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首页> 外文期刊>The Lancet infectious diseases >Effect of HIV-1 low-level viraemia during antiretroviral therapy on treatment outcomes in WHO-guided South African treatment programmes: a multicentre cohort study
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Effect of HIV-1 low-level viraemia during antiretroviral therapy on treatment outcomes in WHO-guided South African treatment programmes: a multicentre cohort study

机译:抗逆转录病毒治疗抗逆转录病毒治疗对南非治疗方案治疗成果的影响:多期队列队列研究

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BackgroundAntiretroviral therapy (ART) that enables suppression of HIV replication has been successfully rolled out at large scale to HIV-positive patients in low-income and middle-income countries. WHO guidelines for these regions define failure of ART with a lenient threshold of viraemia (HIV RNA viral load ≥1000 copies per mL). We investigated the occurrence of detectable viraemia during ART below this threshold and its effect on treatment outcomes in a large South African cohort. MethodsIn this observational cohort study, we included HIV-positive adults registered between Jan 1, 2007, and May 1, 2016, at 57 clinical sites in South Africa, who were receiving WHO-recommended ART regimens and viral load monitoring. Low-level viraemia was defined as the occurrence of at least one viral load measurement of 51–999 copies per mL during ART. Outcomes were WHO-defined virological failure (one or more viral load measurement of ≥1000 copies per mL) and switch to second-line ART. Risks were estimated with Cox proportional hazard models. Findings70?930 patients were included in the analysis, of whom 67?644 received first-line ART, 1476 received second-line ART, and 1810 received both. Median duration of follow-up was 124 weeks (IQR 56–221) for patients on first-line ART and 101 weeks (IQR 51–178) for patients on second-line ART. Low-level viraemia occurred in 16?013 (23%) of 69?454 patients, with an incidence of 11·5 per 100 person-years of follow-up (95% CI 11·4–11·7), during first-line ART. Virological failure during follow-up occurred in 14?380 (22%) of 69?454 patients on first-line ART. Low-level viraemia was associated with increased hazards of virological failure (hazard ratio [HR] 2·6, 95% CI 2·5–2·8; p<0·0001) and switch to second-line ART (HR 5·2, 4·4–6·1; p<0·0001]) compared with virological suppression of less than 50 copies per mL. Risk of virological failure increased further with higher ranges and persistence of low-level viraemia. InterpretationIn this large cohort, low-level viraemia occurred frequently and increased the risk of virological failure and switch to second-line ART. Strategies for management of low-level viraemia need to be incorporated into WHO guidelines to meet UNAIDS-defined targets aimed at halting the global HIV epidemic. FundingNone.
机译:背景前一体化动物疗法(ART)抑制艾滋病毒复制的抑制,以大规模成功推出到低收入和中等收入国家的艾滋病毒阳性患者。世卫组织这些地区的指导方针定义了具有病毒血症的宽阈值的艺术失败(HIV RNA病毒载荷≥1000每ML拷贝)。我们调查了艺术期间可检测的病毒血症的发生及其对大型南非队列治疗成果的影响。方法介绍该观察队队列研究,我们包括2007年1月1日期间的艾滋病毒阳性成年人,2016年5月1日在南非57名临床地点,他正在接受谁推荐的艺术方案和病毒载荷监测。低水平的病毒血症被定义为在艺术期间每毫升51-999拷贝的至少一种病毒负荷测量的发生。结果是世界卫生组织定义的病毒学失败(一个或多个病毒载量≥1000毫升/ mL),切换到第二线艺术。用Cox比例危险模型估算风险。调查结果70?930名患者被列入分析中,其中67岁?644获得的一线艺术,1476件接受了第二线艺术,1810年接受了两者。中位数的后续时间为第一线艺术患者的124周(IQR 56-221),以及用于第二线艺术患者的101周(IQR 51-178)。低水平的病毒血症发生在16岁?013(23%)的69例?454名患者中,发病率为11·每100人的后续时间(95%CI 11·4-11·7),首先-线条艺术。随访期间的病毒学失败发生在14?380(22%)的69岁(22%)的一线艺术患者中。低水平的病毒血症与病毒学失败的危害增加有关(危害比[HR] 2·6,95%CI 2·5-2·8; P <0·0001),并切换到第二线艺术(HR 5· 2,4·4-6·1; p <0·0001])与每mL少于50份的病毒学抑制相比。病毒学失败的风险进一步增加了较高的范围和低水平病毒血症的持续性。解释这种大队列,低水平的病毒血症频繁发生,增加了病毒学失败的风险,并转向二线艺术。低级别病毒管理的策略需要纳入世卫组织,以满足旨在停止全球艾滋病毒流行病的艾滋病规划规定的目标的指导方针。浮标。

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