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Characterization of Neurodevelopmental Abnormalities in iPSC-Derived Striatal Cultures from Patients with Huntington’s Disease

机译:表征的神经发育异常iPSC-Derived纹状体的文化从亨廷顿氏舞蹈症患者

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Background: Huntington’s disease (HD) is an inherited neurodegenerative disease and is characterized by atrophy of certain regions of the brain in a progressive manner. HD patients experience behavioral changes and uncontrolled movements which can be primarily attributed to the atrophy of striatal neurons. Previous publications describe the models of the HD striatum using induced pluripotent stem cells (iPSCs) derived from HD patients with a juvenile onset (JHD). In this model, the JHD iPSC-derived striatal cultures had altered neurodevelopment and contained a high number of nestin expressing progenitor cells at 42 days of differentiation. Objective: To further characterize the altered neurodevelopmental phenotype and evaluate potential phenotypic reversal. Methods: Differentiation of human iPSCs towards striatal fate and characterization by means of immunocytochemistry and stereological quantification. Results: Here this study demonstrates a distinct delay in the differentiation of the JHD neural progenitor population. However, reduction of the JHD aberrant progenitor populations can be accomplished either by targeting the canonical Notch signaling pathway or by treatment with HTT antisense oligonucleotides (ASOs). Conclusions: In summary, this data is postulated to reflect a potential overall developmental delay in JHD.
机译:背景:亨廷顿氏病(HD)是一个遗传性神经退行性疾病和特点是萎缩的某些地区大脑以渐进的方式。行为变化和不受控制的经验运动可以主要归因于纹状体神经元的萎缩。高清的出版物描述模型纹状体使用诱导多能干细胞(万能)来自HD患者少年发作(JHD)。纹状体的文化改变了神经发育,包含大量的巢蛋白表达祖细胞分化的42天。摘要目的:进一步确定改变的特征神经发育表型和评估潜在的表型逆转。人类对纹状体的细胞则的分化命运和描述的免疫细胞化学和stereological量化。演示了一个明显的延迟JHD神经祖细胞的分化人口。异常的祖人群通过针对规范完成Notch信号通路或治疗计画反义寡核苷酸(ASOs)。总之,这些数据是反映了一个假设潜在的JHD总体发育迟缓。

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