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配对结构域转录因子Pax8与大鼠钠/碘同向转运体基因的上游增强子结合,并参与甲状腺特异性转录和环磷酸腺苷依赖性转录。

The paired-domain transcription factor Pax8 binds to the upstream enhancer of the rat sodium/iodide symporter gene and participates in both thyroid-specific and cyclic-AMP-dependent transcription.

作者信息

Ohno M, Zannini M, Levy O, Carrasco N, di Lauro R

机构信息

Stazione Zoologica 'Anton Dohrn', 80121 Naples, Italy.

出版信息

Mol Cell Biol. 1999 Mar;19(3):2051-60. doi: 10.1128/MCB.19.3.2051.

Abstract

The gene encoding the Na/I symporter (NIS) is expressed at high levels only in thyroid follicular cells, where its expression is regulated by the thyroid-stimulating hormone via the second messenger, cyclic AMP (cAMP). In this study, we demonstrate the presence of an enhancer that is located between nucleotides -2264 and -2495 in the 5'-flanking region of the NIS gene and that recapitulates the most relevant aspects of NIS regulation. When fused to either its own or a heterologous promoter, the NIS upstream enhancer, which we call NUE, stimulates transcription in a thyroid-specific and cAMP-dependent manner. The activity of NUE depends on the four most relevant sites, identified by mutational analysis. The thyroid-specific transcription factor Pax8 binds at two of these sites. Mutations that interfere with Pax8 binding also decrease transcriptional activity of the NUE. Furthermore, expression of Pax8 in nonthyroid cells results in transcriptional activation of NUE, strongly suggesting that the paired-domain protein Pax8 plays an important role in NUE activity. The NUE responds to cAMP in both protein kinase A-dependent and -independent manners, indicating that this enhancer could represent a novel type of cAMP responsive element. Such a cAMP response requires Pax8 but also depends on the integrity of a cAMP responsive element (CRE)-like sequence, thus suggesting a functional interaction between Pax8 and factors binding at the CRE-like site.

摘要

编码钠/碘同向转运体(NIS)的基因仅在甲状腺滤泡细胞中高水平表达,在该细胞中其表达由促甲状腺激素通过第二信使环磷酸腺苷(cAMP)进行调控。在本研究中,我们证明在NIS基因5'侧翼区核苷酸-2264至-2495之间存在一个增强子,该增强子概括了NIS调控的最相关方面。当与自身或异源启动子融合时,我们称为NUE的NIS上游增强子以甲状腺特异性和cAMP依赖性方式刺激转录。NUE的活性取决于通过突变分析确定的四个最相关位点。甲状腺特异性转录因子Pax8结合其中两个位点。干扰Pax8结合的突变也会降低NUE的转录活性。此外,Pax8在非甲状腺细胞中的表达导致NUE的转录激活,强烈表明配对结构域蛋白Pax8在NUE活性中起重要作用。NUE以蛋白激酶A依赖性和非依赖性方式对cAMP作出反应,表明该增强子可能代表一种新型的cAMP反应元件。这种cAMP反应需要Pax8,但也取决于类似cAMP反应元件(CRE)序列的完整性,因此提示Pax8与在类似CRE位点结合的因子之间存在功能相互作用。

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