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

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作者
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
机构
[1] Fundación Instituto Leloir-CONICET; Ciudad Autónoma de Buenos Aires,Laboratorio de Terapia Molecular y Celular
[2] Fundación Instituto Leloir-CONICET; Ciudad Autónoma de Buenos Aires,Laboratorio de Microbiología e Inmunología Molecular
[3] ANLIS Dr. Carlos G. Malbrán; Ciudad Autónoma de Buenos Aires,Unidad Operativa Centro de Contención Biológica
[4] Laboratorio Nacional de Referencia de SARS-CoV-2/COVID-19 OPS/OMS,Servicio Virosis Respiratorias, Laboratorio Nacional de Referencia de Enfermedades Respiratorias Virales
[5] INEI-ANLIS Dr Carlos G Malbrán; Ciudad Autónoma de Buenos Aires,Centro de Medicina Comparada
[6] ICiVet-Litoral,Instituto de Investigaciones Biomédicas en Retrovirus y SIDA (UBA
[7] Universidad Nacional del Litoral-CONICET; Esperanza,CONICET)
[8] Ciudad Autónoma de Buenos Aires,Area de Bioterio
[9] Securitas Biosciences,Centro de Re
[10] Fundación Instituto Leloir; Ciudad Autónoma de Buenos Aires,diseño e Ingeniería de Proteínas (CRIP)
[11] Universidad Nacional de San Martín,Departamento de Biología Molecular, Facultad de Ciencias Exactas, Físico
[12] Universidad Nacional de Río Cuarto,Químicas y Naturales, Instituto de Biotecnología Ambiental y Salud, CONICET
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摘要
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.
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