Concordant peripheral lipidome signatures in two large clinical studies of Alzheimer’s disease

Author:

Huynh KevinORCID,Lim Wei Ling FlorenceORCID,Giles Corey,Jayawardana Kaushala S.,Salim Agus,Mellett Natalie A.,Smith Adam Alexander T.,Olshansky Gavriel,Drew Brian G.,Chatterjee PratishthaORCID,Martins IanORCID,Laws Simon M.ORCID,Bush Ashley I.ORCID,Rowe Christopher C.,Villemagne Victor L.,Ames David,Masters Colin L.,Arnold MatthiasORCID,Nho Kwangsik,Saykin Andrew J.ORCID,Baillie RebeccaORCID,Han XianlinORCID,Kaddurah-Daouk RimaORCID,Martins Ralph N.,Meikle Peter J.ORCID

Abstract

Abstract Changes to lipid metabolism are tightly associated with the onset and pathology of Alzheimer’s disease (AD). Lipids are complex molecules comprising many isomeric and isobaric species, necessitating detailed analysis to enable interpretation of biological significance. Our expanded targeted lipidomics platform (569 species across 32 classes) allows for detailed lipid separation and characterisation. In this study we examined peripheral samples of two cohorts (AIBL, n = 1112 and ADNI, n = 800). We are able to identify concordant peripheral signatures associated with prevalent AD arising from lipid pathways including; ether lipids, sphingolipids (notably GM3 gangliosides) and lipid classes previously associated with cardiometabolic disease (phosphatidylethanolamine and triglycerides). We subsequently identified similar lipid signatures in both cohorts with future disease. Lastly, we developed multivariate lipid models that improved classification and prediction. Our results provide a holistic view between the lipidome and AD using a comprehensive approach, providing targets for further mechanistic investigation.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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