- Company Also Granted Expansion of Prophylaxis Therapy Label to Include
Patient Labeling for Self-Administration -
EXTON, Pa., June 4 /PRNewswire-FirstCall/ -- ViroPharma Incorporated
(Nasdaq: VPHM) today announced that it has received a Complete Response letter
from the U.S. Food and Drug Administration (FDA) related to its supplemental
Biologics License Application (sBLA) for Cinryze(TM) (C1 esterase inhibitor
[human]) as a treatment for acute attacks of hereditary angioedema (HAE). The
FDA has requested an additional clinical study, due to their opinion that the
placebo controlled study submitted in support of the sBLA lacked robustness.
In the Complete Response letter, the FDA cited no safety concerns related to
acute treatment with Cinryze in the clinical studies.
In addition, ViroPharma announced that FDA has approved the patient
labeling for Cinryze to include self-administration for routine prophylaxis,
once patients are properly trained by their healthcare provider.
"Though Cinryze is already successfully preventing attacks of HAE in many
patients, there remains an unmet medical need for patients suffering from
acute laryngeal attacks," said Vincent Milano, ViroPharma's president and
chief executive officer. "Despite having a statistically significant result
using the most conservative intent-to-treat (ITT) analysis, the FDA feels that
the data are not robust enough to support approval at this time. We intend to
respond to the FDA about our plans, and we will provide an update on the
second quarter financial call."
In October 2008, Cinryze was approved as the first and only targeted
therapy for routine prophylaxis against angioedema attacks. In clinical
studies and in commercial use, Cinryze has been generally well-tolerated. In
the controlled clinical trials of Cinryze, there were no deaths or serious
adverse reactions related to Cinryze administration, or discontinuations due
to treatment-emergent adverse events.
"Patients in the United States with HAE have been waiting for a safe and
effective emergency treatment for a long time," said Anthony Castaldo,
president of the U.S. and International Hereditary Angioedema Association.
"Cinryze as a prophylactic treatment has changed the lives of many people
living with this debilitating disease; we look forward to a day when this
important therapy will be approved in the acute setting."
Patient Labeling for Self Administration
Self-administration of Cinryze provides patients with the ability to
administer Cinryze themselves, when properly trained, in the comfort of their
own home. This is an important option for some patients because they may no
longer need to travel to their doctor's office - sometimes hours away - every
three to four days for in-office infusions. Cinryze is administered
intravenously though a small needle.
"We are pleased that the FDA has recognized the importance of
self-administration for patients," continued Milano. "Empowering patients to
administer Cinryze themselves allows them greater flexibility in managing
their disease."
About Cinryze(TM) (C1 esterase inhibitor [human])
Cinryze is a highly purified, pasteurized and nanofiltered plasma-derived
C1 esterase inhibitor product that has been approved by FDA for routine
prophylaxis against angioedema attacks in adolescent and adult patients with
HAE. C1 inhibitor therapy has been used acutely for more than 35 years in
Europe to treat patients with C1 inhibitor deficiency.
Cinryze has been generally well tolerated. The most common adverse
reactions observed have been upper respiratory infection, sinusitis, rash and
headache. No drug-related serious adverse events (SAEs) have been observed in
clinical trials. Severe hypersensitivity reactions may occur. Thrombotic
events have occurred in patients receiving high dose off-label C1 inhibitor
therapy well above the approved treatment dosage regimen. With any blood or
plasma derived product, there may be a risk of transmission of infectious
agents, e.g. viruses and, theoretically, the CJD agent. The risk has been
reduced by screening patients for prior exposure to certain virus infections
and by manufacturing steps to reduce the risk of viral transmission including
pasteurization and nanofiltration.
Cinryze is for intravenous use only. A dose of 1000 Units of Cinryze can
be administered every 3 or 4 days for routine prophylaxis against angioedema
attacks in HAE patients. Cinryze is administered at an injection rate of 1 mL
per minute.
About Hereditary Angioedema (HAE)
HAE is a rare, severely debilitating, life-threatening genetic disorder
caused by a deficiency of C1 inhibitor, a human plasma protein. This condition
is the result of a defect in the gene controlling the synthesis of C1
inhibitor. C1 inhibitor maintains the natural regulation of the contact,
complement, and fibrinolytic systems, that when left unrestricted, can
initiate or perpetuate an attack by consuming the already low levels of
endogenous C1 inhibitor in HAE patients. Patients with C1 inhibitor deficiency
experience recurrent, unpredictable, debilitating, and potentially life
threatening attacks of inflammation affecting the larynx, abdomen, face,
extremities and urogenital tract. Patients with HAE experience approximately
20 to 100 days of incapacitation per year. There are estimated to be at least
6,000 people with HAE in the United States.
For more information on HAE, visit the U.S. HAE Association's website at:
www.haea.org.
About ViroPharma Incorporated
ViroPharma Incorporated is a biopharmaceutical company dedicated to the
development and commercialization of products that address serious diseases
treated by physician specialists and in hospital settings. ViroPharma
commercializes Vancocin(R), approved for oral administration for treatment of
antibiotic-associated pseudomembranous colitis caused by Clostridium difficile
and enterocolitis caused by Staphylococcus aureus, including
methicillin-resistant strains. ViroPharma commercializes Cinryze(TM) (C1
esterase inhibitor [human]) for routine prophylaxis against angioedema attacks
in adolescent and adult patients with hereditary angioedema (HAE), also known
as C1 inhibitor deficiency (for prescribing information on ViroPharma's
commercial products, please download the package inserts at
http://www.viropharma.com/Products.aspx). ViroPharma currently focuses its
drug development activities in diseases including cytomegalovirus (CMV), HAE
and C. difficile.
ViroPharma routinely posts information, including press releases, which
may be important to investors in the investor relations and media sections of
our company's web site, www.viropharma.com. The company encourages investors
to consult these sections for more information on ViroPharma and our business.
Forward-Looking Statements
Certain statements in this press release contain forward-looking
statements that involve a number of risks and uncertainties. Forward-looking
statements provide the Company's current expectations or forecasts of future
events. Forward-looking statements in this press release include statements
regarding ViroPharma's clinical development programs. Our actual results could
differ materially from those results expressed in, or implied by, these
forward-looking statements. The development and commercialization of
pharmaceutical products is subject to risks and uncertainties. The Company is
evaluating the complete response letter from the FDA and there can be no
assurance that the Company will either amend its supplemental BLA or conduct
future clinical studies with Cinryze as a treatment for acute attacks of
hereditary angioedema. In the event the Company does conduct additional
clinical studies, there can be no assurance that such studies will demonstrate
that Cinryze successfully treats acute hereditary angioedema attacks or that
the FDA will ever approve Cinryze for the acute treatment of hereditary
angioedema. In addition, there can be no assurance that the FDA will not
approve a competing product which has been granted orphan drug designation
thereby preventing Cinryze from reaching the market for acute treatment of
HAE. These factors, and other factors, including, but not limited to those
described in ViroPharma's annual report on Form 10-K and quarterly reports on
Form 10-Q filed with the Securities and Exchange Commission during 2009, could
cause future results to differ materially from the expectations expressed in
this press release. The forward-looking statements contained in this press
release may become outdated over time. ViroPharma does not assume any
responsibility for updating any forward-looking statements.
SOURCE: ViroPharma Incorporated
- 06/04/2009
CONTACT: Robert A. Doody, Assistant Director, Investor Relations,
+1-610-321-6290, or Kristina M. Broadbelt (for media), Assistant Director,
PR & Advocacy, +1-610-321-2358
Web Site: http://www.viropharma.com
(VPHM)
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