Kappa-selective opiate antagonist nor-binaltorphimine improves outcome after traumatic spinal cord injury in rats.

A I Faden, A E Takemori, P S Portoghese
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引用次数: 44

Abstract

Nor-binaltorphimine (nor-BNI) is a recently developed opiate antagonist that has a high degree of selectivity for kappa-opiate receptors. Because of the proposed role of kappa-opiate receptors in mediating secondary damage after spinal trauma, the effect of nor-BNI was studied in a well-characterized model of traumatic spinal cord injury in rats. Nor-BNI, at a dose of 10 mg/kg administered intravenously at 15 min following impact trauma to T-9, significantly improved neurological recovery, measured both in terms of Tarlov motor scores and ability to maintain position on an inclined plane. Given intrathecally, at doses that were ineffective systemically (0.1 mg/kg), nor-BNI also significantly improved neurological recovery after trauma. These data are consistent with the hypothesis that endogenous opioids, through actions at kappa-opiate receptors within the spinal cord, contribute to the pathophysiological changes after spinal trauma that lead to irreversible tissue damage, and indicate that kappa-receptor antagonists may be beneficial for the treatment of acute spinal cord injury.

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kappa选择性阿片类拮抗剂非双萘托非明改善大鼠创伤性脊髓损伤后的预后。
非甲萘啡胺(non -binaltorphimine, nor-BNI)是一种新开发的阿片拮抗剂,对阿片受体具有高度的选择性。由于kappa-阿片受体在脊髓损伤后介导继发性损伤中的作用,我们在一个具有良好特征的大鼠创伤性脊髓损伤模型中研究了非bni的作用。在T-9撞击损伤后15分钟静脉给予10 mg/kg剂量的no - bni,可显著改善神经系统恢复,包括Tarlov运动评分和在斜面上保持位置的能力。给鞘内注射非bni,在全身无效的剂量下(0.1 mg/kg),也显著改善创伤后神经恢复。这些数据与内源性阿片样物质通过作用于脊髓内的kappa-阿片受体,促进脊髓损伤后的病理生理变化,导致不可逆的组织损伤的假设一致,并表明kappa受体拮抗剂可能有益于急性脊髓损伤的治疗。
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