ETH Zürich, Institute of Integrative Biology, Zürich, Switzerland.
PLoS Pathog. 2011 Nov;7(11):e1002321. doi: 10.1371/journal.ppat.1002321. Epub 2011 Nov 3.
HIV-1 replicative capacity (RC) provides a measure of within-host fitness and is determined in the context of phenotypic drug resistance testing. However it is unclear how these in-vitro measurements relate to in-vivo processes. Here we assess RCs in a clinical setting by combining a previously published machine-learning tool, which predicts RC values from partial pol sequences with genotypic and clinical data from the Swiss HIV Cohort Study. The machine-learning tool is based on a training set consisting of 65000 RC measurements paired with their corresponding partial pol sequences. We find that predicted RC values (pRCs) correlate significantly with the virus load measured in 2073 infected but drug naïve individuals. Furthermore, we find that, for 53 pairs of sequences, each pair sampled in the same infected individual, the pRC was significantly higher for the sequence sampled later in the infection and that the increase in pRC was also significantly correlated with the increase in plasma viral load and with the length of the time-interval between the sampling points. These findings indicate that selection within a patient favors the evolution of higher replicative capacities and that these in-vitro fitness measures are indicative of in-vivo HIV virus load.
HIV-1 复制能力(RC)提供了一种衡量宿主内适应性的方法,是在表型药物耐药性测试的背景下确定的。然而,目前尚不清楚这些体外测量结果与体内过程之间的关系。在这里,我们通过结合先前发表的机器学习工具,在临床环境中评估 RC,该工具可根据来自瑞士艾滋病毒队列研究的基因型和临床数据以及部分 pol 序列预测 RC 值。该机器学习工具基于一个训练集,其中包含 65000 个 RC 测量值以及与其对应的部分 pol 序列。我们发现,预测的 RC 值(pRC)与 2073 名感染但未接受药物治疗的个体中测量的病毒载量显著相关。此外,我们发现,对于 53 对序列,每对序列均在同一感染个体中采样,在感染后期采样的序列的 pRC 明显更高,并且 pRC 的增加与血浆病毒载量的增加以及采样点之间的时间间隔长度呈显著相关。这些发现表明,患者体内的选择有利于更高复制能力的进化,并且这些体外适应性测量结果可指示体内 HIV 病毒载量。
