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Pharmacokinetics of ribavirin in patients with hepatitis C virus.

机译:丙型肝炎病毒患者病毒唑的药代动力学。

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AIM: A population pharmacokinetic analysis was performed using plasma concentration data (n = 7025) from 380 patients to examine the relationship between ribavirin dose and its pharmacokinetics. METHODS: Ribavirin pharmacokinetics were described by a three-compartment model with sequential zero-order and a first-order absorption processes. Interoccasion variability and food effects were included. RESULTS: Lean body weight (range 41-91 kg) was the only covariate with a clinically significant influence on ribavirin pharmacokinetics, affecting clearance (15.3-23.9 l h(-1)) and the volume of the larger peripheral compartment. CONCLUSION: The model provided a good description of the available data, confirmed by accurate estimates of parameter values and low residual variability (17%).
机译:目的:使用380名患者的血浆浓度数据(n = 7025)进行人群药代动力学分析,以检查利巴韦林剂量与其药代动力学之间的关系。方法:利巴韦林的药代动力学由三室模型描述,具有连续的零级和一级吸收过程。包括间际差异和食物影响。结果:瘦体重(41-91 kg)是唯一对利巴韦林药代动力学具有临床显着影响的协变量,影响清除率(15.3-23.9 l h(-1))和较大的外周室容积。结论:该模型提供了对可用数据的良好描述,并通过对参数值的准确估计和较低的残留变异性(17%)得到了证实。

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