Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor

Although the protective role of androgen receptor (AR) in breast cancer (BC) is well established, the mechanisms involved remains largely unexplored. MicroRNAs play fundamental roles in many biological processes, including tumor cell development and metastasis. Herein, we report that androgens reduc...

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Autores principales: Casaburi, Ivan, Cesario, Maria Grazia, Donà, Ada, Rizza, Pietro, Aquila, Saveria, Avena, Paola, Lanzino, Marilena, Pellegrino, Michele, Vivacqua, Adele, Tucci, Paola, Morelli, Catia, Andò, Sebastiano, Sisci, Diego
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4914311/
https://www.ncbi.nlm.nih.gov/pubmed/26862856
http://dx.doi.org/10.18632/oncotarget.7207
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author Casaburi, Ivan
Cesario, Maria Grazia
Donà, Ada
Rizza, Pietro
Aquila, Saveria
Avena, Paola
Lanzino, Marilena
Pellegrino, Michele
Vivacqua, Adele
Tucci, Paola
Morelli, Catia
Andò, Sebastiano
Sisci, Diego
author_facet Casaburi, Ivan
Cesario, Maria Grazia
Donà, Ada
Rizza, Pietro
Aquila, Saveria
Avena, Paola
Lanzino, Marilena
Pellegrino, Michele
Vivacqua, Adele
Tucci, Paola
Morelli, Catia
Andò, Sebastiano
Sisci, Diego
author_sort Casaburi, Ivan
collection PubMed
description Although the protective role of androgen receptor (AR) in breast cancer (BC) is well established, the mechanisms involved remains largely unexplored. MicroRNAs play fundamental roles in many biological processes, including tumor cell development and metastasis. Herein, we report that androgens reduce BC cells proliferation acting as a negative modulator of the onco-miRNA-21. The synthetic androgen miboleron (Mib) decreases BC cell proliferation induced by miR-21 over-expression and AR knockdown evidenced the requirement of AR in the down-regulation of miR-21 expression. These effects seem to be a general mechanism occurring in BC tissues. Chromatin immune-precipitation (ChIP) analysis disclosed the binding of AR to a specific ARE sequence in miR-21 proximal promoter and recognizes the recruitment of HDAC3 as component for AR-mediated transcriptional repression. Such event is associated to a significantly reduced PolII binding in Mib treated extracts confirming that activated AR is a transcriptional repressor of miR-21 expression, providing further insight into the protective role of androgens in breast cancer cells. Collectively, our data and the widespread AR expression in primary and metastatic breast tumours, suggest a careful examination of the therapeutic potential of androgens also in potentiating the effectiveness of anti-oestrogen adjuvant therapies.
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spelling pubmed-49143112016-07-11 Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor Casaburi, Ivan Cesario, Maria Grazia Donà, Ada Rizza, Pietro Aquila, Saveria Avena, Paola Lanzino, Marilena Pellegrino, Michele Vivacqua, Adele Tucci, Paola Morelli, Catia Andò, Sebastiano Sisci, Diego Oncotarget Research Paper Although the protective role of androgen receptor (AR) in breast cancer (BC) is well established, the mechanisms involved remains largely unexplored. MicroRNAs play fundamental roles in many biological processes, including tumor cell development and metastasis. Herein, we report that androgens reduce BC cells proliferation acting as a negative modulator of the onco-miRNA-21. The synthetic androgen miboleron (Mib) decreases BC cell proliferation induced by miR-21 over-expression and AR knockdown evidenced the requirement of AR in the down-regulation of miR-21 expression. These effects seem to be a general mechanism occurring in BC tissues. Chromatin immune-precipitation (ChIP) analysis disclosed the binding of AR to a specific ARE sequence in miR-21 proximal promoter and recognizes the recruitment of HDAC3 as component for AR-mediated transcriptional repression. Such event is associated to a significantly reduced PolII binding in Mib treated extracts confirming that activated AR is a transcriptional repressor of miR-21 expression, providing further insight into the protective role of androgens in breast cancer cells. Collectively, our data and the widespread AR expression in primary and metastatic breast tumours, suggest a careful examination of the therapeutic potential of androgens also in potentiating the effectiveness of anti-oestrogen adjuvant therapies. Impact Journals LLC 2016-02-05 /pmc/articles/PMC4914311/ /pubmed/26862856 http://dx.doi.org/10.18632/oncotarget.7207 Text en Copyright: © 2016 Casaburi et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Casaburi, Ivan
Cesario, Maria Grazia
Donà, Ada
Rizza, Pietro
Aquila, Saveria
Avena, Paola
Lanzino, Marilena
Pellegrino, Michele
Vivacqua, Adele
Tucci, Paola
Morelli, Catia
Andò, Sebastiano
Sisci, Diego
Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title_full Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title_fullStr Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title_full_unstemmed Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title_short Androgens downregulate miR-21 expression in breast cancer cells underlining the protective role of androgen receptor
title_sort androgens downregulate mir-21 expression in breast cancer cells underlining the protective role of androgen receptor
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4914311/
https://www.ncbi.nlm.nih.gov/pubmed/26862856
http://dx.doi.org/10.18632/oncotarget.7207
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