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Comparison of Global versus Epidermal Growth Factor Receptor Pathway Profiling for Prediction of Lapatinib Sensitivity in Bladder Cancer

Authors
Havaleshko, Dmytro M.Smith, Steven ChristopherCho, HyungJunCheon, SooyoungOwens, Charles R.Lee, Jae K.Liotta, Lance A.Espina, VirginiaWulfkuhle, Julia D.Petricoin, Emanuel F.Theodorescu, Dan
Issue Date
11월-2009
Publisher
ELSEVIER SCIENCE INC
Citation
NEOPLASIA, v.11, no.11, pp.1185 - U101
Indexed
SCIE
SCOPUS
Journal Title
NEOPLASIA
Volume
11
Number
11
Start Page
1185
End Page
U101
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/119046
DOI
10.1593/neo.09898
ISSN
1522-8002
Abstract
Chemotherapy for metastatic bladder cancer is rarely curative. The recently developed small molecule, lapatinib, a dual epidermal growth factor receptor (EGFR)/human epidermal growth factor receptor-2 receptor tyrosine kinase inhibitor, might improve this situation. Recent findings suggest that identifying which patients are likely to benefit from targeted therapies is beneficial, although controversy remains regarding what types of evaluation might yield optimal candidate biomarkers of sensitivity. Here, we address this issue by developing and comparing lapatinib sensitivity prediction models for human bladder cancer cells. After empirically determining in vitro sensitivities (drug concentration necessary to cause a 50% growth inhibition) of a panel of 39 such lines to lapatinib treatment, we developed prediction models based on profiling the baseline transcriptome, the phosphorylation status of EGFR pathway signaling targets, or a combination of both data sets. We observed that models derived from microarray gene expression data showed better prediction performance (93%-98% accuracy) compared with models derived from EGFR pathway profiling of 23 selected phosphoproteins known to be involved in EGFR-driven signaling (54%-61% accuracy) or from a subset of the microarray data for transcripts in the EGFR pathway (86% accuracy). Combining microarray data and phosphoprotein profiling provided a combination model with 98% accuracy. Our findings suggest that transcriptome-wide profiling for biomarkers of lapatinib sensitivity in cancer cells provides models with excellent predictive performance and may be effectively combined with EGFR pathway phosphoprotein profiling data. These results have significant implications for the use of such tools in personalizing the approach to cancers treated with EGFR-directed targeted therapies.
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CHO, HYUNG JUN
정경대학 (통계학과)
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