PLoS Biology (May 2023)

Systems biology elucidates the distinctive metabolic niche filled by the human gut microbe Eggerthella lenta.

  • Cecilia Noecker,
  • Juan Sanchez,
  • Jordan E Bisanz,
  • Veronica Escalante,
  • Margaret Alexander,
  • Kai Trepka,
  • Almut Heinken,
  • Yuanyuan Liu,
  • Dylan Dodd,
  • Ines Thiele,
  • Brian C DeFelice,
  • Peter J Turnbaugh

DOI
https://doi.org/10.1371/journal.pbio.3002125
Journal volume & issue
Vol. 21, no. 5
p. e3002125

Abstract

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Human gut bacteria perform diverse metabolic functions with consequences for host health. The prevalent and disease-linked Actinobacterium Eggerthella lenta performs several unusual chemical transformations, but it does not metabolize sugars and its core growth strategy remains unclear. To obtain a comprehensive view of the metabolic network of E. lenta, we generated several complementary resources: defined culture media, metabolomics profiles of strain isolates, and a curated genome-scale metabolic reconstruction. Stable isotope-resolved metabolomics revealed that E. lenta uses acetate as a key carbon source while catabolizing arginine to generate ATP, traits which could be recapitulated in silico by our updated metabolic model. We compared these in vitro findings with metabolite shifts observed in E. lenta-colonized gnotobiotic mice, identifying shared signatures across environments and highlighting catabolism of the host signaling metabolite agmatine as an alternative energy pathway. Together, our results elucidate a distinctive metabolic niche filled by E. lenta in the gut ecosystem. Our culture media formulations, atlas of metabolomics data, and genome-scale metabolic reconstructions form a freely available collection of resources to support further study of the biology of this prevalent gut bacterium.