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小分子与G-四链体的相互作用:利用多分子动力学对构象空间进行系统探索。

Small-molecule G-quadruplex interactions: Systematic exploration of conformational space using multiple molecular dynamics.

作者信息

Husby Jarmila, Todd Alan K, Platts James A, Neidle Stephen

机构信息

School of Pharmacy, University College London, London, WC1N 1AX, UK.

出版信息

Biopolymers. 2013 Dec;99(12):989-1005. doi: 10.1002/bip.22340.

DOI:10.1002/bip.22340
PMID:23828641
Abstract

G-quadruplexes are higher-order four-stranded structures formed from repetitive guanine-containing tracts in nucleic acids. They comprise a core of stacked guanine-quartets linked by loops of length and sequence that vary with the context in which the quadruplex sequence occurs. Such sequences can be found in a number of genomic environments; at the telomeric ends of eukaryotic chromosomes, in promoter regions, in untranslated sequences and in open reading frames. Quadruplex formation can inhibit telomere maintenance, transcription and translation, especially when enhanced by quadruplex-binding small molecules, and quadruplex targeting is currently of considerable interest. The available experimental structural data shows that quadruplexes can have high conformational flexibility, especially in loop regions, which has hampered attempts to use high-throughput docking to find quadruplex-binding small-molecules with new scaffolds or to optimize existing ones with structure-based design methods. An approach to overcome the challenge of quadruplex conformational flexibility is presented here, which uses a combined multiple molecular dynamics and sampling approach. Two test small molecules have been used, RHPS4 and pyridostatin, which themselves have contrasting degrees of conformational flexibility.

摘要

G-四链体是由核酸中含鸟嘌呤的重复序列形成的高阶四链结构。它们由堆叠的鸟嘌呤四联体核心组成,这些四联体通过长度和序列各不相同的环相连,环的长度和序列会因四链体序列所处的环境而有所变化。此类序列可在多种基因组环境中找到,如真核染色体的端粒末端、启动子区域、非翻译序列和开放阅读框中。四链体的形成可抑制端粒维持、转录和翻译,尤其是当被四链体结合小分子增强时,目前四链体靶向研究备受关注。现有的实验结构数据表明,四链体具有较高的构象灵活性,尤其是在环区域,这阻碍了人们利用高通量对接来寻找具有新支架的四链体结合小分子或通过基于结构的设计方法优化现有小分子的尝试。本文提出了一种克服四链体构象灵活性挑战的方法,该方法采用了多分子动力学和采样相结合的方法。使用了两种测试小分子,即RHPS4和吡啶氨菌素,它们自身具有不同程度的构象灵活性。

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