[October 12, 2017] |
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Alzheon to Make Presentations on ALZ-801 and Its Anti-Oligomer Mechanism at the 10th Clinical Trials on Alzheimer's Disease Congress
Alzheon,
Inc., a clinical-stage biopharmaceutical company focused on
developing new medicines for patients suffering from Alzheimer's disease
(AD) and other neurological and psychiatric disorders, today announced
that the company will be making three presentations at the 10th Annual
Clinical Trials on Alzheimer's Disease (CTAD) congress to be held on
November 1-4, 2017 in Boston.
These presentations highlight Alzheon's lead drug candidate, ALZ-801,
an orally-administered, anti-amyloid inhibitor that blocks the formation
of toxic amyloid oligomers associated with the development and
progression of AD. The results presented at CTAD further support the
pivotal Phase 3 development of ALZ-801 as a Precision
Medicine approach to treat Alzheimer's patients with apolipoprotein
e4 (APOE4) genotype, with future expansion to additional Alzheimer's
populations.
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An oral presentation at CTAD will discuss the central role of toxic
amyloid oligomers in AD, highlighting Alzheon's discovery of the novel
mechanism of action of tramiprosate, the active agent in optimized
prodrug ALZ-801 that blocks formation of toxic beta amyloid (Aß)
oligomers. Recent findings also clinically translate the molecular
mechanism of action of tramiprosate to clinical effects in Alzheimer's
disease patients.1,2,3
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The company's Precision Medicine clinical program for ALZ-801 is
further supported by clinical data in a poster presentation at CTAD
that analyzed efficacy and safety in AD patients with two APOE4
alleles (APOE4/4 homozygotes), who after completion of the North
American Phase 3 trial continued into an Extension Study. Those
patients who received tramiprosate showed persistent efficacy,
compared to subjects who had a delayed start on active drug, i.e.,
initial placebo-treated subjects. These clinical benefits in APOE4/4
AD patients are consistent with the key role Aß oligomers play in AD
pathogenesis, and the recently discovered molecular mechanism of
tramiprosate, where tramiprosate inhibits Aß monomer aggregation and
formation of toxic Aß oligomers at clinically relevant doses.1
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In a poster presentation at CTAD, Alzheon will describe results from
clinical studies of ALZ-801, an optimized prodrug of tramiprosate. The
clinical studies demonstrated the improved tolerability and
pharmacokinetics of ALZ-801 in comparison to oral tramiprosate, as
well as establishing a dose that achieves equivalent target drug
exposure. The completed ALZ-801 Phase 1 bridging program supports the
pivotal Phase 3 clinical program for development of ALZ-801 as an
oral, anti-oligomer inhibitor for targeting Aß pathology in the
treatment of Alzheimer's disease.
The details for the presentations are as follows:
Oral Presentation (OC6) Title: Amyloid Beta
Oligomers in Alzheimer's Disease: A Missing Piece of the Alzheimer's
Puzzle Date: Thursday, November 2, 2017 Time:
9:45 am ET Presenter: Jeffrey Cummings, MD, Director,
Cleveland Clinic Lou Ruvo Center for Brain Health in Las Vegas and
Professor of Neurology at Cleveland Clinic Other Authors:
Sandrine Andrieu, MD, MPH, University of Toulouse, France; Philip
Scheltens MD, PhD, VU University Medical Center, Amsterdam, Netherlands;
Kaj Blennow, MD, PhD, The Sahlgrenska Academy at University of
Gothenburg, Molndal, Sweden; Petr Kocis PhD, Alzheon, Inc.; John A. Hey
PhD, Alzheon, Inc.; Aidan Power, MD, Alzheon, Inc.; Martin Tolar, MD,
PhD, Alzheon, Inc.; Susan Abushakra, MD, Alzheon, Inc.
Poster Presentation (P29) Title: Sustained
Clinical Effects of Tramiprosate in APOE4/4 Homozygous Patients with
Alzheimer's Disease Over 130 Weeks: Results of Phase 3 Extension Study Poster
Session: Clinical Trials: Results Date: Wednesday,
November 1 and Thursday, November 2 Presenter: Susan
Abushakra, MD, Chief Medical Officer, Alzheon, Inc. Other
Authors: Anton Porsteinsson, MD, University of Rochester; Carl
Sadowsky, MD, Palm Beach Neurology, Florida; Bruno Vellas, MD,
University of Toulouse, France; Serge Gauthier, MD, McGill University,
Montreal, Canada; Aidan Power, MD, Alzheon, Inc.; Larry Shen, PhD,
Pharmapace, Inc., San Diego; Peter Wang, PhD, Pharmapace, Inc., San
Diego; John Hey, PhD, Alzheon, Inc.; Martin Tolar, MD, PhD, Alzheon, Inc.
Poster Presentation (P65) Title: Beta Amyloid
Anti-Oligomer Action of ALZ-801 and Clinical Dose Translation Analyses
Support Confirmatory Phase 3 Program in Alzheimer's Disease Poster
Session: Clinical Trials: Biomarkers Date: Friday,
November 3 and Saturday, November 4 Presenter: John A. Hey,
PhD, Chief Scientific Officer, Alzheon, Inc. Other Authors:
Petr Kocis, PhD, Alzheon, Inc.; Susan Abushakra, MD, Alzheon, Inc.;
Jeremy Yu, MD, PhD, Alzheon, Inc.; Aidan Power, MD, Alzheon, Inc.; Kaj
Blennow, MD, University of Gothenburg, Molndal, Sweden; Martin Tolar,
MD, PhD, Alzheon, Inc.
About Alzheon Alzheon,
Inc. is committed to developing innovative medicines by directly
addressing the underlying pathology of devastating neurodegenerative
disorders. Our lead Alzheimer's clinical candidate, ALZ-801,
is a Phase 3-ready, first-in-class, small molecule oral inhibitor of
amyloid aggregation and neurotoxicity - hallmarks of Alzheimer's
disease. ALZ-801 is a novel prodrug that builds on the safety and
efficacy profile of the active compound tramiprosate, which has been
evaluated in clinical trials involving over 2,000 Alzheimer's patients.
Our clinical expertise and technology platform is focused on developing
drug candidates using a
Precision Medicine approach based on individual genetic and
biological information to advance therapies with the greatest impact for
patients.
1 Kocis
et al. CNS Drugs, 2017 2 Abushakra
et al. J Prev Alz Dis, 2016 3 Abushakra
et al. J Prev Alz Dis, 2017
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