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首页> 外文期刊>Biochemical and Biophysical Research Communications >In vitro polymerization of Mycobacterium leprae FtsZ OR Mycobacterium tuberculosis FtsZ is revived or abolished, respectively, by reciprocal mutation of a single residue.
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In vitro polymerization of Mycobacterium leprae FtsZ OR Mycobacterium tuberculosis FtsZ is revived or abolished, respectively, by reciprocal mutation of a single residue.

机译:麻风分枝杆菌FtsZ或结核分枝杆菌FtsZ的体外聚合反应是通过单个残基的相互突变而分别复活或废除的。

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摘要

A single residue that dramatically influences polymerization of principal cell division protein FtsZ of Mycobacterium leprae (MlFtsZ) and Mycobacterium tuberculosis (MtFtsZ) has been identified. Soluble, recombinant MlFtsZ did not show polymerization in vitro, in contrast to MtFtsZ, which polymerised. Mutation of the lone non-conserved residue T172 in the N-terminal domain of MlFtsZ to A172, as it exists in MtFtsZ, showed dramatic polymerization of MlFtsZ-T172A in vitro. Reciprocal mutation of A172 in MtFtsZ to T172, as it exists in MlFtsZ, abolished polymerization of MtFtsZ-A172T in vitro. While T172A mutation enhanced weak GTPase activity of MlFtsZ, reciprocal A172T mutation marginally reduced GTPase activity of MtFtsZ in vitro. These observations demonstrate that the residue at position 172 plays critical role in the polymerization of MlFtsZ and MtFtsZ. A possible evolutionary correlation between the presence of polymerization-adversive or polymerization-favouring residue at position 172 in FtsZ andgeneration time of the respective bacterium are discussed.
机译:已鉴定出一个残基,该残基显着影响麻风分枝杆菌(MlFtsZ)和结核分枝杆菌(MtFtsZ)的主要细胞分裂蛋白FtsZ的聚合。与聚合的MtFtsZ相比,可溶性重组MlFtsZ在体外未显示聚合。 MlFtsZ的N末端结构域中孤立的非保守残基T172突变为A172(存在于MtFtsZ中)显示了MlFtsZ-T172A在体外的剧烈聚合。 MtFtsZ中的A172相互突变为MlFtsZ中的T172,从而消除了MtFtsZ-A172T的体外聚合反应。尽管T172A突变增强了MlFtsZ的弱GTPase活性,但相反的A172T突变在体外却微弱地降低了MtFtsZ的GTPase活性。这些观察表明,在172位的残基在MlFtsZ和MtFtsZ的聚合中起关键作用。讨论了在FtsZ位置172上存在不利于聚合反应或不利于聚合反应的残基与相应细菌的生成时间之间可能的进化相关性。

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