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A System for Genome-Wide Histone Variant Dynamics In ES Cells Reveals Dynamic MacroH2A2 Replacement at Promoters

机译:ES细胞中的全基因组组蛋白变异动力学系统揭示了启动子的动态MacroH2A2替代。

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摘要

Dynamic exchange of a subset of nucleosomes in vivo plays important roles in epigenetic inheritance of chromatin states, chromatin insulator function, chromosome folding, and the maintenance of the pluripotent state of embryonic stem cells. Here, we extend a pulse-chase strategy for carrying out genome-wide measurements of histone dynamics to several histone variants in murine embryonic stem cells and somatic tissues, recapitulating expected characteristics of the well characterized H3.3 histone variant. We extended this system to the less-studied MacroH2A2 variant, commonly described as a “repressive” histone variant whose accumulation in chromatin is thought to fix the epigenetic state of differentiated cells. Unexpectedly, we found that while large intergenic blocks of MacroH2A2 were stably associated with the genome, promoter-associated peaks of MacroH2A2 exhibited relatively rapid exchange dynamics in ES cells, particularly at highly-transcribed genes. Upon differentiation to embryonic fibroblasts, MacroH2A2 was gained primarily in additional long, stably associated blocks across gene-poor regions, while overall turnover at promoters was greatly dampened. Our results reveal unanticipated dynamic behavior of the MacroH2A2 variant in pluripotent cells, and provide a resource for future studies of tissue-specific histone dynamics in vivo.
机译:体内核小体子集的动态交换在染色质状态的表观遗传,染色质绝缘子功能,染色体折叠以及胚胎干细胞多能状态的维持中起着重要作用。在这里,我们扩展了一种脉冲追踪策略,用于对小鼠胚胎干细胞和体细胞组织中的几个组蛋白变体进行组蛋白动力学的全基因组测量,概括了特征明确的H3.3组蛋白变体的预期特征。我们将该系统扩展到研究较少的MacroH2A2变异体,通常被称为“抑制性”组蛋白变异体,其在染色质中的积累被认为可以固定分化细胞的表观遗传状态。出乎意料的是,我们发现,虽然MacroH2A2的大型基因间块与基因组稳定相关,但MacroH2A2的启动子相关峰在ES细胞中表现出相对较快的交换动力学,特别是在高度转录的基因处。在分化为胚胎成纤维细胞后,MacroH2A2主要是在基因贫乏地区的其他较长,稳定关联的区域中获得的,而启动子的整体更新则受到了极大的阻碍。我们的研究结果揭示了MacroH2A2变体在多能细胞中的出乎意料的动力学行为,并为体内组织特异性组蛋白动力学的未来研究提供了资源。

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