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Maturation of SARS-CoV-2 Spike-specific memory B cells drives resilience to viral escape
Roberta Marzi; Jessica Bassi; Chiara Silacci-Fregni; Istvan Bartha; Francesco Muoio; Katja Culap; Nicole Sprugasci; Gloria Lombardo; Christian Saliba; Elisabetta Cameroni; Antonino Cassotta; Jun S Low; Alexandra C Walls; Matthew McCallum; M. Alejandra Tortorici; John E Bowen; Exequiel A Dellota Jr.; Josh R Dillen; Nadine Czudnochowski; Laura Pertusini; Tatiana Terrot; Valentino Lepori; Maciej Tarkowski; Agostino Riva; Maira Biggiogero; Alessandra Franzetti Pellanda; Christian Garzoni; Paolo Ferrari; Alessandro Ceschi; Olivier Giannini; Colin Havenar-Daughton; Amalio Telenti; Ann Arvin; Herbert W Virgin; Federica Sallusto; David Veesler; Antonio Lanzavecchia; Davide Corti; Luca Piccoli.
Preprint en Inglés | bioRxiv | ID: ppbiorxiv-509852

RESUMEN

Memory B cells (MBCs) generate rapid antibody responses upon secondary encounter with a pathogen. Here, we investigated the kinetics, avidity and cross-reactivity of serum antibodies and MBCs in 155 SARS-CoV-2 infected and vaccinated individuals over a 16-month timeframe. SARS-CoV-2-specific MBCs and serum antibodies reached steady-state titers with comparable kinetics in infected and vaccinated individuals. Whereas MBCs of infected individuals targeted both pre- and postfusion Spike (S), most vaccine-elicited MBCs were specific for prefusion S, consistent with the use of prefusion-stabilized S in mRNA vaccines. Furthermore, a large fraction of MBCs recognizing postfusion S cross-reacted with human betacoronaviruses. The avidity of MBC-derived and serum antibodies increased over time resulting in enhanced resilience to viral escape by SARS-CoV-2 variants, including Omicron BA.1 and BA.2 sub-lineages, albeit only partially for BA.4 and BA.5 sublineages. Overall, the maturation of high-affinity and broadly-reactive MBCs provides the basis for effective recall responses to future SARS-CoV-2 variants.

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