Keyzor Ian, Martins Ana Maria, Uçar Sema Kalkan, Yamakawa Hiroyuki, Chien Yin-Hsiu, Arslan Nur, Niu Dau-Ming, Tümer Leyla, Baldock Laura, Shohet Simon, Giuliano Joseph D
Amicus Therapeutics Ltd, Marlow, UK.
Universidade Federal de São Paulo, São Paulo, Brazil.
Orphanet J Rare Dis. 2025 Aug 11;20(1):419. doi: 10.1186/s13023-025-03707-2.
Fabry disease (FD) is a rare inherited X-linked lysosomal disorder caused by the deficiency or dysfunction of the enzyme α-galactosidase. This leads to a detrimental accumulation of globotriaosylceramide (Gb3) within multiple cell types. Enzyme replacement therapies (ERTs), including agalsidase alfa and agalsidase beta, can diminish Gb3 levels. Published real-world data on the time, cost and burden associated with the administration of ERTs are limited. These evidence gaps were addressed by generating real-world data quantifying the burden of agalsidase alfa and beta infusions for FD treatment.
The study (ClinicalTrials.gov number: NCT04281537) comprised a prospective time-and-motion and a cross-sectional evaluation of self-reported burden and outcomes associated with ERT administration (including work productivity and out-of-pocket costs) from multiple perspectives (healthcare professionals [HCPs], patients, and caregivers). To assess patient/caregiver experience and burden of ERT, the primary objective was to quantify the total time spent by HCPs in the preparation and administration of a single dose of ERT.
Overall, 76 patients and 6 caregivers were included. Of the 76 patients, (Brazil [n = 23], Japan [n = 4], Taiwan [n = 30] and Turkey [n = 19]), 41% were female and the mean (standard deviation [SD]) age at diagnosis was 41.1 (17.1) years. Overall, most patients (70%, n = 53) had moderate FD and were treated with agalsidase beta (65%, n = 48); this was the predominant ERT administered in Brazil (100%, n = 23) and Turkey (74%, n = 14); most patients in Japan (75%, n = 3) and Taiwan (67%, n = 20) received agalsidase alfa. The mean (SD) HCP time spent on all ERT activities was 151.9 (62.5) minutes (2.5 [1.0] hours); the mean (SD) time spent on pre- and post-infusion activities was 20.9 (13.4) (0.3 [0.2] hours) and 12.8 (9.6) minutes (0.2 [0.2] hours), respectively. The mean (SD) time spent by patients for all ERT activities was 368.5 (191.5) minutes (6.1 [3.2] hours); 21% (n = 16/76) of patients and 50% (n = 3/6) of carers took time off work for an ERT episode.
The multi-region findings provide a more complete picture of the burden associated with ERT administration for FD treatment on patients, caregivers, and HCPs. Results may support further cost-effectiveness modelling for novel treatment approaches and inform treatment decisions and patient management.
法布里病(FD)是一种罕见的X连锁隐性遗传性溶酶体疾病,由α-半乳糖苷酶缺乏或功能障碍引起。这导致多种细胞类型中球三糖基神经酰胺(Gb3)的有害积累。酶替代疗法(ERTs),包括阿加糖酶α和阿加糖酶β,可以降低Gb3水平。关于ERTs给药的时间、成本和负担的已发表真实世界数据有限。通过生成量化阿加糖酶α和β输注治疗FD负担的真实世界数据,解决了这些证据空白。
该研究(ClinicalTrials.gov编号:NCT04281537)包括一项前瞻性时间动作研究,以及从多个角度(医疗保健专业人员[HCPs]、患者和护理人员)对与ERT给药相关的自我报告负担和结果(包括工作生产力和自付费用)进行的横断面评估。为了评估患者/护理人员的ERT体验和负担,主要目标是量化HCPs制备和给药单剂量ERT所花费的总时间。
总体而言,纳入了76名患者和6名护理人员。在76名患者中(巴西[n = 23]、日本[n = 4]、台湾[n = 30]和土耳其[n = 19]),41%为女性,诊断时的平均(标准差[SD])年龄为41.1(17.1)岁。总体而言,大多数患者(70%,n = 53)患有中度FD,接受阿加糖酶β治疗(65%,n = 48);这是巴西(100%,n = 23)和土耳其(74%,n = 14)使用的主要ERT;日本(75%,n = 3)和台湾(67%,n = 20)的大多数患者接受阿加糖酶α治疗。HCPs在所有ERT活动上花费的平均(SD)时间为151.9(62.5)分钟(2.5[1.0]小时);输注前和输注后活动花费的平均(SD)时间分别为20.9(13.4)(0.3[0.2]小时)和12.8(9.6)分钟(0.2[0.2]小时)。患者在所有ERT活动上花费的平均(SD)时间为368.5(191.5)分钟(6.1[3.2]小时);21%(n = 16/76)的患者和50%(n = 3/6)的护理人员因ERT发作而请假。
多地区研究结果更全面地呈现了ERT给药治疗FD对患者、护理人员和HCPs的负担情况。研究结果可能支持对新型治疗方法进行进一步的成本效益建模,并为治疗决策和患者管理提供参考。
