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Studies on the changes of c-fos protein in spinal cord and neurotransmitter in dorsal root ganglion of the rat with an experimental peripheral neuropathy

机译:实验性周围神经病大鼠脊髓c-fos蛋白及背根神经节神经递质的变化

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Animal models for human chronic pain syndromes have been developed and widely used for pain research. One of these neuropathic pain models by Kim and Chung (1992) has many advantages for operation and pain elicitation. In this neuropathic model we have examined the c-fos protein, substance P, CGRP immunoreactivity in dorsal root ganglia and dorsal horn. 50 Sprague-Dawley rats were used for this study. L5 and L6 spinal nerves were ligated tightly to produce the neuropathic pain model. After 2, 4, 8, 16, and 24 hours and 1 week of surgery, rats were anesthetized and sacrificed by perfusion. After confirmation of the roots transected by the surgery, the L5 and L6 dorsal root ganglions and spinal cord were removed and processed for immunohistochemistry. All tissue sections were immunohistochemically stained for substance P, CGRP and c-fos using the peroxidase-antiperoxidase (PAP) method. The number of immunostained substance P and CGRP dorsal root ganglion cells and c-fos immunoreactive dorsal horn cells were counted and analyzed statistically with Mann-Whitney U test. The results are as follows. The number of c-fos protein immunoreactive neurons in the superficial layer of dorsal horn were increased markedly 2 hours after operation, and gradually decreased to normal level 1 week after operation. The number of c-fos protein immunoreactive neurons in the deep layer of the dorsal horn gradually increased to a peak 24 hours after operation, then decreased to the normal level 1 week after operation. The number of substance P and CGRP immunoreactive L5 and L6 dorsal root ganglion neurons were decreased markedly 1 week after the pain model operation. In conclusion, after neuropathic pain model operation, c-fos proteins were immediately expressed in the superficial layer of spinal dorsal horn, thereafter c-fos proteins in the deep layer of spinal dorsal horn were expressed. CGRP and substance P immunoreactive neurons in DRG were decreased markedly 1 week after neuropathic pain model operation. These decrements do not coincide with the other chronic pain models, which show great increases in these pain transmitting substances. Therefore, the relationship between pain and c-fos , SP and CGRP should be investigated further.
机译:已经开发出用于人类慢性疼痛综合征的动物模型,并将其广泛用于疼痛研究。 Kim和Chung(1992)提出的其中一种神经性疼痛模型在操作和诱发疼痛方面具有许多优势。在这种神经病模型中,我们检查了背根神经节和背角中的c-fos蛋白,P物质,CGRP免疫反应性。将50只Sprague-Dawley大鼠用于该研究。紧密结扎L5和L6脊髓神经以产生神经性疼痛模型。在2、4、8、16、24小时和1周的手术后,麻醉大鼠并通过灌注处死。在确认手术切除的根后,将L5和L6背根神经节和脊髓切除,并进行免疫组织化学处理。使用过氧化物酶-抗过氧化物酶(PAP)方法对所有组织切片进行P,CGRP和c-fos免疫组织化学染色。计数免疫染色的物质P和CGRP背根神经节细胞和c-fos免疫反应性背角细胞的数量,并用Mann-Whitney U检验进行统计学分析。结果如下。术后2小时,背角浅层c-fos蛋白免疫反应性神经元数量明显增加,术后1周逐渐下降至正常水平。手术后24小时,背角深层的c-fos蛋白免疫反应性神经元数量逐渐增加至峰值,然后在术后1周降至正常水平。疼痛模型手术后1周,P物质和CGRP免疫反应性L5和L6背根神经节神经元数量明显减少。综上所述,神经性疼痛模型手术后,脊髓背角浅表层立即表达c-fos蛋白,之后脊髓背角深层表达c-fos蛋白。神经性疼痛模型手术后1周,DRG中的CGRP和P物质免疫反应性神经元明显减少。这些减量与其他慢性疼痛模型并不吻合,后者显示出这些疼痛传递物质的大量增加。因此,应进一步研究疼痛与c-fos,SP和CGRP之间的关系。

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