Poly‐refractory Rheumatoid Arthritis: An Uncommon Subset of Difficult to Treat Disease with Distinct Inflammatory and Non‐inflammatory Phenotypes

Author:

David Paula12ORCID,Di Matteo Andrea134,Hen Or12,Dass Shouvik3,Marzo‐Ortega Helena134,Wakefield Richard J134,Bissell Leslie‐Anne3,Nam Jacqueline3,Mankia Kulveer134,Emery Paul134ORCID,Saleem Benazir3,McGonagle Dennis134

Affiliation:

1. University of Leeds Leeds United Kingdom

2. Sheba Medical Center, Tel Hashomer Ramat Gan Israel

3. Leeds Teaching Hospitals NHS Trust Leeds United Kingdom

4. National Institute for Health Research ‐ Leeds Biomedical Research Centre Leeds United Kingdom

Abstract

ObjectivesTo investigate the prevalence of poly‐refractory RA defined as failure of all biologic (b)/targeted synthetic (ts)‐DMARDs. To further investigate whether Persistent inflammatory refractory RA (PIRRA) and non‐inflammatory refractory RA (NIRRA) patients, determined by objective ultrasound (US) synovitis, have distinct clinical phenotypes in both EULAR difficult‐to‐treat Rheumatoid Arthritis (D2T‐RA) and poly‐refractory RA groups.MethodsA cross‐sectional study of 1591 RA patients on biologic b/tsDMARDs that evaluated D2T‐RA criteria and subclassified as poly‐refractory if inefficacy/toxicity to at least one drug of all classes. PIRRA was defined if US synovitis in ≥1 swollen joint (SJ) and NIRRA if absent. Univariate tests and multivariate logistic regression were conducted to investigate factors associated with poly‐refractory, PIRRA, and NIRRA phenotypes.Results122/1591 were excluded due to missing data. 247/1469 (16.8%) had D2T‐RA and only 40/1469 (2.7%) poly‐refractory RA. This latter group had higher DAS‐28‐CRP (median 5.4 vs 5.02, p<0.05), CRP levels (median 13 vs 5mg/l, p<0.01), and smoking (ever) rates (20% vs 4%, p<0.01) compared to other D2T patients. Smoking was associated with poly‐refractory RA (OR= 5.067, 95% CI [1.774‐14.472], p=0.002). Of 107 D2T‐RA patients with recent US, 61 (57%) were PIRRA and 46 (43%), NIRRA. NIRRA patients had elevated BMI (median 30 vs 26, p<0.001) and higher fibromyalgia prevalence (15% vs 3%, p<0.05), lower SJ count (median: 2 vs 5, p<0.001) and lower CRP levels (5 vs 10, p<0.01).ConclusionOnly 2.7% of D2T‐RA failed all classes of b/tsDMARDs. Among D2T‐RA, under 60% had objective signs of inflammation, representing a target for innovative strategies.image

Publisher

Wiley

Subject

Immunology,Rheumatology,Immunology and Allergy

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