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病毒从淋巴组织释放影响血液中1型人类免疫缺陷病毒和丙型肝炎病毒的动力学。

Release of virus from lymphoid tissue affects human immunodeficiency virus type 1 and hepatitis C virus kinetics in the blood.

作者信息

Müller V, Marée A F, De Boer R J

机构信息

Collegium Budapest, Institute for Advanced Study, 1014 Budapest, Hungary.

出版信息

J Virol. 2001 Mar;75(6):2597-603. doi: 10.1128/JVI.75.6.2597-2603.2001.

Abstract

Kinetic parameters of human immunodeficiency virus type 1 (HIV-1) and hepatitis C virus (HCV) infections have been estimated from plasma virus levels following perturbation of the chronically infected (quasi-) steady state. We extend previous models by also considering the large pool of virus localized in the lymphoid tissue (LT) compartment. The results indicate that the fastest time scale of HIV-1 plasma load decay during therapy probably reflects the clearance rate of LT virus and not, as previously supposed, the clearance rate of virus in plasma. This resolves the discrepancy between the clearance rate estimates during therapy and those based on plasma apheresis experiments. In the extended models plasma apheresis measurements are indeed expected to reflect the plasma decay rate. We can reconcile all current HIV-1 estimates with this model when, on average, the clearance rate of virus in plasma is approximately 20 day(-1), that of LT virus is approximately 3 day(-1), and the death rate of virus-producing cells is approximately 0.5 day(-1). The fast clearance in the LT compartment increases current estimates for total daily virus production. Because HCV is produced in the liver, we let virus be produced into the blood compartment of our model. The results suggest that extending current HCV models with an LT compartment is not likely to affect current estimates for kinetic parameters and virus production. Estimates for treatment efficacy might be affected, however.

摘要

人类免疫缺陷病毒1型(HIV-1)和丙型肝炎病毒(HCV)感染的动力学参数已根据慢性感染(准)稳态受到扰动后的血浆病毒水平进行了估算。我们通过同时考虑位于淋巴组织(LT)区室中的大量病毒库,对先前的模型进行了扩展。结果表明,治疗期间HIV-1血浆载量下降的最快时间尺度可能反映了LT病毒的清除率,而不是如先前所认为的血浆中病毒的清除率。这解决了治疗期间清除率估计值与基于血浆置换实验的估计值之间的差异。在扩展模型中,血浆置换测量确实有望反映血浆衰减率。当血浆中病毒的清除率平均约为20天⁻¹、LT病毒的清除率约为3天⁻¹、病毒产生细胞的死亡率约为0.5天⁻¹时,我们可以用该模型协调所有当前的HIV-1估计值。LT区室中的快速清除增加了当前对每日病毒总产生量的估计。由于HCV在肝脏中产生,我们让病毒在模型的血液区室中产生。结果表明,用LT区室扩展当前的HCV模型不太可能影响当前对动力学参数和病毒产生的估计。然而,治疗效果的估计可能会受到影响。

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