Butyrate Driven Raft Disruption Trots off Enteric Pathogen Invasion: Possible Mechanism of Colonization Resistance

Overview

Journal Gut Pathog

Publisher Biomed Central

Specialty Gastroenterology

Date 2023 Apr 21

PMID 37085870

Authors

Oishika Das

Aaheli Masid

Mainak Chakraborty

Animesh Gope

Shanta Dutta

Moumita Bhaumik

Affiliations

Soon will be listed here.

Abstract

The gut microbiome derived short chain fatty acids perform multitude of functions to maintain gut homeostasis. Here we studied how butyrate stymie enteric bacterial invasion in cell using a simplistic binary model. The surface of the mammalian cells is enriched with microdomains rich in cholesterol that are known as rafts and act as entry points for pathogens. We showed that sodium butyrate treated RAW264.7 cells displayed reduced membrane cholesterol and less cholera-toxin B binding coupled with increased membrane fluidity compared to untreated cells indicating that reduced membrane cholesterol caused disruption of lipid rafts. The implication of such cellular biophysical changes on the invasion of enteric pathogenic bacteria was assessed. Our study showed, in comparison to untreated cells, butyrate-treated cells significantly reduced the invasion of Shigella and Salmonella, and these effects were found to be reversed by liposomal cholesterol treatment, increasing the likelihood that the rafts' function against bacterial invasion. The credence of ex vivo studies found to be in concordance in butyrate fed mouse model as evident from the significant drift towards a protective phenotype against virulent enteric pathogen invasion as compared to untreated mice. To produce a cytokine balance towards anti-inflammation, butyrate-treated mice produced more of the gut tissue anti-inflammatory cytokine IL-10 and less of the pro-inflammatory cytokines TNF-α, IL-6, and IFN-γ. In histological studies of Shigella infected gut revealed a startling observation where number of neutrophils infiltration was noted which was correlated with the pathology and was essentially reversed by butyrate treatment. Our results ratchet up a new dimension of our understanding how butyrate imparts resistance to pathogen invasion in the gut.

Citing Articles

The impact of butyrate on group B -induced intestinal barrier disruption.

Dominguez K, Pearah A, Lindon A, Worthington L, Carter R, John-Lewis Edwards N Infect Immun. 2024; 92(10):e0020024.

PMID: 39133019 PMC: 11475668. DOI: 10.1128/iai.00200-24.

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