Consistency between Treatment Effects on Clinical and Brain Atrophy Outcomes in Alzheimer's Disease Trials.

IF 8.5 3区 医学 Q1 CLINICAL NEUROLOGY Jpad-Journal of Prevention of Alzheimers Disease Pub Date : 2024-01-01 DOI:10.14283/jpad.2023.92
M Ten Kate, F Barkhof, A J Schwarz
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Abstract

Background: Longitudinal changes in volumetric MRI outcome measures have been shown to correlate well with longitudinal changes in clinical instruments and have been widely used as biomarker outcomes in clinical trials for Alzheimer's disease (AD). While instances of discordant findings have been noted in some trials, especially the recent amyloid-removing therapies, the overall relationship between treatment effects on brain atrophy and clinical outcomes, and how it might depend on treatment target or mechanism, clinical instrument or imaging variable is not yet clear.

Objective: To systematically assess the consistency and therapeutic class-dependence of treatment effects on clinical outcomes and on brain atrophy in published reports of clinical trials conducted in mild cognitive impairment (MCI) and/or AD.

Design: Quantitative review of the published literature. The consistency of treatment effects on clinical and brain atrophy outcomes was assessed in terms of statistical agreement with hypothesized equal magnitude effects (e.g., 30% slowing of both) and nominal directional concordance, as a function of therapeutic class.

Setting: Interventional randomized clinical trials.

Participants: MCI or AD trial participants.

Intervention: Treatments included were those that involved ingestion or injection of a putatively active substance into the body, encompassing both pharmacological and controlled dietary interventions.

Measurements: Each trial included in the analysis reported at least one of the required clinical outcomes (ADAS-Cog, CDR-SB or MMSE) and at least one of the required imaging outcomes (whole brain, ventricular or hippocampal volume).

Results: Data from 35 trials, comprising 185 pairwise comparisons, were included. Overall, the 95% confidence bounds overlapped with the line of identity for 150/185 (81%) of the imaging-clinical variable pairs. The greatest proportion of outliers was found in trials of anti-amyloid antibodies that have been shown to dramatically reduce the level of PET-detectable amyloid plaques, for which only 13/33 (39%) of observations overlapped the identity line. A Deming regression calculated using all data points yielded a slope of 0.54, whereas if data points from the amyloid remover class were excluded, the Deming regression line had a slope of 0.92. Directional discordance of treatment effects was also most pronounced for the amyloid-removing class, and for comparisons involving ventricular volume.

Conclusion: Our results provide a frame of reference for the interpretation of clinical and brain atrophy results from future clinical trials and highlight the importance of mechanism of action in the interpretation of imaging results.

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阿尔茨海默病试验中治疗效果对临床和脑萎缩结果的一致性。
背景:体积磁共振成像结果测量的纵向变化已被证明与临床工具的纵向变化有很好的相关性,并已被广泛用作阿尔茨海默病(AD)临床试验的生物标记结果。虽然在一些试验中,尤其是最近的淀粉样蛋白清除疗法中发现了一些不一致的结果,但治疗效果对脑萎缩和临床结果之间的总体关系,以及这种关系如何取决于治疗目标或机制、临床工具或成像变量,目前尚不清楚:系统评估已发表的轻度认知障碍(MCI)和/或注意力缺陷(AD)临床试验报告中治疗对临床结果和脑萎缩影响的一致性和治疗类别依赖性:设计:对已发表的文献进行定量综述。设计:对已发表的文献进行定量综述,评估治疗对临床结果和脑萎缩结果影响的一致性,即与假设的等量效应(如两者均减慢30%)和名义方向一致性的统计一致性,作为治疗类别的函数:干预性随机临床试验:干预:干预:纳入的治疗方法包括向体内摄入或注射假定的活性物质,包括药物干预和控制饮食干预:每项纳入分析的试验都至少报告了一项所需的临床结果(ADAS-Cog、CDR-SB 或 MMSE)和至少一项所需的成像结果(全脑、脑室或海马体积):共纳入了 35 项试验的数据,包括 185 项配对比较。总体而言,150/185(81%)对成像-临床变量的95%置信区间与特征线重叠。在抗淀粉样蛋白抗体试验中发现的离群值比例最大,这些抗体已被证明能显著降低 PET 检测到的淀粉样蛋白斑块的水平,其中只有 13/33 (39%)的观察结果与同一性线重叠。使用所有数据点计算的戴明回归斜率为 0.54,而如果排除淀粉样蛋白清除剂类的数据点,戴明回归线的斜率为 0.92。治疗效果的方向性不一致在淀粉样蛋白去除类和涉及心室容积的比较中也最为明显:我们的研究结果为解读未来临床试验的临床和脑萎缩结果提供了参考框架,并强调了作用机制在解读成像结果中的重要性。
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自引率
7.80%
发文量
85
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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