Novel DNA-launched Venezuelan equine encephalitis virus vaccine with rearranged genome

•Live-attenuated V4020 VEEV vaccine with rearranged structural genes is described.•V4020 included attenuating mutations engineered to prevent reversions.•Vaccinated mice developed neutralizing antibodies and survived challenge.•Intracranial injections in mice showed attenuated replication of V4020 c...

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Veröffentlicht in:Vaccine 2019-05, Vol.37 (25), p.3317-3325
Hauptverfasser: Tretyakova, Irina, Tibbens, Alexander, Jokinen, Jenny D., Johnson, Dylan M., Lukashevich, Igor S., Pushko, Peter
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Sprache:eng
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Zusammenfassung:•Live-attenuated V4020 VEEV vaccine with rearranged structural genes is described.•V4020 included attenuating mutations engineered to prevent reversions.•Vaccinated mice developed neutralizing antibodies and survived challenge.•Intracranial injections in mice showed attenuated replication of V4020 compared to the TC83.•V4020 has safety advantage over TC83, while provides equivalent protection after VEEV challenge. Novel live-attenuated V4020 vaccine was prepared for Venezuelan equine encephalitis virus (VEEV), an alphavirus from the Togaviridae family. The genome of V4020 virus was rearranged, with the capsid gene expressed using a duplicate subgenomic promoter downstream from the glycoprotein genes. V4020 also included both attenuating mutations from the TC83 VEEV vaccine secured by mutagenesis to prevent reversion mutations. The full-length infectious RNA of V4020 vaccine virus was expressed from pMG4020 plasmid downstream from the CMV promoter and launched replication of live-attenuated V4020 in vitro or in vivo. BALB/c mice vaccinated with a single dose of V4020 virus or with pMG4020 plasmid had no adverse reactions to vaccinations and developed high titers of neutralizing antibodies. After challenge with the wild type VEEV, vaccinated mice survived with no morbidity, while all unvaccinated controls succumbed to lethal infection. Intracranial injections in mice showed attenuated replication of V4020 vaccine virus as compared to the TC83. We conclude that V4020 vaccine has safety advantage over TC83, while provides equivalent protection in a mouse VEEV challenge model.
ISSN:0264-410X
1873-2518
DOI:10.1016/j.vaccine.2019.04.072