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Major effects on blood-retina barrier passage by minor alterations in design of polybutylcyanoacrylate nanoparticles

机译:用聚丁基芳基丙烯酸酯纳米粒子设计轻微改变对血液视网膜屏障通道的重大影响

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摘要

Because the blood-brain barrier (BBB) is an obstacle for drug-delivery, carrier systems such as polybutylcyanoacrylate (PBCA) nanoparticles (NPs) have been studied. Yet, little is known of how physiochemical features such as size, surfactants and surface charge influence BBB passage in vivo. We now used a rat model of in vivo imaging of the retina - which is brain tissue and can reflect the situation at the BBB - to study how size and surface charge determine NPs' ability to cross the blood-retina barrier (BRB). Interestingly, for poloxamer 188-modified, DEAE-dextran-stabilised, fluorescent PBCA NPs, decreasing the average zeta-size from 272 nm to 172nm by centrifugation reduced the BRB passage of the NPs substantially. Varying the zeta potential within the narrow range of 0-15 mV by adding different amounts of stabiliser revealed that 0mV and 15mV were less desirable than 5mV which facilitated the BRB passage. Moreover, whether the fluorescent marker was adsorbed or incorporated also influenced the transport into the retina tissue. Thus, minor changes in design of nano-carriers can alter physicochemical parameters such as size or zeta potential, thus substantially influencing NPs' biological distribution in vivo, possibly by interactions with blood constituents and peripheral organs.
机译:因为血脑屏障(BBB)是用于药物输送的障碍,所以已经研究了载体系统,例如聚丁基丙烯酸酯(PBCA)纳米颗粒(NPS)。然而,众所周知,诸如尺寸,表面活性剂和表面电荷的基础特征是如何在体内的BBB通道的情况下。我们现在使用了Retina体内成像的大鼠模型 - 这是脑组织,可以反映BBB的情况 - 研究尺寸和表面电荷如何确定NPS的血管屏障(BRB)的能力。有趣的是,对于泊洛沙姆188-修饰的DEAE-葡聚糖稳定的,荧光PBCA NPS,通过离心降低272nm至172nm的平均Zeta大小基本上降低了NP的BRB通道。通过添加不同量的稳定剂,将0mV和15mV的较小量不太理想,改变0-15mV的缩小范围内的Zeta电位,这促进了促进BRB通道的5mV。此外,荧光标记物是否吸附或掺入也影响了转运进入视网膜组织。因此,纳米载体的设计的微小变化可以改变物理化学参数,例如尺寸或ζ电位,从而显着影响体内的NPS生物分布,可能是通过与血液成分和外周器官的相互作用。

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