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Genome-Wide Occupancy of SREBP1 and Its Partners NFY and SP1 Reveals Novel Functional Roles and Combinatorial Regulation of Distinct Classes of Genes

机译:SREBP1及其合作伙伴NFY和SP1的全基因组占有率揭示了不同基因类别的新型功能作用和组合调控

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The sterol regulatory element-binding protein (SREBP) family member SREBP1 is a critical transcriptional regulator of cholesterol and fatty acid metabolism and has been implicated in insulin resistance, diabetes, and other diet-related diseases. We globally identified the promoters occupied by SREBP1 and its binding partners NFY and SP1 in a human hepatocyte cell line using chromatin immunoprecipitation combined with genome tiling arrays (ChIP-chip). We find that SREBP1 occupies the promoters of 1,141 target genes involved in diverse biological pathways, including novel targets with roles in lipid metabolism and insulin signaling. We also identify a conserved SREBP1 DNA-binding motif in SREBP1 target promoters, and we demonstrate that many SREBP1 target genes are transcriptionally activated by treatment with insulin and glucose using gene expression microarrays. Finally, we show that SREBP1 cooperates extensively with NFY and SP1 throughout the genome and that unique combinations of these factors target distinct functional pathways. Our results provide insight into the regulatory circuitry in which SREBP1 and its network partners coordinate a complex transcriptional response in the liver with cues from the diet.
机译:固醇调节元件结合蛋白(SREBP)家族成员SREBP1是胆固醇和脂肪酸代谢的关键转录调节剂,与胰岛素抵抗,糖尿病和其他饮食相关疾病有关。我们使用染色质免疫沉淀结合基因组平铺芯片(芯片),在人类肝细胞系中全球确定了SREBP1及其结合伴侣NFY和SP1所占据的启动子。我们发现SREBP1占据了1141个目标基因的启动子,这些基因参与了多种生物途径,包括在脂质代谢和胰岛素信号传导中起作用的新型目标。我们还确定了SREBP1目标启动子中的保守SREBP1 DNA结合基序,并且我们证明了许多SREBP1目标基因通过使用基因表达微阵列经胰岛素和葡萄糖处理而被转录激活。最后,我们显示SREBP1在整个基因组中与NFY和SP1广泛合作,并且这些因子的独特组合靶向不同的功能途径。我们的结果提供了对SREBP1及其网络伙伴通过饮食中的信号协调肝脏中复杂转录反应的调节电路的见解。

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