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. 2025 Jun 18;73(24):15199-15214.
doi: 10.1021/acs.jafc.5c01674. Epub 2025 Jun 6.

Advanced Microbiome Therapeutics Accelerate MASLD Recovery by Restoring Intestinal Microbiota Equilibrium and the Gut-Liver Axis in a Mouse Model

Johnson Lok  1 Congjia Chen  2 Valeria Iannone  1 Ambrin Farizah Babu  1   3 Emily Kwun Kwan Lo  2 Ruben Vazquez-Uribe  4   5 Troels Holger Vaaben  4 Mikko Kettunen  6 Otto Savolainen  1   7 Ursula Schwab  1   8 Morten Otto Alexander Sommer  4 Kati Hanhineva  1   3   9 Marjukka Kolehmainen  1 Hani El-Nezami  1   2 Carlos Gómez-Gallego  1
Affiliations

Advanced Microbiome Therapeutics Accelerate MASLD Recovery by Restoring Intestinal Microbiota Equilibrium and the Gut-Liver Axis in a Mouse Model

Johnson Lok et al. J Agric Food Chem. .

Abstract

Gut microbiota dysbiosis and endocrine dysregulation are key players in metabolic dysfunction-associated steatotic liver disease (MASLD) development. This study evaluated whether advanced microbiome therapeutics can restore intestinal microbial equilibrium and gut-liver axis balance during MASLD recovery. MASLD was induced in mice using a high-fat, high-sugar diet, and then shifted to a standard diet, where intervention groups received engineered Escherichia coli Nissle 1917 expressing IGF1 (EcNI) or aldafermin (EcNA), and control groups received E. coli Nissle 1917 vehicle (EcN) or no microbial intervention (CTRL). EcNI and EcNA improved MASLD recovery compared to controls by lowering hepatic fat, plasma cholesterol, and body weight, while increasing bacterial diversity, plasma acetate, and propionate, and modulating particular microbial groups, potentially alleviating dysbiosis. Additionally, EcNI and EcNA downregulated acetyl-CoA, the steroid hormone biosynthesis pathway, and EcNA upregulated the pentose phosphate pathway and pyruvate, which are related to oxidative stress reduction. These results suggest that EcNI and EcNA are potential novel treatments for MASLD.

Keywords: E. coli Nissle 1917; aldafermin; fibroblast growth factor 19; insulin-like growth factor 1; integrative multiomics; nonalcoholic fatty liver disease (NAFLD).

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