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Epigenetic Control of Cell Cycle-Dependent Histone Gene Expression Is a Principal Component of the Abbreviated Pluripotent Cell Cycle

机译:细胞周期依赖性组蛋白基因表达的表观遗传控制是缩写的多能细胞周期的主要组成部分。

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摘要

Self-renewal of human pluripotent embryonic stem cells proceeds via an abbreviated cell cycle with a shortened G1 phase. We examined which genes are modulated in this abbreviated period and the epigenetic mechanisms that control their expression. Accelerated upregulation of genes encoding histone proteins that support DNA replication is the most prominent gene regulatory program at the G1/S-phase transition in pluripotent cells. Expedited expression of histone genes is mediated by a unique chromatin architecture reflected by major nuclease hypersensitive sites, atypical distribution of epigenetic histone marks, and a region devoid of histone octamers. We observed remarkable differences in chromatin structure—hypersensitivity and histone protein modifications—between human embryonic stem (hES) and normal diploid cells. Cell cycle-dependent transcription factor binding permits dynamic three-dimensional interactions between transcript initiating and processing factors at 5′ and 3′ regions of the gene. Thus, progression through the abbreviated G1 phase involves cell cycle stage-specific chromatin-remodeling events and rapid assembly of subnuclear microenvironments that activate histone gene transcription to promote nucleosomal packaging of newly replicated DNA during stem cell renewal.
机译:人类多能胚胎干细胞的自我更新通过缩短的G1期细胞周期进行。我们检查了哪些基因在这个简短的时期被调节,以及控制它们表达的表观遗传机制。编码支持DNA复制的组蛋白的基因的加速上调是多能细胞G1 / S相转变中最突出的基因调节程序。组蛋白基因的快速表达由独特的染色质结构介导,该结构由主要的核酸酶超敏位点,表观遗传组蛋白标记的非典型分布以及无组蛋白八聚体的区域反映。我们观察到人类胚胎干细胞(hES)与正常二倍体细胞之间在染色质结构(超敏性和组蛋白修饰)方面存在显着差异。细胞周期依赖性转录因子结合允许在基因的5'和3'区域的转录起始因子和加工因子之间进行动态的三维相互作用。因此,通过缩写的G1期的进展涉及细胞周期阶段特定的染色质重塑事件和亚核微环境的快速组装,这些微环境激活组蛋白基因转录以促进干细胞更新过程中新复制的DNA的核小体包装。

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