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Expert Opin Drug Discov. 2013 Jun;8(6):641-54. doi: 10.1517/17460441.2013.788497. Epub 2013 Apr 9.
2
Predicting intrinsic clearance for drugs and drug candidates metabolized by aldehyde oxidase.预测醛氧化酶代谢的药物和候选药物的内在清除率。
Mol Pharm. 2013 Apr 1;10(4):1262-8. doi: 10.1021/mp300568r. Epub 2013 Feb 13.
3
Strategies for a comprehensive understanding of metabolism by aldehyde oxidase.通过醛氧化酶全面了解代谢的策略。
Expert Opin Drug Metab Toxicol. 2013 Feb;9(2):153-68. doi: 10.1517/17425255.2013.738668. Epub 2012 Dec 12.
4
Interspecies variation in the metabolism of zoniporide by aldehyde oxidase.醛氧化酶对佐尼普明代谢的种间差异。
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J Biol Chem. 2012 Nov 23;287(48):40690-702. doi: 10.1074/jbc.M112.390419. Epub 2012 Sep 27.
6
Evidence for substrate-dependent inhibition profiles for human liver aldehyde oxidase.人肝醛氧化酶的底物依赖抑制谱的证据。
Drug Metab Dispos. 2013 Jan;41(1):24-9. doi: 10.1124/dmd.112.048546. Epub 2012 Sep 20.
7
The role of aldehyde oxidase and xanthine oxidase in the biotransformation of a novel negative allosteric modulator of metabotropic glutamate receptor subtype 5.醛氧化酶和黄嘌呤氧化酶在代谢型谷氨酸受体亚型 5 的新型负变构调节剂生物转化中的作用。
Drug Metab Dispos. 2012 Sep;40(9):1834-45. doi: 10.1124/dmd.112.046136. Epub 2012 Jun 18.
8
The role of aldehyde oxidase in drug metabolism.醛氧化酶在药物代谢中的作用。
Expert Opin Drug Metab Toxicol. 2012 Apr;8(4):487-503. doi: 10.1517/17425255.2012.663352. Epub 2012 Feb 16.
9
Deuterium isotope effects on drug pharmacokinetics. I. System-dependent effects of specific deuteration with aldehyde oxidase cleared drugs.氘同位素对药物药代动力学的影响。I. 醛氧化酶清除药物的特定氘代的系统依赖性效应。
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10
The structural basis for homotropic and heterotropic cooperativity of midazolam metabolism by human cytochrome P450 3A4.人细胞色素 P4503A4 介导的咪达唑仑代谢的同型和异型协同作用的结构基础。
Biochemistry. 2011 Dec 20;50(50):10804-18. doi: 10.1021/bi200924t. Epub 2011 Nov 22.

评价恒河猴和豚鼠肝胞质部分作为人醛氧化酶模型。

Evaluation of rhesus monkey and guinea pig hepatic cytosol fractions as models for human aldehyde oxidase.

机构信息

Department of Chemistry, Washington State University, Pullman, Washington.

出版信息

Drug Metab Dispos. 2013 Oct;41(10):1852-8. doi: 10.1124/dmd.113.052985. Epub 2013 Aug 5.

DOI:10.1124/dmd.113.052985
PMID:23918666
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3781378/
Abstract

Aldehyde oxidase (AOX) is a cytosolic enzyme expressed across a wide range of species, including guinea pig and rhesus monkey. These species are believed to be the best preclinical models for studying human AOX-mediated metabolism. We compared AOX activity in rhesus monkeys, guinea pigs, and humans using phthalazine and N-[2-(dimethylamino)ethyl]acridone-4-carboxamide (DACA) as substrates and raloxifene as an inhibitor. Michaelis-Menten kinetics was observed for phthalazine oxidation in rhesus monkey, guinea pig, and human liver cytosol, whereas substrate inhibition was seen with DACA oxidase activity in all three livers. Raloxifene inhibited phthalazine and DACA oxidase activity uncompetitively in guinea pig, whereas mixed-mode inhibition was seen in rhesus monkey. Our analysis of the primary sequence alignment of rhesus monkey, guinea pig, and human aldehyde oxidase isoform 1 (AOX1) along with homology modeling has led to the identification of several amino acid residue differences within the active site and substrate entrance channel of AOX1. We speculate that some of these residues might be responsible for the differences observed in activity. Overall, our data indicate that rhesus monkeys and guinea pigs would overestimate intrinsic clearance in humans and would be unsuitable to use as animal models. Our study also showed that AOX metabolism in species is substrate-dependent and no single animal model can be reliably used to predict every drug response in humans.

摘要

醛氧化酶(AOX)是一种广泛存在于多种物种中的细胞质酶,包括豚鼠和恒河猴。这些物种被认为是研究人类 AOX 介导的代谢的最佳临床前模型。我们使用酞嗪和 N-[2-(二甲氨基)乙基]吖啶-4-羧酰胺(DACA)作为底物,以及雷洛昔芬作为抑制剂,比较了恒河猴、豚鼠和人类的 AOX 活性。在恒河猴、豚鼠和人肝胞质中观察到酞嗪氧化的米氏动力学,而在所有三种肝脏中均观察到 DACA 氧化酶活性的底物抑制。雷洛昔芬在豚鼠中竞争性抑制酞嗪和 DACA 氧化酶活性,而在恒河猴中则表现为混合模式抑制。我们对恒河猴、豚鼠和人醛氧化酶 1 型(AOX1)同工酶的一级序列比对进行了分析,并进行了同源建模,从而确定了 AOX1 的活性位点和底物入口通道内的几个氨基酸残基差异。我们推测,这些残基中的一些可能是导致观察到的活性差异的原因。总体而言,我们的数据表明,恒河猴和豚鼠会高估人类的内在清除率,不适合作为动物模型。我们的研究还表明,物种的 AOX 代谢是底物依赖性的,没有单一的动物模型可以可靠地用于预测人类的每种药物反应。