Expression of an Activated Integrin Promotes Long-Distance Sensory Axon Regeneration in the Spinal Cord.

JOURNAL OF NEUROSCIENCE(2016)

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摘要
After CNS injury, axon regeneration is blocked by an inhibitory environment consisting of the highly upregulated tenascin-C and chondroitin sulfate proteoglycans (CSPGs). Tenascin-C promotes growth of axons if they express a tenascin-binding integrin, particularly alpha 9 beta 1. Additionally, integrins can be inactivated by CSPGs, and this inhibition can be overcome by the presence of a beta 1-binding integrin activator, kindlin-1. We examined the synergistic effect of alpha 9 integrin and kindlin-1 on sensory axon regeneration in adult rat spinal cord after dorsal root crush and adeno-associated virus transgene expression in dorsal root ganglia. After 12 weeks, axons from C6-C7 dorsal root ganglia regenerated through the tenascin-C-rich dorsal root entry zone into the dorsal column up to C1 level and above (>25 mm axon length) through a normal pathway. Animals also showed anatomical and electrophysiological evidence of reconnection to the dorsal horn and behavioral recovery in mechanical pressure, thermal pain, and ladder-walking tasks. Expression of alpha 9 integrin or kindlin-1 alone promoted much less regeneration and recovery.
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关键词
adeno-associated virus,alpha9 integrin,axon regeneration,dorsal root ganglion,kindlin-1,spinal cord
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