A single microRNA miR-195 rescues the arrested B cell development induced by EBF1 deficiency

  1. Y. Miyatake
  2. T. Ikawa
  3. R. Yanagiya
  4. R. Kotaki
  5. K. Kameda
  6. R. Koyama-Nasu
  7. K. Okuyama
  8. K. Hirano
  9. H. Hosokawa
  10. K. Hozumi
  11. M. Ohtsuka
  12. T. Kishikawa
  13. C. Shibata
  14. M. Otsuka
  15. R. Maruyama
  16. K. Ando
  17. T. Kurosaki
  18. H. Kawamoto
  19. A. Kotani
4 evaluations Published on
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Abstract

Accumulated studies have reported that hematopoietic differentiation was primarily regulated by transcription factors. Early B cell factor 1 (EBF1) is an essential transcription factor for B lymphopoiesis. Contrary to the canonical notion, we found that a single miRNA, miRNA-195 (miR-195) transduction let EBF1 deficient hematopoietic progenitor cells (HPCs) express CD19, carry out V(D)J recombination and class switch recombination, which implied that B cell matured without EBF1. A part of the mechanism was caused by FOXO1 accumulation via inhibition of FOXO1 phosphorylation pathways in which targets of miR-195 are enriched. These results suggested that some miRNA transductions could function as alternatives to transcription factors.

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