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Structure-Guided Molecular Grafting of a Complex Broadly Neutralizing Viral Epitope

Goran Bajic, Max J. Maron, Timothy M. Caradonna, Ming Tian, Adam G. Mermelstein, Daniela Fera, Garnett Kelsoe, Masayuki Kuraoka, Aaron G. Schmidt

2020ACS Infectious Diseases29 citationsDOIOpen Access PDF

Abstract

Antigenic variation and viral evolution have thwarted traditional influenza vaccination strategies. The broad protection afforded by a "universal" influenza vaccine may come from immunogens that elicit humoral immune responses targeting conserved epitopes on the viral hemagglutinin (HA), such as the receptor-binding site (RBS). Here, we engineered candidate immunogens that use noncirculating, avian influenza HAs as molecular scaffolds to present the broadly neutralizing RBS epitope from historical, circulating H1 influenzas. These "resurfaced" HAs (rsHAs) remove epitopes potentially targeted by strain-specific responses in immune-experienced individuals. Through structure-guided optimization, we improved two antigenically different scaffolds to bind a diverse panel of pan-H1 and H1/H3 cross-reactive bnAbs with high affinity. Subsequent serological and single germinal center B cell analyses from murine prime-boost immunizations show that the rsHAs are both immunogenic and can augment the quality of elicited RBS-directed antibodies. Our structure-guided, RBS grafting approach provides candidate immunogens for selectively presenting a conserved viral epitope.

Topics & Concepts

EpitopeVirologyGerminal centerBiologyHemagglutinin (influenza)Epitope mappingAntigenAntibodyImmune systemVirusImmunologyB cellInfluenza Virus Research StudiesImmunotherapy and Immune ResponsesMonoclonal and Polyclonal Antibodies Research
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