A Lipidomics- and Transcriptomics-Based Analysis of the Intestine of Genetically Obese (ob/ob) and Diabetic (db/db) Mice: Links with Inflammation and Gut Microbiota

Author:

Suriano Francesco12ORCID,Manca Claudia34ORCID,Flamand Nicolas3ORCID,Van Hul Matthias12ORCID,Delzenne Nathalie M.1ORCID,Silvestri Cristoforo34ORCID,Cani Patrice D.12ORCID,Di Marzo Vincenzo345ORCID

Affiliation:

1. Metabolism and Nutrition Research Group, Louvain Drug Research Institute (LDRI), UCLouvain, Université Catholique de Louvain, Av. E. Mounier, 73 B1.73.11, 1200 Brussels, Belgium

2. Walloon Excellence in Life Sciences and BIOtechnology (WELBIO), WELBIO Department, WEL Research Institute, Avenue Pasteur, 6, 1300 Wavre, Belgium

3. Quebec Heart and Lung Institute Research Centre, Université Laval, Quebec City, QC G1V 0A6, Canada

4. Institute of Nutrition and Functional Foods, Centre NUTRISS, Université Laval, Quebec City, QC G1V 0A6, Canada

5. Joint International Research Unit for Chemical and Biomolecular Research on the Microbiome and Its Impact on Metabolic Health and Nutrition (JIRU-MicroMeNu) between Université Laval and the Italian Consiglio Nazionale delle Ricerche, Institute of Biomolecular Chemistry, Consiglio Nazionale delle Ricerche, 80078 Pozzuoli, Italy

Abstract

Obesity is associated with a cluster of metabolic disorders, chronic low-grade inflammation, altered gut microbiota, increased intestinal permeability, and alterations of the lipid mediators of the expanded endocannabinoid (eCB) signaling system, or endocannabinoidome (eCBome). In the present study, we characterized the profile of the eCBome and related oxylipins in the small and large intestines of genetically obese (ob/ob) and diabetic (db/db) mice to decipher possible correlations between these mediators and intestinal inflammation and gut microbiota composition. Basal lipid and gene expression profiles, measured by LC/MS-MS-based targeted lipidomics and qPCR transcriptomics, respectively, highlighted a differentially altered intestinal eCBome and oxylipin tone, possibly linked to increased mRNA levels of inflammatory markers in db/db mice. In particular, the duodenal levels of several 2-monoacylglycerols and N-acylethanolamines were increased and decreased, respectively, in db/db mice, which displayed more pronounced intestinal inflammation. To a little extent, these differences were explained by changes in the expression of the corresponding metabolic enzymes. Correlation analyses suggested possible interactions between eCBome/oxylipin mediators, cytokines, and bacterial components and bacterial taxa closely related to intestinal inflammation. Collectively, this study reveals that db/db mice present a higher inflammatory state in the intestine as compared to ob/ob mice, and that this difference is associated with profound and potentially adaptive or maladaptive, and partly intestinal segment-specific alterations in eCBome and oxylipin signaling. This study opens the way to future investigations on the biological role of several poorly investigated eCBome mediators and oxylipins in the context of obesity and diabetes-induced gut dysbiosis and inflammation.

Funder

Fonds de la Recherche Scientifique

Projet de Recherche PDR-convention

La Caixa

WoM Lundgren grant

Publisher

MDPI AG

Subject

General Medicine

Reference34 articles.

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