DSS1 和单链 DNA 调节 BRCA2 的寡聚化。

DSS1 and ssDNA regulate oligomerization of BRCA2.

机构信息

Department of Microbiology and Molecular Genetics, University of California, Davis, Davis, CA 95616-8665, USA.

Department of Molecular and Cellular Biology, University of California, Davis, Davis, CA 95616-8665, USA.

出版信息

Nucleic Acids Res. 2020 Aug 20;48(14):7818-7833. doi: 10.1093/nar/gkaa555.

Abstract

The tumor suppressor BRCA2 plays a key role in initiating homologous recombination by facilitating RAD51 filament formation on single-stranded DNA. The small acidic protein DSS1 is a crucial partner to BRCA2 in this process. In vitro and in cells (1,2), BRCA2 associates into oligomeric complexes besides also existing as monomers. A dimeric structure was further characterized by electron microscopic analysis (3), but the functional significance of the different BRCA2 assemblies remains to be determined. Here, we used biochemistry and electron microscopic imaging to demonstrate that the multimerization of BRCA2 is counteracted by DSS1 and ssDNA. When validating the findings, we identified three self-interacting regions and two types of self-association, the N-to-C terminal and the N-to-N terminal interactions. The N-to-C terminal self-interaction of BRCA2 is sensitive to DSS1 and ssDNA. The N-to-N terminal self-interaction is modulated by ssDNA. Our results define a novel role of DSS1 to regulate BRCA2 in an RPA-independent fashion. Since DSS1 is required for BRCA2 function in recombination, we speculate that the monomeric and oligomeric forms of BRCA2 might be active for different cellular events in recombinational DNA repair and replication fork stabilization.

摘要

抑癌蛋白 BRCA2 通过促进 RAD51 细丝在单链 DNA 上的形成,在启动同源重组中发挥关键作用。酸性小蛋白 DSS1 是 BRCA2 在这个过程中的关键伙伴。在体外和细胞中(1,2),BRCA2 除了以单体形式存在外,还会形成寡聚复合物。电子显微镜分析进一步表征了二聚体结构(3),但不同 BRCA2 组装体的功能意义仍有待确定。在这里,我们使用生物化学和电子显微镜成像来证明 DSS1 和 ssDNA 会拮抗 BRCA2 的多聚化。在验证这些发现时,我们确定了三个自我相互作用区域和两种类型的自我缔合,即 N 端到 C 端和 N 端到 N 端相互作用。BRCA2 的 N 端到 C 端的自我相互作用对 DSS1 和 ssDNA 敏感。ssDNA 调节 BRCA2 的 N 端到 N 端自我相互作用。我们的结果定义了 DSS1 以非 RPA 依赖的方式调节 BRCA2 的新作用。由于 DSS1 是 BRCA2 在重组中发挥功能所必需的,我们推测 BRCA2 的单体和寡聚形式可能在重组 DNA 修复和复制叉稳定化的不同细胞事件中具有活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0645/7641332/a16033b5fe91/gkaa555fig1.jpg

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