Sebastiani Marco, Manfredi Andreina, Iannone Florenzo, Gremese Elisa, Bortoluzzi Alessandra, Favalli Ennio, Bazzani Chiara, Salaffi Fausto, Fusaro Enrico, Foti Rosario, Giannitti Chiara, Caporali Roberto, Cauli Alberto, Cassone Giulia, Lopalco Giuseppe, Petricca Luca, Ferraccioli Gianfranco, Lapadula Giovanni
Azienda Ospedaliera Policlinico Di Modena, University of Modena and Reggio Emilia, Rheumatology Unit, Modena, Italy.
Department of Medicine, Rheumatology Unit, University of Bari, Interdisciplinary Bari, Italy.
Arch Rheumatol. 2020 Feb 7;35(2):163-169. doi: 10.46497/ArchRheumatol.2020.7499. eCollection 2020 Jun.
This study aims to investigate the factors associated with early discontinuation (within one year) of etanercept (ETA) in rheumatoid arthritis (RA) patients who began ETA as first biologic disease-modifying antirheumatic drug (bDMARD) and who were entered into the Gruppo Italiano di Studio sulla Early Arthritis (Italian Group for the Study of Early Arthritis; GISEA) registry.
This registry-based cohort study included 477 RA patients (95 males, 382 females; median age 53 years; range 18 to 83 years) who began ETA as first bDMARD. Patient demographics, disease features and drugs were re-evaluated after 12 months. Baseline predictors of ETA discontinuation were estimated by univariate and multivariate analyses using Cox regression model.
Seventy patients (14.7%) discontinued ETA during the first year (for inefficacy in 55.8%, adverse events in 28.6%, and other reasons in 6.5%). Concurrent conventional synthetic DMARDs (csDMARDs) were reported in 54.3% of patients, mainly methotrexate (MTX), while 52.4% of subjects took low doses of glucocorticoids. Patients stopping ETA more frequently showed one or more comorbidities, mainly cardiovascular diseases (28.6% vs. 15.7% in patients stopping and continuing ETA, respectively, p=0.009). The presence of comorbidities and a combination therapy with csDMARDs other than MTX were independent factors associated with early discontinuation of ETA at multivariate Cox analysis.
Although ETA demonstrated a high persistence in biologic-naïve RA patients, about 15% of patients discontinued the treatment within 12 months. The presence of comorbidities and a combination therapy with csDMARDs other than MTX were the main factors for an early withdrawal of the drug.
本研究旨在调查那些开始使用依那西普(ETA)作为首个生物改善病情抗风湿药物(bDMARD)并纳入意大利早期关节炎研究组(Gruppo Italiano di Studio sulla Early Arthritis;GISERA)登记系统的类风湿关节炎(RA)患者中,与依那西普在一年内早期停用相关的因素。
这项基于登记系统的队列研究纳入了477例开始使用依那西普作为首个bDMARD的RA患者(95例男性,382例女性;中位年龄53岁;范围18至83岁)。12个月后重新评估患者的人口统计学特征、疾病特征和用药情况。使用Cox回归模型通过单因素和多因素分析估计依那西普停药的基线预测因素。
70例患者(14.7%)在第一年停用依那西普(因无效停药占55.8%,因不良事件停药占28.6%,因其他原因停药占6.5%)。54.3%的患者同时使用传统合成DMARDs(csDMARDs),主要是甲氨蝶呤(MTX),而52.4%的受试者使用低剂量糖皮质激素。停用依那西普的患者更频繁地出现一种或多种合并症,主要是心血管疾病(停用依那西普和继续使用依那西普的患者分别为28.6%和15.7%,p = 0.009)。多因素Cox分析显示,合并症的存在以及与除MTX之外的csDMARDs联合治疗是与依那西普早期停用相关的独立因素。
尽管依那西普在初治的RA患者中显示出较高的持续性,但约15%的患者在12个月内停用了该治疗。合并症的存在以及与除MTX之外的csDMARDs联合治疗是药物早期停用的主要因素。
