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mTOR signaling regulates central and peripheral circadian clock function

机译:mTOR信号调节中枢和外围生物钟功能

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摘要

The circadian clock coordinates physiology and metabolism. mTOR (mammalian/mechanistic target of rapamycin) is a major intracellular sensor that integrates nutrient and energy status to regulate protein synthesis, metabolism, and cell growth. Previous studies have identified a key role for mTOR in regulating photic entrainment and synchrony of the central circadian clock in the suprachiasmatic nucleus (SCN). Given that mTOR activities exhibit robust circadian oscillations in a variety of tissues and cells including the SCN, here we continued to investigate the role of mTOR in orchestrating autonomous clock functions in central and peripheral circadian oscillators. Using a combination of genetic and pharmacological approaches we show that mTOR regulates intrinsic clock properties including period and amplitude. In peripheral clock models of hepatocytes and adipocytes, mTOR inhibition lengthens period and dampens amplitude, whereas mTOR activation shortens period and augments amplitude. Constitutive activation of mTOR in Tsc2–/–fibroblasts elevates levels of core clock proteins, including CRY1, BMAL1 and CLOCK. Serum stimulation induces CRY1 upregulation in fibroblasts in an mTOR-dependent but Bmal1- and Period-independent manner. Consistent with results from cellular clock models, mTOR perturbation also regulates period and amplitude in the ex vivo SCN and liver clocks. Further, mTOR heterozygous mice show lengthened circadian period of locomotor activity in both constant darkness and constant light. Together, these results support a significant role for mTOR in circadian timekeeping and in linking metabolic states to circadian clock functions.
机译:生物钟协调生理和新陈代谢。 mTOR(雷帕霉素的哺乳动物/机械靶标)是一种主要的细胞内传感器,集成了营养和能量状态以调节蛋白质的合成,代谢和细胞生长。先前的研究已经确定了mTOR在调节视交叉上核(SCN)的光夹带和中央生物钟同步中的关键作用。鉴于mTOR活动在包括SCN在内的各种组织和细胞中均显示出稳健的昼夜节律振荡,因此我们在此继续研究mTOR在协调中央和外围昼夜节律振荡器的自主时钟功能中的作用。结合遗传学和药理学方法,我们证明mTOR调节内在的时钟特性,包括周期和幅度。在肝细胞和脂肪细胞的外周时钟模型中,mTOR抑制会延长周期并减弱振幅,而mTOR激活会缩短周期并增加振幅。 Tsc2 – / – 成纤维细胞中mTOR的组成性激活可升高核心时钟蛋白(包括CRY1,BMAL1和CLOCK)的水平。血清刺激以mTOR依赖性但Bmal1和周期依赖性的方式诱导成纤维细胞中CRY1上调。与细胞时钟模型的结果一致,mTOR扰动还调节离体SCN和肝脏时钟的周期和幅度。此外,mTOR杂合小鼠在恒定的黑暗和恒定的光照下均显示出自发活动的昼夜节律周期延长。总之,这些结果支持了mTOR在昼夜节律中以及将代谢状态与昼夜节律功能联系起来方面的重要作用。

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