RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage

The Cut homeobox 1 (CUX1) gene is a target of loss-of-heterozygosity in many cancers, yet elevated CUX1 expression is frequently observed and is associated with shorter disease-free survival. The dual role of CUX1 in cancer is illustrated by the fact that most cell lines with CUX1 LOH display amplif...

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Autores principales: Ramdzan, Zubaidah M., Vadnais, Charles, Pal, Ranjana, Vandal, Guillaume, Cadieux, Chantal, Leduy, Lam, Davoudi, Sayeh, Hulea, Laura, Yao, Lu, Karnezis, Anthony N., Paquet, Marilène, Dankort, David, Nepveu, Alain
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3949673/
https://www.ncbi.nlm.nih.gov/pubmed/24618719
http://dx.doi.org/10.1371/journal.pbio.1001807
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author Ramdzan, Zubaidah M.
Vadnais, Charles
Pal, Ranjana
Vandal, Guillaume
Cadieux, Chantal
Leduy, Lam
Davoudi, Sayeh
Hulea, Laura
Yao, Lu
Karnezis, Anthony N.
Paquet, Marilène
Dankort, David
Nepveu, Alain
author_facet Ramdzan, Zubaidah M.
Vadnais, Charles
Pal, Ranjana
Vandal, Guillaume
Cadieux, Chantal
Leduy, Lam
Davoudi, Sayeh
Hulea, Laura
Yao, Lu
Karnezis, Anthony N.
Paquet, Marilène
Dankort, David
Nepveu, Alain
author_sort Ramdzan, Zubaidah M.
collection PubMed
description The Cut homeobox 1 (CUX1) gene is a target of loss-of-heterozygosity in many cancers, yet elevated CUX1 expression is frequently observed and is associated with shorter disease-free survival. The dual role of CUX1 in cancer is illustrated by the fact that most cell lines with CUX1 LOH display amplification of the remaining allele, suggesting that decreased CUX1 expression facilitates tumor development while increased CUX1 expression is needed in tumorigenic cells. Indeed, CUX1 was found in a genome-wide RNAi screen to identify synthetic lethal interactions with oncogenic RAS. Here we show that CUX1 functions in base excision repair as an ancillary factor for the 8-oxoG-DNA glycosylase, OGG1. Single cell gel electrophoresis (comet assay) reveals that Cux1(+/−) MEFs are haploinsufficient for the repair of oxidative DNA damage, whereas elevated CUX1 levels accelerate DNA repair. In vitro base excision repair assays with purified components demonstrate that CUX1 directly stimulates OGG1's enzymatic activity. Elevated reactive oxygen species (ROS) levels in cells with sustained RAS pathway activation can cause cellular senescence. We show that elevated expression of either CUX1 or OGG1 prevents RAS-induced senescence in primary cells, and that CUX1 knockdown is synthetic lethal with oncogenic RAS in human cancer cells. Elevated CUX1 expression in a transgenic mouse model enables the emergence of mammary tumors with spontaneous activating Kras mutations. We confirmed cooperation between Kras(G12V) and CUX1 in a lung tumor model. Cancer cells can overcome the antiproliferative effects of excessive DNA damage by inactivating a DNA damage response pathway such as ATM or p53 signaling. Our findings reveal an alternate mechanism to allow sustained proliferation in RAS-transformed cells through increased DNA base excision repair capability. The heightened dependency of RAS-transformed cells on base excision repair may provide a therapeutic window that could be exploited with drugs that specifically target this pathway.
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spelling pubmed-39496732014-03-12 RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage Ramdzan, Zubaidah M. Vadnais, Charles Pal, Ranjana Vandal, Guillaume Cadieux, Chantal Leduy, Lam Davoudi, Sayeh Hulea, Laura Yao, Lu Karnezis, Anthony N. Paquet, Marilène Dankort, David Nepveu, Alain PLoS Biol Research Article The Cut homeobox 1 (CUX1) gene is a target of loss-of-heterozygosity in many cancers, yet elevated CUX1 expression is frequently observed and is associated with shorter disease-free survival. The dual role of CUX1 in cancer is illustrated by the fact that most cell lines with CUX1 LOH display amplification of the remaining allele, suggesting that decreased CUX1 expression facilitates tumor development while increased CUX1 expression is needed in tumorigenic cells. Indeed, CUX1 was found in a genome-wide RNAi screen to identify synthetic lethal interactions with oncogenic RAS. Here we show that CUX1 functions in base excision repair as an ancillary factor for the 8-oxoG-DNA glycosylase, OGG1. Single cell gel electrophoresis (comet assay) reveals that Cux1(+/−) MEFs are haploinsufficient for the repair of oxidative DNA damage, whereas elevated CUX1 levels accelerate DNA repair. In vitro base excision repair assays with purified components demonstrate that CUX1 directly stimulates OGG1's enzymatic activity. Elevated reactive oxygen species (ROS) levels in cells with sustained RAS pathway activation can cause cellular senescence. We show that elevated expression of either CUX1 or OGG1 prevents RAS-induced senescence in primary cells, and that CUX1 knockdown is synthetic lethal with oncogenic RAS in human cancer cells. Elevated CUX1 expression in a transgenic mouse model enables the emergence of mammary tumors with spontaneous activating Kras mutations. We confirmed cooperation between Kras(G12V) and CUX1 in a lung tumor model. Cancer cells can overcome the antiproliferative effects of excessive DNA damage by inactivating a DNA damage response pathway such as ATM or p53 signaling. Our findings reveal an alternate mechanism to allow sustained proliferation in RAS-transformed cells through increased DNA base excision repair capability. The heightened dependency of RAS-transformed cells on base excision repair may provide a therapeutic window that could be exploited with drugs that specifically target this pathway. Public Library of Science 2014-03-11 /pmc/articles/PMC3949673/ /pubmed/24618719 http://dx.doi.org/10.1371/journal.pbio.1001807 Text en © 2014 Ramdzan et al http://creativecommons.org/licenses/by/4.0/ 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 properly credited.
spellingShingle Research Article
Ramdzan, Zubaidah M.
Vadnais, Charles
Pal, Ranjana
Vandal, Guillaume
Cadieux, Chantal
Leduy, Lam
Davoudi, Sayeh
Hulea, Laura
Yao, Lu
Karnezis, Anthony N.
Paquet, Marilène
Dankort, David
Nepveu, Alain
RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title_full RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title_fullStr RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title_full_unstemmed RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title_short RAS Transformation Requires CUX1-Dependent Repair of Oxidative DNA Damage
title_sort ras transformation requires cux1-dependent repair of oxidative dna damage
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3949673/
https://www.ncbi.nlm.nih.gov/pubmed/24618719
http://dx.doi.org/10.1371/journal.pbio.1001807
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