Dark Microglia Are Abundant in Normal Postnatal Development, where they Remodel Synapses via Phagocytosis and Trogocytosis, and Are Dependent on TREM2

Haley A. Vecchiarelli
Kanchan Bisht
Kaushik Sharma
Sammy Weiser Novak
Marianela E. Traetta
Monica Emili Garcia-Segura
Marie-Kim St-Pierre
Julie C. Savage
Cory Willis
Katherine Picard
Maude Bordeleau
Nathalie Vernoux
Mohammadparsa Khakpour
Rishika Garg
Sophia M. Loewen
Colin J. Murray
Yelena Y. Grinberg
Joel Faustino
Torin Halvorson
Victor Lau
Stefano Pluchino
Zinaida S. Vexler
Monica J. Carson
Uri Manor
Luca Peruzzotti-Jametti
Marie-Ève Tremblay

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Abstract

This study examined dark microglia—a state linked to central nervous system pathology and neurodegeneration—during postnatal development in the mouse ventral hippocampus, finding that dark microglia interact with blood vessels and synapses and perform trogocytosis of pre-synaptic axon terminals. Furthermore, we found that dark microglia in development notably expressed C-type lectin domain family 7 member A (CLEC7a), lipoprotein lipase (LPL) and triggering receptor expressed on myeloid cells 2 (TREM2) and required TREM2, differently from other microglia, suggesting a link between their role in remodeling during development and central nervous system pathology. Together, these results point towards a previously under-appreciated role for dark microglia in synaptic pruning and plasticity during normal postnatal development.

Version published to 10.1101/2024.10.15.618087v1 on bioRxiv
Oct 18, 2024

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