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乳球菌噬菌体 p2 的 ORF35-Sak3 是一种参与 DNA 重组和 AbiK 机制的 ATP 酶。

Lactococcal phage p2 ORF35-Sak3 is an ATPase involved in DNA recombination and AbiK mechanism.

机构信息

Architecture et Fonction des Macromolécules Biologiques, UMR 6098 CNRS and Universités d'Aix-Marseille I & II, Campus de Luminy, case 932, 13288 Marseille cedex 09, France.

出版信息

Mol Microbiol. 2011 Apr;80(1):102-16. doi: 10.1111/j.1365-2958.2011.07561.x. Epub 2011 Feb 15.

DOI:10.1111/j.1365-2958.2011.07561.x
PMID:21276096
Abstract

Virulent phages of the Siphoviridae family are responsible for milk fermentation failures worldwide. Here, we report the characterization of the product of the early expressed gene orf35 from Lactococcus lactis phage p2 (936 group). ORF35(p2), also named Sak3, is involved in the sensitivity of phage p2 to the antiviral abortive infection mechanism AbiK. The localization of its gene upstream of a gene coding for a single-strand binding protein as well as its membership to a superfamily of single-strand annealing proteins (SSAPs) suggested a possible role in homologous recombination. Electron microscopy showed that purified ORF35(p2) form a hexameric ring-like structure that is often found in proteins with a conserved RecA nucleotide-binding core. Gel shift assays and surface plasmon resonance data demonstrated that ORF35(p2) interacts preferentially with single-stranded DNA with nanomolar affinity. Atomic force microscopy showed also that it preferentially binds to sticky DNA substrates over blunt ends. In addition, in vitro assays demonstrated that ORF35(p2) is able to anneal complementary strands. Sak3 also stimulates Escherichia coli RecA-mediated homologous recombination. Remarkably, Sak3 was shown to possess an ATPase activity that is required for RecA stimulation. Collectively, our results demonstrate that ORF35(p2) is a novel SSAP stimulating homologous recombination.

摘要

噬菌体型 Siphoviridae 家族的烈性噬菌体是导致全球牛奶发酵失败的原因。在这里,我们报告了乳球菌噬菌体 p2(936 组)早期表达基因 orf35 的产物的特征。ORF35(p2),也称为 Sak3,参与了噬菌体 p2 对抗病毒性流产感染机制 AbiK 的敏感性。其基因位于编码单链结合蛋白的基因上游的定位以及其属于单链退火蛋白(SSAP)超家族表明其可能在同源重组中发挥作用。电子显微镜显示,纯化的 ORF35(p2) 形成六聚体环状结构,这种结构在具有保守 RecA 核苷酸结合核心的蛋白质中经常发现。凝胶迁移分析和表面等离子体共振数据表明,ORF35(p2) 优先与具有纳摩尔亲和力的单链 DNA 相互作用。原子力显微镜还表明,它优先结合粘性 DNA 底物而不是钝端。此外,体外实验表明,ORF35(p2) 能够使互补链退火。Sak3 还能刺激大肠杆菌 RecA 介导的同源重组。值得注意的是,Sak3 被证明具有激活 RecA 所需的 ATP 酶活性。总的来说,我们的结果表明 ORF35(p2) 是一种新型的 SSAP,可刺激同源重组。

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