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Mosaic sarbecovirus vaccination elicits cross-reactive responses in pre-immunized animals.

Alexander A CohenJennifer R KeeffeAriën SchiepersSandra E DrossAllison J GreaneyAnnie V RorickHan GaoPriyanthi N P GnanapragasamChengcheng FanAnthony P WestArlene I RamsinghJesse H ErasmusJanice D PataHiromi MuramatsuNorbert PardiPaulo J C LinScott BaxterRita CruzMartina Quintanar-AudeloEllis RobbCristina Serrano-AmatriainLeonardo MagneschiIan G FotheringhamDeborah Heydenburg FullerGabriel D VictoraPamela J Bjorkman
Published in: bioRxiv : the preprint server for biology (2024)
Immunization with mosaic-8b [60-mer nanoparticles presenting 8 SARS-like betacoronavirus (sarbecovirus) receptor-binding domains (RBDs)] elicits more broadly cross-reactive antibodies than homotypic SARS-CoV-2 RBD-only nanoparticles and protects against sarbecoviruses. To investigate original antigenic sin (OAS) effects on mosaic-8b efficacy, we evaluated effects of prior COVID-19 vaccinations in non-human primates and mice on sarbecovirus response breadths elicited by mosaic-8b, admix-8b (8 homotypics), and homotypic SARS-CoV-2, finding greatest cross-reactivity for mosaic-8b. As demonstrated by molecular fate-mapping in which antibodies derived from specific cohorts of B cells are differentially detected, B cells primed by WA1 spike mRNA-LNP dominated antibody responses after RBD-nanoparticle boosting. While mosaic-8b- and homotypic-nanoparticles boosted cross-reactive antibodies, de novo antibodies were predominantly induced with mosaic-8b boosting, and these were specific for variant RBDs with increased identity to RBDs on mosaic-8b. These results inform OAS mechanisms and support using mosaic-8b to protect COVID-19 vaccinated/infected humans against as-yet-unknown SARS-CoV-2 variants and animal sarbecoviruses with human spillover potential.
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