MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma

MicroRNA-10b (miR-10b) is commonly elevated in glioblastoma (GBM), while not expressed in normal brain tissues. Targeted inhibition of miR-10b has pleiotropic effects on GBM derived cell lines, it reduces GBM growth in animal models, but does not affect normal neurons and astrocytes. This data raise...

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Autores principales: Teplyuk, Nadiya M., Uhlmann, Erik J., Wong, Andus Hon-Kit, Karmali, Priya, Basu, Meenakshi, Gabriely, Galina, Jain, Anant, Wang, Yang, Chiocca, E. Antonio, Stephens, Robert, Marcusson, Eric, Yi, Ming, Krichevsky, Anna M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4414152/
https://www.ncbi.nlm.nih.gov/pubmed/25738367
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author Teplyuk, Nadiya M.
Uhlmann, Erik J.
Wong, Andus Hon-Kit
Karmali, Priya
Basu, Meenakshi
Gabriely, Galina
Jain, Anant
Wang, Yang
Chiocca, E. Antonio
Stephens, Robert
Marcusson, Eric
Yi, Ming
Krichevsky, Anna M.
author_facet Teplyuk, Nadiya M.
Uhlmann, Erik J.
Wong, Andus Hon-Kit
Karmali, Priya
Basu, Meenakshi
Gabriely, Galina
Jain, Anant
Wang, Yang
Chiocca, E. Antonio
Stephens, Robert
Marcusson, Eric
Yi, Ming
Krichevsky, Anna M.
author_sort Teplyuk, Nadiya M.
collection PubMed
description MicroRNA-10b (miR-10b) is commonly elevated in glioblastoma (GBM), while not expressed in normal brain tissues. Targeted inhibition of miR-10b has pleiotropic effects on GBM derived cell lines, it reduces GBM growth in animal models, but does not affect normal neurons and astrocytes. This data raises the possibility of developing miR-10b-targeting GBM therapy. However, the mechanisms contributing to miR-10b-mediated glioma cell survival and proliferation are unexplored. We found that inhibition of miR-10b has distinct effects on specific glioma cell lines. In cells expressing high levels of tumor suppressor p21WAF1/Cip1, it represses E2F1-mediated transcription, leading to down-regulation of multiple E2F1 target genes encoding for S-phase specific proteins, epigenetic modulators, and miRNAs (e.g. miR-15/16), and thereby stalling progression through the S-phase of cell cycle. Subsequently, miR-15/16 activities are reduced and many of their direct targets are de-repressed, including ubiquitin ligase FBXW7 that destabilizes Cyclin E. Conversely, GBM cells expressing low p21 level, or after p21 knock-down, exhibit weaker or no E2F1 response to miR-10b inhibition. Comparative analysis of The Cancer Genome Atlas revealed a strong correlation between miR-10b and multiple E2F target genes in GBM and low-grade glioma. Taken together, these findings indicate that miR-10b regulates E2F1-mediated transcription in GBM, in a p21-dependent fashion.
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spelling pubmed-44141522015-05-08 MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma Teplyuk, Nadiya M. Uhlmann, Erik J. Wong, Andus Hon-Kit Karmali, Priya Basu, Meenakshi Gabriely, Galina Jain, Anant Wang, Yang Chiocca, E. Antonio Stephens, Robert Marcusson, Eric Yi, Ming Krichevsky, Anna M. Oncotarget Research Paper MicroRNA-10b (miR-10b) is commonly elevated in glioblastoma (GBM), while not expressed in normal brain tissues. Targeted inhibition of miR-10b has pleiotropic effects on GBM derived cell lines, it reduces GBM growth in animal models, but does not affect normal neurons and astrocytes. This data raises the possibility of developing miR-10b-targeting GBM therapy. However, the mechanisms contributing to miR-10b-mediated glioma cell survival and proliferation are unexplored. We found that inhibition of miR-10b has distinct effects on specific glioma cell lines. In cells expressing high levels of tumor suppressor p21WAF1/Cip1, it represses E2F1-mediated transcription, leading to down-regulation of multiple E2F1 target genes encoding for S-phase specific proteins, epigenetic modulators, and miRNAs (e.g. miR-15/16), and thereby stalling progression through the S-phase of cell cycle. Subsequently, miR-15/16 activities are reduced and many of their direct targets are de-repressed, including ubiquitin ligase FBXW7 that destabilizes Cyclin E. Conversely, GBM cells expressing low p21 level, or after p21 knock-down, exhibit weaker or no E2F1 response to miR-10b inhibition. Comparative analysis of The Cancer Genome Atlas revealed a strong correlation between miR-10b and multiple E2F target genes in GBM and low-grade glioma. Taken together, these findings indicate that miR-10b regulates E2F1-mediated transcription in GBM, in a p21-dependent fashion. Impact Journals LLC 2015-02-06 /pmc/articles/PMC4414152/ /pubmed/25738367 Text en Copyright: © 2015 Teplyuk 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
Teplyuk, Nadiya M.
Uhlmann, Erik J.
Wong, Andus Hon-Kit
Karmali, Priya
Basu, Meenakshi
Gabriely, Galina
Jain, Anant
Wang, Yang
Chiocca, E. Antonio
Stephens, Robert
Marcusson, Eric
Yi, Ming
Krichevsky, Anna M.
MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title_full MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title_fullStr MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title_full_unstemmed MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title_short MicroRNA-10b inhibition reduces E2F1-mediated transcription and miR-15/16 activity in glioblastoma
title_sort microrna-10b inhibition reduces e2f1-mediated transcription and mir-15/16 activity in glioblastoma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4414152/
https://www.ncbi.nlm.nih.gov/pubmed/25738367
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