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Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells

Tumor-initiating cells constitute a population within a tumor mass that shares properties with normal stem cells and is considered responsible for therapy failure in many cancers. We have previously demonstrated that knockdown of the nuclear envelope component Lamin A/C in human neuroblastoma cells...

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Autores principales: Nardella, Marta, Guglielmi, Loredana, Musa, Carla, Iannetti, Ilaria, Maresca, Giovanna, Amendola, Donatella, Porru, Manuela, Carico, Elisabetta, Sessa, Giuseppe, Camerlingo, Rosalba, Dominici, Carlo, Megiorni, Francesca, Milan, Marika, Bearzi, Claudia, Rizzi, Roberto, Pirozzi, Giuseppe, Leonetti, Carlo, Bucci, Barbara, Mercanti, Delio, Felsani, Armando, D'Agnano, Igea
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741732/
https://www.ncbi.nlm.nih.gov/pubmed/26439802
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author Nardella, Marta
Guglielmi, Loredana
Musa, Carla
Iannetti, Ilaria
Maresca, Giovanna
Amendola, Donatella
Porru, Manuela
Carico, Elisabetta
Sessa, Giuseppe
Camerlingo, Rosalba
Dominici, Carlo
Megiorni, Francesca
Milan, Marika
Bearzi, Claudia
Rizzi, Roberto
Pirozzi, Giuseppe
Leonetti, Carlo
Bucci, Barbara
Mercanti, Delio
Felsani, Armando
D'Agnano, Igea
author_facet Nardella, Marta
Guglielmi, Loredana
Musa, Carla
Iannetti, Ilaria
Maresca, Giovanna
Amendola, Donatella
Porru, Manuela
Carico, Elisabetta
Sessa, Giuseppe
Camerlingo, Rosalba
Dominici, Carlo
Megiorni, Francesca
Milan, Marika
Bearzi, Claudia
Rizzi, Roberto
Pirozzi, Giuseppe
Leonetti, Carlo
Bucci, Barbara
Mercanti, Delio
Felsani, Armando
D'Agnano, Igea
author_sort Nardella, Marta
collection PubMed
description Tumor-initiating cells constitute a population within a tumor mass that shares properties with normal stem cells and is considered responsible for therapy failure in many cancers. We have previously demonstrated that knockdown of the nuclear envelope component Lamin A/C in human neuroblastoma cells inhibits retinoic acid-mediated differentiation and results in a more aggressive phenotype. In addition, Lamin A/C is often lost in advanced tumors and changes in the nuclear envelope composition occur during tumor progression. Based on our previous data and considering that Lamin A/C is expressed in differentiated tissues, we hypothesize that the lack of Lamin A/C could predispose cells toward a stem-like phenotype, thus influencing the development of tumor-initiating cells in neuroblastoma. This paper demonstrates that knockdown of Lamin A/C triggers the development of a tumor-initiating cell population with self-renewing features in human neuroblastoma cells. We also demonstrates that the development of TICs is due to an increased expression of MYCN gene and that in neuroblastoma exists an inverse relationship between LMNA and MYCN expression.
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spelling pubmed-47417322016-03-11 Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells Nardella, Marta Guglielmi, Loredana Musa, Carla Iannetti, Ilaria Maresca, Giovanna Amendola, Donatella Porru, Manuela Carico, Elisabetta Sessa, Giuseppe Camerlingo, Rosalba Dominici, Carlo Megiorni, Francesca Milan, Marika Bearzi, Claudia Rizzi, Roberto Pirozzi, Giuseppe Leonetti, Carlo Bucci, Barbara Mercanti, Delio Felsani, Armando D'Agnano, Igea Oncotarget Research Paper Tumor-initiating cells constitute a population within a tumor mass that shares properties with normal stem cells and is considered responsible for therapy failure in many cancers. We have previously demonstrated that knockdown of the nuclear envelope component Lamin A/C in human neuroblastoma cells inhibits retinoic acid-mediated differentiation and results in a more aggressive phenotype. In addition, Lamin A/C is often lost in advanced tumors and changes in the nuclear envelope composition occur during tumor progression. Based on our previous data and considering that Lamin A/C is expressed in differentiated tissues, we hypothesize that the lack of Lamin A/C could predispose cells toward a stem-like phenotype, thus influencing the development of tumor-initiating cells in neuroblastoma. This paper demonstrates that knockdown of Lamin A/C triggers the development of a tumor-initiating cell population with self-renewing features in human neuroblastoma cells. We also demonstrates that the development of TICs is due to an increased expression of MYCN gene and that in neuroblastoma exists an inverse relationship between LMNA and MYCN expression. Impact Journals LLC 2015-09-03 /pmc/articles/PMC4741732/ /pubmed/26439802 Text en Copyright: © 2015 Nardella 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
Nardella, Marta
Guglielmi, Loredana
Musa, Carla
Iannetti, Ilaria
Maresca, Giovanna
Amendola, Donatella
Porru, Manuela
Carico, Elisabetta
Sessa, Giuseppe
Camerlingo, Rosalba
Dominici, Carlo
Megiorni, Francesca
Milan, Marika
Bearzi, Claudia
Rizzi, Roberto
Pirozzi, Giuseppe
Leonetti, Carlo
Bucci, Barbara
Mercanti, Delio
Felsani, Armando
D'Agnano, Igea
Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title_full Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title_fullStr Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title_full_unstemmed Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title_short Down-regulation of the Lamin A/C in neuroblastoma triggers the expansion of tumor initiating cells
title_sort down-regulation of the lamin a/c in neuroblastoma triggers the expansion of tumor initiating cells
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741732/
https://www.ncbi.nlm.nih.gov/pubmed/26439802
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