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Identifying kinase dependency in cancer cells by integrating high-throughput drug screening and kinase inhibition data

Authors
Ryall, Karen A.Shin, JiminYoo, MinjaeHinz, Trista K.Kim, JihyeKang, JaewooHeasley, Lynn E.Tan, Aik Choon
Issue Date
1-12월-2015
Publisher
OXFORD UNIV PRESS
Citation
BIOINFORMATICS, v.31, no.23, pp.3799 - 3806
Indexed
SCIE
SCOPUS
Journal Title
BIOINFORMATICS
Volume
31
Number
23
Start Page
3799
End Page
3806
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/91625
DOI
10.1093/bioinformatics/btv427
ISSN
1367-4803
Abstract
Motivation: Targeted kinase inhibitors have dramatically improved cancer treatment, but kinase dependency for an individual patient or cancer cell can be challenging to predict. Kinase dependency does not always correspond with gene expression and mutation status. High-throughput drug screens are powerful tools for determining kinase dependency, but drug polypharmacology can make results difficult to interpret. Results: We developed Kinase Addiction Ranker (KAR), an algorithm that integrates high-throughput drug screening data, comprehensive kinase inhibition data and gene expression profiles to identify kinase dependency in cancer cells. We applied KAR to predict kinase dependency of 21 lung cancer cell lines and 151 leukemia patient samples using published datasets. We experimentally validated KAR predictions of FGFR and MTOR dependence in lung cancer cell line H1581, showing synergistic reduction in proliferation after combining ponatinib and AZD8055.
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Graduate School > Department of Computer Science and Engineering > 1. Journal Articles
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