首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Coevolution between nonhomologous but functionally similar proteins and their conserved partners in the Legionella pathogenesis system
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Coevolution between nonhomologous but functionally similar proteins and their conserved partners in the Legionella pathogenesis system

机译:军团菌发病机制中非同源但功能相似的蛋白质与其保守伴侣之间的共同进化

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Legionella pneumophila, the causative agent of Legionnaires' disease, and other pathogenic Legionella species multiply inside protozoa and human macrophages by using the intracellular multiplication (Icm)/defect in organelle trafficking (Dot) type-IV secretion system. The IcmQ protein, which possesses pore-forming activity, and IcmR, which regulates the IcmQ activity, are two essential components of this system. Analysis of the region expected to contain these two genes from 29 Legionella species revealed the presence of a conserved icmQ gene and a large hypervariable gene family [functional homologues of icmR (fir) genes], located at the icmR genomic position. Although hypervariable in their sequence, the fir genes from all 29 Legionella species were found, together with their corresponding icmQ genes, to function similarly during infection. In addition, all FIR proteins we examined were found to interact with their corresponding IcmQ proteins. Detailed bioinformatic, biochemical, and genetic analysis of the interaction between the variable FIR proteins and conserved IcmQ proteins revealed that their interaction depends on a variable region located between two conserved domains of IcmQ. This variable region was also found to be critical for IcmQ self-interaction, and the region probably coevolved with the corresponding FIR protein. A FIR-IcmQ pair was also found in Coxiella burnetii the only known non-Legionella bacterium that contains an Icm;Dot system, indicating the significance of this protein pair for the function of this type-IV secretion system. We hypothesize that this gene variation, which is probably mediated by positive selection, plays an important role in the evolutionary arms race between the protozoan host cell and the pathogen.
机译:军团菌病的病原体肺炎军团菌和其他致病性军团菌通过在细胞器运输(Dot)IV型分泌系统中使用细胞内增殖(Icm)/缺陷在原生动物和人类巨噬细胞内繁殖。具有成孔活性的IcmQ蛋白和调节IcmQ活性的IcmR是该系统的两个基本组成部分。对预计包含29个军团菌物种的这两个基因的区域的分析显示,存在一个保守的icmQ基因和一个大的高变基因家族[icmR(fir)基因的功能同源物],位于icmR基因组位置。尽管其序列高变,但发现了来自所有29个军团菌种的fir基因,以及它们相应的icmQ基因,在感染过程中的功能相似。此外,发现我们检查的所有FIR蛋白均与其相应的IcmQ蛋白相互作用。详细的生物信息学,生化和遗传分析的可变FIR蛋白和保守的IcmQ蛋白之间的相互作用表明,它们的相互作用取决于位于IcmQ的两个保守域之间的可变区。还发现此可变区对于IcmQ自相互作用至关重要,该区可能与相应的FIR蛋白共同进化。 FIR-IcmQ对还发现于伯氏柯氏杆菌中,是唯一已知的包含Icm; Dot系统的非军团杆菌,这表明该蛋白对对该IV型分泌系统的功能具有重要意义。我们假设这种基因变异可能由正选择介导,在原生动物宿主细胞和病原体之间的进化军备竞赛中起着重要作用。

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