Frontiers in Endocrinology (Jul 2023)

Microbial metabolite p-cresol inhibits gut hormone expression and regulates small intestinal transit in mice

  • Pernille Baumann Toft,
  • Amanda Marie Vanslette,
  • Kajetan Trošt,
  • Thomas Moritz,
  • Matthew Paul Gillum,
  • Fredrik Bäckhed,
  • Fredrik Bäckhed,
  • Fredrik Bäckhed,
  • Tulika Arora

DOI
https://doi.org/10.3389/fendo.2023.1200391
Journal volume & issue
Vol. 14

Abstract

Read online

p-cresol is a metabolite produced by microbial metabolism of aromatic amino acid tyrosine. p-cresol and its conjugated forms, p-cresyl sulfate and p-cresyl glucuronide, are uremic toxins that correlate positively with chronic kidney disease and diabetes pathogenesis. However, how p-cresol affects gut hormones is unclear. Here, we expose immortalized GLUTag cells to increasing concentrations of p-cresol and found that p-cresol inhibited Gcg expression and reduced glucagon-like peptide-1 (GLP-1) secretion in vitro. In mice, administration of p-cresol in the drinking water for 2 weeks reduced the transcript levels of Gcg and other gut hormones in the colon; however, it did not affect either fasting or glucose-induced plasma GLP-1 levels. Furthermore, it did not affect glucose tolerance but promoted faster small intestinal transit in mice. Overall, our data suggest that microbial metabolite p-cresol suppresses transcript levels of gut hormones and regulates small intestinal transit in mice.

Keywords