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埃塞俄比亚HIV-1C分离株中获得性耐药性的上升趋势:一项十年纵向研究。

Upward trends of acquired drug resistances in Ethiopian HIV-1C isolates: A decade longitudinal study.

作者信息

Mulu Andargachew, Maier Melanie, Liebert Uwe Gerd

机构信息

Armauer Hanssen Research Institute (AHRI), Addis Ababa, Ethiopia.

Institute of Virology, Medical Faculty, Leipzig University, Leipzig, Germany.

出版信息

PLoS One. 2017 Oct 19;12(10):e0186619. doi: 10.1371/journal.pone.0186619. eCollection 2017.

Abstract

BACKGROUND

The emergence, accumulation and spread of HIV-1 drug resistance strains in Africa could compromise the effectiveness of HIV treatment programs. This study was aimed at determining the incidence of virological failure and acquired drug resistance mutations overtime and identifying the most common mutational pathways of resistance in a well characterized HIV-1C infected Ethiopian cohort.

METHODS

A total of 320 patients (220 ART naïve and 100 on first lines ART) were included and followed. ART initiation and patients' monitoring was based on the WHO clinical and immunological parameters. HIV viral load measurement and genotypic drug resistance testing were done at baseline (T0-2008) and after on average at a median time of 30 months on ART at three time points (T1-2011, T2-2013, T3-2015).

FINDINGS

The incidence of virological failure has increased overtime from 11 at T1 to 17 at T2 and then to 30% at T3. At all time point's almost all of the patients with virological failure and accumulated drug resistance mutations had not met the WHO clinical and immunologic failure criteria and continued the failing regimen. A steep increase in the incidence and accumulation of major acquired NRTI and NNRTI drug resistance mutations have been observed (from 40% at T1 to 64% at T2 and then to 66% at T3). The most frequent NRTIs drug resistance associated mutations are mainly the lamivudine-induced mutation M184V which was detected in 4 patients at T1 and showed a 2 fold increase in the following time points (T2: n = 8) and at (T3: n = 12) and the thymidine analogue mutations (such as D67N, K70R and K219E) which were not-detected at baseline T0 and T1 but were increased progressively to 10 at T2 and to 17 at T3. The most frequent NNRTIs associated mutations were K103N, V106M and Y188C.

CONCLUSIONS

An upward trend in the incidence of virological failure and accumulation of NRTI and NNRTI associated acquired antiretroviral drug resistance mutations are observed. The data suggest the need for virological monitoring, resistance testing for early detection of failure and access for TDF and PI containing drugs. Population-level and patient targeted interventions to prevent the spread of mutant variants is warranted.

摘要

背景

HIV-1耐药毒株在非洲的出现、积累和传播可能会损害艾滋病治疗项目的有效性。本研究旨在确定病毒学失败的发生率以及随时间推移获得性耐药突变的情况,并在一个特征明确的HIV-1C感染的埃塞俄比亚队列中确定最常见的耐药突变途径。

方法

共纳入320例患者(220例初治患者和100例一线抗逆转录病毒治疗患者)并进行随访。抗逆转录病毒治疗的启动和患者监测基于世界卫生组织的临床和免疫学参数。在基线期(T0 - 2008年)以及平均接受抗逆转录病毒治疗30个月后的三个时间点(T1 - 2011年、T2 - 2013年、T3 - 2015年)进行HIV病毒载量检测和基因型耐药性检测。

结果

病毒学失败的发生率随时间增加,从T1期的11%增至T2期的17%,然后在T3期达到30%。在所有时间点,几乎所有出现病毒学失败和积累了耐药突变的患者均未达到世界卫生组织的临床和免疫学失败标准,并继续使用失败的治疗方案。观察到主要获得性核苷类逆转录酶抑制剂(NRTI)和非核苷类逆转录酶抑制剂(NNRTI)耐药突变的发生率和积累急剧增加(从T1期的40%增至T2期的64%,然后在T3期达到66%)。最常见的与NRTI耐药相关的突变主要是拉米夫定诱导的M184V突变,在T1期有4例患者检测到,在随后的时间点(T2:n = 8)和(T3:n = 12)增加了两倍,以及胸苷类似物突变(如D67N、K70R和K219E),在基线期T0和T1未检测到,但在T2期逐渐增至10例,在T3期增至17例。最常见的与NNRTI相关的突变是K103N、V106M和Y188C。

结论

观察到病毒学失败的发生率以及与NRTI和NNRTI相关的获得性抗逆转录病毒药物耐药突变的积累呈上升趋势。数据表明需要进行病毒学监测、耐药性检测以早期发现治疗失败,并获取含替诺福韦和蛋白酶抑制剂的药物。有必要采取针对人群和患者的干预措施以防止突变变体的传播。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d4f/5648217/dfa4c831828d/pone.0186619.g001.jpg

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