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含三碳间隔分子的高效G-四链体稳定凝血酶结合适体的开发。

Development of an Efficient G-Quadruplex-Stabilised Thrombin-Binding Aptamer Containing a Three-Carbon Spacer Molecule.

作者信息

Aaldering Lukas J, Poongavanam Vasanthanathan, Langkjaer Niels, Murugan N Arul, Jørgensen Per Trolle, Wengel Jesper, Veedu Rakesh N

机构信息

Nucleic Acid Center, Department of Physics, Chemistry and Pharmacy, University of Southern Denmark, Campusvej 55, 5230, Odense M, Denmark.

Institute for Plant Biology and Biotechnology, Westphalian Wilhelms University Münster, Schlossgarten 3, 48149, Münster, Germany.

出版信息

Chembiochem. 2017 Apr 18;18(8):755-763. doi: 10.1002/cbic.201600654. Epub 2017 Mar 15.

Abstract

The thrombin-binding aptamer (TBA), which shows anticoagulant properties, is one of the most studied G-quadruplex-forming aptamers. In this study, we investigated the impact of different chemical modifications such as a three-carbon spacer (spacer-C ), unlocked nucleic acid (UNA) and 3'-amino-modified UNA (amino-UNA) on the structural dynamics and stability of TBA. All three modifications were incorporated at three different loop positions (T3, T7, T12) of the TBA G-quadruplex structure to result in a series of TBA variants and their stability was studied by thermal denaturation; folding was studied by circular dichroism spectroscopy and thrombin clotting time. The results showed that spacer-C introduction at the T7 loop position (TBA-SP7) significantly improved stability and thrombin clotting time while maintaining a similar binding affinity as TBA to thrombin. Detailed molecular modelling experiments provided novel insights into the experimental observations, further supporting the efficacy of TBA-SP7. The results of this study could provide valuable information for future designs of TBA analogues with superior thrombin inhibition properties.

摘要

具有抗凝特性的凝血酶结合适体(TBA)是研究最多的形成G-四链体的适体之一。在本研究中,我们研究了不同化学修饰,如三碳间隔基(间隔基-C)、解锁核酸(UNA)和3'-氨基修饰的UNA(氨基-UNA)对TBA结构动力学和稳定性的影响。所有这三种修饰都被引入到TBA G-四链体结构的三个不同环位置(T3、T7、T12),从而产生一系列TBA变体,并通过热变性研究它们的稳定性;通过圆二色光谱和凝血酶凝血时间研究折叠情况。结果表明,在T7环位置引入间隔基-C(TBA-SP7)显著提高了稳定性和凝血酶凝血时间,同时保持了与TBA对凝血酶相似的结合亲和力。详细的分子建模实验为实验观察提供了新的见解,进一步支持了TBA-SP7的有效性。本研究结果可为未来设计具有优异凝血酶抑制特性的TBA类似物提供有价值的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6da/5413854/b9343d1d42fc/CBIC-18-755-g004.jpg

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