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小克银汉霉生物转化——与人类药物代谢的相似性及其在药物发现过程中的相关性

Cunninghamella Biotransformation--Similarities to Human Drug Metabolism and Its Relevance for the Drug Discovery Process.

作者信息

Piska Kamil, Żelaszczyk Dorota, Jamrozik Marek, Kubowicz-Kwaśny Paulina, Pękala Elżbieta

机构信息

Department of Pharmaceutical Biochemistry, Faculty of Pharmacy, Jagiellonian University Medical College, Medyczna 9 str. 30-688 Kraków, Poland.

出版信息

Curr Drug Metab. 2016;17(2):107-17. doi: 10.2174/1389200216666151103115817.

Abstract

BACKGROUND

Studies of drug metabolism are one of the most significant issues in the process of drug development, its introduction to the market and also in treatment. Even the most promising molecule may show undesirable metabolic properties that would disqualify it as a potential drug. Therefore, such studies are conducted in the early phases of drug discovery and development process. Cunninghamella is a filamentous fungus known for its catalytic properties, which mimics mammalian drug metabolism. It has been proven that C. elegans carries at least one gene coding for a CYP enzyme closely related to the CYP51 family. The transformation profile of xenobiotics in Cunninghamella spp. spans a number of reactions catalyzed by different mammalian CYP isoforms.

OBJECTIVE

This paper presents detailed data on similar biotransformation drug products in humans and Cunninghamella spp. and covers the most important aspects of preparative biosynthesis of metabolites, since this model allows to obtain metabolites in sufficient quantities to conduct the further detailed investigations, as quantification, structure analysis and pharmacological activity and toxicity testing.

CONCLUSION

The metabolic activity of three mostly used Cunninghamella species in obtaining hydroxylated, dealkylated and oxidated metabolites of different drugs confirmed its convergence with human biotransformation. Though it cannot replace the standard methods, it can provide support in the field of biotransformation and identifying metabolic soft spots of new chemicals and in predicting possible metabolic pathways. Another aspect is the biosynthesis of metabolites. In this respect, techniques using Cunninghamella spp. seem to be competitive to the chemical methods currently used.

摘要

背景

药物代谢研究是药物研发、上市及治疗过程中最重要的问题之一。即使是最有前景的分子也可能表现出不良的代谢特性,从而使其失去作为潜在药物的资格。因此,此类研究在药物发现和开发过程的早期阶段进行。小克银汉霉是一种丝状真菌,以其催化特性而闻名,它模拟哺乳动物的药物代谢。已证明小克银汉霉携带至少一个编码与CYP51家族密切相关的CYP酶的基因。小克银汉霉属中异生素的转化谱涵盖了由不同哺乳动物CYP同工型催化的多种反应。

目的

本文介绍了人类和小克银汉霉属中类似生物转化药物产品的详细数据,并涵盖了代谢产物制备生物合成的最重要方面,因为该模型能够获得足够数量的代谢产物以进行进一步的详细研究,如定量、结构分析以及药理活性和毒性测试。

结论

三种最常用的小克银汉霉在获得不同药物的羟基化、脱烷基化和氧化代谢产物方面的代谢活性证实了其与人类生物转化的趋同性。尽管它不能取代标准方法,但它可以在生物转化领域提供支持,识别新化学物质的代谢弱点并预测可能的代谢途径。另一个方面是代谢产物的生物合成。在这方面,使用小克银汉霉属的技术似乎与目前使用的化学方法具有竞争力。

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