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圆二色光谱揭示了重复及其他DNA序列中G-四链体和i-基序的状态。

CD spectra reveal the state of G-quadruplexes and i-motifs in repeated and other DNA sequences.

作者信息

Diggins Levi, Ross Daniel, Bhanot Sundeep, Corallo Rebecca, Daley Rachel, Patel Krishna, Lewis Olivia, Donahue Shane, Thaddeus Jacob, Hiers Lauren, Syed Christopher, Eagerton David, Mohanty Bidyut K

机构信息

Edward Via College of Osteopathic Medicine, Spartanburg, South Carolina.

Edward Via College of Osteopathic Medicine, Spartanburg, South Carolina.

出版信息

Biophys Rep (N Y). 2025 Mar 12;5(1):100187. doi: 10.1016/j.bpr.2024.100187. Epub 2024 Nov 27.

Abstract

The B-DNA of the genome contains numerous sequences that can form various noncanonical structures including G-quadruplex (G4), formed by two or more stacks of four guanine residues in a plane, and intercalating motif (i-motif [iM]) formed by alternately arranged C-C pairs. One of the easy yet sensitive methods to study G4s and iMs is circular dichroism (CD) spectroscopy, which generates characteristic G4 and iM peaks. We have analyzed and compared the effects of various environmental factors including pH, buffer composition, temperature, flanking sequences, complimentary DNA strands, and single-stranded DNA binding protein (SSB) on the CD patterns of G4s and iMs generated by two groups of DNA molecules, one containing tandem repeats of GGGGCC and CCCCGG from the C9ORF72 gene associated with amyotrophic lateral sclerosis and frontotemporal dementia, and the second containing polyG/polyC clusters from oncogene promoter-proximal regions without such tandem repeats. Changes in pH caused drastic changes in CCCCGG-iM and GGGGCC-G4 and the changes were dependent on repeat numbers and G-C basepairing. In contrast, with the DNA sequences from the promoter-proximal regions of oncogenes, iMs disassembled upon pH changes with the peak slowly shifting to lower wavelength but the G4s did not show significant change. Complementary DNA strands and flanking DNA sequences also regulate G4 and iM formation. The SSB disassembled both G4s and iMs formed by almost all sequences suggesting an in vivo role for SSBs in the disassembly of G4s and iMs during DNA replication and other DNA transactions.

摘要

基因组中的B-DNA包含许多能够形成各种非规范结构的序列,包括平面中由两个或更多个四层鸟嘌呤残基堆叠形成的G-四链体(G4),以及由交替排列的C-C对形成的嵌入基序(i-基序[iM])。研究G4和iM的一种简单而灵敏的方法是圆二色性(CD)光谱法,它能产生特征性的G4和iM峰。我们分析并比较了各种环境因素的影响,包括pH值、缓冲液组成、温度、侧翼序列、互补DNA链和单链DNA结合蛋白(SSB)对两组DNA分子产生的G4和iM的CD图谱的影响。第一组DNA分子包含与肌萎缩侧索硬化症和额颞叶痴呆相关的C9ORF72基因中的GGGGCC和CCCCGG串联重复序列,第二组包含来自癌基因启动子近端区域的无此类串联重复序列的聚G/聚C簇。pH值的变化导致CCCCGG-iM和GGGGCC-G4发生剧烈变化,且这些变化取决于重复次数和G-C碱基对。相比之下,对于来自癌基因启动子近端区域的DNA序列,iM在pH值变化时会解体,峰缓慢向较低波长移动,但G4没有显示出显著变化。互补DNA链和侧翼DNA序列也调节G4和iM的形成。SSB使几乎所有序列形成的G4和iM都解体,这表明SSB在体内DNA复制和其他DNA交易过程中对G4和iM的解体具有作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/723c/11699388/a8db5e0ecf17/gr1.jpg

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