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Plasma Metabolites Related to Peripheral and Hepatic Insulin Sensitivity Are Not Directly Linked to Gut Microbiota Composition. | LitMetric

AI Article Synopsis

  • Plasma metabolites play a role in various metabolic functions, including insulin sensitivity (IS), and some of these metabolites are influenced by gut microbiota.
  • A study involving 115 participants with metabolic syndrome assessed the connections between plasma metabolites, gut microbiota composition, and IS using advanced measurement techniques and machine learning.
  • While plasma metabolites accounted for a notable portion of the variance in IS, they did not directly correlate with the gut microbiota composition, suggesting a complex relationship between plasma metabolites, gut microbiota, and insulin sensitivity in individuals with metabolic syndrome.

Article Abstract

Plasma metabolites affect a range of metabolic functions in humans, including insulin sensitivity (IS). A subset of these plasma metabolites is modified by the gut microbiota. To identify potential microbial-metabolite pathways involved in IS, we investigated the link between plasma metabolites, gut microbiota composition, and IS, using the gold-standard for peripheral and hepatic IS measurement in a group of participants with metabolic syndrome (MetSyn). In a cross-sectional study with 115 MetSyn participants, fasting plasma samples were collected for untargeted metabolomics analysis and fecal samples for 16S rRNA gene amplicon sequencing. A two-step hyperinsulinemic euglycemic clamp was performed to assess peripheral and hepatic IS. Collected data were integrated and potential interdependence between metabolites, gut microbiota, and IS was analyzed using machine learning prediction models. Plasma metabolites explained 13.2% and 16.7% of variance in peripheral and hepatic IS, respectively. Fecal microbiota composition explained 4.2% of variance in peripheral IS and was not related to hepatic IS. Although metabolites could partially explain the variances in IS, the top metabolites related to peripheral and hepatic IS did not significantly correlate with gut microbiota composition (both on taxonomical level and alpha-diversity). However, all plasma metabolites could explain 18.5% of the variance in microbial alpha-diversity (Shannon); the top 20 metabolites could even explain 44.5% of gut microbial alpha-diversity. In conclusion, plasma metabolites could partially explain the variance in peripheral and hepatic IS; however, these metabolites were not directly linked to the gut microbiota composition, underscoring the intricate relation between plasma metabolites, the gut microbiota, and IS in MetSyn.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7469041PMC
http://dx.doi.org/10.3390/nu12082308DOI Listing

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