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Genome-wide incorporation dynamics reveal distinct categories of turnover for the histone variant H3.3

机译:全基因组整合动力学揭示了组蛋白变体H3.3的不同营业额类别

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摘要

BackgroundNucleosomes are present throughout the genome and must be dynamically regulated to accommodate binding of transcription factors and RNA polymerase machineries by various mechanisms. Despite the development of protocols and techniques that have enabled us to map nucleosome occupancy genome-wide, the dynamic properties of nucleosomes remain poorly understood, particularly in mammalian cells. The histone variant H3.3 is incorporated into chromatin independently of DNA replication and requires displacement of existing nucleosomes for its deposition. Here, we measure H3.3 turnover at high resolution in the mammalian genome in order to present a genome-wide characterization of replication-independent H3.3-nucleosome dynamics.
机译:背景技术核小体存在于整个基因组中,必须通过各种机制进行动态调节以适应转录因子和RNA聚合酶机制的结合。尽管协议和技术的发展使我们能够在全基因组范围内绘制核小体的占有率,但对核小体的动态特性仍然知之甚少,尤其是在哺乳动物细胞中。组蛋白变体H3.3独立于DNA复制而掺入染色质,需要置换现有的核小体才能沉积。在这里,我们在高分辨率的哺乳动物基因组中测量H3.3营业额,以便提出不依赖复制的H3.3核小体动力学的全基因组表征。

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