首页> 外文期刊>Bulletin of the Korean Chemical Society >One-Pot Synthesis of Highly Monodisperse Poly(lactic-co-glycolic Acid) Particles with Controlled Porosity as Efficient Drug Delivery Vehicles
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One-Pot Synthesis of Highly Monodisperse Poly(lactic-co-glycolic Acid) Particles with Controlled Porosity as Efficient Drug Delivery Vehicles

机译:高盆合成高度单分散聚(乳酸 - 共乙醇酸)颗粒,具有受控孔隙率作为有效的药物递送载体

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摘要

Poly(lactic-co-glycolic acid) (PLGA) particles are one of the most widely used biocompatible and biodegradable materials, and have been extensively investigated as drug delivery vehicles. While a number of different types of additives have been used during and after the synthesis of the PLGA particles for the enhancement of their functions, the shape control of the particles and observations of their shape-dependent properties have been rarely reported to date. To overcome the limitations of conventional PLGA particles, including the slow degradation of PLGA and the resultant slow drug release, we synthesized porous PLGA particles with much higher surface area than in previous works. Unlike in previous studies, the porous PLGA particles in this work exhibit distinctive advantages such as a simpler synthetic scheme, improved size monodispersity, and controllable pore size distribution (approximately 1 um in diameter). Polyethylenimine (PEI) was chosen as a pore-generating material, which simplified the synthesis process significantly. The performance of the porous PLGA particles was evaluated using doxorubicin (DOX) and the A549 cell line as a drug and target cells of a model system, respectively. Based on the observation of the cell viability, the DOX-loaded porous PLGA particles were determined to be five times more efficient than molecular DOX.
机译:聚(乳酸共聚乙醇酸)(PLGA)颗粒是最广泛使用的生物相容性和可生物降解的材料之一,并且已被广泛研究为药物递送载体。虽然在合成其功能的PLGA颗粒的合成期间和之后已经使用了许多不同类型的添加剂,但是迄今为止已经很少报告颗粒的形状和其形状依赖性性质的观察结果。为了克服常规PLGA颗粒的局限性,包括PLGA的缓慢降解和所得的缓慢药物释放,我们合成多孔PLGGA颗粒具有比以前的工作更高的表面积。与先前的研究不同,该工作中的多孔PLGA颗粒表现出具有更简单的合成方案,改进的尺寸单反叠性和可控孔径分布(直径约1μm)的独特优点。选择聚乙烯(PEI)作为孔发电材料,其显着简化了合成过程。使用多柔比星(DOX)和A549细胞系作为模型系统的药物和靶细胞,评价多孔PLGA颗粒的性能。基于对细胞活力的观察,将DOX加载的多孔PLGA颗粒确定为比分子DOX更有效的五倍。

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