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In Vivo Study of the Nucleosome Assembly Functions of ASF1 Histone Chaperones in Human Cells

机译:人体细胞中ASF1组蛋白伴侣的核小体装配功能的体内研究

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摘要

Histone chaperones have been implicated in nucleosome assembly and disassembly as well as histone modification. ASF1 is a highly conserved histone H3/H4 chaperone that synergizes in vitro with two other histone chaperones, chromatin assembly factor 1 (CAF-1) and histone repression A factor (HIRA), in DNA synthesis-coupled and DNA synthesis-independent nucleosome assembly. Here, we identify mutants of histones H3.1 and H3.3 that are unable to interact with human ASF1A and ASF1B isoforms but that are still competent to bind CAF-1 and HIRA, respectively. We show that these mutant histones are inefficiently deposited into chromatin in vivo. Furthermore, we found that both ASF1A and ASF1B participate in the DNA synthesis-independent deposition of H3.3 in HeLa cells, thus highlighting an unexpected role for ASF1B in this pathway. This pathway does not require interaction of ASF1 with HIRA. We provide the first direct determination that ASF1A and ASF1B play a role in the efficiency of nucleosome assembly in vivo in human cells.
机译:组蛋白伴侣已与核小体的组装和拆卸以及组蛋白修饰有关。 ASF1是高度保守的组蛋白H3 / H4分子伴侣,可在体外与DNA合成偶联和独立于DNA合成的核小体装配体中的其他两种组蛋白伴侣(染色质装配因子1(CAF-1)和组蛋白阻抑A因子(HIRA))协同作用。 。在这里,我们识别出无法与人ASF1A和ASF1B亚型相互作用但仍能分别结合CAF-1和HIRA的组蛋白H3.1和H3.3突变体。我们表明,这些突变组蛋白在体内不能有效地沉积到染色质中。此外,我们发现ASF1A和ASF1B均参与HeLa细胞中H3.3的DNA合成非依赖性沉积,从而突显了ASF1B在此途径中的意外作用。该途径不需要ASF1与HIRA相互作用。我们提供了第一个直接确定ASF1A和ASF1B在人类细胞体内体内核小体组装效率中发挥作用的方法。

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