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Shared effects of DISC1 disruption and elevated WNT signaling in human cerebral organoids

机译:DISC1破坏和人脑类器官中WNT信号升高的共同作用

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The development of three-dimensional culture methods has allowed for the study of developing cortical morphology in human cells. This provides a new tool to study the neurodevelopmental consequences of disease-associated mutations. Here, we study the effects of isogenic DISC1 mutation in cerebral organoids. DISC1 has been implicated in psychiatric disease based on genetic studies, including its interruption by a balanced translocation that increases the risk of major mental illness. Isogenic wild-type and DISC1 -disrupted human-induced pluripotent stem cells were used to generate cerebral organoids, which were then examined for morphology and gene expression. We show that DISC1 -mutant cerebral organoids display disorganized structural morphology and impaired proliferation, which is phenocopied by WNT agonism and rescued by WNT antagonism. Furthermore, there are many shared changes in gene expression with DISC1 disruption and WNT agonism, including in neural progenitor and cell fate markers, regulators of neuronal migration, and interneuron markers. These shared gene expression changes suggest mechanisms for the observed morphologic dysregulation with DISC1 disruption and points to new avenues for future studies. The shared changes in three-dimensional cerebral organoid morphology and gene expression with DISC1 interruption and WNT agonism further strengthens the link between DISC1 mutation, abnormalities in WNT signaling, and neuropsychiatric disease.
机译:三维培养方法的发展允许研究人类细胞中皮质形态的发展。这提供了一种研究疾病相关突变的神经发育后果的新工具。在这里,我们研究了脑类器官中同基因DISC1突变的影响。根据基因研究,DISC1与精神疾病有关,包括因平衡易位而中断DISC1,增加重大精神疾病的风险。等基因野生型和DISC1破坏的人类诱导的多能干细胞用于生成脑类器官,然后检查其形态和基因表达。我们表明,DISC1突变的大脑类器官显示混乱的结构形态和受损的增殖,这是由WNT激动表型复制并由WNT拮抗作用挽救的。此外,在DISC1破坏和WNT激动的情况下,基因表达存在许多共同的变化,包括神经祖细胞和细胞命运标志物,神经元迁移的调节剂和中间神经元标志物。这些共有的基因表达变化提示了观察到的DISC1破坏引起的形态失调的机制,并为将来的研究指明了新的途径。三维大脑类器官的形态和基因表达与DISC1中断和WNT激动的共同变化进一步加强了DISC1突变,WNT信号异常和神经精神病之间的联系。

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