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Published in: Irish Journal of Medical Science (1971 -) 4/2011

01-12-2011 | Original Article

Androgen receptor coregulators NOCR1, TIF2, and ARA70 may account for the hydroxyflutamide insensitivity of prostate cancer cells

Authors: Y. Wang, J.-Q. Li, C. Shao, C.-H. Shi, F. Liu, Z.-Y. Yang, J.-X. Qiu, Y.-M. Li, Q. Fu, W. Zhang, W. Xue, Y.-H. Lei, J.-Y. Gao, J.-Y. Wang, X.-P. Gao, J.-L. Yuan, T.-Y. Bao, Y.-T. Zhang

Published in: Irish Journal of Medical Science (1971 -) | Issue 4/2011

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Abstract

Introduction

Prostate cancer cells can switch from an androgen-dependent state to an androgen-independent state after a continuous androgen ablation therapy. However, the molecular mechanisms underlying this switch are still unclear. Therefore, we explored the change in androgen receptor (AR)-related gene expression during this transition in a novel cell model.

Material and methods

Prostate cancer cells were continuously treated with competitive androgen receptor inhibitor hydroxyflutamide for 1.5 years, which yielded an flutamide-insensitive LNCaP subline, LNCaP-flu, as confirmed by MTT assays, flow cytometry, and electron microscopy. We analyzed the differences in gene expression in LNCaP-flu cells and LNCaP cells using gene chips and follow-up RT-PCR.

Results

Over 2,428 genes were differentially expressed between these cell lines: 1,194 were down-regulated and 1,234 were up-regulated. Three genes in particular were considered related to the androgen-dependent transition: NCOR1, TIF2 (NCOA2), and ARA70 (NCOA4). There were no apparent changes in expression of the androgen receptor or prostate-specific antigen.

Conclusion

ARs and associated coregulators play a central role in the flutamide-insensitive transition of prostate cancer cells. Although AR expression does not change during this transition, the change in AR coregulators may be a critical factor in the development of antiandrogen insensitivity
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Metadata
Title
Androgen receptor coregulators NOCR1, TIF2, and ARA70 may account for the hydroxyflutamide insensitivity of prostate cancer cells
Authors
Y. Wang
J.-Q. Li
C. Shao
C.-H. Shi
F. Liu
Z.-Y. Yang
J.-X. Qiu
Y.-M. Li
Q. Fu
W. Zhang
W. Xue
Y.-H. Lei
J.-Y. Gao
J.-Y. Wang
X.-P. Gao
J.-L. Yuan
T.-Y. Bao
Y.-T. Zhang
Publication date
01-12-2011
Publisher
Springer-Verlag
Published in
Irish Journal of Medical Science (1971 -) / Issue 4/2011
Print ISSN: 0021-1265
Electronic ISSN: 1863-4362
DOI
https://doi.org/10.1007/s11845-011-0714-4

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