US military, among others, are intensely interested in its
battlefield potential.
Small wonder that Australian doctors are pushing federal health bureaucrats to
strictly limit the type of patient and the type of specialist who can prescribe
modafinil.
John Swieca, of the Melbourne Sleep Disorders Centre, says modafinil is highly
effective in narcoleptics. He admits there is potential for it to "put a
Band-Aid over sleep", though party-lovers seeking a buzz might be disappointed.
"You won't be able to replace every aspect of sleep," says Mr Swieca, "not in
the foreseeable future." And if we eschewed sleep for days on end through
currently available pharmacology, would we eventually die? "There's no evidence
we would do the same as animals," he says. "But you would get sick through
immune dysfunction."
LOAD-DATE: July 24, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2001 The Age Company Limited
All Rights Reserved
892 of 998 DOCUMENTS
Sydney Morning Herald (Australia)
December 22, 2001 Saturday
Late Edition
Experts awake to pros and cons of sleep drug
BYLINE: Steve Dow
SECTION: NEWS AND FEATURES; Pg. 3
LENGTH: 383 words
A revolutionary "wakefulness pill" is poised to go on the Australian market,
offering hope for the sleep-deprived but raising concerns it will be misused.
Modafinil, which goes by the brand name of Provigil, has proved enormously
effective among narcoleptics people who fall asleep at inappropriate times.
The drug, which leaves over-the-counter stimulants such as Sudafed, caffeine and
guarana in the shade, was discovered in the 1980s, but its efficacy has been
established only recently. It will probably soon arrive in Australia from
Laboratoire Lafon in France via CSL Ltd.
But federal health bureaucrats fear potential misuse and abuse of the drug among
shift workers, executives and nightclubbers.
The American sleep expert David Dinges recently told The New Yorker that
modafinil was "the most tempting drug for our society to come along in decades.
It promises to satisfy our relentless desire to control time."
It works on a relatively newly identified group of neurotransmitters in the
brain called orexins. These are essentially proteins in the hypothalamus. It is
now known that a deficiency of orexins causes narcolepsy.
Unlike traditional stimulants, such as the common narcolepsy-treating
amphetamine Dexedrine, which work on the central nervous system to release
dopamine to suppress sleep, the new drug takes a novel approach.
Instead, modafinil stimulates adrenaline sensors in the brain to promote
wakefulness. It peaks at 40 minutes to an hour, but is effective for six to
eight hours.
There are significantly fewer side-effects: no heart palpitations, no rush and
no hyperactivity. It is far less likely to promote over-confidence than
amphetamines.
Australian doctors are pushing federal health bureaucrats to strictly limit the
type of patient and type of specialist who can prescribe modafinil.
Dr John Swieca, of the Melbourne Sleep Disorders Centre, said modafinil is
highly effective in narcoleptics.
He admitted there was potential for abuse of the drug to "put a Band-Aid over
sleep", although party types seeking a buzz might be disappointed. "You won't be
able to replace every aspect of sleep. Not in the foreseeable future."
Dr David Joffe, of the Royal North Shore Hospital's respiratory and sleep
medicine department, said: "The obvious group [for abuse] would be truck
drivers."
LOAD-DATE: July 24, 2007
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newspaper
Copyright 2001 John Fairfax Publications Pty Ltd
All Rights Reserved
893 of 998 DOCUMENTS
Pittsburgh Post-Gazette (Pennsylvania)
December 18, 2001 Tuesday SOONER EDITION
PITT CONDUCTING STUDY OF A NONADDICTIVE PILL FOR WAKEFULNESS
BYLINE: VIRGINIA LINN, POST-GAZETTE STAFF WRITER
SECTION: HEALTH, Pg.D-1 COVER STORY
LENGTH: 660 words
Imagine a pill that could keep you alert and performing well if you went for
days with little sleep.
University of Pittsburgh Medical Center is conducting a study funded by NASA on
the wake-up pill modafinil. It's one of several studies under way around the
country to see if the drug could be a boon to rescue workers, doctors, military
personnel, pilots, astronauts and others who have to work long hours under
intense conditions.
"The ramifications go beyond NASA," said Timothy H. Monk, a UPMC professor of
psychiatry who is conducting the study.
First used by the French military, modafinil was approved by the Food and Drug
Administration in 1998 to treat excessive daytime sleepiness and narcolepsy, a
disorder that makes people fall asleep many times a day.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from using stimulants like amphetamines or too much
caffeine. Modafinil isn't free of side effects; it can cause mild headaches,
dizziness or other minor symptoms, but it isn't addictive, as amphetamines can
be.
University of Pennsylvania in Philadelphia is studying the drug's effect on
shift workers. The Army also is testing modafinil as a way to help pilots and
soldiers perform without sleep.
Researchers also see a potential to help millions of people with various
disorders that make them sleepy -- everything from multiple sclerosis to
depression.
The parts of the brain activated by modafinil are the same ones that the brain
starts to shut down in sleep-deprived people, said Matthew Miller, a
pharmacologist at Cephalon, the biotech company in West Chester, Chester County,
that is marketing modafinil. The drug seems to prompt the brain to mimic its
well-rested state.
Pitt's study began in July 2000, and it is recruiting participants through next
summer. Healthy participants between the ages of 20 and 59 are getting only 40
percent of their usual time in bed during testing.
"The question is, 'Will modafinil help them function? Will is make them alert
enough to do what is required of them?' " Monk said.
Broadening the use of the drug, however, raises questions. Would companies push
employees to use it so they could work longer hours? Would overachievers use the
drug to get a superhuman amount of work done?
"There is a spectrum of worries," Monk acknowledged. "I would worry that an
employer would force employees to take the drug. I would be very much against
that as violating their rights.
"At the other end of the scale, there may be a tendency to make modafinil the
Viagra of sleep and wakefulness." While there are legitimate uses, people can go
too far.
"We really don't fully understand exactly what all the ramifications are for
reducing sleep on a chronic basis," Monk said.
"Clearly there are times, at Ground Zero, or [during] some terrible fire or an
earthquake, when people for short periods of time -- a couple of weeks, a couple
of months -- have to get by with limited amount of sleep.
"But there could be serious problems adopting a lifestyle dramatically reducing
sleep on a chronic basis for weeks or years."
Monk said researchers are still at over how much sleep people must have each
day. They agree that people need a minimum of five hours, but it's not clear
whether they really need anything beyond that.
"I would never prescribe eight hours for everyone. Some do quite well with four
or five hours of sleep. But most who are getting five or six hours should be
getting seven or eight."
Pitt's random, double-blind study uses a placebo pill. Participants stay
continuously for seven days in laboratory apartments, then return after two
weeks for another seven-day stay. During one stay, they'll be given modafinil,
during the other, the placebo. Both parts are critical to make comparisons.
Those interested in participating can call Joette Zarotney at 412-383-9851.
Compensation is provided.
LOAD-DATE: December 18, 2001
LANGUAGE: ENGLISH
NOTES:
The Philadelphia Inquirer contributed to this report.
GRAPHIC: PHOTO: Suzanne Plunkette/Associated Press: Easy availability of a
wakefulness drug would have drawbacks as well as benefits. Employers could use
it to force employees to work longer hours, and overachievers could use it to
get more done during the time they would normally sleep.
PHOTO: Charlie Riedel/Associated Press: Possible uses of the wake-up pill under
study could be for workers laboring under emergency conditions, such as those at
the World Trade Center cleanup site.
Copyright 2001 P.G. Publishing Co.
894 of 998 DOCUMENTS
Edmonton Journal (Alberta)
December 14, 2001 Friday Final Edition
New pill won't let you die in your sleep
SOURCE: The Edmonton Journal
BYLINE: Bill Sass
SECTION: Living; Out of My Mind; Pg. C3
LENGTH: 634 words
Vivian: "You go too far, Marlowe."
Marlowe: "Those are harsh words to throw at a man, especially when he's walking
out of your bedroom."
Lauren Bacall and Humphrey Bogart dialogue from The Big Sleep
- - -
So, there I was, looking for a meaningful quote about the qualities of sleep
when I ran across this little piece of Bacall-Bogart word play.
It contains all the elements of today's topic, sleep and bedrooms, and isn't as
overused as Hamlet's whine "To sleep; perchance to dream; aye, there's the rub;
For in that sleep of death what dreams may come."
Hamlet was a real downer at parties and, I'm willing to bet, he never walked out
of Lauren Bacall's bedroom.
Anyway, we learned this week that science has found a new way to keep us awake
at night beyond its usual methods of inventing atomic ray death bombs and super
germs that can cause planet-wide pandemics not even private health care clinics
can cure.
It's called Modafinil -- an off-white crystalline powder that is practically
insoluble in water.
You're probably thinking right now: "Oh. It's just another pill. I haven't even
used up the pills I bought last week."
Well, Bunky, this isn't just another pill. It's 2-
[(diphenylmethyl)sulfinyl]acetamide. The molecular formula is C15H15NO2S, in
case you want to make your own batch.
And if that doesn't put the fear of Aesculapius, the Roman god of medicine in
you, then know that Modafinil is a drug powerful enough to keep you awake even
if you're sitting in the 4 p.m. news meeting here at News Central.
In fact, Professor Michel Jouvet, a world-famous authority on sleep, claimed
during an international defence meeting in Paris: "Modafinil could keep an army
on its feet and fighting for three days and nights with no major side effects."
I suppose that's one major benefit of drug-induced alertness, and one especially
good reason to give army recruitment centres a wide berth.
For normal people, people who just bought a $1,989 queen size Simmons Adjustable
Bed, sleep isn't something to be avoided at all costs.
Many people find sleep an attractive option to a news meeting and to be
chemically forced into a state of ready alertness borders on the cruel and/or
unusual.
The real and apparent danger with Modafinil is that it isn't the caffine-stuffed
pills we used to take in college the night before the term paper was due.
Your heart doesn't race, you don't feel like crawling out of your skin and your
roommate doesn't scream at you for keeping him up all night because you spent
the past six weeks not doing the stupid term paper.
In fact, proponents of the new wonder drug say you don't even realize you're
awake and alert until you're in the middle of your second eight-hour stretch at
work after your employer figures out one worker who can stay up all night can do
the work of three who need periodic rest to keep functionally sane.
Researchers say the drug will first be tested on shift workers who report being
intensely sleeply when they're supposed to be doing term papers.
Is there a downside to all this -- beyond the obvious one of acquiring the
ability to stay up all night when the only thing on television is George Foreman
Grill infomercials?
Well, I'm no scientist, but I do know how to dig up a chilling unattributed
scientific-sounding cautionary quote from the Internet when the occasion calls
for it:
"Prudence should be exercised in drastically curtailing one's sleep.
"Prolonged sleeplessness weakens immune function.
"Animals tortured in sleep-deprivation experiments eventually die from massive
bacterial infections of the blood ..."
I guess the upside, then, is we won't die in our sleep.
Comments? Questions? Pillow talk?
Call Bill Sass, 429-5350.
E-mail bsass@thejournal.southam.ca
LOAD-DATE: March 27, 2002
LANGUAGE: ENGLISH
TYPE: Column
Copyright 2001 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
895 of 998 DOCUMENTS
Calgary Herald (Alberta, Canada)
December 10, 2001 Monday Final EDITION
New drug banishes sleepiness
BYLINE: Faye Flam
SOURCE: Knight Ridder Newspapers
SECTION: NEWS, Pg. A4
LENGTH: 231 words
DATELINE: PHILADELPHIA
In an era where the motto seems to be "if you snooze, you lose," can sleep
become optional?
Researchers are studying a novel wake-up pill that could allow night-shift
workers or long-haul pilots to stay alert for long periods of time, with few
apparent side-effects.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from amphetamines or too much coffee, said David Dinges, a
sleep expert at the University of Pennsylvania.
Dinges and his colleagues are now recruiting shift workers from the Philadelphia
region to conduct broader tests of the drug modafinil. The drug was created to
battle narcolepsy, a disorder that makes people fall asleep many times a day.
The drug, he said, could be a lifesaver for those who need to perform dangerous
tasks or make critical decisions in the wee hours -- doctors, nurses, police
officers, and rescue workers. The U.S. army is also testing Modafinil as a way
to help pilots and soldiers perform without sleep.
"It doesn't appear that the drug has any serious medical downside," said Dinges,
who calls modafinil a "revolutionary discovery."
But widespread use of the drug raises questions: Would employers use it to push
more workers into late-night shift work? Would high-achievers use the drug to
get a superhuman amount of work done the way college students have used
amphetamines?
LOAD-DATE: December 10, 2001
LANGUAGE: ENGLISH
TYPE: News
Copyright 2001 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
896 of 998 DOCUMENTS
Edmonton Journal (Alberta)
December 10, 2001 Monday Final Edition
New wake-up drug to keep workers alert but not wired: Pill could be boon for
pilots, doctors, say sleep experts
SOURCE: Knight Ridder
BYLINE: Faye Flam
SECTION: Top Copy; Pg. A3
LENGTH: 689 words
DATELINE: Philadelphia
In a time whose motto seems to be "if you snooze, you lose," can sleep become
optional?
Researchers are studying a novel pill that could allow night-shift workers or
long-haul pilots to stay alert for long periods with few apparent side-effects.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from amphetamines or too much coffee, said David Dinges, a
sleep expert at the University of Pennsylvania.
Dinges and his colleagues are recruiting shift workers from the Philadelphia
region to conduct broader tests of the drug modafinil. The drug was created to
battle narcolepsy, a disorder that makes people fall asleep many times a day.
Dinges said the drug could be a lifesaver for those who need to perform
dangerous tasks or make critical decisions in the wee hours -- doctors, nurses,
police officers, and rescue workers. The Army is also testing modafinil as a way
to help pilots and soldiers.
"It doesn't appear that the drug has any serious medical downside," said Dinges,
who calls it a "revolutionary discovery."
But the drug raises questions: Would employers use it to push more workers into
late-night shift work? Would strivers use it to get a superhuman amount of work
done the way college students have used amphetamines?
Humans have long looked for ways to control sleep. Thomas Edison thought his
electric light would render sleep a thing of the past. The inventor often got by
on only four hours of sleep, according to biographers, and expected those who
worked for him to follow suit.
While modafinil is not addictive, as amphetamines can be, no one knows what
consequences people may suffer if they attempt to substitute drugs for sleep.
In the sleep lab at the university, Dinges has discovered that, beyond the
expected decline in memory and concentration, sleep deprivation can disrupt the
way people secrete insulin.
Modafinil has been used as an anti-narcolepsy drug in France since the late
1980s. In 1998, the West Chester, Pa.-based firm Cephalon gained approval to
market the drug to narcoleptics in the U.S., and soon began to explore wider
applications.
Researchers see a potential to help millions of people with disorders that make
them sleepy -- everything from multiple sclerosis to depression.
First, the drug will be tested on shift workers who report being intensely
sleepy when they're supposed to be working.
Scientists don't really know why people need to sleep as much as they do, but it
appears to be an essential and primal part of life.
"All animals above worms need sleep," said Matthew Miller, a pharmacologist at
Cephalon who has worked on understanding modafinil. Even fruit flies fall asleep
during certain hours, their regular circadian rhythm of sleep and wakefulness
orchestrated by several genes they share with humans and many other species.
Some animals sleep with only one hemisphere of their brains at a time; dolphins
do this so they can continue to surface for air.
Studying modafinil has begun to reshape scientists' view of sleep and
wakefulness, Miller said.
Wakefulness was long thought to be controlled largely by a brain chemical called
dopamine.
Dopamine is involved in vigilance, reward and emotion, Miller said. It helps
humans and animals to respond to threats by becoming hypervigilant.
By triggering the dopamine system, amphetamines and caffeine not only wake you
up, they can raise your pulse and bring on a shot of adrenaline.
"If you're sitting in your office, you don't want all those effects," Miller
said.
Modafinil acts in a completely different way, he said. By giving the drug to
dogs and rats and using brain imaging to see how it acts, researchers found that
it goes to a deep structure in the brain called the hypothalamus.
That part of the brain seems to control the kind of wakefulness that people feel
most of the time: alert, but not wired.
The parts of the brain activated by modafinil are the same ones that the brain
starts to shut down in sleep-deprived people, Miller said.
The drug seems to prompt the brain to mimic its well rested state.
LOAD-DATE: March 27, 2002
LANGUAGE: ENGLISH
GRAPHIC: Photo: AP, File; Inventor Thomas Edison thought his electric light
would make sleep unnecessary.
TYPE: News
Copyright 2001 CanWest Interactive, a division of
CanWest Global Communications Corp.
All Rights Reserved
897 of 998 DOCUMENTS
The Philadelphia Inquirer
December 10, 2001, Monday
Scientists say new wake-up drug keeps a person alert but not wired
BYLINE: By Faye Flam
SECTION: DOMESTIC NEWS
LENGTH: 1273 words
PHILADELPHIA _ In a nation whose motto seems to be "if you snooze, you lose,"
can sleep become optional?
Researchers are studying a novel wake-up pill that could allow night-shift
workers or long-haul pilots to stay alert for long periods of time, with few
apparent side effects.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from amphetamines or too much coffee, said David Dinges, a
sleep expert at the University of Pennsylvania.
Dinges and his colleagues are now recruiting shift workers from the Philadelphia
region to conduct broader tests of the drug modafinil. The drug was created to
battle narcolepsy, a disorder that makes people fall asleep many times a day.
The drug, he said, could be a lifesaver for those who need to perform dangerous
tasks or make critical decisions in the wee hours _ doctors, nurses, police
officers, and rescue workers. The Army is also testing Modafinil as a way to
help pilots and soldiers perform without sleep.
"It doesn't appear that the drug has any serious medical downside," said Dinges,
who calls modafinil a "revolutionary discovery."
But widespread use of the drug raises questions: Would employers use it to push
more workers into late-night shift work? Would strivers use the drug to get a
superhuman amount of work done the way college students have used amphetamines?
Humans have long looked for ways to control sleep. Thomas Edison thought his
electric light would render sleep a thing of the past. The inventor often got by
on only four hours of sleep, according to biographers, and he expected those who
worked for him to follow suit (some say he used electric shocks to discourage
slumber).
Medicine may not eliminate the need for sleep, either. While modafinil is not
addictive, as amphetamines can be, no one knows what consequences people might
suffer if they attempt to substitute drugs for sleep.
In the sleep lab at the university, Dinges has discovered that, beyond the
expected decline in memory and concentration, sleep deprivation can disrupt the
way people secrete insulin _ a problem related to diabetes and obesity.
Modafinil has been used as an anti-narcolepsy drug in France since the late
1980s. In 1998, the West Chester, Pa.-based company Cephalon gained approval to
market the drug to narcoleptics in the United States.
Cephalon soon began to explore wider applications.
Researchers see a potential to help millions of people with various disorders
that make them sleepy _ everything from multiple sclerosis to depression.
First, the drug will be tested on shift workers who report being intensely
sleepy when they're supposed to be working. Such "shift-work sleep disorder" is
not exactly a disease, Dinges said, but more a natural variation in how well
different people tolerate a nocturnal schedule.
Jennifer Hendrickson, an obstetrician at Hahnemann University Hospital who just
finished her residency, knows the rigors of sleeplessness. She often had to stay
on call for 36 hours at a time.
"The first thing to go _ things become more raw," she said. "Emotions come to
the surface." Her medical skills are second nature, she said, but working well
with patients can get tough as the hours wear on.
She drinks coffee to keep awake at times, but said she would hesitate to take
any stronger drug without knowing all the possible side effects. To work as a
doctor, "you need to be in command of all your faculties," she said.
In tests, people taking modafinil seem to perform much better on many tests of
cognitive ability and mood.
Scientists don't really know why people need to sleep as much as they do, but it
appears to be an essential and primal part of life.
"All animals above worms need sleep," said Matthew Miller, a pharmacologist at
Cephalon who has worked on understanding modafinil. Even fruit flies fall asleep
during certain hours, their regular circadian rhythm of sleep and wakefulness
orchestrated by several genes they share with humans and many other species.
Some animals sleep with only one hemisphere of their brains at a time; dolphins
do this so they can continue to surface for air.
Studying modafinil has begun to reshape scientists' view of sleep and
wakefulness, said Miller. Wakefulness was long thought to be controlled largely
by a brain chemical called dopamine. Dopamine is involved in vigilance, reward
and emotion, Miller said. The dopamine system is what helps humans and other
animals to respond to threats by becoming hypervigilant.
By triggering this dopamine system, amphetamines and caffeine not only wake you
up, they can raise your pulse and bring on a shot of adrenaline. That is not
always a good thing.
"If you're sitting in your office, you don't want all those effects," Miller
said.
Modafinil acts in a completely different way, he said. By giving the drug to
dogs and rats and using brain imaging to see how it acts, researchers found that
it goes to a deep structure in the brain called the hypothalamus. That part of
the brain seems to control the kind of wakefulness that people feel most of the
time: alert, but not wired.
"(The drug) produces the kind of wakefulness that seems to be more natural,"
said Karl Doghramji, a sleep researcher at Thomas Jefferson University Hospital
who has studied the new drug.
The parts of the brain activated by modafinil are the same ones that the brain
starts to shut down in sleep-deprived people, Miller said. The drug seems to
prompt the brain to mimic its well-rested state.
People who have participated in preliminary tests report that they are unable to
feel the effects of the drug, as they would feel the buzz from a strong cup of
coffee.
Some of the early experiments were done by Dinges and colleagues in Penn's sleep
lab. Sixteen healthy volunteers lived in the lab for six days. The subjects went
28 hours without sleep, shifting their schedules so that they slept between 11
a.m. and 7 p.m.
At night, they would perform various tasks while being tested for memory,
concentration and other abilities. In one test, for example, they were asked to
memorize various symbols that stood for numbers, and then type the appropriate
number when researchers held up a corresponding symbol.
Half the subjects received modafinil, and half got a placebo. Those on the
placebo made many more errors in the tests that measured memory and attention.
The Army also has tested the drug on sleep-deprived pilots, using flight
simulators to test their skills and reactions under various conditions. Again,
modafinil seemed to bring test subjects back to their well-rested levels.
In other experiments, people were given the drug before they went to sleep, and,
surprisingly, they slept fine, Miller said. Somehow the drug makes it easier for
people to stay awake but still allows them to fall asleep if they choose to.
Cephalon plans to test the drug for many other sleep disorders _ those caused by
chronic fatigue syndrome, sleep apnea, multiple sclerosis, and a rare disorder
called delayed sleep phase syndrome.
Jefferson's Doghramji is interested in testing the drug in patients with
depression. While new antidepressants have helped a great deal, he said, many
people still feel a deep fatigue that this new drug might combat.
But researchers say they don't want modafinil to further deprive a
sleep-deprived nation.
"There's a desire to control time that's characteristic of our age," Dinges
said. "There's a relentless desire to get more done."
___
(c) 2001, The Philadelphia Inquirer.
Visit Philadelphia Online, the Inquirer's World Wide Web site, at
http://www.philly.com/
LOAD-DATE: December 10, 2001
LANGUAGE: ENGLISH
KR-ACC-NO: K4131
JOURNAL-CODE: PH
Copyright 2001 Knight Ridder/Tribune News Service
Knight Ridder/Tribune News Service
898 of 998 DOCUMENTS
The Philadelphia Inquirer
December 10, 2001, Monday
Researchers Tout Drug that Keeps Sleep at Bay Without Side Effects
BYLINE: By Faye Flam
LENGTH: 1282 words
In a nation whose motto seems to be "if you snooze, you lose," can sleep become
optional?
Researchers are studying a novel wake-up pill that could allow night-shift
workers or long-haul pilots to stay alert for long periods of time, with few
apparent side effects.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from amphetamines or too much coffee, said David Dinges, a
sleep expert at the University of Pennsylvania.
Dinges and his colleagues are now recruiting shift workers from around the
Philadelphia region to conduct broader tests of the drug modafinil. The drug was
created to battle narcolepsy, a disorder that makes people fall asleep many
times a day.
The drug, he said, could be a lifesaver for those who need to perform dangerous
tasks or make critical decisions in the wee hours -- doctors, nurses, police
officers and rescue workers. Modafinil also is being tested by the Army as a way
to help pilots and soldiers perform without sleep.
"It doesn't appear that the drug has any serious medical downside," said Dinges,
who calls modafinil a "revolutionary discovery."
But widespread use of the drug could raise many questions: Would employers use
it to push more workers into late-night shift work? Would strivers use the drug
to get a superhuman amount of work done the way college students have used
amphetamines?
Humans have long looked for ways to control sleep. Thomas Edison thought his
electric light would render sleep a thing of the past. The inventor often got by
on only four hours of sleep, according to biographers, and he expected those who
worked for him to follow suit (some say he used electric shocks to discourage
slumber).
Medicine may not eliminate the need for sleep, either. While modafinil is not
addictive, as amphetamines can be, no one knows what consequences people might
suffer if they attempt to substitute drugs for sleep.
In the sleep lab at Penn, Dinges has discovered that, beyond the expected
decline in memory and concentration, sleep deprivation can disrupt the way
people secrete insulin -- a problem related to diabetes and obesity.
Modafinil has been used as an anti-narcolepsy drug in France since the late
1980s. In 1998, the West Chester-based company Cephalon gained approval to
market the drug to narcoleptics in the United States.
Cephalon soon began to explore wider applications.
Researchers see a potential to help millions of people with various disorders
that make them sleepy -- everything from multiple sclerosis to depression.
First, the drug will be tested on shift workers who report being intensely
sleepy when they're supposed to be working. Such "shift-work sleep disorder" is
not exactly a disease, Dinges said, but more a natural variation in how well
different people tolerate a nocturnal schedule.
Jennifer Hendrickson, an obstetrician at Hahnemann University Hospital who just
finished her residency, knows the rigors of sleeplessness. She often had to stay
on call for 36 hours at a time.
"The first thing to go -- things become more raw," she said. "Emotions come to
the surface." Her medical skills are second-nature, she said, but working well
with patients can get tough as the hours wear on.
She drinks coffee to keep awake at times, but said she would hesitate to take
any stronger drug without knowing all the possible side effects. To work as a
doctor, "you need to be in command of all your faculties," she said.
In tests, people taking modafinil seem to perform much better on many tests of
cognitive ability and mood.
Scientists don't really know why people need to sleep as much as they do, but it
appears to be an essential and primal part of life.
"All animals above worms need sleep," said Matthew Miller, a pharmacologist at
Cephalon who has worked on understanding modafinil. Even fruit flies fall asleep
during certain hours, their regular circadian rhythm of sleep and wakefulness
orchestrated by several genes they share with humans and many other species.
Some animals sleep with only one hemisphere of their brains at a time; dolphins
do this so they can continue to surface for air.
Studying modafinil has begun to reshape scientists' view of sleep and
wakefulness, said Cephalon's Miller. Wakefulness was long thought to be
controlled largely by a brain chemical called dopamine. Dopamine is involved in
vigilance, reward and emotion, Miller said. The dopamine system is what helps
humans and other animals to respond to threats by becoming hypervigilant.
By triggering this dopamine system, amphetamines and caffeine not only wake you
up, they can raise your pulse and bring on a shot of adrenaline. That is not
always a good thing. "If you're sitting in your office, you don't want all those
effects," Miller said.
Modafinil acts in a completely different way, he said. By giving the drug to
dogs and rats and using brain imaging to see how it acts, researchers found that
it goes to a deep structure in the brain called the hypothalamus. That part of
the brain seems to control the kind of wakefulness that people feel most of the
time: alert, but not wired.
"[The drug] produces the kind of wakefulness that seems to be more natural,"
said Karl Doghramji, a sleep researcher at Thomas Jefferson University Hospital
who has studied the new drug.
The parts of the brain activated by modafinil are the same ones that the brain
starts to shut down in sleep-deprived people, Miller said. The drug seems to
prompt the brain to mimic its well-rested state.
People who have participated in preliminary tests report that they are unable to
feel the effects of the drug, as they would feel the buzz from a strong cup of
coffee.
Some of the early experiments were done by Dinges and colleagues in Penn's sleep
lab. Sixteen healthy volunteers lived in the lab for six days. The subjects went
28 hours without sleep, shifting their schedules so that they slept between 11
a.m. and 7 p.m.
At night, they would perform various tasks while being tested for memory,
concentration and other abilities. In one test, for example, they were asked to
memorize various symbols that stood for numbers, and then type the appropriate
number when researchers held up a corresponding symbol.
Half the subjects received modafinil, and half got a placebo. Those on the
placebo made many more errors in the tests that measured memory and attention.
The Army also has tested the drug on sleep-deprived pilots, using flight
simulators to test their skills and reactions under various conditions. Again,
modafinil seemed to bring test subjects back to their well-rested levels.
In other experiments, people were given the drug before they went to sleep, and,
surprisingly, they slept fine, Miller said. Somehow the drug makes it easier for
people to stay awake but still allows them to fall asleep if they choose to.
Cephalon plans to test the drug for many other sleep disorders -- those caused
by chronic fatigue syndrome, sleep apnea, multiple sclerosis, and a rare
disorder called delayed sleep phase syndrome.
Jefferson's Doghramji is interested in testing the drug in patients with
depression. While new antidepressants have helped a great deal, he said, many
people still feel a deep fatigue that this new drug might combat.
But researchers say they don't want modafinil to further deprive a
sleep-deprived nation.
"There's a desire to control time that's characteristic of our age," Dinges
said. "There's a relentless desire to get more done."
-----
To see more of The Philadelphia Inquirer, or to subscribe to the newspaper, go
to http://www.philly.com
LOAD-DATE: December 11, 2001
LANGUAGE: ENGLISH
KR-ACC-NO: PH-SLEEP-DRUG
JOURNAL-CODE: PH
Copyright 2001 Knight Ridder/Tribune Business News
Copyright 2001 The Philadelphia Inquirer
899 of 998 DOCUMENTS
The Philadelphia Inquirer
December 9, 2001 Sunday CITY-D EDITION
Rest? No thanks, I'll have a pill;
Researchers tout drug that keeps sleep at bay without side effects
BYLINE: Faye Flam INQUIRER STAFF WRITER
SECTION: NATIONAL; Pg. A01
LENGTH: 1266 words
In a nation whose motto seems to be "if you snooze, you lose," can sleep become
optional?
Researchers are studying a novel wake-up pill that could allow night-shift
workers or long-haul pilots to stay alert for long periods of time, with few
apparent side effects.
Those who have tried it report that they feel alert without the "wired"
sensation that comes from amphetamines or too much coffee, said David Dinges, a
sleep expert at the University of Pennsylvania.
Dinges and his colleagues are now recruiting shift workers from around the
Philadelphia region to conduct broader tests of the drug modafinil. The drug was
created to battle narcolepsy, a disorder that makes people fall asleep many
times a day.
The drug, he said, could be a lifesaver for those who need to perform dangerous
tasks or make critical decisions in the wee hours - doctors, nurses, police
officers and rescue workers. Modafinil also is being tested by the Army as a way
to help pilots and soldiers perform without sleep.
"It doesn't appear that the drug has any serious medical downside," said Dinges,
who calls modafinil a "revolutionary discovery."
But widespread use of the drug could raise many questions: Would employers use
it to push more workers into late-night shift work? Would strivers use the drug
to get a superhuman amount of work done the way college students have used
amphetamines?
Humans have long looked for ways to control sleep. Thomas Edison thought his
electric light would render sleep a thing of the past. The inventor often got by
on only four hours of sleep, according to biographers, and he expected those who
worked for him to follow suit (some say he used electric shocks to discourage
slumber).
Medicine may not eliminate the need for sleep, either. While modafinil is not
addictive, as amphetamines can be, no one knows what consequences people might
suffer if they attempt to substitute drugs for sleep.
In the sleep lab at Penn, Dinges has discovered that, beyond the expected
decline in memory and concentration, sleep deprivation can disrupt the way
people secrete insulin - a problem related to diabetes and obesity.
Modafinil has been used as an anti-narcolepsy drug in France since the late
1980s. In 1998, the West Chester-based company Cephalon gained approval to
market the drug to narcoleptics in the United States.
Cephalon soon began to explore wider applications.
Researchers see a potential to help millions of people with various disorders
that make them sleepy - everything from multiple sclerosis to depression.
First, the drug will be tested on shift workers who report being intensely
sleepy when they're supposed to be working. Such "shift-work sleep disorder" is
not exactly a disease, Dinges said, but more a natural variation in how well
different people tolerate a nocturnal schedule.
Jennifer Hendrickson, an obstetrician at Hahnemann University Hospital who just
finished her residency, knows the rigors of sleeplessness. She often had to stay
on call for 36 hours at a time.
"The first thing to go - things become more raw," she said. "Emotions come to
the surface." Her medical skills are second-nature, she said, but working well
with patients can get tough as the hours wear on.
She drinks coffee to keep awake at times, but said she would hesitate to take
any stronger drug without knowing all the possible side effects. To work as a
doctor, "you need to be in command of all your faculties," she said.
In tests, people taking modafinil seem to perform much better on many tests of
cognitive ability and mood.
Scientists don't really know why people need to sleep as much as they do, but it
appears to be an essential and primal part of life.
"All animals above worms need sleep," said Matthew Miller, a pharmacologist at
Cephalon who has worked on understanding modafinil. Even fruit flies fall asleep
during certain hours, their regular circadian rhythm of sleep and wakefulness
orchestrated by several genes they share with humans and many other species.
Some animals sleep with only one hemisphere of their brains at a time; dolphins
do this so they can continue to surface for air.
Studying modafinil has begun to reshape scientists' view of sleep and
wakefulness, said Cephalon's Miller. Wakefulness was long thought to be
controlled largely by a brain chemical called dopamine. Dopamine is involved in
vigilance, reward and emotion, Miller said. The dopamine system is what helps
humans and other animals to respond to threats by becoming hypervigilant.
By triggering this dopamine system, amphetamines and caffeine not only wake you
up, they can raise your pulse and bring on a shot of adrenaline. That is not
always a good thing. "If you're sitting in your office, you don't want all those
effects," Miller said.
Modafinil acts in a completely different way, he said. By giving the drug to
dogs and rats and using brain imaging to see how it acts, researchers found that
it goes to a deep structure in the brain called the hypothalamus. That part of
the brain seems to control the kind of wakefulness that people feel most of the
time: alert, but not wired.
"[The drug] produces the kind of wakefulness that seems to be more natural,"
said Karl Doghramji, a sleep researcher at Thomas Jefferson University Hospital
who has studied the new drug.
The parts of the brain activated by modafinil are the same ones that the brain
starts to shut down in sleep-deprived people, Miller said. The drug seems to
prompt the brain to mimic its well-rested state.
People who have participated in preliminary tests report that they are unable to
feel the effects of the drug, as they would feel the buzz from a strong cup of
coffee.
Some of the early experiments were done by Dinges and colleagues in Penn's sleep
lab. Sixteen healthy volunteers lived in the lab for six days. The subjects went
28 hours without sleep, shifting their schedules so that they slept between 11
a.m. and 7 p.m.
At night, they would perform various tasks while being tested for memory,
concentration and other abilities. In one test, for example, they were asked to
memorize various symbols that stood for numbers, and then type the appropriate
number when researchers held up a corresponding symbol.
Half the subjects received modafinil, and half got a placebo. Those on the
placebo made many more errors in the tests that measured memory and attention.
The Army also has tested the drug on sleep-deprived pilots, using flight
simulators to test their skills and reactions under various conditions. Again,
modafinil seemed to bring test subjects back to their well-rested levels.
In other experiments, people were given the drug before they went to sleep, and,
surprisingly, they slept fine, Miller said. Somehow the drug makes it easier for
people to stay awake but still allows them to fall asleep if they choose to.
Cephalon plans to test the drug for many other sleep disorders - those caused by
chronic fatigue syndrome, sleep apnea, multiple sclerosis, and a rare disorder
called delayed sleep phase syndrome.
Jefferson's Doghramji is interested in testing the drug in patients with
depression. While new antidepressants have helped a great deal, he said, many
people still feel a deep fatigue that this new drug might combat.
But researchers say they don't want modafinil to further deprive a
sleep-deprived nation.
"There's a desire to control time that's characteristic of our age," Dinges
said. "There's a relentless desire to get more done."
Faye Flam's e-mail address is fflam@phillynews.com.
LOAD-DATE: December 10, 2001
LANGUAGE: ENGLISH
GRAPHIC: PHOTO;
BONNIE WELLER, Inquirer Staff Photographer
Sleep expert David Dinges, overseeing a program at the University of
Pennsylvania, calls modafinil a "revolutionary discovery."
Copyright 2001 Philadelphia Newspapers, LLC
All Rights Reserved
900 of 998 DOCUMENTS
ABC News
December 5, 2001 Wednesday
SHOW: World News Now (2:00 AM ET) - ABC
Video sales and rentals; Sleep drug that keeps you alert and is non-addictive
ANCHORS: DEREK McGINTY; ALISON STEWART
BYLINE: JOHN McKENZIE
LENGTH: 542 words
TEXT:
VIDEO RENTALS
1. LARA CROFT: TOMB RAIDER 2. AMERICA'S SWEETHEARTS 3. SHREK 4. LEGALLY BLONDE
5. SWORDFISH
VIDEO SALES
1. SHREK 2. MICKEY'S MAGICAL CHRISTMAS 3. CATS & DOGS 4. DR. DOLITTLE 2 5.
BARBIE IN THE NUTCRACKER
DEREK McGINTY, co-anchor:
And finally this half-hour, a story that everyone watching the show will be
interested in. It's about a pill that would make the sleep you're already going
without unnecessary; it's a drug that could allow you to stay awake and alert
for days. It sounds too good to be true, which means in the long run, it
probably won't live up to its billing. But right now it is very tempting.
Here's ABC's John McKenzie.
JOHN McKENZIE reporting:
(VO) It is a tantalizing goal: controlling the night. Sleeping less to
accomplish more. A drug that might allow people to stay awake and alert.
Unidentified Woman #1: I would use it if I were traveling, if I had to take a
red-eye.
Unidentified Woman #2: If maybe one of my children or grandchildren were ill and
I was, say, going to be in the hospital with them.
McKENZIE: (VO) The prescription drug called modafinil is approved for people
with a sleeping disorder who cannot stay awake during the day, but it also holds
intriguing promise for millions of others who are sleep deprived.
Dr. EMMANUEL MIGNOT (Stanford University Medical School): If you take modafinil
after sleep deprivation, it can restore you to a normal level of alertness where
you can concentrate, you can do things.
McKENZIE: (VO) No one knows exactly how it works. But unlike other stimulants,
such as caffeine or amphetamines, modafinil shows little sign of being addictive
and has few side effects.
Dr. NEIL KAVEY (Columbia Presbyterian Medical Center): Modafinil is--has the
advantage of not stimulating the cardiovascular system, so people are much less
likely to feel palpitations, feel tremulousness, feel their heart racing.
Ms. TONI HEATH-RICHARD: I don't feel any buzz at all.
McKENZIE: (VO) Toni Heath-Richard uses the drug because breathing problems
disrupt her sleep at night.
Some doctors are prescribing the drug for daytime drowsiness in people with
depression, Parkinson's Disease and Multiple Sclerosis.
(OC) But how many other people should have access to the drug? Doctors warn
that there's no evidence that modafinil can overcome all the harmful
consequences of going without sleep.
Dr. KAVEY: Our cardiovascular system needs sleep. Thyroid function, hormone
levels, the immune system, glucose metabolism, insulin, all seem to be dependent
on sleep for normal function.
McKENZIE: (VO) In other words, before doctors can prescribe this stimulant more
widely, they need to learn more about how much and how often sleep patterns can
be safely disrupted. John McKenzie, ABC News, New York.
ALISON STEWART, co-anchor:
That stuff is gold around here.
McGINTY: What--what do we have to do to get some of that stuff.
STEWART: You know, we need to get you some right now, because a certain anchor
had a little bit of a--during commercial break had a little bit of an issue.
McGINTY: I don't know what you're talking about. I don't think--how is that?
STEWART: That's news and snooze for this half-hour!
(Commercial break)
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Newscast
Copyright 2001 American Broadcasting Companies, Inc.
901 of 998 DOCUMENTS
ABC News
December 5, 2001 Wednesday
SHOW: World News This Morning (6:00 AM ET) - ABC
Modafinil, a new drug to help people with sleep disorders, seems promising
ANCHORS: DEREK McGINTY
BYLINE: JOHN McKENZIE
LENGTH: 373 words
DEREK McGINTY, co-anchor:
People who spend sleepless nights tossing and turning in bed, usually have
trouble keeping their eyes open during the day. Some of them, however, are now
turning to a new pill that promises relief. ABC's John McKenzie has the
details.
JOHN McKENZIE reporting:
(VO) It is a tantalizing goal, controlling the night, sleeping less to
accomplish more, a drug that might allow people to stay awake and alert. The
prescription drug called Modafinil is approved for people with a sleeping
disorder who cannot stay awake during the day, but it also holds intriguing
promise for millions of others who are sleep-deprived.
Dr. EMMANUEL MIGNOT (Stanford University Medical School): If you take Modafinil
after sleep deprivation, it can restore you to a normal level of alertness,
where you can concentrate, you can do things.
McKENZIE: (VO) No one knows exactly how it works, but unlike other stimulants
such as caffeine or amphetamines, Modafinil shows little sign of being addictive
and has few side effects.
Dr. NEIL KAVEY (Columbia Presbyterian Medical Center): Modafinil is--has the
advantage of not stimulating the cardiovascular system, so people are much less
likely to feel palpitations, feel tremulousness, feel their heart racing.
McKENZIE: (VO) Some doctors are prescribing the drug for daytime drowsiness, in
people with depression, Parkinson's disease and multiple sclerosis.
(OC) But how many other people should have access to the drug? Doctors warn
there's no evidence that Modafinil can overcome all the harmful consequences of
going without sleep.
Dr. KAVEY: Our cardiovascular system needs sleep. Thyroid function, hormone
levels, the immune system, glucose metabolism, insulin, all seem to be dependent
on sleep for normal function.
McKENZIE: (VO) In other words, before doctors can prescribe this stimulant more
widely, they need to learn more about how much and how often sleep patterns can
be safely disrupted. John McKenzie, ABC News, New York.
McGINTY: And coming up on "Good Morning America," the drugs your trusted
pharmacist may have left on the shelf far too long.
I'm Derek McGinty. Thanks for watching WORLD NEWS THIS MORNING. Have a great
day! Bye-bye.
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Profile
Copyright 2001 American Broadcasting Companies, Inc.
902 of 998 DOCUMENTS
The Straits Times (Singapore)
Pill makes sleep unnecessary
December 5, 2001, Wednesday
Scientists look at the various uses of modafinil, a stimulant, that has been
found to keep a person awake and alert for days
NEW YORK -- Imagine a pill that would make sleep unnecessary for fighter pilots
on long-range missions, or even the high-powered executives and parents of
newborns among us.
It might not be too far off.
ABC News has reported that scientists are looking at a variety of uses for
modafinil, a stimulant that is currently used to treat narcolepsy, a sleep
disorder characterised by uncontrollable sleepiness and frequent daytime sleep.
Modafinil (sold under the name Provigil) has been found to increase both
wakefulness and what researchers call "vigilance", the ability to stay on task,
thinking clearly and functioning normally.
Other drugs designed to keep people awake, such as amphetamines, or "uppers",
are not nearly as good at keeping users mentally sharp, and they often make
people jumpy and anxious.
"It seems to work dramatically," Dr Thomas Scammell, a sleep expert from the
Beth Israel Deaconess Medical Centre in Boston told Good Morning America.
Most studies of "normal" volunteers have used military recruits, and the maximum
they have kept them up is about four days, with nearly normal performance on
mental tasks.
But that does not mean that people should start taking pills to stay awake three
or four days at a time.
"Even if the drug is safe, it seems dangerous to mess with your body's sleep
needs," Dr Scammell said.
Currently, modafinil is only approved and prescribed for those with narcolepsy.
But it is also being studied as an option to treat syndromes where fatigue plays
a role, such as multiple sclerosis.
Researchers are also exploring the possibility that healthy people could take
the pill in order to stay awake, and mentally alert, for days at a time.
Though sleep experts acknowledge the drug's effectiveness for narcoleptics, they
raise alarms about using it for the average, healthy person who simply wants to
do more and sleep less.
Dr Joyce Walsleben, director of the Sleep Disorder Centre at the New York
University School of Medicine, said that overall, modafinil is good at keeping
people awake without side-effects.
Sleep research took a big step forward three years ago, when scientists
discovered a new family of neurotransmitters called orexins.
Studies showed that a deficiency of orexin causes narcolepsy.
The military is spending more than US$100 million (S$184 million) on similar
research, on the rationale that soldiers who sleep less will give the United
States a military edge, said ABC.
TEST SUBJECTS: Peak performance for days
NEW YORK -- In a recent study, 16 healthy people were placed in a lab where some
were given modafinil and the rest took a placebo.
First, participants had to stay awake for 28 hours to mimic the sleep-deprived
state of shift workers, said the ABC report. Then they began a four-day period
of being awake at night and sleeping from 11 am to 7 pm.
The volunteer subjects who had taken the modafinil sustained their alertness and
the capacity to perform well, while those who had taken the placebo had a higher
error rate.
SECTION: World, Pg. 9
LENGTH: 531 words
LOAD-DATE: December 6, 2001
LANGUAGE: ENGLISH
Copyright 2001 Singapore Press Holdings Limited
903 of 998 DOCUMENTS
ABC News
December 4, 2001 Tuesday
SHOW: World News Tonight (6:30 PM ET) - ABC
New prescription drug called Modafinil might allow you to stay alert and awake
without being addictive and has few side effects
ANCHORS: PETER JENNINGS
BYLINE: JOHN McKENZIE
LENGTH: 459 words
PETER JENNINGS, anchor:
Finally tonight, the future of sleep which so many of us say we don't get enough
of. This is about a pill to keep you awake. One researcher told the New Yorker
magazine, 'It is the most tempting drug for our society to come along in
decades.' Here's ABC's John McKenzie with medicine on THE CUTTING EDGE.
JOHN McKENZIE reporting:
(VO) It is a tantalizing goal: controlling the night. Sleeping less to
accomplish more. A drug that might allow people to stay awake and alert.
Unidentified Woman #1: I would use it if I were traveling, if I had to take a
red eye.
Unidentified Woman #2: If maybe one of my children or grandchildren were ill and
I was, say, going to be in the hospital with them.
McKENZIE: (VO) The prescription drug called Modafinil is approved for people
with a sleeping disorder who cannot stay awake during the day, but it also holds
intriguing promise for millions of other who are sleep deprived.
Dr. EMMANUEL MIGNOT (Stanford University Medical School): If you take Modafinil
after sleep deprivation, it can restore you to a normal level of alertness where
you can concentrate, you can do things.
McKENZIE: (VO) No one knows exactly how it works. But unlike other stimulants,
such as caffeine or amphetamines, Modafinil shows little sign of being addictive
and has few side effects.
Dr. NEIL KAVEY (Columbia Presbyterian Medical Center): Modafinil is--has the
advantage of not stimulating the cardiovascular system, so people are much less
likely to feel palpitations, feel tremulousness, feel their heart racing.
Ms. TONI HEATH-RICHARD: I don't feel any buzz at all.
McKENZIE: (VO) Toni Heath-Richard uses the drug because breathing problems
disrupt her sleep at night.
Some doctors are prescribing the drug for daytime drowsiness in people with
depression, Parkinson's Disease and multiple sclerosis.
(OC) But how many other people should have access to the drug? Doctors warn
that there's no evidence that Modafinil can overcome all the harmful
consequences of going without sleep.
Dr. KAVEY: Our cardiovascular system needs sleep. Thyroid function, hormone
levels, the immune system, glucose metabolism, insulin all seem to be dependent
on sleep for normal function.
McKENZIE: (VO) In other words, before doctors can prescribe this stimulant more
widely, they need to learn more about how much and how often sleep patterns can
be safely disrupted. John McKenzie, ABC News, New York.
JENNINGS: That's our report on WORLD NEWS TONIGHT. Tomorrow on WORLD NEWS,
along with the Middle East and Afghanistan, the Coast Guard revives a 19th
century tradition with its Christmas ship.
I'm Peter Jennings. I hope have you a good evening and you sleep well. Good
night.
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Profile
Copyright 2001 American Broadcasting Companies, Inc.
904 of 998 DOCUMENTS
ABC News
December 3, 2001 Monday
SHOW: Good Morning America (7:00 AM ET) - ABC
Dr. Thomas Scammell of Beth Israel Deaconess Medical Center discusses the new
drug Provigil, approved for treating narcolepsy
ANCHORS: CHARLES GIBSON
LENGTH: 964 words
CHARLES GIBSON, co-host:
Twenty of Americans work in round-the-clock businesses, and for anyone on the
late shift, just staying awake can be a desperate struggle. But now drug
companies are testing a pill. It's on the market with the brand name called
Provigil, to see if it can keep you awake for days on end without losing
alertness. Joining us from Boston, the prominent sleep researcher Dr. Thomas
Scammell of Beth Israel Deaconess Medical Center. He is not part of this study,
but he knows this drug very well. It's good to have you with us, Dr. Scammell.
Dr. THOMAS SCAMMELL (Beth Israel Deaconess Medical Center): Good morning,
Charlie. It's good to be here.
GIBSON: Is this designed for people who need to be up for days on end, to be at
peak capacity? I'm thinking of people like on a long mission for the military,
or is it for someone who's on the late shift and just a little tired?
Dr. SCAMMELL: Well, I think this is really for people who have chronic
problematic sleepiness. The drug has been approved for use in narcolepsy, a
disease where people have daily sleepiness that can often be so difficult that
they have trouble holding a job or driving any long distance. As yet, this drug
is not being used for people who have more casual sleepiness, such as you and I
are familiar with, say due to just, you know, an occasional bit of sleep
depravation.
GIBSON: But I can see that it would have military implications.
Dr. SCAMMELL: I think so. And, in fact, as best as we know, the military is
using it on some long-range missions, such as when they need to send a bomber
from the United States all the way to Afghanistan and back.
GIBSON: Now what's new about it? We have stimulants like caffeine and
amphetamines that will keep you awake.
Dr. SCAMMELL: Right. Those have been available for decades now. Modafinil only
became available to the public about two years ago. And the thing that's so
attractive about it for us is that unlike amphetamines or these more traditional
drugs, modafinil promotes wakefulness in a much gentler fashion. It doesn't have
the jitteriness or the anxiety that many of the amphetamines typically produce.
In fact, most people who say--who--who take it say that it feels simply like
gentle wakefulness. And amazingly enough, they're able to sleep well at night
when they take this during the day.
GIBSON: Now you use the word modafinil and I called it Provigil.
Dr. SCAMMELL: Right. Modafinil is the generic name and Provigil is the brand
name.
GIBSON: OK. Now what do we know so far about alertness with this? You say it's
sort of gently keeps you awake. But what does it do, for instance, to memory,
to coordination, to alertness, to your ability to think, really?
Dr. SCAMMELL: As--so far, nobody has demonstrated that those, if you will,
higher cognitive functions are any different what people take modafinil. What we
do know is that many of the same brain regions that are active during normal,
calm wakefulness appear to be active when people take modafinil. This is also
seen in animal studies that we've done. And so the studies that have been done
generally, you're comparing sleep-deprived people who have taken, say, a placebo
pill to sleep-deprived people who have taken modafinil. And it's clear people
that people taking the modafinil do have better memory, better attention and
they can, for instance, respond more quickly on--on tasks that require that.
GIBSON: After being awake for 24, 36 hours?
Dr. SCAMMELL: There's been studies--there's been studies were they kept people
awake for as much as four days, and remarkably their performance can actually be
pretty good if they continue to take the modafinil during that time.
GIBSON: Side effects? Downside?
Dr. SCAMMELL: There are side effects. About 10 percent of people may have
trouble with headaches and occasionally, people may feel queasy. But in contrast
to the amphetamines, which generally have fairly frequent side effects, this
medicine is very well tolerated.
GIBSON: It's now available. I mean, we talked about it being in study phase.
But this is now on the market, this drug, right?
Dr. SCAMMELL: That's correct. It's on the market. It's approved for use in
narcolepsy. Now I can tell you right now, there's so many prescriptions being
written for this medicine. It's clear that many patients beyond narcoleptics
are taking it. And in my conversations with other doctors, it's clear that
patients with depression in sleepiness, multiple sclerosis in sleepiness,
Parkinson's disease in sleepiness, have been taking it, and some with some
pretty good success.
GIBSON: Well, I was just going to say, the potential for abuse here for people
who just want it because they want to be awake, I mean, it seems to me there's a
huge number of people who will use it as an excuse not to sleep.
Dr. SCAMMELL: This is a concern. We--this--this is the first time I think as a
society we've had to really deal with this question. Modafinil, because it's
such a benign medicine, really is a very tempting one. It's easy to say, well,
let me just get by on three nights of, you now, of sleep per--per night during
the week and maybe I'll take modafinil to keep myself going during that time.
And with a medicine that has almost no side effects, that's really very
tempting. Yet I think it really begins to touch upon some very basic questions
of why do we sleep and what does sleep accomplish?
GIBSON: Well, Dr. Scammell, two people on this broadcast, very curious about
this, Diane and me. Modafinil, the generic name, Provigil, the name of the drug
under which it's marketed. But of course, bottom line, I know, there is no
substitute for sleep.
We'll be right back.
(Commercial break)
LOAD-DATE: January 31, 2002
LANGUAGE: ENGLISH
TYPE: Interview
Copyright 2001 American Broadcasting Companies, Inc.
905 of 998 DOCUMENTS
Espicom Business Intelligence
November 28, 2001
Modafinil in trials for SWSD
LENGTH: 168 words
Researchers at
Stanford University Medical Center are beginning a clinical trial
onCephalon'sProvigil (
modafinil) for shift work sleep disorder (SWSD), a problem caused by the
irregular or nocturnal hours kept by shift workers. Patients suffering from SWSD
may experience excessive on-the-job sleepiness, making it difficult to focus. In
addition, these people often have difficulties sleeping during off hours, which
can compound the problem.
Modafinil will be tested to see if it might enable patients to remain alert
while at work, without feeling over-stimulated or unable to sleep during
off-hours. Modafinil is currently approved by the FDA as a treatment for
excessive sleepiness associated with narcolepsy.
The research at Stanford is part of a US clinical trial currently accepting
volunteers. The 12-week double-blind trial will involve monitoring workers'
response to the drug both as they continue their regular work schedule and
through several sessions in the sleep laboratory.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2001 ESPICOM Business Intelligence Ltd.
906 of 998 DOCUMENTS
Espicom Business Intelligence
October 12, 2001
Cephalon's modafinil improves wakefulness in patients with obstructive sleep
apnea
LENGTH: 299 words
Results from
Cephalon's 327-patient, multi-centre, randomised, double-blind,
placebo-controlled, parallel-group study indicate that
Provigil (
modafinil) Tablets increased daytime wakefulness in patients suffering from
excessive daytime sleepiness (EDS) associated with obstructive sleep apnoea.
Obstructive sleep apnoea patients who use continuous positive airway pressure
received a once-daily dose of modafinil 200 or 400mg, or placebo, for 12 weeks.
Primary endpoint measures were the Maintenance of Wakefulness Test (MWT) and the
Clinical Global Impression of Change (CGI-C). Statistically significant
improvements in wakefulness and overall clinical condition were found at 12
weeks on the MWT (p<0.0001) and CGI-C (p<0.001) in patients treated with either
modafinil dose compared to placebo.
Secondary results were measured using a number of endpoints that assess
patients' wakefulness and quality of life, including the Epworth Sleepiness
Scale, the Functional Outcome of Sleep Questionnaire and the SF36 Health Quality
of Life Survey. The results of the secondary measures also were statistically
significant in patients treated with either modafinil dose compared to placebo.
The most commonly-reported side effects in this study were headache, nausea and
anxiety.
Modafinil is a unique, wake-promoting agent launched in the US in February 1999.
The American Academy of Sleep Medicine regards modafinil as a standard for the
treatment of EDS associated with narcolepsy. In controlled clinical trials,
modafinil has been found to be generally well tolerated with a low incidence of
adverse events relative to placebo. The most commonly observed adverse events
associated with the use of modafinil were headache, infection, nausea,
nervousness, anxiety and insomnia.
LOAD-DATE: October 3, 2002
LANGUAGE: ENGLISH
Copyright 2001 ESPICOM Business Intelligence Ltd.
907 of 998 DOCUMENTS
PR Newswire
May 24, 2001, Thursday
Cephalon Announces Marketing and Distribution Agreements For Modafinil in Mexico
and Taiwan
SECTION: FINANCIAL NEWS
LENGTH: 785 words
DATELINE: WEST CHESTER, Pa., May 24
Cephalon, Inc. (Nasdaq: CEPH), an international biopharmaceutical company,
announced today that it has granted rights to market, sell and distribute
modafinil to Armstrong Laboratorios de Mexico S.A.C.V. in Mexico and Sintong
Chemical Industrial Co., Ltd. in Taiwan. Cephalon markets modafinil as
PROVIGIL(R) (modafinil) tablets [C-IV] in the United States and several other
countries.
PROVIGIL is a unique, wake-promoting agent currently approved in several
countries for the treatment of excessive daytime sleepiness associated with
narcolepsy. The most common side effects associated with PROVIGIL in clinical
trials include headache, nausea, infection, nervousness, anxiety and insomnia.
"PROVIGIL has experienced major growth in the United States and has the
potential for significant growth in other global markets as well," said Frank
Baldino, Jr. Ph.D., chairman and CEO of Cephalon. "Armstrong and Sintong have
extensive experience within their respective markets and demonstrate solid
results in marketing their own brands and those of other global pharmaceutical
companies. We are confident that they will be successful launching modafinil in
Mexico and Taiwan."
Armstrong Laboratorios is a subsidiary of the Organizacion Bago, Latin
America's leading regional pharmaceutical company. Sales volume for Armstrong's
neurology and psychiatry products increased by 29 percent in 2000. The Mexican
pharmaceutical market is the tenth largest in the world and has been
experiencing greater percentage growth than the U.S. market.
Sintong, a diversified pharmaceutical, health care and chemicals company,
was established in Taiwan in 1945. With six regional offices in Taiwan and an
extensive sales channel that spans the medical, neurological and psychiatric
communities, Sintong is positioned for continued growth in Taiwan.
Cephalon markets modafinil in the United States, the United Kingdom,
Ireland, and Italy under the brand name PROVIGIL and promotes the product in
Austria and Switzerland under the brand name MODASOMIL(R). In addition,
Cephalon holds exclusive marketing and distribution rights to PROVIGIL in Japan,
South Korea, Latin America and Taiwan.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an
international biopharmaceutical company dedicated to the discovery, development
and marketing products for sleep and neurological disorders, cancer and pain.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties such as those set forth below and in its
reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange
Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend (and it is not obligated) to update publicly any forward-looking
statements. This discussion is permitted by the Private Securities Litigation
Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at www.cephalon.com. They are also available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804, extension
134563.
MAKE YOUR OPINION COUNT - Click Here
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SOURCE Cephalon, Inc.
CONTACT: Media: Mary Roche, 610-738-6415 or mroche@cephalon.com; or Investors:
Mary Beth Alvin, 610-738-6376 or malvin@cephalon.com, both of Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: May 25, 2001
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 2001 PR Newswire Association, Inc.
908 of 998 DOCUMENTS
Reuters Health Medical News
May 14, 2001 Monday 5:14 PM EST
Modafinil may promote wakefulness in Parkinson-related somnolence
BYLINE: By Paula Moyer
SECTION: CLINICAL
LENGTH: 504 words
DATELINE: PHILADELPHIA
Modafinil (Provigil), which has been approved for narcolepsy, also benefits
patients with somnolence related to Parkinson's disease, Dr. Charles H. Adler of
the Mayo Clinic Scottsdale, in Arizona, told participants here at the 53rd
annual meeting of the American Academy of Neurology.
He reported findings of a small double-blinded, placebo-controlled trial
consisting of 21 patients, 20 of whom completed the study. Dr. Adler and his
and colleagues found that seven patients treated with modafinil had significant
reductions on Epworth Sleepiness Scores (ESS), compared with one patient who
received placebo and two patients treated with both modafinil and placebo.
Modafinil may also have a role in treating depression-related somnolence,
according to Dr. Charles DeBattista of Stanford University School of Medicine.
He presented findings in New Orleans at the 154th annual meeting of the American
Psychiatric Association, which showed that, in a trial of 14 patients with major
depression, 8 of the 11 patients who completed treatment reported an improvement
in fatigue and cognition.
Cephalon, Inc., the manufacturers of Provigil, provided funding for both
studies.
The possibility of expanded indications for modafinil is consistent with
clinicians' findings, Dr. Thomas Kilkenny of Staten Island Hospital in New York
told Reuters Health. Although Dr. Kilkenny was not involved in either study and
has no relationship to the manufacturer, he has clinical experience with the use
of modafinil in his practice.
"I'm surprised it took so long for this to come out," Dr. Kilkenny told Reuters
Health. "There are a lot of illnesses that cause fatigue, and this is a novel
medication that causes a marked improvement in... wakefulness."
Although modafinil's mechanism of action is not fully understood, it may be
similar to amphetamines, yet different enough to have a lower risk of
amphetamine-type adverse effects, such as addiction and tachycardia. "We do
know that modafinil binds to only one of the neuroreceptor sites that
amphetamines do," Dr. Kilkenny said, noting that this may be the reason it has
fewer adverse effects.
In his practice, he often uses modafinil to treat patients with sleep apnea who
have residual sleepiness despite conventional treatment. "People sometimes need
the extra boost to achieve wakefulness," he told Reuters Health. "I think
further studies will [prove] this medication's benefits in fibromyalgia, chronic
fatigue and other conditions associated with daytime somnolence."
Although some patients on modafinil report nausea and headaches, these adverse
effects typically resolve over time, he said. Patients on modafinil do not
typically have any escalating need to increase the medication dose.
Because there are some drug-drug interactions associated with modafinil,
physicians should monitor patients who are on theophylline, diazepam, and some
beta-blockers. Patients on oral contraceptives may need a second mode of
contraception while on modafinil, Dr. Kilkenny told Reuters Health.
LOAD-DATE: July 11, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2001 Reuters Health
All Rights Reserved
909 of 998 DOCUMENTS
Neurology Alert
May 1, 2001
Brief Alert: Modafinil for Myotonic Dystrophy
LENGTH: 245 words
Brief Alert
Modafinil for Myotonic Dystrophy
Source: Damian MS, et al. Modafinil for excessive daytime sleepiness in myotonic
dystrophy. Neurology. 2001;56: 794-796.
Hypersomnia is a prominent feature of myotonic dystrophy (MyD), although,
interestingly, it is more often remarked upon by relatives than by patients. Not
felt to be true narcolepsy, its cause remains obscure. Modafinil, useful in
narcolepsy, may nevertheless be efficacious for excessive daytime sleepiness
(EDS) in MyD. In an open label trial, Damian and colleagues describe 8 patients
with genetically proven MyD (expanded CTG repeat on chromosome 19q13.13) and 1
with maternally inherited proximal myotonic myopathy (PROMM). Each patient
received 200-400 mg/d modafinil for a minimum of 16 weeks. All felt disabled by
their EDS prior to the modafinil. With treatment, mean sleep latency (measured
by MSLT) significantly increased, mean Epworth Sleepiness Scale score decreased,
and all patients felt subjectively better. Modafinil was well tolerated, without
significant side effects, blood pressure remained normal, and nighttime sleep
was unimpaired. Clearly, it is time to proceed with a placebo-controlled,
double-blind, multicenter trial.
Commentary
With this effective response and the relatively small number of persons who
used it, it seems to Damian et al that its duration of effect should first be
tested by the enlarging pioneer patients and providing a 6-month test time
table.-Michael Rubin
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2001 AHC Media LLC
All Rights Reserved
910 of 998 DOCUMENTS
PR Newswire
November 29, 2000, Wednesday
Cephalon Reports That a Recent Study Identifies a Possible Mechanism of Action
Of PROVIGIL-Induced Wakefulness
SECTION: FINANCIAL NEWS
LENGTH: 788 words
DATELINE: WEST CHESTER, Pa., Nov. 29
Cephalon, Inc. (Nasdaq: CEPH) reports today that a preclinical study published
in the November 15 issue of the Journal of Neuroscience provides further
evidence that PROVIGIL(R) (modafinil) activates specific neuronal pathways that
are believed to regulate normal wakefulness. In this study, modafinil strongly
activated two well- defined groups of nerve cells located in the hypothalamus
that have been implicated in the control of wakefulness - the tuberomammillary
nucleus (TMN) and orexin-containing nerve cells. This mechanism of action is
different from the pathways affected by traditional stimulants.
In three separate studies, modafinil was administered to rats at different
times of day in combination with physiological recordings of sleep/wake
behavior. The degree of nerve cell activation was then measured in various
areas of the brain. Results of these experiments showed that nerve cells in the
TMN were four times more active in rats administered modafinil than in control
animals. In addition, the number of activated orexin-containing nerve cells in
the hypothalamus increased threefold in rats administered modafinil.
According to Dr. Thomas Scammell, M.D., Assistant Professor in the
Department of Neurology at Beth Israel Deaconess Medical Center and lead author
of the study, "This is an exciting finding because it represents the first
demonstration of a drug directly activating these regions of the brain.
Selective activation of these regions may represent a novel approach to
producing wakefulness that is free of amphetamine-like subjective effects."
PROVIGIL(R) (modafinil) Tablets [C-IV] was approved by the Food and Drug
Administration (FDA) in December 1998 as a once-a-day therapy to improve
wakefulness in patients experiencing excessive daytime sleepiness associated
with narcolepsy. The most frequently reported adverse events observed in
clinical trials for narcolepsy were headache, nausea, nervousness, anxiety,
infection and insomnia. The exact mechanism of action of PROVIGIL is not known.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an
international biopharmaceutical company dedicated to the discovery, development
and marketing of products for sleep disorders, neurological disorders, pain
management and cancer.
This study was supported in part by a grant from Cephalon.
Reference: Scammell TE, Estabrooke IV, McCarthy MT, Chemelli, RM, Yanagisawa
M, Miller MS, Saper CB. Hypothalamic Arousal Regions are Activated during
Modafinil-Induced Wakefulness. Journal of Neuroscience, 2000 Nov. 15, 20(22):
8620-8628.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties such as those set forth below and in its
reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange
Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend (and it is not obligated) to update publicly any forward-looking
statements. This discussion is permitted by the Private Securities Litigation
Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at www.cephalon.com. They are also available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804, extension
134563.
SOURCE Cephalon, Inc.
CONTACT: Sheryl Williams of Cephalon, 1-800-283-4396, ext. 6493, or
swilliam@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: November 30, 2000
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 2000 PR Newswire Association, Inc.
911 of 998 DOCUMENTS
Deseret News (Salt Lake City)
November 3, 2000, Friday
Medication could fight fatigue in M.S. patients
SECTION: LIFE; Pg. C06
LENGTH: 175 words
SAN DIEGO -- Research presented at a meeting of the American Academy of
Neurology indicated multiple sclerosis patients finally have a more effective
and safe weapon against fatigue, one of the most impairing and disabling
symptoms of the disease.
"Fatigue, a common symptom of multiple sclerosis, can be so disabling that it
may impair one's ability to work at a time where there is minimal physical
disability," according to Kottil Rammohan, M.D., lead author of the study.
"Drugs presently used to treat fatigue are only marginally effective. Many of
the patients who participated in this study had tried conventional fatigue
treatments without benefit, but they responded to modafinil."
Modafinil is currently approved for the treatment of narcolepsy, a disorder of
excessive daytime sleepiness. As the first non-addicting drug effective in
reducing sleepiness and improving alertness, modafinil offers patients a
favorable alternative to commonly prescribed stimulants that can cause serious
long-term effects and have potential for abuse.
LOAD-DATE: November 3, 2000
LANGUAGE: ENGLISH
Copyright 2000 The Deseret News Publishing Co.
912 of 998 DOCUMENTS
Medical Post
October 17, 2000
Modafinil seen as a choice for ADHD: fewer side-effects than traditional
stimulants, once daily dosing a plus
BYLINE: Ross, Marvin
SECTION: Pg. v.36(35) O 17'00 pg 67 ISSN: 0025-7435
LENGTH: 484 words
TORONTO - Modafinil may be a useful alternative treatment for children with
attention deficit/hyperactivity disorder (ADHD), particularly for once a
day dosing or when side-effects limit the use of more traditional
stimulants.
Dr. Thomas Rugino, a pediatrician from Huntington, West Va., told the
participants at the recent American Academy for Celebral Palsy and
Developmental Medicine here, that modafinil is currently only indicated
for narcolepsy.
It is, however, also a stimulant totally unrelated to either
methylphenidate or amphetamine.
In addition to having a 15-hour effect, it has far fewer side-effects than
the traditional stimulants used for ADHD because its uptake in the brain
is much more limited.
It acts almost entirely in the anterior hypothalamus and does not involve
any other area of the brain.
Dr. Rugino carried out an open label trial where subjects were evaluated
before and after administration of modafinil. Every seven to 10 days, data
were collected and dosages adjusted to maximize benefits or reduce
side-effects.
Fifteen subjects, ages 5 to 15 were enrolled who met DSM-IV criteria for
ADHD and who did not suffer from an acute illness, heart or liver
problems, uncontrolled seizures, insomnia, manic episodes, psychosis,
migraines or were on medications that involved the P450 system or
neurotransmitter action.
Children who had been on ADHD treatment were able to participate if
sufficient time had elapsed for a proper washout.
Two children dropped out of the study because they were not compliant, one
child became ill and another had an adverse event.
All children were evaluated on the Connor's Rating Scales, ADHD Rating
Scale IV: School and Home Version and the Test of Variables of Attention
(TOVA). Doses began at 100 mg and increased to 400 mg although most
children were on 100 mg to 250 mg only.
Each child acted as his or her own control and was tested before and after
treatment.
The average treatment time was 4.6 weeks with highly significant
improvements seen for all subjects on all measures. The total TOVA score
showed significant improvements but sub-scores did show differences.
Impulsivity was much more improved than was inattentiveness. Both the
teachers' and the parents' Connor's Ratings showed statistically
significant improvements.
Weight loss, which is a problem with methylphenidate and amphetamines, was
not observed in these children.
Side-effects included headaches, feeling disoriented, and an increase in
biting of hands.
When the medication was given before 8 a.m., parents reported that the
effects lasted throughout the day so that a second dose was not required.
However, parents did notice that the effects began to wear off as the
evening progressed.
As the result of this study, Dr. Rugino feels that a double blind placebo
controlled trial is warranted to confirm these results.
Modafinil, currently indicated for narcolepsy, has fewer side-effects and
can last up to 15 hours
LOAD-DATE: January 8, 2001
LANGUAGE: ENGLISH
ACC-NO: 4969860
DOCUMENT-TYPE: Fulltext; Journal article
PUBLICATION-TYPE: Other
JOURNAL-CODE: 0945
Copyright 2000 Micromedia Limited
All Rights Reserved
Canadian Business and Current Affairs
Copyright 2000 Maclean Hunter Ltd.
913 of 998 DOCUMENTS
OTS Originaltextservice
September 20, 2000
Cephalon Launches Modafinil in Switzerland for Treatment of Narcolepsy
LENGTH: 777 words
DATELINE: West Chester, Pa.
Cephalon, Inc. (Nasdaq: CEPH) announced today that it has launched modafinil in
Switzerland for the treatment of narcolepsy. Modafinil, which is being promoted
by Cephalon in Switzerland under the trade name MODASOMIL(R), is a novel,
wake-promoting drug for the treatment of excessive daytime sleepiness (EDS)
associated with narcolepsy.
Narcolepsy is a chronic sleep disorder of unknown origin and generally begins in
young adulthood. The most common symptom of narcolepsy is EDS, which is
characterized by frequent irresistible sleep attacks that can last from a few
seconds to more than an hour. These attacks can take place any time, such as
during conversation, while attending class or while eating. As a result,
narcolepsy significantly impacts a person's quality of life.
"Swiss neurologists and sleep doctors now have the opportunity to offer their
narcolepsy patients a novel, once-a-day, well-tolerated, effective alternative
to the stimulants that have traditionally been used to treat this disabling
disorder, " said Frank Baldino, Jr., Ph.D., Cephalon's chairman and chief
executive officer. "With this launch, modafinil is now available in each of the
five European countries in which we have rights to market the drug."
Modafinil is a novel, wakefulness-promoting agent. In clinical trials, modafinil
was found to significantly improve daytime wakefulness. Patients also
experienced a significant improvement in the severity of their disease symptoms
and clinical condition. Modafinil has been found to be generally well-tolerated,
with a low incidence of adverse events that is relatively comparable to placebo.
The most commonly observed adverse events associated with modafinil are
headache, infection, nausea, nervousness, anxiety and insomnia.
Modafinil is marketed by Cephalon in the United States, the United Kingdom,
Ireland, and Italy under the brand name PROVIGIL(R) (modafinil) Tablets C-IV and
in Austria and Switzerland under the brand name MODASOMIL. In Switzerland, Mepha
AG is the marketing authorization holder for modafinil. In addition, Cephalon
has exclusive marketing rights to PROVIGIL in Japan, Latin America, South Korea,
and Taiwan.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an international
biopharmaceutical company dedicated to the discovery, development and marketing
of products to treat sleep disorders, neurological disorders and cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties such as those set forth below and in its
reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange
Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend (and it is not obligated) to update publicly any forward-looking
statements. This discussion is permitted by the Private Securities Litigation
Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at www.cephalon.com. They are also available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804, extension
134563.
ots Original Text Service: Cephalon, Inc. Internet:
http://recherche.newsaktuell.de
Contact: Sheryl Williams of Cephalon, +1-800-283-4396, ext. 6493, or
swilliam@cephalon.com
Company News On-Call: http://www.prnewswire.com/comp/134563.html or fax,
+1-800-758-5804, ext. 134563
Web site: http://www.cephalon.com
LOAD-DATE: September 20, 2000
LANGUAGE: English
PUB-TYPE: NewsWire
Copyright 2000 News Aktuell - DPA Firmengruppe
914 of 998 DOCUMENTS
PR Newswire
September 20, 2000, Wednesday
Cephalon Launches Modafinil in Switzerland for Treatment of Narcolepsy
SECTION: FINANCIAL NEWS
LENGTH: 760 words
DATELINE: WEST CHESTER, Pa., Sept. 20
Cephalon, Inc. (Nasdaq: CEPH) announced today that it has launched modafinil in
Switzerland for the treatment of narcolepsy. Modafinil, which is being promoted
by Cephalon in Switzerland under the trade name MODASOMIL(R), is a novel,
wake-promoting drug for the treatment of excessive daytime sleepiness (EDS)
associated with narcolepsy.
Narcolepsy is a chronic sleep disorder of unknown origin and generally
begins in young adulthood. The most common symptom of narcolepsy is EDS, which
is characterized by frequent irresistible sleep attacks that can last from a few
seconds to more than an hour. These attacks can take place any time, such as
during conversation, while attending class or while eating. As a result,
narcolepsy significantly impacts a person's quality of life.
"Swiss neurologists and sleep doctors now have the opportunity to offer
their narcolepsy patients a novel, once-a-day, well-tolerated, effective
alternative to the stimulants that have traditionally been used to treat this
disabling disorder, " said Frank Baldino, Jr., Ph.D., Cephalon's chairman and
chief executive officer. "With this launch, modafinil is now available in each
of the five European countries in which we have rights to market the drug."
Modafinil is a novel, wakefulness-promoting agent. In clinical trials,
modafinil was found to significantly improve daytime wakefulness. Patients also
experienced a significant improvement in the severity of their disease symptoms
and clinical condition. Modafinil has been found to be generally
well-tolerated, with a low incidence of adverse events that is relatively
comparable to placebo. The most commonly observed adverse events associated
with modafinil are headache, infection, nausea, nervousness, anxiety and
insomnia.
Modafinil is marketed by Cephalon in the United States, the United Kingdom,
Ireland, and Italy under the brand name PROVIGIL(R) (modafinil) Tablets [C-IV]
and in Austria and Switzerland under the brand name MODASOMIL. In Switzerland,
Mepha AG is the marketing authorization holder for modafinil. In addition,
Cephalon has exclusive marketing rights to PROVIGIL in Japan, Latin America,
South Korea, and Taiwan.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an
international biopharmaceutical company dedicated to the discovery, development
and marketing of products to treat sleep disorders, neurological disorders and
cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties such as those set forth below and in its
reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange
Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend (and it is not obligated) to update publicly any forward-looking
statements. This discussion is permitted by the Private Securities Litigation
Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at www.cephalon.com. They are also available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804, extension
134563.
SOURCE Cephalon, Inc.
CONTACT: Sheryl Williams of Cephalon, 800-283-4396, ext. 6493, or
swilliam@cephalon.com
URL: http://www.prnewswire.com
LOAD-DATE: September 21, 2000
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 2000 PR Newswire Association, Inc.
915 of 998 DOCUMENTS
PR Newswire Europe
September 20, 2000, Wednesday
CEPHALON LAUNCHES MODAFINIL IN SWITZERLAND FOR TREATMENT OF NARCOLEPSY
SECTION: GENERAL
LENGTH: 797 words
PR Newswire, London, September 20. This press release is transmitted on behalf
of Cephalon, Inc.
West Chester, Pa., September 20 /PR Newswire/ - Cephalon, Inc. (Nasdaq: CEPH)
announced today that it has launched modafinil in Switzerland for the treatment
of narcolepsy. Modafinil, which is being promoted by Cephalon in Switzerland
under the trade name MODASOMIL(R), is a novel, wake-promoting drug for the
treatment of excessive daytime sleepiness (EDS) associated with narcolepsy.
Narcolepsy is a chronic sleep disorder of unknown origin and generally begins in
young adulthood. The most common symptom of narcolepsy is EDS, which is
characterized by frequent irresistible sleep attacks that can last from a few
seconds to more than an hour. These attacks can take place any time, such as
during conversation, while attending class or while eating. As a result,
narcolepsy significantly impacts a person's quality of life.
"Swiss neurologists and sleep doctors now have the opportunity to offer their
narcolepsy patients a novel, once-a-day, well-tolerated, effective alternative
to the stimulants that have traditionally been used to treat this disabling
disorder, " said Frank Baldino, Jr., Ph.D., Cephalon's chairman and chief
executive officer. "With this launch, modafinil is now available in each of the
five European countries in which we have rights to market the drug."
Modafinil is a novel, wakefulness-promoting agent. In clinical trials, modafinil
was found to significantly improve daytime wakefulness. Patients also
experienced a significant improvement in the severity of their disease symptoms
and clinical condition. Modafinil has been found to be generally well-tolerated,
with a low incidence of adverse events that is relatively comparable to placebo.
The most commonly observed adverse events associated with modafinil are
headache, infection, nausea, nervousness, anxiety and insomnia.
Modafinil is marketed by Cephalon in the United States, the United Kingdom,
Ireland, and Italy under the brand name PROVIGIL(R) (modafinil) Tablets [C-IV]
and in Austria and Switzerland under the brand name MODASOMIL. In Switzerland,
Mepha AG is the marketing authorization holder for modafinil. In addition,
Cephalon has exclusive marketing rights to PROVIGIL in Japan, Latin America,
South Korea, and Taiwan.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an international
biopharmaceutical company dedicated to the discovery, development and marketing
of products to treat sleep disorders, neurological disorders and cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These may
include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. Cephalon's performance and financial
results could differ materially from those reflected in these forward-looking
statements due to general financial, economic, regulatory and political
conditions affecting the biotechnology and pharmaceutical industries as well as
more specific risks and uncertainties such as those set forth below and in its
reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and Exchange
Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you should not
rely on any such factors or forward-looking statements. Furthermore, Cephalon
does not intend (and it is not obligated) to update publicly any forward-looking
statements. This discussion is permitted by the Private Securities Litigation
Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at www.cephalon.com. They are also available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804, extension
134563.
UNS
CONTACT: Sheryl Williams of Cephalon, +1 800-283-4396, ext. 6493, or
swilliam@cephalon.com/ Company News On-Call:
http://www.prnewswire.com/comp/134563.html or fax, +1 800-758-5804, ext. 134563/
Web site: http://www.cephalon.com / PAP0029 4 GXX BT 660 ONDIGITAL ADDRESS +ZZZ
UUK NFL GEN NEX CATCHWORD" UNS GENERAL
LOAD-DATE: September 21, 2000
LANGUAGE: ENGLISH
Copyright 2000 PR Newswire Europe Limited
916 of 998 DOCUMENTS
Case Management Advisor
September 1, 2000
Drug promotes better sleep
LENGTH: 145 words
Drug promotes better sleep
Provigil Tablets (modafinil), manufactured by Cephalon in West Chester, PA,
increased daytime wakefulness in patients treated with continuous positive
airway pressure for sleep apnea.
Results of a multicenter, double-blind, placebo-controlled study of 157 sleep
apnea patients indicate that patients who were treated with modafinil performed
better on validated tests of excessive daytime sleepiness as measured by
standardized scales. The most common side effects were headaches, nervousness,
nausea, anxiety, and dizziness.
Cephalon recently initiated additional clinical trials with modafinil in sleep
apnea patients with the intention of pursuing a label extension to include this
additional indication. The drug is currently marketed in the United States for
the treatment of excessive daytime sleepiness associated with narcolepsy.
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 2000 AHC Media LLC
All Rights Reserved
917 of 998 DOCUMENTS
The Weekend Australian
June 24, 2000, Saturday
Wake to a bright new day / STAYING ALIVE
BYLINE: Jill Margo
SECTION: FEATURES; Pg. R31
LENGTH: 907 words
A new drug to combat sleep attacks had its origins in the battlefield
TRY to stay awake to the end of this column. If you do, you will have read about
the latest alert drug that, in the mildest possible way, seems to stop people
nodding off during the day.
The international sleep research community is buzzing with news of modafinil,
which protects people from sleep attacks -- outwardly benign events that can
have disastrous consequences.
Sleep attacks are brief, unwanted episodes occurring at inappropriate times.
They can last seconds or minutes and usually occur during times of reduced
stimulation such as reading, watching television, driving or being driven, or
sitting in a meeting.
About one in 10 adults suffer from excessive daytime sleepiness and
unpredictably drift into sleep. This problem is also one of the primary symptoms
of the rare condition narcolepsy.
For years people have been using amphetamines or caffeine to overcome such
sleepiness. Although amphetamines certainly do the job effectively, they have
unpleasant side effects. Drinking several cups of coffee is usually a safer but
less effective alternative.
Modafinil is said to combine the best of both with the power of amphetamines and
the safety profile of caffeine.
Although the drug is approved and widely used in Europe and the US, it is not
yet officially available in Australia but is bought here via the internet. (The
internet has been progressively used to bypass the cautious and protective
processes of the country's drug approval authority.)
In Europe and the US, modafinil is approved for use in narcolepsy but the French
Laboratoire L Lafon, which developed it, is trying to gain approval for wider
use. It says the drug can be used to treat attention deficit disorder, sleep
apnea, chronic fatigue syndrome and other sleep-wake disorders.
Ron Grunstein, of the Royal Prince Alfred Hospital's Sleep Disorder Centre,
Sydney, is circumspect.
"Modafinil certainly broadens the therapeutic range for the treatment of
narcolepsy, is safer than amphetamines and is not psychoactive, but we don't
know yet if it's better. Further research is needed," he says.
People who suffer excessive daytime sleepiness often have their condition
erroneously attributed to slothfulness, depression or a defective character.
The condition can strain relationships. It also can impair job performance and,
because it occurs so unpredictably, present a serious hazard -- for example,
someone falling asleep at the wheel of machinery.
Devastating industrial accidents such as the Three Mile Island and the Exxon
Valdez disasters in the US were officially attributed to errors of judgment due
to sleepiness in the workplace.
To protect sleep-deprived military troops from errors of judgment during
round-the-clock operations, the military regularly uses stimulants.
During the Gulf War, air crews were recommended amphetamines when unduly
fatigued through sleep loss.
Crack French troops of the Foreign Legion used modafinil during covert
operations inside Iraq during the Gulf War. There have since been newspaper
reports that Australia's elite troops -- officially cleared to use performance-
enhancing chemicals -- have been given the option of modafinil to keep them
going on all-night missions.
One of Europe's most prominent figures in sleep research, Michel Jouvet, from
Lyon University, told an international defence meeting in Paris that "modafinil
could keep an army on its feet and fighting for three days and nights with no
major side effects". Jouvet was a French resistance fighter and knows about
alertness during sustained operations.
Defence personnel have been used in several modafinil studies. The military
wanted to know if it could effectively counteract fatigue and decline in mental
performance due to sleep deprivation in normal populations.
One study of about 40 Canadian Force reservists found modafinil appeared to be
"a good alternative to amphetamine for counteracting the debilitating mood and
cognitive effects of sleep loss during sustained operations".
Although amphetamines induce feelings of euphoria, cause a loss of appetite and
increase heart rate and blood pressure, modafinil does none of these. Its
biggest side effect is a headache and, because it does not induce euphoria, its
potential for abuse is low.
A later Canadian study, however, found the drug tended to make the defence
personnel subjects overconfident when assessing their own cognitive performance
during sleep deprivation.
Just as the military is interested in broader applications, the drug may have
potential as an anti-fatigue agent for truck drivers, airline pilots and others
for whom a wakeful state is a critical.
The uniqueness of modafinil lies in its ability to stimulate only when
stimulation is required. Unlike amphetamines, it is not addictive and does not
affect normal sleep patterns. Although amphetamines keep people awake, those on
modafinil can revert to their usual sleep pattern if they want to. If they want
to remain awake, they will do so with more alertness.
It is said that after the initial dose, users comment that they can't discern
any effect. Several hours later, however, when they realise how they have
remained awake and maintained their attention, they suddenly become aware of the
benefit.
If you've read this far today without dozing off, you probably don't need it.
LOAD-DATE: December 3, 2001
LANGUAGE: ENGLISH
JOURNAL-CODE: AUS
Copyright 2000 Nationwide News Pty Limited
918 of 998 DOCUMENTS
The Weekend Australian
June 24, 2000, Saturday
Wake to a bright new day / STAYING ALIVE
BYLINE: Jill Margo
SECTION: FEATURES; Pg. R31
LENGTH: 907 words
A new drug to combat sleep attacks had its origins in the battlefield
TRY to stay awake to the end of this column. If you do, you will have read about
the latest alert drug that, in the mildest possible way, seems to stop people
nodding off during the day.
The international sleep research community is buzzing with news of modafinil,
which protects people from sleep attacks -- outwardly benign events that can
have disastrous consequences.
Sleep attacks are brief, unwanted episodes occurring at inappropriate times.
They can last seconds or minutes and usually occur during times of reduced
stimulation such as reading, watching television, driving or being driven, or
sitting in a meeting.
About one in 10 adults suffer from excessive daytime sleepiness and
unpredictably drift into sleep. This problem is also one of the primary symptoms
of the rare condition narcolepsy.
For years people have been using amphetamines or caffeine to overcome such
sleepiness. Although amphetamines certainly do the job effectively, they have
unpleasant side effects. Drinking several cups of coffee is usually a safer but
less effective alternative.
Modafinil is said to combine the best of both with the power of amphetamines and
the safety profile of caffeine.
Although the drug is approved and widely used in Europe and the US, it is not
yet officially available in Australia but is bought here via the internet. (The
internet has been progressively used to bypass the cautious and protective
processes of the country's drug approval authority.)
In Europe and the US, modafinil is approved for use in narcolepsy but the French
Laboratoire L Lafon, which developed it, is trying to gain approval for wider
use. It says the drug can be used to treat attention deficit disorder, sleep
apnea, chronic fatigue syndrome and other sleep-wake disorders.
Ron Grunstein, of the Royal Prince Alfred Hospital's Sleep Disorder Centre,
Sydney, is circumspect.
"Modafinil certainly broadens the therapeutic range for the treatment of
narcolepsy, is safer than amphetamines and is not psychoactive, but we don't
know yet if it's better. Further research is needed," he says.
People who suffer excessive daytime sleepiness often have their condition
erroneously attributed to slothfulness, depression or a defective character.
The condition can strain relationships. It also can impair job performance and,
because it occurs so unpredictably, present a serious hazard -- for example,
someone falling asleep at the wheel of machinery.
Devastating industrial accidents such as the Three Mile Island and the Exxon
Valdez disasters in the US were officially attributed to errors of judgment due
to sleepiness in the workplace.
To protect sleep-deprived military troops from errors of judgment during
round-the-clock operations, the military regularly uses stimulants.
During the Gulf War, air crews were recommended amphetamines when unduly
fatigued through sleep loss.
Crack French troops of the Foreign Legion used modafinil during covert
operations inside Iraq during the Gulf War. There have since been newspaper
reports that Australia's elite troops -- officially cleared to use performance-
enhancing chemicals -- have been given the option of modafinil to keep them
going on all-night missions.
One of Europe's most prominent figures in sleep research, Michel Jouvet, from
Lyon University, told an international defence meeting in Paris that "modafinil
could keep an army on its feet and fighting for three days and nights with no
major side effects". Jouvet was a French resistance fighter and knows about
alertness during sustained operations.
Defence personnel have been used in several modafinil studies. The military
wanted to know if it could effectively counteract fatigue and decline in mental
performance due to sleep deprivation in normal populations.
One study of about 40 Canadian Force reservists found modafinil appeared to be
"a good alternative to amphetamine for counteracting the debilitating mood and
cognitive effects of sleep loss during sustained operations".
Although amphetamines induce feelings of euphoria, cause a loss of appetite and
increase heart rate and blood pressure, modafinil does none of these. Its
biggest side effect is a headache and, because it does not induce euphoria, its
potential for abuse is low.
A later Canadian study, however, found the drug tended to make the defence
personnel subjects overconfident when assessing their own cognitive performance
during sleep deprivation.
Just as the military is interested in broader applications, the drug may have
potential as an anti-fatigue agent for truck drivers, airline pilots and others
for whom a wakeful state is a critical.
The uniqueness of modafinil lies in its ability to stimulate only when
stimulation is required. Unlike amphetamines, it is not addictive and does not
affect normal sleep patterns. Although amphetamines keep people awake, those on
modafinil can revert to their usual sleep pattern if they want to. If they want
to remain awake, they will do so with more alertness.
It is said that after the initial dose, users comment that they can't discern
any effect. Several hours later, however, when they realise how they have
remained awake and maintained their attention, they suddenly become aware of the
benefit.
If you've read this far today without dozing off, you probably don't need it.
LOAD-DATE: March 1, 2002
LANGUAGE: ENGLISH
JOURNAL-CODE: AUS
Copyright 2000 Nationwide News Pty Limited
919 of 998 DOCUMENTS
Reuters Health Medical News
June 22, 2000 Thursday
Wake-promoting drug shows promise in healthy, sleep-deprived individuals
BYLINE: By Jill Stein
SECTION: CLINICAL
LENGTH: 563 words
DATELINE: LAS VEGAS Jun 22
Modafinil, a nonamphetamine approved to treat excessive daytime sleepiness
associated with narcolepsy, consistently enhances performance and alertness in
healthy individuals who are sleep-deprived, according to preliminary results
presented at the 14th annual meeting of the Associated Professional Sleep
Societies (APSS).
In three separate studies, researchers found that modafinil improved alertness
and performance deficits in shift workers and military personnel.
"The results are extremely important because of growing numbers of individuals,
particularly in the work setting, whose jobs require lengthy bouts of sleep
deprivation," Dr. David Dinges, of the University of Pennsylvania, in
Philadelphia, said at a symposium where the data were released. "According to
the most recent government statistics, at least 2.9 million Americans work on
night shifts, and nearly 486,000 work as long-haul truck drivers."
"In addition, an estimated 1.5 million Americans are on active military duty,
which involves being awake for protracted periods of time during crises and
deploying highly lethal systems in hostile environments."
At the meeting, Dr. John A. Caldwell, of the US Army Aeromedical Research
Laboratory at Fort Rucker, Alabama, presented data from a flight simulator study
of six helicopter pilots who underwent two 40-hour periods of continuous
wakefulness separated by 1 night of recovery sleep. In one of the two
sleep-deprivation periods, three doses of modafinil (200 mg each) were
administered; placebo was given during the other deprivation period.
Pilots receiving three 200-mg doses of modafinil scored better on tests of
performance and physiological arousal during six flight maneuvers than they did
while on placebo, and had improved self-ratings of vigor, energy, alertness,
talkativeness and confidence.
Dr. Nancy Wesensten, of the Walter Reed Army Institute of Research in
Washington, DC, announced the results of a study that compared three doses of
modafinil (100 mg, 200 mg or 400 mg) to high-dose caffeine (600 mg) and placebo
in 50 healthy volunteers undergoing prolonged sleep deprivation.
In the trial, the active drug or placebo was administered over 40 hours of sleep
deprivation. Alertness, mood, performance and safety were evaluated during a
14-hour period after treatment.
Results showed that the 400-mg dose was effective for restoring cognitive
performance during prolonged sleep deprivation to near baseline levels. The
200-mg dose was slightly less effective.
Dr. Charles A. Czeisler, of the Harvard Medical School, in Boston,
Massachusetts, headed a study that monitored sleep and wake times in 16 healthy
shift workers for 24 hours per day for 4 days and included one 28-hour period of
sleep deprivation. Subjects were randomized to treatment with either 200 mg of
modafinil or placebo.
Modafinil improved alertness and performance compared with placebo, as measured
by standard, validated vigilance scales, and did not interfere with subsequent
daytime sleep opportunities.
In the three studies, the most common side effects related to modafinil
treatment were nausea, headache, vertigo and jitteriness. The investigators
emphasized that the side effects may be related to the dosages used in the
various studies and added that side effects must be decreased before this
medication can be considered for use in shift and military workers.
LOAD-DATE: July 11, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 2000 Reuters Health
All Rights Reserved
920 of 998 DOCUMENTS
Community Pharmacy
June 2000
Waking up to NARCOLEPSY
SECTION: Pg. 28
LENGTH: 1252 words
Narcolepsy is a disabling disorder for which there is no cure. But, as Claire
Waghorn, pharmacist at Papworth Hospital NHS Trust, explains, the symptoms can
be reduced with carefully monitored medication and a daily routine
Narcolepsy is a neurological disorder characterised by excessive daytime
sleepiness and irresistible sleep attacks. It can occur equally in men and women
of any age, although symptoms are often first seen in teenagers and young
adults. It is thought to affect around one in 2,500 people in the UK, although
it is believed that many thousands of sufferers may still remain undiagnosed.
Narcolepsy is a chronic and disabling condition. Treatment may be for life, and
there is very rarely remission. Depression, low self-esteem, problems at school
and loss of employment are common.
There are four classic symptoms of narcolepsy: excessive daytime sleepiness
(EDS); cataplexy; sleep paralysis; and hypnagogic/hypnopompic hallucinations.
Cataplexy is unique to narcolepsy and this sudden loss of muscle control can
range from slight weakness such as a drooping head, sagging jaw or buckling
knees, to complete body collapse, usually in association with strong emotion
such as anger or laughter.
Sleep paralysis creates an inability to move when falling asleep, or upon
waking, while the hallucinations are in the form of vivid, dream- like
experiences while falling asleep or awakening.
Not all people with narcolepsy suffer from every one of these symptoms, although
they all experience EDS.
There is no cure for narcolepsy, but it is possible to control or reduce
symptoms so that patients can lead a more normal life.
Treatments
Treatment can be non-pharmacological or pharmacological. In the former, the
first step is to promote good sleep habits: patients are encouraged to get a
full night's sleep, taken at the same time each day, including weekends. Short
naps should be planned throughout the day, usually after meals. Regular breaks
should be taken from tasks requiring prolonged concentration and work areas
should be well-lit and ventilated.
Alertness can be improved by taking regular exercise and avoiding vigorous
exercise close to bedtime. Caffeine should be avoided within six hours of
bedtime, as should alcohol before any activity for which it is important to
remain awake. Sufferers should also avoid smoking close to bedtime, whilst in
bed or when they feel sleepy.
Pharmacological treatment may also be required.
Patients often drink large quantities of caffeinated drinks but over-
the-counter medicines containing caffeine do not work well and are not
recommended for people with narcolepsy.
Amphetamines
Excessive daytime sleepiness may be controlled by amphetamines and related
drugs. Dexamphetamine (Dexedrine) and methylphenidate (Ritalin, which is not
licensed in the UK for treatment of narcolepsy) are generalised central nervous
system stimulants which decrease the number of sleep attacks, improve task
performance, and increase the time taken to fall asleep. These drugs cannot
eliminate sleep attacks altogether.
The disadvantages of these psychomotor stimulant drugs are that patients can
develop autonomic side effects, as well as motor hyperactivity and a sense of
euphoria which has led to reports of amphetamine abuse.
Common side effects are stomach pain, irritability, nervousness, headaches,
psychotic reactions, hypertension, and anorexia. Abruptly withdrawing these
stimulants can also cause fatigue, sleep rebound, hypersomnia and psychomotor
agitation. Unfortunately, tolerance to the effects of amphetamines may develop
in some patients with narcolepsy and some psychomotor stimulants, such as
dexamphetamine, have mild anti- cataplectic properties.
Both methylphenidate and dexamphetamine are schedule 2 controlled drugs.
Non-amphetamines
Modafinil is a non-amphetamine, wake-promoting agent. The precise mechanisms
through which modafinil promotes wakefulness are unknown. Although the effects
of modafinil are reduced by prazosin, an (1- adrenergic receptor) antagonist,
modafinil is not a direct or indirect (1-adrenergic) agonist.
Modafinil promotes vigilance and wakefulness, and decreases the number of
daytime sleep episodes associated with narcolepsy. To date, there have been no
reports of problems of abuse with modafinil, and withdrawal has not been
associated with any manifestations of drug- related dependency.
The drug is generally well tolerated, with the most common adverse effects being
nausea, headaches and rhinitis. Although it makes patients more alert, it does
not cause the euphoria experienced with the psychomotor stimulants. Further
experience is needed to determine whether tolerance to modafinil occurs.
Modafinil has no effect on cataplexy symptoms.
In vitro studies have shown modafinil to be a potential enzyme inducer and
inhibitor of certain enzymes, possibly reducing the effectiveness of some oral
contraceptives and anticonvulsants.
Shared care guidelines can be developed between the specialist centre and
primary care, outlining the use of modafinil and the responsibilities of the
hospital and the GP, allowing them to be more involved in the patient's
management. The fact that modafinil is not a controlled drug makes for simpler
prescribing and dispensing.
SSRIs
The most effective medications for treating cataplexy are antidepressants, and
both tricyclics and selective serotonin reuptake inhibitors (SSRIs) are used.
The effectiveness of antidepressants for the treatment of cataplexy is down to
their noradrenergic reuptake blocking effects and REM suppressant effects. In
general, tricyclics are more effective, but do have more side effects.
Clomipramine is the most effective tricyclic antidepressant in cataplexy.
Imipramine, protriptyline and the SSRIs fluoxetine and paroxetine, may also be
used.
Patients who require treatment for both sleepiness and cataplexy may be given
psychomotor stimulants and tricyclic antidepressants but will require monitoring
as the combination may produce serious adverse effects such as cardiac
arrhythmias or hypertension.
The antidepressant may also help with the dreams and nightmares experienced by
narcolepsy patients. Any pharmacological treatment should be combined with the
non-pharmacological measures.
SUMMARY
* Narcolepsy is a neurological disorder characterised by excessive daytime
sleepiness and irresistible sleep attacks
* In the UK, an estimated one in 2,500 people suffer from narcolepsy
* There is no cure for narcolepsy but symptoms can be reduced by a careful daily
routine
* Medication, such as amphetamines, can also reduce symptoms but they may
produce side effects and dependency
* OTC medicines containing caffeine are not recommended for sufferers
SLEEP STATISTICS
In a recent survey, Stafford-Miller finds that:
* 62 per cent of women and 38 per cent of men experience sleepless nights
* one person households are more likely to experience sleeplessness
* 60 per cent of sufferers experience a sleepless night two to three times a
week
* Use of OTC sleep aids has increased from 12 per cent in 1995 to 20 per cent in
1999; 24 per cent of users have taken the pharmacist's recommendation
* 46 per cent feel that sleep aids are preferable to prescription drugs
* 52 per cent believe that OTC drugs are safe and natural; 23 per cent stated
that they had no side effects
LOAD-DATE: June 5, 2000
LANGUAGE: English
PUB-TYPE: Magazine
Copyright 2000 CMP Information Ltd
921 of 998 DOCUMENTS
Medical Post
May 23, 2000
Narcolepsy drug improves fatigue in MS patients
BYLINE: Wansbrough, Gillian
SECTION: Pg. v.36(20) My 23'00 pg 16 ISSN: 0025-7435
LENGTH: 515 words
SAN DIEGO - Modafinil, which is currently approved for the treatment of
narcolepsy, may be effective in treating fatigue related to multiple
sclerosis.
Fatigue in these patients can be so disabling that it can impair their
ability to work at a time when there is minimal disability, according to
Dr. Kotti Rammohan, a neurologist at Ohio State University in Columbus.
In a nine-week, phase II, single-blinded trial at Ohio State and Kaiser
Permanente in San Diego, 72 patients received placebo for two weeks, 200
mg modafinil for weeks three and four, 400 mg during weeks four and five,
and placebo again for weeks seven through nine.
Modafinil is a stimulant used for the treatment of excessive daytime
sleepiness in narcolepsy. It has a different profile from the known
stimulants of sympathetic amines, and preliminary studies suggest it does
not affect dopamine, norepinephrine, serotonin, melatonin or histamine.
In a presentation at the meeting here, Dr. Rammohan noted, however, that
modafinil's wake-promoting effect can be nullified by the alpha-1
adrenergic receptor antagonists used in MS.
In contrast to amphetamines, which promote the global stimulation of the
central nervous system, modafinil has very specific stimulatory effects,
so the abuse potential is minor.
The patients in the study ranged in age from 18 to 65 and had mild to
moderate MS (77% were relapsing-remitting) and moderate to severe fatigue.
Most had Extended Disability Status Scores of zero to 3, while some scored
6. Many of these patients had tried conventional fatigue treatments such
as amantadine without benefit.
Exclusion criteria were sleep-related disorders, systemic disorders,
hypertension, substance abuse problems, excess caffeine consumption, or
use of other medications (including OTC) that would influence sleep.
''The 200 mg dose of modafinil did overcome the placebo effect, but not the
400 mg dose,'' said Dr. Rammohan. ''In fact, when comparing the 400 mg to
baseline it has a significant effect but not when compared to the placebo.
''At this point we would not consider 400 mg to be an effective dose.''
Efficacy was evaluated at screening and after each study phase using the
Fatigue Severity Scale (FSS), a visual analogue global fatigue scale
(VAFS)-a global assessment of how the patient is feeling-and the Modified
Fatigue Impact Scale (MFIS), which has physical, cognitive and
psychosocial subgroups.
Mean total scores on the three scales of increasing fatigue for modafinil
200 mg/day and placebo were 42.4 vs 49.4 on the FSS, 5.5 vs 4.3 on the
VAFS, and 37.3 vs 46.2 on the MFIS.
The 200 mg dose had the best effect on the MFIS and the VAFS, while both
doses were effective on the FSS, ''suggesting the mechanism by which
modafinil may act may be different for fatigue as compared to the
mechanism involved in sleep.''
Dr. Rammohan suggested this drug may become the first-line treatment
against fatigue in MS patients. ''Patients' perceptions of accomplishing
daily activities were significantly improved with modafinil treatment,''
he said. The study was funded through a grant from Cephalon, Inc., the
makers of modafinil.
LOAD-DATE: September 5, 2000
LANGUAGE: ENGLISH
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922 of 998 DOCUMENTS
PR Newswire
May 18, 2000, Thursday
Physician Reports First U.S. Study of Modafinil (PROVIGIL(R)) in ADHD
SECTION: FINANCIAL NEWS
LENGTH: 970 words
DATELINE: WEST CHESTER, Pa., May 18
A study presented today at the annual meeting of the American Psychiatric
Association (APA) in Chicago described the effects of modafinil and the drug's
potential as a treatment for Attention Deficit Hyperactivity Disorder (ADHD).
The study conducted by Fletcher B. Taylor, M.D., of Tacoma, WA, compared
modafinil to dextroamphetamine, a commonly used amphetamine, and placebo in
adults with ADHD. Results of the study demonstrated that an average daily dose
of approximately 200 mg of modafinil produced a statistically and clinically
significant reduction (30 percent or more) in the symptoms of ADHD as measured
by the Diagnostic and Statistical Manual of Mental Disorders Fourth Edition
(DSM-IV) ADHD Behavior Checklist for Adults, compared to placebo. Modafinil is
marketed as PROVIGIL(R) (modafinil) Tablets [C-IV] in several countries,
including the United States, by Cephalon, Inc. (Nasdaq: CEPH) for the treatment
of excessive daytime sleepiness associated with narcolepsy.
The double-blind, placebo-controlled, cross-over study included 22 adult
patients meeting the DSM-IV diagnostic criteria for ADHD. In this study,
dextroamphetamine at an average daily dose of approximately 20 mg also reduced
the symptoms of ADHD with an effect similar to that of modafinil. Both
medications were well tolerated. Compared to placebo, the most commonly
reported side effects for both modafinil and dextroamphetamine were insomnia,
irritability, muscle tension and appetite suppression.
Dr. Taylor indicated that he and his colleagues initiated the study because
some of their patients wanted an alternative therapy. Today, stimulants,
including amphetamine, methylphenidate and pemoline are the most established
treatments for ADHD. Treatment of ADHD with traditional stimulants is often
associated with troublesome side effects, tolerance and the potential for abuse.
In addition, some patients do not respond to currently available therapies.
According to Dr. Taylor, "Modafinil, with its low potential for abuse, may
represent a valuable treatment option for adults with ADHD."
ADHD affects an estimated 5 to 7 million adults and children in the United
States. Dr. Taylor noted that while 30 to 70 percent of children with ADHD will
retain the diagnosis through adulthood, in his study 70 percent of the
participants had a relative with ADHD, usually their child.
"We are pleased by the results of this independent study and hope to
corroborate these findings with data from our own studies in adults with ADHD,"
stated Frank Baldino, Jr., Ph.D., chairman and chief executive officer of
Cephalon.
Cephalon currently is conducting studies with PROVIGIL in adults with ADHD
at seven academic medical centers in the United States. In addition, Cephalon
has initiated a pharmacokinetic study and intends to initiate a dose-ranging
study in children by mid-year, as a prelude to a Phase 3 study in children with
ADHD.
PROVIGIL was approved by the Food and Drug Administration (FDA) in December
1998 as a once-a-day therapy to improve wakefulness in patients experiencing
excessive daytime sleepiness due to narcolepsy. The most frequently reported
adverse events observed in clinical trials for narcolepsy were headache, nausea,
nervousness, anxiety, infections and insomnia.
Cephalon, Inc., headquartered in West Chester, Pennsylvania, is an
international biopharmaceutical company dedicated to the discovery, development
and marketing of products to treat neurological disorders, sleep disorders and
cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide Cephalon's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, interpretation of
clinical results, prospects for regulatory approval, manufacturing development
and capabilities, market prospects for its products, sales and earnings
projections, and other statements regarding matters that are not historical
facts. You may identify some of these forward-looking statements by the use of
words in the statements such as "anticipate," "estimate," "expect," "project,"
"intend," "plan," "believe" or other words and terms of similar meaning.
Cephalon's performance and financial results could differ materially from those
reflected in these forward-looking statements due to general financial,
economic, regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties such
as those set forth below and in its reports on Form 8-K, 10-Q and 10-K filed
with the U.S. Securities and Exchange Commission. Given these risks and
uncertainties, any or all of these forward-looking statements may prove to be
incorrect. Therefore, you should not rely on any such factors or
forward-looking statements. Furthermore, Cephalon does not intend (and it is not
obligated) to update publicly any forward-looking statements. This discussion
is permitted by the Private Securities Litigation Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at http://www.cephalon.com. They are also available by fax 24 hours a day
at no charge by calling PR Newswire's Company News On-Call at 800-758-5804,
extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Sandra Menta (Investors), 610-738-6376, or Sheryl Williams (Media),
610-738-6493, both of Cephalon, or Michael Kaplan (Media) of Makovsky & Co,
Inc., 212-508-9673, for Cephalon
URL: http://www.prnewswire.com
LOAD-DATE: May 19, 2000
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923 of 998 DOCUMENTS
PR Newswire
May 2, 2000, Tuesday
Narcolepsy Drug Helps Control Fatigue in Patients With MS
SECTION: FINANCIAL NEWS
LENGTH: 500 words
DATELINE: COLUMBUS, Ohio, May 2
A drug used to treat some of the symptoms of the sleeping disorder narcolepsy
also appears to help control fatigue in-patients with multiple sclerosis.
Researchers found that a 200 milligram-per-day dose of the drug modafinil,
sold under the brand name Provigil, successfully controlled fatigue in-patients
with MS, a disease that attacks the nervous system. "About 70 percent of all MS
patients suffer from fatigue," said Kottil Rammohan, an associate professor of
neurology at Ohio State University. "It's one of the most disabling symptoms of
MS."
Other symptoms of MS include blurred vision, tremors and weakness,
particularly in the legs. Rammohan will present the study's findings on May 1
at the annual meeting of the American Academy of Neurology in San Diego.
Provigil is currently approved to treat excessive daytime sleepiness, which
is one of the major symptoms of patients with narcolepsy.
During a nine-week trial, the researchers studied 72 patients with severe
fatigue and MS. The patients received a placebo during the first two weeks and
again during the final three weeks of the study. During weeks three and four,
each patient received 200 milligrams of modafinil; during weeks five and six,
the dosage was increased to 400 mg daily.
After each phase of treatment, the researchers asked each patient to
evaluate their level of fatigue and sleepiness. Overall, patients reported
significantly less fatigue when they took the 200-mg dose compared to the
placebo. However, when patients took the 400-mg dose, some of them experienced
side effects that "probably overshadowed any favorable effects on fatigue by the
drug," Rammohan said.
In this study, the most common side effects of the 200-mg dosage were
headaches (19 percent of patients); nervousness (14 percent); and loss of
physical strength (12 percent). "None of the side effects reported by patients
were serious, however," Rammohan said.
In addition to helping control fatigue, and unlike similar drugs, modafinil
has little potential for abuse, according to Rammohan.
"There's some stimulant effect with this drug," he said. "But modafinil
targets select areas of the brain -- the areas presumably important to fatigue
and to wakefulness. Stimulants such as Ritalin and amphetamines cause the whole
brain to light up in terms of activity."
Rammohan conducted the study with Charles Pollak, D. Joanne Lynn and Haikady
Nagaraja, all at Ohio State; and Jay Rosenberg and Andrew Blumenfeld, both with
Kaiser Permanente in San Diego. This study was funded by a grant from the
National Institutes of Health, and by Cephalon, Inc. (Nasdaq: CEPH), the
manufacturer of Provigil.
SOURCE Cephalon Inc.
CONTACT: Kottil Rammohan, M.D., Lead Investigator, of OSU School of Medicine,
614-329-7556; or Holly Wagner, Associate Editor of OSU Communications,
614-292-8310
URL: http://www.prnewswire.com
LOAD-DATE: May 3, 2000
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 2000 PR Newswire Association, Inc.
924 of 998 DOCUMENTS
Reuters Health eLine News
May 2, 2000 Tuesday
Narcolepsy drug helps relieve fatigue of multiple sclerosis
LENGTH: 340 words
DATELINE: SAN DIEGO May 2
A medication approved to treat the sleep disorder narcolepsy may help improve
fatigue in patients with multiple sclerosis (MS), according to study results
reported here at the American Academy of Neurology annual meeting.
The drug is known as modafinil, according to Dr. Kottil W. Rammohan, of Ohio
State University in Columbus. Multiple sclerosis is caused by a destruction of
nerve fibers in the brain and spinal cord, which result in muscle weakness,
dizziness and vision problems.
"More than 75% of MS patients have chronic disabling fatigue irrespective of the
severity of their MS, and current treatments are, for the most part,
ineffective," Rammohan said. "The findings suggest that modafinil may be
superior in terms of effectiveness, safety and tolerability, and lack of
potential for abuse."
In a 9-week study, 72 patients with MS took alternating doses of modafinil or an
inactive placebo.
The patients were aged 18 to 65 and were experiencing fatigue that was not
relieved by treatment with the drugs amantadine and pemoline, which are
conventionally used to treat fatigue. The trial excluded patients with
narcolepsy, a condition in which people suffer from episodes of an
uncontrollable desire to sleep.
The results showed that modafinil improved fatigue on each of three assessment
scales. Overall, 85% of patients were able to distinguish the active medication
from placebo solely on the basis of their improvement in fatigue.
The most common side effects were headache, nervousness and weakness, which
occurred more frequently with a higher dose of the drug. Only four patients
withdrew from the study because of side effects related to modafinil. Patients
said they preferred the lower dose of the drug because it was better tolerated.
Rammohan said studies are planned that will examine the use of modafinil in
chronic fatigue syndrome and fatigue associated with chemotherapy.
The present trial was conducted at Kaiser Permanente Medical Center in San Diego
and funded by Cephalon, Inc., the company that manufactures modafinil.
LOAD-DATE: July 21, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
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All Rights Reserved
925 of 998 DOCUMENTS
United Press International
May 2, 2000, Tuesday
Health Tips
BYLINE: By LIDIA WASOWICZ, UPI Science Writer
SECTION: GENERAL NEWS
LENGTH: 625 words
0-
DRUG EASES MS FATIGUE: Multiple sclerosis patients can get a boost from a new
drug. The drug modafinil can help them overcome a serious side effect of their
condition, tiredness, a study indicates. The report, presented at the American
Academy of Neurology's 52nd Annual Meeting in San Diego, points out that fatigue
is a common symptom of multiple sclerosis and that it can be disabling. Lead
study author Dr. Kottil Rammohan, neurologist at Ohio State University in
Columbus, said: "Drugs used to treat fatigue are only marginally effective. Many
of the patients who participated in this study had tried conventional fatigue
treatments without benefit, but they responded to modafinil." Modafinil is
approved for the treatment of narcolepsy, a disorder of excessive daytime
sleepiness.
0-
GENE THERAPY BOOSTS AGING BRAIN: Gene therapy could rejuvenate aging brain
networks, researchers report. The study of monkeys shows age-related
deterioration in critical brain networks night be restored with such treatment.
The study, presented at the American Academy of Neurology's 52nd Annual Meeting
in San Diego, supports another trial testing gene therapy against Alzheimer's
disease. Researchers from the University of California, San Diego, found normal
aging in monkeys causes a 28 percent decline in the density of certain brain
networks originating from nerve cells called neurons deep in the brain. The
scientists could restore these connections by transplanting brain cells
genetically programmed to release a protein called "nerve growth factor." "It
would be inappropriate to suggest that this approach could be used to treat the
course of normal aging, but it is not a far stretch to suggest that this may be
useful in the treatment of Alzheimer's disease," said Dr. Mark Tuszynski,
researcher at the Center for Neural Repair at UCSD and principal study author.
0-
WORKPLACE CAN HELP SMOKERS QUIT: If you're trying to quit smoking, you'll be
better off working in a place that frowns on the unhealthy habit, a study shows.
Researchers at the University of California, Berkeley, found smokers employed in
locations with strong anti-smoking workplace ordinances were 38 percent more
likely to quit over a six-month period than those in regions with no such laws.
The study, published in the American Journal of Public Health, was conducted in
California before the state had a statewide workplace smoking law. "The benefits
of workplace smoking ordinances for non-smokers are well known," said study
co-author Joel Moskowitz, director of UC Berkeley's Center for Family and
Community Health in the School of Public Health. "This is the first time we've
seen such a big benefit for smokers also."
0-
STRESS INCREASES COLITIS RISK: A study shows long-term stress increases the risk
of ulcerative colitis, a potentially serious disease of the digestive tract. The
disease differs from irritable bowel syndrome, which is non-inflammatory. It
causes an inflammation of the inner lining of the colon and rectum. The study
finally gives scientific evidence for what patients and doctors have been saying
all along. "Despite the tenacity of the stress-exacerbation hypothesis, there is
little evidence in its favor," said lead author Dr. Susan Levenstein of the San
Camillo-Forlanini Hospital in Rome, Italy, who conducted the research while at
the Nuovo Regina Margherita Hospital in Rome. Previous studies testing the
effects of stress-reduction techniques and psychotherapy found these therapies
had little impact on ulcerative colitis, but Levenstein suggests better results
might be found if psychologically oriented therapies are offered to select
patients who are likely to benefit rather than being given indiscriminately.
0-
LOAD-DATE: May 3, 2000
LANGUAGE: ENGLISH
Copyright 2000 U.P.I.
926 of 998 DOCUMENTS
United Press International
May 1, 2000, Monday
Sleep disorder drug beats fatigue in MS
BYLINE: By ED SUSMAN, UPI Science News
SECTION: GENERAL NEWS
LENGTH: 540 words
DATELINE: SAN DIEGO, May 1
Doctors said Monday a drug now used for treatment of narcolepsy -- a sleep
disorder -- appears to help most patients who suffer from disabling fatigue due
to multiple sclerosis (MS).
"Patients told us that when they took modafinil is was like a load lifting from
their shoulders," said Dr. Kottil Rammohan, associate professor of neurology at
Ohio State University, Columbus.
Modafinil has been approved for the treatment of narcolepsy in the US and
abroad. Rammohan's study is the first to show effectiveness in fatigue
associated with MS.
"Fatigue is a common problem and among the most disabling symptoms of MS,"
Rammohan said at the annual meeting of the American Academy of Neurology in San
Diego. "Modafinil (Provigil, manufactured by Cephalon, Inc., West Chester,
Penn.) is a novel wake-promoting agent that is effective and well tolerated for
the treatment of excessive daytime sleepiness in patients with narcolepsy."
In the study, 72 confirmed MS patients suffering from fatigue participated in
the 9-week treatment regimen. First they were given dummy pills for two weeks
and then received 200 milligrams of modafinil for two weeks, then 400 mg for two
weeks and then placebo pills again for three weeks.
Although the study was designed so that patients were supposed to be unaware of
when they were receiving the active drug, Rammohan said, "About 85 percent of
the patients knew when they were getting modafinil because their fatigue
improved so markedly."
Two drugs that are currently used to treat fatigue in MS patients, amantadine
and pemoline, have not been shown to have a significant impact on fatigue as
measured by standard scales, Rammohan said.
"These drugs are only marginally effective," he said. "Many of the patients who
participated in this study have tried conventional fatigue treatments without
benefit, but they responded to modafinil."
The study results impressed Dr. Robin Brey, associate professor of radiology at
the University of Texas Health Science Center at San Antonio. "I have begun to
prescribe modafinil to my patients. Fatigue in MS is possibly the most disabling
condition in MS. It comes on suddenly as with other MS symptoms. My patients
describe this fatigue as if they were hitting a wall," Brey said.
"This is truly exciting," she said. "It's going to help a lot of people."
Rammohan said that his patients found the 200 mg dose of the drug was preferred
by his patients. "The higher dose made the patients feel jittery and
uncomfortable," he said at a press briefing.
On standard scales of fatigue, patients were able to record a one point
improvement in their scores. Rammohan said the study would have considered a
half-point improvement a success. the fatigue scale ranges from 1 to 7, with 7
being the worst fatigue experience. Most patients were at a 5-6 level and taking
the drug lowered that by a point.
"Generally the 200 mg dose of modafinil was very well tolerated by patients,"
Rammohan said. "Modafinil has no major toxicity and has a favorable long-term
use in Europe."
Rammohan said further studies of modafinil in fatigue associated with cancer
chemotherapy, chronic fatigue syndrome and other fatigue conditions are planned
by the manufacturer.
LOAD-DATE: May 2, 2000
LANGUAGE: ENGLISH
Copyright 2000 U.P.I.
927 of 998 DOCUMENTS
Reuters Health Medical News
March 14, 2000 Tuesday
Modafinil improves excessive daytime sleepiness in narcolepsy
SECTION: CLINICAL
LENGTH: 363 words
DATELINE: WESTPORT Mar 14
Modafinil, a unique wake-promoting agent, safely reduces excessive daytime
sleepiness in patients with narcolepsy, according to a report in the March 14th
issue of Neurology.
Dr. Paul T. Gross, of the Lahey Clinic in Burlington, Massachusetts, and
colleagues with the US Modafinil in Narcolepsy Multicenter Study Group,
investigated the safety and effectiveness of 9 weeks of modafinil therapy (200
mg/day or 400 mg/day) in 271 patients diagnosed with narcolepsy according to
International Classification of Sleep Disorders criteria.
At the end of 9 weeks, improvements in mean sleep latency were greater in the
modafinil groups than in the placebo group, the authors report. As measured by
the Multiple Sleep Latency Test, mean sleep latency was 5.1 minutes in the
modafinil 400-mg/day group, compared with 4.9 minutes in the 200-mg/day group
and 3.5 minutes in the placebo group.
Similarly, mean sleep latency as measured by the Maintenance of Wakefulness Test
"improved for each modafinil treatment group (200 mg and 400 mg) compared with
placebo at every follow-up visit (weeks 3, 6, and 9)," the investigators note.
Upon discontinuation of medication, the patients' sleepiness returned and, in
the case of the 400-mg group, briefly rebounded above the baseline level, the
results indicate.
"The percent of patients with improved clinician assessment of illness...was
greater for modafinil 200 mg (46/80 patients, 58%) and 400 mg treatment groups
(51/83 patients, 61%) compared with placebo (32/84 patients, 38%) at week 9,"
the authors observe.
Overall, there were no significant differences in the number of adverse
experiences among the three patient groups, the investigators indicate, though
more patients in the modafinil groups experienced nausea and, in the 200-mg
group, rhinitis. There appeared to be no withdrawal symptoms or abuse potential
with modafinil.
"Thus," the authors conclude, "modafinil is not only a well-tolerated and
effective treatment for [excessive daytime sleepiness] associated with
narcolepsy, its minimal side-effect profile during dosing and withdrawal
represent clinical advantages over existing therapeutics."
SOURCE: Neurology 2000;54:1166-1175.
LOAD-DATE: July 11, 2008
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PUBLICATION-TYPE: Newswire
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All Rights Reserved
928 of 998 DOCUMENTS
Reuters Health eLine News
March 14, 2000 Tuesday
New drug helps narcolepsy patients stay awake
LENGTH: 439 words
DATELINE: NEW YORK Mar 14
Modafinil, a new, nonaddicting drug with few side effects, significantly
improves the excessive daytime sleepiness experienced by people with narcolepsy,
report US researchers.
Narcolepsy is a disorder of the sleep-wake cycle. Patients with this disorder
suddenly fall into deep sleep, and experience abnormal daytime sleepiness.
Narcolepsy affects about 1 in every 2,000 people, and often first appears in the
teenage years.
Currently, narcolepsy is treated with amphetamines and amphetamine-like drugs,
but this may lead to side effects such as palpitations, anxiety and nausea, or
to dependence on these drugs.
In a search for an alternative treatment, Dr. Paul T. Gross from Lahey Clinic in
Burlington, Massachusetts, and other members of the US Modafinil in Narcolepsy
Multicenter Study Group tested the safety and effectiveness of modafinil therapy
in 271 narcolepsy patients. The results of the study, funded by the drug's
manufacturer Cephalon, Inc., are published in the March 14th issue of the
journal Neurology.
The researchers tested the drug by asking patients to sit quietly in a darkened
room and try to stay awake. During a 9-week study, they tested two doses of the
drug -- 200 mg and 400 mg -- against a placebo ("dummy") pill. They found that
those taking modafinil could stay awake longer than those taking placebo -- 5
minutes, compared with 3.5 minutes.
Similarly, other tests of the tendency to fall asleep quickly "improved for each
modafinil treatment group (200 mg and 400 mg) compared with placebo at every
follow-up visit (weeks 3, 6, and 9)," the investigators note.
Patients taking the drug also reported feeling less sleepy during the day. But
once the patients stopped taking the medication, their sleepiness returned.
Overall, there were no major differences in the number of side effects, the
investigators indicate, although more patients in the modafinil groups
experienced nausea and, in the 200 mg group, nasal symptoms. There appeared to
be no withdrawal symptoms or potential for drug abuse with modafinil.
"Thus," the authors conclude, "modafinil is not only a well-tolerated and
effective treatment for excessive daytime sleepiness associated with narcolepsy,
its minimal side-effect profile during dosing and withdrawal represent clinical
advantages over existing therapeutics."
"While modafinil significantly improves alertness and has advantages over
existing therapies, we must keep in mind that no treatment for narcolepsy can
completely resolve its symptoms," Gross said in a news release. "Further
research and study of this life-altering disorder is required."
SOURCE: Neurology 2000;54:1166-1175.
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PUBLICATION-TYPE: Newswire
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All Rights Reserved
929 of 998 DOCUMENTS
PR Newswire
September 30, 1999, Thursday - 14:17 Eastern Time
Cephalon Updates Investors on Product Development Programs
SECTION: Financial News
LENGTH: 1057 words
DATELINE: NEW YORK, Sept. 30
Cephalon, Inc. (Nasdaq: CEPH) president and chief executive officer, Frank
Baldino, Jr., Ph.D., today provided an update on the company's lead product,
PROVIGIL(R) (modafinil) Tablets C-IV, its marketing strategy for GABITRIL(R)
(tiagabine hydrochloride), and its advancing pipeline in the fields of neurology
and oncology.
In remarks delivered to investors attending the Warburg Dillon Read Global
Health Care Conference in New York, Dr. Baldino reported on increasing sales of
PROVIGIL and its acceptance in the U.S. narcolepsy market since the product's
launch in February. He noted that the company has been conducting clinical
studies this year to validate the potential use of PROVIGIL in the treatment of
other disorders such as sleep apnea, fatigue in multiple sclerosis, and
attention deficit hyperactivity disorder (ADHD). The company expects to
complete several of these studies by year-end, and will report trial results as
they become available. Results from a small study with PROVIGIL in patients
with hypersomnia will be presented next week at the World Federation Sleep
Research Society meeting in Germany.
Dr. Baldino also reported on a recently published study demonstrating that
administration of modafinil (PROVIGIL) resulted in significant improvements in
several quality of life measurements, and also showed that narcolepsy imposes a
serious burden on a person's quality of life. This study entitled: "The
Health-Related Quality of Life Effects of Modafinil in the Treatment of
Narcolepsy," was published in the September 15th issue of the journal Sleep.
According to Dr. Joyce Walsleben, Ph.D., Assistant Professor of Medicine at NYU
School of Medicine and Director of the NYU Sleep Disorders Center at Bellevue
Hospital Center, and an author of the multi-center study, "This study shows that
this therapy could significantly improve a number of quality-of- life
parameters, such as social functioning and mental health."
Dr. Baldino stated that Cephalon has expanded its sales force to 90 territory
sales specialists, to market PROVIGIL and GABITRIL, a product of Abbott
Laboratories, to neurologists in the United States. Dr. Baldino believes that
the company's experienced sales force can increase the market share of GABITRIL
in the partial seizure marketplace over the next several years, and noted that
the company will co-develop the product with Abbott to maximize the product's
potential in treating partial seizures as well as in treating other neurological
conditions.
Commenting on the company's advancing pipeline in neurology and oncology, Dr.
Baldino reviewed the company's recent collaboration with H. Lundbeck A/S, which
focuses on the discovery, development and marketing of products for the
treatment of neurodegenerative diseases. The company discovered a novel class
of orally active, small molecules, which in preclinical studies, has been shown
to promote neuronal survival in animal models of Parkinson's disease and
Alzheimer's disease; data from these studies will be presented at the Society
for Neuroscience meeting in Miami at the end of November. This past July, the
companies advanced the program's lead molecule, CEP-1347, into Phase 1
development for the treatment of Parkinson's disease.
Dr. Baldino also provided an update on the company's oncology program with TAP
Holdings in prostate and other cancers. Prostate cancer is the second leading
cause of cancer death in men, and current therapies for this disease treat
hormone-dependent tumors. The company's lead molecule, CEP-701, in preclinical
studies, slowed tumor growth in the prostate, and if effective in man, has the
potential to impact both hormone-dependent and hormone- independent tumor
growth. Results of the Phase 1 studies showed that CEP-701 is well tolerated;
this compound is scheduled to enter Phase 2 development later this year for the
treatment of prostate cancer.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company dedicated to the discovery, development and marketing
of products to treat neurological disorders, sleep disorders and cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Forward-looking statements
provide the company's current expectations or forecasts of future events. These
may include statements regarding anticipated scientific progress on its research
programs, development of potential pharmaceutical products, prospects for
regulatory approval, manufacturing development and capabilities, market
prospects for its products, sales and earnings projections, and other statements
regarding matters that are not historical facts. You may identify some of these
forward-looking statements by the use of words in the statements such as
"anticipate," "estimate," "expect," "project," "intend," "plan," "believe" or
other words and terms of similar meaning. The company's performance and
financial results could differ materially from those reflected in these
forward-looking statements due to general financial, economic, regulatory and
political conditions affecting the biotechnology and pharmaceutical industries
as well as more specific risks and uncertainties such as those set forth below
and in its reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities and
Exchange Commission. Given these risks and uncertainties, any or all of these
forward-looking statements may prove to be incorrect. Therefore, you are
cautioned not to place too much reliance on any such factors or forward-looking
statements. Furthermore, Cephalon does not intend (and it is not obligated) to
update publicly any forward-looking statements, whether as a result of new
information, future events or otherwise. This discussion is permitted by the
Private Securities Litigation Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the
company's Web site at http://www.cephalon.com. They are also available by fax
24 hours a day at no charge by calling PR Newswire's Company News On-Call at
800-758-5804, extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Sandra Menta of Cephalon, 610-738-6376
LOAD-DATE: October 1, 1999
LANGUAGE: ENGLISH
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930 of 998 DOCUMENTS
PR Newswire
May 25, 1999, Tuesday - 08:32 Eastern Time
Cephalon Announces Availability of Modafinil in Austria
SECTION: Financial News
LENGTH: 883 words
DATELINE: WEST CHESTER, Pa., May 25
Cephalon, Inc. (Nasdaq: CEPH) today announced the availability of modafinil in
Austria for the treatment of narcolepsy. Modafinil, which is being promoted by
Cephalon in Austria under the tradename MODASOMIL(R), is the first
pharmaceutical product registered in Austria by the Ministry for Work, Health
and Social Issues for treatment of this disorder. Modafinil also is marketed by
Cephalon in the United States, the United Kingdom and Ireland under the
tradename PROVIGIL(R) (modafinil) Tablets C-IV for the treatment of excessive
daytime sleepiness associated with narcolepsy.
Narcolepsy is a chronic, lifelong, neurological sleep disorder that can strike
people of both sexes and all races, with symptoms generally first appearing
during adolescence. The symptoms of narcolepsy include sleep paralysis, sudden
loss of muscle control known as cataplexy, and vivid hallucinations at the onset
of sleep known as hypnagogic hallucinations. The most common and debilitating
symptom of narcolepsy, however, is excessive daytime sleepiness, which is
characterized by uncontrollable sleep attacks that significantly impair a
person's ability to perform basic daily activities.
"The introduction of MODASOMIL is a breakthrough in the treatment of excessive
daytime sleepiness in narcolepsy patients in Austria," stated Univ.- Prof. Dr.
Bernd Saletu, Chairman of the Austrian Sleep Research Association.
Uwe Maschek, Ph.D., Cephalon's country manager, Germany, stated: "We welcome the
opportunity to establish Cephalon's sales and marketing capabilities in Austria,
and look forward to bringing this important new therapy to physicians and their
patients who suffer from this undertreated, disabling sleep disorder."
Cephalon began marketing modafinil (PROVIGIL) in the United States and Ireland
this past February, and has been marketing the product in the United Kingdom
since March 1998. The company received rights from Merckle GmbH to market
modafinil in Austria and in Switzerland, where marketing approval is being
pursued. Cephalon granted rights to Dompe SpA to market modafinil in Italy, and
to Azwell Pharmaceuticals to develop and commercialize the product in Japan.
Cephalon also is pursuing regulatory clearance to market the product in Mexico.
Modafinil is a unique, wake-promoting agent. In landmark clinical trials
involving more than 550 patients with narcolepsy, modafinil was found to be
efficacious in improving daytime wakefulness. Patients also demonstrated
overall clinical improvement in the severity of their disease symptoms.
Modafinil has been found to be generally well-tolerated, with a low incidence of
adverse events relative to placebo. In controlled clinical trials, most adverse
events were mild to moderate. The most commonly observed were headache,
infection, nausea, nervousness, anxiety, and insomnia. No specific symptoms of
withdrawal were observed after discontinuation of therapy.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company dedicated to the discovery, development and
marketing of products to treat neurological disorders, sleep disorders and
cancer.
In addition to historical facts or statements of current condition, this
press release may contain forward-looking statements. Forward-looking
statements provide our current expectations or forecasts of future events.
These may include statements regarding anticipated scientific progress on our
research programs, development of potential pharmaceutical products, prospects
for regulatory approval, manufacturing development and capabilities, market
prospects for our products, sales and earnings projections, and other
statements regarding matters that are not historical facts. You may identify
some of these forward-looking statements by the use of words in the statements
such as "anticipate," "estimate," "expect," "project," "intend," "plan,"
"believe" or other words and terms of similar meaning. Our performance and
financial results could differ materially from those reflected in these
forward-looking statements due to general financial, economic, regulatory and
political conditions affecting the biotechnology and pharmaceutical industries
as well as more specific risks and uncertainties such as those set forth below
and in our reports on Form 8-K, 10-Q and 10-K filed with the U.S. Securities
and Exchange Commission. Given these risks and uncertainties, any or all of
these forward-looking statements may prove to be incorrect. Therefore, you
are cautioned not to place too much reliance on any such factors or forward-
looking statements. Furthermore, we do not intend (and we are not obligated)
to update publicly any forward-looking statements, whether as a result of new
information, future events or otherwise. This discussion is permitted by the
Private Securities Litigation Reform Act of 1995.
NOTE: Cephalon's press releases are posted on the Internet at the
company's Web site at http://www.cephalon.com. They are also available by fax
24 hours a day at no charge by calling PR Newswire's Company News On-Call at
800-758-5804, extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Sandra Menta of Cephalon (U.S.), 610-738-6376, or Carmen Bischof
of Welldone PR (Austria), 011-43-1-402-134-114
LOAD-DATE: May 26, 1999
LANGUAGE: ENGLISH
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931 of 998 DOCUMENTS
Internal Medicine Alert
March 15, 1999
Modafinil for the Treatment of Narcolepsy
LENGTH: 1185 words
Pharmacology Update
Modafinil for the Treatment of Narcolepsy
By William T. Elliott, MD, FACP and James Chan, PharmD, PhD
Cephalon inc. has received approval to market modafinil (Provigil), the first
nonamphetamine drug approved by the FDA for the treatment of excessive daytime
sleepiness associated with narcolepsy. Narcolepsy is a disorder that afflicts
about 125,000 Americans and is characterized by inability to stay awake or alert
in the daytime, sleep attacks, disrupted nocturnal sleep, and cataplexy. Prior
treatment for this disorder has consisted primarily of amphetamine type
drugs-agents that are commonly associated with side effects and eventual
development of tolerance.
While it is known that modafinil is not an amphetamine, the exact mechanism of
action of the drug is not known. It apparently does not appear to bind to
receptors associated with sleep/wake regulation, such as norepinephrine,
serotonin, dopamine, GABA, melatonin, or benzodiazepine.1
Indications
Modafinil is indicated to improve wakefulness in patients with excessive daytime
sleepiness associated with narcolepsy.
Dosage
The recommended dose of modafinil is 200 mg as a single dose in the morning.
There is no consistent evidence that doses greater than 200 mg confer any
additional benefit.1 Patients with severe hepatic impairment should reduce the
dose by half.1 In the elderly population, consideration should be given to use
the lowest effective dose.
Modafinil is supplied as 100 mg and 200 mg tablets. The drug is placed into DEA
Schedule IV.
Potential Advantages
The major advantage of modafinil over other drugs, such as amphetamines and
methylphenidate, used for narcolepsy is its apparent lower abuse potential.
Modafinil is Schedule IV while amphetamine and methylphenidate are Schedule II.
In clinical trials (9 weeks with open label up to 40 weeks), modafinil reduced
daytime sleepiness, was generally well tolerated, did not affect sleep, and
tolerance did not appear to be problematic.1,2,3 The improvement in average
sleep latencies was about 58% based on Maintenance of Wakefulness Test (MWT).
Potential Disadvantages
While modafinil does not appear to have the same abuse potential as amphetamine,
it may produce effects similar to other CNS stimulants such as euphoric effects
and alteration in mood and/or perception. In addition, monkey studies suggest
that modafinil is reinforcing in a manner similar to cocaine.1 Cocaine is one of
the most strongly reinforcing self-administered drugs. A clinical study
suggested that modafinil produced psychoactive and euphoric effects and feelings
consistent with methylphenidate. Patients should be observed for signs of misuse
or abuse.1
Albeit rare, chest pain, palpitations, dyspnea, and transient ischemic T-wave
changes have been observed in association with mitral valve prolapse or left
ventricular hypertrophy. Modafinil is not recommended in patients with a history
of left ventricular or ischemic ECG changes, chest pain, arrhythmia, or
significant manifestations of mitral valve prolapse in association with CNS
stimulants.1
In vitro studies suggest that modafinil has the potential to inhibit cytochrome
P450 2C19, suppress the expression of 2C9, and slightly induce 1A2, 2B6, and
3A4. If coadministration of modafinil and drugs that are substrates for one or
more of these isoenzymes is clinically indicated, the patient should be
monitored for potential toxicity or reduced effectiveness.
In clinical trials, common side effects of modafinil relative to placebo include
headache (50% vs 40%), nausea (13% vs 4%), and diarrhea (8% vs 4%).1 Five
percent of patients discontinue therapy in these trials.
Comments
Modafinil is the first nonamphetamine or non-methylphenidate drug approved for
the treatment of excessive daytime sleepiness associated with narcolepsy.
Effectiveness was established in two U.S. multicenter, placebo-controlled,
double-blind, nine-week trials in more than 550 patients. The primary measures
of efficacy were sleep latency as assessed by the MWT and the change in the
patient's overall disease status, determined by evaluators, as measured by the
Clinical Global Impression of Change (CGI-C). MWT assesses the ability of the
subject to remain awake without using extraordinary measures.
It measures latency (in minutes) to sleep onset averaged over four test sessions
at two-hour intervals. Modafinil improved average sleep latency from 5.07 to
5.35 for placebo to 8.18 to 8.28 for the 200 mg dose. For CGI-C, 58% to 64% of
patients improved compared to 37% to 38% for placebo. There are currently no
comparative trials between modafinil and current agents such as amphetamine or
methylphenidate, and, therefore, comparative efficacy cannot be assessed. A
survey of several agents used to treat narcolepsy suggests that modafinil may be
less effective than dextroamphetamine or methylphenidate based on MWT.4
The wholesale cost of modafinil is about $7 per day for a 200 mg dose.
Clinical Implications
Narcolepsy is a neurologic disorder of unknown cause characterized by excessive
somnolence, cataplexy, sleep paralysis, disrupted nocturnal sleep, and
hypnagogic hallucinations.5 It affects 2-10 individuals per 10,000 and has a
gradual onset between the ages of 15 and 35. Sleep paralysis is a paralysis of
voluntary muscles that occurs at the entry into or emergence from sleep.6
Hypnagogic hallucinations are visual hallucinations with auditory and tactile
components that occur during onset and emergence from sleep.
Cataplexy is a sudden loss of muscle tone (often dropping of the jaw) triggered
by strong emotions such as laughter.6 The symptoms of this condition have
serious personal, social, and economic implications as the ability of the
individual to function in normal daily activity can be significantly
compromised. Excessive daytime sleepiness is generally the most prominent
symptom of narcolepsy. Current pharmacologic treatment includes
dextroamphetamine, methylphenidate, and pemoline. These drugs have potential for
the development of tolerance and unwanted side effects. Modafinil offers an
alternative with milder side effects and may have a lower abuse potential.
Long-term safety and efficacy remains to be established. As with other
stimulants, it does not affect cataplexy, which is generally managed with
tricyclic antidepressants.5,6 Modafinil is only FDA-approved for use in
narcolepsy. Efficacy and safety in improving vigilance in healthy sleep- derived
individuals has not been established. Results from a trial of modafinil in
sleep apnea patients are expected early next year.
References
1. Provigil Product Information. Cephalon, Inc. December 1998.
2. US Modafinil in Narcolepsy Multicenter Study Group. Ann Neurol
1998;43(1):88-97.
3. Broughton RJ, et al. Neurology 1997;49(2):441-451.
4. Mitler MM, et al. Sleep 1991;14(3):218-220.
5. Adams RD, Maurice V, Ropper AH. Sleep and its Abnormalities. In: Principles
of Neurology. 6th ed. McGraw-Hill; 1997:380-402.
6. Fry JM. Sleep Disorders. In: Merritt's Textbook of Neurology. 9th ed. William
& Wilkens; 1995:875-881.
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 1999 AHC Media LLC
All Rights Reserved
932 of 998 DOCUMENTS
The Detroit News
March 14, 1999 Sunday Final Edition
Youth's sleep disorder treated with new drug: New Warren center tries out
Modafinil for the first time
SECTION: METRO; Technician Judy Munro and Ed Shuman of Fraser, who suffers sleep
apnea, demonstrate how electrodes are attached to monitor patients at the Sleep
Disorders Center at Bi-County Community Hospital. Todd McInturf / The Detroit
News; Pg. 5B
LENGTH: 443 words
WARREN -- A Macomb County teen-ager is making medical history, of sorts, at
Bi-County Community Hospital.
The 17-year-old is the first patient at the hospital's new Sleep Disorders
Center -- and possibly in Macomb County -- to receive the new sleep drug,
Modafinil.
Modafinil is used to treat severe cases of the sleep disorder narcolepsy, which
is characterized by sudden overwhelming waves of profound sleepiness. Narcolepsy
sometimes comes after a good night's sleep, said Renee Shimmel, spokeswoman for
Bi-County Hospital in Warren.
The drug went on the market March 1 in Michigan after its approval in January by
the U.S. Food and Drug Administration.
Bi-County's narcolepsy patient "has the most severe case I've ever seen," said
Dr. Leon Rosenthal, director of the Sleep Disorders Center which opened five
weeks ago.
"We're still adjusting the dosage, so it's too early to tell how effective it
will be," Rosenthal said. "Advance studies have been very positive. The drug has
been available in France for many years with good results."
Rosenthal is proceeding cautiously in prescribing Modafinil because of the high
cost of the medication: $3 a pill. Most patients take one pill each day. He
expects the price to drop as Modafinil becomes more popular.
Narcolepsy patients will be on the medication for years, Rosenthal said.
Other symptoms include a sudden loss of muscle control triggered by laughter,
vivid dreams when falling asleep and a temporary sensation of being unable to
move upon going to sleep.
The teen-ager, whose identity was not released, is one of about 25 patients
being treated for various sleep disorders at the new center. More than a dozen
of the patients have spent the night at the center where doctors monitor their
inability to sleep.
"The most prevalent sleep disorder is insomnia," Rosenthal said. "That affects
about one-third of the population. Only 20 percent to 30 percent are easy to
treat. Insomnia is not easy to treat. For about one third it becomes chronic and
is a long-lasting problem and that's when the sleep lab becomes involved."
One of Rosenthal's patients, Amy Ofiara, 24, a graphics designer from Troy, has
been battling narcolepsy for eight years.
"I was falling asleep in class," Ofiara said.
When various tests failed to diagnose her problem, Ofiara overnighted at the
Henry Ford sleep disorders center, and that's when her problem was pinpointed.
Ofiara said that she takes the medication Cylert to help her stay awake and
Vivactil to help her sleep soundly.
Sleep disorders treated by doctors at the Bi-County Community Hospital Sleep
Disorders Center in Warren include:
LOAD-DATE: January 21, 2003
LANGUAGE: ENGLISH
Copyright 1999 The Detroit News
All Rights Reserved
933 of 998 DOCUMENTS
PR Newswire
February 16, 1999, Tuesday - 09:05 Eastern Time
The Narcolepsy Network Welcomes the Introduction of Modafinil for the Treatment
of Narcolepsy;
Availability Provides New Hope For Patients With Debilitating Sleep Disorder
SECTION: Domestic News
LENGTH: 526 words
DATELINE: FAIRFIELD, N.J., Feb. 16
The Narcolepsy Network welcomes the Introduction of Modafinil for the treatment
of excessive daytime sleepiness associated with narcolepsy. Marketed by
Cephalon, Inc. as Provigil it is the first new non-amphetamine treatment in 40
years available to patients for this indication.
"The narcolepsy community has been awaiting the availability of modafinil with
anticipation and hope," says Howard Wolfe, Executive Director of the national
non-profit group, Narcolepsy Network. "For many persons suffering with this
condition, modafinil promises a more normal life both at work and with their
families."
Narcolepsy is a chronic neurological disorder suffered by approx. 1 out of 1000
Americans. The most common symptom is excessive daytime sleepiness (EDS) which
can cause sudden "sleep attacks" that are for the most part, irresistible.
Other key symptoms may include
-- cataplexy -- a sudden loss of muscle control ranging from slight
weakness to total collapse;
-- sleep paralysis -- an inability to talk or move when falling asleep or
waking up;
-- hypnagogic hallucinations -- vivid or frightening dreams and sounds
when falling asleep and;
-- Automatic behavior, performing familiar routines while asleep.
Current treatment for narcolepsy most often includes stimulants to
increase alertness, antidepressants to control cataplexy, and behavior
modifications such as regularly scheduled naps.
Narcolepsy can have a significant impact on a person's daily life, both
personally and professionally. The "sleep attacks" and cataplexy experienced
by many persons with narcolepsy can be embarrassing, disruptive and even
dangerous. In some cases, the symptoms are so severe that the affected
individuals are unable to drive safely or earn a living.
Narcolepsy affects men, woman and children of any age with symptoms
usually appearing after puberty begins. It is not a psychological disorder,
although depression and low self-esteem may occur in persons with narcolepsy
who are untreated, feel misunderstood, or have difficulty coping with their
disorder.
"We urge persons who are suffering with EDS or any other symptoms of
narcolepsy to consult their physician or sleep specialist immediately.
Although there is no cure for narcolepsy, there are treatments available to
minimize the symptoms," said Howard Wolfe.
The Narcolepsy Network is a national non-profit organization founded in
1986. Its members include individuals with narcolepsy, their friends and
family and health professionals. Its goals are to educate the public,
facilitate early diagnosis, encourage research, assist support groups, protect
the rights of those with narcolepsy and to serve as a resource center. For
additional information write or call:
Narcolepsy Network
227 Fairfield Rd., Suite 310B
Fairfield, NJ 07004
973 276-0115
973 227-8224 fax
E-Mail narnet@aol.com
www.websciences.org/narnet
SOURCE The Narcolepsy Network
CONTACT: Howard Wolfe of The Narcolepsy Network, 973-276-0115, or
narnet@aol.com
LOAD-DATE: February 17, 1999
LANGUAGE: ENGLISH
DISTRIBUTION: TO NATIONAL AND MEDICAL EDITORS
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934 of 998 DOCUMENTS
PR Newswire
February 2, 1999, Tuesday - 08:31 Eastern Time
Cephalon Launches PROVIGIL(R) (modafinil) in the Republic of Ireland
SECTION: Financial News
LENGTH: 949 words
DATELINE: WEST CHESTER, Pa., Feb. 2
Cephalon, Inc. (Nasdaq: CEPH) announced today the availability of PROVIGIL(R) (
modafinil) tablets in the Republic of Ireland for the treatment of narcolepsy.
PROVIGIL is the first pharmaceutical product licensed by the Irish Medicines
Board for treatment of this disorder. The company's European subsidiary,
Cephalon U.K. Ltd., which currently markets the drug in the United Kingdom, also
will market PROVIGIL to sleep specialists and neurologists in Ireland.
Narcolepsy is a chronic, neurological, lifelong sleep disorder that generally
begins in young adulthood. Often, 10 to 15 years may pass between onset of
symptoms and proper diagnosis of the disorder. The most common symptom is
excessive daytime sleepiness, which is characterized by uncontrollable sleep
attacks. These attacks impair a person's ability to perform basic daily
activities, significantly impacting their quality of life.
"PROVIGIL is an extremely significant step forward in the treatment of this
disorder," stated Dr. Catherine Crowe, consultant in sleep disorders medicine in
Dublin. "Narcolepsy is a very handicapping condition, which unfortunately is
not well recognized. We know there are many people in Ireland who are living
with narcolepsy but who are currently undiagnosed. PROVIGIL gives us the
opportunity to provide an effective, well-tolerated medical treatment for the
first time. Once a diagnosis is made, we believe it will make a real
difference."
Frank Baldino, Jr., Ph.D., Cephalon's president and chief executive officer,
said, "PROVIGIL is the first licensed agent to be available in Ireland to help
manage this undertreated, disabling disorder. This event reflects Cephalon's
commitment to the PROVIGIL franchise, and more broadly to addressing unmet
medical needs worldwide. We expect to be marketing PROVIGIL in five countries
by the end of this year." Dr. Baldino continued, "We are currently marketing
PROVIGIL in the United Kingdom and we look forward to launching PROVIGIL in the
U.S. later this month."
U.S. clinical trials involving more than 550 patients found PROVIGIL to be
efficacious in improving daytime wakefulness. Patients demonstrated overall
clinical improvement in the severity of their disease symptoms. PROVIGIL has
been found to be generally well-tolerated, with a low incidence of adverse
events relative to placebo. In controlled clinical trials, most adverse events
were mild to moderate. The most frequently reported adverse events that
occurred at a higher rate for PROVIGIL-treated patients than for placebo-
treated patients were headache, infection, nausea, nervousness, anxiety and
insomnia. No specific symptoms of withdrawal were observed after
discontinuation of PROVIGIL therapy.
Cephalon has exclusive rights to market modafinil in the United States, the
United Kingdom, Ireland, Japan, Italy and Mexico. In December 1998, Cephalon
received approval to market PROVIGIL(R) (modafinil) Tablets C IV in the United
States to improve wakefulness in patients with excessive daytime sleepiness
(EDS) associated with narcolepsy and has been marketing the drug in the United
Kingdom since March 1998. The company granted rights to Azwell Inc. to develop
and market modafinil in Japan, and to Dompe Biotech S.p.A., which is currently
pursuing regulatory clearance to promote and distribute the product in Italy.
Cephalon also holds exclusive rights to promote the product in Austria and
Switzerland; commercial launch in Austria is planned for later this year and
approval to market the drug in Switzerland is currently being pursued.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company dedicated to the discovery, development and marketing
of products to treat neurological disorders and cancer.
In addition to historical facts or statements of current condition, this
press release may contain forward-looking statements. Such statements may be
identified by, among other things, the use of forward-looking terminology such
as "believes," or by discussions of strategy or intention, and may include
statements regarding present or anticipated scientific progress, development
of potential pharmaceutical products, manufacturing development and
capabilities, sales and marketing capabilities, and other statements regarding
matters that are not historical facts, or otherwise involve beliefs or
predictions. The company's performance and financial results could differ
materially from those reflected in the forward-looking statements due to
general financial, economic, regulatory and political conditions affecting the
biotechnology and pharmaceutical industries as well as more specific risks and
uncertainties such as those set forth in documents filed by the company with
the SEC (including, but not limited to, its most recent reports on Form 8-K,
Form 10-Q and Form 10-K). Given these risks and uncertainties, any or all of
these forward-looking statements may prove to be incorrect. Therefore,
current or prospective investors are cautioned not to place undue reliance on
any such forward-looking statements. Furthermore, the company has no intent,
and disclaims any obligation, to update any such factors or forward-looking
statements to reflect future events or developments.
NOTE: Cephalon's press releases are posted on the Internet at the
company's Web site at http://www.cephalon.com. They are also available by fax
24 hours a day at no charge by calling PR Newswire's Company News On-Call at
800-758-5804, extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Scott Melville (media), 610-738-6270, or Sandra Menta (investors),
610-738-6376, both of Cephalon, Inc. (U.S.), or Anne Marie Rodriguez of Sante
Communications (Europe), 011-44-1-71-379-7377
LOAD-DATE: February 3, 1999
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 1999 PR Newswire Association, Inc.
935 of 998 DOCUMENTS
NBC News Transcripts
January 27, 1999, Wednesday
SHOW: DATELINE NBC (8:00 PM ET)
WAKE UP CALL; NEW DRUG FOR NARCOLEPSY MAY TEMPT ABUSE FROM NON- NARCOLEPTICS
BYLINE: BOB ARNOT
LENGTH: 1088 words
WAKE UP CALL
Announcer: Here now is Jane Pauley.
JANE PAULEY: In tonight's Healthline, are you exhausted? Millions of Americans
are, but for some the problem is not too little sleep, but having no control
over when they fall asleep. It's a disorder called narcolepsy and it can be
dangerous. But there's a new drug that's giving people who suffer from
narcolepsy new hope of living a normal life. Here's chief medical correspondent
Dr. Bob Arnot.
BOB ARNOT reporting: (Voiceover) It's a feeling most of us have learned to
dread. It's late, the lines of the road blur past, our eyelids heavy, we fight
to resist sleep and stay awake on the road. Now imagine feeling this way,
struggling against sleepiness 16, 18, even 20 hours a day. Welcome to the world
of the narcoleptic.
(Blurred view of driving down road; clock; patient in hospital bed)
Ms. MARIE SIMMONS: You're fighting to stay awake, but you're being pulled into,
kind of, quicksand. It's a pull that's stronger than you.
ARNOT: (Voiceover) For Marie Simmons, the need for sleep had been constant, a
need that hits narcoleptics any time of day and can last nearly all day.
(Maria Simmons stretching; Simmons working out)
Ms. SIMMONS: (Voiceover) I've fallen asleep eating dinner in a restaurant...
(Simmons working out)
Ms. SIMMONS: ...even at the gym while in the process of exercising.
ARNOT: (Voiceover) Marie's fatigue got so bad, a nine-to-five job was out of the
question. She went to work at home as a therapist. But even then, she had to
fight to conceal her secret.
(Simmons hugging man and leaving)
Ms. SIMMONS: I fell asleep while seeing a client, and that really scared me.
ARNOT: (Voiceover) This is what the disease can look like, in dogs studied at
Stanford University, Pluto is a normal, healthy, Doberman pinscher, except for
one thing--bring out his favorite toy, and instead of playing, Pluto collapses,
awake, but completely paralyzed. It's the same thing you and I experience in
the middle of deep sleep, but for Pluto and this dachshund named Bo, the
slightest excitement triggers an attack. The roots of narcolepsy lie deep in
the brain, where special cells control our sleep. Every morning, those cells
sound an alarm that keeps us awake throughout the day. In narcoleptics, the
signal is too weak, causing sudden and unpredictable attacks of sleepiness.
Until now, treatment meant amphetamine type drugs, Marie tried those, but they
made her jumpy and anxious.
(Researcher playing with Pluto; Pluto paralyzed; Bo paralyzed; diagram of brian
indicating normal alarm and weakened alarm in narcoleptic; pills)
Ms. SIMMONS: (Voiceover) Although I was more alert...
(Pills being dropped into pan)
Ms. SIMMONS: ...the cure was almost as bad as the disease.
Dr. JED BLACK: A lot of our patients are not able to work and have to be on
disability because of the sleepiness.
ARNOT: (Voiceover) Dr. Jed Black is Marie's doctor and runs the sleep lab at
Stanford University.
(Jed Black; Black talking to researcher)
Dr. BLACK: (To researcher) Has he fallen asleep on any of his naps?
ARNOT: (Voiceover) He told her about a revolutionary new drug called modafinil,
a drug that promised to push back the night for her and many of the estimated
125,000 Americans with narcolepsy. Four years ago, she became one of the first
in the US to try the drug as part of a clinical trial
(Black pointing to medical chart; Simmons opening modafinil bottle; modafinil
bottle; pill; bottle of modafinil)
ARNOT: Modafinil works differently from any drug before it. Unlike stimulants,
modafinil appears to work by turning up the volume on those so-called alarm
cells in the brain, without any of the jitteriness and nervousness caused by
amphetamines.
(Voiceover) After nearly giving up hope of a normal life, Marie was anxious for
anything that would help. She didn't have to wait long. She still remembers
the very first dose.
(Simmons working out)
Ms. SIMMONS: You know, it was like I was sleepwalking and I just woke up.
ARNOT: (Voiceover) Dr. Black admits Marie's response was the most dramatic he
saw. But he says half the patients he studied responded as well or better to
modafinil as they had to stimulants. The drug is already approved for
narcoleptics in some European countries, where it is tightly controlled. But in
the US, FDA approval means doctors could prescribe it to anyone, so-called
off-label use. That has Dr. Black and others worried about potential abuse of
Modafinil by non-narcoleptics. It's not tough to see how millions of busy people
might find a pill that allows you to go days without sleep hard to resist.
(Empty hospital bed; medical chart; pillow; patient in hospital bed; modafinil
bottle; pills; modafinil bottle; people sleeping)
Dr. BLACK: (Voiceover) It's potentially going to happen.
(Modafinil bottle)
Dr. BLACK: People will be feeling pressured to use this to--to stay awake
to--to--to be more productive.
ARNOT: (Voiceover) What happens when healthy people take the drug? Well, just
such a study was done in 1994 by the Canadian military, which was looking for
ways to fight fatigue on the battle field. You're looking at lab video from
that first experiment. When a small group of Canadian soldiers took modafinil,
they managed to stay awake for 64 hours. All the while performing repetitive
tasks on a computer. Most surprising of all, after the study, the volunteers
seemed perfectly fine. It was as if they hadn't lost any sleep at all. A
remarkable result, but one that only heightened fears of abuse. But for Marie
Simmons, the benefits are clear. Modafinil allowed her the ability to return to
full time work as a nurse. And four years after beginning treatment, she still
thinks about the little pill that made such a big difference.
(Soldiers; soldiers walking; soldier looking through binoculars; soldier on
telephone; lab video showing man working at desk; lab video showing two men
looking at computer screens; lab video showing man sitting at computer; lab
video showing man working at desk; lab video showing two men leaving computers;
Simmons working out; Simmons leaving work out)
Ms. SIMMONS: It was like having a second life. It was wonderful to be able to
do the many things that I was still interested in but I had just withdrawn from.
PAULEY: So, what are the worries about this drug? Doctors say the fundamental
concern is that people will be tempted to use this drug instead of sleep. They
stress that no drug can ever replace sleep, which is beneficial in many ways we
understand and many ways we don't.
Announcer: Coming up--he helped police when he identified a murder suspect. Did
his courage cost him his life?
Mr. CARLOS COLLAZO: If he wouldn't have picked out a photo, I believe he would
have still been here with us, swimming, you know, playing basketball.
Announcer: Who was looking out for B.J. Brown?
Plus--whose fault is it that the president and Monica are still on our minds?
It's DATELINE's Question of the Week.
(Announcements)
Announcer: DATELINE NBC, winner for the last two years of top honors from the
Investigative Reporters and Editors awards. The years most honored
newsmagazine, DATELINE, will be right back.
(Announcements)
LOAD-DATE: January 28, 1999
LANGUAGE: English
TYPE: Profile
Copyright 1999 National Broadcasting Co. Inc.
936 of 998 DOCUMENTS
U.S. Newswire
January 12, 1999 8:57 Eastern Time
New Excessive Daytime Sleepiness Treatment Brings Hope of Reaching Undiagnosed
SECTION: NATIONAL DESK, MEDICAL WRITER
LENGTH: 1473 words
DATELINE: WASHINGTON, Dec. 12
The recent announcement that a new wake-promoting medication, modafinil, will
soon be available to consumers has triggered public discussion about potential
"off-label" uses.
Approved by the Food and Drug Administration (FDA) Dec. 28 for the treatment
of excessive daytime sleepiness (EDS) associated with narcolepsy, modafinil is
considered to be a novel therapy. It is being marketed in the United States by
Cephalon Inc. (Nasdaq: CEPH), as Provigil.
Millions of Americans experience daytime sleepiness, but only a fraction
suffer from narcolepsy. According to a 1998 National Sleep Foundation (NSF)
survey, thirty-seven percent of Americans report being so sleepy during the day
that their fatigue interferes with daily activities. Daytime sleepiness has
numerous causes; it is most frequently the result of sleep deprivation. For
example, in the same survey, one-third of Americans reported getting six or
fewer hours of sleep per night during the work week, in spite of the fact that
the average person needs eight hours of sleep.
"Excessive daytime sleepiness (EDS) for any reason is a cause for concern,"
said NSF President Lorraine Wearley, Ph.D. "At this time, however, we must focus
our concerns on helping the estimated 200,000 Americans who have narcolepsy.
This is a chronic, neurological condition that can be extremely debilitating if
left untreated."
Wearley urged that discussions about use of modafinil maintain a clear
distinction between EDS related to narcolepsy and EDS caused by other condition
s or as a side effect of medications, which can often be helped significantly
through lifestyle changes or other treatments.
As Common as MS, But Only 25 Percent Diagnosed
The National Center on Sleep Disorders Research, part of the National
Institutes of Health, estimates that only 50,000 of the estimated 200,000
Americans with narcolepsy -- as few as one in four -- have been diagnosed.
Narcolepsy, therefore, is considered to be at least as common as multiple
sclerosis or Parkinson s disease, but is by far less well known.
"The interest in this new medication provides an opportunity to help
individuals and their family members better understand narcolepsy," Wearley
added, "and to encourage people to discuss with their physician any symptoms
they might be experiencing."
The most common symptom of narcolepsy is EDS, specifically, a feeling of
overwhelming sleepiness during the daytime, even after a full night's rest.
Other symptoms may include:
-- cataplexy, a sudden loss of muscle control ranging from slight weakness
to total collapse, which is typically triggered by a strong emotion or laughter;
-- sleep paralysis, a temporary sensation of being unable to talk or move
upon falling asleep or waking up; and
-- hypnagogic or hypnopompic hallucinations, vivid and often frightening
dreams or sensations experienced when falling asleep or upon awakening.
Diagnosis is complicated by the fact that these symptoms differ in age of
onset and severity among people with narcolepsy, and they can be experienced
independently of narcolepsy. Furthermore, most narcoleptics do not experience
all of these symptoms. For example, cataplexy was once considered a hallmark of
the disease, but researchers now recognize that individuals with narcolepsy may
experience no or very slight episodes of this symptom.
"The popular perception of narcolepsy among those who have heard or seen
anything about the disease in general, is that of a cataplectic or very sudden
sleep attack," Wearley commented. "Although these are indeed common symptoms, a
person does not need to have a full body collapse or even bang their head onto a
table during an attack to have narcolepsy."
Diagnosis Often Takes Years, Several Consultations
Proper diagnosis of narcolepsy requires a careful medical history and
laboratory testing, usually given under the direction of a sleep specialist.
However, many individuals are reluctant to talk with their health care providers
about their symptoms -- and therefore possibly delay diagnosis -- because they
believe that nearly all sleep problems are psychological in nature. Or, they may
fear that their concerns might be misunderstood or will not be taken seriously.
Unfortunately, these concerns are not unfounded. Many narcoleptic patients
were previously misdiagnosed with psychiatric problems or told that their
sleepiness was due to the effect of an unrelated medication. Patients and
health professionals need to persistently evaluate the individual's symptoms,
their cause, and how they are affected by recommended treatments.
The National Commission on Sleep Disorders reported in 1992 that, on
average, patients had to consult five physicians before being diagnosed with
narcolepsy. In addition, the mean length of time between the onset of symptoms
and the diagnosis of narcolepsy is 15 years.
"This is our frustration and our challenge," said Wearley. "We have an
effective new treatment, but the reality is that many clinicians are unable to
identify and diagnose narcolepsy, and patients end up losing their jobs,
relationships, and other important elements of their lives instead of receiving
the treatment they need."
Treatment Options
Medications to help alleviate excessive daytime sleepiness play a central
role in helping narcoleptics cope and lead a more "normal" life. In addition,
depending on the patient s symptoms, medications to help control other symptoms,
such as cataplexy, might also be needed. Finally, behavioral techniques, such as
daytime naps, may help some patients as an adjunctive therapy.
Scientists have not yet identified the precise pharmacological process that
occur with the use of modafinil. However, they agree that the new drug is
distinct from but has similar "wake-promoting actions" as other central nervous
system (CNS) stimulants used to reduce the effects of excessive daytime
sleepiness in narcoleptics, according to FDA-approved product labeling. U.S.
clinical trials also demonstrated that modafinil is less likely to cause
nervousness or withdrawal-like symptoms than other wake- promoting medications.
The studies confirmed findings from longer-term use of the medication in France.
Modafinil is expected to be available in mid-February. The Drug Enforcement
Agency has recommended that it be classified as a schedule IV medication.
Modafinil therefore may be more readily accessible to patients than most
similarly prescribed stimulants, such as amphetamines, which are registered as
schedule II medications. For example, patients may be able to purchase modafinil
after their provider calls in a prescription to a pharmacy; for schedule II
medications, patients must personally deliver a hand-signed prescription to the
pharmacy before it can be filled.
------
For more information about narcolepsy and how to locate a local sleep
center, visit the Web site of the National Sleep Foundation (NSF) at www.
sleepfoundation.org, or call 202-347-3471. Request a brochure about narcolepsy
by sending a self-addressed, stamped ($.55) envelope to NSF, 729 Fifteenth
Street, N.W., Washington, D.C., 20005. to participate in NSF's National
Narcolepsy Registry, a confidential and voluntary database of genetic
information from individuals diagnosed with narcolepsy and their families.
Scientific evidence suggests that genetics play a key role in the onset of this
condition. Thus, the registry was developed to help researchers find the cause
of narcolepsy and to enhance their understanding of the genetics of sleep in
general.
Another resource for people with narcolepsy is the Narcolepsy Network, a
self-help organization. The organization can be contacted at 277 Fairfield
Ave., Suite 310B, Fairfield, N.J., 07004 or by calling 973-276-0115.
------
Founded in 1990, the National Sleep Foundation (NSF) is an independent,
nonprofit organization that promotes public understanding of sleep and sleep
disorders, and supports sleep-related research and education and advocacy to
improve public health and safety.
------
Note to Editors: The National Sleep Foundation is able to provide additional
background information on narcolepsy, sleep disorders and sleep deprivation, and
related issues. Contact with sleep experts nationwide can also be arranged. Call
202-347-3471 for assistance.
------
Editors: Some computer systems do not recognize the "at" sign. It is an
important component of e-mail addresses and should be used in place of the
symbol (At) in the contact information above.
LOAD-DATE: January 12, 1999
LANGUAGE: ENGLISH
Copyright 1999 PR Newswire Association LLC
All Rights Reserved
937 of 998 DOCUMENTS
The Lancet
Lancet 1999; 353 (9147): 131
January 9, 1999
FDA approves first new narcolepsy drug in USA in decades
AUTHOR: Ault, Alicia
SECTION: News: Policy and People
LENGTH: 274 words
Just before the new year, the US FDA approved the first new therapy for
narcolepsy in 40 years-Cephalon's (West Chester, Pennsylvania, USA) modafinil
(Provigil). About 125 000 Americans have narcolepsy, which is marked by
persistent drowsiness and sudden attacks of sleepiness.
Modafinil is not an amphetamine, but promotes wakefulness. "It really is, to
our knowledge, the first selective wake promoting agent," says Cephalon senior
director of pharmacology Matt Miller. The drug's mechanism of action is not well
understood, but in cat studies, it worked discretely in the hypothalamus, says
Miller.
Modafinil was discovered by the French pharmaceutical company Laboratoire L
Lafon and is already approved in France, the UK, and Ireland. Unlike
conventional stimulants used to treat narcolepsy, modafinil does not cause
withdrawal. It does not work through dopamine or bind to other relevant
receptors for sleep-wake regulation, so there is no hyperactivity and minimal
cardiovascular effects, says Miller.
Even so, because it works in the brain, the US Drug Enforcement
Administration will put modafinil on its list of controlled substances. In
trials, patients taking once-daily doses of modafinil had a statistically
significantly greater ability to stay awake, and an improvement in symptom
severity. Patients rated themselves as having less propensity to fall asleep
during the day. The drug did not affect night-time sleep, said Cephalon. But the
company added that insomnia was a common adverse event. Other side-effects
included headache, infection, nausea, nervousness, and anxiety. A 200 mg daily
dose was approved.
LANGUAGE: ENGLISH
Copyright 1999 by The Lancet Ltd
938 of 998 DOCUMENTS
Austin American-Statesman (Texas)
December 29, 1998
Narcolepsy drug gets FDA approval with restrictions
BYLINE: By Rick Weiss
SECTION: News; Pg. A7
LENGTH: 370 words
WASHINGTON -- The Food and Drug Administration has approved a drug that keeps
people with debilitating sleepiness awake and attentive yet has few of the side
effects associated with caffeine, amphetamines and other commonly used
stimulants.
The drug, modafinil, was approved by the FDA for people with a serious sleep
disorder called narcolepsy, which affects one out of 1,000 to 2,000 people and
is characterized by sudden, overwhelming waves of intense sleepiness.
It will be available only by prescription, under the brand name Provigil, and
will be listed by the Drug Enforcement Administration as a "schedule IV"
substance, which means it will be regulated more tightly than most prescription
drugs.
Despite those restrictions, several experts said they would not be surprised if
the pills quickly gain popularity among some of the millions of people in this
country who suffer from daytime sleepiness caused by problems more mundane than
narcolepsy, such as overwork and stress-related insomnia.
The drug may find a "gray market" among truck drivers, emergency room doctors,
soldiers in battle, college students and others whose jobs demand that they
remain alert for days with little or no sleep. Preliminary studies on Canadian
soldiers found that modafinil increased wakefulness and vigilance in those who
went without sleep for almost three days, without the agitation or the "rebound"
fatigue that typically follows long stretches of amphetamine-induced
wakefulness.
No one knows yet whether modafinil is safe or effective for the vast majority of
the world's fatigued. But clues may arise long before clinical trials are
devised to study the question.
Doctors who are licensed to prescribe scheduled drugs are allowed to prescribe
those drugs for patients who do not have the disorder for which the FDA approved
them. But they must be able to justify to federal officials their reasoning for
writing such "off-label" prescriptions.
Experts said only time would tell whether doctors will feel comfortable
prescribing modafinil to sleepy, non-narcoleptics. If the DEA determines that
the drug is being overprescribed or abused, the agency can reschedule it to a
more restrictive level.
LOAD-DATE: January 7, 1999
LANGUAGE: ENGLISH
Copyright 1998 The Austin American-Statesman
939 of 998 DOCUMENTS
Portland Press Herald (Maine)
December 29, 1998, Tuesday,
Narcolepsy drug gets FDA nod, with limits;
The drug is only approved for people with this serious sleep disorder, but many
believe it will be used more widely.
BYLINE: The Washington Post
SECTION: FRONT, Pg. 3A
LENGTH: 637 words
DATELINE: WASHINGTON
The Food and Drug Administration (FDA) has approved a novel drug that keeps
people with debilitating sleepiness awake and attentive yet has few of the side
effects associated with caffeine, amphetamines and other commonly used
stimulants.
The drug, modafinil, was approved by the FDA for people with a serious sleep
disorder called narcolepsy, which affects 1 out of 1,000 to 2,000 people and is
characterized by sudden, overwhelming waves of intense sleepiness.
It will be available only by prescription, under the brand name Provigil, and
will be listed by the Drug Enforcement Administration (DEA) as a "schedule IV"
substance, which means it will be regulated more tightly than most prescription
drugs.
Despite those restrictions, several experts said they would not be surprised if
the pills quickly gained popularity among some of the millions of people in this
country who suffer from daytime sleepiness caused by problems more mundane than
narcolepsy, such as overwork and stress-related insomnia.
The drug may also find a "gray market" following among truck drivers, emergency
room doctors, soldiers in battle, college students and others whose jobs demand
them to remain alert for days on end with little or no sleep. Preliminary
studies on Canadian soldiers found that modafinil increased wakefulness and
vigilance in soldiers who went without sleep for almost three days, without the
agitation or the "rebound" fatigue that typically follows long stretches of
amphetamine-induced wakefulness.
No one knows yet whether modafinil is safe or effective for the vast majority of
the world's fatigued. But clues may arise long before clinical trials are
devised to study the question.
Doctors who are licensed to prescribe scheduled drugs are allowed to prescribe
those drugs for patients who do not have the disorder for which the FDA approved
them. But they must be able to justify to federal officials their reasoning for
writing such "off-label" prescriptions.
Experts said only time would tell whether doctors will feel comfortable
prescribing modafinil to sleepy, non-narcoleptics. If the DEA determines that
the drug is being overprescribed or abused, the agency can reschedule it to a
more restrictive level.
Frank Baldino, president of West Chester, Pa.-based Cephalon, Inc., which will
market modafinil, emphasized that the drug has been proven safe and effective
only in narcoleptics.
But he acknowledged that the company is pursuing research to test the drug's
usefulness for other sleep-related disorders, including sleep apnea, a nighttime
breathing disorder that disrupts sleep in an estimated 12 million Americans. And
he said the company has been negotiating with branches of the U.S. armed forces
to set up clinical tests of the drug's value in combat situations.
The company announced modafinil's approval Monday, after getting word from the
FDA on Dec. 24. Its stock jumped 12 percent, rising $ 1 to close at $ 9.18 3/4
on the Nasdaq Stock Exchange.
Although scientists still don't know how modafinil works, it appears to interact
much more specifically with the brain's sleep-wake centers than do other
wakefulness-inducing drugs, such as amphetamines, which have many undesirable
side effects.
"The amphetamines are a problem because you get a little overactivated," said
Emmanuel Mignot, an associate professor of psychiatry and director of the center
for narcolepsy at Stanford University. "There is a time when it overshoots and
people get a little speedy and irritable and after that they crash."
Modafinil, Mignon said, is much better tolerated. "It is much smoother and
milder. They feel awake without feeling overagitated, and there is no effect on
the cardiovascular system that we can tell."
The drug is expected to become available in February.
LOAD-DATE: October 29, 1999
LANGUAGE: ENGLISH
Copyright 1998 Blethen Maine Newspapers, Inc.
940 of 998 DOCUMENTS
Reuters Health Medical News
December 29, 1998 Tuesday
FDA grants approval of first nonamphetamine for treatment of narcolepsy
SECTION: REGULATORY
LENGTH: 366 words
DATELINE: WESTPORT Dec 29
Cephalon, of West Chester, PA, received its first US approval late last week,
when the Food and Drug Administration granted approval of modafinil (Provigil)
for treatment of narcolepsy. This is the first nonamphetamine approved for use
in this condition.
Modafinil's mechanism of action is "not well understood," Dr. Russell Rosenberg
of Northside Hospital in Atlanta told Reuters Health. "It's a wake-promoting
agent, it works on that part of the brain." It does not work along the same
pathways as amphetamines, he added.
FDA granted approval based on results of two phase III trials that involved more
than 550 patients with narcolepsy who received either modafinil or placebo. Dr.
Rosenberg was an investigator with the first of those.
Dr. Rosenberg said that modafinil lacks the adverse effects often seen with
amphetamines, such as jitteriness, anxiety and heart palpitations. The new drug
also does not cause hepatotoxicity, which can occur with amphetamine use. "It's
a unique drug. It will offer a great advantage for patients with narcolepsy,"
Dr. Rosenberg commented.
According to Cephalon, 5% of patients who were part of the drug's clinical
studies had to discontinue therapy due to adverse events. Company spokesmen
said that most of the adverse events, which included headache, infection,
nausea, nervousness, anxiety and insomnia, were mild to moderate in severity.
The FDA approval is for the once-daily 200 mg dose of modafinil. According to a
company press release posted on PR Newswire, the company expects the agent to be
classified as a Schedule IV controlled substance.
According to the DEA, a Schedule IV drug is one that "...has a low potential for
abuse relative to the drugs or other substances in Schedule III," which are
drugs that might lead to moderate or low physical dependence or high
psychological dependence. Other Schedule IV drugs include Xanax and Valium.
Off-label uses of modafinil may include treatment of excessive daytime
sleepiness and other symptoms of sleep disorders, according to Dr. Rosenberg.
"We're just scratching the surface of the population at risk," he said.
Cephalon's shares climbed 1-1/8 to 9-5/16 in mid-afternoon trading on Monday.
LOAD-DATE: July 9, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 1998 Reuters Health
All Rights Reserved
941 of 998 DOCUMENTS
The Washington Post
December 29, 1998, Tuesday, Final Edition
Narcolepsy Drug Wins Approval Of FDA; Regulators on Alert For 'Off-Label' Use
Rick Weiss, Washington Post Staff Writer
SECTION: A SECTION; Pg. A01
LENGTH: 1000 words
The Food and Drug Administration has approved a novel drug that keeps people
with debilitating sleepiness awake and attentive yet has very few of the side
effects associated with caffeine, amphetamines and other commonly used
stimulants.
The drug, modafinil, was approved by the FDA for people with a serious sleep
disorder called narcolepsy, which affects at least one in every 2,000 people and
is characterized by sudden, overwhelming waves of intense sleepiness.
It will be available only by prescription, under the brand name Provigil, and
will be listed by the Drug Enforcement Administration (DEA) as a "schedule IV"
substance, which means it will be regulated more tightly than most prescription
drugs.
Despite those restrictions, several experts said they would not be surprised if
the pills quickly gained popularity among some of the millions of people in this
country who suffer from daytime sleepiness caused by problems more mundane than
narcolepsy, such as overwork and stress-related insomnia.
The drug may also find a "gray market" following among truck drivers, emergency
room doctors, soldiers in battle, college students and others whose jobs demand
that they remain alert for days on end with little or no sleep. Preliminary
studies on Canadian soldiers found that modafinil increased wakefulness and
vigilance in those who went without sleep for almost three days, without the
agitation or the "rebound" fatigue that typically follows long stretches of
amphetamine-induced wakefulness.
No one knows yet whether modafinil is safe or effective for the vast majority of
the world's fatigued. But clues may emerge long before clinical trials are
devised to study the question.
Doctors who are licensed to prescribe scheduled drugs are allowed to prescribe
those drugs for patients who do not have the disorder for which the FDA approved
them. But they must be able to justify to federal officials their reasoning for
writing such "off-label" prescriptions.
Experts said only time would tell whether doctors will feel comfortable
prescribing modafinil to sleepy, non-narcoleptic people. If the DEA determines
that the drug is being overprescribed or abused, the agency can reschedule it to
a more restrictive level.
Frank Baldino, president of West Chester, Pa.-based Cephalon, Inc., which will
market modafinil, emphasized that the drug has been proven safe and effective
only in narcoleptics.
But he acknowledged that the company is pursuing research to test the drug's
usefulness for other sleep-related disorders, including sleep apnea, a nighttime
breathing disorder that disrupts sleep in an estimated 12 million Americans. And
he said the company has been negotiating with branches of the U.S. armed forces
to set up clinical tests of the drug's value in combat situations.
The company announced modafinil's approval yesterday, after getting word from
the FDA on Dec. 24. Its stock jumped 12 percent, rising $ 1 to close at $ 9.18
3/4 on the Nasdaq Stock Market.
Modafinil was discovered by French researchers many years ago and has been
approved in France since 1994, where it is sold under more restrictive
conditions than it will be in the United States.
Cephalon, which holds the license to market the drug in the United States and
seven European countries, conducted additional clinical trials involving 550
people at 39 medical centers in the United States to gain the FDA's approval.
Although scientists still don't know how modafinil works, it appears to interact
much more specifically with the brain's sleep-wake centers than do other
wakefulness-inducing drugs, such as amphetamines, which have a panoply of
effects on the brain, the heart and other organs and so have many undesirable
side effects.
Especially problematic, amphetamines influence dopamine centers in the brain,
which are involved in craving and addiction, explaining in part why those drugs
are so often abused.
"The amphetamines are a problem because you get a little overactivated," said
Emmanuel Mignot, an associate professor of psychiatry and director of the center
for narcolepsy at Stanford University. "There is a time when it overshoots and
people get a little speedy and irritable and after that they crash."
Modafinil, Mignon said, is much better tolerated. "It is much smoother and
milder. They feel awake without feeling overagitated, and there is no effect on
the cardiovascular system that we can tell."
Merrill M. Mitler, a professor in the department of neuropharmacology at Scripps
Research Institute in La Jolla, Calif., said he was very excited about the
drug's approval for narcolepsy, which he described as "a miserable disorder."
"They've been relegated to using drugs that have been developed for other
conditions like obesity and attention deficit disorder," Mitler said, adding
that most of those drugs are "schedule II" compounds that can only be prescribed
in person in a doctor's office. "Provigil has been developed for narcoleptics
with their needs in mind, and can be prescribed by telephone to the pharmacist,
which is much more convenient for the patient."
In Cephalon's studies, about 60 percent of patients who took 200 milligrams of
modafinil daily for nine weeks showed a significant decline in symptoms. These
included general daytime sleepiness, the tendency to suddenly fall asleep
without warning, sleep paralysis (in which the mind is awake but the body is
paralyzed as if asleep), and catalexy (a peculiar symptom of narcolepsy in which
a paralytic, sleep-like state is triggered by laughter or other emotional
events).
By contrast, about 37 percent of those who took inactive placebos improved. The
trials did not directly compare modafinil against amphetamines. But side effects
from modafinil -- mostly headaches, infection, nausea, nervousness, anxiety and
insomnia -- were less common and less severe than typically seen with
amphetamines.
The drug is expected to become available in February.
LOAD-DATE: December 29, 1998
LANGUAGE: ENGLISH
Copyright 1998 The Washington Post
942 of 998 DOCUMENTS
PR Newswire
December 28, 1998, Monday - 17:39 Eastern Time
The National Sleep Foundation Welcomes FDA Approval of Modafinil For the
Treatment of Narcolepsy.
SECTION: Washington Dateline
LENGTH: 371 words
DATELINE: WASHINGTON, Dec. 28
The National Sleep Foundation (NSF) welcomes the Food and Drug Administration
(FDA) approval of modafinil, a new treatment for persons with narcolepsy, a
serious neurological sleep disorder that affects an estimated 200,000 Americans.
This chronic sleep disorder, with no known cause, is often disabling and is
characterized by excessive daytime sleepiness, cataplexy (a sudden loss of
muscle tone triggered by strong emotion), sleep paralysis upon falling asleep or
awakening, and hypnagogic hallucinations (vivid dreams upon falling asleep).
"We are exceedingly pleased that a new treatment option will soon be available
for people who suffer from narcolepsy," said Lorraine L. Wearley, Ph.D., NSF
President. "Modafinil represents the first new non-amphetamine drug in 40 years
to be designed for excessive daytime sleepiness associated with narcolepsy."
Modafinil is being marketed by Cephalon, Inc. as Provigil(R). It will be
available in tablet form by prescription after final scheduling by the U.S. Drug
Enforcement Administration.
Founded in 1990, the National Sleep Foundation is an independent, nonprofit
organization that promotes public understanding of sleep and sleep disorders,
and supports sleep-related education, research and advocacy to improve public
health and safety. NSF publishes public education brochures and a professional
newsletter on narcolepsy. In addition, NSF supports the National Narcolepsy
Registry, a confidential and voluntary database of genetic information from
individuals diagnosed with narcolepsy and their families. Scientific evidence
suggests that genetics play a key role in the onset of this condition. Thus,
the registry was developed to help researchers find the cause of narcolepsy and
to enhance their understanding of the genetics of sleep in general.
For more information or to receive a brochure about narcolepsy, the registry, or
other sleep disorders, please call 202-347-3471, fax 202-347-3472 or visit the
NSF Web site at www.sleepfoundation.org.
SOURCE National Sleep Foundation
CONTACT: National Sleep Foundation, 202-347-3471; Pat Britz, ext. 203, or
Susan Sagusti, ext. 208; e-mail, natsleep@erols.com
LOAD-DATE: December 29, 1998
LANGUAGE: ENGLISH
DISTRIBUTION: TO HEALTH/MEDICAL EDITOR
Copyright 1998 PR Newswire Association, Inc.
943 of 998 DOCUMENTS
Reuters Health eLine News
December 28, 1998 Monday
FDA approves narcolepsy drug
LENGTH: 266 words
DATELINE: NEW YORK Dec 28
Cephalon, Inc., of West Chester, Pennsylvania, received its first US approval
late last week, when the Food and Drug Administration (FDA) granted approval of
modafinil (Provigil) for the treatment of narcolepsy. This is the first
non-amphetamine approved for use in narcolepsy -- an illness characterized by
sudden, uncontrollable sleep attacks.
Modafinil's mechanism of action is "not well-understood," investigator Russell
Rosenberg of Northside Hospital in Atlanta, Georgia, told Reuters Health. "It's
a wake-promoting agent, it works on that part of the brain." It does not work
along the same pathways as amphetamines, he added.
FDA granted approval based on results of two trials that involved more than 550
patients with narcolepsy who received modafinil or (an inactive) placebo.
Rosenberg was an investigator on the first of those trials.
He said that modafinil is not associated with the adverse effects that
amphetamines often cause, such as jitteriness, anxiety and heart palpitations.
The new drug does not promote the liver toxicity that can occur with amphetamine
use. "It's a unique drug. It will offer a great advantage for patients with
narcolepsy," Rosenberg commented.
Other uses of modafinil not yet approved by the FDA may include treatment of
excessive daytime sleepiness and other symptoms of sleep disorders. "We're just
scratching the surface of the population at risk," he said.
The most common side effects of the drug are headache, infection, nausea,
nervousness, anxiety and insomnia. Modafinil is not recommended for use in
individuals with certain types of heart problems.
LOAD-DATE: July 23, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 1998 Reuters Health
All Rights Reserved
944 of 998 DOCUMENTS
PR Newswire
December 3, 1998, Thursday - 08:34 Eastern Time
Cephalon to Promote Modafinil in Austria and Switzerland.
SECTION: Financial News
LENGTH: 777 words
DATELINE: WEST CHESTER, Pa., Dec. 3
Cephalon, Inc. (Nasdaq: CEPH) announced today that its U.K. subsidiary, Cephalon
UK Ltd., has gained exclusive rights from Merckle GmbH to promote modafinil in
Austria and Switzerland. Financial terms of this ten-year agreement were not
disclosed. Cephalon already has exclusive rights to market and sell modafinil in
the United States, the United Kingdom, Ireland, Japan, Italy and Mexico.
Modafinil is approved to be marketed in Austria and launch is planned for early
next year. Approval to market modafinil in Switzerland is currently being
pursued. Cephalon will promote modafinil in these territories to neurology and
psychiatry specialists who treat patients suffering from narcolepsy. Narcolepsy
is a chronic, lifelong sleep disorder commonly characterized by excessive
daytime sleepiness or uncontrollable sleep attacks that can hamper a person's
ability to perform basic daily activities.
"Our agreement with Merckle allows us not only to capitalize on our investment
in this important product, but broadens our efforts in increasing awareness of,
and offering a new treatment for, a disabling disease that is currently managed
by few or inadequate therapies," stated Uwe Maschek, Ph.D., Cephalon's country
manager, Germany.
In clinical trials, modafinil has been shown to be effective in promoting
daytime wakefulness, and well tolerated with low abuse potential. The most
commonly observed adverse experiences with modafinil, which occurred more
frequently than placebo, were headache, nausea and diarrhea.
Cephalon licensed rights to modafinil from Laboratoire L. Lafon, the French
pharmaceutical company which discovered the drug and markets it in France.
Cephalon has received market authorization for modafinil in the United Kingdom
and the Republic of Ireland. The company is currently marketing modafinil in
the United Kingdom for the treatment of narcolepsy and will launch the product
in Ireland early next year. Cephalon has received an approvable letter for
modafinil from the U.S. Food and Drug Administration and also is pursuing
regulatory clearance to market the drug in Mexico. The company granted rights
to AZWELL Inc. (a newly formed entity of Nippon Shoji Kaishi Ltd. and Showa
Pharmaceutical Co., Ltd.) to develop and market modafinil in Japan, and to Dompe
Biotech S.p.A. who is currently pursuing regulatory clearance to promote and
distribute the product in Italy.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company dedicated to the discovery, development and marketing
of products to treat neurological disorders and cancer.
In addition to historical facts or statements of current condition, this press
release may contain forward-looking statements. Such statements may be
identified by, among other things, the use of forward-looking terminology such
as "believes," or by discussions of strategy or intention, and may include
statements regarding present or anticipated scientific progress, development of
potential pharmaceutical products, manufacturing development and capabilities,
sales and marketing capabilities, and other statements regarding matters that
are not historical facts, or otherwise involve beliefs or predictions. The
company's performance and financial results could differ materially from those
reflected in the forward-looking statements due to general financial, economic,
regulatory and political conditions affecting the biotechnology and
pharmaceutical industries as well as more specific risks and uncertainties such
as those set forth in documents filed by the company with the SEC (including,
but not limited to, its most recent reports on Form 8-K, Form 10-Q and Form
10-K). Given these risks and uncertainties, any or all of these forward-looking
statements may prove to be incorrect. Therefore, current or prospective
investors are cautioned not to place undue reliance on any such forward-looking
statements. Furthermore, the company has no intent, and disclaims any
obligation, to update any such factors or forward-looking statements to reflect
future events or developments.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at http://www.cephalon.com. They are also available by fax 24 hours a day
at no charge by calling PR Newswire's Company News On-Call at 800-758-5804,
extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Scott Melville (media), 610-738-6270, or Sandra Menta (investor),
610-738-6376, both of Cephalon, or Anne Marie Rodriguez of Sante Communications
(Europe), 011-44-1-71-379-7377
LOAD-DATE: December 4, 1998
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 1998 PR Newswire Association, Inc.
945 of 998 DOCUMENTS
The New York Times
November 3, 1998, Tuesday, Late Edition - Final
New Hope for the Losers in the Battle to Stay Awake
BYLINE: By ERICA GOODE
SECTION: Section F; Page 1; Column 2; Health & Fitness
LENGTH: 1677 words
It is midafternoon on the eastern coast of a chronically sleep-deprived nation
and if you listen carefully, you can hear the whoosh of cappuccino makers and
the ripping open of No-Doz boxes and the yawns of night-shift workers and the
sighs of pilots as they check their watches to see how much longer they must
keep their aircraft aloft.
These are the sounds of the struggle to stay awake, a major enterprise in a
country that long ago exchanged the effortless biological cycle of sleeping and
waking for the tyranny of electric lights, job-plus-kids living, graveyard
shifts and packages that absolutely, positively have to be there overnight.
About two-thirds of workplace accidents in the United States are caused by human
error, studies show, many of them the result of a failure of alertness at
critical times. Jet-lag sufferers, all-night workers, the elderly and the
multitude of Americans with disorders like sleep apnea and narcolepsy wage a
continual battle against excessive daytime sleepiness. And staying awake
supports a multibillion-dollar industry that serves up a variety of stimulants,
legal and illegal, and sleep promoters, offering hope that a good night's sleep
will bring alertness the next day.
Yet the search for artificial compounds to enhance wakefulness is a chronicle of
limited success. Caffeine, for all its appeal, is not especially potent, and in
high doses can be unpleasant, causing irritability, tremor and excessive
urination.
Amphetamines, the wonder drugs of the 1950's and 60's, quickly opened a
Pandora's box of side effects and abuse. The drugs keep people awake, but they
also produce euphoria and the jitters, revving up the central nervous system and
causing the heart rate and blood pressure to jump. And once the effects wear
off, users soon crave more of the drug.
Fearful of lawsuits, drug companies largely stopped trying to improve alertness,
and for 20 years have devoted their efforts to developing new sleep-promoting
drugs, seeking to maximize high quality sleep while minimizing day-after
hangovers.
That may soon change. By Dec. 31, the Food and Drug Administration is to decide
whether a new compound called modafinil can be marketed as a treatment for
excessive sleepiness associated with narcolepsy, a severe sleep disorder that
afflicts about one in 1,000 Americans. Approval of the drug would also open the
door to "off-label" use, allowing doctors to prescribe it for other conditions.
If modafinil goes on the market, many sleep scientists believe, it could usher
in a new era of wakefulness compounds and help researchers unlock the mysteries
of sleep and waking. But at the same time, the arrival of the drug is likely to
raise profound questions about how, as a society, Americans choose to cope with
their perpetual lack of sleep and their constant campaign to stay awake.
Modafinil, to be sold under the trade name Provigil, is licensed to Cephalon
Inc., a small pharmaceutical company in West Chester, Pa. Since its discovery
by French scientists in the late 1970's, the compound has stirred interest among
sleep researchers because it appears to work entirely differently from other
alertness drugs.
"This is the first drug in history to selectively promote wakefulness in a way
analogous to how the brain normally wakes up," said Dr. Dale Edgar, associate
professor of psychiatry and behavioral science at Stanford University, who
conducted preclinical trials of Provigil for Cephalon and has done other animal
studies of the drug financed by the Air Force Office of Research. "Modafinil is
certainly not a real substitute for getting sleep. That would be a misuse of
this drug. But I personally believe it has great promise for a much wider range
of sleep disorders."
In human trials, modafinil appears more effective than caffeine without causing
the anxiety, euphoria and cardiovascular effects of amphetamines. Four years of
on-the-market experience in France, where the drug is sold as Mododial, and
clinical trials financed by Cephalon in this country have revealed few side
effects. The most common complaints are mild headache and slight nausea, and
these are infrequent. Preliminary studies suggest that modafinil is nonaddictive
and that it does not induce tolerance in users.
Dr. Jed Black, director of the Sleep Disorders Clinic at Stanford and a
participant in the clinical trials, said subjects taking the drug reported
feeling "naturally alert, like they'd taken a good nap and felt good." And
modafinil does not seem to touch off rebound sleepiness -- the "crash" familiar
to amphetamine users -- after it is discontinued.
If all this sounds too good to be true, it could turn out to be. Many promising
drugs have shown serious problems once they became widely prescribed. The diet
drugs Fen-phen, withdrawn from the market after patients developed heart valve
problems, are a case in point.
"You've got to have the drug out there, and you've got to see what it does,"
said Dr. Philip Smith, director of the Johns Hopkins University Sleep Disorders
Center, who was not involved in the Provigil trials. "It would really mean
something to have a medication that can stimulate the brain and keep it awake
without juicing the whole system. But the proof is in the pudding."
Clinical trials of new drugs are typically small (558 patients at 39 sleep
disorder clinics around the country took part in two trials of Provigil), and
the studies are almost always financed by the drug company that wants to market
the compound, a fact that some experts believe limits the usefulness of the
research. And while France has four years of experience with Mododial,
prescription of the drug there is tightly controlled, and its users have been
limited to patients suffering from narcolepsy or from idiopathic hypersomnia,
another relatively rare sleep disorder.
Many questions about modafinil remain to be answered. Scientists do not know,
for example, how long the drug can keep people awake, and they are only
beginning to discover its effects on judgment, reaction time and other aspects
of cognitive and physical performance.
In one study, by Dr. Ross Pigeau, Dr. Joseph Baranski and their colleagues at
the Canadian Defence and Civil Institute of Environmental Medicine, 41 military
reservists were deprived of sleep for 64 hours, given modafinil, an amphetamine
or a dummy medication and were required to perform a repeated series of
cognitive tasks. Those given on modafinil or amphetamines performed
significantly better than those given a placebo. But the modafinil group, while
experiencing fewer side effects than the amphetamine group, was also more likely
to be overconfident, overestimating abilities after performance declined -- a
problem that, if it proved common, could severely limit the drug's use in the
general population.
The biggest unanswered question about modafinil, however, is: How does it work?
Central nervous system stimulants like amphetamines achieve their effects by
increasing levels of chemical messengers in areas of the brain associated with
arousal, and also with pleasure and locomotor activity. In particular,
amphetamines act on a brain chemical called dopamine, which scientists believe
is responsible for the euphoria the drugs produce and also their potential for
abuse.
Modafinil, in contrast, does not appear to affect dopamine, or if it does, it
does so only very weakly. Nor does the drug seem to target other
neurotransmitters -- adrenaline and serotonin, for example -- affected by
amphetamines. Caffeine blocks the action of the chemical substance adenosine,
which scientists believe promotes sleep. But modafinil, studies have found,
seems indifferent to adenosine as well.
Instead, work by Dr. Michel Jouvet, a French sleep researcher, and his
colleagues suggests that modafinil increases cellular activity in an area of the
brain adjacent to the suprachiasmatic nucleus, or SCN, the body's circadian
clock. And this fits nicely with scientists' best guess as to how the brain
maintains wakefulness, a theory developed by Dr. Edgar of Stanford.
According to Dr. Edgar's theory, the sleep-wake cycle represents a battle
between oppositional forces: the SCN, on the one hand, and the pressure to sleep
on the other. The SCN, through communication with other brain areas, acts like
an alarm ringing throughout the day to fight back sleepiness and maintain
wakefulness. In the morning, when sleep pressure for humans is low, the SCN does
not need to work very hard to keep a person awake. But as the day goes on, sleep
pressure builds, and the bell rings louder and louder to fight off fatigue. At
night, the clock's output diminishes, the clock stops ringing and the built-up
sleep pressure rushes in, swooping the tired day warrior into the Land of Nod.
Modafinil, Dr. Edgar and others believe, may act by somehow invoking the clock's
natural alerting mechanism, keeping the alarm "ringing" well beyond the time
when it normally shuts off. And if this is the case, modafinil and other drugs
like it would offer the possibility of literally doing away with sleep, fooling
the body into staying "naturally" awake for long periods.
Would such a drug be a cure for shift workers and jet lagged travelers and
overworked mothers with bills to pay and reports to file? Who would be permitted
to take it? Police officers? Soldiers? Airplane pilots? These are questions,
says Dr. David Dinges, chief of the Division of Sleep and Chronobiology in
psychiatry at the University of Pennsylvania, that society will have to address
sooner or later, as the new generation of wake-promoting drugs emerges.
"We are on an inexorable march to uncovering the biology of wakefulness and
manipulating it," Dr. Dinges said. Modafinil may not live up to expectations.
"But when such a drug does arrive, it will change the world. Is it O.K. for us
to become a nation that doesn't sleep? Until we know what sleep is for, and why
it is so overwhelming, we're not going to be able to say it's O.K. to find a
substitute for it."
LOAD-DATE: November 3, 1998
LANGUAGE: ENGLISH
GRAPHIC: Chart: "Fighting To Stay Awake"
Dr. Dale Edgar describes sleep and wakefulness as a battle of oppositional
forces where the desire to sleep, which builds from the moment one awakens, is
countered by signals from the brain's internal clock. In the evening, when the
clock stops ringing, we sleep.
Day
Pressure to sleep builds.Alerting signals counter, staving off immediate sleep.
Night
Signals from the body's clock diminish, and sleep occurs. Sleep pressure
decreases.
THE BRAIN'S INTERNAL CLOCK -- A tiny portion of the brain called the
suprachiasmatic nuclei (or SCN) sends out disinhibitory signals that counter the
inhibiting signals that result in sleepiness.
Copyright 1998 The New York Times Company
946 of 998 DOCUMENTS
Village Voice (New York, NY)
August 11, 1998
CITY NEVER SLEEPS
BYLINE: mark schoofs
SECTION: Columns; Pg. 61
LENGTH: 827 words
When Ross Pigeau, a researcher with the Canadian military, first heard about a
new drug that can keep people awake as effectively as amphetamines but without
the jitters, ''it just sounded too good to be true,'' he recalls. But after
studying the drug, called modafinil, and trying it himself, Pigeau is a
believer, and he ticks off the benefits: ''Apparently not addictive, apparently
no withdrawal, and very few side effects. Someone tried to OD on modafinil by
taking almost a whole bottle, and he just had a night without sleep.''
So far, the drug has caught the attention only of National Public Radio and a
smattering of other media outlets. Perhaps that's because the Food and Drug
Administration is expected to approve modafinil, probably by the end of the
year, for a rare illness which French doctors have for several years been using
the drug to treat: narcolepsy, a disorder in which people fall asleep suddenly
in the middle of the day. But once a drug is approved, doctors can prescribe it
for almost any reason, however frivolous, such as enabling a healthy person to
pull an all-nighter.
The Canadian military--like the French and American armed forces, which have
also studied the drug--wanted to be able to keep soldiers awake for long
stretches. So in Pigeau's experiment, healthy subjects were kept awake for three
days while adhering to a grueling work regimen that permitted only one 15-minute
break every two hours. Modafinil improved performance just as much as
amphetamines, but it didn't give people a high; they simply felt awake. What's
more, when test subjects were finally allowed to get some shut-eye, those on
modafinil had sleep cycles that were normal. The only drawback--which Pigeau
terms ''very interesting''--is that people on modafinil were consistently
overconfident, estimating their proficiency to be better than it actually was.
So will workaholics flock to the drug? ''We are all concerned about that,''
sighs Joyce Walsleben, director of the New York University Sleep Disorders
Center, where modafinil has been studied. She worries that people will ''think
it is a magic bullet so they can do without sleep.'' That's a dangerous
misconception, because the drug does not keep people operating at peak
performance. When Pigeau gave his subjects modafinil after they had been awake
for two nights, the drug only restored them to the level of performance they had
following their first night without sleep--and that was a whopping 35 percent
below their rested performance. Imagine people driving cars, flying planes, or
wielding scalpels at such perilously subpar levels--yet overconfident about
their ability--and suddenly Walsleben's worry seems a lot more urgent.
No one knows the function of sleep--a complex biological phenomenon quite
distinct from mere resting--but it must be extremely important. Sleep renders
animals unconscious, and thus easy prey, yet all mammals, birds, and reptiles
sleep. What's more, they have evolved elaborate adaptations to do so. Horses
sleep while standing, birds while perching, and dolphins while swimming. And
dolphins even sleep with one-half of their brain at a time.
Allan Rechtschaffen, a professor at the University of Chicago and one of the
foremost authorities on sleep, found that rats deprived of sleep die in two to
three weeks. Yet despite extensive study, neither he nor anyone else has been
able to determine the cause of death. In humans, says Rechtschaffen, the record
for staying awake ''is 11 days, by one high school student who did it as a
science project.'' But no lasting physiological harm was detected.
Of course, while people are sleep-deprived, their irritability soars and sense
of humor plummets. ''There is often some hallucination,'' adds Pigeau. ''It's
very subtle: they'll say, 'Did you hear that sound?' or 'I think I saw something
running across the floor.''' Even mild sleep loss has been shown to impair
creative or complex thinking. No one knows how or why sleep deprivation causes
these problems, much less what sleep is ultimately for.
But the inquiry can be flipped on its head: ''What is wakefulness for?'' asks
Merrill Mitler, a clinical professor at the University of California at San
Diego and a consultant to Cephalon, which is developing modafinil for the U.S.
market. Chuckling slyly, he offers an off-the-cuff answer to his own question:
wakefulness is for eating, drinking, and procreating.
Maybe that's true, but it hardly gets at why we value being awake. In a similar
way, even if the Darwinian, biological function of sleep is found, it may have
only limited relevance to our experience of sleep. And that personal, almost
existential understanding of sleep may be the best bulwark against the abuse of
caffeine substitutes. Most people hate feeling sleep-deprived and love feeling
well rested. No drug on the horizon can equal that natural high.
Research assistance: Tyler Schnoebelen, Sam Bruchey
LOAD-DATE: August 05, 1998
LANGUAGE: ENGLISH
Copyright 1998 VV Publishing Corporation
947 of 998 DOCUMENTS
Village Voice (New York, NY)
August 11, 1998
CITY NEVER SLEEPS
BYLINE: mark schoofs
SECTION: Columns; Pg. 61
LENGTH: 827 words
When Ross Pigeau, a researcher with the Canadian military, first heard about a
new drug that can keep people awake as effectively as amphetamines but without
the jitters, ''it just sounded too good to be true,'' he recalls. But after
studying the drug, called modafinil, and trying it himself, Pigeau is a
believer, and he ticks off the benefits: ''Apparently not addictive, apparently
no withdrawal, and very few side effects. Someone tried to OD on modafinil by
taking almost a whole bottle, and he just had a night without sleep.''
So far, the drug has caught the attention only of National Public Radio and a
smattering of other media outlets. Perhaps that's because the Food and Drug
Administration is expected to approve modafinil, probably by the end of the
year, for a rare illness which French doctors have for several years been using
the drug to treat: narcolepsy, a disorder in which people fall asleep suddenly
in the middle of the day. But once a drug is approved, doctors can prescribe it
for almost any reason, however frivolous, such as enabling a healthy person to
pull an all-nighter.
The Canadian military--like the French and American armed forces, which have
also studied the drug--wanted to be able to keep soldiers awake for long
stretches. So in Pigeau's experiment, healthy subjects were kept awake for three
days while adhering to a grueling work regimen that permitted only one 15-minute
break every two hours. Modafinil improved performance just as much as
amphetamines, but it didn't give people a high; they simply felt awake. What's
more, when test subjects were finally allowed to get some shut-eye, those on
modafinil had sleep cycles that were normal. The only drawback--which Pigeau
terms ''very interesting''--is that people on modafinil were consistently
overconfident, estimating their proficiency to be better than it actually was.
So will workaholics flock to the drug? ''We are all concerned about that,''
sighs Joyce Walsleben, director of the New York University Sleep Disorders
Center, where modafinil has been studied. She worries that people will ''think
it is a magic bullet so they can do without sleep.'' That's a dangerous
misconception, because the drug does not keep people operating at peak
performance. When Pigeau gave his subjects modafinil after they had been awake
for two nights, the drug only restored them to the level of performance they had
following their first night without sleep--and that was a whopping 35 percent
below their rested performance. Imagine people driving cars, flying planes, or
wielding scalpels at such perilously subpar levels--yet overconfident about
their ability--and suddenly Walsleben's worry seems a lot more urgent.
No one knows the function of sleep--a complex biological phenomenon quite
distinct from mere resting--but it must be extremely important. Sleep renders
animals unconscious, and thus easy prey, yet all mammals, birds, and reptiles
sleep. What's more, they have evolved elaborate adaptations to do so. Horses
sleep while standing, birds while perching, and dolphins while swimming. And
dolphins even sleep with one-half of their brain at a time.
Allan Rechtschaffen, a professor at the University of Chicago and one of the
foremost authorities on sleep, found that rats deprived of sleep die in two to
three weeks. Yet despite extensive study, neither he nor anyone else has been
able to determine the cause of death. In humans, says Rechtschaffen, the record
for staying awake ''is 11 days, by one high school student who did it as a
science project.'' But no lasting physiological harm was detected.
Of course, while people are sleep-deprived, their irritability soars and sense
of humor plummets. ''There is often some hallucination,'' adds Pigeau. ''It's
very subtle: they'll say, 'Did you hear that sound?' or 'I think I saw something
running across the floor.''' Even mild sleep loss has been shown to impair
creative or complex thinking. No one knows how or why sleep deprivation causes
these problems, much less what sleep is ultimately for.
But the inquiry can be flipped on its head: ''What is wakefulness for?'' asks
Merrill Mitler, a clinical professor at the University of California at San
Diego and a consultant to Cephalon, which is developing modafinil for the U.S.
market. Chuckling slyly, he offers an off-the-cuff answer to his own question:
wakefulness is for eating, drinking, and procreating.
Maybe that's true, but it hardly gets at why we value being awake. In a similar
way, even if the Darwinian, biological function of sleep is found, it may have
only limited relevance to our experience of sleep. And that personal, almost
existential understanding of sleep may be the best bulwark against the abuse of
caffeine substitutes. Most people hate feeling sleep-deprived and love feeling
well rested. No drug on the horizon can equal that natural high.
Research assistance: Tyler Schnoebelen, Sam Bruchey
LOAD-DATE: August 11, 1998
LANGUAGE: ENGLISH
Copyright 1998 VV Publishing Corporation
948 of 998 DOCUMENTS
The Philadelphia Inquirer
JULY 13, 1998 Monday SF EDITION
NEW DRUG HOLDS PROMISE FOR HELPING NARCOLEPTICS / WILL OTHERS - MERELY STRESSED
OUT AND SLEEP-DEPRIVED - ALSO TRY TO OBTAIN IT?
BYLINE: Shankar Vedantam, INQUIRER STAFF WRITER
SECTION: FEATURES MAGAZINE: HEALTH & SCIENCE; Pg. D01
LENGTH: 951 words
While most of America isn't sleeping enough, some people - those with a chronic
condition called narcolepsy - are sleeping too much, dozing off several times a
day, even getting some dangerous shut-eye while they drive.
Soon, there may be help for them. A new medicine marketed by Cephalon, a West
Chester-based pharmaceutical company, promises powerful help to fight daytime
sleepiness. Sleep doctors are unanimous: This is great news for those with
narcolepsy.
The question, however, is whether hyperactive, stressed-out, sleep-deprived
America will also seek the drug in order to stay awake even longer. Although
doctors warn about the dangers of not sleeping, the new drug could add to the
stay-awake arsenal of night-shift workers, truck drivers and students.
The medicine will almost certainly have to be prescribed by a doctor and be sold
under strict supervision, but that hasn't stopped other drugs from being misused
in the past.
"All you have to do is look at the history of Fen-phen and other drugs that were
originally described as being appropriate for one use and ended up being
prescribed by physicians for patients who were not appropriate," said Joan
Goldberg, a spokeswoman at the National Sleep Foundation, a nonprofit
organization in Washington that monitors America's sleep debt.
"Anybody involved in the health business wants to see treatments are used by the
right people for the right reasons," she said.
The Food and Drug Administration has not yet made a ruling on the drug modafinil
, which Cephalon wants to sell under the brand name Provigil. The drug has
cleared testing hurdles, and a decision is expected by the end of the year.
"It's important that we caution anyone who has an interest in this product that
the data only address its potential use in treating daytime sleepiness
associated with narcolepsy," said Cephalon spokesman Jason Rubin.
Would the company dissuade people who were not narcoleptics from using the
medicine?
"I can't answer that question," he said. "If the drug is approved for excessive
daytime sleepiness [as a result of narcolepsy] we would have the freedom to
promote the product for that indication alone," not for other uses.
While the FDA approves a drug for a specific condition, doctors can prescribe
medicines "off-label" for other reasons if they feel such use would help
patients.
Rubin guessed that there were about 125,000 patients with narcolepsy in the
United States. Goldberg and the National Sleep Foundation put the number at
200,000. It is difficult to diagnose narcolepsy because its primary symptom -
sleepiness - is not in itself abnormal.
Predictably, the number of Americans who are sleep-deprived is far larger than
the group of narcoleptics.
"The average person needs eight hours of sleep and the average person gets seven
hours of sleep," said Goldberg. "At least one-third of Americans are suffering
from significant sleep loss during the work week."
About one in five people said that their sleep deprivation interfered with their
daily activities a few days a month, according to the 1998 results of a survey
by the foundation. About one in three people said that their sleepiness
interfered with their job, family duties, relationships and recreation.
Modafinil has several advantages over other stimulants. In studies conducted in
the United States and Europe, the drug has been shown to be safe. It seems to
work well long-term, and does not produce the psychological highs of stimulants
such as coffee or amphetamines.
"It won't be abused because it doesn't make people feel good," said Calvin
Stafford, director of the Sleep Disorder Center at Crozer Chester Medical
Center, who helped conduct trials of modafinil in America.
"It doesn't appear to have the roller-coaster effect," he said. "You don't feel
wired."
Other stimulants cause people to "have periods where the drug levels are high
and they are bright but then they begin to get drowsy. Modafinil is
long-acting," he said.
"I can't say what will happen out there without supervision. It is my hope
people won't use it to stay up for finals, but we have certainly seen such
behavior with other stimulants. We can't guarantee it won't happen with any new
drug."
No one is quite sure how modafinil works. One of its fascinating effects is it
seems to remove the need for sleep.
"We always thought when you take away sleep you have to pay back, but that does
not seem to happen with this medication," said Karl Doghramji, director of the
Sleep Disorders Center at Thomas Jefferson University. "With amphetamines you
have a post-drug crash. Once you stop taking them, you have tremendous
sleepiness.
"What these pills help us do is make sure we get sleep only for six to eight
hours a night," he said. "It ensures that during the time we are awake we stay
awake, but also makes sure the sleep at night is good."
Sleep is as central to human health as food and water. Cognitive functions and
judgment rapidly decline with sleep deprivation, and the body quickly goes
downhill.
"It is not possible to really define all the aspects of what happens to a person
when they are sleep-deprived," said June Fry, director of the sleep disorders
center at the Allegheny University of the Health Sciences. "They are more
susceptible to disease, especially viruses and communicable diseases. It affects
their immune systems, their hormone balances, all their circadian rhythms."
Fry said doctors didn't know what would happen to healthy people if they used
modafinil to stay awake, but said it was pretty certain not to be good for them.
"The only appropriate treatment for sleep deprivation," she said, "is sleep."
LOAD-DATE: October 24, 2002
LANGUAGE: ENGLISH
Copyright 1998 Philadelphia Newspapers, LLC
All Rights Reserved
949 of 998 DOCUMENTS
Internal Medicine Alert
June 29, 1998
Modafinil for Narcolepsy
LENGTH: 819 words
Modafinil for Narcolepsy
ABSTRACT & COMMENTARY
Synopsis: If its relatively low side effects continue, modafinil appears to be
the first non-toxic drug that can improve the disturbing symptoms of narcolepsy.
Source: U.S. Modafinil in Narcolepsy Study Group. Ann Neurol 1998;43:88-97.
Narcolepsy affects approximately 100,000 persons in the United States, with a
sizable fraction of the sufferers experiencing repeated, semi-disabling,
excessive daytime sleepiness. A measurably fewer number suffer from cataplexy,
fractioned nocturnal sleep, hypnagogic hallucinations, and sleep paralysis. The
illness is usually inherited and associated with one of several HLA DRZ or DQB1
haplotype groups plus other factors. Haplotype specificity, however, does not
guarantee expression of the disorder. Disabling daytime sleepiness provides
narcolepsy's dominant dysfunction, for which amphetamines bring only modest
improvement, often with considerable unwanted side effects. Investigators have
suggested that the disease results from insufficient CNS dopamine release plus
an increase in muscarinic acetylcholine receptors generating hypersensitivity to
acetylcholine.
Against this therapeutically unfavorable backdrop, a new wake-provoking stimulus
called modafinil, 2 ([diphenylmethyl] sulfinyl) acetamide has been introduced.
Modafinil stimulates CNS targets known to respond to amphetamine and
methylphenidate. Effects in animals indicate that modafinil increases
wakefulness but induces little amphetamine-like excitation of motor function.
To test the value of modafinil, 283 persons aged 18-68 years were randomized
into three cohorts: placebo (n = 92), 200 mg daily (n = 96), and 400 mg daily (n
= 95). This report provides preliminary results, and a successive open-label
trial is in progress. Participants graded the patient's post-therapy dozing
response as: 1) never, 2) slight chance, 3) moderate, or 4) high. All categories
were applied during times of relatively inactive behavior. Objective evaluations
included Sleep Latency Testing (SLT) and Maintenance of Wakeful Test (MWT).
Severity of disease was evaluated by a clinician's Clinical Global Impression
(CGI). Nocturnal polysomnography was applied before each assessment. Mean age of
the cohort was 42 years, and sex numbered 43 men and 51 women in each cohort.
Mean length of disease amounted to 22 years; 95% had daytime sleep attacks, 88%
had cataplexy, 71% had interrupted nighttime sleep, 69% hallucinated, and 64%
experienced sleep paralysis. Results were appraised at three, six, and nine
weeks following onset of the trial.
Self-reported sleepiness (ESS) events were similar at onset and, in the placebo
group, at nine weeks. Otherwise, at week nine both modafinil cohorts showed less
sleepiness than controls (P < 0.001), with the 400 mg group significantly better
than the 200 mg group (P < 0.001). Sleep latency was similar between the two
modafinil groups but was significantly better than controls (P < 0.001).
Maintenance of wakefulness was better than control in both modafinil groups (P <
0.001) but not different between the two groups. Also, more subjects in the
modafinil groups remained awake longer than in the control group. Blinded
clinical assessment rated modafinil-taking patients as measurably improved
compared to the controls.
Complications were relatively low: one of the 200 mg dose cohort withdrew, as
did 11 (12%) of the 400 mg group. The only symptom significantly higher than
placebo was headache.
A subsequent open-label trial continues beyond the above blind control studies.
In that trial, clinical global impression showed 84% improvement by week two of
taking modafinil with the number rising to 91% by week 40. Both times had
significance at the P < 0.001 level. The authors indicate that "adverse
experiences were mostly mild to moderate." In the open trial, however, 25% of
patients withdrew because of side effects or lack of efficacy.
COMMENT BY FRED PLUM, MD
If its relatively low side effects continue, modafinil appears to be the first
non-toxic drug that can improve the disturbing symptoms of narcolepsy. The drug
clinically appears to reduce daytime sleepiness, and the result of latency tests
supported that conclusion. The general clinical appraisal of the participating
neurologists also concluded that wakefulness improved in the treated group. At
this writing, the reporting participating neurologists estimate that overall
efficacy of modafinil against narcolepsy amounts to about 55%, with Pemoline
providing about an equal help but with amphetamine or methylphenidate each
improving symptoms by about 80%. The latter level, however, produces a
relatively high incidence of unwanted symptoms. As the authors conclude, "
modafinil is a pharmacologically and clinically promising compound for treating
pathological daytime somnolence." (Dr. Plum is Neurologist-in-Chief, New York
Hospital-Cornell Medical Center.)
LOAD-DATE: May 28, 2010
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PUBLICATION-TYPE: Newsletter
Copyright 1998 AHC Media LLC
All Rights Reserved
950 of 998 DOCUMENTS
Reuters Health Medical News
June 12, 1998 Friday
Nippon Shoji to market Cephalon's modafinil in Japan
SECTION: INDUSTRY
LENGTH: 168 words
DATELINE: WESTPORT Jun 12
Nippon Shoji Kaisha, based in Osaka, Japan, will market in Japan Cephalon's
modafinil for the treatment of narcolepsy, according to a Cephalon press release
posted on PR Newswire.
Cephalon will receive milestone payments and royalties based on sales of the
product in Japan. Nippon Shoji will continue development of the drug in Japan
an seek regulatory approval.
West Chester, Pennsylvania-based Cephalon licensed rights to modafinil in France
to Laboratoire L. Lafon. The drug has been approved for marketing in the UK and
Ireland, and Cephalon received an approvable letter from the Food and Drug
Administration in the US. The company is also currently pursuing regulatory
clearance to market modafinil in Mexico and Italy.
Dr. Frank Baldino, Jr., president and CEO of Cephalon, commented, "Japan is a
significant component of the worldwide pharmaceutical marketplace. We are
delighted to partner with Nippon Shoji to bring to Japan what we believe may be
an important new therapy for this disabling disease."
LOAD-DATE: July 9, 2008
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PUBLICATION-TYPE: Newswire
Copyright 1998 Reuters Health
All Rights Reserved
951 of 998 DOCUMENTS
PR Newswire
June 11, 1998, Thursday - 08:35 Eastern Time
Cephalon Grants Nippon Shoji Rights to Modafinil in Japan.
SECTION: Financial News
LENGTH: 467 words
DATELINE: WEST CHESTER, Pa., June 11
Cephalon, Inc. (Nasdaq: CEPH) announced today that it has entered into an
agreement with Nippon Shoji Kaisha, Ltd. (NSK) for the development and marketing
of modafinil in Japan. Under the terms of the agreement, Cephalon will receive
milestone payments and royalties based upon NSK product sales.
Nippon Shoji plans to initially develop and seek regulatory approval for
modafinil for the treatment of narcolepsy, which is a chronic, lifelong sleep
disorder that hampers a person's ability to perform basic daily activities.
"Japan is a significant component of the worldwide pharmaceutical marketplace,"
said Frank Baldino, Jr., Ph.D., Cephalon's president and chief executive
officer. "We are delighted to partner with Nippon Shoji to bring to Japan what
we believe may be an important new therapy for this disabling disease."
Cephalon licensed rights to modafinil in certain territories from Laboratoire L.
Lafon, the French pharmaceutical company which discovered and markets the drug
in France. Cephalon received market authorization for modafinil in the United
Kingdom and the Republic of Ireland. The company is currently marketing
modafinil in the United Kingdom for the treatment of narcolepsy and plans to
market the drug in Ireland upon clearance of U.S. manufacturing arrangements.
Cephalon has received an approvable letter from the U.S. Food and Drug
Administration. Additionally, the company is pursuing regulatory clearance to
market modafinil in Mexico and Italy.
Nippon Shoji Kaisha, Ltd., headquartered in Osaka, Japan, is an integrated
supplier of medical products. Nippon Shoji actively markets and produces
pharmaceutical products, diagnostics and medical devices.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company that discovers, develops and markets products to treat
neurological disorders.
This news release may contain forward-looking statements that involve risks and
uncertainties. A full discussion of Cephalon's operations and financial
condition, including factors that may affect the company's business and future
prospects, is contained in documents the company files with the SEC, such as
form 10-Q and 10-K reports. These documents identify important factors that
could cause the company's actual performance to differ from current
expectations.
NOTE: Cephalon's press releases are posted on the Internet at the company's Web
site at http://www.cephalon.com. They are also available by fax 24 hours a day
at no charge by calling PR Newswire's Company News On-Call at 800-758-5804,
extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Jason Rubin (US) of Cephalon, 610-738-6302, or Shun-Ichi Miyake
(Japan) of Nippon Shoji Kaisha, 011-81-69-42-6192
LOAD-DATE: June 12, 1998
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
Copyright 1998 PR Newswire Association, Inc.
952 of 998 DOCUMENTS
Community Pharmacy
June 1998
Sleep Problems - Waking up to narcolepsy
SECTION: Pg. 20
LENGTH: 1780 words
Will the introduction of a new narcolepsy treatment help control the disease
nightmare for many sufferers? Assistant editor Clare Evans finds out.
Narcolepsy is a chronic and life-long debilitating sleep disorder. As many as
approximately 2,500 diagnosed narcolepsy patients in the UK currently receive
treatment although, due to the difficulties in correctly diagnosing the disease,
this is thought to be simply the tip of the iceberg.
The characteristic feature of narcolepsy is excessive daytime sleepiness (EDS),
but patients may also be affected by a range of other symptoms. These include:
- cataplexy (sudden loss of muscle tone)
- sleep paralysis (the inability to move during the process of falling asleep or
while awakening)
- dreamlike imagery or sound known as visual or auditory hallucinations.
Only 11 per cent of people with narcolepsy suffer from all four symptoms.
Excessive daytime sleepiness (EDS)
EDS is the most disabling and difficult to treat symptom of narcolepsy.
Sufferers are constantly tired, resulting in recurrent, uncontrollable bouts of
sleep throughout the day. EDS is overpowering and sufferers may become irritable
if sleep is resisted or prevented. Attacks typically last for up to 30 minutes.
Up to 80 per cent of narcoleptics also experience changes in alertness
throughout the day lasting a few seconds through to several minutes. During this
time they can undertake irrational and potentially dangerous tasks, of which
they have no recollection. These can include putting things in the oven or
driving to an unplanned, or even unknown, destination.
Cataplexy
Almost three quarters of narcolepsy sufferers develop cataplexy. Attacks involve
sudden decreases in, or loss of, muscle tone which can affect a single muscle or
the whole body. They may last for less than a minute to over 20 minutes and
include a range of symptoms including slurred or lost speech, dropping arms and
a sagging jaw. Cataplexy triggers include strong emotion such as laughter,
surprise, fear, anger, anticipation and excitement.
Sleep paralaysis
Some patients experience the sudden inability to move or speak during the
transition period between sleeping and waking. Sleep paralysis attacks may also
be accompanied by breathing problems - the person may feel as if their chest is
constricted, when their breathing actually continues as normal.
The reported prevalence of sleep paralysis among narcoleptics varies between one
quarter and two thirds of sufferers, possibly due to the fact that few sufferers
seek advice for the condition.
Hypnagogic/hynopompic hallucinations
Many narcoleptics experience dreamlike imagery or sounds while dozing or
awakening. These experiences are clinically known as visual or auditory
hallucinations and can occur just before falling asleep (hypnagogic), or just
after awakening (hypnopompic).
Narcoleptics also demonstrate a different sleep pattern to non- narcolepsy
sufferers. Rapid eye movement (REM) occurs approximately 90 minutes into a
non-sufferers sleep and it is here that dreaming occurs. In narcoleptics, REM
occurs much earlier, generally within 10 minutes of falling asleep. As a result
of the rapid onset of dreaming, the sufferer may experience hallucinations.
Other reported symptoms of the narcoleptic syndrome include facial twitching,
headaches, insomnia, poor concentration and problems with memory.
Prevalence
Narcolepsy can develop at any age and it affects both sexes equally. Symptoms
commonly present during adolescence, although 6 per cent of sufferers are
affected before they reach the age of 10.
The cause of narcolepsy is unknown. Genetic pre-disposition may play a part; 98
per cent of sufferers carry the human leucocyte antigen HLA- DR2, but, as 25 per
cent of the total population also carry it, the antigen itself is not the cause.
Symptomatic narcolepsy has been reported in association with traumatic illnesses
such as brain tumours, stroke, and head trauma, although cases are rare and may
resolve with specific treatment.
Diagnosis
Diagnosing narcolepsy is often difficult. Many sufferers avoid visiting their GP
for fear of being perceived as lazy; others have their symptoms mistakenly
attributed to other illnesses such as hypothyroidism and multiple sclerosis.
The diagnosis of narcolepsy is usually confirmed at a specialist sleep centre
through laboratory tests. These include:
- Polysomnography: a multiple set of physiological tests including EEG, ECG,
measures of oxygen saturation, and respiratory flow and effort
- Multiple Sleep Latency Test (MSLT): a measure of sleepiness levels. The
patient is given the opportunity to sleep at two hourly intervals, four or five
times throughout the day under supervision. If the time it takes the person to
fall asleep is eight minutes or less it suggests that they may be suffering
narcolepsy. The speed of achieving REM sleep is also observed.
- Maintenance of Wakefulness Test (MWT): Patients are placed in comfortable
conditions in a darkened room during the day and asked to try and remain awake.
This test can also be used to measure the effects of treatment.
Treatment options
Since the 1930s, amphetamines have been used to treat the EDS symptom of
narcolepsy. Acting on the central nervous system (CNS), use results in increased
alertness, improved mood and euphoria.
Most sufferers initially respond to treatment and find their sleepiness
controlled to an acceptable degree. However, side-effects including
irritability, headache, palpitations, nausea, muscle jerks, tremor, psychosis
and anorexia, plus a strong association with dependence, has limited amphetamine
use, many patients discontinuing treatment of their own accord.
Three in 10 patients develop tolerance to amphetamines, the dose having to be
increased to have the same therapeutic effect. There is also great potential for
abuse.
A new treatment
Now, though, there is an alternative to amphetamines. Provigil (modafinil) from
Cephalon is a non-amphetamine, wake-promoting agent that is claimed to increase
wakefulness and restore a normal pattern of daytime alertness.
Clinical studies show that modafinil significantly reduces all measures of
sleepiness on physiological and clinical scales, as well as the patient's own
self assessment of sleepiness, without affecting night- time sleep.(1)
Although the exact mechanism of action is unknown, modafinil is known to bind to
specific receptors on the anterior hypothalamus - the area of the brain thought
to be responsible for wakefulness - instead of stimulating the CNS receptors as
with amphetamines.(2) This specificity also reduces the incidence of
adverse-effects, with headache the only reported significant side-effect. (2,3)
Dr John Shneerson, director of the Sleep Disorders Centre, Papworth NHS Trust,
finds modafinil to be equally as effective as dexamphetamine in treating
narcolepsy, although it provides a smoother onset, and cessation, of action and
is longer-acting. He also believes there may be a positioning for combining
modafinil with amphetamine treatment at this sleep centre using this
combination.
Although the concomitant use of amphetamines and modafinil is not recommended by
Cephalon, it is something that the company may address in the future.
Pharmacologically, modafinil differs from amphetamines in that it does not cause
mood 'highs' and 'lows', it appears to retain efficacy in long-term use and has
low potential for abuse.(4)
But the company recommends that people who are stable and well- controlled on
amphetamines should remain on them. "People should not be changed to modafinil
just because it is there", says a company spokesperson.
The drug is also contra-indicated for use during pregnancy and lactation, in
children and in patients with moderate to severe hypertension, left ventricular
hypertrophy, chest pain or arrhythmias. It may impair the effectiveness of oral
contraceptives containing less than 50mcg of ethinyl oestradiol and care should
also be taken with its co-administration with anticonvulsants. To date there has
been no definite drug-drug reactions involving modafinil use.(5)
When a patient is changing from amphetamine to modafinil therapy, the
amphetamine dose should be reduced over a period of two to three days until
zero. The patient should then remain drug-free for a period of two to three days
to allow complete excretion. Modafinil can then be gradually introduced in
titrated doses until the patient's symptoms are stable.
Don Pincham, who chairs the UK Narcolepsy Association (UKAN) believes the launch
of modafinil has finally highlighted the problems with treating the disease.
"Provigil is not a wonder drug and it won't suit everyone. But for those who can
take it, it promises a tremendous improvement in their quality of life as the
side-effects of amphetamines can be as bad as the illness itself.
"One of the real benefits is that Provigil is the only drug designed
specifically for narcolepsy and public awareness of the disease has been greatly
raised as a result."
The references for this article are available from the editor
SUMMARY
- Narcolepsy can develop at any age and affects both sexes equally
- There are 2,500 diagnosed narcolepsy sufferers in the UK currently receiving
treatment
- In addition to excessive daytime sleepiness, patients may also suffer from
cataplexy, sleep paralysis and visual or auditory hallucinations
- Amphetamines have been the mainstay of narcolepsy treatment since the 1930s
- Provigil (modafinil) is a non-amphetamine wake-promoting agent
THE NARCOLEPTIC SYNDROME
The 1990 International Classification of Sleep Disorders defines the narcoleptic
syndrome as: 'a disorder of unknown aetiology which is characterised by
excessive daytime sleepiness that typically is associated with cataplexy and
other REM sleep phenomena such as sleep paralysis and hypnagogic hallucinations'
INTERNATIONAL CLASSIFICATION OF SLEEP DISORDERS
To help improve the accuracy of narcolepsy diagnosis, there is a
set international minimum. This is: B+C or A+D+E+G
A Excessive sleepiness or sudden muscle weakness
B Recurrent daytime sleep episodes 3 months or more
C Cataplexy
D Sleep paralysis, hypnagogic hallucinations, etc
E Polysomnographic:
Sleep latency 10 minutes or less
REM sleep latency 20 minutes or less
MSLT Mean sleep latency 8 minutes or less
Two or more SOREMPS*
F HLA-DR2 positive
G Exclude medical and psychiatric disorders
* Sleep Onset Rapid Eye Movement Periods
LOAD-DATE: February 9, 1999
LANGUAGE: English
PUB-TYPE: Magazine
Copyright 1998 CMP Information Ltd
953 of 998 DOCUMENTS
PR Newswire
May 15, 1998, Friday - 08:07 Eastern Time
Cephalon Receives Authorization to Market PROVIGIL(R) (modafinil) In the
Republic of Ireland.
SECTION: Financial News
LENGTH: 474 words
DATELINE: WEST CHESTER, Pa., May 15
Cephalon, Inc. (Nasdaq: CEPH) announced today that its UK subsidiary, Cephalon
UK Ltd., has received authorization from the Irish Medicines Board (IMB) to
market PROVIGIL(R) (modafinil) tablets in the Republic of Ireland for the
treatment of narcolepsy.
Narcolepsy is a chronic, neurological, lifelong sleep disorder that generally
begins in young adulthood. The most common symptom is excessive daytime
sleepiness, which is characterized by uncontrollable sleep attacks. These
attacks hamper a person's ability to perform basic daily activities. As a
result, narcolepsy significantly impacts a person's quality of life.
Cephalon intends to manufacture PROVIGIL tablets in the United States and launch
the drug in the Republic of Ireland upon IMB approval of the U.S. manufacturing
arrangements.
"This is the first non-amphetamine agent licensed for the treatment of
narcolepsy in Ireland," said Frank Baldino, Jr., Ph.D., Cephalon's president and
chief executive officer. "Our European sales and marketing organization looks
forward to making PROVIGIL available to the neurology community in Ireland for
patients suffering from this disabling disease."
Cephalon licensed modafinil from Laboratoire L. Lafon, the French pharmaceutical
company which discovered and markets the drug in France. Cephalon has exclusive
rights to market modafinil in the United States, Japan, the United Kingdom,
Ireland, Mexico and Italy. In March 1998, Cephalon commenced marketing of
PROVIGIL for the treatment of narcolepsy in the United Kingdom. Cephalon has a
marketing application currently pending in the United States to market PROVIGIL
for the treatment of excessive daytime sleepiness associated with narcolepsy.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company that discovers, develops and markets products to treat
neurological disorders.
This news release may contain forward-looking statements that involve risks and
uncertainties. A full discussion of Cephalon's operations and financial
condition, including factors that may affect the company's business and future
prospects, is contained in documents the company files with the SEC, such as
form 10-Q and 10-K reports. These documents identify important factors that
could cause the company's actual performance to differ from current
expectations.
NOTE: Cephalon's press releases are posted on the Internet at the
company's Web site at http://www.cephalon.com. They are also available by fax
24 hours a day at no charge by calling PR Newswire's Company News On-Call at
800-758-5804, extension 134563.
SOURCE Cephalon, Inc.
CONTACT: Sandra Menta (US) of Cephalon, 610-738-6376, or Anne Marie
Rodriguez (Europe) of Sante Communications, 011-44-171-379-7377
LOAD-DATE: May 16, 1998
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 1998 PR Newswire Association, Inc.
954 of 998 DOCUMENTS
Neurology Alert
May 1, 1998
Modafinil for Treatment of Narcolepsy
LENGTH: 820 words
Modafinil for Treatment of Narcolepsy
ABSTRACT & COMMENTARY
Source: U.S. Modafinil in Narcolepsy Study Group. Randomized trial of modafinil
for the treatment of pathological somnolence in narcolepsy. Ann Neurol
1998;43:88-97.
Narcolepsy affects approximately 100,000 persons in the United States, with a
sizable fraction of the sufferers experiencing repeated, semi-disabling,
excessive daytime sleepiness. A measurably fewer number suffer from cataplexy,
fractioned nocturnal sleep, hypnagogic hallucinations, and sleep paralysis. The
illness is usually inherited and associated with one of several HLA DRZ or DQB1
haplotype groups plus other factors. Haplotype specificity, however, does not
guarantee expression of the disorder. Disabling daytime sleepiness provides
narcolepsy's dominant dysfunction, for which amphetamines bring only modest
improvement, often with considerable unwanted side effects. Investigators have
suggested that the disease results from insufficient CNS dopamine release plus
an increase in muscarinic acetylcholine receptors generating hypersensitivity to
acetylcholine.
Against this therapeutically unfavorable backdrop, a new wake-provoking stimulus
called modafinil, 2 ([diphenylmethyl] sulfinyl) acetamide has been introduced.
Modafinil stimulates CNS targets known to respond to amphetamine and
methylphenidate. Effects in animals indicate that modafinil increases
wakefulness but induces little amphetamine-like excitation of motor function.
To test the value of modafinil, 283 persons aged 18-68 years were randomized
into three cohorts: placebo (n = 92), 200 mg daily (n = 96), and 400 mg daily (n
= 95). This report provides preliminary results, and a successive open-label
trial is in progress. Participants graded the patient's post-therapy dozing
response as: 1) never, 2) slight chance, 3) moderate, or 4) high. All categories
were applied during times of relatively inactive behavior. Objective evaluations
included Sleep Latency Testing (SLT) and Maintenance of Wakeful Test (MWT).
Severity of disease was evaluated by a clinician's Clinical Global Impression
(CGI). Nocturnal polysomnography was applied before each assessment. Mean age of
the cohort was 42 years, and sex numbered 43 men and 51 women in each cohort.
Mean length of disease amounted to 22 years; 95% had daytime sleep attacks, 88%
had cataplexy, 71% had interrupted nighttime sleep, 69% hallucinated, and 64%
experienced sleep paralysis. Results were appraised at three, six, and nine
weeks following onset of the trial.
Self-reported sleepiness (ESS) events were similar at onset and, in the placebo
group, at nine weeks. Otherwise, at week nine both modafinil cohorts showed less
sleepiness than controls (P < 0.001), with the 400 mg group significantly better
than the 200 mg group (P < 0.001). Sleep latency was similar between the two
modafinil groups but was significantly better than controls (P < 0.001).
Maintenance of wakefulness was better than control in both modafinil groups (P <
0.001) but not different between the two groups. Also, more subjects in the
modafinil groups remained awake longer than in the control group. Blinded
clinical assessment rated modafinil-taking patients as measurably improved
compared to the controls.
Complications were relatively low: one of the 200 mg dose cohort withdrew, as
did 11 (12%) of the 400 mg group. The only symptom significantly higher than
placebo was headache.
A subsequent open-label trial continues beyond the above blind control studies.
In that trial, clinical global impression showed 84% improvement by week two of
taking modafinil with the number rising to 91% by week 40. Both times had
significance at the P < 0.001 level. The authors indicate that "adverse
experiences were mostly mild to moderate." In the open trial, however, 25% of
patients withdrew because of side effects or lack of efficacy.
COMMENTARY
If its relatively low side effects continue, modafinil appears to be the first
non-toxic drug that can improve the disturbing symptoms of narcolepsy. The drug
clinically appears to reduce daytime sleepiness, and the result of latency tests
supported that conclusion. The general clinical appraisal of the participating
neurologists also concluded that wakefulness improved in the treated group. At
this writing, the reporting participating neurologists estimate that overall
efficacy of modafinil against narcolepsy amounts to about 55%, with Pemoline
providing about an equal help but with amphetamine or methylphenidate each
improving symptoms by about 80%. The latter level, however, produces a
relatively high incidence of unwanted symptoms. As the authors conclude, "
modafinil is a pharmacologically and clinically promising compound for treating
pathological daytime somnolence."
Modafinil is currently available in Europe and, I'm told, is well along the way
for FDA approval in the United States, possibly by late April or May 1998. -fp
LOAD-DATE: May 28, 2010
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newsletter
Copyright 1998 AHC Media LLC
All Rights Reserved
955 of 998 DOCUMENTS
The Practitioner
April 1998
New product information
SECTION: Pg. 314
LENGTH: 223 words
PROVIGIL (Modafinil, Cephalon UK)
Modafinil is a non-amphetamine wake promoting agent used for the treatment of
narcolepsy. It is also a non-controlled drug. Phase III clinical trials show
that treatment with the non-controlled modafinil reduces all measures of
sleepiness on physiological and clinical scales, as well as patients' own
self-assessments of sleepiness, without affecting night-time sleep.
Cephalon UK, tel 0800 783 4869.
COLAZIDE (Balsalazide, Astra Pharmaceuticals)
Balsalazide provides faster symptom relief and complete remission in a greater
proportion of patients with ulcerative colitis than delayed- release mesalazine,
according to studies. Improved rates of sigmoidoscopic healing have also been
shown. Balsalazide may be a suitable alternative for patients who fail
mesalazine therapy, says the manufacturer. Astra Pharmaceuticals, tel 01923
266191.
MUSE (Alprostadil, Astra Pharmaceuticals)
The Medicated Urethral System for Erection or MUSE? is a sterile single- use
transurethral system thatdelivers alprostadil directly to the male urethra. In
the form of a small pellet (1.4mm across by 3mm or 6mm in length depending on
the strength) contained in a narrow applicator, the treatment is inserted by
pressing a button on theapplicator. Astra Pharmaceuticals, tel 01923 266191.
LOAD-DATE: September 22, 1998
LANGUAGE: English
PUB-TYPE: Magazine
Copyright 1998 CMP Information Ltd
956 of 998 DOCUMENTS
Pharma Marketletter
March 5, 1998
Cephalon's Provigil Launched In UK
LENGTH: 155 words
Cephalon has launched Provigil (modafinil) in the UK for the treatment of
narcolepsy. This represents the first nonamphetamine-based therapy for this
indication to be made available in the UK and is the first narcolepsy drug to be
approved there for 40 years.
The recommended daily dose of modafinil is 200mg-400mg to be taken as two
divided doses in the morning and at noon, or as a single dose in the morning.
The cost to the National Health Service is L60 ($ 98.78) for 30 x 100mg tablets,
said a spokesperson for the company.
Modafinil has been available in France, under the brand name Modiodal, through
originator Laboratoire Lafon since 1994. Cephalon has exclusive marketing rights
in Japan, Mexico, Italy, Ireland and the USA, and marketing applications are
pending in the latter two countries. In December last year, the company received
an "approvable" letter from the US Food and Drug Administration.
LOAD-DATE: November 22, 2002
LANGUAGE: ENGLISH
Copyright 1998 Marketletter Publications Ltd.
957 of 998 DOCUMENTS
The Independent (London)
March 4, 1998, Wednesday
Wonder wake-up boosts alertness
BYLINE: Jeremy Laurance Health Editor
SECTION: NEWS; Page 6
LENGTH: 439 words
A WAKE-UP pill that increases alertness and boosts memory in people who are
sleep-deprived was launched yesterday. It is more effective than coffee but
lacks the side-effects of amphetamine-based stimulants. But it will not be
available to party-goers, students or armies preparing for a long march - yet.
Modafinil is a new pharmacological compound with a unique effect on the brain
that is not fully understood. It has been licensed in the UK as a treatment for
narcolepsy, a rare disorder marked by an intense and overwhelming need to sleep
that can strike at any time. Surveys show a third of people get less sleep than
they need, which is blamed on the invention of electricity. By extending the
waking day, modafinil could provide the pharmaceutical equivalent of the
electric light bulb.
Unlike amphetamines, which stimulate the nervous system, modafinil appears to
target the hypothalamus, the area of the brain thought to be responsible for
wakefulness. Tests in normal volunteers have shown it boosts cognitive
performance, especially memory, and reaction times in the sleep-deprived.
Its main advantage over amphetamines is that it does not produce the euphoria
associated with those drugs and is thought not to be addictive. Yet tests on
normal volunteers show it can keep people going through the night without
causing rebound depression or sleepiness.
Dr Colin Markland, medical director of Cephalon UK, which is marketing the drug,
to be called Provigil, in Britain, said there were no plans to explore its
potential as an alertness pill.
"All our activities have been in the area of narcolepsy. If we wanted to seek
another indication for the drug we would have to go back and conduct other
studies." Military organisations in France, where the drug was first licensed in
1994, the US and Britain are understood to have shown interest. There would be
an obvious military advantage in a pill that could help armies fight through the
day and march through the night.
Dr Markland that in the four years the drug had been available in France there
had been no evidence of abuse but this would be monitored in Britain. It is
available on prescription only and costs pounds 60 for 30 tablets of 100g.
The normal dose for treating narcolepsy would be 200g to 400g a day, costing up
to almost pounds 3,000 a year. If proved safe and effective, modafinil might
become a treatment for jet-lag or for disrupted sleep caused by shift work. But
by far its biggest potential market could be in the treatment of insomnia - by
preventing sleep during the day and thus promoting it at night.
LOAD-DATE: March 04, 1998
LANGUAGE: ENGLISH
Copyright 1998 Independent Print Ltd
958 of 998 DOCUMENTS
PR Newswire
March 4, 1998, Wednesday - 08:38 Eastern Time
Cephalon Launches PROVIGIL(R) (modafinil) in the United Kingdom.
SECTION: Financial News
LENGTH: 557 words
DATELINE: WEST CHESTER, Pa., March 4
Cephalon, Inc. (Nasdaq: CEPH) announced today the availability of PROVIGIL(R) (
modafinil) tablets in the United Kingdom for the treatment of narcolepsy. The
drug will be marketed to sleep specialists and neurologists in the United
Kingdom by Cephalon's U.K. subsidiary, which is based in Guildford, England.
"As the first non-amphetamine treatment for narcolepsy available in the U.K.,
PROVIGIL offers patients a new therapeutic alternative for the management of
daytime sleepiness associated with this debilitating disease," said Frank
Baldino, Jr., Ph.D., Cephalon's president and chief executive officer. "The
launch of PROVIGIL demonstrates our continued commitment to the sleep
community."
Dr. Adrian Williams, Director of the Sleep Disorders Center at St. Thomas'
Hospital in London describes the introduction of PROVIGIL as "a major step
forward in the treatment of narcolepsy. It is very exciting to be able to offer
patients a novel, effective and well tolerated medicine."
Narcolepsy is a chronic, neurological, lifelong sleep disorder that generally
begins in young adulthood. The most common symptom is excessive daytime
sleepiness, which is characterized by uncontrollable sleep attacks. These
attacks hamper a person's ability to perform basic daily activities. As a
result, narcolepsy significantly impacts a person's quality of life.
The most commonly observed adverse experiences associated with the use of
PROVIGIL, which occurred more frequently than placebo were: headache, nausea and
diarrhea.
Cephalon licensed modafinil from Laboratoire L. Lafon, the French pharmaceutical
company which discovered and markets the drug in France. Cephalon has exclusive
rights to market modafinil in the United States, Japan, the United Kingdom,
Ireland, Mexico and Italy. Cephalon has a marketing application currently
pending in the United States to market PROVIGIL for the treatment of excessive
daytime sleepiness associated with narcolepsy. In December 1997, Cephalon
received a letter from the U.S. FDA indicating that the company's application is
approvable, upon the satisfactory completion of product labeling and response to
the agency's comments. A marketing application is also pending in Ireland.
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company that discovers, develops and markets products to treat
neurological disorders.
This news release may contain forward-looking statements that involve
risks and uncertainties. A full discussion of Cephalon's operations and
financial condition, including factors that may affect the company's business
and future prospects, is contained in documents the company files with the
SEC, such as form 10-Q and 10-K reports. These documents identify important
factors that could cause the company's actual performance to differ from
current expectations.
NOTE: Cephalon's press releases are available by fax 24 hours a day at no
charge by calling PR Newswire's Company News On-Call at 800-758-5804,
extension 134563. They are also posted on the Internet at
http://www.prnewswire.com.
SOURCE Cephalon, Inc.
CONTACT: U.S., Kori Beer of Cephalon, 610-738-6532, or Europe, Jacinta
Collins of Sante Communications, 011-44-171-379-7377
LOAD-DATE: March 5, 1998
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
Copyright 1998 PR Newswire Association, Inc.
959 of 998 DOCUMENTS
Reuters Health Medical News
March 4, 1998 Wednesday
UK Medicines Control Agency Approves Modafinil For Narcolepsy
SECTION: REGULATORY
LENGTH: 222 words
DATELINE: LONDON Mar 4
Britain's Medicines Control Agency has approved modafinil (Provigil) for
treatment of narcolepsy in the UK, according to Cephalon UK Ltd.
Modafinil was developed by the private French company, Laboratoire Louis Lafon,
which launched the drug in France in 1994. Britain is the second European
country to market the medication, officials from Cephalon said at a news
briefing on Tuesday.
"This drug is the first alternative to amphetamines and amphetamine-like drugs.
It is the only drug specifically developed for the treatment of narcolepsy," Dr.
Colin G. Markland, medical director of Cephalon UK, told the briefing.
Cephalon has received rights from Lafon to market the drug in Britain as well as
in the US, Mexico, Japan, Ireland and Italy, according to Jason Rubin, vice
president for corporate communications of Cephalon, Inc.
Company officials said that they expect the medication to be approved by the
Food and Drug Administration in late spring or early summer.
The Medicines Control Agency has licensed modafinil in tablet form at a dosage
of 100 mg per tablet. For adults, the recommended daily dose is 200-400 mg.
"Provigil may be taken as two divided doses in the morning and at noon, or as a
single dose in the morning according to physician assessment of the patient and
the patient's response," the agency said in a statement.
LOAD-DATE: July 9, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 1998 Reuters Health
All Rights Reserved
960 of 998 DOCUMENTS
Pharma Marketletter
October 23, 1997
Provigil Cleared In UK
LENGTH: 101 words
Cephalon has been granted a license to market its narcolepsy drug Provigil (
modafinil) in the UK. This is first time that Cephalon has had a product
approved, and the company said it planned to launch it as soon as manufacturing
arrangements are finalized with the UK authorities. Modafinil is the first
narcolepsy drug to be approved there for 40 years.
Cephalon licenses modafinil from the French firm Laboratoires Lafon (which
already sells it in its home market) for sale in the UK, Japan, Mexico, the USA
and Ireland, and marketing applications are pending in the latter two countries.
LOAD-DATE: January 7, 2003
LANGUAGE: ENGLISH
Copyright 1997 Marketletter Publications Ltd.
961 of 998 DOCUMENTS
PR Newswire
October 20, 1997, Monday - 10:38 Eastern Time
Cephalon Granted Approval to Market Provigil in the United Kingdom
SECTION: Financial News
LENGTH: 500 words
DATELINE: WEST CHESTER, Pa., Oct. 20
Cephalon, Inc. (Nasdaq: CEPH) announced today that its U.K. subsidiary has been
granted a license by the Medicines Control Agency (MCA) to market PROVIGIL(R) (
modafinil) Tablets in the United Kingdom for the treatment of narcolepsy.
Narcolepsy is a chronic, lifelong sleep disorder that generally begins in young
adulthood. The most common symptom is excessive daytime sleepiness, which is
characterized by uncontrollable sleep attacks. These attacks hamper a person's
ability to perform basic daily activities. As a result, narcolepsy
significantly impacts a person's quality of life. Currently, amphetamines are
the only agents licensed to treat this disease in the United Kingdom.
Modafinil is a novel, non-amphetamine agent that Cephalon is developing for the
treatment of excessive daytime sleepiness associated with narcolepsy under a
license from Laboratoire L. Lafon, the French pharmaceutical company which
discovered and currently markets the drug in France. Cephalon has exclusive
rights to market modafinil in the United States, Japan, the United Kingdom,
Ireland and Mexico. Marketing applications are currently pending in the United
States and Ireland.
Cephalon intends to manufacture PROVIGIL tablets in the United States and launch
the drug in the United Kingdom upon MCA approval of these manufacturing
arrangements.
"The receipt of the company's first product license is an important milestone
for Cephalon," said Frank Baldino, Jr., Ph.D., Cephalon's president and chief
executive officer. "PROVIGIL is the first new therapy to treat narcolepsy in
the United Kingdom in over 40 years. Our U.K. sales and marketing organization
has been established and is enthusiastic about bringing PROVIGIL to the
neurology community for patients suffering from this debilitating disease."
Cephalon, Inc., headquartered in West Chester, PA, is an international
biopharmaceutical company that discovers, develops and markets products to treat
neurological disorders. The company is developing products for the treatment of
ALS, narcolepsy, peripheral neuropathies, Alzheimer's disease and stroke, and
currently copromotes three products in the United States for the treatment of
neurological conditions.
This news release may contain forward-looking statements that involve risks and
uncertainties. A full discussion of Cephalon's operations and financial
condition, including factors that may affect the company's business and future
prospects, is contained in documents the company files with the SEC, such as
form 10-Q and 10-K reports. These documents identify important factors that
could cause the company's actual performance to differ from current
expectations.
NOTE: Cephalon's press releases are available by fax 24 hours a day at no charge
by calling PR Newswire's Company News On-Call at 800-758-5804, extension 134563.
They are also posted on the Internet at http://www.prnewswire.com
SOURCE Cephalon, Inc.
CONTACT: Jason Rubin of Cephalon, 610-738-6302, or U.K. media, Liz Shanahan
of Sante Communications, 0171-379-7377, for Cephalon
LOAD-DATE: October 21, 1997
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
Copyright 1997 PR Newswire Association, Inc.
962 of 998 DOCUMENTS
Manufacturing Chemist
June 1997
CENTRAL STIMULANT - MODAFINIL
SECTION: Pg. 41
LENGTH: 277 words
Narcolepsy is an uncommon condition characterised by recurrent, unpredictable
and irresistible episodes of sleep, often with hallucinations and muscle
weakness. The attacks may occur several times a day, and are similar to those
that occur in idiopathic daytime sleepiness. These conditions have not always
been recognised, and it is thought that they may be the cause of some otherwise
inexplicable motoring and industrial accidents.
For treatment, reliance has been placed on the amphetamines and methylphenidate,
which are effective but carry the risk of inducing drug dependence. A new
alternative is modafinil.
* Although its action is not yet fully understood, it is known to differ from
that of other central stimulants. It is thought to decrease the brain level of
the neurotransmitter GABA, but its action probably involves the serotonic and
adrenergic receptor systems. In clinical studies, modafinil was given in
morning doses of 200mg, which brought about a significant reduction in the
frequency of sleep attacks in narcoleptic patients as well as improved alertness
during the first part of the day.
Sudden withdrawal of the drug after a course of treatment did not result in any
symptoms of drug dependence. The amount and quality of night-time sleep
remained unaffected, so modafinil appears to be a distinct advance in the
treatment of narcolepsy and idiopathic hypersomnia. It enables patients to play
a more normal part in social and occupational activities, and further studies
are in progress to assess the possible value of the drug in Parkinson's disease
and sleep apnoea.
Drugs of Today 23 (Suppl. 1)
LOAD-DATE: November 11, 1997
LANGUAGE: English
PUB-TYPE: Magazine
Copyright 1997 CMP Information Ltd
963 of 998 DOCUMENTS
Pharma Marketletter
January 13, 1997
Cephalon Files Modafinil Application In USA
LENGTH: 276 words
US biopharmaceutical company Cephalon Inc has now filed a New Drug Application
with the US Food and Drug Administration for marketing approval of modafinil,
its treatment for excessive daytime sleepiness associated with narcolepsy.
Modafinil was discovered by the French company Laboratoire Lafon, which has
granted exclusive marketing rights to Cephalon for the USA, Japan, the UK,
Ireland and Mexico. It is already approved and marketed in France for the
treatment of narcolepsy and idiopathic hypersomnia.
The FDA submission contains results of 14 clinical trials with modafinil
conducted by Cephalon, including two double-blind, placebo-controlled Phase III
studies involving 558 patients with narcolepsy. The Phase III studies were
conducted at 39 sleep centers in the USA and were designed to assess the
patient's ability to stay awake using a number of laboratory and clinical
measures. The studies also measured the patient's well-being, as assessed by an
independent clinician, and the patient's quality of life.
First NDA Filing By Cephalon For Cephalon this is an important milestone,
according to its president and chief executive, Frank Baldino; it is the
company's first NDA filing. Dr Baldino also noted: "to our knowledge, this is
the most comprehensive clinical investigation ever undertaken in the study of
narcolepsy."
Narcolepsy, a chronic, lifelong sleep disorder, affects around 125,000 people in
the USA alone. Therapies to treat excessive daytime sleepiness associated with
the disease have been limited to amphetamine and other stimulants. Modafinil was
designated an orphan drug by the FDA in March 1993.
LOAD-DATE: January 7, 2003
LANGUAGE: ENGLISH
Copyright 1997 Marketletter Publications Ltd.
964 of 998 DOCUMENTS
Reuters Health Medical News
January 1, 1997 Wednesday
Cephalon Submits NDA For Narcolepsy Drug
SECTION: REGULATORY
LENGTH: 174 words
DATELINE: WESTPORT Jan 1
Cephalon, based in West Chester, PA, announced yesterday that it has filed an
NDA with the FDA for clearance to market modafinil. Modafinil is designed to
treat patients with excessive daytime sleepiness associated with narcolepsy.
According to a company press release posted on PR Newswire, the NDA contained
data from 14 clinical studies of modafinil. Dr. Frank Baldino, Jr., president
and CEO of Cephalon, said, "As our first NDA submission, this event marks an
important milestone for Cephalon. To our knowledge, this is the most
comprehensive clinical investigation ever undertaken in the study of
narcolepsy."
The drug was developed by French pharmaceutical firm Laboratoire L. Lafon, which
currently markets modafinil in France to treat patients with narcolepsy and
idiopathic hypersomnia. Cephalon has exclusive rights to market the drug in the
U.S., U.K., Ireland, Mexico and Japan. According to Cephalon, if modafinil is
approved for marketing in the U.S., it would be the first new chemical entity
for narcolepsy in more than 20 years.
LOAD-DATE: July 9, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 1997 Reuters Health
All Rights Reserved
965 of 998 DOCUMENTS
PR Newswire
December 31, 1996, Tuesday - 08:01 Eastern Time
Cephalon Submits New Drug Application For Modafinil to U.S. Food and Drug
Administration
SECTION: Financial News
LENGTH: 599 words
DATELINE: WEST CHESTER, Pa., Dec. 31
Cephalon, Inc. (Nasdaq: CEPH) announced today that the company has submitted a
New Drug Application (NDA) to the U.S. Food and Drug Administration for
clearance to market modafinil for use in treating excessive daytime sleepiness
associated with narcolepsy.
The NDA contains results of 14 clinical studies with modafinil conducted by
Cephalon, including two double-blind, placebo-controlled multicenter Phase 3
trials involving 558 patients with narcolepsy. The Phase 3 studies were
conducted at 39 sleep centers in the United States and were designed to assess
the patient's ability to stay awake using a number of laboratory and clinical
measures. The studies also measured the patient's overall well-being, as
assessed by an independent clinician, and the patient's quality of life.
"As our first NDA submission, this event marks an important milestone for
Cephalon," said Frank Baldino, Jr., Ph.D., Cephalon's president and chief
executive officer. "To our knowledge, this is the most comprehensive clinical
investigation ever undertaken in the study of narcolepsy. We are grateful to
the patients who participated in these studies, and appreciate the dedication of
the physicians and Cephalon employees who are working to improve the lives of
patients with this chronic and debilitating disease."
Modafinil is a novel oral medication that is approved and marketed in France for
the treatment of narcolepsy and idiopathic hypersomnia. Cephalon received
exclusive rights to market modafinil in the United States, Japan, the United
Kingdom, Ireland and Mexico from Laboratoire L. Lafon, the French pharmaceutical
company which developed and currently markets the drug in France. If approved
in the United States, modafinil would be the first new chemical entity available
to treat narcolepsy in more than 20 years.
Narcolepsy is a chronic, lifelong sleep disorder afflicting approximately
125,000 people in the United States. The most common symptom is excessive
daytime sleepiness. Narcolepsy generally begins in young adulthood. Therapies
to treat the excessive daytime sleepiness associated with the disease have been
limited to amphetamine and other stimulants. The FDA designated modafinil an
orphan drug in March 1993 for the treatment of excessive daytime sleepiness in
narcolepsy.
Cephalon is an international biopharmaceutical company that discovers, develops
and markets products to treat neurological disorders. The company is developing
products for the treatment of ALS, narcolepsy, peripheral neuropathies,
Alzheimer's disease, head and spinal injury, and stroke, and currently
copromotes two products in the United States for the treatment of neurological
conditions.
This news release may contain forward-looking statements that involve risks and
uncertainties. The results of the modafinil clinical trials have not been
reviewed by the FDA and there can be no assurance that the FDA will consider
that these results demonstrate sufficient safety and efficacy data to allow the
filing of an NDA to obtain marketing clearance or if the filing is allowed, to
obtain marketing clearance. A full discussion of Cephalon's
operations and financial condition, including factors that may affect the
company's business and future prospects, is contained in documents the company
files with the SEC, such as form 10-Q and 10-K reports. These documents
identify important factors that could cause the company's actual performance
to differ from current expectations.
SOURCE Cephalon, Inc.
CONTACT: Jason Rubin or Kori Beer of Cephalon, 610-344-0200
LOAD-DATE: January 1, 1997
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
Copyright 1996 PR Newswire Association, Inc.
966 of 998 DOCUMENTS
Financial Post Daily
August 9, 1996
Draxis files for use of sleep-disorder drug
SECTION: Pg. v.9(108) August 9, 1996 pg 47
LENGTH: 89 words
Pharmaceutical company Draxis Health has filed a new drug
submission with Canada's health protection branch to market the
sleep disorder drug Modafinil.
In February, Draxis reported
statistically significant results for its clinical study of the drug
in treatment of narcolepsy, which affects 0.05% to 0.1% of
Canadians. No new drug for narcolepsy had been approved in Canada
since 1959. Modafinil is used in France, and Draxis has an exclusive
licence from Laboratoire L. Lafon to market and sell the product in
Canada.
*** END OF DOCUMENT ***
LOAD-DATE: July 08, 1999
LANGUAGE: ENGLISH
ACC-NO: 3680885
DOCUMENT-TYPE: Fulltext; News article
PUBLICATION-TYPE: Other
JOURNAL-CODE: 0341
Copyright 1996 Micromedia Limited
All Rights Reserved
Canadian Business and Current Affairs
967 of 998 DOCUMENTS
Canada NewsWire
August 8, 1996, Thursday
DRAXIS FILES NEW DRUG SUBMISSION FOR MODAFINIL IN CANADA
SECTION: Financial News
LENGTH: 481 words
DATELINE: TORONTO, Aug. 8
DRAXIS Health Inc. (Toronto Stock Exchange: DAX; Nasdaq: DRAXF) today announced
that it has filed a New Drug Submission with Canada's Health Protection Branch
to market Modafinil in Canada for use in treating narcolepsy, a sleep disorder
characterized by uncontrolled episodes of falling asleep at unexpected times or
in unexpected circumstances. In February 1996 DRAXIS reported statistically
significant results for its one-year-long, double-blind, randomized,
placebo-controlled, cross-over clinical study of 200 milligram and 400 milligram
dosages of Modafinil in the treatment of narcolepsy. The primary sleep disorder
affects approximately 0.05 percent to 0.1 percent of the population or
approximately 14,800 to 29,600 Canadians. No new treatment for narcolepsy has
been approved in Canada since 1959. "We are very excited about the prospects
for Modafinil," Dr. Martin Barkin, M.D., stated in making the announcement. "Our
clinical trials showed that Modafinil produced a highly statistically
significant benefit in reducing excessive daytime sleepiness in patients with
narcolepsy and had a good tolerance profile. We also believe that Modafinil has
a low potential for abuse, which gives it a further advantage. Subject to
receiving health regulatory approval, Modafinil will be a significant addition
to the DRAXIS line of neurological products." Modafinil is approved for the
treatment of narcolepsy in France. DRAXIS has an exclusive license from
Laboratoire L. Lafon to market and sell Modafinil in Canada. The licensee for
the United States, United Kingdom and Japan is Cephalon Inc.(Nasdaq: CEPH).
DRAXIS Health Inc., based in Toronto, is an emerging Canadian pharmaceutical
company focused on neurological, dermatological and veterinary markets in Canada
and the United States. Products under development include Modafinil for
narcolepsy and proprietary liposomed topical products for both the prescription
and over-the-counter markets. The company's U.S. units include a division
offering products exclusively to podiatrists and a 50 percent interest in a
consumer products company specializing in cosmeceuticals and nutriceuticals.
DRAXIS holds a controlling interest in Deprenyl Animal Health, Inc. (TSE: DAH;
Nasdaq OTC Bulletin Board: DAHI), which has filed for U.S. approval of its
proprietary compound Aniprylr for canine Cushing's disease. Factors that could
cause forward-looking statements in this news release to differ materially from
actual results are discussed in the company's Form 20F and other periodic
filings with the U.S. Securities and Exchange Commission and Canada's securities
authorities. To receive additional information on DRAXIS Health Inc., via fax
at no charge, dial 1-800-PRO-INFO and enter code DRAXF.
SOURCE Draxis Health, Inc.
-30-
For further information: Dr. Martin Barkin, M.D., DRAXIS Health Inc. (905)
677-5500, or U.S. Investor Relations: The Financial Relations Board -- Jeffrey
D. Bogart, (212) 661-8030, or Canadian Investor Relations: Small-Cap Equity
Investor Relations Ltd. -- Robert Grahovar, (416) 368-7459
LOAD-DATE: August 8, 1996
LANGUAGE: ENGLISH
Copyright 1996 Canada NewsWire Ltd.
968 of 998 DOCUMENTS
PR Newswire
August 8, 1996, Thursday - 09:28 Eastern Time
Draxis Files New Drug Submission for Modafinil in Canada
SECTION: Financial News
LENGTH: 476 words
DATELINE: TORONTO, Aug. 8
DRAXIS Health Inc. (Toronto Stock Exchange: DAX; Nasdaq: DRAXF) today announced
that it has filed a New Drug Submission with Canada's Health Protection Branch
to market Modafinil in Canada for use in treating narcolepsy, a sleep disorder
characterized by uncontrolled episodes of falling asleep at unexpected times or
in unexpected circumstances.
In February 1996 DRAXIS reported statistically significant results for its
one-year-long, double-blind, randomized, placebo-controlled, cross-over clinical
study of 200 milligram and 400 milligram dosages of Modafinil in the treatment
of narcolepsy. The primary sleep disorder affects approximately 0.05 percent to
0.1 percent of the population or approximately 14,800 to 29,600 Canadians. No
new treatment for narcolepsy has been approved in Canada since 1959.
"We are very excited about the prospects for Modafinil," Dr. Martin Barkin,
M.D., stated in making the announcement. "Our clinical trials showed that
Modafinil produced a highly statistically significant benefit in reducing
excessive daytime sleepiness in patients with narcolepsy and had a good
tolerance profile. We also believe that Modafinil has a low potential for
abuse, which gives it a further advantage. Subject to receiving health
regulatory approval, Modafinil will be a significant addition to the DRAXIS line
of neurological products."
Modafinil is approved for the treatment of narcolepsy in France. DRAXIS has an
exclusive license from Laboratoire L. Lafon to market and sell Modafinil in
Canada. The licensee for the United States, United Kingdom and Japan is
Cephalon Inc.(Nasdaq: CEPH).
DRAXIS Health Inc., based in Toronto, is an emerging Canadian pharmaceutical
company focused on neurological, dermatological and veterinary markets in Canada
and the United States. Products under development include Modafinil for
narcolepsy and proprietary liposomed topical products for both the prescription
and over-the-counter markets. The company's U.S. units include a division
offering products exclusively to podiatrists and a 50 percent interest in a
consumer products company specializing in cosmeceuticals and nutriceuticals.
DRAXIS holds a controlling interest in Deprenyl Animal Health, Inc. (TSE: DAH;
Nasdaq OTC Bulletin Board: DAHI), which has filed for U.S. approval of its
proprietary compound Aniprylr for canine Cushing's disease.
Factors that could cause forward-looking statements in this news release to
differ materially from actual results are discussed in the company's Form 20F
and other periodic filings with the U.S. Securities and Exchange Commission and
Canada's securities authorities.
To receive additional information on DRAXIS Health Inc., via fax at no charge,
dial 1-800-PRO-INFO and enter code DRAXF.
SOURCE Draxis Health, Inc.
CONTACT: Dr. Martin Barkin, M.D., DRAXIS Health Inc. 905-677-5500, or U.S.
Investor Relations: The Financial Relations Board -- Jeffrey D. Bogart,
212-661-8030, or Canadian Investor Relations: Small-Cap Equity Investor
Relations Ltd. -- Robert Grahovar, 416-368-7459
LOAD-DATE: August 9, 1996
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS EDITOR
Copyright 1996 PR Newswire Association, Inc.
969 of 998 DOCUMENTS
Biotechnology Newswatch
August 5, 1996
Narcolepsy research gets wake-up call: first new drug in two decades
BYLINE: By Steve Carrell
SECTION: Pg. 13
LENGTH: 346 words
The first new narcolepsy treatment in more than two decades made a solid showing
in studies presented at the recent Association of Professional Sleep Societies
(APSS) convention.
The results triggered a publicity wave lasting weeks after researchers presented
results of their multi-center studies on modafinil (Provigil). The next news on
Cephalon, Inc.'s drug may come when the firm files modafinil's New Drug
Application, probably late this year.
Narcolepsy affects an estimated 125,000 people nationwide. But there's
widespread agreement the ailment is under-diagnosed, and the lag between onset
and diagnosis often spans 10 years. So the actual patient population could be
250,000 or more, said Marguerite Utley, a board member of the Cincinnati-based
Narcolepsy Network.
Cephalon showcased the material at a company-sponsored symposium during the busy
meeting, which is the combined conventions of the American Sleep Disorders
Association and the Sleep Research Society.
U.S. researchers presented partial results of two Phase III trials with a total
of 558 patients. Discussants covering results of the first trial included
principal investigator Merrill Mitler, director of sleep research at the Scripps
Clinic and Research Foundation in La Jolla, Calif.
Cephalon officials summarized the second study during a briefing for stock
analysts. In the studies, modafinil kept patients awake 50 percent to 75 percent
longer than placebo, as measured by the Mean Wakefulness Time (MWT) test.
On the physicians' Clinical Global Impressions scale, modafinil patients scored
20 - 40 points higher than placebo patients. Both tests produced statistically
significant and clinically meaningful scores, researchers said.
Speakers at the symposium also noted that side effects, mainly headache, were
minimal and easily controllable and abuse potential is low. Such data helped
make Cephalon a ''strong buy'' recommendation, said stock analyst Joyce
Lonergan, who attended the meetings. She works for the investment banking firm
Cowen & Co. in Boston.
URL: http://www.platts.com
LOAD-DATE: August 27, 1996
LANGUAGE: ENGLISH
Copyright 1996 McGraw-Hill Inc.
970 of 998 DOCUMENTS
The New York Times
June 11, 1996, Tuesday, Late Edition - Final
Research Suggests Sleep Seizures May Be Linked to Immune System
BYLINE: By WARREN E. LEARY
SECTION: Section C; Page 3; Column 4; Science Desk; Medical Science Page
LENGTH: 1590 words
DATELINE: WASHINGTON
AFTER decades of slow progress in understanding narcolepsy, a disorder
characterized by sudden seizures of sleepiness, researchers say it may be linked
to the immune system and may also be as prevalent in women as it is in men.
Scientists say they are beginning to see narcolepsy as a disorder with both
genetic and environmental components, even though the exact cause remains
unknown. Studies of identical twins, for example, indicate that in only about 20
percent of cases do both develop narcolepsy. This, experts say, indicates the
incurable condition must be triggered by some environmental factors.
Research with humans and animals also suggests that the condition may involve
genetic factors. And although no one has proved it, some suggest that narcolepsy
may be a type of autoimmune disease, in which the body attacks some part of
itself, that is unlike any other form of that disorder.
Dr. Emmanuel Mignot, director of the Stanford University Center for Narcolepsy,
said Japanese scientists first discovered a gene associated with the condition.
That gene was near a location for another gene for a human leucocyte antigen, or
H.L.A. Other H.L.A. genes, which are involved with control of the immune
system, were identified at Stanford to have an association with narcolepsy.
However, while these H.L.A. genes are found in more than 95 percent of
narcolepsy patients, and serve as markers to help diagnose the disease, experts
said, they also are found in 25 percent of those without the disease.
Finding an H.L.A. association suggests that the immune system is involved in the
pathology of the disease, or that an unidentified susceptibility gene is
situated very close to the H.L.A. gene, Dr. Mignot said.
"Most diseases with an H.L.A. association are autoimmune by nature, but all
attempts to prove narcolepsy is an autoimmune disease have failed," Dr. Mignot
said in an interview. "It looks like an autoimmune disease, but does not
manifest itself as one. I believe it is a new type of autoimmune disease that
may affect a very limited area of the brain, but there is no proof -- yet."
The best animal models for narcolepsy are dogs, some of which naturally develop
a form of the disease that appears almost identical to the human variety. A
colony of 30 narcoleptic Doberman pinschers at Stanford is the largest in the
country.
Dogs have leucocyte antigen genes similar to those in humans. Those genes in the
narcoleptic Dobermans also did not appear to be involved with the canine
disease, Stanford researchers said. However, they said, studies indicate the
canine narcolepsy gene is linked with a gene that may be responsible for
switching on antibodies, another indication that the immune system is involved.
While research continues on the basic science of narcolepsy, doctors treating
the condition are excited about a new drug that appears to help patients stay
alert without being a stimulant. Modafinil, being developed under the name
Provigil by Cephalon Inc. of West Chester, Pa., appears to help patients stay
awake with far fewer side effects than current drugs, researchers say.
At the annual meeting of the Associated Professional Sleep Societies this month
in Washington, researchers reported that a clinical trial of modafinil at 21
medical centers in the nation showed the drug to be "significantly effective."
The 273 narcoleptic patients involved took the drug once a day in doses of 200
or 400 milligrams or received a dummy pill for nine weeks followed by a two-week
observation period. Laboratory tests showed patients taking modafinil stayed
awake at least 50 percent longer than those receiving the dummy drug,
researchers said. Patient evaluations by independent doctors not participating
in the study indicated that 60 percent of patients receiving the higher dose and
57 percent of those on the lower-dose regimen showed improvement in disease
symptoms, as against 37 percent for those taking the fake drug.
The company, which said the results were similar to those of an earlier trial
conducted with 285 patients at 18 centers, said it would review the results with
the Food and Drug Administration and apply to market the drug in the United
States. In 1993, the Food and Drug Administration designated modafinil as an
orphan drug, one given special licensing protection to encourage its development
for a condition for which there is not a large market.
Dr. June M. Fry of the Medical College of Pennsylvania and Hahnemann University,
in Philadelphia, called it "exciting that we are on the brink of a new
medication for our patients." Modafinil was not tested in the most severe cases
and may not work for everyone, said Dr. Fry, a leader in the study.
Dr. Dale M. Edgar of Stanford University Medical School, another principal in
the study, said no one was sure how modafinil worked. But the drug, developed in
France, is not like the amphetamine-like stimulants most often used now.
Even with progress in basic research and treatment, narcolepsy researchers say
progress is being hampered by a shortage of research money and a lack of
understanding of how devastating narcolepsy can be to sufferers.
"Narcolepsy is a significant problem and is often a disabling disease," said Dr.
Michael S. Aldrich, director of the University of Michigan's Sleep Disorders
Center in Ann Arbor. "But because it involves sleep, which people see as benign,
and doesn't cause death or put people in wheelchairs, its been underemphasized."
Experts say the Federal Government only spends about $2.5 million a year on
research into narcolepsy, which afflicts 125,000 to 250,000 Americans. That is
less than one-tenth the amount for multiple sclerosis, which afflicts about as
many people.
People with narcolepsy, who are constantly tired and easily fatigued, have bouts
of excessive daytime sleepiness lasting from a few seconds to more than 30
minutes. They fall asleep not only in normally restful situations, but also at
inappropriate times, sometimes during conversations or while driving a car.
In up to 80 percent of cases, these sleep seizures are accompanied by a decrease
or loss of muscle control called cataplexy, which can cause the head or jaw to
droop or the whole body to collapse, the National Sleep Foundation says.
Narcoleptics also experience hypnagogic hallucinations, dreamlike visual and
auditory hallucinations that come on quickly while dozing and falling asleep.
More than 60 percent of narcoleptics also suffer with bouts of sleep paralysis,
a frightening symptom that keeps a patient from moving for several minutes,
often upon falling to sleep or awaking.
Narcolepsy has an incidence of 1 to 2 cases per 2,000 people in the United
States, Europe and Japan. Symptoms generally begin to appear between the onset
of puberty and the age of 25 and the chronic condition gets progressively worse.
Specialists say diagnosis and initial treatment are often delayed for years
because patients and doctors do not readily recognize daytime sleepiness as a
sign of disease.
Until as recently as five years ago, many believed narcolepsy was four times
more common in men than women. However, while some experts still believe men are
slightly more susceptible than women, most specialists now believe the wide
gender gap never existed.
Dr. Meeta Goswami, director of the Narcolepsy Institute at Montefiore Medical
Center in the Bronx, and other experts say the condition is most noticeable in
the workplace and until more women started working outside the home, many female
sufferers were missed.
The psychological and social consequences of narcolepsy can be severe, experts
said, and are usually worse the later it takes to diagnose the problem. "Those
who are diagnosed early know they have a treatable disease and adjust for it,"
said Dr. Goswami, whose center has state financing to offer support services to
narcoleptics throughout New York City. "People who have gone for years not
knowing what was wrong tend to have low self-esteem, feelings of hopelessness
and worthlessness, and social problems. Major social consequences of narcolepsy
include a higher-than-normal divorce rate and clinical depression, which has to
be treated separately."
People who are not familiar with narcolepsy often interpret the symptoms as
signs sufferers are uninterested, disrespectful or lazy, which can be
detrimental to careers and social lives, Dr. Goswami said.
Dr. Merrill M. Mitler, director of sleep research at the Scripps Clinic and
Research Center in San Diego, said most patients with narcolepsy were
successfully treated with amphetamine-like compounds such as methylphenidate and
dextroamphetamine, or other stimulants, like Pemoline and Ritalin, to ward off
sleepiness. Many patients also receive antidepressant drugs to counteract
cataplexy, hallucinations and sleep paralysis.
More than 80 percent of patients can be successfully treated with drugs that
sharply reduce their symptoms, Dr. Mitler said, but doses may have to be
modified or medications changed over time as their bodies get used to the
treatments.
Dr. Aldrich, of the University of Michigan, said some patients also responded to
sleep therapy along with drugs. With this, doctors prescribe a sleep regimen of
set bedtimes and daytime naps which helps some patients get through the day with
fewer unexpected sleep episodes. "Naps can't be the whole answer, but sometimes
they can help," he said, "Narcoleptics do worse if they don't get enough sleep.
It just compounds the problem."
LOAD-DATE: June 11, 1996
LANGUAGE: ENGLISH
GRAPHIC: Photo: Emotional excitement induces cataplexy, a rapid eye movement
sleep with muscle relaxation, in both human and canine narcolepsy. When a
narcoleptic dog like this Doberman pinscher is excited by food, the most
powerful emotional stimulus for dogs, a cataplectic attack occurs, and the dog
finally collapses (lower right). (Courtesy of the Sleep Disorder Center,
Stanford University)
Copyright 1996 The New York Times Company
971 of 998 DOCUMENTS
Pharma Marketletter
March 25, 1996
Positive Results From Second PhII Modafinil Study
LENGTH: 63 words
Cephalon of the USA has reported positive results from its second Phase III
study of Provigil (modafinil), the narcolepsy treatment licensed from Lafon of
France. The 273-patient study found that modafinil was able to increase
patients' ability to stay awake, measured by the maintenance of wakefulness test
and clinical global impression of change, compared to placebo.
LOAD-DATE: January 7, 2003
LANGUAGE: ENGLISH
Copyright 1996 Marketletter Publications Ltd.
972 of 998 DOCUMENTS
Reuters Health Medical News
March 15, 1996 Friday
[] - Cephalon Says Modafinil Effective In Patients With Narcolepsy
LENGTH: 108 words
DATELINE: WEST CHESTER, Pa. Mar 14
Cephalon Inc said on Thursday that results from its second Phase III clinical
trial of its modafinil product, Provigil, in patients with narcolepsy showed
that Provigil increased patients' ability to stay awake. Cephalon said the
results follow positive findings from its first U.S. Phase III clinical study of
Provigil.
Cephalon is planning to review the findings of both Phase III studies with the
FDA and to submit a New Drug Application to the agency for clearance to market
Provigil in the United States. The FDA designated modafinil an orphan drug in
March, 1993, for the treatment of excessive daytime sleepiness in patients with
narcolepsy.
LOAD-DATE: July 9, 2008
LANGUAGE: ENGLISH
PUBLICATION-TYPE: Newswire
Copyright 1996 Reuters Health
All Rights Reserved
973 of 998 DOCUMENTS
PR Newswire
March 14, 1996, Thursday - 07:58 Eastern Time
CEPHALON ANNOUNCES SECOND POSITIVE PHASE III MODAFINIL STUDY IN NARCOLEPSY
SECTION: Financial News
LENGTH: 831 words
Cephalon, Inc. (Nasdaq: CEPH) announced today that results from its second Phase
III clinical trial of Provigil(TM) (modafinil) in patients with narcolepsy
demonstrated that Provigil had a significant benefit in increasing patients'
ability to stay awake as measured by the maintenance of wakefulness test (MWT),
and in improving patients' overall condition as measured by the clinical global
impression of change (CGI-C), the two primary endpoints of the study.
The double-blind, placebo-controlled study of 273 patients with narcolepsy was
conducted at 21 medical centers in the United States. Patients were randomized
to receive once-daily doses of placebo, 200 or 400 milligrams of Provigil for
nine weeks, followed by a two-week observation period.
The MWT is a daytime laboratory test of a person's ability to stay awake over
time. Patients who received 200 or 400 mg of Provigil stayed awake
approximately 50 percent longer than patients who received placebo (p<0.001).
WEST CHESTER, Pa., March 14
The CGI-C is a seven-point scale used in many clinical trials to evaluate
changes in a patient's overall disease status from the time of study entry.
These impressions of change range from very much worse to no change to very much
improved. In this study, CGI-C assessments were made by independent clinicians
who did not participate in any other aspects of the study. Sixty percent of
patients who received 400 mg of Provigil (p<0.001) and 57 percent of those who
received 200 mg of Provigil (p<0.001) demonstrated improvement on this scale
compared to 37 percent of patients who received placebo.
In February, Cephalon reported positive findings from the first U.S. Phase III
clinical study of Provigil, which was conducted at 18 medical centers in the
United States and involved 285 patients with narcolepsy. In that study, patients
randomized to receive 200 or 400 milligrams of Provigil stayed awake up to 61
percent (p<0.001) and 76 percent (p<0.001) longer, respectively, than those who
received placebo. Also, for the CGI-C, 72 percent of patients who received 400
mg of Provigil (p<0.001) and 65 percent of those who received 200 mg of Provigil
(p<0.001) demonstrated improvement compared to 37 percent who received placebo.
"Patients with narcolepsy face tremendous physical, social and economic
challenges as a result of their inability to stay awake," said Michael F.
Murphy, M.D., Ph.D., senior vice president of worldwide clinical research at
Cephalon. "The primary objective of these studies was to evaluate modafinil's
effects on excessive daytime sleepiness, the most common symptom of this
disease. The results of these studies offer clear evidence, from both
laboratory tests and physician assessments, that modafinil provides clinically
important benefits to the patient."
Provigil was well-tolerated at both doses. The most frequent adverse event
reported in both studies was headache. In the first study, headache was
transient and usually mild, with approximately 15 percent greater incidence in
the drug group compared to placebo. In the second study, there were no
significant differences in the incidence of headache between the drug and
placebo groups. The only consistently observed adverse event related to drug in
both studies was dry mouth, which occurred in approximately 5 percent of
patients in the drug group.
The efficacy and safety results of both Phase III studies of Provigil, as well
as findings from preclinical and other clinical studies of the drug, will be
reported by investigators at the Association of Professional Sleep Societies
annual meeting on May 31, 1996, in Washington, D.C.
Cephalon is planning to review these findings with the U.S. Food and Drug
Administration and to submit a New Drug Application to the FDA for clearance to
market Provigil in the United States.
Narcolepsy is a chronic, lifelong sleep disorder afflicting approximately
125,000 people in the United States. The four most common symptoms are
excessive daytime sleepiness, cataplexy, sleep paralysis and hypnagogic
hallucinations. Narcolepsy generally begins in young adulthood. Therapies to
treat the disease have been limited to amphetamine and other stimulants.
Cephalon licensed exclusive rights to market modafinil in the United States,
Japan, the United Kingdom, Ireland and Mexico from Laboratoire L. Lafon, a
French pharmaceutical company which developed and currently markets the drug in
France. The FDA designated modafinil an orphan drug in March 1993 for the
treatment of excessive daytime sleepiness in narcolepsy.
Cephalon discovers, develops and markets products to treat neurological
disorders. The company's principal focus is on neurological disorders such as
ALS, narcolepsy, peripheral neuropathies, Alzheimer's disease, head and spinal
injury, and stroke.
// CONTACT: Jason Rubin or Mary Fisher of Cephalon, 610-344-0200
LOAD-DATE: March 15, 1996
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
Copyright 1996 PR Newswire Association, Inc.
974 of 998 DOCUMENTS
Pharma Marketletter
March 4, 1996
Modafinil Filed In Canada By End-96?
LENGTH: 157 words
Draxis Health, the firm which holds Canadian rights to the narcolepsy drug
modafinil, expects to file for approval of the drug by year-end. Modafinil was
originally developed by France's Lafon, and is licensed by Cephalon in the USA,
the UK and Japan (Marketletters passim).
Draxis has reported the results of a 75-patient study of modafinil, which
reveals that in patients who had received no prior treatment with stimulants, a
decrease in daytime sleepiness was reported in 80% of those taking modafinil
400mg/day, 66% of those taking 200mg/day and 34% of those on placebo. In
previously-treated patients, the values were 53%, 50% and 25% respectively.
Modafinil was found to have no adverse effects on mood, with a single exception.
At the 400mg/day dose, the drug increased tension-anxiety compared to placebo.
However, the scores were still well below pre-study values. Vigor-activity
scores were increased by modafinil.
LOAD-DATE: January 7, 2003
LANGUAGE: ENGLISH
Copyright 1996 Marketletter Publications Ltd.
975 of 998 DOCUMENTS
Business Wire
February 28, 1996, Wednesday
DRAXIS' Modafinil trial results are statistically significant; new treatment for
Narcolepsy
LENGTH: 771 words
DATELINE: MISSISSAUGA, Ontario
Feb. 28, 1996--DRAXIS Health Inc. (TSE:DAX;NASDAQ:DRAXF) Wednesday reported
statistically significant results of its one-year long double-blind randomized
placebo-controlled cross-over clinical study of Modafinil 200 mg and Modafinil
400 mg in the treatment of Narcolepsy.
Seventy-five patients were each studied over a six-week period during which each
patient was given placebo, 200 mg or 400 mg of Modafinil in divided doses.
The primary end points were sleep latency (the time from lights out to sleep
onset) during the Maintenance of Wakefulness Test (a daytime sleep laboratory
test) and daily sleep episodes recorded in the patient dairy. Modafinil
significantly increased the mean sleep latency (the time taken to fall asleep).
The 200 mg dose was 40% better than placebo (p=.002) and the 400 mg dose was 54%
better than placebo (p=.001). The 200 mg dose reduced the mean number of
periods of sleep and severe somnolence by 24% (p=.013) and the 400 mg dose by
27% (p=.008).
Among those patients taking no stimulant medication prior to the study, a
comparative decrease in excessive daytime somnolence was reported by 80% of the
patients while on Modafinil 400 mg, 66% while on Modafinil 200 mg and 34% while
on placebo. Among those patients treated with stimulants prior to the study the
comparative differences were 53%, 50% and 25% for Modafinil 400 mg, Modafinil
200 mg and placebo respectively. Conversely, patients previously treated who
reported deterioration while on the study were for placebo 58%, Modafinil 200 mg
25%, and Modafinil 400 mg 33%.
Using the Epworth Sleepiness Scale, Modafinil 200 mg (p=.018) and 400 mg
(p=.009) both decreased the likelihood of falling asleep.
The Profile of Mood States (POMS) test was used to evaluate changes in mood,
specifically tension-anxiety, anger-hostility, confusion-bewilderment,
vigor-activity, and fatigue-inertia. Modafinil had no adverse effects on mood,
with a single exception. Modafinil 400 mg slightly increased tension-anxiety
compared to placebo (p=.028); but the scores were still well below both the
pre-study scores and published normal scores for this factor. Vigor-activity
increased after Modafinil 200 mg (p=.018) and 400 mg (p=.012).
Neither dose of Modafinil interfered with the patient's ability to sleep
voluntarily during the day nor did either dose interfere with the quantity or
quality of nocturnal sleep.
Only one patient dropped out of the study due to side effects of Modafinil. The
principle side effects were headache, nausea, dry mouth, heartburn, diarrhea,
and dizziness. The side effects were generally limited to the first few days of
treatment.
Narcolepsy is a primary sleep disorder characterized by uncontrolled episodes of
falling asleep at unexpected times and conditions. It affects approximately
0.05% to 0.1% of the population or approximately 14,800 to 29,600 Canadians. No
new treatment for Narcolepsy has been approved in Canada since 1959.
The full results of this study will be used by the company to complete its
submission for regulatory approval in Canada. This file is expected to be ready
for submission to Canadian Health Regulatory authorities towards the end of
1996.
Modafinil is approved for the treatment of Narcolepsy in France. DRAXIS has an
exclusive license to market and sell Modafinil in Canada. The licensor for the
US, UK and Japan is Cephalon Inc. (NASDAQ:CEPH).
DRAXIS, is a marketing and research company that operates Canadian Neurological,
Dermatological, and Veterinary pharmaceutical divisions, a U.S. consumer
marketing company, and offers products exclusively through U.S. podiatrists.
CONTACT: DRAXIS Health Inc.
Kendall McAlister, Coordinator, External Relations
905/677-5500; Fax 905/677-5502
or
Canadian Investor Relations
Small-Cap Equity Investor Relations Ltd.
Robert Grahovar
416/535-4146
or
U.S. Investor Relations
RKC Communications
Robert Kneeley, 954/351-1976
LOAD-DATE: February 29, 1996
LANGUAGE: ENGLISH
DISTRIBUTION: Business Editors
Copyright 1996 Business Wire, Inc.
976 of 998 DOCUMENTS
Canada NewsWire
February 28, 1996, Wednesday
Attention Business/Health Editors: DRAXIS' MODAFINIL TRIAL RESULTS ARE
STATISTICALLY SIGNIFICANT NEW TREATMENT FOR NARCOLEPSY
SECTION: Financial News
LENGTH: 632 words
DATELINE: MISSISSAUGA, Ont., Feb. 28
DRAXIS Health Inc. (TSE:DAX; NASDAQ:DRAXF) today reported statistically
significant results of its one-year long double-blind randomized
placebo-controlled cross-over clinical study of Modafinil 200 mg and Modafinil
400 mg in the treatment of Narcolepsy. Seventy-five patients were each studied
over a six-week period during which each patient was given placebo, 200 mg or
400 mg of Modafinil in divided doses. The primary end points were sleep latency
(the time from lights out to sleep onset) during the Maintenance of Wakefulness
Test (a daytime sleep laboratory test) and daily sleep episodes recorded in the
patient diary. Modafinil significantly increased the mean sleep latency (the
time taken to fall asleep). The 200 mg dose was 40% better than placebo (p
equals .002) and the 400 mg dose was 54% better than placebo (p equals .001).
The 200 mg dose reduced the mean number of periods of sleep and severe
somnolence by 24% (p equals .013) and the 400 mg dose by 27% (p equals .008).
Among those patients taking no stimulant medication prior to the study, a
comparative decrease in excessive daytime somnolence was reported by 80% of the
patients while on Modafinil 400 mg, 66% while on Modafinil 200 mg and 34% while
on placebo. Among those patients treated with stimulants prior to the study the
comparative differences were 53%, 50% and 25% for Modafinil 400 mg, Modafinil
200 mg and placebo respectively. Conversely, patients previously treated who
reported deterioration while on the study were for placebo 58%, Modafinil 200 mg
25%, and Modafinil 400 mg 33%. Using the Epworth Sleepiness Scale, Modafinil
200 mg (p equals .018) and 400 mg (p equals .009) both decreased the likelihood
of falling asleep. The Profile of Mood States (POMS) test was used to evaluate
changes in mood, specifically tension-anxiety, anger-hostility,
confusion-bewilderment, vigor-activity, and fatigue-inertia. Modafinil had no
adverse effects on mood, with a single exception. Modafinil 400 mg slightly
increased tension-anxiety compared to placebo (p equals .028); but the scores
were still well below both the pre-study scores and published normal scores for
this factor. Vigor-activity increased after Modafinil 200 mg (p equals .018) and
400 mg (p equals .012). Neither dose of Modafinil interfered with the
patient's ability to sleep voluntarily during the day nor did either dose
interfere with the quantity or quality of nocturnal sleep. Only one patient
dropped out of the study due to side effects of Modafinil. The principle side
effects were headache, nausea, dry mouth, heartburn, diarrhea, and dizziness.
The side effects were generally limited to the first few days of treatment.
Narcolepsy is a primary sleep disorder characterized by uncontrolled episodes of
falling asleep at unexpected times and conditions. It affects approximately
0.05% to 0.1% of the population or approximately 14,800 to 29,600 Canadians. No
new treatment for Narcolepsy has been approved in Canada since 1959. The full
results of this study will be used by the Company to complete its submission for
regulatory approval in Canada. This file is expected to be ready for submission
to Canadian Health Regulatory authorities towards the end of 1996. Modafinil is
approved for the treatment of Narcolepsy in France. DRAXIS has an exclusive
license to market and sell Modafinil in Canada. The licensor for the US, UK and
Japan is Cephalon Inc. (NASDAQ:CEPH). DRAXIS is a marketing and research
company that operates Canadian Neurological, Dermatological, and Veterinary
pharmaceutical divisions, a U.S. consumer marketing company, and offers products
exclusively through U.S. podiatrists. -30-
For further information: Contacts at DRAXIS - Kendall McAlister, Coordinator,
External Relations, Tel: (905) 677-5500, Fax: (905) 677-5502; Canadian Investor
Relations - Robert Grahovar, Small-Cap Equity Investor Relations Ltd., Tel:
(416) 535-4146; U.S. Investor Relations - Robert Kneeley, RKC Communications,
Tel: (954) 351-1976
LOAD-DATE: February 28, 1996
LANGUAGE: ENGLISH
Copyright 1996 Canada NewsWire Ltd.
977 of 998 DOCUMENTS
PR Newswire
February 12, 1996, Monday
Correction Appended - 07:32 Eastern Time
CEPHALON ANNOUNCES MODAFINIL PHASE III TRIAL RESULTS
SECTION: Financial News
LENGTH: 340 words
Cephalon, Inc. (Nasdaq: CEPH) announced today that a review of data from the
first of two Phase II clinical trials of Provigil(TM) (modafinil) in patients
with narcolepsy demonstrated that Provigil had a highly statistically
significant benefit in reducing excessive daytime sleepiness as measured by the
maintenance of wakefulness test (MWT) and a physician-perceived measure of
benefit to the patient (CGI-C), the two primary endpoints of the study. A
number of adverse experiences were reported in the study, with headache being
the most frequently reported side effect potentially attributable to the drug.
WEST CHESTER, Pa., Feb. 12
The double-blind, placebo-controlled, nine-week study of 285 patients with
narcolepsy was conducted at 18 medical centers in the United States.
Cephalon is continuing to analyze the efficacy and safety results of the Phase
III trial, which will be reported by clinical investigators at an appropriate
medical meeting later this year. Cephalon has not yet reviewed these findings
with the U.S. Food and Drug Administration. Positive findings from two Phase III
studies are expected to be required for submission of a new Drug Application to
the FDA for clearance to market Provigil in the United States. The second Phase
III study of Provigil has not yet been completed.
Cephalon licensed exclusive rights to market Provigil in the United States,
Japan, the United Kingdom, Ireland and Mexico from Laboratoire L. Lafon, a
French pharmaceutical company which developed and currently markets the drug in
France. The FDA designated modafinil an orphan drug in March 1993 for the
treatment of excessive daytime sleepiness in narcolepsy.
Cephalon discovers, develops and markets products to treat neurological
disorders. The company's principal focus is on neurological disorders such as
ALS, narcolepsy, peripheral neuropathies, Alzheimer's disease, head and spinal
injury, and stroke. CONTACT: Jason Rubin or Mary Fisher of Cephalon,
610-344-0200
LOAD-DATE: February 13, 1996
LANGUAGE: ENGLISH
DISTRIBUTION: TO BUSINESS AND MEDICAL EDITORS
CORRECTION-DATE: February 12, 1996, Monday
CORRECTION: In NYM033, Cephalon Announces Modafinil Phase III Trial Results,
moved earlier today, the first graph, third line, should read "first of two
Phase III clinical trials" rather than "Phase II" as incorrectly transmitted by
PR Newswire.;
Copyright 1996 PR Newswire Association, Inc.
978 of 998 DOCUMENTS
Canada NewsWire
February 8, 1996, Thursday
Attention Business/Financial Editors: DRAXIS HEALTH INC. REPORTS $ 0.10 FOURTH
QUARTER $ 16.6 MILLION IN CASH RESERVES
SECTION: Financial News
LENGTH: 3892 words
DATELINE: MISSISSAUGA, Ont., Feb. 8
----------------------------------------------------------------
HIGHLIGHTS FROM CONSOLIDATED STATEMENT OF OPERATIONS
For the three month period For the year ended
ended December 31, 1995
December 31, 1995
1995 1994 1995 1994
$ 3,725,161 $ 4,258,756 REVENUES $ 16,630,712 $ 17,086,116
--------------------- ------------------------
(1,696,378) 1,332,573 INCOME (LOSS) 564,992 4,944,540
-------------------- FROM OPERATIONS ------------------------
GAIN ON SALE OF
3,067,425 --- DUSA OPTION 3,067,425 ---
-------------------- ------------------------
1,883,016 --- GAIN ON DILUTION 1,833,016 ---
-------------------- OF DUSA INVESTMENT------------------------
EQUITY SHARE OF NET
DEVELOPMENT STAGE COSTS
OF AFFILIATED
(204,706) (507,241) COMPANIES (1,533,325) (2,095,430)
--------------------- ------------------------
$ 2,089,854 $ 147,524 NET INCOME $ 2,417,404 $ 1,099,392
--------------------- ------------------------
AFTER TAX EARNINGS
$ 0.10 $ 0.01 PER SHARE $ 0.12 $ 0.06
----------------------------------------------------------------
---------------------------------------------------
CONSOLIDATED BALANCE SHEET HIGHLIGHTS
December 31
1995 1994
CASH AND TREASURY BILLS $ 16,605,970 $ 11,691,434
WORKING CAPITAL $ 16,359,182 $ 12,511,905
-------------------------------------------------
Draxis Health Inc. (TSE: DAX: NASDAQ: DRAXF) today reported
earnings of $ 2.1 million or $ 0.10 per share for the three month
period ended December 31, 1995, on the strength of a non-operating
gain of $ 3,067,425 on the sale of its option to purchase two million
shares of DUSA Pharmaceuticals, Inc. ("DUSA") back to DUSA and a
non-operating gain of $ 1,833,016 on the dilution of the Company's
investment in DUSA as a result of that company's recent public
offering.
In commenting on the sale of the Company's option, Dr. Martin
Barkin, DRAXIS' CEO stated, "The $ 3 million received from the sale
of our DUSA option has further added to the Company's already solid
cash position. Draxis ended the year with no debt and cash reserves
of $ 16.6 million.
The Company's significant investments in the fourth quarter to
upgrade the infrastructure of IHS and launch the Company's Podiatric
product in the United States contributed to the $ 1.7 million loss on
operations in the quarter. The Company also incurred increased R&D
costs for the development of LipoTECA and Modafinil. Additional
product launch costs are expected in 1996 related to these launches
and the launch of Anipryl in Canada and the Skin Care line into the
United States.
Modafinil
Clinical trials on Modafinil have now been fully enrolled. The
Company expects to start analyzing the data in February and file its
New Drug Submission for approval to market the drug in Canada, in
June. Modafinil is licensed to Draxis by Laboratoire L. Lafon of
France. The drug is being developed in the United States by Cephalon
Inc. (NASDAQ: CEPHIN).
Kerasal
The launch of Kerasal, the Company's keratolytic agent, into the
United States market has been received by the podiatric community
with a high level of enthusiasm. The Company anticipates that sales
of Kerasal will contribute to revenue growth in 1996.
LipoTECA
The Company completed the first multicenter, double-blind,
placebo-controlled, 65-patient clinical trial of LipoTECA at the end
of 1995. Preliminary analysis of the final results on the effect of
the topical drug LipoTECA indicate statistically significant
difference against placebo in the treatment of abnormal scar
formations known as keloids. Dr. J.P. Bosse, who made a presentation
at the North-Western Plastic Surgeon Society conference on January
29, 1996 stated, "Until now, there has not been a satisfactory
treatment for keloids. LipoTECA cream will not cure all keloids, but
it is the most effective topical treatment that I have come to
evaluate in my 30 years of practice as a plastic surgeon." The
estimated potential worldwide market for LipoTECA is approximately
$ 300 million. DRAXIS holds the worldwide rights for LipoTECA.
FINANCIAL POSITION
- Cash and treasury bills increased to $ 16.6 million at December
31, 1995; an increase of $ 4.9 million over September 30, 1995;
- Working capital increased to $ 16.4 million at December 31,
1995; an increase of $ 2.6 million over September 30, 1995;
- Shareholders' equity increased to $ 29.8 million at December
31, 1995; an increase of $ 2.0 million over September
30, 1995.
DEPRENYL ANIMAL HEALTH, INC. ("DAHI")
DRAXIS recent marketing agreement has positioned it to increase
its stake in DAHI from a current 44% to up to 52% by conversion of
its loans into DAHI shares. Draxis will commence distribution in
Canada as soon as sufficient supplies are received into inventory.
Anipryl was filed with the United States with the FDA in September
1995.
DUSA PHARMACEUTICALS, INC. ("DUSA")
On December 14, 1995, DUSA raised U.S. $ 16.5 million, before
expenses, in a public offering of 3 million shares of common stock,
thus reducing DRAXIS' equity position from 20.00% to 12.76%. DRAXIS
holds the Canadian rights to any ALA PDT (photodynamic therapy)
products developed by DUSA.
OUTLOOK
In 1995, DRAXIS' mandate was to position itself for growth
through the acquisition, licensing or development of new products and
the creation of new markets. The Company has accomplished this
through the introduction of Kerasal into the United States, the
acquisition of a 50% interest in Innovative Health Systems of
Indianapolis, and the licensing and introduction of Anipryl in
Canada. As a result of these activities, the Company expects sales
growth in 1996 despite full genericization of Eldepryl, and will
commit funds to additional marketing and selling expenses necessary
to support that sales growth.
DRAXIS Health Inc. is a Canadian pharmaceutical company
specializing in the areas of neurology, dermatology, podiatry and
veterinary medicine. It also has two operating companies in the
United States; a consumer market company and a company offering
products exclusively to United States podiatrists.
---------------------------------------------------------------
DRAXIS HEALTH INC.
CONSOLIDATED BALANCE SHEET
(stated in Canadian dollars)
(unaudited)
December 31
1995 1994
ASSETS
Current Assets
Cash and treasury bills $ 16,605,970 $ 11,691,434
Marketable securities - 766,609
Accounts receivable 1,485,953 1,806,793
Income taxes recoverable 170,221 255,389
Inventory 704,551 1,014,038
Current portion of long-term
receivables - 364,676
Prepaid expenses 796,342 946,446
----------- -----------
19,763,037 16,845,385
----------- -----------
Long-term receivables 4,992,186 5,573,271
Long-term investments 3,930,858 3,202,896
Fixed assets 544,556 452,584
Goodwill 1,663,447 1,897,647
Licenses and other deferred charges 4,157,776 5,090,298
----------- -----------
$ 35,051,860 $ 33,062,081
----------- -----------
----------- -----------
LIABILITIES
Current Liabilities
Accounts payable and
accrued charges $ 1,569,289 $ 1,805,852
Royalties payable 1,334,566 1,527,628
Current portion of license
obligation 500,000 1,000,000
----------- -----------
3,403,855 4,333,480
----------- -----------
License obligation - 500,000
----------- -----------
Deferred income taxes 1,799,100 1,070,100
----------- -----------
SHAREHOLDERS' EQUITY
Capital stock 18,665,861 18,392,861
Contributed surplus 9,701,004 9,701,004
Retained earnings (deficit) 1,482,040 (935,364)
----------- -----------
29,848,905 27,158,501
----------- -----------
$ 35,051,860 $ 33,062,081
----------- -----------
----------- -----------
Exchange rate as at
balance sheet date U.S. $ 0.73 U.S. $ 0.71
----------- -----------
---------------------------------------------------------------
---------------------------------------------------------------
DRAXIS HEALTH INC.
CONSOLIDATED STATEMENT OF OPERATIONS
(stated in Canadian dollars)
(unaudited)
FOR THE THREE MONTH PERIOD FOR THE YEAR ENDED
ENDED DECEMBER 31 DECEMBER 31
1995 1994 1995 1994
REVENUES
$ 3,401,211 $ 4,005,870 Sales $ 15,433,813 $ 16,242,892
Interest
323,950 252,886 income 1,196,899 843,224
---------- ----------- ----------- ------------
3,725,161 4,258,756 16,630,712 17,086,116
OPERATING
5,421,539 2,926,183 EXPENSES 16,065,720 12,141,576
---------- ----------- ----------- ------------
INCOME FROM
(1,696,378) 1,332,573 OPERATIONS 564,992 4,944,540
---------- ----------- ----------- ------------
OTHER INCOME (EXPENSE)
Gain(loss) on sales
64,497 (37,544) of securities 549,296 58,630
DUSA Pharmaceuticals, Inc.
Gain on sale
3,067,425 - of option 3,067,425 -
Gain on dilution
1,833,016 - of investment 1,833,016 219,363
- (202,188) Other - (287,671)
---------- ----------- ----------- -----------
INCOME BEFORE INCOME
TAXES AND UNDERNOTED
3,268,560 1,092,841 ITEMS 6,014,729 4,934,862
PROVISION FOR
974,000 438,076 INCOME TAXES 2,064,000 1,740,040
---------- ----------- ----------- ------------
INCOME BEFORE
UNDERNOTED
2,294,560 654,765 ITEMS 3,950,729 3,194,822
EQUITY SHARE OF
NET DEVELOPMENT
STAGE COSTS OF
AFFILIATED
(204,706) (507,241) COMPANIES (1,533,325) (2,095,430)
---------- ---------- ------------ -----------
NET INCOME FOR
$ 2,089,854 $ 147,524 THE YEAR $ 2,417,404 $ 1,099,392
---------- ----------- ----------- ------------
EARNINGS PER
$ 0.10 $ 0.01 SHARE $ 0.12 $ 0.06
---------- ----------- ----------- ------------
WEIGHTED AVERAGE
NUMBER OF SHARES
20,126,718 20,019,297 OUTSTANDING 20,058,062 19,927,427
---------- ----------- ----------- ------------
---------------------------------------------------------------
---------------------------------------------------------------
DRAXIS HEALTH INC.
CONSOLIDATED STATEMENT OF CASH FLOWS
(stated in Canadian dollars)
(unaudited)
FOR THE THREE MONTH PERIOD FOR THE YEAR ENDED
ENDED DECEMBER 31 DECEMBER 31
1995 1994 1995 1994
Cash Flows from (used in)
Operating Activities
Net Income for
$ 2,089,854 $ 147,524 the year $ 2,417,404 $ 1,099,392
Non cash transactions reflected
in net income
Depreciation and
502,465 (33,676) amortization 1,051,066 632,389
Amortization of
58,550 58,550 goodwill 234,200 234,200
Deferred income
658,080 48,000 taxes 729,000 110,100
Equity share of
net development
stage costs of
affiliated
204,706 507,241 companies 1,533,325 2,095,430
(Gain) loss on
sale of
(64,497) 37,544 securities (549,296) (58,630)
Shares issued in
lieu of
- - salary 14,500 12,500
Gain on sale of option
in DUSA
Pharmaceuticals,
(3,067,425) - Inc. (3,067,425) -
Gain on dilution
of investment in
DUSA Pharmaceuticals
(1,833,016) - Inc. (1,833,016) (219,363)
---------------------- -----------------------
(1,451,283) 765,183 529,758 3,906,018
Changes in current
assets and current
liabilities impacting
cash flows from
1,679,302 2,018,532 operations 1,751,879 2,401,594
---------------------- -----------------------
Net cash flows from
operating
228,019 2,783,715 activities 2,281,637 6,307,612
---------------------- -----------------------
Cash flows from (used
in) Investing Activities
Decrease (increase) in other
418,699 50,000 deferred charges 8,487 (4,600)
Acquisition of
(23,086) 466 fixed assets (219,003) (119,370)
License milestone
- - payments (1,000,000) (2,000,000)
Acquisition of subsid-
iary and affiliated
- 1,224 companies (428,271) (297,639)
---------------------- -----------------------
Net Cash flows from
(used in) Investing
395,613 51,690 Activities (1,638,787) (2,421,609)
---------------------- -----------------------
Cash Flows from (used
in) Financing Activities
Long-term
1,213,229 (842,644) receivables 945,761 (3,034,417)
Exercise of stock
- - options 258,500 -
Proceeds from
sale of option
in DUSA Pharma-
3,067,425 - ceuticals, Inc. 3,067,425 -
Income taxes paid on sale
of Company shares owned
- - by subsidiary - (1,663,205)
Issuance of shares for
subsidiary
- (1,224) acquisitions - 297,639
---------------------- -----------------------
Net cash flows from
(used in) financing
4,280,654 (843,868) activities 4,271,686 (4,399,983)
---------------------- -----------------------
Net Increase (decrease)
in cash and treasury
4,904,286 1,991,537 bills 4,914,536 (513,980)
Cash and treasury
bills at beginning of
11,701,684 9,699,897 year 11,691,434 12,205,414
---------------------- ------------------------
Cash and treasury
bills at end of
$ 16,605,970 $ 11,691,434 year $ 16,605,970 $ 11,691,434
----------------------- ------------------------
---------------------- ------------------------
-30-
For further information: Edward L. Foster, CA, Vice President and CFO; Kendall
McAlister, Coordinator, External Relations, TEL: (905) 677-5500, FAX: (905)
677-5502
LOAD-DATE: February 8, 1996
LANGUAGE: ENGLISH
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979 of 998 DOCUMENTS
Reuters Health Medical News
January 10, 1996 Wednesday
[] - Cephalon To Study More Uses For Modafinil
LENGTH: 135 words
DATELINE: SAN FRANCISCO Jan 10
Cephalon Inc. chief executive Frank Baldino said his company plans to begin
studies this year to determine if its drug, Modafinil, can be used to treat
other disorders in addition to narcolepsy.
"We're going to launch studies this year and hopefully apply in 1997 for
approval," with the FDA, Baldino told the audience at the recent Hambrecht &
Quist healthcare conference. Baldino said one of the possible additional uses
may be in treating sleep disorders in patients with multiple sclerosis.
"There's tremendous opportunity here, especially with this low-abuse potential,"
Baldino said. Results from the first phase of a two-part study showed that the
risk of abuse with Modafinil by patients was low, he said.
The company is currently conducting Phase III trials of Modafinil for treatment
of narcolepsy.
LOAD-DATE: July 9, 2008
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PUBLICATION-TYPE: Newswire
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All Rights Reserved
980 of 998 DOCUMENTS
PR Newswire
September 28, 1995, Thursday - 08:36 Eastern Time
CEPHALON EXPANDS MARKETING TERRITORY FOR MODAFINIL
SECTION: Financial News
LENGTH: 443 words
Cephalon, Inc. (Nasdaq: CEPH) announced today the expansion of its marketing
territory for modafinil to include Japan, the third largest pharmaceutical
market in the world, in exchange for milestone and royalty payments to
Laboratoire L. Lafon. With this agreement, Cephalon now has the exclusive right
to market modafinil in the United States, the United Kingdom, Ireland, Mexico
and Japan.
"This territory expansion allows us to strengthen our presence in Japan,
capitalize on our investment in this important product and underscore our global
commercial strategy," said Frank Baldino, Jr., Ph.D., Cephalon's president and
chief executive officer. "We are pleased to broaden our relationship with
Lafon, and look forward to identifying an appropriate partner for this new
program in Japan."
WEST CHESTER, Pa., Sept. 28
Cephalon originally licensed modafinil from Lafon in February 1993 with an
initial focus on its development in narcolepsy. Other potential applications
for modafinil include several sleep disorders, cerebrovascular conditions and
the fatigue associated with a variety of neurological diseases. Lafon currently
markets modafinil in France for the treatment of narcolepsy and idiopathic
hypersomnia.
Cephalon is currently conducting two Phase III clinical studies of modafinil for
the treatment of the excessive daytime sleepiness associated with narcolepsy.
The U.S. Food and Drug Administration designated modafinil an orphan drug in
March 1993 for this indication.
Narcolepsy is a disabling, chronic, lifelong sleep disorder afflicting
approximately 125,000 people in the United States. It is characterized by
uncontrollable sleep attacks that can last from a few seconds to more than one
hour. These attacks can take place at any time, and hamper a person's ability
to perform basic daily activities.
Symptoms of narcolepsy can appear suddenly or develop slowly over many years.
The four most common symptoms are excessive daytime sleepiness, cataplexy, sleep
paralysis and hypnagogic hallucinations. In most cases excessive daytime
sleepiness is the only symptom. Current therapies to treat symptoms of the
disease include amphetamines and other stimulants which have potential for
abuse.
Cephalon is a leader in the discovery and development of products to treat
neurological disorders. The company's principal focus is on neurological
diseases such as amyotrophic lateral sclerosis (Lou Gehrig's disease),
peripheral neuropathies, narcolepsy, Alzheimer's disease, head and spinal injury
and stroke.
// CONTACT: Jason Rubin or Mary Fisher of Cephalon, 610-344-0200
LOAD-DATE: September 29, 1995
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Pharma Marketletter
May 22, 1995
Eight-Year-Old Cephalon Integrates For Success
LENGTH: 1045 words
In the precarious biotechnology industry, too often the news has centered on yet
another firm gambling all on a core technology which falls at the last hurdle
and reveals very little of value in the following field. Highly-publicized
failures have led to a drying-up of investor cash, with more and more start-up
firms foregoing their independence, and looking to the pharmaceutical majors for
support.
A notable exception to this rule is neurological disease specialist Cephalon,
which in the eight years since its inception, has grown into an integrated
biopharmaceutical firm, with research, manufacturing and latterly
sales/marketing capabilities. Chief executive of the company Frank Baldino said
at the Hambrecht & Quist meeting in London this month that he believes it is
this integrative approach which allows him to manage risk effectively.
Cephalon has two products in very late-stage clinical development, one of which,
a licensed-in product called modafinil for narcolepsy, has a high chance of
reaching the market as it is already launched in France by its developer,
Laboratoires Lafon. The other product, Myotrophin (insulin-like growth factor)
for amyotrophic lateral sclerosis, has just one more hurdle to jump (see later).
In addition, Cephalon has already set up a sales and marketing operation for the
comarketing of an opioid analgesic, Stadol NS, (butorphenol tartrate) with
Bristol-Myers Squibb, which will bring in near-term revenues and perhaps more
importantly be in place for when Cephalon's own products reach the market. Dr
Baldino said that analysts estimate that Stadol could generate sales of over $
100 million in fiscal 1995, of which the neurology opportunity is "at least
15-20%."
Dr Baldino noted that there are four key requirements for success in drug
development; a well-designed study, proven safety, bioavailability, and
efficacy. For modafinil, all four of these criteria have been satisfied, while
for Myotrophin three have been satisfied, with the outstanding efficacy data
scheduled for presentation at a neurological conference in France on June 10.
This data will come from a North American Phase II/III study of the drug, which
has now been concluded and the code broken. A similar European Phase II/III
trial should end later this summer, with data available before the end of the
year. Approximately 450 patients have been involved in both studies.
The drug may also have applications outside of ALS; Cephalon has a Phase II
program ongoing with the drug in peripheral neuropathies. Three specific
indications are being pursued in the first instance, namely chemotherapy-induced
neuropathy, post-polio syndrome and diabetic neuropathy. The first two of these
will be investigated at sites in the USA, while the latter is in trials in the
UK. In the future, other neuropathies may be added into the program, eg,
small-fiber painful neuropathy and Guillain-Barre syndrome.
The two pivotal trials of modafinil should both be reported in 1995, said Dr
Baldino. Protocol 301 is fully accrued and the code should be broken in the
summer, while for protocol 302 accrual is scheduled for completion in October.
Modafinil has been studied in over 1,000 patients by Lafon, and the data reveals
that the drug can achieve a significant decrease in daytime sleep attacks.
Already on the market in France, modafinil dossiers have been filed with the
European Union Committee for Proprietary Medicinal Products. Cephalon has
marketing rights in the UK, Ireland, the USA and Mexico.
Like Myotrophin, modafinil potentially has a far greater target population than
its first indication would suggest (approximately 125,000 people suffer from
narcolepsy in the USA with a similar number affected in Europe). "The real
opportunity with modafinil goes beyond narcolepsy," said Dr Baldino. A prime
example is Alzheimer's disease. Although modafinil will not affect the cognitive
performance in these patients, it has beneficial effects on vigilance and
awareness which may have marked effects on AD patients. Most of these patients
are not institutionalized because of their cognitive deficits, rather they are
institutionalized because they cannot focus on anything, are apathetic and have
a short attention span.
Similarly, patients with multiple sclerosis are fatigued, and this is
exacerbated by treatment with interferon products such as Chiron/Schering's
Betaseron (interferon beta). Modafinil could be used to treat this fatigue,
which affects 250,000 people in the USA. "The point I'm trying to make to you
today is that modafinil is not a niche product for narcolepsy. It's a very big
product, and I think it will be the biggest product in our portfolio within the
next three years," said Dr Baldino.
Other potential indications include hypersomnia, and also children with
attention-deficit disorder. The latter patients are currently treated with
amphetamine drugs and methylphenidate HCl, which also happen to be the two
classes which are used to treat narcoleptics in the USA and Europe. Modafinil
will have considerable advantages over them, particularly as it does not appear
to have abuse potential.
Further back in the pipeline, Dr Baldino commented on a series of programs,
targeting several diseases, which focus on three core technologies; protease
inhibitors, neurotrophic factors and receptor tyrosine kinase effectors. The
latter program is centering, amongst other things, on the development of small
molecule mimics of neurotrophic factors, and Cephalon is due to publish an
account of this work in a journal in the next few months. The programs are also
throwing out a lot of compounds which may have applications in non-core
diseases, and these are being licensed out as the opportunities occur (eg, a
prostate cancer drug was licensed to TAP Holdings last year).
In the future, Cephalon has promised Wall Street an Investigational New Drug
every year, and Dr Baldino is confident this is achievable. Certainly funding is
not an obstacle - the company is financially strong, with more than $ 110
million in cash (and $ 10 million in a partnership fund for the development of
Myotrophin), as well as projected product revenues of more than $ 30 million in
fiscal 1995.
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982 of 998 DOCUMENTS
PR Newswire
February 21, 1995, Tuesday - 08:39 Eastern Time
CEPHALON ANNOUNCES 1994 FINANCIAL RESULTS
SECTION: Financial News
LENGTH: 1102 words
DATELINE: WEST CHESTER, Pa., Feb. 21
Cephalon, Inc. (Nasdaq: CEPH) today reported a net loss of $36.1 million, or
$2.13 per share, for the year ended December 31, 1994, compared to a loss of
$19.2 million, or $1.77 per share, reported for 1993. For the quarter ended
December 31, 1994, the company reported a loss of $9.9 million, or $.54 per
share, compared to a loss of $6.3 million, or $.53 per share for the same period
in 1993.
"In 1994 clinical research represented a significant portion of our
expenditures," said Frank Baldino, Jr., Ph.D., Cephalon's president and chief
executive. "The increase in clinical research expense last year reflected our
progress toward the completion of the Myotrophin(TM) (rhIGF-1) clinical
development program in North America and Europe in patients with amyotrophic
lateral sclerosis (ALS), and the initiation of Phase III clinical trials of
modafinil for the treatment of excessive daytime sleepiness associated with
narcolepsy. The Myotrophin ALS studies are now fully enrolled, and enrollment
in the modafinil studies is actively proceeding. These studies are expected to
be completed later this year."
Revenues for 1994 increased 28 percent to $21.7 million compared to $16.9
million for 1993. The increase in revenue resulted principally from revenues
under agreements with TAP Pharmaceuticals, SmithKline Beecham and Cephalon
Clinical Partners, L.P.
Cephalon incurred operating expenses of $60.8 million in 1994 compared to $38.0
million in 1993. The increase in expenses resulted primarily from increases in
research and development activities, including expenses associated with clinical
testing of Myotrophin and modafinil. Research and development expenses totaled
$13.0 million during the fourth quarter and $51.6 million for the year, compared
to $9.2 million for the quarter and $33.2 million for the year in 1993. The
fourth quarter 1994 expense also reflected accrual of a $1.1 million license fee
payment due in 1995 for modafinil as required under the company's agreement with
Laboratoire L. Lafon.
Selling, general and administrative expenses increased 91 percent to $9.2
million in 1994, primarily due to the addition of a 30-person neurology sales
organization to support sales of Stadol NS(R) (butorphanol tartrate) under the
company's co-promotion agreement with Bristol-Myers Squibb, as well as growth in
various support functions.
As of December 31, 1994, Cephalon had approximately $114 million in cash and
marketable securities, and approximately $12 million available from Cephalon
Clinical Partners, L.P. to fund Myotrophin's clinical development in North
America and Europe.
Cephalon discovers, develops and markets products to treat neurological
disorders. The company's principal focus is on neurological diseases such as
amyotrophic lateral sclerosis (Lou Gehrig's disease), narcolepsy, peripheral
neuropathies, Alzheimer's disease, head and spinal injury, and stroke.
CEPHALON, INC. AND SUBSIDIARIES
Consolidated Statement of Operations
(Amounts in Thousands, Except Per Share)
Three Months Ended Year Ended
Dec. 31, Dec. 31,
1994 1993 1994 1993
Revenues $5,924 $3,640 $21,681 $16,922
Expenses:
Research and development 13,020 9,187 51,613 33,158
Selling, general and
administrative 3,735 1,095 9,180 4,794
Total 16,755 10,282 60,793 37,952
Loss from operations (10,831) (6,642) (39,112) (21,030)
Interest income (net) 916 369 3,047 1,794
Loss ($9,915) ($6,273) ($36,065) ($19,236)
Loss per share ($0.54) ($0.53) ($2.13) ($1.77)
Weighted average shares
outstanding 18,278 11,869 16,929 10,885
Selected Cash Flow Data
(Amounts in Thousands)
Three Months Ended Year Ended
Dec. 31, Dec. 31,
1994 1993 1994 1993
Cash, cash equivalents
and investments $121,781 $50,033 $49,438 $43,847
Cash (used for) provided
by operations (3,564) 923 (25,850) (10,600)
Capital expenditures (2,567) (1,962) (10,677) (6,932)
Sale leaseback of
property & equipment 11,750 0 11,750 0
Cash (used for) provided
by financing activities (12,942) 444 89,797 23,123
Cash, cash equivalents
and investments $114,458 $49,438 $114,458 $49,438
Selected Balance Sheet Data
(Amounts in Thousands)
Dec. 31, Dec. 31,
1994 1993
Cash, cash equivalents and investments $114,458 $49,438
Total assets 140,173 78,108
Long-term debt, including current portion 18,991 11,570
Accumulated deficit (71,679) (35,614)
Stockholders' equity 112,767 63,105
//
/EDITORS' ADVISORY: Cephalon's press releases are available at no
charge through PR Newswire's Company News On-Call fax service. For a
menu of available Cephalon press releases or to retrieve a specific
release, call 800-758-5804, ext. 134563./
CONTACT: Jason Rubin of Cephalon, 610-344-0200, ext. 302
LOAD-DATE: February 22, 1995
LANGUAGE: ENGLISH
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983 of 998 DOCUMENTS
APPLIED GENETICS NEWS
September, 1994
Narcolepsy Drug Enters Phase III
SECTION: BIOPROCESS TECHNOLOGY; Vol. 15, No. 2
LENGTH: 94 words
Narcolepsy is a disabling disease, characterized by uncontrollable sleep
attacks. In the U.S., about 125,000 have the disorder. Cephalon (145 Brandywine
Parkway, West Chester, PA 19380-4245; tel. 215-344-0200) is now starting Phase
III clinical trials of its treatment for narcolepsy, a drug called modafinil.
Modafinil is a synthetic compound that acts selectively on the part of the
central nervous system that controls sleep and wakefulness. If approved for
marketing, modafinil will be the first new treatment for narcolepsy in more than
30 years.
LOAD-DATE: March 22, 1997
LANGUAGE: ENGLISH
Copyright 1994 Business Communications Co.
984 of 998 DOCUMENTS
Pharma Marketletter
August 15, 1994
Cephalon Starts Phase III Modafinil Trials
LENGTH: 328 words
Cephalon has begun Phase III clinical trials of modafinil, its treatment for
narcolepsy. The sleep disorder affects around 125,000 people in the USA,
according to the company.
The company says it plans to conduct the two double-blind trials, which will
evaluate modafinil's efficacy in reducing the number of daytime sleep attacks,
at more than 40 leading sleep research centers across the USA. After initial
screening, patients will receive modafinil or placebo daily for nine weeks.
Cephalon licenses modafinil from Laboratoires Lafon of France, and has exclusive
rights to market the product in the USA, the UK, Republic of Ireland and Mexico.
Cephalon also says it is expecting data analysis of Phase II/III studies of its
lead product Myotrophin (recombinant human insulin-like growth factor-1) for
amyotrophic lateral sclerosis to be completed in the first quarter of 1995.
Comarketing Agreement With B-MS Meantime, Cephalon has entered into an agreement
with Bristol-Myers Squibb under which Cephalon will extend direct marketing of
the opioid nasal spray Stadol NS (butorphanol) to neurologists via a
newly-formed specialty sales force. The analgesic is currently marketed to
general practitioners and to a lesser extent obstetricians/gynecologists.
After training by B-MS, the Cephalon sales force will promote Stadol NS
primarily for use in migraine headache, and detailing could begin as early as
October. The drug has a broad-ranging indication - the management of pain when
the use of an opioid analgesic is appropriate, including postsurgical,
musculoskeletal, dental and trauma pain as well as migraines.
The agreement is renewable and on an initial three-year contract, reports the
Pink Sheet, and will split revenues on a 50/50 basis after a base sales level is
reached. Sales of Stadol NS were estimated to be $ 50 million in 1993. Cephalon
said it is seeking other agreements similar to the one it has struck with B-MS.
LOAD-DATE: January 7, 2003
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985 of 998 DOCUMENTS
PR Newswire
August 4, 1994, Thursday - 08:01 Eastern Time
CEPHALON BEGINS PHASE III MODAFINIL CLINICAL TRIALS
SECTION: Financial News
LENGTH: 443 words
DATELINE: WEST CHESTER, Pa., Aug. 4
Cephalon, Inc. (Nasdaq: CEPH) announced today the start of Phase III clinical
trials of modafinil for the treatment of narcolepsy, a chronic, debilitating
sleep disorder which affects 125,000 Americans. Modafinil is a synthetic
compound which acts selectively on the part of the central nervous system that
controls sleep and wakefulness.
"Narcolepsy is a disabling disease with serious economic and social consequences
for patients and their families," said Frank Baldino, Jr., Ph.D., Cephalon's
president and chief executive officer. "Modafinil has received marketing
approval for narcolepsy and idiopathic hypersomnia in France. If approved for
marketing in the United States, modafinil would be the first new treatment
option for U.S. patients with narcolepsy in more than thirty years."
Narcolepsy is characterized by uncontrollable sleep attacks. As a result,
narcolepsy significantly impacts a person's ability to perform basic daily
activities. Symptoms of the disorder can appear all at once or develop slowly
over many years. The four most common symptoms are excessive daytime
sleepiness, cataplexy, sleep paralysis and hypnagogic hallucinations. In most
cases excessive daytime sleepiness is the only symptom. Narcolepsy usually
begins in young adulthood. Current therapies to treat symptoms of the disease
include amphetamines and other stimulants which may have potential for abuse.
Cephalon plans to conduct two multi-center, double-blind, placebo- controlled
trials at more than forty leading sleep research centers nationwide to evaluate
modafinil's efficacy in reducing day-time sleep attacks. After initial
screening, patients will receive modafinil or placebo daily for nine weeks.
Modafinil is the second Cephalon product to enter late-stage clinical
development. Last year, the company began Phase II/III trials with
Myotrophin(TM) (rhIGF-1) in patients with amyotrophic lateral sclerosis (ALS).
Cephalon has exclusive rights to market modafinil in the United States, the
United Kingdom, Ireland and Mexico. The U.S. Food and Drug Administration
designated modafinil an orphan drug in March 1993 for the treatment of excessive
daytime sleepiness in narcolepsy.
Cephalon is a leader in the discovery and development of products to treat
neurological disorders. The company's principal focus is on neurological
diseases such as amyotrophic lateral sclerosis (Lou Gehrig's disease),
peripheral neuropathies, Alzheimer's disease, head and spinal injury and stroke.
// CONTACT: Mary Fisher, Corporate Communications of Cephalon, 610-344-0200
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Pharma Marketletter
September 6, 1993
US MODAFINIL TRIAL STARTED
LENGTH: 81 words
Cephalon has initiated clinical studies in the USA on its narcolepsy treatment,
modafinil. The study, involving healthy volunteers, will support dose selection
for pivotal Phase III efficacy trials. In January, Cephalon obtained development
and marketing rights in the USA and Mexico for modafinil from Laboratoires Lafon
of France. Now, under an extension to the existing agreement, Cephalon also
gains an expansion of its marketing rights to include the UK and Ireland.
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PHILADELPHIA INQUIRER
August 18, 1993, Wednesday
CEPHALON TO BEGIN TRIALS
SECTION: Section D; Page 3, Column 1
LENGTH: 40 words
West Chester, Pa-based Cephalon Inc says it will begin US clinical trials of
modafinil for treatment of narcolepsy; company will expand marketing for
modafinil to include United Kingdom and Ireland (S)
LANGUAGE: ENGLISH
JOURNAL-CODE: PHI
Copyright 1993 The New York Times Company: Abstracts
988 of 998 DOCUMENTS
PR Newswire
August 17, 1993, Tuesday - 08:02 Eastern Time
CEPHALON BEGINS MODAFINIL CLINICAL TRIAL IN UNITED STATES; EXPANDS MARKETING
TERRITORY TO U.K. AND IRELAND
SECTION: Financial News
LENGTH: 463 words
DATELINE: WEST CHESTER, Pa., Aug. 17
Cephalon, Inc. (NASDAQ: CEPH) announced today the initiation of U.S. clinical
trials of modafinil for the treatment of narcolepsy as well as the expansion of
its marketing territory for modafinil to include the United Kingdom and Ireland.
Cephalon is initiating the U.S. studies in healthy volunteers to support dose
selection for pivotal efficacy trials. Phase III pivotal studies in patients
with narcolepsy are planned to begin at leading U.S. sleep centers following the
completion of the current study.
In January 1993, Cephalon licensed modafinil from Laboratoire L. Lafon of Paris
for development in the United States and Mexico. Under a recent amendment to
that agreement, Cephalon now has the exclusive right to market mondafinil in the
United Kingdom and Ireland upon approval in those countries.
"We are pleased to begin the clinical development program for modafinil on
schedule," said Cephalon President and CEO Frank Baldino Jr., Ph.D. "The
expansion of our territory for modafinil into the United Kingdom and Ireland
represents an important potential market opportunity for the company and
underscores our intent to develop products around the globe."
Modafinil is a synthetic compound developed by Lafon that acts selectively on
the alpha adrenergic system in the brain. Researchers believe this system is
involved with narcolepsy, a debilitating sleep disorder that affects more than
125,000 people in the United States. In 1992 Lafon received regulatory approval
for modafinil in France, and expects to seek regulatory approval of modafinil in
other European countries later this year.
Narcolepsy is generally characterized by an uncontrollable propensity to fall
asleep and has no known cure. Current therapies that treat disease symptoms,
such as amphetamine-type stimulants, may be addictive or have other side
effects. If approved, modafinil would be the first new product in the United
States to address this disorder in many years.
Founded in 1951, Lafon is a privately owned, research-based, mid- size ethical
pharmaceutical company located in France. Lafon research specializes in
discovery and development of innovative compounds, especially in CNS and
cardiovascular therapies.
Cephalon is a leader in the discovery and development of products to treat
neurological diseases and disorders. The company's principal focus is on
neurodegenerative diseases such as amyotrophic lateral sclerosis (Lou Gehrig's
disease), peripheral neuropathy, Alzheimer's disease, head and spinal cord
injury, and stroke.
// CONTACT: Jason Rubin or Lyn Hyduke of Cephalon, 215-344-0200; or Karen
Bergman of Burns McClellan, 212-505-1919, for Cephalon; or Bill Mattson for
Laboratoire L. Lafon, 314-469-7600
LOAD-DATE: August 18, 1993
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989 of 998 DOCUMENTS
Pharma Marketletter
July 26, 1993
MERCKLE GAINS LICENSE FROM LAFON
LENGTH: 342 words
German pharmaceutical company Merckle and France's Laboratoire Lafon have
reached agreement for the former to acquire the exclusive right to develop,
market and sell modafinil in Germany, Switzerland, Austria and the former Soviet
Union as well as selected eastern European countries.
Lafon, a privately-owned research-based drugmaker specializing in the discovery
and development of innovative drugs, especially in the cardiovascular and
central nervous system arena, and Merckle, specializing in similar areas as well
as sports medicine, respiratory and pulmonary products, and likewise
privately-owned, are two partners in the Euro-Alliance Group, which was formed
in 1990 as a cooperation agreement which encourages the partners to collaborate
on the licensing and development of their pipeline products amongst themselves.
All the EuroAlliance partners maintain autonomy and continue to focus on their
home countries, where they maintain strong positions.
Modafinil is a synthetic compound discovered and developed by Lafon. It acts
selectively on the alpha adrenergic system in the brain. This system has been
shown by leading scientists to be involved in the etiology of narcolepsy (a
debilitating, lifelong sleep disorder that is estimated to affect over 50,000
people in Germany alone), and for which there is no cure.
Results from a four-year series of European studies in nearly 1,000 patients
demonstrates that modafinil significantly reduces daytime sleep attacks and
drowsiness, which endanger and reduce the quality of life of patients suffering
this condition. The compound has shown no significant adverse effects, compared
with current therapies, which are often addictive and may have other unpleasant
side effects.
Modafinil was approved by the French Ministry of Health as safe and effective in
February 1992, and commercialization there will commence once pricing and
reimbursement has been agreed. The compound has also been licensed to Cephalon
for marketing in the USA and Mexico (Marketletter July 5).
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Pharma Marketletter
July 19, 1993
CEPHALON FILES US IND FOR MODAFINIL
LENGTH: 137 words
Cephalon has filed an Investigational New Drug Application in the USA for
modafinil, its new compound for the treatment of narcolepsy. The company
licensed the drug from French pharmaceutical firm Laboratoires Lafon
(Marketletter July 5). Modafinil has already been approved for the treatment of
this condition in France.
Cephalon chief executive Frank Baldino said that the company had filed the IND
in order to carry out additional studies required to supplement the data
generated in the European clinical trial program for the drug. Phase III studies
in the USA should be starting by the end of the year, he added.
Earlier this year, the US Food and Drug Administration granted orphan drug
designation for modafinil in the treatment of narcolepsy. Cephalon has rights to
the drug in the USA and Mexico.
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991 of 998 DOCUMENTS
Business Wire
July 6, 1993, Tuesday
Cephalon Inc. files Investigational New Drug Application for the use of
modafinil for the treatment of narcolepsy
LENGTH: 423 words
DATELINE: WEST CHESTER, Pa.
Inc. (NASDAQ:CEPH) Tuesday announced that the company filed an Investigational
New Drug (IND) application with the United States Food and Drug Administration
(FDA) for clinical trials of modafinil which is being developed for the
treatment of narcolepsy.
Narcolepsy is a debilitating disorder which often originates in adolescence and
is most notably characterized by uncontrollable daytime sleep attacks. These
attacks can take place during conversation, while eating, and even while
driving, and significantly impact the patient's ability to perform daily
activities. Narcolepsy affects more than 125,000 people in the United States.
"We continue to make excellent progress towards our goal of submitting a New
Drug Application (NDA) for modafinil," stated Dr. Frank Baldino Jr., president
and CEO of Cephalon.
"We filed this IND to allow us to perform the additional clinical studies
required by the FDA to supplement the data package used to obtain market
approval for modafinil in France. The modafinil program is advancing as
anticipated and we are targeting the end of this year for the initiation of
Phase III clinical studies."
Modafinil represents an important development in the treatment of narcolepsy.
Data from over 1,000 patients in Europe demonstrated that modafinil
significantly reduced daytime sleep attacks and drowsiness seen in this
disorder, while showing no significant adverse side effects. Modafinil received
regulatory approval in France for the treatment of narcolepsy in February 1992.
Earlier this year the FDA granted orphan drug designation for modafinil in the
treatment of narcolepsy. Cephalon has the exclusive right to develop, market and
sell modafinil in the U.S. and Mexico. Cephalon Inc. discovers and develops
pharmaceutical products for the treatment of neurological diseases and
disorders. The company's primary focus is on neurodegenerative diseases, which
are characterized by the death of neurons, the specialized conducting cells of
the nervous system.
The company has concentrated its research programs on the prevention of neuronal
death in several disorders, including amyotrophic lateral sclerosis and
peripheral neuropathy, Alzheimer's disease, head and spinal cord injury and
stroke.
CONTACT: Cephalon Inc., West Chester
Lyn Hyduke, corporate communications, 215/344-0200
by
Burns McClellan, New York
Karen L. Bergman, 212/505-1919
LANGUAGE: ENGLISH
DISTRIBUTION: Business Editors/Health Editors
Copyright 1993 Business Wire, Inc.
992 of 998 DOCUMENTS
Business Wire
May 5, 1993, Wednesday
Cephalon announces first-quarter financial results
LENGTH: 1033 words
DATELINE: WEST CHESTER, Pa.
Inc. (NASDAQ:CEPH) Wednesday reported its financial results for the first
quarter ended March 31, 1993.
Revenues for the quarter were $2 million. No revenues were reported for the same
period in 1992. The company had a net loss of $5.8 million (64 cents per share)
for the quarter, as compared with a loss of $3 million (34 cents per share)
reported for the same 1992 period.
The results for the 1993 period reflect a $1 million charge to earnings for a
payment made to Laboratoire L. Lafon upon the execution of an agreement
providing Cephalon with exclusive rights to develop, market and sell modafinil
for the treatment of narcolepsy in the United States and Mexico.
In the March 31, 1993 quarter, the company incurred operating expenses of $6.4
million, compared with $3.9 million during the same period last year. The
increase in expenses results primarily from the payment to Lafon, and the
increases in research and development costs, including costs associated with the
development of Myotrophin, which entered pivotal Phase II/III clinical testing
for the treatment of amyotrophic lateral sclerosis (ALS) during this first
quarter 1993.
"The licensing of modafinil provides Cephalon with another product in late stage
clinical development. We are excited about its potential use in treating
narcolepsy, a debilitating, lifelong disorder that adversely affects over
125,000 Americans. It fits well within that segment of our product pipeline
directed toward the niche neurology marketplace," stated Dr. Frank Baldino Jr.,
president and CEO of Cephalon.
Modafinil is a synthetic compound that acts selectively on the alpha adrenergic
system in the brain. This system has been shown by leading scientists in the
field to be involved in the etiology of narcolepsy. Current therapies to treat
narcolepsy, such as amphetamine-like stimulants and antidepressants, are often
addictive and have other undesirable side effects.
In European studies, conducted over a four-year period, modafinil significantly
reduced daytime sleep attacks and drowsiness seen in this disorder, while
showing no significant adverse side effects. Subsequent to these trials,
modafinil was judged by the French Ministry of Health to be safe and effective,
receiving regulatory approval in France.
In April of this year Cephalon completed a secondary offering of 2.3 million
shares of common stock which resulted in net proceeds to the company of
approximately $20.5 million in funds. At April 30, 1993, Cephalon had access to
over $85 million, both on and off the balance sheet, including approximately $33
million available from Cephalon Clinical Partners L.P. to fund Myotrophin's
clinical development in the United States and Europe.
Cephalon discovers and develops pharmaceutical products for the treatment of
neurological diseases and disorders. The company's primary focus is on
neurodegenerative diseases, which are characterized by the death of neurons, the
specialized conducting cells of the nervous system.
The company has concentrated its research and development efforts on the
prevention of neuronal death in several disorders, including ALS and peripheral
neuropathy, Alzheimer's disease, head and spinal cord injury and stroke. -0-
cephalon Inc. and Subsidiaries
Consolidated Statement of Operations
(Amounts in thousands, except per share)
(Unaudited)
Three Months Ended
March 31,
1993 1992
Revenues $ 1,975 $ --
Expenses:
Research and development 7,384 3,252
General and administrative 976 623
8,360 3,875
Loss from operations (6,385) (3,875)
Interest income (net) 559 877
Loss [5,826) [2,998)
Loss per share (64 cents) (34 cents)
Weighted average
shares outstanding 9,103 8,855
Selected Balance Sheet Data
(Amounts in thousands)
March 31, Dec. 31,
1993 1992
(Unaudited)
Cash, cash equivalents
& investments $ 36,492 $ 43,847
Total assets 64,859 71,061
Long-term debt, net of current portion 12,010 12,010
Accumulated deficit (22,204) (16,378)
Stockholders' equity $ 51,232 $ 56,733
CONTACT: Cephalon Inc., West Chester
Lyn Hyduke, 215/344-0200
or
Burns McClellan Inc., New York
Karen L. Bergman (media), 212/505-1919
Emily Calmer Magowan (investors), 212/505-1919
LANGUAGE: ENGLISH
DISTRIBUTION: Business Editors & Health/Medical Writers
Copyright 1993 Business Wire, Inc.
993 of 998 DOCUMENTS
Business Wire
March 25, 1993, Thursday
Cephalon, Inc. receives orphan drug status for modafinil
LENGTH: 400 words
DATELINE: WEST CHESTER, Pa.
, Inc. (NASDAQ:CEPH) Thursday announced the Company was granted orphan drug
designation for modafinil in the treatment of narcolepsy from the Food and Drug
Administration.
Narcolepsy affects 125,000 people in the United States. Cephalon received the
exclusive right to develop, market and sell modafinil in the United States and
Mexico from Laboratoire L. Lafon of Paris, France in February of this year.
"This is the first step in our development program for modafinil," stated Dr.
Frank Baldino, Jr., President and Chief Executive Officer of Cephalon. "
Modafinil represents a product opportunity that fits our strategic objectives
within the neurology field. We are rapidly advancing this potential product
though the development process and expect to file an IND later this year."
Narcolepsy is a debilitating disorder which often originates in late childhood
and is most notably characterized by uncontrollable daytime sleep attacks. These
attacks take place during conversation, while eating, even while driving, and
significantly impact the patient's ability to perform daily activities.
Currently, there is no cure for narcolepsy, and current therapies that treat
disease symptoms, such as amphetamine-like stimulants, are often addictive and
have other undesirable side effects.
Results of a four-year series of European studies in more than 1,000 patients
demonstrated that modafinil significantly reduced daytime sleep attacks and
drowsiness seen in this disorder, while showing no significant adverse side
effects. Modafinil received regulatory approval in France for the treatment of
narcolepsy in February 1992.
Cephalon, Inc. discovers and develops pharmaceutical products for the treatment
of neurological diseases and disorders. The Company's primary focus is on
neurodegenerative diseases, which are characterized by the death of neurons, the
specialized conducting cells of the nervous system. The Company has concentrated
its research programs on the prevention of neuronal death in several disorders,
including ALS and peripheral neuropathy, Alzheimer's disease, head and spinal
cord injury and stroke.
CONTACT: Cephalon Inc., West Chester
Lyn Hyduke, 215/344-0200
or
Burns McClellan, New York
Karen L. Bergman, 212/505-1919
LANGUAGE: ENGLISH
DISTRIBUTION: Business, Health & Medical Editors
Copyright 1993 Business Wire, Inc.
994 of 998 DOCUMENTS
PHILADELPHIA INQUIRER
February 2, 1993, Tuesday
CEPHALON GETS DRUG RIGHTS
SECTION: Section C; Page 3, Column 1
LENGTH: 43 words
Laboratoire L Lafon, of Paris, France, has granted Cephalon Inc, of West
Chester, Pa, exclusive right to develop, market and sell modafinil in US and
Mexico; Modafinil is a compound developed by Lafon to treat narcolepsy (S)
LANGUAGE: ENGLISH
JOURNAL-CODE: PHI
Copyright 1993 The New York Times Company: Abstracts
995 of 998 DOCUMENTS
PR Newswire
February 1, 1993, Monday - 09:11 Eastern Time
CEPHALON LICENSES NOVEL PRODUCT TO TREAT NARCOLEPSY FROM LABORATOIRE L. LAFON
SECTION: Financial News
LENGTH: 630 words
DATELINE: WEST CHESTER, Pa. and PARIS, Feb. 1
Cephalon, Inc. (NASDAQ: CEPH) of West Chester, Pennsylvania and Laboratoire L.
Lafon of Paris announced today an agreement under which Cephalon receives the
exclusive right to develop, market and sell modafinil in the United States and
Mexico. The announcement came jointly from Frank Baldino, Jr., Ph.D., President
and CEO of Cephalon, and Francois Lafon, CEO of Lafon.
Modafinil is a synthetic compound developed by Lafon that acts selectively on
the alpha adrenergic system in the brain. This system has been shown by leading
scientists in the field to be involved with the etiology of narcolepsy, a
debilitating, lifelong sleep disorder that is estimated to affect over 125,000
Americans. Results of a four-year series of European studies in more than 1,000
patients demonstrated that modafinil significantly reduced daytime sleep attacks
and drowsiness seen in this disorder, while showing no adverse side effects.
Subsequent to these trials, modafinil was judged by the French Ministry of
Health to be safe and effective, receiving regulatory approval for narcolepsy in
France in February 1992. Product sales in France will be initiated by Lafon
upon receipt of pricing and reimbursement approval.
"The acquisition of marketing rights for modafinil fits within the company's
strategic objective to license in product opportunities directed toward
neurologists," stated Dr. Frank Baldino, Jr. "Modafinil is a product with
proven safety in man that has already gained French regulatory approval. The
company is planning to perform a Phase III study in the U.S. to facilitate the
filing of an NDA for marketing approval for the treatment of narcolepsy."
Narcolepsy is a sleep disorder which has severe negative impacts on public
safety, sense of self-worth, social image and the ability to retain a job.
Symptoms of this disease often originate in late childhood and are most notably
characterized by an uncontrollable propensity to fall asleep during the day.
There is no cure for narcolepsy. Current therapies that treat disease symptoms,
such as amphetamine-type stimulants, are often addictive and may have other side
effects.
Cephalon's results for the first quarter of 1993 will include a charge to
earnings to reflect the payment made to Lafon upon execution of the agreement.
Additionally, under the agreement Cephalon will purchase supplies of modafinil
from Lafon and fund modafinil's clinical development in the U.S. and Mexico.
The agreement also provides for royalty and certain other payments to Lafon.
Mr. Francois Lafon commented that, "We are pleased to be working with a dynamic
and focused company like Cephalon for the U.S. development and commercialization
of modafinil." Founded in 1951, Lafon is a privately owned, research based,
mid-size ethical pharmaceutical company in France. Lafon research specializes
in discovery and development of innovative compounds, especially in CNS and
cardiovascular therapies.
Cephalon, Inc. is a leader in the development of products to treat neurological
diseases and disorders. The company's primary focus is on neurodegenerative
diseases which are characterized by the death of neurons, specialized conducting
cells of the nervous system. The company has concentrated its research and
development efforts on the prevention of neuronal death in several disorders,
including Alzheimer's disease, amyotrophic lateral sclerosis, head and spinal
cord injuries, peripheral neuropathy, retinopathy, and stroke. CONTACT: Lyn
Hyduke, assistant director of corporate communications of Cephalon, Inc.,
215-344-0200; Karen L. Bergman of Burns McClellan, 212-505-1919, for Cephalon,
Inc.; or Bill Mattson, 314-469-7600, for Laboratoire L. Lafon
LOAD-DATE: February 2, 1993
LANGUAGE: ENGLISH
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Copyright 1993 PR Newswire Association, Inc.
996 of 998 DOCUMENTS
Canada NewsWire
November 19, 1992, Thursday
CANADIAN LICENSE FOR NEW NEUROLOGY DRUG ACQUIRED BY DEPRENYL RESEARCH LIMITED
FROM LABORATOIRE L. LAFON OF FRANCE
SECTION: Financial News
LENGTH: 247 words
DATELINE: TORONTO, Nov. 19
Laboratoire L. Lafon of Paris, France and Deprenyl Research Limited (TSE: DEP;
NASDAQ: DEPLF) announced today that they have concluded an agreement whereby
Deprenyl Research has acquired an exclusive license to market Modafinil in
Canada.
Modafinil, recently approved in France, is a new drug for Narcolepsy, a disorder
which affects an estimated 26,000 Canadians according to Sleep-Wake Disorders
Canada, a national patient group. The drug received extensive testing in Europe
including testing on French military personnel during the Gulf war. Modafinil
regulates wakefulness without cardiovascular effects in patients with sleeping
disorders. It is an original new drug with a novel mechanism of action entirely
unrelated to amphetamines or methylphenidate (Ritalin(R)). Modafinil has been
shown to have a very good safe profile and a low abuse potential.
Dr. Roger Mailhot, Deprenyl's Vice President Scientific Affairs, indicated that
Deprenyl expects to submit the drug to Canadian regulatory authorities within
the next ninety days.
Deprenyl Research Limited is a Canadian pharmaceutical company which currently
markets three neurologic drugs for Parkinson's disease. It is carrying out and
sponsoring research in Alzheimer's disease, Epilepsy, Multiple Sclerosis and
other neurologic disorders. The Company recently launched in Canada four of its
drugs from its dermatologic division through its affiliate Lipopharm Inc. of
Montreal, Quebec.
For further information: AT THE COMPANY, Martin Barkin, MD, President & CEO,
Deborah Worobec, Investor Relations (416) 537-4372, (416) 537-1653 fax; UNITED
STATES CONTACT: O'Connor Biro & Associates, Jim Tolan, Senior Vice President
(708) 498-2284, (708) 498-3144 fax
LOAD-DATE: November 19, 1992
LANGUAGE: ENGLISH
DISTRIBUTION: Attention Business Editors
Copyright 1992 Canada NewsWire Ltd.
997 of 998 DOCUMENTS
PR Newswire
November 19, 1992, Thursday - 09:03 Eastern Time
CANADIAN LICENSE FOR NEW NEUROLOGY DRUG ACQUIRED BY DEPRENYL RESEARCH LIMITED
FROM LABORATOIRE L. LAFON OF FRANCE
SECTION: Financial News
LENGTH: 247 words
DATELINE: TORONTO, Nov. 19
Laboratoire L. Lafon of Paris, France and Deprenyl Research Limited (TSE: DEP;
NASDAQ: DEPLF) announced today that they have concluded an agreement whereby
Deprenyl Research has acquired an exclusive license to market Modafinil in
Canada.
Modafinil, recently approved in France, is a new drug for narcolepsy, a disorder
which affects an estimated 26,000 Canadians, according to Sleep-Wake Disorders
Canada, a national patient group. The drug received extensive testing in Europe
including testing on French military personnel during the Gulf war. Modafinil
regulates wakefulness without cardiovascular effects in patients with sleeping
disorders. It is an original new drug with a novel mechanism of action entirely
unrelated to amphetamines or methylphenidate (Ritalin R). Modafinil has been
shown to have a good safety profile and a low abuse potential.
Dr. Roger Mailhot, Deprenyl's vice president-scientific affairs, indicated that
Deprenyl expects to submit the drug to Canadian regulatory authorities within
the next ninety days.
Deprenyl Research Limited is a Canadian pharmaceutical company which currently
markets three neurologic drugs for Parkinson's disease. It is carrying out and
sponsoring research in Alzheimer's disease, epilepsy, multiple sclerosis and
other neurologic disorders. The company recently launched in Canada four of its
drugs from its dermatologic division through its affiliate Lipopharm Inc. of
Montreal, Quebec.
LOAD-DATE: November 20, 1992
LANGUAGE: ENGLISH
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998 of 998 DOCUMENTS
Pharma Marketletter
November 2, 1992
MODAFINIL APPROVED IN FRANCE
LENGTH: 253 words
Despite fears of misuse, the French regulatory authorities have granted
marketing approval to Laboratoires L Lafon for modafinil, the so-called
"anti-sleep pill" publicized during the Gulf war, where it was tested on French
military personnel.
Modafinil, a member of the adrafanil group of compounds, will have relatively
limited indications once launched, namely narcolepsy and idiopathic hypersomnia.
The fear of misuse of the compound has led to its inclusion in the context of
new legislation covering the prescription of certain drugs.
Under this legislation, modafinil will be included in the List I category
(formerly Schedule A), and while prescribable by physicians working in office
practice and hospital doctors, prescriptions must be made out using a dangerous
substances pad. Nevertheless, the prescriptions will remain renewable on a
monthly basis for a maximum of one year.
The suggested dosing regimen for the product in the recommended indications is
two to four tablets per 24 hours, given in the morning and at noon. Evening
doses, while not recommended, have not been linked to insomnia. The most common
adverse reaction reported, with an overall incidence of about 6%, is tension and
agitation. These reactions come about as a result of modafinil's mode of action,
as a stimulator of the central noradrenergic system.
The price of modafinil has not yet been determined, and awaits consideration by
the Medications Transparency Committee of documentation concerning the drug.
LOAD-DATE: January 13, 2003
LANGUAGE: ENGLISH
Copyright 1992 Marketletter Publications Ltd.