Johns Hopkins University School of Medicine Baltimore, MD, United States
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Carlos Aude1, Deanna Jannat-Khah2, Karmela Kim Chan2, Nilasha Ghosh1, Clifton Bingham3, Vivian Bykerk2 and Anne Bass1, 1Hospital for Special Surgery, Weill Cornell Medicine, New York, NY, 2Hospital For Special Surgery, New York, NY, 3Johns Hopkins University, Baltimore, MD
Background/Purpose: Immune checkpoint inhibitors (ICIs) have transformed cancer treatment but may trigger immune-related adverse events (irAEs) such as ICI-induced inflammatory arthritis (ICI-IA). Although ICI-IA and rheumatoid arthritis (RA) exhibit clinical similarities, it remains uncertain if ICI-IA represents an early form of RA or a distinct disease. Our study aimed to elucidate their relationship by comparing joint involvement patterns in patients with ICI-IA and early RA.
Methods: Clinical data from 89 ICI-IA patients in our institutional rheumatic irAE registry and 163 early RA patients from the Consortium of early ArThritis CoHorts-USA (CATCH-US) cohort were analyzed. Rheumatologists recorded the Swollen and Tender Joint Counts (SJC, TJC) at the patients' baseline visit. A multivariable logistic regression model was first utilized to identify variables associated with specific joint swelling and/or tenderness in the ICI-IA cohort. Separately, we compared the overall joint involvement pattern of ICI-IA and early RA using Fisher's exact test, while SJC, TJC, and joint symmetry were compared using multivariable linear and logistic regressions, correspondingly. Specific joint comparisons were compared with multivariable logistic regression models. All models were adjusted for demographics, BMI, seropositivity, steroid use, DMARD use, and time from symptom onset to study inclusion; ICI-IA-exclusive models were additionally adjusted for cancer type, ICI regimen, and time from ICI initiation to study inclusion.
Results: ICI-IA patients were older, more likely to be male, and less frequently seropositive than early RA patients (Table 1). In the ICI-IA-exclusive analysis, female patients exhibited a higher probability of knee tenderness (aOR=9.02, p=0.03) and a lower probability of PIP swelling (aOR=0.11, p=0.005) relative to male patients. Additionally, younger patients showed an increased likelihood of knee swelling (aOR=0.93, p=0.03) compared to their older counterparts. Notably, no other variables, including the ICI treatment regimen, were associated with specific joint involvement among ICI-IA patients. Comparative analysis between ICI-IA and early RA patients revealed higher odds of symmetrical swelling in early RA (aOR=2.44, p=0.02), despite no substantial differences in either SJC or TJC. There was a significant difference in the overall swollen joint distribution between the two cohorts (p=0.008), particularly with regard to PIP (45% vs. 60%, p=0.02) and knee involvement (54% vs. 27%, p=0.03) (Table 2). After adjusting for confounding variables, ICI-IA patients continued to exhibit higher odds of knee swelling (aOR=4.76, p=0.007), though PIP involvement did not significantly differ (p=0.08) (Figure 1). A subanalysis comparing ICI-IA and seronegative early RA patients yielded similar results.
Conclusion: We demonstrated distinct joint involvement patterns between ICI-IA and early RA patients, with more frequent knee swelling in ICI-IA and more PIP and symmetrical joint involvement in early RA. These results could inform the development of ICI-IA classification criteria, thereby enhancing differential diagnosis and treatment strategies.
Table 1. Demographic and Clinical Characteristics of Early RA and ICI-IA Patients
Table 2. Distribution of Swelling and Tenderness for Individual Joints in Early RA and ICI-IA Patients
Figure 1. Forest Plot and Log Adjusted Odds Ratios (aOR) with 95% Confidence Intervals for Joint Swelling and Tenderness Comparing Early RA and ICI-IA Patients (*Adjusted for demographics, BMI, seropositivity, steroid use, DMARD use, and time from arthritis onset to study inclusion)
C. Aude: None; D. Jannat-Khah: AstraZeneca, 12, stock ownership, Cytodyn, 12, stock ownershil[, Walgreens Boots Alliance, 12, stock ownership; K. Chan: None; N. Ghosh: None; C. Bingham: AbbVie/Abbott, 2, Bristol-Myers Squibb(BMS), 5, Eli Lilly, 2, Janssen, 2, Pfizer, 2, Sanofi, 2; V. Bykerk: Abbvie, 2, BMS, 2, Pfizer, 2; A. Bass: None.