Amelioration of chronic neuropathic pain after partial nerve injury by adeno-associated viral (AAV) vector-mediated over-expression of BDNF in the rat spinal cord

神经病理性疼痛 脊髓 医学 痛觉超敏 神经营养因子 坐骨神经 脑源性神经营养因子 慢性疼痛 痛觉过敏 麻醉 腺相关病毒 神经损伤 中枢神经系统 原位杂交 脊髓损伤 神经营养素 病理 伤害 内科学 生物 载体(分子生物学) 受体 基因表达 重组DNA 生物化学 精神科 基因
作者
Mary J. Eaton,Bas Blits,Marc J. Ruitenberg,Joost Verhaagen,Martin Oudega
出处
期刊:Gene Therapy [Springer Nature]
卷期号:9 (20): 1387-1395 被引量:140
标识
DOI:10.1038/sj.gt.3301814
摘要

Changing the levels of neurotrophins in the spinal cord micro-environment after nervous system injury has been proposed to recover normal function, such that behavioral response to peripheral stimuli does not lead to chronic pain. We have investigated the effects of recombinant adeno-associated viral (rAAV)-mediated over-expression of brain-derived neurotrophic factor (BDNF) in the spinal cord on chronic neuropathic pain after unilateral chronic constriction injury (CCI) of the sciatic nerve. The rAAV-BDNF vector was injected into the dorsal horn at the thirteenth thoracic spinal cord vertebra (L1 level) 1 week after CCI. Allodynia and hyperalgesia induced by CCI in the hindpaws were permanently reversed, beginning 1 week after vector injection, compared with a similar injection of a control rAAV-GFP vector (green fluorescent protein) or saline. In situ hybridization for BDNF demonstrated that both dorsal and ventral lumbar spinal neurons contained an intense signal for BDNF mRNA, at 1 to 8 weeks after vector injection. There was no similar BDNF mRNA over-expression associated with either injections of saline or rAAV-GFP. These data suggest that chronic neuropathic pain is sensitive to early spinal BDNF levels after partial nerve injury and that rAAV-mediated gene transfer could potentially be used to reverse chronic pain after nervous system injuries in humans.

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