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利用单细胞RNA测序和电生理学预测人诱导多能干细胞衍生神经元的功能状态。

Predicting the functional states of human iPSC-derived neurons with single-cell RNA-seq and electrophysiology.

作者信息

Bardy C, van den Hurk M, Kakaradov B, Erwin J A, Jaeger B N, Hernandez R V, Eames T, Paucar A A, Gorris M, Marchand C, Jappelli R, Barron J, Bryant A K, Kellogg M, Lasken R S, Rutten B P F, Steinbusch H W M, Yeo G W, Gage F H

机构信息

Salk Institute for Biological Studies, Stanford Consortium for Regenerative Medicine, La Jolla, CA, USA.

SAHMRI Mind & Brain, Laboratory for Human Neurophysiology and Genetics, School of Medicine Flinders University, Adelaide, SA, Australia.

出版信息

Mol Psychiatry. 2016 Nov;21(11):1573-1588. doi: 10.1038/mp.2016.158. Epub 2016 Oct 4.

DOI:10.1038/mp.2016.158
PMID:27698428
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5071135/
Abstract

Human neural progenitors derived from pluripotent stem cells develop into electrophysiologically active neurons at heterogeneous rates, which can confound disease-relevant discoveries in neurology and psychiatry. By combining patch clamping, morphological and transcriptome analysis on single-human neurons in vitro, we defined a continuum of poor to highly functional electrophysiological states of differentiated neurons. The strong correlations between action potentials, synaptic activity, dendritic complexity and gene expression highlight the importance of methods for isolating functionally comparable neurons for in vitro investigations of brain disorders. Although whole-cell electrophysiology is the gold standard for functional evaluation, it often lacks the scalability required for disease modeling studies. Here, we demonstrate a multimodal machine-learning strategy to identify new molecular features that predict the physiological states of single neurons, independently of the time spent in vitro. As further proof of concept, we selected one of the potential neurophysiological biomarkers identified in this study-GDAP1L1-to isolate highly functional live human neurons in vitro.

摘要

源自多能干细胞的人类神经祖细胞以异质速率发育成具有电生理活性的神经元,这可能会混淆神经学和精神病学中与疾病相关的发现。通过结合对体外单个人类神经元的膜片钳记录、形态学和转录组分析,我们定义了一个从功能较差到功能高度活跃的连续电生理状态的分化神经元。动作电位、突触活动、树突复杂性和基因表达之间的强相关性突出了分离功能可比的神经元用于脑部疾病体外研究的方法的重要性。尽管全细胞膜片钳电生理是功能评估的金标准,但它往往缺乏疾病建模研究所需要的可扩展性。在这里,我们展示了一种多模态机器学习策略,以识别预测单个神经元生理状态的新分子特征,而与体外培养时间无关。作为概念的进一步验证,我们选择了本研究中确定的潜在神经生理生物标志物之一——GDAP1L1,以在体外分离功能高度活跃的活人类神经元。

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