Abstract
Background: Awareness 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. Methods: The 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.
Original language | English |
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Article number | 162 |
Pages (from-to) | 162 |
Number of pages | 1 |
Journal | BMC medical research methodology |
Volume | 20 |
Issue number | 1 |
DOIs | |
Publication status | Published - 22 Jun 2020 |
Keywords
- Adaptive trial design
- Clinical trial design
- Dose-finding
- Late toxicity
- Phase I
- TiTE-CRM