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Characterization of the Filamentous Hemagglutinin-Like Protein FhaS in Bordetella bronchiseptica

机译:支气管败血博德特氏菌丝状血凝素样蛋白FhaS的表征

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摘要

Filamentous hemagglutinin (FHA) is a large (>200 kDa), rod-shaped protein expressed by bordetellae that is both surface-associated and secreted. FHA mediates bacterial adherence to epithelial cells and macrophages in vitro and is absolutely required for tracheal colonization in vivo. The recently sequenced Bordetella bronchiseptica genome revealed the presence of a gene, fhaS, that is nearly identical to fhaB, the FHA structural gene. We show that although fhaS expression requires the BvgAS virulence control system, it is maximal only under a subset of conditions in which BvgAS is active, suggesting an additional level of regulation. We also show that, like FHA, FhaS undergoes a C-terminal proteolytic processing event and is both surface-associated and secreted and that export across the outer membrane requires the channel-forming protein FhaC. Unlike FHA, however, FhaS was unable to mediate adherence of B. bronchiseptica to epithelial cell lines in vitro and was not required for respiratory tract colonization in vivo. In a coinfection experiment, a ΔfhaS strain was out-competed by wild-type B. bronchiseptica, indicating that fhaS is expressed in vivo and that FhaS contributes to bacterial fitness in a manner revealed when the mutant must compete with wild-type bacteria. These data suggest that FHA and FhaS perform distinct functions during the Bordetella infectious cycle. A survey of various Bordetella strains revealed two distinct fhaS alleles that segregate according to pathogen host range and that B. parapertussishu most likely acquired its fhaS allele from B. pertussis horizontally, suggesting fhaS may contribute to host-species specificity.
机译:丝状血凝素(FHA)是由bordetellae表达的大杆状蛋白(> 200 kDa),既与表面相关又被分泌。 FHA在体外介导细菌对上皮细胞和巨噬细胞的粘附,并且在体内气管定植是绝对必需的。最近测序的支气管败血博德特氏菌基因组揭示了基因fhaS的存在,该基因与fhaB(FHA结构基因)几乎相同。我们显示,尽管fhaS表达需要BvgAS毒力控制系统,但它仅在BvgAS活跃的条件子集中才最大,这表明需要额外的调节水平。我们还显示,像FHA一样,FhaS经历C端蛋白水解加工事件,并且与表面相关并被分泌,并且穿过外膜的出口需要通道形成蛋白FhaC。但是,与FHA不同,FhaS无法在体外介导支气管败血性博德特氏菌对上皮细胞系的粘附,并且在体内呼吸道定植不是必需的。在共同感染实验中,ΔfhaS菌株与野生型支气管败血性博德特氏菌竞争,表明fhaS在体内表达,并且当突变体必须与野生型细菌竞争时,FhaS有助于细菌适应性。这些数据表明FHA和FhaS在博德特氏菌感染周期中执行不同的功能。一项对各种博德特氏菌菌株的调查显示,两个不同的fhaS等位基因根据病原体宿主范围进行分离,而副百日咳博德特氏菌最有可能从百日咳博德特氏菌水平获取其fhaS等位基因,表明fhaS可能有助于宿主物种特异性。

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