53BP1 contributes to a robust genomic stability in human fibroblasts

Faithful repair of damaged DNA is a crucial process in maintaining cell viability and function. A multitude of factors and pathways guides this process and includes repair proteins and cell cycle checkpoint factors. Differences in the maintenance of genomic processes are one feature that may contrib...

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Autores principales: Fink, Lauren S., Roell, Michaela, Caiazza, Emanuela, Lerner, Chad, Stamato, Thomas, Hrelia, Silvana, Lorenzini, Antonello, Sell, Christian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2011
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3227449/
https://www.ncbi.nlm.nih.gov/pubmed/21931182
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author Fink, Lauren S.
Roell, Michaela
Caiazza, Emanuela
Lerner, Chad
Stamato, Thomas
Hrelia, Silvana
Lorenzini, Antonello
Sell, Christian
author_facet Fink, Lauren S.
Roell, Michaela
Caiazza, Emanuela
Lerner, Chad
Stamato, Thomas
Hrelia, Silvana
Lorenzini, Antonello
Sell, Christian
author_sort Fink, Lauren S.
collection PubMed
description Faithful repair of damaged DNA is a crucial process in maintaining cell viability and function. A multitude of factors and pathways guides this process and includes repair proteins and cell cycle checkpoint factors. Differences in the maintenance of genomic processes are one feature that may contribute to species-specific differences in lifespan. We predicted that 53BP1, a key transducer of the DNA damage response and cell cycle checkpoint control, is highly involved in maintaining genomic stability and may function differently in cells from different species. We demonstrate a difference in the levels and recruitment of 53BP1 in mouse and human cells following DNA damage. In addition, we show that unresolved DNA damage persists more in mouse cells than in human cells, as evidenced by increased numbers of micronuclei. The difference in micronuclei seems to be related to the levels of 53BP1 present in cells. Finally, we present evidence that unresolved DNA damage correlates with species lifespan. Taken together, these studies suggest a link between recruitment of 53BP1, resolution of DNA damage, and increased species lifespan.
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spelling pubmed-32274492011-12-01 53BP1 contributes to a robust genomic stability in human fibroblasts Fink, Lauren S. Roell, Michaela Caiazza, Emanuela Lerner, Chad Stamato, Thomas Hrelia, Silvana Lorenzini, Antonello Sell, Christian Aging (Albany NY) Research Paper Faithful repair of damaged DNA is a crucial process in maintaining cell viability and function. A multitude of factors and pathways guides this process and includes repair proteins and cell cycle checkpoint factors. Differences in the maintenance of genomic processes are one feature that may contribute to species-specific differences in lifespan. We predicted that 53BP1, a key transducer of the DNA damage response and cell cycle checkpoint control, is highly involved in maintaining genomic stability and may function differently in cells from different species. We demonstrate a difference in the levels and recruitment of 53BP1 in mouse and human cells following DNA damage. In addition, we show that unresolved DNA damage persists more in mouse cells than in human cells, as evidenced by increased numbers of micronuclei. The difference in micronuclei seems to be related to the levels of 53BP1 present in cells. Finally, we present evidence that unresolved DNA damage correlates with species lifespan. Taken together, these studies suggest a link between recruitment of 53BP1, resolution of DNA damage, and increased species lifespan. Impact Journals LLC 2011-09-08 /pmc/articles/PMC3227449/ /pubmed/21931182 Text en Copyright: © 2011 Fink 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
Fink, Lauren S.
Roell, Michaela
Caiazza, Emanuela
Lerner, Chad
Stamato, Thomas
Hrelia, Silvana
Lorenzini, Antonello
Sell, Christian
53BP1 contributes to a robust genomic stability in human fibroblasts
title 53BP1 contributes to a robust genomic stability in human fibroblasts
title_full 53BP1 contributes to a robust genomic stability in human fibroblasts
title_fullStr 53BP1 contributes to a robust genomic stability in human fibroblasts
title_full_unstemmed 53BP1 contributes to a robust genomic stability in human fibroblasts
title_short 53BP1 contributes to a robust genomic stability in human fibroblasts
title_sort 53bp1 contributes to a robust genomic stability in human fibroblasts
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3227449/
https://www.ncbi.nlm.nih.gov/pubmed/21931182
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