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表达HIV-1 gp120的鼠伤寒沙门氏菌疫苗载体的构建及免疫原性

Construction and immunogenicity of Salmonella typhimurium vaccine vectors that express HIV-1 gp120.

作者信息

Fouts T R, Tuskan R G, Chada S, Hone D M, Lewis G K

机构信息

Department of Geographic Medicine, School of Medicine, University of Maryland at Baltimore 21201, USA.

出版信息

Vaccine. 1995 Dec;13(17):1697-705. doi: 10.1016/0264-410x(95)00106-b.

DOI:10.1016/0264-410x(95)00106-b
PMID:8719522
Abstract

Since the human immunodeficiency virus (HIV-1) is transmitted either parenterally or sexually, both mucosal and systemic immune responses may be required to provide protective immunity. Attenuated Salmonella vectors expressing heterologous antigen can stimulate responses in both compartments. To evaluate the utility of Salmonella vectors as an HIV-1 vector vaccine, a gene expression cassette encoding recombinant HIV-1 gp120 (rgp120) was integrated into the hisOGD locus of Salmonella typhimurium aroA strain, SL3261 (SL3261::120). To test if increased antigen expression potentiates immunogenicity, strains were constructed that express rgp120 from a multicopy asd-stabilized plasmid (SL7207 pYA:120). Immunoblot analysis demonstrated that SL7207 pYA:120 expressed approximately 50-fold more rgp120 than SL3261::120. Oral immunization of BALB/c mice with these strains did not stimulate an env-specific CTL response or a significant rise in antigp120 antibody titer as compared to controls. However, splenic T cells from SL7207 pYA::120 immunized mice proliferated upon restimulation with gp120 in vitro while splenocytes from SL3261::120 immunized mice did not, gp120 restimulated splenic T cells from SL7207 pYA:120 immune mice also produced IFN-gamma but no IL-5. Two conclusions can be drawn from these results. First, high level expression of rgp120 in Salmonella vectors is necessary to stimulate a gp120-specific immune response in mice. Second, Salmonella::rgp120 stimulates a gp120-specific Th1 response in mice. This is the first report to describe the construction of a Salmonella::rgp120 vector vaccine that is immunogenic in mice.

摘要

由于人类免疫缺陷病毒1型(HIV-1)可通过肠道外途径或性途径传播,因此可能需要黏膜免疫反应和全身免疫反应来提供保护性免疫。表达异源抗原的减毒沙门氏菌载体可刺激这两个部位的免疫反应。为了评估沙门氏菌载体作为HIV-1载体疫苗的效用,将编码重组HIV-1 gp120(rgp120)的基因表达盒整合到鼠伤寒沙门氏菌aroA菌株SL3261的hisOGD位点(SL3261::120)。为了测试增加的抗原表达是否能增强免疫原性,构建了从多拷贝asd稳定质粒表达rgp120的菌株(SL7207 pYA:120)。免疫印迹分析表明,SL7207 pYA:120表达的rgp120比SL3261::120多约50倍。与对照组相比,用这些菌株对BALB/c小鼠进行口服免疫并未刺激env特异性CTL反应或抗gp120抗体滴度显著升高。然而,来自SL7207 pYA::120免疫小鼠的脾T细胞在体外经gp120再刺激后增殖,而来自SL3261::120免疫小鼠的脾细胞则没有,来自SL7207 pYA:120免疫小鼠的gp120再刺激脾T细胞也产生IFN-γ但不产生IL-5。从这些结果可以得出两个结论。第一,沙门氏菌载体中rgp120的高水平表达对于在小鼠中刺激gp120特异性免疫反应是必要的。第二,沙门氏菌::rgp120在小鼠中刺激gp120特异性Th1反应。这是第一篇描述在小鼠中具有免疫原性的沙门氏菌::rgp120载体疫苗构建的报告。

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