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Is the subarachnoid administration of mesenchymal stromal cells a useful strategy to treat chronic brain damage?

机译:蛛网膜下腔间质基质细胞给药是治疗慢性脑损伤的有用策略吗?

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Traumatic brain injury (TBI) is a leading cause of mortality and morbidity worldwide. Developing effective protocols for the administration of mesenchymal stromal cells (MSCs) is a promising therapeutic strategy to treat TBI. It is important to develop alternatives to direct parenchymal injection at the injury site because direct injection is an expensive and invasive technique. Subarachnoid transplantation, a minimally invasive and low-risk procedure, may be an important and clinically applicable strategy. The aim of this study was to test the therapeutic effect of subarachnoid administration of MSCs on functional outcome 2 months after an experimental TBI in rats. Methods. Two months after TBI, 30 female Wistar rats were divided into 3 groups (n = 10 in each group): sham, MSC (received 2 × 10~6 MSCs) and saline (received only saline) groups. Neurological function, brain and spinal cords samples and cerebrospinal fluid were studied. Results. No significant differences were found in neurological evaluation and after histological analysis; differences in the expression of neurotrophins were present but were not statistically significant. MSCs survived in the host tissue, and some expressed neural markers. Conclusions. Similar to direct parenchymal injections, transplanted MSCs survive, migrate to the injury cavity and differentiate into mature neural cell types for at least 6 months after engraftment. These results open the possibility that MSC administration through subarachnoid administration may be a treatment for the consequences of TBI. The transplantation technique and cell number should be adjusted to obtain functional outcome and neurotrophin production differences.
机译:颅脑外伤(TBI)是世界范围内死亡率和发病率的主要原因。制定有效的间充质基质细胞(MSCs)管理方案是一种有前途的治疗TBI的治疗策略。开发直接在损伤部位进行实质性注射的替代方法非常重要,因为直接注射是一种昂贵且具有侵入性的技术。蛛网膜下腔移植是一种微创,低风险的手术方法,可能是一项重要的临床应用策略。这项研究的目的是测试大鼠实验性TBI后2个月,蛛网膜下腔给予MSCs对功能结局的治疗作用。方法。 TBI后两个月,将30只雌性Wistar大鼠分为3组(每组10只):假手术,MSC(接受2×10〜6 MSC)和生理盐水(仅接受生理盐水)组。研究了神经功能,脑和脊髓样品以及脑脊液。结果。神经学评估和组织学分析后均未发现明显差异。存在神经营养蛋白表达差异,但无统计学意义。 MSC在宿主组织中存活,并且表达了一些神经标记。结论与直接进行实质性注射相似,移植的MSC在移植后存活至少6个月,可存活,迁移至损伤腔并分化为成熟的神经细胞类型。这些结果打开了通过蛛网膜下腔施用MSC可能治疗TBI后果的可能性。应当调整移植技术和细胞数以获得功能结果和神经营养蛋白产生差异。

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