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Genetic and clinical correlates of two neuroanatomical AI dimensions in the Alzheimer’s disease continuum

Authors :
Junhao Wen
Zhijian Yang
Ilya M. Nasrallah
Yuhan Cui
Guray Erus
Dhivya Srinivasan
Ahmed Abdulkadir
Elizabeth Mamourian
Gyujoon Hwang
Ashish Singh
Mark Bergman
Jingxuan Bao
Erdem Varol
Zhen Zhou
Aleix Boquet-Pujadas
Jiong Chen
Arthur W. Toga
Andrew J. Saykin
Timothy J. Hohman
Paul M. Thompson
Sylvia Villeneuve
Randy Gollub
Aristeidis Sotiras
Katharina Wittfeld
Hans J. Grabe
Duygu Tosun
Murat Bilgel
Yang An
Daniel S. Marcus
Pamela LaMontagne
Tammie L. Benzinger
Susan R. Heckbert
Thomas R. Austin
Lenore J. Launer
Mark Espeland
Colin L. Masters
Paul Maruff
Jurgen Fripp
Sterling C. Johnson
John C. Morris
Marilyn S. Albert
R. Nick Bryan
Susan M. Resnick
Luigi Ferrucci
Yong Fan
Mohamad Habes
David Wolk
Li Shen
Haochang Shou
Christos Davatzikos
Source :
Translational Psychiatry, Vol 14, Iss 1, Pp 1-14 (2024)
Publication Year :
2024
Publisher :
Nature Publishing Group, 2024.

Abstract

Abstract Alzheimer’s disease (AD) is associated with heterogeneous atrophy patterns. We employed a semi-supervised representation learning technique known as Surreal-GAN, through which we identified two latent dimensional representations of brain atrophy in symptomatic mild cognitive impairment (MCI) and AD patients: the “diffuse-AD” (R1) dimension shows widespread brain atrophy, and the “MTL-AD” (R2) dimension displays focal medial temporal lobe (MTL) atrophy. Critically, only R2 was associated with widely known sporadic AD genetic risk factors (e.g., APOE ε4) in MCI and AD patients at baseline. We then independently detected the presence of the two dimensions in the early stages by deploying the trained model in the general population and two cognitively unimpaired cohorts of asymptomatic participants. In the general population, genome-wide association studies found 77 genes unrelated to APOE differentially associated with R1 and R2. Functional analyses revealed that these genes were overrepresented in differentially expressed gene sets in organs beyond the brain (R1 and R2), including the heart (R1) and the pituitary gland, muscle, and kidney (R2). These genes were enriched in biological pathways implicated in dendritic cells (R2), macrophage functions (R1), and cancer (R1 and R2). Several of them were “druggable genes” for cancer (R1), inflammation (R1), cardiovascular diseases (R1), and diseases of the nervous system (R2). The longitudinal progression showed that APOE ε4, amyloid, and tau were associated with R2 at early asymptomatic stages, but this longitudinal association occurs only at late symptomatic stages in R1. Our findings deepen our understanding of the multifaceted pathogenesis of AD beyond the brain. In early asymptomatic stages, the two dimensions are associated with diverse pathological mechanisms, including cardiovascular diseases, inflammation, and hormonal dysfunction—driven by genes different from APOE—which may collectively contribute to the early pathogenesis of AD. All results are publicly available at https://labs-laboratory.com/medicine/ .

Details

Language :
English
ISSN :
21583188
Volume :
14
Issue :
1
Database :
Directory of Open Access Journals
Journal :
Translational Psychiatry
Publication Type :
Academic Journal
Accession number :
edsdoj.56d631e8319148739bce0f8e8b35d005
Document Type :
article
Full Text :
https://doi.org/10.1038/s41398-024-03121-5