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1 August 2002, Volume 21, Number 33, Pages 5069-5080
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Original Paper
Regulation of FGF8 expression by the androgen receptor in human prostate cancer
Vincent J Gnanapragasam, Craig N Robson, David E Neal and Hing Y Leung

Prostate Research Group, School of Surgical Sciences, University of Newcastle-upon-Tyne, Framlington Place, Newcastle-upon-Tyne, NE2 4HH, UK

Correspondence to: H Y Leung, E-mail: H.Y.Leung@ncl.ac.uk

Abstract

Fibroblast growth factor 8 (FGF8) has been shown to play a key role in prostate carcinogenesis. It was initially cloned as an androgen induced protein in mouse mammary cancer SC3 cells. In this study, we examined if FGF8 was also regulated by the androgen receptor in human prostate cancer. FGF8b protein expression in resected clinical prostate cancer correlated closely with expression of the androgen receptor (AR). In the androgen sensitive CWR22 prostate xenograft, we observed up-regulation of FGF8b immunoreactivity in testosterone supplemented mice while castration markedly reduced its signal. Furthermore, FGF8b protein expression in AR positive LNCaP cells was similarly enhanced by androgens. The proximal promoter of the human FGF8 gene was cloned into a luciferase reporter construct (FGF8.luc). FGF8.luc activity in AR positive LNCaP and SC3 cells was increased 2.5-fold by androgens. In AR negative DU145 cells, maximal induction of FGF8.luc required both co-transfection of the AR and the presence of androgens. The anti-androgen bicalutamide completely abolished AR mediated FGF8.luc induction. Deletion constructs from FGF8.luc have further defined an active promoter region and an androgen responsive region. Nucleotide analysis of this androgen responsive region has revealed putative androgen response elements. Finally, using ChIP assays we confirmed in vivo interaction between the AR and the androgen responsive region of the FGF8 promoter. Taken together these data provide first evidence that expression of the mitogen FGF8 in prostate cancer is, at least in part, regulated by the androgen receptor at the transcriptional level.

Oncogene (2002) 21, 5069-5080. doi:10.1038/sj.onc.1205663

Keywords

FGF8; prostate cancer; androgen receptor; gene promoter

Abbreviations

AR, androgen receptor; ARE, androgen response element; FGF8, fibroblast growth factor 8; ChIP, chromatin immunoprecipitation; CWR22, Case Western Reserve Prostate Xenograft strain 22; MMTV, mouse mammary tumour virus; PCR, polymerase chain reaction; PSA, prostate specific antigen; SHR, steroid hormone receptor

Received 29 October 2001; revised 17 April 2002; accepted 10 May 2002
1 August 2002, Volume 21, Number 33, Pages 5069-5080
Table of contents    Previous  Abstract  Next   Full text  PDF
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