Gut metabolome and microbiota signatures predict response to treatment with exclusive enteral nutrition in a prospective study in children with active Crohn's disease

Ben Nichols; Anny Briola; Michael Logan; Jaroslav Havlik; Anna Mascellani; Konstantinos Gkikas; Simon Milling; Umer Zeeshan Ijaz; Christopher Quince; Vaios Svolos; Richard K Russell; Richard Hansen; Konstantinos Gerasimidis

doi:10.1016/j.ajcnut.2023.12.027

Gut metabolome and microbiota signatures predict response to treatment with exclusive enteral nutrition in a prospective study in children with active Crohn's disease

Am J Clin Nutr. 2024 Apr;119(4):885-895. doi: 10.1016/j.ajcnut.2023.12.027. Epub 2024 Feb 19.

Affiliations

¹ Human Nutrition, School of Medicine, University of Glasgow, Glasgow Royal Infirmary, Glasgow, United Kingdom.
² Department of Food Science, Czech University of Life Sciences Prague, Prague, Czech Republic.
³ School of Infection and Inflammation, University of Glasgow, Glasgow, United Kingdom.
⁴ Civil Engineering, School of Engineering, University of Glasgow, Glasgow, United Kingdom.
⁵ Organisms and Ecosystems, Earlham Institute, Norwich, United Kingdom.
⁶ Department of Paediatric Gastroenterology, Hepatology and Nutrition, Royal Hospital for Children and Young People, Edinburgh, United Kingdom.
⁷ Department of Paediatric Gastroenterology, Hepatology and Nutrition, Royal Hospital for Children, Glasgow, United Kingdom; Department of Child Health, Division of Clinical and Molecular Medicine, School of Medicine, University of Dundee, Dundee, United Kingdom.
⁸ Human Nutrition, School of Medicine, University of Glasgow, Glasgow Royal Infirmary, Glasgow, United Kingdom. Electronic address: Konstantinos.gerasimidis@glasgow.ac.uk.

Abstract

Background: Predicting response to exclusive enteral nutrition (EEN) in active Crohn's disease (CD) could lead to therapy personalization and pretreatment optimization.

Objectives: This study aimed to explore the ability of pretreatment parameters to predict fecal calprotectin (FCal) levels at EEN completion in a prospective study in children with CD.

Methods: In children with active CD, clinical parameters, dietary intake, cytokines, inflammation-related blood proteomics, and diet-related metabolites, metabolomics and microbiota in feces, were measured before initiation of 8 wk of EEN. Prediction of FCal levels at EEN completion was performed using machine learning. Data are presented with medians (IQR).

Results: Of 37 patients recruited, 15 responded (FCal < 250 μg/g) to EEN (responders) and 22 did not (nonresponders). Clinical and immunological parameters were not associated with response to EEN. Responders had lesser (μmol/g) butyrate [responders: 13.2 (8.63-18.4) compared with nonresponders: 22.3 (12.0-32.0); P = 0.03], acetate [responders: 49.9 (46.4-68.4) compared with nonresponders: 70.4 (57.0-95.5); P = 0.027], phenylacetate [responders: 0.175 (0.013-0.611) compared with nonresponders: 0.943 (0.438-1.35); P = 0.021], and a higher microbiota richness [315 (269-347) compared with nonresponders: 243 (205-297); P = 0.015] in feces than nonresponders. Responders consumed (portions/1000 kcal/d) more confectionery products [responders: 0.55 (0.38-0.72) compared with nonresponders: 0.19 (0.01-0.38); P = 0.045]. A multicomponent model using fecal parameters, dietary data, and clinical and immunological parameters predicted response to EEN with 78% accuracy (sensitivity: 80%; specificity: 77%; positive predictive value: 71%; negative predictive value: 85%). Higher taxon abundance from Ruminococcaceae, Lachnospiraceae, and Bacteroides and phenylacetate, butyrate, and acetate were the most influential variables in predicting lack of response to EEN.

Conclusions: We identify microbial signals and diet-related metabolites in feces, which could comprise targets for pretreatment optimization and personalized nutritional therapy in pediatric CD.

Keywords: Crohn’s disease; cytokines; exclusive enteral nutrition; metabolome; microbiome; o'link; precision therapy; short chain fatty acids.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Acetates
Butyrates
Child
Crohn Disease* / metabolism
Crohn Disease* / therapy
Enteral Nutrition
Humans
Metabolome
Microbiota*
Phenylacetates
Prospective Studies
Remission Induction

Substances

Butyrates
Acetates
Phenylacetates