Nature Communications (May 2024)

Repression of developmental transcription factor networks triggers aging-associated gene expression in human glial progenitor cells

  • John N. Mariani,
  • Benjamin Mansky,
  • Pernille M. Madsen,
  • Dennis Salinas,
  • Deniz Kesmen,
  • Nguyen P. T. Huynh,
  • Nicholas J. Kuypers,
  • Erin R. Kesel,
  • Janna Bates,
  • Casey Payne,
  • Devin Chandler-Militello,
  • Abdellatif Benraiss,
  • Steven A. Goldman

DOI
https://doi.org/10.1038/s41467-024-48118-2
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract Human glial progenitor cells (hGPCs) exhibit diminished expansion competence with age, as well as after recurrent demyelination. Using RNA-sequencing to compare the gene expression of fetal and adult hGPCs, we identify age-related changes in transcription consistent with the repression of genes enabling mitotic expansion, concurrent with the onset of aging-associated transcriptional programs. Adult hGPCs develop a repressive transcription factor network centered on MYC, and regulated by ZNF274, MAX, IKZF3, and E2F6. Individual over-expression of these factors in iPSC-derived hGPCs lead to a loss of proliferative gene expression and an induction of mitotic senescence, replicating the transcriptional changes incurred during glial aging. miRNA profiling identifies the appearance of an adult-selective miRNA signature, imposing further constraints on the expansion competence of aged GPCs. hGPC aging is thus associated with acquisition of a MYC-repressive environment, suggesting that suppression of these repressors of glial expansion may permit the rejuvenation of aged hGPCs.