THU0207 HELPER AND CYTOTOXIC FOLLICULAR T-CELLS IN SJÖGREN’S SYNDROME

Abstract

Background: Follicular T-cells, characterized by the expression of CXCR5, secrete interleukin 21 (IL-21) and help B-cell differentiation in lymphoid follicles. They are also found in circulation and may play a key role in Sjogren’s syndrome’s (pSS) chronic autoimmune epithelitis. Objectives: To characterize circulating follicular helper (Tfh) and cytotoxic (Tfc) T-cells in peripheral blood (PB) from pSS patients, Rheumatoid Arthritis (RA) patients and healthy controls (HC), and to investigate how they correlate with B-cell subsets. We also aimed to explore associations between the Tfh and Tfc cells and clinical and laboratory features of pSS. Methods: PB from 57 pSS patients, 20 RA patients and 24 HC was analysed by flow cytometry to characterize T and B-cell subsets, with CXCR5 defining Tfh and Tfc within CD4 and CD8 T cells, respectively. A stimulation assay was used to assess the production of IL-21 by CD4+ and CD8+ T-cells. Results: Compared to HC, pSS and RA patients presented significantly lower lymphocyte absolute counts (1615 and 1935 cells/μL respectively, compared to 2228 cells/μL in HC, p pSS patients presented lower absolute counts of CXCR5+ Tfh compared to RA (134 vs 181 cells/μL, p=0.038) and HC (134 vs 241 cells/μL, p pSS patients exhibited higher percentages of IL21+CD4 and IL21+CD8 T cells (IL21+CD4 T cells: 12.4% in pSS vs 9.0% in RA, p=0.046; vs 9.7% in HC, p=0.028; IL21+CD8 T cells: 4.1% in pSS vs 2.3% in RA, p=0.001; vs 2.8% in HC, p=0.030). In pSS patients, CXCR5+ Tfh correlated positively with the percentages of plasmablasts (r=0.262 for CD24-CD38++ cells, and r=0.282 for IgM-/+CD38++ cells). IL21+CD8 T cells correlated positively with the Naive/Memory B cells ratio (r=0.323; p=0.014) and negatively with Bm1 memory B cells (r=-0.370; p=0.005). IL21+CD4 T cells behaved similarly, though without statistical significance. Anti-SSA-positive patients (n=38) presented higher CD4+IL21+(13.3 vs 8.5%, p=0.025) and CD8+IL21+ cells percentages (4.4 vs 4.0%, p=0.198) than SSA-negative patients (n=19). Although there were no differences between pSS patients with active (n=27) and inactive disease (n=30), a tendency for positive correlations was found between IL-21+CD4 and IL21+CD8 T-cells and the ESSDAI score (r= 0.229, p=0.086 for CD4, r= 0.223, p=0.096 for CD8). Moreover, ESSDAI correlated positively with the Tfh1/Tfh17 ratio. Conclusion: pSS patients present a profile of circulating Tfh and Tfc distinct from RA and HC, both phenotypically and functionally. Moreover, our data support a crucial role for these cells in B cell development, as they correlate with B cells, in pSS patients, which are known to exhibit a typical circulating B cell compartment. Both Tfc and Tfh cells can be critical for disease pathophysiology and activity, as underlined by the correlations between these cells and ESSDAI scores. Disclosure of Interests: Filipe Barcelos Consultant for: Pfizer; Ely-Lilly, Speakers bureau: Novartis, Catarina Martins: None declared, Ricardo Monteiro: None declared, Carlos Geraldes: None declared, Ana Luisa Papoila: None declared, Joana Cardigos: None declared, Nathalie Madeira: None declared, Nuno Alves: None declared, Jose Vaz-Patto: None declared, Jaime Branco: None declared, Luis Miguel Borrego Grant/research support from: MSD, Consultant for: MSD; Tecnifar, Paid instructor for: MSD; AstraZeneca, Speakers bureau: MSD; Tecnifar; AstraZeneca