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用质粒DNA和带有35型纤维的嵌合5型腺病毒载体进行初免-加强免疫接种可诱导针对HIV的保护性免疫。

Prime-boost vaccination with plasmid DNA and a chimeric adenovirus type 5 vector with type 35 fiber induces protective immunity against HIV.

作者信息

Xin K-Q, Jounai N, Someya K, Honma K, Mizuguchi H, Naganawa S, Kitamura K, Hayakawa T, Saha S, Takeshita F, Okuda K, Honda M, Klinman D M, Okuda K

机构信息

Department of Molecular Biodefense Research, Yokohama City University, Graduate School of Medicine, Yokohama, Japan.

出版信息

Gene Ther. 2005 Dec;12(24):1769-77. doi: 10.1038/sj.gt.3302590.

Abstract

Immunization involving a DNA vaccine prime followed by an adenovirus type 5 (Ad5) boost elicited a protective immune response against SHIV challenge in monkeys. However, the hepatocellular tropism of Ad5 limits the safety of this viral vector. This study examines the safety and immunogenicity of a replication-defective chimeric Ad5 vector with the Ad35 fiber (Ad5/35) in BALB/c mice and rhesus monkeys. This novel Ad5/35 vector showed minimal hepatotoxicity after intramuscular administration with the novel Ad5/35 vector. In addition, an Ad5/35 vector expressing HIV Env gp160 protein (Ad5/35-HIV) generated strong HIV-specific immune responses in both animal models. Priming with a DNA vaccine followed by Ad5/35-HIV boosting yielded protection against a gp160-expressing vaccinia virus challenge in BALB/c mice. The Ad5/35-HIV vector was significantly less susceptible to the pre-existing Ad5 immunity than a comparable Ad5 vector. These findings indicate that an Ad5/35 vector-based HIV vaccine may be of considerable value for clinical use.

摘要

先接种DNA疫苗再用5型腺病毒(Ad5)加强免疫,可在猴子体内引发针对猿猴免疫缺陷病毒(SHIV)攻击的保护性免疫反应。然而,Ad5的肝细胞嗜性限制了这种病毒载体的安全性。本研究检测了一种带有35型腺病毒纤维的复制缺陷型嵌合Ad5载体(Ad5/35)在BALB/c小鼠和恒河猴中的安全性和免疫原性。用新型Ad5/35载体肌肉注射后,这种新型Ad5/35载体显示出最小的肝毒性。此外,一种表达HIV包膜糖蛋白160(HIV Env gp160)的Ad5/35载体(Ad5/35-HIV)在两种动物模型中均产生了强烈的HIV特异性免疫反应。先用DNA疫苗免疫,再用Ad5/35-HIV加强免疫,可使BALB/c小鼠对表达gp160的痘苗病毒攻击产生保护作用。与类似的Ad5载体相比,Ad5/35-HIV载体对预先存在的Ad5免疫力的敏感性显著降低。这些发现表明,基于Ad5/35载体的HIV疫苗可能具有相当大的临床应用价值。

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