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Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression

Chrysotile, like other types of asbestos, has been associated with mesothelioma, lung cancer and asbestosis. However, the cellular abnormalities induced by these fibers involved in cancer development have not been elucidated yet. Previous works show that chrysotile fibers induce features of cancer c...

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Autores principales: Cortez, Beatriz Araujo, Teixeira, Paula Rezende, Redick, Sambra, Doxsey, Stephen, Machado-Santelli, Glaucia Maria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4891019/
https://www.ncbi.nlm.nih.gov/pubmed/26788989
http://dx.doi.org/10.18632/oncotarget.6924
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author Cortez, Beatriz Araujo
Teixeira, Paula Rezende
Redick, Sambra
Doxsey, Stephen
Machado-Santelli, Glaucia Maria
author_facet Cortez, Beatriz Araujo
Teixeira, Paula Rezende
Redick, Sambra
Doxsey, Stephen
Machado-Santelli, Glaucia Maria
author_sort Cortez, Beatriz Araujo
collection PubMed
description Chrysotile, like other types of asbestos, has been associated with mesothelioma, lung cancer and asbestosis. However, the cellular abnormalities induced by these fibers involved in cancer development have not been elucidated yet. Previous works show that chrysotile fibers induce features of cancer cells, such as aneuploidy, multinucleation and multipolar mitosis. In the present study, normal and cancer derived human cell lines were treated with chrysotile and the cellular and molecular mechanisms related to generation of aneuploid cells was elucidated. The first alteration observed was cytokinesis regression, the main cause of multinucleated cells formation and centrosome amplification. The multinucleated cells formed after cytokinesis regression were able to progress through cell cycle and generated aneuploid cells after abnormal mitosis. To understand the process of cytokinesis regression, localization of cytokinetic proteins was investigated. It was observed mislocalization of Anillin, Aurora B, Septin 9 and Alix in the intercellular bridge, and no determination of secondary constriction and abscission sites. Fiber treatment also led to overexpression of genes related to cancer, cytokinesis and cell cycle. The results show that chrysotile fibers induce cellular and molecular alterations in normal and tumor cells that have been related to cancer initiation and progression, and that tetraploidization and aneuploid cell formation are striking events after fiber internalization, which could generate a favorable context to cancer development.
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spelling pubmed-48910192016-06-20 Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression Cortez, Beatriz Araujo Teixeira, Paula Rezende Redick, Sambra Doxsey, Stephen Machado-Santelli, Glaucia Maria Oncotarget Research Paper Chrysotile, like other types of asbestos, has been associated with mesothelioma, lung cancer and asbestosis. However, the cellular abnormalities induced by these fibers involved in cancer development have not been elucidated yet. Previous works show that chrysotile fibers induce features of cancer cells, such as aneuploidy, multinucleation and multipolar mitosis. In the present study, normal and cancer derived human cell lines were treated with chrysotile and the cellular and molecular mechanisms related to generation of aneuploid cells was elucidated. The first alteration observed was cytokinesis regression, the main cause of multinucleated cells formation and centrosome amplification. The multinucleated cells formed after cytokinesis regression were able to progress through cell cycle and generated aneuploid cells after abnormal mitosis. To understand the process of cytokinesis regression, localization of cytokinetic proteins was investigated. It was observed mislocalization of Anillin, Aurora B, Septin 9 and Alix in the intercellular bridge, and no determination of secondary constriction and abscission sites. Fiber treatment also led to overexpression of genes related to cancer, cytokinesis and cell cycle. The results show that chrysotile fibers induce cellular and molecular alterations in normal and tumor cells that have been related to cancer initiation and progression, and that tetraploidization and aneuploid cell formation are striking events after fiber internalization, which could generate a favorable context to cancer development. Impact Journals LLC 2016-01-15 /pmc/articles/PMC4891019/ /pubmed/26788989 http://dx.doi.org/10.18632/oncotarget.6924 Text en Copyright: © 2016 Cortez 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
Cortez, Beatriz Araujo
Teixeira, Paula Rezende
Redick, Sambra
Doxsey, Stephen
Machado-Santelli, Glaucia Maria
Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title_full Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title_fullStr Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title_full_unstemmed Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title_short Multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
title_sort multipolar mitosis and aneuploidy after chrysotile treatment: a consequence of abscission failure and cytokinesis regression
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4891019/
https://www.ncbi.nlm.nih.gov/pubmed/26788989
http://dx.doi.org/10.18632/oncotarget.6924
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