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视交叉上核中生物钟基因产物的表达与昼夜节律行为的关系。

Expression of clock gene products in the suprachiasmatic nucleus in relation to circadian behaviour.

作者信息

Hastings M H, Reddy A B, Garabette M, King V M, Chahad-Ehlers S, O'Brien J, Maywood E S

机构信息

Neurobiology Division, Laboratory of Molecular Biology, MRC Centre, Hills Road, Cambridge CB2 2QH, UK.

出版信息

Novartis Found Symp. 2003;253:203-17; discussion 102-9, 218-22, 281-4. doi: 10.1002/0470090839.ch15.

Abstract

Circadian timing within the suprachiasmatic nucleus (SCN) is modelled around cell-autonomous, autoregulatory transcriptional/post-translational feedback loops, in which protein products of canonical clock genes Period and Cryptochrome periodically oppose transcription driven by CLOCK:BMAL complexes. Consistent with this model, mCLOCK is a nuclear antigen constitutively expressed in mouse SCN, whereas nuclear mPER and mCRY are expressed rhythmically. Peaking in late subjective day, mPER and mCRY form heteromeric complexes with mCLOCK, completing the negative feedback loop as levels of mPer and mCry mRNA decline. Circadian resetting by light or non-photic resetting (mediated by neuropeptide Y) involves acute up- and down-regulation of mPer mRNA, respectively. Expression of Per mRNA also peaks in subjective day in the SCN of the ground squirrel, indicating common clock and entrainment mechanisms for nocturnal and diurnal species. Oscillation within the SCN is dependent on intercellular signals, in so far as genetic ablation of the VPAC2 receptor for vasoactive intestinal polypeptide (VIP) suspends SCN circadian gene expression. The pervasive effect of the SCN on peripheral physiology is underscored by cDNA microarray analysis of the circadian gene expression in liver, which involves ca. 10% of the genome and almost all aspects of cell function. Moreover, the same molecular regulatory mechanisms driving the SCN appear also to underpin peripheral cycles.

摘要

视交叉上核(SCN)内的昼夜节律定时是围绕细胞自主、自动调节的转录/翻译后反馈环建立的,在这个反馈环中,典型时钟基因Period和Cryptochrome的蛋白质产物周期性地抑制由CLOCK:BMAL复合物驱动的转录。与该模型一致,mCLOCK是在小鼠SCN中组成性表达的核抗原,而核mPER和mCRY则有节律地表达。mPER和mCRY在主观日后期达到峰值,与mCLOCK形成异源复合物,随着mPer和mCry mRNA水平下降,完成负反馈环。光或非光重置(由神经肽Y介导)引起的昼夜节律重置分别涉及mPer mRNA的急性上调和下调。在松鼠的SCN中,Per mRNA的表达也在主观日达到峰值,这表明夜行性和昼行性物种存在共同的时钟和同步机制。SCN内的振荡依赖于细胞间信号,因为血管活性肠肽(VIP)的VPAC2受体的基因消融会使SCN昼夜节律基因表达暂停。肝脏中昼夜节律基因表达的cDNA微阵列分析强调了SCN对周围生理学的普遍影响,这涉及约10%的基因组以及细胞功能的几乎所有方面。此外,驱动SCN的相同分子调节机制似乎也支撑着外周循环。

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