Comparative Lipidomic Analysis of Mouse and Human Brain with Alzheimer Disease

Robin B. Chan; Tiago G. Oliveira; Etty P. Cortes; Lawrence S. Honig; Karen E. Duff; Scott A. Small; Markus R. Wenk; Guanghou Shui; Gilbert Di Paolo

doi:10.1074/jbc.M111.274142

Comparative Lipidomic Analysis of Mouse and Human Brain with Alzheimer Disease*

From the Departments of ^‡Pathology and Cell Biology and
^**Neurology,
^§Taub Institute for Research on Alzheimer's Disease and the Aging Brain, Columbia University Medical Center, New York, New York 10032,
the ^¶Life and Health Science Research Institute (ICVS), School of Health Sciences,
the ^‖Life and Health Science Research Institute/3B's (Biomaterials, Biodegradables and Biomimetics), Portuguese Government Associate Laboratory, University of Minho, 4710-057 Braga, Portugal,
the ^‡‡Department of Biochemistry, National University of Singapore, Singapore 117597, and
the ^§§Department of Biological Sciences, National University of Singapore, Singapore 117543

↵1 To whom correspondence may be addressed: Centre for Life Sciences, 28 Medical Dr., 04-21 Singapore 117456. Tel.: 65-6516-6683; E-mail: guanghou_shui{at}nuhs.edu.sg.
↵2 To whom correspondence may be addressed: 630 West 168th St., P&S 12–510, New York, NY 10032. Tel.: 212-304-5500; E-mail: gil.dipaolo{at}columbia.edu.

Background: Lipid dyshomeostasis has been linked to Alzheimer disease (AD).

Results: Lipidomic analyses of brain tissue from AD patients reveal region-specific changes in multiple bioactive lipids, some of which are phenocopied in AD mouse models.

Conclusion: Lipid anomalies observed in AD may be linked to pathogenesis, including endolysosomal dysfunction.

Significance: This study highlights the hypothesis-generating potential of lipidomics and its applicability to other diseases.

Abstract

Lipids are key regulators of brain function and have been increasingly implicated in neurodegenerative disorders including Alzheimer disease (AD). Here, a systems-based approach was employed to determine the lipidome of brain tissues affected by AD. Specifically, we used liquid chromatography-mass spectrometry to profile extracts from the prefrontal cortex, entorhinal cortex, and cerebellum of late-onset AD (LOAD) patients, as well as the forebrain of three transgenic familial AD (FAD) mouse models. Although the cerebellum lacked major alterations in lipid composition, we found an elevation of a signaling pool of diacylglycerol as well as sphingolipids in the prefrontal cortex of AD patients. Furthermore, the diseased entorhinal cortex showed specific enrichment of lysobisphosphatidic acid, sphingomyelin, the ganglioside GM3, and cholesterol esters, all of which suggest common pathogenic mechanisms associated with endolysosomal storage disorders. Importantly, a significant increase in cholesterol esters and GM3 was recapitulated in the transgenic FAD models, suggesting that these mice are relevant tools to study aberrant lipid metabolism of endolysosomal dysfunction associated with AD. Finally, genetic ablation of phospholipase D₂, which rescues the synaptic and behavioral deficits of an FAD mouse model, fully normalizes GM3 levels. These data thus unmask a cross-talk between the metabolism of phosphatidic acid, the product of phospholipase D₂, and gangliosides, and point to a central role of ganglioside anomalies in AD pathogenesis. Overall, our study highlights the hypothesis generating potential of lipidomics and identifies novel region-specific lipid anomalies potentially linked to AD pathogenesis.

Footnotes

↵* This work was supported, in whole or in part, by National Institutes of Health Grants R01 HD05547 (to G. D. P.) and P50 AG008702 (to M. Shelanski), and a Lejeune Foundation grant (to G. D. P.), National Research Foundation–Competitive Research Programme Grant R-183-000-218-281, Biomedical Research Council Grant R-183-000-234-305, and National University of Singapore–Life Sciences Institute (SLING) Grant R-711-000-021-133 (to M. R. W.).
↵ This article contains supplemental Figs. S1–S6 and Datasets S1–S3.