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Combination effect of anti-rheumatic medications for coronary artery diseases risk in rheumatoid arthritis: a nationwide population-based cohort study

机译:冠状动脉疾病抗风湿药物的组合效应类风湿性关节炎的风险:全国范围的人口队列队列研究

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Objectives: To determine whether a combination of anti-rheumatic drugs is associated with the risk of coronary artery diseases (CAD) in incident rheumatoid arthritis (RA) patients. Methods: This population-based cohort study used administrative data to identify 6260 newly-diagnosed patients with RA (age = 20 years) as the study group. The study end-point was occurrence of CAD according to the ICD-9-CM codes. Exposure to different combinations of drugs and the risk of CAD was assessed. These included different combinatiosn of celecoxib (Cx), hydroxychloroquine (HCQ), methotrexate (MTX), and sulfasalazine (SSZ). Patients who never used Cx, HCQ, MTX, or SSZ were used as a reference group. A Cox proportional hazards model was used to estimate the hazard ratio (HR) of disease after controlling for demographic and other co-morbidities. When the proportionality assumption was violated, the spline curve of the Scaled Schoenfeld residuals was fitted to demonstrate the estimated effect on CAD over time for drug usage. Results: Among RA patients, the adjusted HR (95% confidence interval) of CAD for "Cx only", "Cx and HCQ ever", and "Cx, HCQ, MTX, and SSZ ever", were 0.29 (0.19-0.44), 0.46 (0.24-0.88), and 0.42 (0.24- 0.75), respectively, during the first period of 0-3, 4, or 7 years. However, they became 1.04 (0.78-1.38), 1.16 (0.62-2.19), and 0.59 (0.32-1.08), respectively, during the second time period of 3, 4, or 7-10 years. The adjusted HR (95% CI) of CAD for "Cx, MTX, and SSZ ever" remains constant at 0.12 (0.02-0.89). Conclusions: Celecoxib-DMARDs drug combinations were associated with reduced CAD risk on incident RA patients, and some of them exhibited the time-varying drug effect.
机译:目的:确定抗风湿药物的组合是否与入射类风湿性关节炎(RA)患者的冠状动脉疾病(CAD)的风险有关。方法:基于人群的队列研究使用了行政数据,以鉴定6260名新诊断的RA(年龄& = 20年)作为研究组。根据ICD-9-CM代码,研究终点是CAD的发生。对药物的不同组合和CAD的风险接触。这些包括Celecoxib(CX),羟基氯喹(HCQ),甲氨蝶呤(MTX)和磺基碱(SSZ)的不同组合。从未使用CX,HCQ,MTX或SSZ的患者用作参考组。使用Cox比例危害模型来估算控制人口统计和其他共病理学后疾病的危害比(HR)。违反比例假设时,缩放的Schoenfeld残差的样条曲线被拟合以证明药物使用时间对CAD的估计作用。结果:在RA患者中,CAD的调整后的HR(95%置信区间)为“CX仅”,“CX和HCQ”,以及“CX,HCQ,MTX和SSZ”为0.29(0.19-0.44) ,0.46(0.24-0.88)和0.42(0.24- 0.75),分别在0-3,4或7年的第一个期间。然而,它们分别为1.04(0.78-1.38),1.16(0.62-2.19)和0.59(0.32-1.08),在3,4或7 - 10年的第二次。 CAD的“CX,MTX和SSZ”的调整后的HR(95%CI)保持恒定在0.12(0.02-0.89)。结论:Celecoxib-Dmards药物组合与事件RA患者的CAD风险降低有关,其中一些人表现出时变的药物作用。

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