Nature Communications (Nov 2023)

Dietary L-Tryptophan consumption determines the number of colonic regulatory T cells and susceptibility to colitis via GPR15

  • Nguyen T. Van,
  • Karen Zhang,
  • Rachel M. Wigmore,
  • Anne I. Kennedy,
  • Carolina R. DaSilva,
  • Jialing Huang,
  • Manju Ambelil,
  • Jose H. Villagomez,
  • Gerald J. O’Connor,
  • Randy S. Longman,
  • Miao Cao,
  • Adam E. Snook,
  • Michael Platten,
  • Gerard Kasenty,
  • Luis J. Sigal,
  • George C. Prendergast,
  • Sangwon V. Kim

DOI
https://doi.org/10.1038/s41467-023-43211-4
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 15

Abstract

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Abstract Environmental factors are the major contributor to the onset of immunological disorders such as ulcerative colitis. However, their identities remain unclear. Here, we discover that the amount of consumed L-Tryptophan (L-Trp), a ubiquitous dietary component, determines the transcription level of the colonic T cell homing receptor, GPR15, hence affecting the number of colonic FOXP3+ regulatory T (Treg) cells and local immune homeostasis. Ingested L-Trp is converted by host IDO1/2 enzymes, but not by gut microbiota, to compounds that induce GPR15 transcription preferentially in Treg cells via the aryl hydrocarbon receptor. Consequently, two weeks of dietary L-Trp supplementation nearly double the colonic GPR15+ Treg cells via GPR15-mediated homing and substantially reduce the future risk of colitis. In addition, humans consume 3–4 times less L-Trp per kilogram of body weight and have fewer colonic GPR15+ Treg cells than mice. Thus, we uncover a microbiota-independent mechanism linking dietary L-Trp and colonic Treg cells, that may have therapeutic potential.