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基于 G-四链体的靶向人凝血酶适体:发现、化学修饰及抗血栓作用。

G-quadruplex-based aptamers targeting human thrombin: Discovery, chemical modifications and antithrombotic effects.

机构信息

Department of Chemical Sciences, University of Naples Federico II, via Cintia 21, I-80126 Naples, Italy; Department of Advanced Medical and Surgical Sciences, 2(nd) Division of Neurology, Center for Rare Diseases and InterUniversity Center for Research in Neurosciences, University of Campania Luigi Vanvitelli, via Sergio Pansini, 5, I-80131 Naples, Italy.

Department of Chemical Sciences, University of Naples Federico II, via Cintia 21, I-80126 Naples, Italy.

出版信息

Pharmacol Ther. 2021 Jan;217:107649. doi: 10.1016/j.pharmthera.2020.107649. Epub 2020 Aug 7.

DOI:10.1016/j.pharmthera.2020.107649
PMID:32777331
Abstract

First studies on thrombin-inhibiting DNA aptamers were reported in 1992, and since then a large number of anticoagulant aptamers has been discovered. TBA - also named HD1, a 15-mer G-quadruplex (G4)-forming oligonucleotide - is the best characterized thrombin binding aptamer, able to specifically recognize the protein exosite I, thus inhibiting the conversion of soluble fibrinogen into insoluble fibrin strands. Unmodified nucleic acid-based aptamers, in general, and TBA in particular, exhibit limited pharmacokinetic properties and are rapidly degraded in vivo by nucleases. In order to improve the biological performance of aptamers, a widely investigated strategy is the introduction of chemical modifications in their backbone at the level of the nucleobases, sugar moieties or phosphodiester linkages. Besides TBA, also other thrombin binding aptamers, able to adopt a well-defined G4 structure, e.g. mixed duplex/quadruplex sequences, as well as homo- and hetero-bivalent constructs, have been identified and optimized. Considering the growing need of new efficient anticoagulant agents associated with the strong therapeutic potential of these thrombin inhibitors, the research on thrombin binding aptamers is still a very hot and intriguing field. Herein, we comprehensively described the state-of-the-art knowledge on the DNA-based aptamers targeting thrombin, especially focusing on the optimized analogues obtained by chemically modifying the oligonucleotide backbone, and their biological performances in therapeutic applications.

摘要

1992 年首次报道了凝血酶抑制 DNA 适体的研究,此后发现了大量的抗凝适体。TBA-也称为 HD1,是一种 15 个碱基的 G-四链体(G4)形成寡核苷酸-是最具特征的凝血酶结合适体,能够特异性识别蛋白质外切位点 I,从而抑制可溶性纤维蛋白原转化为不溶性纤维蛋白链。未修饰的基于核酸的适体,一般来说,特别是 TBA,表现出有限的药代动力学特性,并且在体内被核酸酶迅速降解。为了提高适体的生物学性能,广泛研究的策略是在碱基、糖部分或磷酸二酯键水平上对其骨架进行化学修饰。除了 TBA,还鉴定并优化了其他能够采用明确的 G4 结构的凝血酶结合适体,例如混合双链/四链体序列以及同型和异型双价构建体。考虑到与这些凝血酶抑制剂的强大治疗潜力相关的对新型高效抗凝剂的日益增长的需求,凝血酶结合适体的研究仍然是一个非常热门和有趣的领域。在此,我们全面描述了针对凝血酶的基于 DNA 的适体的最新知识,特别是重点介绍了通过化学修饰寡核苷酸骨架获得的优化类似物及其在治疗应用中的生物学性能。

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