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Protective effect of γ‐tocopherol‐enriched diet on N ‐methyl‐ N ‐nitrosourea‐induced epithelial dysplasia in rat ventral prostate
Author(s) -
Sanches Lucas D.,
Santos Sergio A. A.,
Carvalho Jaqueline R.,
Jeronimo Gabriela D. M.,
Favaro Wagner J.,
Reis Maria D. G.,
Felisbino Sérgio L.,
Justulin Luis A.
Publication year - 2013
Publication title -
international journal of experimental pathology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.671
H-Index - 72
eISSN - 1365-2613
pISSN - 0959-9673
DOI - 10.1111/iep.12042
Subject(s) - testosterone propionate , endocrinology , medicine , prostate cancer , apoptosis , prostate , dysplasia , hyperplasia , nitrosourea , biology , androgen , cancer , biochemistry , hormone , chemotherapy
Summary Despite recent advances in understanding the biological basis of prostate cancer ( PC a), the management of this disease remains a challenge. Chemoprotective agents have been used to protect against or eradicate prostate malignancies. Here, we investigated the protective effect of γ‐tocopherol on N ‐methyl‐ N ‐nitrosourea ( MNU )‐induced epithelial dysplasia in the rat ventral prostate ( VP ). Thirty‐two male Wistar rats were divided into four groups ( n  = 8): control ( CT ): healthy control animals fed a standard diet; control+γ‐tocopherol ( CT +γT): healthy control animals without intervention fed a γ‐tocopherol‐enriched diet (20 mg/kg); N ‐methyl‐ N ‐nitrosourea ( MNU ): rats that received a single dose of MNU (30 mg/kg) plus testosterone propionate (100 mg/kg) and were fed a standard diet; and MNU +γ‐tocopherol ( MNU +γT): rats that received the same treatment of MNU plus testosterone and were fed with a γ‐tocopherol‐enriched diet (20 mg/kg). After 4 months, the VP s were excised to evaluate morphology, cell proliferation and apoptosis, as well as cyclooxygenase‐2 (Cox‐2), glutathione‐S‐transferase‐pi ( GST ‐pi) and androgen receptor ( AR ) protein expression, and matrix metalloproteinase‐9 ( MMP ‐9) activity. An increase in the incidence of epithelial dysplasias, such as stratified epithelial hyperplasia and squamous metaplasia, in the MNU group was accompanied by augmented cell proliferation, GST ‐pi and Cox‐2 immunoexpression and pro‐ MMP ‐9 activity. Stromal thickening and inflammatory foci were also observed. The administration of a γ‐tocopherol‐enriched diet significantly attenuated the adverse effects of MNU in the VP . The incidence of epithelial dysplasia decreased, along with the cell proliferation index, GST ‐pi and Cox‐2 immunoexpression. The gelatinolytic activity of pro‐ MMP ‐9 returned to the levels observed for the CT group. These results suggest that γ‐tocopherol acts as a protective agent against MNU ‐induced prostatic disorders in the rat ventral prostate.

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