THE WOODLANDS, Texas--(BUSINESS WIRE)--
Opexa Therapeutics, Inc. (NASDAQ: OPXA), a biopharmaceutical
company developing personalized otherapies for autoimmune disorders
including multiple sclerosis (MS) and neuromyelitis optica (NMO), today
announced results of a preclinical study, which show that T-cell
immunotherapy with attenuated antigen-specific T-cells suppress the
T-cell response to Aquaporin-4 (AQP4) in a dose-dependent manner,
compared to vehicle control, as measured by reduction in both
Aquaporin-4 reactive T-cell (ARTC) proliferation and associated cytokine
activity. The results were statistically significant.
In NMO, activated T-cells (ARTC) mount an attack against Aquaporin-4,
the autoantigen in NMO, leading to secondary demyelination of nerve
fibers within the optic nerves and the spinal cord, resulting in the
clinical symptoms of the disease. Opexa’s therapeutic approach is to
suppress or reduce the number of these activated ARTC in patients with
NMO. The results of the preclinical animal study provide evidence that
T-cell immunotherapy reduces the level of activated ARTC in a murine
(mouse) model.
“The results of the bioactivity study are encouraging as they support
our proposed mechanism of action for OPX-212 in NMO,” stated Neil K.
Warma, Opexa’s President and Chief Executive Officer. “NMO is a complex
autoimmune disorder and we believe we are unique in developing a
targeted and personalized T-cell immunotherapy for this disease which
currently has no approved treatments. We believe that OPX-212, by
addressing the T-cell component of the disease, may target the root
cause of NMO. There is a significant unmet medical need for patients
with NMO and this animal study is an important step in our development
program for the treatment of patients with this debilitating disease. We
are continuing with the preclinical development activities of OPX-212,
including completing the manufacturing runs and expect to submit the IND
to the U.S. FDA and be in a position to open a Phase 1/2 clinical study
in NMO patients in the first half of 2016, assuming the availability of
sufficient resources.”
“Opexa’s T-cell immunotherapy, OPX-212, has an hypothesized mechanism of
action to reduce the number of and/or regulate Aquaporin-4 reactive
T-cells, thereby reducing the frequency of clinical relapses and
subsequent progression in disability,” stated Donald Healey, PhD,
Opexa’s Chief Scientific Officer. “Aquaporin-4 reactive T-cells support
pathogenic autoantibody production from B-cells in NMO, but also drive
the T-cell mediated cytokine signaling and infiltration of inflammatory
cells that also contribute to disease pathology. OPX-212 aims to restore
immune tolerance in NMO patients by specifically targeting ARTC while
leaving the rest of the patient’s immune system intact.”
As part of Opexa’s preclinical development activities for OPX-212, Opexa
conducted a bioactivity study to demonstrate the ability of T-cell
immunotherapy using attenuated T-cells to suppress a T-cell response to
the NMO-associated autoantigen, AQP4. No animal model of NMO has been
described that exhibits both endogenous T-cell dependent immunity and
autoantibody production to AQP4 and that subsequently leads to the
immunopathology and clinical symptoms observed in human NMO. To study
the bio-activity of attenuated T-cells on AQP4 T-cell immunity, mice
were pre-treated with attenuated antigen-specific T-cells and
subsequently primed with AQP4 antigen, following which ARTC and
associated inflammatory cytokine levels were measured.
NMO, also known as neuromyelitis optica spectrum disorder (NMOSD), is a
rare autoimmune disorder, which is designated as an Orphan Disease by
the U.S. Food and Drug Administration. There is currently no cure and
there are no approved therapies for this disease, worldwide.
About OPX-212
OPX-212 is Opexa’s personalized T-cell immunotherapy in development for
the treatment of NMO. It will be specifically tailored to each patient’s
immune response to Aquaporin-4. In NMO, activated T-cells mount an
attack against Aquaporin-4, the autoantigen in NMO, leading to secondary
demyelination of nerve fibers within the optic nerves and the spinal
cord, resulting in the clinical symptoms of the disease. Symptoms of the
attack include blindness in one or both eyes followed within days or
weeks by varying degrees of paralysis in the arms and legs. OPX-212 has
an hypothesized mechanism of action to reduce the number and/or regulate
aquaporin-4 reactive T-cells (ARTCs), thereby reducing the frequency of
clinical relapses and subsequent progression in disability. OPX-212 will
be manufactured using ImmPath®, Opexa Therapeutics’
proprietary T-cell immunotherapy platform technology.
About Opexa
Opexa is a biopharmaceutical company developing a personalized
immunotherapy with the potential to treat major illnesses, including
multiple sclerosis (MS) as well as other autoimmune diseases such as
neuromyelitis optica (NMO). These therapies are based on Opexa’s
proprietary T-cell technology. The Company’s leading therapy candidate,
Tcelna®, is a personalized T-cell immunotherapy that is in a Phase IIb
clinical development program (the Abili-T trial) for the treatment of
secondary progressive MS. Tcelna consists of myelin-reactive T-cells,
which are expanded ex vivo from the patient’s peripheral blood and
reintroduced into the same patient in an attenuated form via
subcutaneous injections. This process triggers a potent immune response
against specific subsets of autoreactive T-cells known to attack myelin
for each individual patient.
For more information, visit the Opexa Therapeutics website at www.opexatherapeutics.com
or follow company news on Twitter
via @OpexaCEO.
Cautionary Statement Relating to Forward-Looking Information for the
Purpose of "Safe Harbor" Provisions of the Private Securities Litigation
Reform Act of 1995
Statements contained in this release, other than statements of
historical fact, constitute "forward-looking statements" within the
meaning of the Private Securities Litigation Reform Act of 1995. The
words "expects," "believes," "may," "intends," "potential" and similar
expressions are intended to identify forward-looking statements. These
forward-looking statements do not constitute guarantees of future
performance. Investors are cautioned that forward-looking statements,
including without limitation statements regarding the safety, efficacy
and projected development timeline of drug candidates such as Tcelna®
and OPX-212 constitute forward-looking statements. These forward-looking
statements are based upon our current expectations and involve
assumptions that may never materialize or may prove to be incorrect.
Actual results and the timing of events could differ materially from
those anticipated in such forward-looking statements as a result of
various risks and uncertainties, which include without limitation our
ability to raise additional capital to continue our development
programs, our ability to successfully develop potential products such as
Tcelna and OPX-212, our ability to obtain, maintain and protect
intellectual property rights (including for Tcelna and OPX-212), as well
as other risks associated with the process of discovering, developing
and commercializing drug candidates that are safe and effective for use
as human therapeutics. These and other risks are described in detail in
our SEC filings, including our Annual Report on Form 10-K for the year
ended December 31, 2021 and our Quarterly Report on Form 10-Q for the
quarter ended September 30, 2022. All forward-looking statements
contained in this release speak only as of the date on which they were
first made by us, and we undertake no obligation to update such
statements to reflect events that occur or circumstances that exist
after such date.
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Source: Opexa Therapeutics, Inc.