Surrogacy assessment using principal stratification with multivariate normal and Gaussian copula models

Background The validation of intermediate markers as surrogate markers (S) for the true outcome of interest (T) in clinical trials offers the possibility for trials to be run more quickly and cheaply by using the surrogate endpoint in place of the true endpoint. Purpose Working within a principal st...

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Bibliographic Details
Published inClinical trials (London, England) Vol. 12; no. 4; pp. 317 - 322
Main Authors Taylor, Jeremy MG, Conlon, Anna SC, Elliott, Michael R
Format Journal Article
LanguageEnglish
Published London, England SAGE Publications 01.08.2015
Sage Publications Ltd
Subjects
Bayes Theorem
Bayesian analysis
Biomarkers - analysis
Causality
Clinical outcomes
Clinical trials
Clinical Trials as Topic
Colorectal Neoplasms
Humans
Models, Statistical
Multivariate Analysis
Normal Distribution
potential outcomes
Bayesian estimation
surrogate endpoint
causal inference
Gaussian copula
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Summary:Background The validation of intermediate markers as surrogate markers (S) for the true outcome of interest (T) in clinical trials offers the possibility for trials to be run more quickly and cheaply by using the surrogate endpoint in place of the true endpoint. Purpose Working within a principal stratification framework, we propose causal quantities to evaluate surrogacy using a Gaussian copula model for an ordinal surrogate and time-to-event final outcome. The methods are applied to data from four colorectal cancer clinical trials, where S is tumor response and T is overall survival. Methods For the Gaussian copula model, a Bayesian estimation strategy is used and, as some parameters are not identifiable from the data, we explore the use of informative priors that are consistent with reasonable assumptions in the surrogate marker setting to aid in estimation. Results While there is some bias in the estimation of the surrogacy quantities of interest, the estimation procedure does reasonably well at distinguishing between poor and good surrogate markers. Limitations Some of the parameters of the proposed model are not identifiable from the data, and therefore, assumptions must be made in order to aid in their estimation. Conclusions The proposed quantities can be used in combination to provide evidence about the validity of S as a surrogate marker for T.
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ISSN:1740-7745
1740-7753
DOI:10.1177/1740774514561046