- Interim Data: Study Achieves Primary End
Point Demonstrating Clinical and Statistically Significant
Reductions Compared to Placebo in Agitation Associated with
Dementia Due to Alzheimer’s Disease -
IGC Pharma, Inc. (“IGC Pharma”, “IGC”, or the “Company”) (NYSE
American: IGC) today announced the results of an interim analysis
of its ongoing Phase 2 trial investigating IGC-AD1 as a treatment
for Agitation in dementia from Alzheimer’s Disease (“AAD”).
The interim data demonstrates a clinical and statistically
significant reduction in agitation compared to placebo in patients
with Alzheimer’s disease, indicating strong therapeutic potential
for IGC-AD1.
The study's primary goal is to assess the change in AAD after
six weeks using a standard scale, the Cohen Mansfield Agitation
Inventory (“CMAI”). Based on interim data, patients taking IGC-AD1,
on average, experienced a more significant reduction in agitation
scores compared to those on placebo, and the positive effects were
observed as early as week two of the trial.
At the primary outcome, assessing the change in agitation as
measured by the CMAI at week 6, the Cohen’s d effect size
indicating the superiority of IGC-ADI over placebo was 0.66. The
CMAI Least Square (“LS”) mean difference between active, and
placebo was -10.45, with a p-value of 0.037 (for combined week two
and week six results). In addition, at the pre-specified secondary
endpoint, change at week two, the effect size was 0.79. The Cohen’s
d is a standardized statistical effect size that describes the
magnitude of the difference between two groups, taking into account
the variability in outcomes.
Pre-Specified Interim
Results:
The IGC-AD1 Phase 2 is an ongoing multi-site, randomized,
double-blind, placebo-controlled clinical trial that continues to
enroll. IGC-AD1 is an oral liquid formulation administered twice
daily for six weeks with no placebo run-in and titration to full
dose over two days. Agitation is rated at the trial site, at
baseline, week 2, and week 6, by a trained practitioner using the
CMAI, a scale designed to measure AAD.
"We are excited with the positive interim results from the Phase
2 trial of IGC-AD1 for agitation in dementia due to Alzheimer's
disease. IGC-AD1’s interim results demonstrate a clinical and
statistically significant reduction in agitation compared to
placebo, suggesting a strong plausibility to address a substantial
unmet medical need. This interim data validates IGC-AD1's potential
as a transformative therapeutic option with a large market
opportunity in Alzheimer's disease management. We are actively
pursuing next steps, including with regulators, and remain
committed to advancing IGC-AD1 toward commercialization. We foresee
a medication that can help alleviate caregiver burden and family
distress as managing Alzheimer’s patients, especially ones with
agitation, can have a significant emotional toll on families. With
IGC-AD1's promising clinical profile, we are confident in its
ability, subject to further trials, to improve patient outcomes and
drive shareholder value,” said Ram Mukunda, CEO of IGC Pharma.
IGC-AD1 interim
Statistics
Table 1 sets out the difference in LS mean from the baseline
CMAI score for the active and the placebo groups at week six. The
LS mean CMAI score difference between the active and placebo groups
at week six is -10.45. At weeks 2 and 6, the interim Cohen's d
effect size is 0.79 and 0.66, respectively, with a p-value of 0.037
for weeks 2 and 6 combined. This interim data suggests clinical and
statistically significant improvement in AAD for the group
receiving IGC-AD1 compared to placebo.
Comparison with Existing
Treatment
In May 2023, the U.S. Food and Drug Administration (“FDA”)
approved Brexpiprazole, an atypical antipsychotic, with a boxed
warning. This approval followed a significantly larger 12- week
Phase 3 trial, which showed a difference in LS mean from baseline
CMAI between active and placebo of -5.32, a Cohen's d effect size
of 0.35, and a p-value of 0.003 (Lee et al., 2023). The findings
from several Brexpiprazole trials are summarized in Table 1
below.
Table 1. Results of IGC-AD1 Interim Analysis
and Illustrative Brexpiprazole Phase 3 Results1
IGC AD1
Brexpiprazole Phase 3
Phase 2 Interim
results
Phase 3
Two fixed doses
(Lee et al. 2023)
Phase 3
fixed dose
(Grossberg et al.
2020)
Phase 3
Post Hoc (subgroup)
(Grossberg et al.
2020)
Trial Duration
6-weeks
12-weeks
12-weeks
12-weeks
ClinicalTrials.gov ID
NCT05543681
NCT03548584
NCT01862640
NCT01922258
Dosing
1 ml (bid)
2mg/3mg (qd)
2mg (qd)
2mg (qd)
End Of Treatment (EOT)
Week 6
Week 12
Week 12
Week 12
Primary Outcome
Baseline to Week
6
Baseline to Week 12
Baseline to Week 12
Baseline to Week 12
Statistical Model
MMRM
MMRM
MMRM
MMRM
Agitation Scale
CMAI
CMAI
CMAI
CMAI
Treatment Difference in LS Mean
from Baseline CMAI between Active and Placebo at EOT (95% CI)
-10.46
(-20.20, -0.72)
-5.32
(-8.77, -1.87)
-3.77
(-7.38, -0.17)
-5.06
(-8.99, -1.13)
Cohen’s d Effect Size
0.66
0.35
0.25
0.41
p-value
0.037
0.003
0.040
0.012
- The comparison is for illustrative purposes and is not intended
to provide a direct comparison of effectiveness between IGC-AD1 and
Brexpiprazole.
IGC-AD1 as a Treatment for Agitation in
Alzheimer’s Disease
In 2023, the number of Americans living with Alzheimer’s was
estimated at 6.7 million. According to one estimate, as many as 76%
of them suffer from AAD (Van der Mussele et al., 2015), which is
associated with an accelerated cognitive decline, increased
caregiver burden, increased hospitalization, and increased need for
medication, all significantly diminishing the quality of life for
patients. Current therapies carry black box warnings, indicative of
serious adverse reactions that may lead to death or serious injury.
IGC-AD1 is designed to target AAD’s underlying causes and address
the unmet need for a safe and effective therapy.
Neuroinflammation, neurotransmitter imbalance, and CB1 receptor
dysfunctions are all associated with agitation in Alzheimer’s
disease (Yasuno et al., 2023; Manuel et al., 2014). In addition,
upregulation of inflammasome-3 has been shown to lead to
neuroinflammation, consequently leading to aggressive behavior (Yu
et al., 2023). IGC-AD1’s formulation combines a CB1 receptor
partial agonist with anti-neuroinflammatory properties that help
balance neurotransmitter imbalance and an inflammasome inhibitor
that targets the upregulation of inflammasome-3.
The 146-pateint IGC-AD1 trial, for which these interim results
are presented, continues to enroll in the U.S. and Canada. As the
interim results are based on a small number of patients (n=26),
there is no guarantee that the positive interim results will hold
up as more patients are enrolled in the trial. Learn more and find
information about recruitment centers at
https://clinicaltrials.gov/study/NCT05543681.
About IGC Pharma Inc. (IGC):
IGC Pharma Inc. (“IGC”) is focused on Alzheimer's disease,
developing innovative solutions to address this devastating
illness. The Company's mission is to transform the landscape of
Alzheimer's treatment with a robust pipeline of five promising drug
candidates. IGC-AD1 and LMP target the hallmarks of Alzheimer's
disease, including neuroinflammation, Aβ plaques, and
neurofibrillary tangles. IGC-AD1 is currently undergoing a Phase 2
clinical trial for agitation in dementia associated with
Alzheimer's (clinicaltrials.gov, CT05543681). TGR-63 disrupts the
progression of Alzheimer's by targeting Aβ plaques. IGC-M3,
currently in preclinical development, aims to inhibit the
aggregation of Aβ plaques, potentially impacting early-stage
Alzheimer's. IGC-1C, also in preclinical stages, targets tau
protein and neurofibrillary tangles, representing a
forward-thinking approach to Alzheimer's therapy. In addition to
its drug development pipeline, IGC Pharma seeks to leverage
Artificial Intelligence (“AI”) for Alzheimer's research. Their AI
projects encompass various areas, including clinical trial
optimization and early detection of Alzheimer's.
Forward-Looking Statements:
This press release contains forward-looking statements. These
forward-looking statements are based largely on IGC Pharma’s
expectations and are subject to several risks and uncertainties,
certain of which are beyond IGC Pharma’s control. Actual results
could differ materially from these forward-looking statements as a
result of, among other factors, the Company’s failure or inability
to commercialize one or more of the Company’s products or
technologies, including the products or formulations described in
this release, or failure to obtain regulatory approval for the
products or formulations, where required, or government regulations
affecting AI or the AI algorithms not working as intended or
producing accurate predictions; general economic conditions that
are less favorable than expected; the FDA’s general position
regarding cannabis- and hemp-based products; and other factors,
many of which are discussed in IGC Pharma’s U.S. Securities and
Exchange Commission ("SEC") filings. IGC Pharma incorporates by
reference the human trial disclosures and Risk Factors identified
in its Annual Report on Form 10-K filed with the SEC on July 7,
2023, and Quarterly Report on Form 10-Q filed with the SEC on
February 14, 2024, as if fully incorporated and restated herein.
Considering these risks and uncertainties, there can be no
assurance that the forward-looking information contained in this
release will occur.
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Investors IMS Investor Relations Rosalyn Christian
igc@imsinvestorrelations.com (203) 972-9200
Media JVPRNY Janet Vasquez jvasquez@jvprny.com (212)
645-5498
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