PI3Kα inhibitors that inhibit metastasis.

Oleg Schmidt-Kittler; Jiuxiang Zhu; Jian Yang; Guosheng Liu; William Hendricks; Christoph Lengauer; Sandra B. Gabelli; Kenneth W. Kinzler; Bert Vogelstein; David L. Huso; Shibin Zhou

doi:10.18632/oncotarget.166

PI3Kα inhibitors that inhibit metastasis.

Oleg Schmidt-Kittler, Jiuxiang Zhu, Jian Yang, Guosheng Liu, William Hendricks, Christoph Lengauer, Sandra B. Gabelli, Kenneth W. Kinzler, Bert Vogelstein, David L. Huso, Shibin Zhou

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

39 Scopus citations

Abstract

Previous genetic analyses have suggested that mutations of the genes encoding PI3Kα facilitate invasion and metastasis but have less effect on primary tumor growth. These findings have major implications for therapeutics but have not been factored into pre-clinical drug development designs. Here we show that the inhibition of PI3Kα by newly designed small molecule inhibitors prevented metastasis formation in mice but had much less effect on the growth of subcutaneous xenografts or primary intra-abdominal tumors. These data support the idea that PI3Kα plays an important role in the metastatic process and suggest a more informed strategy for selecting drugs worthy of further development for clinical application.

Original language	English (US)
Pages (from-to)	339-348
Number of pages	10
Journal	Oncotarget
Volume	1
Issue number	5
DOIs	https://doi.org/10.18632/oncotarget.166
State	Published - 2010
Externally published	Yes

ASJC Scopus subject areas

Oncology

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10.18632/oncotarget.166

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title = "PI3Kα inhibitors that inhibit metastasis.",

abstract = "Previous genetic analyses have suggested that mutations of the genes encoding PI3Kα facilitate invasion and metastasis but have less effect on primary tumor growth. These findings have major implications for therapeutics but have not been factored into pre-clinical drug development designs. Here we show that the inhibition of PI3Kα by newly designed small molecule inhibitors prevented metastasis formation in mice but had much less effect on the growth of subcutaneous xenografts or primary intra-abdominal tumors. These data support the idea that PI3Kα plays an important role in the metastatic process and suggest a more informed strategy for selecting drugs worthy of further development for clinical application.",

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AU - Schmidt-Kittler, Oleg

AU - Zhu, Jiuxiang

AU - Yang, Jian

AU - Liu, Guosheng

AU - Hendricks, William

AU - Lengauer, Christoph

AU - Gabelli, Sandra B.

AU - Kinzler, Kenneth W.

AU - Vogelstein, Bert

AU - Huso, David L.

AU - Zhou, Shibin

PY - 2010

Y1 - 2010

N2 - Previous genetic analyses have suggested that mutations of the genes encoding PI3Kα facilitate invasion and metastasis but have less effect on primary tumor growth. These findings have major implications for therapeutics but have not been factored into pre-clinical drug development designs. Here we show that the inhibition of PI3Kα by newly designed small molecule inhibitors prevented metastasis formation in mice but had much less effect on the growth of subcutaneous xenografts or primary intra-abdominal tumors. These data support the idea that PI3Kα plays an important role in the metastatic process and suggest a more informed strategy for selecting drugs worthy of further development for clinical application.

AB - Previous genetic analyses have suggested that mutations of the genes encoding PI3Kα facilitate invasion and metastasis but have less effect on primary tumor growth. These findings have major implications for therapeutics but have not been factored into pre-clinical drug development designs. Here we show that the inhibition of PI3Kα by newly designed small molecule inhibitors prevented metastasis formation in mice but had much less effect on the growth of subcutaneous xenografts or primary intra-abdominal tumors. These data support the idea that PI3Kα plays an important role in the metastatic process and suggest a more informed strategy for selecting drugs worthy of further development for clinical application.

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PI3Kα inhibitors that inhibit metastasis.

Abstract

ASJC Scopus subject areas

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