Pfizer says HIV drug suppresses
virus
A new study has revealed that Pfizer's HIV drug maraviroc achieved twice
the levels of virus suppression compared to other treatments and suggests the
drug could work in patients where all other therapies have failed.
Maraviroc is part of a class of drugs known as CCR5 inhibitors and works in a
new way to existing therapies. The drug blocks the virus' entry to cells T
cells, a type of white blood cell, so that the HIV virus can no longer
replicate.
The drug was examined in two phase III trials. The first trial that showed
60.4% of those who took maraviroc achieved a level of less than 400 HIV copies
per milliliter of blood, compared to 54.7% on a once-daily dose and 31.4% on
background therapy.
The second trial found that 61.3% of twice-daily maraviroc patients achieved
target HIV levels, compared with 55.5% on once-daily dose and 23.1% treated
with other drugs.
"HIV therapies have, for so long, focused on people needing drugs for their
initial treatment. But there is a huge and growing number of people who've
failed on first and second-line therapies, who need other drugs later on",
said Michael Carter, an HIV expert from the UK's National Aids Manual.
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An expert panel has recommended Sanofi-Aventis' avian flu vaccine to the
FDA
Despite concerns over lack of efficacy, Sanofi-Aventis' experimental
vaccine against the H5N1 influenza strain has become the first such product to
receive backing from an FDA advisory panel. However, the vaccine may face
significant competition in the long-term from several other companies
developing H5N1 vaccines using more advanced adjuvant technology.
The vaccine was shown to trigger a response in only 45% of patients receiving
the highest dose during clinical testing, which falls short of the agency's
standards. While the advisory panel has acknowledged the vaccine's
shortcomings, their backing of vaccine was based on the benefits of having a
licensed vaccine against a potential influenza pandemic as opposed to having
no vaccine at all.
In the US alone, there are an estimated 2550 million cases of influenza per
year, leading to 150,000 hospitalizations and 30,00040,000 deaths. However,
there are grave concerns at the health and economic devastation that could be
caused by the influenza A subtype H5N1. It has spread rapidly from Asia to
Africa and Europe, and although there have been no reported human-to-human
transmissions, this threat alone has driven demand for proactive development
of a suitable vaccine.
GlaxoSmithKline, Baxter International Inc, and Novartis AG are also developing
testing H5N1 influenza vaccines. However, they have focused development on
increased efficacy through novel adjuvant technologies.
Novartis' alternative strategy is to have authorization in place that can be
changed rapidly once the responsible pandemic virus strain has been identified
and incorporated. Focetria has recently received EU recommendations for
marketing authorization from the Committee for Medicinal Products for Human
Use.
Sanofi's first-to-market status may be a short-term advantage, but adjuvant
use will reduce antigen volume requirements. Sanofi's manufacturing capacity
may initially offset this disadvantage, but competitor products are likely to
be more cost effective to produce, leaving Sanofi reliant on developing a
similar adjuvant delivery system to compete profitably.
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Abbott cleared to market Crohn's drug in US
Abbott Laboratories has received FDA approval to market Humira as a
treatment for reducing the symptoms and inducing clinical remission in adults
with Crohn's disease who have had an inadequate response to conventional
therapy.
Humira is also indicated for reducing the signs and symptoms and inducing
clinical remission in these patients if they have also lost response to or are
intolerant to infliximab, the only other approved biologic for treatment of
Crohn's disease.
Crohn's disease is a serious chronic, inflammatory disease of the
gastrointestinal tract. Common symptoms of Crohn's disease include diarrhea,
cramping, abdominal pain, weight loss, fever, and in some cases, rectal
bleeding.
Humira also comes with the strongest possible warning because the drug has
been associated with serious infections, sepsis, tuberculosis and
opportunistic infections, including fatalities.
This approval establishes Humira as the first and only self-administered
biologic for the treatment of Crohn's disease. Crohn's disease is the fourth
FDA approval in immune-mediated diseases for Humira.
"The approval in Crohn's disease extends the reach of Humira beyond
rheumatology and dermatology to an underserved patient population in
gastroenterology," said Eugene Sun, vice president, Global Pharmaceutical
Clinical Development at Abbott.
"In addition to rapid and sustained response, Humira offers patients with
moderate to severe Crohn's disease the convenience of self-injection in the
comfort of their home."
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The FDA has approved Cymbalta to treat generalized anxiety disorder (GAD).
Eli Lilly's Cymbalta has gained the approval of the FDA for use in
patients with GAD. The expanded indication is positive news for Cymbalta,
which is already approved in the US for the treatment of major depressive
disorder and the management of diabetic peripheral neuropathic pain.
Cymbalta (duloxetine HCl) is serotonin and norepinephrine reuptake inhibitor (SNRI),
which is a class of drugs that is primarily indicated for the treatment of
depression, but may also be prescribed for a variety of other mental health
issues, including panic, anxiety and eating disorders.
The FDA's approval of Cymbalta to treat GAD as well as depression and
neuropathic pain is based on three randomized, double-blind studies in
non-depressed adults with the disorder. The results of these studies have
shown that 46% of patients treated with Cymbalta had improved anxiety-related
symptoms as compared to 32% of patients treated with a placebo. In addition,
46% of patients who took Cymbalta experienced an improvement in their
abilities to perform everyday activities related to work, home and social
situations as compared to 26% of patients in the placebo group.
With sales in 2006 of $1.316 billion, up from $680 million in 2005, Cymbalta
is a promising driver of growth for Lilly. Despite the strength of this drug
the market, it has not been without its opponents. Detractors point to both
the exponential growth in the number of prescriptions for SNRIs in recent
years and the link that has been made between these drugs and a potential for
increased risk of suicide in children and teenagers. Cymbalta is not approved
for use in pediatric patients.
It is estimated that approximately 6.5 million Americans are diagnosed with
GAD each year. Many of those diagnosed will seek treatment in the form of
cognitive behavior therapy. However, because of the chronic nature of the
disorder and because GAD has been linked with irregular levels of
neurotransmitters in the brains of those affected, many individuals find they
are better able to manage the disorder with the help of pharmaceutical drugs.
Cymbalta's expanded indication is good news for adult patients and prescribers
who are looking for additional pharmaceutical options for the treatment of
generalized anxiety disorder and for Eli Lilly, which is counting on the drug
to prove to be a safe and effective treatment for a wide range of mental and
physician disorders related to serotonin and norepinephrine absorption.
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GSK hay fever drug relieves symptoms
A GlaxoSmithKline allergy medicine currently under review by the FDA, was
effective and well-tolerated in treating a range of nasal allergy symptoms
such as congestion, sneezing, itchy and runny nose, according to phase III
clinical studies.
In two separate phase III studies, fluticasone furoate nasal spray (FFNS) was
more effective than placebo in relieving both the nasal and eye symptoms of
patients 12 years and older with seasonal allergic rhinitis, commonly known as
hay fever.
One additional phase III study among individuals with perennial allergic
rhinitis (year-round nasal allergies) found FFNS to be more effective than
placebo in relieving nasal symptoms. Moreover, the symptom-relief lasted 24
hours in all three studies.
"These are the first two prospectively-designed phase III studies to
demonstrate consistent and significant improvement in eye-related allergy
symptoms with an intranasal steroid," commented lead investigator William
Lumry, Asthma & Allergy Specialists, Dallas.
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