Abstract

The long-term objective of this project is to develop molecular biomarker strategies for alkylanilines that are based on DMA and protein adducts and reveal exposure and biologically effective dose in people. Alkylanilines are a class of aromatic amines that have been linked to a variety of health outcomes, including bladder cancer in humans. Present understanding of their mechanisms of action is imperfect but indicates that their toxic properties may be considerably greater in terms of both potency and variety than currently recognized. Moreover, as this project has previously discovered, human exposure to alkylanilines is nearly universal and is associated with atmospheric contamination.
The specific aims are to characterize the genotoxicity of the reactive metabolites of alkylanilines, to identify the DNA adducts that the metabolites produce, to determine the role of phenolic metabolites in generating oxidative stress, to assess exposure through hemoglobin adducts in selected populations and relate the biomarker-based exposure assessment with ambient air concentration measurements, and to develop urinary biomarkers to assess the effects of chemointerventions. Accelerator mass spectrometry will be used to determine the fate and transport of C-14 labeled alkylanilines in experimental systems used to characterize metabolism, biomarker formation, and mechanisms of action. State-of-the-art conventional mass spectrometry will be the principal means of chemical structure identification and development of methods for quantitative analysis of biomarkers. This project is designed to develop the advanced exposure assessment methods needed to discern hazards for human populations where ambient exposure levels are low, but the toxicologic hazards of the exposures remain high. Application of the biomarker methods will enable studies that have the power to assess the importance of prevalent ambient exposures to human health. The biomarker methods developed in this project will also enable studies that can assess the effects of chemointervention on human health risk.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Program Projects (P01)
Project #
5P01ES006052-16
Application #
7849773
Study Section
Special Emphasis Panel (ZES1)
Project Start
Project End
Budget Start
2009-06-01
Budget End
2010-05-31
Support Year
16
Fiscal Year
2009
Total Cost
$489,408
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Chen, Taoyang; Qian, Gengsun; Fan, Chunsun et al. (2018) Qidong hepatitis B virus infection cohort: a 25-year prospective study in high risk area of primary liver cancer. Hepatoma Res 4:
Yang, Li; Palliyaguru, Dushani L; Kensler, Thomas W (2016) Frugal chemoprevention: targeting Nrf2 with foods rich in sulforaphane. Semin Oncol 43:146-153
Watson, Sinead; Chen, Gaoyun; Sylla, Abdoulaye et al. (2016) Dietary exposure to aflatoxin and micronutrient status among young children from Guinea. Mol Nutr Food Res 60:511-8
Ravindra, Kodihalli C; Trudel, Laura J; Wishnok, John S et al. (2016) Hydroxyphenylation of Histone Lysines: Post-translational Modification by Quinone Imines. ACS Chem Biol 11:1230-7
Chao, Ming-Wei; Erkekoglu, P?nar; Tseng, Chia-Yi et al. (2015) Protective effects of ascorbic acid against the genetic and epigenetic alterations induced by 3,5-dimethylaminophenol in AA8 cells. J Appl Toxicol 35:466-77
Techapiesancharoenkij, Nirachara; Fiala, Jeannette L A; Navasumrit, Panida et al. (2015) Sulforaphane, a cancer chemopreventive agent, induces pathways associated with membrane biosynthesis in response to tissue damage by aflatoxin B1. Toxicol Appl Pharmacol 282:52-60
Shirima, Candida P; Kimanya, Martin E; Routledge, Michael N et al. (2015) A prospective study of growth and biomarkers of exposure to aflatoxin and fumonisin during early childhood in Tanzania. Environ Health Perspect 123:173-8
Hernandez-Vargas, Hector; Castelino, Jovita; Silver, Matt J et al. (2015) Exposure to aflatoxin B1 in utero is associated with DNA methylation in white blood cells of infants in The Gambia. Int J Epidemiol 44:1238-48
Chawanthayatham, Supawadee; Thiantanawat, Apinya; Egner, Patricia A et al. (2015) Prenatal exposure of mice to the human liver carcinogen aflatoxin B1 reveals a critical window of susceptibility to genetic change. Int J Cancer 136:1254-62
Castelino, Jovita M; Routledge, Michael N; Wilson, Shona et al. (2015) Aflatoxin exposure is inversely associated with IGF1 and IGFBP3 levels in vitro and in Kenyan schoolchildren. Mol Nutr Food Res 59:574-81

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