Optimal, minimax and admissible two-stage design for phase II oncology clinical trials.
Fei QinJingwei WuFeng ChenYongyue WeiYang ZhaoZhiwei JiangJianling BaiHao YuPublished in: BMC medical research methodology (2020)
Whenever (p0, p1) is pre-specified, it is better to explore in the range of probability q, based on relative importance between maximum sample size and expected sample size, and determine which design to choose. When q is unknown, optimal design may be more favorable for drugs with limited efficacy. Contrarily, minimax design is recommended if treatment demonstrates impressive efficacy.