Prior flavivirus immunity skews the yellow fever vaccine response to cross-reactive antibodies with potential to enhance dengue virus infection

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作者
Antonio Santos-Peral
Fabian Luppa
Sebastian Goresch
Elena Nikolova
Magdalena Zaucha
Lisa Lehmann
Frank Dahlstroem
Hadi Karimzadeh
Julia Thorn-Seshold
Elena Winheim
Ev-Marie Schuster
Gerhard Dobler
Michael Hoelscher
Beate M. Kümmerer
Stefan Endres
Kilian Schober
Anne B. Krug
Michael Pritsch
Giovanna Barba-Spaeth
Simon Rothenfusser
机构
[1] LMU University Hospital,Division of Clinical Pharmacology
[2] LMU Munich,Division of Infectious Diseases and Tropical Medicine
[3] LMU University Hospital,Department of Veterinary Sciences
[4] LMU Munich,Faculty of Chemistry and Pharmacy
[5] LMU Munich,Institute for Immunology, Biomedical Center (BMC)
[6] LMU Munich,Mikrobiologisches Institut–Klinische Mikrobiologie, Immunologie und Hygiene
[7] Medical Faculty,German Centre for Infection Research
[8] LMU Munich,Fraunhofer Institute for Translational Medicine and Pharmacology
[9] Universitätsklinikum Erlangen,Institute of Virology, Medical Faculty
[10] Friedrich-Alexander Universität Erlangen-Nürnberg,German Centre for Infection Research
[11] Bundeswehr Institute of Microbiology,FAU Profile Center Immunomedicine
[12] Partner Site Munich,Institut Pasteur
[13] Immunology,undefined
[14] Infection and Pandemic Research,undefined
[15] University of Bonn,undefined
[16] Partner Site Bonn-Cologne,undefined
[17] Einheit für Klinische Pharmakologie (EKLiP) Helmholtz Zentrum München German Research Center for Environmental Health (HMGU),undefined
[18] FAU Erlangen-Nürnberg,undefined
[19] Université Paris Cité,undefined
[20] CNRS UMR 3569,undefined
[21] Unité de Virologie Structurale,undefined
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摘要
The yellow fever 17D vaccine (YF17D) is highly effective but is frequently administered to individuals with pre-existing cross-reactive immunity, potentially impacting their immune responses. Here, we investigate the impact of pre-existing flavivirus immunity induced by the tick-borne encephalitis virus (TBEV) vaccine on the response to YF17D vaccination in 250 individuals up to 28 days post-vaccination (pv) and 22 individuals sampled one-year pv. Our findings indicate that previous TBEV vaccination does not affect the early IgM-driven neutralizing response to YF17D. However, pre-vaccination sera enhance YF17D virus infection in vitro via antibody-dependent enhancement (ADE). Following YF17D vaccination, TBEV-pre-vaccinated individuals develop high amounts of cross-reactive IgG antibodies with poor neutralizing capacity. In contrast, TBEV-unvaccinated individuals elicit a non-cross-reacting neutralizing response. Using YF17D envelope protein mutants displaying different epitopes, we identify quaternary dimeric epitopes as the primary target of neutralizing antibodies. Additionally, TBEV-pre-vaccination skews the IgG response towards the pan-flavivirus fusion loop epitope (FLE), capable of mediating ADE of dengue and Zika virus infections in vitro. Together, we propose that YF17D vaccination conceals the FLE in individuals without prior flavivirus exposure but favors a cross-reactive IgG response in TBEV-pre-vaccinated recipients directed to the FLE with potential to enhance dengue virus infection.
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