Long-term maturation of human cortical organoids matches key early postnatal transitions

被引:0
|
作者
Aaron Gordon
Se-Jin Yoon
Stephen S. Tran
Christopher D. Makinson
Jin Young Park
Jimena Andersen
Alfredo M. Valencia
Steve Horvath
Xinshu Xiao
John R. Huguenard
Sergiu P. Pașca
Daniel H. Geschwind
机构
[1] University of California Los Angeles,Department of Neurology, David Geffen School of Medicine
[2] Stanford University,Department of Psychiatry and Behavioral Sciences
[3] Stanford University,Stanford Brain Organogenesis, Wu Tsai Neurosciences Institute
[4] University of California San Diego,Department of Psychiatry
[5] University of California Los Angeles,Department of Integrative Biology
[6] Stanford University School of Medicine,Department of Neurology and Neurological Sciences
[7] University of California Los Angeles,Department of Biostatistics, Fielding School of Public Health
[8] University of California,Department of Human Genetics, David Geffen School of Medicine
[9] University of California Los Angeles,Molecular Biology Institute
[10] University of California Los Angeles,Institute for Quantitative and Computational Biology
[11] University of California Los Angeles,Program in Neurobehavioral Genetics, Semel Institute, David Geffen School of Medicine
[12] University of California Los Angeles,Center for Autism Research and Treatment, Semel Institute, David Geffen School of Medicine
来源
Nature Neuroscience | 2021年 / 24卷
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摘要
Human stem-cell-derived models provide the promise of accelerating our understanding of brain disorders, but not knowing whether they possess the ability to mature beyond mid- to late-fetal stages potentially limits their utility. We leveraged a directed differentiation protocol to comprehensively assess maturation in vitro. Based on genome-wide analysis of the epigenetic clock and transcriptomics, as well as RNA editing, we observe that three-dimensional human cortical organoids reach postnatal stages between 250 and 300 days, a timeline paralleling in vivo development. We demonstrate the presence of several known developmental milestones, including switches in the histone deacetylase complex and NMDA receptor subunits, which we confirm at the protein and physiological levels. These results suggest that important components of an intrinsic in vivo developmental program persist in vitro. We further map neurodevelopmental and neurodegenerative disease risk genes onto in vitro gene expression trajectories to provide a resource and webtool (Gene Expression in Cortical Organoids, GECO) to guide disease modeling.
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页码:331 / 342
页数:11
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