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On Characterizing the Interactions between Proteins and Guanine Quadruplex Structures of Nucleic Acids

机译:表征蛋白质与核酸鸟嘌呤四链体结构之间的相互作用

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摘要

Guanine quadruplexes (G4s) are four-stranded secondary structures of nucleic acids which are stabilized by noncanonical hydrogen bonding systems between the nitrogenous bases as well as extensive base stacking, or pi-pi, interactions. Formation of these structures in either genomic DNA or cellular RNA has the potential to affect cell biology in many facets including telomere maintenance, transcription, alternate splicing, and translation. Consequently, G4s have become therapeutic targets and several small molecule compounds have been developed which can bind such structures, yet little is known about how G4s interact with their native protein binding partners. This review focuses on the recognition of G4s by proteins and small peptides, comparing the modes of recognition that have thus far been observed. Emphasis will be placed on the information that has been gained through high-resolution crystallographic and NMR structures of G4/peptide complexes as well as biochemical investigations of binding specificity. By understanding the molecular features that lead to specificity of G4 binding by native proteins, we will be better equipped to target protein/G4 interactions for therapeutic purposes.
机译:鸟嘌呤四链体(G4s)是核酸的四链二级结构,可通过含氮碱基之间的非规范氢键键合系统以及广泛的碱基堆积或pi-pi相互作用来稳定。这些结构在基因组DNA或细胞RNA中的形成都可能影响许多方面的细胞生物学,包括端粒的维持,转录,交替剪接和翻译。因此,G4已经成为治疗靶标,并且已经开发了可以结合这种结构的几种小分子化合物,但是关于G4如何与其天然蛋白结合伴侣相互作用的了解还很少。这篇综述着重于蛋白质和小肽对G4s的识别,比较了迄今观察到的识别方式。重点将放在通过G4 /肽复合物的高分辨率晶体学和NMR结构以及结合特异性的生化研究获得的信息上。通过了解导致天然蛋白质与G4结合的特异性的分子特征,我们将可以更好地针对治疗目的靶向蛋白质/ G4相互作用。

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