PVP和PEG表面修饰对有序介孔碳纳米粒分散性及细胞毒性的影响

目的通过聚乙烯吡咯烷酮(PVP)和培化磷脂酰乙醇胺(DSPE-mPEG2000)对制备的有序介孔碳纳米粒(MCN)进行表面修饰,以改善材料的疏水性质,并考察其对MCN分散性和细胞毒性的影响。方法采用低浓度水热法合成MCN,并用PVP和DSPE-mPEG2000对其表面修饰,采用透射电镜(TEM)、扫描电镜(SEM)、氮气吸附脱附仪、粒径仪和红外(IR)等表征其性质。考察了表面修饰对MCN分散性的影响,并用CCK-8法考察材料的细胞毒性,用流式细胞术检测材料对细胞氧化应激的影响。结果制备的MCN粒径分布均一,平均粒径约90nm,修饰后的粒径略有增大,Zeta电位稍有升高,分散性明显提高,但修饰前后材料对小鼠成纤维细胞(L929)和宫颈癌细胞(HeLa)的毒性没有显著性差异,在相同浓度下,修饰后的MCN能明显减少细胞氧化应激的产生。结论 MCN具有良好的生物相容性,用PVP和DSPE-mPEG2000修饰后的MCN能明显减少细胞氧化应激的发生。

基于介孔碳纳米粒包载胰岛素实现口服递药的研究

目的利用介孔碳纳米粒(MCN)包载胰岛素从而实现口服缓释递药。方法 (1)制备与表征:制备包载胰岛素的介孔碳纳米粒(MCN-I),通过扫描电镜和透射电镜进行表征,高效液相色谱测定包封率和载药量,激光粒度仪测定粒径、多分散系数及Zeta电位,考察MCN-I的体外释放性能。(2)体内分布实验:按照体重将SD大鼠随机分为4组:荧光标记胰岛素(FI)灌胃组(10 mg·kg^(-1))、介孔碳纳米粒包载荧光标记胰岛素(MCN-FI)灌胃组(10 mg·kg^(-1))、尾静脉注射FI组(10 mg·kg^(-1))和空白组(灌胃0.9%的生理盐水),每组3只。用荧光显微镜观察并统计大鼠心、肝、脾、肺、肾和脑的平均荧光强度。(3)体内药效实验:将糖尿病模型大鼠随机分4组:皮下注射胰岛素组(5 U·kg^(-1)),MCN-I灌胃组(50 U·kg^(-1)),MCN灌胃组(5 mg·kg^(-1))和胰岛素灌胃组(50 U·kg^(-1)),每组6只。用血糖仪测定12 h内的血糖变化。结果 (1)成功制备MCN-I,包封率为(65.18±1.59)%,载药量为(20.19±1.18)%,平均粒径为(195.00±2.80) nm,多分散系数为0.24±0.01,Zeta电位为(-26.47±1.28)mV,MCN-I在盐酸溶液(pH 1.0)中2 h和磷酸盐缓冲液(pH 6.8)中6 h的累积释放量分别为(36.0±2.0)%和(70.3±3.6)%。(2)MCN-FI灌胃组和尾静脉注射FI组的心、肝、脾、肺、肾组织平均荧光强度与空白组比较,差异均有统计学意义(均P<0.0001),说明MCN可以保护FI通过口服吸收进入血液循环。(3)MCN-I灌胃给予糖尿病模型大鼠在2 h后开始缓慢降低血糖,8 h时达到最低血糖值,为初始血糖值的(28.5±3.6)%,具有缓释降糖效果。结论介孔碳纳米粒可保护胰岛素口服吸收进入血液循环发挥药效,有望开发成为一种多肽、蛋白质类药物口服递药的载体。

Size-control growth of thermally stable Au nanoparticles encapsulated within ordered mesoporous carbon framework

Simultaneously controlling the size of Au nanoparticles and immobilizing their location to specific active sites while hindering migration and sintering at elevated temperatures is a current challenge within materials chemistry.Typical methods require the use of protecting agents to control the properties of Au nanoparticles and therefore it is difficult to decouple the influence of the protecting agent and the support material.By functionalizing the internal surface area of mesoporous carbon supports with thiol groups and implementing a simple acid extraction step,we are able to design the resulting materials with precise control over the Au nanoparticle size without the need for the presence of any protecting group,whilst simultaneously confining the nanoparticles to within the internal porous network.Monodispersed Au nanoparticles in the absence of protecting agents were encapsulated into ordered mesoporous carbon at various loading levels via a coordination-assisted self-assembly approach.The X-ray diffractograms and transmission electron microscopy micrographs show that the particles have controlled and well-defined diameters between 3 and 18 nm at concentrations between 1.1 and 9.0 wt%.The Au nanoparticles are intercalated into the pore matrix to different degrees depending on the synthesis conditions and are stable after high temperature treatment at 600 °C.N2 adsorption-desorption isotherms show that the Au functionalized mesoporous carbon catalysts possess high surface areas（1269–1743 m^2/g）,large pore volumes（0.78–1.38 cm^3/g）and interpenetrated,uniform bimodal mesopores with the primary larger mesopore lying in the range of 3.4–5.7 nm and the smaller secondary mesopore having a diameter close to 2 nm.X-ray absorption near extended spectroscopy analysis reveals changes to the electronic properties of the Au nanoparticles as a function of reduced particle size.The predominant factors that significantly determine the end Au nanoparticle size is both the thiol group concentration and subjecting the as-made materials to an additional concentrated sulfuric acid extraction step.