Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.

In colon cancer, a highly aggressive disease, progression through the malignant sequence is accompanied by increasingly numerous chromosomal rearrangements. To colonize target organs, invasive cells cross several tissues of various elastic moduli. Whether soft tissue increases malignancy or in contr...

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Main Authors: Morgane Rabineau, Leyla Kocgozlu, Denis Dujardin, Bernard Senger, Youssef Haikel, Jean-Claude Voegel, Jean-Noel Freund, Pierre Schaaf, Philippe Lavalle, Dominique Vautier
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3805547?pdf=render
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spelling doaj-4080e90125974780a0e4377755a02c6b2020-11-24T21:10:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01810e7846810.1371/journal.pone.0078468Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.Morgane RabineauLeyla KocgozluDenis DujardinBernard SengerYoussef HaikelJean-Claude VoegelJean-Noel FreundPierre SchaafPhilippe LavalleDominique VautierIn colon cancer, a highly aggressive disease, progression through the malignant sequence is accompanied by increasingly numerous chromosomal rearrangements. To colonize target organs, invasive cells cross several tissues of various elastic moduli. Whether soft tissue increases malignancy or in contrast limits invasive colon cell spreading remains an open question. Using polyelectrolyte multilayer films mimicking microenvironments of various elastic moduli, we revealed that human SW480 colon cancer cells displayed increasing frequency in chromosomal segregation abnormalities when cultured on substrates with decreasing stiffness. Our results show that, although decreasing stiffness correlates with increased cell lethality, a significant proportion of SW480 cancer cells did escape from the very soft substrates, even when bearing abnormal chromosome segregation, achieve mitosis and undergo a new cycle of replication in contrast to human colonic HCoEpiC cells which died on soft substrates. This observation opens the possibility that the ability of cancer cells to overcome defects in chromosome segregation on very soft substrates could contribute to increasing chromosomal rearrangements and tumor cell aggressiveness.http://europepmc.org/articles/PMC3805547?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Morgane Rabineau
Leyla Kocgozlu
Denis Dujardin
Bernard Senger
Youssef Haikel
Jean-Claude Voegel
Jean-Noel Freund
Pierre Schaaf
Philippe Lavalle
Dominique Vautier
spellingShingle Morgane Rabineau
Leyla Kocgozlu
Denis Dujardin
Bernard Senger
Youssef Haikel
Jean-Claude Voegel
Jean-Noel Freund
Pierre Schaaf
Philippe Lavalle
Dominique Vautier
Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
PLoS ONE
author_facet Morgane Rabineau
Leyla Kocgozlu
Denis Dujardin
Bernard Senger
Youssef Haikel
Jean-Claude Voegel
Jean-Noel Freund
Pierre Schaaf
Philippe Lavalle
Dominique Vautier
author_sort Morgane Rabineau
title Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
title_short Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
title_full Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
title_fullStr Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
title_full_unstemmed Contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
title_sort contribution of soft substrates to malignancy and tumor suppression during colon cancer cell division.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description In colon cancer, a highly aggressive disease, progression through the malignant sequence is accompanied by increasingly numerous chromosomal rearrangements. To colonize target organs, invasive cells cross several tissues of various elastic moduli. Whether soft tissue increases malignancy or in contrast limits invasive colon cell spreading remains an open question. Using polyelectrolyte multilayer films mimicking microenvironments of various elastic moduli, we revealed that human SW480 colon cancer cells displayed increasing frequency in chromosomal segregation abnormalities when cultured on substrates with decreasing stiffness. Our results show that, although decreasing stiffness correlates with increased cell lethality, a significant proportion of SW480 cancer cells did escape from the very soft substrates, even when bearing abnormal chromosome segregation, achieve mitosis and undergo a new cycle of replication in contrast to human colonic HCoEpiC cells which died on soft substrates. This observation opens the possibility that the ability of cancer cells to overcome defects in chromosome segregation on very soft substrates could contribute to increasing chromosomal rearrangements and tumor cell aggressiveness.
url http://europepmc.org/articles/PMC3805547?pdf=render
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