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Dynamic changes in chromatin states during specification and differentiation of adult intestinal stem cells

机译:成人肠道细胞规范和分化期间染色质态的动态变化

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Epigenetic mechanisms, including chromatin structure, chromatin dynamics and histone modifications play an important role for maintenance and differentiation of pluripotent embryonic stem cells. However, little is known about the molecular mechanisms of adult stem cell specification and differentiation. Here, we used intestinal stem cells (ISCs) as a model system to reveal the epigenetic changes coordinating gene expression programs during these processes. We found that two distinct epigenetic mechanisms participate in establishing the transcriptional program promoting ISC specification from embryonic progenitors. A large number of adult ISC signature genes are targets of repressive DNA methylation in embryonic intestinal epithelial progenitors. On the other hand, genes essential for embryonic development acquire H3K27me3 and are silenced during ISC specification. We also show that the repression of ISC signature genes as well as the activation of enterocyte specific genes is accompanied by a global loss of H2A.Z during ISCs differentiation. Our results reveal that, already during ISC specification, an extensive remodeling of chromatin both at promoters and distal regulatory elements organizes transcriptional landscapes operating in differentiated enterocytes, thus explaining similar chromatin modification patterns in the adult gut epithelium.
机译:表观遗传机制,包括染色质结构,染色质动力学和组蛋白修饰在多能胚胎干细胞的维护和分化起着重要作用。然而,关于成人干细胞规格和分化的分子机制很少。在此,我们使用肠道干细胞(ISC)作为模型系统,以揭示在这些过程中协调基因表达程序的表观遗传改变。我们发现,两个不同的表观遗传机制参与建立从胚胎祖细胞的ISC规范的转录程序。大量成年ISC签名基因是胚胎肠上皮祖细胞抑制DNA甲基化的靶标。另一方面,胚胎发育必需的基因获得H3K27ME3,在ISC规范期间沉默。我们还表明,ISC签名基因的抑制以及肠​​细胞特异性基因的激活伴随着ISCS分化期间H2A.z的全局丧失。我们的结果表明,已经在ISC规范期间,在启动子和远端调节元件中,染色质的广泛重塑组织在分化的肠细胞中操作的转录景观,因此在成人肠道上皮中解释了类似的染色质修饰模式。

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