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LSH 催化由 ATP 驱动的组蛋白变体 macroH2A1 和 macroH2A2 的交换。

LSH catalyzes ATP-driven exchange of histone variants macroH2A1 and macroH2A2.

机构信息

Epigenetics Section, Mouse Cancer Genetics Program, National Cancer Institute, Frederick, MD 21702, USA.

Epigenetics Section, Frederick National Laboratory for Cancer Research in the Mouse Cancer Genetics Program, National Cancer Institute, Frederick, MD 21702, USA.

出版信息

Nucleic Acids Res. 2021 Aug 20;49(14):8024-8036. doi: 10.1093/nar/gkab588.

Abstract

LSH, a homologue of the ISWI/SNF2 family of chromatin remodelers, is required in vivo for deposition of the histone variants macroH2A1 and macroH2A2 at specific genomic locations. However, it remains unknown whether LSH is directly involved in this process or promotes other factors. Here we show that recombinant LSH interacts in vitro with macroH2A1-H2B and macroH2A2-H2B dimers, but not with H2A.Z-H2B dimers. Moreover, LSH catalyzes the transfer of macroH2A into mono-nucleosomes reconstituted with canonical core histones in an ATP dependent manner. LSH requires the ATP binding site and the replacement process is unidirectional leading to heterotypic and homotypic nucleosomes. Both variants macroH2A1 and macroH2A2 are equally well incorporated into the nucleosome. The histone exchange reaction is specific for histone variant macroH2A, since LSH is not capable to incorporate H2A.Z. These findings define a previously unknown role for LSH in chromatin remodeling and identify a novel molecular mechanism for deposition of the histone variant macroH2A.

摘要

LSH 是染色质重塑剂 ISWI/SNF2 家族的同源物,在体内需要沉积组蛋白变体 macroH2A1 和 macroH2A2 到特定的基因组位置。然而,目前尚不清楚 LSH 是否直接参与该过程,还是促进其他因素。在这里,我们显示重组 LSH 在体外与 macroH2A1-H2B 和 macroH2A2-H2B 二聚体相互作用,但不与 H2A.Z-H2B 二聚体相互作用。此外,LSH 以 ATP 依赖的方式催化将 macroH2A 转移到用经典核心组蛋白重建的单核小体中。LSH 需要 ATP 结合位点,并且取代过程是单向的,导致异质和同质核小体。两种变体 macroH2A1 和 macroH2A2 都同样容易被纳入核小体。组蛋白交换反应是针对组蛋白变体 macroH2A 的特异性,因为 LSH 不能掺入 H2A.Z。这些发现定义了 LSH 在染色质重塑中的一个以前未知的作用,并确定了沉积组蛋白变体 macroH2A 的新分子机制。

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