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介孔有机硅纳米载体的功能化用于 pH/谷胱甘肽双重响应药物递送和癌症治疗过程的成像。

Functionalization of mesoporous organosilica nanocarrier for pH/glutathione dual-responsive drug delivery and imaging of cancer therapy process.

机构信息

Research Center for Analytical Sciences, College of Sciences, Northeastern University, Box 332, Shenyang 110819, China.

Institute of Biotechnology, College of Life and Health Sciences, Northeastern University, Shenyang 110169, China.

出版信息

Talanta. 2018 Jan 15;177:203-211. doi: 10.1016/j.talanta.2017.07.017. Epub 2017 Jul 13.

DOI:10.1016/j.talanta.2017.07.017
PMID:29108577
Abstract

A multifunctional drug nanocarrier is developed by incorporating acetaldehyde-modified-cystine (AMC) into mesoporous organosilica nanoparticles (MONs), shortly termed as MONs-AMC. The anticancer drug doxorubicin (DOX) links directly to MONs-AMC through electrostatic interaction between DOX and AMC to produce a conjugate, MONs-AMC-DOX, with a drug loading efficiency of 26.24 ± 1.35%, corresponding to a loading capacity of 0.26 ± 0.01mgmg for DOX. Schiff base AMC contains a -S-S- bond and two -C˭N- bonds which cleave in the presence of certain level of GSH and in an acidic medium, providing MONs-AMC-DOX the capability for triggering pH and glutathione (GSH) dual-responsive drug release. Further, the self-fluorescent nature of AMC offers the tracing capability without the need of fluorescent label, which facilitates real-time tracing of the drug delivery and cancer therapy process. With 10mmolL GSH and at pH 5.0, a drug release efficiency of 52.27 ± 2.84% is achieved. The intracellular drug release process is traced with confocal laser scanning microscope by monitoring the green fluorescence of MONs-AMC-DOX and red fluorescence of DOX with excitation at 408nm and 488nm, respectively. The drug loaded nanocarriers exhibit a time-dependent cellular uptake behavior, providing an enhanced therapeutic effect to A549 cancer cells.

摘要

多功能药物纳米载体通过将乙二醛修饰的半胱氨酸(AMC)纳入介孔有机硅纳米颗粒(MONs)中开发而成,简称 MONs-AMC。抗癌药物阿霉素(DOX)通过 DOX 和 AMC 之间的静电相互作用直接与 MONs-AMC 连接,产生一种药物负载效率为 26.24±1.35%,相应的 DOX 负载量为 0.26±0.01mgmg 的缀合物,MONs-AMC-DOX。席夫碱 AMC 含有一个 -S-S-键和两个 -C˭N-键,在一定水平的 GSH 和酸性介质存在下会断裂,使 MONs-AMC-DOX 具有触发 pH 和谷胱甘肽 (GSH) 双重响应药物释放的能力。此外,AMC 的自荧光性质提供了无需荧光标记的追踪能力,这有利于药物输送和癌症治疗过程的实时追踪。在 10mmolL GSH 和 pH 5.0 下,实现了 52.27±2.84%的药物释放效率。通过监测 MONs-AMC-DOX 的绿色荧光和 DOX 的红色荧光,分别在 408nm 和 488nm 处激发,用共聚焦激光扫描显微镜追踪细胞内药物释放过程。载药纳米载体表现出时间依赖性的细胞摄取行为,为 A549 癌细胞提供了增强的治疗效果。

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