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首页> 外文期刊>Developmental cell >Global Landscape and Regulatory Principles of DNA Methylation Reprogramming for Germ Cell Specification by Mouse Pluripotent Stem Cells
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Global Landscape and Regulatory Principles of DNA Methylation Reprogramming for Germ Cell Specification by Mouse Pluripotent Stem Cells

机译:通过小鼠多能干细胞的生殖细胞规范DNA甲基化重编程的全球格局和监管原则。

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摘要

Specification of primordial germ cells (PGCs) activates epigenetic reprogramming for totipotency, the elucidation of which remains a fundamental challenge. Here, we uncover regulatory principles for DNA methylation reprogramming during in vitro PGC specification, in which mouse embryonic stem cells (ESCs) are induced into epiblast-like cells (EpiLCs) and then PGC-like cells (PGCLCs). While ESCs reorganize their methylome to form EpiLCs, PGCLCs essentially dilute the EpiLC methylome at constant, yet different, rates between unique sequence regions and repeats. ESCs form hypomethylated domains around pluripotency regulators for their activation, whereas PGCLCs create demethylation-sensitive domains around developmental regulators by accumulating abundant H3K27me3 for their repression. Loss of PRDM14 globally upregulates methylation and diminishes the hypomethylated domains, but it preserves demethylation-sensitive domains. Notably, female ESCs form hypomethylated lamina-associated domains, while female PGCLCs effectively reverse such states into a more normal configuration. Our findings illuminate the unique orchestration of DNA methylation and histone modification reprogramming during PGC specification.
机译:原始生殖细胞(PGC)的规范激活了全能性的表观遗传重编程,其阐明仍然是一项基本挑战。在这里,我们揭示了体外PGC规范中DNA甲基化重编程的调控原理,其中将小鼠胚胎干细胞(ESC)诱导为上皮样细胞(EpiLCs),然后诱导为PGC样细胞(PGCLC)。当ESC重新组织其甲基化组以形成EpiLC时,PGCLC基本上以独特序列区和重复序列之间恒定但不同的速率稀释EpiLC甲基化组。 ESC在其多能性调节子周围形成低甲基化结构域,以使其激活,而PGCLC通过在其积累的H3K27me3上积累大量的抑制因子,从而在发育性调节子周围形成去甲基化敏感结构域。 PRDM14的丢失全局上调甲基化并减少了低甲基化的域,但保留了对甲基化敏感的域。值得注意的是,雌性ESC形成低甲基化的椎板相关结构域,而雌性PGLCC有效地将这种状态逆转为更正常的构型。我们的发现阐明了PGC规范期间DNA甲基化和组蛋白修饰重编程的独特编排。

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