A Proteomics Analysis of 5xFAD Mouse Brain Regions Reveals the Lysosome-associated Protein Arl8b As a Candidate Biomarker for Alzheimer's Disease

Overview

Journal Genome Med

Publisher Biomed Central

Specialty Genetics

Date 2023 Jul 19

PMID 37468900

Authors

Annett Boeddrich

Christian Haenig

Nancy Neuendorf

Eric Blanc

Andranik Ivanov

Marieluise Kirchner

Philipp Schleumann

Irem Bayraktaroglu

Matthias Richter

Christine Mirjam Molenda

Anje Sporbert

Martina Zenkner

Sigrid Schnoegl

Christin Suenkel

Luisa-Sophie Schneider

Agnieszka Rybak-Wolf

Bianca Kochnowsky

Lauren M Byrne

Edward J Wild

Jorgen E Nielsen

Gunnar Dittmar

Oliver Peters

Dieter Beule

Erich E Wanker

Affiliations

Soon will be listed here.

Abstract

Background: Alzheimer's disease (AD) is characterized by the intra- and extracellular accumulation of amyloid-β (Aβ) peptides. How Aβ aggregates perturb the proteome in brains of patients and AD transgenic mouse models, remains largely unclear. State-of-the-art mass spectrometry (MS) methods can comprehensively detect proteomic alterations, providing relevant insights unobtainable with transcriptomics investigations. Analyses of the relationship between progressive Aβ aggregation and protein abundance changes in brains of 5xFAD transgenic mice have not been reported previously.

Methods: We quantified progressive Aβ aggregation in hippocampus and cortex of 5xFAD mice and controls with immunohistochemistry and membrane filter assays. Protein changes in different mouse tissues were analyzed by MS-based proteomics using label-free quantification; resulting MS data were processed using an established pipeline. Results were contrasted with existing proteomic data sets from postmortem AD patient brains. Finally, abundance changes in the candidate marker Arl8b were validated in cerebrospinal fluid (CSF) from AD patients and controls using ELISAs.

Results: Experiments revealed faster accumulation of Aβ42 peptides in hippocampus than in cortex of 5xFAD mice, with more protein abundance changes in hippocampus, indicating that Aβ42 aggregate deposition is associated with brain region-specific proteome perturbations. Generating time-resolved data sets, we defined Aβ aggregate-correlated and anticorrelated proteome changes, a fraction of which was conserved in postmortem AD patient brain tissue, suggesting that proteome changes in 5xFAD mice mimic disease-relevant changes in human AD. We detected a positive correlation between Aβ42 aggregate deposition in the hippocampus of 5xFAD mice and the abundance of the lysosome-associated small GTPase Arl8b, which accumulated together with axonal lysosomal membranes in close proximity of extracellular Aβ plaques in 5xFAD brains. Abnormal aggregation of Arl8b was observed in human AD brain tissue. Arl8b protein levels were significantly increased in CSF of AD patients.

Conclusions: We report a comprehensive biochemical and proteomic investigation of hippocampal and cortical brain tissue derived from 5xFAD transgenic mice, providing a valuable resource to the neuroscientific community. We identified Arl8b, with significant abundance changes in 5xFAD and AD patient brains. Arl8b might enable the measurement of progressive lysosome accumulation in AD patients and have clinical utility as a candidate biomarker.

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