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Influence of morphology and drug distribution on the release process of FITC-dextran-loaded microspheres prepared with different types of PLGA

机译:形态和药物分布对不同类型PLGA制备的FITC-右旋糖酐微球释放过程的影响

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The aim of the present work was to understand the collaborative roles and the comprehensive effects of polymer nature, morphology, drug distribution and release behaviour for PLGA microspheres prepared by the double emulsion method. The morphology and drug distribution of the FITC-dextran-loaded microspheres were investigated by scanning electron microscopy (SEM) and confocal laser scanning microscopy (CLSM), respectively. The results show that the morphology and release profiles depend on the polymer nature. For the capped PLGA RG502, the porosity, pore size and drug distribution had no pronounced influence on the release profile beyond the initial release. No significant changes in size and morphology were found and there was negligible water uptake during the release process. PEG addition as a pore maker indicated a possible way to modify the release rate at the second release stage. However, in the case of the uncapped PLGA RG503H, release profiles were dependent upon changes in porosity, pore size and drug loading. Increases in porosity, internal pore size and loading resulted in a continuous release profile. Previous studies have shown the importance of different process parameters on morphology and drug release, but in this work it is clear that polymer nature is a determining factor.
机译:本工作的目的是了解双乳液法制备的PLGA微球的聚合物性质,形态,药物分布和释放行为的协同作用和综合影响。分别通过扫描电子显微镜(SEM)和共聚焦激光扫描显微镜(CLSM)研究了FITC-葡聚糖微球的形态和药物分布。结果表明,形态和释放曲线取决于聚合物的性质。对于封端的PLGA RG502,孔隙率,孔径和药物分布对初始释放后释放曲线没有明显影响。没有发现大小和形态的显着变化,并且在释放过程中吸水量可以忽略不计。加入PEG作为造孔剂表明了在第二释放阶段改变释放速率的可能方法。但是,对于未封盖的PLGA RG503H,释放曲线取决于孔隙率,孔径和载药量的变化。孔隙率,内部孔径和载荷的增加导致了连续释放曲线。先前的研究表明,不同工艺参数对形态和药物释放的重要性,但在这项工作中,很明显聚合物的性质是决定性因素。

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