首页> 美国卫生研究院文献>Nucleic Acids Research >A unique ISRE in the TATA-less human Isg20 promoter confers IRF-1-mediated responsiveness to both interferon type I and type II
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A unique ISRE in the TATA-less human Isg20 promoter confers IRF-1-mediated responsiveness to both interferon type I and type II

机译:不含TATA的人类Isg20启动子中的独特ISRE赋予IRF-1介导的对I型和II型干扰素的反应性。

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摘要

Interferons (IFNs) encode a family of secreted proteins involved in a number of regulatory functions such as control of cell proliferation, differentiation and regulation of the immune system. Their diverse biological actions are thought to be mediated by the products of specific but usually overlapping sets of cellular genes induced in the target cells. We have recently isolated a human cDNA encoding a new nuclear bodies-associated protein (PML-NBs), which we have termed Isg20. In this report, we describe the cloning and functional characterization of the Isg20 promoter region and the identification of sequence elements and trans-acting factors implicated in its regulation. In the absence of any recognizable TATA or CAAT elements, Isg20 promoter basal activity is dependent upon the positive transcription factors Sp-1 and USF-1. Interestingly, we demonstrate that a unique interferon stimulated response element (ISRE) mediates both IFN type I and type II Isg20 induction in the absence of functional γ-activated sequence. These inductions are strictly dependent upon of the IFN regulatory factor 1 (IRF-1). In addition, we show that the ISRE is also implicated in the constitutive transcriptional activity of Isg20 gene.
机译:干扰素(IFN)编码分泌蛋白家族,涉及许多调节功能,例如控制细胞增殖,分化和调节免疫系统。人们认为它们的多种生物学作用是由在靶细胞中诱导的特定但通常重叠的细胞基因集的产物介导的。我们最近分离了一种人类cDNA,它编码一种新的核小体相关蛋白(PML-NBs),我们将其称为Isg20。在此报告中,我们描述了Isg20启动子区域的克隆和功能表征,以及涉及其调控的序列元件和反式作用因子的鉴定。在没有任何可识别的TATA或CAAT元件的情况下,Isg20启动子的基础活性取决于正转录因子Sp-1和USF-1。有趣的是,我们证明了在没有功能性γ激活序列的情况下,独特的干扰素刺激反应元件(ISRE)介导了I型和II型IFN的Isg20诱导。这些诱导严格依赖于IFN调节因子1(IRF-1)。此外,我们表明ISRE也与Isg20基因的组成型转录活性有关。

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