A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

Most approved vaccines against COVID-19 have to be administered in a prime/boost regimen. We engineered a novel vaccine based on a chimeric human adenovirus 5 (hAdV5) vector. The vaccine (named CoroVaxG.3) is based on three pillars: (i) high expression of Spike to enhance its immunodominance by usin...

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Veröffentlicht in:Vaccines (Basel) 2021-09, Vol.9 (10), p.1106, Article 1106
Hauptverfasser: Lopez, M. Veronica, Vinzon, Sabrina E., Cafferata, Eduardo G. A., Nunez, Felipe J., Soto, Ariadna, Sanchez-Lamas, Maximiliano, Afonso, M. Jimena, Aguilar-Cortes, Diana, Rios, Gregorio D., Maricato, Juliana T., T. Braconi, Carla, B. Silveira, Vanessa, M. Andrad, Tatiane, C. S. Bonetti, Tatiana, Ramos Janini, Luiz M., Girao, Manoel J. B. C., Llera, Andrea S., Gomez, Karina A., Ortega, Hugo H., Berguer, Paula M., Podhajcer, Osvaldo L.
Format: Artikel
Sprache:eng
Schlagworte:
Adenoviruses
Antibodies
Clinical trials
Cloning
Conformation
Coronaviruses
COVID vaccine
COVID-19
COVID-19 vaccines
Dendritic cells
Disease transmission
Domains
Humoral immunity
hybrid adenovirus vector
Immune response
Immune system
Immunity
Immunodominance
Immunology
Life Sciences & Biomedicine
Lymphocytes T
Medicine, Research & Experimental
Monocytes
mRNA
Muscles
Plasmids
Research & Experimental Medicine
Science & Technology
Severe acute respiratory syndrome coronavirus 2
Software
Vaccines
variants of concern
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Zusammenfassung:Most approved vaccines against COVID-19 have to be administered in a prime/boost regimen. We engineered a novel vaccine based on a chimeric human adenovirus 5 (hAdV5) vector. The vaccine (named CoroVaxG.3) is based on three pillars: (i) high expression of Spike to enhance its immunodominance by using a potent promoter and an mRNA stabilizer; (ii) enhanced infection of muscle and dendritic cells by replacing the fiber knob domain of hAdV5 by hAdV3; (iii) use of Spike stabilized in a prefusion conformation. The transduction with CoroVaxG.3-expressing Spike (D614G) dramatically enhanced the Spike expression in human muscle cells, monocytes and dendritic cells compared to CoroVaxG.5 that expressed the native fiber knob domain. A single dose of CoroVaxG.3 induced a potent humoral immunity with a balanced Th1/Th2 ratio and potent T-cell immunity, both lasting for at least 5 months. Sera from CoroVaxG.3-vaccinated mice was able to neutralize pseudoviruses expressing B.1 (wild type D614G), B.1.117 (alpha), P.1 (gamma) and B.1.617.2 (delta) Spikes, as well as an authentic P.1 SARS-CoV-2 isolate. Neutralizing antibodies did not wane even after 5 months, making this kind of vaccine a likely candidate to enter clinical trials.
ISSN:2076-393X
2076-393X
DOI:10.3390/vaccines9101106