生物
蛋白质组
蛋白质稳态
昼夜节律
隐色素
表型
蛋白质组学
细胞生物学
平衡
生物钟
蛋白质周转
遗传学
作者
David C S Wong,Estere Seinkmane,Aiwei Zeng,Alessandra Stangherlin,Nina M Rzechorzek,Andrew D. Beale,Jason Day,Martin Reed,Sew Y. Peak-Chew,Christine T. Styles,Rachel S. Edgar,Marrit Putker,John S. O’Neill
标识
DOI:10.15252/embj.2021108883
摘要
The daily organisation of most mammalian cellular functions is attributed to circadian regulation of clock-controlled protein expression, driven by daily cycles of CRYPTOCHROME-dependent transcriptional feedback repression. To test this, we used quantitative mass spectrometry to compare wild-type and CRY-deficient fibroblasts under constant conditions. In CRY-deficient cells, we found that temporal variation in protein, phosphopeptide, and K+ abundance was at least as great as wild-type controls. Most strikingly, the extent of temporal variation within either genotype was much smaller than overall differences in proteome composition between WT and CRY-deficient cells. This proteome imbalance in CRY-deficient cells and tissues was associated with increased susceptibility to proteotoxic stress, which impairs circadian robustness, and may contribute to the wide-ranging phenotypes of CRY-deficient mice. Rather than generating large-scale daily variation in proteome composition, we suggest it is plausible that the various transcriptional and post-translational functions of CRY proteins ultimately act to maintain protein and osmotic homeostasis against daily perturbation.
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