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机构地区:[1]同济医科大学计划生育研究所,武汉430030
出 处:《同济医科大学学报》1994年第6期473-475,共3页Acta Universitatis Medicinae Tongji
摘 要:利洛司酮与米非司酮均为孕酮受体拮抗剂,它们能在受体水平阻断孕酮作用而发挥催经止孕作用。本文将国产利洛司酮与米非司酮的实验药效学进行了比较性研究,结果表明:利洛司酮与米非司酮经口给药终止小鼠早孕的半数有效量即ED_50(95%可信限)分别为0.38mg/kg(0.27~0.55mg/kg)及0.67mg/kg(0.43~1.06mg/kg),两者药效有显著性差异(P<O.05);其终止大鼠早孕的ED_50(95%可信限)为1.06mg/kg(0.68~1.64mg/kg),及2.46mg/kg(1.72~3.51mg/kg),两者药效有极显著性差异(P<0.01)。此外,利洛司酮经口给药与塞普酮肌内注射给药联合应用时,终止小鼠早孕的效果呈明显的协同效应。Lilopristine and Mifepristone are steroid derivatives with antiprogestrogen property.They block progestrone receptor(PR) and show menses-induction and pregnancytermination effects.In this study,the pharmacodynamic properties of Lilopristone and Mifepristone were compared in experiment.The results are summarized as follows:The oral ED_50 with 95% limits of confidence for Lilopristone in termination of early pregnancy in mice was 0.38mg/kg(0.27~0.55mg/kg),while ED_50 of Mifepristone was 0.67mg/kg(0.43~l.06mg/kg)、Significant difference has been revealed(P<0.05).Results of studies in Sprague Dawley rats showed that the ED_50(oral) of Lilopristone was l.06mg/kg)(0.68~l.64mg/kg),while that of Mifepristone was 2.46mg/kg(1.72~3.51mg/kg).Very significant difference was found(P<0.o1).Interceptive of treatment with Lilopristone (oral) in combination with a PGs-analogue Sulprostone(i.m.) in mice was assessed.The qvalue was l.29(P>0.05).Lilopristone in combination with Sulprostone showed syneristiceffect.
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