S100PBP interacts with nucleoporin TPR and facilitates XY crossover formation in mice.

IF 6.5 1区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

EMBO Reports Pub Date : 2025-05-01 Epub Date: 2025-04-09 DOI:10.1038/s44319-025-00391-y

Yufan Wu, Yang Li, Huan Zhang, Jingwei Ye, Ming Li, Jianteng Zhou, Xuefeng Xie, Hao Yin, Min Chen, Gang Yang, Suixing Fan, Baolu Shi, Hanwei Jiang, Qinghua Shi, Hui Ma

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引用次数: 0

Abstract

During meiosis, at least one crossover is selectively generated per pair of homologous chromosomes through homologous recombination to ensure their faithful segregation. The molecular mechanisms controlling meiotic recombination, particularly in XY chromosomes that share a tiny region of homology (i.e., the pseudoautosomal region, PAR), remain poorly understood. Here, we identify S100PBP as a key modulator of both XY and autosomal recombination in mice. S100pbp-knockout mice exhibit male infertility and spermatogenesis arrest at meiotic metaphase I, resulting from a drastic reduction in XY crossovers. This failure in XY crossover formation is due to a reduction in TEX11/M1AP-bound recombination intermediates at the PAR. By contrast, disruption of S100PBP significantly increases the number of recombination intermediates and crossovers on autosomes. Co-immunoprecipitation mass spectrometry revealed that S100PBP interacts with the nucleoporin TPR. Furthermore, S100PBP is localized specifically to the nuclear pores of meiocytes, likely in a TPR-dependent manner. These findings demonstrate that S100PBP promotes XY crossover formation while limiting excess autosomal crossovers and shed light on the potential role of nuclear pores in regulating meiotic recombination.

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S100PBP与核孔蛋白TPR相互作用，促进小鼠XY交叉形成。

在减数分裂过程中，每对同源染色体通过同源重组至少选择性地产生一次交叉，以确保其忠实分离。控制减数分裂重组的分子机制，特别是在共享一个微小同源区域（即假常染色体区域，PAR）的XY染色体中，仍然知之甚少。在这里，我们发现S100PBP是小鼠XY和常染色体重组的关键调节剂。s100pbp敲除小鼠在减数分裂中期I表现出雄性不育和精子发生停止，这是由于XY交叉的急剧减少。XY交叉形成的失败是由于PAR上TEX11/ m1ap结合的重组中间体的减少。相比之下，S100PBP的破坏显著增加了常染色体上重组中间体和交叉的数量。免疫共沉淀质谱分析显示S100PBP与核孔蛋白TPR相互作用。此外，S100PBP特异性定位于减数细胞的核孔，可能以tpr依赖的方式存在。这些发现表明，S100PBP促进XY交叉形成，同时限制过多的常染色体交叉，并揭示了核孔在调节减数分裂重组中的潜在作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

EMBO Reports 生物-生化与分子生物学

CiteScore

11.20

自引率

1.30%

发文量

267

审稿时长

1 months

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