Emerging medications and pharmacological treatment approaches for substance use disorders
- PMID: 39719161
- PMCID: PMC12078786
- DOI: 10.1016/j.pbb.2024.173952
Emerging medications and pharmacological treatment approaches for substance use disorders
Abstract
Medications to treat substance use disorders (SUDs) remain suboptimal or, in the case of stimulants and cannabis, non-existent. Many factors have contributed to this paucity, including the biological complexity of addiction, regulatory challenges, and a historical lack of enthusiasm among pharmaceutical companies to commit resources to this disease space. Despite these headwinds, the recent opioid crisis has highlighted the devastating consequences of SUDs for both individuals and society, stimulating urgent efforts to identify novel treatment approaches. In addition, several neurobiological systems have been recently implicated in unique aspects of drug reward, opening the door to candidate medications with novel mechanisms of action. Here, we provide an overview of efforts to target several of these new systems, with a focus on those that are the subject of ongoing clinical trials as well as being areas of interest among the authors' research groups (MHJ, MTB, NAE). Specifically, we discuss new classes of medications targeting the serotonin 2A receptor (i.e., psychedelics), glucagon-like peptide 1 receptor, cannabidiol, dynorphin/kappa opioid receptor, orexin/hypocretin, and oxytocin receptor systems, as well as emergent approaches for modulating the more canonical dopaminergic system via agonist therapies for stimulant use disorders. Collectively, innovations in this space give reason for optimism for an improved therapeutic landscape for substance use disorders in the near future.
Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.
Conflict of interest statement
Declaration of interests MHJ is an inventor on patent application PCT/US23/27918, and provisional patent applications US 63/601,522, and US 63/702,018 which describe novel treatments for psychiatric illnesses, including substance use disorders. In addition to his academic role, MTB is co-founder and Chief Scientific Officer of Kinoxis Therapeutics Pty Ltd., an Australian-based company developing novel small molecule treatments for brain disorders, including the treatment of substance use disorders and social impairments in psychiatric conditions. In addition to his academic role, NAE is Head of Behavioral Neuroscience at Kinoxis Therapeutics, and Head of Behavioral Pharmacology at Psylo Pty Ltd. MTB and NAE receive research funding from Kinoxis Therapeutics, and NAE receives research funding from Psylo. RS is an employee of Kinoxis Therapeutics. The work presented in this manuscript is unrelated to RE's, MTB's and NAE's role with Kinoxis Therapeutics, or NAE's role with Psylo. All other authors declare no conflicts of interest.
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