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首页> 外文期刊>Carbohydrate Polymers: Scientific and Technological Aspects of Industrially Important Polysaccharides >Glycol chitosan in situ coating on PLGA nanoparticle curtails extraneous paclitaxel precipitates and imparts protein corona independent hemocompatibility
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Glycol chitosan in situ coating on PLGA nanoparticle curtails extraneous paclitaxel precipitates and imparts protein corona independent hemocompatibility

机译:在PLGA纳米粒子上的乙二醇壳聚糖在PLGA纳米粒子上延长了外来紫杉醇沉淀物,并赋予蛋白质电晕独立的血液组合

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摘要

Poly (lactide-co-glycolide) (PLGA) nanoparticles surface functionalized with water soluble glycol chitosan (GC) and carboxymethyl chitosan (CMC) has been studied for their drug (Paclitaxel and Doxorubicin) loading, yield, cellular uptake, serum protein adsorption and hemocompatibility. It was observed that Paclitaxel (Ptxl) phase out as Extraneous Ptxl Precipitates (EPP) (> 25 %) in case of uncoated and CMC coated low molecular weight (LMW) PLGA nanoparticles (PNPs). The EPP formation was significantly reduced to similar to 5 % with GC coating as it enhanced LMW PLGA precipitation and yield predominantly spherical polymeric nanoparticles towards better encapsulation of Ptxl and thus uniform intracellular drug distribution. Interestingly, protein corona analysis showed cmcPNPs and gcPNPs to be distinct from each other in associating mainly with serum proteins of molecular weight < 30 kDa and > 30 kDa respectively. While CMC functionalization showed > 10 % hemolysis, at similar concentration GC coating was found to provide superior hemocompatibility even in the absence of protein corona.
机译:已经研究了用水可溶性二醇壳聚糖(GC)和羧甲基壳聚糖(CMC)官能化的聚(丙交酯 - 共乙酰胺)(PLGA)纳米颗粒表面对其药物(紫杉醇和多柔比星)负荷,产率,细胞吸收,血清蛋白质吸附和血清蛋白质吸附和血液相位性。在未涂覆的和CMC涂覆的低分子量(LMW)PLGA纳米颗粒(PNPS)的情况下,观察到紫杉醇(PTX1)逐渐逐渐逐渐淘汰外来PTX1沉淀物(EPP)(> 25%)。 EPP形成显着降低至类似GC涂层的5%,因为它增强了LMW PLGA沉淀并产生主要是球形聚合物纳米颗粒,以更好地封装PTX1,从而均匀的细胞内药物分布。有趣的是,蛋白质电晕分析显示CMCPNPS和GCPNP分别在主要与分子量<30kDa和> 30kDa的血清蛋白分别与血清蛋白相互作用。虽然CMC官能化显示出> 10%溶血,但在类似的浓度下,也发现GC涂层即使在没有蛋白质电晕的情况下也能提供出色的血液相作。

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