Scientific Reports (Jan 2021)

Essential role of autophagy in protecting neonatal haematopoietic stem cells from oxidative stress in a p62-independent manner

  • Naho Nomura,
  • Chiaki Ito,
  • Takako Ooshio,
  • Yuko Tadokoro,
  • Susumu Kohno,
  • Masaya Ueno,
  • Masahiko Kobayashi,
  • Atsuko Kasahara,
  • Yusuke Takase,
  • Kenta Kurayoshi,
  • Sha Si,
  • Chiaki Takahashi,
  • Masaaki Komatsu,
  • Toru Yanagawa,
  • Atsushi Hirao

DOI
https://doi.org/10.1038/s41598-021-81076-z
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 14

Abstract

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Abstract Autophagy is a cellular degradation system contributing to homeostasis of tissue stem cells including haematopoietic stem cells (HSCs). It plays pleiotropic roles in HSC characteristics throughout life, but its stage-specific roles in HSC self-renewal are unclear. To investigate the effects of Atg5 deletion on stage-specific HSC functions, we compared the repopulating capacity of HSCs in Atg5 f/f ;Vavi-cre mice from postnatal day (P) 0–7 weeks of age. Interestingly, Atg5 deficiency led to no remarkable abnormality in the HSC self-renewal capacity at P0, but significant defects at P7, followed by severe defects. Induction of Atg5 deletion at P5 by tamoxifen administration to Atg5 f/f ;Rosa26-Cre-ER T2 mice resulted in normal haematopoiesis, including the HSC population, until around 1 year, suggesting that Atg5 in the early neonatal period was critical for haematopoiesis in adults. Mitochondrial oxidative stress was increased by Atg5 loss in neonatal HSC/progenitor cells. Although p62 had accumulated in immature bone marrow cells of Atg5 f/f ;Vavi-cre mice, p62 deletion did not restore defective HSC functions, indicating that Atg5-dependent haematopoietic regulation in the developmental period was independent of p62. This study proposes a critical role of autophagy in HSC protection against harsh environments in the early neonatal stage, which is essential for healthy long-term haematopoiesis.