Changes in contractile characteristics of rat skeletal muscles associated with P2-receptor activation after spinal cord transection

Q3 Multidisciplinary
A. E. Khairullin, D. V. Efimova, M. A. Mukhamedyarov, M. Baltin, T. Baltina, S. Grishin, A. Ziganshin
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Abstract

Introduction. Traumatic spinal cord and peripheral-nerve injury is associated with release of proinflammatory cytokines and chemokines, which may stimulate neuronal activity. Adenosine triphosphoric acid (ATP) is an important pain mediator involved in the acute and chronic neuropathic pain development. Its excessive release from primary injured tissue leads to activation of P2-receptors, which may further start secondary injury mechanisms. Although the effects of ATP on the peripheral nervous system are relatively well studied, the pathophysiological role of purinergic signaling after spinalization remains unclear. The study was aimed at assessing the post-spinalization effects of P2-receptors on the contractile characteristics of rat skeleton muscles. Materials and methods. The objects of the study were the soleus muscle, the extensor digitorum longus (EDL) muscle, and diaphragm in intact rats and spinalized rats. Seven days after laminectomy followed by spinal cord transection, animals were anesthetized, exsanguinated, and their muscles with nerve stumps were isolated. Contractile response parameters were recorded using mechanomyography (MMG). To study effects of ATP on ligand binding, ATP was added to a bath and mechanical responses in the rat muscles were assessed 7 min after. After washing with Krebs–Henseleit solution, the preparations were incubated with suramin solution for 20 min with subsequent ATP application. Then the mechanical responses in the muscles were again recorded. Statistical significance was assessed using Student's t-test for independent (unpaired) and paired samples. Results. We found a significant (p 0.05) decrease in the modulating activity of ATP, as the main endogenous signaling agent, in the cholinergic synapse of the soleus muscle from 32.4 to 5.8% and from 13.7 to 5.6% for the EDL muscle after the spinalization (spinal cord injury at the Th6–Th7 level) compared with intact animals. No such dramatic changes were observed in the diaphragm. Conclusions. Abnormal ATP-mediated modulation of neuromuscular transmission demonstrated in this study supports the involvement of purinergic signaling in the neurotrophic control and functioning of various motor units.
脊髓横断后与 P2 受体激活相关的大鼠骨骼肌收缩特性的变化
简介创伤性脊髓和外周神经损伤与促炎细胞因子和趋化因子的释放有关,这些因子可刺激神经元活动。三磷酸腺苷(ATP)是一种重要的疼痛介质,参与急性和慢性神经病理性疼痛的发展。它从原发性损伤组织中过度释放,导致 P2 受体被激活,从而可能进一步启动继发性损伤机制。虽然 ATP 对周围神经系统的影响研究相对较多,但脊髓化后嘌呤能信号的病理生理作用仍不清楚。本研究旨在评估脊髓化后 P2 受体对大鼠骨骼肌收缩特性的影响。材料和方法。研究对象是完整大鼠和脊髓化大鼠的比目鱼肌、伸肌和膈肌。在椎板切除术和脊髓横断术后七天,对动物进行麻醉、放血,并分离带神经残端的肌肉。使用机械肌电图(MMG)记录收缩反应参数。为了研究 ATP 对配体结合的影响,将 ATP 加入水浴中,7 分钟后评估大鼠肌肉的机械反应。用克雷布斯-亨斯莱特溶液清洗后,将制备物与苏拉明溶液孵育 20 分钟,随后加入 ATP。然后再次记录肌肉的机械反应。采用学生 t 检验法对独立样本(非配对)和配对样本进行统计意义评估。结果我们发现,与完整动物相比,脊髓化(Th6-Th7水平脊髓损伤)后比目鱼肌胆碱能突触中作为主要内源性信号物质的 ATP 的调节活性明显降低(p 0.05),从 32.4% 降至 5.8%,EDL 肌从 13.7% 降至 5.6%。在膈肌中没有观察到如此显著的变化。结论本研究证明 ATP 介导的神经肌肉传导调节异常支持嘌呤能信号参与各种运动单元的神经营养控制和功能。
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来源期刊
Annals of Clinical and Experimental Neurology
Annals of Clinical and Experimental Neurology Medicine-Neurology (clinical)
CiteScore
0.80
自引率
0.00%
发文量
32
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