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Preclinical efficacy, safety, and immunogenicity of PHH-1V, a second-generation COVID-19 vaccine candidate based on a novel recombinant RBD fusion heterodimer of SARS-CoV-2.
Antonio Barreiro; Antoni Prenafeta; Gregori Bech-Sabat; Merce Roca; Eva Perozo; Ricard March; Luis Gonzalez; Laia Madrenas; Julia Corominas; Alex Fernandez; Alexandra Moros; Merce Molas; Thais Pentinat; Clara Panosa; Alberto Moreno; Ester Puigvert; Eva Pol; Jordi Palmada; Carme Garriga; Teresa Prat; Julia Vergara-Alert; Cristina Lorca-Oro; Nuria Roca; Leira Fernandez-Bastit; Jordi Rodon; Monica Perez; Joaquim Segales; Edwards Pradenas; Silvia Marfil; Benjamin Trinite; Raquel Ortiz; Bonaventura Clotet; Julia Blanco; Jorge Diaz Pedroza; Rosa Ampudia Carrasco; Yaiza Rosales Salgado; Jordina Loubat Casanovas; Sara Capdevila Larripa; Julia Garcia Prado; Jordi Barretina Ginesta; Marta Sistere-Oro; Paula Cebollada Rica; Andreas Meyerhans; Laura Ferrer.
Preprint in English | bioRxiv | ID: ppbiorxiv-469117

ABSTRACT

The current COVID-19 vaccines have been associated with a decline in infection rates, prevention of severe disease and decrease in mortality rates. However, new variants of concern (VoCs) are continuously evolving, making the development of new accessible COVID-19 vaccines essential in order to mitigate the pandemic. Here we present data on preclinical studies in mice of a receptor-binding domain (RBD)-based recombinant protein vaccine candidate (PHH-1V) consisting of an RBD fusion heterodimer containing the B.1.351 and B.1.1.7 SARS-CoV-2 VoCs and formulated with the SQBA adjuvant, an oil-in-water emulsion produced by HIPRA. BALB/c and K18-hACE2 mice were immunized with different recombinant RBD fusion heterodimer doses, following a two-dose prime-and-boost schedule. Vaccination induced a CD4+ and CD8+ T cell response and RBD-binding antibodies with neutralising activity against various VoCs with a good tolerability profile. Significantly, a 10-{micro}g or 20-{micro}g RBD fusion heterodimer/dose vaccination conferred 100% efficacy, preventing mortality in SARS-CoV-2 infected K18-hACE2 mice. These findings demonstrate the feasibility of this recombinant vaccine strategy.

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