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Develop a 3D neurological disease model of human cortical glutamatergic neurons using micropillar-based scaffolds

机译:使用基于微柱的支架开发人类皮质谷氨酸能神经元的3D神经疾病模型

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摘要

Establishing an effective three-dimensional (3D) in vitro culture system to better model human neurological diseases is desirable, since the human brain is a 3D structure. Here, we demonstrated the development of a polydimethylsiloxane (PDMS) pillar-based 3D scaffold that mimicked the 3D microenvironment of the brain. We utilized this scaffold for the growth of human cortical glutamatergic neurons that were differentiated from human pluripotent stem cells. In comparison with the 2D culture, we demonstrated that the developed 3D culture promoted the maturation of human cortical glutamatergic neurons by showing significantly more MAP2 and less Ki67 expression. Based on this 3D culture system, we further developed an in vitro disease-like model of traumatic brain injury (TBI), which showed a robust increase of glutamate-release from the neurons, in response to mechanical impacts, recapitulating the critical pathology of TBI. The increased glutamate-release from our 3D culture model was attenuated by the treatment of neural protective drugs, memantine or nimodipine. The established 3D in vitro human neural culture system and TBI-like model may be used to facilitate mechanistic studies and drug screening for neurotrauma or other neurological diseases.
机译:由于人脑是3D结构,因此建立一种有效的三维(3D)体外培养系统以更好地模拟人类神经疾病是人们所期望的。在这里,我们演示了模仿大脑3D微环境的基于聚二甲基硅氧烷(PDMS)支柱的3D支架的开发。我们利用这种支架的人类皮层谷氨酸能神经元的增长与人类多能干细胞分化。与2D文化相比,我们证明了发达的3D文化通过显示明显更多的MAP2和更少的Ki67表达来促进人类皮质谷氨酸能神经元的成熟。基于此3D培养系统,我们进一步开发了创伤性脑损伤(TBI)的体外疾病样模型,该模型显示了对机械冲击的响应,神经元中谷氨酸释放的强劲增加,概括了TBI的关键病理。神经保护剂美金刚或尼莫地平的治疗减弱了我们3D培养模型中谷氨酸释放的增加。建立的3D体外人类神经培养系统和TBI样模型可用于促进神经损伤或其他神经系统疾病的机理研究和药物筛选。

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