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Conversion of Human Umbilical Cord Mesenchymal Stem Cells in Wharton’s Jelly to Dopamine Neurons Mediated by the Lmx1a and Neurturin In Vitro: Potential Therapeutic Application for Parkinson’s Disease in a Rhesus Monkey Model

机译:沃顿氏胶中的人类脐带间充质干细胞向Lmx1a和Neurturin介导的多巴胺神经元的体外转化:在恒河猴模型中帕金森氏病的潜在治疗应用

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摘要

hUC-MSCs hold great promise in vitro neuronal differentiation and therapy for neurodegenerative disorders including Parkinson’s disease. Recent studies provided that Lmx1α play an important role in the midbrain dopamine cells differentiation. Neurturin is desired candidate gene for providing a neuroprotective to DA neurons. In this study, we investigated a novel neuronal differentiation strategy in vitro with Lmx1α and NTN. We transferred these two genes to hUC-MSCs by recombinant adenovirus combined with Lmx1α regulatory factor and other inductor to improve the efficiency of inducing. Then those induced cells were implanted into the striatum and substantia nigra of MPTP lesioned hemi-parkinsonian rhesus monkeys. Monkeys were monitored by using behavioral test for six months after implantation. The result showed that cells isolated from the umbilical cord were negative for CD45, CD34 and HLA-DR, but were positive for CD44, CD49d, CD29. After those cells were infected with recombinant adenovirus, RT-PCR result shows that both Lmx1α and NTN genes were transcribed in hUC-MSCs. We also observed that the exogenous were highly expressed in hUC-MSCs from immunofluorescence and western blot. Experiments in vitro have proved that secretion NTN could maintain the survival of rat fetal midbrain dopaminergic neurons. After hUC-MSCs were induced with endogenous and exogenous factors, the mature neurons specific gene TH, Pitx3 was transcripted and the neurons specific protein TH, β-tubulinIII, NSE, Nestin, MAP-2 was expressed in those differentiated cells. In addition, the PD monkeys, transplanted with the induced cells demonstrated the animals’ symptoms amelioration by the behavioral measures. Further more, pathological and immunohistochemistry data showed that there were neuronal-like cells survived in the right brain of those PD monkeys, which may play a role as dopaminergic neurons. The findings from this study may help us to better understand the inside mechanisms of PD pathogenesis and may also help developing effective therapy for Parkinson’s disease.
机译:hUC-MSC在神经元分化和神经退行性疾病(包括帕金森氏病)的治疗方面具有广阔的前景。最近的研究提供了Lmx1α在中脑多巴胺细胞分化中起重要作用。 Neurturin是为DA神经元提供神经保护的理想候选基因。在这项研究中,我们调查了Lmx1α和NTN在体外的新型神经元分化策略。我们通过重组腺病毒结合Lmx1α调节因子和其他诱导剂将这两个基因转移到hUC-MSCs中,以提高诱导效率。然后将这些诱导的细胞植入MPTP病变的半帕金森氏恒河猴的纹状体和黑质中。植入后六个月通过行为测试监测猴子。结果表明,从脐带分离的细胞对CD45,CD34和HLA-DR呈阴性,而对CD44,CD49d,CD29呈阳性。用重组腺病毒感染这些细胞后,RT-PCR结果显示Lmx1α和NTN基因均在hUC-MSC中转录。我们还观察到,通过免疫荧光和蛋白质印迹,hUC-MSC中高表达外源基因。体外实验证明,分泌NTN可以维持大鼠胎儿中脑多巴胺能神经元的存活。用内源性和外源性因子诱导hUC-MSCs后,成熟的神经元特异性基因TH,Pitx3被转录,并在这些分化的细胞中表达神经元特异性蛋白TH,β-微管蛋白III,NSE,Nestin,MAP-2。此外,移植了诱导细胞的PD猴子通过行为措施证明动物的症状得到缓解。此外,病理和免疫组织化学数据表明,那些PD猴的右脑中存在神经元样细胞,其可能起多巴胺能神经元的作用。这项研究的发现可能有助于我们更好地了解PD发病机理的内部机制,也可能有助于开发针对帕金森氏病的有效疗法。

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