Next-Generation Sequencing Reveals a High Frequency of HIV-1 Minority Variants and an Expanded Drug Resistance Profile among Individuals on First-Line ART

Viruses Pub Date : 2024-09-13 DOI:10.3390/v16091454
Maria Nannyonjo, Jonah Omooja, Daniel Lule Bugembe, Nicholas Bbosa, Sandra Lunkuse, Stella Esther Nabirye, Faridah Nassolo, Hamidah Namagembe, Andrew Abaasa, Anne Kazibwe, Pontiano Kaleebu, Deogratius Ssemwanga
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Abstract

We assessed the performance and clinical relevance of Illumina MiSeq next-generation sequencing (NGS) for HIV-1 genotyping compared with Sanger sequencing (SS). We analyzed 167 participants, 45 with virologic failure (VL ≥ 1000 copies/mL), i.e., cases, and 122 time-matched participants with virologic suppression (VL < 1000 copies/mL), i.e., controls, 12 months post-ART initiation. Major surveillance drug resistance mutations (SDRMs) detected by SS were all detectable by NGS. Among cases at 12 months, SS identified SDRMs in 32/45 (71.1%) while NGS identified SDRMs among 35/45 (77.8%), increasing the number of cases with SDRMs by 3/45 (6.7%). Participants identified with, and proportions of major SDRMs increased when NGS was used. NGS vs. SS at endpoint revealed for NNRTIs: 36/45 vs. 33/45; Y181C: 26/45 vs. 24/45; K103N: 9/45 vs. 6/45 participants with SDRMs, respectively. At baseline, NGS revealed major SDRMs in 9/45 (20%) cases without SDRMs by SS. Participant MBL/043, among the nine, the following major SDRMs existed: L90M to PIs, K65R and M184V to NRTIs, and Y181C and K103N to NNRTIs. The SDRMs among the nine increased SDRMs to NRTIs, NNRTIs, and PIs. Only 43/122 (25.7%) of participants had pre-treatment minority SDRMs. Also, 24.4% of the cases vs. 26.2 of controls had minority SDRMs (p = 0.802); minority SDRMs were not associated with virologic failure. NGS agreed with SS in HIV-1 genotyping but detected additional major SDRMs and identified more participants harboring major SDRMs, expanding the HIV DRM profile of this cohort. NGS could improve HIV genotyping to guide treatment decisions for enhancing ART efficacy, a cardinal pre-requisite in the pursuit of the UNAIDS 95-95-95 targets.
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下一代测序揭示了一线抗逆转录病毒疗法患者中 HIV-1 少数变异株的高频率和耐药性特征的扩展
我们评估了 Illumina MiSeq 下一代测序(NGS)与 Sanger 测序(SS)相比在 HIV-1 基因分型方面的性能和临床意义。我们对 167 名参与者进行了分析,其中包括 45 名病毒学失败者(VL ≥ 1000 copies/mL),即病例,以及 122 名病毒学抑制(VL < 1000 copies/mL)的时间匹配参与者,即对照组。SS 检测到的主要监测耐药突变 (SDRM) 均可通过 NGS 检测到。在 12 个月的病例中,SS 在 32/45 例(71.1%)中发现了 SDRMs,而 NGS 在 35/45 例(77.8%)中发现了 SDRMs,使发现 SDRMs 的病例增加了 3/45 例(6.7%)。使用 NGS 时,发现主要 SDRM 的参与者人数和比例均有所增加。NGS 与 SS 在终点显示的 NNRTIs 的对比:36/45 vs. 33/45;Y181C:26/45 vs. 24/45;K103N:9/45 vs. 6/45 参与者分别有 SDRMs。基线时,NGS 发现 9/45 个病例(20%)存在主要的 SDRM,而 SS 没有发现 SDRM。在 9 名 MBL/043 参与者中,存在以下主要 SDRM:L90M 与 PIs 有关,K65R 和 M184V 与 NRTIs 有关,Y181C 和 K103N 与 NNRTIs 有关。在九种增加的 SDRMs 中,对 NRTIs、NNRTIs 和 PIs 的 SDRMs 增加。只有 43/122 名参与者(25.7%)在治疗前有少数 SDRMs。此外,24.4% 的病例与 26.2% 的对照组相比具有少数 SDRMs(p = 0.802);少数 SDRMs 与病毒学失败无关。NGS 与 SS 的 HIV-1 基因分型结果一致,但检测出了更多的主要 SDRM,并发现了更多携带主要 SDRM 的参与者,从而扩大了该队列的 HIV DRM 特征。NGS 可以改进 HIV 基因分型,为提高抗逆转录病毒疗法疗效的治疗决策提供指导,这是实现联合国艾滋病规划署 95-95-95 目标的一个重要前提条件。
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