Fc mediated pan-sarbecovirus protection after alphavirus vector vaccination

Author:

Adams Lily E.,Leist Sarah R.,Dinnon Kenneth H.,West Ande,Gully Kendra L.,Anderson Elizabeth J.,Loome Jennifer F.,Madden Emily A.,Powers John M.,Schäfer Alexandra,Sarkar Sanjay,Castillo Izabella N.,Maron Jenny S.,McNamara Ryan P.,Bertera Harry L.,Zweigert Mark R.,Higgins Jaclyn S.,Hampton Brea K.ORCID,Premkumar Lakshmanane,Alter GalitORCID,Montgomery Stephanie A.,Baxter Victoria K.,Heise Mark T.,Baric Ralph S.

Abstract

ABSTRACTTwo group 2B β-coronaviruses (sarbecoviruses) have caused regional and global epidemics in modern history. The mechanisms of cross protection driven by the sarbecovirus spike, a dominant immunogen, are less clear yet critically important for pan-sarbecovirus vaccine development. We evaluated the mechanisms of cross-sarbecovirus protective immunity using a panel of alphavirus-vectored vaccines covering bat to human strains. While vaccination did not prevent virus replication, it protected against lethal heterologous disease outcomes in both SARS-CoV-2 and clade 2 bat sarbecovirus HKU3-SRBD challenge models. The spike vaccines tested primarily elicited a highly S1-specific homologous neutralizing antibody response with no detectable cross-virus neutralization. We found non-neutralizing antibody functions that mediated cross protection in wild-type mice were mechanistically linked to FcgR4 and spike S2-binding antibodies. Protection was lost in FcR knockout mice, further supporting a model for non-neutralizing, protective antibodies. These data highlight the importance of FcR-mediated cross-protective immune responses in universal pan-sarbecovirus vaccine designs.

Publisher

Cold Spring Harbor Laboratory

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