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The putative lytic transglycosylase VirB1 from Brucella suis interacts with the type IV secretion system core components VirB8, VirB9 and VirB11

机译:来自Brucella suis的推定的裂解型转基质血糖酶Virb1与IV型分泌系统核心组件VIRB8,VIRB9和VIRB11相互作用

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VirB1-like proteins are believed to act as lytic transglycosylases, which facilitate the assembly of type IV secretion systems via localized lysis of the peptidoglycan. This paper presents the biochemical analysis of interactions of purified Brucella suis VirB1 with core components of the type IV secretion system. Genes encoding VirB1, VirB8, VirB9, VirB10 and VirB11 were cloned into expression vectors; the affinity-tagged proteins were purified from Escherichia coli, and analyses by gel filtration chromatography showed that they form monomers or homo-multimers. Analysis of protein–protein interactions by affinity precipitation revealed that VirB1 bound to VirB9 and VirB11. The results of bicistron expression experiments followed by gel filtration further supported the VirB1–VirB9 interaction. Peptide array mapping identified regions of VirB1 that interact with VirB8, VirB9 and VirB11 and underscored the importance of the C-terminus, especially for the VirB1–VirB9 interaction. The binding sites were localized on a structure model of VirB1, suggesting that different portions of VirB1 may interact with other VirB proteins during assembly of the type IV secretion machinery.
机译:据信virb1样蛋白是充当裂解的转基质胶酶,其通过肽聚糖的局部裂解促进IV型分泌系统的组装。本文介绍了纯化的Brucella suisVerb1与IV型分泌系统核心组分的生物化学分析。编码virb1,virb8,virb9,virb10和virb11的基因被克隆到表达载体中;从大肠杆菌中纯化亲和标记的蛋白质,并通过凝胶过滤色谱分析显示它们形成单体或同源多数。亲和沉淀的蛋白质 - 蛋白质相互作用揭示了virb1与virb9和virb11结合。双铸龙表达实验的结果,然后进一步支持凝胶过滤的相互作用。肽阵列映射确定了与virb8,virb9和virb11相互作用的virb1的区域,并强调了C-terminus的重要性,特别是对于VIRB1-VIRB9相互作用。将结合位点定位在VIRB1的结构模型上,表明在IV型分泌机械组装期间,vIRB1的不同部分可以与其他病毒蛋白相互作用。

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