Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer

Yi Hsin Hsu; Jun Yao; Li Chuan Chan; Ting Jung Wu; Jennifer L. Hsu; Yueh Fu Fang; Yongkun Wei; Yun Wu; Wen Chien Huang; Chien Liang Liu; Yuan Ching Chang; Ming Yang Wang; Chia Wei Li; Jia Shen; Mei Kuang Chen; Aysegul A. Sahin; Anil Sood; Gordon B. Mills; Dihua Yu; Gabriel N. Hortobagyi; Mien Chie Hung

doi:10.1158/0008-5472.CAN-14-0584

Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer

Yi Hsin Hsu, Jun Yao, Li Chuan Chan, Ting Jung Wu, Jennifer L. Hsu, Yueh Fu Fang, Yongkun Wei, Yun Wu, Wen Chien Huang, Chien Liang Liu, Yuan Ching Chang, Ming Yang Wang, Chia Wei Li, Jia Shen, Mei Kuang Chen, Aysegul A. Sahin, Anil Sood, Gordon B. Mills, Dihua Yu, Gabriel N. HortobagyiMien Chie Hung

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Abstract

Triple-negative breast cancer (TNBC) is a highly heterogeneous and recurrent subtype of breast cancer that lacks an effective targeted therapy. To identify candidate therapeutic targets, we profiled global gene expression in TNBC and breast tumor-initiating cells with a patient survival dataset. Eight TNBC-related kinases were found to be overexpressed in TNBC cells with stem-like properties. Among them, expression of PKC-α, MET, and CDK6 correlated with poorer survival outcomes. In cases coexpressing two of these three kinases, survival rates were lower than in cases where only one of these kinases was expressed. In functional tests, two-drug combinations targeting these three kinases inhibited TNBC cell proliferation and tumorigenic potential in a cooperative manner. A combination of PKC-α-MET inhibitors also attenuated tumor growth in a cooperative manner in vivo. Our findings define three kinases critical for TNBC growth and offer a preclinical rationale for their candidacy as effective therapeutic targets in treating TNBC.

Original language	English (US)
Pages (from-to)	4822-4835
Number of pages	14
Journal	Cancer Research
Volume	74
Issue number	17
DOIs	https://doi.org/10.1158/0008-5472.CAN-14-0584
State	Published - Sep 1 2014

ASJC Scopus subject areas

Oncology
Cancer Research

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Hsu, Y. H., Yao, J., Chan, L. C., Wu, T. J., Hsu, J. L., Fang, Y. F., Wei, Y., Wu, Y., Huang, W. C., Liu, C. L., Chang, Y. C., Wang, M. Y., Li, C. W., Shen, J., Chen, M. K., Sahin, A. A., Sood, A., Mills, G. B., Yu, D., ... Hung, M. C. (2014). Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer. Cancer Research, 74(17), 4822-4835. https://doi.org/10.1158/0008-5472.CAN-14-0584

Hsu, YH, Yao, J, Chan, LC, Wu, TJ, Hsu, JL, Fang, YF, Wei, Y , Wu, Y, Huang, WC, Liu, CL, Chang, YC, Wang, MY, Li, CW, Shen, J, Chen, MK, Sahin, AA , Sood, A, Mills, GB, Yu, D, Hortobagyi, GN & Hung, MC 2014, 'Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer', Cancer Research, vol. 74, no. 17, pp. 4822-4835. https://doi.org/10.1158/0008-5472.CAN-14-0584

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title = "Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer",

abstract = "Triple-negative breast cancer (TNBC) is a highly heterogeneous and recurrent subtype of breast cancer that lacks an effective targeted therapy. To identify candidate therapeutic targets, we profiled global gene expression in TNBC and breast tumor-initiating cells with a patient survival dataset. Eight TNBC-related kinases were found to be overexpressed in TNBC cells with stem-like properties. Among them, expression of PKC-α, MET, and CDK6 correlated with poorer survival outcomes. In cases coexpressing two of these three kinases, survival rates were lower than in cases where only one of these kinases was expressed. In functional tests, two-drug combinations targeting these three kinases inhibited TNBC cell proliferation and tumorigenic potential in a cooperative manner. A combination of PKC-α-MET inhibitors also attenuated tumor growth in a cooperative manner in vivo. Our findings define three kinases critical for TNBC growth and offer a preclinical rationale for their candidacy as effective therapeutic targets in treating TNBC.",

author = "Hsu, {Yi Hsin} and Jun Yao and Chan, {Li Chuan} and Wu, {Ting Jung} and Hsu, {Jennifer L.} and Fang, {Yueh Fu} and Yongkun Wei and Yun Wu and Huang, {Wen Chien} and Liu, {Chien Liang} and Chang, {Yuan Ching} and Wang, {Ming Yang} and Li, {Chia Wei} and Jia Shen and Chen, {Mei Kuang} and Sahin, {Aysegul A.} and Anil Sood and Mills, {Gordon B.} and Dihua Yu and Hortobagyi, {Gabriel N.} and Hung, {Mien Chie}",

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doi = "10.1158/0008-5472.CAN-14-0584",

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AU - Wu, Ting Jung

AU - Hsu, Jennifer L.

AU - Fang, Yueh Fu

AU - Wei, Yongkun

AU - Wu, Yun

AU - Huang, Wen Chien

AU - Liu, Chien Liang

AU - Chang, Yuan Ching

AU - Wang, Ming Yang

AU - Li, Chia Wei

AU - Shen, Jia

AU - Chen, Mei Kuang

AU - Sahin, Aysegul A.

AU - Sood, Anil

AU - Mills, Gordon B.

AU - Yu, Dihua

AU - Hortobagyi, Gabriel N.

AU - Hung, Mien Chie

PY - 2014/9/1

Y1 - 2014/9/1

N2 - Triple-negative breast cancer (TNBC) is a highly heterogeneous and recurrent subtype of breast cancer that lacks an effective targeted therapy. To identify candidate therapeutic targets, we profiled global gene expression in TNBC and breast tumor-initiating cells with a patient survival dataset. Eight TNBC-related kinases were found to be overexpressed in TNBC cells with stem-like properties. Among them, expression of PKC-α, MET, and CDK6 correlated with poorer survival outcomes. In cases coexpressing two of these three kinases, survival rates were lower than in cases where only one of these kinases was expressed. In functional tests, two-drug combinations targeting these three kinases inhibited TNBC cell proliferation and tumorigenic potential in a cooperative manner. A combination of PKC-α-MET inhibitors also attenuated tumor growth in a cooperative manner in vivo. Our findings define three kinases critical for TNBC growth and offer a preclinical rationale for their candidacy as effective therapeutic targets in treating TNBC.

AB - Triple-negative breast cancer (TNBC) is a highly heterogeneous and recurrent subtype of breast cancer that lacks an effective targeted therapy. To identify candidate therapeutic targets, we profiled global gene expression in TNBC and breast tumor-initiating cells with a patient survival dataset. Eight TNBC-related kinases were found to be overexpressed in TNBC cells with stem-like properties. Among them, expression of PKC-α, MET, and CDK6 correlated with poorer survival outcomes. In cases coexpressing two of these three kinases, survival rates were lower than in cases where only one of these kinases was expressed. In functional tests, two-drug combinations targeting these three kinases inhibited TNBC cell proliferation and tumorigenic potential in a cooperative manner. A combination of PKC-α-MET inhibitors also attenuated tumor growth in a cooperative manner in vivo. Our findings define three kinases critical for TNBC growth and offer a preclinical rationale for their candidacy as effective therapeutic targets in treating TNBC.

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Definition of PKC-α, CDK6, and MET as therapeutic targets in triple-negative breast cancer

Abstract

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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