The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders

BACKGROUND: Vaccination against SARS-CoV-2 is a highly effective strategy to protect against infection, which is predominantly mediated by vaccine-induced antibodies. Postvaccination antibodies are robustly produced by those with inflammatory bowel disease (IBD) even on immune-modifying therapies bu...

Descripción completa

Detalles Bibliográficos
Autores principales: Li, Dalin, Xu, Alexander, Mengesha, Emebet, Elyanow, Rebecca, Gittelman, Rachel M., Chapman, Heidi, Prostko, John C., Frias, Edwin C., Stewart, James L., Pozdnyakova, Valeriya, Debbas, Philip, Mujukian, Angela, Horizon, Arash A, Merin, Noah, Joung, Sandy, Botwin, Gregory J., Sobhani, Kimia, Figueiredo, Jane C., Cheng, Susan, Kaplan, Ian M., McGovern, Dermot P.B., Merchant, Akil, Melmed, Gil Y., Braun, Jonathan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8669852/
https://www.ncbi.nlm.nih.gov/pubmed/34909785
http://dx.doi.org/10.1101/2021.12.08.21267444
_version_ 1784614862011236352
author Li, Dalin
Xu, Alexander
Mengesha, Emebet
Elyanow, Rebecca
Gittelman, Rachel M.
Chapman, Heidi
Prostko, John C.
Frias, Edwin C.
Stewart, James L.
Pozdnyakova, Valeriya
Debbas, Philip
Mujukian, Angela
Horizon, Arash A
Merin, Noah
Joung, Sandy
Botwin, Gregory J.
Sobhani, Kimia
Figueiredo, Jane C.
Cheng, Susan
Kaplan, Ian M.
McGovern, Dermot P.B.
Merchant, Akil
Melmed, Gil Y.
Braun, Jonathan
author_facet Li, Dalin
Xu, Alexander
Mengesha, Emebet
Elyanow, Rebecca
Gittelman, Rachel M.
Chapman, Heidi
Prostko, John C.
Frias, Edwin C.
Stewart, James L.
Pozdnyakova, Valeriya
Debbas, Philip
Mujukian, Angela
Horizon, Arash A
Merin, Noah
Joung, Sandy
Botwin, Gregory J.
Sobhani, Kimia
Figueiredo, Jane C.
Cheng, Susan
Kaplan, Ian M.
McGovern, Dermot P.B.
Merchant, Akil
Melmed, Gil Y.
Braun, Jonathan
author_sort Li, Dalin
collection PubMed
description BACKGROUND: Vaccination against SARS-CoV-2 is a highly effective strategy to protect against infection, which is predominantly mediated by vaccine-induced antibodies. Postvaccination antibodies are robustly produced by those with inflammatory bowel disease (IBD) even on immune-modifying therapies but are blunted by anti-TNF therapy. In contrast, T-cell response which primarily determines long-term efficacy against disease progression, is less well understood. We aimed to assess the post-vaccination T-cell response and its relationship to antibody responses in patients with inflammatory bowel disease (IBD) on immune-modifying therapies. METHODS: We evaluated IBD patients who completed SARS-CoV-2 vaccination using samples collected at four time points (dose 1, dose 2, 2 weeks after dose 2, 8 weeks after dose 2). T-cell clonal analysis was performed by T-cell Receptor (TCR) immunosequencing. The breadth (number of unique sequences to a given protein) and depth (relative abundance of all the unique sequences to a given protein) of the T-cell clonal response were quantified using reference datasets and were compared to antibody responses. RESULTS: Overall, 303 subjects were included (55% female; 5% with prior COVID) (Table). 53% received BNT262b (Pfizer), 42% mRNA-1273 (Moderna) and 5% Ad26CoV2 (J&J). The Spike-specific clonal response peaked 2 weeks after completion of the vaccine regimen (3- and 5-fold for breadth and depth, respectively); no changes were seen for non-Spike clones, suggesting vaccine specificity. Reduced T-cell clonal depth was associated with chronologic age, male sex, and immunomodulator treatment. It was preserved by non-anti-TNF biologic therapies, and augmented clonal depth was associated with anti-TNF treatment. TCR depth and breadth were associated with vaccine type; after adjusting for age and gender, Ad26CoV2 (J&J) exhibited weaker metrics than mRNA-1273 (Moderna) (p=0.01 for each) or BNT262b (Pfizer) (p=0.056 for depth). Antibody and T-cell responses were only modestly correlated. While those with robust humoral responses also had robust TCR clonal expansion, a substantial fraction of patients with high antibody levels had only a minimal T-cell clonal response. CONCLUSION: Age, sex and select immunotherapies are associated with the T-cell clonal response to SARS-CoV-2 vaccines, and T-cell responses are low in many patients despite high antibody levels. These factors, as well as differences seen by vaccine type may help guide reimmunization vaccine strategy in immune-impaired populations. Further study of the effects of anti-TNF therapy on vaccine responses are warranted.
format Online
Article
Text
id pubmed-8669852
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Cold Spring Harbor Laboratory
record_format MEDLINE/PubMed
spelling pubmed-86698522021-12-15 The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders Li, Dalin Xu, Alexander Mengesha, Emebet Elyanow, Rebecca Gittelman, Rachel M. Chapman, Heidi Prostko, John C. Frias, Edwin C. Stewart, James L. Pozdnyakova, Valeriya Debbas, Philip Mujukian, Angela Horizon, Arash A Merin, Noah Joung, Sandy Botwin, Gregory J. Sobhani, Kimia Figueiredo, Jane C. Cheng, Susan Kaplan, Ian M. McGovern, Dermot P.B. Merchant, Akil Melmed, Gil Y. Braun, Jonathan medRxiv Article BACKGROUND: Vaccination against SARS-CoV-2 is a highly effective strategy to protect against infection, which is predominantly mediated by vaccine-induced antibodies. Postvaccination antibodies are robustly produced by those with inflammatory bowel disease (IBD) even on immune-modifying therapies but are blunted by anti-TNF therapy. In contrast, T-cell response which primarily determines long-term efficacy against disease progression, is less well understood. We aimed to assess the post-vaccination T-cell response and its relationship to antibody responses in patients with inflammatory bowel disease (IBD) on immune-modifying therapies. METHODS: We evaluated IBD patients who completed SARS-CoV-2 vaccination using samples collected at four time points (dose 1, dose 2, 2 weeks after dose 2, 8 weeks after dose 2). T-cell clonal analysis was performed by T-cell Receptor (TCR) immunosequencing. The breadth (number of unique sequences to a given protein) and depth (relative abundance of all the unique sequences to a given protein) of the T-cell clonal response were quantified using reference datasets and were compared to antibody responses. RESULTS: Overall, 303 subjects were included (55% female; 5% with prior COVID) (Table). 53% received BNT262b (Pfizer), 42% mRNA-1273 (Moderna) and 5% Ad26CoV2 (J&J). The Spike-specific clonal response peaked 2 weeks after completion of the vaccine regimen (3- and 5-fold for breadth and depth, respectively); no changes were seen for non-Spike clones, suggesting vaccine specificity. Reduced T-cell clonal depth was associated with chronologic age, male sex, and immunomodulator treatment. It was preserved by non-anti-TNF biologic therapies, and augmented clonal depth was associated with anti-TNF treatment. TCR depth and breadth were associated with vaccine type; after adjusting for age and gender, Ad26CoV2 (J&J) exhibited weaker metrics than mRNA-1273 (Moderna) (p=0.01 for each) or BNT262b (Pfizer) (p=0.056 for depth). Antibody and T-cell responses were only modestly correlated. While those with robust humoral responses also had robust TCR clonal expansion, a substantial fraction of patients with high antibody levels had only a minimal T-cell clonal response. CONCLUSION: Age, sex and select immunotherapies are associated with the T-cell clonal response to SARS-CoV-2 vaccines, and T-cell responses are low in many patients despite high antibody levels. These factors, as well as differences seen by vaccine type may help guide reimmunization vaccine strategy in immune-impaired populations. Further study of the effects of anti-TNF therapy on vaccine responses are warranted. Cold Spring Harbor Laboratory 2021-12-08 /pmc/articles/PMC8669852/ /pubmed/34909785 http://dx.doi.org/10.1101/2021.12.08.21267444 Text en https://creativecommons.org/licenses/by-nd/4.0/This work is licensed under a Creative Commons Attribution-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, and only so long as attribution is given to the creator. The license allows for commercial use.
spellingShingle Article
Li, Dalin
Xu, Alexander
Mengesha, Emebet
Elyanow, Rebecca
Gittelman, Rachel M.
Chapman, Heidi
Prostko, John C.
Frias, Edwin C.
Stewart, James L.
Pozdnyakova, Valeriya
Debbas, Philip
Mujukian, Angela
Horizon, Arash A
Merin, Noah
Joung, Sandy
Botwin, Gregory J.
Sobhani, Kimia
Figueiredo, Jane C.
Cheng, Susan
Kaplan, Ian M.
McGovern, Dermot P.B.
Merchant, Akil
Melmed, Gil Y.
Braun, Jonathan
The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title_full The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title_fullStr The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title_full_unstemmed The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title_short The T-cell clonal response to SARS-CoV-2 vaccination in inflammatory bowel disease patients is augmented by anti-TNF therapy and often deficient in antibody-responders
title_sort t-cell clonal response to sars-cov-2 vaccination in inflammatory bowel disease patients is augmented by anti-tnf therapy and often deficient in antibody-responders
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8669852/
https://www.ncbi.nlm.nih.gov/pubmed/34909785
http://dx.doi.org/10.1101/2021.12.08.21267444
work_keys_str_mv AT lidalin thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT xualexander thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mengeshaemebet thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT elyanowrebecca thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT gittelmanrachelm thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT chapmanheidi thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT prostkojohnc thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT friasedwinc thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT stewartjamesl thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT pozdnyakovavaleriya thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT debbasphilip thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mujukianangela thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT horizonarasha thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT merinnoah thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT joungsandy thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT botwingregoryj thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT sobhanikimia thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT figueiredojanec thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT chengsusan thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT kaplanianm thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mcgoverndermotpb thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT merchantakil thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT melmedgily thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT braunjonathan thetcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT lidalin tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT xualexander tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mengeshaemebet tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT elyanowrebecca tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT gittelmanrachelm tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT chapmanheidi tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT prostkojohnc tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT friasedwinc tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT stewartjamesl tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT pozdnyakovavaleriya tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT debbasphilip tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mujukianangela tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT horizonarasha tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT merinnoah tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT joungsandy tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT botwingregoryj tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT sobhanikimia tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT figueiredojanec tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT chengsusan tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT kaplanianm tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT mcgoverndermotpb tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT merchantakil tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT melmedgily tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders
AT braunjonathan tcellclonalresponsetosarscov2vaccinationininflammatoryboweldiseasepatientsisaugmentedbyantitnftherapyandoftendeficientinantibodyresponders

Ejemplares similares