Accelerated axon outgrowth, guidance, and target reinnervation across nerve transection gaps following a brief electrical stimulation paradigm

神经再支配 神经科学 再生(生物学) 神经突 医学 轴突 刺激 轴突切开术 电生理学 神经损伤 运动神经元 坐骨神经 周围神经损伤 感觉系统 解剖 生物 中枢神经系统 细胞生物学 体外 脊髓 生物化学
作者
Bhagat Singh,Qing-Gui Xu,Colin K. Franz,Rumi Zhang,Colin Dalton,T. Gordon,Valerie M. K. Verge,Rajiv Midha,Douglas W. Zochodne
出处
期刊:Journal of Neurosurgery [American Association of Neurological Surgeons]
卷期号:116 (3): 498-512 被引量:110
标识
DOI:10.3171/2011.10.jns11612
摘要

Regeneration of peripheral nerves is remarkably restrained across transection injuries, limiting recovery of function. Strategies to reverse this common and unfortunate outcome are limited. Remarkably, however, new evidence suggests that a brief extracellular electrical stimulation (ES), delivered at the time of injury, improves the regrowth of motor and sensory axons.In this work, the authors explored and tested this ES paradigm, which was applied proximal to transected sciatic nerves in mice, and identified several novel and compelling impacts of the approach. Using thy-1 yellow fluorescent protein mice with fluorescent axons that allow serial in vivo tracking of regeneration, the morphological, electrophysiological, and behavioral indices of nerve regrowth were measured.The authors show that ES is associated with a 30%-50% improvement in several indices of regeneration: regrowth of axons and their partnered Schwann cells across transection sites, maturation of regenerated fibers in gaps spanning transection zones, and entry of axons into their muscle and cutaneous target zones. In parallel studies, the authors analyzed adult sensory neurons and their response to extracellular ES while plated on a novel microelectrode array construct designed to deliver the identical ES paradigm used in vivo. The ES accelerated neurite outgrowth, supporting the concept of a neuron-autonomous mechanism of action.Taken together, these results support a robust role for brief ES following peripheral nerve injuries in promoting regeneration. Electrical stimulation has a wider repertoire of impact than previously recognized, and its impact in vitro supports the hypothesis that a neuron-specific reprogrammed injury response is recruited by the ES protocol.

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