Deletion of the Fractalkine Receptor, CX3CR1, Improves Endogenous Repair, Axon Sprouting, and Synaptogenesis after Spinal Cord Injury in Mice

Camila M Freria; Jodie C E Hall; Ping Wei; Zhen Guan; Dana M McTigue; Phillip G Popovich

doi:10.1523/JNEUROSCI.2841-16.2017

Deletion of the Fractalkine Receptor, CX3CR1, Improves Endogenous Repair, Axon Sprouting, and Synaptogenesis after Spinal Cord Injury in Mice

J Neurosci. 2017 Mar 29;37(13):3568-3587. doi: 10.1523/JNEUROSCI.2841-16.2017. Epub 2017 Mar 6.

Authors

Camila M Freria¹, Jodie C E Hall¹, Ping Wei¹, Zhen Guan¹, Dana M McTigue¹, Phillip G Popovich²

Affiliations

¹ Department of Neuroscience and Center for Brain and Spinal Cord Repair, Ohio State University, Wexner Medical Center, Columbus, Ohio 43210.
² Department of Neuroscience and Center for Brain and Spinal Cord Repair, Ohio State University, Wexner Medical Center, Columbus, Ohio 43210 phillip.popovich@osumc.edu.

Abstract

Impaired signaling via CX3CR1, the fractalkine receptor, promotes recovery after traumatic spinal contusion injury in mice, a benefit achieved in part by reducing macrophage-mediated injury at the lesion epicenter. Here, we tested the hypothesis that CX3CR1-dependent changes in microglia and macrophage functions also will enhance neuroplasticity, at and several segments below the injury epicenter. New data show that in the presence of inflammatory stimuli, CX3CR1-deficient (CX3CR1^-/-) microglia and macrophages adopt a reparative phenotype and increase expression of genes that encode neurotrophic and gliogenic proteins. At the lesion epicenter (mid-thoracic spinal cord), the microenvironment created by CX3CR1^-/- microglia/macrophages enhances NG2 cell responses, axon sparing, and sprouting of serotonergic axons. In lumbar spinal cord, inflammatory signaling is reduced in CX3CR1^-/- microglia. This is associated with reduced dendritic pathology and improved axonal and synaptic plasticity on ventral horn motor neurons. Together, these data indicate that CX3CR1, a microglia-specific chemokine receptor, is a novel therapeutic target for enhancing neuroplasticity and recovery after SCI. Interventions that specifically target CX3CR1 could reduce the adverse effects of inflammation and augment activity-dependent plasticity and restoration of function. Indeed, limiting CX3CR1-dependent signaling could improve rehabilitation and spinal learning.SIGNIFICANCE STATEMENT Published data show that genetic deletion of CX3CR1, a microglia-specific chemokine receptor, promotes recovery after traumatic spinal cord injury in mice, a benefit achieved in part by reducing macrophage-mediated injury at the lesion epicenter. Data in the current manuscript indicate that CX3CR1 deletion changes microglia and macrophage function, creating a tissue microenvironment that enhances endogenous repair and indices of neuroplasticity, at and several segments below the injury epicenter. Interventions that specifically target CX3CR1 might be used in the future to reduce the adverse effects of intraspinal inflammation and augment activity-dependent plasticity (e.g., rehabilitation) and restoration of function.

Keywords: CX3CR1; inflammation; macrophages; microglia; plasticity; spinal cord injury.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
CX3C Chemokine Receptor 1
Female
Gene Deletion
Genetic Therapy / methods
Male
Mice
Mice, Inbred C57BL
Neuronal Outgrowth / physiology*
Receptors, Chemokine / genetics
Receptors, Chemokine / metabolism*
Spinal Cord Injuries / pathology*
Spinal Cord Injuries / physiopathology*
Spinal Cord Injuries / therapy
Spinal Cord Regeneration / physiology*
Synapses / pathology
Synapses / physiology*
Treatment Outcome

Substances

CX3C Chemokine Receptor 1
Cx3cr1 protein, mouse
Receptors, Chemokine

Grants and funding

R01 NS083942/NS/NINDS NIH HHS/United States