| Literature DB >> 32358170 |
Kurt A Swanson1, Jennifer N Rainho-Tomko2, Zachary P Williams2, Lilibeth Lanza2, Michael Peredelchuk2, Michael Kishko3, Vincent Pavot4, Judith Alamares-Sapuay3, Haritha Adhikarla3, Sankalp Gupta3, Sudha Chivukula3, Scott Gallichan5, Linong Zhang3, Nicholas Jackson3, Heesik Yoon2, Darin Edwards2, Chih-Jen Wei6, Gary J Nabel7.
Abstract
A stabilized form of the respiratory syncytial virus (RSV) fusion (F) protein has been explored as a vaccine to prevent viral infection because it presents several potent neutralizing epitopes. Here, we used a structure-based rational design to optimize antigen presentation and focus antibody (Ab) responses to key epitopes on the pre-fusion (pre-F) protein. This protein was fused to ferritin nanoparticles (pre-F-NP) and modified with glycans to mask nonneutralizing or poorly neutralizing epitopes to further focus the Ab response. The multimeric pre-F-NP elicited durable pre-F-specific Abs in nonhuman primates (NHPs) after >150 days and elicited potent neutralizing Ab (NAb) responses in mice and NHPs in vivo, as well as in human cells evaluated in the in vitro MIMIC system. This optimized pre-F-NP stimulated a more potent Ab response than a representative pre-F trimer, DS-Cav1. Collectively, this pre-F vaccine increased the generation of NAbs targeting the desired pre-F conformation, an attribute that facilitates the development of an effective RSV vaccine.Entities:
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Year: 2020 PMID: 32358170 DOI: 10.1126/sciimmunol.aba6466
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468