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用表达耶尔森氏鼠疫杆菌分泌型F1和V抗原的减毒鼠伤寒沙门氏菌经鼻内和/或联合口服免疫小鼠后,对实验性鼠疫的免疫原性和保护性免疫的比较。

A comparison of immunogenicity and protective immunity against experimental plague by intranasal and/or combined with oral immunization of mice with attenuated Salmonella serovar Typhimurium expressing secreted Yersinia pestis F1 and V antigen.

作者信息

Liu Wen-Tssann, Hsu Hui-Ling, Liang Chung-Chih, Chuang Chuan-Chang, Lin Huang-Chi, Liu Yu-Tien

机构信息

Institute of Preventive Medicine, National Defence Medical Center, Taipei, Taiwan.

出版信息

FEMS Immunol Med Microbiol. 2007 Oct;51(1):58-69. doi: 10.1111/j.1574-695X.2007.00280.x. Epub 2007 Jul 19.

DOI:10.1111/j.1574-695X.2007.00280.x
PMID:17640293
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2121146/
Abstract

We investigated the relative immunogenicity and protective efficacy of recombinant X85MF1 and X85V strains of DeltacyaDeltacrpDeltaasd-attenuated Salmonella Typhimurium expressing, respectively, secreted Yersinia pestis F1 and V antigens, following intranasal (i.n.) or i.n. combined with oral immunization for a mouse model. A single i.n. dose of 10(8) CFU of X85MF1 or X85V induced appreciable serum F1- or V-specific IgG titres, although oral immunization did not. Mice i.n. immunized three times (i.n. x 3) with Salmonella achieved the most substantial F1/V-specific IgG titres, as compared with corresponding titres for an oral-primed, i.n.-boosted (twice; oral-i.n. x 2) immunization regimen. The level of V-specific IgG was significantly greater than that of F1-specific IgG (P<0.001). Analysis of the IgG antibodies subclasses revealed comparable levels of V-specific Th-2-type IgG1 and Th-1-type IgG2a, and a predominance of F1-specific Th-1-type IgG2a antibodies. In mice immunized intranasally, X85V stimulated a greater IL-10-secreting-cell response in the lungs than did X85MF1, but impaired the induction of gamma-interferon-secreting cells. A program of i.n. x 3 and/or oral-i.n. x 2 immunization with X85V provided levels of protection against a subsequent lethal challenge with Y. pestis, of, respectively, 60% and 20%, whereas 80% protection was provided following the same immunization but with X85MF1.

摘要

我们研究了分别表达分泌型鼠疫耶尔森菌F1和V抗原的重组X85MF1和X85V菌株(缺失cya、crp和asd基因的减毒鼠伤寒沙门氏菌)在小鼠模型中经鼻内(i.n.)或经鼻内联合口服免疫后的相对免疫原性和保护效力。单剂量经鼻内给予10⁸CFU的X85MF1或X85V可诱导产生可观的血清F1或V特异性IgG滴度,而口服免疫则不能。与口服初免、经鼻内加强免疫(两次;口服 - 经鼻内×2)的免疫方案相比,经鼻内三次免疫(经鼻内×3)的小鼠获得了最高的F1/V特异性IgG滴度。V特异性IgG水平显著高于F1特异性IgG(P<0.001)。IgG抗体亚类分析显示,V特异性Th - 2型IgG1和Th - 1型IgG2a水平相当,而F1特异性Th - 1型IgG2a抗体占优势。在经鼻内免疫的小鼠中,X85V在肺部刺激产生的分泌IL - 10的细胞反应比X85MF1更强,但损害了γ干扰素分泌细胞的诱导。用X85V进行经鼻内×3和/或口服 - 经鼻内×2免疫方案分别提供了60%和20%的保护水平,以抵御随后的鼠疫耶尔森菌致死性攻击,而用X85MF1进行相同免疫后提供了80%的保护。

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