Proportional Hazards Violations in Phase III Cancer Clinical Trials: A Potential Source of Trial Misinterpretation.

IF 10 1区 医学 Q1 ONCOLOGY
Timothy A Lin, Zachary R McCaw, Alex Koong, Christine Lin, Joseph Abi Jaoude, Roshal Patel, Ramez Kouzy, Molly B El Alam, Alexander D Sherry, Sonal S Noticewala, Clifton D Fuller, Charles R Thomas, Ryan Sun, J Jack Lee, Ruitao Lin, Ying Yuan, Yu Shyr, Tomer Meirson, Ethan B Ludmir
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Abstract

Purpose: Survival analyses of novel agents with long-term responders often exhibit differential hazard rates over time. Such proportional hazards violations (PHV) may reduce the power of the log-rank test and lead to misinterpretation of trial results. We aimed to characterize the incidence and study attributes associated with PHVs in phase III oncology trials and assess the utility of restricted mean survival time and maximum combination test as additional analyses.

Experimental design: Clinicaltrials.gov and PubMed were searched to identify two-arm, randomized, phase III superiority-design cancer trials with time-to-event primary endpoints and published results through 2020. Patient-level data were reconstructed from published Kaplan-Meier curves. PHVs were assessed using Schoenfeld residuals.

Results: Three hundred fifty-seven Kaplan-Meier comparisons across 341 trials were analyzed, encompassing 292,831 enrolled patients. PHVs were identified in 85/357 [23.8%; 95% confidence interval (CI), 19.7%, 28.5%] comparisons. In multivariable analysis, non-overall survival endpoints [OR, 2.16 (95% CI, 1.21, 3.87); P = 0.009] were associated with higher odds of PHVs, and immunotherapy comparisons [OR 1.94 (95% CI, 0.98, 3.86); P = 0.058] were weakly suggestive of higher odds of PHVs. Few trials with PHVs (25/85, 29.4%) prespecified a statistical plan to account for PHVs. Fourteen trials with PHVs exhibited discordant statistical signals with restricted mean survival time or maximum combination test, of which 10 (71%) reported negative results.

Conclusions: PHVs are common across therapy types, and attempts to account for PHVs in statistical design are lacking despite the potential for results exhibiting nonproportional hazards to be misinterpreted.

癌症 3 期临床试验中的比例危害违规行为:试验误解的潜在来源。
背景:对有长期应答者的新型药物进行生存期分析时,往往会出现不同时间段的危险率差异。这种比例危险违规(PHVs)可能会降低对数秩检验的能力,并导致对试验结果的误读。我们旨在描述 3 期肿瘤试验中与 PHV 相关的发生率和研究属性,并评估限制性平均生存时间(RMST)和 MaxCombo 作为附加分析的效用:对Clinicaltrials.gov和PubMed进行了检索,以确定在2020年之前进行的两臂、随机、3期优越性设计的癌症试验,这些试验的主要终点为时间到事件,并已公布结果。根据已发表的 Kaplan-Meier 曲线重建患者水平数据。使用舍恩费尔德残差法评估PHV:结果:分析了341项试验中的357项卡普兰-梅耶比较,包括292,831名入选患者。在 85/357 次(23.8%;95%CI 19.7%,28.5%)比较中发现了 PHV。在多变量分析中,非OS终点(几率比[OR] 2.16 [95%CI 1.21, 3.87];P=.009)与较高的PHV几率相关,免疫疗法比较(OR 1.94 [95%CI 0.98, 3.86];P=.058)弱提示较高的PHV几率。有PHVs的试验很少(25/85,29.4%)预先指定了考虑PHVs的统计计划。14项含有PHVs的试验显示出与RMST或MaxCombo不一致的统计信号,其中10项(71%)报告了阴性结果:PHV在各种疗法中都很常见,尽管非比例危险的结果有可能被误读,但在统计设计中考虑PHV的尝试还很缺乏。
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来源期刊
Clinical Cancer Research
Clinical Cancer Research 医学-肿瘤学
CiteScore
20.10
自引率
1.70%
发文量
1207
审稿时长
2.1 months
期刊介绍: Clinical Cancer Research is a journal focusing on groundbreaking research in cancer, specifically in the areas where the laboratory and the clinic intersect. Our primary interest lies in clinical trials that investigate novel treatments, accompanied by research on pharmacology, molecular alterations, and biomarkers that can predict response or resistance to these treatments. Furthermore, we prioritize laboratory and animal studies that explore new drugs and targeted agents with the potential to advance to clinical trials. We also encourage research on targetable mechanisms of cancer development, progression, and metastasis.
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