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富含鸟嘌呤的 DNA 序列形成 G-四链体:两个四联体平行四链体不进行分子内折叠。

G-Quadruplex Formation by DNA Sequences Deficient in Guanines: Two Tetrad Parallel Quadruplexes Do Not Fold Intramolecularly.

机构信息

Institute of Biophysics of the Czech Academy of Sciences, Královopolská 135, 612 65, Brno, Czech Republic.

Central European Institute of Technology, Masaryk University, Kamenice 753/3, 625 00, Brno, Czech Republic.

出版信息

Chemistry. 2021 Aug 19;27(47):12115-12125. doi: 10.1002/chem.202100895. Epub 2021 Jul 20.

Abstract

Guanine quadruplexes (G4s) are noncanonical forms of nucleic acids that are frequently found in genomes. The stability of G4s depends, among other factors, on the number of G-tetrads. Three- or four-tetrad G4s and antiparallel two-tetrad G4s have been characterized experimentally; however, the existence of an intramolecular (i. e., not dimeric or multimeric) two-tetrad parallel-stranded DNA G4 has never been experimentally observed. Many sequences compatible with two-tetrad G4 can be found in important genomic regions, such as promoters, for which parallel G4s predominate. Using experimental and theoretical approaches, the propensity of the model sequence AATGGGTGGGTTTGGGTGGGTAA to form an intramolecular parallel-stranded G4 upon increasing the number of GGG-to-GG substitutions has been studied. Deletion of a single G leads to the formation of intramolecular G4s with a stacked G-triad, whose topology depends on the location of the deletion. Removal of another guanine from another G-tract leads to di- or multimeric G4s. Further deletions mostly prevent the formation of any stable G4. Thus, a solitary two-tetrad parallel DNA G4 is not thermodynamically stable and requires additional interactions through capping residues. However, transiently populated metastable two-tetrad species can associate to form stable dimers, the dynamic formation of which might play additional delicate roles in gene regulation. These findings provide essential information for bioinformatics studies searching for potential G4s in genomes.

摘要

鸟嘌呤四链体 (G4s) 是一种非典型的核酸结构,经常在基因组中发现。G4s 的稳定性取决于许多因素,其中包括 G-四联体的数量。三或四联体 G4s 和反平行二联体 G4s 已经在实验中得到了表征;然而,一直没有实验观察到分子内(即非二聚体或多聚体)二联体平行链 DNA G4 的存在。许多与二联体 G4 相容的序列可以在重要的基因组区域中找到,例如启动子,其中平行 G4s 占主导地位。使用实验和理论方法,研究了模型序列 AATGGGTGGGTTTGGGTGGGTAA 在增加 GGG 到 GG 取代数量时形成分子内平行 G4 的倾向。单个 G 的缺失会导致形成具有堆叠 G-三联体的分子内 G4,其拓扑结构取决于缺失的位置。从另一个 G-链段中除去另一个鸟嘌呤会导致二聚体或多聚体 G4 的形成。进一步的缺失大多阻止任何稳定 G4 的形成。因此,孤立的二联体平行 DNA G4 在热力学上不稳定,需要通过帽状残基的额外相互作用。然而,瞬态存在的亚稳态二联体物种可以缔合成稳定的二聚体,其动态形成可能在基因调控中发挥额外的微妙作用。这些发现为在基因组中寻找潜在 G4s 的生物信息学研究提供了重要信息。

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