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对具有潜在非正态和不完整纵向数据的抗逆转录病毒免疫疗法试验的分析。

Analysis of antiretroviral immunotherapy trials with potentially non-normal and incomplete longitudinal data.

作者信息

Mogg Robin, Mehrotra Devan V

机构信息

Merck Research Laboratories, UN-A102, 785 Jolly Road, Bldg. C, Blue Bell, PA 19422, USA.

出版信息

Stat Med. 2007 Feb 10;26(3):484-97. doi: 10.1002/sim.2555.

DOI:10.1002/sim.2555
PMID:16625520
Abstract

For many HIV-infected patients, use of antiretroviral therapy (ART) results in a sustained suppression of plasma viral load to undetectable levels. However, due to lack of antigenic stimulation, this may also result in a gradual loss of cell-mediated immune (CMI) responses that help control HIV infection. In concept, augmenting ART with periodic administrations of an HIV vaccine that boosts CMI responses could enhance control of viral replication. Researchers are designing 'antiretroviral immunotherapy' (ARI) trials to test this hypothesis. In a typical ARI trial, HIV-infected patients with sustained viral suppression will receive inoculations of an experimental HIV vaccine or a placebo, and subsequently stop taking their antiretroviral drugs. The goal is to assess whether plasma viral loads during the ART interruption phase are generally lower in the vaccine group. Assessment of a vaccine effect will be challenging if some subjects resume ART or drop out before the end of the treatment interruption phase. To tackle this 'missing' data problem and potential non-normality of the viral loads in ARI trials, we propose a two-step approach: multiple imputation of the missing values followed by use of the Wei-Lachin method with Wilcoxon scores. We use a numerical example and extensive simulations to illustrate the robustness and power advantages of our proposed method compared with other methods for incomplete longitudinal data, including REML, weighted GEE, last observation carried forward, and 'worst-rank' methods. Our proposed method is general enough for the robust analysis of longitudinal data in other therapeutic areas as well.

摘要

对于许多感染HIV的患者来说,使用抗逆转录病毒疗法(ART)可使血浆病毒载量持续抑制至检测不到的水平。然而,由于缺乏抗原刺激,这也可能导致有助于控制HIV感染的细胞介导免疫(CMI)反应逐渐丧失。从概念上讲,通过定期接种增强CMI反应的HIV疫苗来强化ART,可能会增强对病毒复制的控制。研究人员正在设计“抗逆转录病毒免疫疗法”(ARI)试验来验证这一假设。在典型的ARI试验中,病毒载量得到持续抑制的HIV感染患者将接种实验性HIV疫苗或安慰剂,随后停止服用抗逆转录病毒药物。目的是评估在ART中断阶段,疫苗组的血浆病毒载量总体上是否更低。如果一些受试者在治疗中断阶段结束前恢复ART或退出,那么评估疫苗效果将具有挑战性。为了解决ARI试验中这个“缺失”数据问题以及病毒载量可能的非正态性,我们提出一种两步法:对缺失值进行多次插补,然后使用带有Wilcoxon分数的Wei-Lachin方法。我们通过一个数值示例和广泛的模拟来说明,与其他处理不完全纵向数据的方法(包括限制最大似然法、加权广义估计方程、末次观察值结转法和“最差秩”法)相比,我们提出的方法具有稳健性和功效优势。我们提出的方法通用性足够强,也可用于其他治疗领域纵向数据的稳健分析。

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