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Increased neutralization and IgG epitope identification after MVA-MERS-S booster vaccination against Middle East respiratory syndrome
Publikationstyp
Journal Article
Date Issued
2022-12-01
Sprache
English
Author(s)
Krähling, Verena
Kupke, Alexandra
Okba, Nisreen M.A.
Raadsen, Matthijs P.
Müller, Marcel A.
Lassen, Susan
Klüver, Michael
Ly, My L.
Fux, Robert
Tscherne, Alina
Kalodimou, Georgia
Corman, Victor M.
Hesterkamp, Thomas
Haagmans, Bart L.
Journal
Volume
13
Issue
1
Article Number
4182
Citation
Nature Communications 13 (1): 4182 (2022)
Publisher DOI
Scopus ID
Vaccine development is essential for pandemic preparedness. We previously conducted a Phase 1 clinical trial of the vector vaccine candidate MVA-MERS-S against the Middle East respiratory syndrome coronavirus (MERS-CoV), expressing its full spike glycoprotein (MERS-CoV-S), as a homologous two-dose regimen (Days 0 and 28). Here, we evaluate the safety (primary objective) and immunogenicity (secondary and exploratory objectives: magnitude and characterization of vaccine-induced humoral responses) of a third vaccination with MVA-MERS-S in a subgroup of trial participants one year after primary immunization. MVA-MERS-S booster vaccination is safe and well-tolerated. Both binding and neutralizing anti-MERS-CoV antibody titers increase substantially in all participants and exceed maximum titers observed after primary immunization more than 10-fold. We identify four immunogenic IgG epitopes, located in the receptor-binding domain (RBD, n = 1) and the S2 subunit (n = 3) of MERS-CoV-S. The level of baseline anti-human coronavirus antibody titers does not impact the generation of anti-MERS-CoV antibody responses. Our data support the rationale of a booster vaccination with MVA-MERS-S and encourage further investigation in larger trials.
DDC Class
600: Technology