生物信息学
代谢物
化学
代谢组学
生物化学
微粒体
体外
药理学
生物
色谱法
基因
作者
A. F. M. Motiur Rahman,Wencui Yin,Adnan A. Kadi,Yurngdong Jahng
出处
期刊:Molecules
[Multidisciplinary Digital Publishing Institute]
日期:2020-12-13
卷期号:25 (24): 5903-5903
被引量:3
标识
DOI:10.3390/molecules25245903
摘要
H37Rv, chemo-preventive potential, and moderate topoisomerase inhibitory activity. Here, in silico metabolism and toxicity prediction of galeon by CYP450, in vitro metabolic profiling study in rat liver microsomes (RLMs), and molecular interactions of galeon-CYP450 isoforms were performed. An in silico metabolic prediction study showed demethyl and mono-hydroxy galeon were the metabolites with the highest predictability. Among the predicted metabolites, mono-hydroxy galeon was found to have plausible toxicities such as skin sensitization, thyroid toxicity, chromosome damage, and carcinogenicity. An in vitro metabolism study of galeon, incubated in RLMs, revealed eighteen Phase-I metabolites, nine methoxylamine, and three glutathione conjugates. Identification of possible metabolites and confirmation of their structures were carried out using ion-trap tandem mass spectrometry. In silico docking analysis of galeon demonstrated significant interactions with active site residues of almost all CYP450 isoforms.
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