Treatment patterns in a real-world cohort of patients with Wilson disease in the United States

Valentina Medici, Nehemiah Kebede, Jennifer Stephens, Mary Kunjappu, John M. Vierling
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Abstract

Wilson disease (WD) is a rare and potentially fatal genetic disorder caused by accumulation of toxic levels of copper. Current treatments include chelating agents and/or zinc. We characterized real-world US treatment patterns in patients with WD.This retrospective, observational medical chart review utilized deidentified clinical data, including treatment patterns, abstracted from patient medical charts between 01/2012 and 06/2017. Line of therapy was assessed based on disease presentation and aggregated. Index treatment was defined as the first line of therapy, followed by second line of therapy and third line of therapy. Results were summarized using descriptive statistics.A total of 225 patients were included (mean [SD] age at diagnosis: 24.7 [9.8] years). Initial disease presentation was both neurologic/psychiatric and hepatic in 52.9%, followed by neurologic/psychiatric (20.0%), hepatic (16.9%), and asymptomatic (10.2%). Median (first and third quartiles) duration of follow-up from diagnosis was 39.5 (33.8–60.4) months. The most common first line of therapy was penicillamine monotherapy in 45.5%, followed by trientine monotherapy (26.1%) and chelator/zinc combination therapy (21.2%). A total of 167/222 (75.2%) patients remained on first line of therapy during the follow-up period. Of the 13.5% who switched to second line of therapy, most changed to trientine monotherapy (53.3%). All those who switched to third line of therapy transitioned to zinc monotherapy (100.0%). Unexpectedly, 11.3% discontinued first line of therapy without transitioning to a subsequent therapy. The primary rationale for index monotherapy selection was improved efficacy (61.6%). Most discontinuations were due to side effects/tolerability (40.8%). Treatment patterns varied by initial disease presentation, practice setting, physician specialty, and geographic location.These results demonstrate a lack of consensus in the US regarding first-line treatment for patients with WD. Evidence-based treatment pathways informed by high-quality clinical trials for improved health outcomes are needed.
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美国威尔逊病患者真实世界队列中的治疗模式
威尔逊病(WD)是一种罕见的遗传性疾病,有可能致命,其病因是铜的毒性积累。目前的治疗方法包括螯合剂和/或锌。这项回顾性、观察性病历审查利用了2012年1月至2017年6月期间从患者病历中抽取的去标识化临床数据,包括治疗模式。根据疾病表现评估并汇总治疗方案。指数治疗被定义为一线治疗,其次是二线治疗和三线治疗。共纳入 225 名患者(平均 [SD] 诊断年龄:24.7 [9.8] 岁)。52.9%的患者最初表现为神经/精神症状和肝病,其次是神经/精神症状(20.0%)、肝病(16.9%)和无症状(10.2%)。自确诊起的随访时间中位数(第一和第三四分位数)为 39.5(33.8-60.4)个月。最常见的一线疗法是青霉素单药治疗(45.5%),其次是三苯氧胺单药治疗(26.1%)和螯合剂/锌联合疗法(21.2%)。在随访期间,共有 167/222 名患者(75.2%)仍在使用一线疗法。在13.5%转为二线治疗的患者中,大多数转为三苯氧胺单药治疗(53.3%)。所有转为三线治疗的患者都转为锌单药治疗(100.0%)。意外的是,有 11.3% 的患者停止了一线治疗,但没有过渡到后续治疗。选择指数单药疗法的主要原因是疗效更好(61.6%)。大多数停药是因为副作用/耐受性(40.8%)。这些结果表明,美国对WD患者的一线治疗缺乏共识。这些结果表明,美国对 WD 患者的一线治疗缺乏共识,需要通过高质量的临床试验来确定循证治疗路径,以改善健康状况。
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