人诱导多能干细胞衍生的神经元揭示了Ras信号增强在科斯特洛综合征中的影响。
Human iPS Cell-Derived Neurons Uncover the Impact of Increased Ras Signaling in Costello Syndrome.
作者信息
Rooney Gemma E, Goodwin Alice F, Depeille Philippe, Sharir Amnon, Schofield Claude M, Yeh Erika, Roose Jeroen P, Klein Ophir D, Rauen Katherine A, Weiss Lauren A, Ullian Erik M
机构信息
Departments of Ophthalmology.
Orofacial Sciences.
出版信息
J Neurosci. 2016 Jan 6;36(1):142-52. doi: 10.1523/JNEUROSCI.1547-15.2016.
UNLABELLED
Increasing evidence implicates abnormal Ras signaling as a major contributor in neurodevelopmental disorders, yet how such signaling causes cortical pathogenesis is unknown. We examined the consequences of aberrant Ras signaling in the developing mouse brain and uncovered several critical phenotypes, including increased production of cortical neurons and morphological deficits. To determine whether these phenotypes are recapitulated in humans, we generated induced pluripotent stem (iPS) cell lines from patients with Costello syndrome (CS), a developmental disorder caused by abnormal Ras signaling and characterized by neurodevelopmental abnormalities, such as cognitive impairment and autism. Directed differentiation toward a neuroectodermal fate revealed an extended progenitor phase and subsequent increased production of cortical neurons. Morphological analysis of mature neurons revealed significantly altered neurite length and soma size in CS patients. This study demonstrates the synergy between mouse and human models and validates the use of iPS cells as a platform to study the underlying cellular pathologies resulting from signaling deficits.
SIGNIFICANCE STATEMENT
Increasing evidence implicates Ras signaling dysfunction as a major contributor in psychiatric and neurodevelopmental disorders, such as cognitive impairment and autism, but the underlying cortical cellular pathogenesis remains unclear. This study is the first to reveal human neuronal pathogenesis resulting from abnormal Ras signaling and provides insights into how these phenotypic abnormalities likely contribute to neurodevelopmental disorders. We also demonstrate the synergy between mouse and human models, thereby validating the use of iPS cells as a platform to study underlying cellular pathologies resulting from signaling deficits. Recapitulating human cellular pathologies in vitro facilitates the future high throughput screening of potential therapeutic agents that may reverse phenotypic and behavioral deficits.
未标注
越来越多的证据表明,异常的Ras信号传导是神经发育障碍的主要促成因素,但这种信号传导如何导致皮质病变尚不清楚。我们研究了发育中小鼠大脑中异常Ras信号传导的后果,发现了几种关键表型,包括皮质神经元生成增加和形态缺陷。为了确定这些表型是否在人类中重现,我们从科斯特洛综合征(CS)患者中生成了诱导多能干细胞(iPS)系,CS是一种由异常Ras信号传导引起的发育障碍,其特征是神经发育异常,如认知障碍和自闭症。定向分化为神经外胚层命运显示祖细胞阶段延长,随后皮质神经元生成增加。对成熟神经元的形态分析显示,CS患者的神经突长度和胞体大小有显著改变。这项研究证明了小鼠和人类模型之间的协同作用,并验证了使用iPS细胞作为研究信号缺陷导致的潜在细胞病理学的平台。
意义声明
越来越多的证据表明,Ras信号传导功能障碍是精神和神经发育障碍(如认知障碍和自闭症)的主要促成因素,但潜在的皮质细胞发病机制仍不清楚。这项研究首次揭示了由异常Ras信号传导导致的人类神经元发病机制,并深入了解了这些表型异常可能如何导致神经发育障碍。我们还证明了小鼠和人类模型之间的协同作用,从而验证了使用iPS细胞作为研究信号缺陷导致的潜在细胞病理学的平台。在体外重现人类细胞病理学有助于未来高通量筛选可能逆转表型和行为缺陷的潜在治疗药物。
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