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肌萎缩侧索硬化症和额颞叶痴呆相关的 GGGGCC 重复含 DNA 寡核苷酸折叠成两种不同的 G-四链体。

ALS and FTD linked GGGGCC-repeat containing DNA oligonucleotide folds into two distinct G-quadruplexes.

机构信息

Slovenian NMR Center, National Institute of Chemistry, Ljubljana, Slovenia.

Slovenian NMR Center, National Institute of Chemistry, Ljubljana, Slovenia; Faculty of Chemistry and Chemical Technology, University of Ljubljana, Ljubljana, Slovenia; EN-FIST Center of Excellence, Ljubljana, Slovenia.

出版信息

Biochim Biophys Acta Gen Subj. 2017 May;1861(5 Pt B):1237-1245. doi: 10.1016/j.bbagen.2016.11.018. Epub 2016 Nov 14.

Abstract

BACKGROUND

The most common genetic cause of neurological disorders ALS and FTD is a largely increased number of GGGGCC repeats in C9orf72 gene. Non-canonical structures including G-quadruplexes adopted by expanded repeats are hypothesized to be crucial in pathogenesis. Recently, we have shown that structural polymorphism of oligonucleotide d(GC)G is reduced by dG to 8Br-dG substitution. High-resolution structure of one of the two major G-quadruplexes adopts antiparallel topology comprising of four G-quartets. Herein, we describe the topology of the second major G-quadruplex structure and influence of folding conditions on relative populations of the two folds.

METHODS

Influence of folding conditions was explored by 1H D NMR. Determination of topology was achieved by 2D NMR complemented with PAGE and CD. UV melting experiment was used to explore thermal stability of structures.

RESULTS

Two structures adopted by oligonucleotide d(GC)GGGG denoted AQU and NAN coexist in solution and ratio of their populations is determined by pH and rate of cooling when folding from thermally denatured state in the presence of K ions.

CONCLUSIONS

AQU is kinetically favored and forms by folding at low pH, while NAN is favored thermodynamically and at neutral pH. AQU and NAN share similar antiparallel topology with four G-quartets and three edgewise loops, however they exhibit distinct structural and dynamic properties.

GENERAL SIGNIFICANCE

Novel G-quadruplex topology adds insight into diverse polymorphism of DNA sequences comprising potentially pathological GGGGCC repeat. Relative populations of the two structures and their dependence on folding conditions contribute to understanding of factors that govern G-quadruplex folding. This article is part of a Special Issue entitled "Gquadruplex" Guest Editor: Dr. Concetta Giancola and Dr. Daniela Montesarchio.

摘要

背景

导致神经退行性疾病 ALS 和 FTD 的最常见遗传原因是 C9orf72 基因中 GGGGCC 重复序列的大量增加。推测扩张重复序列形成的非典型结构,包括 G-四链体,在发病机制中起关键作用。最近,我们已经表明,寡核苷酸 d(GC)G 的结构多态性通过 dG 至 8Br-dG 取代而降低。两种主要 G-四链体结构之一的高分辨率结构采用包含四个 G-四联体的反平行拓扑。在此,我们描述了第二种主要 G-四链体结构的拓扑结构以及折叠条件对两种构象相对丰度的影响。

方法

通过 1H D NMR 探索折叠条件的影响。通过二维 NMR 与 PAGE 和 CD 相结合确定拓扑结构。使用 UV 熔融实验探索结构的热稳定性。

结果

寡核苷酸 d(GC)GGGG 采用的两种结构 AQU 和 NAN 共存于溶液中,其比例由 pH 和在 K 离子存在下从热变性状态折叠时的冷却速率决定。

结论

AQU 在动力学上有利,在低 pH 下折叠形成,而 NAN 在热力学上有利,在中性 pH 下形成。AQU 和 NAN 具有相似的反平行拓扑结构,包含四个 G-四联体和三个边缘环,但它们表现出不同的结构和动态特性。

一般意义

新的 G-四链体拓扑结构增加了对包含潜在病理 GGGGCC 重复序列的 DNA 序列多样性的了解。两种结构的相对丰度及其对折叠条件的依赖性有助于理解控制 G-四链体折叠的因素。本文是题为“G-四链体”的特刊的一部分,客座编辑:Concetta Giancola 博士和 Daniela Montesarchio 博士。

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