Integrative brain omics approach reveals key role for sn-1 lysophosphatidylethanolamine in Alzheimer's dementia

Author:

Ortlund Eric1ORCID,Chen Chih-Yu2,Maner-Smith Kristal1ORCID,Khadka Manoj2,Ahn Jun2,Gulbin Xueyun3,Ivanova Anna2,Dammer Eric4ORCID,Seyfried Nicholas1ORCID,Bennett David5,Hajjar Ihab6

Affiliation:

1. Emory University School of Medicine

2. Emory integrated metabolomics and lipidomics core

3. Emory University,

4. Emory University

5. Rush University Medical Center

6. University of Texas Southwestern

Abstract

Abstract The biology of individual lipid species and their relevance in Alzheimer’s disease (AD) remains incompletely understood. We utilized non-targeted mass spectrometry to examine brain lipids variations across 316 post-mortem brains from participants in the Religious Orders Study (ROS) or Rush Memory and Aging Project (MAP) cohorts classified as either control, asymptomatic AD (AAD), or symptomatic AD (SAD) and integrated the lipidomics data with untargeted proteomic characterization on the same individuals. Lipid enrichment analysis and analysis of variance identified significantly lower abundance of lysophosphatidylethanolamine (LPE) and lysophosphatidylcholine (LPC) species in SAD than controls or AAD. Lipid-protein co-expression network analyses revealed that lipid modules consisting of LPE and LPC exhibited a significant association to protein modules associated with MAPK/metabolism, post-synaptic density, and Cell-ECM interaction pathways and were associated with better antemortem cognition and with neuropathological changes seen in AD. Particularly, LPE 22:6 [sn-1] levels are significantly decreased across AD cases (SAD) and show the most influence on protein changes compared to other lysophospholipid species. LPE 22:6 may be a lipid signature for AD and could be leveraged as potential therapeutic or dietary targets for AD.

Publisher

Research Square Platform LLC

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