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Protein encapsulated magnetic carriers for micro/nanoscale drug delivery systems

机译:用于微/纳米药物输送系统的蛋白质包封磁性载体

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Novel methods for drug delivery may be based on nanotechnology using non-invasive magnetic guidance of drug loaded magnetic carriers to the targeted site and thereafter released by external ultrasound energy. The key building block of this system is to successfully synthesize biodegradable, magnetic drug carriers. Magnetic carriers using poly(D,L-lactide-co-glycolide) (PLGA) or poly(lactic acid)-poly(ethylene glycol) (PLA-PEG) as matrix materials were loaded with bovine serum albumin (BSA) by a double-emulsion technique. BSA-loaded magnetic microspheres were characterized for size, morphology, surface charge, and magnetization. The BSA encapsulation efficiency was determined by recovering albumin from the microspheres using dimethyl sulfoxide and 0.05N NaOH/0.5% SDS then quantifying with the Micro-BCA protein assay. BSA release profiles were also determined by the Micro-BCA protein assay. The microspheres had drug encapsulation efficiencies up to 90% depending on synthesis parameters. Particles were spherical with a smooth or porous surface having a size range less than 5 /spl mu/m. The surface charge (expressed as zeta potential) was near neutral, optimal for prolonged intravascular survival. The magnetization of these BSA loaded magnetic carriers was 2 to 6 emu/g, depending on the specific magnetic materials used during synthesis.
机译:用于药物递送的新方法可以基于使用药物负载磁性载体的非侵入性磁载体到靶向位点的纳米技术,然后通过外部超声能量释放。该系统的关键构建块是成功地合成可生物降解的磁性药物载体。使用聚(D,L-丙交酯 - 共乙酰化)(PLGA)或聚(乳酸) - 聚(乙二醇)(PLA-PEG)作为基质材料的磁性载体用双倍加载牛血清白蛋白(BSA)。 - 乳液技术。 BSA负载磁性微球的特征在于尺寸,形态,表面电荷和磁化。通过使用二甲基亚砜和0.05N NaOH / 0.5%SDS从微球回收白蛋白,然后用微BCA蛋白质测定来测定BSA封装效率。 BSA释放型材也由Micro-BCA蛋白质测定确定。根据合成参数,微球的药物包封效率高达90%。颗粒是球形的,具有尺寸范围小于5 / SPL mu / m的光滑或多孔表面。表面电荷(表达为Zeta电位)是延长血管内存活的中性近期,最佳。根据合成过程中使用的特定磁性材,这些BSA负载磁性载体的磁化为2至6兆/克。

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