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Reprogramming factor expression initiates widespread targeted chromatin remodeling.

机译:重编程因子表达启动广泛的靶向染色质重塑。

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Despite rapid progress in characterizing transcription factor-driven reprogramming of somatic cells to an induced pluripotent stem cell (iPSC) state, many mechanistic questions still remain. To gain insight into the earliest events in the reprogramming process, we systematically analyzed the transcriptional and epigenetic changes that occur during early factor induction after discrete numbers of divisions. We observed rapid, genome-wide changes in the euchromatic histone modification, H3K4me2, at more than a thousand loci including large subsets of pluripotency-related or developmentally regulated gene promoters and enhancers. In contrast, patterns of the repressive H3K27me3 modification remained largely unchanged except for focused depletion specifically at positions where H3K4 methylation is gained. These chromatin regulatory events precede transcriptional changes within the corresponding loci. Our data provide evidence for an early, organized, and population-wide epigenetic response to ectopic reprogramming factors that clarify the temporal order through which somatic identity is reset during reprogramming.
机译:尽管在表征转录因子驱动的体细胞重编程为诱导性多能干细胞(iPSC)状态方面取得了快速进展,但仍然存在许多机制问题。为了深入了解重新编程过程中的最早事件,我们系统地分析了离散分裂次数后早期因子诱导期间发生的转录和表观遗传变化。我们在超过一千个基因座上观察了常染色体组蛋白修饰H3K4me2的快速全基因组变化,包括多潜能相关或发育调控基因启动子和增强子的大子集。相比之下,抑制性的H3K27me3修饰的模式基本上保持不变,除了集中消耗特别是在获得H3K4甲基化的位置上。这些染色质调节事件在相应基因座内的转录变化之前。我们的数据提供了对异位重编程因子的早期,有组织的和整个人群的表观遗传反应的证据,这些因子阐明了在重编程过程中重置身体身份的时间顺序。

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