Human and preclinical studies of the host-gut microbiome co-metabolite hippurate as a marker and mediator of metabolic health

宿主肠道微生物组共代谢物马尿酸作为代谢健康标志物和介质的人体和临床前研究

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作者:François Brial, Julien Chilloux, Trine Nielsen, Sara Vieira-Silva, Gwen Falony, Petros Andrikopoulos, Michael Olanipekun, Lesley Hoyles, Fatima Djouadi, Ana L Neves, Andrea Rodriguez-Martinez, Ghiwa Ishac Mouawad, Nicolas Pons, Sofia Forslund, Emmanuelle Le-Chatelier, Aurélie Le Lay, Jeremy Nicholso

Conclusion

Our human and experimental studies show that a high urine hippurate concentration is a general marker of metabolic health, and in the context of obesity induced by high-fat diets, hippurate contributes to metabolic improvements, highlighting its potential as a mediator of metabolic health.

Objective

Gut microbial products are involved in regulation of host metabolism. In human and experimental studies, we explored the potential role of hippurate, a hepatic phase 2 conjugation product of microbial benzoate, as a marker and mediator of metabolic health. Design: In 271 middle-aged non-diabetic Danish individuals, who were stratified on habitual dietary intake, we applied 1H-nuclear magnetic resonance (NMR) spectroscopy of urine samples and shotgun-sequencing-based metagenomics of the gut microbiome to explore links between the urine level of hippurate, measures of the gut microbiome, dietary fat and markers of metabolic health. In mechanistic experiments with chronic subcutaneous infusion of hippurate to high-fat-diet-fed obese mice, we tested for causality between hippurate and metabolic phenotypes.

Results

In the human study, we showed that urine hippurate positively associates with microbial gene richness and functional modules for microbial benzoate biosynthetic pathways, one of which is less prevalent in the Bacteroides 2 enterotype compared with Ruminococcaceae or Prevotella enterotypes. Through dietary stratification, we identify a subset of study participants consuming a diet rich in saturated fat in which urine hippurate concentration, independently of gene richness, accounts for links with metabolic health. In the high-fat-fed mice experiments, we demonstrate causality through chronic infusion of hippurate (20 nmol/day) resulting in improved glucose tolerance and enhanced insulin secretion.

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