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Controlled released of drug from doubled-walled PVA hydrogel/PCL microspheres prepared by single needle electrospraying method

机译:由单针电喷雾方法制备的双壁PVA水凝胶/ PCL微球的控制释放

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Poly(vinyl alcohol) (PVA) hydrogels have been extensively studied as drug delivery systems. However, due to the high hydrophilicity of PVA, these hydrogels have weak abilities to efficiently load drugs and control the initial burst release. In this study, we present a one-step simple and rapid single needle electrospraying (SNESy) method that combines PVA hydrogels with another biocompatible polymer polycaprolactone (PCL). A distinct core-shell structure was obtained with the PVA hydrogel core and PCL shell after the system was properly set up. The results revealed that the volume ratio between PVA hydrogel and PCL played an important role in determining the particle size and the formation of a spherical structure. The double-walled structure of the microsphere was confirmed by taking the fluorescent images and conducting the ATR-FTIR method. Furthermore, doxorubicin hydrochloride was used as a model drug to evaluate the drug loading capacity and the in vitro release behavior of this PVA hydrogel/PCL microsphere. The results indicated that coating a layer of PCL polymer significantly enhanced the drug loading capacity and reduced the drug initial burst release compared to the single-layer PVA hydrogel nanoparticles, demonstrating these biocompatible double-walled microspheres can be applied as excellent drug delivery carriers.
机译:聚(乙烯醇)(PVA)水凝胶已被广泛地研究药物递送系统。然而,由于PVA的高亲水性,这些水凝胶具有有效载有药物并控制初始爆发释放的能力较弱。在这项研究中,我们介绍了一种单一的简单和快速的单针电喷雾(Snesy)方法,将PVA水凝胶与另一种生物相容性聚合物聚己内酯(PCL)组合。在适当设置后,用PVA水凝胶核和PCL壳获得了不同的核壳结构。结果表明,PVA水凝胶和PCL之间的体积比在确定球形结构的粒度和形成方面发挥了重要作用。通过采用荧光图像并进行ATR-FTIR方法,确认微球的双壁结构。此外,盐酸多柔比星被用作模型药物,以评估该PVA水凝胶/ PCL微球的药物负载能力和体外释放行为。结果表明,与单层PVA水凝胶纳米粒子相比,涂覆一层PCL聚合物显着增强了药物负载能力并降低了药物初始爆发释放,证明这些生物相容性双壁微球可用作优异的药物输送载体。

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