4.8 Article

Haematopoietic stem cell induction by somite-derived endothelial cells controlled by meox1

Journal

NATURE
Volume 512, Issue 7514, Pages 314-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nature13678

Keywords

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Funding

  1. National Health and Medical Research Council of Australia (NHMRC)
  2. Australian Research Council
  3. Cancer Institute NSW (CINSW)
  4. Australian Postgraduate Award
  5. NHMRC
  6. CINSW
  7. RT Hall Foundation
  8. State Government of Victoria
  9. Australian Federal Government

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Haematopoietic stem cells (HSCs) are self-renewing stem cells capable of replenishing all blood lineages. In all vertebrate embryos that have been studied, definitive HSCs are generated initially within the dorsal aorta (DA) of the embryonic vasculature by a series of poorly understood inductive events(1-3). Previous studies have identified that signalling relayed from adjacent somites coordinates HSC induction, but the nature of this signal has remained elusive(4). Here we reveal that somite specification of HSCs occurs via the deployment of a specific endothelial precursor population, which arises within a sub-compartment of the zebrafish somite that we have defined as the endotome. Endothelial cells of the endotomeare specified within the nascent somite by the activity of the homeobox genemeox(1). Specified endotomal cells consequently migrate and colonize the DA, where they induce HSC formation through the deployment of chemokine signalling activated in these cells during endotome formation. Loss of meox(1) activity expands the endotome at the expense of a second somitic cell type, the muscle precursors of the dermomyotomal equivalent in zebrafish, the external cell layer. The resulting increase in endotome-derived cells that migrate to colonize the DA generates a dramatic increase in chemokine-dependent HSC induction. This study reveals the molecular basis for a novel somite lineage restriction mechanism and defines a new paradigm in induction of definitive HSCs.

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