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Comparative effect of immature neuronal or glial cell transplantation on motor functional recovery following experimental traumatic brain injury in rats

机译:实验性脑外伤后未成熟神经元或神经胶质细胞移植对运动功能恢复的比较作用

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摘要

The present study evaluated the comparative effect of stereotaxically transplanted immature neuronal or glial cells in brain on motor functional recovery and cytokine expression after cold-induced traumatic brain injury (TBI) in adult rats. A total of 60 rats were divided into four groups (n=15/group): Sham group; TBI only group; TBI plus neuronal cells-transplanted group (NC-G); and TBI plus glial cells-transplanted group (GC-G). Cortical lesions were induced by a touching metal stamp, frozen with liquid nitrogen, to the dura mater over the motor cortex of adult rats. Neuronal and glial cells were isolated from rat embryonic and newborn cortices, respectively, and cultured in culture flasks. Rats received neurons or glia grafts (~1×106 cells) 5 days after TBI was induced. Motor functional evaluation was performed with the rotarod test prior to and following glial and neural cell grafts. Five rats from each group were sacrificed at 2, 4 and 6 weeks post-cell transplantation. Immunofluorescence staining was performed on brain section to identify the transplanted neuronal or glial cells using neural and astrocytic markers. The expression levels of cytokines, including transforming growth factor-β, glial cell-derived neurotrophic factor and vascular endothelial growth factor, which have key roles in the proliferation, differentiation and survival of neural cells, were analyzed by immunohistochemistry and western blotting. A localized cortical lesion was evoked in all injured rats, resulting in significant motor deficits. Transplanted cells successfully migrated and survived in the injured brain lesion, and the expression of neuronal and astrocyte markers were detected in the NC-G and GC-G groups, respectively. Rats in the NC-G and GC-G cell-transplanted groups exhibited significant motor functional recovery and reduced histopathologic lesions, as compared with the TBI-G rats that did not receive neural cells (P<0.05, respectively). Furthermore, GC-G treatment induced significantly improved motor functional recovery, as compared with the NC-G group (P<0.05). Increased cytokine expression levels were detected in the NC-G and GC-G groups, as compared with the TBI-G; however, no differences were found between the two groups. These data suggested that transplanted immature neural cells may promote the survival of neural cells in cortical lesion and motor functional recovery. Furthermore, transplanted glial cells may be used as an effective therapeutic tool for TBI patients with abnormalities in motor functional recovery and cytokine expression.
机译:本研究评估了成年大鼠冷定向脑外伤后脑部立体定向移植的神经元或神经胶质细胞对运动功能恢复和细胞因子表达的比较作用。将60只大鼠分为四组(n = 15 /组):假手术组;假手术组。仅TBI组; TBI加神经元细胞移植组(NC-G); TBI +神经胶质细胞移植组(GC-G)。通过用液氮冷冻的接触金属印章诱导成年大鼠运动皮层硬膜上的皮层损伤。分别从大鼠胚胎和新生皮层中分离神经元和神经胶质细胞,并在培养瓶中培养。诱导TBI后5天,大鼠接受了神经元或神经胶质移植物(〜1×10 6 细胞)。在神经胶质和神经细胞移植之前和之后,通过旋转试验进行运动功能评估。在细胞移植后第2、4和6周处死每组的5只大鼠。在脑部进行免疫荧光染色,以使用神经和星形细胞标记物识别移植的神经元或神经胶质细胞。通过免疫组织化学和蛋白质印迹分析了在转化神经细胞的增殖,分化和存活中起关键作用的细胞因子的表达水平,包括转化生长因子-β,神经胶质细胞衍生的神经营养因子和血管内皮生长因子。在所有受伤的大鼠中诱发局部皮质病变,导致明显的运动缺陷。移植的细胞在受损的脑病变中成功迁移并存活,并且分别在NC-G和GC-G组中检测到神经元和星形胶质细胞标志物的表达。与未接受神经细胞的TBI-G大鼠相比,NC-G和GC-G细胞移植组的大鼠表现出显着的运动功能恢复并减少了组织病理学损害(分别为P <0.05)。此外,与NC-G组相比,GC-G治疗可显着改善运动功能恢复(P <0.05)。与TBI-G相比,NC-G和GC-G组中检测到的细胞因子表达水平增加;但是,两组之间没有发现差异。这些数据表明,移植的未成熟神经细胞可能促进神经细胞在皮层病变中的存活和运动功能的恢复。此外,移植的神经胶质细胞可以用作患有运动功能恢复和细胞因子表达异常的TBI患者的有效治疗工具。

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