Genetic rescue of nonclassical ERα signaling normalizes energy balance in obese Erα-null mutant mice
Cheryl J. Park, … , J. Larry Jameson, Jon E. Levine
Cheryl J. Park, … , J. Larry Jameson, Jon E. Levine
Published January 18, 2011
Citation Information: J Clin Invest. 2011;121(2):604-612. https://doi.org/10.1172/JCI41702.
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Genetic rescue of nonclassical ERα signaling normalizes energy balance in obese Erα-null mutant mice

Abstract

In addition to its role in reproduction, estradiol-17β is critical to the regulation of energy balance and body weight. Estrogen receptor α–null (Erα–/–) mutant mice develop an obese state characterized by decreased energy expenditure, decreased locomotion, increased adiposity, altered glucose homeostasis, and hyperleptinemia. Such features are reminiscent of the propensity of postmenopausal women to develop obesity and type 2 diabetes. The mechanisms by which ERα signaling maintains normal energy balance, however, have remained unclear. Here we used knockin mice that express mutant ERα that can only signal through the noncanonical pathway to assess the role of nonclassical ERα signaling in energy homeostasis. In these mice, we found that nonclassical ERα signaling restored metabolic parameters dysregulated in Erα–/– mutant mice to normal or near-normal values. The rescue of body weight and metabolic function by nonclassical ERα signaling was mediated by normalization of energy expenditure, including voluntary locomotor activity. These findings indicate that nonclassical ERα signaling mediates major effects of estradiol-17β on energy balance, raising the possibility that selective ERα agonists may be developed to reduce the risks of obesity and metabolic disturbances in postmenopausal women.

Authors

Cheryl J. Park, Zhen Zhao, Christine Glidewell-Kenney, Milos Lazic, Pierre Chambon, Andrée Krust, Jeffrey Weiss, Deborah J. Clegg, Andrea Dunaif, J. Larry Jameson, Jon E. Levine

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Figure 3

Leptin, but not E2, activates STAT3.

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Leptin, but not E2, activates STAT3. (A) Representative Western blot...
(A) Representative Western blot analysis of pSTAT3 and STAT3 in MBH of Erα+/+ mice 30 and 60 minutes after injection with leptin and EB, respectively. (B) Representative images of leptin-induced pSTAT3 immunoreactivity in the ARC of Erα+/+, Erα–/–, and Erα–/AA mice 30 minutes after vehicle or leptin injection. Scale bar: 100 μm. (C) The number of leptin-induced pSTAT3-ir cells was significantly lower in Erα–/– mice (***P < 0.001 versus Erα+/+ and Erα–/AA; n = 5–8). (D) In 4- to 6-week-old Erα+/+, Erα–/–, and Erα–/AA mice, there were no differences in the number of leptin-induced pSTAT3-ir cells in the ARC (n = 4–6).