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首页> 外文期刊>Experimental Neurology >A clonal line of mesencephalic progenitor cells converted to dopamine neurons by hematopoietic cytokines: a source of cells for transplantation in Parkinson's disease.
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A clonal line of mesencephalic progenitor cells converted to dopamine neurons by hematopoietic cytokines: a source of cells for transplantation in Parkinson's disease.

机译:中脑祖细胞的克隆系通过造血细胞因子转化为多巴胺神经元:这是帕金森氏病移植的细胞来源。

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Neural progenitor cells potentially provide a limitless, on-demand source of cells for grafting into patients with Parkinson's disease (PD) if the signals needed to control their conversion into dopamine (DA) neurons could be identified. We have recently shown that cytokines which instruct cell division and differentiation within the hematopoeitic system may provide similar functions in the central nervous system. We have shown that mitotic progenitor cells can be isolated from embryonic rat mesencephalon and that these cells respond to a combination of interleukin-1, interleukin-11, leukemia inhibitory factor, and glial cell line-derived neurotrophic factor yielding a tyrosine hydroxylase-immunoreactive (THir) phenotype in 20-25% of total cells. In the present study, 24 clonal cell lines derived from single cells of mesencephalic proliferation spheres were examined for their response to the cytokine mixture. The clone yielding the highest percentage of THir neurons (98%) was selected for further study. This clone expressed several phenotypic characteristics of DA neurons and expression of Nurr1. The response to cytokines was stable for several passages and after cryopreservation for several months. When grafted into the striatum of DA-depleted rats, these cells attenuated rotational asymmetry to the same extent as freshly harvested embryonic DA neurons. These data demonstrate that mesencephalic progenitor cells can be clonally expanded in culture and differentiated in the presence of hematopoietic cytokines to yield enriched populations of DA neurons. When transplanted, these cells provide significant functional benefit in the rat model of PD. Copyright 2001 Academic Press.
机译:如果能够识别出控制其转化为多巴胺(DA)神经元所需的信号,则神经祖细胞可能会为植入帕金森病(PD)患者提供无限量的按需细胞来源。我们最近已经表明,指示造血系统内细胞分裂和分化的细胞因子可能在中枢神经系统中提供类似的功能。我们已经证明,可以从胚胎大鼠中脑中分离出有丝分裂祖细胞,并且这些细胞对白介素-1,白介素11,白血病抑制因子和神经胶质细胞系神经营养因子的组合产生酪氨酸羟化酶免疫反应性( THir)表型占总细胞的20-25%。在本研究中,检查了源自中脑增殖球单细胞的24个克隆细胞系对细胞因子混合物的反应。选择产生最高百分比的THir神经元(98%)的克隆进行进一步研究。该克隆表达了DA神经元的几种表型特征和Nurr1的表达。对细胞因子的反应在几次传代中和冷冻保存几个月后均保持稳定。当这些细胞被移植到贫DA大鼠的纹状体中时,它们的旋转不对称性减弱程度与刚收获的胚胎DA神经元相同。这些数据表明,中脑祖细胞可以在培养中克隆扩增,并在存在造血细胞因子的情况下分化,从而产生丰富的DA神经元。移植后,这些细胞在PD大鼠模型中具有明显的功能优势。版权所有2001,学术出版社。

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