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Nouveaux mécanismes physiopathologiques du Syndrome Métabolique: implication des récepteurs nucléaires orphelins?

Auteurs : Kuhn E1, Fève B, Lombès M
Affiliations : 1Inserm U693, 94276 le Kremlin Bicêtre, France.
Date 2012 Octobre, Vol 73 Suppl 1, pp S9-16Revue : Annales d'endocrinologieType de publication : article de périodique; revue de la littérature; DOI : 10.1016/S0003-4266(12)70010-0
Résumé

This review focuses on a number of new data on biology and pathophysiology of the metabolic syndrome (MetS) and the involvement of nuclear receptors that have been presented during the last Endocrine Society meeting, held in Houston in June 2012. Several studies have reported beneficial effects of various orphan nuclear receptors, including SHP (Small Heterodimeric Partner, NR0B2) and LXR (Liver X Receptor, NR1H3 and NR1H2), on various components of MetS. By using an inactivation model of SHP, David Moore has shown that SHP exerts "antidiabetic" effects but associated with hepatic steatosis development. He also showed that DLPC (dilauroyl phosphatidylcholine), an unconventional phospholipid, exhibited anti-diabetic properties through its binding to LRH-1 (Liver Receptor Homolog-1, NR5A2), a molecular partner of SHP. Interestingly, Carolyn Cummins investigated LXR α and β isoforms knock-out mice and provided experimental evidence for the detailed mechanisms involved in the deleterious metabolic effects of glucocorticoids, pointing out to the functional interaction between LXRβ, and the glucocorticoid receptor. These new and original studies open new therapeutic opportunities for the management of metabolic disorders in humans by selective modulators of these receptors.

 Source : MEDLINE©/Pubmed© U.S National Library of Medicine
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Kuhn E, Fève B, Lombès M. Nouveaux mécanismes physiopathologiques du Syndrome Métabolique: implication des récepteurs nucléaires orphelins?. Ann. Endocrinol. (Paris). 2012 Oct;73 Suppl 1:S9-16.
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Dernière date de mise à jour : 29/08/2017.


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