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Publication : Sirt6 deletion in hepatocytes increases insulin sensitivity of female mice by enhancing ERĪ± expression.

First Author  Tang C Year  2019
Journal  J Cell Physiol Volume  234
Issue  10 Pages  18615-18625
PubMed ID  30912134 Mgi Jnum  J:290982
Mgi Id  MGI:6443468 Doi  10.1002/jcp.28500
Citation  Tang C, et al. (2019) Sirt6 deletion in hepatocytes increases insulin sensitivity of female mice by enhancing ERalpha expression. J Cell Physiol 234(10):18615-18625
abstractText  Sirtuin 6 (Sirt6), a NAD(+) -dependent protein deacetylase, is involved in hepatic glucose metabolism and insulin sensitivity, which impact metabolic homeostasis. In this paper, we discover that Sirt6 affects the insulin sensitivity of mice in a gender-dependent manner; few studies have been conducted on this issue. Based on reports revealing the influences of sex hormones on insulin signaling, this investigation explores the mechanism by which Sirt6 regulates the estrogen pathway and disrupts insulin signal transduction. Hepatocyte-specific Sirt6 knockout (Sirt6HKO) mice were generated to investigate the function of Sirt6 in hepatocytes. Mice were castrated or spayed to eliminate sex hormones. Insulin sensitivity was assessed via an insulin tolerance test (ITT) in vivo. The interaction of Sirt6 with the estrogen pathway and their impacts on insulin signal transduction were revealed by immunoblot and immunoprecipitation. Sirt6 deletion in hepatocytes significantly enhanced insulin sensitivity and signal transduction in female mice but not in male or spayed female mice as demonstrated by ITT and the phosphorylation level of Akt in the liver. We also identified upregulation of p300, ERalpha, and interaction of ERalpha with p85 in the liver of female Sirt6HKO mice. Additionally, Sirt6 was found to inhibit ERalpha protein stability in a p300-dependent manner without interacting directly with ERalpha. Our findings show that hepatic Sirt6 downregulates the ERalpha protein level in a p300-dependent manner and thus disturbs estrogen-induced improvement in insulin sensitivity in the liver, which may partially explain the gender difference in insulin sensitivity.
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