Exclusive enteral nutrition initiates individual protective microbiome changes to induce remission in pediatric Crohn's disease.

完全肠内营养可启动个体保护性微生物群的变化,从而诱导儿童克罗恩病缓解

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作者:Häcker Deborah, Siebert Kolja, Smith Byron J, Köhler Nikolai, Riva Alessandra, Mahapatra Aritra, Heimes Helena, Nie Jiatong, Metwaly Amira, Hölz Hannes, Manz Quirin, De Zen Federica, Heetmeyer Jeannine, Socas Katharina, Le Thi Giang, Meng Chen, Kleigrewe Karin, Pauling Josch K, Neuhaus Klaus, List Markus, Pollard Katherine S, Schwerd Tobias, Haller Dirk
Exclusive enteral nutrition (EEN) is a first-line therapy for pediatric Crohn's disease (CD), but protective mechanisms remain unknown. We established a prospective pediatric cohort to characterize the function of fecal microbiota and metabolite changes of treatment-naive CD patients in response to EEN (German Clinical Trials DRKS00013306). Integrated multi-omics analysis identified network clusters from individually variable microbiome profiles, with Lachnospiraceae and medium-chain fatty acids as protective features. Bioorthogonal non-canonical amino acid tagging selectively identified bacterial species in response to medium-chain fatty acids. Metagenomic analysis identified high strain-level dynamics in response to EEN. Functional changes in diet-exposed fecal microbiota were further validated using gut chemostat cultures and microbiota transfer into germ-free Il10-deficient mice. Dietary model conditions induced individual patient-specific strain signatures to prevent or cause inflammatory bowel disease (IBD)-like inflammation in gnotobiotic mice. Hence, we provide evidence that EEN therapy operates through explicit functional changes of temporally and individually variable microbiome profiles.

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