| Literature DB >> 28063598 |
Teresa C Rice1, Stephanie M Armocida1, Joshua W Kuethe1, Emily F Midura1, Ayushi Jain1, David A Hildeman2, Daniel P Healy3, Erich Gulbins4, Charles C Caldwell5.
Abstract
Following burn injury, a key factor for patients susceptible to opportunistic infections is immune suppression. Butyrate levels are important in maintaining a functional immune system and these levels can be altered after injury. The acid sphingomyelinase (Asm) lipid signaling system has been implicated in a T cell actions with some evidence of being influenced by butyrate. Here, we hypothesized that burn-injury changes in butyrate levels would mediate Asm activity and, consequently, T cell homeostasis. We demonstrate that burn injury temporally decreases butyrate levels. We further determined that T cell Asm activity is increased by butyrate and decreased after burn injury. We additionally observed decreased T cell numbers in Asm-deficient, burn-injured, and microbiota-depleted mice. Finally, we demonstrate that butyrate reduced T cell death in an Asm-dependent manner. These data suggest that restoration of butyrate after burn injury may ameliorate the T cell lost observed in burn-injured patients by Asm regulation.Entities:
Keywords: Acid sphingomyelinase; Apoptosis; Burn injury; Butyrate; T cells
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Year: 2016 PMID: 28063598 PMCID: PMC5559081 DOI: 10.1016/j.cellimm.2016.12.004
Source DB: PubMed Journal: Cell Immunol ISSN: 0008-8749 Impact factor: 4.868