PLoS Biology (Feb 2019)

Boosting subdominant neutralizing antibody responses with a computationally designed epitope-focused immunogen.

  • Fabian Sesterhenn,
  • Marie Galloux,
  • Sabrina S Vollers,
  • Lucia Csepregi,
  • Che Yang,
  • Delphyne Descamps,
  • Jaume Bonet,
  • Simon Friedensohn,
  • Pablo Gainza,
  • Patricia Corthésy,
  • Man Chen,
  • Stéphane Rosset,
  • Marie-Anne Rameix-Welti,
  • Jean-François Éléouët,
  • Sai T Reddy,
  • Barney S Graham,
  • Sabine Riffault,
  • Bruno E Correia

DOI
https://doi.org/10.1371/journal.pbio.3000164
Journal volume & issue
Vol. 17, no. 2
p. e3000164

Abstract

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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.