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利用 III 型分泌系统传递抗原的减毒活沙门氏菌结核分枝杆菌疫苗。

Live attenuated Salmonella vaccines against Mycobacterium tuberculosis with antigen delivery via the type III secretion system.

机构信息

Center for Infectious Diseases and Vaccinology at Biodesign Institute, Arizona State University, Tempe, Arizona, USA.

出版信息

Infect Immun. 2012 Feb;80(2):798-814. doi: 10.1128/IAI.05525-11. Epub 2011 Dec 5.

Abstract

Tuberculosis remains a global health threat, and there is dire need to develop a vaccine that is safe and efficacious and confers long-lasting protection. In this study, we constructed recombinant attenuated Salmonella vaccine (RASV) strains with plasmids expressing fusion proteins consisting of the 80 amino-terminal amino acids of the type 3 secretion system effector SopE of Salmonella and the Mycobacterium tuberculosis antigens early secreted antigenic target 6-kDa (ESAT-6) protein and culture filtrate protein 10 (CFP-10). We demonstrated that the SopE-mycobacterial antigen fusion proteins were translocated into the cytoplasm of INT-407 cells in cell culture assays. Oral immunization of mice with RASV strains synthesizing SopE-ESAT-6-CFP-10 fusion proteins resulted in significant protection of the mice against aerosol challenge with M. tuberculosis H37Rv that was similar to the protection afforded by immunization with Mycobacterium bovis bacillus Calmette-Guérin (BCG) administered subcutaneously. In addition, oral immunization with the RASV strains specifying these mycobacterial antigens elicited production of significant antibody titers to ESAT-6 and production of ESAT-6- or CFP-10-specific gamma interferon (IFN-γ)-secreting and tumor necrosis factor alpha (TNF-α)-secreting splenocytes.

摘要

结核病仍然是全球健康威胁,因此迫切需要开发一种安全、有效、能提供长期保护的疫苗。在这项研究中,我们构建了表达融合蛋白的重组减毒沙门氏菌疫苗(RASV)菌株,融合蛋白由沙门氏菌 III 型分泌系统效应物 SopE 的 80 个 N 端氨基酸与结核分枝杆菌抗原早期分泌抗原靶 6-kDa(ESAT-6)蛋白和培养滤液蛋白 10(CFP-10)组成。我们证明,在细胞培养试验中,SopE-分枝杆菌抗原融合蛋白被转运到 INT-407 细胞的细胞质中。用合成 SopE-ESAT-6-CFP-10 融合蛋白的 RASV 菌株对小鼠进行口服免疫,可显著保护小鼠免受雾化感染 H37Rv 结核分枝杆菌的攻击,其保护效果与皮下接种牛分枝杆菌卡介苗(BCG)相似。此外,用这些分枝杆菌抗原特异性 RASV 菌株进行口服免疫可诱导产生针对 ESAT-6 的显著抗体滴度,并诱导产生 ESAT-6 或 CFP-10 特异性γ干扰素(IFN-γ)分泌和肿瘤坏死因子α(TNF-α)分泌的脾细胞。

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