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一种基于霍乱弧菌“幽灵”的亚单位疫苗可诱导交叉保护性衣原体免疫,霍乱毒素无毒衍生物CTA2B可增强这种免疫。

A Vibrio cholerae ghost-based subunit vaccine induces cross-protective chlamydial immunity that is enhanced by CTA2B, the nontoxic derivative of cholera toxin.

作者信息

Ekong Eno E, Okenu Daniel N, Mania-Pramanik Jayanti, He Qing, Igietseme Joseph U, Ananaba Godwin A, Lyn Deborah, Black Carolyn, Eko Francis O

机构信息

Morehouse School of Medicine, Atlanta, GA 30310, USA.

出版信息

FEMS Immunol Med Microbiol. 2009 Mar;55(2):280-91. doi: 10.1111/j.1574-695X.2008.00493.x. Epub 2008 Nov 18.

DOI:10.1111/j.1574-695X.2008.00493.x
PMID:19040663
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3062614/
Abstract

The Vibrio cholerae ghost (rVCG) platform is an effective carrier and delivery system for designing efficacious Chlamydia vaccines. We investigated whether CTA2B, the nontoxic derivative of cholera toxin, can augment protective immunity conferred by an rVCG-based chlamydial vaccine and enhance cross-protection against heterologous chlamydial strains. An rVCG vaccine coexpressing chlamydial major outer membrane protein and CTA2B was genetically constructed and antigens were targeted to the inner membrane of V. cholerae before ghost production by gene E-mediated lysis. Effective immunomodulation by CTA2B was demonstrated by the ability of the vaccine construct to enhance the activation and maturation of dendritic cells in vitro. Also, C57BL/6 mice immunized via mucosal and systemic routes showed increased specific mucosal and systemic antibody and T-helper type-1 (Th1) responses, irrespective of the route. The enhanced production of IFN-gamma, but not IL-4 by genital mucosal and splenic T cells, indicated a predominantly Th1 response. Clearance of the Chlamydia muridarum vaginal infection was significantly enhanced by codelivery of the vaccine with CTA2B, with the intravaginal route showing a moderate advantage. These results indicate that the rVCG-based vaccine is capable of inducing cross-protection against heterologous chlamydial serovars and that incorporation of mucosal adjuvants, such as CTA2B in the rVCG delivery platform, may enhance protective immunity.

摘要

霍乱弧菌菌影(rVCG)平台是一种用于设计有效的衣原体疫苗的有效载体和递送系统。我们研究了霍乱毒素的无毒衍生物CTA2B是否能增强基于rVCG的衣原体疫苗所赋予的保护性免疫,并增强对异源衣原体菌株的交叉保护作用。通过基因构建了一种共表达衣原体主要外膜蛋白和CTA2B的rVCG疫苗,并在通过基因E介导的裂解产生菌影之前,将抗原靶向霍乱弧菌的内膜。疫苗构建体在体外增强树突状细胞激活和成熟的能力证明了CTA2B的有效免疫调节作用。此外,通过黏膜和全身途径免疫的C57BL/6小鼠,无论途径如何,均显示出特异性黏膜和全身抗体以及1型辅助性T细胞(Th1)反应增加。生殖黏膜和脾脏T细胞中IFN-γ而非IL-4的产生增加,表明主要是Th1反应。疫苗与CTA2B共同递送可显著增强对鼠衣原体阴道感染的清除,阴道内途径显示出适度优势。这些结果表明,基于rVCG的疫苗能够诱导对异源衣原体血清型的交叉保护,并且在rVCG递送平台中加入黏膜佐剂(如CTA2B)可能会增强保护性免疫。

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Comparative immunogenicity of the hepatitis B virus core 149 antigen displayed on the inner and outer membrane of bacterial ghosts.展示在细菌幽灵内外膜上的乙肝病毒核心149抗原的比较免疫原性
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