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MEILB2-BRME1 在减数分裂重组中与 BRCA2 结合形成 V 形 DNA 夹。

MEILB2-BRME1 forms a V-shaped DNA clamp upon BRCA2-binding in meiotic recombination.

机构信息

Wellcome Centre for Cell Biology, Institute of Cell Biology, University of Edinburgh, Edinburgh, UK.

Department of Chemistry and Molecular Biology, University of Gothenburg, Gothenburg, Sweden.

出版信息

Nat Commun. 2024 Aug 2;15(1):6552. doi: 10.1038/s41467-024-50920-x.

Abstract

DNA double-strand break repair by homologous recombination has a specialised role in meiosis by generating crossovers that enable the formation of haploid germ cells. This requires meiosis-specific MEILB2-BRME1, which interacts with BRCA2 to facilitate loading of recombinases onto resected DNA ends. Here, we report the crystal structure of the MEILB2-BRME1 2:2 core complex, revealing a parallel four-helical assembly that recruits BRME1 to meiotic double-strand breaks in vivo. It forms an N-terminal β-cap that binds to DNA, and a MEILB2 coiled-coil that bridges to C-terminal ARM domains. Upon BRCA2-binding, MEILB2-BRME1 2:2 complexes dimerize into a V-shaped 2:4:4 complex, with rod-like MEILB2-BRME1 components arranged at right-angles. The β-caps located at the tips of the MEILB2-BRME1 limbs are separated by 25 nm, allowing them to bridge between DNA molecules. Thus, we propose that BRCA2 induces MEILB2-BRME1 to function as a DNA clamp, connecting resected DNA ends or homologous chromosomes to facilitate meiotic recombination.

摘要

同源重组介导的 DNA 双链断裂修复在减数分裂中具有特殊作用,通过产生交叉来促进单倍体生殖细胞的形成。这需要减数分裂特异性的 MEILB2-BRME1,它与 BRCA2 相互作用,促进重组酶加载到切除的 DNA 末端。在这里,我们报告了 MEILB2-BRME1 2:2 核心复合物的晶体结构,揭示了一种平行的四螺旋组装,将 BRME1 募集到体内减数分裂双链断裂。它形成一个结合 DNA 的 N 端 β-帽和一个桥接 C 端 ARM 结构域的 MEILB2 卷曲螺旋。在 BRCA2 结合后,MEILB2-BRME1 2:2 复合物二聚形成一个 V 形 2:4:4 复合物,棒状的 MEILB2-BRME1 组件呈直角排列。位于 MEILB2-BRME1 臂尖端的 β-帽之间的分离距离为 25nm,允许它们在 DNA 分子之间形成桥接。因此,我们提出 BRCA2 诱导 MEILB2-BRME1 作为 DNA 夹,连接切除的 DNA 末端或同源染色体,以促进减数分裂重组。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebda/11297322/0f7fecf7ba74/41467_2024_50920_Fig1_HTML.jpg

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