REUTERS/Frederick
Murphy/CDC/Handout
Some of the ultrastructural morphology
displayed by an Ebola virus virion is revealed in this undated handout
colorized transmission electron micrograph obtained by Reuters on Aug. 1.
Sarepta Therapeutics could become an
even bigger part of the Ebola trade.
On Thursday, the company announced that two studies involving its Ebola
treatment candidates, "demonstrated no clinical or toxicologic safety
concerns with the company's drug candidates for the treatment of Ebola."
In premarket trade on Friday, shares of
Sarepta — which has a market cap a bit over $900 million — were soaring,
gaining as much as 11%.
In a statement, Michael Wong, senior
medical director at Sarepta said: "We believe these promising early
clinical safety results, coupled with the strong safety and efficacy data
generated from animal studies for all four PMO compounds, reinforce the use of
our PMOplus ®
chemistry platform to pursue potential treatments for deadly infectious
diseases such as Ebola and Marburg."
The results of the study are set
to be published in the November issue of the American Society for
Microbiology's journal " Antimicrobial Agents and Chemotherapy."
Sarepta is engaged in the development of
treatments for rare and infectious diseases and has been part of the
"Ebola trade" that has taken place since the summer and includes
stocks like Tekmira Pharmaceuticals and BioCryst Pharmaceuticals, as well as
the protective-gear-makers Lakeland Industries and Alpha Pro Tech.
Back in July, shares of Sarepta plunged after results from a trial involving the company's
drug eteplirsen for the treatment of patients with Duchenne muscular
dystrophy disappointed.
Year-to-date, Sarepta shares are up
about 9%, and just this week the stock was up 18% before Friday's premarket
gains.
Here's Thursday's full release from Sarepta:
CAMBRIDGE, Mass.--(BUSINESS WIRE)--Oct.
16, 2014-- Sarepta Therapeutics, Inc. (SRPT), a developer of innovative
RNA-based therapeutics, today announced the publication of results from two
single ascending-dose studies that demonstrated no clinical or toxicologic
safety concerns with the company's drug candidates for the treatment of Ebola
and Marburg virus, respectively. The study results are to be published in the
November issue of the American Society for Microbiology's
journal, Antimicrobial Agents and
Chemotherapy and are available online at dx.doi.org/10.1128/AAC.03442-14.
AVI-6002 for the treatment of Ebola is a
combination therapy of two phosphorodiamidate morpholino oligomers (PMOs
AVI-7537 and AVI-7539), which target the viral matrix proteins VP24 and VP35,
respectively. AVI-6003 for the treatment of Marburg is a combination therapy of
two PMOs, (AVI-7287 and AVI-7288), which target the viral proteins VP24 and NP,
respectively. These drug candidates use Sarepta's advanced and proprietary PMOplus®chemistry, which is also the basis of the
company's clinical-stage influenza drug candidate, AVI-7100. Results from
previous viral challenge studies of AVI-6002 and AVI-6003 in non-human primates
demonstrated prevention of disease development and death following exposure to
Ebola or Marburg virus. Subsequent animal studies demonstrated that for each
combination therapy, only one oligomer contributed to efficacy, and therefore,
the lead drug candidates for Ebola and Marburg have since become the single
compounds AVI-7537 and AVI-7288.
"We believe these promising early
clinical safety results, coupled with the strong safety and efficacy data
generated from animal studies for all four PMO compounds, reinforce the use of
our PMOplus® chemistry platform to
pursue potential treatments for deadly infectious diseases such as Ebola and
Marburg," said Michael Wong, senior medical director, infectious
diseases at Sarepta Therapeutics. "We are particularly encouraged to
see results such as these in the healthy human volunteers to what we have
learned to be the effective agents, AVI-7537 and AVI-7288. These compounds have
protected up to 80-100 percent of the non-human primates to Ebola and Marburg
virus challenge infections, respectively."
The two Phase I clinical studies were
randomized, double-blind, placebo-controlled trials designed to characterize
the safety, tolerability and pharmacokinetics of single doses of intravenous
formulations of AVI-6002 or AVI-6003 in healthy adult volunteers. In each
study, 30 subjects were enrolled in six cohorts receiving up to 9 mg/kg of the
combination drug candidates (4 active:1 placebo per cohort) for a total of 60
subjects. Results showed the compounds to be well-tolerated with no dose
limiting level demonstrated. No clinically significant or dose-dependent
effects were observed at any of the safety endpoints evaluated. The safety and
pharmacokinetics of the four PMOplus® compounds
comprising the two combination therapies were similar, regardless of the target
RNA sequence.
A previously reported Phase I MAD study
of AVI-7288 for the treatment of Marburg found no clinically significant or
dose-dependent effects on any of the safety endpoints evaluated when tested at
up to 16 mg/kg/day for 14 days in healthy adult volunteers. The results of
these clinical studies add to a growing body of evidence supporting the safety
of Sarepta's PMO-based chemistry platform across a broad range of disease
targets.
This work was conducted under contract
with the Joint Product Management Office of BioDefense
Therapeutics (BD-Tx).
When News Breaks Out, We Break In. (The 2014 Bloggies Finalist)
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