Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel

The molecular pathways that contribute to the proliferation and drug response of cancer cells are highly complex and currently insufficiently characterized. We have identified a previously unknown microRNA-based mechanism that provides cancer cells means to stimulate tumorigenesis via increased geno...

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Autores principales: Tambe, Mahesh, Pruikkonen, Sofia, Mäki-Jouppila, Jenni, Chen, Ping, Elgaaen, Bente Vilming, Straume, Anne Hege, Huhtinen, Kaisa, Cárpen, Olli, Lønning, Per Eystein, Davidson, Ben, Hautaniemi, Sampsa, Kallio, Marko J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper: Chromosome
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4914283/
https://www.ncbi.nlm.nih.gov/pubmed/26943585
http://dx.doi.org/10.18632/oncotarget.7860
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author Tambe, Mahesh
Pruikkonen, Sofia
Mäki-Jouppila, Jenni
Chen, Ping
Elgaaen, Bente Vilming
Straume, Anne Hege
Huhtinen, Kaisa
Cárpen, Olli
Lønning, Per Eystein
Davidson, Ben
Hautaniemi, Sampsa
Kallio, Marko J.
author_facet Tambe, Mahesh
Pruikkonen, Sofia
Mäki-Jouppila, Jenni
Chen, Ping
Elgaaen, Bente Vilming
Straume, Anne Hege
Huhtinen, Kaisa
Cárpen, Olli
Lønning, Per Eystein
Davidson, Ben
Hautaniemi, Sampsa
Kallio, Marko J.
author_sort Tambe, Mahesh
collection PubMed
description The molecular pathways that contribute to the proliferation and drug response of cancer cells are highly complex and currently insufficiently characterized. We have identified a previously unknown microRNA-based mechanism that provides cancer cells means to stimulate tumorigenesis via increased genomic instability and, at the same time, evade the action of clinically utilized microtubule drugs. We demonstrate miR-493-3p to be a novel negative regulator of mitotic arrest deficient-2 (MAD2), an essential component of the spindle assembly checkpoint that monitors the fidelity of chromosome segregation. The microRNA targets the 3′ UTR of Mad2 mRNA thereby preventing translation of the Mad2 protein. In cancer cells, overexpression of miR-493-3p induced a premature mitotic exit that led to increased frequency of aneuploidy and cellular senescence in the progeny cells. Importantly, excess of the miR-493-3p conferred resistance of cancer cells to microtubule drugs. In human neoplasms, miR-493-3p and Mad2 expression alterations correlated with advanced ovarian cancer forms and high miR-493-3p levels were associated with reduced survival of ovarian and breast cancer patients with aggressive tumors, especially in the paclitaxel therapy arm. Our results suggest that intratumoral profiling of miR-493-3p and Mad2 levels can have diagnostic value in predicting the efficacy of taxane chemotherapy.
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spelling pubmed-49142832016-07-11 Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel Tambe, Mahesh Pruikkonen, Sofia Mäki-Jouppila, Jenni Chen, Ping Elgaaen, Bente Vilming Straume, Anne Hege Huhtinen, Kaisa Cárpen, Olli Lønning, Per Eystein Davidson, Ben Hautaniemi, Sampsa Kallio, Marko J. Oncotarget Research Paper: Chromosome The molecular pathways that contribute to the proliferation and drug response of cancer cells are highly complex and currently insufficiently characterized. We have identified a previously unknown microRNA-based mechanism that provides cancer cells means to stimulate tumorigenesis via increased genomic instability and, at the same time, evade the action of clinically utilized microtubule drugs. We demonstrate miR-493-3p to be a novel negative regulator of mitotic arrest deficient-2 (MAD2), an essential component of the spindle assembly checkpoint that monitors the fidelity of chromosome segregation. The microRNA targets the 3′ UTR of Mad2 mRNA thereby preventing translation of the Mad2 protein. In cancer cells, overexpression of miR-493-3p induced a premature mitotic exit that led to increased frequency of aneuploidy and cellular senescence in the progeny cells. Importantly, excess of the miR-493-3p conferred resistance of cancer cells to microtubule drugs. In human neoplasms, miR-493-3p and Mad2 expression alterations correlated with advanced ovarian cancer forms and high miR-493-3p levels were associated with reduced survival of ovarian and breast cancer patients with aggressive tumors, especially in the paclitaxel therapy arm. Our results suggest that intratumoral profiling of miR-493-3p and Mad2 levels can have diagnostic value in predicting the efficacy of taxane chemotherapy. Impact Journals LLC 2016-03-02 /pmc/articles/PMC4914283/ /pubmed/26943585 http://dx.doi.org/10.18632/oncotarget.7860 Text en Copyright: © 2016 Tambe 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: Chromosome
Tambe, Mahesh
Pruikkonen, Sofia
Mäki-Jouppila, Jenni
Chen, Ping
Elgaaen, Bente Vilming
Straume, Anne Hege
Huhtinen, Kaisa
Cárpen, Olli
Lønning, Per Eystein
Davidson, Ben
Hautaniemi, Sampsa
Kallio, Marko J.
Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title_full Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title_fullStr Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title_full_unstemmed Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title_short Novel Mad2-targeting miR-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
title_sort novel mad2-targeting mir-493-3p controls mitotic fidelity and cancer cells’ sensitivity to paclitaxel
topic Research Paper: Chromosome
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4914283/
https://www.ncbi.nlm.nih.gov/pubmed/26943585
http://dx.doi.org/10.18632/oncotarget.7860
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