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Effects of bfp Mutations on Biogenesis of Functional Enteropathogenic Escherichia coli Type IV Pili

机译:bfp突变对功能性肠病性大肠杆菌IV型菌毛的生物发生的影响

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摘要

Enteropathogenic Escherichia coli expresses a type IV fimbria known as the bundle-forming pilus (BFP) that is required for autoaggregation and localized adherence (LA) to host cells. A cluster of 14 genes is sufficient to reconstitute BFP biogenesis in a laboratory strain of E. coli. We have undertaken a systematic mutagenesis of the individual genes to determine the effect of each mutation on BFP biogenesis and LA. Here we report the construction and analysis of nonpolar mutations in six genes of the bfp cluster, bfpG, bfpB, bfpC, bfpD, bfpP, and bfpH, as well as the further analysis of a previously described bfpA mutant strain that is unable to express bundlin, the pilin protein. We found that mutations in bfpB, which encodes an outer membrane protein; bfpD, which encodes a putative nucleotide-binding protein; and bfpG and bfpC, which do not have sequence homologues in other type IV pilus systems, do not affect prebundlin expression or processing but block both BFP biogenesis and LA. The mutation in bfpP, the prepilin peptidase gene, does not affect prebundlin expression but blocks signal sequence cleavage of prebundlin, BFP biogenesis, and LA. The mutation in bfpH, which is predicted to encode a lytic transglycosylase, has no effect on prebundlin expression, prebundlin processing, BFP biogenesis, or LA. For each mutant for which altered phenotypes were detected, complementation with a plasmid containing the corresponding wild-type allele restored the wild-type phenotypes. We also found that association of prebundlin or bundlin with sucrose density flotation gradient fractions containing both inner and outer membrane proteins does not require any accessory proteins. These studies indicate that many bfp gene products are required for biogenesis of functional type IV pili but that mutations in the individual genes do not lead to the identification of new phases of pilus assembly.
机译:肠致病性大肠杆菌表达被称为成束菌毛(BFP)的IV型菌毛,这是宿主细胞自动聚集和局部粘附(LA)所必需的。 14个基因的簇足以重构大肠杆菌实验室菌株中的BFP生物发生。我们对各个基因进行了系统诱变,以确定每种突变对BFP生物发生和LA的影响。在这里,我们报告了bfp簇,bfpG,bfpB,bfpC,bfpD,bfpP和bfpH的六个基因中非极性突变的构建和分析,以及对先前描述的无法表达Bundlin的bfpA突变菌株的进一步分析。 ,pilin蛋白。我们发现bfpB中的突变编码了一个外膜蛋白。 bfpD,其编码假定的核苷酸结合蛋白; bfpG和bfpC和bfpG和bfpC在其他IV型菌毛系统中没有序列同源物,它们不影响前邦德林的表达或加工,但会阻断BFP生物发生和LA。 bfpP中的突变,即前pilin肽酶基因,不会影响前邦德林的表达,但会阻止前邦德林的信号序列切割,BFP生物发生和LA。 bfpH中的突变预计可编码裂解转糖基化酶,但对前邦德林表达,前邦德林加工,BFP生物发生或LA均无影响。对于检测到改变的表型的每个突变体,用含有相应的野生型等位基因的质粒进行互补可以恢复野生型的表型。我们还发现,prebundlin或bundlin与包含内膜和外膜蛋白的蔗糖密度浮选梯度级分关联,不需要任何辅助蛋白。这些研究表明功能性IV型菌毛的生物发生需要许多 bfp 基因产物,但是单个基因中的突变不会导致菌毛组装新阶段的鉴定。

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