| Literature DB >> 31768048 |
Jian-Fei Pei1, Xun-Kai Li1, Wen-Qi Li1, Qian Gao2,3, Yang Zhang1, Xiao-Man Wang1, Jia-Qi Fu1, Shen-Shen Cui1, Jia-Hua Qu1, Xiang Zhao1, De-Long Hao1, Dapeng Ju4, Na Liu4,5, Kate S Carroll6, Jing Yang7, Eric Erquan Zhang4, Ji-Min Cao2,8, Hou-Zao Chen9, De-Pei Liu10.
Abstract
Redox balance, an essential feature of healthy physiological steady states, is regulated by circadian clocks, but whether or how endogenous redox signalling conversely regulates clockworks in mammals remains unknown. Here, we report circadian rhythms in the levels of endogenous H2O2 in mammalian cells and mouse livers. Using an unbiased method to screen for H2O2-sensitive transcription factors, we discovered that rhythmic redox control of CLOCK directly by endogenous H2O2 oscillations is required for proper intracellular clock function. Importantly, perturbations in the rhythm of H2O2 levels induced by the loss of p66Shc, which oscillates rhythmically in the liver and suprachiasmatic nucleus (SCN) of mice, disturb the rhythmic redox control of CLOCK function, reprogram hepatic transcriptome oscillations, lengthen the circadian period in mice and modulate light-induced clock resetting. Our findings suggest that redox signalling rhythms are intrinsically coupled to the circadian system through reversible oxidative modification of CLOCK and constitute essential mechanistic timekeeping components in mammals.Entities:
Mesh:
Substances:
Year: 2019 PMID: 31768048 PMCID: PMC7184292 DOI: 10.1038/s41556-019-0420-4
Source DB: PubMed Journal: Nat Cell Biol ISSN: 1465-7392 Impact factor: 28.824