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Childhood-Onset Schizophrenia: Insights from Induced Pluripotent Stem Cells

机译:童年期精神分裂症:诱导多能干细胞的见解。

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摘要

Childhood-onset schizophrenia (COS) is a rare psychiatric disorder characterized by earlier onset, more severe course, and poorer outcome relative to adult-onset schizophrenia (AOS). Even though, clinical, neuroimaging, and genetic studies support that COS is continuous to AOS. Early neurodevelopmental deviations in COS are thought to be significantly mediated through poorly understood genetic risk factors that may also predispose to long-term outcome. In this review, we discuss findings from induced pluripotent stem cells (iPSCs) that allow the generation of disease-relevant cell types from early brain development. Because iPSCs capture each donor’s genotype, case/control studies can uncover molecular and cellular underpinnings of COS. Indeed, recent studies identified alterations in neural progenitor and neuronal cell function, comprising dendrites, synapses, electrical activity, glutamate signaling, and miRNA expression. Interestingly, transcriptional signatures of iPSC-derived cells from patients with COS showed concordance with postmortem brain samples from SCZ, indicating that changes in vitro may recapitulate changes from the diseased brain. Considering this progress, we discuss also current caveats from the field of iPSC-based disease modeling and how to proceed from basic studies to improved diagnosis and treatment of COS.
机译:儿童发作性精神分裂症(COS)是一种罕见的精神疾病,其特征在于,与成人发作性精神分裂症(AOS)相比,其发作时间更早,病程更重且预后较差。即使临床,神经影像学和遗传学研究都支持COS与AOS连续存在。 COS的早期神经发育偏差被认为是由于人们对遗传风险因素了解不足而引起的,而遗传风险因素也可能导致长期预后。在这篇综述中,我们讨论了诱导多能干细胞(iPSC)的发现,这些发现允许从早期大脑发育中产生与疾病相关的细胞类型。因为iPSC捕获了每个供体的基因型,所以病例/对照研究可以发现COS的分子和细胞基础,实际上,最近的研究发现了神经祖细胞和神经元细胞功能的变化,包括树突,突触,电活动,谷氨酸信号转导和miRNA表达。有趣的是,来自COS患者的iPSC来源的细胞的转录特征与来自SCZ的死后大脑样本一致,表明体外变化可能概括了患病大脑的变化。考虑到这一进展,我们还将讨论基于iPSC的疾病建模领域的当前警告,以及如何从基础研究转向改善COS的诊断和治疗。

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