Glycolipids Promote Virulence by Thwarting Immune Cell Clearance

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2024 May 29

PMID 38809989

Authors

Luke R Joyce

Sol Kim

Brady L Spencer

Priya M Christensen

Kelli L Palmer

Ziqiang Guan

Julie A Siegenthaler

Kelly S Doran

Affiliations

Soon will be listed here.

Abstract

[group B (GBS)] is a leading cause of neonatal meningitis, with late-onset disease (LOD) occurring after gastrointestinal tract colonization in infants. Bacterial membrane lipids are essential for host-pathogen interactions, and the functions of glycolipids are yet to be fully elucidated. GBS synthesizes three major glycolipids: glucosyl-diacylglycerol (Glc-DAG), diglucosyl-DAG (Glc-DAG), and lysyl-Glc-DAG (Lys-Glc-DAG). Here, we identify the enzyme, IagB, as responsible for biosynthesis of Glc-DAG, the precursor for the two other glycolipids in GBS. To examine the collective role of glycolipids to GBS virulence, we adapted a murine model of neonatal meningitis to simulate LOD. The GBS∆ mutant traversed the gut-epithelial barrier comparable to wild type but was severely attenuated in bloodstream survival, resulting in decreased bacterial loads in the brain. The GBS∆ mutant was more susceptible to neutrophil killing and membrane targeting by host antimicrobial peptides. This work reveals an unexplored function of GBS glycolipids with their ability to protect the bacterial cell from host antimicrobial killing.

Citing Articles

Identification of two glycosyltransferases required for synthesis of membrane glycolipids in .

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PMID: 39964170 PMC: 11898633. DOI: 10.1128/mbio.03512-24.

Identification of two glycosyltransferases required for synthesis of membrane glycolipids in .

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Identification of Glyoxalase A in Group B and its contribution to methylglyoxal tolerance and virulence.

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PMID: 39131367 PMC: 11312555. DOI: 10.1101/2024.07.30.605887.

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