Five-Year Drug Survival and Discontinuation Reasons for Eight Biological Disease-Modifying Antirheumatic Drugs for Rheumatoid Arthritis: A Retrospective Analysis of 1182 Patients from the Niigata Orthopedic Surgery Rheumatoid Arthritis Database (NOSRAD)
Nariaki Hao, Naoki Kondo, Katsumitsu Arai, Naoko Kudo, Takehiro Murai, Junichi Fujisawa, Yasufumi Kijima, Rika Kakutani, Hiroyuki Kawashima

TL;DR
This study analyzed 5-year drug survival and discontinuation reasons for eight biologic drugs used to treat rheumatoid arthritis in over 1,000 patients.
Contribution
The study provides real-world 5-year drug survival data and identifies factors influencing discontinuation for various biologic treatments in rheumatoid arthritis.
Findings
Tocilizumab had the highest 5-year drug survival (50.8%) in biologic-naïve patients, while golimumab had the lowest (22.6%).
Male sex, lower baseline DAS28-ESR, and absence of methotrexate co-therapy predicted discontinuation in biologic-naïve patients.
Inadequate response was the most common reason for discontinuation (27.1%), followed by non-adverse events (25.3%).
Abstract
Background: Continuity of care for rheumatoid arthritis patients within regional networks enables stable long-term clinical data collection, despite chronic rheumatologist shortages in Japan. We determined 5-year drug survival and discontinuation reasons for eight biological disease-modifying antirheumatic drugs (bDMARDs) using a regional multicenter registry. Methods: We retrospectively analyzed 1182 patients initiating their first (naïve, n = 784) or subsequent (switch, n = 398) bDMARD between May 2001 and August 2022 across five institutions. The primary endpoint (5-year drug survival) and secondary endpoints (discontinuation risk factors and cumulative incidence of reasons) were evaluated using Kaplan–Meier curves, Cox proportional hazards, and Fine & Gray models. Results: Baseline characteristics varied significantly among bDMARDs. Five-year drug survival in the naïve cohort ranged…
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Taxonomy
TopicsRheumatoid Arthritis Research and Therapies · Pharmaceutical Economics and Policy · Pharmacovigilance and Adverse Drug Reactions
