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Drug Transport to Brain with Targeted Nanoparticles

机译:靶向纳米颗粒将药物转运到大脑

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摘要

>Summary: Nanoparticle drug carriers consist of solid biodegradable particles in size ranging from 10 to 1000 nm (50–300 nm generally). They cannot freely diffuse through the blood-brain barrier (BBB) and require receptor-mediated transport through brain capillary endothelium to deliver their content into the brain parenchyma. Polysorbate 80-coated polybutylcyanoacrylate nanoparticles can deliver drugs to the brain by a still debated mechanism. Despite interesting results these nanoparticles have limitations, discussed in this review, that may preclude, or at least limit, their potential clinical applications. Long-circulating nanoparticles made of methoxypoly(ethylene glycol)- polylactide or poly(lactide-co-glycolide) (mPEG-PLA/PLGA) have a good safety profiles and provide drug-sustained release. The availability of functionalized PEG-PLA permits to prepare target-specific nanoparticles by conjugation of cell surface ligand. Using peptidomimetic antibodies to BBB transcytosis receptor, brain-targeted pegylated immunonanoparticles can now be synthesized that should make possible the delivery of entrapped actives into the brain parenchyma without inducing BBB permeability alteration. This review presents their general properties (structure, loading capacity, pharmacokinetics) and currently available methods for immunonanoparticle preparation.
机译:>摘要:纳米颗粒药物载体由可生物降解的固体颗粒组成,粒径范围为10至1000 nm(通常为50-300 nm)。它们不能通过血脑屏障(BBB)自由扩散,并且需要受体介导的通过脑毛细血管内皮的转运才能将其内容物传递到脑实质中。聚山梨酯80涂层的聚氰基丙烯酸丁酯纳米颗粒可以通过尚有争议的机制将药物递送至大脑。尽管获得了有趣的结果,但这些纳米颗粒仍存在局限性,如本综述所述,可能会限制或至少限制其潜在的临床应用。由甲氧基聚(乙二醇)-聚丙交酯或聚(丙交酯-共-乙交酯)(mPEG-PLA / PLGA)制成的长循环纳米颗粒具有良好的安全性,可提供药物持续释放。官能化PEG-PLA的可用性允许通过缀合细胞表面配体来制备靶标特异性纳米颗粒。现在,使用针对BBB转胞吞作用受体的拟肽抗体,可以合成针对大脑的聚乙二醇化免疫纳米颗粒,这应该可以将捕获的活性物质递送到脑实质中,而不会引起BBB通透性的改变。这篇综述介绍了它们的一般性质(结构,负载能力,药代动力学)和目前可用的免疫纳米颗粒制备方法。

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