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Human ESC-Derived Dopamine Neurons Show Similar Preclinical Efficacy and Potency to Fetal Neurons when Grafted in a Rat Model of Parkinson's Disease

机译:在帕金森氏病大鼠模型中移植人类ESC衍生的多巴胺神经元显示出与胎儿神经元相似的临床前功效和效力

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Considerable progress has been made in generating fully functional and transplantable dopamine neurons from human embryonic stem cells (hESCs). Before these cells can be used for cell replacement therapy in Parkinson's disease (PD), it is important to verify their functional properties and efficacy in animal models. Here we provide a comprehensive preclinical assessment of hESC-derived midbrain dopamine neurons in a rat model of PD. We show long-term survival and functionality using clinically relevant MRI and PET imaging techniques and demonstrate efficacy in restoration of motor function with a potency comparable to that seen with human fetal dopamine neurons. Furthermore, we show that hESC-derived dopamine neurons can project sufficiently long distances for use in humans, fully regenerate midbrain-to-forebrain projections, and innervate correct target structures. This provides strong preclinical support for clinical translation of hESC-derived dopamine neurons using approaches similar to those established with fetal cells for the treatment of Parkinson's disease.
机译:从人类胚胎干细胞(hESCs)生成功能齐全且可移植的多巴胺神经元方面已经取得了可观的进展。在将这些细胞用于帕金森氏病(PD)的细胞替代治疗之前,重要的是要在动物模型中验证其功能特性和功效。在这里,我们提供了PD大鼠模型中hESC衍生的中脑多巴胺神经元的全面临床前评估。我们显示了使用临床相关的MRI和PET成像技术的长期生存和功能,并展示了在恢复运动功能方面的功效,其效力与人类胎儿多巴胺神经元相当。此外,我们表明,hESC衍生的多巴胺神经元可以投射足够长的距离供人类使用,充分再生中脑到前脑的投影,并支配正确的目标结构。这为使用hESC来源的多巴胺神经元的临床翻译提供了强有力的临床前支持,使用的方法与用胎儿细胞建立的方法相似,可用于治疗帕金森氏病。

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