Multipronged Design of Light-Triggered Nanoparticles To Overcome Cisplatin Resistance for Efficient Ablation of Resistant Tumor

前药 顺铂 细胞毒性 胶束 流出 生物物理学 癌细胞 多重耐药 化学 癌症研究 光热治疗 抗药性 材料科学 纳米技术 化疗 癌症 生物化学 生物 体外 抗生素 遗传学 物理化学 水溶液 微生物学
作者
Yanli Li,Yibin Deng,Xin Tian,Hengte Ke,Miao Guo,Aijun Zhu,Tao Yang,Zhengqing Guo,Zhishen Ge,Xiangliang Yang,Huabing Chen
出处
期刊:ACS Nano [American Chemical Society]
卷期号:9 (10): 9626-9637 被引量:145
标识
DOI:10.1021/acsnano.5b05097
摘要

Chemotherapeutic drugs frequently encounter multiple drug resistance in the field of cancer therapy. The strategy has been explored with limited success for the ablation of drug-resistant tumor via intravenous administration. In this work, the rationally designed light-triggered nanoparticles with multipronged physicochemical and biological features are developed to overcome cisplatin resistance via the assembly of Pt(IV) prodrug and cyanine dye (Cypate) within the copolymer for efficient ablation of cisplatin-resistant tumor. The micelles exhibit good photostability, sustained release, preferable tumor accumulation, and enhanced cellular uptake with reduced efflux on both A549 cells and resistant A549R cells. Moreover, near-infrared light not only triggers the photothermal effect of the micelles for remarkable photothermal cytotoxicity, but also leads to the intracellular translocation of the micelles and reduction-activable Pt(IV) prodrug into cytoplasm through the lysosomal disruption, as well as the remarkable inhibition on the expression of a drug-efflux transporter, multidrug resistance-associated protein 1 (MRP1) for further reversal of drug resistance of A549R cells. Consequently, the multipronged effects of light-triggered micelles cause synergistic cytotoxicity against both A549 cells and A549R cells, and thus efficient ablation of cisplatin-resistant tumor without regrowth. The multipronged features of light-triggered micelles represent a versatile synergistic approach for the ablation of resistant tumor in the field of cancer therapy.

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