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褪黑素受体 MT1 是褪黑素在体外纹状体神经元中对神经元“时钟”基因表达产生差异调节作用所必需的。

The melatonin receptor MT1 is required for the differential regulatory actions of melatonin on neuronal 'clock' gene expression in striatal neurons in vitro.

机构信息

Department of Psychiatry, The Psychiatric Institute, University of Illinois at Chicago, Chicago, IL, USA.

出版信息

J Pineal Res. 2009 Jan;46(1):87-94. doi: 10.1111/j.1600-079X.2008.00634.x. Epub 2008 Sep 16.

Abstract

Through inhibitory G protein-coupled melatonin receptors, melatonin regulates intracellular signaling systems and also the transcriptional activity of certain genes. Clock genes are proposed as regulatory factors in forming dopamine-related behaviors and mood and melatonin has the ability to regulate these processes. Melatonin-mediated changes in clock gene expression have been reported in brain regions, including the striatum, that are crucial for the development of dopaminergic behaviors and mood. However, it is not known whether melatonin receptors present in striatum mediate these effects. Therefore, we investigated the role of the melatonin/melatonin receptor system on clock gene expression using a model of primary neuronal cultures prepared from striatum. We found that melatonin at the receptor affinity range (i.e., nm) affects the expression of the clock genes mPer1, mClock, mBmal1 and mNPAS2 (neuronal PAS domain protein 2) differentially in a pertussis toxin-sensitive manner: a decrease in Per1 and Clock, an increase in NPAS2 and no change in Bmal1 expression. Furthermore, mutating MT1 melatonin receptor (i.e., MT1 knockouts, MT1(-/-)) reversed melatonin-induced changes, indicating the involvement of MT1 receptor in the regulatory action of melatonin on neuronal clock gene expression. Therefore, by controlling clock gene expression we propose melatonin receptors (i.e., MT1) as novel therapeutic targets for the pathobiologies of dopamine-related behaviors and mood.

摘要

通过抑制性 G 蛋白偶联的褪黑素受体,褪黑素调节细胞内信号系统,也调节某些基因的转录活性。时钟基因被认为是形成多巴胺相关行为和情绪的调节因子,而褪黑素具有调节这些过程的能力。已经报道了褪黑素介导的时钟基因表达变化在大脑区域,包括纹状体,这对多巴胺能行为和情绪的发展至关重要。然而,目前尚不清楚纹状体中的褪黑素受体是否介导这些效应。因此,我们使用来自纹状体的原代神经元培养物模型研究了褪黑素/褪黑素受体系统对时钟基因表达的作用。我们发现,在受体亲和力范围内(即纳米)的褪黑素以百日咳毒素敏感的方式差异地影响时钟基因 mPer1、mClock、mBmal1 和 mNPAS2(神经元 PAS 结构域蛋白 2)的表达:Per1 和 Clock 的减少,NPAS2 的增加,Bmal1 的表达没有变化。此外,突变 MT1 褪黑素受体(即 MT1 敲除,MT1(-/-)) 逆转了褪黑素诱导的变化,表明 MT1 受体参与了褪黑素对神经元时钟基因表达的调节作用。因此,通过控制时钟基因表达,我们提出褪黑素受体(即 MT1)作为与多巴胺相关行为和情绪的病理生物学相关的新型治疗靶点。

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