Modifiable dementia risk associated with smaller white matter volume and altered 1/f aperiodic brain activity: cross-sectional insights from the LEISURE study.

IF 6 2区 医学 Q1 GERIATRICS & GERONTOLOGY Age and ageing Pub Date : 2024-11-04 DOI:10.1093/ageing/afae243
Thomas Pace, Jacob M Levenstein, Toomas E Anijärv, Alicia J Campbell, Ciara Treacy, Daniel F Hermens, Sophie C Andrews
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Abstract

Background: The rising prevalence of dementia necessitates identifying early neurobiological markers of dementia risk. Reduced cerebral white matter volume and flattening of the slope of the electrophysiological 1/f spectral power distribution provide neurobiological markers of brain ageing alongside cognitive decline. However, their association with modifiable dementia risk remains to be understood.

Methods: A cross-sectional sample of 98 healthy older adults (79 females, mean age = 65.44) underwent structural magnetic resonance imaging (sMRI), resting-state electroencephalography (EEG), cognitive assessments and dementia risk scoring using the CogDrisk framework. Univariate and multivariate linear regression models were conducted to investigate the relationships between modifiable dementia risk and sMRI brain volumes, the exponent of EEG 1/f spectral power, and cognition, whilst controlling for non-modifiable factors.

Results: Smaller global white matter volume (F(1,87) = 6.884, R2 = 0.073, P = .010), and not grey (F(1,87) = 0.540, R2 = 0.006, P = .468) or ventricle volume (F(1,87) = 0.087, R2 = 0.001, P = .769), was associated with higher modifiable dementia risk. A lower exponent, reflecting a flatter 1/f spectral power distribution, was associated with higher dementia risk at frontal (F(1,92) = 4.096, R2 = 0.043, P = .046) but not temporal regions. No significant associations were found between cognitive performance and dementia risk. In multivariate analyses, both white matter volume and the exponent of the 1/f spectral power distribution independently associated with dementia risk.

Conclusions: Structural and functional neurobiological markers of early brain ageing, but not cognitive function, are independently associated with modifiable dementia risk in healthy older adults.

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可改变的痴呆症风险与较小的白质体积和改变的 1/f 非周期性大脑活动有关:LEISURE 研究的横断面见解。
背景:随着痴呆症发病率的上升,有必要确定痴呆症风险的早期神经生物学标志物。脑白质体积缩小和电生理 1/f 频谱功率分布斜率变平提供了伴随认知能力下降的大脑老化的神经生物学标志。然而,它们与可改变的痴呆症风险之间的关系仍有待了解:98名健康老年人(79名女性,平均年龄=65.44岁)接受了结构性磁共振成像(sMRI)、静息态脑电图(EEG)、认知评估,并使用CogDrisk框架进行了痴呆风险评分。通过单变量和多变量线性回归模型研究了可改变的痴呆风险与sMRI脑容量、脑电图1/f频谱功率指数和认知能力之间的关系,同时控制了不可改变的因素:全球白质体积较小(F(1,87) = 6.884, R2 = 0.073, P = .010),而灰质体积(F(1,87) = 0.540, R2 = 0.006, P = .468)或脑室体积(F(1,87) = 0.087, R2 = 0.001, P = .769)较小,则与较高的可改变痴呆风险无关。指数越低,反映出 1/f 频谱功率分布越平坦,与额叶(F(1,92) = 4.096,R2 = 0.043,P = .046)痴呆风险越高有关,但与颞叶区域无关。认知能力与痴呆症风险之间没有发现明显的关联。在多变量分析中,白质体积和1/f频谱功率分布指数都与痴呆症风险有独立关联:结论:在健康的老年人中,大脑早期老化的结构性和功能性神经生物学标志物(而非认知功能)与可改变的痴呆症风险有独立的关联。
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来源期刊
Age and ageing
Age and ageing 医学-老年医学
CiteScore
9.20
自引率
6.00%
发文量
796
审稿时长
4-8 weeks
期刊介绍: Age and Ageing is an international journal publishing refereed original articles and commissioned reviews on geriatric medicine and gerontology. Its range includes research on ageing and clinical, epidemiological, and psychological aspects of later life.
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