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吲哚醌抗肿瘤药物:醌结构、重组人NAD(P)H:醌氧化还原酶代谢速率与体外细胞毒性之间的相关性

Indolequinone antitumor agents: correlation between quinone structure, rate of metabolism by recombinant human NAD(P)H:quinone oxidoreductase, and in vitro cytotoxicity.

作者信息

Beall H D, Winski S, Swann E, Hudnott A R, Cotterill A S, O'Sullivan N, Green S J, Bien R, Siegel D, Ross D, Moody C J

机构信息

School of Pharmacy and Cancer Center, University of Colorado Health Sciences Center, Box C-238, 4200 East Ninth Avenue, Denver, Colorado 80262, USA.

出版信息

J Med Chem. 1998 Nov 19;41(24):4755-66. doi: 10.1021/jm980328r.

Abstract

A series of indolequinones bearing various functional groups has been synthesized, and the effects of substituents on the metabolism of the quinones by recombinant human NAD(P)H:quinone oxidoreductase (NQO1) were studied. Thus 5-methoxyindolequinones were prepared by the Nenitzescu reaction, followed by functional group interconversions. The methoxy group was subsequently displaced by amine nucleophiles to give a series of amine-substituted quinones. Metabolism of the quinones by NQO1 revealed that, in general, compounds with electron-withdrawing groups at the indole 3-position were among the best substrates, whereas those with amine groups at the 5-position were poor substrates. Compounds with a leaving group at the 3-indolyl methyl position generally inactivated the enzyme. The toxicity toward non-small-cell lung cancer cells with either high NQO1 activity (H460) or no detectable activity (H596) was also studied in representative quinones. Compounds which were good substrates for NQO1 showed the highest selectivity between the two cell lines.

摘要

已合成了一系列带有各种官能团的吲哚醌,并研究了取代基对重组人NAD(P)H:醌氧化还原酶(NQO1)催化醌类代谢的影响。因此,通过涅尼茨埃斯库反应制备了5-甲氧基吲哚醌,随后进行官能团相互转化。甲氧基随后被胺亲核试剂取代,得到一系列胺取代的醌。NQO1对醌类的代谢表明,一般来说,吲哚3位带有吸电子基团的化合物是最佳底物之一,而5位带有胺基的化合物是较差的底物。在3-吲哚甲基位置带有离去基团的化合物通常会使该酶失活。还研究了具有代表性的醌类对具有高NQO1活性(H460)或无可检测活性(H596)的非小细胞肺癌细胞的毒性。作为NQO1良好底物的化合物在两种细胞系之间表现出最高的选择性。

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