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Autodisplay Efficacious Surface Exposure of Antigenic UreA Fragments from Helicobacter pylori in Salmonella Vaccine Strains

机译:沙门氏菌疫苗株中幽门螺杆菌抗原UreA片段的自动展示有效表面暴露。

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Live attenuated Salmonella strains expressing antigens of pathogens are promising oral vaccine candidates. There is growing evidence that the topology of expression of the foreign antigens can have a dramatic impact on the immunogenicity. We examined the potential of the AIDA-I (Escherichia coli adhesin involved in diffuse adherence) autotransporter domain to display antigenic fragments of the urease A subunit of Helicobacter pylori for the induction of a protective immune response. In the murine H. pylori model, protection is mainly mediated by CD4+ T cells, and we therefore used the AIDA-I expression system to successfully express both nearly full-length UreA and defined T-helper-cell epitopes on the surface of an attenuated Salmonella enterica serovar Typhimurium vaccine strain. Surface exposure of the large UreA fragment or of one UreA T-cell epitope mediated a significant reduction in the level of H. pylori in immunized mice after challenge infection, whereas conventional cytoplasmic expression of UreA in Salmonella had no effect. These results support the concept that surface display increases the immunogenicity of recombinant antigens expressed on oral live vaccine carriers and further demonstrate the feasibility of immunizing against H. pylori with Salmonella vaccine strains expressing CD4+ T-cell epitopes.
机译:表达病原体抗原的减毒活沙门氏菌菌株是很有希望的口服疫苗候选物。越来越多的证据表明,外源抗原的表达拓扑可对免疫原性产生巨大影响。我们检查了AIDA-I(参与弥漫性粘附的大肠杆菌粘附素)自转运蛋白结构域展示 Helicobacter pylori 的脲酶A亚基抗原片段的诱导SNP的潜力。保护性免疫反应。在鼠类中,H。 pylori 模型,保护作用主要由CD4 + T细胞介导,因此我们使用AIDA-I表达系统成功表达了近乎全长的UreA和定义的T-helper细胞肠沙门氏菌减毒鼠伤寒疫苗株表面上的抗原决定簇。大的UreA片段或一个UreA T细胞表位的表面暴露介导了 H水平的显着降低。感染后免疫的小鼠体内出现幽门螺杆菌,而沙门氏菌中UreA的常规细胞质表达没有作用。这些结果支持这样的概念,即表面展示增加了在口服活疫苗载体上表达的重组抗原的免疫原性,并进一步证明了针对 H进行免疫的可行性。 pylori 与表达CD4 + T细胞表位的沙门氏菌疫苗株。

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