Frontiers in Cell and Developmental Biology (Nov 2023)

Single-cell analysis reveals specific neuronal transition during mouse corticogenesis

  • Ziheng Zhou,
  • Ziheng Zhou,
  • Ziheng Zhou,
  • Yueyang Pan,
  • Si Zhou,
  • Shuguang Wang,
  • Dengwei Zhang,
  • Ye Cao,
  • Ye Cao,
  • Xiaosen Jiang,
  • Jie Li,
  • Linnan Zhu,
  • Lijian Zhao,
  • Shen Gu,
  • Ge Lin,
  • Zirui Dong,
  • Zirui Dong,
  • Hai-Xi Sun

DOI
https://doi.org/10.3389/fcell.2023.1209320
Journal volume & issue
Vol. 11

Abstract

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Background: Currently, the mechanism(s) underlying corticogenesis is still under characterization.Methods: We curated the most comprehensive single-cell RNA-seq (scRNA-seq) datasets from mouse and human fetal cortexes for data analysis and confirmed the findings with co-immunostaining experiments.Results: By analyzing the developmental trajectories with scRNA-seq datasets in mice, we identified a specific developmental sub-path contributed by a cell-population expressing both deep- and upper-layer neurons (DLNs and ULNs) specific markers, which occurred on E13.5 but was absent in adults. In this cell-population, the percentages of cells expressing DLN and ULN markers decreased and increased, respectively, during the development suggesting direct neuronal transition (namely D-T-U). Whilst genes significantly highly/uniquely expressed in D-T-U cell population were significantly enriched in PTN/MDK signaling pathways related to cell migration. Both findings were further confirmed by co-immunostaining with DLNs, ULNs and D-T-U specific markers across different timepoints. Furthermore, six genes (co-expressed with D-T-U specific markers in mice) showing a potential opposite temporal expression between human and mouse during fetal cortical development were associated with neuronal migration and cognitive functions. In adult prefrontal cortexes (PFC), D-T-U specific genes were expressed in neurons from different layers between humans and mice.Conclusion: Our study characterizes a specific cell population D-T-U showing direct DLNs to ULNs neuronal transition and migration during fetal cortical development in mice. It is potentially associated with the difference of cortical development in humans and mice.

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