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The structure formed by inverted repeats in p53 response elements determines the transactivation activity of p53 protein

机译:在P53响应元件中反转重复形成的结构决定了p53蛋白的反膜激活活性

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摘要

The TP53 gene is the most frequently mutated gene in human cancer and p53 protein plays a crucial role in gene expression and cancer protection. Its role is manifested by interactions with other proteins and DNA. p53 is a transcription factor that binds to DNA response elements (REs). Due to the palindromic nature of the consensus binding site, several p53-REs have the potential to form cruciform structures. However, the influence of cruciform formation on the activity of p53-REs has not been evaluated. Therefore, we prepared sets of p53-REs with identical theoretical binding affinity in their linear state, but different probabilities to form extra helical structures, for in vitro and in vivo analyses. Then we evaluated the presence of cruciform structures when inserted into plasmid DNA and employed a yeast-based assay to measure transactivation potential of these p53-REs cloned at a chromosomal locus in isogenic strains. We show that transactivation in vivo correlated more with relative propensity of an RE to form cruciforms than to its predicted in vitro DNA binding affinity for wild type p53. Structural features of p53-REs could therefore be an important determinant of p53 transactivation function. (C) 2016 Elsevier Inc. All rights reserved.
机译:TP53基因是人类癌症中最常见的突变基因,P53蛋白在基因表达和癌症保护中起着至关重要的作用。其作用表现为与其他蛋白质和DNA的相互作用。 P53是与DNA响应元素(RE)结合的转录因子。由于共有粘合位点的回文性质,几个p53-res具有形成十字形结构的可能性。然而,尚未评估十字形形成对P53-RES活性的影响。因此,我们在其线性状态下制备了一组P53-Res,其具有相同的理论结合亲和力,但在体外和体内分析中形成额外螺旋结构的不同概率。然后,我们在插入质粒DNA时评估了坩埚结构的存在,并使用酵母基测定法测量在等离子体菌株的染色体轨迹处克隆这些p53-res的转移潜力。我们表明,体内的反式激活更多地与RE形成十字形的相对倾向相关,而不是其预测对野生型P53的体外DNA结合亲和力。因此,P53-Res的结构特征可以是P53转移功能的重要决定因素。 (c)2016年Elsevier Inc.保留所有权利。

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