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CHD1 Motor Protein Is Required for Deposition of Histone Variant H3.3 into Chromatin in Vivo

机译:体内将组蛋白变体H3.3沉积到染色质中需要CHD1运动蛋白

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The organization of chromatin affects all aspects of nuclear DNA metabolism in eukaryotes. H3.3 is an evolutionarily conserved histone variant and a key substrate for replication-independent chromatin assembly. Elimination of chromatin remodeling factor CHD1 in Drosophila embryos abolishes incorporation of H3.3 into the male pronucleus, renders the paternal genome unable to participate in zygotic mitoses, and leads to the development of haploid embryos. Furthermore, CHD1, but not ISWI, interacts with HIRA in cytoplasmic extracts. Our findings establish CHD1 as a major factor in replacement histone metabolism in the nucleus and reveal a critical role for CHD1 in the earliest developmental instances of genome-scale, replication-independent nucleosome assembly. Furthermore, our results point to the general requirement of adenosine triphosphate (ATP)—utilizing motor proteins for histone deposition in vivo.
机译:染色质的组织影响真核生物中核DNA代谢的所有方面。 H3.3是进化保守的组蛋白变体,是复制非依赖性染色质组装的关键底物。果蝇胚胎中染色质重塑因子CHD1的消除消除了将H3.3掺入雄性原核,使父本基因组无法参与合子有丝分裂,并导致了单倍体胚胎的发育。此外,CHD1,而不是ISWI,与细胞质提取物中的HIRA相互作用。我们的发现将CHD1确立为替代细胞核中组蛋白代谢的主要因素,并揭示了CHD1在基因组规模,不依赖复制的核小体组装的最早发育过程中的关键作用。此外,我们的结果指出了三磷酸腺苷(ATP)的一般要求-利用运动蛋白在体内进行组蛋白沉积。

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