Abstract

The objectives of this continuation grant are to characterize the molecular, cellular and biochemical processes of genotoxicity in human kidney and skin epithelial cells. Specifically we will address the hypotheses that DNA repair plays a critical role in protecting human cells from the cytotoxic, mutagenic and carcinogenic effects of environmental agents. Over the past 5 years we have extensively studied the processes responsible for repairing premutagenic/procarcinogenic O6-alkylguanine (O6- alkylGua), O4-alkylthymine (O4-alkylThy) and pyrimidine dimers in cell-free extracts and cell cultures derived from human kidney and skin. These studies have provided new insights into repair activity in tissue and cultured cell populations. With the emergence of molecular and cellular techniques, we are now beginning to focus on the organ, cell and gene specific responses to genotoxin exposure. Two organs, human kidney and skin, of differing activity for repairing O6-alkylGua, will help determine the organ specific responses to genotoxins. Within these 2 tissue and in cells cultured from the tissues, in situ hybridization techniques are beginning to identify, in vivo, the cellular diversity of the O6-methylGua- DNA methyltransferase (O6-MT) mRNA. This is especially important since the O6-MT is consumed during the repair of the O6-alkylGua adduct. Thus this system should establish the organ and cell specific susceptibility to genotoxins. Once the distribution of DNA repair in the various cell types of the kidney and skin tissue is established, the nature and spectra of mutations induced by O6-EthylGua and O4-EthylThy and modified by DNA repair will be determined in these cell types cultured from these organs. The mutational analyses will utilize the well characterized coding sequence of the HPRT gene. These studies will lead to a better understanding of the molecular mechanisms of DNA repair in genotoxicity and its relationship to the organ and cell specific sensitivity to the cytotoxic, mutagenic and carcinogenic effects of alkylating agents. Thus, the studies of this renewal grant application are designed to provide new information and insights into those pivotal questions relating alkylation of DNA and DNA repair processes to human genotoxicity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES003101-12
Application #
2153221
Study Section
Toxicology Subcommittee 2 (TOX)
Project Start
1983-06-20
Project End
1997-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
12
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Ohio State University
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
098987217
City
Columbus
State
OH
Country
United States
Zip Code
43210

  Publications

Tong, H H; Park, J H; Brady, T et al. (1997) Molecular characterization of mutations in the hprt gene of normal human skin keratinocytes treated with N-ethyl-N-nitrosourea: influence of O6-alkylguanine alkyltransferase. Environ Mol Mutagen 29:168-79
Wani, G; Wani, A A; D'Ambrosio, S M (1992) In situ hybridization of human kidney tissue reveals cell-type-specific expression of the O6-methylguanine-DNA methyltransferase gene. Carcinogenesis 13:463-8
Gibson-D'Ambrosio, R E; D'Ambrosio, S M (1992) Long-term culture of normal human kidney glomerular cells. In Vitro Cell Dev Biol 28A:471-4
D'Ambrosio, S M; Wani, G; Samuel, M et al. (1990) Repair of O6-methylguanine damage in normal human tissues. Basic Life Sci 53:397-416
Wani, A A; Wani, G; D'Ambrosio, S M (1990) A human DNA repair activity specific for O4-ethylthymine: identification and partial characterization. Carcinogenesis 11:1419-24
Wani, A A; Wani, G; D'Ambrosio, S M (1990) Repair of O4-alkylthymine damage in human cells. Basic Life Sci 53:417-35
Wani, G; Wani, A A; Gibson-D'Ambrosio, R et al. (1989) Absence of DNA damage-mediated induction of human methyltransferase specific for precarcinogenic O6-methylguanine. Teratog Carcinog Mutagen 9:259-72
Milo, G E; D'Ambrosio, S; Kun, E (1989) Benzamide prevention of ultraviolet radiation-induced transformation as measured by anchorage-independent growth and the absence of correlation with thymidine dimer formation and DNA repair. Teratog Carcinog Mutagen 9:167-76
Wani, A A; D'Ambrosio, S M; Alvi, N K (1987) Quantitation of pyrimidine dimers by immunoslot blot following sublethal UV-irradiation of human cells. Photochem Photobiol 46:477-82
Chang, C C; Trosko, J E; el-Fouly, M H et al. (1987) Contact insensitivity of a subpopulation of normal human fetal kidney epithelial cells and of human carcinoma cell lines. Cancer Res 47:1634-45

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