Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth

Thuy L. Phung; Wa Du; Qi Xue; Sriram Ayyaswamy; Damien Gerald; Zeus Antonello; Sokha Nhek; Carole A. Perruzzi; Isabel Acevedo; Rajesh Ramanna-Valmiki; Paul Rodriguez-Waitkus; Ladan Enayati; Marcelo L. Hochman; Dina Lev; Sandaruwan Geeganage; Laura E. Benjamin

doi:10.1158/0008-5472.CAN-13-2961

Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth

Thuy L. Phung, Wa Du, Qi Xue, Sriram Ayyaswamy, Damien Gerald, Zeus Antonello, Sokha Nhek, Carole A. Perruzzi, Isabel Acevedo, Rajesh Ramanna-Valmiki, Paul Rodriguez-Waitkus, Ladan Enayati, Marcelo L. Hochman, Dina Lev, Sandaruwan Geeganage, Laura E. Benjamin

Cancer Biology

Research output: Contribution to journal › Article › peer-review

41 Scopus citations

Abstract

Vascular tumors are endothelial cell neoplasms whose mechanisms of tumorigenesis are poorly understood. Moreover, current therapies, particularly those for malignant lesions, have little beneficial effect on clinical outcomes. In this study, we show that endothelial activation of the Akt1 kinase is suffi cient to drive de novo tumor formation. Mechanistic investigations uncovered opposing functions for different Akt isoforms in this regulation, where Akt1 promotes and Akt3 inhibits vascular tumor growth. Akt3 exerted negative effects on tumor endothelial cell growth and migration by inhibiting activation of the translation regulatory kinase S6-Kinase (S6K) through modulation of Rictor expression. S6K in turn acted through a negative feedback loop to restrain Akt3 expression. Conversely, S6K signaling was increased in vascular tumor cells where Akt3 was silenced, and the growth of these tumor cells was inhibited by a novel S6K inhibitor. Overall, our findings offer a preclinical proof of concept for the therapeutic utility of treating vascular tumors, such as angiosarcomas, with S6K inhibitors.

Original language	English (US)
Pages (from-to)	40-50
Number of pages	11
Journal	Cancer Research
Volume	75
Issue number	1
DOIs	https://doi.org/10.1158/0008-5472.CAN-13-2961
State	Published - Jan 1 2015

ASJC Scopus subject areas

Oncology
Cancer Research

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Phung, T. L., Du, W., Xue, Q., Ayyaswamy, S., Gerald, D., Antonello, Z., Nhek, S., Perruzzi, C. A., Acevedo, I., Ramanna-Valmiki, R., Rodriguez-Waitkus, P., Enayati, L., Hochman, M. L., Lev, D., Geeganage, S., & Benjamin, L. E. (2015). Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth. Cancer Research, 75(1), 40-50. https://doi.org/10.1158/0008-5472.CAN-13-2961

Phung, TL, Du, W, Xue, Q, Ayyaswamy, S, Gerald, D, Antonello, Z, Nhek, S, Perruzzi, CA, Acevedo, I, Ramanna-Valmiki, R, Rodriguez-Waitkus, P, Enayati, L, Hochman, ML, Lev, D, Geeganage, S & Benjamin, LE 2015, 'Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth', Cancer Research, vol. 75, no. 1, pp. 40-50. https://doi.org/10.1158/0008-5472.CAN-13-2961

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title = "Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth",

abstract = "Vascular tumors are endothelial cell neoplasms whose mechanisms of tumorigenesis are poorly understood. Moreover, current therapies, particularly those for malignant lesions, have little beneficial effect on clinical outcomes. In this study, we show that endothelial activation of the Akt1 kinase is suffi cient to drive de novo tumor formation. Mechanistic investigations uncovered opposing functions for different Akt isoforms in this regulation, where Akt1 promotes and Akt3 inhibits vascular tumor growth. Akt3 exerted negative effects on tumor endothelial cell growth and migration by inhibiting activation of the translation regulatory kinase S6-Kinase (S6K) through modulation of Rictor expression. S6K in turn acted through a negative feedback loop to restrain Akt3 expression. Conversely, S6K signaling was increased in vascular tumor cells where Akt3 was silenced, and the growth of these tumor cells was inhibited by a novel S6K inhibitor. Overall, our findings offer a preclinical proof of concept for the therapeutic utility of treating vascular tumors, such as angiosarcomas, with S6K inhibitors.",

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AU - Phung, Thuy L.

AU - Du, Wa

AU - Xue, Qi

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AU - Antonello, Zeus

AU - Nhek, Sokha

AU - Perruzzi, Carole A.

AU - Acevedo, Isabel

AU - Ramanna-Valmiki, Rajesh

AU - Rodriguez-Waitkus, Paul

AU - Enayati, Ladan

AU - Hochman, Marcelo L.

AU - Lev, Dina

AU - Geeganage, Sandaruwan

AU - Benjamin, Laura E.

PY - 2015/1/1

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N2 - Vascular tumors are endothelial cell neoplasms whose mechanisms of tumorigenesis are poorly understood. Moreover, current therapies, particularly those for malignant lesions, have little beneficial effect on clinical outcomes. In this study, we show that endothelial activation of the Akt1 kinase is suffi cient to drive de novo tumor formation. Mechanistic investigations uncovered opposing functions for different Akt isoforms in this regulation, where Akt1 promotes and Akt3 inhibits vascular tumor growth. Akt3 exerted negative effects on tumor endothelial cell growth and migration by inhibiting activation of the translation regulatory kinase S6-Kinase (S6K) through modulation of Rictor expression. S6K in turn acted through a negative feedback loop to restrain Akt3 expression. Conversely, S6K signaling was increased in vascular tumor cells where Akt3 was silenced, and the growth of these tumor cells was inhibited by a novel S6K inhibitor. Overall, our findings offer a preclinical proof of concept for the therapeutic utility of treating vascular tumors, such as angiosarcomas, with S6K inhibitors.

AB - Vascular tumors are endothelial cell neoplasms whose mechanisms of tumorigenesis are poorly understood. Moreover, current therapies, particularly those for malignant lesions, have little beneficial effect on clinical outcomes. In this study, we show that endothelial activation of the Akt1 kinase is suffi cient to drive de novo tumor formation. Mechanistic investigations uncovered opposing functions for different Akt isoforms in this regulation, where Akt1 promotes and Akt3 inhibits vascular tumor growth. Akt3 exerted negative effects on tumor endothelial cell growth and migration by inhibiting activation of the translation regulatory kinase S6-Kinase (S6K) through modulation of Rictor expression. S6K in turn acted through a negative feedback loop to restrain Akt3 expression. Conversely, S6K signaling was increased in vascular tumor cells where Akt3 was silenced, and the growth of these tumor cells was inhibited by a novel S6K inhibitor. Overall, our findings offer a preclinical proof of concept for the therapeutic utility of treating vascular tumors, such as angiosarcomas, with S6K inhibitors.

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Akt1 and Akt3 exert opposing roles in the regulation of vascular tumor growth

Abstract

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