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首页> 外文期刊>Infection and immunity >Unusual Genetic Organization of a Functional Type I Protein Secretion System in Neisseria meningitidis
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Unusual Genetic Organization of a Functional Type I Protein Secretion System in Neisseria meningitidis

机译:脑膜炎奈瑟氏球菌的功能性I型蛋白质分泌系统的异常遗传组织

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Proteins secreted by Neisseria meningitidis are thought to play important roles in the pathogenesis of meningococcal disease. These proteins include the iron-repressible repeat-in-toxin (RTX) exoprotein FrpC. Related proteins in other pathogens are secreted via a type I secretion system (TOSS), but such a system has not been demonstrated in N. meningitidis. An in silico search of the group B meningococcal genome suggested the presence of a uniquely organized TOSS. Genes encoding homologs of the Escherichia coli HlyB (ATP-binding), HlyD (membrane fusion), and TolC (outer membrane channel) proteins were identified. In contrast to the cistronic organization of the secretion genes in most other rtx operons, the hlyD and tolC genes were adjacent but unlinked to hlyB; neither locus was part of an operon containing genes encoding putative TOSS substrates. Both loci were flanked by genes normally associated with mobile genetic elements. The three genes were shown to be expressed independently. Mutation at either locus resulted in an inability to secrete FrpC and a related protein, here called FrpC2. Successful complementation of these mutations at an ectopic site confirmed the observed phenotypes were caused by loss of function of the putative TOSS genes. We show that genes scattered in the meningococcal genome encode a functional TOSS required for secretion of the meningococcal RTX proteins.
机译:脑膜炎奈瑟菌(Neisseria meningitidis)分泌的蛋白质被认为在脑膜炎球菌病的发病机理中起着重要作用。这些蛋白质包括铁抑制性重复毒素(RTX)外蛋白FrpC。其他病原体中的相关蛋白质是通过I型分泌系统(TOSS)分泌的,但在 N中尚未得到证明。脑膜炎。在计算机上对B组脑膜炎球菌基因组进行的计算机搜索表明存在独特组织的TOSS。鉴定了编码大肠杆菌 HlyB(ATP结合),HlyD(膜融合)和TolC(外膜通道)蛋白同源物的基因。与大多数其他 rtx 操纵子中分泌基因的顺反子组织相反, hlyD tolC 基因相邻但未与关联hlyB ;这两个基因座都不是包含编码推定的TOSS底物的基因的操纵子的一部分。两个基因座的侧翼通常是与流动遗传元件相关的基因。显示这三个基因是独立表达的。任一基因座处的突变均导致无法分泌FrpC和相关蛋白(此处称为FrpC2)。这些突变在异位点的成功互补证实了观察到的表型是由假定的TOSS基因功能丧失引起的。我们显示散布在脑膜炎球菌基因组中的基因编码为脑膜炎球菌RTX蛋白质的分泌所需的功能性TOSS。

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