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用表达猿猴免疫缺陷病毒Gag蛋白的重组牛分枝杆菌卡介苗进行皮内和口服免疫可在豚鼠中诱导持久的抗原特异性免疫反应。

Intradermal and oral immunization with recombinant Mycobacterium bovis BCG expressing the simian immunodeficiency virus Gag protein induces long-lasting, antigen-specific immune responses in guinea pigs.

作者信息

Kawahara Mamoru, Matsuo Kazuhiro, Honda Mitsuo

机构信息

National Institute of Infectious Diseases, 1-23-1 Toyama, Tokyo 162-8640, Japan.

出版信息

Clin Immunol. 2006 Apr;119(1):67-78. doi: 10.1016/j.clim.2005.11.005. Epub 2006 Jan 4.

DOI:10.1016/j.clim.2005.11.005
PMID:16386958
Abstract

To develop a new recombinant BCG (rBCG) vaccine, we constructed rBCG that expresses the full-length Gag protein of simian immunodeficiency virus (rBCG-SIVGag) at a level of 0.5 ng/mg after 3 weeks of bacterial cell culture. Intradermal (i.d.) inoculation of guinea pigs with 0.1 mg of rBCG-SIVGag resulted in the induction of delayed-type hypersensitivity (DTH) responses to both purified protein derivative (PPD) of tuberculin and SIV Gag p27 protein; responses that were maintained for the duration of the 50-week study. In contrast, guinea pigs orally vaccinated with 160 mg of the same antigen exhibited a long-lasting DTH response to the SIV Gag p27 protein, but mounted no response to PPD. Proliferative responses to SIV Gag p27 and PPD antigens were detected in both i.d. and orally immunized animals; however, the levels of PPD-specific responses were significantly higher in guinea pigs immunized by the i.d. than the oral route. A significant increase in the level of PPD- and SIV Gag p27-specific IFNgamma mRNA expression was also detected in both immunization groups receiving rBCG-SIVGag. In addition, both i.d. and oral immunization with rBCG-SIVGag induced PPD- and SIV Gag p27-specific serum IgG responses. Insertion of the SIV gag gene into BCG did not appear to change the ability of rBCG-immunized animals to elicit PPD-specific immune responses. These results indicate that rBCG-SIVGag has the ability to effectively induce long-lasting, cell-mediated and humoral immunity against both viral and bacterial antigens in guinea pigs, suggesting that rBCG-Gag has the potential to elicit immunities specific not only for tuberculosis but also for HIV at human doses.

摘要

为开发一种新型重组卡介苗(rBCG)疫苗,我们构建了在细菌细胞培养3周后表达猴免疫缺陷病毒全长Gag蛋白(rBCG - SIVGag)的rBCG,其表达水平为0.5 ng/mg。用0.1 mg rBCG - SIVGag对豚鼠进行皮内接种,可诱导对结核菌素纯蛋白衍生物(PPD)和SIV Gag p27蛋白的迟发型超敏反应(DTH);这些反应在为期50周的研究期间一直维持。相比之下,用160 mg相同抗原口服接种的豚鼠对SIV Gag p27蛋白表现出持久的DTH反应,但对PPD无反应。在皮内和口服免疫的动物中均检测到对SIV Gag p27和PPD抗原的增殖反应;然而,皮内免疫的豚鼠中PPD特异性反应水平显著高于口服途径。在接受rBCG - SIVGag的两个免疫组中还检测到PPD和SIV Gag p27特异性IFNγ mRNA表达水平显著增加。此外,用rBCG - SIVGag进行皮内和口服免疫均诱导了PPD和SIV Gag p27特异性血清IgG反应。将SIV gag基因插入卡介苗似乎并未改变rBCG免疫动物引发PPD特异性免疫反应的能力。这些结果表明,rBCG - SIVGag有能力在豚鼠中有效诱导针对病毒和细菌抗原的持久细胞介导免疫和体液免疫,这表明rBCG - Gag有潜力在人体剂量下引发不仅针对结核病而且针对HIV的特异性免疫。

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