| Literature DB >> 32343675 |
Jennifer H Madenspacher1, Eric D Morrell2, Kymberly M Gowdy3,4, Jeffrey G McDonald5, Bonne M Thompson5, Ginger Muse1, Jennifer Martinez1, Seddon Thomas1, Carmen Mikacenic2, Jerry A Nick6, Edward Abraham7, Stavros Garantziotis1, Renee D Stapleton8, Julie M Meacham1, Mary Jane Thomassen9, William J Janssen6, Donald N Cook1, Mark M Wurfel2, Michael B Fessler1.
Abstract
Alveolar macrophages (AM) play a central role in initiation and resolution of lung inflammation, but the integration of these opposing core functions is poorly understood. AM expression of cholesterol 25-hydroxylase (CH25H), the primary biosynthetic enzyme for 25-hydroxycholesterol (25HC), far exceeds the expression of macrophages in other tissues, but no role for CH25H has been defined in lung biology. As 25HC is an agonist for the antiinflammatory nuclear receptor, liver X receptor (LXR), we speculated that CH25H might regulate inflammatory homeostasis in the lung. Here, we show that, of natural oxysterols or sterols, 25HC is induced in the inflamed lung of mice and humans. Ch25h-/- mice fail to induce 25HC and LXR target genes in the lung after LPS inhalation and exhibit delayed resolution of airway neutrophilia, which can be rescued by systemic treatment with either 25HC or synthetic LXR agonists. LXR-null mice also display delayed resolution, suggesting that native oxysterols promote resolution. During resolution, Ch25h is induced in macrophages upon their encounter with apoptotic cells and is required for LXR-dependent prevention of AM lipid overload, induction of Mertk, efferocytic resolution of airway neutrophilia, and induction of TGF-β. CH25H/25HC/LXR is, thus, an inducible metabolic axis that programs AMs for efferocytic resolution of inflammation.Entities:
Keywords: Cholesterol; Inflammation; Innate immunity; Macrophages; Pulmonology
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Year: 2020 PMID: 32343675 PMCID: PMC7308063 DOI: 10.1172/jci.insight.137189
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708