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作 者:胡雄彬[1,2,3] 李风梅 李胜男 王妍 向大雄[1,2,3] 刘新义 HU Xiong-bin;LI Feng-mei;LI Sheng-nan;WANG Yan;XIANG Da-xiong;LIU Xin-yi(Department of Pharmacy,The Second Xiangya Hospital,Central South University,Changsha 410011;Hunan Provincial Engineering Research Centre of Translational Medicine and Innovative Drug,Changsha 410011;Institute of Clinical Pharmacy,Central South University,Changsha 410011)
机构地区:[1]中南大学湘雅二医院药学部,长沙410011 [2]湖南省转化医学与创新药物工程技术研究中心,长沙410011 [3]中南大学临床药学研究所,长沙410011
出 处:《中南药学》2024年第11期2880-2887,共8页Central South Pharmacy
基 金:湖南省自然科学基金项目(No.2024JJ8126);湖南省卫健委项目(No.W20243065);中南大学研究生教育教学改革项目(No.2024JGB158);长沙市自然科学基金项目(No.kq2403088)。
摘 要:目的构建载葛根素的TPP阳离子/MMP肽双修饰脂质体(PUE@T/M-L),并研究其减少心肌缺血/再灌注(I/R)损伤的作用。方法合成TPP-PEG-PE和MMP-PEG-PE高分子材料来修饰脂质体,采用薄膜水化法制备PUE@T/M-L,考察其线粒体靶向性和溶酶体逃逸效果;构建心肌I/R损伤模型,评价PUE@T/M-L对心肌I/R损伤的作用。结果PUE@T/M-L呈圆球形结构,平均粒径为144 nm,Zeta电位为-19.4 mV,具有较好的线粒体靶向性和溶酶体逃逸效果。动物实验结果表明,PUE@T/M-L能显著减少心肌梗死面积,降低心肌细胞凋亡率,其减少心肌I/R损伤作用明显优于其他类型的脂质体,可能与MMP肽靶向和滞留于缺血心肌,再由TPP阳离子靶向递送进入心肌细胞线粒体有关。结论PUE@T/M-L可将药物高效递送至缺血心肌细胞线粒体,从而显著增强葛根素降低心肌I/R损伤的作用。Objective To establish puerarin-carrying TPP cation/MMP peptide co-modified liposomes(PUE@T/M-L)and to determine their effect on myocardial ischemia/reperfusion(I/R)injury.Methods TPP-PEG-PE and MMP-PEG-PE target-head polymer materials were synthesized to modify liposomes.PUE@T/M-L was prepared by thin-film hydration to determine their mitochondrial targeting and lysosomal escape effect,to establish a model of myocardial I/R injury,and to evaluate the effect of PUE@T/M-L in reducing myocardial I/R injury.Results PUE@T/M-L showed a spherical structure with an average particle size of 144 nm and a zeta potential of-19.4 mV,with fair mitochondrial targeting and lysosomal escape effect.PUE@T/M-L largely reduced the area of myocardial infarction and the apoptosis rate of cardiomyocytes.The efficacy of PUE@T/M-L was obviously better than that of other liposomes,which might be related to MMP peptide targeting and retention in the ischemic myocardium,and then the target delivery into the mitochondria of cardiomyocytes by TPP cation.Conclusion PUE@T/M-L can efficiently deliver the drug into the mitochondria of ischemic cardiomyocytes,thus enhancing the drug effect on reducing myocardial I/R injury.
关 键 词:葛根素 心肌缺血/再灌注损伤 线粒体靶向 脂质体
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