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首页> 外文期刊>Journal of viral hepatitis. >Modelling hepatitis C virus kinetics during treatment with pegylated interferon alpha-2b: errors in the estimation of viral kinetic parameters.
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Modelling hepatitis C virus kinetics during treatment with pegylated interferon alpha-2b: errors in the estimation of viral kinetic parameters.

机译:在聚乙二醇化干扰素α-2b治疗期间模拟丙型肝炎病毒动力学:病毒动力学参数估计中的错误。

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摘要

Neumann et al. [1] developed a widely used model for the analysis of hepatitis C virus (HCV) dynamics after the initiation of interferon therapy that assumes the effectiveness of therapy in blocking virion production, epsilon, is constant. However, with pegylated interferon alpha-2b (PEG-IFN) given weekly, there are significant changes in drug concentration between doses, leading to changes in drug effectiveness and viral rebounds. To investigate the appropriateness of the constant effectiveness (CE) model [1] for studies involving PEG-IFN, we simulated PEG-IFN treatment, using 294 sets of pharmacokinetic/pharmacodynamic (PK/PD) parameters that span observed ranges and fit the simulated data to the CE model. For most combinations of PK/PD parameters, the fits resulted in an infected cell loss rate, delta, that underestimates the true value used in the simulations and yielded over-estimates of the average effectiveness of PEG-IFN. In the setting of PEG-IFN therapy, the use of the CE model of HCV kinetics has to be reevaluated and the validity of its use depends on the amount of HCV RNA rebound observed between doses.
机译:Neumann等。 [1]建立了一种广泛使用的模型,用于分析干扰素治疗开始后的丙型肝炎病毒(HCV)动力学分析,该模型假定该疗法在阻止病毒粒子产生中的有效性是恒定的。但是,每周使用聚乙二醇化干扰素α-2b(PEG-IFN),两次给药之间的药物浓度会发生显着变化,从而导致药物效力和病毒反弹的变化。为了研究恒定有效性(CE)模型[1]在涉及PEG-IFN研究中的适用性,我们使用跨越观察范围并符合模拟条件的294组药代动力学/药效学(PK / PD)参数模拟了PEG-IFN治疗数据输入到CE模型。对于PK / PD参数的大多数组合,拟合结果导致感染的细胞丢失率delta低估了模拟中使用的真实值,并高估了PEG-IFN的平均有效性。在PEG-IFN治疗的背景下,必须重新评估HCV动力学的CE模型的使用,其有效性取决于剂量之间观察到的HCV RNA反弹的量。

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