Substitution therapy for patients with alcohol dependence: Mechanisms of action and efficacy.

International review of neurobiology Pub Date : 2024-01-01 Epub Date: 2024-03-16 DOI:10.1016/bs.irn.2024.03.005
Julien Guiraud, Rainer Spanagel, Wim van den Brink
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Abstract

New approaches for the treatment of alcohol dependence (AD) may improve patient outcomes. Substitution maintenance therapy is one of the most effective treatment options for opioid and nicotine use disorders. So far, there has been little attention to substitution therapy for the treatment of AD. Here, we explain the mechanistic foundations of alcohol substitution maintenance therapy. Alcohol has many primary targets in the brain (and other organs) and the physical interaction of ethanol molecules with these specific ethanol-sensitive sites on a variety of ionotropic receptors (e.g. GABA-A, NMDA, and nicotinic acetylcholine (nACh) receptors) and ion channels provides the rationale for substitution. As such, a variety of compounds can interact with those ethanol-sensitive sites and can thus substitute for some of the effects of alcohol. For some of these compounds, alcohol discrimination studies have shown their substitution potential. Accordingly, potential substitution treatments include agonists acting at GABA receptors such as sodium oxybate, baclofen and benzodiazepines, NMDA receptor antagonists such as ketamine and memantine, or nAChRs agonists such as varenicline. All these compounds are already approved for other indications and we present clinical evidence for these drugs in the treatment of alcohol withdrawal syndrome (AWS) and in the long-term treatment of AD, and outline future steps for their acceptance as substitution treatment in AD. Finally, we discuss the substitution approach of managed alcohol programs for the most severely affected homeless populations. Results showed that sodium oxybate is probably the closest to a substitution therapy for AD and is already approved for the treatment of AWS and in the long-term treatment of AD in some countries. In conclusion, we argue that better AD treatment can be provided if substitution maintenance treatments for alcohol are implemented at a similar scale as for opioid and nicotine use disorder.

酒精依赖症患者的替代疗法:作用机制和疗效。
治疗酒精依赖症(AD)的新方法可能会改善患者的治疗效果。替代维持疗法是治疗阿片类药物和尼古丁使用障碍最有效的方法之一。迄今为止,人们很少关注替代疗法治疗酒精依赖症。在此,我们将解释酒精替代维持疗法的机理基础。酒精在大脑(和其他器官)中有许多主要靶点,乙醇分子与各种离子受体(如 GABA-A、NMDA 和烟碱乙酰胆碱(nACh)受体)和离子通道上的这些特定乙醇敏感点之间的物理相互作用为替代疗法提供了理论依据。因此,多种化合物可与这些乙醇敏感点相互作用,从而替代酒精的某些作用。对其中一些化合物进行的酒精鉴别研究显示了它们的替代潜力。因此,潜在的替代疗法包括作用于 GABA 受体的激动剂,如羟巴酸钠、巴氯芬和苯二氮卓;NMDA 受体拮抗剂,如氯胺酮和美金刚;或 nAChRs 激动剂,如伐尼克兰。所有这些化合物都已被批准用于其他适应症,我们将介绍这些药物在治疗酒精戒断综合征(AWS)和长期治疗注意力缺失症方面的临床证据,并概述这些药物被接受为注意力缺失症替代治疗的未来步骤。最后,我们讨论了针对受影响最严重的无家可归人群的酒精管理计划的替代方法。研究结果表明,羟基乙酸钠可能是最接近于注意力缺失症替代疗法的药物,在一些国家已被批准用于 AWS 治疗和注意力缺失症的长期治疗。总之,我们认为,如果以类似于治疗阿片类药物和尼古丁使用障碍的规模实施酒精替代维持疗法,就能更好地治疗注意力缺失症。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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