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神经认知障碍诊断前主观认知能力下降的不同轨迹:18年纵向建模

Distinct trajectories of subjective cognitive decline before diagnosis of neurocognitive disorders: Longitudinal modelling over 18 years.

作者信息

Liew Tau Ming

机构信息

Department of Psychiatry, Singapore General Hospital, Singapore; SingHealth Duke-NUS Medicine Academic Clinical Programme, Duke-NUS Medical School, Singapore; Health Services and Systems Research, Duke-NUS Medical School, Singapore; Saw Swee Hock School of Public Health, National University of Singapore, Singapore.

出版信息

J Prev Alzheimers Dis. 2025 May;12(5):100123. doi: 10.1016/j.tjpad.2025.100123. Epub 2025 Mar 8.

Abstract

BACKGROUND

Subjective cognitive decline (SCD) is an established predictor of neurocognitive disorders (NCD) (i.e. mild cognitive impairment and dementia). Yet, its construct remains contentious. Many individuals with SCD do not progress to NCD, leading to an alternative term in the literature - 'functional cognitive disorders' - to describe the SCD experience in these individuals.

OBJECTIVES

To examine the distinct differences in trajectories of SCD between those who did and did not eventually develop NCD.

DESIGN

Case-control study.

SETTING

Alzheimer's Disease Centers across USA.

PARTICIPANTS

A total of 5,167 participants aged ≥50 years were followed up near-annually to evaluate for SCD and NCD (median follow-up=8.1 years; range=1.0-18.0). Cases were defined as those who developed incident NCD during follow-up; controls completed ≥10 years of follow-up and had normal cognition throughout follow-up period.

MEASUREMENTS

SCD was evaluated with a yes/no question based on "perceived decline in memory relative to previously attained abilities". The trajectories of SCD were modelled with mixed-effect logistic regression, using a backward timescale.

RESULTS

Those who developed NCD (cases) had new onset of SCD within past 20 years, which became particularly noticeable 13-14 years before diagnosis, and became even more evident in the last 4 years. Those who did not develop NCD (controls) reported SCD since younger age, with the probability of SCD remaining constant over time. The distinctive trajectories were consistent across Alzheimer's and non-Alzheimer's disease, and among those with higher baseline rates of SCD due to psychiatric conditions.

CONCLUSIONS

SCD exhibits distinctive trajectories among those who do and do not progress to NCD. These distinctive trajectories can inform NCD risk for early interventions, and guide public health messaging to distinguish high-risk SCD from normal ageing. Future SCD scales may possibly need to evaluate symptom changes over a longer, 20-year horizon to better capture the new onset of SCD within this longer timeframe.

摘要

背景

主观认知下降(SCD)是神经认知障碍(NCD,即轻度认知障碍和痴呆)的既定预测指标。然而,其概念仍存在争议。许多患有SCD的个体并未发展为NCD,这导致文献中出现了另一个术语——“功能性认知障碍”,用于描述这些个体的SCD经历。

目的

研究最终发展为NCD和未发展为NCD的个体在SCD轨迹上的明显差异。

设计

病例对照研究。

设置

美国各地的阿尔茨海默病中心。

参与者

共有5167名年龄≥50岁的参与者接受了近年度随访,以评估SCD和NCD(中位随访时间 = 8.1年;范围 = 1.0 - 18.0年)。病例定义为随访期间发生新发NCD的个体;对照完成了≥10年的随访且在整个随访期间认知正常。

测量

基于“相对于先前获得的能力,感觉记忆力下降”的是/否问题评估SCD。使用向后时间尺度,通过混合效应逻辑回归对SCD轨迹进行建模。

结果

发展为NCD的个体(病例)在过去20年内出现新发SCD,在诊断前13 - 14年变得尤为明显,在最后4年更加显著。未发展为NCD的个体(对照)自年轻时就报告有SCD,且SCD发生的概率随时间保持不变。这些独特的轨迹在阿尔茨海默病和非阿尔茨海默病患者中一致,在因精神疾病导致SCD基线发生率较高的个体中也一致。

结论

SCD在发展为NCD和未发展为NCD的个体中表现出独特的轨迹。这些独特的轨迹可为早期干预的NCD风险提供信息,并指导公共卫生信息传递,以区分高风险SCD与正常衰老。未来的SCD量表可能需要在更长的20年时间范围内评估症状变化,以便在这个更长的时间框架内更好地捕捉SCD的新发情况。

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