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首页> 外文期刊>Alzheimer’s & dementia: the journal of the Alzheimer’s Association >Brain size and the compensation of Alzheimer's disease symptoms: A longitudinal cohort study
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Brain size and the compensation of Alzheimer's disease symptoms: A longitudinal cohort study

机译:脑规模和阿尔茨海默氏病症状的补偿:一项纵向队列研究

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摘要

Background: Greater intracranial volume (ICV) has been associated with less severe Alzheimer's disease (AD) symptoms at a given level of cerebral pathology. In this study we examine whether ICV modulates the association between clinical disease progression on the one hand and brain atrophy or the apolipoprotein E genotype on the other. Methods: Six hundred seventy-four subjects were studied from the AD Neuroimaging Initiative (ADNI). Subjects included 204 controls, 144 patients with AD dementia, and 326 with amnestic mild cognitive impairment (aMCI). Longitudinal analyses were conducted applying generalized estimating equations to examine the influence of ICV on clinical deterioration and atrophy progression. Follow-up data were available for up to 60 months after the baseline visit (mean 31.42 months, SD 13.12 months). Results: ICV was not directly associated with clinical worsening or atrophy progression. However, ICV attenuated the impact of atrophy and the apolipoprotein E ε4 allele on clinical disease progression in aMCI. Conclusion: Greater ICV, that is, premorbid brain size, seems to protect against clinical deterioration in the face of AD-related brain atrophy in aMCI. The results support the theory of a compensatory role of brain reserve in contrast to a neuroprotective role. The protective effects of morphologic reserve seem to be limited to early clinical AD; once a certain threshold of neurodegenerative burden is passed, a larger premorbid brain no longer offers an advantage in this context.
机译:背景:在给定的脑部病理学水平下,颅内容积(ICV)增大与较轻的阿尔茨海默氏病(AD)症状相关。在这项研究中,我们检查了ICV一方面调节临床疾病进展与另一方面脑萎缩或载脂蛋白E基因型之间的关联。方法:从AD Neuroimaging Initiative(ADNI)研究了674名受试者。受试者包括204名对照,144名AD痴呆患者和326名轻度轻度认知障碍(aMCI)。应用广义估计方程进行纵向分析,以检查ICV对临床恶化和萎缩进展的影响。基线访视后长达60个月的随访数据(平均31.42个月,SD 13.12个月)。结果:ICV与临床恶化或萎缩没有直接关系。但是,ICV减弱了aMCI中萎缩和载脂蛋白Eε4等位基因对临床疾病进展的影响。结论:面对aMCI中与AD相关的脑萎缩,更大的ICV(即病前大脑的大小)似乎可以防止临床恶化。结果支持与神经保护作用相反的大脑储备的补偿作用的理论。形态学储备的保护作用似乎仅限于早期临床AD。一旦超过一定程度的神经退行性负担,在这种情况下,更大的病前大脑将不再具有优势。

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