托法替布与生物性改善病情抗风湿药的批准后比较安全性研究:来自美国类风湿关节炎注册研究的5年结果
Postapproval Comparative Safety Study of Tofacitinib and Biological Disease-Modifying Antirheumatic Drugs: 5-Year Results from a United States-Based Rheumatoid Arthritis Registry.
作者信息
Kremer Joel M, Bingham Clifton O, Cappelli Laura C, Greenberg Jeffrey D, Madsen Ann M, Geier Jamie, Rivas Jose L, Onofrei Alina M, Barr Christine J, Pappas Dimitrios A, Litman Heather J, Dandreo Kimberly J, Shapiro Andrea B, Connell Carol A, Kavanaugh Arthur
机构信息
Albany Medical College, Center for Rheumatology, Albany, New York.
Johns Hopkins University, Baltimore, Maryland.
出版信息
ACR Open Rheumatol. 2021 Mar;3(3):173-184. doi: 10.1002/acr2.11232. Epub 2021 Feb 11.
OBJECTIVE
Tofacitinib is an oral Janus kinase inhibitor for the treatment of rheumatoid arthritis (RA). We compared 5-year adverse event (AE) incidence rates (IRs) between patients initiating tofacitinib and those initiating new biological disease-modifying antirheumatic drugs (bDMARDs) within the United States (US) Corrona RA registry.
METHODS
IRs (number of first events/100 patient-years) of major adverse cardiovascular events (MACE), serious infection events (SIEs), herpes zoster (HZ), malignancies, and death were estimated among tofacitinib and bDMARD initiators, regardless of dose/schedule, between November 6, 2012 (US Food and Drug Administration tofacitinib approval), and July 31, 2018 (follow-up through January 31, 2019). Propensity score (PS) methods were used to control for nonrandom prescribing practices. Hazard ratios (HRs) were calculated to compare rates using multivariable-adjusted Cox regression. Different risk windows were used for acute (MACE, SIEs, HZ, and venous thromboembolic events [VTEs]) and long-term (malignancy and death) events. VTEs were assessed descriptively.
RESULTS
For MACE, SIEs, and HZ, 1999 (3152.1 patient-years) and 8358 (12 869.4 years) tofacitinib and bDMARD initiators were included, respectively; for malignancy/death, 1999 (4505.6 patient-years) and 6354 (16 670.8 patient-years) initiators were included, respectively. AE rates were similar across cohorts, except for HZ, which was significantly higher with tofacitinib versus bDMARDs (PS-trimmed adjusted HR 2.32; 95% confidence interval [CI] 1.43-3.75). There were 45 (zero serious) and 88 (five serious) HZ events with tofacitinib and bDMARDs, respectively. Sensitivity analyses demonstrated similar results. VTE IRs (95% CI) were 0.29 (0.13-0.54) and 0.33 (0.24-0.45) for tofacitinib and bDMARDs, respectively.
CONCLUSION
In this registry analysis, both cohorts had similar MACE, SIE, malignancy, death, and VTE rates; HZ rates were higher for tofacitinib initaitors than for bDMARD initiators.
目的
托法替布是一种用于治疗类风湿关节炎(RA)的口服Janus激酶抑制剂。我们在美国Corrona RA注册中心比较了开始使用托法替布的患者与开始使用新型生物抗风湿药物(bDMARDs)的患者之间的5年不良事件(AE)发生率。
方法
在2012年11月6日(美国食品药品监督管理局批准托法替布)至2018年7月31日(随访至2019年1月31日)期间,对托法替布和bDMARDs起始治疗者(无论剂量/用药方案)的主要不良心血管事件(MACE)、严重感染事件(SIEs)、带状疱疹(HZ)、恶性肿瘤和死亡的发生率(首次事件数/100患者年)进行了估计。采用倾向评分(PS)方法控制非随机处方行为。使用多变量调整的Cox回归计算风险比(HRs)以比较发生率。对急性事件(MACE、SIEs、HZ和静脉血栓栓塞事件 [VTEs])和长期事件(恶性肿瘤和死亡)使用了不同的风险窗口。对VTEs进行了描述性评估。
结果
对于MACE、SIEs和HZ,分别纳入了1999例(3152.1患者年)托法替布起始治疗者和8358例(12869.4患者年)bDMARDs起始治疗者;对于恶性肿瘤/死亡,分别纳入了1999例(4505.6患者年)和6354例(16670.8患者年)起始治疗者。除HZ外,各队列的AE发生率相似,托法替布组的HZ发生率显著高于bDMARDs组(PS调整后HR 2.32;95%置信区间 [CI] 1.43 - 3.75)。托法替布组和bDMARDs组分别有45例(无严重事件)和88例(5例严重事件)HZ事件。敏感性分析显示了相似的结果。托法替布组和bDMARDs组的VTE发生率(95% CI)分别为0.29(0.13 - 0.54)和0.33(0.24 - 0.45)。
结论
在本注册中心分析中,两个队列的MACE、SIE、恶性肿瘤、死亡和VTE发生率相似;托法替布起始治疗者的HZ发生率高于bDMARDs起始治疗者。
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