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对裂殖酵母以及Dmc1和Rad51重组酶的小鼠Hop2-Mnd1的刺激。

Stimulation of fission yeast and mouse Hop2-Mnd1 of the Dmc1 and Rad51 recombinases.

作者信息

Ploquin Mickaël, Petukhova Galina V, Morneau Dany, Déry Ugo, Bransi Ali, Stasiak Andrzej, Camerini-Otero R Daniel, Masson Jean-Yves

机构信息

Genome Stability Laboratory, Laval University Cancer Research Center, Hôtel-Dieu de Québec, 9 McMahon, Quebec city, QC, Canada G1R 2J6.

出版信息

Nucleic Acids Res. 2007;35(8):2719-33. doi: 10.1093/nar/gkm174. Epub 2007 Apr 10.

Abstract

Genetic analysis of fission yeast suggests a role for the spHop2-Mnd1 proteins in the Rad51 and Dmc1-dependent meiotic recombination pathways. In order to gain biochemical insights into this process, we purified Schizosaccharomyces pombe Hop2-Mnd1 to homogeneity. spHop2 and spMnd1 interact by co-immunoprecipitation and two-hybrid analysis. Electron microscopy reveals that S. pombe Hop2-Mnd1 binds single-strand DNA ends of 3'-tailed DNA. Interestingly, spHop2-Mnd1 promotes the renaturation of complementary single-strand DNA and catalyses strand exchange reactions with short oligonucleotides. Importantly, we show that spHop2-Mnd1 stimulates spDmc1-dependent strand exchange and strand invasion. Ca(2+) alleviate the requirement for the order of addition of the proteins on DNA. We also demonstrate that while spHop2-Mnd1 affects spDmc1 specifically, mHop2 or mHop2-Mnd1 stimulates both the hRad51 and hDmc1 recombinases in strand exchange assays. Thus, our results suggest a crucial role for S. pombe and mouse Hop2-Mnd1 in homologous pairing and strand exchange and reveal evolutionary divergence in their specificity for the Dmc1 and Rad51 recombinases.

摘要

裂殖酵母的遗传分析表明,spHop2-Mnd1蛋白在依赖Rad51和Dmc1的减数分裂重组途径中发挥作用。为了从生化角度深入了解这一过程,我们将粟酒裂殖酵母Hop2-Mnd1纯化至同质状态。通过免疫共沉淀和双杂交分析发现,spHop2和spMnd1相互作用。电子显微镜显示,粟酒裂殖酵母Hop2-Mnd1可结合3'端带尾DNA的单链DNA末端。有趣的是,spHop2-Mnd1能促进互补单链DNA的复性,并催化与短寡核苷酸的链交换反应。重要的是,我们发现spHop2-Mnd1能刺激spDmc1依赖的链交换和链入侵。Ca(2+)可减轻对DNA上蛋白质添加顺序的要求。我们还证明,虽然spHop2-Mnd1对spDmc1有特异性影响,但在链交换实验中,mHop2或mHop2-Mnd1能刺激hRad51和hDmc1重组酶。因此,我们的结果表明粟酒裂殖酵母和小鼠Hop2-Mnd1在同源配对和链交换中起关键作用,并揭示了它们对Dmc1和Rad51重组酶特异性的进化差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5df6/1885673/2e73b7d428f0/gkm174f1.jpg

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