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百岁老人的β-淀粉样蛋白病理学与认知表现

Amyloid-Beta Pathology and Cognitive Performance in Centenarians.

作者信息

Rohde Susan K, Luimes Maruelle C, Lorenz Linda M C, Fierro-Hernández Patricia, Rozemuller Annemieke J M, Hulsman Marc, Zhang Meng, Graat Marieke J I, van der Hoorn Myke E, Daatselaar Dominique A H, Scheltens Philip, Richardson Timothy E, Walker Jamie M, Sikkes Sietske A M, Hoozemans Jeroen J M, Holstege Henne

机构信息

Department of Human Genetics, Genomics of Neurodegenerative Diseases and Aging, Vrije Universiteit Amsterdam, Amsterdam, the Netherlands.

Department of Neurology and Alzheimer Center Amsterdam, Amsterdam UMC location VUmc, Amsterdam, the Netherlands.

出版信息

JAMA Neurol. 2025 Jun 30. doi: 10.1001/jamaneurol.2025.1734.

Abstract

IMPORTANCE

Older individuals without dementia often have amyloid-beta (Aβ) Thal phases similar to patients with Alzheimer disease (AD), suggesting that Aβ pathology may be a benign consequence of aging.

OBJECTIVE

To explore whether Aβ pathology in centenarians is associated with cognitive performance.

DESIGN, SETTING, AND PARTICIPANTS: This longitudinal cohort study used cross-sectional data on antemortem cognitive performance and postmortem neuropathology of participants in the Dutch 100-plus Study. Cognitive performance was measured a median of 10 (IQR, 3-13) months before postmortem brain donation. From January 2013 to July 2022, 1187 centenarians who self-reported being cognitively healthy, confirmed by proxy, were approached: 406 were included and 95 donated their brain. Centenarians were compared with patients with clinicopathologically confirmed AD from the Netherlands Brain Bank. Data were analyzed from June 2022 to October 2024.

MAIN OUTCOMES AND MEASURES

Aβ pathology was assessed with the Thal phase for Aβ progression and by determining quantitative Aβ loads (percentage positive area) in the frontal, parietal, temporal, and occipital neocortices, 3 parahippocampal, and 5 hippocampal subregions. Aβ pathology was associated with performance on 13 neuropsychological tests assessing memory, fluency, attention/processing speed, and executive functioning, as well as 4 measures of global cognition.

RESULTS

This study evaluated Aβ pathology in 95 centenarians (median age at brain donation, 103.5 [IQR, 102.3-104.7] years; 71 female [75%] and 24 male [25%]) and 38 patients with AD (median age, 84 [IQR, 78-90] years; 18 female [47%] and 20 male [53%]). Global cognition parameters were available for all 95 centenarians and complete cognitive assessment for 72 centenarians (76%). A fraction of the centenarians had no Aβ load (9 of 95 [9%]), most had low Aβ load (53 of 95 [56%]) and, despite high Thal phases, about one-third (33 of 95 [35%]) had high Aβ load comparable with patients with AD. Centenarians with no or low Aβ load had significantly higher cognitive performance than centenarians with high Aβ loads. Higher Aβ loads across all 4 neocortical regions, cornu ammonis 3, cornu ammonis 1/subiculum, and the entorhinal cortex specifically affected executive functioning. Interestingly, 5 resilient centenarians maintained high cognitive performance despite having high Aβ loads; they had significantly less tau pathology compared with centenarians with high Aβ loads and low cognitive performance.

CONCLUSIONS AND RELEVANCE

These results indicate that Aβ pathology is not a benign consequence of aging. Even in the oldest individuals, Aβ and tau pathology interaction was consistent with the amyloid cascade hypothesis.

摘要

重要性

无痴呆症的老年人通常具有与阿尔茨海默病(AD)患者相似的淀粉样蛋白β(Aβ)分期,这表明Aβ病理可能是衰老的良性后果。

目的

探讨百岁老人的Aβ病理与认知表现是否相关。

设计、背景和参与者:这项纵向队列研究使用了荷兰百岁老人研究中参与者生前认知表现和死后神经病理学的横断面数据。认知表现是在死后大脑捐赠前中位数为10(四分位间距,3 - 13)个月时测量的。从2013年1月至2022年7月,对1187名自我报告认知健康且经代理人确认的百岁老人进行了随访:406人被纳入,95人捐赠了大脑。将百岁老人与荷兰脑库中经临床病理确诊的AD患者进行比较。数据于2022年6月至2024年10月进行分析。

主要结局和指标

通过Aβ进展的Thal分期以及测定额叶、顶叶、颞叶和枕叶新皮质、3个海马旁回和5个海马亚区域的定量Aβ负荷(阳性面积百分比)来评估Aβ病理。Aβ病理与13项评估记忆、流畅性、注意力/处理速度和执行功能的神经心理学测试表现以及4项整体认知指标相关。

结果

本研究评估了95名百岁老人(大脑捐赠时的中位年龄为103.5[四分位间距,102.3 - 104.7]岁;71名女性[75%]和24名男性[25%])和38名AD患者(中位年龄,84[四分位间距,78 - 90]岁;18名女性[47%]和20名男性[53%])的Aβ病理。所有95名百岁老人均有整体认知参数,72名百岁老人(76%)进行了完整的认知评估。一部分百岁老人没有Aβ负荷(95人中的9人[9%]),大多数有低Aβ负荷(95人中的53人[56%]),尽管Thal分期较高,但约三分之一(95人中的33人[35%])的高Aβ负荷与AD患者相当。无或低Aβ负荷的百岁老人的认知表现显著高于高Aβ负荷的百岁老人。所有4个新皮质区域、海马角3、海马角1/下托以及内嗅皮质中较高的Aβ负荷特别影响执行功能。有趣的是,5名有弹性的百岁老人尽管有高Aβ负荷但仍保持高认知表现;与高Aβ负荷和低认知表现的百岁老人相比,他们的tau病理明显更少。

结论和意义

这些结果表明Aβ病理不是衰老的良性后果。即使在最年长的个体中,Aβ和tau病理的相互作用也与淀粉样蛋白级联假说一致。

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