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Publication : G-protein-coupled receptor 84 regulates acute inflammation in normal and diabetic skin wounds.

First Author  Cooper PO Year  2024
Journal  Cell Rep Volume  43
Issue  6 Pages  114288
PubMed ID  38814782 Mgi Jnum  J:357565
Mgi Id  MGI:7665946 Doi  10.1016/j.celrep.2024.114288
Citation  Cooper PO, et al. (2024) G-protein-coupled receptor 84 regulates acute inflammation in normal and diabetic skin wounds. Cell Rep 43(6):114288
abstractText  Lipids have emerged as potent regulators of immune cell function. In the skin, adipocyte lipolysis increases the local pool of free fatty acids and is essential for coordinating early macrophage inflammation following injury. Here, we investigate G-protein-coupled receptor 84 (GPR84), a medium-chain fatty acid (MCFA) receptor, for its potential to propagate pro-inflammatory signaling after skin injury. GPR84 signaling was identified as a key component of regulating myeloid cell numbers and subsequent tissue repair through in vivo administration of a pharmacological antagonist and the MCFA decanoic acid. We found that impaired injury-induced dermal adipocyte lipolysis is a hallmark of diabetes, and lipidomic analysis demonstrated that MCFAs are significantly reduced in diabetic murine wounds. Furthermore, local administration of decanoic acid rescued myeloid cell numbers and tissue repair during diabetic wound healing. Thus, GPR84 is a readily targetable lipid signaling pathway for manipulating injury-induced tissue inflammation with beneficial effects on acute diabetic healing.
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