DNA replication is intrinsically hindered in terminally differentiated myotubes.

DNA replication is intrinsically hindered in terminally differentiated myotubes.

Terminally differentiated (TD) cells permanently exit the mitotic cycle while acquiring specialized characteristics. Although TD cells can be forced to reenter the cell cycle by different means, they cannot be made to stably proliferate, as attempts to induce their replication constantly result in c...

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Main Authors: Deborah Pajalunga, Eleonora M R Puggioni, Alessia Mazzola, Valentina Leva, Alessandra Montecucco, Marco Crescenzi
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-07-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2903488?pdf=render
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spelling doaj-6a7bde853bd348ada5d5899136fb9de22020-11-25T01:46:10ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-07-0157e1155910.1371/journal.pone.0011559DNA replication is intrinsically hindered in terminally differentiated myotubes.Deborah PajalungaEleonora M R PuggioniAlessia MazzolaValentina LevaAlessandra MontecuccoMarco CrescenziTerminally differentiated (TD) cells permanently exit the mitotic cycle while acquiring specialized characteristics. Although TD cells can be forced to reenter the cell cycle by different means, they cannot be made to stably proliferate, as attempts to induce their replication constantly result in cell death or indefinite growth arrest. There is currently no biological explanation for this failure.Here we show that TD mouse myotubes, reactivated by depletion of the p21 and p27 cell cycle inhibitors, are unable to complete DNA replication and sustain heavy DNA damage, which triggers apoptosis or results in mitotic catastrophe. In striking contrast, quiescent, non-TD fibroblasts and myoblasts, reactivated in the same way, fully replicate their DNA, do not suffer DNA damage, and proliferate even in the absence of growth factors. Similar results are obtained when myotubes and fibroblasts are reactivated by forced expression of E1A or cyclin D1 and cdk4.We conclude that the inability of myotubes to complete DNA replication must be ascribed to peculiar features inherent in their TD state, rather than to the reactivation method. On reviewing the literature concerning reactivation of other TD cell types, we propose that similar mechanisms underlie the general inability of all kinds of TD cells to proliferate in response to otherwise mitogenic stimuli. These results define an unexpected basis for the well known incompetence of mammalian postmitotic cells to proliferate. Furthermore, this trait might contribute to explain the inability of these cells to play a role in tissue repair, unlike their counterparts in extensively regenerating species.http://europepmc.org/articles/PMC2903488?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Deborah Pajalunga
Eleonora M R Puggioni
Alessia Mazzola
Valentina Leva
Alessandra Montecucco
Marco Crescenzi
spellingShingle Deborah Pajalunga
Eleonora M R Puggioni
Alessia Mazzola
Valentina Leva
Alessandra Montecucco
Marco Crescenzi
DNA replication is intrinsically hindered in terminally differentiated myotubes.
PLoS ONE
author_facet Deborah Pajalunga
Eleonora M R Puggioni
Alessia Mazzola
Valentina Leva
Alessandra Montecucco
Marco Crescenzi
author_sort Deborah Pajalunga
title DNA replication is intrinsically hindered in terminally differentiated myotubes.
title_short DNA replication is intrinsically hindered in terminally differentiated myotubes.
title_full DNA replication is intrinsically hindered in terminally differentiated myotubes.
title_fullStr DNA replication is intrinsically hindered in terminally differentiated myotubes.
title_full_unstemmed DNA replication is intrinsically hindered in terminally differentiated myotubes.
title_sort dna replication is intrinsically hindered in terminally differentiated myotubes.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-07-01
description Terminally differentiated (TD) cells permanently exit the mitotic cycle while acquiring specialized characteristics. Although TD cells can be forced to reenter the cell cycle by different means, they cannot be made to stably proliferate, as attempts to induce their replication constantly result in cell death or indefinite growth arrest. There is currently no biological explanation for this failure.Here we show that TD mouse myotubes, reactivated by depletion of the p21 and p27 cell cycle inhibitors, are unable to complete DNA replication and sustain heavy DNA damage, which triggers apoptosis or results in mitotic catastrophe. In striking contrast, quiescent, non-TD fibroblasts and myoblasts, reactivated in the same way, fully replicate their DNA, do not suffer DNA damage, and proliferate even in the absence of growth factors. Similar results are obtained when myotubes and fibroblasts are reactivated by forced expression of E1A or cyclin D1 and cdk4.We conclude that the inability of myotubes to complete DNA replication must be ascribed to peculiar features inherent in their TD state, rather than to the reactivation method. On reviewing the literature concerning reactivation of other TD cell types, we propose that similar mechanisms underlie the general inability of all kinds of TD cells to proliferate in response to otherwise mitogenic stimuli. These results define an unexpected basis for the well known incompetence of mammalian postmitotic cells to proliferate. Furthermore, this trait might contribute to explain the inability of these cells to play a role in tissue repair, unlike their counterparts in extensively regenerating species.
url http://europepmc.org/articles/PMC2903488?pdf=render
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