一种结构解释抗血栓活性的 ARC1172,一个 DNA 适体结合 von Willebrand 因子域 A1。
A structural explanation for the antithrombotic activity of ARC1172, a DNA aptamer that binds von Willebrand factor domain A1.
机构信息
Department of Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.
出版信息
Structure. 2009 Nov 11;17(11):1476-84. doi: 10.1016/j.str.2009.09.011.
Abstract
ARC1172 is a 41-mer DNA aptamer selected to bind the A1 domain of von Willebrand factor (VWF). A derivative of ARC1172 with modifications to increase intravascular survival inhibits carotid artery thrombosis in a Cynomolgus macaque model and inhibits VWF-dependent platelet aggregation in humans, suggesting that such aptamers may be useful to prevent or treat thrombosis. In the crystal structure of a VWF A1-ARC1172 complex, the aptamer adopts a three-stem structure of mainly B-form DNA with three noncanonical base pairs and 9 unpaired residues, 6 of which are stabilized by base-base or base-deoxyribose stacking interactions. The aptamer-protein interface is characterized by cation-pi interactions involving Arg, Lys, and Gln residues, often stabilized by H-bonds with adjacent bases. The ARC1172 binding site on the A1 domain overlaps with that of botrocetin and clashes with glycoprotein Ibalpha binding at an adjacent site, which accounts for the antithrombotic activity of ARC1172 and related aptamers.
摘要
ARC1172 是一种 41 个碱基对的 DNA 适体,经过筛选能与血管性血友病因子(VWF)的 A1 结构域结合。ARC1172 的一种衍生物经过修饰,以提高血管内的存活率,可抑制恒河猴模型的颈动脉血栓形成,并抑制人类 VWF 依赖性血小板聚集,这表明此类适体可能有助于预防或治疗血栓形成。在 VWF A1-ARC1172 复合物的晶体结构中,适体采用主要由 B 型 DNA 组成的三茎结构,其中有三个非经典碱基对和 9 个未配对残基,其中 6 个残基通过碱基-碱基或碱基-脱氧核糖堆叠相互作用稳定。适体-蛋白界面的特征是涉及精氨酸、赖氨酸和谷氨酰胺残基的阳离子-π 相互作用,通常通过与相邻碱基的氢键稳定。ARC1172 在 A1 结构域上的结合位点与 botrocetin 重叠,与相邻位点的糖蛋白 Ibα 结合发生冲突,这解释了 ARC1172 和相关适体的抗血栓活性。
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