The role of DAB2IP in androgen receptor activation during prostate cancer progression

K. Wu; J. Liu; S. F. Tseng; C. Gore; Z. Ning; N. Sharifi; L. Fazli; M. Gleave; P. Kapur; G. Xiao; X. Sun; O. K. Oz; W. Min; G. Alexandrakis; C. R. Yang; C. L. Hsieh; H. C. Wu; D. He; D. Xie; J. T. Hsieh

doi:10.1038/onc.2013.143

The role of DAB2IP in androgen receptor activation during prostate cancer progression

K. Wu
, J. Liu
, S. F. Tseng
, C. Gore
, Z. Ning
, N. Sharifi
, L. Fazli
, M. Gleave
, P. Kapur
, G. Xiao
, X. Sun
, O. K. Oz
, W. Min
, G. Alexandrakis
, C. R. Yang
, C. L. Hsieh
, H. C. Wu
, D. He
, D. Xie
, J. T. Hsieh

医学部

University of Texas Southwestern Medical Center
University of Texas at Arlington
Xi'an Jiaotong University
University of British Columbia
Yale University
China Medical University Taichung
Asia University Taiwan
Huazhong University of Science and Technology

科研成果: 期刊稿件 › 文章 › 同行评审

45 引用（Scopus）

摘要

Altered androgen-receptor (AR) expression and/or constitutively active AR are commonly associated with prostate cancer (PCa) progression. Targeting AR remains a focal point for designing new strategy of PCa therapy. Here, we have shown that DAB2IP, a novel tumor suppressor in PCa, can inhibit AR-mediated cell growth and gene activation in PCa cells via distinct mechanisms. DAB2IP inhibits the genomic pathway by preventing AR nuclear translocation or phosphorylation and suppresses the non-genomic pathway via its unique functional domain to inactivate c-Src. Also, DAB2IP is capable of suppressing AR activation in an androgen-independent manner. In addition, DAB2IP can inhibit several AR splice variants showing constitutive activity in PCa cells. In DAB2IP -/- mice, the prostate gland exhibits hyperplastic epithelia, in which AR becomes more active. Consistently, DAB2IP expression inversely correlates with AR activation status particularly in recurrent or metastatic PCa patients. Taken together, DAB2IP is a unique intrinsic AR modulator in normal cells, and likely can be further developed into a therapeutic agent for PCa.

源语言	英语
页（从-至）	1954-1963
页数	10
期刊	Oncogene
卷	33
期	15
DOI	https://doi.org/10.1038/onc.2013.143
出版状态	已出版 - 10 4月 2014

联合国可持续发展目标

此成果有助于实现下列可持续发展目标：

可持续发展目标 3 良好健康与福祉

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10.1038/onc.2013.143

其它文件与链接

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引用此

Wu, K., Liu, J., Tseng, S. F., Gore, C., Ning, Z., Sharifi, N., Fazli, L., Gleave, M., Kapur, P., Xiao, G., Sun, X., Oz, O. K., Min, W., Alexandrakis, G., Yang, C. R., Hsieh, C. L., Wu, H. C., He, D., Xie, D., & Hsieh, J. T. (2014). The role of DAB2IP in androgen receptor activation during prostate cancer progression. Oncogene, 33(15), 1954-1963. https://doi.org/10.1038/onc.2013.143

@article{f2e2d5d428db4075bc147a420da62e65,

title = "The role of DAB2IP in androgen receptor activation during prostate cancer progression",

abstract = "Altered androgen-receptor (AR) expression and/or constitutively active AR are commonly associated with prostate cancer (PCa) progression. Targeting AR remains a focal point for designing new strategy of PCa therapy. Here, we have shown that DAB2IP, a novel tumor suppressor in PCa, can inhibit AR-mediated cell growth and gene activation in PCa cells via distinct mechanisms. DAB2IP inhibits the genomic pathway by preventing AR nuclear translocation or phosphorylation and suppresses the non-genomic pathway via its unique functional domain to inactivate c-Src. Also, DAB2IP is capable of suppressing AR activation in an androgen-independent manner. In addition, DAB2IP can inhibit several AR splice variants showing constitutive activity in PCa cells. In DAB2IP -/- mice, the prostate gland exhibits hyperplastic epithelia, in which AR becomes more active. Consistently, DAB2IP expression inversely correlates with AR activation status particularly in recurrent or metastatic PCa patients. Taken together, DAB2IP is a unique intrinsic AR modulator in normal cells, and likely can be further developed into a therapeutic agent for PCa.",

keywords = "DAB2IP, Src, androgen receptor, genomic pathway, prostate cancer",

author = "K. Wu and J. Liu and Tseng, \{S. F.\} and C. Gore and Z. Ning and N. Sharifi and L. Fazli and M. Gleave and P. Kapur and G. Xiao and X. Sun and Oz, \{O. K.\} and W. Min and G. Alexandrakis and Yang, \{C. R.\} and Hsieh, \{C. L.\} and Wu, \{H. C.\} and D. He and D. Xie and Hsieh, \{J. T.\}",

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Wu, K, Liu, J, Tseng, SF, Gore, C, Ning, Z, Sharifi, N, Fazli, L, Gleave, M, Kapur, P, Xiao, G, Sun, X, Oz, OK, Min, W, Alexandrakis, G, Yang, CR, Hsieh, CL, Wu, HC, He, D, Xie, D & Hsieh, JT 2014, 'The role of DAB2IP in androgen receptor activation during prostate cancer progression', Oncogene, 卷 33, 号码 15, 页码 1954-1963. https://doi.org/10.1038/onc.2013.143

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T1 - The role of DAB2IP in androgen receptor activation during prostate cancer progression

AU - Wu, K.

AU - Liu, J.

AU - Tseng, S. F.

AU - Gore, C.

AU - Ning, Z.

AU - Sharifi, N.

AU - Fazli, L.

AU - Gleave, M.

AU - Kapur, P.

AU - Xiao, G.

AU - Sun, X.

AU - Oz, O. K.

AU - Min, W.

AU - Alexandrakis, G.

AU - Yang, C. R.

AU - Hsieh, C. L.

AU - Wu, H. C.

AU - He, D.

AU - Xie, D.

AU - Hsieh, J. T.

PY - 2014/4/10

Y1 - 2014/4/10

N2 - Altered androgen-receptor (AR) expression and/or constitutively active AR are commonly associated with prostate cancer (PCa) progression. Targeting AR remains a focal point for designing new strategy of PCa therapy. Here, we have shown that DAB2IP, a novel tumor suppressor in PCa, can inhibit AR-mediated cell growth and gene activation in PCa cells via distinct mechanisms. DAB2IP inhibits the genomic pathway by preventing AR nuclear translocation or phosphorylation and suppresses the non-genomic pathway via its unique functional domain to inactivate c-Src. Also, DAB2IP is capable of suppressing AR activation in an androgen-independent manner. In addition, DAB2IP can inhibit several AR splice variants showing constitutive activity in PCa cells. In DAB2IP -/- mice, the prostate gland exhibits hyperplastic epithelia, in which AR becomes more active. Consistently, DAB2IP expression inversely correlates with AR activation status particularly in recurrent or metastatic PCa patients. Taken together, DAB2IP is a unique intrinsic AR modulator in normal cells, and likely can be further developed into a therapeutic agent for PCa.

AB - Altered androgen-receptor (AR) expression and/or constitutively active AR are commonly associated with prostate cancer (PCa) progression. Targeting AR remains a focal point for designing new strategy of PCa therapy. Here, we have shown that DAB2IP, a novel tumor suppressor in PCa, can inhibit AR-mediated cell growth and gene activation in PCa cells via distinct mechanisms. DAB2IP inhibits the genomic pathway by preventing AR nuclear translocation or phosphorylation and suppresses the non-genomic pathway via its unique functional domain to inactivate c-Src. Also, DAB2IP is capable of suppressing AR activation in an androgen-independent manner. In addition, DAB2IP can inhibit several AR splice variants showing constitutive activity in PCa cells. In DAB2IP -/- mice, the prostate gland exhibits hyperplastic epithelia, in which AR becomes more active. Consistently, DAB2IP expression inversely correlates with AR activation status particularly in recurrent or metastatic PCa patients. Taken together, DAB2IP is a unique intrinsic AR modulator in normal cells, and likely can be further developed into a therapeutic agent for PCa.

KW - DAB2IP

KW - Src

KW - androgen receptor

KW - genomic pathway

KW - prostate cancer

UR - https://www.scopus.com/pages/publications/84899446436

U2 - 10.1038/onc.2013.143

DO - 10.1038/onc.2013.143

M3 - 文章

C2 - 23604126

AN - SCOPUS:84899446436

SN - 0950-9232

VL - 33

SP - 1954

EP - 1963

JO - Oncogene

JF - Oncogene

IS - 15

ER -

The role of DAB2IP in androgen receptor activation during prostate cancer progression

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