材料科学
纳米颗粒
化学工程
封装(网络)
PLGA公司
共聚物
纳米技术
聚合物
复合材料
计算机科学
计算机网络
工程类
作者
Mengyue Gan,Wenping Zhang,Shijie Wei,Dang Hong-wan
标识
DOI:10.3109/21691401.2016.1167700
摘要
The influence of mPEG-PCL and mPEG-PLGA on encapsulation efficiency and drug-loading of nanoparticles was very important. SN-38 NPs were prepared from a series of diblock copolymers: mPEG1000-PLGA2000, mPEG2000-PCLs, mPEG5000-PCLs, mPEG2000-PLGAs, and mPEG5000-PLGAs by the thin film-hydration method. The prepared nanoparticles were characterized by morphology, size, encapsulation efficiency, drug-loading, and in vitro release behavior. This experiment suggested that the encapsulation efficiency and drug-loading of SN-38 NPs were attained the maximum values when the ratio of hydrophilic to hydrophobic block was between 1:2 and 1:3.
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