Abstract

The objectives of this project are: (1) to evaluate age- and dosing-related changes in pharmacokinetics, biochemical markers, liver cell proliferation, and histopathology in male Fischer 344 chronically (up to 2 yrs) exposed to low levels of a chemical mixture of 7 organic and inorganic groundwater pollutants (arsenic, benzene, chloroform, chromium, lead, phenol, trichloroethylene); (2) to explore pharmacokinetic modeling of chemical mixtures; (3) to incorporate time-course information on biochemical markers, cell proliferation and histopathology into pharmacokinetic and pharmacodynamic modeling. In all of the studies proposed, pharmacokinetics refer to physiologically based pharmacokinetic modeling, using a simple and noninvasive method (gas uptake technique) to assess the kinetics of trichloroethylene, a model chemical and a top groundwater pollutant, with or without the modulation of drinking water exposure of the chemical mixture. Blood and liver levels of lead and chromium, two components of the mixture, will be analyzed and the results will be utilized for possible pharmacokinetic modeling. Biochemical markers to be measured include glutathione (GSH) content, cytochrome P450 content and activity, glutathione S-transferase activity and cysteine beta-lyase activity in liver and kidney. Liver cell proliferation rate will be investigated at various time points in parallel with the 2-year study. Clinical and histopathology will be conducted such that comparative evaluations may be made among rats (this project) and rabbits (Project 3). Because of logistic restrictions, the experiments in this project will be divided into two phases. Phase I studies which will be conducted in the first 6 mos involve the time-course (1 and 4 days, 1 and 2 wks) investigation of pharmacokinetics, biochemical markers, and cell proliferation (liver). It is during these short-term studies the exploration for the endpoint(s) for future studies on teasing out the possible additivity or synergism or antagonism by component chemicals responsible for the toxic responses will be effected. Phase II which will be initiated after the completion of Phase I studies, similarly, will be time-course I1, 3, 6, 12, 18, 24 mos) investigation of pharmacokinetics, biochemical markers, cell proliferation (liver) plus clinical and histopathology.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Hazardous Substances Basic Research Grants Program (NIEHS) (P42)
Project #
5P42ES005949-03
Application #
3755272
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Colorado State University-Fort Collins
Department
Type
DUNS #
112617480
City
Fort Collins
State
CO
Country
United States
Zip Code
80523

  Publications

Veeramachaneni, D N Rao (2012) Ultrastructural evaluation of semen to assess effects of exposure to toxicants. Toxicol Pathol 40:382-90
Zimbron, Julio A; Reardon, Kenneth F (2011) Continuous combined Fenton's oxidation and biodegradation for the treatment of pentachlorophenol-contaminated water. Water Res 45:5705-14
Lee, Sun Ku; Hamer, Dwayne; Bedwell, Cathy L et al. (2009) Effect of PCBs on the lactational transfer of methyl mercury in mice: PBPK modeling. Environ Toxicol Pharmacol 27:75-83
Veeramachaneni, D N Rao (2008) Impact of environmental pollutants on the male: effects on germ cell differentiation. Anim Reprod Sci 105:144-57
Yang, Raymond S H; Dennison, James E (2007) Initial analyses of the relationship between ""Thresholds"" of toxicity for individual chemicals and ""Interaction Thresholds"" for chemical mixtures. Toxicol Appl Pharmacol 223:133-8
Belfiore, Carol J; Yang, Raymond S H; Chubb, Laura S et al. (2007) Hepatic sequestration of chlordecone and hexafluoroacetone evaluated by pharmacokinetic modeling. Toxicology 234:59-72
Lee, Sun Ku; Ou, Ying C; Andersen, Melvin E et al. (2007) A physiologically based pharmacokinetic model for lactational transfer of PCB 153 with or without PCB 126 in mice. Arch Toxicol 81:101-11
Zimbron, Julio A; Reardon, Kenneth F (2005) Hydroxyl free radical reactivity toward aqueous chlorinated phenols. Water Res 39:865-9
Chubb, Laura S; Andersen, Melvin E; Broccardo, Carolyn J et al. (2004) Regional induction of CYP1A1 in rat liver following treatment with mixtures of PCB 126 and PCB 153. Toxicol Pathol 32:467-73
Bae, Dong-Soon; Handa, Robert J; Yang, Raymond S H et al. (2003) Gene expression patterns as potential molecular biomarkers for malignant transformation in human keratinocytes treated with MNNG, arsenic, or a metal mixture. Toxicol Sci 74:32-42

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