| Literature DB >> 33837212 |
Kevin O Saunders1,2,3,4, Norbert Pardi5, Robert Parks6,7, Sampa Santra8, Zekun Mu6,9, Laura Sutherland6,7, Richard Scearce6,7, Maggie Barr6,7, Amanda Eaton10, Giovanna Hernandez6,7, Derrick Goodman6,10, Michael J Hogan5, Istvan Tombacz5, David N Gordon11, R Wes Rountree6,7, Yunfei Wang6,7, Mark G Lewis11, Theodore C Pierson12, Chris Barbosa13, Ying Tam13, Xiaoying Shen6,10, Guido Ferrari6,10, Georgia D Tomaras6,10, David C Montefiori6,10, Drew Weissman14, Barton F Haynes15,16,17.
Abstract
The development of an effective AIDS vaccine remains a challenge. Nucleoside-modified mRNAs formulated in lipid nanoparticles (mRNA-LNP) have proved to be a potent mode of immunization against infectious diseases in preclinical studies, and are being tested for SARS-CoV-2 in humans. A critical question is how mRNA-LNP vaccine immunogenicity compares to that of traditional adjuvanted protein vaccines in primates. Here, we show that mRNA-LNP immunization compared to protein immunization elicits either the same or superior magnitude and breadth of HIV-1 Env-specific polyfunctional antibodies. Immunization with mRNA-LNP encoding Zika premembrane and envelope or HIV-1 Env gp160 induces durable neutralizing antibodies for at least 41 weeks. Doses of mRNA-LNP as low as 5 μg are immunogenic in macaques. Thus, mRNA-LNP can be used to rapidly generate single or multi-component vaccines, such as sequential vaccines needed to protect against HIV-1 infection. Such vaccines would be as or more immunogenic than adjuvanted recombinant protein vaccines in primates.Entities:
Year: 2021 PMID: 33837212 DOI: 10.1038/s41541-021-00307-6
Source DB: PubMed Journal: NPJ Vaccines ISSN: 2059-0105 Impact factor: 7.344