4.7 Article

Risk of serious infections in arthritis patients treated with biological drugs: a matched cohort study and development of prediction model

Journal

RHEUMATOLOGY
Volume 60, Issue 8, Pages 3834-3844

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/rheumatology/keaa876

Keywords

epidemiology; infection; biologicals

Categories

Funding

  1. Danish Rheumatism Association

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This study compared the risk of serious infection between patients with inflammatory joint diseases receiving biological drug treatment and the general population, and developed a simple prediction model for individual risk assessment. The results showed that patients initiating bDMARD treatment had a four times higher risk of serious infection compared to the general population, and the developed prediction model demonstrated moderate discriminative power for risk assessment.
Objectives. Serious infection is a concern for patients with inflammatory joint diseases treated with biological drugs (bDMARDs). The objectives were to compare risk of serious infection, defined as infection leading to hospitalization, in patients initiating bDMARD treatment with that in the general population and, second, to develop a simple clinical prediction model and to obtain risk estimates for individual patients. Methods. This was a matched-cohort study based on nationwide registries in Denmark. Patients with RA, axial SpA and PsA initiating first bDMARD monitored in the DANBIO registry were matched 1:10 by age, gender and postal code with controls from the general population. The risk of serious infection during 12 months' follow-up was assessed with Cox regression. Prediction models were developed using logistic regression and compared using area under the receiver operating characteristic curve (AUC). Results. We included 11 372 patients and 113 715 controls. During follow-up, 522 patients (4.6%) and 1434 controls (1.3%) developed a serious infection (hazard ratio 3.7, 95% CI 3.4, 4.1). Age-stratified risk was largely similar across diagnoses. A simple prediction model, the 'DANBIO infection risk score', based on age and a count of six clinical risk factors had moderate discriminative power (internal validation: AUC 0.69) that was comparable to that of the existing RABBIT (Rheumatoide Arthritis Beobachtung der Blologika-Therapie) Risk Score (external validation: AUC 0.68). Conclusion. Patients with inflammatory joint diseases initiating bDMARD treatment had a four times increased risk of serious infection compared with the general population. A simple prediction model, feasible for shared decision-making, was developed to obtain risk estimates for individual patients.

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