Three immunizations with Novavax's protein vaccines increase antibody breadth and provide durable protection from SARS-CoV-2

接种三剂诺瓦瓦克斯公司的蛋白疫苗可提高抗体广度,并提供针对SARS-CoV-2的持久保护。

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作者:Klara Lenart ,Rodrigo Arcoverde Cerveira # ,Fredrika Hellgren # ,Sebastian Ols ,Daniel J Sheward ,Changil Kim ,Alberto Cagigi ,Matthew Gagne ,Brandon Davis ,Daritza Germosen ,Vicky Roy ,Galit Alter ,Hélène Letscher ,Jérôme Van Wassenhove ,Wesley Gros ,Anne-Sophie Gallouët ,Roger Le Grand ,Harry Kleanthous ,Mimi Guebre-Xabier ,Ben Murrell ,Nita Patel ,Gregory Glenn ,Gale Smith ,Karin Loré

Abstract

The immune responses to Novavax's licensed NVX-CoV2373 nanoparticle Spike protein vaccine against SARS-CoV-2 remain incompletely understood. Here, we show in rhesus macaques that immunization with Matrix-MTM adjuvanted vaccines predominantly elicits immune events in local tissues with little spillover to the periphery. A third dose of an updated vaccine based on the Gamma (P.1) variant 7 months after two immunizations with licensed NVX-CoV2373 resulted in significant enhancement of anti-spike antibody titers and antibody breadth including neutralization of forward drift Omicron variants. The third immunization expanded the Spike-specific memory B cell pool, induced significant somatic hypermutation, and increased serum antibody avidity, indicating considerable affinity maturation. Seven months after immunization, vaccinated animals controlled infection by either WA-1 or P.1 strain, mediated by rapid anamnestic antibody and T cell responses in the lungs. In conclusion, a third immunization with an adjuvanted, low-dose recombinant protein vaccine significantly improved the quality of B cell responses, enhanced antibody breadth, and provided durable protection against SARS-CoV-2 challenge.

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