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Patterns of emergent resistance-associated mutations after initiation of non-nucleoside reverse-transcriptase inhibitor-containing antiretroviral regimens in Taiwan: a multicenter cohort study

机译:台湾非核苷类逆转录酶抑制剂的抗逆转录病毒治疗方案启动后出现的与耐药相关的突变模式:一项多中心队列研究

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Background: Increasing trends of resistance-associated mutations (RAMs) to non-nucleoside reverse-transcriptase inhibitors (nNRTIs) have raised concerns about the effectiveness of the regimens in the national HIV treatment programs in resource-limited countries. We aimed to retrospectively investigate the incidence and patterns of emergent RAMs of HIV-1 in HIV-positive adults experiencing virological failure to first-line nNRTI-containing combination antiretroviral therapy (cART) in Taiwan. Patients and methods: Between June 2012 and March 2016, 1138 antiretroviral-na?ve HIV-positive adults without baseline RAMs who initiated nNRTI-containing regimens were included for analysis. Virological failure was defined as plasma viral load (PVL) ≥200?copies/mL after 6?months of cART or confirmed PVL ≥200?copies/mL after achieving PVL <50?copies/mL. Population sequencing was retrospectively performed to detect baseline and emergent RAMs. RAMs were interpreted using the International AIDS Society-USA 2016 mutations list. Results: Seventy-one patients (6.2%) developed virological failure, which occurred in 14.8% (43/291), 3.9% (26/675), and 1.2% (2/172) of patients receiving 2 nucleoside reverse-transcriptase inhibitors (NRTIs) plus nevirapine, efavirenz, and rilpivirine, respectively. Among those, 53 (74.6%) had emergent RAMs identified, which included 43 (81.1%), 53 (100.0%), and 1 (1.9%) with RAMs to NRTIs, nNRTIs, and protease inhibitors, respectively; and 43 (81.1%) had multi-drug resistance. The most common emergent RAMs to NRTIs were M184V/I (42.3%) and K65R (28.2%), and those to nNRTIs were Y181C (42.3%), K103N (15.5%), G190A/E/Q (12.7%), V179D/E (12.7%), and V108I (9.9%). Conclusion: While the rates of virological failure varied with the nNRTI used, the rate of emergent RAMs of HIV-1 to NRTIs and nNRTIs among the antiretroviral-na?ve patients who failed nNRTI-containing cART remained low.
机译:背景:对非核苷类逆转录酶抑制剂(nNRTIs)的耐药相关突变(RAM)的增长趋势引起了人们对该方案在资源有限国家的国家HIV治疗计划中的有效性的担忧。我们旨在回顾性调查台湾地区一线含nNRTI联合抗逆转录病毒疗法(cART)病毒学失败的HIV阳性成年人中HIV-1阳性RAM的发生率和模式。患者和方法:在2012年6月至2016年3月之间,纳入了1138例没有基线RAM的抗逆转录病毒纯正HIV成人,这些成人开始了包含nNRTI的治疗方案。病毒学失败的定义是在cART服用6个月后血浆病毒载量(PVL)≥200拷贝/ mL,或在达到PVL <50拷贝/ mL后确认的PVL≥200拷贝/ mL。回顾性地进行群体测序以检测基线和紧急RAM。使用国际艾滋病学会-美国2016突变列表对RAM进行解释。结果:71名患者(6.2%)发生病毒学衰竭,其中接受2种核苷类逆转录酶抑制剂的患者发生病毒学衰竭的比例为14.8%(43/291),3.9%(26/675)和1.2%(2/172)。 (NRTIs)加奈韦拉平,依非韦伦和利比韦林。其中53个(74.6%)已鉴定出紧急RAM,包括43个(81.1%),53个(100.0%)和1个(1.9%)分别具有针对NRTIs,nNRTIs和蛋白酶抑制剂的RAM。有43人(81.1%)具有多重耐药性。 NRTI最常见的出现RAM是M184V / I(42.3%)和K65R(28.2%),nNRTI出现的RAM是Y181C(42.3%),K103N(15.5%),G190A / E / Q(12.7%),V179D / E(12.7%)和V108I(9.9%)。结论:尽管病毒学失败率随所使用的nNRTI的不同而变化,但在未接受含nNRTI的cART的抗逆转录病毒初治患者中,HIV-1向RAMNs和nNRTIs的RAM出现率仍然较低。

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