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首页> 外文期刊>Spine >Direct application of the TNF-alpha inhibitor, etanercept, does not affect CGRP expression and phenotypic change of DRG neurons following application of nucleus pulposus onto injured sciatic nerves in rats.
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Direct application of the TNF-alpha inhibitor, etanercept, does not affect CGRP expression and phenotypic change of DRG neurons following application of nucleus pulposus onto injured sciatic nerves in rats.

机译:将髓核应用于大鼠坐骨神经损伤后,直接应用TNF-α抑制剂etanercept不会影响CGRP表达和DRG神经元的表型改变。

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STUDY DESIGN: Immunohistological and behavioral analysis of the effect of a tumor necrosis factor alpha (TNF-alpha) inhibitor in an injured-nerve model. OBJECTIVE: To examine the effect of direct application of a TNF-alpha inhibitor (etanercept) on injured-nerve pain caused by nucleus pulposus. SUMMARY AND BACKGROUND DATA: TNF-alpha is thought to play a crucial role in radicular pain. Calcitonin gene-related peptide (CGRP) is an inflammatory neuropeptide found in small sensory neurons. We have reported that CGRP appears in medium and large dorsal root ganglion (DRG) neurons that transmit proprioception in physiologic conditions. The purpose of the current study was to examine the change in behavior and phenotypic change of CGRP-immunoreactive DRG neurons by the TNF-alpha inhibitor, etanercept, in a disc herniation model. METHODS: For the injured-nerve model, nucleus pulposus was applied to the sciatic nerve and the sciatic nerve pinched. Saline (10 microL; n = 10), as a control, or etanercept (150 microg: n = 10) were applied to sciatic nerves simultaneously. Mechanical allodynia was examined. Immunohistochemistry was used to examine CGRP expression in L5 DRGs. RESULTS: Significant mechanical allodynia for 10 days was seen in the injured-nerve group compared with sham-operated animals. Etanercept ameliorated the mechanical allodynia slightly on day 2; however, there was no effect on other days. CGRP immunoreactivity was upregulated in the L5 DRG neurons of injured-nerve groups compared with the sham-operated group (P < 0.01). However, etanercept did not affect CGRP expression after nerve injury (P > 0.05). Proportions of CGRP- immunoreactive medium and large neurons were not significantly different in the nerve injury + saline group compared with the injury + etanercept group (P > 0.05). CONCLUSION: Our results indicate that direct application of a TNF-alpha inhibitor had a small effect on acute pain behavior and may not be effective for suppression of inflammatory peptides in the current disc-herniation model.
机译:研究设计:肿瘤坏死因子α(TNF-alpha)抑制剂在受伤的神经模型中的作用的免疫组织学和行为分析。目的:研究直接应用TNF-α抑制剂(依那西普)对髓核引起的神经痛的作用。摘要和背景数据:TNF-α被认为在神经痛中起着至关重要的作用。降钙素基因相关肽(CGRP)是一种在小感觉神经元中发现的炎性神经肽。我们已经报道,CGRP出现在生理条件下传递本体感受的中型和大型背根神经节(DRG)神经元中。本研究的目的是检查在椎间盘突出症模型中TNF-α抑制剂etanercept对CGRP免疫反应性DRG神经元的行为和表型变化的影响。方法:对于受伤的神经模型,将髓核应用于坐骨神经并捏紧坐骨神经。同时将生理盐水(10 microL; n = 10)或依那西普(150 microg:n = 10)应用于坐骨神经。检查机械性异常性疼痛。免疫组织化学用于检查L5 DRG中CGRP的表达。结果:与假手术组相比,受伤神经组有10天的明显机械异常性疼痛。依那西普在第2天稍微改善了机械性异常性疼痛;但是,其他日期没有任何影响。与假手术组相比,受伤神经组的L5 DRG神经元中的CGRP免疫反应性上调(P <0.01)。但是,依那西普不影响神经损伤后的CGRP表达(P> 0.05)。与损伤+依那西普组相比,神经损伤+盐水组中CGRP-免疫反应介质和大神经元的比例无显着差异(P> 0.05)。结论:我们的结果表明,直接应用TNF-α抑制剂对急性疼痛行为影响不大,在目前的椎间盘突出症模型中可能无法有效抑制炎症肽。

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