AI Article Synopsis

  • Persistent inflammation in spinal cord injury (SCI) hinders nerve repair due to continuous activation of M1-like macrophages/microglia, which release macrophage extracellular traps (Mets).
  • A study using a spinal cord contusion model revealed that Mets promote the differentiation of macrophages/microglia into M1-like cells through a novel inflammatory signaling pathway involving LL37-P2X37-NF-B.
  • Findings suggest that targeting Mets may enhance recovery from SCI and that the presence of Met-related proteins in human serum correlates with the severity of SCI, indicating potential for both therapeutic and diagnostic applications.

Article Abstract

Persistent inflammation in the secondary spinal cord injury (SCI) is an important reason for the failure of nerve repair, which is partly due to the continuous activation of local M1-like macrophage/microglia. It is reported that extracellular trap (ET) has been a new way of cell death, which can be released by macrophages and named macrophage extracellular trap (Met). Furthermore, it exists widely in the pathophysiological process of many diseases, but it has been rarely studied in the field of SCI. In this study, we constructed a spinal cord contusion model and assessed the function outcome of SCI rats. We used immunofluorescence, flow cytometry, and transmission electron microscope (TEM) to demonstrate the existence of Mets. Besides, some related experiments had also been employed to explore the relationship between Mets and M1 polarization of macrophage/microglia. We also performed Co-IP and Western blotting to reveal a new extracellular proinflammatory signal pathway. Finally, we made a linear regression analysis between the concentrations of specific markers of Mets in human serum and ASIA scores. Briefly, our results suggested that macrophages infiltrated in SCI area could induce macrophage/microglia to differentiate into M1-like cells by releasing Mets, which may be achieved partly through LL37-P2X37-NF-B signal pathway. However, limiting Mets could effectively inhibit M1 polarization and promote function recovery. In addition, the concentrations of Met related proteins in human serum showed high correlation with ASIA scores and could be applied to reflect the severity of SCI. In conclusion, Mets may be a new target for SCI therapy and a promising index for SCI assessment.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9713475PMC
http://dx.doi.org/10.1155/2022/9197940DOI Listing

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