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Use of induced pluripotent stem cell derived neurons engineered to express BDNF for modulation of stressor related pathology

机译:工程化表达BDNF的诱导多能干细胞衍生神经元在调节应激相关病理学中的用途

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摘要

Combined cell and gene-based therapeutic strategies offer potential in the treatment of neurodegenerative and psychiatric conditions that have been associated with structural brain disturbances. In the present investigation, we used a novel virus-free re-programming method to generate induced pluripotent stem cells (iPSCs), and then subsequently transformed these cells into neural cells which over-expressed brain derived neurotrophic factor (BDNF). Importantly, the infusion of iPSC derived neural cells (as a cell replacement and gene delivery tool) and BDNF (as a protective factor) influenced neuronal outcomes. Specifically, intracerebroventricular transplantation of iPSC-derived neural progenitors that over-expressed BDNF reversed the impact of immune (lipopolysaccharide) and chronic stressor challenges upon subventricular zone adult neurogenesis, and the iPSC-derived neural progenitor cells alone blunted the stressor-induced corticosterone response. Moreover, our findings indicate that mature dopamine producing neurons can be generated using iPSC procedures and appear to be viable when infused in vivo. Taken together, these data could have important implications for using gene-plus-cell replacement methods to modulate stressor related pathology.
机译:基于细胞和基因的组合治疗策略为治疗与结构性脑部疾病相关的神经变性和精神疾病提供了潜力。在本研究中,我们使用了一种新颖的无病毒重编程方法来生成诱导性多能干细胞(iPSC),然后将这些细胞转化为过表达脑源性神经营养因子(BDNF)的神经细胞。重要的是,输注iPSC衍生的神经细胞(作为细胞替代和基因传递工具)和BDNF(作为保护因子)影响了神经元的预后。具体来说,过度表达BDNF的iPSC衍生的神经祖细胞的脑室内移植逆转了免疫(脂多糖)和慢性应激源对成年脑室下层神经发生的影响,而仅iPSC衍生的神经祖细胞则使应激源诱导的皮质酮反应减弱。此外,我们的发现表明,可以使用iPSC程序生成成熟的产生多巴胺的神经元,并且在体内注入时似乎是可行的。综上所述,这些数据可能对使用基因加细胞置换方法调节应激相关病理具有重要意义。

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