Cell Death and Dis：适用于研究帕金森病神经退行性变的新模型

2019-12-10 QQY MedSci原创

帕金森病的一个主要特征是黑质致密带（SNpc）多巴胺能神经元的丧失。但这种相对选择性的神经退行性变的病理生理机制尚不明确，因此需要研究多巴胺能神经元功能障碍的实验系统。而诱导多能干细胞（iPSC）向多巴胺能神经元分化的实验也为获得人源性的多巴胺能神经元提供了宝贵的来源。但就目前可用的实验方案而言，将人源hiPSC诱导成多巴胺能神经元的产量也有所不同。在本研究中，研究人员开发了一种基于HBA启动子驱

帕金森病的一个主要特征是黑质致密带（SNpc）多巴胺能神经元的丧失。但这种相对选择性的神经退行性变的病理生理机制尚不明确，因此需要研究多巴胺能神经元功能障碍的实验系统。而诱导多能干细胞（iPSC）向多巴胺能神经元分化的实验也为获得人源性的多巴胺能神经元提供了宝贵的来源。

但就目前可用的实验方案而言，将人源hiPSC诱导成多巴胺能神经元的产量也有所不同。在本研究中，研究人员开发了一种基于HBA启动子驱动的转录因子瞬时表达的方案，通过腺相关病毒(AAV)载体，能够从四种不同的人iPSC系获得数量一样的多巴胺能神经元。

研究人员还证明了AAV载体表达的来自神经元特异性hSyn1启动子的报告基因可用来充当hiPSC诱导分化的多巴胺能神经元成熟的标记。

通过转录因子表达诱导分化的多巴胺能神经元，在α-突触核蛋白（α-synuclein）过表达时，可发生神经变性加剧，但对γ-突触核蛋白（γ-synuclein）过表达不敏感，该结果提示这些诱导分化出的神经元非常适合研究帕金森病背景下的神经变性。

原始出处：

Mahajani et al. Homogenous generation of dopaminergic neurons from multiple hiPSC lines by transient expression of transcription factors.Cell Death and Disease ( 2019) 10：898

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2020-04-13 cmj8wellington

#Dis#

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2020-04-16 维他命

#CEL#

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2020-07-01 liuyiping

#神经退行性变#

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2020-07-02 12498b37m72暂无昵称

#神经退行#

79 0
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2020-07-28 zhaozhouchifen

#Cell#

89 0
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2019-12-12 cy0328

#Death#

61 0
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2019-12-10 CHANGE

梅斯里提供了很多疾病的模型计算公式，赞一个！

89 0

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