首页> 外文期刊>The Journal of Clinical Pharmacology: Official Journal of the American College of Clinical Pharmacology >Limited sampling strategies for the estimation of sirolimus daily exposure in kidney transplant recipients on a calcineurin inhibitor-free regimen.
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Limited sampling strategies for the estimation of sirolimus daily exposure in kidney transplant recipients on a calcineurin inhibitor-free regimen.

机译:在无钙调神经磷酸酶抑制剂的方案下,估计肾移植接受者西罗莫司每日暴露量的有限采样策略。

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摘要

Sirolimus (SRL) is a novel immunosuppressive agent characterized by a narrow therapeutic index. Monitoring of SRL concentrations is mandatory to optimize drug dosing. The area under the concentration-time curve (AUC) is generally accepted as the best pharmacokinetic marker of daily drug exposure. Assessment of full SRL AUC, however, requires the collection of multiple blood samples, imposing both time and cost constraints. Limited sampling strategies (LSS) may be of clinical relevance to improve the therapeutic drug monitoring of SRL. In this study, stepwise multiple regression analysis is conducted on 30 SRL pharmacokinetic profiles obtained from kidney transplant recipients on a cyclosporine-free regimen, and different LSS equations are identified based on 2 or 3 sampling points collected within the first 6 hours after drug intake. The performance of these equations is tested in a separate validation set (n=30). Most of the proposed algorithms are associated with good correlations with the measured AUC and acceptable bias and imprecision. Two equations--based on 2 time points collected within the first 4 hours after dosing--are identified that reliably predict SRL exposure in routine clinical practice compared with the traditional C0-based approach. These tools provide additional information to optimize SRL therapeutic drug monitoring in renal transplant recipients.
机译:西罗莫司(SRL)是一种新型的免疫抑制剂,具有较窄的治疗指数。必须监测SRL浓度以优化药物剂量。浓度-时间曲线(AUC)下的面积通常被认为是每日药物暴露的最佳药代动力学指标。但是,对完整SRL AUC的评估需要采集多个血液样本,这对时间和成本都造成了限制。有限采样策略(LSS)可能对改善SRL的治疗药物监测具有临床意义。在这项研究中,采用无环孢素方案对从肾移植接受者获得的30种SRL药代动力学概况进行了逐步多元回归分析,并基于服药后头6小时内收集的2个或3个采样点,确定了不同的LSS方程。这些方程的性能在单独的验证集中进行测试(n = 30)。大多数提出的算法都与测得的AUC以及相关的偏差和不精确度具有良好的相关性。与传统的基于C0的方法相比,确定了两个方程式-基于给药后头4个小时内收集的2个时间点-可以可靠地预测常规临床实践中的SRL暴露。这些工具提供了其他信息,可以优化肾移植接受者中的SRL治疗药物监测。

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