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DraC 引发尿路致病性大肠杆菌 Dr(+)菌株菌毛生物发生。

The DraC usher in Dr fimbriae biogenesis of uropathogenic E. coli Dr(+) strains.

机构信息

Department of Microbiology, Gdańsk University of Technology, Poland.

出版信息

Arch Microbiol. 2010 May;192(5):351-63. doi: 10.1007/s00203-010-0564-x. Epub 2010 Mar 28.

Abstract

Biogenesis of Dr fimbriae encoded by the dra gene cluster of uropathogenic Escherichia coli strains requires the chaperone-usher pathway. This secretion system is based on two non-structural assembly components, the DraB periplasmic chaperone and DraC outer-membrane usher. The DraB controls the folding of DraE subunits, and DraC forms the assembly and secretion platform for polymerization of subunits in linear fibers. In this study, mutagenesis of the DraC N-terminus was undertaken to select residues critical for Dr fimbriae bioassembly. The DraC-F4A, DraC-C64, DraC-C100A and DraC-W142A significantly reduced the adhesive ability of E. coli strains. The biological activity of the DraC mutants as a assembly platform for Dr fimbriae polymerization was verified by agglutination of human erythrocytes and adhesion to DAF localized at the surface of CHO-DAF(+) and HeLa cells. The residue F4 of the DraC usher conserved among FGL and FGS chaperone-assembled adhesive organelles can be used to design pillicides blocking the biogenesis of Dr fimbriae. Because the draC and afaC-III genes share 100% identity the range of the virulence determinant inhibitors could also be extended to E. coli strains encoding afa-3 gene cluster. The investigations performed showed that the usher N-terminus plays an important role in biogenesis of complete fiber.

摘要

由尿路致病性大肠埃希菌菌株的 dra 基因簇编码的 Dr 菌毛的生物发生需要伴侣蛋白-usher 途径。这个分泌系统基于两个非结构组装成分,即 DraB 周质伴侣和 DraC 外膜 usher。DraB 控制 DraE 亚基的折叠,而 DraC 形成用于亚基在线性纤维中聚合的组装和分泌平台。在这项研究中,对 DraC N 端进行了诱变,以选择对 Dr 菌毛生物组装至关重要的残基。DraC-F4A、DraC-C64、DraC-C100A 和 DraC-W142A 显著降低了大肠埃希菌菌株的粘附能力。DraC 突变体作为 Dr 菌毛聚合组装的组装平台的生物学活性通过人红细胞的凝集和对定位于 CHO-DAF(+)和 HeLa 细胞表面的 DAF 的粘附来验证。在 FGL 和 FGS 伴侣组装的粘附细胞器中保守的 DraC usher 上的残基 F4 可用于设计抑制 Dr 菌毛生物发生的 pillicides。由于 draC 和 afaC-III 基因具有 100%的同一性,因此可以将毒力决定因子抑制剂的范围扩展到编码 afa-3 基因簇的大肠埃希菌菌株。进行的研究表明,usher N 端在完整纤维的生物发生中起着重要作用。

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