Self-assembly of DNA nanospheres with controllable size and self-degradable property for enhanced antitumor chemotherapy

连接器 DNA 内化 生物物理学 体内 纳米技术 药物输送 荧光 化学 材料科学 组合化学 生物化学 细胞 生物 物理 生物技术 量子力学 计算机科学 操作系统
作者
Hui Liu,Yunshan Zhang,Zhoumin Zhang,Zhiwei Deng,Jiaqi Bu,Tianhao Li,Jing Nie,Xiangxiang Qin,Yanjing Yang,Shian Zhong
出处
期刊:Colloids and Surfaces B: Biointerfaces [Elsevier]
卷期号:222: 113122-113122 被引量:2
标识
DOI:10.1016/j.colsurfb.2022.113122
摘要

Controllable size, self-degradability and targeting property are important for a precise improvement of anticancer effects and reduction of side effects of drug vehicles. Here, a series of DNA nanospheres with controllable size and self-degradation ability were constructed through the hybridization of two i-motif strands and two linker strands for targeted cancer therapy. DNA nanospheres with different sizes were fabricated by regulating the linker sequence, and their pH-responsive self-degradation property was realized by the introduction of the i-motif strand. Moreover, the ZY11 aptamer was introduced to endow the DNA nanospheres with targeting property toward SMMC-7721 cancer cells. The results revealed that the appropriate size of DNA nanospheres (80 nm) highly promoted the internalization by mammalian cells. The results of DLS, AFM and CD spectra showed that the DNA nanospheres were stable in a physiological environment but they self-degraded in a slightly acidic environment due to the existence of the i-motif strand. Moreover, the fluorescence of DOX@AP-NSs2 was triple at pH = 5.0 than at pH = 7.4, which further confirmed the pH-responsive drug release performance. The above results proved that the use of DOX@AP-NSs2 is a promising approach to accelerate the rapid release of drugs into the tumors and avoid drug leakage into the normal tissue. The results at a cellular level and in vivo confirmed the pH-responsive targeted antitumor effect. Hence, the novel DNA nanospheres with controllable size and self-degradable property represent a potential tool for targeted drug delivery and cancer therapy.
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