适体
生物
DNA
G-四倍体
离解常数
凝血酶
环状DNA
鸟嘌呤
计算生物学
生物物理学
分子生物学
生物化学
基因
核苷酸
基因组
血小板
受体
免疫学
作者
Yu Mao,Jimmy Gu,Dingran Chang,Lei Wang,Lili Yao,Qihui Ma,Zhaofeng Luo,Hao Qu,Yingfu Li,Lei Zheng
摘要
Abstract Circular DNA aptamers are powerful candidates for therapeutic applications given their dramatically enhanced biostability. Herein we report the first effort to evolve circular DNA aptamers that bind a human protein directly in serum, a complex biofluid. Targeting human thrombin, this strategy has led to the discovery of a circular aptamer, named CTBA4T-B1, that exhibits very high binding affinity (with a dissociation constant of 19 pM), excellent anticoagulation activity (with the half maximal inhibitory concentration of 90 pM) and high stability (with a half-life of 8 h) in human serum, highlighting the advantage of performing aptamer selection directly in the environment where the application is intended. CTBA4T-B1 is predicted to adopt a unique structural fold with a central two-tiered guanine quadruplex capped by two long stem–loops. This structural arrangement differs from all known thrombin binding linear DNA aptamers, demonstrating the added advantage of evolving aptamers from circular DNA libraries. The method described here permits the derivation of circular DNA aptamers directly in biological fluids and could potentially be adapted to generate other types of aptamers for therapeutic applications.
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