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分子间三链螺旋形成诱导的DNA结构变化

DNA Structural Changes Induced by Intermolecular Triple Helix Formation.

作者信息

Sayoh Ibrahim, Rusling David A, Brown Tom, Fox Keith R

机构信息

School of Biological Sciences, Life Sciences Building 85, University of Southampton, Southampton SO17 1BJ, U.K.

Department of Chemistry, University of Oxford, Oxford OX1 3TA, U.K.

出版信息

ACS Omega. 2020 Jan 15;5(3):1679-1687. doi: 10.1021/acsomega.9b03776. eCollection 2020 Jan 28.

Abstract

DNase I footprints of intermolecular DNA triplexes are often accompanied by enhanced cleavage at the 3'-end of the target site at the triplex-duplex junction. We have systematically studied the sequence dependence of this effect by examining oligonucleotide binding to sites flanked by each base in turn. For complexes with a terminal T.AT triplet, the greatest enhancement is seen with ApC, followed by ApG and ApT, with the weakest enhancement at ApA. Similar DNase I enhancements were observed for a triplex with a terminal C.GC triplet, though with little difference between the different GpN sites. Enhanced reactivity to diethylpyrocarbonate was observed at As that flank the triplex-duplex junction at AA or AC but not AG or AT. Fluorescence melting experiments demonstrated that the flanking base affected the stability with a 4 °C difference in between a flanking C and G. Sequences that produced the strongest enhancement correlated with those having the lower thermal stability. These results are interpreted in terms of oligonucleotide-induced changes in DNA structure and/or flexibility.

摘要

分子间DNA三链体的DNA酶I足迹通常伴随着三链体-双链体交界处靶位点3'端切割增强。我们通过依次检查寡核苷酸与每个碱基侧翼位点的结合,系统地研究了这种效应的序列依赖性。对于具有末端T·AT三联体的复合物,ApC的增强作用最大,其次是ApG和ApT,ApA的增强作用最弱。对于具有末端C·GC三联体的三链体,也观察到了类似的DNA酶I增强作用,尽管不同的GpN位点之间差异不大。在AA或AC的三链体-双链体交界处侧翼的A处观察到对焦碳酸二乙酯的反应性增强,但在AG或AT处未观察到。荧光熔解实验表明,侧翼碱基影响稳定性,侧翼C和G之间的Tm相差4°C。产生最强增强作用的序列与热稳定性较低的序列相关。这些结果是根据寡核苷酸诱导的DNA结构和/或柔韧性变化来解释的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b90/6990630/135eafde8ef8/ao9b03776_0001.jpg

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