| Literature DB >> 35231399 |
George I Georgiev1, Ryan J Malonis1, Ariel S Wirchnianski2, Alex W Wessel3, Helen S Jung1, Sean M Cahill1, Elisabeth K Nyakatura1, Olivia Vergnolle1, Kimberly A Dowd4, David Cowburn1, Theodore C Pierson4, Michael S Diamond5, Jonathan R Lai6.
Abstract
Zika virus (ZIKV) is a flavivirus that can cause severe disease, but there are no approved treatments or vaccines. A complication for flavivirus vaccine development is the potential of immunogens to enhance infection via antibody-dependent enhancement (ADE), a process mediated by poorly neutralizing and cross-reactive antibodies. Thus, there is a great need to develop immunogens that minimize the potential to elicit enhancing antibodies. Here we utilized structure-based protein engineering to develop "resurfaced" (rs) ZIKV immunogens based on E glycoprotein domain III (ZDIIIs), in which epitopes bound by variably neutralizing antibodies were masked by combinatorial mutagenesis. We identified one resurfaced ZDIII immunogen (rsZDIII-2.39) that elicited a protective but immune-focused response. Compared to wild type ZDIII, immunization with resurfaced rsZDIII-2.39 protein nanoparticles produced fewer numbers of ZIKV EDIII antigen-reactive B cells and elicited serum that had a lower magnitude of induced ADE against dengue virus serotype 1 (DENV1) Our findings enhance our understanding of the structural and functional determinants of antibody protection against ZIKV.Entities:
Keywords: DENV; ZIKV; combinatorial mutagenesis; flavivirus; immune focusing; immunogen resurfacing; nanoparticle; phage display; protein engineering; vaccine
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Year: 2022 PMID: 35231399 PMCID: PMC9133142 DOI: 10.1016/j.chembiol.2022.02.004
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 9.039