Fu Pingfu, Dowlati Afshin, Schluchter Mark
Department of Epidemiology and Biostatistics, Case Western Reserve University, 10900 Euclid Ave, Cleveland, OH 44106, USA.
J Clin Oncol. 2009 Sep 1;27(25):4135-41. doi: 10.1200/JCO.2008.19.6709. Epub 2009 Jul 27.
Enrichment based on molecular characteristics has emerged as an important inclusion criterion in phase II trials of targeted anticancer agents. In this study, we evaluate a well-described method of population enrichment by tumor growth characteristics in the early development stage of targeted cytostatic agents.
For some solid tumors, such as pancreatic carcinoma, using a time-to-event end point (eg, time to disease progression) to evaluate the efficacy of a cytostatic agent in a phase II trial is more relevant than clinical response by Response Evaluation Criteria in Solid Tumors. In this setting, we compared the power of the randomized discontinuation and upfront randomization designs under two previously proposed tumor growth models for treatment effect when the end point is time-to-event.
By selecting patients with more homogeneous tumor growth characteristics, the randomized discontinuation design is more efficient than the upfront randomization design when treatment benefit is restricted to slow-growing tumors. Under a model where only a subset of patients expressing the molecular target are sensitive to the agent, the randomized discontinuation design is more powerful than the upfront randomization design when the treatment effect is small; and vice versa when the treatment effect is moderate to large.
For selected targeted agents where a bioassay to select patients expressing the specific molecular target is not available, the randomized discontinuation design is a feasible alternative patient enrichment strategy in certain disease settings and provides a reasonable platform to evaluate drugs before phase III testing.
基于分子特征的富集已成为靶向抗癌药物II期试验的一项重要纳入标准。在本研究中,我们在靶向细胞生长抑制剂的早期研发阶段,评估一种通过肿瘤生长特征进行人群富集的成熟方法。
对于某些实体瘤,如胰腺癌,在II期试验中使用事件发生时间终点(如疾病进展时间)来评估细胞生长抑制剂的疗效,比实体瘤疗效评价标准中的临床反应更具相关性。在此背景下,当终点为事件发生时间时,我们在两种先前提出的肿瘤生长模型下,比较了随机停药设计和预先随机化设计检测治疗效果的效能。
通过选择肿瘤生长特征更均匀的患者,当治疗益处仅限于生长缓慢的肿瘤时,随机停药设计比预先随机化设计更有效。在只有一部分表达分子靶点的患者对药物敏感的模型下,当治疗效果较小时,随机停药设计比预先随机化设计效能更高;而当治疗效果为中度至较大时,情况则相反。
对于某些没有生物测定法来选择表达特定分子靶点患者的靶向药物,随机停药设计在某些疾病背景下是一种可行的替代患者富集策略,并为III期试验前评估药物提供了一个合理的平台。