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首页> 外文期刊>International journal of molecular medicine >Identification of a new p53 responsive element in the promoter region of anillin
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Identification of a new p53 responsive element in the promoter region of anillin

机译:鉴定Anillin启动子区的新P53响应元件

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摘要

The expression of anillin mRNA and protein is regulated in a cell cycle-dependent manner. However, the mechanism underlying this process is unclear. Previous studies analyzing the sequence of the 5 ' -untranslated region of anillin have unveiled several putative p53 binding sites. Therefore, the present study hypothesized that the anillin gene may be repressed by p53 and that the commonly observed mutation (or loss of function) of p53 may serve a role in this phenotype. Bioinformatic analysis of the anillin promoter region revealed potential p53 responsive elements. Of those identified, 2 were able to bind p53 protein, as determined via a chromatin immunoprecipitation assay. Although it was hypothesized that DNA damage and resultant p53 expression would repress anillin expression, the results revealed that anillin mRNA and protein expression levels were negatively regulated by DNA damage in the wild-type p53 cells, but not in the isogenic p53 null cells. Furthermore, DNA sequences encompassing the p53 binding site downregulated luciferase transgenes in a p53 dependent manner. Taken together, these data indicated that anillin was negatively regulated by p53 and that anillin overexpression observed in cancer may be a p53-mediated phenomenon. The data from the present study provided further evidence for the role of p53 in the biologically crucial process of cytokinesis.
机译:以细胞周期依赖性方式调节anillin mRNA和蛋白的表达。然而,这个过程的基础尚不清楚。以前的研究分析了anillin的5' - 淘汰区域的序列已经推出了几个推定的P53结合位点。因此,本研究假设Anillin基因可以通过P53抑制,并且P53的常见突变(或功能丧失)可以在该表型中发挥作用。 Anillin启动子区域的生物信息分析显示潜在的P53响应元件。其中鉴定的那些,2能够通过染色质免疫沉淀测定法测定p53蛋白。虽然假设DNA损伤和结果P53表达将抑制亚麻酸肽表达,但结果表明,在野生型P53细胞中的DNA损伤,但不在中源P53含量细胞中的DNA损伤负调节Anillin mRNA和蛋白质表达水平。此外,DNA序列包括P53结合位点以p53依赖性方式下调荧光素酶转基因。占据,这些数据表明,Anillin受P53负调节,并且在癌症中观察到的Anillin过表达可能是p53介导的现象。本研究中的数据提供了P53在细胞因子的生物学关键过程中的作用的进一步证据。

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