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细胞“昼夜节律”周期:哺乳动物核心生物钟基因的新作用。

Cell "circadian" cycle: new role for mammalian core clock genes.

作者信息

Borgs Laurence, Beukelaers Pierre, Vandenbosch Renaud, Belachew Shibeshih, Nguyen Laurent, Malgrange Brigitte

机构信息

Developmental Neurobiology Unit, Center for Cellular and Molecular Neurobiology, University of Liège, Liège, Belgium.

出版信息

Cell Cycle. 2009 Mar 15;8(6):832-7. doi: 10.4161/cc.8.6.7869. Epub 2009 Mar 16.

Abstract

In mammals, 24 hours rhythms are organized as a biochemical network of molecular clocks that are operative in all tissues, with the master clock residing in the hypothalamic suprachiasmatic nucleus (SCN). The core pacemakers of these clocks consist of auto-regulatory transcriptional/post-transcriptional feedback loops. Several lines of evidence suggest the existence of a crosstalk between molecules that are responsible for the generation of circadian rhythms and molecules that control the cell cycle progression. In addition, highly specialized cell cycle checkpoints involved in DNA repair after damage seem also, at least in part, mediated by clock proteins. Recent studies have also highlighted a putative connection between clock protein dysfunction and cancer progression. This review discusses the intimate relation that exists between cell cycle progression and components of the circadian machinery.

摘要

在哺乳动物中,24小时节律被组织成一个分子时钟的生化网络,该网络在所有组织中都起作用,主时钟位于下丘脑视交叉上核(SCN)。这些时钟的核心起搏器由自动调节的转录/转录后反馈环组成。几条证据表明,负责昼夜节律产生的分子与控制细胞周期进程的分子之间存在相互作用。此外,参与损伤后DNA修复的高度专业化的细胞周期检查点似乎至少部分也由时钟蛋白介导。最近的研究还强调了时钟蛋白功能障碍与癌症进展之间的假定联系。本综述讨论了细胞周期进程与昼夜节律机制各组成部分之间存在的密切关系。

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