Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status

MicroRNAs (miRNAs), single-stranded non-coding RNAs, influence myriad biological processes that can contribute to cancer. Although tumor-suppressive and oncogenic functions have been characterized for some miRNAs, the majority of microRNAs have not been investigated for their ability to promote and...

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Autores principales: Di Leva, Gianpiero, Piovan, Claudia, Gasparini, Pierluigi, Ngankeu, Apollinaire, Taccioli, Cristian, Briskin, Daniel, Cheung, Douglas G., Bolon, Brad, Anderlucci, Laura, Alder, Hansjuerg, Nuovo, Gerard, Li, Meng, Iorio, Marilena V., Galasso, Marco, Ramasamy, Santhanam, Marcucci, Guido, Perrotti, Danilo, Powell, Kimerly A., Bratasz, Anna, Garofalo, Michela, Nephew, Kenneth P., Croce, Carlo M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3591271/
https://www.ncbi.nlm.nih.gov/pubmed/23505378
http://dx.doi.org/10.1371/journal.pgen.1003311
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author Di Leva, Gianpiero
Piovan, Claudia
Gasparini, Pierluigi
Ngankeu, Apollinaire
Taccioli, Cristian
Briskin, Daniel
Cheung, Douglas G.
Bolon, Brad
Anderlucci, Laura
Alder, Hansjuerg
Nuovo, Gerard
Li, Meng
Iorio, Marilena V.
Galasso, Marco
Ramasamy, Santhanam
Marcucci, Guido
Perrotti, Danilo
Powell, Kimerly A.
Bratasz, Anna
Garofalo, Michela
Nephew, Kenneth P.
Croce, Carlo M.
author_facet Di Leva, Gianpiero
Piovan, Claudia
Gasparini, Pierluigi
Ngankeu, Apollinaire
Taccioli, Cristian
Briskin, Daniel
Cheung, Douglas G.
Bolon, Brad
Anderlucci, Laura
Alder, Hansjuerg
Nuovo, Gerard
Li, Meng
Iorio, Marilena V.
Galasso, Marco
Ramasamy, Santhanam
Marcucci, Guido
Perrotti, Danilo
Powell, Kimerly A.
Bratasz, Anna
Garofalo, Michela
Nephew, Kenneth P.
Croce, Carlo M.
author_sort Di Leva, Gianpiero
collection PubMed
description MicroRNAs (miRNAs), single-stranded non-coding RNAs, influence myriad biological processes that can contribute to cancer. Although tumor-suppressive and oncogenic functions have been characterized for some miRNAs, the majority of microRNAs have not been investigated for their ability to promote and modulate tumorigenesis. Here, we established that the miR-191/425 cluster is transcriptionally dependent on the host gene, DALRD3, and that the hormone 17β-estradiol (estrogen or E2) controls expression of both miR-191/425 and DALRD3. MiR-191/425 locus characterization revealed that the recruitment of estrogen receptor α (ERα) to the regulatory region of the miR-191/425-DALRD3 unit resulted in the accumulation of miR-191 and miR-425 and subsequent decrease in DALRD3 expression levels. We demonstrated that miR-191 protects ERα positive breast cancer cells from hormone starvation-induced apoptosis through the suppression of tumor-suppressor EGR1. Furthermore, enforced expression of the miR-191/425 cluster in aggressive breast cancer cells altered global gene expression profiles and enabled us to identify important tumor promoting genes, including SATB1, CCND2, and FSCN1, as targets of miR-191 and miR-425. Finally, in vitro and in vivo experiments demonstrated that miR-191 and miR-425 reduced proliferation, impaired tumorigenesis and metastasis, and increased expression of epithelial markers in aggressive breast cancer cells. Our data provide compelling evidence for the transcriptional regulation of the miR-191/425 cluster and for its context-specific biological determinants in breast cancers. Importantly, we demonstrated that the miR-191/425 cluster, by reducing the expression of an extensive network of genes, has a fundamental impact on cancer initiation and progression of breast cancer cells.
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spelling pubmed-35912712013-03-15 Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status Di Leva, Gianpiero Piovan, Claudia Gasparini, Pierluigi Ngankeu, Apollinaire Taccioli, Cristian Briskin, Daniel Cheung, Douglas G. Bolon, Brad Anderlucci, Laura Alder, Hansjuerg Nuovo, Gerard Li, Meng Iorio, Marilena V. Galasso, Marco Ramasamy, Santhanam Marcucci, Guido Perrotti, Danilo Powell, Kimerly A. Bratasz, Anna Garofalo, Michela Nephew, Kenneth P. Croce, Carlo M. PLoS Genet Research Article MicroRNAs (miRNAs), single-stranded non-coding RNAs, influence myriad biological processes that can contribute to cancer. Although tumor-suppressive and oncogenic functions have been characterized for some miRNAs, the majority of microRNAs have not been investigated for their ability to promote and modulate tumorigenesis. Here, we established that the miR-191/425 cluster is transcriptionally dependent on the host gene, DALRD3, and that the hormone 17β-estradiol (estrogen or E2) controls expression of both miR-191/425 and DALRD3. MiR-191/425 locus characterization revealed that the recruitment of estrogen receptor α (ERα) to the regulatory region of the miR-191/425-DALRD3 unit resulted in the accumulation of miR-191 and miR-425 and subsequent decrease in DALRD3 expression levels. We demonstrated that miR-191 protects ERα positive breast cancer cells from hormone starvation-induced apoptosis through the suppression of tumor-suppressor EGR1. Furthermore, enforced expression of the miR-191/425 cluster in aggressive breast cancer cells altered global gene expression profiles and enabled us to identify important tumor promoting genes, including SATB1, CCND2, and FSCN1, as targets of miR-191 and miR-425. Finally, in vitro and in vivo experiments demonstrated that miR-191 and miR-425 reduced proliferation, impaired tumorigenesis and metastasis, and increased expression of epithelial markers in aggressive breast cancer cells. Our data provide compelling evidence for the transcriptional regulation of the miR-191/425 cluster and for its context-specific biological determinants in breast cancers. Importantly, we demonstrated that the miR-191/425 cluster, by reducing the expression of an extensive network of genes, has a fundamental impact on cancer initiation and progression of breast cancer cells. Public Library of Science 2013-03-07 /pmc/articles/PMC3591271/ /pubmed/23505378 http://dx.doi.org/10.1371/journal.pgen.1003311 Text en © 2013 Di Leva et al http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Di Leva, Gianpiero
Piovan, Claudia
Gasparini, Pierluigi
Ngankeu, Apollinaire
Taccioli, Cristian
Briskin, Daniel
Cheung, Douglas G.
Bolon, Brad
Anderlucci, Laura
Alder, Hansjuerg
Nuovo, Gerard
Li, Meng
Iorio, Marilena V.
Galasso, Marco
Ramasamy, Santhanam
Marcucci, Guido
Perrotti, Danilo
Powell, Kimerly A.
Bratasz, Anna
Garofalo, Michela
Nephew, Kenneth P.
Croce, Carlo M.
Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title_full Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title_fullStr Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title_full_unstemmed Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title_short Estrogen Mediated-Activation of miR-191/425 Cluster Modulates Tumorigenicity of Breast Cancer Cells Depending on Estrogen Receptor Status
title_sort estrogen mediated-activation of mir-191/425 cluster modulates tumorigenicity of breast cancer cells depending on estrogen receptor status
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3591271/
https://www.ncbi.nlm.nih.gov/pubmed/23505378
http://dx.doi.org/10.1371/journal.pgen.1003311
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