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使用MRX-408对血凝块进行结合和溶解。

Binding and lysing of blood clots using MRX-408.

作者信息

Wu Y, Unger E C, McCreery T P, Sweitzer R H, Shen D, Wu G, Vielhauer M D

机构信息

ImaRx Pharmaceutical Corp., Tucson, Arizona 85719, USA.

出版信息

Invest Radiol. 1998 Dec;33(12):880-5. doi: 10.1097/00004424-199812000-00006.

DOI:10.1097/00004424-199812000-00006
PMID:9851822
Abstract

RATIONALE AND OBJECTIVES

A thrombus-specific ultrasound contrast agent, MRX-408, has been developed recently. This agent consists of phospholipid-coated microbubbles with a ligand capable of targeting the GPIIb/IIIa receptor, thereby allowing the microbubbles to bind with thrombi rich in activated platelets. In vitro and in vivo animal experiments have been conducted to examine imaging enhancement and sonothrombolysis using this agent compared with a nontargeted agent.

METHODS

For clot binding, blood-smeared slides were incubated with microbubbles and examined under a light microscope. Change in backscatter signals from the blood clots after binding was examined by both an ultrasound scanner and two single-element transducers arranged in a transmitter-receiver pair. For clot lysis, either 1-MHz or 20-KHz ultrasound was used to enhance the lysing effects of MRX-408 with or without urokinase.

RESULTS

Evidence of binding was demonstrated under a microscope. In vitro experiments showed that the "acoustic signature", or properties, of blood clots changed after binding. Clots became more echogenic and nonlinear. In vivo fundamental ultrasound imaging confirmed that as a result of binding, blood clots were more visible, the area of detection was improved, and shadowing behind clots was more noticeable. Under 1-MHz ultrasound and 30 minutes of treatment, lysis efficiency reached 34% with MRX-408, whereas there was no visible clot lysis with saline.

CONCLUSION

The results of these preliminary studies show that as a contrast agent, MRX-408 enhanced clots under ultrasound imaging and facilitated sonothrombolysis with or without thrombolytic drugs.

摘要

原理与目的

一种血栓特异性超声造影剂MRX - 408最近已被研发出来。该造影剂由包裹着磷脂的微泡组成,带有一种能够靶向糖蛋白IIb/IIIa受体的配体,从而使微泡能够与富含活化血小板的血栓结合。已经进行了体外和体内动物实验,以研究与非靶向造影剂相比,使用这种造影剂时的成像增强效果和超声溶栓作用。

方法

对于血栓结合实验,将涂有血液的载玻片与微泡一起孵育,并在光学显微镜下检查。通过超声扫描仪和两个以发射 - 接收对形式排列的单元素换能器,检查结合后血凝块背向散射信号的变化。对于血栓溶解实验,使用1兆赫或20千赫的超声来增强MRX - 408在有或没有尿激酶情况下的溶解效果。

结果

在显微镜下证实了结合的证据。体外实验表明,血凝块结合后其“声学特征”或特性发生了变化。血凝块变得更具回声且呈非线性。体内基础超声成像证实,由于结合作用,血凝块更清晰可见,检测区域得到改善,并且血凝块后方的阴影更明显。在1兆赫超声和30分钟治疗下,使用MRX - 408时溶解效率达到34%,而使用生理盐水时没有可见的血栓溶解。

结论

这些初步研究结果表明,作为一种造影剂,MRX - 408在超声成像下增强了血栓显示,并在有或没有溶栓药物的情况下促进了超声溶栓。

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