Induction of transglutaminase 2 by a liver X receptor/retinoic acid receptor α pathway increases the clearance of apoptotic cells by human Macrophages

Cédric Rébé, Magalie Raveneau, Angélique Chevriaux, Daniela Lakomy, Anne Laure Sberna, Annie Costa, Ginette Bessède, Anne Athias, Eric Steinmetz, Jean Marc A. Lobaccaro, Georges Alves, Alexandre Menicacci, Sébastien Vachenc, Eric Solary, Philippe Gambert, David Masson

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Résumé

RAtionale: Liver X receptors (LXRs) are oxysterol-activated nuclear receptors that are involved in the control of cholesterol homeostasis and inflammatory response. Human monocytes and macrophages express high levels of these receptors and are appropriate cells to study the response to LXR agonists. objective:The purpose of this study was to identify new LXR targets in human primary monocytes and macrophages and the consequences of their activation. METHODS AND RESULTS:: We show that LXR agonists significantly increase the mRNA and protein levels of the retinoic acid receptor (RAR)α in primary monocytes and macrophages. LXR agonists promote RARα gene transcription through binding to a specific LXR response element on RARα gene promoter. Preincubation of monocytes or macrophages with LXR agonists before RARα agonist treatment enhances synergistically the expression of several RARα target genes. One of these genes encodes transglutaminase (TGM)2, a key factor required for macrophage phagocytosis. Accordingly, the combination of LXR and RARα agonists at concentrations found in human atherosclerotic plaques markedly enhances the capabilities of macrophages to engulf apoptotic cells in a TGM2-dependent manner. CONCLUSIONS:: These results indicate an important role for LXRs in the control of phagocytosis through an RARα-TGM2-dependent mechanism. A combination of LXR/RARα agonists that may operate in atherosclerosis could also constitute a promising strategy to improve the clearance of apoptotic cells by macrophages in other pathological situations.

langue originaleAnglais
Pages (de - à)393-401
Nombre de pages9
journalCirculation Research
Volume105
Numéro de publication4
Les DOIs
étatPublié - 14 août 2009
Modification externeOui

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