Protective mucosal immunity against SARS-CoV-2 after heterologous systemic prime-mucosal boost immunization

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作者
Dennis Lapuente
Jana Fuchs
Jonas Willar
Ana Vieira Antão
Valentina Eberlein
Nadja Uhlig
Leila Issmail
Anna Schmidt
Friederike Oltmanns
Antonia Sophia Peter
Sandra Mueller-Schmucker
Pascal Irrgang
Kirsten Fraedrich
Andrea Cara
Markus Hoffmann
Stefan Pöhlmann
Armin Ensser
Cordula Pertl
Torsten Willert
Christian Thirion
Thomas Grunwald
Klaus Überla
Matthias Tenbusch
机构
[1] University Hospital Erlangen,Institute of Clinical and Molecular Virology
[2] Friedrich-Alexander University Erlangen-Nürnberg,Department of Immunology
[3] Fraunhofer Institute for Cell Therapy and Immunology,National Center for Global Health
[4] IZI,Infection Biology Unit
[5] Fraunhofer Cluster of Excellence Immune-mediated Diseases CIMD,Faculty of Biology and Psychology
[6] Istituto Superiore di Sanità,undefined
[7] German Primate Center-Leibniz Institute for Primate Research,undefined
[8] Georg-August-University Göttingen,undefined
[9] Sirion Biotech,undefined
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摘要
Several effective SARS-CoV-2 vaccines are currently in use, but effective boosters are needed to maintain or increase immunity due to waning responses and the emergence of novel variants. Here we report that intranasal vaccinations with adenovirus 5 and 19a vectored vaccines following a systemic plasmid DNA or mRNA priming result in systemic and mucosal immunity in mice. In contrast to two intramuscular applications of an mRNA vaccine, intranasal boosts with adenoviral vectors induce high levels of mucosal IgA and lung-resident memory T cells (TRM); mucosal neutralization of virus variants of concern is also enhanced. The mRNA prime provokes a comprehensive T cell response consisting of circulating and lung TRM after the boost, while the plasmid DNA prime induces mostly mucosal T cells. Concomitantly, the intranasal boost strategies lead to complete protection against a SARS-CoV-2 infection in mice. Our data thus suggest that mucosal booster immunizations after mRNA priming is a promising approach to establish mucosal immunity in addition to systemic responses.
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