怀疑先验对二元结果适应性临床试验绩效的影响。

IF 1.3 4区 医学 Q4 PHARMACOLOGY & PHARMACY Pharmaceutical Statistics Pub Date : 2024-09-01 Epub Date: 2024-03-29 DOI:10.1002/pst.2387
Anders Granholm, Theis Lange, Michael O Harhay, Anders Perner, Morten Hylander Møller, Benjamin Skov Kaas-Hansen
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引用次数: 0

摘要

目前还不清楚怀疑先验如何影响适应性试验。我们评估了表达各种怀疑态度的先验对几种贝叶斯、多阶段、适应性临床试验设计在不同临床情况下使用二元结果的性能的影响。我们使用固定停止规则和校准停止规则进行了模拟,以将类型1错误率保持在5%左右。我们评估了总样本量、事件发生率、事件计数、确证概率和选择最佳臂的概率、所选臂中估计治疗效果的均方根误差(RMSE)以及理想设计百分比(IDPs;结合了臂选择概率、功率和选择劣质臂的后果),仅在确证试验中估算了RMSEs和IDPs,在未确证试验中则在选择对照臂后估算了RMSEs和IDPs。使用固定的停止规则时,先验的怀疑程度越高,样本量越大、事件越多、模拟结果为优时的IDP越高,而在模拟结果为不确定时,RMSE越低、确定性/选择最佳臂的概率越低、选择对照臂的IDP越低。通过校准停止规则,怀疑度提高对样本量和事件计数的影响减弱了,怀疑度提高增加了得出结论/选择最佳臂的概率,以及在无结果模拟中选择对照组时的IDP,而不会大幅增加样本量。采用温和适应和非信息性先验的试验设计的结果与采用弱到中度怀疑先验的更激进适应设计的结果相似。总之,在同时考虑多个性能指标时,在二元结果的自适应试验设计中使用略带怀疑的先验似乎是合理的。
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Effects of sceptical priors on the performance of adaptive clinical trials with binary outcomes.

It is unclear how sceptical priors impact adaptive trials. We assessed the influence of priors expressing a spectrum of scepticism on the performance of several Bayesian, multi-stage, adaptive clinical trial designs using binary outcomes under different clinical scenarios. Simulations were conducted using fixed stopping rules and stopping rules calibrated to keep type 1 error rates at approximately 5%. We assessed total sample sizes, event rates, event counts, probabilities of conclusiveness and selecting the best arm, root mean squared errors (RMSEs) of the estimated treatment effect in the selected arms, and ideal design percentages (IDPs; which combines arm selection probabilities, power, and consequences of selecting inferior arms), with RMSEs and IDPs estimated in conclusive trials only and after selecting the control arm in inconclusive trials. Using fixed stopping rules, increasingly sceptical priors led to larger sample sizes, more events, higher IDPs in simulations ending in superiority, and lower RMSEs, lower probabilities of conclusiveness/selecting the best arm, and lower IDPs when selecting controls in inconclusive simulations. With calibrated stopping rules, the effects of increased scepticism on sample sizes and event counts were attenuated, and increased scepticism increased the probabilities of conclusiveness/selecting the best arm and IDPs when selecting controls in inconclusive simulations without substantially increasing sample sizes. Results from trial designs with gentle adaptation and non-informative priors resembled those from designs with more aggressive adaptation using weakly-to-moderately sceptical priors. In conclusion, the use of somewhat sceptical priors in adaptive trial designs with binary outcomes seems reasonable when considering multiple performance metrics simultaneously.

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来源期刊
Pharmaceutical Statistics
Pharmaceutical Statistics 医学-统计学与概率论
CiteScore
2.70
自引率
6.70%
发文量
90
审稿时长
6-12 weeks
期刊介绍: Pharmaceutical Statistics is an industry-led initiative, tackling real problems in statistical applications. The Journal publishes papers that share experiences in the practical application of statistics within the pharmaceutical industry. It covers all aspects of pharmaceutical statistical applications from discovery, through pre-clinical development, clinical development, post-marketing surveillance, consumer health, production, epidemiology, and health economics. The Journal is both international and multidisciplinary. It includes high quality practical papers, case studies and review papers.
期刊最新文献
Beyond the Fragility Index. A Model-Based Trial Design With a Randomization Scheme Considering Pharmacokinetics Exposure for Dose Optimization in Oncology. Potential Bias Models With Bayesian Shrinkage Priors for Dynamic Borrowing of Multiple Historical Control Data. Subgroup Identification Based on Quantitative Objectives. A Bayesian Dynamic Model-Based Adaptive Design for Oncology Dose Optimization in Phase I/II Clinical Trials.
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