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Peer-reviewed veterinary case report

Single-cell RNA profiling identifies immune cell population shifts in diabetes associated mucosal inflammation.

Journal:
Mucosal immunology
Year:
2025
Authors:
Alghamdi, Bushra et al.
Affiliation:
Department of Periodontics · United States
Species:
rodent

Abstract

Poorly controlled diabetes significantly worsens periodontal disease, affecting millions worldwide, yet the mechanisms driving this destructive synergy remain unclear. We generated single-cell RNA sequencing profiles of diabetic periodontal tissue, revealing increased γT-cells, a loss of Tregs and greater neutrophil polarization as key mediators of diabetes-enhanced periodontitis. Flow cytometry confirmed significant expansion of IL-17AγT-cells and reduced Tregs in diabetic mice, with parallel findings of elevated CD3IL-17A cells and reduced Tregs in human diabetic periodontal specimens. scRNAseq determined that diabetes caused a global increase in pro-inflammatory and a decrease in pro-resolving transcripts and enhanced inflammatory neutrophil polarization. Selective γT-cell inhibition reversed diabetes-enhanced periodontal destruction while minimally affecting normoglycemic controls and returned neutrophil infiltration to normoglycemic levels. These findings point to unique aspects of diabetes-induced dysregulation, implicate γT-cells as a driving factor and point to them as a potential therapeutic target in periodontitis and other diabetic complications.

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Original publication: https://pubmed.ncbi.nlm.nih.gov/40582570/