Wiczling Paweł, Liem Robert I, Panepinto Julie A, Garg Uttam, Abdel-Rahman Susan M, Kearns Gregory L, Neville Kathleen A
Department of Biopharmaceutics and Pharmacokinetics, Medical University of Gdansk, Gdansk, Poland.
J Clin Pharmacol. 2014 Sep;54(9):1016-22. doi: 10.1002/jcph.303. Epub 2014 Apr 11.
The objective of this study was to develop a population pharmacokinetic (PK) model sufficient to describe hydroxyurea (HU) concentrations in serum and urine following oral drug administration in pediatric patients with sickle cell disease. Additionally, the measured hydroxyurea concentrations for particular sampling time were correlated with exposure measures (AUC) to find the most predictive relationship. Hydroxyurea concentrations were determined in 21 subjects. Using a population nonlinear mixed-effect modeling, the HU PK was best described by a one-compartment model with two elimination pathways (metabolic and renal) and a transit compartment absorption. The typical mean absorption time was 0.222 hour. The typical apparent volume of distribution was 21.8 L and the apparent systemic clearance was 6.88 L/h for an average weight patient of 30.7 kg. The 50% of the HU dose was renally excreted. Linear correlations were apparent between the plasma HU concentration at 1, 1.5, 2, 4, and 6 hours post-dose and AUC with the most significant (R(2) = 0.71) observed at 1.5 hours. A population PK model was successful in describing HU disposition in plasma and urine. Data from the model also demonstrated that HU plasma concentrations at 1.5 hours after an oral dose of the drug were highly predictive of systemic drug exposure.
本研究的目的是建立一个群体药代动力学(PK)模型,该模型足以描述镰状细胞病儿科患者口服药物后血清和尿液中的羟基脲(HU)浓度。此外,将特定采样时间测得的羟基脲浓度与暴露量度(AUC)进行关联,以找出最具预测性的关系。测定了21名受试者的羟基脲浓度。使用群体非线性混合效应模型,HU的PK最好用具有两种消除途径(代谢和肾脏)和一个转运室吸收的单室模型来描述。典型的平均吸收时间为0.222小时。对于平均体重为30.7 kg的患者,典型的表观分布容积为21.8 L,表观全身清除率为6.88 L/h。50%的HU剂量经肾脏排泄。给药后1、1.5、2、4和6小时的血浆HU浓度与AUC之间存在明显的线性相关性,其中在1.5小时观察到的相关性最为显著(R(2) = 0.71)。一个群体PK模型成功地描述了HU在血浆和尿液中的处置情况。该模型的数据还表明,口服该药物后1.5小时的HU血浆浓度对全身药物暴露具有高度预测性。
