Issue 13, 2024

Musculus senhousei peptides alleviated alcoholic liver injury via the gut–liver axis

Abstract

Alcoholic liver injury has become a leading threat to human health, with complicated pathogenesis and limited therapeutic options. Our previous study showed that Musculus senhousei peptides (MSPs) exhibit protective potential against early-stage alcoholic liver injury, although the underlying mechanism is not yet clear. In this study, histopathological analysis, mRNA abundance of injury-associated biomarkers, the gut microbiota, and faecal metabolome were evaluated using a mouse model subjected to acute alcohol exposure, aiming to identify the mechanism by which MSP can alleviate alcoholic hepatotoxicity. The results showed that MSP intervention significantly ameliorated symptoms of liver injury (suppressed serum ALT increment, hepatic lipid accumulation, and neutrophil infiltration in liver tissue), and reversed the abnormal mRNA abundance of biomarkers associated with oxidative stress (iNOS), inflammation (TNF-α, IL-1β, MCP-1, TNF-R1, and TLR4), and apoptosis (Bax and Casp. 3) in the liver. Moreover, MSP improved intestinal barrier function by increasing the expression of tight junction proteins (Claudin-1 and Claudin-3). Further analysis of faecal microbiota and metabolome revealed that MSP promoted the growth of tryptophan-metabolizing bacteria (Clostridiales, Alistipes, and Odoribacter), leading to increased production of indole derivatives (indole-3-lactic acid and N-acetyltryptophan). These results suggested that MSPs may alleviate alcohol-induced liver injury targeting the gut–liver axis, and could be an effective option for the prevention of alcoholic liver injury.

Graphical abstract: Musculus senhousei peptides alleviated alcoholic liver injury via the gut–liver axis

Supplementary files

Article information

Article type
Paper
Submitted
05 Mar 2024
Accepted
24 May 2024
First published
29 May 2024

Food Funct., 2024,15, 7124-7135

Musculus senhousei peptides alleviated alcoholic liver injury via the gut–liver axis

C. Xiao, R. Jia, X. Li, M. Zhao, W. Liao, S. Zhao, F. Xu and F. Toldrá, Food Funct., 2024, 15, 7124 DOI: 10.1039/D4FO01070A

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