Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.

Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.

Little information is available on the ability of terminally differentiated cells to efficiently repair DNA double strand breaks (DSBs), and one might reasonably speculate that efficient DNA repair of these threatening DNA lesions, is needed in cells of long life span with no or limited regeneration...

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Main Authors: Aline Meulle, Bernard Salles, Danièle Daviaud, Philippe Valet, Catherine Muller
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2556389?pdf=render
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spelling doaj-4d33cca44b0b442c85902a1446e3f5882020-11-24T22:00:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032008-01-01310e334510.1371/journal.pone.0003345Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.Aline MeulleBernard SallesDanièle DaviaudPhilippe ValetCatherine MullerLittle information is available on the ability of terminally differentiated cells to efficiently repair DNA double strand breaks (DSBs), and one might reasonably speculate that efficient DNA repair of these threatening DNA lesions, is needed in cells of long life span with no or limited regeneration from precursor. Few tissues are available besides neurons that allow the study of DNA DSBs repair activity in very long-lived cells. Adipocytes represent a suitable model since it is generally admitted that there is a very slow turnover of adipocytes in adult. Using both Pulse Field Gel Electrophoresis (PFGE) and the disappearance of the phosphorylated form of the histone variant H2AX, we demonstrated that the ability to repair DSBs is increased during adipocyte differentiation using the murine pre-adipocyte cell line, 3T3F442A. In mammalian cells, DSBs are mainly repaired by the non-homologous end-joining pathway (NHEJ) that relies on the DNA dependent protein kinase (DNA-PK) activity. During the first 24 h following the commitment into adipogenesis, we show an increase in the expression and activity of the catalytic sub-unit of the DNA-PK complex, DNA-PKcs. The increased in DNA DSBs repair activity observed in adipocytes was due to the increase in DNA-PK activity as shown by the use of DNA-PK inhibitor or sub-clones of 3T3F442A deficient in DNA-PKcs using long term RNA interference. Interestingly, the up-regulation of DNA-PK does not regulate the differentiation program itself. Finally, similar positive regulation of DNA-PKcs expression and activity was observed during differentiation of primary culture of pre-adipocytes isolated from human sub-cutaneous adipose tissue. Our results show that DNA DSBs repair activity is up regulated during the early commitment into adipogenesis due to an up-regulation of DNA-PK expression and activity. In opposition to the general view that DNA DSBs repair is decreased during differentiation, our results demonstrate that an up-regulation of this process might be observed in post-mitotic long-lived cells.http://europepmc.org/articles/PMC2556389?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Aline Meulle
Bernard Salles
Danièle Daviaud
Philippe Valet
Catherine Muller
spellingShingle Aline Meulle
Bernard Salles
Danièle Daviaud
Philippe Valet
Catherine Muller
Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
PLoS ONE
author_facet Aline Meulle
Bernard Salles
Danièle Daviaud
Philippe Valet
Catherine Muller
author_sort Aline Meulle
title Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
title_short Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
title_full Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
title_fullStr Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
title_full_unstemmed Positive regulation of DNA double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
title_sort positive regulation of dna double strand break repair activity during differentiation of long life span cells: the example of adipogenesis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2008-01-01
description Little information is available on the ability of terminally differentiated cells to efficiently repair DNA double strand breaks (DSBs), and one might reasonably speculate that efficient DNA repair of these threatening DNA lesions, is needed in cells of long life span with no or limited regeneration from precursor. Few tissues are available besides neurons that allow the study of DNA DSBs repair activity in very long-lived cells. Adipocytes represent a suitable model since it is generally admitted that there is a very slow turnover of adipocytes in adult. Using both Pulse Field Gel Electrophoresis (PFGE) and the disappearance of the phosphorylated form of the histone variant H2AX, we demonstrated that the ability to repair DSBs is increased during adipocyte differentiation using the murine pre-adipocyte cell line, 3T3F442A. In mammalian cells, DSBs are mainly repaired by the non-homologous end-joining pathway (NHEJ) that relies on the DNA dependent protein kinase (DNA-PK) activity. During the first 24 h following the commitment into adipogenesis, we show an increase in the expression and activity of the catalytic sub-unit of the DNA-PK complex, DNA-PKcs. The increased in DNA DSBs repair activity observed in adipocytes was due to the increase in DNA-PK activity as shown by the use of DNA-PK inhibitor or sub-clones of 3T3F442A deficient in DNA-PKcs using long term RNA interference. Interestingly, the up-regulation of DNA-PK does not regulate the differentiation program itself. Finally, similar positive regulation of DNA-PKcs expression and activity was observed during differentiation of primary culture of pre-adipocytes isolated from human sub-cutaneous adipose tissue. Our results show that DNA DSBs repair activity is up regulated during the early commitment into adipogenesis due to an up-regulation of DNA-PK expression and activity. In opposition to the general view that DNA DSBs repair is decreased during differentiation, our results demonstrate that an up-regulation of this process might be observed in post-mitotic long-lived cells.
url http://europepmc.org/articles/PMC2556389?pdf=render
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