Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study

Multiple sclerosis patients treated with anti-CD20 therapy (aCD20-MS) are considered especially vulnerable to complications from SARS-CoV-2 infection due to severe B-cell depletion with limited viral antigen-specific immunoglobulin production. Therefore, multiple vaccine doses as part of the primary...

Descripción completa

Detalles Bibliográficos
Autores principales: Alfonso-Dunn, Roberto, Lin, Jerry, Lei, Joyce, Liu, Jiayuan, Roche, Morgan, De Oliveira, Antonia, Raisingani, Amol, Kumar, Anjali, Kirschner, Vanessa, Feuer, Grant, Malin, Michaela, Sadiq, Saud A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10338057/
https://www.ncbi.nlm.nih.gov/pubmed/37449202
http://dx.doi.org/10.3389/fimmu.2023.1194671
_version_ 1785071547172519936
author Alfonso-Dunn, Roberto
Lin, Jerry
Lei, Joyce
Liu, Jiayuan
Roche, Morgan
De Oliveira, Antonia
Raisingani, Amol
Kumar, Anjali
Kirschner, Vanessa
Feuer, Grant
Malin, Michaela
Sadiq, Saud A.
author_facet Alfonso-Dunn, Roberto
Lin, Jerry
Lei, Joyce
Liu, Jiayuan
Roche, Morgan
De Oliveira, Antonia
Raisingani, Amol
Kumar, Anjali
Kirschner, Vanessa
Feuer, Grant
Malin, Michaela
Sadiq, Saud A.
author_sort Alfonso-Dunn, Roberto
collection PubMed
description Multiple sclerosis patients treated with anti-CD20 therapy (aCD20-MS) are considered especially vulnerable to complications from SARS-CoV-2 infection due to severe B-cell depletion with limited viral antigen-specific immunoglobulin production. Therefore, multiple vaccine doses as part of the primary vaccination series and booster updates have been recommended for this group of immunocompromised individuals. Even though much less studied than antibody-mediated humoral responses, T-cell responses play an important role against CoV-2 infection and are induced efficiently in vaccinated aCD20-MS patients. For individuals with such decoupled adaptive immunity, an understanding of the contribution of T-cell mediated immunity is essential to better assess protection against CoV-2 infection. Here, we present results from a prospective, single-center study for the assessment of humoral and cellular immune responses induced in aCD20-MS patients (203 donors/350 samples) compared to a healthy control group (43/146) after initial exposure to CoV-2 spike antigen and subsequent re-challenges. Low rates of seroconversion and RBD-hACE2 blocking activity were observed in aCD20-MS patients, even after multiple exposures (responders after 1st exposure = 17.5%; 2nd exposure = 29.3%). Regarding cellular immunity, an increase in the number of spike-specific monofunctional IFNγ(+)-, IL-2(+)-, and polyfunctional IFNγ(+)/IL-2(+)-secreting T-cells after 2nd exposure was found most noticeably in healthy controls. Nevertheless, a persistently higher T-cell response was detected in aCD20-MS patients compared to control individuals before and after re-exposure (mean fold increase in spike-specific IFNγ(+)-, IL-2(+)-, and IFNγ(+)/IL-2(+)-T cells before re-exposure = 3.9X, 3.6X, 3.5X/P< 0.001; after = 3.2X, 1.4X, 2.2X/P = 0.002, P = 0.05, P = 0.004). Moreover, cellular responses against sublineage BA.2 of the currently circulating omicron variant were maintained, to a similar degree, in both groups (15-30% T-cell response drop compared to ancestral). Overall, these results highlight the potential for a severely impaired humoral response in aCD20-MS patients even after multiple exposures, while still generating a strong T-cell response. Evaluating both humoral and cellular responses in vaccinated or infected MS patients on B-cell depletion therapy is essential to better assess individual correlations of immune protection and has implications for the design of future vaccines and healthcare strategies.
format Online
Article
Text
id pubmed-10338057
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-103380572023-07-13 Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study Alfonso-Dunn, Roberto Lin, Jerry Lei, Joyce Liu, Jiayuan Roche, Morgan De Oliveira, Antonia Raisingani, Amol Kumar, Anjali Kirschner, Vanessa Feuer, Grant Malin, Michaela Sadiq, Saud A. Front Immunol Immunology Multiple sclerosis patients treated with anti-CD20 therapy (aCD20-MS) are considered especially vulnerable to complications from SARS-CoV-2 infection due to severe B-cell depletion with limited viral antigen-specific immunoglobulin production. Therefore, multiple vaccine doses as part of the primary vaccination series and booster updates have been recommended for this group of immunocompromised individuals. Even though much less studied than antibody-mediated humoral responses, T-cell responses play an important role against CoV-2 infection and are induced efficiently in vaccinated aCD20-MS patients. For individuals with such decoupled adaptive immunity, an understanding of the contribution of T-cell mediated immunity is essential to better assess protection against CoV-2 infection. Here, we present results from a prospective, single-center study for the assessment of humoral and cellular immune responses induced in aCD20-MS patients (203 donors/350 samples) compared to a healthy control group (43/146) after initial exposure to CoV-2 spike antigen and subsequent re-challenges. Low rates of seroconversion and RBD-hACE2 blocking activity were observed in aCD20-MS patients, even after multiple exposures (responders after 1st exposure = 17.5%; 2nd exposure = 29.3%). Regarding cellular immunity, an increase in the number of spike-specific monofunctional IFNγ(+)-, IL-2(+)-, and polyfunctional IFNγ(+)/IL-2(+)-secreting T-cells after 2nd exposure was found most noticeably in healthy controls. Nevertheless, a persistently higher T-cell response was detected in aCD20-MS patients compared to control individuals before and after re-exposure (mean fold increase in spike-specific IFNγ(+)-, IL-2(+)-, and IFNγ(+)/IL-2(+)-T cells before re-exposure = 3.9X, 3.6X, 3.5X/P< 0.001; after = 3.2X, 1.4X, 2.2X/P = 0.002, P = 0.05, P = 0.004). Moreover, cellular responses against sublineage BA.2 of the currently circulating omicron variant were maintained, to a similar degree, in both groups (15-30% T-cell response drop compared to ancestral). Overall, these results highlight the potential for a severely impaired humoral response in aCD20-MS patients even after multiple exposures, while still generating a strong T-cell response. Evaluating both humoral and cellular responses in vaccinated or infected MS patients on B-cell depletion therapy is essential to better assess individual correlations of immune protection and has implications for the design of future vaccines and healthcare strategies. Frontiers Media S.A. 2023-06-28 /pmc/articles/PMC10338057/ /pubmed/37449202 http://dx.doi.org/10.3389/fimmu.2023.1194671 Text en Copyright © 2023 Alfonso-Dunn, Lin, Lei, Liu, Roche, De Oliveira, Raisingani, Kumar, Kirschner, Feuer, Malin and Sadiq https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Alfonso-Dunn, Roberto
Lin, Jerry
Lei, Joyce
Liu, Jiayuan
Roche, Morgan
De Oliveira, Antonia
Raisingani, Amol
Kumar, Anjali
Kirschner, Vanessa
Feuer, Grant
Malin, Michaela
Sadiq, Saud A.
Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title_full Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title_fullStr Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title_full_unstemmed Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title_short Humoral and cellular responses to repeated COVID-19 exposure in multiple sclerosis patients receiving B-cell depleting therapies: a single-center, one-year, prospective study
title_sort humoral and cellular responses to repeated covid-19 exposure in multiple sclerosis patients receiving b-cell depleting therapies: a single-center, one-year, prospective study
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10338057/
https://www.ncbi.nlm.nih.gov/pubmed/37449202
http://dx.doi.org/10.3389/fimmu.2023.1194671
work_keys_str_mv AT alfonsodunnroberto humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT linjerry humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT leijoyce humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT liujiayuan humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT rochemorgan humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT deoliveiraantonia humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT raisinganiamol humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT kumaranjali humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT kirschnervanessa humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT feuergrant humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT malinmichaela humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy
AT sadiqsauda humoralandcellularresponsestorepeatedcovid19exposureinmultiplesclerosispatientsreceivingbcelldepletingtherapiesasinglecenteroneyearprospectivestudy

Ejemplares similares