OP168 Costs And Effectiveness Of Whole Exome Sequencing (WES) In Patients With Unsolved Rare Disease Through The Diagnostic Pathway

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Deborah A Marshall, Koen Degeling, Toni Tagimacruz, Trevor A. Seeger, Kym M Boycott, Francois Bernier, Roberto Mendoza-Londona, Karen V. MacDonald, Taila Hartley, Robin Z. Hayeems
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Abstract

IntroductionPatients suspected of having a rare genetic disease often experience lengthy and costly diagnostic odysseys. The timing of whole exome sequencing (WES) in the testing sequence, its diagnostic yield and test costs in the sequence all factor into estimates of cost-effectiveness analysis for health technology assessment.MethodsWe modeled the diagnostic pathway using a discrete event simulation model, starting with the first test result. We defined and populated the simulation based on data from the electronic medical records of n=307 from the Care-for-Rare SOLVE multi-center Canadian observational cohort. Five alternative diagnostic pathways were modeled based on the observed data: no WES, and WES as the first, second, third or fourth test in the sequence. WES as the second test in the sequence is considered standard of care in medical genetic centers in Canada. We assessed effectiveness of WES in terms of diagnostic yield, time to diagnosis, and costs as patient-level overall test costs (2020 CAD/USD) across the diagnostic pathway.ResultsCompared to molecular and specialized diagnostic tests only (i.e., no WES), WES increased diagnostic yield from 5 percent to 40 percent. The shortest time to diagnosis for those with a diagnosis was 1.82 years in the diagnostic pathway with WES as the second test. Test costs for each pathway were CAD2,800 (USD2,087, no WES), CAD2,700 (USD2,013, WES as first test), CAD3,500 (USD2,609, WES as second test), CAD4,500 (USD3,354, WES as third test), and CAD5,300 (USD3,951, WES as fourth test).ConclusionsPlacing WES earlier in the diagnostic pathway for patients suspected of having a rare disease is associated with an increased diagnostic yield, reduced time to diagnosis and lower overall test costs with the benefits being greater the earlier in the pathway that WES is implemented.
OP168 通过诊断途径对未解决的罕见病患者进行全外显子组测序(WES)的成本和效果
导言怀疑患有罕见遗传病的患者往往要经历漫长而昂贵的诊断过程。全外显子组测序(WES)在检测序列中的时间、诊断率和检测成本都是影响卫生技术评估成本效益分析估算的因素。我们根据加拿大 Care-for-Rare SOLVE 多中心观察队列中约 307 人的电子病历数据定义并填充了模拟模型。根据观察到的数据,我们模拟了五种可供选择的诊断路径:无 WES,WES 作为序列中的第一、第二、第三或第四次检验。在加拿大的医学遗传中心,将 WES 作为序列中的第二项检测被认为是标准的治疗方法。我们从诊断率、诊断时间以及整个诊断路径中患者层面的总体检测成本(2020 加元/美元)等方面评估了 WES 的有效性。结果与仅进行分子和专科诊断检测(即不进行 WES)相比,WES 可将诊断率从 5% 提高到 40%。在以 WES 作为第二项检验的诊断途径中,确诊患者的最短诊断时间为 1.82 年。每种途径的检测成本分别为 2,800 加元(2,087 美元,无 WES)、2,700 加元(2,013 美元,WES 作为第一项检测)、3,500 加元(2,609 美元,WES 作为第二项检测)、4,500 加元(3,354 美元,WES 作为第三项检测)和 5,300 加元(3,951 美元,WES 作为第四项检测)。结论 在诊断罕见病疑似患者的过程中尽早进行 WES 可提高诊断率、缩短诊断时间并降低总体检验成本,而且在诊断过程中越早进行 WES,获益越大。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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