The Gut Microbiome on a Periodized Low-Protein Diet Is Associated With Improved Metabolic Health

Li, Zhencheng; Rasmussen, Torben Solbeck; Rasmussen, Mette Line; Li, Jingwen; Olguin, Carlos Henriquez; Kot, Witold; Nielsen, Dennis Sandris; Jensen, Thomas Elbenhardt

Abstract

A periodized (14 days on/14 days off) 5% low protein-high carbohydrate (pLPHC) diet protects against weight gain, improves glucose tolerance in mice and interacts with concurrent voluntary activity wheel training on several parameters including weight maintenance and liver FGF21 secretion. The gut microbiome (GM) responds to both diet and exercise and may influence host metabolism. This study compared the cecal GM after a 13.5-week intervention study in mice on a variety of dietary interventions +/- concurrent voluntary exercise training in activity wheels. The diets included chronic chow diet, LPHC diet, 40 E% high protein-low carbohydrate (HPLC) diet, an obesigenic chronic high-fat diet (HFD) and the pLPHC diet. Our hypothesis was that the GM changes with pLPHC diet would generally reflect the improved metabolic health of the host and interact with concurrent exercise training. The GM analyses revealed greater abundance phylum Bacteroidetes and the genus Akkermansia on chronic and periodized LPHC and higher abundance of Oscillospira and Oscillibacter on HFD. The differences in diet-induced GM correlated strongly with the differences in a range of host metabolic health-measures. In contrast, no significant effect of concurrent exercise training was observed. In conclusion, pLPHC diet elicits substantial changes in the GM. In contrast, only subtle and non-significant effects of concurrent activity wheel exercise were observed. The pLPHC-associated microbiome may contribute to the healthier host phenotype observed in these mice.

Más información

Título según WOS: ID WOS:000463404400001 Not found in local WOS DB
Título de la Revista: FRONTIERS IN MICROBIOLOGY
Volumen: 10
Editorial: Frontiers Media S. A.
Fecha de publicación: 2019
DOI:

10.3389/fmicb.2019.00709

Notas: ISI