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Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia

BACKGROUND: Functional dyspepsia is characterised by chronic symptoms of post-prandial distress or epigastric pain not associated with defined structural pathology. Increased peripheral gut-homing T cells have been previously identified in patients. To date, it is unknown if these T cells were antig...

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Autores principales: Burns, Grace L., Bruce, Jessica K., Minahan, Kyra, Mathe, Andrea, Fairlie, Thomas, Cameron, Raquel, Naudin, Crystal, Nair, Prema M., Potter, Michael D. E., Irani, Mudar Zand, Bollipo, Steven, Foster, Robert, Gan, Lay T., Shah, Ayesha, Koloski, Natasha A., Foster, Paul S., Horvat, Jay C., Veysey, Martin, Holtmann, Gerald, Powell, Nick, Walker, Marjorie M., Talley, Nicholas J., Keely, Simon
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9852875/
https://www.ncbi.nlm.nih.gov/pubmed/36685573
http://dx.doi.org/10.3389/fimmu.2022.1051632
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author Burns, Grace L.
Bruce, Jessica K.
Minahan, Kyra
Mathe, Andrea
Fairlie, Thomas
Cameron, Raquel
Naudin, Crystal
Nair, Prema M.
Potter, Michael D. E.
Irani, Mudar Zand
Bollipo, Steven
Foster, Robert
Gan, Lay T.
Shah, Ayesha
Koloski, Natasha A.
Foster, Paul S.
Horvat, Jay C.
Veysey, Martin
Holtmann, Gerald
Powell, Nick
Walker, Marjorie M.
Talley, Nicholas J.
Keely, Simon
author_facet Burns, Grace L.
Bruce, Jessica K.
Minahan, Kyra
Mathe, Andrea
Fairlie, Thomas
Cameron, Raquel
Naudin, Crystal
Nair, Prema M.
Potter, Michael D. E.
Irani, Mudar Zand
Bollipo, Steven
Foster, Robert
Gan, Lay T.
Shah, Ayesha
Koloski, Natasha A.
Foster, Paul S.
Horvat, Jay C.
Veysey, Martin
Holtmann, Gerald
Powell, Nick
Walker, Marjorie M.
Talley, Nicholas J.
Keely, Simon
author_sort Burns, Grace L.
collection PubMed
description BACKGROUND: Functional dyspepsia is characterised by chronic symptoms of post-prandial distress or epigastric pain not associated with defined structural pathology. Increased peripheral gut-homing T cells have been previously identified in patients. To date, it is unknown if these T cells were antigen-experienced, or if a specific phenotype was associated with FD. OBJECTIVE: This study aimed to characterise T cell populations in the blood and duodenal mucosa of FD patients that may be implicated in disease pathophysiology. METHODS: We identified duodenal T cell populations from 23 controls and 49 Rome III FD patients by flow cytometry using a surface marker antibody panel. We also analysed T cell populations in peripheral blood from 37 controls and 61 patients. Where available, we examined the number of duodenal eosinophils in patients and controls. RESULTS: There was a shift in the duodenal T helper cell balance in FD patients compared to controls. For example, patients had increased duodenal mucosal Th2 populations in the effector (13.03 ± 16.11, 19.84 ± 15.51, p=0.038), central memory (23.75 ± 18.97, 37.52 ± 17.51, p=0.007) and effector memory (9.80±10.50 vs 20.53±14.15, p=0.001) populations. Th17 populations were also increased in the effector (31.74±24.73 vs 45.57±23.75, p=0.03) and effector memory (11.95±8.42 vs 18.44±15.63, p=0.027) subsets. Peripheral T cell populations were unchanged between FD and control. CONCLUSION: Our findings identify an association between lymphocyte populations and FD, specifically a Th2 and Th17 signature in the duodenal mucosa. The presence of effector and memory cells suggest that the microinflammation in FD is antigen driven.
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spelling pubmed-98528752023-01-21 Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia Burns, Grace L. Bruce, Jessica K. Minahan, Kyra Mathe, Andrea Fairlie, Thomas Cameron, Raquel Naudin, Crystal Nair, Prema M. Potter, Michael D. E. Irani, Mudar Zand Bollipo, Steven Foster, Robert Gan, Lay T. Shah, Ayesha Koloski, Natasha A. Foster, Paul S. Horvat, Jay C. Veysey, Martin Holtmann, Gerald Powell, Nick Walker, Marjorie M. Talley, Nicholas J. Keely, Simon Front Immunol Immunology BACKGROUND: Functional dyspepsia is characterised by chronic symptoms of post-prandial distress or epigastric pain not associated with defined structural pathology. Increased peripheral gut-homing T cells have been previously identified in patients. To date, it is unknown if these T cells were antigen-experienced, or if a specific phenotype was associated with FD. OBJECTIVE: This study aimed to characterise T cell populations in the blood and duodenal mucosa of FD patients that may be implicated in disease pathophysiology. METHODS: We identified duodenal T cell populations from 23 controls and 49 Rome III FD patients by flow cytometry using a surface marker antibody panel. We also analysed T cell populations in peripheral blood from 37 controls and 61 patients. Where available, we examined the number of duodenal eosinophils in patients and controls. RESULTS: There was a shift in the duodenal T helper cell balance in FD patients compared to controls. For example, patients had increased duodenal mucosal Th2 populations in the effector (13.03 ± 16.11, 19.84 ± 15.51, p=0.038), central memory (23.75 ± 18.97, 37.52 ± 17.51, p=0.007) and effector memory (9.80±10.50 vs 20.53±14.15, p=0.001) populations. Th17 populations were also increased in the effector (31.74±24.73 vs 45.57±23.75, p=0.03) and effector memory (11.95±8.42 vs 18.44±15.63, p=0.027) subsets. Peripheral T cell populations were unchanged between FD and control. CONCLUSION: Our findings identify an association between lymphocyte populations and FD, specifically a Th2 and Th17 signature in the duodenal mucosa. The presence of effector and memory cells suggest that the microinflammation in FD is antigen driven. Frontiers Media S.A. 2023-01-06 /pmc/articles/PMC9852875/ /pubmed/36685573 http://dx.doi.org/10.3389/fimmu.2022.1051632 Text en Copyright © 2023 Burns, Bruce, Minahan, Mathe, Fairlie, Cameron, Naudin, Nair, Potter, Irani, Bollipo, Foster, Gan, Shah, Koloski, Foster, Horvat, Veysey, Holtmann, Powell, Walker, Talley and Keely 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
Burns, Grace L.
Bruce, Jessica K.
Minahan, Kyra
Mathe, Andrea
Fairlie, Thomas
Cameron, Raquel
Naudin, Crystal
Nair, Prema M.
Potter, Michael D. E.
Irani, Mudar Zand
Bollipo, Steven
Foster, Robert
Gan, Lay T.
Shah, Ayesha
Koloski, Natasha A.
Foster, Paul S.
Horvat, Jay C.
Veysey, Martin
Holtmann, Gerald
Powell, Nick
Walker, Marjorie M.
Talley, Nicholas J.
Keely, Simon
Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title_full Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title_fullStr Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title_full_unstemmed Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title_short Type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
title_sort type 2 and type 17 effector cells are increased in the duodenal mucosa but not peripheral blood of patients with functional dyspepsia
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9852875/
https://www.ncbi.nlm.nih.gov/pubmed/36685573
http://dx.doi.org/10.3389/fimmu.2022.1051632
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