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褪黑素在调节小鼠结节部的节律性生物钟基因表达中起着关键作用。

Melatonin plays a crucial role in the regulation of rhythmic clock gene expression in the mouse pars tuberalis.

作者信息

von Gall Charlotte, Weaver David R, Moek Juliane, Jilg Antje, Stehle Jörg H, Korf Horst-Werner

机构信息

Dr. Senckenbergische Anatomie, Anatomisches Institut II, JW Goethe-Universität Frankfurt, Germany.

出版信息

Ann N Y Acad Sci. 2005 Apr;1040:508-11. doi: 10.1196/annals.1327.105.

Abstract

Circadian rhythms in physiology and behavior are driven by a central clock residing within the hypothalamic suprachiasmatic nucleus (SCN). Molecularly, the biological clock is based on the transcriptional/translational feedback loop of clock genes (mPer, mCry, Clock, and Bmal1). Circadian expression of clock genes is not limited to the SCN, but is found in many peripheral tissues. Peripheral rhythms depend on neuroendocrine/neuronal output from the SCN. Melatonin, the hormone of darkness, represents an important neuroendocrine output of the circadian clock. The hypophyseal pars tuberalis (PT) is one of the main target regions for melatonin. The aim of the study was to test whether mPer, mCry, Clock, and Bmal1 are rhythmically expressed in the mouse PT and how the absence of melatonin receptors affects clock gene expression. We analyzed clock gene expression by in situ hybridization and compared wild-type (WT), melatonin 1 receptor knockout (MT1 ko), and melatonin 2 receptor knockout (MT2 ko) mice. mPer1, mCry1, Clock, and Bmal1, but not mPer2 and mCry2, were rhythmically expressed in the PT of WT and MT2 ko mice. In the PT of MT1 ko mice, expression of mPer1, mCry1, Clock, and Bmal1 was dramatically reduced. We conclude that melatonin, acting through the MT1 receptor, is an important regulator of rhythmic clock gene expression in the mouse PT.

摘要

生理和行为中的昼夜节律由位于下丘脑视交叉上核(SCN)的中央时钟驱动。在分子层面,生物钟基于时钟基因(mPer、mCry、Clock和Bmal1)的转录/翻译反馈回路。时钟基因的昼夜表达不仅限于SCN,在许多外周组织中也有发现。外周节律依赖于SCN的神经内分泌/神经元输出。褪黑素,即黑暗中的激素,是生物钟的一种重要神经内分泌输出。垂体结节部(PT)是褪黑素的主要靶区之一。本研究的目的是测试mPer、mCry、Clock和Bmal1在小鼠PT中是否有节律性表达,以及褪黑素受体缺失如何影响时钟基因表达。我们通过原位杂交分析时钟基因表达,并比较野生型(WT)、褪黑素1受体敲除(MT1 ko)和褪黑素2受体敲除(MT2 ko)小鼠。mPer1、mCry1、Clock和Bmal1在WT和MT2 ko小鼠的PT中有节律性表达,但mPer2和mCry2没有。在MT1 ko小鼠的PT中,mPer1、mCry1、Clock和Bmal1的表达显著降低。我们得出结论,通过MT1受体起作用的褪黑素是小鼠PT中有节律的时钟基因表达的重要调节因子。

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