Icariin, a phytoestrogen, exerts rapid estrogenic actions through crosstalk of estrogen receptors in osteoblasts

Ka-Ying Wong, Tsz Hung Kong, Chui Wa Christina Poon, Wenxuan Yu, Liping Zhou (Corresponding Author), Man Sau Wong (Corresponding Author)

Research output: Journal article publicationJournal articleAcademic researchpeer-review

5 Citations (Scopus)

Abstract

Icariin, a flavonoid glycoside derived from Epimedium brevicornum Maxim, exerts bone protective effects via estrogen receptors (ERs). This study aimed to investigate the role of ER-α66, ER-α36, and GPER in bone metabolism in osteoblasts following treatment with icariin. Human osteoblastic MG-63 cells and osteoblast-specific ER-α66 knockout mice were employed. The ERs crosstalk in the estrogenic action of icariin was evaluated in ER-α66-negative human embryonic kidney HEK293 cells. Icariin, like E2, regulated ER-α36 and GPER protein expression in osteoblasts by downregulating them and upregulating ER-α66. ER-α36 and GPER suppressed the actions of icariin and E2 in bone metabolism. However, the in vivo administration of E2 (2 mg/kg/day) or icariin (300 mg/kg/day) restored bone conditions in KO osteoblasts. ER-α36 and GPER expression increased significantly and rapidly activated and translocated in KO osteoblasts after treatment with E2 or icariin. ER-α36 overexpression in KO osteoblasts further promoted the OPG/RANKL ratio induced by E2 or icariin
treatment. This study showed icariin and E2 elicit rapid estrogenic responses in bone
through recruiting ER-α66, ER-α36, and GPER. Notably, in osteoblasts lacking ERα66, ER-α36, and GPER mediate the estrogenic effects of icariin and E2, while in intact osteoblasts, ER-α36 and GPER act as negative regulators of ER-α66.
Original languageEnglish
Pages (from-to)4706-4721
Number of pages16
JournalPhytotherapy Research
Volume37
Issue number10
DOIs
Publication statusPublished - 8 Jul 2023

Keywords

  • estradio
  • estrogen receptors
  • icariin
  • natural product
  • osteoblast
  • receptor crosstalk

ASJC Scopus subject areas

  • Pharmacology

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