AI Article Synopsis

  • Current rotavirus vaccines are expensive and pose a risk of intussusception, highlighting the need for safer, cost-effective alternatives.
  • A new P24-VP8* nanoparticle vaccine demonstrated significant protection in gnotobiotic pigs, reducing diarrhea and virus shedding after exposure to rotavirus.
  • The vaccine elicited strong immune responses, particularly in serum IgG, but did not trigger strong responses in serum or intestinal IgA and T cells, making it a promising candidate for future clinical trials.

Article Abstract

Current live rotavirus vaccines are costly with increased risk of intussusception due to vaccine replication in the gut of vaccinated children. New vaccines with improved safety and cost-effectiveness are needed. In this study, we assessed the immunogenicity and protective efficacy of a novel P24-VP8* nanoparticle vaccine using the gnotobiotic (Gn) pig model of human rotavirus infection and disease. Three doses of P24-VP8* (200 μg/dose) intramuscular vaccine with Al(OH) adjuvant (600 μg) conferred significant protection against infection and diarrhea after challenge with virulent Wa strain rotavirus. This was indicated by the significant reduction in the mean duration of diarrhea, virus shedding in feces, and significantly lower fecal cumulative consistency scores in post-challenge day (PCD) 1-7 among vaccinated pigs compared to the mock immunized controls. The P24-VP8* vaccine was highly immunogenic in Gn pigs. It induced strong VP8*-specific serum IgG and Wa-specific virus-neutralizing antibody responses from post-inoculation day 21 to PCD 7, but did not induce serum or intestinal IgA antibody responses or a strong effector T cell response, which are consistent with the immunization route, the adjuvant used, and the nature of the non-replicating vaccine. The findings are highly translatable and thus will facilitate clinical trials of the P24-VP8* nanoparticle vaccine.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963946PMC
http://dx.doi.org/10.3390/vaccines7040177DOI Listing

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