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阿密曲替林在核壳-冠型三嵌段共聚物胶束中的包埋和释放行为。

Incorporation and release behavior of amitriptylene in core-shell-corona type triblock copolymer micelles.

机构信息

Department of Chemistry, Faculty of Science and Engineering, Saga University, 1 Honjo-machi, Saga 840-8502, Japan.

出版信息

Colloids Surf B Biointerfaces. 2011 Dec 1;88(2):734-40. doi: 10.1016/j.colsurfb.2011.08.009. Epub 2011 Aug 17.

Abstract

A cationic antidepressant drug, amitriptylene (AMT), was successfully incorporated into core-shell-corona micelles of poly[styrene-b-sodium 2-(acrylamido)-2-methyl-1-propanesulfonate-b-ethylene oxide] (PS-b-PAMPS-b-PEO). Zeta-potential measurements revealed that both electrostatic and hydrophobic interactions contributed to the binding of the drug to the polymer. The AMT/PS-b-PAMPS-b-PEO nanocomplexes were characterized by dynamic light scattering, scanning electron microscopy, and transmission electron microscopy. The hydrodynamic diameter of the AMT loaded nanocomplexes decreased from 80 to 40nm depending on the amount of the drug loaded on the polymer. This is attributed to the cancellation of the negative charge of the PAMPS group by the cationic drug. The AMT/PS-b-PAMPS-b-PEO nanocomplexes were stable in aqueous solution exhibiting no aggregation or no precipitation for several months. Release of the AMT from the nanocomplexes was investigated in vitro in salt-free and 0.1M NaCl solutions. The drug was released faster in the 0.1M NaCl solution than in the salt-free solution. This is due to the shielding effect of the salt on the electrostatic interaction. However, in both cases, the drug release mainly occurs by the Fickian diffusion mechanism.

摘要

阳离子抗抑郁药阿米替林(AMT)成功地掺入了聚苯乙烯-b-聚(2-丙烯酰胺基-2-甲基-1-丙磺酸)-b-聚环氧乙烷(PS-b-PAMPS-b-PEO)的核壳冠状胶束中。Zeta 电位测量表明,静电和疏水相互作用都有助于药物与聚合物的结合。通过动态光散射、扫描电子显微镜和透射电子显微镜对 AMT/PS-b-PAMPS-b-PEO 纳米复合物进行了表征。载药纳米复合物的水动力直径取决于聚合物上载药量的多少,从 80nm 降低到 40nm。这归因于阳离子药物中和了 PAMPS 基团的负电荷。AMT/PS-b-PAMPS-b-PEO 纳米复合物在水溶液中稳定,数月内无聚集或沉淀。在无盐和 0.1M NaCl 溶液中体外研究了 AMT 从纳米复合物中的释放情况。在 0.1M NaCl 溶液中药物释放速度比在无盐溶液中快。这是由于盐对静电相互作用的屏蔽效应。然而,在这两种情况下,药物释放主要通过菲克扩散机制发生。

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