通过多孔球囊导管沉积在动脉血管中的纳米颗粒:共聚焦激光扫描显微镜和透射电子显微镜的定位。

AAPS PharmSci Pub Date : 2002-01-01 DOI:10.1208/ps040441
Ulrich Westedt, Lucian Barbu-Tudoran, Andreas K Schaper, Marc Kalinowski, Heiko Alfke, Thomas Kissel
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引用次数: 63

摘要

再狭窄仍然是经皮腔内血管成形术(PTA)和支架置入术治疗动脉粥样硬化性疾病患者的主要限制。以导管为基础的局部药物递送提供了减少再狭窄和最小化不良全身副作用的潜在治疗方法。然而,液体药剂的内部滞留率很低。因此,为了实现治疗剂的持续和局部释放,必须将其封装在纳米颗粒载体系统中。本研究的目的是研究纳米颗粒局部进入新西兰大白兔腹主动脉血管壁后穿透的大小依赖性。2毫升0.025%荧光标记的聚苯乙烯纳米颗粒悬浮液,直径范围为110至514 nm,以2atm和8atm的恒定PTA压力注入腹主动脉。去除注入的片段后,用激光共聚焦扫描显微镜和透射电镜观察纳米颗粒的位置。该研究证明了纳米颗粒对完整血管壁的穿透与尺寸有关。大约100和200 nm的纳米颗粒沉积在血管壁的内部区域,514 nm的纳米颗粒主要积聚在主动脉的管腔表面。观察结果证实,大小在动脉血管壁颗粒分布中起关键作用。此外,它还受到压力诱导的输注通道的形成以及主动脉腔面或结缔组织的解剖障碍(如斑块)的存在的影响。
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Deposition of nanoparticles in the arterial vessel by porous balloon catheters: localization by confocal laser scanning microscopy and transmission electron microscopy.

Restenosis remains the major limitation of percutaneous transluminal angioplasty (PTA) and stenting in the treatment of patients with atherosclerotic disease. Catheter-based local delivery of pharmacologic agents offers a potential therapeutic approach to reducing restenosis and minimizing undesirable systemic side effects. However, the intramural retention of liquid agents is low. Therefore, to achieve a sustained and regional release of the therapeutic agent it must be encapsulated in nanoparticle carrier systems. The purpose of this study was to investigate the size dependence of the penetration of nanoparticles after local delivery into the vessel wall of the aorta abdominalis of New Zealand white rabbits. Two milliliters of a 0.025% fluorescence-labeled polystyrene nanoparticle suspension with diameters ranging from 110 to 514 nm were infused at 2 atm and at constant PTA pressure of 8 atm into the aorta abdominalis. After the infused segments were removed, the location of nanoparticles was visualized using confocal laser scanning microscopy and transmission electron microscopy. The study demonstrates a size-dependent nanoparticle penetration into the intact vessel wall. While nanoparticles of about 100 and 200 nm were deposited in the inner regions of the vessel wall, 514-nm nanoparticles accumulated primarily at the luminal surface of the aorta. The observations confirm that size plays a critical role in the distribution of particles in the arterial vessel wall. It is additionally influenced by the formation of pressure-induced infusion channels, as well as by the existence of anatomic barriers, such as plaques, at the luminal surface of the aorta or the connective elastic tissue.

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