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坎尼恩菌作为组氨酸 H(3)受体拮抗剂 1-[3-(4-叔丁基苯氧基)丙基]哌啶代谢的微生物模型。

Cunninghamella as a microbiological model for metabolism of histamine H(3) receptor antagonist 1-[3-(4-tert-butylphenoxy)propyl]piperidine.

机构信息

Department of Technology and Biotechnology of Drugs, Faculty of Pharmacy, Jagiellonian University Medical College, Cracow, Poland.

出版信息

Appl Biochem Biotechnol. 2012 Nov;168(6):1584-93. doi: 10.1007/s12010-012-9880-8. Epub 2012 Sep 16.

Abstract

The aim of the study was to analyze the ability of the microorganism Cunninghamella to carry out the biotransformation of 1-[3-(4-tert-butylphenoxy)propyl]piperidine (DL76) and to compare the obtained results with in silico models. Biotransformation was carried out by three strains of filamentous fungus: Cunninghamella echinulata, Cunninghamella blakesleeana, and Cunninghamella elegans. Most probable direction of DL76 metabolic transition was the oxidation of the methyl group in the tert-butyl moiety leading to the formation of the metabolite with I° alcohol properties. This kind of reaction was conducted by all three strains tested. However, only in the case of C. blakesleeana that biotransformation product had a structure of carboxylic acid. CYP2C19 was identified by Metasite software to be the isoform of major importance in the oxidation process in the tert-butyl moiety of DL76. In silico data coincide with the results of experiments conducted in vitro. It was confirmed that Cunninghamella fungi are a very good model to study the metabolism of xenobiotics. The computational methods and microbial models of metabolism can be used as useful tools in early ADME-Tox assays in the process of developing new drug candidates.

摘要

本研究旨在分析枝孢菌属微生物进行 1-[3-(4-叔丁基苯氧基)丙基]哌啶(DL76)生物转化的能力,并将所得结果与计算机模拟模型进行比较。生物转化由三种丝状真菌菌株:刺孢小克银汉霉、多形小克银汉霉和雅致枝孢菌进行。DL76 代谢转化的最可能方向是叔丁基部分甲基的氧化,导致形成具有 I°醇性质的代谢物。这三种测试菌株均进行了这种反应。然而,只有在 C. blakesleeana 的情况下,生物转化产物才具有羧酸的结构。Metasite 软件鉴定 CYP2C19 为 DL76 叔丁基部分氧化过程中重要的同工酶。计算机模拟数据与体外实验结果一致。证实枝孢菌是研究外源性物质代谢的非常好的模型。代谢的计算方法和微生物模型可作为开发新候选药物的早期 ADME-Tox 试验中的有用工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9594/3501165/435ac9d42824/12010_2012_9880_Fig1_HTML.jpg

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