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TAAR1 与精神兴奋剂成瘾。

TAAR1 and Psychostimulant Addiction.

机构信息

Department of Pharmacology and Toxicology, University At Buffalo, The State University of New York, 955 Main Street, Buffalo, NY, 14203, USA.

出版信息

Cell Mol Neurobiol. 2020 Mar;40(2):229-238. doi: 10.1007/s10571-020-00792-8. Epub 2020 Jan 23.

Abstract

Trace amine-associated receptor 1 is one of the best-characterized receptors of trace amines. Growing evidence shows that TAAR1 negatively regulates the monoaminergic activity, including dopamine transmission in the mesocorticolimbic system. Neurochemical assays demonstrated that selective TAAR1 full and partial agonists were effective to prevent psychostimulants-induced dopamine transmission in vitro and in vivo. In the last decade, many preclinical models of psychostimulant addiction such as drug-induced behavioral sensitization, drug-induced conditioned place preference, drug self-administration, drug discrimination, and relapse models were used to assess the effects of TAAR1 agonists on psychostimulants' behavioral effects. In general, activation of TAAR1 attenuated while knockout of TAAR1 potentiated psychostimulant abuse-related behaviors. Here, we review the advances in TAAR1 and its agonists in modulating psychostimulant addiction. We discuss the similarities and differences between the neurochemical and behavioral effects of TAAR1 full and partial agonists. We also discuss several concerns including the abuse liability, sleep reduction, and species-dependent effects that might affect the successful translation of TAAR1 agonists from preclinical studies to clinical application. In conclusion, although further investigations are in need to address certain concerns and the underlying neural mechanisms, TAAR1 agonists appear to be a promising pharmacotherapy to treat psychostimulant addiction and prevent relapse.

摘要

痕量胺相关受体 1 是研究最充分的痕量胺受体之一。越来越多的证据表明,TAAR1 负调控单胺能活性,包括中皮质边缘系统中的多巴胺传递。神经化学测定表明,选择性 TAAR1 完全和部分激动剂可有效预防体外和体内精神兴奋剂诱导的多巴胺传递。在过去的十年中,许多精神兴奋剂成瘾的临床前模型,如药物诱导的行为敏感化、药物诱导的条件性位置偏爱、药物自我给药、药物辨别和复发模型,被用于评估 TAAR1 激动剂对精神兴奋剂行为效应的影响。一般来说,激活 TAAR1 可减弱,而敲除 TAAR1 可增强与精神兴奋剂滥用相关的行为。在此,我们综述了 TAAR1 及其激动剂在调节精神兴奋剂成瘾方面的研究进展。我们讨论了 TAAR1 完全和部分激动剂的神经化学和行为效应的相似性和差异性。我们还讨论了几个关注的问题,包括滥用倾向、睡眠减少和种属依赖性效应,这些问题可能会影响 TAAR1 激动剂从临床前研究到临床应用的成功转化。总之,尽管需要进一步研究来解决某些问题和潜在的神经机制,但 TAAR1 激动剂似乎是一种有前途的药物治疗方法,可用于治疗精神兴奋剂成瘾和预防复发。

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