Intelligent Gold Nanoparticles with Oncogenic MicroRNA-Dependent Activities to Manipulate Tumorigenic Environments for Synergistic Tumor Therapy

被引:76
作者
Wang, Xiangdong [1 ]
Yang, Tianfeng [2 ]
Yu, Zhi [1 ]
Liu, Tao [1 ]
Jin, Ronghua [1 ]
Weng, Lin [1 ]
Bai, Yongkang [1 ]
Gooding, J. Justin [3 ,4 ]
Zhang, Yanmin [2 ]
Chen, Xin [1 ]
机构
[1] Xi An Jiao Tong Univ, Sch Chem Engn & Technol, Inst Polymer Sci Chem Engn, Dept Chem Engn,Shaanxi Key Lab Energy Chem Proc I, Xian 710049, Peoples R China
[2] Xi An Jiao Tong Univ, Hlth Sci Ctr, Sch Pharm, Xian 710061, Peoples R China
[3] Univ New South Wales, Sch Chem, Sydney, NSW 2052, Australia
[4] Univ New South Wales, Australian Ctr NanoMed, Sydney, NSW 2052, Australia
关键词
intelligent gold nanoparticles; miR-155-triggered chemotherapy; oncogenic microRNA (miR-155; miR-21); photothermal therapy; tumorigenic environment; GENE-THERAPY; OLIGONUCLEOTIDE; DELIVERY;
D O I
10.1002/adma.202110219
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Tumorigenic environments, especially aberrantly overexpressed oncogenic microRNAs, play a critical role in various activities of tumor progression. However, developing strategies to effectively utilize and manipulate these oncogenic microRNAs for tumor therapy is still a challenge. To address this challenge, spherical nucleic acids (SNAs) consisting of gold nanoparticles in the core and antisense oligonucleotides as the shell are fabricated. Hybridized to the oligonucleotide shell is a DNA sequence to which doxorubicin is conjugated (DNA-DOX). The oligonucleotides shell is designed to capture overexpressed miR-21/miR-155 and inhibit the expression of these oncogenic miRNAs in tumor cells after tumor accumulation to manipulate genetic environment for accurate gene therapy. This process further induces the aggregation of these SNAs, which not only generates photothermal agents to achieve on-demand photothermal therapy in situ, but also enlarges the size of SNAs to enhance the retention time in the tumor for sustained therapy. The capture of the relevant miRNAs simultaneously triggers the intracellular release of the DNA-DOX from the SNAs to deliver tumor-specific chemotherapy. Both in vivo and in vitro results indicate that this combination strategy has excellent tumor inhibition properties with high survival rate of tumor-bearing mice, and can thus be a promising candidate for effective tumor treatment.
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页数:13
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