The INO80 Chromatin Remodeling Complex Regulates Histone H2A.Z Mobility and the G1-S Transition in Oligodendrocyte Precursors

IF 5.1 2区 医学 Q1 NEUROSCIENCES Glia Pub Date : 2025-02-28 DOI:10.1002/glia.70006
Jordan L. Wright, Yi Jiang, Stuart G. Nayar, Huiliang Li, William D. Richardson
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Abstract

Chromatin remodeling complexes (CRCs) participate in oligodendrocyte (OL) differentiation, survival, and maintenance. We asked whether CRCs also control the proliferation of OL precursors (OPs)—focusing on the INO80 complex, which is known to regulate the proliferation of a variety of other cell types during development and disease. CRISPR/Cas9-mediated inactivation of Ino80 in vitro, or Cre-mediated deletion in vivo, slowed the OP cell cycle substantially by prolonging G1. RNAseq analysis revealed that E2F target genes were dysregulated in OPs from INO80-deficient mice, but correlated RNAseq and ATAC-seq uncovered no general correlation between gene expression and altered nucleosome positioning at transcription start sites. Fluorescence photobleaching experiments in cultured OPs demonstrated that histone H2A.Z mobility increased following the loss of INO80, suggesting that INO80 regulates the cell cycle machinery in OPs through H2A.Z/H2A exchange. We also present evidence that INO80 associates with OLIG2, a master regulator of OL development.

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INO80染色质重塑复合体调控组蛋白H2A。少突胶质细胞前体的Z迁移率和G1-S转变。
染色质重塑复合物(CRCs)参与少突胶质细胞(OL)的分化、生存和维持。我们询问crc是否也控制OL前体(OPs)的增殖,重点关注INO80复合物,已知INO80复合物在发育和疾病期间调节多种其他细胞类型的增殖。体外CRISPR/ cas9介导的Ino80失活,或体内cre介导的缺失,通过延长G1期,显著减缓了OP细胞周期。RNAseq分析显示,在ino80缺陷小鼠的OPs中,E2F靶基因表达异常,但相关RNAseq和ATAC-seq分析显示,基因表达与转录起始位点核小体定位改变之间没有普遍相关性。荧光光漂白实验表明,组蛋白H2A。在INO80缺失后,Z迁移率增加,表明INO80通过H2A调控OPs的细胞周期机制。Z / H2A交换。我们还提供了INO80与OLIG2相关的证据,OLIG2是OL发展的主要调节因子。
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来源期刊
Glia
Glia 医学-神经科学
CiteScore
13.10
自引率
4.80%
发文量
162
审稿时长
3-8 weeks
期刊介绍: GLIA is a peer-reviewed journal, which publishes articles dealing with all aspects of glial structure and function. This includes all aspects of glial cell biology in health and disease.
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