Abstract

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.

Highlights

  • Flavin-containing monooxygenases (FMOs) (EC 1.14.13.8) catalyze the NADPH-dependent oxidative metabolism of a wide array of foreign chemicals, including drugs, dietary-derived compounds, and environmental pollutants (Krueger and Williams, 2005)

  • 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

  • We discuss the importance of the TMA/TMA N-oxide (TMAO) microbiome-host axis in health and disease, considering factors that affect bacterial production and host metabolism of TMA, the involvement of TMAO and Flavin-containing monooxygenase 3 (FMO3) in disease, and the implications of the host-microbiome axis for management of TMAU

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Summary

Introduction

Flavin-containing monooxygenases (FMOs) (EC 1.14.13.8) catalyze the NADPH-dependent oxidative metabolism of a wide array of foreign chemicals, including drugs, dietary-derived compounds, and environmental pollutants (Krueger and Williams, 2005). Rare genetic variants of the FMO3 gene that abolish or severely impair activity of the enzyme give rise to the inherited disorder primary trimethylaminuria (TMAU) (Phillips and Shephard, 2008) because of inefficient conversion of microbiome-derived odorous TMA to nonodorous TMAO. Knowledge of the microbial species that give rise to TMA would contribute greatly to our understanding of the consequences for human health of the complex interrelationships of diet, the microbiome, and the capacity for FMO3-catalyzed conversion of TMA to TMAO. 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

Origins and Metabolic Fate of TMA
Metabolism of TMA by Gut Bacteria
Oral and Vaginal Microbiota
Noncommensal Bacteria Able to Produce TMA
Burkholderia Campylobacter Stigmatella Sinorhizobiumb
Conclusions
Findings
Authorship Contributions
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