首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Inosine Accelerates the Regeneration and Anticipates the Functional Recovery after Sciatic Nerve Crush Injury in Mice
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Inosine Accelerates the Regeneration and Anticipates the Functional Recovery after Sciatic Nerve Crush Injury in Mice

机译:Inosine加速再生,并预测小鼠坐骨神经压碎损伤后的功能恢复

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Trauma to the peripheral nervous system (PNS) results in loss of motor and sensory functions. After an injury, a complex series of events begins, allowing axonal regeneration and target reinnervation. However, this regenerative potential is limited by several factors such as age, distance from the lesion site to the target and severity of lesion. Many studies look for ways to overcome these limitations. Inosine, a purine nucleoside derived from adenosine, emerges as a potential treatment, due to its capacity to regulate axonal growth, neuroprotection and immunomodulation, contributing to motor recovery. However, no studies demonstrated their effects on PNS. C57/Black6 mice were submitted to sciatic nerve crush and received intraperitoneal injections of saline or inosine (70 mg/kg), one hour after injury and daily for one week. To evaluate axonal regeneration and functional recovery, electroneuromyography, Sciatic Function Index (SFI), rotarod and pinprick tests were performed. Our results showed that the inosine group presented a higher number of myelinated fibers and a large amount of fibers within the ideal G-ratio. In addition, the results of electroneuromyography showed greater amplitude of the compound muscle action potentials in the first and second weeks, suggesting anticipation of regeneration in the inosine group. We also observed in the inosine group, motor and sensory neurons survival, reduction in the number of macrophages and myelin ovoids in the sciatic nerves, and an early recovery of motor and sensory functions. Thus, we conclude that the use of inosine accelerates axonal regeneration promoting an early recovery of motor and sensory functions. (C) 2019 IBRO. Published by Elsevier Ltd. All rights reserved.
机译:外周神经系统(PNS)的创伤导致电机和感官功能丢失。受伤后,一系列复杂的事件开始,允许轴突再生和目标重新生成。然而,这种再生潜力受到近期年龄,距离病变部位的距离和病变的严重程度的影响的限制。许多研究寻找克服这些限制的方法。 Inosine,衍生自腺苷的嘌呤核苷作为潜在的处理,由于其调节轴突生长,神经保护和免疫调节的能力,有助于电动机恢复。然而,没有研究证明了它们对PNS的影响。将C57 / Black6小鼠提交给坐骨神经粉碎,并在损伤后1小时后腹腔注射尿布或肌苷(70mg / kg),每天一小时。为了评估轴突再生和功能恢复,进行电轴切性,坐标函数指数(SFI),滚子和针刺试验。我们的研究结果表明,Inosine组在理想的G比内呈现了更高数量的髓鞘纤维和大量的纤维。此外,电轴上的电子体积结果在第一周和第二周内显示出更大的复合肌动作电位幅度,这表明在伊内塞斯基因中预期再生。我们还观察到Inosine组,电机和感官神经元存活,减少巨噬细胞和髓鞘中的骨髓卵体中的数量,以及电动机和感官功能的早期恢复。因此,我们得出结论,inosine的使用加速了轴突再生,促进了电动机和感官功能的早期恢复。 (c)2019年IBRO。 elsevier有限公司出版。保留所有权利。

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