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Luminescent mesoporous nanoreservoirs for the effective loading and intracellular delivery of therapeutic drugs

机译:发光的中孔纳米储库,用于有效加载和细胞内递送治疗药物

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Development of biocompatible and multifunctional nanocarriers is important for the therapeutic efficacy of drug molecules in the treatment of disease and tissue repair. A novel nanocarrier of luminescent hollowed mesoporous silica (L-hMS) was explored for the loading and controlled delivery of drugs. For the synthesis of L-hMS, self-activated luminescence hydroxyapatite (LHA) was used as a template. Different thicknesses (~7-62 nm) of mesoporous silica shell were obtained by varying the volume of silica precursor and the subsequent removal of the LHA core, which resulted in hollow-cored (size of ~40 nm × 10 nm) mesoporous silica nanoreservoirs, L-hMS. While the silica shell provided a highly mesoporous structure, enabling an effective loading of drug molecules, the luminescent property of LHA was also well preserved in both the silica-shelled and the hollow-cored nanocarriers. Doxorubicin (DOX), used as a model drug, was shown to be effectively loaded onto the mesopore structure and within the hollow space of the nanoreservoir. The DOX release was fairly pH-dependent, occurring more rapidly at pH 5.3 than at pH 7.4, and a long-term sustainable delivery over the test period of 2 weeks was observed. The nanoreservoir exhibited favorable cell compatibility with low cytotoxicity and excellent cell uptake efficiency (over 90%). Treatment of HeLa cells with DOX-loaded L-hMS elicited a sufficient degree of biological efficacy of DOX, as confirmed in the DOX-induced apoptotic behaviors, including stimulation in caspase-3 expression, and was even more effective than the direct DOX treatment. Overall, the newly developed L-hMS nanoreservoirs may be potentially useful as a multifunctional (luminescent, mesoporous and biocompatible) carrier system to effectively load and sustainably deliver small molecules, including anticancer drugs.
机译:生物相容性和多功能纳米载体的开发对于药物分子在疾病治疗和组织修复中的治疗功效非常重要。探索了一种新型的发光空心中孔二氧化硅(L-hMS)纳米载体,用于药物的加载和控制传递。对于L-hMS的合成,以自活化发光羟基磷灰石(LHA)为模板。通过改变二氧化硅前体的体积并随后去除LHA核,获得了不同厚度(约7-62 nm)的介孔二氧化硅壳,从而形成了中空的(约40 nm×10 nm大小)介孔二氧化硅纳米储库,L-hMS。尽管二氧化硅壳提供了高度介孔的结构,能够有效装载药物分子,但在二氧化硅壳和空心纳米载体中,LHA的发光特性也得到了很好的保留。已显示用作模型药物的阿霉素(DOX)可有效地加载到中孔结构上和纳米储器的中空空间内。 DOX的释放相当依赖于pH值,在pH 5.3时比在pH 7.4时发生更快,并且在2周的测试期间内观察到了长期可持续的释放。纳米储库显示出良好的细胞相容性,低细胞毒性和优异的细胞摄取效率(超过90%)。如在DOX诱导的凋亡行为(包括刺激caspase-3表达)中所证实的那样,用DOX加载的L-hMS处理HeLa细胞引起了足够程度的DOX生物学功效,甚至比直接DOX处理更有效。总体而言,新开发的L-hMS纳米储库可能具有作为多功能(发光,中孔和生物相容性)载体系统的潜力,可有效装载和可持续地输送包括抗癌药在内的小分子。

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