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Development of surface engineered mesoporous alumina nanoparticles: drug release aspects and cytotoxicity assessment

机译:表面工程介孔氧化铝纳米颗粒的开发:药物释放方面和细胞毒性评估

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The present investigation deals with successful synthesis and surface functionalisation of mesoporous alumina (MeAl) nanoparticles by simplified sol-gel method using cetyl trimethyl ammonium bromide (CTAB) and pluronic as a template. Surface functionalisation of MeAl was performed to determine the selectivity of surface groups for coupling with model drug molecule. Repaglinide a BCS class II drug was loaded as a model drug on synthesised MeAl nanoparticle and studied for its sustained release capability. The synthesised and repaglinide loaded MeAl nanoparticles were characterised by Fourier transform infrared Spectroscopy, X-ray diffraction, field emission scanning electron microscopy with EDAX, Transmission electron microscopy and differential scanning calorimetric. Results from the dissolution study confirmed the sustained release behaviour of the nanparticles which was up to 24 h. The cell viability assay demonstrated that 0.2 to 1 mg/ml concentration of MeAl was significantly less cytotoxic to the Chinese Hamster Ovary (CHO) cells. The authors' experimental studies suggest that MeAl can be used as drug carrier and have a potential to increase the stability, loading efficiency and patient compliance for poorly water-soluble drugs such as repaglinide.
机译:本研究涉及通过使用十六烷基三甲基溴化铵(CTAB)和普朗尼克为模板的简化溶胶-凝胶法成功地合成和介孔氧化铝(MeAl)纳米粒子的表面功能化。进行MeAl的表面官能化以确定表面基团与模型药物分子偶联的选择性。将瑞格列奈BCS II类药物作为模型药物装载在合成的MeAl纳米颗粒上,并对其持续释放能力进行了研究。通过傅立叶变换红外光谱,X射线衍射,EDAX场发射扫描电子显微镜,透射电子显微镜和差示扫描量热法对合成的和负载瑞格列奈的MeAl纳米颗粒进行了表征。溶出度研究的结果证实了纳米颗粒的持续释放行为长达24小时。细胞活力测定表明,浓度为0.2-1 mg / ml的MeAl对中国仓鼠卵巢(CHO)细胞的细胞毒性明显较小。作者的实验研究表明,MeAl可用作药物载体,具有提高水溶性差的药物(例如瑞格列奈)的稳定性,负载效率和患者依从性的潜力。

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