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Publication : An active vesicle priming machinery suppresses axon regeneration upon adult CNS injury.

First Author  Hilton BJ Year  2022
Journal  Neuron Volume  110
Issue  1 Pages  51-69.e7
PubMed ID  34706221 Mgi Jnum  J:324897
Mgi Id  MGI:6877248 Doi  10.1016/j.neuron.2021.10.007
Citation  Hilton BJ, et al. (2022) An active vesicle priming machinery suppresses axon regeneration upon adult CNS injury. Neuron 110(1):51-69.e7
abstractText  Axons in the adult mammalian central nervous system fail to regenerate after spinal cord injury. Neurons lose their capacity to regenerate during development, but the intracellular processes underlying this loss are unclear. We found that critical components of the presynaptic active zone prevent axon regeneration in adult mice. Transcriptomic analysis combined with live-cell imaging revealed that adult primary sensory neurons downregulate molecular constituents of the synapse as they acquire the ability to rapidly grow their axons. Pharmacogenetic reduction of neuronal excitability stimulated axon regeneration after adult spinal cord injury. Genetic gain- and loss-of-function experiments uncovered that essential synaptic vesicle priming proteins of the presynaptic active zone, but not clostridial-toxin-sensitive VAMP-family SNARE proteins, inhibit axon regeneration. Systemic administration of Baclofen reduced voltage-dependent Ca(2+) influx in primary sensory neurons and promoted their regeneration after spinal cord injury. These findings indicate that functional presynaptic active zones constitute a major barrier to axon regeneration.
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