Structure and neutralization mechanism of a human antibody targeting a complex Epitope on Zika virus

Author:

Adams Cameron,Carbaugh Derek L.,Shu Bo,Ng Thiam-Seng,Castillo Izabella N.,Bhowmik Ryan,Segovia-Chumbez Bruno,Puhl Ana C.,Graham Stephen,Diehl Sean A.,Lazear Helen M.,Lok Shee-mei,de Silva Aravinda M.ORCID,Premkumar Lakshmanane

Abstract

We currently have an incomplete understanding of why only a fraction of human antibodies that bind to flaviviruses block infection of cells. Here we define the footprint of a strongly neutralizing human monoclonal antibody (mAb G9E) with Zika virus (ZIKV) by both X-ray crystallography and cryo-electron microscopy. Flavivirus envelope (E) glycoproteins are present as homodimers on the virion surface, and G9E bound to a quaternary structure epitope spanning both E protomers forming a homodimer. As G9E mainly neutralized ZIKV by blocking a step after viral attachment to cells, we tested if the neutralization mechanism of G9E was dependent on the mAb cross-linking E molecules and blocking low-pH triggered conformational changes required for viral membrane fusion. We introduced targeted mutations to the G9E paratope to create recombinant antibodies that bound to the ZIKV envelope without cross-linking E protomers. The G9E paratope mutants that bound to a restricted epitope on one protomer poorly neutralized ZIKV compared to the wild-type mAb, demonstrating that the neutralization mechanism depended on the ability of G9E to cross-link E proteins. In cell-free low pH triggered viral fusion assay, both wild-type G9E, and epitope restricted paratope mutant G9E bound to ZIKV but only the wild-type G9E blocked fusion. We propose that, beyond antibody binding strength, the ability of human antibodies to cross-link E-proteins is a critical determinant of flavivirus neutralization potency.

Funder

Centers for Disease Control and Prevention

Division of Microbiology and Infectious Diseases, National Institute of Allergy and Infectious Diseases

US National Institutes of Health

National Research Foundation Singapore

Ministry of Health, Singapore

Publisher

Public Library of Science (PLoS)

Subject

Virology,Genetics,Molecular Biology,Immunology,Microbiology,Parasitology

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