Kearsley-Fleet Lianne, Rokad Aasiyah, Tsoi Man-Fung, Zhao Sizheng Steven, Lunt Mark, Watson Kath D, Hyrich Kimme L
Centre for Epidemiology Versus Arthritis, Centre for Musculoskeletal Research, Division of Musculoskeletal and Dermatological Sciences, Faculty of Biology Medicine and Health, The University of Manchester, Manchester Academic Health Science Centre, Manchester, UK.
NIHR Manchester Biomedical Research Centre, Manchester University NHS Foundation Trust, Manchester, UK.
Rheumatology (Oxford). 2024 Aug 1;63(8):2082-2092. doi: 10.1093/rheumatology/kead470.
Adults with RA are being switched from etanercept originator to biosimilar in non-medical/cost-saving switching. This analysis aims to investigate outcomes in these patients, including (i) drug survival and (ii) disease activity at 6 months and 12 months, compared with those who remain on the originator.
Using BSRBR-RA, those who switched directly from etanercept originator to biosimilar were identified and matched to patients receiving the originator, based on gender, age, disease duration and originator start year. Drug survival was calculated; Cox-proportional hazard models assessed differences in drug persistence between those who switched vs remaining on originator. Change in DAS28 after 6 months and 12 months was compared between cohorts. Multiple imputation was used.
A total of 1024 adults with RA switching from etanercept originator to biosimilar were included, with a matched cohort of patients remaining on the originator. Patients who switched onto a biosimilar product were no more likely to discontinue etanercept treatment vs those who remained on the originator; hazard ratio 1.06 (95%CI 0.89-1.26), with 65% of patients remaining on treatment at three years. Ninety-five (9%) patients switched back to the originator within the first year. After 6 months and 12 months, biosimilar patients were no more likely to have a worsening of DAS28 (>0.6 units) compared with those who remained on the originator.
This is the largest matched comparative effectiveness analysis showing patients switching from etanercept originator to biosimilar appearing to do just as well with regard to disease activity and drug persistence compared with those who remained on the originator. These data will be reassuring to clinicians and patients regarding non-medical switching.
在非医疗/节省成本的换药过程中,类风湿关节炎(RA)成人患者正从原研依那西普转换为生物类似药。本分析旨在研究这些患者的治疗结果,包括(i)药物留存率,以及(ii)与继续使用原研药的患者相比,6个月和12个月时的疾病活动度。
利用英国风湿病学会生物制剂注册数据库(BSRBR-RA),识别出直接从原研依那西普转换为生物类似药的患者,并根据性别、年龄、病程和原研药起始年份,将其与接受原研药治疗的患者进行匹配。计算药物留存率;Cox比例风险模型评估换药患者与继续使用原研药患者在药物持续使用方面的差异。比较两组在6个月和12个月时28关节疾病活动评分(DAS28)的变化。采用多重填补法。
共纳入1024例从原研依那西普转换为生物类似药的RA成人患者,并匹配了一组继续使用原研药的患者。与继续使用原研药的患者相比,转换为生物类似药产品的患者停用依那西普治疗的可能性并无增加;风险比为1.06(95%置信区间0.89-1.26),三年时65%的患者仍在接受治疗。95例(9%)患者在第一年内换回了原研药。6个月和12个月后,与继续使用原研药的患者相比,使用生物类似药的患者DAS28恶化(>0.6个单位)的可能性并无增加。
这是规模最大的匹配比较疗效分析,结果显示,与继续使用原研药的患者相比,从原研依那西普转换为生物类似药的患者在疾病活动度和药物持续使用方面表现相当。这些数据将让临床医生和患者对非医疗换药放心。
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