Development of SARS-CoV-2 mRNA vaccines encoding spike N-terminal and receptor binding domains

Author:

Stewart-Jones Guillaume B.E.ORCID,Elbashir Sayda M.,Wu Kai,Lee Diana,Renzi Isabella,Ying Baoling,Koch Matthew,Sein Caralyn E.,Choi Angela,Whitener Bradley,Garcia-Dominguez Dario,Henry Carole,Woods Angela,Ma LingZhi,Montes Berrueta Daniela,Avena Laura E.,Quinones Julian,Falcone Samantha,Hsiao Chiaowen J.,Scheaffer Suzanne M.,Thackray Larissa B.,White Phil,Diamond Michael S.,Edwards Darin K.,Carfi Andrea

Abstract

AbstractWith the success of mRNA vaccines against coronavirus disease 2019 (COVID-19), strategies can now focus on improving vaccine potency, breadth, and stability. We present the design and preclinical evaluation of domain-based mRNA vaccines encoding the wild-type spike-protein receptor-binding (RBD) and/or N-terminal domains (NTD). An NTD-RBD linked candidate vaccine, mRNA-1283, showed improved antigen expression, antibody responses, and stability at refrigerated temperatures (2-8°C) compared with the clinically available mRNA-1273, which encodes the full-length spike protein. In mice administered mRNA-1283 as a primary series, booster, or variant-specific booster, similar or greater immune responses and protection from viral challenge were observed against wild-type, beta, delta, or omicron (BA. 1) compared with mRNA-1273 immunized mice, especially at lower vaccine dosages. These results support clinical assessment of mRNA-1283 (NCT05137236).One Sentence SummaryA domain-based mRNA vaccine, mRNA-1283, is immunogenic and protective against SARS-CoV-2 and emerging variants in mice.

Publisher

Cold Spring Harbor Laboratory

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