评估β淀粉样蛋白靶向疫苗AFFITOPE®AD02在早期阿尔茨海默病中的作用的II期研究方法学方面-新型复合量表的前瞻性使用

IF 8.5 3区 医学 Q1 CLINICAL NEUROLOGY Jpad-Journal of Prevention of Alzheimers Disease Pub Date : 2015-06-01 DOI:10.14283/JPAD.2015.67
S. Hendrix, N. Ellison, S. Stanworth, L. Tierney, F. Mattner, W. Schmidt, B. Dubois, A. Schneeberger
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Delayed Word Recall and Digit Cancellation were among the items excluded due to lack of improved sensitivity to decline. Highly weighted ADL items included in the adapted functional scale (aADCS-ADL) were using the telephone, traveling, preparing a meal/snack, selecting clothing, shopping and using appliances. Excluded items were primarily basic ADLs such as eating, walking, toileting and bathing. Comparisons between traditional scales and primary outcome adapted scales show improved sensitivity to group differences with the adapted scales in the phase II trial. Most of the improvement in the sensitivity of the aADAS-cog and the aADCS-ADL is due to a larger treatment difference observed rather than the improved sensitivity to decline in the comparison groups.\n\n\nCONCLUSION\nTo our knowledge, this is the first study to prospectively use optimized scales as primary endpoints and to demonstrate the superior power of optimized scales and composites in early disease. 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引用次数: 13

摘要

优化的量表和综合结果被提出作为一种更准确地测量阿尔茨海默病相关衰退的方法。AFFITOPE®AD02是一种靶向淀粉样蛋白β (Aβ)的疫苗,可引发抗Aβ抗体。IMM-AD04,通常被称为明矾,最初被指定为对照剂,在早期AD患者的多中心平行组II期研究中似乎具有疾病改善活性。目的:基于历史数据,开发认知、功能和对早期AD(轻度加前驱AD)衰退和治疗效果敏感性提高的复合量表的适应性结果,并在本II期研究中评估这些适应性结果。使用偏最小二乘模型分析来自公共数据集的DESIGNData,以确定最佳加权认知结果adaptadas -cog和最佳加权ADL结果adaptadcs -ADL,这两个结果被前瞻性地定义为研究的共同主要终点,并合并为复合量表。来自ADCS研究中安慰剂组162例患者和ADNI I研究中156例轻度患者的数据被汇总用于本分析。适应性adas - adl量表包括13个ADAS-cog项目以及几个神经心理测试项目和认知状态项目,适应性ADCS-ADL量表包括所有ADCS-ADL项目。在预先指定的分析完成后,额外的适应和复合量表以事后的方式进行了调查。对AFFITOPE®AD02 (AFF006,临床试验标识符:NCT01117818)的II期试验数据和早期AD的历史数据进行了适应性和复合量表的评估。比较II期研究中5个治疗组的适应量表、复合量表和传统量表的最小二乘法均值、标准差和最小二乘法均值与标准差比,以及总体历史数据。还比较了II期研究的治疗效应大小和p值。结果在适应性认知量表(aADAS-cog)中选择的权重最高的认知项目是单词回忆、单词识别和定向。由于缺乏对衰退的敏感性,延迟单词回忆和数字取消被排除在外。适应功能量表(aADCS-ADL)中权重较高的ADL项目包括使用电话、旅行、准备膳食/零食、选择服装、购物和使用电器。排除的项目主要是基本的日常生活习惯,如吃饭、走路、如厕和洗澡。传统量表和主要结局调整量表的比较显示,在II期试验中,调整量表对组间差异的敏感性有所提高。aADAS-cog和aADCS-ADL的敏感性的提高主要是由于观察到的治疗差异较大,而不是由于对照组的敏感性下降。据我们所知,这是第一个前瞻性地使用优化量表作为主要终点,并证明优化量表和复合量表在早期疾病中的优越功效的研究。虽然随机分组之间的治疗差异可能是由于治疗本身以外的因素造成的,例如基线不平衡,但检测这些差异的改进能力仍然有利于调整量表。检测治疗效果的过度敏感问题是通过选择显著性的α水平来控制的,在我们的情况下,这种情况发生的概率不到5%。治疗差异的临床相关性应与统计显著性分开评估,并且在本II期研究中,对功能、行为和生活质量结果的显著或类似大小的影响支持,这对患者和护理人员很重要。
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Methodological Aspects of the Phase II Study AFF006 Evaluating Amyloid-beta -Targeting Vaccine AFFITOPE® AD02 in Early Alzheimer's Disease - Prospective Use of Novel Composite Scales.
BACKGROUND Optimized scales and composite outcomes have been proposed as a way to more accurately measure Alzheimer's disease related decline. AFFITOPE® AD02, is an amyloid-beta (Aβ)-targeting vaccine to elicit anti-Aβ antibodies. IMM-AD04, commonly known as Alum, originally designated as a control agent, appeared to have disease-modifying activity in a multicenter, parallel group phase II study in early AD patients. OBJECTIVES To develop adapted outcomes for cognition, function and a composite scale with improved sensitivity to decline and treatment effects in early AD (mild plus prodromal AD) based on historical data and to assess these adapted outcomes in this phase II study. DESIGN Data from public datasets was analyzed using a partial least squares model in order to identify an optimally weighted cognitive outcome, Adapted ADAS-cog, and an optimally weighted ADL outcome, Adapted ADCS-ADL which were prospectively defined as co-primary endpoints for the study and were also combined into a composite scale. Data from 162 patients in the placebo groups of ADCS studies and 156 mild patients in the ADNI I study were pooled for this analysis. The Adapted ADAS-cog scale considered 13 ADAS-cog items as well as several Neuropsychological test items and CogState items, the Adapted ADCS-ADL considered all ADCS-ADL items. After the pre-specified analyses were complete, additional adapted and composite scales were investigated in a post-hoc manner. Evaluation of the adapted and composite scales was performed on Phase II trial data for AFFITOPE® AD02 (AFF006, Clinical Trial Identifier: NCT01117818) and historic data in early AD. Least square means, standard deviations, and least squares mean to standard deviation ratios were compared among adapted and composite scales and traditional scales for the 5 treatment groups in the phase II study and overall for the historic data. Treatment effect sizes and p-values were also compared for the phase II study. RESULTS Cognitive items that were selected for the adapted cognitive scale (aADAS-cog) and had the highest weights were Word Recall, Word Recognition, and Orientation. Delayed Word Recall and Digit Cancellation were among the items excluded due to lack of improved sensitivity to decline. Highly weighted ADL items included in the adapted functional scale (aADCS-ADL) were using the telephone, traveling, preparing a meal/snack, selecting clothing, shopping and using appliances. Excluded items were primarily basic ADLs such as eating, walking, toileting and bathing. Comparisons between traditional scales and primary outcome adapted scales show improved sensitivity to group differences with the adapted scales in the phase II trial. Most of the improvement in the sensitivity of the aADAS-cog and the aADCS-ADL is due to a larger treatment difference observed rather than the improved sensitivity to decline in the comparison groups. CONCLUSION To our knowledge, this is the first study to prospectively use optimized scales as primary endpoints and to demonstrate the superior power of optimized scales and composites in early disease. Although it is possible that the treatment difference between randomized groups is due to a factor other than the treatment itself, for instance baseline imbalance, the improved power to detect these differences still argues in favor of the adapted scales. The issue of oversensitivity to detect treatment effects is controlled by selection of the alpha level for significance, and in our case will happen less than 5% of the time. Clinical relevance of the treatment difference should be assessed separately from statistical significance, and in this phase II study, is supported by significant or similar sizes of effect on function, behaviour and quality of life outcomes, which are important to patients and caregivers.
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期刊介绍: The JPAD « Journal of Prevention of Alzheimer’Disease » will publish reviews, original research articles and short reports to improve our knowledge in the field of Alzheimer prevention including : neurosciences, biomarkers, imaging, epidemiology, public health, physical cognitive exercise, nutrition, risk and protective factors, drug development, trials design, and heath economic outcomes. JPAD will publish also the meeting abstracts from Clinical Trial on Alzheimer Disease (CTAD) and will be distributed both in paper and online version worldwide.
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