• Sally Hunsberger, Lawrence V Rubinstein, Janet Dancey, and Edward L Korn.
• Biometrics Research Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA. sallyh@ctep.nci.nih.gov
• Stat Med. 2005 Jul 30; 24 (14): 2171-81.

AbstractTraditional phase I dose-finding studies for chemotoxic agents base dose escalation on toxicity, with escalation continuing until unacceptable toxicity is observed. Recent development of molecularly targeted agents that have little or no toxicity in the therapeutic dose range has raised questions over the best study designs for phase I studies. Two types of designs are proposed and evaluated in this paper. In these designs, escalation is based on a binary response that indicates whether or not the agent has had the desired effect on the molecular target. One design is developed to ensure that if the true target response rate is low there will be a high probability of escalating and if the true target response rate is high there will be a low probability of escalating. The other design is developed to continue to escalate as long as the true response rate is increasing and to stop escalating when the response rate plateaus or decreases. A limited simulation study is performed and the designs are compared with respect to the dose level at the end of escalation and the number of patients treated on study.

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