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位于人类c-kit癌基因转录激活位点的一个保守四链体基序。

A conserved quadruplex motif located in a transcription activation site of the human c-kit oncogene.

作者信息

Fernando Himesh, Reszka Anthony P, Huppert Julian, Ladame Sylvain, Rankin Sarah, Venkitaraman Ashok R, Neidle Stephen, Balasubramanian Shankar

机构信息

Department of Chemistry, University of Cambridge, Lensfield Road, Cambridge, CB2 1EW, United Kingdom.

出版信息

Biochemistry. 2006 Jun 27;45(25):7854-60. doi: 10.1021/bi0601510.

Abstract

The c-kit gene encodes a receptor tyrosine kinase, whose engagement by its ligand triggers signals leading to cell proliferation. c-kit activity is elevated in gastrointestinal stromal tumors (GISTs), and its therapeutic inhibition by small molecules such as imatinib is clinically validated. We identified a putative quadruplex forming 21-nucleotide sequence upstream of the c-kit transcription initiation site (c-kit21), on the G-rich strand, which occupies a site required for core promoter activity. Here, we show by nuclear magnetic resonance (NMR), circular dichroism (CD), and ultraviolet (UV) spectroscopic methods that c-kit21 forms quadruplexes under physiological conditions. Mutational analysis of c-kit21 has provided insights into its structural polymorphism. In particular, one mutated form appears to form a single quadruplex species that adopts a parallel conformation. The quadruplex-forming sequence shows a high level of sequence conservation across human, mouse, rat, and chimpanzee. The small variation in sequence between the quadruplex in human/chimpanzee as compared to the rat/mouse was examined more closely by biophysical methods. Despite a variation in the sequence and length of loop 2, the quadruplexes showed both comparable CD spectra, indicative of parallel quadruplexes, and also similar thermal-stability profiles, suggesting conservation of biophysical characteristics. Collectively, the evidence suggests that this quadruplex is a serious target for a detailed functional investigation at the cell-biology level.

摘要

c-kit基因编码一种受体酪氨酸激酶,其配体与之结合会触发导致细胞增殖的信号。c-kit活性在胃肠道间质瘤(GISTs)中升高,并且其被伊马替尼等小分子的治疗性抑制在临床上得到了验证。我们在c-kit转录起始位点(c-kit21)上游的富含G的链上鉴定出一个假定的形成四链体的21核苷酸序列,该序列占据核心启动子活性所需的位点。在这里,我们通过核磁共振(NMR)、圆二色性(CD)和紫外(UV)光谱方法表明,c-kit21在生理条件下形成四链体。对c-kit21的突变分析为其结构多态性提供了见解。特别是,一种突变形式似乎形成了一种采用平行构象的单一四链体物种。形成四链体的序列在人类、小鼠、大鼠和黑猩猩中显示出高度的序列保守性。通过生物物理方法更仔细地研究了人类/黑猩猩与大鼠/小鼠四链体之间序列的微小差异。尽管环2的序列和长度存在差异,但四链体显示出可比的CD光谱,表明是平行四链体,并且还具有相似的热稳定性谱,这表明生物物理特性具有保守性。总的来说,证据表明这种四链体是细胞生物学水平详细功能研究的一个重要靶点。

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