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Chromatin remodeling, metabolism and circadian clocks: the interplay of CLOCK and SIRT1.

机译:染色质重塑,新陈代谢和昼夜节律:CLOCK和SIRT1的相互作用。

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Circadian rhythms govern a wide variety of physiological and metabolic functions in almost all organisms. These are controlled by the circadian clock machinery, which is mostly based on transcriptional-translational feedback loops. Importantly, 10-15% of the mammalian transcripts oscillate in a circadian manner. The complex program of gene expression that characterizes circadian physiology is possible through dynamic changes in chromatin transitions. These remodeling events are therefore of great importance to insure the proper timing and extent of circadian regulation. Recent advances in the field have revealed unexpected links between circadian regulators, chromatin remodeling and cellular metabolism. Specifically, the central clock protein CLOCK has HAT enzymatic properties. It directs acetylation of histone H3 and of its dimerization partner BMAL1 at K537, an event essential for circadian function. In addition, the HDAC activity of the NAD(+)-dependent SIRT1 enzyme is regulated in a circadian manner. It has been proposed that SIRT1 functions as an enzymatic rheostat of circadian function, transducing signals originated by cellular metabolites to the circadian clock. Thus, a specialized program of chromatin remodeling appears to be at the core of the circadian machinery.
机译:昼夜节律控制着几乎所有生物体的多种生理和代谢功能。这些受生物钟机制的控制,该机制主要基于转录-翻译反馈环。重要的是,10-15%的哺乳动物转录本以昼夜节律方式振荡。通过染色质转变的动态变化,可以表征生物钟生理的复杂基因表达程序。因此,这些重塑事件对于确保生物钟调节的适当时机和程度非常重要。该领域的最新进展揭示了昼夜节律调节器,染色质重塑和细胞代谢之间的意外联系。具体而言,中央时钟蛋白CLOCK具有HAT酶特性。它在K537上指导组蛋白H3及其二聚体伴侣BMAL1的乙酰化,这对昼夜节律功能至关重要。此外,NAD(+)依赖的SIRT1酶的HDAC活性以昼夜节律的方式进行调节。已经提出SIRT1起昼夜功能的酶变阻器作用,将由细胞代谢产物产生的信号转导至昼夜时钟。因此,专门的染色质重塑程序似乎是生物钟机制的核心。

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