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Daily Sampling of an HIV-1 Patient with Slowly Progressing Disease Displays Persistence of Multiple env Subpopulations Consistent with Neutrality

机译:疾病进展缓慢的HIV-1患者的每日采样显示与中性一致的多个env亚群的持久性

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摘要

The molecular evolution of HIV-1 is characterized by frequent substitutions, indels and recombination events. In addition, a HIV-1 population may adapt through frequency changes of its variants. To reveal such population dynamics we analyzed HIV-1 subpopulation frequencies in an untreated patient with stable, low plasma HIV-1 RNA levels and close to normal CD4+ T-cell levels. The patient was intensively sampled during a 32-day period as well as approximately 1.5 years before and after this period (days −664, 1, 2, 3, 11, 18, 25, 32 and 522). 77 sequences of HIV-1 env (approximately 3100 nucleotides) were obtained from plasma by limiting dilution with 7–11 sequences per time point, except day −664. Phylogenetic analysis using maximum likelihood methods showed that the sequences clustered in six distinct subpopulations. We devised a method that took into account the relatively coarse sampling of the population. Data from days 1 through 32 were consistent with constant within-patient subpopulation frequencies. However, over longer time periods, i.e. between days 1…32 and 522, there were significant changes in subpopulation frequencies, which were consistent with evolutionarily neutral fluctuations. We found no clear signal of natural selection within the subpopulations over the study period, but positive selection was evident on the long branches that connected the subpopulations, which corresponds to >3 years as the subpopulations already were established when we started the study. Thus, selective forces may have been involved when the subpopulations were established. Genetic drift within subpopulations caused by de novo substitutions could be resolved after approximately one month. Overall, we conclude that subpopulation frequencies within this patient changed significantly over a time period of 1.5 years, but that this does not imply directional or balancing selection. We show that the short-term evolution we study here is likely representative for many patients of slow and normal disease progression.
机译:HIV-1的分子进化以频繁的取代,插入缺失和重组事件为特征。此外,HIV-1人群可能会通过其变体的频率变化来适应。为了揭示此类人群动态,我们分析了未经治疗的血浆HIV-1 RNA水平稳定,CD4 + T细胞水平接近正常且未经治疗的患者的HIV-1亚群频率。在32天期间以及此期间前后约1.5年(第-664、1、2、3、11、18、25、32和522天)对患者进行了密集采样。通过在每个时间点(第-664天除外)用7-11个序列进行有限稀释来从血浆中获得77个HIV-1 env序列(约3100个核苷酸)。使用最大似然法的系统发育分析表明,该序列聚簇在六个不同的亚群中。我们设计了一种方法,该方法考虑了人口的相对粗略抽样。第1天到第32天的数据与恒定的患者亚人群频率一致。但是,在较长的时间段内,即在1到32天到522天之间,亚种群的频率发生了显着变化,这与进化中性波动一致。在研究期间,我们没有发现亚群内自然选择的明确信号,但是在连接亚群的长分支上有明显的正选择,这对应于> 3年,因为当我们开始研究时已经建立了亚群。因此,当建立亚群时可能涉及选择性力。从头取代引起的亚群内的遗传漂移可以在大约一个月后解决。总体而言,我们得出的结论是,该患者的亚人群频率在1.5年的时间内发生了显着变化,但这并不意味着方向性或平衡选择。我们表明,我们在这里研究的短期演变可能代表许多疾病进展缓慢和正常的患者。

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