MeiraGTx Holdings plc (Nasdaq: MGTX), a vertically integrated,
clinical-stage genetic medicines company, today announced top-line
data from its clinical bridging study of AAV-GAD for the treatment
of Parkinson’s disease, MGT-GAD-025.
MGT-GAD-025 is a 6-month, three-arm, randomized, double-blind,
sham-controlled study using AAV-GAD drug product manufactured by
MeiraGTx at its wholly-owned facilities with its commercial
platform process. Participants had idiopathic Parkinson's disease,
a history of levodopa responsiveness for at least 12 months, and a
UPDRS Part 3 score of ≥25 points in the "off" state. Fourteen
subjects were randomized to one of three groups (high dose n=5, low
dose n=5, and sham n=4).
Subjects received either AAV-GAD infused bilaterally into the
subthalamic nucleus or a sham procedure in a blinded fashion. The
total dose per treated participant was 7.0×1010 vg (low dose
group) or 21×1010 vg (high dose group). The primary objective
of the study was to evaluate the safety and tolerability of
AAV-GAD, with exploratory efficacy endpoints including the mean
change from baseline to Week 26 in MDS-UPDRS Part 3 (motor
examination) scores in the “off” state and the Parkinson’s Disease
Questionnaire (PDQ-39) score, a key patient-reported quality of
life measure in Parkinson’s disease. Subjects who completed this
trial may enroll in a long-term follow-up study (NCT05894343),
where they will be monitored for a total of five years
post-treatment.
Top-line data summary:
- AAV-GAD was safe and well tolerated, with no serious adverse
events (SAEs) related to AAV-GAD treatment.
- At Week 26, a statistically significant 18-point average
improvement from baseline in UPDRS Part 3 “off” medication score
was demonstrated in the high dose group (p=0.03), with no
significant change in the sham or low dose groups.
- Significant improvements from baseline in the disease-specific,
patient-reported quality of life PDQ-39 score were demonstrated in
both the high and low dose groups with no significant change in the
sham group at Week 26:
- In the high dose AAV-GAD group, the PDQ-39 score improved by 8
points from baseline (p=0.02), the low dose group improved by 6
points from baseline (p=0.04), while the 0.2 point worsening in the
sham surgery group was not statistically significant.
- A dose response in PDQ-39 score was observed, with 100% of
participants in the high dose group, 60% of participants in the low
dose group, and 25% of participants in the sham surgery group
reporting an improvement.
- For the PDQ-39 score, there was a trend to significance between
the high dose and sham surgery groups at 6 months (n=4 evaluable
per group).
Dr. Ali Rezai, M.D., executive chair of the Rockefeller
Neuroscience Institute at West Virginia University (WVU), past
president of the Congress of Neurological Surgeons, and principal
investigator of the AAV-GAD study, stated, “These safety and
outcome results are excellent. The extent of motor score
improvements in patients who received the high dose treatment
combined with significant quality of life improvement measures are
very encouraging for both patients and physicians.”
“We are excited about these impressive clinical data in
Parkinson’s disease,” said Alexandria Forbes, Ph.D., president and
chief executive officer of MeiraGTx. “With material made using our
proprietary production process at commercial scale, we have
demonstrated that AAV-GAD is safe at all doses studied, including a
higher dose than previously tested. We have now treated a total of
58 patients in this development program in 3 independent
multicenter clinical studies and have seen no SAEs related to
AAV-GAD treatment.”
Dr. Forbes continued, “With the completion of this randomized,
double-blinded bridging study, we have also demonstrated with even
very small numbers of subjects that AAV-GAD treatment results in
significant and clinically meaningful changes in key efficacy
endpoints in Parkinson’s disease. For the UPDRS Part 3 in the “off”
state, a change of 5 to 10 points is considered clinically
meaningful. The 18-point change observed in the high dose arm in
this study underscores the very substantial impact of AAV-GAD
treatment in these Parkinson’s patients. Similarly, for the PDQ-39,
where a 2 to 4-point change is considered clinically meaningful,
the 8-point and 6-point changes observed in the high and low dose
groups, respectively, again indicate a substantial and clinically
meaningful impact of AAV-GAD treatment.”
“These data demonstrate the impact of using highly targeted
local delivery of gene-based therapy to correct the aberrant
circuitry that results from the depletion of dopamine in the brain
of idiopathic Parkinson’s patients as the disease progresses.
AAV-GAD treatment is designed to normalize circuit function in all
forms of Parkinson’s disease with its potential benefit not limited
to any single type of Parkinson’s. The significant, substantial,
and clinically meaningful changes observed in this small,
sham-controlled study provide us with a clear path forward in our
clinical development strategy and underpin our discussions with
regulators in the US, Europe, and Japan with the goal of initiating
a Phase 3 study to support approval of this disease-modifying
treatment globally.”
About AAV-GAD
Parkinson’s disease (PD) is the second most common
neurodegenerative disease after Alzheimer’s, with nearly one
million people in the U.S. currently living with Parkinson’s
disease and approximately 90,000 new patients diagnosed annually in
the U.S. There are more than 10 million people worldwide currently
living with PD. Most individuals with PD initially respond to
dopamine replacement therapy, yet for a large percentage of
patients, over time, this type of treatment is no longer
sufficiently helpful while adverse effects of medication can also
occur, leading to a considerable reduction in quality of life and
the ability to function effectively. The cause of Parkinson’s
disease is unknown for a majority of patients, while a much smaller
percentage have a known genetic cause, but in all cases, there is
dysfunction of the key circuits that control movement. AAV-GAD is
an investigational gene therapy designed to reprogram these
dysfunctional brain circuits through the local production of GABA,
a chemical neurotransmitter that can help restore more normal
activity to these critical cells in any form of PD. AAV-GAD is
delivered via a one-time infusion through a minimally invasive
procedure, using a MeiraGTx proprietary device that allows infusion
of the equivalent of one drop of gene therapy solution into the
subthalamic nucleus, a key regulator of the circuits responsible
for normal movement.
About MeiraGTx
MeiraGTx (Nasdaq: MGTX) is a vertically integrated,
clinical-stage genetic medicines company with a broad pipeline of
late-stage clinical programs supported by end-to-end manufacturing
capabilities. MeiraGTx has internal plasmid production for GMP, two
GMP viral vector production facilities as well as an in-house
Quality Control hub for stability and release, all fit for IND
through commercial supply. In addition, MeiraGTx has developed a
proprietary manufacturing platform with leading yield and quality
aspects and commercial readiness, MeiraGTx has core capabilities in
viral vector design and optimization and a transformative
riboswitch gene regulation platform technology that allows for the
precise, dose-responsive control of gene expression by oral small
molecules. MeiraGTx is focusing the riboswitch platform on
the delivery of metabolic peptides, including GLP-1, GIP,
Glucagon, and PYY, using oral small molecules, as well as cell
therapy for oncology and autoimmune diseases. MeiraGTx has
developed the technology to apply genetic medicine to more common
diseases, increasing efficacy, addressing novel targets, and
expanding access in some of the largest disease areas where the
unmet need remains high.
For more information, please visit www.meiragtx.com
Forward Looking Statement
This press release contains forward-looking statements within
the meaning of the Private Securities Litigation Reform Act of
1995. All statements contained in this press release that do not
relate to matters of historical fact should be considered
forward-looking statements, including, without limitation,
statements regarding the development and efficacy of AAV-GAD, plans
to advance AAV-GAD into Phase 3 clinical trial and anticipated
milestones regarding our clinical data, reporting of such data and
the timing of results of data and regulatory matters, as well as
statements that include the words “expect,” “will,” “intend,”
“plan,” “believe,” “project,” “forecast,” “estimate,” “may,”
“could,” “should,” “would,” “continue,” “anticipate” and similar
statements of a future or forward-looking nature. These
forward-looking statements are based on management’s current
expectations. These statements are neither promises nor guarantees,
but involve known and unknown risks, uncertainties and other
important factors that may cause actual results, performance or
achievements to be materially different from any future results,
performance or achievements expressed or implied by the
forward-looking statements, including, but not limited to, our
incurrence of significant losses; any inability to achieve or
maintain profitability, raise additional capital, repay our debt
obligations, identify additional and develop existing product
candidates, successfully execute strategic transactions or
priorities, bring product candidates to market, expansion of our
manufacturing facilities and processes, successfully enroll
patients in and complete clinical trials, accurately predict growth
assumptions, recognize benefits of any orphan drug designations,
retain key personnel or attract qualified employees, or incur
expected levels of operating expenses; the impact of pandemics,
epidemics, or outbreaks of infectious diseases on the status,
enrollment, timing and results of our clinical trials and on our
business, results of operations and financial condition; failure of
early data to predict eventual outcomes; failure to obtain FDA or
other regulatory approval for product candidates within expected
time frames or at all; the novel nature and impact of negative
public opinion of gene therapy; failure to comply with ongoing
regulatory obligations; contamination or shortage of raw materials
or other manufacturing issues; changes in healthcare laws; risks
associated with our international operations; significant
competition in the pharmaceutical and biotechnology industries;
dependence on third parties; risks related to intellectual
property; changes in tax policy or treatment; our ability to
utilize our loss and tax credit carryforwards; litigation risks;
and the other important factors discussed under the caption “Risk
Factors” in our Quarterly Report on Form 10-Q for the quarter ended
June 30, 2024, as such factors may be updated from time to time in
our other filings with the SEC, which are accessible on the SEC’s
website at www.sec.gov. These and other important factors could
cause actual results to differ materially from those indicated by
the forward-looking statements made in this press release. Any such
forward-looking statements represent management’s estimates as of
the date of this press release. While we may elect to update such
forward-looking statements at some point in the future, unless
required by law, we disclaim any obligation to do so, even if
subsequent events cause our views to change. Thus, one should not
assume that our silence over time means that actual events are
bearing out as expressed or implied in such forward-looking
statements. These forward-looking statements should not be relied
upon as representing our views as of any date subsequent to the
date of this press release.
Contacts
Investors:MeiraGTxInvestors@meiragtx.com
or
Media:Jason Braco, Ph.D.LifeSci
Communicationsjbraco@lifescicomms.com
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