Division of Endocrinology, Diabetes, and Metabolism, Department of Medicine, Department of Genetics, The Institute for Diabetes, Obesity, and Metabolism, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.
Genes Dev. 2012 Apr 1;26(7):657-67. doi: 10.1101/gad.186858.112.
The nuclear receptor Rev-erbα regulates circadian rhythm and metabolism, but its effects are modest and it has been considered to be a secondary regulator of the cell-autonomous clock. Here we report that depletion of Rev-erbα together with closely related Rev-erbβ has dramatic effects on the cell-autonomous clock as well as hepatic lipid metabolism. Mouse embryonic fibroblasts were rendered arrhythmic by depletion of both Rev-erbs. In mouse livers, Rev-erbβ mRNA and protein levels oscillate with a diurnal pattern similar to that of Rev-erbα, and both Rev-erbs are recruited to a remarkably similar set of binding sites across the genome, enriched near metabolic genes. Depletion of both Rev-erbs in liver synergistically derepresses several metabolic genes as well as genes that control the positive limb of the molecular clock. Moreover, deficiency of both Rev-erbs causes marked hepatic steatosis, in contrast to relatively subtle changes upon loss of either subtype alone. These findings establish the two Rev-erbs as major regulators of both clock function and metabolism, displaying a level of subtype collaboration that is unusual among nuclear receptors but common among core clock proteins, protecting the organism from major perturbations in circadian and metabolic physiology.
核受体 Rev-erbα 调节昼夜节律和代谢,但它的作用有限,被认为是细胞自主时钟的次要调节剂。在这里,我们报告说,Rev-erbα 与密切相关的 Rev-erbβ 的耗竭对细胞自主时钟以及肝脏脂质代谢有显著影响。通过耗竭这两种 Rev-erb,使小鼠胚胎成纤维细胞失去节律性。在小鼠肝脏中,Rev-erbβ mRNA 和蛋白质水平呈昼夜节律性波动,与 Rev-erbα 的波动模式相似,并且这两种 Rev-erb 都被招募到基因组上非常相似的一组结合位点,这些结合位点富集在代谢基因附近。肝脏中这两种 Rev-erb 的同时耗竭协同地下调了几种代谢基因以及控制分子钟正相的基因。此外,这两种 Rev-erb 的缺乏会导致明显的肝脂肪变性,而单独缺失任何一种亚型只会引起相对细微的变化。这些发现确立了这两种 Rev-erb 作为时钟功能和代谢的主要调节剂,表现出核受体中不常见但核心时钟蛋白中常见的亚基协作水平,保护机体免受昼夜节律和代谢生理学中重大干扰。
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