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Modeling heterogeneous patients with a clinical diagnosis of schizophrenia with induced pluripotent stem cells

机译:用诱导性多能干细胞对异型患者进行临床诊断的精神分裂症建模

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摘要

Schizophrenia (SZ) is a devastating complex genetic mental condition that is heterogeneous in terms of clinical etiologies, symptoms, and outcomes. Despite decades of postmortem, neuroimaging, pharmacological, and genetic studies of patients, in addition to animal models, much of the biological mechanisms that underlie the pathology of SZ remain unknown. The ability to reprogram adult somatic cells into human induced pluripotent stem cells (hiPSCs) provides a new tool that supplies live human neurons for modeling complex genetic conditions such as SZ. The purpose of this review is to discuss the technical and clinical constraints currently limiting hiPSC-based studies. We posit that reducing the clinical heterogeneity of hiPSC-based studies, by selecting subjects with common clinical manifestations or rare genetic variants, will help our ability to draw meaningful insights from the necessarily small patient cohorts that can be studied at this time.
机译:精神分裂症(SZ)是一种破坏性的复杂遗传性心理疾病,在临床病因,症状和预后方面均不相同。尽管进行了数十年的事后尸检,神经影像学,药理学和遗传学研究,除了动物模型之外,SZ病理基础的许多生物学机制仍然未知。将成人体细胞重编程为人诱导多能干细胞(hiPSC)的能力提供了一种新工具,可为模拟复杂遗传条件(例如SZ)提供活人神经元。这篇综述的目的是讨论目前限制基于hiPSC的研究的技术和临床限制。我们认为,通过选择具有常见临床表现或罕见遗传变异的受试者,降低基于hiPSC的研究的临床异质性,将有助于我们从目前可以研究的必要的小型患者队列中得出有意义的见解。

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