Post-exposure vaccination with MP-12 lacking NSs protects mice against lethal Rift Valley fever virus challenge

•A model of RVFV infection in C57BL/6 mice was used for post-exposure vaccination studies.•Early post-exposure vaccination with NSs deletion viruses improves survival outcome.•Reduced viral loads and disease severity are associated with post-exposure vaccination efficacy. Rift Valley fever virus (RV...

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Veröffentlicht in:Antiviral research 2013-05, Vol.98 (2), p.135-143
Hauptverfasser: Gowen, Brian B., Bailey, Kevin W., Scharton, Dionna, Vest, Zachery, Westover, Jonna B., Skirpstunas, Ramona, Ikegami, Tetsuro
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Sprache:eng
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Zusammenfassung:•A model of RVFV infection in C57BL/6 mice was used for post-exposure vaccination studies.•Early post-exposure vaccination with NSs deletion viruses improves survival outcome.•Reduced viral loads and disease severity are associated with post-exposure vaccination efficacy. Rift Valley fever virus (RVFV) causes severe disease in humans and livestock. There are currently no approved antivirals or vaccines for the treatment or prevention of RVF disease in humans. A major virulence factor of RVFV is the NSs protein, which inhibits host transcription including the interferon (IFN)-β gene and promotes the degradation of dsRNA-dependent protein kinase, PKR. We analyzed the efficacy of the live-attenuated MP-12 vaccine strain and MP-12 variants that lack the NSs protein as post-exposure vaccinations. Although parental MP-12 failed to elicit a protective effect in mice challenged with wild-type (wt) RVFV by the intranasal route, significant protection was demonstrated by vaccination with MP-12 strains lacking NSs when they were administered at 20–30min post-exposure. Viremia and virus replication in liver, spleen and brain were also inhibited by post-exposure vaccination with MP-12 lacking NSs. The protective effect was mostly lost when vaccination was delayed 6 or 24h after intranasal RVFV challenge. When mice were challenged subcutaneously, efficacy of MP-12 lacking NSs was diminished, most likely due to more rapid dissemination of wt RVFV. Our findings suggest that post-exposure vaccination with MP-12 lacking NSs may be developed as a novel post-exposure treatment to prevent RVF.
ISSN:0166-3542
1872-9096
DOI:10.1016/j.antiviral.2013.03.009