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NR5A1和NR5A2在人颗粒细胞中通过Clock基因和骨形态发生蛋白调节类固醇生成中的作用。

Roles of NR5A1 and NR5A2 in the regulation of steroidogenesis by Clock gene and bone morphogenetic proteins by human granulosa cells.

作者信息

Suyama Atsuhito, Iwata Nahoko, Soejima Yoshiaki, Nakano Yasuhiro, Yamamoto Koichiro, Nada Takahiro, Otsuka Fumio

机构信息

Department of General Medicine, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Okayama 700-8558, Japan.

出版信息

Endocr J. 2021 Nov 29;68(11):1283-1291. doi: 10.1507/endocrj.EJ21-0223. Epub 2021 Jun 26.

Abstract

The functional role of the transcription factors NR5A1 and NR5A2 and their interaction with Clock gene and bone morphogenetic proteins (BMPs) were investigated in human granulosa KGN cells. Treatment with BMP-15 and GDF-9 suppressed forskolin (FSK)-induced steroidogenesis as shown by the mRNA expression levels of StAR and P450scc but not the mRNA expression level of P450arom. Of interest, treatment with BMP-15 and GDF-9 also suppressed FSK-induced NR5A2 mRNA expression. Treatment with BMP-15 suppressed NR5A2 mRNA and protein expression but increased Clock mRNA and protein expression levels by granulosa cells. The mRNA expression levels of NR5A1, but not those of NR5A2, were positively correlated with the levels of Clock mRNA, while the mRNA levels of Id-1, the target gene of BMP signaling, were positively correlated with those of NR5A1 but not with those of NR5A2. It was also demonstrated that the mRNA expression levels of NR5A1 were positively correlated with those of P450arom and 3βHSD, whereas the mRNA expression level of NR5A2 was correlated with those of StAR and P450scc. Furthermore, inhibition of Clock gene expression by siRNA attenuated the expression of NR5A1, and the mRNA levels of Clock gene were significantly correlated with those of NR5A1. Collectively, the results suggested a novel mechanism by which Clock gene expression induced by BMP-15 is functionally linked to the expression of NR5A1, whereas NR5A2 expression is suppressed by BMP-15 in granulosa cells. The interaction between Clock NR5A1/NR5A2 and BMP-15 is likely to be involved in the fine-tuning of steroidogenesis by ovarian granulosa cells.

摘要

在人颗粒细胞KGN中研究了转录因子NR5A1和NR5A2的功能作用及其与Clock基因和骨形态发生蛋白(BMP)的相互作用。如StAR和P450scc的mRNA表达水平所示,用BMP - 15和GDF - 9处理可抑制福斯可林(FSK)诱导的类固醇生成,但P450arom的mRNA表达水平不受影响。有趣的是,用BMP - 15和GDF - 9处理也抑制了FSK诱导的NR5A2 mRNA表达。用BMP - 15处理可抑制颗粒细胞中NR5A2 mRNA和蛋白表达,但增加Clock mRNA和蛋白表达水平。NR5A1的mRNA表达水平而非NR5A2的表达水平与Clock mRNA水平呈正相关,而BMP信号的靶基因Id - 1的mRNA水平与NR5A1的水平呈正相关,与NR5A2的水平无关。还证明NR5A1的mRNA表达水平与P450arom和3βHSD的表达水平呈正相关,而NR5A2的mRNA表达水平与StAR和P450scc的表达水平相关。此外,siRNA抑制Clock基因表达减弱了NR5A1的表达,并且Clock基因的mRNA水平与NR5A1的水平显著相关。总体而言,结果提示了一种新机制,即BMP - 15诱导的Clock基因表达在功能上与NR5A1的表达相关联,而颗粒细胞中BMP - 15抑制NR5A2的表达。Clock NR5A1/NR5A2与BMP - 15之间的相互作用可能参与卵巢颗粒细胞对类固醇生成的精细调节。

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