胶束
苯硼酸
药品
化学
药物输送
组合化学
阿霉素
毒品携带者
两亲性
接受者
共聚物
有机化学
药理学
聚合物
化疗
水溶液
医学
催化作用
物理
外科
凝聚态物理
作者
Yu‐Chen Wu,Shixian Lv,Jia Li,Hua He,Yong Ji,Mingfeng Zheng,Yong Liu,Lichen Yin
出处
期刊:Biomaterials Science
[The Royal Society of Chemistry]
日期:2020-01-01
卷期号:8 (3): 949-959
被引量:42
摘要
Simultaneous delivery of multiple chemotherapeutics using polymeric micelles often suffers from unsatisfactory drug loading, drug ratio management, and drug release. Herein, we report a feasible strategy to prepare micelles with ultra-high drug loading and a controllable drug ratio through the introduction of donor-acceptor interactions between drugs and polymeric carriers. An amphiphilic copolymer modified with phenylboronic acid moieties on the hydrophobic segment was synthesized, in which phenylboronic acid functioned as an electron acceptor and formed donor-acceptor coordination with doxorubicin (DOX) and irinotecan (IR). The obtained dual-drug-loaded micelles possessed high drug loading (up to 50%), a tunable drug ratio, and a uniform particle size. Furthermore, both of the encapsulated drug cargoes could be effectively and selectively released in cancer cells with over-produced reactive oxygen species (ROS), and thus the drug-loaded micelles exhibited synergistic anticancer efficacy and reduced systemic toxicity.
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