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Hauptverfasser: Boulet, Sandrine, Comets, Emmanuelle, Guillon, Antoine, Aulin, Linda B. S., Michelet, Robin, Kloft, Charlotte, Zohar, Sarah, Ursino, Moreno
Format: Preprint
Veröffentlicht: 2024
Schlagworte:
Online-Zugang:https://arxiv.org/abs/2412.03298
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author Boulet, Sandrine
Comets, Emmanuelle
Guillon, Antoine
Aulin, Linda B. S.
Michelet, Robin
Kloft, Charlotte
Zohar, Sarah
Ursino, Moreno
author_facet Boulet, Sandrine
Comets, Emmanuelle
Guillon, Antoine
Aulin, Linda B. S.
Michelet, Robin
Kloft, Charlotte
Zohar, Sarah
Ursino, Moreno
contents Conventionally, a first-in-human phase I trial in healthy volunteers aims to confirm the safety of a drug in humans. In such situations, volunteers should not suffer from any safety issues and simple algorithm-based dose-escalation schemes are often used. However, to avoid too many clinical trials in the future, it might be appealing to design these trials to accumulate information on the link between dose and efficacy/activity under strict safety constraints. Furthermore, an increasing number of molecules for which the increasing dose-activity curve reaches a plateau are emerging.In a phase I dose-finding trial context, our objective is to determine, under safety constraints, among a set of doses, the lowest dose whose probability of activity is closest to a given target. For this purpose, we propose a two-stage dose-finding design. The first stage is a typical algorithm dose escalation phase that can both check the safety of the doses and accumulate activity information. The second stage is a model-based dose-finding phase that involves selecting the best dose-activity model according to the plateau location.Our simulation study shows that our proposed method performs better than the common Bayesian logistic regression model in selecting the optimal dose.
format Preprint
id arxiv_https___arxiv_org_abs_2412_03298
institution arXiv
publishDate 2024
record_format arxiv
spellingShingle Straightforward Phase I Dose-Finding Design for Healthy Volunteers Accounting for Surrogate Activity Biomarkers
Boulet, Sandrine
Comets, Emmanuelle
Guillon, Antoine
Aulin, Linda B. S.
Michelet, Robin
Kloft, Charlotte
Zohar, Sarah
Ursino, Moreno
Applications
Conventionally, a first-in-human phase I trial in healthy volunteers aims to confirm the safety of a drug in humans. In such situations, volunteers should not suffer from any safety issues and simple algorithm-based dose-escalation schemes are often used. However, to avoid too many clinical trials in the future, it might be appealing to design these trials to accumulate information on the link between dose and efficacy/activity under strict safety constraints. Furthermore, an increasing number of molecules for which the increasing dose-activity curve reaches a plateau are emerging.In a phase I dose-finding trial context, our objective is to determine, under safety constraints, among a set of doses, the lowest dose whose probability of activity is closest to a given target. For this purpose, we propose a two-stage dose-finding design. The first stage is a typical algorithm dose escalation phase that can both check the safety of the doses and accumulate activity information. The second stage is a model-based dose-finding phase that involves selecting the best dose-activity model according to the plateau location.Our simulation study shows that our proposed method performs better than the common Bayesian logistic regression model in selecting the optimal dose.
title Straightforward Phase I Dose-Finding Design for Healthy Volunteers Accounting for Surrogate Activity Biomarkers
topic Applications
url https://arxiv.org/abs/2412.03298