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斑马鱼与人类的生物活化潜力及代谢谱研究。

An investigation of the bioactivation potential and metabolism profile of Zebrafish versus human.

作者信息

Chng Hui Ting, Ho Han Kiat, Yap Chun Wei, Lam Siew Hong, Chan Eric Chun Yong

机构信息

Department of Pharmacy, National University of Singapore, Singapore.

出版信息

J Biomol Screen. 2012 Aug;17(7):974-86. doi: 10.1177/1087057112447305. Epub 2012 May 29.

Abstract

The zebrafish model has been increasingly explored as an alternative model for toxicity screening of pharmaceutical drugs. However, little is understood about the bioactivation of drug to reactive metabolite and phase I and II metabolism of chemical in zebrafish as compared with human. The primary aim of our study was to establish the bioactivation potential of zebrafish using acetaminophen as a probe substrate. Our secondary aim was to perform metabolite profiling experiments on testosterone, a CYP3A probe substrate, in zebrafish and compare the metabolite profiles with that of human. The glutathione trapping assay of N-acetyl-p-benzoquinone imine demonstrated that zebrafish generates the same reactive metabolite as humans from the bioactivation of acetaminophen. Zebrafish possesses functional CYP3A4/5-like and UDP-glucuronosyltransferase metabolic activities on testosterone. Differential testosterone metabolism was observed among the two species. In silico docking studies suggested that the zebrafish CYP3A65 was responsible for the bioactivation of acetaminophen and phase I hydroxylation of testosterone. Our findings reinforce the need to further characterize the drug metabolism phenotype of zebrafish before the model can fully achieve its potential as an alternative toxicity screening model in drug research.

摘要

斑马鱼模型已越来越多地被用作药物毒性筛选的替代模型。然而,与人类相比,对于斑马鱼体内药物生物活化成反应性代谢物以及化学物质的I相和II相代谢了解甚少。我们研究的主要目的是使用对乙酰氨基酚作为探针底物来确定斑马鱼的生物活化潜力。我们的次要目的是对斑马鱼体内的细胞色素P450 3A(CYP3A)探针底物睾酮进行代谢物谱分析实验,并将代谢物谱与人类的进行比较。对N - 乙酰 - 对苯醌亚胺的谷胱甘肽捕获试验表明,斑马鱼从对乙酰氨基酚的生物活化中产生与人类相同的反应性代谢物。斑马鱼对睾酮具有功能性的CYP3A4/5样和尿苷二磷酸葡萄糖醛酸基转移酶代谢活性。在这两个物种中观察到了不同的睾酮代谢情况。计算机模拟对接研究表明,斑马鱼的CYP3A65负责对乙酰氨基酚的生物活化和睾酮的I相羟基化。我们的研究结果强化了在该模型能够充分发挥其作为药物研究中替代毒性筛选模型的潜力之前,进一步表征斑马鱼药物代谢表型的必要性。

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