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From the Departments of * Department of Surgery,
Division of Urology and
Laboratory Medicine
and Pathology, UMDNJ-New Jersey Medical School, Newark, New Jersey, and VA
Medical Center, East Orange, New Jersey.
| Correspondence to: Dr Hosea F. S. Huang, Department of Surgery, Division of Urology, UMD-New Jersey Medical School, 185 South Orange Ave, Newark, NJ 07103 (e-mail: huanghf{at}umdnj.edu). |
, -ß, and -
in human prostate tissues
exhibiting different pathologic conditions. In histologically normal
epithelium, both RAR-
and -
were present throughout the
epithelium with minimal nuclear accumulation. RAR-ß was present only in
basal epithelial nuclei. On the contrary, RAR-
was significantly
increased in the nuclei of luminal epithelial cells, and both RAR-ß and
-
were increased in basal and luminal epithelial nuclei in glands
exhibiting benign prostatic hyperplasia (BPH). RAR-
was also increased
in luminal epithelial nuclei in glands exhibiting prostatic intra-epithelial
neoplasia (PIN). In these glands, RAR-ß was persisting in basal
epithelial nuclei that were also RAR-
positive. In low- and
intermediate-grade cancerous glands, RAR-
was also significantly
increased in luminal epithelial nuclei, and a strong RAR-
signal was
seen in some cells. RAR-ß was absent in these glands. Both RAR-
and -
were also increased in high-grade cancer cells. In conclusion,
current results demonstrated changes in cellular distribution of RAR-
and -
in human prostate tissues exhibiting different pathologies. These
results suggest links between altered RAR signaling and deregulated cell
growth and/or tumorigenic transformation of prostate epithelial cells.
Key words: Prostate carcinoma
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