Back to Search Start Over

Dendritic cells drive profibrotic inflammation and aberrant T cell polarization in systemic sclerosis

Authors :
Jose Alberto, Choreño-Parra
Diana, Cervantes-Rosete
Luis Armando, Jiménez-Alvarez
Gustavo, Ramírez-Martínez
Jose Eduardo, Márquez-García
Alfredo, Cruz-Lagunas
Ana Yelli, Magaña-Sanchez
Guadalupe, Lima
Humberto, López-Maldonado
Emanuel, Gaytán-Guzmán
Adrian, Caballero
Rosario, Fernández-Plata
Janette, Furuzawa-Carballeda
Criselda, Mendoza-Milla
Maria Del Carmen, Navarro-González
Luis, Llorente
Joaquin, Zuniga
Tatiana Sofia, Rodriguez-Reyna
Source :
Rheumatology. 62:1687-1698
Publication Year :
2022
Publisher :
Oxford University Press (OUP), 2022.

Abstract

Objectives SSc is a devastating autoimmune disease characterized by fibrosis and obliterative vasculopathy affecting the skin and visceral organs. While the processes mediating excessive extracellular matrix deposition and fibroblast proliferation are clear, the exact link between autoimmunity and fibrosis remains elusive. Th17 cells have been proposed as critical drivers of profibrotic inflammation during SSc, but little is known about the immune components supporting their pathogenic role. Our aim was to determine cytokine responses of stimulated monocyte-derived dendritic cells (Mo-DCs) and to determine how they influence T-cell cytokine production in SSc. Material and methods Dendritic cells (DCs) activate and shape T cell differentiation by producing polarizing cytokines. Hence, we investigated the cytokine responses of monocyte-derived DCs (Mo-DCs) from patients with limited cutaneous SSc (lcSSc), diffuse cutaneous SSc (dcSSc) and healthy controls (HCs) after stimulation with toll-like receptor (TLR) agonists. Also, using co-culture assays, we analysed T cell subpopulations after contact with autologous TLR-activated Mo-DCs. Results In general, we observed an increased production of Th17-related cytokines like IL-1β, IL-17F, IL-21 and IL-22 by SSc compared with HC Mo-DCs, with variations between lcSSc vs dcSSc and early- vs late-stage subgroups. Noticeably, we found a significant increment in IL-33 production by Mo-DCs in all SSc cases regardless of their clinical phenotype. Strikingly, T cells displayed Th2, Th17 and dual Th2–Th17 phenotypes after exposure to autologous TLR-stimulated Mo-DCs from SSc patients but not HCs. These changes were pronounced in individuals with early-stage dcSSc and less significant in the late-stage lcSSc subgroup. Conclusions Our findings suggest that functional alterations of DCs promote immune mechanisms favouring the aberrant T cell polarization and profibrotic inflammation behind clinical SSc heterogeneity.

Details

ISSN :
14620332 and 14620324
Volume :
62
Database :
OpenAIRE
Journal :
Rheumatology
Accession number :
edsair.doi.dedup.....88fdc476e435f85383da86a7f8e34c6c