Vigil Neuroscience Announces Interim Data from its Ongoing Phase 1 Clinical Trial Evaluating VG-3927 in Healthy Volunteers Supporting Continued Development in Alzheimer’s Disease
July 24 2024 - 7:00AM
Vigil Neuroscience, Inc. (Nasdaq: VIGL), a clinical-stage
biotechnology company committed to harnessing the power of
microglia for the treatment of neurodegenerative diseases, today
announced interim data from its ongoing Phase 1 clinical trial of
VG-3927 in healthy volunteers. Collectively, the interim safety,
tolerability, pharmacokinetic (PK) and pharmacodynamic (PD) profile
supports continued clinical development of VG-3927 as a potential
once-daily oral therapy for AD. Additionally, these data showed
that VG-3927 demonstrated functional and durable target engagement.
“We are encouraged by these data which
demonstrate that VG-3927 has the potential to become a
differentiated approach to treating AD,” said Ivana
Magovčević-Liebisch, Ph.D., J.D., President and Chief Executive
Officer of Vigil. “With approximately 6.7 million Americans living
with AD, there is a critical need for new therapies with improved
safety and efficacy that can broadly address multiple aspects of AD
disease pathophysiology.”
“These interim clinical findings showed that
VG-3927 had a significant impact on sTREM2, a key biomarker in AD,
and supports VG-3927 as a potent molecule that functionally engages
TREM2 receptors in the brain. We achieved similar levels of sTREM2
target engagement with our monoclonal antibody iluzanebart in its
Phase 1 clinical trial. These data further strengthen our belief
that VG-3927 is acting as a TREM2 agonist and converting microglia
into a neuroprotective state,” said Petra Kaufmann, M.D., F.A.A.N.,
Chief Medical Officer of Vigil. “Combined with the extensive
preclinical data that we have collected, we believe VG-3927 is
well-positioned for further development in AD. We look forward to
advancing VG-3927 with the goal of ultimately providing a new
therapy to those impacted by AD.”
The ongoing trial is a Phase 1 single and
multiple ascending dose trial to assess the safety, tolerability,
PK and PD of VG-3927. As of June 30, 2024, the trial had enrolled
80 healthy volunteers, of which 60 have received VG-3927 across
multiple SAD and MAD cohorts.
Key takeaways from the interim data include the
following:
- Safety and tolerability profile
observed in individual doses in six SAD and two MAD cohorts in the
ongoing Phase 1 clinical trial supports continued clinical
development of VG-3927.
- All adverse events (AEs) were mild
or moderate in severity, and all AEs resolved without intervention.
No serious adverse events have been reported to date.
- VG-3927 demonstrated a predictable
PK profile that is supportive of once-daily dosing.
- In the SAD and MAD cohorts, VG-3927
achieved a robust and sustained decrease of sTREM2 in the CSF.
- VG-3927 also showed an increase in
osteopontin/secreted phosphoprotein 1 (SPP1), a biomarker
associated with neuroprotective microglia, after repeat
dosing.
- An effect on soluble Colony
Stimulating Factor 1 Receptor (sCSF1R), a microglial trophic
factor, has not been observed to date.
As part of the Phase 1 clinical trial, the
Company has commenced screening for a cohort of AD patients,
including some participants who carry TREM2 or other
disease-related variants to explore the biomarker response of
VG-3927 after a single dose. The Company plans to use these data to
inform the development strategy for subsequent and larger trials
evaluating VG-3927 in AD. Vigil plans to report the complete Phase
1 clinical data, including data from the AD patient cohort, in the
first quarter of 2025.
The Company also announced today that it plans
to present new preclinical data from its small molecule program,
including in vivo AD-related functional data, and clinical data
from the VG-3927 SAD cohorts in the Phase 1 clinical trial, in an
oral presentation at the upcoming 2024 Alzheimer’s Association
International Conference (AAIC) taking place on July 28 – August 1,
2024 in Philadelphia, Pennsylvania and virtually. Please click here
for more information on Vigil’s presentations at AAIC.
About Vigil
Neuroscience Vigil Neuroscience is a clinical-stage
biotechnology company focused on developing treatments for both
rare and common neurodegenerative diseases by restoring the
vigilance of microglia, the sentinel immune cells of the brain.
Vigil is utilizing the tools of modern neuroscience drug
development across multiple therapeutic modalities in its efforts
to develop precision-based therapies to improve the lives of
patients and their families. Iluzanebart, Vigil’s lead clinical
candidate, is a fully human monoclonal antibody agonist targeting
human triggering receptor expressed on myeloid cells 2 (TREM2) in
people with adult-onset leukoencephalopathy with axonal spheroids
and pigmented glia (ALSP), a rare and fatal neurodegenerative
disease. Vigil is also developing VG-3927, a novel small molecule
TREM2 agonist, to treat common neurodegenerative diseases
associated with microglial dysfunction, with an initial focus on
Alzheimer’s disease (AD) patients, including some who carry TREM2
and other disease-associated variants.
Forward-Looking Statements
This press release includes certain disclosures
that contain “forward-looking statements” of Vigil Neuroscience
(“Vigil” or the “Company”) that are made pursuant to the safe
harbor provisions of the federal securities laws, including,
without limitation, express or implied statements regarding:
Vigil’s strategy, business plans and focus; the potential
therapeutic benefit of our product candidates, including VG-3927,
and the expected therapeutic benefits of such programs as well as
the potential market size and ability to address a major unmet
medical need; the timing and availability of future interim data
readouts as well as the complete Phase 1 clinical data from
VG-3927’s Phase 1 clinical trial; VG-3927’s potential as a TREM2
agonist and its ability to convert microglia into a neuroprotective
state. Forward-looking statements are based on Vigil’s current
expectations and are subject to inherent uncertainties, risks and
assumptions that are difficult to predict. Factors that could cause
actual results to differ include, but are not limited to, risks and
uncertainties related to uncertainties inherent in the development
of product candidates, including the conduct of research activities
and the conduct of clinical trials; whether results from
preclinical studies and clinical trials will be predictive of the
results of later preclinical studies and clinical trials; the
timing and content of additional regulatory interactions with the
FDA – including the Company’s discussions regarding the partial
clinical hold on VG-3927; as well as the risks and uncertainties
identified in the Company’s filings with the Securities and
Exchange Commission (SEC), including Vigil’s Quarterly Report on
Form 10-Q for the quarter ended March 31, 2024 and in any
subsequent filings Vigil makes with the SEC. Forward-looking
statements contained in this announcement are made as of this date,
and Vigil undertakes no duty to update such information except as
required under applicable law. Readers should not rely upon the
information on this page as current or accurate after its
publication date.
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that may be important to investors in the 'Investors' section of
its website at https://www.vigilneuro.com. The company encourages
investors and potential investors to consult our website regularly
for important information about Vigil Neuroscience.
Investor Contact: Leah
Gibson Vice President, Investor Relations &
Corporate Communications Vigil Neuroscience,
Inc. lgibson@vigilneuro.com
Media Contact:Megan McGrath CTD
Comms, LLC megan@ctdcomms.com
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