Regional desynchronization of microglial activity is associated with cognitive decline in Alzheimer's disease.

BORIS DOI
Publisher DOI
PubMed ID
39238030
Description
Background
Microglial activation is one hallmark of Alzheimer disease (AD) neuropathology but the impact of the regional interplay of microglia cells in the brain is poorly understood. We hypothesized that microglial activation is regionally synchronized in the healthy brain but experiences regional desynchronization with ongoing neurodegenerative disease. We addressed the existence of a microglia connectome and investigated microglial desynchronization as an AD biomarker.
Methods
To validate the concept, we performed microglia depletion in mice to test whether interregional correlation coefficients (ICCs) of 18 kDa translocator protein (TSPO)-PET change when microglia are cleared. Next, we evaluated the influence of dysfunctional microglia and AD pathophysiology on TSPO-PET ICCs in the mouse brain, followed by translation to a human AD-continuum dataset. We correlated a personalized microglia desynchronization index with cognitive performance. Finally, we performed single-cell radiotracing (scRadiotracing) in mice to ensure the microglial source of the measured desynchronization.
Results
Microglia-depleted mice showed a strong ICC reduction in all brain compartments, indicating microglia-specific desynchronization. AD mouse models demonstrated significant reductions of microglial synchronicity, associated with increasing variability of cellular radiotracer uptake in pathologically altered brain regions. Humans within the AD-continuum indicated a stage-depended reduction of microglia synchronicity associated with cognitive decline. scRadiotracing in mice showed that the increased TSPO signal was attributed to microglia.
Conclusion
Using TSPO-PET imaging of mice with depleted microglia and scRadiotracing in an amyloid model, we provide first evidence that a microglia connectome can be assessed in the mouse brain. Microglia synchronicity is closely associated with cognitive decline in AD and could serve as an independent personalized biomarker for disease progression.
Date of Publication
2024-09-05
Publication Type
Article
Subject(s)
600 - Technology::610 - Medicine & health
Keyword(s)
Alzheimer’s disease
Brain connectivity
Dementia
Microglia
Microglia desynchronization
Microglia synchronicity
Neuroinflammation
PET
TSPO
Language(s)
en
Contributor(s)
Zatcepin, Artem
Gnörich, Johannes
Rauchmann, Boris-Stephan
Bartos, Laura M
Franzmeier, Nicolai
Malpetti, Maura
Xiang, Xianyuan
Parhizkar, Samira
Grosch, Maximilian
Wind-Mark, Karin
Kunte, Sebastian T
Beyer, Leonie
Brösamle, Desirée
Wendeln, Ann-Christin
Osei-Sarpong, Collins
Heindl, Steffanie
Liesz, Arthur
Stoecklein, Sophia
Biechele, Gloria
Finze, Anika
Eckenweber, Florian
Lindner, Simon
Bartenstein, Peter
Willem, Michael
Tahirovic, Sabina
Herms, Jochen
Buerger, Katharina
Simons, Mikael
Haass, Christian
Rupprecht, Rainer
Riemenschneider, Markus J
Albert, Nathalie L
Beyer, Marc
Neher, Jonas J
Paeger, Lars
Levin, Johannes
Höglinger, Günter U
Perneczky, Robert
Ziegler, Sibylle I
Brendel, Matthias
Additional Credits
Clinic of Nuclear Medicine
Series
Molecular Neurodegeneration
Publisher
BioMed Central
ISSN
1750-1326
Access(Rights)
open.access
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