催化作用
材料科学
小RNA
纳米技术
DNA
癌症
纳米颗粒
计算生物学
组合化学
化学
生物化学
生物
基因
遗传学
作者
Xucheng Luo,Zhi Li,Ganglin Wang,Xuewen He,Xiaoqin Shen,Quanhong Sun,Li Wang,Renye Yue,Nan Ma
标识
DOI:10.1021/acsami.7b09420
摘要
The use of cancer-relevant microRNA molecules as endogenous drug release stimuli is promising for personalized cancer treatment yet remains a great challenge because of their low abundance. Herein, we report a new type of microRNA-catalyzed drug release system based on DNA-programmed gold nanoparticle (GNP)-quantum dot (QD) complex. We show that a trace amount of miRNA-21 molecules could specifically catalyze the disassembly of doxorubicin (Dox)-loaded GNP-QDs complex through entropy driven process, during which the Dox-intercalating sites are destructed for drug release. This catalytic reaction could proceed both in fixed cells and live cells with miRNA-21 overexpression. Dox molecules could be efficiently released in the cells and translocate to cell nuclei. QD photoluminescence is simultaneously activated during catalytic disassembly process, thus providing a reliable feedback for microRNA-triggered drug release. The GNP-QDs-Dox complex exhibits much higher drug potency than free Dox molecules, and therefore represents a promising platform for accurate and effective cancer cell treatment.
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