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首页> 外文期刊>Bone marrow transplantation >Evaluation of existing limited sampling models for busulfan kinetics in children with beta thalassaemia major undergoing bone marrow transplantation.
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Evaluation of existing limited sampling models for busulfan kinetics in children with beta thalassaemia major undergoing bone marrow transplantation.

机译:评价现有的有限样本量模型对正在接受骨髓移植的重型β地中海贫血儿童的丁硫磺动力学。

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摘要

Busulfan pharmacokinetic parameters are useful in predicting the outcome of allogeneic bone marrow transplantation (BMT). Standard pharmacokinetic measurements require multiple blood samples. Various limited sampling models (LSM) have been proposed for reducing the sample number required for these measurements, essentially for patients with malignant disorders undergoing BMT. This study was undertaken to evaluate the existing LSM for busulfan pharmacokinetics to find out the most suitable method for patients with thalassaemia major undergoing BMT. Busulfan levels in plasma samples were analysed by HPLC. The AUC calculated by non-compartmental analysis using the program 'TOPFIT' was compared with previously published LSMs. Our seven sample pharmacokinetic data for AUC calculation was compared with the published LSMs. The three sample models suggested by Chattergoon et al and Schuler et al showed significant agreement with AUC TOPFIT (R(2) = 0.98 and 0.94, respectively) in our clinical context. Other models resulted in significant over or under representation of observed values (Vassal's model R(2) = 0.61; Chattergoon's two sample model R(2) = 0.84; four sample model R(2) = 0.83; Schuler's two sample model R(2) = 0.79). By these data the three sample LSM proposed by Chattergoon et al and Schuler et al are suitable for calculation of the AUC in patients with thalassaemia major undergoing BMT conditioned with oral busulfan.
机译:白消安的药代动力学参数可用于预测同种异体骨髓移植(BMT)的结果。标准药代动力学测量需要多个血液样本。已经提出了各种有限采样模型(LSM)来减少这些测量所需的样本数量,主要是针对患有BMT的恶性疾病患者。这项研究是为了评估现有的LSM对白消安的药代动力学,以找出最适合接受BMT治疗的重型地中海贫血患者的方法。通过HPLC分析血浆样品中的白消安水平。将使用“ TOPFIT”程序通过非隔室分析计算出的AUC与先前发布的LSM进行了比较。将我们用于AUC计算的七个样本药代动力学数据与已发布的LSM进行了比较。在我们的临床环境中,Chattergoon等人和Schuler等人建议的三个样本模型显示出与AUC TOPFIT的显着一致性(分别为R(2)= 0.98和0.94)。其他模型导致观测值的显着过量或不足表示(Vassal模型R(2)= 0.61; Chattergoon的两个样本模型R(2)= 0.84;四个样本模型R(2)= 0.83; Schuler的两个样本模型R(2 )= 0.79)。通过这些数据,Chattergoon等人和Schuler等人提出的三个样本LSM适用于患有严重地中海贫血的接受口服白硫丹治疗的BMT的患者的AUC的计算。

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