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解释抗逆转录病毒治疗依从性与HIV突变积累之间关系的变异性。

Explaining variability in the relationship between antiretroviral adherence and HIV mutation accumulation.

作者信息

Braithwaite R S, Shechter S, Roberts M S, Schaefer A, Bangsberg D R, Harrigan P R, Justice A C

机构信息

Section of General Internal Medicine, Yale University School of Medicine and VA Connecticut Healthcare System, New Haven, CT, USA.

出版信息

J Antimicrob Chemother. 2006 Nov;58(5):1036-43. doi: 10.1093/jac/dkl386. Epub 2006 Oct 5.

Abstract

OBJECTIVES

Determining the relationship between antiretroviral adherence and resistance accumulation is important for the design and evaluation of adherence interventions. Our objective was to explain heterogeneity observed in this relationship.

METHODS

We first conducted a systematic review to locate published reports describing the relationship between adherence and resistance. We then used a validated computer simulation to simulate the patient populations in these reports, exploring the impact of changes in individual patient characteristics (age, CD4, viral load, prior antiretroviral experience) on the shape of the adherence-resistance (A-R) curve.

RESULTS

The search identified 493 titles, of which 3 contained relevant primary data and 2 had sufficient follow-up for inclusion (HOMER and REACH cohorts). When simulating HOMER, the A-R curve had a high peak with a greatly increased hazard ratio (HR) of accumulating mutations at partial compared to complete adherence (simulation, HR 2.9; HOMER, HR 2.7). When simulating REACH, the A-R curve had a shallow peak with a slightly increased hazard of accumulating mutations at partial adherence (simulation, HR 1.2; REACH, HR 1.4). This heterogeneity was primarily attributable to differences in antiretroviral experience between the cohorts.

CONCLUSIONS

Our computer simulation was able to explain much of the heterogeneity in observed A-R curves.

摘要

目的

确定抗逆转录病毒治疗依从性与耐药性积累之间的关系对于依从性干预措施的设计和评估至关重要。我们的目的是解释在这种关系中观察到的异质性。

方法

我们首先进行了一项系统综述,以查找描述依从性与耐药性之间关系的已发表报告。然后,我们使用经过验证的计算机模拟来模拟这些报告中的患者群体,探讨个体患者特征(年龄、CD4、病毒载量、既往抗逆转录病毒治疗经历)的变化对依从性-耐药性(A-R)曲线形状的影响。

结果

检索到493篇文献标题,其中3篇包含相关原始数据,2篇有足够的随访数据可供纳入(HOMER和REACH队列)。模拟HOMER队列时,A-R曲线有一个高峰值,与完全依从相比,部分依从时积累突变的风险比(HR)大幅增加(模拟,HR 2.9;HOMER,HR 2.7)。模拟REACH队列时,A-R曲线有一个浅峰值,部分依从时积累突变的风险略有增加(模拟,HR 1.2;REACH,HR 1.4)。这种异质性主要归因于各队列之间抗逆转录病毒治疗经历的差异。

结论

我们的计算机模拟能够解释观察到的A-R曲线中大部分的异质性。

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