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Effects of pore size on in vitro and in vivo anticancer efficacies of mesoporous silica nanoparticles

机译:孔径对介孔二氧化硅纳米粒子体内外抗癌效果的影响

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Mesoporous silica nanoparticles (MSN) have been widely applied for drug delivery systems. To investigate the effects of pore size on anticancer efficacies, MSN with different pore sizes but similar particle sizes and surface charges were synthesized via a microemulsion method. The pore structures of MSN were characterized by transmission electron microscopy (TEM), small-angle X-ray scattering (SAXS), and N _(2) adsorption–desorption isotherms. Doxorubicin loaded MSN (DOX/MSN) were prepared and the minimum drug loading capacity was detected in DOX/MSN with a pore size of 2.3 nm (DOX/MSN2). DOX/MSN with a pore size of 8.2 nm (DOX/MSN8) showed a comparable drug loading amount in comparison with ones with a pore size of 5.4 nm (DOX/MSN5). In vitro drug release profiles showed that DOX/MSN5 could release DOX quickly and completely. Compared with DOX/MSN2 and DOX/MSN8, DOX/MSN5 showed the higher cellular uptake and nucleic concentration of DOX in QGY-7703 cells, which led to efficient cell-apoptosis induction and anti-proliferation effect, and thus the optimal in vivo anticancer activities. Taken together, these results highlighted the importance of pore size in anticancer efficacies, which would serve as a guideline in the rational design of MSN for cancer therapy.
机译:介孔二氧化硅纳米颗粒(MSN)已广泛应用于药物输送系统。为了研究孔径对抗癌效果的影响,通过微乳液法合成了孔径不同但粒径和表面电荷相似的MSN。 MSN的孔结构通过透射电子显微镜(TEM),小角X射线散射(SAXS)和N _(2)吸附-解吸等温线表征。制备了载有阿霉素的MSN(DOX / MSN),并在孔径为2.3 nm(DOX / MSN2)的DOX / MSN中检测到最小载药量。孔径为8.2 nm的DOX / MSN(DOX / MSN8)与孔径为5.4 nm的DOX / MSN(DOX / MSN5)具有可比的载药量。体外药物释放曲线表明,DOX / MSN5可以快速完全释放DOX。与DOX / MSN2和DOX / MSN8相比,DOX / MSN5在QGY-7703细胞中具有更高的细胞摄取和DOX核酸浓度,从而导致有效的细胞凋亡诱导和抗增殖作用,因此是最佳的体内抗癌药活动。综上所述,这些结果突出了孔径在抗癌功效中的重要性,这可作为合理设计MSN用于癌症治疗的指南。

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