Sample size determination in group-sequential clinical trials with two co-primary endpoints

AsakuraK.; HamasakiT.; SugimotoT.; HayashiK.; EvansS.R.; SozuT.

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Sample size determination in group-sequential clinical trials with two co-primary endpoints

机译：在具有两个共同主要终点的组序贯临床试验中确定样本量

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We discuss sample size determination in group-sequential designs with two endpoints as co-primary. We derive the power and sample size within two decision-making frameworks. One is to claim the test intervention's benefit relative to control when superiority is achieved for the two endpoints at the same interim timepoint of the trial. The other is when superiority is achieved for the two endpoints at any interim timepoint, not necessarily simultaneously. We evaluate the behaviors of sample size and power with varying design elements and provide a real example to illustrate the proposed sample size methods. In addition, we discuss sample size recalculation based on observed data and evaluate the impact on the power and Type I error rate.

机译：我们讨论以两个端点为共同主要指标的群体顺序设计中的样本量确定。我们在两个决策框架内得出功效和样本量。一种是声称在试验的相同过渡时间点上两个终点均达到优势时，测试干预相对于对照的益处。另一个是在任何过渡时间点（不一定同时）实现两个端点的优势时。我们使用不同的设计元素评估样本量和功效的行为，并提供一个真实的例子来说明所提出的样本量方法。此外，我们讨论了基于观测数据的样本量重新计算，并评估了对功效和I型错误率的影响。

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《Statistics in medicine》 |2014年第17期|共17页
作者
AsakuraK.; HamasakiT.; SugimotoT.; HayashiK.; EvansS.R.; SozuT.;
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正文语种 eng
中图分类卫生调查与统计;
关键词
Average sample number; Co-primary endpoints; Conditional power; Cui-Hung-Wang statistics; Group-sequential methods; Maximum sample size; Sample size recalculation; Type I error;

机译：平均样本数;共同主要终点;条件功效;崔鸿旺统计;群序法;最大样本量;样本量重新计算;I型误差;

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专利

1. Sample size determination in group-sequential clinical trials with two co-primary endpoints [J] . AsakuraK., HamasakiT., SugimotoT., Statistics in medicine . 2014,第17期

机译：在具有两个共同主要终点的组序贯临床试验中确定样本量
2. Sample size determination in superiority clinical trials with multiple co-primary correlated endpoints. [J] . Sozu T., Sugimoto T., Hamasaki T. Journal of biopharmaceutical statistics . 2011,第4期

机译：具有多个共同主要相关终点的优越性临床试验中的样本量确定。
3. Sample Size Determination in Superiority Clinical Trials with Multiple Co-Primary Correlated Endpoints [J] . Takashi Sozua* Tomoyuki Sugimotob, Toshimitsu Hamasakib Journal of Biopharmaceutical Statistics . 2011,第4期

机译：具有多个共同主要相关终点的优势临床试验中的样本量确定
4. Hybrid research simulation modeling for making decisions on sample size and power of randomized clinical trials considering expected net benefits [C] . Ismail Abbas Simulation Conference . 2017

机译：混合研究模拟模型，用于在考虑预期净收益的情况下决定随机临床试验的样本量和功效
5. Applying survival analysis techniques to interim analysis and sample size reassessment of clinical trials with a dichotomous endpoint. [D] . Pedley, Alison L. 2011

机译：将生存分析技术应用于具有二分终点的临床试验的中期分析和样本量重新评估。
6. Sample size determination in group-sequential clinical trials with two co-primary endpoints [O] . Koko Asakura, Toshimitsu Hamasaki, Tomoyuki Sugimoto, -1

机译：在具有两个共同主要终点的小组连续临床试验中确定样本量
7. Sample size determination in group-sequential clinical trials with two co-primary endpoints [O] . Koko Asakura, Toshimitsu Hamasaki, Tomoyuki Sugimoto, 2014

机译：具有两个共同初级终点的分组顺序临床试验中的样本尺寸测定

Sample size determination in group-sequential clinical trials with two co-primary endpoints

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