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本文引用的文献

1
Development of GABA-sensitive spasticity and rigidity in rats after transient spinal cord ischemia: a qualitative and quantitative electrophysiological and histopathological study.短暂性脊髓缺血后大鼠GABA敏感性痉挛和强直的发展:一项定性和定量的电生理及组织病理学研究。
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Combined immunosuppressive agents or CD4 antibodies prolong survival of human neural stem cell grafts and improve disease outcomes in amyotrophic lateral sclerosis transgenic mice.联合免疫抑制剂或CD4抗体可延长人神经干细胞移植的存活时间,并改善肌萎缩侧索硬化转基因小鼠的疾病预后。
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Development of functional human embryonic stem cell-derived neurons in mouse brain.功能性人胚胎干细胞衍生神经元在小鼠大脑中的发育。
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Measurement of peripheral muscle resistance in rats with chronic ischemia-induced paraplegia or morphine-induced rigidity using a semi-automated computer-controlled muscle resistance meter.使用半自动计算机控制的肌肉阻力计测量慢性缺血性截瘫或吗啡诱导的僵硬大鼠的外周肌肉阻力。
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Human neural stem cells differentiate and promote locomotor recovery in spinal cord-injured mice.人类神经干细胞可分化并促进脊髓损伤小鼠的运动功能恢复。
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Spinal implantation of hNT neurons and neuronal precursors: graft survival and functional effects in rats with ischemic spastic paraplegia.人神经嵴来源神经元及神经前体细胞的脊髓植入:对缺血性痉挛性截瘫大鼠移植体存活及功能的影响
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人脊髓干细胞脊髓移植后缺血性截瘫大鼠的功能恢复

Functional recovery in rats with ischemic paraplegia after spinal grafting of human spinal stem cells.

作者信息

Cizkova D, Kakinohana O, Kucharova K, Marsala S, Johe K, Hazel T, Hefferan M P, Marsala M

机构信息

Institute of Neurobiology, Centrum of Excellence, Slovak Academy of Science, Kosice, Soltesovej 4, Slovakia.

出版信息

Neuroscience. 2007 Jun 29;147(2):546-60. doi: 10.1016/j.neuroscience.2007.02.065. Epub 2007 May 23.

DOI:10.1016/j.neuroscience.2007.02.065
PMID:17524565
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3417127/
Abstract

Transient spinal cord ischemia in humans can lead to the development of permanent paraplegia with prominent spasticity and rigidity. Histopathological analyses of spinal cords in animals with ischemic spastic paraplegia show a selective loss of small inhibitory interneurons in previously ischemic segments but with a continuing presence of ventral alpha-motoneurons and descending cortico-spinal and rubro-spinal projections. The aim of the present study was to examine the effect of human spinal stem cells (hSSCs) implanted spinally in rats with fully developed ischemic paraplegia on the recovery of motor function and corresponding changes in motor evoked potentials. In addition the optimal time frame for cell grafting after ischemia and the optimal dosing of grafted cells were also studied. Spinal cord ischemia was induced for 10 min using aortic occlusion and systemic hypotension. In the functional recovery study, hSSCs (10,000-30,000 cells/0.5 mul/injection) were grafted into spinal central gray matter of L2-L5 segments at 21 days after ischemia. Animals were immunosuppressed with Prograf (1 mg/kg or 3 mg/kg) for the duration of the study. After cell grafting the recovery of motor function was assessed periodically using the Basso, Beattie and Bresnahan (BBB) scoring system and correlated with the recovery of motor evoked potentials. At predetermined times after grafting (2-12 weeks), animals were perfusion-fixed and the survival, and maturation of implanted cells were analyzed using antibodies recognizing human-specific antigens: nuclear protein (hNUMA), neural cell adhesion molecule (hMOC), neuron-specific enolase (hNSE) and synapthophysin (hSYN) as well as the non-human specific antibodies TUJ1, GFAP, GABA, GAD65 and GLYT2. After cell grafting a time-dependent improvement in motor function and suppression of spasticity and rigidity was seen and this improvement correlated with the recovery of motor evoked potentials. Immunohistochemical analysis of grafted lumbar segments at 8 and 12 weeks after grafting revealed intense hNSE immunoreactivity, an extensive axo-dendritic outgrowth as well as rostrocaudal and dorsoventral migration of implanted hNUMA-positive cells. An intense hSYN immunoreactivity was identified within the grafts and in the vicinity of persisting alpha-motoneurons. On average, 64% of hSYN terminals were GAD65 immunoreactive which corresponded to GABA immunoreactivity identified in 40-45% of hNUMA-positive grafted cells. The most robust survival of grafted cells was seen when cells were grafted 21 days after ischemia. As defined by cell survival and laminar distribution, the optimal dose of injected cells was 10,000-30,000 cells per injection. These data indicate that spinal grafting of hSSCs can represent an effective therapy for patients with spinal ischemic paraplegia.

摘要

人类短暂性脊髓缺血可导致永久性截瘫,并伴有明显的痉挛和僵硬。对缺血性痉挛性截瘫动物的脊髓进行组织病理学分析发现,先前缺血节段的小型抑制性中间神经元选择性丧失,但腹侧α运动神经元以及下行皮质脊髓和红核脊髓投射仍持续存在。本研究的目的是研究将人类脊髓干细胞(hSSCs)脊髓内植入已完全发展为缺血性截瘫的大鼠后,对运动功能恢复及运动诱发电位相应变化的影响。此外,还研究了缺血后细胞移植的最佳时间框架以及移植细胞的最佳剂量。通过主动脉阻断和全身低血压诱导脊髓缺血10分钟。在功能恢复研究中,于缺血后21天将hSSCs(10,000 - 30,000个细胞/0.5微升/注射)移植到L2 - L5节段的脊髓中央灰质中。在研究期间,用普乐可复(1毫克/千克或3毫克/千克)对动物进行免疫抑制。细胞移植后,使用Basso、Beattie和Bresnahan(BBB)评分系统定期评估运动功能恢复情况,并将其与运动诱发电位的恢复情况相关联。在移植后的预定时间(2 - 12周),对动物进行灌注固定,并使用识别人类特异性抗原的抗体:核蛋白(hNUMA)、神经细胞黏附分子(hMOC)、神经元特异性烯醇化酶(hNSE)和突触素(hSYN)以及非人类特异性抗体TUJ1、GFAP、GABA、GAD65和GLYT2分析植入细胞的存活和成熟情况。细胞移植后,观察到运动功能随时间的改善以及痉挛和僵硬的抑制,这种改善与运动诱发电位的恢复相关。移植后8周和12周对移植的腰段进行免疫组织化学分析发现,hNSE免疫反应强烈,有广泛的轴突 - 树突生长,以及植入的hNUMA阳性细胞的头尾向和背腹向迁移。在移植物内和持续存在的α运动神经元附近发现强烈的hSYN免疫反应。平均而言,64%的hSYN终末为GAD65免疫反应阳性,这与在40 - 45%的hNUMA阳性移植细胞中鉴定出的GABA免疫反应相对应。当在缺血后21天移植细胞时,观察到移植细胞的存活最为强劲。根据细胞存活和层状分布确定,每次注射的最佳细胞剂量为10,000 - 30,000个细胞。这些数据表明,hSSCs的脊髓移植可为脊髓缺血性截瘫患者提供一种有效的治疗方法。