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大鼠催乳素基因的雌激素反应性需要Pit-1和雌激素受体两者。

Both Pit-1 and the estrogen receptor are required for estrogen responsiveness of the rat prolactin gene.

作者信息

Day R N, Koike S, Sakai M, Muramatsu M, Maurer R A

机构信息

Department of Physiology and Biophysics, University of Iowa, Iowa City 52242.

出版信息

Mol Endocrinol. 1990 Dec;4(12):1964-71. doi: 10.1210/mend-4-12-1964.

Abstract

To examine the functional relationship between distinct cis-active elements within the distal enhancer region of the rat PRL gene, we have used deletional and mutational analysis of that region in transient transfection studies in GH3 pituitary tumor cells. Results from these studies demonstrate that the region of the PRL distal enhancer containing the Pit-1-binding sites is critical not only for enhancer activity and the response to cAMP, but also for the response to estradiol. An interaction of the estrogen receptor with factors conferring basal enhancer activity is suggested by studies with a mutant distal enhancer region in which the PRL estrogen response element was converted to a palindromic estrogen response element. To directly examine potential interactions, cotransfection studies using PRL distal enhancer reporter gene constructs and expression vectors for Pit-1 and rat estrogen receptor were performed in two heterologous cell lines. The activity of the reporter gene under the control of the PRL distal enhancer linked to either the thymidine kinase promoter or the PRL proximal promoter was not significantly altered by cotransfection with the Pit-1 expression vector in COS-1 or RAT-1 cells. Coexpression of these reporter constructs and an expression vector for estrogen receptor resulted in only a slight response to estradiol. However, when both Pit-1 and estrogen receptor were cotransfected with the distal enhancer reporter gene, a marked induction was observed in response to estradiol, and this activity was dependent upon the concentration of the Pit-1 expression vector.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

为了研究大鼠催乳素(PRL)基因远端增强子区域内不同顺式作用元件之间的功能关系,我们在GH3垂体瘤细胞的瞬时转染研究中对该区域进行了缺失和突变分析。这些研究结果表明,PRL远端增强子中包含Pit-1结合位点的区域不仅对增强子活性和对cAMP的反应至关重要,而且对雌二醇的反应也很关键。对一个突变的远端增强子区域的研究表明,雌激素受体与赋予基础增强子活性的因子之间存在相互作用,在该突变区域中,PRL雌激素反应元件被转化为回文雌激素反应元件。为了直接检测潜在的相互作用,我们在两种异源细胞系中进行了共转染研究,使用PRL远端增强子报告基因构建体以及Pit-1和大鼠雌激素受体的表达载体。在COS-1或RAT-1细胞中,与Pit-1表达载体共转染后,与胸苷激酶启动子或PRL近端启动子相连的PRL远端增强子控制下的报告基因活性没有明显改变。这些报告构建体与雌激素受体表达载体的共表达仅导致对雌二醇的轻微反应。然而,当Pit-1和雌激素受体都与远端增强子报告基因共转染时,观察到对雌二醇有明显的诱导作用,并且这种活性取决于Pit-1表达载体的浓度。(摘要截短于250字)

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