Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection

Petra Mooij; Daniella Mortier; Aafke Aartse; Alexandre B. Murad; Ricardo Correia; António Roldão; Paula M. Alves; Zahra Fagrouch; Dirk Eggink; Norbert Stockhofe; Othmar G. Engelhardt; Ernst J. Verschoor; Marit J. van Gils; Willy M. Bogers; Manuel J. T. Carrondo; Edmond J. Remarque; Gerrit Koopman

doi:https://doi.org/10.3389/fimmu.2023.1256094

Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection

Petra Mooij, Daniella Mortier, Aafke Aartse, Alexandre B. Murad, Ricardo Correia, António Roldão, Paula M. Alves, Zahra Fagrouch, Dirk Eggink, Norbert Stockhofe, Othmar G. Engelhardt, Ernst J. Verschoor, Marit J. van Gils, Willy M. Bogers, Manuel J. T. Carrondo, Edmond J. Remarque, Gerrit Koopman

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

The first exposure to influenza is presumed to shape the B-cell antibody repertoire, leading to preferential enhancement of the initially formed responses during subsequent exposure to viral variants. Here, we investigated whether this principle remains applicable when there are large genetic and antigenic differences between primary and secondary influenza virus antigens. Because humans usually have a complex history of influenza virus exposure, we conducted this investigation in influenza-naive cynomolgus macaques. Two groups of six macaques were immunized four times with influenza virus-like particles (VLPs) displaying either one (monovalent) or five (pentavalent) different hemagglutinin (HA) antigens derived from seasonal H1N1 (H1N1) strains. Four weeks after the final immunization, animals were challenged with pandemic H1N1 (H1N1pdm09). Although immunization resulted in robust virus-neutralizing responses to all VLP-based vaccine strains, there were no cross-neutralization responses to H1N1pdm09, and all animals became infected. No reductions in viral load in the nose or throat were detected in either vaccine group. After infection, strong virus-neutralizing responses to H1N1pdm09 were induced. However, there were no increases in virus-neutralizing titers against four of the five H1N1 vaccine strains; and only a mild increase was observed in virus-neutralizing titer against the influenza A/Texas/36/91 vaccine strain. After H1N1pdm09 infection, both vaccine groups showed higher virus-neutralizing titers against two H1N1 strains of intermediate antigenic distance between the H1N1 vaccine strains and H1N1pdm09, compared with the naive control group. Furthermore, both vaccine groups had higher HA-stem antibodies early after infection than the control group. In conclusion, immunization with VLPs displaying HA from antigenically distinct H1N1 variants increased the breadth of the immune response during subsequent H1N1pdm09 challenge, although this phenomenon was limited to intermediate antigenic variants.

Original language	English
Article number	1256094
Journal	Frontiers in immunology
Volume	14
DOIs	https://doi.org/10.3389/fimmu.2023.1256094
Publication status	Published - 2023

Keywords

antibody response
back-boosting
influenza
non-human primates
original antigenic sin
primary response

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https://doi.org/10.3389/fimmu.2023.1256094

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Mooij, P., Mortier, D., Aartse, A., Murad, A. B., Correia, R., Roldão, A., Alves, P. M., Fagrouch, Z., Eggink, D., Stockhofe, N., Engelhardt, O. G., Verschoor, E. J., van Gils, M. J., Bogers, W. M., Carrondo, M. J. T., Remarque, E. J., & Koopman, G. (2023). Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection. Frontiers in immunology, 14, Article 1256094. https://doi.org/10.3389/fimmu.2023.1256094

@article{bb2e07c1e39b4dd5809e4585844375bb,

title = "Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection",

abstract = "The first exposure to influenza is presumed to shape the B-cell antibody repertoire, leading to preferential enhancement of the initially formed responses during subsequent exposure to viral variants. Here, we investigated whether this principle remains applicable when there are large genetic and antigenic differences between primary and secondary influenza virus antigens. Because humans usually have a complex history of influenza virus exposure, we conducted this investigation in influenza-naive cynomolgus macaques. Two groups of six macaques were immunized four times with influenza virus-like particles (VLPs) displaying either one (monovalent) or five (pentavalent) different hemagglutinin (HA) antigens derived from seasonal H1N1 (H1N1) strains. Four weeks after the final immunization, animals were challenged with pandemic H1N1 (H1N1pdm09). Although immunization resulted in robust virus-neutralizing responses to all VLP-based vaccine strains, there were no cross-neutralization responses to H1N1pdm09, and all animals became infected. No reductions in viral load in the nose or throat were detected in either vaccine group. After infection, strong virus-neutralizing responses to H1N1pdm09 were induced. However, there were no increases in virus-neutralizing titers against four of the five H1N1 vaccine strains; and only a mild increase was observed in virus-neutralizing titer against the influenza A/Texas/36/91 vaccine strain. After H1N1pdm09 infection, both vaccine groups showed higher virus-neutralizing titers against two H1N1 strains of intermediate antigenic distance between the H1N1 vaccine strains and H1N1pdm09, compared with the naive control group. Furthermore, both vaccine groups had higher HA-stem antibodies early after infection than the control group. In conclusion, immunization with VLPs displaying HA from antigenically distinct H1N1 variants increased the breadth of the immune response during subsequent H1N1pdm09 challenge, although this phenomenon was limited to intermediate antigenic variants.",

keywords = "antibody response, back-boosting, influenza, non-human primates, original antigenic sin, primary response",

author = "Petra Mooij and Daniella Mortier and Aafke Aartse and Murad, {Alexandre B.} and Ricardo Correia and Ant{\'o}nio Rold{\~a}o and Alves, {Paula M.} and Zahra Fagrouch and Dirk Eggink and Norbert Stockhofe and Engelhardt, {Othmar G.} and Verschoor, {Ernst J.} and {van Gils}, {Marit J.} and Bogers, {Willy M.} and Carrondo, {Manuel J. T.} and Remarque, {Edmond J.} and Gerrit Koopman",

note = "Funding Information: This work was supported by EU-funded project “EDUFLUVAC” (FP7-HEALTH-2013-INNOVATION-1, GA n. 602640), by Funda{\c c}{\~a}o para a Ci{\^e}ncia e Tecnologia/Minist{\'e}rio da Ci{\^e}ncia, Tecnologia e Ensino Superior (FCT/MCTES, Portugal) through several initiatives (iNOVA4Health (UIDB/04462/2020 and UIDP/04462/2020), Associate Laboratory LS4FUTURE (LA/P/0087/2020), “Investigador FCT” Program (IF/01704/2014), Exploratory Research and Development Project (IF/01704/2014/CP1229/CT0001), and PhD fellowship (Ricardo Correia-SFRH/BD/134107/2017)), and by PhD fellowship (Alexandre Murad-SWE program, CAPES 2000116/2016-9) and PVE program (CAPES 407565/2013-2) and internal funding by the BPRC. Acknowledgments Publisher Copyright: Copyright {\textcopyright} 2023 Mooij, Mortier, Aartse, Murad, Correia, Rold{\~a}o, Alves, Fagrouch, Eggink, Stockhofe, Engelhardt, Verschoor, van Gils, Bogers, Carrondo, Remarque and Koopman.",

year = "2023",

doi = "https://doi.org/10.3389/fimmu.2023.1256094",

language = "English",

volume = "14",

journal = "Frontiers in immunology",

issn = "1664-3224",

publisher = "Frontiers Media S.A.",

}

Mooij, P, Mortier, D, Aartse, A, Murad, AB, Correia, R, Roldão, A, Alves, PM, Fagrouch, Z, Eggink, D, Stockhofe, N, Engelhardt, OG, Verschoor, EJ, van Gils, MJ, Bogers, WM, Carrondo, MJT, Remarque, EJ & Koopman, G 2023, 'Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection', Frontiers in immunology, vol. 14, 1256094. https://doi.org/10.3389/fimmu.2023.1256094

TY - JOUR

T1 - Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection

AU - Mooij, Petra

AU - Mortier, Daniella

AU - Aartse, Aafke

AU - Murad, Alexandre B.

AU - Correia, Ricardo

AU - Roldão, António

AU - Alves, Paula M.

AU - Fagrouch, Zahra

AU - Eggink, Dirk

AU - Stockhofe, Norbert

AU - Engelhardt, Othmar G.

AU - Verschoor, Ernst J.

AU - van Gils, Marit J.

AU - Bogers, Willy M.

AU - Carrondo, Manuel J. T.

AU - Remarque, Edmond J.

AU - Koopman, Gerrit

N1 - Funding Information: This work was supported by EU-funded project “EDUFLUVAC” (FP7-HEALTH-2013-INNOVATION-1, GA n. 602640), by Fundação para a Ciência e Tecnologia/Ministério da Ciência, Tecnologia e Ensino Superior (FCT/MCTES, Portugal) through several initiatives (iNOVA4Health (UIDB/04462/2020 and UIDP/04462/2020), Associate Laboratory LS4FUTURE (LA/P/0087/2020), “Investigador FCT” Program (IF/01704/2014), Exploratory Research and Development Project (IF/01704/2014/CP1229/CT0001), and PhD fellowship (Ricardo Correia-SFRH/BD/134107/2017)), and by PhD fellowship (Alexandre Murad-SWE program, CAPES 2000116/2016-9) and PVE program (CAPES 407565/2013-2) and internal funding by the BPRC. Acknowledgments Publisher Copyright: Copyright © 2023 Mooij, Mortier, Aartse, Murad, Correia, Roldão, Alves, Fagrouch, Eggink, Stockhofe, Engelhardt, Verschoor, van Gils, Bogers, Carrondo, Remarque and Koopman.

PY - 2023

Y1 - 2023

N2 - The first exposure to influenza is presumed to shape the B-cell antibody repertoire, leading to preferential enhancement of the initially formed responses during subsequent exposure to viral variants. Here, we investigated whether this principle remains applicable when there are large genetic and antigenic differences between primary and secondary influenza virus antigens. Because humans usually have a complex history of influenza virus exposure, we conducted this investigation in influenza-naive cynomolgus macaques. Two groups of six macaques were immunized four times with influenza virus-like particles (VLPs) displaying either one (monovalent) or five (pentavalent) different hemagglutinin (HA) antigens derived from seasonal H1N1 (H1N1) strains. Four weeks after the final immunization, animals were challenged with pandemic H1N1 (H1N1pdm09). Although immunization resulted in robust virus-neutralizing responses to all VLP-based vaccine strains, there were no cross-neutralization responses to H1N1pdm09, and all animals became infected. No reductions in viral load in the nose or throat were detected in either vaccine group. After infection, strong virus-neutralizing responses to H1N1pdm09 were induced. However, there were no increases in virus-neutralizing titers against four of the five H1N1 vaccine strains; and only a mild increase was observed in virus-neutralizing titer against the influenza A/Texas/36/91 vaccine strain. After H1N1pdm09 infection, both vaccine groups showed higher virus-neutralizing titers against two H1N1 strains of intermediate antigenic distance between the H1N1 vaccine strains and H1N1pdm09, compared with the naive control group. Furthermore, both vaccine groups had higher HA-stem antibodies early after infection than the control group. In conclusion, immunization with VLPs displaying HA from antigenically distinct H1N1 variants increased the breadth of the immune response during subsequent H1N1pdm09 challenge, although this phenomenon was limited to intermediate antigenic variants.

AB - The first exposure to influenza is presumed to shape the B-cell antibody repertoire, leading to preferential enhancement of the initially formed responses during subsequent exposure to viral variants. Here, we investigated whether this principle remains applicable when there are large genetic and antigenic differences between primary and secondary influenza virus antigens. Because humans usually have a complex history of influenza virus exposure, we conducted this investigation in influenza-naive cynomolgus macaques. Two groups of six macaques were immunized four times with influenza virus-like particles (VLPs) displaying either one (monovalent) or five (pentavalent) different hemagglutinin (HA) antigens derived from seasonal H1N1 (H1N1) strains. Four weeks after the final immunization, animals were challenged with pandemic H1N1 (H1N1pdm09). Although immunization resulted in robust virus-neutralizing responses to all VLP-based vaccine strains, there were no cross-neutralization responses to H1N1pdm09, and all animals became infected. No reductions in viral load in the nose or throat were detected in either vaccine group. After infection, strong virus-neutralizing responses to H1N1pdm09 were induced. However, there were no increases in virus-neutralizing titers against four of the five H1N1 vaccine strains; and only a mild increase was observed in virus-neutralizing titer against the influenza A/Texas/36/91 vaccine strain. After H1N1pdm09 infection, both vaccine groups showed higher virus-neutralizing titers against two H1N1 strains of intermediate antigenic distance between the H1N1 vaccine strains and H1N1pdm09, compared with the naive control group. Furthermore, both vaccine groups had higher HA-stem antibodies early after infection than the control group. In conclusion, immunization with VLPs displaying HA from antigenically distinct H1N1 variants increased the breadth of the immune response during subsequent H1N1pdm09 challenge, although this phenomenon was limited to intermediate antigenic variants.

KW - antibody response

KW - back-boosting

KW - influenza

KW - non-human primates

KW - original antigenic sin

KW - primary response

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U2 - https://doi.org/10.3389/fimmu.2023.1256094

DO - https://doi.org/10.3389/fimmu.2023.1256094

M3 - Article

C2 - 37691927

SN - 1664-3224

VL - 14

JO - Frontiers in immunology

JF - Frontiers in immunology

M1 - 1256094

ER -

Vaccine-induced neutralizing antibody responses to seasonal influenza virus H1N1 strains are not enhanced during subsequent pandemic H1N1 infection

Abstract

Keywords

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