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Preparation and drug controlled-release of polyion complex micelles as drug delivery systems

机译:聚硫代复合胶束的制备和药物控制释放作为药物递送系统

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Block copolymers, poly(N-vinylprrolidone)-block-poly(styrene-alter-maleic anhydride) (PVP-b-PSMA) and poly(N-vinylprrolidone)-block-poly(N,N-dimethylaminoethyl methacrylate) (PVP-b-PDMAEMA), were synthesized by reversible addition-fragmentation chain transfer (RAFT) polymerization. In aqueous media, this a pair of oppositely-charged diblock copolymers could self-assemble into stable and narrow distribution polyion complex micelles (PICMs). Transmission electron micrographs (TEM) and dynamic light scattering (DLS) analysis showed that the micelles to be spherically shaped with mean hydrodynamic diameter around 70 nm. In addition, the PICMs display ability to response to external stimuli. All of theses features are quite feasible for utilizing it as a novel intelligent drug delivery system. In order to assess its application in biomedical area, release profiles of coenzyme A (Co A) from PICMs were studied under both simulated gastric and intestinal pH conditions. The release was much quicker in pH 7.4 buffer than in pH 2.0 solution. Based on these results, these PICMs could be a potential pH-sensitive carrier for colon-specific drug delivery system. (C) 2008 Published by Elsevier B.V.
机译:嵌段共聚物,聚(N-乙烯基普利酮) - 嵌段 - 聚(苯乙烯 - 改性 - 马来酸酐)(PVP-B-PSMA)和聚(N-乙烯基普利酮) - Block-poly(N,N-二甲基氨基甲基甲基丙烯酸酯)(PVP- B-PDMAEMA)通过可逆添加 - 破碎链转移(筏)聚合来合成。在水性介质中,这对一对相反的带电二嵌体共聚物可以自组装成稳定且窄的分布聚硫酮胶束(PICMS)。透射电子显微照片(TEM)和动态光散射(DLS)分析表明,胶束形状以约70nm的平均水动力直径。此外,PICMS显示响应外部刺激的能力。所有这些功能对于利用它作为一种新颖的智能药物输送系统。为了评估其在生物医学区域的应用,在模拟胃和肠pH条件下研究来自PICMS的辅酶A(CO)的释放谱。在pH 7.4缓冲液中释放比在pH 2.0溶液中更快。基于这些结果,这些PICMS可以是用于结肠特异性药物输送系统的潜在pH敏感载体。 (c)2008由elestvier b.v发布。

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