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转录因子Sp家族对人及小鼠MUC2基因启动子的调控

The Sp family of transcription factors in the regulation of the human and mouse MUC2 gene promoters.

作者信息

Aslam F, Palumbo L, Augenlicht L H, Velcich A

机构信息

Department of Oncology, Albert Einstein Cancer Center/Montefiore Medical Center, Bronx, New York 10467, USA.

出版信息

Cancer Res. 2001 Jan 15;61(2):570-6.

Abstract

Modulation of mucin gene expression is an important component both in the early steps of colon cancer development and in later tumor progression. Previous work from our laboratory and others has suggested that the Sp family of transcription factors may play an important role in the regulation of the human MUC2 gene. To determine whether this was an essential element, we extended our work to the cloning and analysis of 3.5 kb of the 5'-flanking region of the mouse Muc2 (mMuc2) gene. Comparative analysis between the mouse and human MUC2 promoter regions has identified a strong sequence homology between the mouse and human genes, including the presence of GC-rich boxes, the location and composition of which are maintained in the mouse and human genes. We show that these GC boxes are binding sites for Sp-family transcription factors and are functionally important since mithramycin, an inhibitor of Sp1/Sp3 binding, blocks MUC2 gene expression in HT29 cells. Furthermore, by a combination of gel shift analysis and site-directed mutagenesis, we have identified the relative contribution of individual GC boxes, and of the factors they bind, to the regulation of the mouse Muc2 promoter, which appears to be different in the mouse and human genes. Finally, we demonstrate by overexpressing Sp1 and Sp3 that the functional difference between the proximal promoter region of the MUC2 gene in the two species is not attributable to differential ability of this region to bind members of the Sp family of transcription factors, but rather to the different anatomy of the individual GC boxes in the mouse and human proximal promoters.

摘要

粘蛋白基因表达的调控是结肠癌发生早期阶段以及后期肿瘤进展过程中的一个重要组成部分。我们实验室和其他研究机构之前的工作表明,转录因子Sp家族可能在人类MUC2基因的调控中发挥重要作用。为了确定这是否是一个关键因素,我们将工作扩展到对小鼠Muc2(mMuc2)基因5'侧翼区域3.5 kb的克隆和分析。小鼠和人类MUC2启动子区域之间的比较分析确定了小鼠和人类基因之间存在很强的序列同源性,包括富含GC的框的存在,其位置和组成在小鼠和人类基因中得以保留。我们发现这些GC框是Sp家族转录因子的结合位点,并且具有功能重要性,因为放线菌素D(一种Sp1/Sp3结合抑制剂)可阻断HT29细胞中的MUC2基因表达。此外,通过凝胶迁移分析和定点诱变相结合的方法,我们确定了各个GC框及其结合的因子对小鼠Muc2启动子调控的相对贡献,这在小鼠和人类基因中似乎有所不同。最后,我们通过过表达Sp1和Sp3证明,这两个物种中MUC2基因近端启动子区域的功能差异并非归因于该区域结合Sp家族转录因子成员的能力不同,而是由于小鼠和人类近端启动子中各个GC框的结构不同。

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