| Literature DB >> 33427208 |
Caroline Atyeo1,2, Matthew D Slein1, Stephanie Fischinger1,3, John Burke1, Alexandra Schäfer4, Sarah R Leist4, Natalia A Kuzmina5,6, Chad Mire5,6, Anna Honko7,8, Rebecca Johnson7,8, Nadia Storm7,8, Matthew Bernett9, Pei Tong10, Teng Zuo10, Junrui Lin10, Adam Zuiani10, Caitlyn Linde11, Todd Suscovich11, Duane R Wesemann10, Anthony Griffiths7,8, John R Desjarlais9, Boris D Juelg1, Jaap Goudsmit12, Alexander Bukreyev5,6,13, Ralph Baric4,14,15, Galit Alter1.
Abstract
The rapid spread of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), coupled with a lack of therapeutics, has paralyzed the globe. Although significant effort has been invested in identifying antibodies that block infection, the ability of antibodies to target infected cells through Fc interactions may be vital to eliminate the virus. To explore the role of Fc activity in SARS-CoV-2 immunity, the functional potential of a cross-SARS-reactive antibody, CR3022, was assessed. CR3022 was able to broadly drive antibody effector functions, providing critical immune clearance at entry and upon egress. Using selectively engineered Fc variants, no protection was observed after administration of WT IgG1 in mice or hamsters. Conversely, the functionally enhanced Fc variant resulted in increased pathology in both the mouse and hamster models, causing weight loss in mice and enhanced viral replication and weight loss in the more susceptible hamster model, highlighting the pathological functions of Fc-enhancing mutations. These data point to the critical need for strategic Fc engineering for the treatment of SARS-CoV-2 infection.Entities:
Keywords: Antigen; COVID-19; Epidemiology; Immunology
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Year: 2021 PMID: 33427208 DOI: 10.1172/jci.insight.143129
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708