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使用机理模型对临床进展和生物标志物动态进行联合建模。

Joint modeling of the clinical progression and of the biomarkers' dynamics using a mechanistic model.

作者信息

Guedj Jeremie, Thiébaut Rodolphe, Commenges Daniel

机构信息

Laboratory of Viral Dynamics, Faculty of Life Sciences, Bar-Ilan University, Ramat-Gan 52900, Israel.

出版信息

Biometrics. 2011 Mar;67(1):59-66. doi: 10.1111/j.1541-0420.2010.01418.x.

Abstract

Joint models are used to rigorously explore the relationship between the dynamics of biomarkers and clinical events. In the context of HIV infection, where the multivariate dynamics of HIV-RNA and CD4 are complex, a mechanistic approach based on a system of nonlinear differential equations naturally takes into account the correlation between the biomarkers. Using data from a randomized clinical trial comparing dual antiretroviral therapy to a single drug regimen, a full maximum likelihood approach is proposed to explore the relationship between the evolution of the biomarkers and the time to a clinical event. The role of each marker as an independent predictor of disease progression is assessed. We show that the joint dynamics of HIV-RNA and CD4 captures the effect of antiretroviral treatment; the CD4 dynamics alone is found to capture most but not all of the treatment effect.

摘要

联合模型用于严格探究生物标志物动态与临床事件之间的关系。在HIV感染的背景下,HIV-RNA和CD4的多变量动态较为复杂,基于非线性微分方程系统的机制方法自然会考虑生物标志物之间的相关性。利用一项比较双联抗逆转录病毒疗法与单一药物疗法的随机临床试验数据,提出了一种完全最大似然方法来探究生物标志物的演变与临床事件发生时间之间的关系。评估了每个标志物作为疾病进展独立预测指标的作用。我们表明,HIV-RNA和CD4的联合动态反映了抗逆转录病毒治疗的效果;仅CD4动态就可反映大部分但并非全部的治疗效果。

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