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Smart Microgel Studies. Interaction of Polyether-Modified Poly(Acrylic Acid) Microgels with Anticancer Drugs

机译:智能微凝胶研究。聚醚改性聚(丙烯酸)微凝胶与抗癌药物的相互作用

摘要

Studies of submillimeter gels composed of covalently cross-linked poly(acrylic acid)-g-poly(ethylene oxide)-b-poly(propylene oxide)-b-poly(ethylene oxide) (Pluronic-PAA) networks are reviewed in light of potential applications of the microgels as drug carriers in oral delivery. The microgels are capable of volumetric transitions in response to environmental stimulae such as pH and temperature. It is shown that the type of Pluronic used in the microgel synthesis changes the structure of the resulting microgels, with the more hydrophobic Pluronic imparting porosity. Microgels based on Pluronic L92 (L92-PAA-EGDMA) possess higher ion-exchange capacity than microgels based on Pluronic F127 (F127-PAA-EGDMA), albeit the former are more hydrophobic. Analogously, more hydrophobic but heterogeneous L92-PAA-EGDMA exhibit superior capacity for equilibrium loading of hydrophobic drugs such as taxol, camptothecin and steroid hormones, as well as higher capacity for weakly basic drugs such as doxorubicin, mitomycin C, and mitoxantrone.
机译:综述了共价交联的聚(丙烯酸)-g-聚环氧乙烷-b-聚环氧丙烷-b-聚环氧乙烷(Pluronic-PAA)网络组成的亚毫米凝胶的研究。微凝胶作为药物载体在口服给药中的潜在应用。所述微凝胶能够响应于诸如pH和温度的环境刺激而发生体积转变。结果表明,在微凝胶合成中使用的Pluronic的类型改变了所得微凝胶的结构,同时疏水性更高的Pluronic赋予了孔隙度。基于Pluronic L92的微凝胶(L92-PAA-EGDMA)比基于Pluronic F127的微凝胶(F127-PAA-EGDMA)具有更高的离子交换能力,尽管前者具有更高的疏水性。类似地,疏水性更高但异构性更高的L92-PAA-EGDMA对疏水性药物(如紫杉醇,喜树碱和类固醇激素)的平衡负载表现出较高的容量,对弱碱性药物(如阿霉素,丝裂霉素C和米托蒽醌)的容量较高。

著录项

  • 作者

    Bromberg Lev; Hatton T. Alan;

  • 作者单位
  • 年度 2003
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  • 原文格式 PDF
  • 正文语种 en_US
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