The antiandrogenic effect of finasteride against a mutant androgen receptor

Finasteride is known to inhibit Type 2 5α-reductase and thus block the conversion of testosterone to dihydrotestosterone (DHT). The structural similarity of finasteride to DHT raises the possibility that finasteride may also interfere with the function of the androgen receptor (AR). Experiments were...

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Bibliographic Details
Published in:Cancer biology & therapy 2011-05, Vol.11 (10), p.902-909
Main Authors: Wu, Yue, Chhipa, Rishi Raj, Zhang, Haitao, Ip, Clement
Format: Article
Language:English
Subjects:
Androgen Antagonists - pharmacology
Androgen Receptor Antagonists - pharmacology
Anilides - pharmacology
Binding
Biology
Bioscience
Calcium
Cancer
Cell
Cell Line, Tumor
Cell Proliferation - drug effects
Cycle
Dihydrotestosterone - metabolism
Finasteride - pharmacology
Gene Expression Regulation - drug effects
Gene Knockdown Techniques
Homeodomain Proteins - genetics
Humans
Landes
Mutation - genetics
Nitriles - pharmacology
Organogenesis
Proteins
Receptors, Androgen - genetics
Receptors, Androgen - metabolism
Research Paper
Tosyl Compounds - pharmacology
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Summary:Finasteride is known to inhibit Type 2 5α-reductase and thus block the conversion of testosterone to dihydrotestosterone (DHT). The structural similarity of finasteride to DHT raises the possibility that finasteride may also interfere with the function of the androgen receptor (AR). Experiments were carried out to evaluate the antiandrogenic effect of finasteride in LNCaP, C4-2 and VCaP human prostate cancer cells. Finasteride decreased DHT binding to AR, and DHT-stimulated AR activity and cell growth in LNCaP and C4-2 cells, but not in VCaP cells. LNCaP and C4-2 (derived from castration-resistant LNCaP) cells express the T877A mutant AR, while VCaP cells express the wild type AR. When PC-3 cells, which are AR-null, were transfected with either the wild type or the T877A mutant AR, only the mutant AR-expressing cells were sensitive to finasteride inhibition of DHT binding. Peroxiredoxin-1 (Prx1) is a novel endogenous facilitator of AR binding to DHT. In Prx1-rich LNCaP cells, the combination of Prx1 knockdown and finasteride was found to produce a greater inhibitory effect on AR activity and cell growth than either treatment alone. The observation suggests that cells with a low expression of Prx1 are likely to be more responsive to the antiandrogenic effect of finasteride. Additional studies showed that the efficacy of finasteride was comparable to that of bicalutamide (a widely used non-steroidal antiandrogen). The implication of the above findings is discussed in the context of developing strategies to improve the outcome of androgen deprivation therapy.
ISSN:1538-4047
1555-8576
DOI:10.4161/cbt.11.10.15187