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Nucleosome eviction along with H3K9ac deposition enhances Sox2 binding during human neuroectodermal commitment

机译:核小体驱逐与H3K9ac沉积增强了人类神经外胚层承诺过程中的Sox2结合

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摘要

Neuroectoderm is an important neural precursor. However, chromatin remodeling and its epigenetic regulatory roles during the differentiation of human neuroectodermal cells (hNECs) from human embryonic stem cells (hESCs) remain largely unexplored. Here, we obtained hNECs through directed differentiation from hESCs, and determined chromatin states in the two cell types. Upon differentiation, H2A.Z-mediated nucleosome depletion leads to an open chromatin structure in promoters and upregulates expression of neuroectodermal genes. Increase in H3K9ac signals and decrease in H3K27me3 signals in promoters result in an active chromatin state and activate neuroectodermal genes. Conversely, decrease in H3K9ac signals and increase in H3K27me3 signals in promoters repress pluripotency genes. Moreover, H3K9ac signals facilitate the pluripotency factor Sox2 binding to target sites unique to hNECs. Knockdown of the acetyltransferase Kat2b erases H3K9ac signals, disrupts Sox2 binding, and fails the differentiation. Our results demonstrate a hierarchy of epigenetic regulation of gene expression during the differentiation of hNECs from hESCs through chromatin remodeling.
机译:神经外皮是重要的神经前体。然而,染色质重塑及其在人类神经外胚层细胞(hNECs)与人类胚胎干细胞(hESCs)分化过程中的表观遗传调控作用仍未开发。在这里,我们通过与hESC的定向分化获得了hNEC,并确定了两种细胞类型中的染色质状态。分化后,H2A.Z介导的核小体耗竭导致启动子中的染色质结构开放,并上调神经外胚层基因的表达。启动子中H3K9ac信号的增加和H3K27me3信号的减少会导致活跃的染色质状态并激活神经外胚层基因。相反,启动子中H3K9ac信号的减少和H3K27me3信号的增加会抑制多能性基因。此外,H3K9ac信号促进多能性因子Sox2与hNEC特有的靶位点结合。敲除乙酰基转移酶Kat2b会擦除H3K9ac信号,破坏Sox2结合,并使分化失败。我们的结果证明了通过染色质重塑从hESC分化出hNEC的过程中,基因表达的表观遗传调控。

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