教授 博士生导师 硕士生导师
主要任职: Professor/ Doctoral Supervisor
性别: 男
毕业院校: 日本秋田大学
学位: 博士
所在单位: 化工海洋与生命学院
联系方式: changhaocui@dlut.edu.cn
电子邮箱: changhaocui@dlut.edu.cn
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论文类型: 期刊论文
发表时间: 2019-11-27
发表刊物: ACS APPLIED MATERIALS & INTERFACES
收录刊物: EI、SCIE
卷号: 11
期号: 47
页面范围: 44582-44592
ISSN号: 1944-8244
关键字: Janus nanoparticles; mesoporous silica nanoparticles; charge reversal; targeted drug delivery; doxorubicin
摘要: Janus nanoparticles with an anisotropic feature concentrated multiple properties on a single carrier, providing synergistic effects. In this study, dual-functionalized Janus nanoparticles (HA-JMSN/DOX-DMMA) were constructed with a tumor-targeting ligand (hyaluronic acid, HA) modified on the one side and a charge reversal group (2,3-dimethylmaleic anhydride, DMMA) on the other side. The drug release of HA-JMSN/DOX-DMMA was positively correlated with the acidity of the environment. The cytotoxicity and cell uptake of HA-JMSN/DOX-DMMA were superior to the isotropous nanoparticles. The endocytosis pathway of HA-JMSN/DOX-DMMA involved the clathrin-mediated endocytosis (HA) and the micropinocytosis (DMMA) at the same time, which indicated that they both participated in the interaction between nanoparticles and tumor cells. After being injected intravenously in mice, the distribution of HA-JMSN/DOX-DMMA in tumor was enhanced significantly. The antitumor therapy study in vivo showed that HA-JMSN/DOX-DMMA inhibited tumor growth and improved the survival rate of tumor-bearing mice effectively. In general, HA-JMSN/DOX-DMMA could take the synergistic effect of active targeting and charge reversal to deliver drug in tumor cells and kill them efficiently, which was a promising antitumor nanodrug.