Abstract

In living cells, polycyclic aromatic hydrocarbons, a well known class of chemical carcinogens, are metabolically activated to mutagenic and tumorigenic bay-region diol epoxide derivatives. The mechanisms by which these chemicals cause cancer are not well understood. However, there is experimental evidence which indicates that these reactive molecules bind chemically to DNA, and that these lesions somehow give rise to mutations. Subtle differences in the steric orientations of the diol and epoxide groups, as well as other, seemingly small structural variations, can give rise to profound differences in the tumorigenic and mutagenic potentials of these molecules. The specific genomic DNA sequences in which these covalently bound carcinogens are located, may also be of critical importance. The objectives of this work are to characterize the type of DNA damage, and the differences in adduct conformations and surrounding DNA nucleotide sequences, caused by specific pairs of biologically active and inactive, but structurally related pairs of PAH diol epoxide molecules. The approach consists of synthesizing site-specific covalent adducts derived from the binding of these pairs of related PAH diol epoxide molecules to oligodeoxynucleotides of defined base sequence. The characteristics of these modified DNA sequences, and the perturbations of normal base pairing processes caused by the covalently bound polycyclic aromatic residues, will be studied by sensitive physico-chemical, spectroscopic, and biochemical techniques. The existence of carcinogen-base stacking interactions, solvent-exposed adduct conformations, and the formation of kinks, bends, or flexible hinge points at the binding sites will be studied. Carcinogen-modified sequences which can be synthesized in sufficiently high yields, and which have appropriate characteristics for NM studies, will be subjected to one-dimensional and two-dimensional NMR analysis. The long range objectives of this work are to elucidate those features, on a molecular level, which distinguish mutation-prone PAH diol epoxide-DNA lesions derived from biologically highly active molecules, from benign adducts, derived from inactive structurally related PAH diol epoxide derivatives. This knowledge should ultimately lead to a better understanding of the molecular basis of mutagenesis induced by this class of carcinogens and mutagens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA020851-14
Application #
3165419
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1977-08-01
Project End
1994-07-31
Budget Start
1991-08-01
Budget End
1992-07-31
Support Year
14
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

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

  Publications

Zhao, Bo; Wang, Jillian; Geacintov, Nicholas E et al. (2006) Poleta, Polzeta and Rev1 together are required for G to T transversion mutations induced by the (+)- and (-)-trans-anti-BPDE-N2-dG DNA adducts in yeast cells. Nucleic Acids Res 34:417-25
Baskunov, Vladimir B; Subach, Fedor V; Kolbanovskiy, Alexandr et al. (2005) Effects of benzo[a]pyrene-deoxyguanosine lesions on DNA methylation catalyzed by EcoRII DNA methyltransferase and on DNA cleavage effected by EcoRII restriction endonuclease. Biochemistry 44:1054-66
Wu, Min; Yan, S Frank; Tan, Jian et al. (2004) Conformational searches elucidate effects of stereochemistry on structures of deoxyadenosine covalently bound to tumorigenic metabolites of benzo[C] phenanthrene. Front Biosci 9:2807-18
Yan, Shixiang; Wu, Min; Patel, Dinshaw J et al. (2003) Simulating structural and thermodynamic properties of carcinogen-damaged DNA. Biophys J 84:2137-48
Xie, Zhongwen; Braithwaite, Elena; Guo, Dongyu et al. (2003) Mutagenesis of benzo[a]pyrene diol epoxide in yeast: requirement for DNA polymerase zeta and involvement of DNA polymerase eta. Biochemistry 42:11253-62
Huang, Xuanwei; Kolbanovskiy, Alexander; Wu, Xiaohua et al. (2003) Effects of base sequence context on translesion synthesis past a bulky (+)-trans-anti-B[a]P-N2-dG lesion catalyzed by the Y-family polymerase pol kappa. Biochemistry 42:2456-66
Rechkoblit, Olga; Zhang, Yanbin; Guo, Dongyu et al. (2002) trans-Lesion synthesis past bulky benzo[a]pyrene diol epoxide N2-dG and N6-dA lesions catalyzed by DNA bypass polymerases. J Biol Chem 277:30488-94
Huang, Xuanwei; Colgate, Katharine C; Kolbanovskiy, Aleksandr et al. (2002) Conformational changes of a benzo[a]pyrene diol epoxide-N(2)-dG adduct induced by a 5'-flanking 5-methyl-substituted cytosine in a (Me)CG double-stranded oligonucleotide sequence context. Chem Res Toxicol 15:438-44
Zhang, Yanbin; Wu, Xiaohua; Guo, Dongyu et al. (2002) Lesion bypass activities of human DNA polymerase mu. J Biol Chem 277:44582-7
Zhang, Yanbin; Wu, Xiaohua; Guo, Dongyu et al. (2002) Two-step error-prone bypass of the (+)- and (-)-trans-anti-BPDE-N2-dG adducts by human DNA polymerases eta and kappa. Mutat Res 510:23-35

Showing the most recent 10 out of 82 publications