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Mark-specific hazard ratio model with missing multivariate marks

机译:缺少多元标记的特定于标记的危险比模型

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An objective of randomized placebo-controlled preventive HIV vaccine efficacy (VE) trials is to assess the relationship between vaccine effects to prevent HIV acquisition and continuous genetic distances of the exposing HIVs to multiple HIV strains represented in the vaccine. The set of genetic distances, only observed in failures, is collectively termed the 'mark.' The objective has motivated a recent study of a multivariate mark-specific hazard ratio model in the competing risks failure time analysis framework. Marks of interest, however, are commonly subject to substantial missingness, largely due to rapid post-acquisition viral evolution. In this article, we investigate the mark-specific hazard ratio model with missing multivariate marks and develop two inferential procedures based on (i) inverse probability weighting (IPW) of the complete cases, and (ii) augmentation of the IPW estimating functions by leveraging auxiliary data predictive of the mark. Asymptotic properties and finite-sample performance of the inferential procedures are presented. This research also provides general inferential methods for semiparametric density ratio/biased sampling models with missing data. We apply the developed procedures to data from the HVTN 502 'Step' HIV VE trial.
机译:随机安慰剂对照的预防性HIV疫苗效力(VE)试验的目标是评估预防HIV的疫苗效果与暴露的HIV与疫苗中代表的多种HIV株之间连续的遗传距离之间的关系。仅在失败中观察到的一组遗传距离统称为“标记”。该目标推动了对竞争风险失效时间分析框架中的多元标记特定风险比模型的最新研究。然而,感兴趣的标记通常容易遭受实质性缺失,这在很大程度上是由于采集后病毒的快速进化。在本文中,我们研究了缺少多变量标记的特定于标记的危险比模型,并基于(i)完整案例的逆概率加权(IPW),以及(ii)利用杠杆作用来增强IPW估计功能,开发了两种推理程序预测商标的辅助数据。给出了推理过程的渐近性质和有限样本性能。这项研究还为缺少数据的半参数密度比/有偏抽样模型提供了一般的推论方法。我们将开发的程序应用于HVTN 502“阶梯式” HIV VE试验的数据。

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