| Literature DB >> 24049737 |
Kathryn E Davis1, Michael D Neinast, Kai Sun, William M Skiles, Jessica D Bills, Jordan A Zehr, Daniel Zeve, Lisa D Hahner, Derek W Cox, Lana M Gent, Yong Xu, Zhao V Wang, Sohaib A Khan, Deborah J Clegg.
Abstract
Our data demonstrate that estrogens, estrogen receptor-α (ERα), and estrogen receptor-β (ERβ) regulate adipose tissue distribution, inflammation, fibrosis, and glucose homeostasis, by determining that αERKO mice have increased adipose tissue inflammation and fibrosis prior to obesity onset. Selective deletion of adipose tissue ERα in adult mice using a novel viral vector technology recapitulated the findings in the total body ERα null mice. Generation of a novel mouse model, lacking ERα specifically from adipocytes (AdipoERα), demonstrated increased markers of fibrosis and inflammation, especially in the males. Additionally, we found that the beneficial effects of estrogens on adipose tissue require adipocyte ERα. Lastly, we determined the role of ERβ in regulating inflammation and fibrosis, by breeding the AdipoERα into the βERKO background and found that in the absence of adipocyte ERα, ERβ has a protective role. These data suggest that adipose tissue and adipocyte ERα protects against adiposity, inflammation, and fibrosis in both males and females.Entities:
Keywords: BAT, brown adipose tissue; ERα, estrogen receptor alpha; ERβ, estrogen receptor beta; Estrogen receptor alpha (ERα); Fibrosis; Inflammation; WAT, white adipose tissue; White adipose tissue (WAT)
Year: 2013 PMID: 24049737 PMCID: PMC3773827 DOI: 10.1016/j.molmet.2013.05.006
Source DB: PubMed Journal: Mol Metab ISSN: 2212-8778 Impact factor: 7.422