Single-cell spatial proteomic imaging for human neuropathology

Author:

Vijayaragavan Kausalia,Cannon Bryan J.,Tebaykin Dmitry,Bossé Marc,Baranski Alex,Oliveria J. P.,Bukhari Syed A.,Mrdjen Dunja,Corces M. Ryan,McCaffrey Erin F.,Greenwald Noah F.,Sigal Yari,Marquez Diana,Khair Zumana,Bruce Trevor,Goldston Mako,Bharadwaj Anusha,Montine Kathleen S.,Angelo R. Michael,Montine Thomas J.,Bendall Sean C.ORCID

Abstract

Abstract Neurodegenerative disorders are characterized by phenotypic changes and hallmark proteopathies. Quantifying these in archival human brain tissues remains indispensable for validating animal models and understanding disease mechanisms. We present a framework for nanometer-scale, spatial proteomics with multiplex ion beam imaging (MIBI) for capturing neuropathological features. MIBI facilitated simultaneous, quantitative imaging of 36 proteins on archival human hippocampus from individuals spanning cognitively normal to dementia. Customized analysis strategies identified cell types and proteopathies in the hippocampus across stages of Alzheimer’s disease (AD) neuropathologic change. We show microglia-pathologic tau interactions in hippocampal CA1 subfield in AD dementia. Data driven, sample independent creation of spatial proteomic regions identified persistent neurons in pathologic tau neighborhoods expressing mitochondrial protein MFN2, regardless of cognitive status, suggesting a survival advantage. Our study revealed unique insights from multiplexed imaging and data-driven approaches for neuropathologic analysis and serves broadly as a methodology for spatial proteomic analysis of archival human neuropathology. Teaser Multiplex Ion beam Imaging enables deep spatial phenotyping of human neuropathology-associated cellular and disease features.

Funder

NIH

NCI

Stanford University

Canadian Institute of Health

Schweizerischer Nationalfonds zur Förderung der Wissenschaftlichen Forschung

Novartis Foundation for medical-biological Research

Glenn Foundation for Medical Research

Publisher

Springer Science and Business Media LLC

Subject

Cellular and Molecular Neuroscience,Neurology (clinical),Pathology and Forensic Medicine

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