Abstract
Fibroblasts express androgen receptor (AR) in the normal prostate and during prostate cancer development. We have reported that loss of AR expression in prostate cancer-associated fibroblasts is a poor prognostic indicator. Here we report outcomes of direct and indirect co-cultures of immortalised AR-positive (PShTert-AR) or AR-negative (PShTert) myofibroblasts with prostate cancer cells.In the initial co-cultures the AR-negative PC3 cell line was used so AR expression and signalling were restricted to the myofibroblasts. In both direct and indirect co-culture with PShTert-AR myofibroblasts, paracrine signalling to the PC3 cells slowed proliferation and induced apoptosis. In contrast, PC3 cells proliferated with PShTert myofibroblasts irrespective of the co-culture method. In direct co-culture PC3 cells induced apoptosis in and destroyed PShTerts by direct signalling. Similar results were seen in direct co-cultures with AR-negative DU145 and AR-positive LNCaP and C4-2B prostate cancer cell lines. The AR ligand 5α-dihydrotestosterone (DHT) inhibited the proliferation of the PShTert-AR myofibroblasts, thereby reducing the extent of their inhibitory effect on cancer cell growth.These results suggest loss of stromal AR would favour prostate cancer cell growth in vivo, providing an explanation for the clinical observation that reduced stromal AR is associated with a poorer outcome.
Highlights
Androgens are essential for the normal development of the prostate, and, in the adult, are required for prostate epithelial cell survival and function
The expression of androgen receptor (AR) in stromal fibroblasts is required for the development and maintenance of the normal prostate, and for the development of prostate cancer, yet interestingly stromal AR expression is frequently reduced in prostate cancer where it is associated with poor clinical outcomes [5]
We have studied the effect of AR expression in prostate myofibroblasts on the outcomes of direct and indirect co-culture with prostate cancer cells
Summary
Androgens are essential for the normal development of the prostate, and, in the adult, are required for prostate epithelial cell survival and function. In the early phases of prostate development the androgen receptor (AR) is expressed exclusively in mesenchymal cells, which in turn regulate epithelial cell growth and differentiation, and thereby prostate size [1]. AR is expressed in both stromal and epithelial compartments [2, 3]. Androgens and AR play a pivotal role in the development and progression of prostate cancer. The majority of studies investigating the role of AR in prostate cancer have focused on its function in the malignant epithelial cells, it is becoming increasingly www.oncotarget.com apparent that androgen signalling in the stroma can influence cancer development and progression
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