Accelerated long-term forgetting: A sensitive paradigm for detecting subtle cognitive impairment and evaluating BACE1 inhibitor efficacy in preclinical Alzheimer's disease

M. Ohno
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Abstract

Given a long preclinical stage of Alzheimer's disease (AD) continuum before the onset of dementia, there is a growing demand for tools capable of detecting the earliest feature of subtle cognitive impairment and optimizing recruitment to clinical trials for potentially disease-modifying therapeutic interventions such as BACE1 inhibitors. Now that all BACE1 inhibitor programs in symptomatic and prodromal AD populations have ended in failure, trials need to shift to target the earlier preclinical stage. However, evaluating cognitive efficacy (if any) in asymptomatic AD individuals is a great challenge. In this context, accelerated long-term forgetting (ALF) is emerging as a sensitive cognitive measure that can discriminate between presymptomatic individuals with high risks for developing AD and healthy controls. ALF is characterized by increased forgetting rates over extended delays (e.g., days, weeks, months) despite normal learning and short-term retention on standard memory assessments that typically use around 30-min delays. This review provides an overview of recent progress in animal model and clinical studies on this topic, focusing on the utility and underlying mechanism of ALF that may be applicable to earlier diagnosis and BACE1 inhibitor efficacy evaluation at a preclinical stage of AD.
加速长期遗忘:在临床前阿尔茨海默病中检测细微认知障碍和评估BACE1抑制剂疗效的敏感范例
鉴于阿尔茨海默病(AD)在痴呆发病前的临床前阶段持续时间较长,因此对能够检测细微认知障碍早期特征的工具的需求不断增长,并优化临床试验中潜在疾病改善治疗干预措施(如BACE1抑制剂)的招募。现在,在症状性和前驱性AD人群中,所有BACE1抑制剂项目都以失败告终,试验需要转向针对更早的临床前阶段。然而,评估无症状AD个体的认知疗效(如果有的话)是一个巨大的挑战。在这种背景下,加速长期遗忘(ALF)正成为一种敏感的认知测量方法,可以区分阿尔茨海默病高风险的症状前个体和健康对照者。ALF的特点是遗忘率在延长的延迟(例如,几天,几周,几个月)中增加,尽管在标准记忆评估中正常的学习和短期保留通常使用大约30分钟的延迟。本文综述了近年来关于该主题的动物模型和临床研究进展,重点介绍了ALF在阿尔茨海默病临床前早期诊断和BACE1抑制剂疗效评估中的应用及其潜在机制。
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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