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首页> 外文期刊>BMC Medical Research Methodology >Impact of a non-constant baseline hazard on detection of time-dependent treatment effects: a simulation study
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Impact of a non-constant baseline hazard on detection of time-dependent treatment effects: a simulation study

机译:非恒定基线危害对时间依赖治疗效果检测的影响:模拟研究

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摘要

Non-proportional hazards are common with time-to-event data but the majority of randomised clinical trials (RCTs) are designed and analysed using approaches which assume the treatment effect follows proportional hazards (PH). Recent advances in oncology treatments have identified two forms of non-PH of particular importance - a time lag until treatment becomes effective, and an early effect of treatment that ceases after a period of time. In sample size calculations for treatment effects on time-to-event outcomes where information is based on the number of events rather than the number of participants, there is crucial importance in correct specification of the baseline hazard rate amongst other considerations. Under PH, the shape of the baseline hazard has no effect on the resultant power and magnitude of treatment effects using standard analytical approaches. However, in a non-PH context the appropriateness of analytical approaches can depend on the shape of the underlying hazard. A simulation study was undertaken to assess the impact of clinically plausible non-constant baseline hazard rates on the power, magnitude and coverage of commonly utilized regression-based measures of treatment effect and tests of survival curve difference for these two forms of non-PH used in RCTs with time-to-event outcomes. In the presence of even mild departures from PH, the power, average treatment effect size and coverage were adversely affected. Depending on the nature of the non-proportionality, non-constant event rates could further exacerbate or somewhat ameliorate the losses in power, treatment effect magnitude and coverage observed. No single summary measure of treatment effect was able to adequately describe the full extent of a potentially time-limited treatment benefit whilst maintaining power at nominal levels. Our results show the increased importance of considering plausible potentially non-constant event rates when non-proportionality of treatment effects could be anticipated. In planning clinical trials with the potential for non-PH, even modest departures from an assumed constant baseline hazard could appreciably impact the power to detect treatment effects depending on the nature of the non-PH. Comprehensive analysis plans may be required to accommodate the description of time-dependent treatment effects.
机译:非比例危害与时间 - 事件数据很常见,但是大多数随机临床试验(RCT)使用方法设计和分析,所述方法假设治疗效果遵循比例危害(pH)。肿瘤学治疗的最新进展已经确定了两种形式的非pH值特别重要 - 在治疗生效之前的时间滞后,并且在一段时间后停止的治疗早期效果。在样本量计算的处理效果的情况下,信息基于事件的数量而不是参与者的数量,在其他考虑因素之间的正确规范中具有至关重要的重要性。在pH下,基线危险的形状对使用标准分析方法的处理效果的所得功率和幅度没有影响。然而,在非pH的情况下,分析方法的适当性可以取决于潜在危险的形状。进行了模拟研究,以评估临床合理的非恒定基线危险率对普通利用基于回归措施的功率,幅度和覆盖的影响以及对使用这两种形式的非pH值的存活曲线差异的试验曲线差异在RCT中,与事件发生时间结果。在从pH的温和偏离的情况下,对电力,平均处理效果大小和覆盖产生不利影响。根据非比例性的性质,非恒定事件率可以进一步加剧或有些改善能力的损失,观察到的损失,观察到的损失。没有单一的处理效果测量能够充分描述潜在限量的治疗益处的全部范围,同时保持标称水平的功率。我们的结果表明,当可以预期的治疗效果的非比例时,考虑合理的潜在非恒定事件率的重要性增加。在规划具有非pH的潜力的临床试验中,即使是假设的恒定基线危害的偏离偏离也可能会显着影响根据非pH的性质来检测治疗效果的能力。可能需要综合分析计划来适应时间依赖治疗效果的描述。

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