XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage

XRCC1 is a scaffold protein capable of interacting with several DNA repair proteins. Here we provide evidence for the presence of XRCC1 in different complexes of sizes from 200 to 1500 kDa, and we show that immunoprecipitates using XRCC1 as bait are capable of complete repair of AP sites via both sh...

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Autores principales: Hanssen-Bauer, Audun, Solvang-Garten, Karin, Sundheim, Ottar, Peña-Diaz, Javier, Andersen, Sonja, Slupphaug, Geir, Krokan, Hans E, Wilson, David M, Akbari, Mansour, Otterlei, Marit
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wiley Subscription Services, Inc., A Wiley Company 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3229989/
https://www.ncbi.nlm.nih.gov/pubmed/21786338
http://dx.doi.org/10.1002/em.20663
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author Hanssen-Bauer, Audun
Solvang-Garten, Karin
Sundheim, Ottar
Peña-Diaz, Javier
Andersen, Sonja
Slupphaug, Geir
Krokan, Hans E
Wilson, David M
Akbari, Mansour
Otterlei, Marit
author_facet Hanssen-Bauer, Audun
Solvang-Garten, Karin
Sundheim, Ottar
Peña-Diaz, Javier
Andersen, Sonja
Slupphaug, Geir
Krokan, Hans E
Wilson, David M
Akbari, Mansour
Otterlei, Marit
author_sort Hanssen-Bauer, Audun
collection PubMed
description XRCC1 is a scaffold protein capable of interacting with several DNA repair proteins. Here we provide evidence for the presence of XRCC1 in different complexes of sizes from 200 to 1500 kDa, and we show that immunoprecipitates using XRCC1 as bait are capable of complete repair of AP sites via both short patch (SP) and long patch (LP) base excision repair (BER). We show that POLβ and PNK colocalize with XRCC1 in replication foci and that POLβ and PNK, but not PCNA, colocalize with constitutively present XRCC1-foci as well as damage-induced foci when low doses of a DNA-damaging agent are applied. We demonstrate that the laser dose used for introducing DNA damage determines the repertoire of DNA repair proteins recruited. Furthermore, we demonstrate that recruitment of POLβ and PNK to regions irradiated with low laser dose requires XRCC1 and that inhibition of PARylation by PARP-inhibitors only slightly reduces the recruitment of XRCC1, PNK, or POLβ to sites of DNA damage. Recruitment of PCNA and FEN-1 requires higher doses of irradiation and is enhanced by XRCC1, as well as by accumulation of PARP-1 at the site of DNA damage. These data improve our understanding of recruitment of BER proteins to sites of DNA damage and provide evidence for a role of XRCC1 in the organization of BER into multiprotein complexes of different sizes. Environ. Mol. Mutagen. 2011. © 2011 Wiley-Liss, Inc.
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spelling pubmed-32299892011-12-05 XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage Hanssen-Bauer, Audun Solvang-Garten, Karin Sundheim, Ottar Peña-Diaz, Javier Andersen, Sonja Slupphaug, Geir Krokan, Hans E Wilson, David M Akbari, Mansour Otterlei, Marit Environ Mol Mutagen Research Article XRCC1 is a scaffold protein capable of interacting with several DNA repair proteins. Here we provide evidence for the presence of XRCC1 in different complexes of sizes from 200 to 1500 kDa, and we show that immunoprecipitates using XRCC1 as bait are capable of complete repair of AP sites via both short patch (SP) and long patch (LP) base excision repair (BER). We show that POLβ and PNK colocalize with XRCC1 in replication foci and that POLβ and PNK, but not PCNA, colocalize with constitutively present XRCC1-foci as well as damage-induced foci when low doses of a DNA-damaging agent are applied. We demonstrate that the laser dose used for introducing DNA damage determines the repertoire of DNA repair proteins recruited. Furthermore, we demonstrate that recruitment of POLβ and PNK to regions irradiated with low laser dose requires XRCC1 and that inhibition of PARylation by PARP-inhibitors only slightly reduces the recruitment of XRCC1, PNK, or POLβ to sites of DNA damage. Recruitment of PCNA and FEN-1 requires higher doses of irradiation and is enhanced by XRCC1, as well as by accumulation of PARP-1 at the site of DNA damage. These data improve our understanding of recruitment of BER proteins to sites of DNA damage and provide evidence for a role of XRCC1 in the organization of BER into multiprotein complexes of different sizes. Environ. Mol. Mutagen. 2011. © 2011 Wiley-Liss, Inc. Wiley Subscription Services, Inc., A Wiley Company 2011-10 2011-07-22 /pmc/articles/PMC3229989/ /pubmed/21786338 http://dx.doi.org/10.1002/em.20663 Text en Copyright © 2011 Wiley-Liss, Inc., A Wiley Company http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Research Article
Hanssen-Bauer, Audun
Solvang-Garten, Karin
Sundheim, Ottar
Peña-Diaz, Javier
Andersen, Sonja
Slupphaug, Geir
Krokan, Hans E
Wilson, David M
Akbari, Mansour
Otterlei, Marit
XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title_full XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title_fullStr XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title_full_unstemmed XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title_short XRCC1 Coordinates Disparate Responses and Multiprotein Repair Complexes Depending on the Nature and Context of the DNA Damage
title_sort xrcc1 coordinates disparate responses and multiprotein repair complexes depending on the nature and context of the dna damage
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3229989/
https://www.ncbi.nlm.nih.gov/pubmed/21786338
http://dx.doi.org/10.1002/em.20663
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