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嵌合西尼罗河病毒减毒活疫苗:安全性、免疫原性和有效性的临床前评估

ChimeriVax-West Nile virus live-attenuated vaccine: preclinical evaluation of safety, immunogenicity, and efficacy.

作者信息

Arroyo Juan, Miller Chuck, Catalan John, Myers Gwendolyn A, Ratterree Marion S, Trent Dennis W, Monath Thomas P

机构信息

Acambis Inc., 38 Sidney Street, Cambridge, MA 02139, USA.

出版信息

J Virol. 2004 Nov;78(22):12497-507. doi: 10.1128/JVI.78.22.12497-12507.2004.

Abstract

The availability of ChimeriVax vaccine technology for delivery of flavivirus protective antigens at the time West Nile (WN) virus was first detected in North America in 1999 contributed to the rapid development of the vaccine candidate against WN virus described here. ChimeriVax-Japanese encephalitis (JE), the first live- attenuated vaccine developed with this technology has successfully undergone phase I and II clinical trials. The ChimeriVax technology utilizes yellow fever virus (YF) 17D vaccine strain capsid and nonstructural genes to deliver the envelope gene of other flaviviruses as live-attenuated chimeric viruses. Amino acid sequence homology between the envelope protein (E) of JE and WN viruses facilitated targeting attenuating mutation sites to develop the WN vaccine. Here we discuss preclinical studies with the ChimeriVax-WN virus in mice and macaques. ChimeriVax-WN virus vaccine is less neurovirulent than the commercial YF 17D vaccine in mice and nonhuman primates. Attenuation of the virus is determined by the chimeric nature of the construct containing attenuating mutations in the YF 17D virus backbone and three point mutations introduced to alter residues 107, 316, and 440 in the WN virus E protein gene. The safety, immunogenicity, and efficacy of the ChimeriVax-WN(02) vaccine in the macaque model indicate the vaccine candidate is expected to be safe and immunogenic for humans.

摘要

1999年西尼罗河(WN)病毒首次在北美被发现时,ChimeriVax疫苗技术可用于递送黄病毒保护性抗原,这推动了本文所述的针对WN病毒的候选疫苗的快速研发。ChimeriVax-日本脑炎(JE)疫苗是首个采用该技术研发的减毒活疫苗,已成功完成I期和II期临床试验。ChimeriVax技术利用黄热病毒(YF)17D疫苗株的衣壳基因和非结构基因,以减毒活嵌合病毒的形式递送其他黄病毒的包膜基因。JE病毒和WN病毒包膜蛋白(E)之间的氨基酸序列同源性有助于确定减毒突变位点,从而研发WN疫苗。在此,我们讨论ChimeriVax-WN病毒在小鼠和猕猴中的临床前研究。在小鼠和非人灵长类动物中,ChimeriVax-WN病毒疫苗的神经毒性低于市售的YF 17D疫苗。病毒的减毒是由在YF 17D病毒骨架中含有减毒突变的构建体的嵌合性质以及为改变WN病毒E蛋白基因中第107、316和440位残基而引入的三个点突变所决定的。ChimeriVax-WN(02)疫苗在猕猴模型中的安全性、免疫原性和有效性表明,该候选疫苗有望对人类安全且具有免疫原性。

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