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首页> 外文期刊>Journal of the American College of Cardiology >A new drug delivery system for intravenous coronary thrombolysis with thrombus targeting and stealth activity recoverable by ultrasound
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A new drug delivery system for intravenous coronary thrombolysis with thrombus targeting and stealth activity recoverable by ultrasound

机译:一种新的药物输送系统,用于静脉内冠状动脉溶栓治疗,可通过超声恢复血栓靶向和隐身活动

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摘要

Objectives: The purpose of this study was to develop a new intelligent drug delivery system for intracoronary thrombolysis with a strong thrombolytic effect without increasing bleeding risk. Background: Rapid recanalization of an occluded coronary artery is essential for better outcomes in acute myocardial infarction. Catheter-based recanalization is widely accepted, but it takes time to transport patients. Although the current fibrinolytic therapy can be started quickly, it cannot achieve a high reperfusion rate. Recently, we generated nanoparticles comprising tissue-type plasminogen activator (tPA), basic gelatin, and zinc ions, which suppress tPA activity by 50% with 100% recovery by ultrasound (US) in vitro. Methods: The thrombus-targeting property of nanoparticles was examined by an in vitro binding assay with von Wilbrand factor and with a mouse arterial thrombosis model in vivo. The thrombolytic efficacy of nanoparticles was evaluated with a swine acute myocardial infarction model. Results: Nanoparticles bound to von Wilbrand factor in vitro and preferentially accumulated at the site of thrombus in a mouse model. In a swine acute myocardial infarction model, plasma tPA activity after intravenous injection of nanoparticles was approximately 25% of tPA alone and was recovered completely by transthoracic US (1.0 MHz, 1.0 W/cm2). During US application, plasma tPA activity near the affected coronary artery was recovered and was higher than that near the femoral artery. Although treatment with tPA alone (55,000 IU/kg) recanalized the occluded coronary artery in only 1 of 10 swine, nanoparticles containing the same dose of tPA with US achieved recanalization in 9 of 10 swine within 30 min. Conclusions: We developed an intelligent drug delivery system with promising potential for better intravenous coronary thrombolysis.
机译:目的:本研究的目的是开发一种新型的智能冠状动脉内溶栓药物输送系统,该系统具有很强的溶栓作用而不会增加出血风险。背景:阻塞性冠状动脉的快速再通对于在急性心肌梗塞中取得更好的疗效至关重要。基于导管的再通术已被广泛接受,但运输患者需要时间。尽管目前的纤维蛋白溶解疗法可以迅速开始,但不能实现高的再灌注率。最近,我们生成了包含组织型纤溶酶原激活剂(tPA),碱性明胶和锌离子的纳米粒子,这些纳米粒子可在体外通过超声(US)将tPA活性抑制50%,回收率100%。方法:通过体外结合试验,von Wilbrand因子和小鼠动脉血栓形成模型,检测纳米颗粒的血栓靶向特性。用猪急性心肌梗塞模型评估纳米颗粒的溶栓功效。结果:在小鼠模型中,纳米粒子在体外与von Wilbrand因子结合,并优先聚集在血栓部位。在猪急性心肌梗塞模型中,静脉内注射纳米颗粒后血浆tPA活性约为tPA的25%,并通过经胸腔超声(1.0 MHz,1.0 W / cm2)完全恢复。在美国应用期间,受影响的冠状动脉附近的血浆tPA活性得以恢复,并高于股动脉附近。尽管仅使用tPA(55,000 IU / kg)的治疗可以在10头猪中的1头再次闭塞冠状动脉,但是在30分钟内,含有相同剂量tPA和US的纳米颗粒在10头猪中的9头可以实现再通。结论:我们开发了一种智能药物输送系统,具有改善静脉内冠状动脉溶栓治疗的潜力。

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