Estrogen Regulates Hepcidin Expression via GPR30-BMP6-Dependent Signaling in Hepatocytes

Yasumasa Ikeda,Keisuke Ishizawa,Shuhei Tomita,Yoshitaka Kihira,Toshiaki Tamaki,Koichiro Tsuchiya,Yuki Izawa-Ishizawa,Soichiro Tajima,Carlos Hermenegildo

doi:10.1371/journal.pone.0040465

Yasumasa Ikeda, Keisuke Ishizawa + Show 7 more

Open Access

https://doi.org/10.1371/journal.pone.0040465

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Journal: PLoS ONE	Publication Date: Jul 11, 2012
Citations: 147	License type: CC BY 4.0

Affiliation: Tokushima University

Abstract

Hepcidin, a liver-derived iron regulatory protein, plays a crucial role in iron metabolism. It is known that gender differences exist with respect to iron storage in the body; however, the effects of sex steroid hormones on iron metabolism are not completely understood. We focused on the effects of the female sex hormone estrogen on hepcidin expression. First, ovariectomized (OVX) and sham-operated mice were employed to investigate the effects of estrogen on hepcidin expression in an in vivo study. Hepcidin expression was decreased in the livers of OVX mice compared to the sham-operated mice. In OVX mice, bone morphologic protein-6 (BMP6), a regulator of hepcidin, was also found to be downregulated in the liver, whereas ferroportin (FPN), an iron export protein, was upregulated in the duodenum. Both serum and liver iron concentrations were elevated in OVX mice relative to their concentrations in sham-operated mice. In in vitro studies, 17β-estradiol (E2) increased the mRNA expression of hepcidin in HepG2 cells in a concentration-dependent manner. E2-induced hepatic hepcidin upregulation was not inhibited by ICI 182720, an inhibitor of the estrogen receptor; instead, hepcidin expression was increased by ICI 182720. E2 and ICI 182720 exhibit agonist actions with G-protein coupled receptor 30 (GPR30), the 7-transmembrane estrogen receptor. G1, a GPR30 agonist, upregulated hepcidin expression, and GPR30 siRNA treatment abolished E2-induced hepcidin expression. BMP6 expression induced by E2 was abolished by GPR30 silencing. Finally, both E2 and G1 supplementation restored reduced hepatic hepcidin and BMP6 expression and reversed the augmentation of duodenal FPN expression in the OVX mice. In contrast, serum hepcidin was elevated in OVX mice, which was reversed in these mice with E2 and G1. Thus, estrogen is involved in hepcidin expression via a GPR30-BMP6-dependent mechanism, providing new insight into the role of estrogen in iron metabolism.

Highlights

Iron is an essential trace element that is necessary for all living cells and organisms
We found that hepatic hepcidin expression was downregulated in OVX mice
Estrogen played a role in hepcidin expression in a G-protein coupled receptor 30 (GPR30)-bone morphologic protein-6 (BMP6)-dependent manner in vitro

Summary

Introduction

Iron is an essential trace element that is necessary for all living cells and organisms. 3–5 g of iron is stored by healthy adults, and the amount of stored iron varies during the lifetime. It is well known that gender differences exist with respect to iron storage. Women exhibit low levels of iron storage from adolescence to menopause. Iron levels in the body increase to levels similar to those in men of the same age [1]. Lower iron storage levels in women is believed to be associated with blood loss during menstruation, which explains the increase in iron storage by women during perimenopause [2]

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