First Exposure to the Pandemic H1N1 Virus Induced Broadly Neutralizing Antibodies Targeting Hemagglutinin Head Epitopes

Overview

Journal Sci Transl Med

Specialties General Medicine
Science

Date 2021 Jun 3

PMID 34078743

Citations 35

Authors

Jenna J Guthmiller

Julianna Han

Lei Li

Alec W Freyn

Sean T H Liu

Olivia Stovicek

Christopher T Stamper

Haley L Dugan

Micah E Tepora

Henry A Utset

Dalia J Bitar

Natalie J Hamel

Siriruk Changrob

Nai-Ying Zheng

Min Huang

Florian Krammer

Raffael Nachbagauer

Peter Palese

Andrew B Ward

Patrick C Wilson

Affiliations

Soon will be listed here.

Abstract

Broadly neutralizing antibodies are critical for protection against both drifted and shifted influenza viruses. Here, we reveal that first exposure to the 2009 pandemic H1N1 influenza virus recalls memory B cells that are specific to the conserved receptor-binding site (RBS) or lateral patch epitopes of the hemagglutinin (HA) head domain. Monoclonal antibodies (mAbs) generated against these epitopes are broadly neutralizing against H1N1 viruses spanning 40 years of viral evolution and provide potent protection in vivo. Lateral patch-targeting antibodies demonstrated near universal binding to H1 viruses, and RBS-binding antibodies commonly cross-reacted with H3N2 viruses and influenza B viruses. Lateral patch-targeting mAbs were restricted to expressing the variable heavy-chain gene VH3-23 with or without the variable kappa-chain gene VK1-33 and often had a Y-x-R motif within the heavy-chain complementarity determining region 3 to make key contacts with HA. Moreover, lateral patch antibodies that used both VH3-23 and VK1-33 maintained neutralizing capability with recent pH1N1 strains that acquired mutations near the lateral patch. RBS-binding mAbs used a diverse repertoire but targeted the RBS epitope similarly and made extensive contacts with the major antigenic site Sb. Together, our data indicate that RBS- and lateral patch-targeting clones are abundant within the human memory B cell pool, and universal vaccine strategies should aim to drive antibodies against both conserved head and stalk epitopes.

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