胞磷胆碱预处理对大鼠脊髓缺血再灌注损伤模型具有神经保护作用。

Citicoline and postconditioning provides neuroprotection in a rat model of ischemic spinal cord injury.

机构信息

Department of Neurosurgery, Uludag University School of Medicine, 16059 Bursa, Turkey.

出版信息

Acta Neurochir (Wien). 2010 Jun;152(6):1033-42. doi: 10.1007/s00701-010-0598-5. Epub 2010 Jan 30.

DOI:10.1007/s00701-010-0598-5

PMID:20112033

Abstract

BACKGROUND

Ischemic spinal cord injury is a chain of events caused by the reduction and/or cessation of spinal cord blood flow, which results in neuronal degeneration and loss. Ischemic postconditioning is defined as a series of intermittent interruptions of blood flow in the early phase of reperfusion and has been shown to reduce the infarct size in cerebral ischemia. Our study aimed to characterize the relationship between the neuronal injury-decreasing effects of citicoline and ischemic postconditioning, which were proven to be effective against the apoptotic process.

METHOD

Spinal cord ischemia was produced in rats using an intrathoracic approach to implement the synchronous arcus aorta and subclavian artery clipping method. In our study, 42 male Sprague-Dawley rats (309 +/- 27 g) were used. Animals were divided into sham operated, spinal ischemia, citicoline, postconditioning, and postconditioning citicoline groups. Postconditioning was generated by six cycles of 1 min occlusion/5 min reperfusion. A 600 mmol/kg dose of citicoline was given intraperitoneally before ischemia in the citicoline and postconditioning citicoline groups. All rats were sacrificed 96 h after reperfusion. For immunohistochemical analysis, bcl-2, caspase 3, caspase 9, and bax immune staining were performed. Caspase 3, caspase 9, bax, and bcl-2 were used as apoptotic and antiapoptotic markers, respectively.

FINDINGS

The blood pressure values obtained at the onset of reperfusion were significantly lower than the preischemic values. A difference in immunohistochemical scoring was detected between the caspase 3, caspase 9, bax, and bcl-2 groups. When comparisons between the ischemia (groups 2, 3, 4, and 5) and sham groups (group 1) were performed, a significant increase in caspase 3, caspase 9, bax, and bcl-2 was detected. When comparing the subgroups, the average score of caspase 9 was found to be significantly higher in ischemia group 2. The average score of bcl-2 was also found to be significantly higher in postconditioning and citicoline group 5.

CONCLUSIONS

It is thus thought that combining citicoline with postconditioning provides protection by inhibiting the caspase pathway and by increasing the antiapoptotic proteins.

摘要

背景

缺血性脊髓损伤是由脊髓血流减少和/或停止引起的一系列事件，导致神经元变性和丧失。缺血后处理定义为再灌注早期血流的一系列间歇性中断，已被证明可减少脑缺血中的梗死面积。我们的研究旨在描述胞磷胆碱的神经元损伤减少作用与缺血后处理之间的关系，这两种方法都被证明能有效对抗细胞凋亡过程。

方法

通过胸腔内方法实施同步主动脉弓和锁骨下动脉夹闭法，在大鼠中产生脊髓缺血。在本研究中，使用了 42 只雄性 Sprague-Dawley 大鼠（309 ± 27 g）。动物分为假手术、脊髓缺血、胞磷胆碱、后处理和后处理胞磷胆碱组。通过 6 个 1 分钟闭塞/5 分钟再灌注周期产生后处理。在胞磷胆碱和后处理胞磷胆碱组中，在缺血前给予 600 mmol/kg 剂量的胞磷胆碱腹腔内给药。所有大鼠在再灌注后 96 小时处死。用于免疫组织化学分析，进行 bcl-2、caspase 3、caspase 9 和 bax 免疫染色。Caspase 3、caspase 9、bax 和 bcl-2 分别用作凋亡和抗凋亡标志物。

结果

再灌注开始时获得的血压值明显低于缺血前值。在 caspase 3、caspase 9、bax 和 bcl-2 组之间检测到免疫组织化学评分的差异。当将缺血（第 2、3、4 和 5 组）与假手术组（第 1 组）进行比较时，发现 caspase 3、caspase 9、bax 和 bcl-2 明显增加。在比较亚组时，发现缺血组 2 中的 caspase 9 平均评分显着升高。还发现后处理和胞磷胆碱组 5 中的 bcl-2 平均评分显着升高。