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探究致癌性c-Myc DNA启动子区域双链、G-四链体和i-基序结构之间的竞争

Probing the Competition between Duplex, G-Quadruplex and i-Motif Structures of the Oncogenic c-Myc DNA Promoter Region.

作者信息

Pandey Akanksha, Roy Sarupa, Srivatsan Seergazhi G

机构信息

Department of Chemistry, Indian Institute of Science Education and Research (IISER), Pune, Dr. Homi Bhabha Road, Pune, 411008, India.

出版信息

Chem Asian J. 2023 Sep 1;18(17):e202300510. doi: 10.1002/asia.202300510. Epub 2023 Aug 4.

Abstract

Development of probe systems that provide unique spectral signatures for duplex, G-quadruplex (GQ) and i-motif (iM) structures is very important to understand the relative propensity of a G-rich-C-rich promoter region to form these structures. Here, we devise a platform using a combination of two environment-sensitive nucleoside analogs namely, 5-fluorobenzofuran-modified 2'-deoxyuridine (FBF-dU) and 5-fluoro-2'-deoxyuridine (F-dU) to study the structures adopted by a promoter region of the c-Myc oncogene. FBF-dU serves as a dual-purpose probe containing a fluorescent and F NMR label. When incorporated into the C-rich sequence, it reports the formation of different iMs via changes in its fluorescence properties and F signal. F-dU incorporated into the G-rich ON reports the formation of a GQ structure whose F signal is clearly different from the signals obtained for iMs. Rewardingly, the labeled ONs when mixed with respective complementary strands allows us to determine the relative population of different structures formed by the c-Myc promoter by the virtue of the probe's ability to produce distinct and resolved F signatures for different structures. Our results indicate that at physiological pH and temperature the c-Myc promoter forms duplex, random coil and GQ structures, and does not form an iM. Whereas at acidic pH, the mixture largely forms iM and GQ structures. Taken together, our system will complement existing tools and provide unprecedented insights on the population equilibrium and dynamics of nucleic acid structures under different conditions.

摘要

开发能够为双链、G-四链体(GQ)和i-基序(iM)结构提供独特光谱特征的探针系统,对于理解富含G和富含C的启动子区域形成这些结构的相对倾向非常重要。在此,我们设计了一个平台,使用两种对环境敏感的核苷类似物,即5-氟苯并呋喃修饰的2'-脱氧尿苷(FBF-dU)和5-氟-2'-脱氧尿苷(F-dU)的组合,来研究c-Myc癌基因启动子区域所采用的结构。FBF-dU用作包含荧光和F NMR标记的两用探针。当掺入富含C的序列中时,它通过其荧光特性和F信号的变化报告不同iM的形成。掺入富含G的链中的F-dU报告GQ结构的形成,其F信号与iM获得的信号明显不同。值得庆幸的是,当标记的链与各自的互补链混合时,凭借探针为不同结构产生独特且可分辨的F特征的能力,我们能够确定c-Myc启动子形成的不同结构的相对比例。我们的结果表明,在生理pH和温度下,c-Myc启动子形成双链、无规卷曲和GQ结构,不形成iM。而在酸性pH下,混合物主要形成iM和GQ结构。综上所述,我们的系统将补充现有工具,并为不同条件下核酸结构的群体平衡和动力学提供前所未有的见解。

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