Engineering self-catabolic DNAzyme nanospheres for synergistic anticancer therapy

被引:0
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作者
Yu Chen [1 ]
Yu Guo [1 ]
Jiaoli Wang [1 ]
Ruiting Liu [1 ]
Xiaohai Yang [1 ]
Kemin Wang [1 ]
Ying Pu [2 ]
Hui Shi [1 ]
Jin Huang [1 ]
机构
[1] Key Laboratory of Chemo/Biosensing and Chemometrics,College of Chemistry and Chemical Engineering,Key Laboratory for Bio-Nanotechnology and Molecular Engineering of Hunan Province,Hunan University
[2] National Clinical Research Center for Geriatric Disorders,Department of Geriatrics,Xiangya Hospital,Central South
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TB383.1 []; R943 [制剂学];
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摘要
DNAzyme-based gene therapy faces some challenges including cell penetration, activity limitation, and co-delivery functions.Self-assembled DNA nanomedicine has attracted widespread attention due to its many advantages. It is urgent to develop a universal DNA degradation strategy for precise programmable drug release. Herein, we reported a self-catabolic DNAzyme nanospheres(SCNS), which could simultaneously achieve cell penetration, activity enhancement, and co-delivery functions. The SCNS were assembled through Y-DNA stepwise hybridization with each other, which were then loaded with aptamer(Apt),doxorubicin(Dox), and zinc oxide nanoparticles(ZnO NPs). The acid-triggered dissociation of ZnO NPs leads to the generation of Zn2+ ions cofactors for immediately self-catabolic DNAzyme nanospheres. After the disassembly of the SCNS, three types of anticancer treatments would be activated, which include Zn2+ involved reactive oxygen species(ROS), Dox-induced chemotherapy, and DNAzyme-based gene therapy. The experimental results show that the nanoplatform(Apt-SCNS-Dox-ZnO) has a good tumor-killing effect and minimal side effects. As a smart self-driven drug delivery nanoplatform, it is anticipated to displace extraordinary potential in biomedicine and bioengineering.
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页码:2412 / 2422
页数:11
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