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Comparative molecular field analysis (CoMFA). 1. Effect of shape on binding of steroids to carrier proteins.比较分子场分析(CoMFA)。1. 形状对类固醇与载体蛋白结合的影响。
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The functional role of CYP2B6 in human drug metabolism: substrates and inhibitors in vitro, in vivo and in silico.细胞色素P450 2B6(CYP2B6)在人体药物代谢中的功能作用:体外、体内及计算机模拟的底物与抑制剂
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In vitro screening of drug metabolism during drug development: can we trust the predictions?药物研发过程中药物代谢的体外筛选:我们能相信这些预测吗?
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Predictive three-dimensional quantitative structure-activity relationship of cytochrome P450 1A2 inhibitors.细胞色素P450 1A2抑制剂的预测性三维定量构效关系
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Predicting drug-drug interactions in drug discovery: where are we now and where are we going?药物研发中药物相互作用的预测:我们现在处于什么阶段,又将走向何方?
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Quantitative structure-activity relationship analysis of inhibitors of the nicotine metabolizing CYP2A6 enzyme.尼古丁代谢酶CYP2A6抑制剂的定量构效关系分析
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Selective inhibition of CYP2B6-catalyzed bupropion hydroxylation in human liver microsomes in vitro.体外对人肝微粒体中CYP2B6催化的安非他酮羟基化反应的选择性抑制作用。
Drug Metab Dispos. 2004 Jun;32(6):626-31. doi: 10.1124/dmd.32.6.626.
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Potent mechanism-based inhibition of human CYP2B6 by clopidogrel and ticlopidine.氯吡格雷和噻氯匹定对人CYP2B6基于机制的强效抑制作用。
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10
Triethylenethiophosphoramide is a specific inhibitor of cytochrome P450 2B6: implications for cyclophosphamide metabolism.三乙烯硫代磷酰胺是细胞色素P450 2B6的特异性抑制剂:对环磷酰胺代谢的影响。
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基于三维定量构效关系(3D-QSAR)分析的新型强效选择性细胞色素P450 2B6(CYP2B6)抑制剂

New potent and selective cytochrome P450 2B6 (CYP2B6) inhibitors based on three-dimensional quantitative structure-activity relationship (3D-QSAR) analysis.

作者信息

Korhonen L E, Turpeinen M, Rahnasto M, Wittekindt C, Poso A, Pelkonen O, Raunio H, Juvonen R O

机构信息

Department of Pharmacology and Toxicology, University of Kuopio, Kuopio, Finland.

出版信息

Br J Pharmacol. 2007 Apr;150(7):932-42. doi: 10.1038/sj.bjp.0707173. Epub 2007 Feb 26.

DOI:10.1038/sj.bjp.0707173
PMID:17325652
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2013880/
Abstract

BACKGROUND AND PURPOSE

The cytochrome P450 2B6 (CYP2B6) enzyme metabolises a number of clinically important drugs. Drug-drug interactions resulting from inhibition or induction of CYP2B6 activity may cause serious adverse effects. The aims of this study were to construct a three-dimensional structure-activity relationship (3D-QSAR) model of the CYP2B6 protein and to identify novel potent and selective inhibitors of CYP2B6 for in vitro research purposes.

EXPERIMENTAL APPROACH

The inhibition potencies (IC(50) values) of structurally diverse chemicals were determined with recombinant human CYP2B6 enzyme. Two successive models were constructed using Comparative Molecular Field Analysis (CoMFA).

KEY RESULTS

Three compounds proved to be very potent and selective competitive inhibitors of CYP2B6 in vitro (IC(50)<1 microM): 4-(4-chlorobenzyl)pyridine (CBP), 4-(4-nitrobenzyl)pyridine (NBP), and 4-benzylpyridine (BP). A complete inhibition of CYP2B6 activity was achieved with 0.1 microM CBP, whereas other CYP-related activities were not affected. Forty-one compounds were selected for further testing and construction of the final CoMFA model. The created CoMFA model was of high quality and predicted accurately the inhibition potency of a test set (n=7) of structurally diverse compounds.

CONCLUSIONS AND IMPLICATIONS

Two CoMFA models were created which revealed the key molecular characteristics of inhibitors of the CYP2B6 enzyme. The final model accurately predicted the inhibitory potencies of several structurally unrelated compounds. CBP, BP and NBP were identified as novel potent and selective inhibitors of CYP2B6 and CBP especially is a suitable inhibitor for in vitro screening studies.

摘要

背景与目的

细胞色素P450 2B6(CYP2B6)酶可代谢多种具有临床重要性的药物。由CYP2B6活性的抑制或诱导导致的药物相互作用可能会引起严重的不良反应。本研究的目的是构建CYP2B6蛋白的三维构效关系(3D-QSAR)模型,并识别用于体外研究目的的新型强效且选择性的CYP2B6抑制剂。

实验方法

使用重组人CYP2B6酶测定结构多样的化学物质的抑制效力(IC50值)。采用比较分子场分析(CoMFA)构建了两个连续的模型。

关键结果

三种化合物在体外被证明是非常强效且选择性的CYP2B6竞争性抑制剂(IC50<1 microM):4-(4-氯苄基)吡啶(CBP)、4-(4-硝基苄基)吡啶(NBP)和4-苄基吡啶(BP)。0.1 microM的CBP可完全抑制CYP2B6活性,而其他与CYP相关的活性未受影响。选择了41种化合物进行进一步测试并构建最终的CoMFA模型。所创建的CoMFA模型质量很高,准确预测了一组结构多样的化合物(n=7)的抑制效力。

结论与意义

创建了两个CoMFA模型,揭示了CYP2B6酶抑制剂的关键分子特征。最终模型准确预测了几种结构不相关化合物的抑制效力。CBP、BP和NBP被鉴定为新型强效且选择性的CYP2B6抑制剂,尤其是CBP是体外筛选研究的合适抑制剂。