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揭示褪黑素MT2受体在睡眠、焦虑及其他神经精神疾病中的作用:精神药理学中的一个新靶点。

Unveiling the role of melatonin MT2 receptors in sleep, anxiety and other neuropsychiatric diseases: a novel target in psychopharmacology.

作者信息

Comai Stefano, Gobbi Gabriella

机构信息

Neurobiological Psychiatry Unit, Department of Psychiatry, McGill University and McGill University Health Centre, Montréal, Que., Canada.

出版信息

J Psychiatry Neurosci. 2014 Jan;39(1):6-21. doi: 10.1503/jpn.130009.

Abstract

BACKGROUND

Melatonin (MLT) is a pleiotropic neurohormone controlling many physiological processes and whose dysfunction may contribute to several different diseases, such as neurodegenerative diseases, circadian and mood disorders, insomnia, type 2 diabetes and pain. Melatonin is synthesized by the pineal gland during the night and acts through 2 G-protein coupled receptors (GPCRs), MT1 (MEL1a) and MT2 (MEL1b). Although a bulk of research has examined the physiopathological effects of MLT, few studies have investigated the selective role played by MT1 and MT2 receptors. Here we have reviewed current knowledge about the implications of MT2 receptors in brain functions.

METHODS

We searched PubMed, Web of Science, Scopus, Google Scholar and articles' reference lists for studies on MT2 receptor ligands in sleep, anxiety, neuropsychiatric diseases and psychopharmacology, including genetic studies on the MTNR1B gene, which encodes the melatonin MT2 receptor.

RESULTS

These studies demonstrate that MT2 receptors are involved in the pathophysiology and pharmacology of sleep disorders, anxiety, depression, Alzheimer disease and pain and that selective MT2 receptor agonists show hypnotic and anxiolytic properties.

LIMITATIONS

Studies examining the role of MT2 receptors in psychopharmacology are still limited.

CONCLUSION

The development of novel selective MT2 receptor ligands, together with further preclinical in vivo studies, may clarify the role of this receptor in brain function and psychopharmacology. The superfamily of GPCRs has proven to be among the most successful drug targets and, consequently, MT2 receptors have great potential for pioneer drug discovery in the treatment of mental diseases for which limited therapeutic targets are currently available.

摘要

背景

褪黑素(MLT)是一种多效神经激素,可控制多种生理过程,其功能障碍可能导致多种不同疾病,如神经退行性疾病、昼夜节律和情绪障碍、失眠、2型糖尿病和疼痛。褪黑素在夜间由松果体合成,并通过2种G蛋白偶联受体(GPCRs),即MT1(MEL1a)和MT2(MEL1b)发挥作用。尽管大量研究已考察了褪黑素的生理病理效应,但很少有研究调查MT1和MT2受体所起的选择性作用。在此,我们综述了关于MT2受体在脑功能中的作用的现有知识。

方法

我们在PubMed、科学网、Scopus、谷歌学术以及文章的参考文献列表中搜索了关于MT2受体配体在睡眠、焦虑、神经精神疾病和精神药理学方面的研究,包括对编码褪黑素MT2受体的MTNR1B基因的遗传学研究。

结果

这些研究表明,MT2受体参与睡眠障碍、焦虑、抑郁、阿尔茨海默病和疼痛的病理生理学和药理学过程,且选择性MT2受体激动剂具有催眠和抗焦虑特性。

局限性

考察MT2受体在精神药理学中作用的研究仍然有限。

结论

新型选择性MT2受体配体的开发,以及进一步的临床前体内研究,可能会阐明该受体在脑功能和精神药理学中的作用。GPCRs超家族已被证明是最成功的药物靶点之一,因此,MT2受体在治疗目前治疗靶点有限的精神疾病方面具有巨大的先导药物发现潜力。

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