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Polycomb PHF19 binds H3K36me3 and recruits PRC2 and demethylase NO66 to embryonic stem cell genes during differentiation

机译:Polycomb PHF19结合H3K36me3并在分化过程中募集PRC2和脱甲基酶NO66至胚胎干细胞基因

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Polycomb group proteins are repressive chromatin modifiers with essential roles in metazoan development, cellular differentiation and cell fate maintenance. How Polycomb proteins access active chromatin to confer transcriptional silencing during lineage transitions remains unclear. Here we show that the Polycomb repressive complex 2 (PRC2) component PHF19 binds trimethylated histone H3 Lys36 (H3K36me3), a mark of active chromatin, via its Tudor domain. PHF19 associates with the H3K36me3 demethylase NO66, and it is required to recruit the PRC2 complex and NO66 to stem cell genes during differentiation, leading to PRC2-mediated trimethylation of histone H3 Lys27 (H3K27), loss of H3K36me3 and transcriptional silencing. We propose a model whereby PHF19 functions during mouse embryonic stem cell differentiation to transiently bind the H3K36me3 mark via its Tudor domain, forming essential contact points that allow recruitment of PRC2 and H3K36me3 demethylase activity to active gene loci during their transition to a Polycomb-repressed state.
机译:聚梳组蛋白是抑制性染色质修饰剂,在后生发育,细胞分化和细胞命运维持中起重要作用。尚不清楚Polycomb蛋白如何在谱系过渡期间访问活性染色质以赋予转录沉默。在这里,我们显示Polycomb阻抑复合物2(PRC2)组件PHF19通过其Tudor域结合三甲基化组蛋白H3 Lys36(H3K36me3),这是活性染色质的标记。 PHF19与H3K36me3脱甲基酶NO66相关,在分化过程中需要募集PRC2复合物和NO66到干细胞基因中,导致PRC2介导的组蛋白H3 Lys27(H3K27)三甲基化,H3K36me3丢失和转录沉默。我们提出了一种模型,其中PHF19在小鼠胚胎干细胞分化过程中发挥功能,以通过其Tudor结构域短暂结合H3K36me3标记,形成必需的接触点,从而使PRC2和H3K36me3脱甲基酶活性在过渡到Polycomb抑制状态的过程中募集到活性基因位点。

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