Abstract
Objective: Rheumatoid arthritis (RA) is a chronic inflammatory disease mediated through complex immunologic pathways. Among RA patients receiving low-dose methotrexate (MTX) monotherapy, approximately one-half exhibit a meaningful clinical response within the first 6 months of starting treatment. Whether baseline immune phenotypes differ between subsequent MTX responders and nonresponders is unknown. This study utilized comprehensive T cell immunophenotyping to identify specific immunologic pathways associated with MTX-nonresponsive joint inflammation in patients with RA. Methods: In total, 32 patients with recent-onset RA were treated with MTX therapy. After 6 months, 15 patients were categorized as responders and 17 as nonresponders. Comprehensive blood T cell immunophenotyping, using multiparameter immunofluorescence flow cytometry analyses, was performed at baseline and following 6 months of treatment. Results: Baseline measures of disease activity (Disease Activity Score in 28 joints [DAS28], C-reactive protein level, and erythrocyte sedimentation rate) did not differ between MTX responders and nonresponders following MTX treatment. Frequencies of CD4+ and CD8+ T cells were skewed to favor higher CD4:CD8 T cell ratios in MTX responders compared to nonresponders (P < 0.05). The proportion of inducible costimulator–expressing Treg cells was significantly greater among MTX nonresponders. Interleukin-13 (IL-13)–producing, but not interferon-γ– or IL-17–producing, CD4+ effector memory T (Tem) cells were significantly more frequent in MTX nonresponders (P < 0.05). The ratio of IL-13+:IL-17+ Tem cells among CD4+ Tem cells was 1.9-fold higher in MTX nonresponders compared to responders (P < 0.05). Both the CD4:CD8 T cell ratio and the frequency of IL-13+CD4+ Tem cells correlated with changes in the DAS28 score following MTX treatment, whereas T cell expression of immune checkpoint inhibitor markers (CTLA-4, programmed death 1, and T cell immunoglobulin and mucin domain–containing protein 3) did not differ between MTX responders and nonresponders. Conclusion: We observed a bias toward type 2–polarized T cell inflammatory responses in the peripheral blood of MTX-nonresponsive RA patients. Targeting the IL-13+CD4+ T cell pathway could be a new therapeutic strategy in RA patients whose disease remains resistant to MTX.
| Original language | English |
|---|---|
| Pages (from-to) | 1091-1102 |
| Number of pages | 12 |
| Journal | Arthritis and Rheumatology |
| Volume | 72 |
| Issue number | 7 |
| DOIs | |
| Publication status | Published - Jul 1 2020 |
Bibliographical note
Funding Information:We gratefully acknowledge the following staff rheumatologists for their support in recruiting patients to the study: Dr. Souad Shatshat, Dr. Elana Murphy, Dr. Trudy Taylor, Dr. Volodko Bakowsky, Dr. Jill Wong, Dr. Emily Shaw, Dr. Evelyn Sutton, Dr. Juris Lazovskis, and Dr. Janet Roberts. We also thank participating patients from the Rheumatology Clinic at the Queen Elizabeth II Health Sciences Centre and healthy control volunteers for donating samples, and Tatjana Brauer-Chapin and Maria Vaci for their excellent technical assistance.
Publisher Copyright:
© 2020, American College of Rheumatology
ASJC Scopus Subject Areas
- Immunology and Allergy
- Rheumatology
- Immunology