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http://hdl.handle.net/10553/21773
Título: | The nuclear receptor LXR modulates interleukin-18 levels in macrophages through multiple mechanisms | Autores/as: | Pourcet, Benoit Gage, Matthew C. León, Theresa E. Waddington, Kirsty E. Pello, Oscar M. Steffensen, Knut R. Castrillo Viguera, Antonio Valledor, Annabel F. Pineda-Torra, Inés |
Clasificación UNESCO: | 3206 Ciencias de la nutrición 230219 Procesos metabólicos |
Palabras clave: | Liver X-Receptor Sequence-Binding-Protein Gamma-Inducing Factor Gene-Expression Ifn-Gamma, et al. |
Fecha de publicación: | 2016 | Publicación seriada: | Scientific Reports | Resumen: | IL-18 is a member of the IL-1 family involved in innate immunity and inflammation. Deregulated levels of IL-18 are involved in the pathogenesis of multiple disorders including inflammatory and metabolic diseases, yet relatively little is known regarding its regulation. Liver X receptors or LXRs are key modulators of macrophage cholesterol homeostasis and immune responses. Here we show that LXR ligands negatively regulate LPS-induced mRNA and protein expression of IL-18 in bone marrowderived macrophages. Consistent with this being an LXR-mediated process, inhibition is abolished in the presence of a specific LXR antagonist and in LXR-deficient macrophages. Additionally, IL-18 processing of its precursor inactive form to its bioactive state is inhibited by LXR through negative regulation of both pro-caspase 1 expression and activation. Finally, LXR ligands further modulate IL-18 levels by inducing the expression of IL-18BP, a potent endogenous inhibitor of IL-18. This regulation occurs via the transcription factor IRF8, thus identifying IL-18BP as a novel LXR and IRF8 target gene. In conclusion, LXR activation inhibits IL-18 production through regulation of its transcription and maturation into an active pro-inflammatory cytokine. This novel regulation of IL-18 by LXR could be applied to modulate the severity of IL-18 driven metabolic and inflammatory disorders. | URI: | http://hdl.handle.net/10553/21773 | ISSN: | 2045-2322 | DOI: | 10.1038/srep25481 | Fuente: | Scientific Reports [ISSN 2045-2322], v. 6 (article number 25481) | Derechos: | by-nc-nd |
Colección: | Artículos |
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