Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations

The progressive lung destruction in cystic fibrosis (CF) is tightly associated with chronic bacterial infection and neutrophil-dominated airway inflammation. CF pulmonary disease is complicated by episodes of acute exacerbations, contributing to irreversible lung damage. We hypothesized that circula...

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Autores principales: Martin, Clémence, Dhôte, Théo, Ladjemi, Maha Zohra, Andrieu, Muriel, Many, Souganya, Karunanithy, Vaarany, Pène, Frédéric, Da Silva, Jennifer, Burgel, Pierre-Régis, Witko-Sarsat, Véronique
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9560797/
https://www.ncbi.nlm.nih.gov/pubmed/36248793
http://dx.doi.org/10.3389/fimmu.2022.1012310
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author Martin, Clémence
Dhôte, Théo
Ladjemi, Maha Zohra
Andrieu, Muriel
Many, Souganya
Karunanithy, Vaarany
Pène, Frédéric
Da Silva, Jennifer
Burgel, Pierre-Régis
Witko-Sarsat, Véronique
author_facet Martin, Clémence
Dhôte, Théo
Ladjemi, Maha Zohra
Andrieu, Muriel
Many, Souganya
Karunanithy, Vaarany
Pène, Frédéric
Da Silva, Jennifer
Burgel, Pierre-Régis
Witko-Sarsat, Véronique
author_sort Martin, Clémence
collection PubMed
description The progressive lung destruction in cystic fibrosis (CF) is tightly associated with chronic bacterial infection and neutrophil-dominated airway inflammation. CF pulmonary disease is complicated by episodes of acute exacerbations, contributing to irreversible lung damage. We hypothesized that circulating subsets of neutrophils from clinically stable adults with CF present some phenotypic specificities that could amplify their activation during an infectious episode. The aim of the present study was to examine the different neutrophil subsets in whole blood and in the low density neutrophils (LDN) that co-purify with peripheral blood mononuclear cells (PBMC) in clinically stable adults with CF and in CF adults during pulmonary exacerbations compared to healthy donors. Blood samples were obtained from 22 adults with CF (16 in stable state and 6 during pulmonary exacerbations) and from 20 healthy donors. Flow cytometry analysis of 13 different markers related to lineage (CD45, CD15), maturity (CD16, CD10, and CD33), activation (CD62L, CD11b, CD66b, and CD114), metabolism (GLUT-1, LOX1) and immunosuppression (PD1, PD-L1) was carried out within whole blood and within the LDN fraction. Unsupervised analysis of flow cytometry data was performed using visual t-distributed stochastic neighbor embedding (vi-tSNE). A significant increase in the CD11b expression in neutrophils from CF patients during exacerbations was observed compared to neutrophils from stable CF patients or to healthy donors, indicative of a circulating activation state due to an infectious status. The percentage of LDN was not increased in stable CF patients but increased during exacerbations. Analysis of neutrophil subsets using the double CD16/CD62L labeling revealed a significant increase in the CD16(high)/CD62L(low) subset in all CF patients compared to healthy donors. In contrast, an increase in the CD16(low)/CD62L(high) subset was observed only in CF patients during exacerbations. Unsupervised analysis identified a PD-L1(high)/CD114(high) population that was present in stable CF patients and as well as in CF patients during exacerbations.
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spelling pubmed-95607972022-10-14 Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations Martin, Clémence Dhôte, Théo Ladjemi, Maha Zohra Andrieu, Muriel Many, Souganya Karunanithy, Vaarany Pène, Frédéric Da Silva, Jennifer Burgel, Pierre-Régis Witko-Sarsat, Véronique Front Immunol Immunology The progressive lung destruction in cystic fibrosis (CF) is tightly associated with chronic bacterial infection and neutrophil-dominated airway inflammation. CF pulmonary disease is complicated by episodes of acute exacerbations, contributing to irreversible lung damage. We hypothesized that circulating subsets of neutrophils from clinically stable adults with CF present some phenotypic specificities that could amplify their activation during an infectious episode. The aim of the present study was to examine the different neutrophil subsets in whole blood and in the low density neutrophils (LDN) that co-purify with peripheral blood mononuclear cells (PBMC) in clinically stable adults with CF and in CF adults during pulmonary exacerbations compared to healthy donors. Blood samples were obtained from 22 adults with CF (16 in stable state and 6 during pulmonary exacerbations) and from 20 healthy donors. Flow cytometry analysis of 13 different markers related to lineage (CD45, CD15), maturity (CD16, CD10, and CD33), activation (CD62L, CD11b, CD66b, and CD114), metabolism (GLUT-1, LOX1) and immunosuppression (PD1, PD-L1) was carried out within whole blood and within the LDN fraction. Unsupervised analysis of flow cytometry data was performed using visual t-distributed stochastic neighbor embedding (vi-tSNE). A significant increase in the CD11b expression in neutrophils from CF patients during exacerbations was observed compared to neutrophils from stable CF patients or to healthy donors, indicative of a circulating activation state due to an infectious status. The percentage of LDN was not increased in stable CF patients but increased during exacerbations. Analysis of neutrophil subsets using the double CD16/CD62L labeling revealed a significant increase in the CD16(high)/CD62L(low) subset in all CF patients compared to healthy donors. In contrast, an increase in the CD16(low)/CD62L(high) subset was observed only in CF patients during exacerbations. Unsupervised analysis identified a PD-L1(high)/CD114(high) population that was present in stable CF patients and as well as in CF patients during exacerbations. Frontiers Media S.A. 2022-09-29 /pmc/articles/PMC9560797/ /pubmed/36248793 http://dx.doi.org/10.3389/fimmu.2022.1012310 Text en Copyright © 2022 Martin, Dhôte, Ladjemi, Andrieu, Many, Karunanithy, Pène, Da Silva, Burgel and Witko-Sarsat 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
Martin, Clémence
Dhôte, Théo
Ladjemi, Maha Zohra
Andrieu, Muriel
Many, Souganya
Karunanithy, Vaarany
Pène, Frédéric
Da Silva, Jennifer
Burgel, Pierre-Régis
Witko-Sarsat, Véronique
Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title_full Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title_fullStr Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title_full_unstemmed Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title_short Specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
title_sort specific circulating neutrophils subsets are present in clinically stable adults with cystic fibrosis and are further modulated by pulmonary exacerbations
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9560797/
https://www.ncbi.nlm.nih.gov/pubmed/36248793
http://dx.doi.org/10.3389/fimmu.2022.1012310
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