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REVERBa couples the circadian clock to hepatic glucocorticoid action

机译:REVERBa将昼夜节律与肝糖皮质激素作用相结合

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摘要

The glucocorticoid receptor (GR) is a major drug target in inflammatory disease. However, chronic glucocorticoid (GC) treatment leads to disordered energy metabolism, including increased weight gain, adiposity, and hepatosteatosis — all programs modulated by the circadian clock. We demonstrated that while antiinflammatory GC actions were maintained irrespective of dosing time, the liver was significantly more GC sensitive during the day. Temporal segregation of GC action was underpinned by a physical interaction of GR with the circadian transcription factor REVERBa and co-binding with liver-specific hepatocyte nuclear transcription factors (HNFs) on chromatin. REVERBa promoted efficient GR recruitment to chromatin during the day, acting in part by maintaining histone acetylation, with REVERBa-dependent GC responses providing segregation of carbohydrate and lipid metabolism. Importantly, deletion of Reverba inverted circadian liver GC sensitivity and protected mice from hepatosteatosis induced by chronic GC administration. Our results reveal a mechanism by which the circadian clock acts through REVERBa in liver on elements bound by HNF4A/HNF6 to direct GR action on energy metabolism.
机译:糖皮质激素受体(GR)是炎性疾病中的主要药物靶标。但是,慢性糖皮质激素(GC)治疗会导致能量代谢紊乱,包括体重增加,肥胖和肝脂肪变性增加-所有这些程序都由昼夜节律调节。我们证明,尽管无论给药时间长短,抗炎GC的作用都得以维持,但肝脏在白天对GC的敏感性更高。 GR作用的时间分隔是由GR与昼夜节律转录因子REVERBa的物理相互作用以及与染色质上肝脏特异性肝细胞核转录因子(HNFs)的共结合所支撑的。 REVERBa在一天中促进了有效的GR募集到染色质,部分通过维持组蛋白乙酰化而起作用,REVERBa依赖的GC反应提供了碳水化合物和脂质代谢的分离。重要的是,Reverba倒置的昼夜节律性肝GC敏感性降低,可保护小鼠免于长期用GC诱导的肝脂肪变性。我们的结果揭示了生物钟通过肝脏中的REVERBa作用于由HNF4A / HNF6结合的元素上的机制,从而指导GR对能量代谢的作用。

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