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Bayesian nonparametric estimation of targeted agent effects on biomarker change to predict clinical outcome
Author(s) -
Graziani Rebecca,
Guindani Michele,
Thall Peter F.
Publication year - 2015
Publication title -
biometrics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.298
H-Index - 130
eISSN - 1541-0420
pISSN - 0006-341X
DOI - 10.1111/biom.12250
Subject(s) - biomarker , covariate , nonparametric statistics , bayesian probability , outcome (game theory) , clinical trial , bayes' theorem , oncology , medicine , computer science , econometrics , machine learning , artificial intelligence , biology , mathematics , biochemistry , mathematical economics
Summary The effect of a targeted agent on a cancer patient's clinical outcome putatively is mediated through the agent's effect on one or more early biological events. This is motivated by pre‐clinical experiments with cells or animals that identify such events, represented by binary or quantitative biomarkers. When evaluating targeted agents in humans, central questions are whether the distribution of a targeted biomarker changes following treatment, the nature and magnitude of this change, and whether it is associated with clinical outcome. Major difficulties in estimating these effects are that a biomarker's distribution may be complex, vary substantially between patients, and have complicated relationships with clinical outcomes. We present a probabilistically coherent framework for modeling and estimation in this setting, including a hierarchical Bayesian nonparametric mixture model for biomarkers that we use to define a functional profile of pre‐versus‐post‐treatment biomarker distribution change. The functional is similar to the receiver operating characteristic used in diagnostic testing. The hierarchical model yields clusters of individual patient biomarker profile functionals, and we use the profile as a covariate in a regression model for clinical outcome. The methodology is illustrated by analysis of a dataset from a clinical trial in prostate cancer using imatinib to target platelet‐derived growth factor, with the clinical aim to improve progression‐free survival time.

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