Vesicular Stomatitis Virus-Based Vaccine Protects Hamsters against Lethal Challenge with Andes Virus

被引:69
作者
Brown, Kyle S. [2 ,3 ]
Safronetz, David [1 ]
Marzi, Andrea [1 ]
Ebihara, Hideki [1 ]
Feldmann, Heinz [1 ,2 ,3 ]
机构
[1] NIAID, Virol Lab, Div Intramural Res, NIH,Rocky Mt Labs, Hamilton, MT 59840 USA
[2] Univ Manitoba, Dept Med Microbiol, Winnipeg, MB, Canada
[3] Publ Hlth Agcy Canada, Natl Microbiol Lab, Winnipeg, MB, Canada
基金
加拿大健康研究院; 美国国家卫生研究院;
关键词
HANTAVIRUS PULMONARY SYNDROME; TO-PERSON TRANSMISSION; M GENOME SEGMENT; NONHUMAN-PRIMATES; SEOUL-VIRUS; HEMORRHAGIC-FEVER; CARDIOPULMONARY SYNDROME; PEROMYSCUS-MANICULATUS; GENETIC IDENTIFICATION; ENVELOPE GLYCOPROTEINS;
D O I
10.1128/JVI.00794-11
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Andes virus (ANDV) is a highly pathogenic South American hantavirus that causes hantavirus pulmonary syndrome (HPS). A high case fatality rate, the potential for human-to-human transmission, the capacity to infect via aerosolization, and the absence of effective therapies make it imperative that a safe, fast-acting, and effective ANDV vaccine be developed. We generated and characterized a recombinant vesicular stomatitis virus (VSV) vector expressing the ANDV surface glycoprotein precursor (VSV Delta G/ANDVGPC) as a possible vaccine candidate and tested its efficacy in the only lethal-disease animal model of HPS. Syrian hamsters immunized with a single injection of VSV Delta G/ANDVGPC were fully protected against disease when challenged at 28, 14, 7, or 3 days postimmunization with a lethal dose of ANDV; however, the mechanism of protection seems to differ depending on when the immunization occurs. At 28 days postimmunization, a lack of detectable ANDV RNA in lung, liver, and blood tissue samples, as well as a lack of seroconversion to the ANDV nucleocapsidprotein in nearly all animals, suggested largely sterile immunity. The vaccine was able to generate high levels of neutralizing anti-ANDV G(N)/G(C) antibodies, which seem to play a role as a mechanism of vaccine protection. Administration of the vaccine at 7 or 3 days before challenge also resulted in full protection but with no specific neutralizing humoral immune response, suggesting a possible role of innate responses in protection against challenge virus replication. Administration of the vaccine 24 h postchallenge was successful in protecting 90% of hamsters and again suggested the induction of a potent antiviral state by the recombinant vector as a potential mechanism. Overall, our data suggest the potential for the use of the VSV platform as a fast-acting and effective prophylaxis/postexposure treatment against lethal hantavirus infections.
引用
收藏
页码:12781 / 12791
页数:11
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