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引入纵向累积剂量来描述随时间变化的化疗模式:以结肠癌试验为例。

Introducing longitudinal cumulative dose to describe chemotherapy patterns over time: Case study of a colon cancer trial.

机构信息

Department of Epidemiology, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.

Department of Medicine, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.

出版信息

Int J Cancer. 2021 Jul 15;149(2):394-402. doi: 10.1002/ijc.33565. Epub 2021 Mar 26.

Abstract

Adjuvant chemotherapy regimens take months to complete. Despite this, studies evaluate chemotherapy adherence via measures assessed at the end of treatment (eg, number of patients missing any dose, relative dose intensity [RDI]). This approach ignores information like the timing of treatment delays. We propose longitudinal cumulative dose (LCD) to integrate impacts of dose reductions, missed doses and dose delays over time. We obtained data from the 2246 participants in the MOSAIC trial randomized to FOLFOX (all three agents) or 5-FU/LV (only 5-fluorouracil and leucovorin). We evaluated proportions of patients stopping treatment early and reducing, missing or delaying a dose in each arm for each chemotherapy agent at each cycle. We calculated LCD, the fraction of the final standard dose a participant reached by a given day, for each participant and each agent and compared it over time and at 24 weeks between treatment arms. Participants randomized to FOLFOX were more likely to stop treatment, reduce doses, miss doses or delay cycles; these differences increased over time. Median LCD for oxaliplatin in the FOLFOX arm at 24 weeks was 77%. The LCD for 5-fluorouracil differed between arms (FOLFOX arm median: 81%; 5-FU/LV arm median: 96%). Visualizing LCD highlighted the timing of deviations from standard administration in a way RDI could not, with major differences in 5-fluorouracil LCD across treatment arms beginning after the sixth dose. Further evaluation of LCD and its impacts on clinical outcomes may clarify mechanisms for heterogeneous patient outcomes.

摘要

辅助化疗方案需要数月时间才能完成。尽管如此,研究仍通过治疗结束时评估的措施(例如,错过任何剂量的患者数量、相对剂量强度 [RDI])来评估化疗的依从性。这种方法忽略了治疗延迟的时间等信息。我们提出了纵向累积剂量(LCD),以整合剂量减少、错过剂量和剂量延迟随时间的影响。我们从 MOSAIC 试验的 2246 名参与者中获得了数据,这些参与者被随机分配到 FOLFOX(三种药物均使用)或 5-FU/LV(仅使用氟尿嘧啶和亚叶酸)。我们评估了每个周期中每个手臂的每个化疗药物中提前停止治疗、减少剂量、错过剂量或延迟剂量的患者比例。我们为每个参与者和每个药物计算了 LCD,即参与者在特定日期达到最终标准剂量的分数,并比较了不同治疗手臂之间随时间的变化和 24 周时的变化。接受 FOLFOX 治疗的参与者更有可能停止治疗、减少剂量、错过剂量或延迟周期;这些差异随着时间的推移而增加。在 24 周时,FOLFOX 组奥沙利铂的中位 LCD 为 77%。氟尿嘧啶的 LCD 在两组之间存在差异(FOLFOX 组中位数:81%;5-FU/LV 组中位数:96%)。可视化 LCD 以 RDI 无法实现的方式突出了标准给药偏离的时间,治疗组之间的氟尿嘧啶 LCD 差异在第六次剂量后开始出现。进一步评估 LCD 及其对临床结果的影响可能有助于阐明导致患者结果异质性的机制。

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