Motivation
In gene expression and genome-wide association studies, the identification of interaction effects is an important and challenging issue owing to its ultrahigh-dimensional nature. In particular, contaminated data and right-censored survival outcome make the associated feature screening even challenging.
Results
In this article, we propose an inverse probability-of-censoring weighted Kendall’s tau statistic to measure association of a survival trait with biomarkers, as well as a Kendall’s partial correlation statistic to measure the relationship of a survival trait with an interaction variable conditional on the main effects. The Kendall’s partial correlation is then used to conduct interaction screening. Simulation studies under various scenarios are performed to compare the performance of our proposal with some commonly available methods. In the real data application, we utilize our proposed method to identify epistasis associated with the clinical survival outcomes of non-small-cell lung cancer, diffuse large B-cell lymphoma and lung adenocarcinoma patients. Both simulation and real data studies demonstrate that our method performs well and outperforms existing methods in identifying main and interaction biomarkers.
Availability and implementation
R-package ‘IPCWK’ is available to implement this method, together with a reference manual describing how to perform the ‘IPCWK’ package.
Supplementary information
Supplementary data are available at Bioinformatics online.
Motivation
In high-dimensional genetic/genomic data, the identification of genes related to clinical survival trait is a challenging and important issue. In particular, right-censored survival outcomes and contaminated biomarker data make the relevant feature screening difficult. Several independence screening methods have been developed, but they fail to account for gene–gene dependency information, and may be sensitive to outlying feature data.
Results
We improve the inverse probability-of-censoring weighted (IPCW) Kendall’s tau statistic by using Google’s PageRank Markov matrix to incorporate feature dependency network information. Also, to tackle outlying feature data, the nonparanormal approach transforming the feature data to multivariate normal variates are utilized in the graphical lasso procedure to estimate the network structure in feature data. Simulation studies under various scenarios show that the proposed network-adjusted weighted Kendall’s tau approach leads to more accurate feature selection and survival prediction than the methods without accounting for feature dependency network information and outlying feature data. The applications on the clinical survival outcome data of diffuse large B-cell lymphoma and of The Cancer Genome Atlas lung adenocarcinoma patients demonstrate clearly the advantages of the new proposal over the alternative methods.
Supplementary information
Supplementary data are available at Bioinformatics online.
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