Mutagenic potency of food-derived heterocyclic amines

The understanding of mutagenic potency has been primarily approached using "quantitative structure-activity relationships" (QSAR). Often this method allows the prediction of mutagenic potency of the compound based on its structure. But it does not give the underlying reason why the mutagen...

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Published inMutation Research-Fundamental and Molecular Mechanisms of Mutagenesis Vol. 616; no. 1-2; pp. 90 - 94
Main Authors Felton, James S, Knize, Mark G, Wu, Rebekah W, Colvin, Michael E, Hatch, Frederick T, Malfatti, Michael A
Format Journal Article
LanguageEnglish
Published Netherlands 01.03.2007
Subjects
Amines - adverse effects
Computer Simulation
DNA Repair
Food - adverse effects
Heterocyclic Compounds - adverse effects
Imidazoles - adverse effects
Isomerism
Models, Biological
Molecular Structure
Mutagens
Quantitative Structure-Activity Relationship
Salmonella
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Summary:The understanding of mutagenic potency has been primarily approached using "quantitative structure-activity relationships" (QSAR). Often this method allows the prediction of mutagenic potency of the compound based on its structure. But it does not give the underlying reason why the mutagenic activities differ. We have taken a set of heterocyclic amine structures and used molecular dynamic calculations to dock these molecules into the active site of a computational model of the cytochrome P4501A2 enzyme. The calculated binding strength using Boltzman distribution constants was then compared to the QSAR value (HF/6-31G* optimized structures) and the Ames/Salmonella mutagenic potency. Further understanding will only come from knowing the complete set of mutagenic determinants. These include the nitrenium ion half-life, DNA adduct half-life, efficiency of repair of the adduct, and ultimately fixation of the mutation through cellular processes. For two isomers, PhIP and 3-Me-PhIP, we showed that for the 100-fold difference in the mutagenic potency a 5-fold difference can be accounted for by differences in the P450 oxidation. The other factor of 20 is not clearly understood but is downstream from the oxidation step. The application of QSAR (chemical characteristics) to biological principles related to mutagenesis is explored in this report.
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ISSN:0027-5107
1386-1964
0027-5107
DOI:10.1016/j.mrfmmm.2006.11.010