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通过冷冻干燥技术制备的载蛋白质多孔聚左旋乳酸微球的形态学及释放动力学

Morphology and release kinetics of protein-loaded porous poly(l-lactic Acid) spheres prepared by freeze-drying technique.

作者信息

Sasaki Takashi, Tanaka Kazuki, Morino Daisuke, Sakurai Kensuke

机构信息

Department of Materials Science and Engineering, University of Fukui, 3-9-1 Bunkyo, Fukui 910 8507, Japan.

出版信息

ISRN Pharm. 2011;2011:490567. doi: 10.5402/2011/490567. Epub 2011 Aug 15.

Abstract

Freeze-drying a biodegradable polymer, poly(L-lactic acid) (PLLA), from 1,4-dioxane solutions provided very porous spherical particles of ca. 3 mm in radius with specific surface area of 8-13 m(2) g(-1). The surface of the particle was found to be less porous compared with its interior. To apply the freeze-dried PLLA (FDPLLA) to drug delivery system, its morphology and drug releasing kinetics were investigated, bovine serum albumin (BSA) being used as a model drug compound. Immersion of FDPLLA into a BSA aqueous solution gave BSA-loaded FDPLLA, where mass fraction of the adsorbed BSA reached up to 79%. Time-dependent release profile of BSA in water suggested a two-step mechanism: (1) very rapid release of BSA deposited on and near the particle surface, which results in an initial burst, and (2) leaching of BSA from the interior of the particle by the diffusion process. It was suggested that the latter process is largely governed by the surface porosity. The porosity of both the interior and surface was found to decrease remarkably as the concentration of the original PLLA/1,4-dioxane solution increases, C(0). Thus, C(0) is a key parameter that controls the loading and releasing of BSA.

摘要

将可生物降解聚合物聚(L-乳酸)(PLLA)从1,4-二氧六环溶液中冻干,可得到半径约为3毫米、比表面积为8 - 13平方米/克的非常多孔的球形颗粒。发现颗粒表面的孔隙率低于其内部。为了将冻干的PLLA(FDPLLA)应用于药物递送系统,研究了其形态和药物释放动力学,使用牛血清白蛋白(BSA)作为模型药物化合物。将FDPLLA浸入BSA水溶液中得到负载BSA的FDPLLA,其中吸附的BSA的质量分数高达79%。BSA在水中随时间的释放曲线表明有两步机制:(1)沉积在颗粒表面及其附近的BSA非常快速地释放,这导致初始爆发,以及(2)通过扩散过程从颗粒内部浸出BSA。有人认为后一过程在很大程度上受表面孔隙率的控制。发现内部和表面的孔隙率都随着原始PLLA/1,4-二氧六环溶液的浓度C(0)增加而显著降低。因此,C(0)是控制BSA负载和释放的关键参数。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8fbe/3263714/a09d1bcf1692/PHARMACEUTICS2011-490567.001.jpg

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