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Structure?activity relationship and in vitro inhibition of human cytochrome CYP2A6 and CYP2A13 by flavonoids

机译:结构α活性关系和体外CYP2A6和FYP2A13的体外抑制黄酮类化合物

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Cigarette smoking is one of the major risk factors of various diseases including respiratory diseases and lung cancer. While the liver-specific CYP2A6 is associated with the nicotine clearance and smoking addiction, the metabolic activation of the tobacco-specific nitrosamine by lung-specific CYP2A13 can lead to lung tumorigenesis. It has been reported that inhibition of CYP2A6 and CYP2A13 enzymes by flavonoids constituents could be an aids in smoking cessation. This study demonstrates the inhibition activity of kaempferol and myricetin and the structure?function relationship of these two flavonoids and previously isolated flavonoids from Vernonia cinerea and Pluchea indica against both enzymes. Kaempferol could inhibit CYP2A6 with K-ic value of 1.77???0.47 ?M while inhibit CYP2A13 with K-ic value of 0.12???0.01 ?M. Myricetin could inhibit CYP2A6 with K-ic value of 4.06???0.52 ?M while inhibit CYP2A13 with K-ic value of 1.88???0.03 ?M. Molecular docking indicated that CYP2A13 enzyme has strong hydrophobic interaction with ring B of flavonoids compared to CYP2A6 enzyme. The presence of the hydroxyl group at C3 position of ring C and the hydroxyl group at C5? of ring B affected inhibitory activity on both enzymes.
机译:吸烟是各种疾病的主要危险因素之一,包括呼吸系统疾病和肺癌。虽然肝脏特异性CYP2A6与尼古丁间隙和吸烟成瘾有关,但是肺部特异性CYP2A13的烟草特异性亚硝胺的代谢活化可以导致肺肿瘤鉴定。据报道,黄酮类化合物的CYP2A6和CYP2A13酶的抑制可能是吸烟的艾滋病。该研究证明了kaempferol和Myricetin的抑制活性和结构?这些两种黄酮类化合物的功能关系和预先分离的来自vernonia cinerea和pluchea indica对两种酶的蛋白。 Kaempferol可以抑制CYP2A6的K-IC值为1.77 ???0.47Ωm,而抑制CYP2A13,K-IC值为0.12≤0.01Ωm。 Myricetin可以抑制CYP2A6,K-IC值为4.06 ???0.52Ωm,而抑制CYP2A13,K-IC值为1.88 ???0.03Ωm。分子对接表明,与CYP2A6酶相比,CYP2A13酶与黄酮族环族的强疏水相互作用。在C3环C和C5的羟基的C3位置存在羟基的存在?环B对两种酶的抑制活性。

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