Finding Treatment Effects in Alzheimer Trials in the Face of Disease Progression Heterogeneity

临床痴呆评级 痴呆 阿尔茨海默病 内科学 认知功能衰退 临床试验 安慰剂 疾病 阿尔茨海默病神经影像学倡议 神经影像学 认知 载脂蛋白E 评定量表 医学 心理学 精神科 病理 发展心理学 替代医学
作者
Roos J. Jutten,Sietske A.M. Sikkes,Wiesje M. van der Flier,Philip Scheltens,Pieter Jelle Visser,Betty M. Tijms
出处
期刊:Neurology [Lippincott Williams & Wilkins]
卷期号:96 (22): e2673-e2684 被引量:26
标识
DOI:10.1212/wnl.0000000000012022
摘要

To investigate the influence of heterogeneity in disease progression for detecting treatment effects in Alzheimer disease (AD) trials, using a simulation study.Individuals with an abnormal amyloid PET scan, diagnosis of mild cognitive impairment or dementia, baseline Mini-Mental State Examination (MMSE) score ≥24, global Clinical Dementia Rating (CDR) score of 0.5, and ≥1 follow-up cognitive assessment were selected from the Alzheimer's Disease Neuroimaging Initiative database (n = 302, age 73 ± 6.7; 44% female; 16.1 ± 2.7 years of education; 69% APOE ε4 carrier). We simulated a clinical trial by randomly assigning individuals to a "placebo" and "treatment" group and subsequently computed group differences on the CDR-sum of boxes (CDR-SB), Alzheimer's Disease Assessment Scale-cognitive subscale-13 and MMSE after 18 months follow-up. We repeated this simulation 10,000 times to determine the 95% range of effect sizes. We further studied the influence of known AD risk factors (age, sex, education, APOE ε4 status, CSF total tau levels) on the variability in effect sizes.Individual trajectories on all cognitive outcomes were highly variable, and the 95% ranges of possible effect sizes at 18 months were broad (e.g., ranging from 0.35 improvement to 0.35 decline on the CDR-SB). Results of recent anti-amyloid trials mostly fell within these 95% ranges of effect sizes. APOE ε4 carriers and individuals with abnormal baseline tau levels showed faster decline at group level, but also greater within-group variability, as illustrated by broader 95% effect size ranges (e.g., ±0.70 points for the CDR-SB).Individuals with early AD show heterogeneity in disease progression, which increases when stratifying on risk factors associated with progression. We provide guidance for a priori effect sizes on cognitive outcomes for detecting true change, which is crucial for future AD trials.

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