Abstract

Contamination of our environment with organic pollutants generates serious contemporary public health problems. A major mechanism contributing to human disease involves toxic activation of organic pollutants after they enter the body. This process features oxidation of the pollutants catalyzed by cytochrome P450 enzymes in the liver, followed by damage of genetic material (i. e. DNA) by activated pollutants. Chemicals activated in this way include styrene, benzo[a]pyrene, and many others. Organohalide pollutants such as chlorodioxins and polychlorinated biphenyls are not as easily activated, but they elevate cytochrome P450 levels in the body, promoting the chance of metabolic dysfunction. For example, excess cytochrome P450 can catalyze undesirable oxidation of membrane lipids or other functional biomolecules. These oxidation products may also damage DNA. Knowledge of molecular details and enzyme specificities of toxic activation and DNA damage can lead to new ways to treat pollutant-caused diseases and improve the future health of our citizens. The broad long-term goals of this project are to develop new, thin-film electrode coatings for in-vitro studies of DNA damage by activated pollutants, and as simple toxicity screens for new chemicals activated by enzymes.
Specific aims i nclude developing systems based on electrode-driven enzyme-catalyzed pollutant activation, using enzymes and DNA in thin films prepared by casting and layer-by-layer growth. Systems will be designed to mimic natural toxic activation of pollutants and DNA damage. Enzymes used will proceed from a model heme protein, myoglobin, to bacterial cytochrome P450, to human cytochromes P450. Natural redox partners of the cytochrome P450 enzymes may be included in the films if needed. Target devices will employ electron injection from electrodes to drive a series of events involving enzyme-catalyzed pollutant activation, and damage of DNA by the activated pollutants. Electrochemical and chromatographic analyses will be used to monitor DNA damage in the films. Validation of toxic screen assays will be done by correlating DNA damage rates for known toxic pollutants with mutagenicity and carcinogenicity data bases. In addition to new devices for screening toxic chemicals, this project will result in relatively simple probes for establishing detailed substrate specificities of human cytochrome P450s, the relative distribution of which may be important in individual susceptibility to pollutant-caused disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES003154-17
Application #
6138100
Study Section
Metallobiochemistry Study Section (BMT)
Program Officer
Thompson, Claudia L
Project Start
1983-03-01
Project End
2003-12-31
Budget Start
2000-01-01
Budget End
2000-12-31
Support Year
17
Fiscal Year
2000
Total Cost
$191,078
Indirect Cost

  Institution

Name
University of Connecticut
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
City
Storrs-Mansfield
State
CT
Country
United States
Zip Code
06269

  Publications

Rusling, James F (2018) Developing Microfluidic Sensing Devices Using 3D Printing. ACS Sens 3:522-526
Chang, Zheng; Yang, Yue; He, Jie et al. (2018) Gold nanocatalysts supported on carbon for electrocatalytic oxidation of organic molecules including guanines in DNA. Dalton Trans 47:14139-14152
Malla, Spundana; Kadimisetty, Karteek; Jiang, Di et al. (2018) Pathways of Metabolite-Related Damage to a Synthetic p53 Gene Exon 7 Oligonucleotide Using Magnetic Enzyme Bioreactor Beads and LC-MS/MS Sequencing. Biochemistry 57:3883-3893
Hvastkovs, Eli G; Rusling, James F (2017) Modern Approaches to Chemical Toxicity Screening. Curr Opin Electrochem 3:18-22
Bist, Itti; Bhakta, Snehasis; Jiang, Di et al. (2017) Evaluating Metabolite-Related DNA Oxidation and Adduct Damage from Aryl Amines Using a Microfluidic ECL Array. Anal Chem 89:12441-12449
Bist, Itti; Bano, Kiran; Rusling, James F (2017) Screening Genotoxicity Chemistry with Microfluidic Electrochemiluminescent Arrays. Sensors (Basel) 17:
Kadimisetty, Karteek; Malla, Spundana; Rusling, James F (2017) Automated 3-D Printed Arrays to Evaluate Genotoxic Chemistry: E-Cigarettes and Water Samples. ACS Sens 2:670-678
Jiang, Di; Malla, Spundana; Fu, You-Jun et al. (2017) Direct LC-MS/MS Detection of Guanine Oxidations in Exon 7 of the p53 Tumor Suppressor Gene. Anal Chem 89:12872-12879
Mosa, Islam M; Pattammattel, Ajith; Kadimisetty, Karteek et al. (2017) Ultrathin Graphene-Protein Supercapacitors for Miniaturized Bioelectronics. Adv Energy Mater 7:
Malla, Spundana; Kadimisetty, Karteek; Fu, You-Jun et al. (2017) Methyl-Cytosine-Driven Structural Changes Enhance Adduction Kinetics of an Exon 7 fragment of the p53 Gene. Sci Rep 7:40890

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