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Analysis of cohesin-dockerin interactions using mutant dockerin proteins

机译:使用突变的dockerin蛋白分析cohesin-dockerin相互作用

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Clostridial cellulosomes are cellulolytic complexes that are formed by highly specific interactions between one of the repeated cohesin modules present in the scaffolding protein and a dockerin module of the catalytic components. Although Clostridium thermocellum Xyn11A dockerin has a typical C. thermocellum dockerin sequence, in which two amino acid residues are species specifically conserved within the two segments of the dockerin modules, it can recognize Clostridium josui cohesin modules in a non-species-specific manner. The importance of these two conserved amino acids, which are part of the recognition site of the cohesin and dockerin interaction, was investigated by introducing mutations into the first and/or the second segments of the Xyn11A dockerin. Mutations in the first segment did not affect the interactions between dockerin and C. thermocellum and C. josui cohesins. However, mutations in the second segment prevented binding to cohesin proteins. A second round of mutations within the first segment re-established the affinity for both the C. thermocellum and the C. josui cohesins. However, this was not observed for a 'conventional' dockerin, Xyn10C. These results suggest that the combination of the first and second dockerin segments is important for the target recognition.
机译:梭菌纤维素体是纤维素分解复合物,它是由存在于支架蛋白中的重复黏附素模块之一与催化成分的码头蛋白模块之间的高度特异性相互作用形成的。尽管热纤梭菌Xyn11A dockerin具有典型的热纤梭菌dockerin序列,其中两个氨基酸残基是在dockerin模块的两个片段内特异性保守的物种,但它可以以非物种特异性的方式识别约氏梭菌黏附素模块。通过将突变引入Xyn11A dockerin的第一个和/或第二个片段,研究了这两个保守氨基酸的重要性,它们是黏着蛋白和dockerin相互作用的识别位点的一部分。第一段中的突变不会影响dockerin与C.thermocellum和C.josui黏蛋白之间的相互作用。然而,第二节段中的突变阻止了与粘着蛋白的结合。第一段内的第二轮突变重新建立了对热纤梭菌和约瑟梭菌粘着素的亲和力。但是,对于“常规” dockerin Xyn10C,未观察到此情况。这些结果表明,第一个和第二个dockerin片段的组合对于目标识别很重要。

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