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Mammalian circadian clock and metabolism - the epigenetic link.

机译:哺乳动物昼夜节律和新陈代谢-表观遗传联系。

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摘要

Circadian rhythms regulate a wide variety of physiological and metabolic processes. The clock machinery comprises complex transcriptional-translational feedback loops that, through the action of specific transcription factors, modulate the expression of as many as 10% of cellular transcripts. This marked change in gene expression necessarily implicates a global regulation of chromatin remodeling. Indeed, various descriptive studies have indicated that histone modifications occur at promoters of clock-controlled genes (CCGs) in a circadian manner. The finding that CLOCK, a transcription factor crucial for circadian function, has intrinsic histone acetyl transferase (HAT) activity has paved the way to unraveling the molecular mechanisms that govern circadian chromatin remodeling. A search for the histone deacetylase (HDAC) that counterbalances CLOCK activity revealed that SIRT1, a nicotinamide adenin dinucleotide (NAD(+))-dependent HDAC, functions in a circadian manner. Importantly, SIRT1 is a regulator of aging, inflammation and metabolism. As many transcripts that oscillate in mammalian peripheral tissues encode proteins that have central roles in metabolic processes, these findings establish a functional and molecular link between energy balance, chromatin remodeling and circadian physiology. Here we review recent studies that support the existence of this link and discuss their implications for understanding mammalian physiology and pathology.
机译:昼夜节律调节各种生理和代谢过程。时钟机制包括复杂的转录-翻译反馈环,该环通过特定转录因子的作用来调节多达10%的细胞转录本的表达。基因表达的这种明显变化必然暗示着染色质重塑的整体调控。实际上,各种描述性研究已经表明,组蛋白修饰以昼夜节律的方式发生在时钟控制基因(CCG)的启动子上。 CLOCK是昼夜节律功能的关键转录因子具有内在的组蛋白乙酰转移酶(HAT)活性的发现,为阐明控制昼夜节律染色质重塑的分子机制铺平了道路。搜索组蛋白脱乙酰基酶(HDAC),以抵消CLOCK的活动表明,SIRT1,烟酰胺腺嘌呤二核苷酸(NAD(+))依赖的HDAC,以昼夜节律的方式起作用。重要的是,SIRT1是衰老,炎症和新陈代谢的调节剂。由于在哺乳动物外周组织中振荡的许多转录物都编码在代谢过程中起关键作用的蛋白质,因此这些发现建立了能量平衡,染色质重塑和昼夜生理之间的功能和分子联系。在这里,我们回顾了支持该链接存在的最新研究,并讨论了它们对理解哺乳动物生理学和病理学的意义。

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