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使用磁铁矿纳米颗粒进行溶栓治疗中的植入物辅助磁性药物靶向。

The use of magnetite nanoparticles for implant-assisted magnetic drug targeting in thrombolytic therapy.

机构信息

Biomedical Polymer Technology, Department of Experimental Medical Science, Lund University, BMC D11, SE-22184 Lund, Sweden.

出版信息

Biomaterials. 2010 Dec;31(36):9499-510. doi: 10.1016/j.biomaterials.2010.07.107. Epub 2010 Aug 21.

Abstract

Implant-assisted targeting of magnetic particles under the influence of an external magnetic field has previously been verified through mathematical modeling, in vitro studies, and in vivo studies on rat carotid arteries as a feasible method for localized drug delivery. The present study focuses on the development of nanoparticles for the treatment of in-stent thrombosis. Magnetic nanoparticles in the size-range 10-30 nm were synthesized in a one-pot procedure by precipitation of ferrous hydroxide followed by oxidation to magnetite. The nanoparticles were silanized with tetraethyl orthosilicate in the presence of triethylene glycol and/or polyethylene glycol. The surface coated magnetite nanoparticles were activated with either N-hydroxysulfosuccinimide or tresyl chloride for covalent immobilization of tissue plasminogen activator (tPA). Hysteresis loops showed saturation magnetizations of 55.8, 44.1, and 43.0 emu/g for the naked nanoparticles, the surface coated nanoparticles, and the tPA-nanoparticle conjugates, respectively. The hemolytic activity of the nanoparticles in blood was negligible. An initial in vivo biocompatibility test in pig, carried out by intravascular injection of the nanoparticles in a stented brachial artery, showed no short-term adverse effects. In vitro evaluation in a flow-through model proved that the nanoparticles were captured efficiently to the surface of a ferromagnetic coiled wire at the fluid velocities typical for human arteries. A preliminary test of the tPA-nanoparticle conjugates in a pig model suggested that the conjugates may be used for treatment of in-stent thrombosis in coronary arteries.

摘要

在外部磁场的影响下,通过数学建模、体外研究和大鼠颈动脉的体内研究,已经证实了磁性粒子的植入物靶向作用是一种可行的局部药物输送方法。本研究专注于用于治疗支架内血栓形成的纳米颗粒的开发。通过沉淀氢氧化亚铁随后氧化为磁铁矿,在一锅法中合成了尺寸为 10-30nm 的磁性纳米颗粒。纳米颗粒在三乙烯二醇和/或聚乙二醇的存在下用四乙氧基硅烷硅烷化。用 N-羟基琥珀酰亚胺或三氟甲磺酸酯将表面涂覆的磁铁矿纳米颗粒激活,用于组织型纤溶酶原激活剂(tPA)的共价固定化。滞后回线显示,裸纳米颗粒、表面涂覆的纳米颗粒和 tPA-纳米颗粒缀合物的饱和磁化强度分别为 55.8、44.1 和 43.0 emu/g。纳米颗粒在血液中的溶血活性可以忽略不计。在猪体内进行的初步体内生物相容性试验,通过将纳米颗粒静脉内注射到支架肱动脉中,未显示出短期的不良反应。在流动模型中的体外评估证明,纳米颗粒在人动脉典型的流体速度下可以有效地被捕获到铁磁盘管的表面。在猪模型中对 tPA-纳米颗粒缀合物的初步测试表明,缀合物可能用于治疗冠状动脉内支架内血栓形成。

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