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有丝分裂抑制对脊髓对半切伤和外周轴突切断叠加损伤反应的影响。

The effects of mitotic inhibition on the spinal cord response to the superimposed injuries of spinal cord hemisection and peripheral axotomy.

作者信息

Gould D J, Goshgarian H G

机构信息

Department of Anatomy and Neurobiology, University of Kentucky Medical Center, Lexington, Kentucky, 40536, USA.

出版信息

Exp Neurol. 1999 Aug;158(2):394-402. doi: 10.1006/exnr.1999.7136.

Abstract

The present study was carried out to test the hypothesis that dividing microglia are responsible for the depression of crossed phrenic nerve activity documented at 2 weeks postphrenicotomy in an injury model which superimposes the effects of spinal cord injury on peripheral axotomy. Crossed phenic nerve activity is defined as the respiratory activity recorded from the phrenic nerve during the crossed phrenic phenomenon (CPP) which is a respiratory reflex induced by respiratory stress following an ispsilateral spinal cord hemisection. Young adult female Sprague-Dawley rats were subjected to left intrathoracic phrenicotomies. Cytarabine (Cyt-A, a powerful antimitotic drug) or saline-filled miniosmotic pumps were then implanted into the cisterna magna and 2 weeks were allowed to pass at which time the CPP was induced by a left C2 spinal cord hemisection and transection of the contralateral phrenic nerve. Control studies including bromodeoxyuridine labeling of mitotic cells and a triple immunofluorescent protocol were carried out to verify that microglial cells were the primary cell type undergoing mitosis in the current injury model and that Cyt-A completely inhibited cellular proliferation. Quantitative electrophysiological analysis of crossed phrenic nerve activity showed that there is a statistically significant depression of activity at 2 weeks postphrenicotomy when animals were infused with saline compared to controls. Crossed phrenic nerve activity levels were not significantly different, however, from control levels when 2-week postphrenicotomized rats were infused with Cyt-A. Immunofluorescent studies showed that the majority of cells dividing in response to phrenicotomy were microglia. Furthermore, there were no astrocytes seen dividing at any time. From the results, we conclude that activated microglial cells may be responsible for the depression in crossed phrenic activity normally seen 2 weeks postphrenicotomy. Further, the activation of microglia may be related to the astrocytic response to injury. The activated microglial cell may be acting as a coordinator of various aspects of the injury response. Alternatively, the activation of microglia may be a necessary step in the cascade of multiple events that take place in the spinal cord after injury.

摘要

本研究旨在验证以下假设

在一种将脊髓损伤的影响叠加于外周轴突切断的损伤模型中,处于分裂状态的小胶质细胞是膈神经切断术后2周所记录到的交叉膈神经活动抑制的原因。交叉膈神经活动被定义为在交叉膈神经现象(CPP)期间从膈神经记录到的呼吸活动,交叉膈神经现象是在同侧脊髓半横断后由呼吸应激诱导的一种呼吸反射。对年轻成年雌性Sprague-Dawley大鼠实施左胸内膈神经切断术。然后将阿糖胞苷(Cyt-A,一种强效抗有丝分裂药物)或装有生理盐水的微型渗透泵植入大池,让其经过2周时间,此时通过左C2脊髓半横断和对侧膈神经横断诱导出交叉膈神经现象。开展了包括对有丝分裂细胞进行溴脱氧尿苷标记以及三重免疫荧光实验的对照研究,以验证小胶质细胞是当前损伤模型中经历有丝分裂的主要细胞类型,且Cyt-A完全抑制细胞增殖。对交叉膈神经活动的定量电生理分析表明,与对照组相比,在膈神经切断术后2周给动物注入生理盐水时,活动存在统计学上的显著抑制。然而,当给膈神经切断术后2周的大鼠注入Cyt-A时,交叉膈神经活动水平与对照水平并无显著差异。免疫荧光研究表明,因膈神经切断术而分裂的大多数细胞是小胶质细胞。此外,在任何时候都未见星形胶质细胞分裂。根据这些结果,我们得出结论,活化的小胶质细胞可能是膈神经切断术后2周通常所见的交叉膈神经活动抑制的原因。此外,小胶质细胞的活化可能与星形胶质细胞对损伤的反应有关。活化的小胶质细胞可能在损伤反应的各个方面起到协调作用。或者,小胶质细胞的活化可能是损伤后脊髓中发生的一系列多事件级联反应中的一个必要步骤。

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