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组蛋白变体H2A.W7抑制异染色质中的减数分裂交叉形成。

Histone variant H2A.W7 represses meiotic crossover formation in heterochromatin.

作者信息

Kuo Pallas, Tock Andrew J, Liu Xuexia, Topp Stephanie D, Zhong Zhenhui, Henderson Ian R, Lambing Christophe

机构信息

Department of Plant Sciences, Rothamsted Research, Harpenden AL5 2JQ, United Kingdom.

Department of Plant Sciences, University of Cambridge, Cambridge CB2 3EA, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2025 Jun 3;122(22):e2414166122. doi: 10.1073/pnas.2414166122. Epub 2025 May 29.

DOI:10.1073/pnas.2414166122
PMID:40440068
Abstract

In eukaryotic genomes, DNA is packaged into nucleosomes to form chromatin. The incorporation of canonical or variant histones into nucleosomes confers different properties and influences chromatin structure to regulate cellular processes, including recombination. During meiosis, DNA double-strand breaks (DSBs) are formed and repaired as interhomolog crossovers. Nucleosome occupancy is generally associated with low crossover frequency, but it remains unclear which histone variants are involved in this process. In , three variants of H2A coexist: H2A.X, H2A.Z, and H2A.W. Here, we show that H2A.W7 has a suppressive role on meiotic recombination. Genome-wide mapping of the crossover landscape revealed increased centromere-proximal recombination in . Moreover, H2A.W7 can be recruited to the crossover hotspot via 21-24-nucleotide siRNAs during RNA-directed DNA methylation, causing increased nucleosome occupancy and decreased crossover frequency. Cytological analysis reveals that H2A.W7 restricts heterochromatin clustering during meiosis, which can form a mechanism to limit interhomolog recombination. Conversely, the linker histone H1, of which its loading is known to be restricted by H2A.W, promotes heterochromatin clustering and crossover on a heterochromatic genetic interval. Our study reveals a role for H2A.W7 in repressing crossover formation in .

摘要

在真核生物基因组中,DNA被包装成核小体以形成染色质。将标准组蛋白或变体组蛋白纳入核小体赋予不同特性并影响染色质结构,从而调节包括重组在内的细胞过程。在减数分裂期间,DNA双链断裂(DSB)形成并作为同源染色体间交换进行修复。核小体占据通常与低交换频率相关,但尚不清楚哪些组蛋白变体参与此过程。在[具体物种名称未给出]中,H2A的三种变体共存:H2A.X、H2A.Z和H2A.W。在此,我们表明H2A.W7对减数分裂重组具有抑制作用。全基因组交换图谱显示[具体物种名称未给出]中着丝粒近端重组增加。此外,在RNA指导的DNA甲基化过程中,H2A.W7可通过21 - 24个核苷酸的小干扰RNA被招募到交换热点,导致核小体占据增加和交换频率降低。细胞学分析表明,H2A.W7在减数分裂期间限制异染色质聚集,这可能形成一种限制同源染色体间重组的机制。相反,已知其加载受H2A.W限制的连接组蛋白H1促进异染色质聚集以及在异染色质遗传区间的交换。我们的研究揭示了H2A.W7在[具体物种名称未给出]中抑制交换形成的作用。

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本文引用的文献

1
H1 restricts euchromatin-associated methylation pathways from heterochromatic encroachment.H1 限制了常染色质相关的甲基化途径,防止其被异染色质侵占。
Elife. 2024 May 30;12:RP89353. doi: 10.7554/eLife.89353.
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Structural variation and DNA methylation shape the centromere-proximal meiotic crossover landscape in Arabidopsis.结构变异和 DNA 甲基化塑造了拟南芥着丝粒近端减数分裂交叉的景观。
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Arabidopsis γ-H2A.X-INTERACTING PROTEIN participates in DNA damage response and safeguards chromatin stability.
拟南芥 γ-H2A.X 相互作用蛋白参与 DNA 损伤反应,保障染色质稳定性。
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CTAB DNA Extraction and Genotyping-by-Sequencing to Map Meiotic Crossovers in Plants.CTAB法提取DNA及测序基因分型以绘制植物减数分裂交叉图谱
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Diffusion-mediated HEI10 coarsening can explain meiotic crossover positioning in Arabidopsis.扩散介导的 HEI10 粗化可以解释拟南芥减数分裂交叉定位。
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The histone variant H2A.W and linker histone H1 co-regulate heterochromatin accessibility and DNA methylation.组蛋白变体 H2A.W 和连接组蛋白 H1 共同调节异染色质的可及性和 DNA 甲基化。
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A Synthetic Approach to Reconstruct the Evolutionary and Functional Innovations of the Plant Histone Variant H2A.W.一种重建植物组蛋白变体 H2A.W 的进化和功能创新的综合方法
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The Configuration of RPA, RAD51, and DMC1 Binding in Meiosis Reveals the Nature of Critical Recombination Intermediates.在减数分裂中 RPA、RAD51 和 DMC1 结合的构象揭示了关键重组中间体的本质。
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ASY1 acts as a dosage-dependent antagonist of telomere-led recombination and mediates crossover interference in .ASY1作为端粒引导的重组的剂量依赖性拮抗剂,并介导交叉干扰。 (注:原文句子不完整,翻译可能会稍显突兀,但严格按要求进行了翻译。)
Proc Natl Acad Sci U S A. 2020 Jun 16;117(24):13647-13658. doi: 10.1073/pnas.1921055117. Epub 2020 Jun 4.
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