Hormone replacement therapy for postmenopausal atherosclerosis is offset by late age iron deposition

Postmenopausal atherosclerosis (AS) has been attributed to estrogen deficiency. However, the beneficial effect of hormone replacement therapy (HRT) is lost in late postmenopausal women with atherogenesis. We asked whether aging-related iron accumulation affects estrogen receptor α (ERα) expression,...

Full description

Saved in:
Bibliographic Details
Published in:eLife 2023-08, Vol.12
Main Authors: Xu, Tianze, Cai, Jing, Wang, Lei, Xu, Li, Zhao, Hongting, Wang, Fudi, Meyron-Holtz, Esther G, Missirlis, Fanis, Qiao, Tong, Li, Kuanyu
Format: Article
Language:English
Subjects:
17β-Estradiol
Aging
Angiogenesis
Apolipoprotein E
Arteriosclerosis
Atherogenesis
Atherosclerosis
Cardiovascular disease
Cell Biology
Cell culture
Chelation
Cholesterol
Down-regulation
estrogen receptor α
Estrogen receptors
Estrogens
Females
Genetic engineering
Homeostasis
Hormone replacement therapy
Iron
iron metabolism
Kinases
Lipids
MDM2 protein
Menopause
Metabolism
Ovariectomy
Post-menopause
Proteins
Proteolysis
Ubiquitin-protein ligase
Womens health
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Postmenopausal atherosclerosis (AS) has been attributed to estrogen deficiency. However, the beneficial effect of hormone replacement therapy (HRT) is lost in late postmenopausal women with atherogenesis. We asked whether aging-related iron accumulation affects estrogen receptor α (ERα) expression, thus explaining HRT inefficacy. A negative correlation has been observed between aging-related systemic iron deposition and ERα expression in postmenopausal AS patients. In an ovariectomized mouse model, estradiol treatment had contrasting effects on ERα expression in early versus late postmenopausal mice. ERα expression was inhibited by iron treatment in cell culture and iron-overloaded mice. Combined treatment with estradiol and iron further decreased ERα expression, and the latter effect was mediated by iron-regulated E3 ligase Mdm2. In line with these observations, cellular cholesterol efflux was reduced, and endothelial homeostasis was disrupted. Consequently, AS was aggravated. Accordingly, systemic iron chelation attenuated estradiol-triggered progressive AS in late postmenopausal mice. Thus, iron and estradiol together downregulate ERα through Mdm2-mediated proteolysis, providing a potential explanation for failures of HRT in late postmenopausal subjects with aging-related iron accumulation. This study suggests that immediate HRT after menopause, along with appropriate iron chelation, might provide benefits from AS.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.80494