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首页> 外文期刊>Peptides: An International Journal >Orexins/hypocretins increase the promoter activity of selective steroidogenic enzymes.
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Orexins/hypocretins increase the promoter activity of selective steroidogenic enzymes.

机译:食欲素/ hypocretins增加选择性类固醇生成酶的启动子活性。

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Orexins (hypocretins) regulate multiple physiological functions, including central regulation of energy homeostasis and sleep-wake behavior but also peripheral hormonal actions. Recent data suggest specific effects of orexins at adrenal glands. To further assess the mechanism by which orexins regulate steroidogenesis we analyzed the effect of orexin A and B on the transcriptional activity of the luciferase reporter gene driven by the human steroid 21-hydroxylase (CYP21), 3beta-hydroxysteroid dehydrogenase (HSD3B2), 11beta-hydroxylase (CYP11B1), and aldosterone synthase (CYP11B2) gene promoter regions. After transient transfection of the reporter gene constructs into human NCI H295R cells, treatment with orexin A and B for 6 and 12h increased the promoter activity of the CYP11B2, HSD3B2 and, to a lesser extend, CYP21 genes. The activity of the CYP11B1 was increased by both orexins after 3h of treatment. Compared to the effects of forskolin or angiotensin II, however, the effect of orexins on the transcriptional activity of the steroidogenic enzyme genes was moderate. Our results suggest that orexins increase the expression of steroidogenic enzymes at the transcriptional level and that orexins play a role in the long term regulation of adrenal steroid production.
机译:食欲素(hypocretins)调节多种生理功能,包括能量稳态和睡眠觉醒行为的中央调节,以及周围激素的作用。最近的数据表明食欲素对肾上腺的特定作用。为了进一步评估orexin调节类固醇生成的机制,我们分析了orexin A和B对人类固醇21-羟化酶(CYP21),3beta-羟基类固醇脱氢酶(HSD3B2),11beta-羟化酶(CYP11B1)和醛固酮合酶(CYP11B2)基因启动子区域。在将报告基因构建体瞬时转染到人NCI H295R细胞后,用orexin A和B处理6h和12h可增加CYP11B2,HSD3B2和CYP21基因的启动子活性。在治疗3小时后,两种orexins均增加了CYP11B1的活性。但是,与福司可林或血管紧张素II的作用相比,食欲素对类固醇生成酶基因转录活性的作用中等。我们的结果表明,orexins在转录水平上增加了类固醇生成酶的表达,并且orexins在肾上腺类固醇产生的长期调节中起作用。

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