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HIV-1感染中结构化抗逆转录病毒药物治疗中断的风险与益处。

Risks and benefits of structured antiretroviral drug therapy interruptions in HIV-1 infection.

作者信息

Bonhoeffer S, Rembiszewski M, Ortiz G M, Nixon D F

机构信息

Friedrich Miescher Institut, Basel, Switzerland.

出版信息

AIDS. 2000 Oct 20;14(15):2313-22. doi: 10.1097/00002030-200010200-00012.

Abstract

BACKGROUND

Structured interruptions of antiretroviral therapy of HIV-1 infected individuals are currently being tested in clinical trials to study the effect interruptions have on the immune responses and control of virus replication.

OBJECTIVE

To investigate the potential risks and benefits of interrupted therapy using standard population dynamical models of HIV replication kinetics.

METHODS

Standard population dynamical models were used to study the effect of structured therapy interruptions on the immune effector cells, the latent cell compartment and the emergence of drug resistance.

CONCLUSIONS

The models suggest that structured therapy interruption only leads to transient or sustained virus control if the immune effector cells increase during therapy. This increase must more than counterbalance the increase in susceptible target cells induced by therapy. The risk of inducing drug resistance by therapy interruptions or the risk of repopulating the pool of latent cells during drug-free periods may be small if the virus population remains at levels considerably below baseline. However, if the virus load increases during drug-free periods to levels similar to or higher than baseline before therapy, both these risks increase dramatically.

摘要

背景

目前正在临床试验中测试对感染HIV-1个体的抗逆转录病毒疗法进行结构化中断,以研究中断对免疫反应和病毒复制控制的影响。

目的

使用HIV复制动力学的标准群体动力学模型研究中断疗法的潜在风险和益处。

方法

使用标准群体动力学模型研究结构化疗法中断对免疫效应细胞、潜伏细胞区室和耐药性出现的影响。

结论

模型表明,只有在治疗期间免疫效应细胞增加时,结构化疗法中断才会导致短暂或持续的病毒控制。这种增加必须超过治疗诱导的易感靶细胞增加的幅度。如果病毒群体保持在远低于基线的水平,中断治疗诱导耐药性的风险或在无药期重新填充潜伏细胞库的风险可能很小。然而,如果在无药期病毒载量增加到与治疗前基线相似或更高的水平,这两种风险都会急剧增加。

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