Abstract

The genetic effects of metal compounds have been difficult to study. Altering exposure protocols and genetic endpoints enabled this laboratory to detect the mutagenicity of some metal compounds. Other compounds, while not mutagenic per se, could enhance the mutagenicity of ultraviolet light (UV). This proposal will address the mechanisms for these two phenomena. Since the effects of chromium and nickel on DNA have been well studied by others, the focus of this project will be to elucidate the effects on DNA by mutagenic or comutagenic compounds of copper, lead, iron, manganese, arsenic, molybdenum, tungsten and zinc (in order of priority) either alone or with UV irradiation. The ability of metal compounds to damage DNA, or to enhance UV- induced damage, will be studied using sequencing gel techniques. Sites of strand breaks, alkali-lability, DNA repair enzyme recognition and polymerase inhibition will be determined on at least one restriction fragment within the E. coli gpt coding sequence. Preliminary data suggests that in some cases (e.g. Cu2+), the comutagenic effect may be mediated by hydroxyl radicals formed by a Fenton reaction causing random strand breaks which can be inhibited by KI. In cases where specific sites of damage are identified, the nature of the lesions will be determined by physical chemical means. The effects on cellular DNA will be studied for those metal compounds which do not damage plasmid DNA or enhance UV-induced damage, using alkaline elution techniques. The ability of metal compounds to damage DNA will also be studied by genetic means. The plasmid pSV2 gpt will be treated, and the transfection frequency and mutation frequency (to gpt-) will be determined using Chinese hamster V79 hprt- cells as a host. In addition, mutagenesis of a stable V79 (gpt) transfectant will be carried out, and the frequency of large deletions will be measured. It is expected that mutagenesis at this locus will be more sensitive to multi-locus deletions (known to be caused by oxidative damage) compared to the endogenous hprt locus. Using the same genetic target (E. coli gpt) for the studies on DNA damage sites and mutagenesis will ultimately enable the determination of the mutagenic consequences of specific types of damage.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA029258-07A1
Application #
3168599
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1980-12-01
Project End
1993-03-31
Budget Start
1988-04-01
Budget End
1989-03-31
Support Year
7
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Type
Schools of Medicine
DUNS #
004514360
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Klein, C B; Su, L; Rossman, T G et al. (1994) Transgenic gpt+ V79 cell lines differ in their mutagenic response to clastogens. Mutat Res 304:217-28
Wang, Z; Hou, G; Rossman, T G (1994) Induction of arsenite tolerance and thermotolerance by arsenite occur by different mechanisms. Environ Health Perspect 102 Suppl 3:97-100
Wang, Z; Rossman, T G (1994) Large-scale supercoiled plasmid preparation by acidic phenol extraction. Biotechniques 16:460-3
Goncharova, E I; Rossman, T G (1994) A role for metallothionein and zinc in spontaneous mutagenesis. Cancer Res 54:5318-23
Wang, Z; Rossman, T G (1993) Stable and inducible arsenite resistance in Chinese hamster cells. Toxicol Appl Pharmacol 118:80-6
Lee, Y W; Pons, C; Tummolo, D M et al. (1993) Mutagenicity of soluble and insoluble nickel compounds at the gpt locus in G12 Chinese hamster cells. Environ Mol Mutagen 21:365-71
Rossman, T G; Roy, N K; Lin, W C (1992) Is cadmium genotoxic? IARC Sci Publ :367-75
Roy, N K; Rossman, T G (1992) Mutagenesis and comutagenesis by lead compounds. Mutat Res 298:97-103
Rossman, T G; Wolosin, D (1992) Differential susceptibility to carcinogen-induced amplification of SV40 and dhfr sequences in SV40-transformed human keratinocytes. Mol Carcinog 6:203-13
Li, J H; Rossman, T G (1991) Comutagenesis of sodium arsenite with ultraviolet radiation in Chinese hamster V79 cells. Biol Met 4:197-200

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