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性别、载脂蛋白Eε4(APOE ε4)和触发受体表达于髓样细胞2(TREM2)对内嗅皮质和新皮质区域tau蛋白沉积的可变及交互作用。

Variable and interactive effects of Sex, APOE ε4 and TREM2 on the deposition of tau in entorhinal and neocortical regions.

作者信息

Giorgio Joseph, Jonson Caroline, Wang Yilin, Yokoyama Jennifer S, Wang Jingshen, Jagust William J

机构信息

Department of Neuroscience, University of California Berkeley, Berkeley, CA, 94720, USA.

School of Psychological Sciences, College of Engineering, Science and the Environment, University of Newcastle, Newcastle, NSW, 2308, Australia.

出版信息

Nat Commun. 2025 Jul 1;16(1):5812. doi: 10.1038/s41467-025-60370-8.

Abstract

The canonical Alzheimer's Disease (AD) pathological cascade posits that the accumulation of amyloid beta (Aβ) is the initiating event, accelerating the accumulation of tau in the entorhinal cortex (EC), which subsequently spreads into the neocortex. Here in a multi-cohort study (ADNI, A4, HABS-HD) of 1354 participants with multimodal imaging and genetic information we queried how genetic variation affects these stages of the AD cascade. We observed that females and APOE-ε4 homozygotes are more susceptible to the effects of Aβ on the primary accumulation of tau, with greater EC tau for a given level of Aβ. Furthermore, we observed for individuals who have rare risk variants in TREM2 and/or APOE-ε4 homozygotes there was a greater spread of primary tau from the EC into the neocortex. These findings offer insights into the function of sex, APOE and microglia in AD progression and have implications for determining personalised treatment with drugs targeting Aβ and tau.

摘要

典型的阿尔茨海默病(AD)病理级联反应认为,β淀粉样蛋白(Aβ)的积累是起始事件,加速了内嗅皮质(EC)中tau蛋白的积累,随后tau蛋白扩散到新皮质。在这项针对1354名参与者的多队列研究(ADNI、A4、HABS-HD)中,我们获取了多模态成像和基因信息,以探究基因变异如何影响AD级联反应的这些阶段。我们观察到,女性和APOE-ε4纯合子更容易受到Aβ对tau蛋白初始积累的影响,在给定的Aβ水平下,EC中的tau蛋白含量更高。此外,我们观察到,对于在TREM2中具有罕见风险变异的个体和/或APOE-ε4纯合子,初始tau蛋白从EC扩散到新皮质的程度更大。这些发现为性别、APOE和小胶质细胞在AD进展中的作用提供了见解,并对确定针对Aβ和tau蛋白的个性化药物治疗具有启示意义。

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