EMBO Molecular Medicine (Sep 2024)

Multiomics reveals microbial metabolites as key actors in intestinal fibrosis in Crohn’s disease

  • Xuehua Li,
  • Shixian Hu,
  • Xiaodi Shen,
  • Ruonan Zhang,
  • Caiguang Liu,
  • Lin Xiao,
  • Jinjiang Lin,
  • Li Huang,
  • Weitao He,
  • Xinyue Wang,
  • Lili Huang,
  • Qingzhu Zheng,
  • Luyao Wu,
  • Canhui Sun,
  • Zhenpeng Peng,
  • Minhu Chen,
  • Ziping Li,
  • Rui Feng,
  • Yijun Zhu,
  • Yangdi Wang,
  • Zhoulei Li,
  • Ren Mao,
  • Shi-Ting Feng

DOI
https://doi.org/10.1038/s44321-024-00129-8
Journal volume & issue
Vol. 16, no. 10
pp. 2427 – 2449

Abstract

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Abstract Intestinal fibrosis is the primary cause of disability in patients with Crohn’s disease (CD), yet effective therapeutic strategies are currently lacking. Here, we report a multiomics analysis of gut microbiota and fecal/blood metabolites of 278 CD patients and 28 healthy controls, identifying characteristic alterations in gut microbiota (e.g., Lachnospiraceae, Ruminococcaceae, Muribaculaceae, Saccharimonadales) and metabolites (e.g., L-aspartic acid, glutamine, ethylmethylacetic acid) in moderate-severe intestinal fibrosis. By integrating multiomics data with magnetic resonance enterography features, putative links between microbial metabolites and intestinal fibrosis-associated morphological alterations were established. These potential associations were mediated by specific combinations of amino acids (e.g., L-aspartic acid), primary bile acids, and glutamine. Finally, we provided causal evidence that L-aspartic acid aggravated intestinal fibrosis both in vitro and in vivo. Overall, we offer a biologically plausible explanation for the hypothesis that gut microbiota and its metabolites promote intestinal fibrosis in CD while also identifying potential targets for therapeutic trials.

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