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利用神经心理学过程评分识别细微认知下降并预测向轻度认知障碍的进展。

Using Neuropsychological Process Scores to Identify Subtle Cognitive Decline and Predict Progression to Mild Cognitive Impairment.

机构信息

Veteran Affairs San Diego Healthcare System, San Diego, CA, USA.

Department of Psychiatry, University of California, San Diego, School of Medicine, La Jolla, CA, USA.

出版信息

J Alzheimers Dis. 2018;64(1):195-204. doi: 10.3233/JAD-180229.

Abstract

BACKGROUND

We previously operationally-defined subtle cognitive decline (SCD) in preclinical Alzheimer's disease (AD) using total scores on neuropsychological (NP) tests. NP process scores (i.e., provide information about how a total NP score was achieved) may be a useful tool for identifying early cognitive inefficiencies prior to objective impairment seen in mild cognitive impairment (MCI) and dementia.

OBJECTIVE

We aimed to integrate process scores into the SCD definition to identify stages of SCD and improve early detection of those at risk for decline.

METHODS

Cognitively "normal" participants from the Alzheimer's Disease Neuroimaging Initiative were classified as "early" SCD (E-SCD; >1 SD below norm-adjusted mean on 2 process scores or on 1 process score plus 1 NP total score), "late" SCD (L-SCD; existing SCD criteria of >1 SD below norm-adjusted mean on 2 NP total scores in different domains), or "no SCD" (NC). Process scores considered in the SCD criteria were word-list intrusion errors, retroactive interference, and learning slope. Cerebrospinal fluid AD biomarkers were used to examine pathologic burden across groups.

RESULTS

E-SCD and L-SCD progressed to MCI 2.5-3.4 times faster than the NC group. Survival curves for E-SCD and L-SCD converged at 7-8 years after baseline. The combined (E-SCD+L-SCD) group had improved sensitivity to detect progression to MCI relative to L-SCD only. AD biomarker positivity increased across NC, SCD, and MCI groups.

CONCLUSIONS

Process scores can be integrated into the SCD criteria to allow for increased sensitivity and earlier identification of cognitively normal older adults at risk for decline prior to frank impairment on NP total scores.

摘要

背景

我们之前使用神经心理学 (NP) 测试的总分来操作定义临床前阿尔茨海默病 (AD) 中的轻微认知衰退 (SCD)。NP 过程分数(即提供有关如何实现总 NP 分数的信息)可能是在轻度认知障碍 (MCI) 和痴呆症中看到的客观损伤之前识别早期认知效率低下的有用工具。

目的

我们旨在将过程分数纳入 SCD 定义中,以确定 SCD 的阶段,并提高对有衰退风险的人的早期检测。

方法

来自阿尔茨海默病神经影像学倡议的认知“正常”参与者被分类为“早期”SCD(E-SCD;在 2 个过程分数或 1 个过程分数加 1 个 NP 总分上的 2 个 NP 总分的正常调整平均值的 1 个标准偏差以下),“晚期”SCD(L-SCD;在不同领域的 2 个 NP 总分上存在 1 个标准偏差以下的现有 SCD 标准)或“无 SCD”(NC)。在 SCD 标准中考虑的过程分数是单词列表侵入错误、逆行干扰和学习斜率。脑脊液 AD 生物标志物用于检查各组的病理负担。

结果

E-SCD 和 L-SCD 进展为 MCI 的速度比 NC 组快 2.5-3.4 倍。E-SCD 和 L-SCD 的生存曲线在基线后 7-8 年收敛。与仅 L-SCD 相比,组合(E-SCD+L-SCD)组提高了检测向 MCI 进展的敏感性。AD 生物标志物阳性率在 NC、SCD 和 MCI 组中增加。

结论

可以将过程分数纳入 SCD 标准,以提高敏感性并更早识别在 NP 总分明显受损之前有认知能力下降风险的认知正常老年人。

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