Signaling through Estrogen Receptors Modulates Telomerase Activity in human prostate cancer
Autor: | Simona Nanni, 1, 2 Michela Narducci, 1 Linda Della Pietra, 3 Fabiola Moretti, 4 Annalisa Grasselli, 4 Piero De Carli, 1 Ada Sacchi, 1 Alfredo Pontecorvi, 2, Antonella Farsetti1, 4 |
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Jazyk: | angličtina |
Rok vydání: | 2002 |
Zdroj: | The Journal of clinical investigation 110 (2002): 219–227. info:cnr-pdr/source/autori:Simona Nanni,1,2 Michela Narducci,1 Linda Della Pietra,1,3 Fabiola Moretti,1,4 Annalisa Grasselli,1,4 Piero De Carli,1 Ada Sacchi,1 Alfredo Pontecorvi,1,2 and Antonella Farsetti1,4/titolo:Signaling through Estrogen Receptors Modulates Telomerase Activity in human prostate cancer./doi:/rivista:The Journal of clinical investigation/anno:2002/pagina_da:219/pagina_a:227/intervallo_pagine:219–227/volume:110 |
Popis: | Sex steroid hormone receptors play a central role in all stages of prostate cancer. Here we tested whether estrogen receptor (ER) signaling contributes to telomerase activation, an early event in prostate tumorigenesis. Following 17b-estradiol (E2) treatment, both mRNA encoding the catalytic subunit of human telomerase (hTERT) and telomerase activity were promptly induced in human prostate normal epithelial cells, fresh explants from benign prostate hyperplasia, and prostate cancer explants and cell lines. Reporter expression studies and in vivo chromatin immunoprecipitation assays revealed E2-dependent hTERT promoter induction and showed that both ERa and ERb bound this sequence. Crucially, addition of the anti-estrogen 4-hydroxytamoxifen caused a differential recruitment in vivo of ERa and ERb onto hTERT promoter and inhibited telomerase activity. Treatment with the aromatase inhibitor letrozole which prevented testosterone-mediated interaction between ER and the hTERT estrogen response element, resulted in a negative regulation of telomerase activity. Thus, intracellular conversion of androgens to estrogens may contribute to the ethiopathogenesis of prostate cancer. Given the present evidence for direct control of hTERT gene expression and telomerase activity in the prostate by ER, we suggest that this transcriptional regulator represents a possible therapeutic target in prostate cancer. |
Databáze: | OpenAIRE |
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