Neurology Study Finds Approved Dose of AVONEX(R) (Interferon Beta-1a) Equally Effective as Higher Dose in Treating Relapsing Multiple Sclerosis

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Neurology Study Finds Approved Dose of AVONEX(R) (Interferon Beta-1a) Equally Effective as Higher Dose in Treating Relapsing Multiple Sclerosis

		BIOGEN LOGO Biogen Logo. (PRNewsFoto)[KC] CAMBRIDGE, MA USA

    CAMBRIDGE, Mass., Nov. 26 /PRNewswire-FirstCall/ --
Biogen, Inc. (Nasdaq: BGEN) Data published in the November 26, 2002 issue of
the journal Neurology determine that the commercially available dose of
Biogen, Inc.'s multiple sclerosis therapy AVONEX 30 mcg once weekly is equally
as effective in treating patients with relapsing-remitting multiple sclerosis
as a higher dose of 60 mcg once weekly.
    (Photo: http://www.newscom.com/cgi-bin/prnh/19990824/BIOLOGO )
    "For many years, neurologists have been debating what the optimal dose of
Interferon beta-1a (IFNbeta-1a) is and whether a higher dose may be more
effective in treating patients with relapsing forms of MS," said Alfred W.
Sandrock, MD, PhD, Biogen's Senior Director of Medical Research and co-author
of the study.  "This study shows that a 60 mcg dose of AVONEX is not more
effective than a 30 mcg IM once weekly dose of AVONEX."
    This study "provides clear, high-quality evidence that the higher dosage
of this preparation given on a once-weekly basis confers no therapeutic
advantage," said Karl Kieburtz, MD, and Michael McDermott, PhD, both of the
Department of Neurology, University of Rochester Medical Center, in an
independent editorial in the same issue of Neurology.  "This type of study is
of great utility to clinicians and patients in avoiding the unnecessary use of
higher dosages, which may be associated with higher long-term toxicity and
higher costs."
    The objective of the study was to determine whether a higher dose of
AVONEX, 60 mcg IM once weekly, is clinically more effective than AVONEX 30 mcg
IM once weekly in reducing disability progression in relapsing-remitting MS.
The 60-mcg dose was chosen for comparison to the commercially available dose
because pharmacodynamic data have suggested that increasing the IFNbeta-1a
dose from 30 mcg to 60 mcg potentially led to a greater level of induction of
biological markers (i.e., neopterin and beta2-microglobulin), without a
notable increase in side effects.
    The randomized, double-blind, parallel-group, dose-comparison study was
conducted at 38 centers in Europe.  Over 800 participants with varying levels
of disability participated.
    Patients were randomized to receive AVONEX 30 mcg or 60 mcg IM once weekly
for at least 36 months.  Subjects were included in the study if they had a
definite diagnosis of relapsing MS for at least one year and at least two
medically documented relapses within the 3 years prior to randomization.
    The primary endpoint was disability progression, defined as time to a
sustained increase on the Expanded Disability Status Scale (EDSS).  Both
groups showed equal rates of disability progression.  The rate of disability
progression after 36 months was 37 percent in both the 30 mcg and 60 mcg
groups.  Additional endpoints included relapses, MRI, safety, and subgroup
analyses of disability progression.  No significant differences were observed
among any of these endpoints.
    Regarding antigenicity in this study, the data continue to demonstrate the
low neutralizing antibody rate for AVONEX.  In this trial, the neutralizing
antibody rate for the 30 mcg dose was 2.3% (9 of 400 patients) and the
neutralizing antibody rate for the 60 mcg dose was 5.8% (23 of 395 patients).
The neutralizing antibody rate for the 30 mcg dose is consistent with a recent
U.S. Food and Drug Administration approved label change.  This label change
was based on recent studies with multiple sclerosis patients given AVONEX for
at least 1 year, which showed the presence of neutralizing antibodies at the
rate of 5 percent (13 of 261 patients).  The clinical significance of
neutralizing antibodies to AVONEX is unknown.
     "According to the results of this study, there is no clinical benefit for
people with relapsing-remitting MS to take a higher dose of AVONEX," said
Professor Michel Clanet, University of Toulouse, and chief investigator of the
European Avonex Dose Comparison Study.  "Both doses were equally effective and
generally well-tolerated.  However, we did find higher incidences of some side
effects in the individuals receiving the higher, 60 mcg dose."

    About AVONEX(R) (Interferon beta-1a)
    AVONEX is the leading treatment for relapsing forms of multiple sclerosis
worldwide, with more than 120,000 patients on therapy. It was launched in the
U.S. in 1996 and later in Europe for the treatment of relapsing forms of MS to
slow the progression of disability and reduce relapses. AVONEX is marketed
internationally in more than 65 countries.
    The most common side effects associated with AVONEX treatment are flu-like
symptoms, muscle ache, fever, and chills. Other common side effects seen, but
not statistically different between AVONEX and control groups, were headache,
pain and asthenia (weakness). These side effects usually go away within a day
after the injection and occur less often as the treatment continues. AVONEX
should be used with caution in people with depression and people with seizure
disorders. AVONEX should not be used by pregnant women. People with cardiac
disease should be closely monitored. Routine periodic blood chemistry and
hematology tests are recommended during treatment with AVONEX. Please see
complete prescribing information available at http://www.AVONEX.com.

    About Biogen
    Biogen, Inc., winner of the U.S. National Medal of Technology, is a
biopharmaceutical company principally engaged in discovering and developing
drugs for human healthcare through genetic engineering. Headquartered in
Cambridge, MA, the Company's revenues are generated from U.S. and worldwide
sales of AVONEX(R) (Interferon beta-1a) for treatment of relapsing forms of
multiple sclerosis, and from the worldwide sales by licensees of a number of
products, including alpha interferon and hepatitis B vaccines and diagnostic
products. Biogen's research and development activities are focused on novel
products to treat inflammatory and autoimmune diseases, neurological diseases,
cancer, fibrosis and congestive heart failure. The Company maintains active
clinical research programs in protein therapeutics, small molecules, genomics
and gene therapy. For copies of press releases and additional information
about the Company, please consult Biogen's Homepage on the World Wide Web at
http://www.Biogen.com.

    Media Contacts:
     Tim Hunt
     Director, Public Affairs
     Biogen
     617-914-6524

    Investment Community Contact:
     Christina Dillon
     Manager, Investor Relations
     Biogen, Inc.
     (617) 679-2812

SOURCE Biogen, Inc.

http://www.biogen.com
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CONTACT:
Media, Tim Hunt, Director, Public Affairs,
+1-617-914-6524, or Investment Community, Christina Dillon,
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