MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma

Glioblastomas are aggressive adult brain tumors, characterized by inadequately organized vasculature and consequent nutrient and oxygen (O(2))-depleted areas. Adaptation to low nutrients and hypoxia supports glioblastoma cell survival, progression, and therapeutic resistance. However, specific mecha...

Descripción completa

Detalles Bibliográficos
Autores principales: Mucaj, Vera, Lee, Samuel S., Skuli, Nicolas, Giannoukos, Dionysios N., Qiu, Bo, Eisinger-Mathason, T.S. Karin, Nakazawa, Michael S., Shay, Jessica E.S., Gopal, Pallavi P., Venneti, Sriram, Lal, Priti, Minn, Andy J., Simon, M. Celeste, Mathew, Lijoy K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4275412/
https://www.ncbi.nlm.nih.gov/pubmed/24954504
http://dx.doi.org/10.1038/onc.2014.168
_version_ 1782350121071017984
author Mucaj, Vera
Lee, Samuel S.
Skuli, Nicolas
Giannoukos, Dionysios N.
Qiu, Bo
Eisinger-Mathason, T.S. Karin
Nakazawa, Michael S.
Shay, Jessica E.S.
Gopal, Pallavi P.
Venneti, Sriram
Lal, Priti
Minn, Andy J.
Simon, M. Celeste
Mathew, Lijoy K.
author_facet Mucaj, Vera
Lee, Samuel S.
Skuli, Nicolas
Giannoukos, Dionysios N.
Qiu, Bo
Eisinger-Mathason, T.S. Karin
Nakazawa, Michael S.
Shay, Jessica E.S.
Gopal, Pallavi P.
Venneti, Sriram
Lal, Priti
Minn, Andy J.
Simon, M. Celeste
Mathew, Lijoy K.
author_sort Mucaj, Vera
collection PubMed
description Glioblastomas are aggressive adult brain tumors, characterized by inadequately organized vasculature and consequent nutrient and oxygen (O(2))-depleted areas. Adaptation to low nutrients and hypoxia supports glioblastoma cell survival, progression, and therapeutic resistance. However, specific mechanisms promoting cellular survival under nutrient and O(2) deprivation remain incompletely understood. Here, we show that miR-124 expression is negatively correlated with a hypoxic gene signature in glioblastoma patient samples, suggesting that low miR-124 levels contribute to pro-survival adaptive pathways in this disease. Since miR-124 expression is repressed in various cancers (including glioblastoma), we quantified miR-124 abundance in normoxic and hypoxic regions in glioblastoma patient tissue, and investigated whether ectopic miR-124 expression compromises cell survival, during tumor ischemia. Our results indicate that miR-124 levels are further diminished in hypoxic/ischemic regions within individual glioblastoma patient samples, compared to regions replete in O(2) and nutrients. Importantly, we also show that increased miR-124 expression affects the ability of tumor cells to survive under O(2) and/or nutrient deprivation. Moreover, miR-124 re-expression increases cell death in vivo, and enhances the survival of mice bearing intracranial xenograft tumors. miR-124 exerts this phenotype in part by directly regulating TEAD1, MAPK14/p38α and SERP1, factors involved in cell proliferation and survival under stress. Simultaneous suppression of these miR-124 targets results in similar levels of cell death as caused by miR-124 restoration. Importantly, we further demonstrate that SERP1 re-introduction reverses the hypoxic cell death elicited by miR-124, indicating the importance of SERP1 in promoting tumor cell survival. In support of our experimental data, we observed a significant correlation between high SERP1 levels and poor patient outcome in glioblastoma patients. Collectively, among the many pro-tumorigeneic properties of miR-124 repression in glioblastoma, we delineated a novel role in promoting tumor cell survival under stressful microenvironments, thereby supporting tumor progression.
format Online
Article
Text
id pubmed-4275412
institution National Center for Biotechnology Information
language English
publishDate 2014
record_format MEDLINE/PubMed
spelling pubmed-42754122015-10-23 MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma Mucaj, Vera Lee, Samuel S. Skuli, Nicolas Giannoukos, Dionysios N. Qiu, Bo Eisinger-Mathason, T.S. Karin Nakazawa, Michael S. Shay, Jessica E.S. Gopal, Pallavi P. Venneti, Sriram Lal, Priti Minn, Andy J. Simon, M. Celeste Mathew, Lijoy K. Oncogene Article Glioblastomas are aggressive adult brain tumors, characterized by inadequately organized vasculature and consequent nutrient and oxygen (O(2))-depleted areas. Adaptation to low nutrients and hypoxia supports glioblastoma cell survival, progression, and therapeutic resistance. However, specific mechanisms promoting cellular survival under nutrient and O(2) deprivation remain incompletely understood. Here, we show that miR-124 expression is negatively correlated with a hypoxic gene signature in glioblastoma patient samples, suggesting that low miR-124 levels contribute to pro-survival adaptive pathways in this disease. Since miR-124 expression is repressed in various cancers (including glioblastoma), we quantified miR-124 abundance in normoxic and hypoxic regions in glioblastoma patient tissue, and investigated whether ectopic miR-124 expression compromises cell survival, during tumor ischemia. Our results indicate that miR-124 levels are further diminished in hypoxic/ischemic regions within individual glioblastoma patient samples, compared to regions replete in O(2) and nutrients. Importantly, we also show that increased miR-124 expression affects the ability of tumor cells to survive under O(2) and/or nutrient deprivation. Moreover, miR-124 re-expression increases cell death in vivo, and enhances the survival of mice bearing intracranial xenograft tumors. miR-124 exerts this phenotype in part by directly regulating TEAD1, MAPK14/p38α and SERP1, factors involved in cell proliferation and survival under stress. Simultaneous suppression of these miR-124 targets results in similar levels of cell death as caused by miR-124 restoration. Importantly, we further demonstrate that SERP1 re-introduction reverses the hypoxic cell death elicited by miR-124, indicating the importance of SERP1 in promoting tumor cell survival. In support of our experimental data, we observed a significant correlation between high SERP1 levels and poor patient outcome in glioblastoma patients. Collectively, among the many pro-tumorigeneic properties of miR-124 repression in glioblastoma, we delineated a novel role in promoting tumor cell survival under stressful microenvironments, thereby supporting tumor progression. 2014-06-23 2015-04-23 /pmc/articles/PMC4275412/ /pubmed/24954504 http://dx.doi.org/10.1038/onc.2014.168 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Mucaj, Vera
Lee, Samuel S.
Skuli, Nicolas
Giannoukos, Dionysios N.
Qiu, Bo
Eisinger-Mathason, T.S. Karin
Nakazawa, Michael S.
Shay, Jessica E.S.
Gopal, Pallavi P.
Venneti, Sriram
Lal, Priti
Minn, Andy J.
Simon, M. Celeste
Mathew, Lijoy K.
MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title_full MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title_fullStr MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title_full_unstemmed MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title_short MicroRNA-124 expression counteracts pro-survival stress responses in glioblastoma
title_sort microrna-124 expression counteracts pro-survival stress responses in glioblastoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4275412/
https://www.ncbi.nlm.nih.gov/pubmed/24954504
http://dx.doi.org/10.1038/onc.2014.168
work_keys_str_mv AT mucajvera microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT leesamuels microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT skulinicolas microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT giannoukosdionysiosn microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT qiubo microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT eisingermathasontskarin microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT nakazawamichaels microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT shayjessicaes microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT gopalpallavip microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT vennetisriram microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT lalpriti microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT minnandyj microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT simonmceleste microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma
AT mathewlijoyk microrna124expressioncounteractsprosurvivalstressresponsesinglioblastoma

Ejemplares similares