Literature DB >> 24529390

Increased levels of Th17 cells are associated with non-neuronal acetylcholine in COPD patients.

Mirella Profita1, Giusy Daniela Albano2, Loredana Riccobono3, Caterina Di Sano3, Angela Marina Montalbano3, Rosalia Gagliardo3, Giulia Anzalone3, Anna Bonanno3, Michael Paul Pieper4, Mark Gjomarkaj3.   

Abstract

T-lymphocytes, including Th17-cells and T-cells expressing acetylcholine (ACh), are key components of systemic inflammation in chronic obstructive pulmonary disease (COPD). We investigated whether ACh promotes Th17 cells in COPD. ACh, IL-17A, IL-22, RORγt, FOXP3 expression and AChIL-17A, AChIL-22, AChRORγt coexpression was evaluated in peripheral blood mononuclear cells (PBMC) from COPD patients (n=16), healthy smokers (HS) (n=12) and healthy control subjects (HC) (n=13) (cultured for 48 h with PMA) by flow cytometry. Furthermore, we studied the effect of Tiotropium (Spiriva®) (100 nM) and Olodaterol (1nM) alone or in combination, and of hemicholinium-3 (50 μM) on AChIL-17A, AChIL-22, AChRORγt, and FOXP3 expression in CD3+PBT-cells of PBMC from COPD patients (n=6) cultured for 48 h with PMA. CD3+PBT-cells expressing ACh, IL-17A, IL-22 and RORγt together with CD3+PBT-cells co-expressing AChIL-17A, AChIL-22 and AChRORγt were significantly increased in COPD patients compared to HC and HS subjects with higher levels in HS than in HC without a significant difference. CD3+FOXP3+PBT-cells were increased in HS than in HC and COPD. Tiotropium and Olodaterol reduced the percentage of CD3+PBT-cells co-expressing AChIL-17A, AChIL-22, and AChRORγt while increased the CD3+FOXP3+PBT-cells in PBMC from COPD patients, cultured in vitro for 48 h, with an additive effect when used in combination. Hemicholnium-3 reduced the percentage of ACh+IL-17A+, ACh+IL-22+, and ACh+RORγt+ while it did not affect FOXP3+ expression in CD3+PBT-cells from cultured PBMC from COPD patients. We concluded that ACh might promote the increased levels of Th17-cells in systemic inflammation of COPD. Long-acting β2-agonists and anticholinergic drugs might contribute to control this event.
Copyright © 2014 Elsevier GmbH. All rights reserved.

Entities:  

Keywords:  Anticholinergic drugs; Beta-2 long acting; Systemic inflammation; Th-17 cells

Mesh:

Substances:

Year:  2014        PMID: 24529390     DOI: 10.1016/j.imbio.2014.01.004

Source DB:  PubMed          Journal:  Immunobiology        ISSN: 0171-2985            Impact factor:   3.144


  13 in total

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Authors:  Angela Marina Montalbano; Giusy Daniela Albano; Anna Bonanno; Loredana Riccobono; Caterina Di Sano; Maria Ferraro; Liboria Siena; Giulia Anzalone; Rosalia Gagliardo; Michael Paul Pieper; Mark Gjomarkaj; Mirella Profita
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