Inhibition of prostate carcinogenesis in probasin/SV40 T antigen transgenic rats by raloxifene, an antiestrogen with anti-androgen action, but not nimesulide, a selective cyclooxygenase-2 inhibitor

doi:10.1093/carcin/bgi056

Carcinogenesis Advance Access originally published online on February 24, 2005
Carcinogenesis 2005 26(6):1109-1116; doi:10.1093/carcin/bgi056

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Inhibition of prostate carcinogenesis in probasin/SV40 T antigen transgenic rats by raloxifene, an antiestrogen with anti-androgen action, but not nimesulide, a selective cyclooxygenase-2 inhibitor

Yu Zeng^1,², Masanao Yokohira¹, Kousuke Saoo¹, Hijiri Takeuchi¹, Yan Chen³, Keiko Yamakawa¹, Yoko Matsuda¹, Yoshiyuki Kakehi² and Katsumi Imaida^1,^*

¹ Onco-Pathology, Department of Pathology and Host-Defense, ² Department of Urology, and ³ The Second Department of Internal Medicine, Faculty of Medicine, Kagawa University, 1750-1 Ikenobe, Miki-cho, Kita-gun, Kagawa 761-0793, Japan

^* To whom correspondence should be addressed. Tel: +81 87 891 2111; Fax: +81 87 891 2112; Email: imaida{at}med.kagawa-u.ac.jp

The chemopreventive efficacies of raloxifene and nimesulide,an anti-estrogen but with anti-androgen action and a cyclooxygenase-2(COX-2) selective inhibitor, respectively, were evaluated inprobasin/SV40 T antigen (Tag) transgenic (TG) rats. The treatmentgroups were placebo, nimesulide (400 p.p.m. in basal diet p.o.),raloxifene (slow-release pellets implanted s.c., 5 mg/kg/day),raloxifene (5 mg/kg/day) plus nimesulide (400 p.p.m.), and raloxifene(10 mg/kg/day) plus nimesulide (400 p.p.m.). Animals were killedat 17 weeks of age, and prostate tissues were harvested andweighed by lobes. Tissues were evaluated by histology, immunohistochemistry,and western blot analyses and blood was collected to measurethe testosterone levels. All the animals in the placebo grouphad tumors in each lobe compared with only 43% each in the dorsolateral(DLP) and anterior prostate (AP) of the animals treated withraloxifene (10 mg/kg/day) plus nimesulide. The total prostateweights and adenocarcinoma portions were significantly reducedin the three raloxifene-treated groups, whereas atrophic glandswere increased. There were no significant differences betweenthe nimesulide alone and placebo groups or between the raloxifene(5 mg/kg/day) alone and raloxifene (5 mg/kg/day) plus nimesulidegroup, suggesting a lack of cancer preventive effects of theCOX-2 inhibitor in this animal model. PCNA positive rates inventral prostate (VP) and DLP, and androgen receptor (AR) levelsin VP were significantly reduced in the three raloxifene-treatedgroups. Furthermore, circulating testosterone was decreasedafter raloxifene (10 mg/kg/day) plus nimesulide treatment. Theseresults demonstrate that raloxifene, but not nimesulide, inhibitsprostate carcinogenesis in SV40 Tag TG rats associated witha decline in circulating testosterone levels and a loss of ARexpression, as well as an inhibition of cell proliferation.

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