miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs

microRNA miR-221 is frequently over-expressed in a variety of human neoplasms. Aim of this study was to identify new miR-221 gene targets to improve our understanding on the molecular tumor-promoting mechanisms affected by miR-221. Gene expression profiling of miR-221-transfected-SNU-398 cells was a...

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Autores principales: Lupini, Laura, Bassi, Cristian, Ferracin, Manuela, Bartonicek, Nenad, D'Abundo, Lucilla, Zagatti, Barbara, Callegari, Elisa, Musa, Gentian, Moshiri, Farzaneh, Gramantieri, Laura, Corrales, Fernando J., Enright, Anton J., Sabbioni, Silvia, Negrini, Massimo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2013
Materias:
Genetics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3635019/
https://www.ncbi.nlm.nih.gov/pubmed/23630541
http://dx.doi.org/10.3389/fgene.2013.00064
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author Lupini, Laura
Bassi, Cristian
Ferracin, Manuela
Bartonicek, Nenad
D'Abundo, Lucilla
Zagatti, Barbara
Callegari, Elisa
Musa, Gentian
Moshiri, Farzaneh
Gramantieri, Laura
Corrales, Fernando J.
Enright, Anton J.
Sabbioni, Silvia
Negrini, Massimo
author_facet Lupini, Laura
Bassi, Cristian
Ferracin, Manuela
Bartonicek, Nenad
D'Abundo, Lucilla
Zagatti, Barbara
Callegari, Elisa
Musa, Gentian
Moshiri, Farzaneh
Gramantieri, Laura
Corrales, Fernando J.
Enright, Anton J.
Sabbioni, Silvia
Negrini, Massimo
author_sort Lupini, Laura
collection PubMed
description microRNA miR-221 is frequently over-expressed in a variety of human neoplasms. Aim of this study was to identify new miR-221 gene targets to improve our understanding on the molecular tumor-promoting mechanisms affected by miR-221. Gene expression profiling of miR-221-transfected-SNU-398 cells was analyzed by the Sylamer algorithm to verify the enrichment of miR-221 targets among down-modulated genes. This analysis revealed that enforced expression of miR-221 in SNU-398 cells caused the down-regulation of 602 mRNAs carrying sequences homologous to miR-221 seed sequence within their 3′UTRs. Pathways analysis performed on these genes revealed their prominent involvement in cell proliferation and apoptosis. Activation of E2F, MYC, NFkB, and β-catenin pathways was experimentally proven. Some of the new miR-221 target genes, including RB1, WEE1 (cell cycle inhibitors), APAF1 (pro-apoptotic), ANXA1, CTCF (transcriptional repressor), were individually validated as miR-221 targets in SNU-398, HepG2, and HEK293 cell lines. By identifying a large set of miR-221 gene targets, this study improves our knowledge about miR-221 molecular mechanisms involved in tumorigenesis. The modulation of mRNA level of 602 genes confirms the ability of miR-221 to promote cancer by affecting multiple oncogenic pathways.
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spelling pubmed-36350192013-04-29 miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs Lupini, Laura Bassi, Cristian Ferracin, Manuela Bartonicek, Nenad D'Abundo, Lucilla Zagatti, Barbara Callegari, Elisa Musa, Gentian Moshiri, Farzaneh Gramantieri, Laura Corrales, Fernando J. Enright, Anton J. Sabbioni, Silvia Negrini, Massimo Front Genet Genetics microRNA miR-221 is frequently over-expressed in a variety of human neoplasms. Aim of this study was to identify new miR-221 gene targets to improve our understanding on the molecular tumor-promoting mechanisms affected by miR-221. Gene expression profiling of miR-221-transfected-SNU-398 cells was analyzed by the Sylamer algorithm to verify the enrichment of miR-221 targets among down-modulated genes. This analysis revealed that enforced expression of miR-221 in SNU-398 cells caused the down-regulation of 602 mRNAs carrying sequences homologous to miR-221 seed sequence within their 3′UTRs. Pathways analysis performed on these genes revealed their prominent involvement in cell proliferation and apoptosis. Activation of E2F, MYC, NFkB, and β-catenin pathways was experimentally proven. Some of the new miR-221 target genes, including RB1, WEE1 (cell cycle inhibitors), APAF1 (pro-apoptotic), ANXA1, CTCF (transcriptional repressor), were individually validated as miR-221 targets in SNU-398, HepG2, and HEK293 cell lines. By identifying a large set of miR-221 gene targets, this study improves our knowledge about miR-221 molecular mechanisms involved in tumorigenesis. The modulation of mRNA level of 602 genes confirms the ability of miR-221 to promote cancer by affecting multiple oncogenic pathways. Frontiers Media S.A. 2013-04-25 /pmc/articles/PMC3635019/ /pubmed/23630541 http://dx.doi.org/10.3389/fgene.2013.00064 Text en Copyright © 2013 Lupini, Bassi, Ferracin, Bartonicek, D'Abundo, Zagatti, Callegari, Musa, Moshiri, Gramantieri, Corrales, Enright, Sabbioni and Negrini. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in other forums, provided the original authors and source are credited and subject to any copyright notices concerning any third-party graphics etc.
spellingShingle Genetics
Lupini, Laura
Bassi, Cristian
Ferracin, Manuela
Bartonicek, Nenad
D'Abundo, Lucilla
Zagatti, Barbara
Callegari, Elisa
Musa, Gentian
Moshiri, Farzaneh
Gramantieri, Laura
Corrales, Fernando J.
Enright, Anton J.
Sabbioni, Silvia
Negrini, Massimo
miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title_full miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title_fullStr miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title_full_unstemmed miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title_short miR-221 affects multiple cancer pathways by modulating the level of hundreds messenger RNAs
title_sort mir-221 affects multiple cancer pathways by modulating the level of hundreds messenger rnas
topic Genetics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3635019/
https://www.ncbi.nlm.nih.gov/pubmed/23630541
http://dx.doi.org/10.3389/fgene.2013.00064
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