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Using human induced pluripotent stem cells to model cerebellar disease: Hope and hype

机译:使用人类诱导的多能干细胞来模拟小脑疾病:希望和炒作

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The cerebellum forms a highly ordered and indispensible component of motor function within the adult neuraxis, consisting of several distinct cellular subtypes. Cerebellar disease, through a variety of genetic and acquired causes, results in the loss of function of defined subclasses of neurons, and remains a significant and untreatable health care burden. The scarcity of therapies in this arena can partially be explained by unresolved disease mechanisms due to inaccessibility of human cerebellar neurons in a relevant experimental context where initiating disease mechanisms could be functionally elucidated, or drug screens conducted. In this review we discuss the potential promise of human induced pluripotent stem cells (hiPSCs) for regenerative neurology, with a particular emphasis on in vitro modelling of cerebellar degeneration. We discuss progress made thus far using hiPSC-based models of neurodegeneration, noting the relatively slower pace of discovery made in modelling cerebellar dysfunction. We conclude by speculating how strategies attempting cerebellar differentiation from hiPSCs can be refined to allow the generation of accurate disease models. This in turn will permit a greater understanding of cerebellar pathophysiology to inform mechanistically rationalised therapies, which are desperately needed in this field.
机译:小脑在成人神经轴内形成运动功能的高度有序且不可缺少的组成部分,由几种不同的细胞亚型组成。小脑疾病通过各种遗传和后天原因导致特定神经元亚类功能的丧失,并且仍然是重大且无法治疗的医疗保健负担。由于在相关实验环境中人类小脑神经元难以接近,因此可以从功能上阐明引发疾病的机制或进行药物筛选,部分原因可能是由于尚未解决的疾病机制,因此无法解释该领域的疗法缺乏。在这篇综述中,我们讨论了人类诱导的多能干细胞(hiPSC)在再生神经病学方面的潜在前景,特别着重于小脑变性的体外建模。我们讨论了迄今为止使用基于hiPSC的神经退行性模型取得的进展,并指出在建模小脑功能障碍时发现的速度相对较慢。通过推测如何从hiPSC尝试小脑分化的策略可以完善以允许生成准确的疾病模型,我们得出结论。反过来,这将使人们对小脑病理生理有更多的了解,从而为机械合理化的治疗提供信息,这是该领域急需的。

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