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荷兰各医院治疗 III 期和 IV 期非小细胞肺癌患者的时间差异。

Variation in the time to treatment for stage III and IV non-small cell lung cancer patients for hospitals in the Netherlands.

机构信息

Health Technology and Services Research Department, Technical Medical Centre, University of Twente, Hallenweg 17, 7522 NH, Enschede, the Netherlands.

Health Technology and Services Research Department, Technical Medical Centre, University of Twente, Hallenweg 17, 7522 NH, Enschede, the Netherlands; Division of Psychosocial Research and Epidemiology, Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital (NKI-AVL), Plesmanlaan 121, 1066, CX, Amsterdam, the Netherlands.

出版信息

Lung Cancer. 2019 Aug;134:34-41. doi: 10.1016/j.lungcan.2019.05.023. Epub 2019 May 21.

Abstract

OBJECTIVES

Increased emphasis on molecular diagnostics can lead to increased variation in time to treatment (TTT) for patients with stage III and IV non-small cell lung cancer. This article presents the variation in TTT for advanced NSCLC patients observed in Dutch hospitals before the widespread use of immunotherapy. The aim of this article was to explore the variation in TTT between patients, as well as between hospitals.

MATERIAL AND METHODS

Based on the Netherlands Cancer Registry, we used patient-level data (n = 4096) from all 78 hospitals that diagnosed stage III or IV NSCLC in the Netherlands in 2016. To investigate how patient characteristics and hospital-level effects are associated with TTT (from diagnosis until start treatment), we interpreted regression model results for five common patient profiles to analyze the influence of age, gender, tumor stage, performance status, histology, and referral status as well as hospital-level characteristics on the TTT.

RESULTS AND CONCLUSIONS

TTT varies substantially between and within hospitals. The median TTT was 28 days with an inter-quartile range of 22 days. The hospital-level median TTT ranges from 17 to 68 days. TTT correlates significantly with tumor stage, performance status, and histology. The hospital-level effect, unrelated to hospital volume and type, affected TTT by several weeks at most. For most patients, TTT is within range as recommended in current guidelines. Variation in TTT seems higher for patients receiving either radiotherapy or targeted therapy, or for patients referred to another hospital and we hypothesize this is related to the complexity of the diagnostic pathway. With further advances in molecular diagnostics and precision oncology we expect variation in TTT to increase and this needs to be considered in designing optimal cancer care delivery.

摘要

目的

对分子诊断的重视程度增加,可能导致 III 期和 IV 期非小细胞肺癌患者的治疗时间(TTT)出现差异。本文介绍了在免疫治疗广泛应用之前,荷兰医院观察到的晚期 NSCLC 患者 TTT 的变化。本文旨在探讨患者之间以及医院之间 TTT 的差异。

材料和方法

基于荷兰癌症登记处,我们使用了 2016 年荷兰所有诊断为 III 期或 IV 期 NSCLC 的 78 家医院的患者水平数据(n=4096)。为了研究患者特征和医院水平的影响与 TTT(从诊断到开始治疗)之间的关系,我们对五种常见患者特征的回归模型结果进行了解释,以分析年龄、性别、肿瘤分期、体能状态、组织学和转诊状态以及医院水平特征对 TTT 的影响。

结果和结论

医院之间和内部的 TTT 差异很大。TTT 的中位数为 28 天,四分位间距为 22 天。医院水平的 TTT 中位数范围为 17 至 68 天。TTT 与肿瘤分期、体能状态和组织学显著相关。与医院规模和类型无关的医院水平效应最多影响 TTT 数周。对于大多数患者,TTT 在当前指南推荐的范围内。对于接受放疗或靶向治疗的患者,或转诊到其他医院的患者,TTT 的变化似乎更高,我们假设这与诊断途径的复杂性有关。随着分子诊断和精准肿瘤学的进一步发展,我们预计 TTT 的变化将会增加,这在设计最佳癌症治疗方案时需要考虑。

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