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BNT162b2 vaccine induces antibody release in saliva: a possible role for mucosal viral protection?

Authors :
Abbass Darwich
Chiara Pozzi
Giulia Fornasa
Michela Lizier
Elena Azzolini
Ilaria Spadoni
Francesco Carli
Antonio Voza
Antonio Desai
Carlo Ferrero
Luca Germagnoli
ICH COVID‐19 Task‐force
Alberto Mantovani
Maria Rescigno
Aghemo Alessio
Anfray Clement
Badalamenti Salvatore
Belgiovine Cristina
Bertocchi Alice
Bombace Sara
Brescia Paola
Calcaterra Francesca
Calvi Michela
Cancellara Assunta
Capucetti Arianna
Carenza Claudia
Carloni Sara
Carnevale Silvia
Cazzetta Valentina
Cecconi Maurizio
Ciccarelli Michele
Coianiz Nicolò
Darwich Abbass
Ana Lleo De Nalda
De Paoli Federica
Di Donato Rachele
Digifico Elisabeth
Durante Barbara
Farina Floriana Maria
Ferrari Valentina
Fornasa Giulia
Franzese Sara
Gil Gomez Antonio
Giugliano Silvia
Ana Rita Gomes
Lizier Michela
Lo Cascio Antonino
Melacarne Alessia
Mozzarelli Alessandro
My Ilaria
Oresta Bianca
Pasqualini Fabio
Pastò Anna
Pelamatti Erica
Perucchini Chiara
Pozzi Chiara
Rimoldi Valeria
Rimoldi Monica
Scarpa Alice
Selmi Carlo
Silvestri Alessandra
Sironi Marina
Spadoni Ilaria
Spano' Salvatore
Spata Gianmarco
Supino Domenico
Tentorio Paolo
Ummarino Aldo
Valentino Sonia
Voza Antonio
Zaghi Elisa
Zanon Veronica
Source :
EMBO Molecular Medicine, Vol 14, Iss 5, Pp 1-9 (2022)
Publication Year :
2022
Publisher :
Springer Nature, 2022.

Abstract

Abstract Vaccination against an airborne pathogen is very effective if it induces also the development of mucosal antibodies that can protect against infection. The mRNA‐based vaccine‐encoding SARS‐CoV‐2 full‐length spike protein (BNT162b2, Pfizer/BioNTech) protects also against infection despite being administered systemically. Here, we show that upon vaccination, cognate IgG molecules are also found in the saliva and are more abundant in SARS‐CoV‐2 previously exposed subjects, paralleling the development of plasma IgG. The antibodies titer declines at 3 months from vaccination. We identified a concentration of specific IgG in the plasma above which the relevant IgG can be detected in the saliva. Regarding IgA antibodies, we found only protease‐susceptible IgA1 antibodies in plasma while they were present at very low levels in the saliva over the course of vaccination of SARS‐CoV‐2‐naïve subjects. Thus, in response to BNT162b2 vaccine, plasma IgG can permeate into mucosal sites and participate in viral protection. It is not clear why IgA1 are detected in low amount, they may be proteolytically cleaved.

Subjects

Subjects :
BNT162b2
IgA
IgG
mucosal immunity
SARS‐CoV‐2
Medicine (General)
R5-920
Genetics
QH426-470

Details

Language :
English
ISSN :
17574676 and 17574684
Volume :
14
Issue :
5
Database :
Directory of Open Access Journals
Journal :
EMBO Molecular Medicine
Publication Type :
Academic Journal
Accession number :
edsdoj.14c45332365a4e8394c289e662be5d7d
Document Type :
article
Full Text :
https://doi.org/10.15252/emmm.202115326
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