MacroH2A has been linked to transcriptional silencing, cell identity, and is a hallmark of the inactive X chromosome (Xi). However, it remains unclear whether macroH2A plays a role in DNA replication. Using knockdown/knockout cells for each macroH2A isoform, we show that macroH2A-containing nucleosomes slow down replication progression rate in the Xi reflecting the higher nucleosome stability. Moreover, macroH2A1, but not macroH2A2, regulates the number of nano replication foci in the Xi, and macroH2A1 downregulation increases DNA loop sizes corresponding to replicons. This relates to macroH2A1 regulating replicative helicase loading during G1 by interacting with it. We mapped this interaction to a phenylalanine in macroH2A1 that is not conserved in macroH2A2 and the C-terminus of Mcm3 helicase subunit. We propose that macroH2A1 enhances the licensing of pre-replication complexes via DNA helicase interaction and loading onto the Xi.
Histone variant macroH2A1 regulates synchronous firing of replication origins in the inactive X chromosome.
组蛋白变体 macroH2A1 调节非活性 X 染色体中复制起点的同步激活
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作者:Arroyo Maria, Casas-Delucchi Corella S, Pabba Maruthi K, Prorok Paulina, Pradhan Sunil K, Rausch Cathia, Lehmkuhl Anne, Maiser Andreas, Buschbeck Marcus, Pasque Vincent, Bernstein Emily, Luck Katja, Cardoso M Cristina
| 期刊: | Nucleic Acids Research | 影响因子: | 13.100 |
| 时间: | 2024 | 起止号: | 2024 Oct 28; 52(19):11659-11688 |
| doi: | 10.1093/nar/gkae734 | 研究方向: | 其它 |
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