4.8 Article

Transcriptional networks identify synaptotagmin-like 3 as a regulator of cortical neuronal migration during early neurodevelopment

Journal

CELL REPORTS
Volume 34, Issue 9, Pages -

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2021.108802

Keywords

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Categories

Funding

  1. National Key Research and Development Program of China [2018YFA0108000, 2016YFC0905100]
  2. National Natural Science Foundation of China [81974174, 81571471, 81501289]
  3. Natural Science Foundation of Shanghai [17ZR1448500]
  4. Excellent Medical Talents Training Program of Shanghai [2017YQ074]
  5. Shen Kang Hospital Development Center of Shanghai [SHDC12017110]
  6. Municipal Health and Family Planning Committee of Shanghai [20174Y0026]

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SYTL3, identified as a top driver of early human brain development, plays a crucial role in regulating cortical neuronal migration in both human and mouse developing brains. Its high activity but low expression levels are key factors in this process.
Human brain development is a complex process involving neural proliferation, differentiation, and migration that are directed by many essential cellular factors and drivers. Here, using the NetBID2 algorithm and developing human brain RNA sequencing dataset, we identify synaptotagmin-like 3 (SYTL3) as one of the top drivers of early human brain development. Interestingly, SYTL3 exhibits high activity but low expression in both early developmental human cortex and human embryonic stem cell (hESC)-derived neurons. Knockout of SYTL3 (SYTL3-KO) in human neurons or knockdown of Sytl3 in embryonic mouse cortex markedly promotes neuronal migration. SYTL3-KO causes an abnormal distribution of deep-layer neurons in brain organoids and reduces presynaptic neurotransmitter release in hESC-derived neurons. We further demonstrate that SYTL3-KO-accelerated neuronal migration is modulated by high expression of matrix metalloproteinases. Together, based on bioinformatics and biological experiments, we identify SYTL3 as a regulator of cortical neuronal migration in human and mouse developing brains.

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