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黑皮质素激素对睡眠-觉醒行为的控制。

Melanin-concentrating hormone control of sleep-wake behavior.

机构信息

Department of Pharmacology and Therapeutics, School of Medicine Clinics Hospital, Montevideo 11600, Uruguay.

出版信息

Sleep Med Rev. 2013 Aug;17(4):293-8. doi: 10.1016/j.smrv.2012.10.002. Epub 2013 Mar 9.

Abstract

The melanin-concentrating hormone (MCH) is a 19 aminoacid peptide found in mammals predominantly in neurons located in the lateral hypothalamus and incerto-hypothalamic area. The biological function of MCH is mediated by two G-protein-coupled receptors known as MCHR1 and MCHR2, although the latter is expressed only in carnivores, primates and man. The MCHR1 couples to Gi, Gq and Go proteins, with Gi leading to the inhibition of both excitatory and inhibitory synaptic events. Within the central nervous system (CNS) MCH participates in a number of functions including sleep-wake behavior. In this respect, MCHergic neurons project widely throughout the CNS to brain regions involved in the regulation of behavioral states. MCHergic neurons are silent during wakefulness (W), increase their firing during slow wave sleep (SWS) and still more during REM sleep (REMS). Studies in knockout mice for MCH (MCH(-/-)) have shown a reduction in SWS and an increase of W during the light and the dark phase of the light-dark cycle. Moreover, in response to food deprivation a marked reduction in REMS time was observed in these animals. Conflicting effects on sleep variables have been reported in MCHR1(-/-) mice by different authors. The i.c.v. administration of MCH increases REMS and SWS in the rat. In addition, an enhancement of REMS has been described following the microinjection of the neuropeptide into the nucleus pontis oralis of the cat, while its infusion into the dorsal raphe nucleus (DR) and the basal forebrain (horizontal limb of the diagonal band of Broca) is followed by an increase of REMS and a reduction of W in the rat. Immunoneutralization of MCH in the DR augmented W and suppressed REMS in the rat, as did the s.c. injection of selective MCHR1 antagonists. The robust REMS-inducing effect of MCH is likely related to the deactivation of monoaminergic, orexinergic, glutamatergic, cholinergic (W-on) and GABAergic (REM-off) neurons involved in the generation of W and the inhibition of REMS. On the basis of preclinical studies, it can be proposed that selective MCHR1 receptor agonists could constitute potential therapeutic modalities in the arsenal of insomnia pharmacotherapy. Due to the lack of adequate animal models, the role of the MCHR2 on sleep is still unknown.

摘要

黑色素浓缩激素 (MCH) 是一种 19 个氨基酸的肽,在哺乳动物中主要存在于位于外侧下丘脑和下丘脑间脑区域的神经元中。MCH 的生物学功能由两种 G 蛋白偶联受体介导,称为 MCHR1 和 MCHR2,尽管后者仅在肉食动物、灵长类动物和人类中表达。MCHR1 与 Gi、Gq 和 Go 蛋白偶联,Gi 导致兴奋性和抑制性突触事件的抑制。在中枢神经系统 (CNS) 内,MCH 参与许多功能,包括睡眠-觉醒行为。在这方面,MCH 能神经元广泛投射到参与调节行为状态的脑区。MCH 能神经元在觉醒 (W) 时处于沉默状态,在慢波睡眠 (SWS) 期间增加其放电,在快速眼动睡眠 (REMS) 期间增加更多。MCH 敲除 (MCH(-/-)) 小鼠的研究表明,在光-暗周期的亮相和暗相期间,SWS 减少,W 增加。此外,在这些动物中,对食物剥夺的反应是 REM 时间明显减少。不同作者在 MCHR1(-/-) 小鼠中报告了对睡眠变量的矛盾影响。MCH 的脑室内给药增加了大鼠的 REMS 和 SWS。此外,在猫的脑桥嘴侧核内微注射神经肽后,描述了 REMS 的增强,而将其注入中缝背核 (DR) 和基底前脑 (Broca 水平直带的水平支) 后,大鼠的 REMS 增加和 W 减少。DR 中的 MCH 免疫中和增加了大鼠的 W 并抑制了 REMS,皮下注射选择性 MCHR1 拮抗剂也是如此。MCH 强烈的 REMS 诱导作用可能与参与 W 产生和 REMS 抑制的单胺能、食欲素能、谷氨酸能、胆碱能 (W-on) 和 GABA 能 (REM-off) 神经元的失活有关。基于临床前研究,可以提出选择性 MCHR1 受体激动剂可能构成失眠药物治疗武器库中的潜在治疗方式。由于缺乏足够的动物模型,MCHR2 对睡眠的作用仍不清楚。

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