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霍乱弧菌上幽门螺杆菌HpaA黏附抗原的表面表达,通过共表达产肠毒素大肠杆菌菌毛抗原来增强。

Surface expression of Helicobacter pylori HpaA adhesion antigen on Vibrio cholerae, enhanced by co-expressed enterotoxigenic Escherichia coli fimbrial antigens.

作者信息

Tobias Joshua, Lebens Michael, Wai Sun Nyunt, Holmgren Jan, Svennerholm Ann-Mari

机构信息

Department of Microbiology and Immunology, Institute of Biomedicine, University of Gothenburg Vaccine Research Institute (GUVAX), University of Gothenburg, S-40530 Göteborg, Sweden.

Department of Microbiology and Immunology, Institute of Biomedicine, University of Gothenburg Vaccine Research Institute (GUVAX), University of Gothenburg, S-40530 Göteborg, Sweden.

出版信息

Microb Pathog. 2017 Apr;105:177-184. doi: 10.1016/j.micpath.2017.02.021. Epub 2017 Feb 17.

Abstract

Helicobacter pylori infection can cause peptic ulceration and is associated with gastric adenocarcinoma. This study aimed to construct and characterize a non-virulent Vibrio cholerae O1 strain, which grows more rapidly than H. pylori, as vector for H. pylori antigens for possible use as a vaccine strain against H. pylori. This was done by recombinant expression of the H. pylori adhesion antigen HpaA alone or, as a proof of principle, together with different colonization factor (CF) antigens of enterotoxigenic Escherichia coli (ETEC) which may enhance immune responses against HpaA. A recombinant V. cholerae strain co-expressing HpaA and a fimbrial CF antigens CFA/I or CS5, but not the non-fimbrial CF protein CS6, was shown to express larger amounts of HpaA on the surface when compared with the same V. cholerae strain expressing HpaA alone. Mutations in the CFA/I operon showed that the chaperon, possibly together with the usher, was involved in enhancing the surface expression of HpaA. Oral immunization of mice with formaldehyde-inactivated recombinant V. cholerae expressing HpaA alone or together with CFA/I induced significantly higher serum antibody responses against HpaA than mice similarly immunized with inactivated HpaA-expressing H. pylori bacteria. Our results demonstrate that a non-virulent V. cholerae strain can be engineered to allow strong surface expression of HpaA, and that the expression can be further increased by co-expressing it with ETEC fimbrial antigens. Such recombinant V. cholerae strains expressing HpaA, and possibly also other H. pylori antigens, may have the potential as oral inactivated vaccine candidates against H. pylori.

摘要

幽门螺杆菌感染可导致消化性溃疡,并与胃腺癌相关。本研究旨在构建并鉴定一种无毒的霍乱弧菌O1菌株,该菌株生长速度比幽门螺杆菌更快,作为幽门螺杆菌抗原的载体,有可能用作抗幽门螺杆菌的疫苗菌株。这是通过单独重组表达幽门螺杆菌黏附抗原HpaA,或者作为原理验证,与产肠毒素大肠杆菌(ETEC)的不同定植因子(CF)抗原一起表达来实现的,这些抗原可能增强针对HpaA的免疫反应。与单独表达HpaA的相同霍乱弧菌菌株相比,共表达HpaA和菌毛CF抗原CFA/I或CS5但不表达非菌毛CF蛋白CS6的重组霍乱弧菌菌株在表面表达了更多的HpaA。CFA/I操纵子中的突变表明,伴侣蛋白可能与外膜蛋白转运酶一起参与增强HpaA的表面表达。用甲醛灭活的单独表达HpaA或与CFA/I一起表达的重组霍乱弧菌口服免疫小鼠,诱导产生的针对HpaA的血清抗体反应明显高于用灭活的表达HpaA的幽门螺杆菌细菌进行类似免疫的小鼠。我们的结果表明,可以对无毒的霍乱弧菌菌株进行改造,使其在表面强力表达HpaA,并且通过与ETEC菌毛抗原共表达可以进一步增加其表达量。这种表达HpaA以及可能还表达其他幽门螺杆菌抗原的重组霍乱弧菌菌株,可能有潜力作为抗幽门螺杆菌的口服灭活疫苗候选物。

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