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慢性坐骨神经压迫损伤后背根神经节神经元的重组:与吗啡和利多卡因镇痛的相关性

Reorganization of dorsal root ganglion neurons following chronic sciatic nerve constriction injury: correlation with morphine and lidocaine analgesia.

作者信息

Kolesnikov Yuri, El-Maarouf Abderrahman, Rutishauser Urs, Pasternak Gavril

机构信息

Department of Anesthesiology, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, NY 10021, USA.

出版信息

Eur J Pharmacol. 2007 Jul 30;568(1-3):124-33. doi: 10.1016/j.ejphar.2007.04.045. Epub 2007 May 8.

DOI:10.1016/j.ejphar.2007.04.045
PMID:17543299
Abstract

Chronic constriction injury of the sciatic nerve is an animal model for neuropathic pain. In this model, the analgesic potency of systemic morphine was significantly diminished in nerve-injured mice (ED(50) 19.4 mg/kg) compared with sham-operated mice (ED(50) 3.3 mg/kg) using a unilateral hot plate withdrawal test, with a similar reduction in sensitivity of intrathecal morphine. The sciatic nerve injury resulted in a reorganization of the dorsal root ganglion (DRG) neurons. Immunohistochemically, the chronic constriction injury triggered a withdrawal of C-fibers from the ipsilateral dorsal horn of the spinal cord. Although A-beta terminals centrally sprouted into Lamina II of the dorsal horn of the spinal cord, the peripheral A-beta fibers in the skin retracted from the epidermis to deeper layers of the dermis. To explore the functional significance of these dermal changes, we examined the topical morphine and lidocaine analgesia following chronic sciatic nerve constriction. Both morphine and lidocaine retained topical activity following chronic sciatic nerve injury, but their analgesic dose-response curves were shifted to the right when compared to sham-operated mice. Thus, the chronic nerve constriction injury model is associated with pathological changes in distribution of the central and peripheral axons of the dorsal root ganglion neurons that correspond to a decreased pharmacological sensitivity to topical analgesic agents.

摘要

坐骨神经慢性缩窄损伤是一种神经性疼痛的动物模型。在该模型中,与假手术小鼠(半数有效剂量[ED(50)]为3.3mg/kg)相比,使用单侧热板撤离试验时,神经损伤小鼠中全身吗啡的镇痛效力显著降低(ED(50)为19.4mg/kg),鞘内注射吗啡的敏感性也有类似降低。坐骨神经损伤导致背根神经节(DRG)神经元发生重组。免疫组织化学显示,慢性缩窄损伤引发C纤维从脊髓同侧背角撤出。虽然A-β终末在脊髓背角Ⅱ层向中枢侧芽生长,但皮肤中的外周A-β纤维从表皮退缩至真皮深层。为探究这些皮肤变化的功能意义,我们检测了慢性坐骨神经缩窄后局部应用吗啡和利多卡因的镇痛效果。慢性坐骨神经损伤后,吗啡和利多卡因均保留局部活性,但与假手术小鼠相比,它们的镇痛剂量-反应曲线右移。因此,慢性神经缩窄损伤模型与背根神经节神经元中枢和外周轴突分布的病理变化有关,这与局部镇痛药的药理敏感性降低相对应。

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