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

Academic Article
Publication Date:
2015
abstract:
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 acidmediated 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 tumorinitiating 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.
Iris type:
01.01 Articolo in rivista
Keywords:
neuroblastoma; TICs; Lamin A/C; MYCN; miRNAs
List of contributors:
Mercanti, Delio; Felsani, Armando; Rizzi, Roberto; Bearzi, Claudia; D'Agnano, Igea
Authors of the University:
BEARZI CLAUDIA
D'AGNANO IGEA
RIZZI ROBERTO
Handle:
https://iris.cnr.it/handle/20.500.14243/296118
Published in:
ONCOTARGET
Journal
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Overview

URL

https://www.oncotarget.com/article/5104/text/
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