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The nuclear receptor REV- ERB α represses the transcription of growth/differentiation factor 10 and 15 genes in rat endometrium stromal cells.

Authors :
Zhao, Lijia
Isayama, Keishiro
Chen, Huatao
Yamauchi, Nobuhiko
Shigeyoshi, Yasufumi
Hashimoto, Seiichi
Hattori, Masa‐aki
Source :
Physiological Reports; Feb2016, Vol. 4 Issue 2, pn/a-N.PAG, 16p
Publication Year :
2016

Abstract

Cellular oscillators in the uterus play critical roles in the gestation processes of mammals through entraining of the clock proteins to numerous downstream genes, including growth/differentiation factor ( Gdf) 10 and Gdf15. The expression of Gdf10 and Gdf15 is significantly increased in the uterus during decidualization, but the mechanism underlying the regulation of Gdf gene expression in the uterus is poorly understood. Here, we focused on the function of the cellular oscillators in the expression of Gdf family by using uterine endometrial stromal cells ( UESCs) isolated from pregnant Per2- dLuc transgenic rats. A significant decline of Per2- dLuc bioluminescence activity was induced in in vitro decidualized UESCs, and concomitantly the expression of canonical clock genes was downregulated. Conversely, the expression of Gdf10 and Gdf15 of the Gdf was upregulated. In UESCs transfected with Bmal1-specific si RNA, in which Rev-erbα expression was downregulated, Gdf10 and Gdf15 were upregulated. However, Gdf5, Gdf7, and Gdf11 were not significantly affected by Bmal1 silencing. The expression of Gdf10 and Gdf15 was enhanced after treatment with a REV- ERB α antagonist in the presence or absence of progesterone. Chromatin immunoprecipitation- PCR analysis revealed the inhibitory effect of REV- ERB α on the expression of Gdf10 and Gdf15 in UESCs by recognizing their gene promoters. Collectively, our findings indicate that the attenuation of REV- ERB α leads to an upregulation of Gdf10 and Gdf15 in decidual cells, in which cellular oscillators are impaired. Our results provide novel evidence regarding the functions of cellular oscillators regulating the expression of downstream genes during the differentiation of UESCs. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
2051817X
Volume :
4
Issue :
2
Database :
Complementary Index
Journal :
Physiological Reports
Publication Type :
Academic Journal
Accession number :
112507653
Full Text :
https://doi.org/10.14814/phy2.12663