npj Vaccines (Oct 2023)

Cross-protection and cross-neutralization capacity of ancestral and VOC-matched SARS-CoV-2 adenoviral vector-based vaccines

  • Sabrina E. Vinzón,
  • María V. Lopez,
  • Eduardo G. A. Cafferata,
  • Ariadna S. Soto,
  • Paula M. Berguer,
  • Luciana Vazquez,
  • Leonora Nusblat,
  • Andrea V. Pontoriero,
  • Eduardo M. Belotti,
  • Natalia R. Salvetti,
  • Diego L. Viale,
  • Ariel E. Vilardo,
  • Martin M. Avaro,
  • Estefanía Benedetti,
  • Mara L. Russo,
  • María E. Dattero,
  • Mauricio Carobene,
  • Maximiliano Sánchez-Lamas,
  • Jimena Afonso,
  • Mauro Heitrich,
  • Alejandro E. Cristófalo,
  • Lisandro H. Otero,
  • Elsa G. Baumeister,
  • Hugo H. Ortega,
  • Alexis Edelstein,
  • Osvaldo L. Podhajcer

DOI
https://doi.org/10.1038/s41541-023-00737-4
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 15

Abstract

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Abstract COVID-19 vaccines were originally designed based on the ancestral Spike protein, but immune escape of emergent Variants of Concern (VOC) jeopardized their efficacy, warranting variant-proof vaccines. Here, we used preclinical rodent models to establish the cross-protective and cross-neutralizing capacity of adenoviral-vectored vaccines expressing VOC-matched Spike. CoroVaxG.3-D.FR, matched to Delta Plus Spike, displayed the highest levels of nAb to the matched VOC and mismatched variants. Cross-protection against viral infection in aged K18-hACE2 mice showed dramatic differences among the different vaccines. While Delta-targeted vaccines fully protected mice from a challenge with Gamma, a Gamma-based vaccine offered only partial protection to Delta challenge. Administration of CorovaxG.3-D.FR in a prime/boost regimen showed that a booster was able to increase the neutralizing capacity of the sera against all variants and fully protect aged K18-hACE2 mice against Omicron BA.1, as a BA.1-targeted vaccine did. The neutralizing capacity of the sera diminished in all cases against Omicron BA.2 and BA.5. Altogether, the data demonstrate that a booster with a vaccine based on an antigenically distant variant, such as Delta or BA.1, has the potential to protect from a wider range of SARS-CoV-2 lineages, although careful surveillance of breakthrough infections will help to evaluate combination vaccines targeting antigenically divergent variants yet to emerge.