Identification of Novel Gene Targets and Putative Regulators of Arsenic-Associated DNA Methylation in Human Urothelial Cells and Bladder Cancer

There is strong epidemiologic evidence linking chronic exposure to inorganic arsenic (iAs) to myriad adverse health effects, including cancer of the bladder. We set out to identify DNA methylation patterns associated with arsenic and its metabolites in exfoliated urothelial cells (EUCs) that origina...

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Bibliographic Details
Published in:Chemical research in toxicology 2015-06, Vol.28 (6), p.1144-1155
Main Authors: Rager, Julia E, Tilley, Sloane K, Tulenko, Samantha E, Smeester, Lisa, Ray, Paul D, Yosim, Andrew, Currier, Jenna M, Ishida, María C, González-Horta, Maria del Carmen, Sánchez-Ramírez, Blanca, Ballinas-Casarrubias, Lourdes, Gutiérrez-Torres, Daniela S, Drobná, Zuzana, Del Razo, Luz M, García-Vargas, Gonzalo G, Kim, William Y, Zhou, Yi-Hui, Wright, Fred A, Stýblo, Miroslav, Fry, Rebecca C
Format: Article
Language:English
Subjects:
Adult
Aged
Arsenic - metabolism
Arsenic - toxicity
Cell Transformation, Neoplastic - chemically induced
DNA Methylation - drug effects
DNA Methylation - genetics
Female
Humans
Middle Aged
Urinary Bladder Neoplasms - chemically induced
Urinary Bladder Neoplasms - genetics
Urinary Bladder Neoplasms - pathology
Urothelium - cytology
Urothelium - drug effects
Young Adult
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Summary:There is strong epidemiologic evidence linking chronic exposure to inorganic arsenic (iAs) to myriad adverse health effects, including cancer of the bladder. We set out to identify DNA methylation patterns associated with arsenic and its metabolites in exfoliated urothelial cells (EUCs) that originate primarily from the urinary bladder, one of the targets of arsenic-induced carcinogenesis. Genome-wide, gene-specific promoter DNA methylation levels were assessed in EUCs from 46 residents of Chihuahua, Mexico, and the relationship was examined between promoter methylation profiles and the intracellular concentrations of total arsenic and arsenic species. A set of 49 differentially methylated genes was identified with increased promoter methylation associated with EUC tAs, iAs, and/or monomethylated As (MMAs) enriched for their roles in metabolic disease and cancer. Notably, no genes had differential methylation associated with EUC dimethylated As (DMAs), suggesting that DMAs may influence DNA methylation-mediated urothelial cell responses to a lesser extent than iAs or MMAs. Further analysis showed that 22 of the 49 arsenic-associated genes (45%) are also differentially methylated in bladder cancer tissue identified using The Cancer Genome Atlas repository. Both the arsenic- and cancer-associated genes are enriched for the binding sites of common transcription factors known to play roles in carcinogenesis, demonstrating a novel potential mechanistic link between iAs exposure and bladder cancer.
ISSN:0893-228X
1520-5010
DOI:10.1021/tx500393y