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神经营病性大鼠背角中脑源性神经营养因子(BDNF)和γ-氨基丁酸(GABA)的释放

Release of BDNF and GABA in the dorsal horn of neuropathic rats.

作者信息

Lever Isobel, Cunningham Joanna, Grist John, Yip Ping K, Malcangio Marzia

机构信息

Sensory Function, Centre for Neuroscience Research, London WC1, E6BN, UK.

出版信息

Eur J Neurosci. 2003 Sep;18(5):1169-74. doi: 10.1046/j.1460-9568.2003.02848.x.

Abstract

Damage to peripheral nerves is associated with changes in excitability and/or phenotype of primary afferent neurons as well as increased neuronal excitability (central sensitization) and reduced inhibitory tone in the dorsal horn. For instance, in dorsal root ganglia (DRG) brain derived neurotrophic factor (BDNF) is down-regulated in small cells whilst de novo expressed in large diameter cells. In the dorsal horn, GABA content is decreased. In this study, in a dorsal horn, 'with dorsal roots attached' preparation obtained from spinal nerve lesioned Wistar rats, stimulation of ipsilateral dorsal roots at either A fibre or A + C fibre strength did not evoke release of BDNF. In separate experiments, activity-induced release of GABA in the isolated dorsal horn of neuropathic rats was significantly reduced compared to release in sham operated rats. GABA release could be significantly restored following topical application of BDNF through the dorsal horn preparation. Finally, neuropathic rats developed thermal and mechanical hypersensitivity and thermal hyperalgesia was reduced by intrathecal injection of BDNF. We concluded that BDNF-induced release of GABA could be a mechanism to explain the antinociceptive action of intrathecal BDNF in neuropathic animals. Furthermore, reduced availability of sensory neuron-derived BDNF might contribute to the reduced GABAergic tone in the dorsal horn of neuropathic rats.

摘要

外周神经损伤与初级传入神经元的兴奋性和/或表型变化相关,同时也与神经元兴奋性增加(中枢敏化)和背角抑制性张力降低有关。例如,在背根神经节(DRG)中,脑源性神经营养因子(BDNF)在小细胞中表达下调,而在大直径细胞中重新表达。在背角,GABA含量降低。在本研究中,从脊髓神经损伤的Wistar大鼠获得的“带背根”背角制备物中,以A纤维或A + C纤维强度刺激同侧背根并未引起BDNF的释放。在单独的实验中,与假手术大鼠相比,神经性大鼠离体背角中活性诱导的GABA释放显著减少。通过背角制备物局部应用BDNF后,GABA释放可显著恢复。最后,神经性大鼠出现热和机械超敏反应,鞘内注射BDNF可减轻热痛觉过敏。我们得出结论,BDNF诱导的GABA释放可能是解释鞘内BDNF在神经性动物中抗伤害感受作用的一种机制。此外,感觉神经元源性BDNF的可用性降低可能导致神经性大鼠背角中GABA能张力降低。

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