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临床试验中西蒙两阶段设计的确切p值。

Exact p-values for Simon's two-stage designs in clinical trials.

作者信息

Shan Guogen, Zhang Hua, Jiang Tao, Peterson Hanna, Young Daniel, Ma Changxing

机构信息

Department of Environmental and Occupational Health, Epidemiology and Biostatistics Program, School of Community Health Sciences, University of Nevada Las Vegas, Las Vegas, NV 89154.

Zhejiang Gongshang University, Hangzhou, Zhejiang, China, 310018.

出版信息

Stat Biosci. 2016;8(2):351-357. doi: 10.1007/s12561-016-9152-1. Epub 2016 Jun 16.

DOI:10.1007/s12561-016-9152-1
PMID:28003856
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5167475/
Abstract

In a one-sided hypothesis testing problem in clinical trials, the monotonic condition of a tail probability function is fundamentally important to guarantee that the actual type I and II error rates occur at the boundary of their associated parameter spaces. Otherwise, one has to search for the actual rates over the complete parameter space, which could be very computationally intensive. This important property has been extensively studied in traditional one-stage study settings (e.g., non-inferiority or superiority between two binomial proportions), but there is very limited research for this property in a two-stage design setting, e.g., Simon's two-stage design. In this note, we theoretically prove that the tail probability is an increasing function of the parameter in Simon's two-stage design. This proof not only provides theoretical justification that p-value occurs at the boundary of the parameter space, but also helps to reduce the computational intensity for study design search.

摘要

在临床试验的单侧假设检验问题中,尾概率函数的单调性对于确保实际的I型和II型错误率出现在其相关参数空间的边界至关重要。否则,就必须在整个参数空间中搜索实际错误率,这在计算上可能非常密集。这一重要性质在传统的单阶段研究设置(例如,两个二项比例之间的非劣效性或优越性)中已得到广泛研究,但在两阶段设计设置(例如西蒙两阶段设计)中对该性质的研究非常有限。在本笔记中,我们从理论上证明了在西蒙两阶段设计中尾概率是参数的增函数。这一证明不仅为p值出现在参数空间边界提供了理论依据,还有助于降低研究设计搜索的计算强度。

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