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抗逆转录病毒治疗前参与者体内较低的HIV-1 pol基因多样性可能与成人病毒学失败无关。

Lower pre-ART intra-participant HIV-1 pol diversity may not be associated with virologic failure in adults.

作者信息

Kearney Mary F, Spindler Jonathan, Wiegand Ann, Shao Wei, Haubrich Richard, Riddler Sharon, Lalama Christina M, Hughes Michael D, Coffin John M, Mellors John W

机构信息

HIV Dynamics and Replication Program, National Cancer Institute, Frederick, MD, United States of America.

Advanced Biomedical Computing Center, Leidos Biomedical Research, Inc., Frederick National Laboratory for Cancer Research, Frederick, MD, United States of America.

出版信息

PLoS One. 2018 Jan 25;13(1):e0190438. doi: 10.1371/journal.pone.0190438. eCollection 2018.

Abstract

BACKGROUND

Identifying pre-ART factors associated with the emergence of HIV-1 drug resistance is critical for optimizing strategies to prevent virologic failure. A previous study reported that lower pre-ART HIV-1 pol diversity was associated with higher risk of virologic failure in HIV-1-infected children. To investigate this association in adults, we measured HIV-1 diversity with deep sequencing in pre-ART samples from adults with well-characterized virologic outcomes in a study (A5142) of initial ART conducted by the AIDS Clinical Trials Group (ACTG).

METHODS

We identified 22 cases in ACTG A5142 who experienced virologic failure with drug resistance mutations in RT and 44 matched controls who did not experience virologic failure. cDNA was synthesized from plasma HIV-1 RNA. Each cDNA molecule was tagged with a unique primer ID and RT codons 41-103 were amplified and deep sequenced. Sequences with the same tag were aligned and a consensus was generated to reduce PCR and sequencing errors. Diversity was calculated by measuring average pairwise distance (APD) of the consensus sequences. An exact conditional logistic regression model with percent APD as the risk factor estimated the odds ratio for VF and the corresponding 95% confidence interval.

RESULTS

Consensus single-genome sequences and diversity estimates of pol were obtained for pre-ART samples from 21 cases and 42 controls. The median (IQR) pre-ART percent APD was 0.71 (0.31-1.13) in cases and 0.58 (0.32-0.94) in controls. A possible trend was found for higher diversity being associated with greater risk of virologic failure in adults (OR = 2.2 per one percent APD increase, 95% CI = [0.8, 7.2]; p = 0.15).

CONCLUSIONS

This study in adults suggests there is a positive association between higher pre-ART pol diversity and the risk of virologic failure in adults rather than an inverse relationship reported in children.

摘要

背景

确定与HIV-1耐药性出现相关的抗病毒治疗前因素对于优化预防病毒学失败的策略至关重要。先前的一项研究报告称,抗病毒治疗前HIV-1 pol基因多样性较低与HIV-1感染儿童病毒学失败风险较高相关。为了在成人中研究这种关联,我们在艾滋病临床试验组(ACTG)进行的一项初始抗病毒治疗研究(A5142)中,通过深度测序测量了具有明确病毒学结果的成人抗病毒治疗前样本中的HIV-1多样性。

方法

我们在ACTG A5142中确定了22例出现病毒学失败且逆转录酶存在耐药突变的病例,以及44例未出现病毒学失败的匹配对照。从血浆HIV-1 RNA合成cDNA。每个cDNA分子用独特的引物ID进行标记,对逆转录酶密码子41-103进行扩增并深度测序。具有相同标签的序列进行比对并生成共识序列以减少PCR和测序错误。通过测量共识序列的平均成对距离(APD)来计算多样性。以APD百分比作为风险因素的精确条件逻辑回归模型估计病毒学失败的比值比及相应的95%置信区间。

结果

获得了21例病例和42例对照的抗病毒治疗前样本的pol基因共识单基因组序列和多样性估计值。病例组抗病毒治疗前APD百分比的中位数(IQR)为0.71(0.31-1.13),对照组为0.58(0.32-0.94)。发现成人中多样性较高与病毒学失败风险较大之间可能存在一种趋势(每增加1%的APD,OR = 2.2,95%CI = [0.8, 7.2];p = 0.15)。

结论

这项针对成人的研究表明,抗病毒治疗前pol基因多样性较高与成人病毒学失败风险之间存在正相关,而非儿童中报告的负相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/172b/5784902/747f3e2bc9cb/pone.0190438.g001.jpg

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