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首页> 外文期刊>Biochemical Pharmacology >Survey of variants of human flavin-containing monooxygenase 3 (FMO3) and their drug oxidation activities
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Survey of variants of human flavin-containing monooxygenase 3 (FMO3) and their drug oxidation activities

机译:人类含黄素单加氧酶3(FMO3)的变体及其药物氧化活性的调查

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摘要

Human flavin-containing monooxygenase 3 (FMO3, EC 1.14.13.8) in liver catalyzes a variety of oxygenations of nitrogen- and sulfur-containing medicines and xenobiotic substances. Loss-of-function mutations of the FMO3 gene, the enzyme responsible for trimethylamine N-oxygenation, cause the inherited disorder trimethylaminuria (also known as fish odor syndrome). In this mini-review, mutations of the FMO3 gene reported in the literature and in the National Center for Biotechnology Information single nucleotide polymorphism database were surveyed. Then, the activities of FMO3 variants in human liver microsomes and the activities of recombinantly expressed FMO3 variant proteins with respect to the oxygenation of nitrogen- and sulfur-containing drugs were summarized and the potential for drug interactions was demonstrated. Individual differences in FMO3 function were seen in subjects genotyped for homozygous FMO3 variants. Specific regions of the FMO3 C-terminus are required for functional activity. Naturally truncated FMO3 is believed to have barely detectable function, thereby explaining the relationship with severe impaired phenotypes. The present article provides fundamental, up-to-date information on the importance of human FMO3 in individual xenobiotic oxygenations, including those of new medicines and dietary-derived trimethylamine.
机译:肝脏中含有人黄素的单加氧酶3(FMO3,EC 1.14.13.8)会催化含氮和硫的药物以及异生物质物质的多种氧化作用。 FMO3基因(负责三甲胺N-加氧的酶)的功能丧失突变导致遗传性疾病三甲胺症(也称为鱼味综合症)。在本篇小型综述中,对文献和国家生物技术信息中心单核苷酸多态性数据库中报告的FMO3基因突变进行了调查。然后,总结了人肝微粒体中FMO3变体的活性以及重组表达的FMO3变体蛋白在含氮和硫的药物氧化方面的活性,并证明了药物相互作用的潜力。在对纯合FMO3变体进行基因分型的受试者中,观察到了FMO3功能的个体差异。功能活动需要FMO3 C端的特定区域。天然截短的FMO3被认为几乎没有可检测的功能,从而解释了与严重受损表型的关系。本文提供了有关人类FMO3在各种异种生物氧合中的重要性的基本,最新信息,包括新药和饮食中的三甲胺。

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