| Literature DB >> 22210316 |
Robin Winkler1, Verena Benz, Markus Clemenz, Mandy Bloch, Anna Foryst-Ludwig, Sami Wardat, Nicole Witte, Manuela Trappiel, Pawel Namsolleck, Knut Mai, Joachim Spranger, Gabriele Matthias, Tim Roloff, Oliver Truee, Kai Kappert, Michael Schupp, Patrick Matthias, Ulrich Kintscher.
Abstract
In the current study, we investigated the importance of histone deacetylase (HDAC)6 for glucocorticoid receptor-mediated effects on glucose metabolism and its potential as a therapeutic target for the prevention of glucocorticoid-induced diabetes. Dexamethasone-induced hepatic glucose output and glucocorticoid receptor translocation were analyzed in wild-type (wt) and HDAC6-deficient (HDAC6KO) mice. The effect of the specific HDAC6 inhibitor tubacin was analyzed in vitro. wt and HDAC6KO mice were subjected to 3 weeks' dexamethasone treatment before analysis of glucose and insulin tolerance. HDAC6KO mice showed impaired dexamethasone-induced hepatic glucocorticoid receptor translocation. Accordingly, dexamethasone-induced expression of a large number of hepatic genes was significantly attenuated in mice lacking HDAC6 and by tubacin in vitro. Glucose output of primary hepatocytes from HDAC6KO mice was diminished. A significant improvement of dexamethasone-induced whole-body glucose intolerance as well as insulin resistance in HDAC6KO mice compared with wt littermates was observed. This study demonstrates that HDAC6 is an essential regulator of hepatic glucocorticoid-stimulated gluconeogenesis and impairment of whole-body glucose metabolism through modification of glucocorticoid receptor nuclear translocation. Selective pharmacological inhibition of HDAC6 may provide a future therapeutic option against the prodiabetogenic actions of glucocorticoids.Entities:
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Year: 2011 PMID: 22210316 PMCID: PMC3266407 DOI: 10.2337/db11-0313
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461