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Pancreatic islet enhancer clusters enriched in type 2 diabetes risk-associated variants

机译:富含2型糖尿病风险相关变异的胰岛增强剂簇

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Type 2 diabetes affects over 300 million people, causing severe complications and premature death, yet the underlying molecular mechanisms are largely unknown. Pancreatic islet dysfunction is central in type 2 diabetes pathogenesis, and understanding islet genome regulation could therefore provide valuable mechanistic insights. We have now mapped and examined the function of human islet cis-regulatory networks. We identify genomic sequences that are targeted by islet transcription factors to drive islet-specific gene activity and show that most such sequences reside in clusters of enhancers that form physical three-dimensional chromatin domains. We find that sequence variants associated with type 2 diabetes and fasting glycemia are enriched in these clustered islet enhancers and identify trait-associated variants that disrupt DNA binding and islet enhancer activity. Our studies illustrate how islet transcription factors interact functionally with the epigenome and provide systematic evidence that the dysregulation of islet enhancers is relevant to the mechanisms underlying type 2 diabetes.
机译:2型糖尿病影响3亿多人,造成严重的并发症和过早死亡,但基本的分子机制尚不清楚。胰腺胰岛功能障碍是2型糖尿病发病机制的中心,因此了解胰岛基因组调控可能会提供有价值的机理见解。现在,我们已经映射并研究了人类胰岛顺式调节网络的功能。我们确定了以胰岛转录因子为目标的基因组序列,以驱动胰岛特定的基因活性,并表明大多数此类序列位于形成物理三维染色质域的增强子簇中。我们发现与这些2型糖尿病和空腹血糖相关的序列变异体富含这些簇状的胰岛增强剂,并鉴定了破坏DNA结合和胰岛增强剂活性的性状相关变异体。我们的研究说明了胰岛转录因子如何与表观基因组功能性相互作用,并提供了系统的证据表明胰岛增强剂的失调与2型糖尿病的潜在机制有关。

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