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证明靶向非霍奇金淋巴瘤中 MYC 的药物下调是通过启动子 G-四链体直接介导的。

Demonstration that drug-targeted down-regulation of MYC in non-Hodgkins lymphoma is directly mediated through the promoter G-quadruplex.

机构信息

College of Pharmacy, University of Arizona, Tucson, Arizona 85721, USA.

出版信息

J Biol Chem. 2011 Nov 25;286(47):41018-27. doi: 10.1074/jbc.M111.274720. Epub 2011 Sep 28.

DOI:10.1074/jbc.M111.274720
PMID:21956115
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3220475/
Abstract

Most transcription of the MYC proto-oncogene initiates in the near upstream promoter, within which lies the nuclease hypersensitive element (NHE) III(1) region containing the CT-element. This dynamic stretch of DNA can form at least three different topologies: single-stranded DNA, double-stranded DNA, or higher order secondary structures that silence transcription. In the current report, we identify the ellipticine analog GQC-05 (NSC338258) as a high affinity, potent, and selective stabilizer of the MYC G-quadruplex (G4). In cells, GQC-05 induced cytotoxicity with corresponding decreased MYC mRNA and altered protein binding to the NHE III(1) region, in agreement with a G4 stabilizing compound. We further describe a unique feature of the Burkitt's lymphoma cell line CA46 that allowed us to clearly demonstrate the mechanism and location of action of GQC-05 within this region of DNA and through the G4. Most importantly, these data present, as far as we are aware, the most direct evidence of intracellular G4-mediated control of a particular promoter.

摘要

大多数 MYC 原癌基因的转录起始于近上游启动子,其中包含核酶超敏元件(NHE)III(1)区域,该区域包含 CT 元件。这个动态伸展的 DNA 可以形成至少三种不同的拓扑结构:单链 DNA、双链 DNA 或更高阶的二级结构,这些结构会使转录沉默。在本报告中,我们确定椭圆碱类似物 GQC-05(NSC338258)是 MYC G-四链体(G4)的高亲和力、强效和选择性稳定剂。在细胞中,GQC-05 诱导细胞毒性,相应地降低 MYC mRNA,并改变蛋白质与 NHE III(1)区域的结合,与 G4 稳定化合物一致。我们进一步描述了 Burkitt 淋巴瘤细胞系 CA46 的一个独特特征,这使我们能够清楚地证明 GQC-05 在该 DNA 区域内以及通过 G4 发挥作用的机制和位置。最重要的是,这些数据提供了迄今为止最直接的证据,证明了细胞内 G4 对特定启动子的控制作用。

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