Abstract
BackgroundIL6-related T cell activation and TNFα-dependent cell proliferation are major targets of therapy in the RA synovium. We investigated whether expression of these pathways in RA synovial biopsies is associated with disease activity and response to therapy.MethodCorrelation and gene set enrichment studies were performed using gene expression profiles from RA synovial biopsies. Immunostaining experiments of GADD45B and PDE4D were performed on independent additional sets of early untreated RA samples, obtained in two different centers by needle-arthroscopy or US-guided biopsies.ResultsIn 65 RA synovial biopsies, transcripts correlating with disease activity were strongly enriched in TNFα-induced genes. Out of the individual variables used in disease-activity scores, tender joint count, swollen joint count and physician’s global assessment, but not CRP or patient’s global assessment displayed a similar correlation with the expression of TNFα-dependent genes. In addition, TNFα-induced genes were also significantly enriched in transcripts over-expressed in synovial biopsy samples obtained from poor-responders to methotrexate or tocilizumab, prior to initiation of therapy.GADD45B (induced by TNFα in monocytes) and PDE4D (induced by TNFα in FLS) immunostaining was significantly higher in overall poor-responders to therapy in 46 independent baseline samples obtained from early untreated RA patients prior to initiation of therapy. GADD45B (but not PDE4D) immunostaining was significantly higher in the sub-group of patients with poor-response to methotrexate therapy, and this was confirmed in another population of methotrexate-treated patients.ConclusionHigher expression of TNFα-induced transcripts in early RA synovitis is associated with higher disease activity, and predicts poor response to first-line therapy. That over-expression of TNFα-induced genes predicts poor-response to therapy regardless of the drug administered, indicates that this molecular signature is associated with disease severity, rather than with specific pathways of escape to therapy.Electronic supplementary materialThe online version of this article (doi:10.1186/s13075-016-0919-z) contains supplementary material, which is available to authorized users.
Highlights
interleukin 6 (IL6)-related T cell activation and tumor necrosis factor alpha (TNFα)-dependent cell proliferation are major targets of therapy in the rheumatoid arthritis (RA) synovium
growth arrest and DNA-damage-inducible (GADD45B) and phosphodiesterase 4D (PDE4D) immunostaining was significantly higher in overall poor-responders to therapy in 46 independent baseline samples obtained from early untreated RA patients prior to initiation of therapy
Gene set enrichment analyses indicated that almost all these transcripts are downregulated by tocilizumab in the synovium in early RA, which indicates that they are, directly or indirectly, IL6-dependent (Fig. 1c)
Summary
IL6-related T cell activation and TNFα-dependent cell proliferation are major targets of therapy in the RA synovium. Tocilizumab and rituximab display very similar molecular effects in RA synovitis, characterized by a decrease in T cell activation genes [5, 6]. Higher baseline expression of TNFα-induced transcripts in RA synovial tissue was associated with decreased responses to TNF blockade in methotrexate-resistant patients [7, 8]. These observations probably indicate that, in some cases, tissue impregnation in TNFα is too high to be blocked using standard TNF blockade regimens
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
