首页> 外文期刊>Behavioural Brain Research: An International Journal >Long term behavioral effects of functional dopaminergic neurons generated from human neural stem cells in the rat 6-OH-DA Parkinson's disease model. Effects of the forced expression of BCL-X L
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Long term behavioral effects of functional dopaminergic neurons generated from human neural stem cells in the rat 6-OH-DA Parkinson's disease model. Effects of the forced expression of BCL-X L

机译:在大鼠6-OH-DA帕金森氏病模型中,由人神经干细胞产生的功能性多巴胺能神经元的长期行为影响。 BCL-X L强制表达的作用

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Parkinson's disease (PD) motor symptoms are caused by the progressive degeneration of ventral mesencephalic (VM) dopaminergic neurons (DAn) in the Substantia Nigra pars compacta (SNpc). Cell replacement therapy for PD is based on the concept that the implantation of DAn in the striatum can functionally restore the dopamine levels lost in the disease. In the current study we have used an immortalized human VM neural stem cell line (hVM1) that generates DAn with the A9 phenotype. We have previously found that the forced expression of Bcl-X L in these cells enhances DAn generation and improves, short-term, d-amphetamine-induced rotation after transplantation in the 6-OH-DA rat model of PD 2-month post-grafting. Since functional maturation of human A9 DAn in vivo requires long survival times, in the present study we investigated the behavioral amelioration induced by the transplantation of these precursors (na?ve and Bcl-X L-modified) in the striatum of Parkinsonian rats for up to 5 months. The main findings observed are an improvement on drug-induced behaviour and importantly, in spontaneous behavior tests for both cell-transplanted groups. Finally, we have also tested whether the grafts could ameliorate cognitive performance in PD, in addition to motor deficits. Significant difference was observed for T-maze alternation test in the cell-transplanted animals as compared to sham operated ones. To our knowledge, this is the first report showing an amelioration in spontaneous motor behavior and in cognitive performance in Parkinsonian animals after receiving human VM neural stem cell grafts. Histological studies confirmed that the grafts generated mature dopaminergic cells.
机译:帕金森氏病(PD)运动症状是由黑质致密部(SNpc)中的腹侧中脑(VM)多巴胺能神经元(DAn)逐渐退化引起的。 PD的细胞替代疗法基于以下概念:纹状体中植入DAn可以在功能上恢复疾病中损失的多巴胺水平。在当前的研究中,我们使用了永生化的人类VM神经干细胞系(hVM1),它可以产生具有A9表型的DAn。我们先前已经发现,在PD的6-OH-DA大鼠模型中,在移植后2个月,Bcl-X L在这些细胞中的强制表达增强了DAn的产生,并改善了短期D-苯异丙胺诱导的旋转。嫁接。由于人A9 DAn在体内的功能成熟需要较长的生存时间,因此在本研究中,我们研究了帕金森氏大鼠纹状体中这些前体(幼稚和Bcl-X L修饰的)前体的移植诱导的行为改善。到5个月。观察到的主要发现是对药物诱导行为的改善,并且重要的是,在两个细胞移植组的自发行为测试中。最后,我们还测试了除运动功能障碍外,移植物是否还能改善PD的认知功能。与假手术的动物相比,在细胞移植的动物中观察到了T迷宫交替测试的显着差异。据我们所知,这是第一个报告,显示在接受人类VM神经干细胞移植后,帕金森氏动物的自发运动行为和认知能力得到改善。组织学研究证实,移植物产生了成熟的多巴胺能细胞。

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