Sesterhenn, Fabian and Galloux, Marie and Vollers, Sabrina S. and Csepregi, Lucia and Yang, Che and Descamps, Delphyne and Bonet, Jaume and Friedensohn, Simon and Gainza, Pablo and Corthésy, Patricia and Chen, Man and Rosset, Stéphane and Rameix-Welti, Marie-Anne and Éléouët, Jean-François and Reddy, Sai T. and Graham, Barney S. and Riffault, Sabine and Correia, Bruno E. and Munro, James (2019) Boosting subdominant neutralizing antibody responses with a computationally designed epitope-focused immunogen. PLOS Biology, 17 (2). e3000164. ISSN 1545-7885
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Abstract
Throughout the last several decades, vaccination has been key to prevent and eradicate infectious diseases. However, many pathogens (e.g., respiratory syncytial virus [RSV], influenza, dengue, and others) have resisted vaccine development efforts, largely because of the failure to induce potent antibody responses targeting conserved epitopes. Deep profiling of human B cells often reveals potent neutralizing antibodies that emerge from natural infection, but these specificities are generally subdominant (i.e., are present in low titers). A major challenge for next-generation vaccines is to overcome established immunodominance hierarchies and focus antibody responses on crucial neutralization epitopes. Here, we show that a computationally designed epitope-focused immunogen presenting a single RSV neutralization epitope elicits superior epitope-specific responses compared to the viral fusion protein. In addition, the epitope-focused immunogen efficiently boosts antibodies targeting the palivizumab epitope, resulting in enhanced neutralization. Overall, we show that epitope-focused immunogens can boost subdominant neutralizing antibody responses in vivo and reshape established antibody hierarchies.
Item Type: | Article |
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Subjects: | STM Digital Press > Biological Science |
Depositing User: | Unnamed user with email support@stmdigipress.com |
Date Deposited: | 16 Jan 2023 10:27 |
Last Modified: | 07 May 2024 05:17 |
URI: | http://publications.articalerewriter.com/id/eprint/22 |