Cancer biomarker discovery is improved by accounting for variability in general levels of drug sensitivity in pre-clinical models

被引:0
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作者
Paul Geeleher
Nancy J. Cox
R. Stephanie Huang
机构
[1] The University of Chicago,Section of Hematology/Oncology
[2] University of Chicago,Section of Genetic Medicine, Department of Medicine
[3] Vanderbilt University,Division of Genetic Medicine
来源
Genome Biology | / 17卷
关键词
False Discovery Rate; Chronic Myeloid Leukemia; Drug Sensitivity; PARP Inhibitor; Bosutinib;
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摘要
We show that variability in general levels of drug sensitivity in pre-clinical cancer models confounds biomarker discovery. However, using a very large panel of cell lines, each treated with many drugs, we could estimate a general level of sensitivity to all drugs in each cell line. By conditioning on this variable, biomarkers were identified that were more likely to be effective in clinical trials than those identified using a conventional uncorrected approach. We find that differences in general levels of drug sensitivity are driven by biologically relevant processes. We developed a gene expression based method that can be used to correct for this confounder in future studies.
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