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评估单纯疱疹病毒抑制疗法对血浆 HIV-1 病毒载量影响的公共卫生效果。

Estimating the public health impact of the effect of herpes simplex virus suppressive therapy on plasma HIV-1 viral load.

机构信息

MRC Centre for Outbreak Analysis and Modelling, Department of Infectious Disease Epidemiology, Imperial College London, St Mary's Campus, Norfolk Place, London W2 1PG, UK.

出版信息

AIDS. 2009 May 15;23(8):1005-13. doi: 10.1097/QAD.0b013e32832aadf2.

Abstract

OBJECTIVE

Trials of herpes simplex virus (HSV) suppressive therapy among HSV-2/HIV-1-infected individuals have reported an impact on plasma HIV-1 viral loads (PVLs). Our aim was to estimate the population-level impact of suppressive therapy on female-to-male HIV-1 sexual transmission.

DESIGN AND METHODS

By comparing prerandomization and postrandomization individual-level PVL data from the first two HSV suppressive therapy randomized controlled trials in sub-Saharan Africa, we estimated the effect of treatment on duration of asymptomatic infection and number of HIV-1 transmission events for each trial.

RESULTS

Assuming that a reduction in PVL is accompanied by an increased duration of HIV-1 asymptomatic infection, 4-6 years of HSV suppressive therapy produce a 1-year increase in the duration of this stage. To avert one HIV-1 transmission requires 8.8 [95% confidence interval (CI), 5.9-14.9] and 11.4 (95% CI, 7.8-27.5) women to be treated from halfway through their HIV-1 asymptomatic period, using results from Burkina Faso and South African trials, respectively. Regardless of the timing of treatment initiation, 51.6 (95% CI, 30.4-137.0) and 66.5 (95% CI, 36.7-222.6) treatment-years are required to avert one HIV-1 infection. Distributions of set-point PVL values from sub-Saharan African populations suggest that unintended adverse consequences of therapy at the population level (i.e. increased HIV-1 transmission due to increased duration of infection) are unlikely to occur in these settings.

CONCLUSION

HSV suppressive therapy may avert relatively few HIV-1 transmission events per person-year of treatment. Its use as a prevention intervention may be limited; however, further research into its effect on rate of CD4 cell count decline and the impact of higher dosing schedules is warranted.

摘要

目的

针对单纯疱疹病毒(HSV)抑制疗法在单纯疱疹病毒 2 型(HSV-2)/人类免疫缺陷病毒 1 型(HIV-1)感染者中的试验报告称,该疗法对血浆 HIV-1 病毒载量(PVL)有影响。我们的目的是评估抑制疗法对女性向男性 HIV-1 性传播的人群层面影响。

设计和方法

通过比较撒哈拉以南非洲前两个 HSV 抑制性治疗随机对照试验中个体在随机分组前和随机分组后的个体 PVL 数据,我们估计了治疗对每个试验中无症状感染持续时间和 HIV-1 传播事件数量的影响。

结果

假设 PVL 降低伴随着 HIV-1 无症状感染持续时间的延长,4-6 年的 HSV 抑制性治疗会使这一阶段的持续时间延长 1 年。为了避免 1 次 HIV-1 传播,需要在 HIV-1 无症状期的中途开始治疗,每位女性需要治疗 8.8(95%置信区间[CI],5.9-14.9)和 11.4(95%CI,7.8-27.5)年,这分别是来自布基纳法索和南非试验的结果。无论治疗开始的时间如何,为避免 1 例 HIV-1 感染,需要 51.6(95%CI,30.4-137.0)和 66.5(95%CI,36.7-222.6)治疗年。来自撒哈拉以南非洲人群的 PVL 设定点值分布表明,治疗对人群层面产生的意想不到的不良后果(即由于感染持续时间延长而导致 HIV-1 传播增加)不太可能在这些环境中发生。

结论

HSV 抑制性治疗可能会使每人每年的治疗中避免相对较少的 HIV-1 传播事件。它作为一种预防干预措施的使用可能受到限制;然而,进一步研究其对 CD4 细胞计数下降速度的影响以及更高剂量方案的影响是有必要的。

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