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复杂的调控相互作用控制促肾上腺皮质激素释放激素(CRH)基因的表达。

Complex regulatory interactions control CRH gene expression.

作者信息

Nicholson Richard C, King Bruce R, Smith Roger

机构信息

Mothers and Babies Research Centre, Hunter Medical Research Institute, University of Newcastle, NSW 2310, Australia.

出版信息

Front Biosci. 2004 Jan 1;9:32-9. doi: 10.2741/1204.

Abstract

Glucocorticoids inhibit corticotrophin releasing hormone (CRH) production in the hypothalamus but stimulate production from the placenta. To identify key elements regulating the CRH gene, mouse pituitary tumor-derived cells (AtT20 cells) were used as a hypothalamic model in an analysis of the CRH promoter. Two cAMP responsive elements were identified: (I) a consensus cAMP response element (CRE) and (II) a previously unrecognized caudal-type homeobox response element (CDXRE). Glucocorticoids inhibit only the component of cAMP-stimulation occurring via the CRE through an action involving a negative glucocorticoid response element (nGRE). We also identified two regions that, in the absence of the nGRE, can be stimulated by glucocorticoids: (I) the CRE and (II) a region between -213 to -99bps. Electrophoretic mobility shift assays identified binding of the transcription factors CREB and Fos at the CRE in AtT20 cells, whereas CREB and cJun were detected in placental cells. In addition, a novel CRE-binding transcription factor has been identified that is expressed in the brain and in placenta. A model is presented whereby CRH gene regulation is mediated via tissue specific expression of transcription factors.

摘要

糖皮质激素可抑制下丘脑促肾上腺皮质激素释放激素(CRH)的产生,但会刺激胎盘产生CRH。为了确定调节CRH基因的关键元件,在对CRH启动子的分析中,将小鼠垂体肿瘤衍生细胞(AtT20细胞)用作下丘脑模型。鉴定出了两个cAMP反应元件:(I)一个共有cAMP反应元件(CRE)和(II)一个先前未被识别的尾型同源框反应元件(CDXRE)。糖皮质激素仅通过涉及负糖皮质激素反应元件(nGRE)的作用抑制经由CRE发生的cAMP刺激成分。我们还鉴定出了两个区域,在没有nGRE的情况下,它们可被糖皮质激素刺激:(I)CRE和(II)-213至-99碱基对之间的区域。电泳迁移率变动分析确定了转录因子CREB和Fos在AtT20细胞的CRE处结合,而在胎盘细胞中检测到了CREB和cJun。此外,还鉴定出了一种新型的CRE结合转录因子,其在脑和胎盘中表达。提出了一种模型,即CRH基因调控是通过转录因子的组织特异性表达介导的。

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