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Early growth response protein 1 acts as an activator of SOX18 promoter

机译:早期生长反应蛋白1充当SOX18启动子的激活剂

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摘要

Sex-determining region Y box 18 (Sox18/SOX18) gene is an important regulator of vascular development playing a role in endothelial cell specification or differentiation, angiogenesis and atherogenesis. The aim of this study was to perform comprehensive functional characterization of the human SOX18 promoter, including determination of transcription start point (tsp) and identification of control elements involved in the regulation of SOX18 gene expression, with an emphasis on angiogenesis-related transcription factors. Analyses were performed in HeLa cells, representing a tumor cell line, and in EA.hy926 cells used as an endothelial model system. We have determined unique tsp of SOX18 gene, located 172 nucleotides upstream from ATG codon. Further, we have shown that SOX18 promoter region, -726 to -89 bp relative to tsp, contains positive cis-regulatory element(s) that stimulates SOX18 promoter activity, while region -89 to + 166 represents the minimal promoter. Within this region we have recognized the presence of essential element(s), positioned from -89 to +29, which harbors cluster of three putative early growth response 1 (EGR1) binding sites. By in vitro binding assays and functional analyses we have shown that these three putative binding sites are functionally relevant and sufficient for EGR1-induced SOX18 transcription. Mutations of these binding sites significantly impaired activity of the SOX18 promoter, particularly in EA.hy926 cells, indicating the importance of these regulatory elements for SOX18 promoter activity in endothelial setting. By data presented in this study, we have established SOX18 as a novel target gene regulated by EGR1 transcription factor, thus providing the first functional link between two transcription factors previously shown to be involved in the control of angiogenesis.
机译:性别决定区Y box 18(Sox18 / SOX18)基因是重要的血管发育调节因子,在内皮细胞规格或分化,血管生成和动脉粥样硬化中发挥作用。这项研究的目的是对人类SOX18启动子进行全面的功能表征,包括确定转录起点(tsp)和鉴定参与SOX18基因表达调控的控制元件,重点是与血管生成相关的转录因子。在代表肿瘤细胞系的HeLa细胞中以及在用作内皮模型系统的EA.hy926细胞中进行了分析。我们确定了独特的tsp的SOX18基因,位于ATG密码子上游172个核苷酸处。此外,我们已经显示,相对于tsp的-726至-89 bp的SOX18启动子区域包含刺激SOX18启动子活性的正顺式调控元件,而-89至+ 166区域代表最小启动子。在这个区域内,我们已经认识到必需元素的存在,其位置介于-89至+29之间,具有三个推定的早期生长响应1(EGR1)结合位点。通过体外结合测定和功能分析,我们已经表明这三个推定的结合位点在功能上相关并且足以用于EGR1诱导的SOX18转录。这些结合位点的突变显着损害了SOX18启动子的活性,特别是在EA.hy926细胞中,表明这些调节元件对内皮设置中SOX18启动子活性的重要性。根据这项研究中提供的数据,我们已经将SOX18建立为受EGR1转录因子调控的新型靶基因,从而提供了先前证明参与血管生成控制的两个转录因子之间的第一个功能联系。

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