Hepatic overexpression of steroid sulfatase ameliorates mouse models of obesity and type 2 diabetes through sex-specific mechanisms

DOI

10.1074/jbc.M113.535914

Authors

Mengxi Jiang, University of Pittsburgh
Jinhan He, University of Pittsburgh
Heidi Kucera, University of California, Davis
Nilesh W. Gaikwad, University of California, Davis
Bin Zhang, University of Pittsburgh
Meishu Xu, University of Pittsburgh
Robert M. O'Doherty, University of Pittsburgh
Kyle W. Selcer, Duquesne University
Wen Xie, University of Pittsburgh

Document Type

Journal Article

Publication Date

3-21-2014

Publication Title

Journal of Biological Chemistry

Volume

289

Issue

12

First Page

8086

Last Page

8097

ISSN

219258

Abstract

The steroid sulfatase (STS)-mediated desulfation is a critical metabolic mechanism that regulates the chemical and functional homeostasis of endogenous and exogenous molecules. In this report, we first showed that the liver expression of Sts was induced in both the high fat diet (HFD) and ob/ob models of obesity and type 2 diabetes and during the fed to fasting transition. In defining the functional relevance of STS induction in metabolic disease, we showed that overexpression of STS in the liver of transgenic mice alleviated HFD and ob/ob models of obesity and type 2 diabetes, including reduced body weight, improved insulin sensitivity, and decreased hepatic steatosis and inflammation. Interestingly, STS exerted its metabolic benefit through sex-specific mechanisms. In female mice, STS may have increased hepatic estrogen activity by converting biologically inactive estrogen sulfates to active estrogens and consequently improved the metabolic functions, whereas ovariectomy abolished this protective effect. In contrast, the metabolic benefit of STS in males may have been accounted for by the male-specific decrease of inflammation in white adipose tissue and skeletal muscle as well as a pattern of skeletal muscle gene expression that favors energy expenditure. The metabolic benefit in male STS transgenic mice was retained after castration. Treatment with the STS substrate estrone sulfate also improved metabolic functions in both the HFD and ob/ob models. Our results have uncovered a novel function of STS in energy metabolism and type 2 diabetes. Liver-specific STS induction or estrogen/estrogen sulfate delivery may represent a novel approach to manage metabolic syndrome. © 2014 by The American Society for Biochemistry and Molecular Biology, Inc.

Open Access

Green Final

Repository Citation

Jiang, M., He, J., Kucera, H., Gaikwad, N., Zhang, B., Xu, M., O'Doherty, R., Selcer, K., & Xie, W. (2014). Hepatic overexpression of steroid sulfatase ameliorates mouse models of obesity and type 2 diabetes through sex-specific mechanisms. Journal of Biological Chemistry, 289 (12), 8086-8097. https://doi.org/10.1074/jbc.M113.535914