Brain Cell-based Genetic Subtyping and Drug Repositioning for Alzheimer Disease

Author:

Sahelijo Nathan,Rajagopalan Priya,Qian Lu,Rahman Rufuto,Priyadarshi Dhawal,Goldstein Daniel,Thomopoulos Sophia I.ORCID,Bennett David A.,Farrer Lindsay A.,Stein Thor D., ,Shen Li,Huang Heng,Nho Kwangsik,Andrew Saykin J.ORCID,Davatzikos Christos,Thompson Paul M.,TCW Julia,Jun Gyungah R.

Abstract

AbstractAlzheimer’s Disease (AD) is characterized by its complex and heterogeneous etiology and gradual progression, leading to high drug failure rates in late-stage clinical trials. In order to better stratify individuals at risk for AD and discern potential therapeutic targets we employed a novel procedure utilizing cell-based co-regulated gene networks and polygenic risk scores (cbPRSs). After defining genetic subtypes using extremes of cbPRS distributions, we evaluated correlations of the genetic subtypes with previously defined AD subtypes defined on the basis of domain-specific cognitive functioning and neuroimaging biomarkers. Employing a PageRank algorithm, we identified priority gene targets for the genetic subtypes. Pathway analysis of priority genes demonstrated associations with neurodegeneration and suggested candidate drugs currently utilized in diabetes, hypertension, and epilepsy for repositioning in AD. Experimental validation utilizing human induced pluripotent stem cell (hiPSC)-derived astrocytes demonstrated the modifying effects of estradiol, levetiracetam, and pioglitazone on expression ofAPOEand complementC4genes, suggesting potential repositioning for AD.

Publisher

Cold Spring Harbor Laboratory

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