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随机撤药设计:在细胞毒性抗肿瘤药物中的应用。

Randomized discontinuation design: application to cytostatic antineoplastic agents.

作者信息

Rosner Gary L, Stadler Walter, Ratain Mark J

机构信息

Cancer and Leukemia Group B Statistical Office and Department of Biostatistics, The University of Texas M.D. Anderson Cancer Center, Houston, TX 77030-4009, USA.

出版信息

J Clin Oncol. 2002 Nov 15;20(22):4478-84. doi: 10.1200/JCO.2002.11.126.

Abstract

PURPOSE

Propose a phase II study design to evaluate the activity of a putative cytostatic agent, acknowledging heterogeneity of tumor growth rates in the population of patients.

METHODS

In the setting of renal cell carcinoma, some patients' tumors will grow slowly naturally. An appropriate design has to distinguish antiproliferative activity attributable to the novel agent from indolent disease. We propose a randomized discontinuation design that initially treats all patients with the study agent (stage 1) and then randomizes in a double-blind fashion to continuing therapy or placebo only those patients whose disease is stable (stage 2). This design allows the investigators to determine if apparent slow tumor growth is attributable to the drug or to selection of patients with naturally slow-growing tumors.

RESULTS

By selecting a more homogeneous population, the randomized portion of the study requires fewer patients than would a study randomizing all patients at entry. The design also avoids potential confounding because of heterogeneous tumor growth. Because the two randomly assigned treatment groups each comprise patients with apparently slow growing tumors, any difference between the groups in disease progression after randomization is more likely a result of the study drug and less likely a result of imbalance with respect to tumor growth rates. Stopping rules during the initial open-label stage and the subsequent randomized trial stage allow one to reduce the overall sample size. Expected average tumor growth rate is an important consideration when deciding the duration of follow-up for the two stages.

CONCLUSION

The randomized discontinuation design is a feasible alternative phase II study design for determining activity of possibly cytostatic anticancer agents.

摘要

目的

提出一项II期研究设计,以评估一种假定的细胞生长抑制剂的活性,同时认识到患者群体中肿瘤生长速率的异质性。

方法

在肾细胞癌的背景下,一些患者的肿瘤自然生长缓慢。一种合适的设计必须区分新型药物引起的抗增殖活性与惰性疾病。我们提出一种随机停药设计,该设计最初用研究药物治疗所有患者(第1阶段),然后仅将疾病稳定的患者以双盲方式随机分为继续治疗组或安慰剂组(第2阶段)。这种设计使研究人员能够确定明显缓慢的肿瘤生长是归因于药物还是归因于选择了自然生长缓慢的肿瘤患者。

结果

通过选择更具同质性的人群,该研究的随机分组部分所需的患者人数比在入组时将所有患者随机分组的研究要少。该设计还避免了由于肿瘤生长异质性导致的潜在混杂因素。由于两个随机分配的治疗组均包括肿瘤生长明显缓慢的患者,因此随机分组后两组在疾病进展方面的任何差异更可能是研究药物的结果,而不太可能是肿瘤生长速率不平衡的结果。初始开放标签阶段和随后的随机试验阶段的停药规则可以减少总体样本量。在确定两个阶段的随访持续时间时,预期的平均肿瘤生长速率是一个重要的考虑因素。

结论

随机停药设计是确定可能的细胞生长抑制性抗癌药物活性的一种可行的替代II期研究设计。

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