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Human Motor Neuron Progenitor Transplantation Leads to Endogenous Neuronal Sparing in 3 Models of Motor Neuron Loss

机译:人类运动神经元祖细胞移植导致3种运动神经元丢失模型中的内源性神经元备用。

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Motor neuron loss is characteristic of many neurodegenerative disorders and results in rapid loss of muscle control, paralysis, and eventual death in severe cases. In order to investigate the neurotrophic effects of a motor neuron lineage graft, we transplanted human embryonic stem cell-derived motor neuron progenitors (hMNPs) and examined their histopathological effect in three animal models of motor neuron loss. Specifically, we transplanted hMNPs into rodent models of SMA (Δ7SMN), ALS (SOD1 G93A), and spinal cord injury (SCI). The transplanted cells survived and differentiated in all models. In addition, we have also found that hMNPs secrete physiologically active growth factorsin vivo, including NGF and NT-3, which significantly enhanced the number of spared endogenous neurons in all three animal models. The ability to maintain dying motor neurons by delivering motor neuron-specific neurotrophic support represents a powerful treatment strategy for diseases characterized by motor neuron loss.
机译:运动神经元丧失是许多神经退行性疾病的特征,并导致严重情况下肌肉控制,瘫痪和最终死亡的迅速丧失。为了研究运动神经元谱系移植物的神经营养作用,我们移植了人类胚胎干细胞衍生的运动神经元祖细胞(hMNPs),并在三种运动神经元缺失动物模型中检查了它们的组织病理学作用。具体来说,我们将hMNPs移植到了SMA(Δ7SMN),ALS(SOD1 G93A)和脊髓损伤(SCI)的啮齿动物模型中。移植的细胞在所有模型中均存活并分化。此外,我们还发现hMNP在体内分泌具有生理活性的生长因子,包括NGF和NT-3,这在所有三种动物模型中均显着增加了剩余的内源性神经元的数量。通过提供运动神经元特异性神经营养支持维持垂死的运动神经元的能力代表了以运动神经元丧失为特征的疾病的有效治疗策略。

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