Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner

MicroRNAs (miRs) are a large class of small regulatory RNAs that function as nodes of signaling networks. This implicates that miRs expression has to be finely tuned, as observed during cell cycle progression. Here, using an expression profiling approach, we provide evidence that the CDK inhibitor p...

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Autores principales: Armenia, Joshua, Fabris, Linda, Lovat, Francesca, Berton, Stefania, Segatto, Ilenia, D'Andrea, Sara, Ivan, Cristina, Cascione, Luciano, Calin, George A., Croce, Carlo M., Colombatti, Alfonso, Vecchione, Andrea, Belletti, Barbara, Baldassarre, Gustavo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Priority Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4012735/
https://www.ncbi.nlm.nih.gov/pubmed/24727437
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author Armenia, Joshua
Fabris, Linda
Lovat, Francesca
Berton, Stefania
Segatto, Ilenia
D'Andrea, Sara
Ivan, Cristina
Cascione, Luciano
Calin, George A.
Croce, Carlo M.
Colombatti, Alfonso
Vecchione, Andrea
Belletti, Barbara
Baldassarre, Gustavo
author_facet Armenia, Joshua
Fabris, Linda
Lovat, Francesca
Berton, Stefania
Segatto, Ilenia
D'Andrea, Sara
Ivan, Cristina
Cascione, Luciano
Calin, George A.
Croce, Carlo M.
Colombatti, Alfonso
Vecchione, Andrea
Belletti, Barbara
Baldassarre, Gustavo
author_sort Armenia, Joshua
collection PubMed
description MicroRNAs (miRs) are a large class of small regulatory RNAs that function as nodes of signaling networks. This implicates that miRs expression has to be finely tuned, as observed during cell cycle progression. Here, using an expression profiling approach, we provide evidence that the CDK inhibitor p27(Kip1) regulates miRs expression following cell cycle exit. By using wild type and p27KO cells harvested in different phases of the cell cycle we identified several miRs regulated by p27(Kip1) during the G1 to S phase transition. Among these miRs, we identified miR-223 as a miR specifically upregulated by p27(Kip1) in G1 arrested cells. Our data demonstrate that p27(Kip1) regulated the expression of miR-223, via two distinct mechanisms. p27(Kip1) directly stabilized mature miR-223 expression, acting as a RNA binding protein and it controlled E2F1 expression that, in turn, regulated miR-223 promoter activity. The resulting elevated miR-223 levels ultimately participated to arresting cell cycle progression following contact inhibition. Importantly, this mechanism of growth control was conserved in human cells and deranged in breast cancers. Here, we identify a novel and conserved function of p27(Kip1) that, by modulating miR-223 expression, contributes to proper regulation of cell cycle exit following contact inhibition. Thus we propose a new role for miR-223 in the regulation of breast cancer progression.
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spelling pubmed-40127352014-05-09 Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner Armenia, Joshua Fabris, Linda Lovat, Francesca Berton, Stefania Segatto, Ilenia D'Andrea, Sara Ivan, Cristina Cascione, Luciano Calin, George A. Croce, Carlo M. Colombatti, Alfonso Vecchione, Andrea Belletti, Barbara Baldassarre, Gustavo Oncotarget Priority Research Paper MicroRNAs (miRs) are a large class of small regulatory RNAs that function as nodes of signaling networks. This implicates that miRs expression has to be finely tuned, as observed during cell cycle progression. Here, using an expression profiling approach, we provide evidence that the CDK inhibitor p27(Kip1) regulates miRs expression following cell cycle exit. By using wild type and p27KO cells harvested in different phases of the cell cycle we identified several miRs regulated by p27(Kip1) during the G1 to S phase transition. Among these miRs, we identified miR-223 as a miR specifically upregulated by p27(Kip1) in G1 arrested cells. Our data demonstrate that p27(Kip1) regulated the expression of miR-223, via two distinct mechanisms. p27(Kip1) directly stabilized mature miR-223 expression, acting as a RNA binding protein and it controlled E2F1 expression that, in turn, regulated miR-223 promoter activity. The resulting elevated miR-223 levels ultimately participated to arresting cell cycle progression following contact inhibition. Importantly, this mechanism of growth control was conserved in human cells and deranged in breast cancers. Here, we identify a novel and conserved function of p27(Kip1) that, by modulating miR-223 expression, contributes to proper regulation of cell cycle exit following contact inhibition. Thus we propose a new role for miR-223 in the regulation of breast cancer progression. Impact Journals LLC 2014-03-04 /pmc/articles/PMC4012735/ /pubmed/24727437 Text en Copyright: © 2014 Armenia 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 Priority Research Paper
Armenia, Joshua
Fabris, Linda
Lovat, Francesca
Berton, Stefania
Segatto, Ilenia
D'Andrea, Sara
Ivan, Cristina
Cascione, Luciano
Calin, George A.
Croce, Carlo M.
Colombatti, Alfonso
Vecchione, Andrea
Belletti, Barbara
Baldassarre, Gustavo
Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title_full Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title_fullStr Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title_full_unstemmed Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title_short Contact inhibition modulates intracellular levels of miR-223 in a p27kip1-dependent manner
title_sort contact inhibition modulates intracellular levels of mir-223 in a p27kip1-dependent manner
topic Priority Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4012735/
https://www.ncbi.nlm.nih.gov/pubmed/24727437
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