确定最大耐受累积剂量:TITE-CRM内的剂量重新分配

Thomas M. Braun Ph.D. , John E. Levine M.D. , James L.M. Ferrara M.D.
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引用次数: 17

摘要

我们提出的第一阶段设计是对Cheung和Chappell提出的事件持续时间再评估方法(time-to-event continuous reassessment method, TITE-CRM)的改进,该方法在每次剂量实际表示药物使用时间时非常有用。由于受试者接受较高剂量所需的时间较长,我们在每位受试者符合条件的情况下,根据最大耐受累积剂量(MTCD)的最佳估计入组每位受试者。一旦对每个先前入组的受试者进行了充分评估,我们就更新我们对MTCD的估计,并修改当前入组的受试者,如果他们目前正在接受非最佳剂量,则接受MTCD。因此,我们的方法既适用于学科之间,也适用于学科内部。我们通过模拟表明,我们的研究设计具有优异的操作特性,与TITE-CRM一样好,同时不会使更多的受试者暴露于超出MTCD的剂量。我们的模拟基于一项对骨髓移植患者的研究,该研究旨在确定重组人角质细胞生长因子可以施用多少周,同时将毒性率保持在所需的阈值以下。
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Determining a maximum tolerated cumulative dose: dose reassignment within the TITE-CRM

We present a phase I design that is a modification to the time-to-event continual reassessment method (TITE-CRM) by Cheung and Chappell that is useful when each dose actually denotes how long a drug is administered. Because of the lengthy duration required for subjects receiving the higher doses, we enroll each subject on the best estimate of the maximum tolerated cumulative dose (MTCD) as soon as each subject is eligible. Once each previously enrolled subject is fully evaluated, we update our estimate of the MTCD and modify currently enrolled subjects to receive the MTCD if they are currently receiving a nonoptimal dose. Thus, our method is adaptive both between subjects and within subjects. We show through simulation that our study design has excellent operating characteristics that are as good as the TITE-CRM while not exposing greater numbers of subjects to doses beyond the MTCD. Our simulations are based upon a study in bone marrow transplant patients that seeks to determine how many weeks of recombinant human keratinocyte growth factor can be administered while keeping toxicity rates below a desired threshold.

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