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核受体 REVERBα 是一种依赖状态的肝脏能量代谢调节剂。

Nuclear receptor REVERBα is a state-dependent regulator of liver energy metabolism.

机构信息

Centre for Biological Timing, Faculty of Biology, Medicine and Health, University of Manchester, M13 9PT Manchester, United Kingdom.

Genome Editing Unit, Faculty of Biology, Medicine and Health, University of Manchester, M13 9PT Manchester, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2020 Oct 13;117(41):25869-25879. doi: 10.1073/pnas.2005330117. Epub 2020 Sep 28.

Abstract

The nuclear receptor REVERBα is a core component of the circadian clock and proposed to be a dominant regulator of hepatic lipid metabolism. Using antibody-independent ChIP-sequencing of REVERBα in mouse liver, we reveal a high-confidence cistrome and define direct target genes. REVERBα-binding sites are highly enriched for consensus RORE or RevDR2 motifs and overlap with corepressor complex binding. We find no evidence for transcription factor tethering and DNA-binding domain-independent action. Moreover, hepatocyte-specific deletion of drives only modest physiological and transcriptional dysregulation, with derepressed target gene enrichment limited to circadian processes. Thus, contrary to previous reports, hepatic REVERBα does not repress lipogenesis under basal conditions. REVERBα control of a more extensive transcriptional program is only revealed under conditions of metabolic perturbation (including mistimed feeding, which is a feature of the global mouse). Repressive action of REVERBα in the liver therefore serves to buffer against metabolic challenge, rather than drive basal rhythmicity in metabolic activity.

摘要

核受体 REVERBα 是昼夜节律钟的核心组成部分,被认为是肝脏脂质代谢的主要调节因子。我们采用非抗体依赖的 ChIP-seq 技术在小鼠肝脏中研究 REVERBα,揭示了一个高可信度的顺式作用元件组,并定义了直接靶基因。REVERBα 结合位点高度富含共识 RORE 或 RevDR2 基序,并与共抑制复合物结合重叠。我们没有发现转录因子固定和 DNA 结合域非依赖性作用的证据。此外,肝细胞特异性缺失仅导致适度的生理和转录失调,受抑制靶基因富集仅限于昼夜节律过程。因此,与先前的报告相反,肝脏中的 REVERBα 在基础条件下不会抑制脂肪生成。只有在代谢扰动的条件下(包括时间不当的喂养,这是全球 小鼠的一个特征),REVERBα 才能控制更广泛的转录程序。因此,REVERBα 在肝脏中的抑制作用有助于缓冲代谢挑战,而不是驱动代谢活性的基础节律性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc1a/7568238/557ca9121c78/pnas.2005330117fig01.jpg

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