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Different duplex/quadruplex junctions determine the properties of anti-thrombin aptamers with mixed folding

机译:不同的双链/四链连接决定了混合折叠的抗凝血酶适体的性质

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摘要

Mixed duplex/quadruplex oligonucleotides have attracted great interest as therapeutic targets as well as effective biomedical aptamers. In the case of thrombin-binding aptamer (TBA), the addition of a duplex motif to the G-quadruplex module improves the aptamer resistance to biodegradation and the affinity for thrombin. In particular, the mixed oligonucleotide RE31 is significantly more effective than TBA in anticoagulation experiments and shows a slower disappearance rate in human plasma and blood. In the crystal structure of the complex with thrombin, RE31 adopts an elongated structure in which the duplex and quadruplex regions are perfectly stacked on top of each other, firmly connected by a well-structured junction. The lock-and-key shape complementarity between the TT loops of the G-quadruplex and the protein exosite I gives rise to the basic interaction that stabilizes the complex. However, our data suggest that the duplex motif may have an active role in determining the greater anti-thrombin activity in biological fluids with respect to TBA. This work gives new information on mixed oligonucleotides and highlights the importance of structural data on duplex/quadruplex junctions, which appear to be varied, unpredictable, and fundamental in determining the aptamer functional properties.
机译:混合双链体/四链体寡核苷酸作为治疗靶标以及有效的生物医学适体引起了极大的兴趣。在凝血酶结合适体(TBA)的情况下,向G-四链体模块添加双链体基序可提高适体对生物降解的抗性和对凝血酶的亲和力。特别地,在抗凝实验中,混合的寡核苷酸RE31比TBA明显更有效,并且在人血浆和血液中的消失速度较慢。在具有凝血酶的复合物的晶体结构中,RE31采用拉长的结构,其中双链体和四链体区域完美地堆叠在彼此的顶部,并通过结构良好的结点牢固地连接。 G-四链体的TT环与蛋白质异位点I之间的锁键形状互补产生了稳定该复合物的基本相互作用。但是,我们的数据表明,双链体基序可能在确定生物液中相对于TBA的更大的抗凝血酶活性方面具有积极作用。这项工作提供了有关混合寡核苷酸的新信息,并突出了双链体/四链体连接结构数据的重要性,这些数据似乎是变化的,不可预测的,并且是确定适体功能特性的基础。

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