A gene expression signature of RAS pathway dependence predicts response to PI3K and RAS pathway inhibitors and expands the population of RAS pathway activated tumors

Paweletz Cloud; Nagashima Kumiko; Andersen Jannik; Haines Brian; Chenard Melissa; Zhang Theresa; Roberts Brian; Arthur William; Chastain Michael; Frazier Jason; Klinghoffer Rich; Nebozhyn Michael; Loboda Andrey; Lynch Bethany; Feldman Igor; Dai Hongyue; Huang Pearl; Watters James

doi:10.1186/1755-8794-3-26

BMC Medical Genomics (Jun 2010)

A gene expression signature of RAS pathway dependence predicts response to PI3K and RAS pathway inhibitors and expands the population of RAS pathway activated tumors

Paweletz Cloud,
Nagashima Kumiko,
Andersen Jannik,
Haines Brian,
Chenard Melissa,
Zhang Theresa,
Roberts Brian,
Arthur William,
Chastain Michael,
Frazier Jason,
Klinghoffer Rich,
Nebozhyn Michael,
Loboda Andrey,
Lynch Bethany,
Feldman Igor,
Dai Hongyue,
Huang Pearl,
Watters James

Affiliations

Paweletz Cloud
Nagashima Kumiko
Andersen Jannik
Haines Brian
Chenard Melissa
Zhang Theresa
Roberts Brian
Arthur William
Chastain Michael
Frazier Jason
Klinghoffer Rich
Nebozhyn Michael
Loboda Andrey
Lynch Bethany
Feldman Igor
Dai Hongyue
Huang Pearl
Watters James

DOI: https://doi.org/10.1186/1755-8794-3-26
Journal volume & issue: Vol. 3, no. 1
p. 26

Abstract

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Abstract Background Hyperactivation of the Ras signaling pathway is a driver of many cancers, and RAS pathway activation can predict response to targeted therapies. Therefore, optimal methods for measuring Ras pathway activation are critical. The main focus of our work was to develop a gene expression signature that is predictive of RAS pathway dependence. Methods We used the coherent expression of RAS pathway-related genes across multiple datasets to derive a RAS pathway gene expression signature and generate RAS pathway activation scores in pre-clinical cancer models and human tumors. We then related this signature to KRAS mutation status and drug response data in pre-clinical and clinical datasets. Results The RAS signature score is predictive of KRAS mutation status in lung tumors and cell lines with high (> 90%) sensitivity but relatively low (50%) specificity due to samples that have apparent RAS pathway activation in the absence of a KRAS mutation. In lung and breast cancer cell line panels, the RAS pathway signature score correlates with pMEK and pERK expression, and predicts resistance to AKT inhibition and sensitivity to MEK inhibition within both KRAS mutant and KRAS wild-type groups. The RAS pathway signature is upregulated in breast cancer cell lines that have acquired resistance to AKT inhibition, and is downregulated by inhibition of MEK. In lung cancer cell lines knockdown of KRAS using siRNA demonstrates that the RAS pathway signature is a better measure of dependence on RAS compared to KRAS mutation status. In human tumors, the RAS pathway signature is elevated in ER negative breast tumors and lung adenocarcinomas, and predicts resistance to cetuximab in metastatic colorectal cancer. Conclusions These data demonstrate that the RAS pathway signature is superior to KRAS mutation status for the prediction of dependence on RAS signaling, can predict response to PI3K and RAS pathway inhibitors, and is likely to have the most clinical utility in lung and breast tumors.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

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