Dual Role of Microglial TREM2 in Neuronal Degeneration and Regeneration After Axotomy
After nerve injuries, microglia proliferate and migrate towards injured motoneurons, where they attach to the cell bodies. The significance of microglia enwrapping of axotomized motoneurons remains unclear. We found that within the same motor pools, some motoneurons degenerate while others regenerate, and each is associated with different microglia phenotypes and interactions. Microglia surrounding degenerating motoneurons form tight cell clusters (death clusters) that fully envelop the cell body and express high TREM2 and large CD68 granules, suggesting a macrophagocyte phenotype. Microglia surrounding motoneurons during the regeneration process are individualized and upregulate TREM2 and CD68; however, the CD68 granules are smaller. These microglia extend processes that scan the motoneuron surface through sweeping motions, sampling contents, and likely incorporating components through microphagocytosis. Removal of TREM2, either globally throughout development or specifically in microglia prior to nerve injuries, reduces p-SYK signaling and CD68 expression in all activated microglia, but with a sex effect: CD68 downregulation is significant in females, but not in males. Lack of TREM2 also prevents motoneuron cell body swelling (in both sexes), characteristic of the early chromatolytic reaction at the start of regeneration. This correlates with delays in muscle reinnervation. We conclude that within the same motor pools, TREM2 directs some microglia to remove degenerating motoneurons while it facilitates the regenerative phenotype of other motoneurons. The signals that direct these different microglia phenotypes over degenerating and regenerating motoneurons, as well as the mechanisms that induce degeneration in some motoneurons while most others regenerate, remain to be investigated.