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首页> 外文期刊>Journal of neurotrauma >The delayed post-injury administration of soluble fas receptor attenuates post-traumatic neural degeneration and enhances functional recovery after traumatic cervical spinal cord injury
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The delayed post-injury administration of soluble fas receptor attenuates post-traumatic neural degeneration and enhances functional recovery after traumatic cervical spinal cord injury

机译:创伤后延迟施用可溶性fas受体可减轻创伤后神经脊髓损伤后的神经变性并增强功能恢复

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摘要

Spinal cord injury (SCI) is a devastating condition that currently lacks clinically-relevant and effective neuroprotective therapeutic options. Optimal therapeutic agents for clinical translation should show efficacy in a cervical compression/contusion model using a clinically-relevant post-injury therapeutic time window. To date, few compounds have met that rigorous standard. The objective of this work was to evaluate the efficacy of delayed post-injury administration of soluble Fas receptor (sFasR) via intrathecal catheter following acute cervical SCI in a clinically-relevant contusion/compression model. Female Wistar rats were given a C7-T1 moderately severe clip compression injury, followed by either 8-h or 24-h delayed treatment initiation. Long-term neurobehavioral analysis of motor recovery and neuropathic pain development was undertaken. The extent of oligodendrocyte and neuron survival was assessed in peri-lesional cord sections 8 weeks post-SCI. This was complemented by an evaluation of the level of tissue preservation at and adjacent to the site of injury. In animals treated with sFasR delayed 8 h post-injury, significant behavioral effects were observed, coinciding with enhanced cell survival, peri-lesional tissue sparing, and enhanced integrity of descending fiber tracts compared to control treatments. Animals treated with sFasR delayed by 24 h showed more modest improvements in behavioral recovery, and had consistent improvements in cell survival and tissue preservation. This work has shown for the first time that the Fas-mediated apoptotic pathway can be therapeutically targeted in a clinically-relevant time window post-SCI.
机译:脊髓损伤(SCI)是一种破坏性疾病,目前缺乏临床相关且有效的神经保护性治疗选择。使用临床相关的损伤后治疗时间窗,用于临床翻译的最佳治疗剂应在宫颈压迫/挫伤模型中显示疗效。迄今为止,很少有化合物达到该严格标准。这项工作的目的是评估在临床相关的挫伤/压迫模型中,急性宫颈SCI术后通过鞘内导管延迟给予可溶性Fas受体(sFasR)的疗效。雌性Wistar大鼠受到C7-T1中等严重的夹子压缩损伤,然后延迟8小时或24小时开始治疗。进行了运动恢复和神经性疼痛发展的长期神经行为分析。 SCI后8周,在病灶周围的脊髓切片中评估少突胶质细胞和神经元存活的程度。通过评估损伤部位及其附近组织的保存水平来补充这一点。与对照组相比,用sFasR治疗的动物在受伤后延迟8 h进行了观察,观察到了显着的行为效果,与细胞存活率提高,病灶周围组织稀疏和下行纤维束完整性增强相吻合。用sFasR治疗延迟24小时的动物在行为恢复方面表现出更适度的改善,并且在细胞存活和组织保存方面具有持续改善。这项工作首次表明,可以在SCI后的临床相关时间窗内以Fas介导的凋亡途径为治疗靶标。

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