检索规则说明:AND代表“并且”;OR代表“或者”;NOT代表“不包含”;(注意必须大写,运算符两边需空一格)
检 索 范 例 :范例一: (K=图书馆学 OR K=情报学) AND A=范并思 范例二:J=计算机应用与软件 AND (U=C++ OR U=Basic) NOT M=Visual
名 称:
注 释:
作 者:张小兰[1] 王志强 孙建国[1] 彭英[1] 仲云熙[1] 郝琨[1] 张仓 王广基[1]
机构地区:[1]中国药科大学江苏省药物代谢动力学重点实验室 [2]南京圣和药业有限公司
出 处:《中国临床药理学与治疗学》2013年第11期1205-1210,共6页Chinese Journal of Clinical Pharmacology and Therapeutics
基 金:创新平台提升项目(BM2012012);"十二五"重大新药创制资助项目(2011ZX09401-003)
摘 要:目的:采用LC-MS/MS技术比较研究Combretastatin(CA4)及其磷酸酯二钠(CA4P)前药分别给药于SD大鼠后的药代动力学差异。方法:12只SD大鼠禁食后分别单次尾静脉给予50mg/kg CA4P或36mg/kg CA4(等摩尔量),采集不同时间点血样,采用LC-MS/MS方法进行血样药物浓度测定,求算相应的药代动力学参数,并建立CA4P-CA4转化的药动学模型。结果:大鼠单剂量i.v.50mg/kg CA4P或36mg/kg CA4后,CA4P和CA4血浆药物浓度-时间曲线下面积AUC0-∞分别为(27126±4142)、(7751±801)、(5037±1433)ng·h·mL-1,消除半衰期t1/2分别为(0.85±0.35)、(1.27±0.33)和(0.95±0.65)h。CA4P和CA4在SD大鼠体内药动学行为均无性别差异。结论:大鼠单剂量i.v.50mg/kg CA4P后,CA4P在体内迅速转化为CA4,相比于直接i.v.36mg/kg CA4,CA4在体内的暴露量(AUC0-∞)显著性提高(P<0.05),消除半衰期t1/2也有所增加,为前药CA4P的药代动力学优势。AIM. An LCMS/MS method was set up for the comparative evaluation of pharma cokinetics of CA4P and CA4 in SD rats. METH ODS: 12 fasted SD rats were single intravenous administration of 50 mg/kg CA4P or 36 mg/kg CA4 (same molar amount). Plasma samples were collected at different time points and con centrations of CA4P and CA4 were analyzed by LCMS/MS. The pharmacokinetic parameters were calculated and CA4PCA4 transformation were simulated by pharmacokinetie model. RE SULTS: After i. v. administration of 50 mg/kg CA4P or 36 mg/kg CA4, the AUCof CA4P orCA4 were (27126±4142), (7751±801) and(5037±1433) ng. h. mL-1, respectively, the tw2 were (0.85 ±0.35 ), ( 1.27 ±0.33 ) and (0.95±0.65) h, respectively. No gender differ ences were found in rats. CONCLUSION: The exposure of CA4 was increased significantly by soluble CA4 phosphate in SD rats. CA4P was rapidly transformed into CA4 after a single i. v. administration of CA4P in rats, according to the pharmacokinetic model of CA4PCA4 transfor mation set up by us.
正在载入数据...
正在载入数据...
正在载入数据...
正在载入数据...
正在载入数据...
正在载入数据...
正在载入数据...
正在链接到云南高校图书馆文献保障联盟下载...
云南高校图书馆联盟文献共享服务平台 版权所有©
您的IP:216.73.216.49