整合神经退行性和血管风险的多基因评分可为痴呆风险分层提供信息。
Polygenic score integrating neurodegenerative and vascular risk informs dementia risk stratification.
作者信息
D'Aoust Tim, Clocchiatti-Tuozzo Santiago, Rivier Cyprien A, Mishra Aniket, Hachiya Tsuyoshi, Grenier-Boley Benjamin, Soumaré Aïcha, Duperron Marie-Gabrielle, Le Grand Quentin, Bouteloup Vincent, Proust-Lima Cécile, Samieri Cécilia, Neuffer Jeanne, Sargurupremraj Muralidharan, Chêne Geneviève, Helmer Catherine, Thibault Mura, Amouyel Philippe, Lambert Jean-Charles, Kamatani Yoichiro, Jacqmin-Gadda Hélène, Tregouët David-Alexandre, Inouye Michael, Dufouil Carole, Falcone Guido J, Debette Stéphanie
机构信息
Bordeaux Population Health Center, INSERM, UMR U1219, University of Bordeaux, Bordeaux, France.
Department of Neurology, Yale School of Medicine, New Haven, Connecticut, USA.
出版信息
Alzheimers Dement. 2025 Mar;21(3):e70014. doi: 10.1002/alz.70014.
INTRODUCTION
An integrative polygenic risk score (iPRS) capturing the neurodegenerative and vascular contribution to dementia could identify high-risk individuals and improve risk prediction.
METHODS
We developed an iPRS for dementia (iPRS-DEM) in Europeans (aged 65+), comprising genetic risk for Alzheimer's disease (AD) and 23 vascular or neurodegenerative traits (excluding apolipoprotein E [APOE]). iPRS-DEM was evaluated across cohorts comprising older community-dwelling people (N = 3702), a multi-ancestry biobank (N = 130,797 Europeans; 105,404 non-Europeans), and dementia-free memory clinic participants (N = 2032).
RESULTS
iPRS-DEM was associated with dementia risk independently of APOE in the elderly (subdistribution hazard ratio [sHR]= 1.15, 95% confidence interval [CI]: 1.03 to 1.28), which generalized to Europeans (EUR-sHR= 1.28, 95% CI: 1.09 to 1.51]), East-Asians (EAS-sHR= 5.29, 95% CI: 1.43 to 34.36), and memory-clinic participants (sHR= 1.25, 95% CI: 1.11 to 1.42). Prediction was comparable to clinical risk factors in older community-dwelling people, with improved performance among memory-clinic patients. Risk stratification was enhanced by defining four genetic risk groups with iPRS-DEM and APOE ε4, reaching five-fold increased risk in APOE ε4+/iPRS-DEM+ memory-clinic participants.
DISCUSSION
Alongside APOE ε4, iPRS-DEM may refine risk stratification for the enrichment of dementia clinical trials and prevention programs.
HIGHLIGHTS
iPRS-DEM reflects neurodegenerative and vascular contribution to dementia. We show iPRS-DEM captures additional dementia genetic risk beyond APOE and AD-PRS. iPRS-DEM, in combination with APOE ε4, shows promise for dementia risk stratification. Our results generalize across both population-based and memory-clinic settings. We show transportability of iPRS-DEM to East Asian ancestry.
引言
一个综合多基因风险评分(iPRS)能够捕捉神经退行性和血管因素对痴呆症的影响,从而识别高危个体并改善风险预测。
方法
我们为欧洲65岁及以上人群开发了一种痴呆症的iPRS(iPRS-DEM),它包含阿尔茨海默病(AD)的遗传风险以及23种血管或神经退行性特征(不包括载脂蛋白E [APOE])。iPRS-DEM在多个队列中进行了评估,这些队列包括社区居住的老年人(N = 3702)、一个多血统生物样本库(N = 130797名欧洲人;105404名非欧洲人)以及无痴呆症的记忆门诊参与者(N = 2032)。
结果
在老年人中,iPRS-DEM与痴呆症风险独立相关,不依赖于APOE(亚分布风险比[sHR]= 1.15,95%置信区间[CI]:1.03至1.28),这一结果在欧洲人(EUR-sHR= 1.28,95% CI:1.09至1.51)、东亚人(EAS-sHR= 5.29,95% CI:1.43至34.36)以及记忆门诊参与者(sHR= 1.25,95% CI:1.11至1.42)中均得到验证。在社区居住的老年人中,iPRS-DEM的预测能力与临床风险因素相当,在记忆门诊患者中表现更佳。通过使用iPRS-DEM和APOE ε4定义四个遗传风险组,风险分层得到了加强,在APOE ε4+/iPRS-DEM+的记忆门诊参与者中,风险增加了五倍。
讨论
除了APOE ε4之外,iPRS-DEM可能会优化风险分层,以丰富痴呆症的临床试验和预防项目。
要点
iPRS-DEM反映了神经退行性和血管因素对痴呆症的影响。我们表明,iPRS-DEM捕捉到了除APOE和AD-PRS之外的额外痴呆症遗传风险。iPRS-DEM与APOE ε4相结合,在痴呆症风险分层方面显示出前景。我们的结果在基于人群和记忆门诊的环境中均具有普遍性。我们展示了iPRS-DEM在东亚血统人群中的可转移性。
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