The Role of Foxo3 in Leydig Cells.
10.3349/ymj.2015.56.6.1590
- Author:
Young Suk CHOI
1
;
Joo Eun SONG
;
Byung Soo KONG
;
Jae Won HONG
;
Silvia NOVELLI
;
Eun Jig LEE
Author Information
1. Endocrinology, Institute of Endocrine Research, Brain Korea 21 PLUS Project for Medical Science and Yonsei University College of Medicine, Seoul, Korea. EJLEE423@yuhs.ac
- Publication Type:Original Article ; Research Support, Non-U.S. Gov't
- Keywords:
Foxo3;
Leydig cell;
testosterone;
StAR
- MeSH:
Animals;
Cell Aging/*physiology;
Cell Nucleus/metabolism;
Cytoplasm/metabolism;
Forkhead Transcription Factors/*metabolism;
HEK293 Cells;
Humans;
Leydig Cells/*drug effects/*enzymology/metabolism;
Luteinizing Hormone/blood;
Male;
Mice;
Phosphatidylinositol 3-Kinases;
Phosphoproteins/metabolism;
Phosphorylation;
Signal Transduction/drug effects;
Testosterone/blood/*metabolism
- From:Yonsei Medical Journal
2015;56(6):1590-1596
- CountryRepublic of Korea
- Language:English
-
Abstract:
PURPOSE: Foxo3 in female reproduction has been reported to regulate proliferation of granulose cells that form follicles. There are no reports so far that discuss on the role of Foxo3 in males. This study was designed to outline the role of Foxo3 in the testes. MATERIALS AND METHODS: Testes from mice at birth to postpartum week (PPW) 5 were isolated and examined for the expression of Foxo3 using immunostaining. To elucidate role of Foxo3 in Leydig cells, R2C cells were treated with luteinizing hormone (LH) and the phosphorylation of Foxo3. Testosterone and steroidogenic acute regulatory (StAR) protein levels were measured after constitutive active [triple mutant (TM)] human FOXO3 adenovirus was transduced and StAR promoter assay was performed. RESULTS: Foxo3 expression in the testicles started from birth and lasted until PPW 3. After PPW 3, most Foxo3 expression occurred in the nuclei of Leydig cells; however, at PPW 5, Foxo3 was expressed in both the nucleus and cytoplasm. When R2C cells were treated with luteinizing hormone, Foxo3 phosphorylation levels by AKT increased. After blocking the PI3K pathway, LH-induced phosphorylated Foxo3 levels decreased, indicating that LH signaling regulates Foxo3 localization. When active FOXO3-TM adenovirus was introduced into a Leydig tumor cell line, the concentrations of testosterone and StAR protein decreased. When FOXO3 and a StAR promoter vector were co-transfected into HEK293 cells for a reporter assay, FOXO3 inhibited the StAR promoter. CONCLUSION: FOXO3 affects testosterone synthesis by inhibiting the formation of StAR protein. LH hormone, meanwhile, influences Foxo3 localization, mediating its function.
