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AP2启动子的比较和功能分析表明,保守的八聚体和起始子元件对活性至关重要。

Comparative and functional analysis of the AP2 promoter indicates that conserved octamer and initiator elements are critical for activity.

作者信息

Creaser P C, D'Argenio D A, Williams T

机构信息

Department of Biology, Yale University, New Haven, CT 06520-8103, USA.

出版信息

Nucleic Acids Res. 1996 Jul 1;24(13):2597-605. doi: 10.1093/nar/24.13.2597.

Abstract

AP-2 is a developmentally-regulated transcription factor expressed in ectodermal cell lineages. The AP-2 protein is essential for neural tube, craniofacial and body wall morphogenesis and has been implicated in oncogenesis. Here we report the isolation of the AP-2 promoter from human, mouse and chicken. The initiation sites for the human gene have been mapped in a variety of cell lines, including several derived from breast tumours. Initiation occurs just upstream of an IR3-like repetitive element, present in the human and mouse genes, but absent in chicken. The cis-acting elements responsible for promoter activity in human HeLa cells have been mapped both in vivo and in vitro. The proximal promoter contains binding sites for transcription factors AP-2, NF-1 and octamer proteins, but lacks a TATA box motif. Functional analysis demonstrates that the octamer binding site is the critical component of basal promoter activity. In addition, the promoter relies on an initiator element for efficient start site utilization. There is an excellent correlation between the requirement for the initiator and octamer elements in transcription assays and the conservation of these cis-acting sequences between chicken, mouse and human.

摘要

AP-2是一种在发育过程中受到调控的转录因子,在外胚层细胞谱系中表达。AP-2蛋白对于神经管、颅面和体壁的形态发生至关重要,并且与肿瘤发生有关。在此,我们报告了从人、小鼠和鸡中分离出AP-2启动子。人类基因的起始位点已在多种细胞系中定位,包括几种源自乳腺肿瘤的细胞系。起始发生在人类和小鼠基因中存在但鸡基因中不存在的类IR3重复元件的上游。负责人类HeLa细胞中启动子活性的顺式作用元件已在体内和体外进行了定位。近端启动子包含转录因子AP-2、NF-1和八聚体蛋白的结合位点,但缺乏TATA盒基序。功能分析表明,八聚体结合位点是基础启动子活性的关键组成部分。此外,启动子依赖于起始子元件来有效利用起始位点。在转录分析中对起始子和八聚体元件的需求与鸡、小鼠和人类之间这些顺式作用序列的保守性之间存在极好的相关性。

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