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Drug delivery system composed of mesoporous silica and hollow mesoporous silica nanospheres for chemotherapeutic drug delivery

机译:药物递送系统由介孔二氧化硅和中空介孔二氧化硅纳米体组成,用于化学治疗药物递送

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摘要

Mesoporous silica nanoparticles (MSN) and hollow mesoporous silica nanoparticles (HMSN) of the size of similar to 200 nm have been synthesized from iron silicate via selective etching of iron oxide and were used to deliver a prominent anticancer drug doxorubicin under external stimuli. The facile synthesis of MSN and HMSN involves synthesis of iron silicate coated by iron oxide and silica in a layer by layer (LbL) fashion followed by selective etching of iron oxide under mild conation. Among all the particles, HMSN has less surface area (100 m(2)/g) and larger pore size (4.62 nm). We demonstrated that both MSN and HMSN release the drug over a period of 4 h under external stimuli (acidic pH). The release profile reveals that HMSN release comparatively less amount of drug as compared to MSN. This could be attributed to the larger pore volume (0.52 cc/g) of MSN as compared to HMSN (0.20 cc/g). The particles neither show any cytotoxicity towards the HeLa cells up to 350 mu g/ml nor any morphological change to the nucleus of the cells. The cytotoxicity value was much higher compared to the literature reports on MSN. This implies a better biocompatibility of the particles prepared through this methodology.
机译:通过选择性蚀刻铁氧化铁,通过选择性蚀刻来合成了与200nm相似的介孔二氧化硅纳米颗粒(MSN)和中空介孔二氧化硅纳米颗粒(HMSN),并用于在外部刺激下递送突出的抗癌药物多柔比星。 MSN和HMSN的容易合成涉及通过层(LBL)时的层中的氧化铁和二氧化硅涂覆的铁硅酸盐的合成,然后在温和的旋转中选择性蚀刻氧化铁。在所有颗粒中,HMSN具有较少的表面积(100m(2)/ g)和较大的孔径(4.62nm)。我们证明了MSN和HMSN在外部刺激(酸性pH)下在4小时内释放药物。释放型材显示,与MSN相比,HMSN释放相对较少的药物。与HMSN(0.20cc / g)相比,这可能归因于MSN的较大孔体积(0.52cc / g)。颗粒既不显示出朝向HeLa细胞的任何细胞毒性,高达350μg/ ml也不是细胞核的任何形态变化。与MSN上的文献报告相比,细胞毒性值得高得多。这意味着通过该方法制备的颗粒的更好的生物相容性。

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