北京大学学报(医学版) ›› 2018, Vol. 50 ›› Issue (6): 1070-1077. doi: 10.3969/j.issn.1671-167X.2018.06.023
郭李盈1,刘晓昕1,李子圆1,覃小雅1,范则杨2,李真真2,关海涛2,宋莉2,邹英华2,范田园1,△()
Li-ying GUO1,Xiao-xin LIU1,Zi-yuan LI1,Xiao-ya QIN1,Ze-yang FAN2,Zhen-zhen LI2,Hai-tao GUAN2,Li SONG2,Ying-hua ZOU2,Tian-yuan FAN1,△()
摘要:
目的: 研究离子交换型载阿霉素聚丙烯酸栓塞微球的制备方法与性质评价。方法: 采用反相悬浮聚合法制备空白聚丙烯酸栓塞微球[poly (acrylic acid) microspheres,PMs],通过离子交换原理将阿霉素载入该微球,制备载阿霉素的聚丙烯酸栓塞微球[doxorubicin-loaded poly (acrylic acid) microspheres,DPMs]。采用光学显微镜考察两种微球的形态和粒径分布,荧光显微镜和激光扫描共聚焦显微镜考察载药微球中阿霉素的分布,物性测定仪测定PMs和DPMs的弹性,HPLC法测定PMs的载药性质和DPMs的释药性质。以0.1 mL的DPMs栓塞家兔肝动脉评价其在动物体内的栓塞效果。结果: 制备的PMs和DPMs形态圆整、表面光滑,能够均匀分散,阿霉素主要分布在靠近微球表面的区域且分布均匀。PMs和DPMs的平均粒径分别为(283±136) μm和(248±149) μm,杨氏模量分别为(62.63±1.65) kPa和(93.94±1.10) kPa,空白和载药微球均具有良好的抗压缩能力。PMs在12 h时达到载药平衡,包封率大于99%,在浓度为5.0 g/L和12.5 g/L的阿霉素溶液中微球的载药量分别为(19.78±0.27) g/L和(49.45±0.37) g/L;DPMs在磷酸盐缓冲液(phosphate buffered saline,PBS)中缓慢释放阿霉素,载药量为(19.78±0.27) g/L和(49.45±0.37) g/L的微球24 h体外累积释放百分数分别为6.82%±0.02%和2.83%±0.10%。影像学结果显示,DPMs成功地栓塞了家兔的肝动脉。结论: 聚丙烯酸微球具有良好的载阿霉素性能,DPMs是一种潜在的可用于动脉化疗栓塞的新型药物递送系统。
中图分类号:
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