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灵长类动物经呼吸道局部免疫成功抵御埃博拉病毒。

Successful topical respiratory tract immunization of primates against Ebola virus.

作者信息

Bukreyev Alexander, Rollin Pierre E, Tate Mallory K, Yang Lijuan, Zaki Sherif R, Shieh Wun-Ju, Murphy Brian R, Collins Peter L, Sanchez Anthony

机构信息

Laboratory of Infectious Disease, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892-8007, USA.

出版信息

J Virol. 2007 Jun;81(12):6379-88. doi: 10.1128/JVI.00105-07. Epub 2007 Apr 11.

Abstract

Ebola virus causes outbreaks of severe viral hemorrhagic fever with high mortality in humans. The virus is highly contagious and can be transmitted by contact and by the aerosol route. These features make Ebola virus a potential weapon for bioterrorism and biological warfare. Therefore, a vaccine that induces both systemic and local immune responses in the respiratory tract would be highly beneficial. We evaluated a common pediatric respiratory pathogen, human parainfluenza virus type 3 (HPIV3), as a vaccine vector against Ebola virus. HPIV3 recombinants expressing the Ebola virus (Zaire species) surface glycoprotein (GP) alone or in combination with the nucleocapsid protein NP or with the cytokine adjuvant granulocyte-macrophage colony-stimulating factor were administered by the respiratory route to rhesus monkeys--in which HPIV3 infection is mild and asymptomatic--and were evaluated for immunogenicity and protective efficacy against a highly lethal intraperitoneal challenge with Ebola virus. A single immunization with any construct expressing GP was moderately immunogenic against Ebola virus and protected 88% of the animals against severe hemorrhagic fever and death caused by Ebola virus. Two doses were highly immunogenic, and all of the animals survived challenge and were free of signs of disease and of detectable Ebola virus challenge virus. These data illustrate the feasibility of immunization via the respiratory tract against the hemorrhagic fever caused by Ebola virus. To our knowledge, this is the first study in which topical immunization through respiratory tract achieved prevention of a viral hemorrhagic fever infection in a primate model.

摘要

埃博拉病毒可引发严重的病毒性出血热疫情,导致人类高死亡率。该病毒具有高度传染性,可通过接触和气溶胶途径传播。这些特性使埃博拉病毒成为生物恐怖主义和生物战的潜在武器。因此,一种能在呼吸道诱导全身和局部免疫反应的疫苗将非常有益。我们评估了一种常见的儿科呼吸道病原体——人副流感病毒3型(HPIV3),作为针对埃博拉病毒的疫苗载体。将单独表达埃博拉病毒(扎伊尔种)表面糖蛋白(GP),或与核衣壳蛋白NP联合表达,或与细胞因子佐剂粒细胞巨噬细胞集落刺激因子联合表达的HPIV3重组体经呼吸道接种给恒河猴(HPIV3感染在恒河猴中症状轻微且无症状),并评估其对埃博拉病毒高致死性腹腔内攻击的免疫原性和保护效力。用任何表达GP的构建体进行单次免疫对埃博拉病毒具有中等免疫原性,并保护88%的动物免受埃博拉病毒引起的严重出血热和死亡。两剂免疫具有高度免疫原性,所有动物在攻击后存活,且无疾病迹象和可检测到的埃博拉病毒攻击病毒。这些数据说明了通过呼吸道免疫预防埃博拉病毒引起的出血热的可行性。据我们所知,这是第一项通过呼吸道局部免疫在灵长类动物模型中实现预防病毒性出血热感染的研究。

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