Oligodendrocyte precursor cells ingest axons in the mouse neocortex

Author:

Buchanan JoAnn1ORCID,Elabbady Leila1,Collman Forrest1,Jorstad Nikolas L.1,Bakken Trygve E.1ORCID,Ott Carolyn2ORCID,Glatzer Jenna3ORCID,Bleckert Adam A.1,Bodor Agnes L.1,Brittain Derrick1,Bumbarger Daniel J.1,Mahalingam Gayathri1ORCID,Seshamani Sharmishtaa1,Schneider-Mizell Casey1,Takeno Marc M.1ORCID,Torres Russel1,Yin Wenjing1,Hodge Rebecca D.1ORCID,Castro Manuel4,Dorkenwald Sven45,Ih Dodam4,Jordan Chris S.4,Kemnitz Nico4,Lee Kisuk45,Lu Ran4,Macrina Thomas45,Mu Shang4,Popovych Sergiy5,Silversmith William M.5ORCID,Tartavull Ignacio5,Turner Nicholas L.45,Wilson Alyssa M.4,Wong William4,Wu Jingpeng4ORCID,Zlateski Aleksandar4,Zung Jonathan4,Lippincott-Schwartz Jennifer2ORCID,Lein Ed S.1ORCID,Seung H. Sebastian45ORCID,Bergles Dwight E.36ORCID,Reid R. Clay1,da Costa Nuno Maçarico1ORCID

Affiliation:

1. Allen Institute for Brain Sciences, Seattle, WA 98109

2. Janelia Research Campus, Howard Hughes Medical Institute, Ashburn, VA 20147

3. The Solomon H. Snyder Department of Neuroscience, John Hopkins University School of Medicine, Baltimore, MD 21205

4. Princeton Neuroscience Institute, Princeton University, Princeton, NJ 08540

5. Computer Science Department, Princeton University, Princeton, NJ 08554

6. Johns Hopkins Kavli Neuroscience Discovery Institute, Baltimore, MD 21205

Abstract

Neurons in the developing brain undergo extensive structural refinement as nascent circuits adopt their mature form. This physical transformation of neurons is facilitated by the engulfment and degradation of axonal branches and synapses by surrounding glial cells, including microglia and astrocytes. However, the small size of phagocytic organelles and the complex, highly ramified morphology of glia have made it difficult to define the contribution of these and other glial cell types to this crucial process. Here, we used large-scale, serial section transmission electron microscopy (TEM) with computational volume segmentation to reconstruct the complete 3D morphologies of distinct glial types in the mouse visual cortex, providing unprecedented resolution of their morphology and composition. Unexpectedly, we discovered that the fine processes of oligodendrocyte precursor cells (OPCs), a population of abundant, highly dynamic glial progenitors, frequently surrounded small branches of axons. Numerous phagosomes and phagolysosomes (PLs) containing fragments of axons and vesicular structures were present inside their processes, suggesting that OPCs engage in axon pruning. Single-nucleus RNA sequencing from the developing mouse cortex revealed that OPCs express key phagocytic genes at this stage, as well as neuronal transcripts, consistent with active axon engulfment. Although microglia are thought to be responsible for the majority of synaptic pruning and structural refinement, PLs were ten times more abundant in OPCs than in microglia at this stage, and these structures were markedly less abundant in newly generated oligodendrocytes, suggesting that OPCs contribute substantially to the refinement of neuronal circuits during cortical development.

Funder

DNI | Intelligence Advanced Research Projects Activity

HHS | NIH | National Institute of Neurological Disorders and Stroke

HHS | National Institutes of Health

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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