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核因子与体细胞细胞色素c启动子中多个位点的相互作用。上游NRF-1、ATF及内含子Sp1识别序列的特征分析。

Interaction of nuclear factors with multiple sites in the somatic cytochrome c promoter. Characterization of upstream NRF-1, ATF, and intron Sp1 recognition sequences.

作者信息

Evans M J, Scarpulla R C

机构信息

Department of Molecular Biology, Northwestern University Medical School, Chicago, Illinois 60611.

出版信息

J Biol Chem. 1989 Aug 25;264(24):14361-8.

PMID:2547796
Abstract

The rat somatic cytochrome c promoter is resolved into a mosaic of cis-acting upstream and intron elements required for maximal activity. Mutations in each diminished cytochrome c promoter activity and eliminated the specific binding of cognate nuclear factors. Among these is the recognition sequence for a nuclear factor designated NRF-1 (nuclear respiratory factor 1) also found in the upstream regions of several other nuclear genes whose products function in the mitochondria. The NRF-1 site was tightly coupled to a second functionally independent element (region I), and together these sites constitute a major determinant of cytochrome c expression. In addition to these novel sequence elements, the promoter also contained recognition sites for the common transcriptional activators ATF and Sp1. A potent promoter element within the first intron consisted of two adjacent Sp1 binding sites. Point mutations in the first site eliminated the promoter activity of the element as well as Sp1 binding to both sites. An ATF recognition sequence in the upstream promoter was identical to an authentic cyclic AMP (cAMP) responsive element in stimulating promoter activity and in conferring a cAMP response upon a heterologous promoter. These promoter elements and their cognate nuclear factors likely contribute to the housekeeping function of cytochrome c and to the coordinate modulation of respiratory gene expression according to cellular energy demands.

摘要

大鼠体细胞细胞色素c启动子可分解为多个顺式作用的上游元件和内含子元件,这些元件共同作用以实现最大活性。每个元件发生突变都会降低细胞色素c启动子的活性,并消除同源核因子的特异性结合。其中包括一种名为NRF-1(核呼吸因子1)的核因子的识别序列,该序列也存在于其他几个在线粒体中发挥作用的核基因的上游区域。NRF-1位点与第二个功能独立的元件(区域I)紧密相连,这些位点共同构成了细胞色素c表达的主要决定因素。除了这些新的序列元件外,该启动子还包含常见转录激活因子ATF和Sp1的识别位点。第一个内含子中的一个强效启动子元件由两个相邻的Sp1结合位点组成。第一个位点的点突变消除了该元件的启动子活性以及Sp1与两个位点的结合。上游启动子中的一个ATF识别序列在刺激启动子活性以及赋予异源启动子cAMP反应方面与真正的环磷酸腺苷(cAMP)反应元件相同。这些启动子元件及其同源核因子可能有助于细胞色素c的管家功能,并根据细胞能量需求对呼吸基因表达进行协调调节。

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