Abstract

BackgroundPro-inflammatory cytokines are directly implicated in the pathogenesis of Rheumatoid arthritis (RA). Variable clinical response to cytokine targeted therapies as TNFalpha and IL-6, strongly highlights the heterogeneity of inflammatory process in RA. Another cytokine, IL-15 has also been related to the inflammatory process in RA. Recently we described for the first time, the presence of its specific receptor, IL-15Ralpha, in synovial fluid (SF). The aim of this work was to compare the expression profile of IL-15Ralpha, its ligand IL-15, TNFalpha and IL-6 and how these cytokines are correlated in SF from RA patients taking as a reference Osteoarthritis (OA), an articular but not autoinmmune disease.MethodsSynovial fluids were obtained from the knee joints of 60 patients, 30 with confirmed diagnosis of RA and 30 with OA diagnosis. The levels of TNFalpha, IL-6, IL-15 and IL-15Ralpha were measured by ELISA. A statistical analysis was performed with GraphPad Prism v5.0 using the Mann–Whitney U test and Spearman’s rank correlation. A cluster analysis was run in MeV software v4.9.0 and differences across clusters were evaluated by an ANOVA including post-test analysis.ResultsWe found higher and significant levels of TNFalpha, IL-6 and IL-15Ralpha but not of IL-15 in RA compared with the OA group. Additionally, a high inter-individual variability in the levels of these 4 cytokines was observed in RA, although we identified 4 patients’ subgroups by cluster analysis of cytokines concentration in SF. We also found a positive correlation between IL-15Ralpha-IL-6 and IL-15Ralpha-IL-15, but not for other pairs of cytokines in RA. In addition we found correlation between the value of IL-15Ralpha in SF and disease activity score, DAS28.ConclusionsIn our current work we found a high inter-individual variability in the levels of TNFalpha, IL-6, IL-15 and IL-15Ralpha in SF of RA patients and were identified four principal clusters of cytokines concentration in SF, suggesting the importance of identifying disease subset of patients for personalized treatment. Finally, we found a correlation between IL-15Ralpha-IL-6, IL-15Ralpha-IL-15, but we did not find any correlation between other pairs of studied cytokines in SF.

Highlights

  • Pro-inflammatory cytokines are directly implicated in the pathogenesis of Rheumatoid arthritis (RA)

  • As a result we found a correlation between IL-15Ralpha and Disease Activity Score 28 (DAS28), but neither to ESR nor CRP. (Figure 4)

  • We found a correlation between IL-15Ralpha and DAS28 suggesting a relation between IL-15Ralpha level and disease activity

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Summary

Introduction

Pro-inflammatory cytokines are directly implicated in the pathogenesis of Rheumatoid arthritis (RA). IL-15Ralpha may be secreted as a functional soluble molecule (s-IL-15Ralpha) and could behave as antagonist or agonist by forming a complex with IL-15 [19,20,21], it has been described that soluble IL-15Ralpha could bind to membrane bound IL-15 to induce a reverse signaling mechanism up-regulating the production of IL-6, IL-8, and TNFalpha by human monocytes and in the cancer cell line PC-3 [22,23] These antecedents highlight the importance of this receptor in IL-15 biology and trigger previous studies of IL-15Ralpha in synovial fluids, where we have detected increasing levels of this receptor in synovial fluids from RA regards to OA [24]. We will assess inter-individual expression of these cytokines and will analyze how this cytokines are correlated

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