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血清素5-HT2A和5-HT2C受体作为调节精神兴奋剂使用和成瘾的潜在靶点。

Serotonin 5-HT2A and 5-HT2C receptors as potential targets for modulation of psychostimulant use and dependence.

作者信息

Bubar Marcy J, Cunningham Kathryn A

机构信息

Center for Addiction Research and the Department of Pharmacology and Toxicology, University of Texas Medical Branch, Galveston, TX 77555-1031, USA.

出版信息

Curr Top Med Chem. 2006;6(18):1971-85. doi: 10.2174/156802606778522131.

DOI:10.2174/156802606778522131
PMID:17017968
Abstract

The development of novel pharmacological agents for the treatment of psychostimulant use disorders is an important research imperative. One potential target system that has been largely overlooked is the serotonin (5-HT) neurotransmitter system. Preclinical studies indicate that 5-HT may be important in modulating the reinforcing properties of various drugs of abuse. While the potential sites of action of 5-HT within the brain are extensive, the natural starting point to examine the mechanisms by which 5-HT may be useful in treatment of psychostimulant use disorders is the interaction between 5-HT and dopamine (DA), a primary mediator of the "rewarding" effects of psychostimulants. Two key modulators of DA output are the serotonin (5-HT)2A receptor (5-HT2A R) and the 5-HT2C R. These receptors are known to control the neurochemical and behavioral effects of psychostimulants, and in particular, the in vivo effects of cocaine. Preclinical studies indicate that 5-HT2A R antagonists and/or 5-HT2C R agonists may effectively reduce craving and/or relapse, and likewise, enhance abstinence, while 5-HT2C R agonists may also effectively reduce cocaine intake in active cocaine users. At present, the progression of studies to probe the effectiveness of 5-HT2A R and 5-HT2C R ligands in the clinical setting is hindered by a lack of available selective 5-HT2A R antagonists or 5-HT2C R agonists for use in human cocaine abusers. However, a number of selective 5-HT2 R ligands currently under development, or in early clinical trials for psychiatric and/or neurological disorders, may soon be available for translational studies to explore their effectiveness in modulating drug use and dependence.

摘要

开发用于治疗精神兴奋剂使用障碍的新型药物制剂是一项重要的研究任务。一个在很大程度上被忽视的潜在靶标系统是5-羟色胺(5-HT)神经递质系统。临床前研究表明,5-HT在调节各种滥用药物的强化特性方面可能很重要。虽然5-HT在大脑中的潜在作用位点广泛,但研究5-HT在治疗精神兴奋剂使用障碍中可能有用的机制的自然起点是5-HT与多巴胺(DA)之间的相互作用,DA是精神兴奋剂“奖赏”效应的主要介质。DA输出的两个关键调节因子是5-羟色胺(5-HT)2A受体(5-HT2A R)和5-HT2C R。已知这些受体可控制精神兴奋剂的神经化学和行为效应,尤其是可卡因的体内效应。临床前研究表明,5-HT2A R拮抗剂和/或5-HT2C R激动剂可能有效减少渴望和/或复发,同样,增强戒断,而5-HT2C R激动剂也可能有效减少活跃可卡因使用者的可卡因摄入量。目前,由于缺乏可用于人类可卡因滥用者的选择性5-HT2A R拮抗剂或5-HT2C R激动剂,阻碍了在临床环境中探究5-HT2A R和5-HT2C R配体有效性的研究进展。然而,目前正在开发或处于精神疾病和/或神经疾病早期临床试验阶段的一些选择性5-HT2 R配体,可能很快可用于转化研究,以探索它们在调节药物使用和依赖方面的有效性。

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