Journal ArticleDOI
Some practical improvements in the continual reassessment method for phase I studies
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Modifications to the Continual Reassessment Method (CRM) are presented, in which one assigns more than one subject at a time to each dose level, and each dose increase is limited to one level, which makes the CRM acceptable to clinical investigators.Abstract:
The Continual Reassessment Method (CRM) is a Bayesian phase I design whose purpose is to estimate the maximum tolerated dose of a drug that will be used in subsequent phase II and III studies. Its acceptance has been hindered by the greater duration of CRM designs compared to standard methods, as well as by concerns with excessive experimentation at high dosage levels, and with more frequent and severe toxicity. This paper presents the results of a simulation study in which one assigns more than one subject at a time to each dose level, and each dose increase is limited to one level. We show that these modifications address all of the most serious criticisms of the CRM, reducing the duration of the trial by 50-67 per cent, reducing toxicity incidence by 20-35 per cent, and lowering toxicity severity. These are achieved with minimal effects on accuracy. Most important, based on our experience at our institution, such modifications make the CRM acceptable to clinical investigators.read more
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Phase I Study of Navitoclax (ABT-263), a Novel Bcl-2 Family Inhibitor, in Patients With Small-Cell Lung Cancer and Other Solid Tumors
Leena Gandhi,D. Ross Camidge,Moacyr Ribeiro de Oliveira,Philip Bonomi,David R. Gandara,Divis Khaira,Christine L. Hann,Evelyn McKeegan,Elizabeth Litvinovich,Philip M. Hemken,Caroline Dive,Sari H. Enschede,Cathy E. Nolan,Yi-Lin Chiu,Todd A. Busman,Hao Xiong,Andrew Krivoshik,Rod A. Humerickhouse,Geoffrey I. Shapiro,Charles M. Rudin +19 more
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Sequential designs for phase I clinical trials with late-onset toxicities.
Ying Kuen Cheung,Rick Chappell +1 more
TL;DR: A simulation study shows the method's accuracy and safety are comparable with CRM's while the former takes a much shorter trial duration: a trial that would take up to 12 years to complete by the CRM could be reduced to 2–4 years by the TITE‐CRM.
References
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Journal ArticleDOI
Continual reassessment method: a practical design for phase 1 clinical trials in cancer.
TL;DR: A new approach to the design and analysis of Phase 1 clinical trials in cancer and a particularly simple model is looked at that enables the use of models whose only requirements are that locally they reasonably well approximate the true probability of toxic response.
Journal ArticleDOI
Design and analysis of phase I clinical trials.
TL;DR: In Monte Carlo simulations, two two-stage designs are found to provide reduced bias in maximum likelihood estimation of the MTD in less than ideal dose-response settings and several designs to be nearly as conservative as the standard design in terms of the proportion of patients entered at higher dose levels.
Journal ArticleDOI
Methods for dose finding studies in cancer clinical trials: a review and results of a Monte Carlo study.
John O'Quigley,Sylvie Chevret +1 more
TL;DR: It appears that the continual reassessment method is preferable to other contending schemes.
Journal ArticleDOI
The continual reassessment method in cancer phase i clinical trials: A simulation study
TL;DR: It appears that the performance ofCRM can be improved by using vague priors and initial tuning of the model to allow flexibility, and through a simulation study, the sensitivity of CRM is examined.