Human neutralizing antibodies against SARS-CoV-2 require intact Fc effector functions and monocytes for optimal therapeutic protection

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Author Name

Emma S Winkler

Pavlo Gilchuk

Jinsheng Yu

Published 1 Project

Immunology

Adam L Bailey

Published 2 Projects

Immunology Microbiology

Rita E. Chen

Uploader

Seth J. Zost

Hyesun Jang

Published 1 Project

Immunology

Ying Huang

Published 1 Project

Immunology

James D. Allen

Published 1 Project

Immunology

James Brett Case

Rachel E Sutton

Robert H. Carnahan

Tamarand L. Darling

Published 2 Projects

Immunology

Adrianus C. M. Boon

Published 1 Project

Immunology

Matthias Mack

Richard D Head

Published 1 Project

Immunology

Ted M Ross

Published 1 Project

Immunology

James E. Crowe

Michael Diamond

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SARS-CoV-2 has caused the global COVID-19 pandemic. Although passively delivered neutralizing antibodies against SARS-CoV-2 show promise in clinical trials, their mechanism of action in vivo is incompletely understood. Here, we define correlates of protection of neutralizing human monoclonal antibodies (mAbs) in SARS-CoV-2-infected animals. Whereas Fc effector functions are dispensable when representative neutralizing mAbs are administered as prophylaxis, they are required for optimal protection as therapy. When given after infection, intact mAbs reduce SARS-CoV-2 burden and lung disease in mice and hamsters better than loss-of-function Fc variant mAbs. Fc engagement of neutralizing antibodies mitigates inflammation and improves respiratory mechanics, and transcriptional profiling suggests these phenotypes are associated with diminished innate immune signaling and preserved tissue repair. Immune cell depletions establish that neutralizing mAbs require monocytes for therapeutic efficacy. Thus, potently neutralizing mAbs require Fc effector functions for maximal therapeutic benefit during therapy to modulate protective immune responses and mitigate lung disease.

Immunology
Immunology 63 Projects