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首页> 外文期刊>Nanotechnology >The grafting and release behavior of doxorubincin from Fe3O4@SiO2 core-shell structure nanoparticles via an acid cleaving amide bond: the potential for magnetic targeting drug delivery
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The grafting and release behavior of doxorubincin from Fe3O4@SiO2 core-shell structure nanoparticles via an acid cleaving amide bond: the potential for magnetic targeting drug delivery

机译:阿霉素从Fe3O4 @ SiO2核壳结构纳米粒子的接枝和释放行为通过酸裂解酰胺键:磁性靶向药物输送的潜力。

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摘要

Fe3O4@SiO2 core-shell structure nanoparticles were first prepared and characterized by TEM, FTIR, XPS and XRD. Subsequently the widely used anticancer agent doxorubincin ( DOX) was successfully grafted to the surface of the core-shell nanoparticles via an amide bond with the aid of a spacer arm we synthesized. The spacer arm met two needs: one end can couple to the core-shell nanoparticles' surface while the other end was the active -COOH group, which can react with the -NH2 group of DOX molecules. The synthesized spacer arm and the conjugation of the drug with nanoparticles through amidation were confirmed by FTIR. The DOX-loading efficiency determined by UV-vis spectrometer was 86.5%. Drug release experiments displayed a pH-dependent behavior that DOX was cleaved from the nanoparticles easily under low pH conditions in the presence of protease and that most of the conjugated doxorubincin were released within the first 12 h. The prepared DOX-grafted Fe3O4@SiO2 core-shell structure nanoparticles showed a superparamagnetic property with a saturation magnetization value of 49.3 emu g(-1), indicating a great potential application in the treatment of cancer using magnetic targeting drug-delivery technology.
机译:首先制备了Fe3O4 @ SiO2核壳结构纳米粒子,并通过TEM,FTIR,XPS和XRD对其进行了表征。随后,借助于我们合成的间隔臂,通过酰胺键成功地将广泛使用的抗癌药阿霉素(DOX)接枝到核-壳纳米颗粒的表面。间隔臂满足两个需求:一端可以偶联到核壳纳米粒子的表面,而另一端是活性的-COOH基团,该基团可以与DOX分子的-NH2基团反应。 FTIR证实了合成的间隔臂和酰胺化作用下药物与纳米颗粒的结合。紫外可见分光光度计测得的DOX负载率为86.5%。药物释放实验显示了pH依赖性的行为,即在蛋白酶存在下,在低pH条件下,DOX容易从纳米颗粒上裂解下来,并且大多数缀合的阿霉素都在最初的12小时内释放出来。制备的DOX接枝的Fe3O4 @ SiO2核-壳结构纳米粒子表现出超顺磁性,饱和磁化值为49.3 emu g(-1),表明使用磁性靶向药物递送技术在癌症治疗中具有巨大的潜力。

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