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基于阿巴卡韦的三联核苷方案用于HIV患者的维持治疗。

Abacavir-based triple nucleoside regimens for maintenance therapy in patients with HIV.

作者信息

Cruciani Mario, Mengoli Carlo, Serpelloni Giovanni, Parisi Saverio G, Malena Marina, Bosco Oliviero

机构信息

Center of Community Medicine and Infectious Diseases Service, ULSS 20 Verona, Verona, Italy.

出版信息

Cochrane Database Syst Rev. 2013 Jun 5;2013(6):CD008270. doi: 10.1002/14651858.CD008270.pub2.

Abstract

BACKGROUND

Regimen simplification can be defined as a change in established effective therapy to reduce pill burden and dosing frequency, to enhance tolerability, or to decrease specific food and fluid requirements. Many patients on suppressive antiretroviral therapy may be considered candidates for a simplification strategy and, among them, those who have achieved virologic suppression. Several clinical trials have evaluated the efficacy of triple nucleoside combination as a simplification therapy in patients who achieved virologic suppression

OBJECTIVES

The aim of this review is to combine randomised, controlled trials to examine whether in patients with undetectable viraemia on a Protease inhibitor (PI) based regimen simplification treatment with abacavir (ABC)-based triple-nucleoside combinations has similar rates of efficacy and tolerability compared with a PI regimen or simplification with a NNRTIs (efavirenz-EFV- or nevirapine-NVP) containing regimen. Studies were included if they had at least two of the three interventions, including one 3NRTI arm.

SEARCH METHODS

Electronic databases and conference proceedings were searched (1996-2012) with relevant search terms without limits to language.

SELECTION CRITERIA

Randomised controlled trials (RCTs) only are included in this review. Patients population is represented by HIV-infected adult patients treated with a PI-containing regimen (PI or boosted PI),  with undetectable viral load. Patients on a PI-containing regimen had three possibilities: continue the PI regimen or switch to a simplification maintenance regimen, including switch to a NNRTI (EFV or NVP) containing regimen, or switch to a triple-NRTI regimen (ABC-zidovudine-lamivudine)

DATA COLLECTION AND ANALYSIS

The primary outcomes were: proportion of patients discontinuing or switching antiretroviral therapy due to virologic failure or to adverse events; death (all cause) and AIDS defining illness; occurrence of myocardial infarction and cardiovascular disease. Secondary outcomes  were: proportion of patients maintaining an undetectable viral load (e.g. HIV-RNA <50 or <400 copies/mm(3)); change in mean CD4+ cell count; occurrence of lipodystrophy. We applied Cochrane Collaboration tools to assess each individual study for risk for bias.

MAIN RESULTS

We included eight RCT, for a total of 1,610 patients. All the studies included HIV-1 infected patients virologically suppressed after a successful treatment with PI containing ART. Articles included in the analysis were published between 2001 and 2010, and could be classified as low risk of bias trials in most of the domains considered. Overall, there was no significant difference between the participants on triple nucleoside combination and controls, either PI-based or NNRTI based in terms of overall failures, death and AIDS related events, and rates of patients with viral load below the detectability cut-off. For the outcomes discontinuation for adverse events and virologic failures, the RRs were not significant , albeit  being not far from the alpha level of 0.05, thus suggesting a weak evidence of lower incidence of side effects  and an higher incidence of virologic failure in the 3NRTI group compared to controls . Change in lipids and in CD4 cells from baselines were reported in 7 studies, but inconsistency in reporting these data did not allow quantitative analysis. However, all agreed that simplification with ABC had a favourable and significant impact on lipid metabolism compared to control group. An increase in CD4 cells count from baseline was evident in all analysed studies, without significant differences between ABC and controls in individual studies.

AUTHORS' CONCLUSIONS: The strategy of switching to triple nucleoside regimens shows weak evidence of lower incidence of side effects and a higher incidence of virologic failure in the 3NRTI group compared to controls. Simplification with 3NRTI holds the advantages of preserving other classes of antiretroviral drugs, to lower blood lipids, and to be cost effective and simple to administer.Thus, simplification with triple nucleoside regimens AZT + 3TC + ABC should be still considered for individuals who are unable to tolerate or have contraindications to NNRTI or PI based regimens. Additional data are needed on longer-term efficacy of triple NRTI regimens, particularly on the development of antiretroviral resistance. Though studies in the current review were conducted between 2001 and 2010, the large majority of patients from studies analysed received old PI regimens (e.g., indinavir, ritonavir, nelfinavir, saquinavir) not longer recommended by International Guidelines. Since current guidelines recommend new "lipid -friendly" PI, future studies should compare regimens containing these news PIs to triple NRTI regimens. More realistically, however, there are opportunities to examine these issues in existing cohorts.

摘要

背景

方案简化可定义为对既定有效治疗方案进行改变,以减轻服药负担和给药频率、提高耐受性或减少特定食物及液体需求。许多接受抑制性抗逆转录病毒治疗的患者可能被视为方案简化策略的候选对象,其中包括那些已实现病毒学抑制的患者。多项临床试验评估了三联核苷组合作为方案简化疗法在实现病毒学抑制的患者中的疗效。

目的

本综述的目的是综合随机对照试验,以研究在基于蛋白酶抑制剂(PI)的方案简化治疗中,对于病毒血症检测不到的患者,使用基于阿巴卡韦(ABC)的三联核苷组合与基于PI的方案或含非核苷类逆转录酶抑制剂(NNRTIs,依非韦伦 - EFV - 或奈韦拉平 - NVP)的方案简化相比,疗效和耐受性是否相似。如果研究具有三项干预措施中的至少两项,包括一个三联核苷逆转录酶抑制剂(3NRTI)组,则纳入研究。

检索方法

检索电子数据库和会议论文集(1996 - 2012年),使用相关检索词,不限语言。

入选标准

本综述仅纳入随机对照试验(RCT)。患者群体为接受含PI方案(PI或增强型PI)治疗且病毒载量检测不到的HIV感染成年患者。接受含PI方案的患者有三种可能性:继续PI方案或切换至简化维持方案,包括切换至含NNRTI(EFV或NVP)的方案,或切换至三联核苷逆转录酶抑制剂方案(ABC - 齐多夫定 - 拉米夫定)。

数据收集与分析

主要结局为:因病毒学失败或不良事件而停止或切换抗逆转录病毒治疗的患者比例;死亡(全因)和艾滋病定义疾病;心肌梗死和心血管疾病的发生情况。次要结局为:维持病毒载量检测不到的患者比例(例如,HIV - RNA <50或<400拷贝/mm³);CD4⁺细胞计数的均值变化;脂肪代谢障碍的发生情况。我们应用Cochrane协作工具评估每项个体研究的偏倚风险。

主要结果

我们纳入了8项RCT,共1610名患者。所有研究均纳入了经含PI的抗逆转录病毒治疗成功后病毒学得到抑制的HIV - 1感染患者。纳入分析的文章发表于2001年至2010年之间,在大多数考虑的领域可归类为低偏倚风险试验。总体而言,三联核苷组合组与对照组(基于PI或基于NNRTI)在总体失败、死亡和艾滋病相关事件以及病毒载量低于检测下限的患者比例方面无显著差异。对于因不良事件和病毒学失败而停药的结局,相对危险度无显著差异,尽管接近0.05的α水平,这表明与对照组相比,3NRTI组副作用发生率较低和病毒学失败发生率较高的证据较弱。7项研究报告了脂质和CD4细胞相对于基线的变化,但报告这些数据的不一致性不允许进行定量分析。然而,所有研究均认为与对照组相比,使用ABC进行简化对脂质代谢有有利且显著的影响。在所有分析的研究中,CD4细胞计数从基线开始均有明显增加,在个体研究中ABC组与对照组之间无显著差异。

作者结论

与对照组相比,切换至三联核苷方案的策略显示3NRTI组副作用发生率较低和病毒学失败发生率较高的证据较弱。使用3NRTI进行简化具有保留其他类别抗逆转录病毒药物、降低血脂、具有成本效益且易于给药的优点。因此,对于无法耐受或有NNRTI或基于PI方案的禁忌症的个体,仍应考虑使用三联核苷方案AZT + 3TC + ABC进行简化。需要关于三联核苷逆转录酶抑制剂方案长期疗效的更多数据,特别是关于抗逆转录病毒耐药性的发展。尽管本综述中的研究在2001年至2010年之间进行,但分析研究中的大多数患者接受的是国际指南不再推荐的旧PI方案(例如,茚地那韦、利托那韦、奈非那韦、沙奎那韦)。由于当前指南推荐新的“脂质友好型”PI,未来研究应将含这些新PI的方案与三联核苷逆转录酶抑制剂方案进行比较。然而,更实际的是,有机会在现有队列中研究这些问题。

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