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The Balance of Beneficial and Deleterious Health Effects of Quinones: A Case Study of the Chemical Properties of Genistein and Estrone Quinones

机译:醌对人体有益和有害健康之间的平衡:染料木黄酮和雌酮醌的化学性质研究

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摘要

Substances containing a phenolic moiety are often metabolized to quinones whose high reactivity makes them difficult to study. Some of these precursors have clear health benefits, and some quinones themselves are used in cancer therapy, whereas others are deleterious. For example, dietary intake of phytoestrogen, genistein (Gen), seems to play a preventive role in breast cancer (BC) whereas prolonged exposure to chemically similar mammalian estrogens is clearly associated with elevated incidence of BC. Although both can be metabolized to reactive quinones, the catechol estrogen quinones (CEQs) modify DNA by redox cycling and/or depurination via a Michael addition. Here, we report an investigation of the chemical reactivity of Gen and estrone quinones to determine the chemical differences in of these two biologically important molecules. The catechol genistein quinone (CGenQ), has a half life of 4 ± 1 s under physiological condition, as determined by glutathione trapping. It disappears by reacting with H2O to give a dihydrate, CGenQ·(H2O)2, whose structure was proved by NMR. Under reductive conditions, CGenQ·(H2O)2 is readily reduced to reform the catechol genistein (CGen). This reversible oxidation of CGen to CGenQ and the prompt moderation of its reactivity by hydration to CGenQ·(H2O)2 effectively moderates any redox cycling or depurination reaction of CGenQ with DNA. Catechol estrogen quinones, on the other hand, are sufficiently long-lived that they can damage DNA via a Michael addition or by redox cycling. Although the reactivity of CEQ in a nonaqueous solvent is similar to that of CGenQ, its reactivity in aqueous media with the free Ade base is more than 600 times that of CGenQ. These results suggest that rapid hydration of a quinone can moderate its reactivity toward biomolecules, allowing them to express, for example, estrogen-like properties without exhibiting the deleterious properties of redox cycling or directly damaging DNA via depurination reactions.
机译:含有酚部分的物质通常被代谢为醌,其高反应活性使它们难以研究。这些前体中的一些具有明显的健康益处,一些醌本身用于癌症治疗,而另一些则有害。例如,饮食中摄入的植物雌激素染料木黄酮(Genistein)似乎在乳腺癌(BC)中起预防作用,而长时间接触化学相似的哺乳动物雌激素显然与BC发病率升高有关。尽管两者都可以代谢为反应性醌,但儿茶酚雌激素醌(CEQ)通过氧化还原循环和/或通过迈克尔加成进行脱嘌呤来修饰DNA。在这里,我们报告Gen和雌酮醌化学反应的调查,以确定这两个生物学上重要分子的化学差异。邻苯二酚金雀异黄素醌(CGenQ)在生理条件下的半衰期为4±1 s(通过谷胱甘肽捕获法测定)。通过与H2O反应消失,生成二水合物CGenQ·(H2O)2,其结构已通过NMR证实。在还原条件下,CGenQ·(H2O)2容易还原以重整儿茶酚染料木黄酮(CGen)。 CGen向CGenQ的可逆氧化,以及通过水合为CGenQ·(H2O)2而迅速降低其反应性,有效地缓解了CGenQ与DNA的任何氧化还原循环或去纯化反应。另一方面,儿茶酚雌激素醌寿命足够长,它们可以通过迈克尔加成反应或氧化还原循环来破坏DNA。尽管CEQ在非水溶剂中的反应性与CGenQ相似,但其在水性介质中与游离Ade碱的反应性是CGenQ的600倍以上。这些结果表明,醌的快速水合可减轻其对生物分子的反应性,从而使其表现出类似雌激素的特性,而不会表现出氧化还原循环的有害特性或通过去纯化反应直接破坏DNA。

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