| Literature DB >> 34618692 |
Sita Awasthi1, James J Knox2, Angela Desmond1,3, Mohamad-Gabriel Alameh1, Brian T Gaudette2, John M Lubinski1, Alexis Naughton1, Lauren M Hook1, Kevin P Egan1, Ying K Tam4, Norbert Pardi1, David Allman2, Eline T Luning Prak2, Michael P Cancro2, Drew Weissman1, Gary H Cohen5, Harvey M Friedman1.
Abstract
Nucleoside-modified mRNA vaccines have gained global attention because of COVID-19. We evaluated a similar vaccine approach for preventing a chronic, latent genital infection rather than an acute respiratory infection. We used animal models to compare an HSV-2 trivalent nucleoside-modified mRNA vaccine with the same antigens prepared as proteins, with an emphasis on antigen-specific memory B cell responses and immune correlates of protection. In guinea pigs, serum neutralizing-antibody titers were higher at 1 month and declined far less by 8 months in mRNA- compared with protein-immunized animals. Both vaccines protected against death and genital lesions when infected 1 month after immunization; however, protection was more durable in the mRNA group compared with the protein group when infected after 8 months, an interval representing greater than 15% of the animal's lifespan. Serum and vaginal neutralizing-antibody titers correlated with protection against infection, as measured by genital lesions and vaginal virus titers 2 days after infection. In mice, the mRNA vaccine generated more antigen-specific memory B cells than the protein vaccine at early times after immunization that persisted for up to 1 year. High neutralizing titers and robust B cell immune memory likely explain the more durable protection by the HSV-2 mRNA vaccine.Entities:
Keywords: Adaptive immunity; Infectious disease; Vaccines
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Year: 2021 PMID: 34618692 PMCID: PMC8631595 DOI: 10.1172/JCI152310
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808