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首页> 外文期刊>Molecular cell >Phosphorylation and Recruitment of BAF60c in Chromatin Remodeling for Lipogenesis in Response to Insulin
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Phosphorylation and Recruitment of BAF60c in Chromatin Remodeling for Lipogenesis in Response to Insulin

机译:BAF60c的磷酸化和招募在染色质重塑成脂反应胰岛素。

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Fatty acid and triglyceride synthesis is induced in response to feeding and insulin. This lipogenic induction involves coordinate transcriptional activation of lipogenic enzymes, including fatty acid synthase and glycerol-3-phosphate acyltransferase. We recently reported the importance of USF-1 phosphorylation and subsequent acetylation in insulin-induced lipogenic gene activation. Here, we show that Brg1/Brm-associated factor (BAF) 60c is a specific chromatin remodeling component for lipogenic gene transcription in liver. In response to insulin, BAF60c is phosphorylated at S247 by atypical PKCζ/λ, which causes translocation of BAF60c to the nucleus and allows a direct interaction of BAF60c with USF-1 that is phosphorylated by DNA-PK and acetylated by P/CAF. Thus, BAF60c is recruited to form the lipoBAF complex to remodel chromatin structure and to activate lipogenic genes. Consequently, BAF60c promotes lipogenesis in vivo and increases triglyceride levels, demonstrating its role in metabolic adaption to activate the lipogenic program in response to feeding and insulin.
机译:脂肪酸和甘油三酸酯的合成是由于进食和胰岛素引起的。这种脂肪诱导涉及脂肪酶的协调转录激活,包括脂肪酸合酶和3-磷酸甘油酰基转移酶。我们最近报道了USF-1磷酸化和随后的乙酰化在胰岛素诱导的致脂基因激活中的重要性。在这里,我们显示Brg1 / Brm相关因子(BAF)60c是肝脏中脂肪基因转录的特定染色质重塑成分。响应胰岛素,BAF60c在S247处被非典型PKCζ/λ磷酸化,导致BAF60c易位至细胞核,并使BAF60c与USF-1直接相互作用,而USF-1被DNA-PK磷酸化并被P / CAF乙酰化。因此,募集BAF60c以形成lipoBAF复合物,以重塑染色质结构并激活生脂基因。因此,BAF60c在体内促进脂肪生成并增加甘油三酸酯水平,表明其在代谢适应中的作用,以响应于进食和胰岛素而激活脂肪生成程序。

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