- Quantitative Electroencephalogram (qEEG) in healthy subjects
administered single doses of oral brexanolone, a neuroactive
steroid (NAS), confirmed GABAA modulation
- Rapid and durable CNS target engagement confirms effective
oral delivery of bioidentical brexanolone
- Promising results support continued development of oral
brexanolone for the treatment of neuropsychiatric
disorders
SALT
LAKE CITY, Oct. 10, 2024 /PRNewswire/ -- Lipocine
Inc. (NASDAQ: LPCN), a biopharmaceutical company leveraging its
proprietary technology platform to augment therapeutics through
effective oral delivery, today announced positive data from its
qEEG study of its oral brexanolone, a proprietary bioidentical NAS
being developed for the treatment of post-partum depression (PPD).
Changes in spectral power (a quantitative measure of the strength
or intensity of specific brain wave frequencies) are frequently
used to characterize the effects of drug candidates and may have
utility in indication and dose selection in CNS clinical
trials. The results indicate robust central nervous system
(CNS) activity of oral brexanolone, with concentration- and
time-dependent post-dose changes in qEEG. These results confirm
GABAA positive allosteric modulation and support future
development of oral brexanolone in neuropsychiatric
indications.
"We are pleased with the qEEG results that confirm target
engagement of oral bioidentical brexanolone, which suggests
potential utility in treating numerous psychiatry indications,
including depression and anxiety, and neurology indications such as
essential tremor and epilepsy," said Dr. Mahesh Patel, President and CEO of Lipocine Inc.
"These positive biomarker results and favorable safety profile
support further development of oral brexanolone."
This Phase 1 study evaluated qEEG spectral power changes after
administration of oral brexanolone. Healthy postmenopausal females
(N=12) were administered single doses of oral brexanolone. EEG
recordings and blood samples were collected pre- and post-dose (2,
4 and 12 hours). EEG recordings were obtained using a wireless,
19-electrode EEG monitoring device (Zeto Inc., Santa Clara, CA). Spectral analysis was
performed and EEG band amplitudes were analyzed for the oscillatory
spectra. Pre-dose-adjusted spectral power values at each
single-electrode location were determined for each post-dose
timepoint.
Following a single clinically relevant dose of oral brexanolone,
subjects showed mean changes in all oscillatory spectral power
bands. As shown in Fig. 1, theta and alpha1 band power were
significantly increased in posterior cortical regions, while alpha2
band power decreased. There was considerable beta band amplitude
increase, including significant increase in beta2 amplitude across
all cortical brain areas Most of the treatment-related EEG changes
were rapid occurring as early as 2 hours, with maximum and
significant mean contrast values at 4 hours post dose (consistent
with Tmax) with appreciable effects lasting 12 hours
post-dose.
The observed qEEG changes following oral brexanolone
administration are consistent with therapies effective in managing
depression, anxiety, tremor, and seizures.1-5
Oral brexanolone was well-tolerated in this Phase 1 study. The
safety profile was consistent with safety data from clinical
studies previously conducted by Lipocine with minimal CNS
depressant effects.
Lipocine plans to present the additional details and analyses
from this EEG study at upcoming scientific meetings.
About Quantitative Electroencephalogram (qEEG)
Quantitative Electroencephalogram (qEEG) is an advanced
neuroimaging technique used to measure electrical activity in the
brain with a high degree of precision and detail. qEEG uses
mathematical and statistical methods to analyze the electrical
signals generated by the brain and convert them into quantitative
metrics. By translating these signals into a digital format, qEEG
allows for the identification and assessment of specific brain wave
frequencies -- such as delta, theta, alpha, beta, and gamma waves
-- associated with different states of cognition, emotion, and
behavior. This analysis allows researchers to detect subtle changes
in brain function that may be induced by a drug, providing
important insights into its mechanism of action. In the context of
drug development, qEEG is used to evaluate the effect of new
therapies on the central nervous system (CNS) by monitoring shifts
in brain wave patterns that correlate with therapeutic outcomes.
This helps determine whether the drug is acting on the desired
neural circuits, provides early evidence of efficacy, and may
support dose selection for future clinical trials.
About Lipocine
Lipocine is a biopharmaceutical company leveraging its
proprietary technology platform to augment therapeutics through
effective oral delivery to develop differentiated products.
Lipocine has drug candidates in development as well as drug
candidates for which we are exploring partnerships. Our drug
candidates represent enablement of differentiated, patient friendly
oral delivery options for favorable benefit to risk profile which
target large addressable markets with significant unmet medical
needs.
Lipocine's clinical development candidates include: LPCN 1154,
oral brexanolone, for the potential treatment of postpartum
depression, LPCN 2101 for the potential treatment of epilepsy, LPCN
2203 an oral candidate targeted for the management of essential
tremor, LPCN 2401 an oral proprietary anabolic androgen receptor
agonist, as an adjunct therapy to incretin mimetics, as an aid for
improved body composition in obesity management and LPCN 1148, a
novel androgen receptor agonist prodrug for oral administration
targeted for the management of symptoms associated with liver
cirrhosis. Lipocine is exploring partnering opportunities for
LPCN 1107, our candidate for prevention of preterm birth, LPCN
1154, for rapid relief of postpartum depression, LPCN 2401 for
obesity management, LPCN 1148, for the management of decompensated
cirrhosis, and LPCN 1144, our candidate for treatment of
non-cirrhotic NASH. TLANDO, a novel oral prodrug of
testosterone containing testosterone undecanoate developed by
Lipocine, is approved by the FDA for conditions associated with a
deficiency of endogenous testosterone, also known as hypogonadism,
in adult males. For more information, please visit
www.lipocine.com.
Forward-Looking Statements
This release contains
"forward-looking statements" that are made pursuant to the safe
harbor provisions of the Private Securities Litigation Reform Act
of 1995 and include statements that are not historical facts
regarding our product development efforts, our strategic plans for
developing products, our ability to monetize product candidates,
including through entering into partnering arrangements, our
product candidates and related clinical trials, the achievement of
milestones within and completion of clinical trials, the timing and
completion of regulatory reviews, outcomes of clinical trials of
our product candidates, and the potential uses and benefits of our
product candidates. Investors are cautioned that all such
forward-looking statements involve risks and uncertainties,
including, without limitation, the risks that we may not be
successful in developing product candidates, we may not have
sufficient capital to complete the development processes for our
product candidates, we may not be able to enter into partnerships
or other strategic relationships to monetize our non-core assets,
the FDA will not approve any of our products, risks related to our
products, expected product benefits not being realized, clinical
and regulatory expectations and plans not being realized, new
regulatory developments and requirements, risks related to the FDA
approval process including the receipt of regulatory approvals, and
our ability to utilize a streamlined approval pathway for LPCN
1154, the results and timing of clinical trials, patient acceptance
of Lipocine's products, the manufacturing and commercialization of
Lipocine's products, and other risks detailed in Lipocine's filings
with the SEC, including, without limitation, its Form 10-K and
other reports on Forms 8-K and 10-Q, all of which can be obtained
on the SEC website at www.sec.gov. Lipocine assumes no
obligation to update or revise publicly any forward-looking
statements contained in this release, except as required by
law.
- Meltzer-Brody et al. Lancet 2018; 392(10152): 1058-1070.
- Buchsbaum et al. Biol Psychiatry 1985; 20(8): 832-842.
- Ibanez et al. Plos One 2014; 9(3): e93159.
- Huang and Shen Clin Electroencephalography 1994; 24(4):
179-187
- Biondi et al. Sci Rep 2022; 12(1): 1919.
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SOURCE Lipocine Inc.
