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Evaluations of rationally designed rift valley fever vaccine candidate RVax-1 in mosquito and rodent models.

Tetsuro IkegamiEduardo Jurado-CobenaCigdem AlkanJennifer K SmithLihong ZhangBirte KalveramTerry L JuelichAllen T EsterlyJahnavi R BhaskarSaravanan ThangamaniAlexander N Freiberg
Published in: NPJ vaccines (2022)
Rift Valley fever (RVF) is a mosquito-borne zoonosis endemic to Africa and the Arabian Peninsula, which causes large outbreaks among humans and ruminants. Single dose vaccinations using live-attenuated RVF virus (RVFV) support effective prevention of viral spread in endemic countries. Due to the segmented nature of RVFV genomic RNA, segments of vaccine strain-derived genomic RNA could be incorporated into wild-type RVFV within co-infected mosquitoes or animals. Rationally designed vaccine candidate RVax-1 displays protective epitopes fully identical to the previously characterized MP-12 vaccine. Additionally, all genome segments of RVax-1 contribute to the attenuation phenotype, which prevents the formation of pathogenic reassortant strains. This study demonstrated that RVax-1 cannot replicate efficiently in orally fed Aedes aegypti mosquitoes, while retaining strong immunogenicity and protective efficacy in an inbred mouse model, which were indistinguishable from the MP-12 vaccine. These findings support further development of RVax-1 as the next generation MP-12-based vaccine for prevention of Rift Valley fever in humans and animals.
Keyphrases
  • aedes aegypti
  • dengue virus
  • zika virus
  • mouse model
  • escherichia coli
  • wild type
  • copy number
  • nucleic acid