跨种族分析确定了对阿尔茨海默病具有保护作用的SORL1基因变异和单倍型。
Transethnic analysis identifies SORL1 variants and haplotypes protective against Alzheimer's disease.
作者信息
Zhou Xiaopu, Cao Han, Jiang Yuanbing, Chen Yuewen, Zhong Huan, Fu Wing Yu, Lo Ronnie Ming Nok, Wong Bonnie Wing Yan, Cheng Elaine Yee Ling, Mok Kin Ying, Kwok Timothy C Y, Mok Vincent C T, Ip Fanny C F, Miyashita Akinori, Hara Norikazu, Ikeuchi Takeshi, Hardy John, Chen Yu, Fu Amy K Y, Ip Nancy Y
机构信息
Division of Life Science, State Key Laboratory of Molecular Neuroscience, Molecular Neuroscience Center, The Hong Kong University of Science and Technology, Hong Kong, China.
Hong Kong Center for Neurodegenerative Diseases, Hong Kong, China.
出版信息
Alzheimers Dement. 2025 Jan;21(1):e14214. doi: 10.1002/alz.14214. Epub 2024 Dec 10.
INTRODUCTION
The SORL1 locus exhibits protective effects against Alzheimer's disease (AD) across ancestries, yet systematic studies in diverse populations are sparse.
METHODS
Logistic regression identified AD-associated SORL1 haplotypes in East Asian (N = 5249) and European (N = 8588) populations. Association analysis between SORL1 haplotypes and AD-associated traits or plasma biomarkers was conducted. The effects of non-synonymous mutations were assessed in cell-based systems.
RESULTS
Protective SORL1 variants/haplotypes were identified in the East Asian and European populations. Haplotype Hap_A showed a strong protective effect against AD in East Asians, linked to less severe AD phenotypes, higher SORL1 transcript levels, and plasma proteomic changes. A missense variant within Hap_A, rs2282647-C allele, was linked to a lower risk of AD and decreased expression of a truncated SORL1 protein isoform.
DISCUSSION
Our transethnic analysis revealed key SORL1 haplotypes that exert protective effects against AD, suggesting mechanisms of the protective role of SORL1 in AD.
HIGHLIGHTS
We examined the AD-protective mechanisms of SORL1 in the general population across diverse ancestral backgrounds by jointly analyzing data from three East Asian cohorts (ie, mainland China, Hong Kong, and Japan) and a European cohort. Comparative analysis unveiled key ethnic-specific SORL1 genetic variants and haplotypes. Among these, the SORL1 minor haplotype, Hap_A, emerged as the primary AD-protective factor in East Asians. Hap_A exerts significant AD-protective effects in both APOE ε4 carriers and non-carriers. SORL1 haplotype Hap_A is associated with cognitive function, brain volume, and the activity of specific neuronal and immune-related pathways closely connected to AD risk. Protective variants within Hap_A are linked to increased SORL1 expression in human tissues. We identified an isoform-specific missense variant in Hap_A that modifies the function and levels of a truncated SORL1 protein isoform that is poorly investigated.
引言
SORL1基因座在不同种族中均对阿尔茨海默病(AD)具有保护作用,但针对不同人群的系统性研究较少。
方法
采用逻辑回归在东亚人群(N = 5249)和欧洲人群(N = 8588)中确定与AD相关的SORL1单倍型。对SORL1单倍型与AD相关性状或血浆生物标志物进行关联分析。在基于细胞的系统中评估非同义突变的影响。
结果
在东亚和欧洲人群中鉴定出具有保护作用的SORL1变异体/单倍型。单倍型Hap_A在东亚人群中对AD具有强大的保护作用,与较轻的AD表型、较高的SORL1转录水平和血浆蛋白质组变化相关。Hap_A内的一个错义变异体rs2282647 - C等位基因与较低的AD风险和截短的SORL1蛋白异构体表达降低有关。
讨论
我们的跨种族分析揭示了对AD具有保护作用的关键SORL1单倍型,提示了SORL1在AD中发挥保护作用的机制。
重点
我们通过联合分析来自三个东亚队列(即中国大陆、香港和日本)和一个欧洲队列的数据,研究了SORL1在不同祖先背景的普通人群中的AD保护机制。比较分析揭示了关键的种族特异性SORL1基因变异体和单倍型。其中,SORL1小单倍型Hap_A成为东亚人群中主要的AD保护因子。Hap_A在APOE ε4携带者和非携带者中均发挥显著的AD保护作用。SORL1单倍型Hap_A与认知功能、脑容量以及与AD风险密切相关的特定神经元和免疫相关途径的活性有关。Hap_A内的保护性变异体与人体组织中SORL1表达增加有关。我们在Hap_A中鉴定出一个异构体特异性错义变异体,该变异体改变了研究较少的截短的SORL1蛋白异构体的功能和水平。
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