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单细胞分析揭示了人类皮质中神经祖细胞的转录异质性。

Single-cell analysis reveals transcriptional heterogeneity of neural progenitors in human cortex.

作者信息

Johnson Matthew B, Wang Peter P, Atabay Kutay D, Murphy Elisabeth A, Doan Ryan N, Hecht Jonathan L, Walsh Christopher A

机构信息

1] Division of Genetics and Genomics, Boston Children's Hospital, Boston, Massachusetts, USA. [2] Manton Center for Orphan Disease Research, Boston Children's Hospital, Boston, Massachusetts, USA. [3] Howard Hughes Medical Institute, Boston Children's Hospital, Boston, Massachusetts, USA.

1] Department of Pathology, Beth Israel Deaconess Medical Center, Boston, Massachusetts, USA. [2] Department of Pathology, Harvard Medical School, Boston, Massachusetts, USA.

出版信息

Nat Neurosci. 2015 May;18(5):637-46. doi: 10.1038/nn.3980. Epub 2015 Mar 3.

Abstract

The human cerebral cortex depends for its normal development and size on a precisely controlled balance between self-renewal and differentiation of diverse neural progenitor cells. Specialized progenitors that are common in humans but virtually absent in rodents, called outer radial glia (ORG), have been suggested to be crucial to the evolutionary expansion of the human cortex. We combined progenitor subtype-specific sorting with transcriptome-wide RNA sequencing to identify genes enriched in human ORG, which included targets of the transcription factor neurogenin and previously uncharacterized, evolutionarily dynamic long noncoding RNAs. Activating the neurogenin pathway in ferret progenitors promoted delamination and outward migration. Finally, single-cell transcriptional profiling in human, ferret and mouse revealed more cells coexpressing proneural neurogenin targets in human than in other species, suggesting greater neuronal lineage commitment and differentiation of self-renewing progenitors. Thus, we find that the abundance of human ORG is paralleled by increased transcriptional heterogeneity of cortical progenitors.

摘要

人类大脑皮层的正常发育和大小取决于多种神经祖细胞自我更新与分化之间精确控制的平衡。一种在人类中常见但在啮齿动物中几乎不存在的特殊祖细胞,称为外放射状胶质细胞(ORG),被认为对人类皮层的进化扩张至关重要。我们将祖细胞亚型特异性分选与全转录组RNA测序相结合,以鉴定在人类ORG中富集的基因,其中包括转录因子神经生成素的靶标以及先前未表征的、具有进化动态性的长链非编码RNA。在雪貂祖细胞中激活神经生成素途径可促进脱层和向外迁移。最后,对人类、雪貂和小鼠进行的单细胞转录谱分析显示,与其他物种相比,人类中更多细胞共表达神经生成素的神经前体靶标,这表明自我更新祖细胞的神经元谱系定向和分化程度更高。因此,我们发现人类ORG的丰度与皮层祖细胞转录异质性的增加是平行的。

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