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Tissue plasminogen activator-based clot busting: Controlled delivery approaches

机译:基于组织纤维蛋白溶酶原激活物的血块破坏:受控的递送方法

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摘要

Cardiovascular diseases are the leading cause of death worldwide. Thrombosis, the formation of blood clot (thrombus) in the circulatory system obstructing the blood flow, is one of the main causes behind various ischemic arterial syndromes such as ischemic stroke and myocardial infarction, as well as vein syndromes such as deep vein thrombosis, and consequently, pulmonary emboli. Several thrombolytic agents have been developed for treating thrombosis, the most common being tissue plasminogen activator (tPA), administrated systemically or locally via IV infusion directly proximal to the thrombus, with the aim of restoring and improving the blood flow. TPA triggers the dissolution of thrombi by inducing the conversion of plasminogen to protease plasmin followed by fibrin digestion that eventually leads to clot lysis. Although tPA provides powerful thrombolytic activity, it has many shortcomings, including poor pharmacokinetic profiles, impairment of the reestablishment of normal coronary flow, and impairment of hemostasis, leading to life-threatening bleeding consequences. The bleeding consequence is ascribed to the ability of tPA to circulate throughout the body and therefore can lysis all blood clots in the circulation system, even the good ones that prevent the bleeding and promote injury repair. This review provides an overview of the different delivery approaches for tPA including: liposomes, ultrasound-triggered thrombolysis, anti-fibrin antibody-targeted tPA, camouflaged-tPA, tpA-loaded microcarriers, and nano-modulated delivery approaches.
机译:心血管疾病是全球范围内主要的死亡原因。血栓形成是血液循环系统中的血栓(血栓)形成,阻碍了血流,是各种缺血性动脉综合征(例如缺血性中风和心肌梗塞)以及深静脉血栓形成等静脉综合征的主要原因之一因此,肺栓子。已经开发了几种用于治疗血栓形成的血栓溶解剂,最常见的是组织纤溶酶原激活物(tPA),其通过直接或直接在血栓附近静脉输注全身或局部给药,目的是恢复和改善血流。 TPA通过诱导纤溶酶原向蛋白酶纤溶酶的转化,然后进行血纤蛋白消化(最终导致血块溶解)来触发血栓溶解。尽管tPA提供了强大的溶栓活性,但它具有许多缺点,包括不良的药代动力学特性,正常冠状动脉血流重建的障碍和止血的障碍,导致危及生命的出血后果。出血的后果归因于tPA在全身循环的能力,因此可以溶解循环系统中的所有血块,甚至可以防止出血并促进损伤修复的好血块。这篇综述概述了tPA的不同递送方法,包括:脂质体,超声触发的溶栓,抗血纤蛋白抗体靶向的tPA,伪装的tPA,装载tpA的微载体以及纳米调节的递送方法。

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