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首页> 外文期刊>Endocrinology >Regulation of steroidogenic acute regulatory protein transcription in largemouth bass by orphan nuclear receptor signaling pathways.
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Regulation of steroidogenic acute regulatory protein transcription in largemouth bass by orphan nuclear receptor signaling pathways.

机译:通过孤核受体信号传导通路调节大口黑鲈中类固醇生成的急性调节蛋白转录。

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摘要

The steroidogenic acute regulatory (StAR) protein mediates the rate-limiting step of mitochondrial transport of cholesterol for steroid biosynthesis. To investigate the regulation of this protein in lower vertebrates, we cloned the StAR coding region from large-mouth bass for analysis. Induction of the mRNA corresponded with increasing levels of plasma sex steroids in vivo. Cultures of largemouth bass ovarian follicles were exposed to dibutyryl cAMP (dbcAMP), a potent signaling molecule for steroidogenesis. StAR mRNA expression was significantly up-regulated by dbcAMP signaling, suggesting that the 5' regulatory region of the gene is functionally conserved. To further analyze its transcriptional regulation, a 2.9-kb portion of the promoter was cloned and transfected into Y-1 cells, a steroidogenic mouse adrenocortical cell line. The promoter activity was induced in a dose-responsive manner upon stimulation with dbcAMP; however, deletion of 1 kb from the 5' end of the promoter segment significantly diminished the transcriptional activation. A putative retinoic acid-related receptor-alpha/rev-erb alpha element was identified between the -1.86- and -2.9-kb region and mutated to assess its potential role in dbcAMP regulation of the promoter. Mutation of the rev-erb alpha element significantly impeded dbcAMP-induced activation. Chromatin immunoprecipitation and EMSA results revealed rev-erb alpha and retinoic acid-related receptor-alpha enrichment at the site under basal and dbcAMP-induced conditions, respectively. These results implicate important roles for these proteins previously uncharacterized for the StAR promoter. Altogether these data suggest novel regulatory mechanisms for dbcAMP up-regulation of StAR transcription in the distal part of the largemouth bass promoter.
机译:类固醇生成的急性调节蛋白(StAR)介导胆固醇的线粒体运输速率限制步骤,以进行类固醇生物合成。为了研究这种蛋白质在低等脊椎动物中的调控,我们从大嘴鲈中克隆了StAR编码区进行分析。 mRNA的诱导与体内血浆性类固醇水平的升高相对应。大嘴鲈鱼卵泡培养物暴露于二丁酰cAMP(dbcAMP),这是类固醇生成的有效信号分子。 dbcAMP信号转导显着上调了StAR mRNA的表达,表明该基因的5'调控区在功能上是保守的。为了进一步分析其转录调控,克隆了一个2.9kb的启动子,并将其转染到Y-1细胞(一种类固醇生成的小鼠肾上腺皮质细胞系)中。 dbcAMP刺激后以剂量反应方式诱导启动子活性。然而,从启动子节段的5'端缺失1 kb会大大减少转录激活。推定的视黄酸相关受体α/ rev-erbα元素被确定在-1.86和-2.9-kb区域之间,并进行突变以评估其在启动子的dbcAMP调节中的潜在作用。 rev-erb alpha元素的突变显着阻碍了dbcAMP诱导的激活。染色质免疫沉淀和EMSA结果分别显示在基础和dbcAMP诱导的条件下,rev-erbα和视黄酸相关受体α富集。这些结果暗示了以前对于StAR启动子而言尚未表征的这些蛋白质的重要​​作用。总而言之,这些数据表明在大口黑鲈启动子的远端,dbcAMP上调StAR转录的新调控机制。

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