Structure, Conformations, and Repair of DNA Adducts from Dibenzo[a,l]pyrene: 32P-Postlabeling and Fluorescence Studies
- 13 May 1998
- journal article
- research article
- Published by American Chemical Society (ACS) in Chemical Research in Toxicology
- Vol. 11 (6) , 674-685
- https://doi.org/10.1021/tx970232k
Abstract
The nature of stable DNA adducts derived from the very potent carcinogen dibenzo[a,l]pyrene (DB[a,l]P) in the presence of rat liver microsomes in vitro and in mouse skin in vivo has been studied using 32P-postlabeling and laser-based fluorescence techniques. Analysis of DB[a,l]P−DNA adducts via 32P-postlabeling has been obtained by comparison of the adduct patterns to those obtained from reactions of synthetic (±)-anti-, (+)-anti-, (−)-anti-, and (±)-syn-DB[a,l]P-11,12-diol 13,14-epoxide (DB[a,l]PDE) with single nucleotides and calf thymus DNA. anti-DB[a,l]PDE−dA adducts derived from the (−)-enantiomer are the major adducts formed in calf thymus DNA and in mouse skin DNA. The ratio of deoxyadenosine to deoxyguanosine modification is approximately 2:1 in mouse skin exposed to DB[a,l]P; activation by rat liver microsomes leads to a similar profile of adducts but with two additional spots. The conformations of DB[a,l]P adducts in native DNA, as well as the possibility of conformation-dependent repair, have been explored by low-temperature fluorescence spectroscopy. These studies have been performed using polynucleotides and calf thymus DNA reacted in vitro with DB[a,l]PDE and native DNA from mouse epidermis exposed to DB[a,l]P. The results show that adducts are heterogeneous, possess different structures, and adopt different conformations. External, external but base-stacked and intercalated adduct conformations are observed in calf thymus DNA and in mouse skin DNA samples. Differences in adduct repair rates are also revealed; namely, the analysis of mouse skin DNA samples obtained at 24 and 48 h after exposure to DB[a,l]P clearly shows that external adducts are repaired more efficiently than intercalated adducts. These results, taken together with those for B[a]P−DNA adducts [Suh et al. (1995) Carcinogenesis 16, 2561−2569], indicate that the repair of DNA damage resulting from PAH diol epoxides is conformation-dependent.Keywords
This publication has 6 references indexed in Scilit:
- Conformational studies of the (+)-trans, (−)-trans, (+)-cis, and (−)-cis adducts of anti-benzo[a]pyrene diolepoxide to N2-dG in duplex oligonucleotides using polyacrylamide gel electrophoresis and low-temperature fluorescence spectroscopyBiophysical Chemistry, 1995
- Tumorigenicity in newborn mice of fjord region and other sterically hindered diol epoxides of benzo[g]chrysene, dibenzo[a, l]pyrene (dibenzo[def, p]chrysene), 4H-cyclopenta[def]chrysene and fluorantheneCarcinogenesis: Integrative Cancer Research, 1995
- Stereoselective activation of dibenzo[a,l]pyrene to (—)-anti(11R, 12S, 13S, 14R)- and (+)-syn(11S, 12R, 13S, 14R)- 11, 12-diol-13, 14-epoxides which bind extensively to deoxyadenosine residues of DNA in the human mammary carcinoma cell line MCF-7Carcinogenesis: Integrative Cancer Research, 1995
- Synthesis and tumor-initiating activity in mouse skin of dibenzo[a,l]pyrene syn- and anti-fjord-region diolepoxidesCarcinogenesis: Integrative Cancer Research, 1994
- Solution Conformation of the (+)-cis-anti-[BP]dG Adduct Opposite a Deletion Site in a DNA Duplex: Intercalation of the Covalently Attached Benzo[a]pyrene into the Helix with Base Displacement of the Modified Deoxyguanosine into the Minor GrooveBiochemistry, 1994
- AP sites are not significantly involved in mutagenesis by the (+)-anti diol epoxide of benzo[a]pyrene: The complexicity of its mutagenic specificity is likely to arise from adduct conformational polymorphismBiochemistry, 1993