4.8 Article

The Lin28b-let-7-Hmga2 axis determines the higher self-renewal potential of fetal haematopoietic stem cells

Journal

NATURE CELL BIOLOGY
Volume 15, Issue 8, Pages 916-U341

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/ncb2783

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Funding

  1. National Cancer Institute of Canada (NCIC)
  2. Terry Fox Run
  3. Canadian Institutes of Health Research (CIHR)
  4. Canadian Cancer Society [700374]
  5. Terry Fox Foundation
  6. Michael Smith Foundation for Health Research (MSFHR)
  7. University of British Columbia
  8. Deutsche Forschungsgemeinschaft [KU2288/3-1]
  9. Frederick Banting and Charles Best Canada Graduate Scholarship
  10. Kay Kendall Leukemia Fund Intermediate Fellowship from the UK
  11. Deutsche Krebshilfe [109420]
  12. European Hematology Association [2010/04]

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Mouse haematopoietic stem cells (HSCs) undergo a postnatal transition in several properties, including a marked reduction in their self-renewal activity. We now show that the developmentally timed change in this key function of HSCs is associated with their decreased expression of Lin28b and an accompanying increase in their let-7 microRNA levels. Lentivirus-mediated overexpression of Lin28 in adult HSCs elevates their self-renewal activity in transplanted irradiated hosts, as does overexpression of Hmga2, a well-established let-7 target that is upregulated in fetal HSCs. Conversely, HSCs from fetal Hmga2(-/-) mice do not exhibit the heightened self-renewal activity that is characteristic of wild-type fetal HSCs. Interestingly, overexpression of Hmga2 in adult HSCs does not mimic the ability of elevated Lin28 to activate a fetal lymphoid differentiation program. Thus, Lin28b may act as a master regulator of developmentally timed changes in HSC programs with Hmga2 serving as its specific downstream modulator of HSC self-renewal potential.

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