Literature DB >> 29103208

Model selection and averaging of nonlinear mixed-effect models for robust phase III dose selection.

Yasunori Aoki1,2, Daniel Röshammar3,4, Bengt Hamrén3, Andrew C Hooker5.   

Abstract

Population model-based (pharmacometric) approaches are widely used for the analyses of phase IIb clinical trial data to increase the accuracy of the dose selection for phase III clinical trials. On the other hand, if the analysis is based on one selected model, model selection bias can potentially spoil the accuracy of the dose selection process. In this paper, four methods that assume a number of pre-defined model structure candidates, for example a set of dose-response shape functions, and then combine or select those candidate models are introduced. The key hypothesis is that by combining both model structure uncertainty and model parameter uncertainty using these methodologies, we can make a more robust model based dose selection decision at the end of a phase IIb clinical trial. These methods are investigated using realistic simulation studies based on the study protocol of an actual phase IIb trial for an oral asthma drug candidate (AZD1981). Based on the simulation study, it is demonstrated that a bootstrap model selection method properly avoids model selection bias and in most cases increases the accuracy of the end of phase IIb decision. Thus, we recommend using this bootstrap model selection method when conducting population model-based decision-making at the end of phase IIb clinical trials.

Entities:  

Keywords:  Dose finding study; Dose–effect relationship; Mathematical modelling; Model averaging; Model selection; Pharmacometrics; Phase IIb clinical trial

Mesh:

Substances:

Year:  2017        PMID: 29103208      PMCID: PMC5686275          DOI: 10.1007/s10928-017-9550-0

Source DB:  PubMed          Journal:  J Pharmacokinet Pharmacodyn        ISSN: 1567-567X            Impact factor:   2.745


  15 in total

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Authors:  Yasunori Aoki; Rikard Nordgren; Andrew C Hooker
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  12 in total

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2.  Comparison of Model Averaging and Model Selection in Dose Finding Trials Analyzed by Nonlinear Mixed Effect Models.

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Journal:  AAPS J       Date:  2018-03-29       Impact factor: 4.009

3.  Feasibility of Exposure-Response Analyses for Clinical Dose-Ranging Studies of Drug Combinations.

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8.  Dose Finding in the Clinical Development of 60 US Food and Drug Administration-Approved Drugs Compared With Learning vs. Confirming Recommendations.

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9.  Dose-Response Mixed Models for Repeated Measures - a New Method for Assessment of Dose-Response.

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10.  Pharmacometrics meets statistics-A synergy for modern drug development.

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