生物正交化学
四嗪
分子成像
化学
微气泡
预定位
血栓
点击化学
组合化学
体内
纳米技术
超声波
材料科学
放射科
有机化学
抗体
医学
生物技术
外科
免疫学
单克隆抗体
放射免疫疗法
生物
作者
Tuan‐Tuan Wang,Chuxiao Yuan,Bingyang Dai,Yang Liu,Mingxi Li,Zhenqiang Feng,Qing Jiang,Zhihong Xu,Ningwei Zhao,Ning Gu,Fang Yang
出处
期刊:ChemBioChem
[Wiley]
日期:2017-04-20
卷期号:18 (14): 1364-1368
被引量:19
标识
DOI:10.1002/cbic.201700068
摘要
Bioorthogonal coupling chemistry has been studied as a potentially advantageous approach for molecular imaging because it offers rapid, efficient, and strong binding, which might also benefit stability, production, and chemical conjugation. The inverse-electron-demand Diels-Alder reaction between a 1,2,4,5-tetrazine and trans-cyclooctene (TCO) is an example of a highly selective and rapid bioorthogonal coupling reaction that has been used successfully to prepare targeted molecular imaging probes. Here we report a fast, reliable, and highly sensitive approach, based on a two-step pretargeting bioorthogonal approach, to achieving activated-platelet-specific CD62p-targeted thrombus ultrasound molecular imaging. Tetrazine-modified microbubbles (tetra-MBs) could be uniquely and rapidly captured by subsequent click chemistry of thrombus tagged with a trans-cyclooctene-pretreated CD62p antibody. Moreover, such tetra-MBs showed great long-term stability under physiological conditions, thus offering the ability to monitor thrombus changes in real time. We demonstrated for the first time that a bioorthogonal targeting molecular ultrasound imaging strategy based on tetra-MBs could be a simple but powerful tool for rapid diagnosis of acute thrombosis.
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