Aligos Therapeutics, Inc. (Nasdaq: ALGS, “Aligos”), a clinical
stage biopharmaceutical company focused on developing novel
therapeutics to address unmet medical needs in liver and viral
diseases, today announced positive data from one late-breaker oral
and three poster presentations at the American Association for the
Study of Liver Disease’s (AASLD) The Liver Meeting (TLM) 2024,
being held November 15 – 19, 2024 in San Diego, CA.
The clinical poster presentation highlighted the continued
potent antiviral activity of ALG-000184 for chronic hepatitis B
(CHB) virus infection in both HBeAg-positive and HBeAg-negative
subjects, demonstrating the potential for the molecule to become
first-line therapy for chronic suppression and the backbone for
regimens aimed at functional cure.
Data from ≤84 weeks following an oral daily dose of 300 mg
ALG-000184 monotherapy demonstrated sustained HBV DNA suppression
(<LLOQ <10 IU/mL) in 7/7 (100%) HBeAg-positive CHB subjects.
All HBeAg- subjects achieved sustained HBV DNA suppression by Week
24 and 11/11 (100%) subjects achieved sustained HBV DNA <LLOQ at
Week 48 with 10/11 (91%) subjects further achieving HBV DNA below
the lower limit of detection (LLOD <4.92 IU/mL). Importantly, no
subject demonstrated viral resistance to ALG-000184 monotherapy and
suppression was maintained throughout the dosing period.
All subjects achieved sustained HBV RNA < LLOQ by Week 44 in
HBeAg+ subjects and Week 8 in HBeAg- subjects. Multi-log10
reductions in HBsAg, HBeAg, and HBcrAg were observed in HBeAg+
subjects, and HBcrAg decline was observed in HBeAg- subjects. In
both patient populations, ALG-000184 continues to be well tolerated
with no viral breakthrough observed and no known CAM resistant
mutations identified with monotherapy treatment.
Additionally, the late-breaker oral presentation highlighted the
best-in-class potential of ALG-055009, a purpose built THR-β
agonist discovered by Aligos scientists. 12-weeks of once daily
ALG-055009 treatment in MASH patients met the primary endpoint,
with robust reductions in liver fat content at Week 12. Doses of
0.5 mg to 0.9 mg ALG-055009 demonstrated statistically significant
reductions in liver fat at Week 12, with placebo-adjusted median
relative reductions up to 46.2% as measured by MRI-PDFF. Up to 70%
of subjects achieved ≥30% relative reduction in liver fat compared
to baseline, a positive prognostic indicator of histological
improvements in MASH resolution and fibrosis reduction. Eighteen
subjects who were on stable GLP-1 agonist therapy qualified for
enrollment in the study, with liver fat content meeting the
inclusion criteria of ≥10% at baseline as measured by MRI-PDFF.
Notably, 11/14 subjects on stable GLP-1 agonists treated with
ALG-055009 had liver fat decreases, whereas 4/4 subjects on stable
GLP-1 agonists treated with placebo had increases in liver fat over
the 12-week dosing period.
Significant reductions in atherogenic lipids, including LDL-C,
lipoprotein (a) and apolipoprotein B and dose-dependent increases
in SHBG were observed. In particular, ALG-055009 demonstrated a
dose-dependent reduction from baseline of up to 26.8% at Week 12
for lipoprotein (a), which is an established risk factor for
cardiovascular disease that has been resistant to treatment with
statin therapy. Treatment with ALG-055009 was well-tolerated, with
rates of gastrointestinal-related AEs similar to placebo.
“The presentation of longer duration dosing of ALG-000184 in CHB
patients strengthens our belief that this therapy will become both
first-line for chronic suppression as well as the backbone of next
generation HBV treatments aimed at functional cure,” stated
Lawrence Blatt, PhD, MBA, Chairman, President, & CEO of Aligos
Therapeutics. “Additionally, we are pleased to have presented the
HERALD data, showing robust reductions in liver fat for patients
treated with ALG-055009. The subgroup analysis in patients enrolled
in the study on stable GLP-1 agonist therapy suggests a role for
ALG-055009 to augment liver fat reductions in patients receiving
incretin therapy.”
Details of the presentations are as follows:
ALG-000184: Potential first-/best-in-class small
molecule CAM-E for chronic hepatitis
B (CHB)
Abstract #: 1213
Title: Monotherapy with the Capsid Assembly
Modulator, ALG-000184, Results in High Viral Suppression Rates in
Untreated HBeAg+ and HBeAg- Subjects with Chronic Hepatitis B Virus
Infection
Presenter: Professor Man-Fung Yuen, MBBS, MD,
PhD, DSc, Chair and Chief of the Division of Gastroenterology and
Hepatology, University of Hong Kong
Date/Time: November 15, 2024, 8:00am – 5:00pm
PT
Abstract #: 1266
Title: Capsid Assembly Modulators Such as
ALG-001075 Induce Profound HBV DNA Knockdown and Directly Target
HBeAg In Vitro
Presenter: Cheng Liu, PhD
Date/Time: November 15, 2024, 8:00am – 5:00pm
PT
ALG-055009: Potential best-in-class small molecule
THR-β for Metabolic
Dysfunction-Associated Steatohepatitis (MASH)
Format: Oral presentation
Title: ALG-055009, a Novel Thyroid Hormone
Receptor Beta (THR-β) Agonist, was Well-tolerated with Significant
Reductions in Liver Fat at Week 12 in Non-cirrhotic MASH Patients
in the Ongoing Randomized, Double-Blind, Placebo-controlled Phase
2
Presenter: Rohit Loomba, MD, MHSc, Chief,
Division of Gastroenterology and Hepatology, University of
California, San Diego
Date/Time: November 19, 2024 at 10:30am –
10:40am PT
Abstract #: 3226
Title: Nonclinical Toxicology Profile of
ALG-055009, a Novel and Potent Thyroid Hormone Receptor β Agonist,
for the Treatment of Metabolic Dysfunction-Associated
Steatohepatitis (MASH)
Presenter: Dinah Misner, PhD
Date/Time: November 17, 2024, 8:00am – 5:00pm
PT
The presentations can be found on the Posters &
Presentations section of the Aligos website
(www.aligos.com).
About AligosAligos Therapeutics, Inc. (NASDAQ:
ALGS) is a clinical stage biopharmaceutical company founded with
the mission to improve patient outcomes by developing best-in-class
therapies for the treatment of liver and viral diseases. Aligos
applies its science driven approach and deep R&D expertise to
advance its purpose-built pipeline of therapeutics for metabolic
dysfunction-associated steatohepatitis (MASH) and viruses with high
unmet medical need such as hepatitis B and coronaviruses.
For more information, please visit www.aligos.com or follow us
on LinkedIn or X.
Forward-Looking Statements This press release
contains forward-looking statements within the meaning of the U.S.
Private Securities Litigation Reform Act of 1995. Any statements in
this press release that are not historical facts may be considered
“forward-looking statements,” including without limitation,
statements regarding Aligos’ financial results and performance as
well as research and development activities, including regulatory
status and the timing of announcements and updates relating to our
regulatory filings and clinical trials. Such forward looking
statements are subject to substantial risks and uncertainties that
could cause our development programs, future results, performance,
or achievements to differ materially from those anticipated in the
forward-looking statements. Such risks and uncertainties include,
without limitation, risks and uncertainties inherent in the drug
development process, including Aligos’ clinical stage of
development, the process of designing and conducting clinical
trials, the regulatory approval processes, and other matters that
could affect the sufficiency of Aligos’ capital resources to fund
operations. For a further description of the risks and
uncertainties that could cause actual results to differ from those
anticipated in these forward-looking statements, as well as risks
relating to the business of Aligos in general, see Aligos’
Quarterly Report on Form 10-Q filed with the Securities and
Exchange Commission on November 6, 2024 and its future periodic
reports to be filed or submitted with the Securities and Exchange
Commission. Except as required by law, Aligos undertakes no
obligation to update any forward-looking statements to reflect new
information, events or circumstances, or to reflect the occurrence
of unanticipated events.
Investor ContactJordyn TaraziVice President,
Investor Relations & Corporate Communications+1 (650)
910-0427jtarazi@aligos.com
Media ContactInizio EvokeJake RobisonVice
PresidentJake.Robison@inizioevoke.com
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