Tymms Kathleen, Kelly Ayano, Bird Paul, Griffiths Hedley, de Jager Julien, Littlejohn Geoff, Louw Sandra, Roberts Lynden, Youssef Peter, Zochling Jane, Nichols Dave
Canberra Rheumatology, Canberra, Australian Capital Territory, Australia.
Rheumatology Department, Canberra Hospital, Canberra, Australian Capital Territory, Australia.
Int J Rheum Dis. 2018 Feb;21(2):510-516. doi: 10.1111/1756-185X.13127. Epub 2017 Jul 21.
To describe the treatment regimens, duration of therapy and reasons for disease-modifying antirheumatic drug (DMARD) cessation in a large psoriatic arthritis (PsA) cohort.
A retrospective non-interventional multi-centre study using Audit4 electronic medical records, with de-identified, routinely collected clinical data from rheumatology practices in the OPAL consortium (Optimising Patient outcomes in Australian rheumatoLogy) during November 2015. Baseline characteristics, type and duration of conventional and biologic DMARDs (cDMARD and bDMARD, respectively), disease activity (Disease Activity Score of 28 joints C-reactive protein [DAS28-CRP]), and reasons for treatment cessation were recorded.
A total of 3422 rheumatologist-diagnosed PsA patients were included: 60% female, mean age 54 years and disease duration 10 years. Of patients with treatment recorded (n = 2948), 46% were on cDMARD monotherapy, 19% bDMARD monotherapy, 13% combination bDMARD and cDMARDs, 11% combination cDMARDs and 10% no DMARDs. Of those with DAS28-CRP results (n = 494), the highest mean DAS28-CRP was 3.32 on combination cDMARDs, and the lowest was 2.19 on bDMARD monotherapy. Median duration on cDMARD monotherapy was 33.5 months (n = 2232), on bDMARD monotherapy 110.1 months (n = 751), on combination bDMARD and cDMARDs 68.5 months (n = 559). The most common reasons for cessation of cDMARD monotherapy was adverse reactions (41%), for bDMARD monotherapy lack of efficacy (26%), and for combination bDMARD and cDMARDs treatment completed or no longer required (37%).
Most PsA patients were prescribed DMARD therapies with a large proportion receiving cDMARDs. Patients on combination cDMARD therapies had the highest DAS28-CRP results. Adverse reactions were the most common reason for cessation of cDMARD monotherapy, whereas for bDMARD monotherapy it was lack of efficacy.
描述一个大型银屑病关节炎(PsA)队列中疾病改善抗风湿药物(DMARD)的治疗方案、治疗持续时间以及停药原因。
一项回顾性非干预性多中心研究,使用Audit4电子病历,收集了2015年11月OPAL联盟(澳大利亚风湿病优化患者结局)中风湿病诊疗机构常规收集的匿名临床数据。记录了患者的基线特征、传统和生物DMARD(分别为cDMARD和bDMARD)的类型及持续时间、疾病活动度(28个关节疾病活动评分- C反应蛋白[DAS28-CRP])以及停药原因。
共纳入3422例经风湿病学家诊断的PsA患者:60%为女性,平均年龄54岁,病程10年。在有治疗记录的患者(n = 2948)中,46%接受cDMARD单药治疗,19%接受bDMARD单药治疗,13%接受bDMARD与cDMARD联合治疗,11%接受cDMARD联合治疗,10%未接受DMARD治疗。在有DAS28-CRP结果的患者(n = 494)中,cDMARD联合治疗时平均DAS28-CRP最高,为3.32,bDMARD单药治疗时最低,为2.19。cDMARD单药治疗的中位持续时间为33.5个月(n = 2232),bDMARD单药治疗为110.1个月(n = 751),bDMARD与cDMARD联合治疗为68.5个月(n = 559)。cDMARD单药治疗停药的最常见原因是不良反应(41%),bDMARD单药治疗是疗效不佳(26%),bDMARD与cDMARD联合治疗是治疗完成或不再需要(37%)。
大多数PsA患者接受了DMARD治疗,其中很大一部分接受了cDMARD治疗。接受cDMARD联合治疗的患者DAS28-CRP结果最高。不良反应是cDMARD单药治疗停药的最常见原因,而bDMARD单药治疗停药的最常见原因是疗效不佳。
