光热治疗
药物输送
脂质体
材料科学
体内
介孔二氧化硅
纳米技术
纳米颗粒
螯合作用
化学
介孔材料
冶金
生物化学
生物技术
生物
催化作用
作者
Yuhao Gao,Si‐Cong Yang,Mao‐Hua Zhu,Xin‐Di Zhu,Xin Luan,Xue‐Liang Liu,Xing Lai,Yihang Yuan,Qin Lu,Peng Sun,Jonathan F. Lovell,Hongzhuan Chen,Chao Fang
出处
期刊:Small
[Wiley]
日期:2021-06-17
卷期号:17 (29)
被引量:26
标识
DOI:10.1002/smll.202100789
摘要
Abstract Metal‐phenolic networks (MPNs) are an emerging class of supramolecular surface modifiers with potential use in various fields including drug delivery. Here, the development of a unique MPN‐integrated core‐satellite nanosystem (CS‐NS) is reported. The “core” component of CS‐NS comprises a liposome loaded with EDTA (a metal ion chelator) in the aqueous core and DiR (a near‐infrared photothermal transducer) in the bilayer. The “satellite” component comprises mesoporous silica nanoparticles (MSNs) encapsulating doxorubicin and is coated with a Cu 2+ ‐tannic acid MPN. Liposomes and MSNs self‐assemble into the CS‐NS through adhesion mediated by the MPN. When irradiated with an 808 nm laser, CS‐NS liberated the entrapped EDTA, leading to Cu 2+ chelation and subsequent disassembly of the core‐satellite nanostructure. Photo‐conversion from the large assembly to the small constituent particles proceeded within 5 min. Light‐triggered CS‐NS disassembly enhanced the carrier and cargo penetration and accumulation in tumor spheroids in vitro and in orthotopic murine mammary tumors in vivo. CS‐NS is long circulating in the blood and conferred improved survival outcomes to tumor‐bearing mice treated with light, compared to controls. These results demonstrate an MPN‐integrated multistage nanosystem for improved solid tumor treatment.
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