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Autodisplay: Development of an Efficacious System for Surface Display of Antigenic Determinants in Salmonella Vaccine Strains

机译:自动显示:沙门氏菌疫苗株中的抗原决定簇表面展示的有效系统的开发。

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To optimize antigen delivery by Salmonella vaccine strains, a system for surface display of antigenic determinants was established by using the autotransporter secretion pathway of gram-negative bacteria. A modular system for surface display allowed effective targeting of heterologous antigens or fragments thereof to the bacterial surface by the autotransporter domain of AIDA-I, the Escherichia coli adhesin involved in diffuse adherence. A major histocompatibility complex class II-restricted epitope, comprising amino acids 74 to 86 of the Yersinia enterocolitica heat shock protein Hsp60 (Hsp6074-86), was fused to the AIDA-I autotransporter domain, and the resulting fusion protein was expressed at high levels on the cell surface of E. coli and Salmonella enterica serovar Typhimurium. Colonization studies in mice vaccinated with Salmonella strains expressing AIDA-I fusion proteins demonstrated high genetic stability of the generated vaccine strain in vivo. Furthermore, a pronounced T-cell response against Yersinia Hsp6074-86 was induced in mice vaccinated with a Salmonella vaccine strain expressing the Hsp6074-86-AIDA-I fusion protein. This was shown by monitoring Yersinia Hsp60-stimulated IFN-γ secretion and proliferation of splenic T cells isolated from vaccinated mice. These results demonstrate that the surface display of antigenic determinants by the autotransporter pathway deserves special attention regarding the application in live attenuated Salmonella vaccine strains.
机译:为了优化沙门氏菌疫苗株的抗原传递,利用革兰氏阴性细菌的自转运蛋白分泌途径建立了抗原决定簇表面展示系统。用于表面展示的模块化系统允许通过AIDA-1的自转运域(参与弥漫性粘附的大肠杆菌粘附素)将异源抗原或其片段有效靶向细菌表面。将主要的组织相容性复合物II类限制性表位与AIDA融合,该表位包含小肠结肠炎耶尔森氏菌热休克蛋白Hsp60(Hsp60 74-86 )的第74至86位氨基酸。 -I自转运蛋白结构域,并且得到的融合蛋白在 E的细胞表面上高水平表达。大肠杆菌和肠沙门氏菌血清型鼠伤寒。在接种表达AIDA-I融合蛋白的 Salmonella 株的小鼠中的定植研究表明,所产生的疫苗株在体内具有很高的遗传稳定性。此外,在接种了表达Hsp60 沙门氏菌疫苗株的小鼠中,诱导了针对耶尔森氏菌 Hsp60 74-86 的明显的T细胞应答。 > 74-86 -AIDA-1融合蛋白。通过监测耶尔森氏菌 Hsp60刺激的IFN-γ分泌和从接种小鼠中分离的脾T细胞的增殖可以证明这一点。这些结果表明通过自转运蛋白途径的抗原决定簇的表面展示在减毒活的沙门氏菌疫苗株中的应用值得特别关注。

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