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首页> 外文期刊>Journal of Materials Science >Effect of amino-functionalization on insulin delivery and cell viability for two types of silica mesoporous structures
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Effect of amino-functionalization on insulin delivery and cell viability for two types of silica mesoporous structures

机译:氨基官能化对两种类型的二氧化硅介孔结构的胰岛素传递和细胞活力的影响

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Inorganic mesoporous structures are a class of novel biomaterials that have shown practical applications in delivery of a variety of therapeutic agents. In the present study, two mesoporous structures were prepared, and the effect of surface modification on their insulin delivery and in vitro cytotoxicity was evaluated. Morphological and structural characterizations of silica particles were accomplished by different analytical techniques, including scanning electron microscopy, X-ray diffraction, Fourier transform infrared spectroscopy (FTIR), and Brunauer-Emmett-Teller (BET) surface area analyses. The drug loading capacity and in vitro drug release behavior of silica structures were investigated under simulated gastrointestinal conditions and phosphate-buffered saline solution using FTIR and UV-Vis spectroscopy. In vitro cytotoxicity evaluation was carried out via MTT assay. Results showed that the morphology of MCM-41 was round, while SBA-15 was wheat like, both possessed almost homogeneous size distribution. Also, modification with amine did not influence the morphology and structure of the particles. Both MCM-41 and SBA-15 particles were found to have narrow pore-size distributions of 2.8 and 6.8 nm, respectively. SBA-15 particles demonstrated a high insulin loading capacity of about 15.1 %, while MCM-41 and modified MCM-41 (mMCM-41) were observed to load virtually no insulin at all. The surface modification by amino groups resulted in higher insulin loading and the slower rate of release for modified SBA-15 (mSBA-15) compared to the non-modified SBA-15 (SBA-15). According to the cytotoxicity evaluation results, all of the samples showed cytotoxicity Grade 0-1, in a concentration-dependent manner. Moreover, insulin-loaded mSBA-15 particles exhibited higher cell viability compared to the others. It was concluded that amine modification of SBA-15 could result in higher loading and extended release of insulin and more cell viability.
机译:无机介孔结构是一类新颖的生物材料,已显示出在输送各种治疗剂中的实际应用。在本研究中,制备了两个中孔结构,并评估了表面修饰对其胰岛素递送和体外细胞毒性的影响。二氧化硅颗粒的形态和结构表征是通过不同的分析技术完成的,包括扫描电子显微镜,X射线衍射,傅立叶变换红外光谱(FTIR)和Brunauer-Emmett-Teller(BET)表面积分析。使用FTIR和UV-Vis光谱在模拟胃肠道条件和磷酸盐缓冲盐溶液下研究了二氧化硅结构的载药量和体外释药行为。经由MTT测定法进行体外细胞毒性评估。结果表明,MCM-41的形态为圆形,而SBA-15的形态类似于小麦,两者的大小分布几乎均一。同样,用胺改性不会影响颗粒的形态和结构。发现MCM-41和SBA-15颗粒分别具有2.8和6.8 nm的窄孔径分布。 SBA-15颗粒显示出约15.1%的高胰岛素负载能力,而观察到MCM-41和修饰的MCM-41(mMCM-41)几乎根本没有负载胰岛素。与未修饰的SBA-15(SBA-15)相比,修饰的SBA-15(mSBA-15)的氨基表面修饰导致较高的胰岛素负载和较慢的释放速率。根据细胞毒性评估结果,所有样品均以浓度依赖的方式显示出0-1级的细胞毒性。此外,与其他药物相比,载有胰岛素的mSBA-15颗粒具有更高的细胞活力。结论是,SBA-15的胺修饰可导致更高的负载量和胰岛素的延长释放以及更多的细胞活力。

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