水溶性β-环糊精与华法林/阿魏酸包合物的制备及抗凝血性质测试和机理分析

采用研磨法和蒸馏法制备了阿魏酸(Ferulic acid,FA)和华法林(Warfarin,W)与β-环糊精(β-CD)的二元包合物,并采用红外光谱、紫外光谱、差热分析、扫描电镜和X粉末衍射法对其进行了表征,并在生理条件下研究了包合物的抗凝血性质及其与人血清白蛋白(Human serum albumin,HSA)的相互作用。结果表明,包合物的水溶性(包和物的溶解度约为5 g/L,华法林和阿魏酸为难溶物)和抗凝血指标都优于阿魏酸和华法林。与HSA作用的光谱结果表明,包合物可与HSA相互结合,增强了药物的血溶性,通过生成包合物避免了药物阿魏酸被氧化而失去原有的药效作用。说明华法林和阿魏酸经医药载体β-CD包合后水溶性增大,疗效增强,与HSA结合后可以达到药物通过血液输送的目的。

稀土华法林阿魏酸三元配合物的制备及抗凝血作用

用华法林(W)、阿魏酸(FA)与La,Nd,Ce,Eu的稀土硝酸盐反应合成了4个三元稀土配合物,并用红外光谱、热重分析、元素分析、X射线粉末衍射和核磁共振波谱等方法对配合物进行了表征,确定了三元配合物的组成.在生理条件下测试了该三元配合物的全血凝血时间(CT)、复钙时间(RT)、活化部分凝血活酶时间(APTT)、凝血酶原时间(PT)和生物相容性,并与稀土华法灵、稀土阿魏酸二元配合物及配体的抗凝血性质进行了比较.结果表明,4个三元稀土配合物均具有比二元配合物和配体更好的抗凝血性质.生物相容性实验结果表明4个配合物对人肝癌细胞(Hep G2)、人肺癌细胞(A549)和人宫颈癌细胞(He La)的活性无明显影响.通过荧光光谱、紫外光谱和圆二色谱考察了三元配合物与人血清白蛋白(HSA)之间的相互作用.结果表明,配合物可以与HSA相互结合从而增强药物的血溶性,避免了阿魏酸被氧化而失去原有的药效.

PEGylation of Hirudin and Analysis of Its Antithrombin Activity in vitro

Hirudin is the most anticoagulant drug found in nature, but its short serum half-life significantly inhibits its clinical anpplication. The PEGvlation of hirudin, the most promising anticoagulant drug, was performed in this paper. The optimal reaction conditions for PEG ylated hirudin were investigated, wh.en the PEGylation react, on.wasconducted under 4℃ after 10h, in the borate buffer at pH 8.5 .with the molar ratio 230 ： 1 of PEG to hirudin, a higher modification extent was achieved. Finally, the bioactivity of PEGylated hirudin was measured in vitro.Compared with unmodified hirudin, 26% of anti-thrombin activity was retained.