Preclinical evaluation of a COVID-19 vaccine candidate based on a recombinant RBD fusion heterodimer of SARS-CoV-2

Antonio Barreiro
Antoni Prenafeta
Gregori Bech-Sabat
Mercè Roca
Eva Perozo Mur
Ricard March
Luis González-González
Laia Madrenas
Júlia Corominas
Alex Fernández
Alexandra Moros
Manuel Cañete
Mercè Molas
Thais Pentinat-Pelegrin
Clara Panosa
Alberto Moreno
Ester Puigvert Molas
Eva Pol Vilarrassa
Jordi Palmada
Carme Garriga
Teresa Prat Cabañas
Javier Iglesias-Fernández
Júlia Vergara-Alert
Cristina Lorca-Oró
Núria Roca
Leira Fernández-Bastit
Jordi Rodon
Mònica Pérez
Joaquim Segalés
Edwards Pradenas
Silvia Marfil
Benjamin Trinité
Raquel Ortiz
Bonaventura Clotet
Julià Blanco
Jorge Díaz Pedroza
Rosa Ampudia Carrasco
Yaiza Rosales Salgado
Jordina Loubat-Casanovas
Sara Capdevila Larripa
Julia Garcia Prado
Jordi Barretina
Marta Sisteré-Oró
Paula Cebollada Rica
Andreas Meyerhans
Laura Ferrer

1 evaluations Published on Jan 30, 2023

This article on Sciety

Abstract

Current C0VID-19 vaccines have been associated with a decline in infection rates, prevention of severe disease and a decrease in mortality rates. However, SARS-CoV-2 variants are continuously evolving, and development of new accessible COVID-19 vaccines is essential to mitigate the pandemic. Here, we present data on preclinical studies in mice of a receptor-binding domain (RBD)-based recombinant protein vaccine (PHH-1V) consisting of an RBD fusion heterodimer comprising the B.1.351 and B.1.1.7 SARS-CoV-2 variants formulated in SQBA adjuvant, an oil-in-water emulsion. A prime-boost immunisation with PHH-1V in BALB/c and K18-hACE2 mice induced a CD4⁺and CD8⁺T cell response and RBD-binding antibodies with neutralising activity against several variants, and also showed a good tolerability profile. Significantly, RBD fusion heterodimer vaccination conferred 100% efficacy, preventing mortality in SARS-CoV-2 infected K18-hACE2 mice, but also reducing Beta, Delta and Omicron infection in lower respiratory airways. These findings demonstrate the feasibility of this recombinant vaccine strategy.

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