单宁酸
细胞凋亡
癌症
化学
多重耐药
癌症研究
阿霉素
癌细胞
程序性细胞死亡
药理学
细胞生物学
活性氧
生物化学
生物
化疗
有机化学
遗传学
抗生素
作者
Yuxin Guo,Xiaodong Zhang,Wei Sun,Hao‐Ran Jia,Ya‐Xuan Zhu,Xinping Zhang,Ningxuan Zhou,Fu‐Gen Wu
标识
DOI:10.1021/acs.chemmater.9b03042
摘要
Discovering new pathways for overcoming multidrug resistance (MDR) of cancer is important to the development of chemotherapy. Herein, by mixing the metal–phenolic network formed by tannic acid and Fe3+ with the doxorubicin (DOX)-loaded dendrimer (Den), we prepare the Den–DOX–tannic acid–Fe3+ (DDTF) nanocomplex which can combat MDR of cancer cells via an apoptosis/ferroptosis hybrid pathway. The elevated reactive oxygen species (ROS) level caused by DOX-induced apoptosis sensitizes cancer cells to the Fenton reaction-induced ferroptosis and improves the efficiency of chemodynamic therapy (CDT). More interestingly, DDTF can preferably kill the cancer cells over the normal ones, possibly due to the higher hydrogen peroxide content in cancer cells. Besides, DDTF can efficiently transport DOX to the cytosol by evading the drug efflux transporters that are located on the plasma membranes of drug-resistant cancer cells and deliver DOX to the nuclei with the help of Fenton reaction-induced ferroptosis. Afterward, the Fenton reaction- and DOX-induced excessive ROS ultimately kill the drug-resistant cancer cells. In vivo experiments demonstrate that DDTF efficiently targets the tumor after intravenous injection and almost completely eliminates the tumor tissue. This work may foster the development of novel strategies for realizing cancer CDT and overcoming cancer MDR.
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