Boosting compromised SARS-CoV-2-specific immunity with mRNA vaccination in liver transplant recipients

Liver transplant recipients (LTRs) demonstrate a reduced response to COVID-19 mRNA vaccination; however, a detailed understanding of the interplay between humoral and cellular immunity, especially after a third (and fourth) vaccine dose, is lacking. We longitudinally compared the humoral, as well as...

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Veröffentlicht in:Journal of hepatology 2023-05, Vol.78 (5), p.1017-1027
Hauptverfasser: Luxenburger, Hendrik, Reeg, David B., Lang-Meli, Julia, Reinscheid, Matthias, Eisner, Miriam, Bettinger, Dominik, Oberhardt, Valerie, Salimi Alizei, Elahe, Wild, Katharina, Graeser, Anne, Karl, Vivien, Sagar, Emmerich, Florian, Klein, Florian, Panning, Marcus, Huzly, Daniela, Bengsch, Bertram, Boettler, Tobias, Elling, Roland, Thimme, Robert, Hofmann, Maike, Neumann-Haefelin, Christoph
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container_end_page 1027
container_issue 5
container_start_page 1017
container_title Journal of hepatology
container_volume 78
creator Luxenburger, Hendrik
Reeg, David B.
Lang-Meli, Julia
Reinscheid, Matthias
Eisner, Miriam
Bettinger, Dominik
Oberhardt, Valerie
Salimi Alizei, Elahe
Wild, Katharina
Graeser, Anne
Karl, Vivien
Sagar
Emmerich, Florian
Klein, Florian
Panning, Marcus
Huzly, Daniela
Bengsch, Bertram
Boettler, Tobias
Elling, Roland
Thimme, Robert
Hofmann, Maike
Neumann-Haefelin, Christoph
description Liver transplant recipients (LTRs) demonstrate a reduced response to COVID-19 mRNA vaccination; however, a detailed understanding of the interplay between humoral and cellular immunity, especially after a third (and fourth) vaccine dose, is lacking. We longitudinally compared the humoral, as well as CD4+ and CD8+ T-cell, responses between LTRs (n = 24) and healthy controls (n = 19) after three (LTRs: n = 9 to 16; healthy controls: n = 9 to 14 per experiment) to four (LTRs: n = 4; healthy controls: n = 4) vaccine doses, including in-depth phenotypical and functional characterization. Compared to healthy controls, development of high antibody titers required a third vaccine dose in most LTRs, while spike-specific CD8+ T cells with robust recall capacity plateaued after the second vaccine dose, albeit with a reduced frequency and epitope repertoire compared to healthy controls. This overall attenuated vaccine response was linked to a reduced frequency of spike-reactive follicular T helper cells in LTRs. Three doses of a COVID-19 mRNA vaccine induce an overall robust humoral and cellular memory response in most LTRs. Decisions regarding additional booster doses may thus be based on individual vaccine responses as well as evolution of novel variants of concern. Due to immunosuppressive medication, liver transplant recipients (LTR) display reduced antibody titers upon COVID-19 mRNA vaccination, but the impact on long-term immune memory is not clear. Herein, we demonstrate that after three vaccine doses, the majority of LTRs not only exhibit substantial antibody titers, but also a robust memory T-cell response. Additional booster vaccine doses may be of special benefit for a small subset of LTRs with inferior vaccine response and may provide superior protection against evolving novel viral variants. These findings will help physicians to guide LTRs regarding the benefit of booster vaccinations. [Display omitted] •Narrower CD8+ T-cell repertoire in liver transplant recipients vs. healthy controls after three vaccine doses.•Reduced frequencies of spike-specific CD8+ T cells in liver transplant recipients vs. healthy controls after three vaccine doses.•Formation of a functional CD8+ T-cell memory pool after vaccination in liver transplant recipients.•Altered subset distribution of CD4+ T cells after vaccination in liver transplant recipients.•A third mRNA shot significantly improves antibody responses in liver transplant recipients.
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Decisions regarding additional booster doses may thus be based on individual vaccine responses as well as evolution of novel variants of concern. Due to immunosuppressive medication, liver transplant recipients (LTR) display reduced antibody titers upon COVID-19 mRNA vaccination, but the impact on long-term immune memory is not clear. Herein, we demonstrate that after three vaccine doses, the majority of LTRs not only exhibit substantial antibody titers, but also a robust memory T-cell response. Additional booster vaccine doses may be of special benefit for a small subset of LTRs with inferior vaccine response and may provide superior protection against evolving novel viral variants. These findings will help physicians to guide LTRs regarding the benefit of booster vaccinations. 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subjects Antibodies, Viral
COVID-19
COVID-19 - prevention & control
COVID-19 Vaccines
Humans
Immunity, Cellular
immunological memory
immunosuppression
Liver Transplantation
RNA, Messenger - genetics
SARS-CoV-2
Transplant Recipients
Vaccination
vaccine response
title Boosting compromised SARS-CoV-2-specific immunity with mRNA vaccination in liver transplant recipients
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