Factors in AIDS dementia complex trial design: results and lessons from the abacavir trial.

PLoS clinical trials Pub Date : 2007-03-30 DOI:10.1371/journal.pctr.0020013

Bruce J Brew, Mark Halman, Jose Catalan, Ned Sacktor, Richard W Price, Steve Brown, Hamp Atkinson, David B Clifford, David Simpson, Gabriel Torres, Colin Hall, Christopher Power, Karen Marder, Justin C Mc Arthur, William Symonds, Carmen Romero

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引用次数: 69

Abstract

Objectives: To determine the efficacy of adding abacavir (Ziagen, ABC) to optimal stable background antiretroviral therapy (SBG) to AIDS dementia complex (ADC) patients and address trial design.

Design: Phase III randomized, double-blind placebo-controlled trial.

Setting: Tertiary outpatient clinics.

Participants: ADC patients on SBG for > or = 8 wk.

Interventions: Participants were randomized to ABC or matched placebo for 12 wk.

Outcome measures: The primary outcome measure was the change in the summary neuropsychological Z score (NPZ). Secondary measures were HIV RNA and the immune activation markers beta-2 microglobulin, soluble tumor necrosis factor (TNF) receptor 2, and quinolinic acid.

Results: 105 participants were enrolled. The median change in NPZ at week 12 was +0.76 for the ABC + SBG and +0.63 for the SBG groups (p = 0.735). The lack of efficacy was unlikely related to possible limited antiviral efficacy of ABC: at week 12 more ABC than placebo participants had plasma HIV RNA < or = 400 copies/mL (p = 0.002). There were, however, other factors. Two thirds of patients were subsequently found to have had baseline resistance to ABC. Second, there was an unanticipated beneficial effect of SBG that extended beyond 8 wk to 5 mo, thereby rendering some of the patients at baseline unstable. Third, there was an unexpectedly large variability in neuropsychological performance that underpowered the study. Fourth, there was a relative lack of activity of ADC: 56% of all patients had baseline cerebrospinal fluid (CSF) HIV-1 RNA < 100 copies/mL and 83% had CSF beta-2 microglobulin < 3 nmol/L at baseline.

Conclusions: The addition of ABC to SBG for ADC patients was not efficacious, possibly because of the inefficacy of ABC per se, baseline drug resistance, prolonged benefit from existing therapy, difficulties with sample size calculations, and lack of disease activity. Assessment of these trial design factors is critical in the design of future ADC trials.

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艾滋病痴呆复杂试验设计的因素:阿巴卡韦试验的结果和教训。

目的:确定在最优稳定背景抗逆转录病毒治疗(SBG)中加入阿巴卡韦(Ziagen, ABC)治疗艾滋病痴呆复合物(ADC)患者的疗效，并改进试验设计。设计:III期随机、双盲、安慰剂对照试验。环境:三级门诊。参与者:接受SBG治疗≥8周的ADC患者。干预措施:参与者被随机分配到ABC组或匹配的安慰剂组12周。结果测量:主要结果测量是神经心理学Z总分(NPZ)的变化。次要指标是HIV RNA和免疫激活标志物β -2微球蛋白、可溶性肿瘤坏死因子(TNF)受体2和喹啉酸。结果:105名受试者入组。第12周，ABC + SBG组NPZ的中位变化为+0.76,SBG组为+0.63 (p = 0.735)。缺乏疗效不太可能与ABC有限的抗病毒疗效有关:在第12周时，ABC比安慰剂参与者的血浆HIV RNA <或= 400拷贝/mL (p = 0.002)。然而，还有其他因素。三分之二的患者随后发现对ABC有基线耐药性。其次，SBG的有益作用超出8周至5个月，因此使一些患者在基线时不稳定。第三，神经心理学表现出乎意料的大变异性削弱了研究的动力。第四，ADC活性相对缺乏:56%的患者基线脑脊液(CSF) HIV-1 RNA < 100拷贝/mL, 83%的患者基线脑脊液β -2微球蛋白< 3 nmol/L。结论:在ADC患者的SBG中添加ABC无效，可能是由于ABC本身无效、基线耐药、现有治疗的长期获益、样本量计算困难以及缺乏疾病活动性。评估这些试验设计因素对未来ADC试验的设计至关重要。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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PLoS clinical trials

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