Gut microbiome-derived glycine lipids are diet-dependent modulators of hepatic injury and atherosclerosis

Courtney L Millar,Liya Anto,Chelsea Garcia,Mi-Bo Kim,Anisha Jain,Anthony A Provatas,Robert B Clark,Ji-Young Lee,Frank C Nichols,Christopher N Blesso

doi:10.1016/j.jlr.2022.100192

Abstract

Oral and gut Bacteroidetes produce unique classes of serine-glycine lipodipeptides and glycine aminolipids that signal through host Toll-like receptor 2. These glycine lipids have also been detected in human arteries, but their effects on atherosclerosis are unknown. Here, we sought to investigate the bioactivity of bacterial glycine lipids in mouse models of atherosclerosis. Lipid 654 (L654), a serine-glycine lipodipeptide species, was first tested in a high-fat diet (HFD)-fed Ldlr−/− model of atherosclerosis. Intraperitoneal administration of L654 over 7 weeks to HFD-fed Ldlr−/− mice resulted in hypocholesterolemic effects and significantly attenuated the progression of atherosclerosis. We found that L654 also reduced liver inflammatory and extracellular matrix gene expression, which may be related to inhibition of macrophage activation as demonstrated in vivo by lower major histocompatibility complex class II gene expression and confirmed in cell experiments. In addition, L654 and other bacterial glycine lipids in feces, liver, and serum were markedly reduced alongside changes in Bacteroidetes relative abundance in HFD-fed mice. Finally, we tested the bioactivities of L654 and related lipid 567 in chow-fed Apoe−/− mice, which displayed much higher fecal glycine lipids relative to HFD-fed Ldlr−/− mice. Administration of L654 or lipid 567 for 7 weeks to these mice reduced the liver injury marker alanine aminotransferase, but other effects seen in Ldlr−/− were not observed. Therefore, we conclude that conditions in which gut microbiome-derived glycine lipids are lost, such as HFD, may exacerbate the development of atherosclerosis and liver injury, whereas correction of such depletion may protect from these disorders.

Highlights

Supplementary key words liver dietary fat cholesterol heart inflammation high-fat diet lipid 654 (L654) lipid 567 (L567) alanine aminotransferase mouse models Bacteroidetes Bacteroidota uconn.edu
Since the gene ontology of RNA sequencing (RNA-Seq) liver data indicated that differentially expressed genes were enriched in phagosomerelated pathways and major histocompatibility complex (MHC) class II-related gene expression, we examined if bacterial glycine lipids modulated macrophage activation and induction of MHC class II genes, H2aa and H2eb1, in RAW264.7 murine macrophages
Despite evidence suggesting that L654 and other glycine lipids activate TLR2 signaling, we report here protective effects against hepatic inflammation and atherosclerosis with chronic exposure, in high-fat diet (HFD) conditions where fecal and serum glycine lipids are reduced

Summary

Introduction

Besides the well-known role of lipopolysaccharide (LPS) in Toll-like receptor (TLR) activation, emerging classes of gut microbiota-derived lipids relevant to inflammation-related disease are the glycine lipids first identified in P. gingivalis and found to be broadly expressed in the Bacteroidetes phylum [11–13]. These unique classes of bacterial lipids signal through TLR2 and include the glycine amino lipid species, lipid 342 (L342) and lipid 567 (L567) [12], named for their negative ion mass, as well as the serine-glycine lipodipeptides, lipid 430 (L430), lipid 654 (L654), and lipid 1256 (L1256) (Fig. 1A) [11, 13].

Methods

Results

Conclusion