Addex GABAB Positive Allosteric Modulator Demonstrates Promise in Alcohol Use Disorder
February 16 2021 - 1:00AM
Review from Linköping University
Published in Alcohol and Alcoholism Journal
Geneva, Switzerland, February 16,
2021 – Addex Therapeutics (SIX: ADXN and Nasdaq: ADXN), a
clinical-stage pharmaceutical company pioneering allosteric
modulation-based drug discovery and development, today announced
that a review published in Alcohol and Alcoholism suggests that
positive allosteric modulators (PAMs) of the gamma-aminobutyric
acid B (GABAB) receptor could offer a new treatment option for
patients with severe alcohol use disorder (AUD). Direct,
orthosteric, GABAB receptor agonists, such as baclofen, have been
shown to attenuate addiction-related behaviors in preclinical
studies. However, the therapeutic use of baclofen is very limited
due to significant side-effects, including sedation, drowsiness and
sleepiness.
Following analysis of a number of studies, the
review emphasized that all preclinical behavioral results have
shown the efficacy of GABAB PAMs for addiction treatment and offer
similar mechanistic and therapeutic effects, while avoiding the
tolerance and toxicity issues associated with baclofen. In
particular, Addex’s GABAB PAM, ADX71441, demonstrated efficacy on
several alcohol-related behaviors in rat models. ADX71441 potently
decreased binge-like drinking, reduced relapse-like drinking, and
dose-dependently reduced alcohol self-administration as well as
decreasing motivation to consume alcohol. These data support the
hypothesis of GABAB PAMs offering a better and broader approach to
address alcoholism symptoms. The high translational value of these
preclinical studies strongly supports clinical testing of GABAB
PAMs.
“The groundbreaking work carried out with
ADX71441 in alcohol and other addiction disorders has laid a solid
foundation supporting the development of our GABAB PAMs as novel
treatment for addiction disorders. This review shows the growing
body of research in this field and summarises data suggesting that
the effects seen in preclinical models of AUD could translate to
humans,” said Robert Lütjens, Head of Discovery Biology of Addex.
"Our research collaboration with Indivior evaluating new GABAB PAMs
in addiction is progressing rapidly, with an aim to begin clinical
studies in 2022.”
Relevant publications:
Augier E. (2021) Recent Advances in the
Potential of Positive Allosteric Modulators of the GABAB Receptor
to Treat Alcohol Use Disorder. Alcohol and Alcoholism, 1–11; doi:
10.1093/alcalc/agab003
Hwa LS, Kalinichev M, Haddouk H, et al. (2014)
Reduction of excessive alcohol drinking by a novel GABAB receptor
positive allosteric modulator ADX71441 in mice. Psychopharmacology
231:333–43.
Augier E, Dulman RS, Damadzic R, et al. (2017)
The GABAB positive allosteric modulator ADX71441 attenuates alcohol
self-administration and relapse to alcohol seeking in rats.
Neuropsychopharmacology 42:1789–99.
About GABAB Activation with PAM
Activation of the GABAB receptor, a Family C
class of GPCR, is clinically and commercially validated. The
generic GABAB receptor agonist, baclofen, is marketed for
spasticity and some spinal cord injuries, and is used for
overactive bladder (OAB), but it is not commonly used due to a
variety of side effects of the drug and rapid clearance. Potent,
selective oral positive allosteric modulators (PAM) that potentiate
GABA responses at the GABAB receptor, rather than an
orthosteric agonist at the GABAB receptor, like baclofen, only
act when the natural ligand (GABA) activates the receptor,
therefore respecting the physiological cycle of activation. It has
been proposed that PAMs produce less adverse effects and could lead
to less tolerance than direct agonists (May and Christopoulos 2003;
Langmead and Christopoulos 2006; Perdona et al. 2011; Urwyler 2011;
Gjoni et al., 2008; Ahnaou et al., 2015).
About Addex Therapeutics
Addex Therapeutics is a clinical-stage
pharmaceutical company focused on the development and
commercialization of an emerging class of novel orally available
small molecule drugs known as allosteric modulators for
neurological disorders. Allosteric modulators offer several
potential advantages over conventional non-allosteric molecules and
may offer an improved therapeutic approach to conventional
"orthosteric" small molecule or biological drugs. Addex's
allosteric modulator drug discovery platform targets receptors and
other proteins that are recognized as essential for therapeutic
intervention. Addex's lead drug candidate, dipraglurant (mGlu5
negative allosteric modulator or NAM), is poised to start a
pivotal registration clinical trial for Parkinson’s disease
levodopa induced dyskinesia (PD-LID) in H1 2021. Addex is also
investigating dipraglurant's therapeutic use in blepharospasm (a
type of dystonia), for which a clinical trial is expected to be
initiated in H1 2021. Addex's third clinical program, ADX71149
(mGlu2 positive allosteric modulator or PAM), developed in
collaboration with Janssen Pharmaceuticals, Inc, is scheduled to
enter a phase 2a proof of concept clinical study for the treatment
of epilepsy in Q2 2021. Addex’s GABAB PAM program has been
licensed to Indivior PLC who are focused on development for the
treatment of addiction. Preclinical programs include GABAB PAM
for CMT1A, mGlu7 NAM for PTSD, mGlu2 NAM for mild neurocognitive
disorders, mGlu4 PAM for Parkinson’s disease and mGlu3 PAM for
neurodegenerative disorders. Addex is listed
on the SIX Swiss Exchange and the NASDAQ Capital Market and trades
under the ticker symbol "ADXN".
Press Contacts:
Tim DyerChief Executive OfficerTelephone: +41 22 884 15
55Email: PR@addextherapeutics.com |
Mike SinclairPartner, Halsin Partners+44 (0)20 7318
2955msinclair@halsin.com |
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