Abstract
BackgroundAwareness of model-based designs for dose-finding studies such as the Continual Reassessment Method (CRM) is now becoming more commonplace amongst clinicians, statisticians and trial management staff. In some settings toxicities can occur a long time after treatment has finished, resulting in extremely long, interrupted, CRM design trials. The Time-to-Event CRM (TiTE-CRM), a modification to the original CRM, accounts for the timing of late-onset toxicities and results in shorter trial duration. In this article, we discuss how to design and deliver a trial using this method, from the grant application stage through to dissemination, using two radiotherapy trials as examples.MethodsThe TiTE-CRM encapsulates the dose-toxicity relationship with a statistical model. The model incorporates observed toxicities and uses a weight to account for the proportion of completed follow-up of participants without toxicity. This model uses all available data to determine the next participant’s dose and subsequently declare the maximum tolerated dose.We focus on two trials designed by the authors to illustrate practical issues when designing, setting up, and running such studies.ResultsIn setting up a TiTE-CRM trial, model parameters need to be defined and the time element involved might cause complications, therefore looking at operating characteristics through simulations is essential. At the grant application stage, we suggest resources to fund statisticians’ time before funding is awarded and make recommendations for the level of detail to include in funding applications. While running the trial, close contact of all involved staff is required as a dose decision is made each time a participant is recruited. We suggest ways of capturing data in a timely manner and give example code in R for design and delivery of the trial. Finally, we touch upon dissemination issues while the trial is running and upon completion.ConclusionModel-based designs can be complex. We hope this paper will help clinical trial teams to demystify the conduct of TiTE-CRM trials and be a starting point for using this methodology in practice.
Highlights
Awareness of model-based designs for dose-finding studies such as the Continual Reassessment Method (CRM) is becoming more commonplace amongst clinicians, statisticians and trial management staff
We hope this paper will help clinical trial teams to demystify the conduct of TiTE-CRM trials and be a starting point for using this methodology in practice
The biggest challenge with the amount of time required to design a TiTE-CRM study, for academic trials units, is how to fund the statisticians’ time during this period. This is a consideration for all clinical trial grant applications, TiTE-CRM designs
Summary
Awareness of model-based designs for dose-finding studies such as the Continual Reassessment Method (CRM) is becoming more commonplace amongst clinicians, statisticians and trial management staff. Continual reassessment method (CRM) designs for early-phase trials are beginning to be discussed outside of the statistical literature [1]. The TiTE-CRM may be applied to settings where dose limiting toxicities are expected to occur beyond a typical observation period of a few weeks. This is relevant to the field of radiotherapy, where toxicities can often occur up to and sometimes longer than 6 months after treatment [5]. Participants can be continually recruited, reducing the overall duration of the trial, and all information is used to assign new participants to the best dose [6]
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