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Pharmacokinetics of treosulfan and its active monoepoxide in pediatric patients after intravenous infusion of high-dose treosulfan prior to HSCT

机译:在HSCT之前静脉输注高剂量雷科甘蔗静脉输注后小儿患者葡萄干的药代动力学及其活性单氧化物

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Pro-drug treosulfan (TREO) is currently evaluated in randomized phase III clinical trials as a conditioning agent prior to HSCT. In the present paper pharmacokinetics of both TREO and its biologically active monoepoxide (S,S-EBDM) was investigated in pediatric patients for the first time. The studies were carried out in 16 children (median age 7.5 years) undergoing TREO-based preparative regimen prior to HSCT, who received 10, 12 or 14 g/m(2) of the drug as a 1 h or 2 h intravenous infusion. Plasma concentrations of TREO as well as S,S-EBDM were determined using the validated HPLC-MS/MS method. The changes in S,S-EBDM concentration over time followed TREO levels. The area under the curve (AUC) of TREO was 100-fold higher than AUC of S,S-EBDM. No statistically significant dependency of the dose-normalized AUC of either TREO or S,S-EBDM on the patients' age and body surface area was stated. Moreover, plasma Cm a as well as AUC of S,S-EBDM demonstrated linear correlation with the C-max and AUC of TREO, respectively. The biological half-lives of TREO and S,S-EBDM were similar. This indicates that S,S-EBDM was completely eliminated from the patients' blood within relatively short time, comparable to TREO. (C) 2014 Elsevier B.V. All rights reserved.
机译:目前在随机化期III临床试验中评估PRE-药物三胞素(TREO)作为HSCT之前的调理剂。在本文的本文中,首次在儿科患者中研究了Treo及其生物活性单氧化锑的药代动力学。在HSCT之前,在HSCT之前的16名儿童(中位数7.5岁)中进行了研究,将Treo基础制备植物中的Treo-Creative植物中进行10,12或14g / m(2)作为1小时或2小时静脉输注。使用验证的HPLC-MS / MS法测定Treo的血浆浓度以及S,S-EBDM。随着时间的推移,S,S-EBDM浓度的变化跟踪Treo水平。 Treo曲线(AUC)下的区域比S,S-EBDM的AUC高100倍。没有说明Treo或S,S-EBDM的剂量标准化AUC对患者年龄和体表面积的统计学显着的依赖性。此外,S等离子体CM A以及S,S-EBDM的AUC分别与Treo的C-Max和Auc分别表现出线性相关性。 Treo和S,S-EBDM的生物半衰期相似。这表明S,S-EBDM完全从患者的血液中被完全消除,而与Treo相当。 (c)2014 Elsevier B.v.保留所有权利。

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