The Injured Sciatic Nerve Atlas (iSNAAT), Insights Into the Cellular and Molecular Basis of Neural Tissue Degeneration and Regeneration

Author(s)

Xiao-Feng Zhao
Lucas D. Huffman
Hannah Hafner
Mitre Athaiya
Matthew C. Finneran
Ashley L. Kalinski
Rafi Kohen
Corey Flynn
Ryan Passino
Craig N. Johnson
David Kohrman
Riki Kawaguchi
Lynda JS Yang
Jeffery L. Twiss, University of South CarolinaFollow
Daniel H. Geschwind
Gabriel Corfas
Roman J. Giger

Document Type

Article

Abstract

Upon trauma, the adult murine peripheral nervous system (PNS) displays a remarkable degree of spontaneous anatomical and functional regeneration. To explore extrinsic mechanisms of neural repair, we carried out single-cell analysis of naïve mouse sciatic nerve, peripheral blood mononuclear cells, and crushed sciatic nerves at 1 day, 3 days, and 7 days following injury. During the first week, monocytes and macrophages (Mo/Mac) rapidly accumulate in the injured nerve and undergo extensive metabolic reprogramming. Proinflammatory Mo/Mac with a high glycolytic flux dominate the early injury response and rapidly give way to inflammation resolving Mac, programmed toward oxidative phosphorylation. Nerve crush injury causes partial leakiness of the blood–nerve barrier, proliferation of endoneurial and perineurial stromal cells, and entry of opsonizing serum proteins. Micro-dissection of the nerve injury site and distal nerve, followed by single-cell RNA-sequencing, identified distinct immune compartments, triggered by mechanical nerve wounding and Wallerian degeneration, respectively. This finding was independently confirmed with Sarm1-/- mice, in which Wallerian degeneration is greatly delayed. Experiments with chimeric mice showed that wildtype immune cells readily enter the injury site in Sarm1-/- mice, but are sparse in the distal nerve, except for Mo. We used CellChat to explore intercellular communications in the naïve and injured PNS and report on hundreds of ligand–receptor interactions. Our longitudinal analysis represents a new resource for neural tissue regeneration, reveals location- specific immune microenvironments, and reports on large intercellular communication networks. To facilitate mining of scRNAseq datasets, we generated the injured sciatic nerve atlas (iSNAT): https://cdb-rshiny.med.umich.edu/Giger_iSNAT/.

Digital Object Identifier (DOI)

https://doi.org/10.7554/eLife.80881

Publication Info

Published in eLife, Volume 11, 2023.

Rights

©Zhao, Huffman, Hafner et al. This article is distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use and redistribution provided that the original author and source are credited.

APA Citation

Zhao, X.-F., Huffman, L. D., Hafner, H., Mitre Athaiya, Finneran, M. C., Kalinski, A. L., Kohen, R., Flynn, C., Passino, R., Johnson, C. N., Kohrman, D., Kawaguchi, R., Lynda JS Yang, Twiss, J. L., Geschwind, D. H., Corfas, G., & Giger, R. J. (2022). The injured sciatic nerve atlas (iSNAT), insights into the cellular and molecular basis of neural tissue degeneration and regeneration. ELife, 11. https://doi.org/10.7554/eLife.80881