Xiaosong Shi , Jo A. Wick , Danielle N. Christifano , Susan E. Carlson , Alexandra R. Brown , Dinesh Pal Mudaranthakam , Byron J. Gajewski
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This survey's inclusion in future trials can provide critical insights for informing clinical practices.</p></div><div><h3>Objective</h3><p>To optimize a Phase III trial design, ADORE Precision, aiming at assessing DHA supplement (200 vs. 1000 mg/day) on reducing ePTB among pregnant women with a low baseline DHA.</p></div><div><h3>Methods</h3><p>We propose a Bayesian Hybrid Response Adaptive Randomization (RAR) Design utilizing a finite mixture model to characterize gestational age at birth. Subsequently, a dichotomized ePTB outcome is used to inform trial design using RAR. Simulation studies were conducted to compare a Fixed Design, an Adaptive Design with early stopping, an ADORE-like Adaptive RAR Design, and two new Hybrid Designs with different hyperpriors.</p></div><div><h3>Discussion</h3><p>Simulation reveals several advantages of the RAR designs, such as higher allocation to the more promising dose and a trial duration reduction. 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引用次数: 0
摘要
背景:早期早产(ePTB)--妊娠 34 周前出生--是一项重大的公共卫生挑战。两项随机试验表明,接受高剂量二十二碳六烯酸(DHA)补充剂的孕妇早产率有所下降。其中一项是 "DHA 减少早期早产评估"(ADORE)。该研究在二次分析中采用了一项调查,确定了 DHA 水平较低的妇女,发现她们从高剂量 DHA 补充剂中获益更大。将这项调查纳入未来的试验可为临床实践提供重要的启示:优化 ADORE Precision III 期试验设计,旨在评估 DHA 补充剂(200 毫克/天与 1000 毫克/天)对减少基线 DHA 水平较低的孕妇中的 ePTB 感染的作用:我们提出了一种贝叶斯混合反应自适应随机化(RAR)设计,利用有限混合模型来描述出生时的胎龄。随后,利用 RAR 将 ePTB 结果二分法用于试验设计。模拟研究比较了固定设计、早期停止的自适应设计、类似 ADORE 的自适应 RAR 设计以及两种具有不同超前性的新型混合设计:讨论:模拟显示了 RAR 设计的几个优点,如更多分配到更有前景的剂量和缩短试验持续时间。提出的混合 RAR 设计解决了自适应 RAR 中观察到的统计功率下降问题。新的设计模型显示出对超前选择的稳健性。我们向 ADORE Precision 推荐混合 RAR 设计 1,希望它能产生精确的测定结果,这对促进我们对该领域的了解至关重要。
DHA supplementation for early preterm birth prevention: An application of Bayesian finite mixture models to adaptive clinical trial design optimization
Background
Early preterm birth (ePTB) - born before 34 weeks of gestation - poses a significant public health challenge. Two randomized trials indicated an ePTB reduction among pregnant women receiving high-dose docosahexaenoic acid (DHA) supplementation. One of them is Assessment of DHA on Reducing Early Preterm Birth (ADORE). A survey employed in its secondary analysis identified women with low DHA levels, revealing that they derived greater benefits from high-dose DHA supplementation. This survey's inclusion in future trials can provide critical insights for informing clinical practices.
Objective
To optimize a Phase III trial design, ADORE Precision, aiming at assessing DHA supplement (200 vs. 1000 mg/day) on reducing ePTB among pregnant women with a low baseline DHA.
Methods
We propose a Bayesian Hybrid Response Adaptive Randomization (RAR) Design utilizing a finite mixture model to characterize gestational age at birth. Subsequently, a dichotomized ePTB outcome is used to inform trial design using RAR. Simulation studies were conducted to compare a Fixed Design, an Adaptive Design with early stopping, an ADORE-like Adaptive RAR Design, and two new Hybrid Designs with different hyperpriors.
Discussion
Simulation reveals several advantages of the RAR designs, such as higher allocation to the more promising dose and a trial duration reduction. The proposed Hybrid RAR Designs addresses the statistical power drop observed in Adaptive RAR. The new design model shows robustness to hyperprior choices. We recommend Hybrid RAR Design 1 for ADORE Precision, anticipating that it will yield precise determinations, which is crucial for advancing our understanding in this field.
期刊介绍:
Contemporary Clinical Trials is an international peer reviewed journal that publishes manuscripts pertaining to all aspects of clinical trials, including, but not limited to, design, conduct, analysis, regulation and ethics. Manuscripts submitted should appeal to a readership drawn from disciplines including medicine, biostatistics, epidemiology, computer science, management science, behavioural science, pharmaceutical science, and bioethics. Full-length papers and short communications not exceeding 1,500 words, as well as systemic reviews of clinical trials and methodologies will be published. Perspectives/commentaries on current issues and the impact of clinical trials on the practice of medicine and health policy are also welcome.