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首页> 外文期刊>Journal of nanoscience and nanotechnology >Stability of Hepatoprotecting Agent IFC-305 Encapsulated into Sol-Gel Titania Nanoparticles and Drug Release Evaluation: Water and Drug Concentration Effect
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Stability of Hepatoprotecting Agent IFC-305 Encapsulated into Sol-Gel Titania Nanoparticles and Drug Release Evaluation: Water and Drug Concentration Effect

机译:溶胶-凝胶二氧化钛纳米颗粒中保肝剂IFC-305的稳定性和药物释放评价:水和药物浓度的影响

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摘要

IFC-305 was encapsulated into nanostructured titania and functionalized with OH groups by the sol-gel process using titanium n-butoxide, to be used in a drug delivery system for the treatment of liver cancer. Synthesis was carried out at different molar hydrolysis ratios: 4, 8, 16 and 24 mol of water; and drug concentration of 10, 20 and 30%. Characterization of IFC-titania reservoirs was carried out by Fourier transformed infrared spectroscopy (FTIR), X-ray diffraction (XRD), thermal analysis (DTA-TGA), scanning electron microscopy (SEM), and N_2 adsorption-desorption isotherms (BET), confirms that IFC-305 is entrapped and stabilized in the TiO_2-OH matrix. Drug liberation in vitro was determined by UV spectrometry over a period of 1000 h. This study demonstrated that the higher water content and the higher amount of loaded IFC, favored hydrogen bonding between titania-OH surface and IFC-NH groups, increasing the rate of drug release.
机译:将IFC-305封装到纳米结构的二氧化钛中,并使用正丁醇钛通过溶胶-凝胶法将其用OH基团官能化,以用于治疗肝癌的药物递送系统。合成是在不同的摩尔水解比下进行的:4、8、16和24摩尔水;药物浓度分别为10%,20%和30%。通过傅里叶变换红外光谱(FTIR),X射线衍射(XRD),热分析(DTA-TGA),扫描电子显微镜(SEM)和N_2吸附-解吸等温线(BET)对IFC-二氧化钛储层进行表征证实IFC-305被捕获并稳定在TiO_2-OH基体中。通过紫外光谱在1000小时内测定体外药物释放。这项研究表明,较高的水分含量和较高的IFC负载量有利于二氧化钛-OH表面与IFC-NH基团之间的氢键结合,从而增加了药物释放的速率。

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