Computational study of mutagen X

Authors
Cho, SJ
Issue Date
2003-06-20
Publisher
KOREAN CHEMICAL SOC
Citation
BULLETIN OF THE KOREAN CHEMICAL SOCIETY, v.24, no.6, pp.731 - 732
Abstract
Mutagen X (MX), 3-chloro-4-(dichloromethyl)-5-hydroxy-2(5H)-furanone is one of the most potent directing acting mutagen ever tested in SAL TA100 assay. Although MX analogues have been synthesized, tested for mutagenicity and modeled by structure-activity relationship (SAR) methods, the mechanism of interaction of these compounds with DNA to produce their remarkable mutagenic potency remains unresolved. MX exists as an equilibrium mixture of both ring and open form in water. This equilibrium is very fast for Ames test. Because the mixture is not separable by experimental methods, it is not clear which one is really responsible for the observed mutagenicity. There have been many debates that which one is really responsible for the observed mutagenicity. We used ab initio methods for the MX analogues. It seems both ring and open form could react with DNA bases as electrophiles. However, every open form has consistently lower LUMO energy than corresponding ring form. It is reasonable to assume that the major reaction will go through via open form for MX analogues. This suggest that the open form is more likely really mutagenic.
Keywords
TYPHIMURIUM TA100 MUTAGENICITY; POTENT BACTERIAL MUTAGEN; CHLORINE-TREATED WATER; HYDROXYL GROUP; MX COMPOUNDS; 3-CHLORO-4-(DICHLOROMETHYL)-5-HYDROXY-2(5H)-FURANONE MX; MUCOCHLORIC ACID; STEPWISE REMOVAL; SALMONELLA; IDENTIFICATION; TYPHIMURIUM TA100 MUTAGENICITY; POTENT BACTERIAL MUTAGEN; CHLORINE-TREATED WATER; HYDROXYL GROUP; MX COMPOUNDS; 3-CHLORO-4-(DICHLOROMETHYL)-5-HYDROXY-2(5H)-FURANONE MX; MUCOCHLORIC ACID; STEPWISE REMOVAL; SALMONELLA; IDENTIFICATION; mutagen X; mutagenicity; SAR; ab initio; molecular modeling
ISSN
0253-2964
URI
https://pubs.kist.re.kr/handle/201004/138457
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KIST Article > 2003
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