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Molecular mechanisms of DNA damage initiated by alpha beta-unsaturated carbonyl compounds as criteria for genotoxicity and mutagenicity.

机译:由αβ-不饱和羰基化合物引发的DNA损伤的分子机制作为遗传毒性和诱变性的标准。

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摘要

alpha, beta-Unsaturated carbonyl compounds are important not only from a theoretical but also a practical standpoint. These ubiquitous compounds can interact with DNA through various mechanisms. The predominant interaction is the formation of cyclic 1,N2-deoxyguanosine adducts; 7,8-cyclic guanine adducts are also found. We have synthesized and characterized the stereoisomers of adducts formed by about 20 alpha, beta-unsaturated carbonyl compounds. The different types of adducts and the mutagenic and genotoxic response can be explained by the molecular structures of the agents. Compounds forming saturated cyclic adducts are mutagenic in S. typhimurium strain TA100 and to a lesser extent in TA1535. Substances with a leaving group at the C-3 position form unsaturated conjugated cyclic adducts and are mutagenic only in the His D3052 frameshift strains with an intact excision repair system (no urvA mutation). Metabolic epoxidation of the double bond and other metabolic activation, e.g., activation of the nitrogroups via nitroreductases, were also found to contribute to genotoxic and mutagenic activities. Our results have further elucidated the genotoxic mechanisms of these compounds; however, additional investigations are required for a complete understanding of the genotoxic activity of this class of compounds.
机译:α,β-不饱和羰基化合物不仅在理论上而且在实践上都很重要。这些无处不在的化合物可以通过各种机制与DNA相互作用。主要的相互作用是形成环1,N2-脱氧鸟苷加合物。还发现了7,8-环鸟嘌呤加合物。我们已经合成和表征了由约20个α,β-不饱和羰基化合物形成的加合物的立体异构体。加合物的不同类型以及诱变和遗传毒性反应可以通过试剂的分子结构来解释。形成饱和环状加合物的化合物在鼠伤寒沙门氏菌菌株TA100中诱变,而在TA1535中诱变程度较小。在C-3位置带有离去基团的物质形成不饱和共轭环状加合物,并且仅在具有完整切除修复系统(无urvA突变)的His D3052移码菌株中具有致突变性。还发现双键的代谢环氧化和其他代谢活化,例如经由硝基还原酶的硝基的活化,有助于遗传毒性和诱变活性。我们的结果进一步阐明了这些化合物的遗传毒性机制。但是,需要进一步研究才能完全了解这类化合物的遗传毒性。

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