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Dopaminergic-primed fetal liver mesenchymal stromal-like cells can reverse parkinsonian symptoms in 6-hydroxydopamine-lesioned mice

机译:多巴胺能引发的胎儿肝间充质样细胞可以逆转6-羟基多巴胺损伤小鼠的帕金森氏症

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Background aims. Cell replacement therapy is considered a promising alternative in the treatment of degenerative diseases, and in this context, mesenchymal stromal cells (MSCs) have been proposed for transplantation in Parkinson disease (PD). Thus far, the results of animal studies are found to be inconsistent and inconclusive regarding the therapeutic ability of the cells. This study investigated the efficacy of fetal liver (FL)-MSC-derived dopaminergic (DA) neuronal primed cells for correction of parkinsonian symptoms in mice. Methods. FL-MSCs were differentiated for 21 days in the presence of a combination of neurotropic factors. The extent of cellular reprogramming was analyzed by quantitative polymerase chain reaction for DA-specific neuronal gene expressions and protein expressions by immuno-cytochemistry. The functionality of the cells was determined by electrophysiology and dopamine release assays. Ten-day-primed neuron-like cells or unprimed MSCs were transplanted into the 6-hydroxydopamine (6-OHDA)-lesioned striatum using a stereotaxic device. Dopamine-secreting properties and behavioral studies were used to assess improvement of parkinsonian symptoms. Results. The differentiated cells expressed DA-specific genes and proteins, while exhibiting a high level of voltage-gated potassium current. Furthermore, neuronal primed cells differentiated into tyrosine hydroxylase immunoreactive and dopamine-secreting functional neuron like cells. Symptomatic correction of PD in the recipient mice within 2 months of transplantation was also observed. Discussion. FL-MSC-derived primed neuron-like cells integrated into the striatum of PD mice, improving parkinsonian symptoms. This study demonstrates an effective cell-based therapy for PD.
机译:背景目标。细胞替代疗法被认为是治疗退行性疾病的一种有前途的替代方法,在这种情况下,间充质基质细胞(MSCs)已被提议用于帕金森病(PD)的移植。迄今为止,发现动物研究的结果在细胞的治疗能力方面是不一致的和不确定的。这项研究调查了胎肝(FL)-MSC衍生的多巴胺能(DA)神经元引发细胞对小鼠帕金森氏症校正的功效。方法。在存在神经营养因子的情况下,将FL-MSC分化21天。通过定量聚合酶链反应,通过免疫细胞化学分析DA特异性神经元基因表达和蛋白质表达,分析了细胞重编程的程度。细胞的功能通过电生理学和多巴胺释放测定来确定。使用立体定位设备将十天初免的神经元样细胞或未初免的MSCs移植到6-羟基多巴胺(6-OHDA)受损的纹状体中。多巴胺分泌特性和行为研究被用来评估帕金森病症状的改善。结果。分化的细胞表达DA特异性基因和蛋白质,同时表现出高水平的电压门控钾电流。此外,神经元引发的细胞分化为酪氨酸羟化酶免疫反应性和多巴胺分泌功能性神经元样细胞。还观察到移植后2个月内接受小鼠PD的症状校正。讨论。 FL-MSC衍生的引发神经元样细胞整合到PD小鼠的纹状体中,改善了帕金森病症状。这项研究证明了一种有效的基于细胞的PD疗法。

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