Sex differences in glucoprivic regulation of glycogen metabolism in hypothalamic primary astrocyte cultures: Role of estrogen receptor signaling

被引:10
|
作者
Ibrahim, Mostafa M. H. [1 ]
Bheemanapally, Khaggeswar [1 ]
Sylvester, Paul W. [1 ]
Briski, Karen P. [1 ]
机构
[1] Univ Louisiana Monroe, Coll Pharm, Sch Basic Pharmaceut & Toxicol Sci, 356 Bienville Bldg,1800 Bienville Dr, Monroe, LA 71201 USA
关键词
Estrogen receptor-beta; G protein-coupled estrogen receptor; Glycogen synthase; Glycogen phosphorylase; 5 '-AMP-Activated protein kinase; Glucoprivation; Glycogen; ACTIVATED PROTEIN-KINASE; NEUROPROTECTIVE ACTIONS; PROGESTERONE SYNTHESIS; GLUCOSE DEPRIVATION; ESTRADIOL;
D O I
10.1016/j.mce.2020.111000
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Hypoglycemia causes sex-reliant changes in hypothalamic astrocyte glycogen metabolism in vivo. The role of nuclear versus membrane astrocyte estrogen receptors (ER) in glucoprivic regulation of glycogen is unclear. Here, primary hypothalamic astrocyte cultures were treated with selective ER antagonists during glucoprivation to investigate the hypothesis that ER mediate sex-specific glycogen responses to glucoprivation. Results show that glucoprivic down-regulation of glycogen synthase expression is mediated by transmembrane G protein-coupled ER-1 (GPER) signaling in each sex and estrogen receptor (ER)-beta (ER beta) activity in females. Glucoprivic inhibition of glycogen phosphorylase involves GPER and ERp in females, but ER-independent mechanisms in males. GPER, ER beta, and ER-alpha (ER alpha) inhibit or stimulate AMPK protein expression in male versus female astrocytes, respectively. Glucoprivic augmentation of phospho-AMPK profiles in male glia was opposed by GPER activation, whereas GPER and ER beta suppress this protein in females. Astrocyte ER alpha and GPER content was downregulated in each sex during glucose deficiency, whereas ER beta levels was unaltered (males) or increased (females). Glucoprivation correspondingly elevated or diminished male versus female astrocyte glycogen content; ER antagonism reversed this response in males, but not females. Results identify distinctive ER variants involved in sex-similar versus sex-specific astrocyte protein responses to withdrawal of this substrate fuel. Notably, glucoprivation elicits a directional switch or gain-of-effect of GPER and ER beta on specific glial protein profiles. Outcomes infer that ERs are crucial for glucoprivic regulation of astrocyte glycogen accumulation in males. Alternatively, estradiol may act independently of ER signaling to disassemble this reserve in females.
引用
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页数:10
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