首页> 美国卫生研究院文献>Drug Metabolism and Disposition >Trimethylamine and Trimethylamine N-Oxide a Flavin-Containing Monooxygenase 3 (FMO3)-Mediated Host-Microbiome Metabolic Axis Implicated in Health and Disease
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Trimethylamine and Trimethylamine N-Oxide a Flavin-Containing Monooxygenase 3 (FMO3)-Mediated Host-Microbiome Metabolic Axis Implicated in Health and Disease

机译:三甲胺和三甲胺N-氧化物一种含黄素的单加氧酶3(FMO3)介导的宿主-微生物组代谢轴涉及健康和疾病。

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摘要

Flavin-containing monooxygenase 3 (FMO3) is known primarily as an enzyme involved in the metabolism of therapeutic drugs. On a daily basis, however, we are exposed to one of the most abundant substrates of the enzyme trimethylamine (TMA), which is released from various dietary components by the action of gut bacteria. FMO3 converts the odorous TMA to nonodorous TMA N-oxide (TMAO), which is excreted in urine. Impaired FMO3 activity gives rise to the inherited disorder primary trimethylaminuria (TMAU). Affected individuals cannot produce TMAO and, consequently, excrete large amounts of TMA. A dysbiosis in gut bacteria can give rise to secondary TMAU. Recently, there has been much interest in FMO3 and its catalytic product, TMAO, because TMAO has been implicated in various conditions affecting health, including cardiovascular disease, reverse cholesterol transport, and glucose and lipid homeostasis. In this review, we consider the dietary components that can give rise to TMA, the gut bacteria involved in the production of TMA from dietary precursors, the metabolic reactions by which bacteria produce and use TMA, and the enzymes that catalyze the reactions. Also included is information on bacteria that produce TMA in the oral cavity and vagina, two key microbiome niches that can influence health. Finally, we discuss the importance of the TMA/TMAO microbiome-host axis in health and disease, considering factors that affect bacterial production and host metabolism of TMA, the involvement of TMAO and FMO3 in disease, and the implications of the host-microbiome axis for management of TMAU.
机译:含黄素的单加氧酶3(FMO3)主要是作为参与治疗药物代谢的酶。但是,每天,我们都会接触到三甲胺(TMA)酶中含量最丰富的底物之一,该酶通过肠道细菌的作用从各种饮食成分中释放出来。 FMO3将有味的TMA转换为无味的TMA N-氧化物(TMAO),并从尿液中排出。 FMO3活性受损会引起遗传性疾病原发性三甲基尿症(TMAU)。受影响的个体无法产生TMAO,因此会排泄大量TMA。肠道细菌的营养不良会引起继发性TMAU。最近,人们对FMO3及其催化产物TMAO产生了浓厚的兴趣,因为TMAO已牵涉到影响健康的各种状况,包括心血管疾病,胆固醇逆向转运以及葡萄糖和脂质体内稳态。在这篇综述中,我们考虑了可引起TMA的饮食成分,从饮食前体中产生TMA的肠道细菌,细菌产生和使用TMA的代谢反应以及催化反应的酶。还包括有关在口腔和阴道中产生TMA的细菌的信息,这是两个可能影响健康的关键微生物组。最后,我们讨论了TMA / TMAO微生物宿主轴在健康和疾病中的重要性,考虑了影响TMA细菌产生和宿主代谢的因素,TMAO和FMO3在疾病中的参与以及宿主微生物群轴的影响用于管理TMAU。

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