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用于靶向RNA的准分子形成新型双探针的合理设计与研究

Rational design and studies of excimer forming novel dual probes to target RNA.

作者信息

Krasheninina O A, Lomzov A A, Fishman V S, Novopashina D S, Venyaminova A G

机构信息

Institute of Chemical Biology and Fundamental Medicine SB RAS, 8 Lavrentiev Ave., Novosibirsk 630090, Russia; Novosibirsk State University, 2 Pirogov str., Novosibirsk 630090, Russia.

Institute of Chemical Biology and Fundamental Medicine SB RAS, 8 Lavrentiev Ave., Novosibirsk 630090, Russia; Novosibirsk State University, 2 Pirogov str., Novosibirsk 630090, Russia.

出版信息

Bioorg Med Chem. 2017 Apr 1;25(7):2244-2250. doi: 10.1016/j.bmc.2017.02.042. Epub 2017 Feb 27.

Abstract

In this paper, we report structure-based rational design and physico-chemical and biological studies of novel pyrene excimer forming dual probes for visualization of intracellular RNAs. Herein, the probes based on 2'-O-methyl RNA with linkers of different structure and length between pyrene moiety and ribose are studied with respect to their hybridization and spectral properties. We found optimal linkers that provide more intense excimer emission (at ∼480nm) of RNA-bound probes; particularly, the length of the linker arm of the 3'-component of dual probes plays a key role in formation of pyrene excimer. Calculated molecular dynamics trajectories and probability distributions of pyrene-pyrene dimer formation upon hybridization of the dual probes with RNA target are in agreement with the obtained fluorescence spectroscopy data for the corresponding duplexes. Our study demonstrates the excellent binding properties of new dual probes to structured RNA and their feasibility for the visualization of intracellular RNA targets.

摘要

在本文中,我们报告了基于结构的新型芘激基缔合物形成双探针的合理设计以及物理化学和生物学研究,用于细胞内RNA的可视化。在此,研究了基于2'-O-甲基RNA且芘部分与核糖之间具有不同结构和长度连接子的探针的杂交和光谱特性。我们发现了能使与RNA结合的探针产生更强激基缔合物发射(在~480nm处)的最佳连接子;特别是,双探针3'-组分连接子臂的长度在芘激基缔合物的形成中起关键作用。双探针与RNA靶标杂交时芘-芘二聚体形成的计算分子动力学轨迹和概率分布与相应双链体获得的荧光光谱数据一致。我们的研究证明了新型双探针与结构化RNA具有优异的结合特性,以及它们用于细胞内RNA靶标可视化的可行性。

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