Runx1+ vascular smooth muscle cells are essential for hematopoietic stem and progenitor cell development in vivo

Author:

Gonzalez Galofre Zaniah N.ORCID,Kilpatrick Alastair M.ORCID,Marques MadalenaORCID,Sá da Bandeira DianaORCID,Ventura Telma,Gomez Salazar Mario,Bouilleau Léa,Marc Yvan,Barbosa Ana B.,Rossi Fiona,Beltran Mariana,van de Werken Harmen J. G.ORCID,van IJcken Wilfred F. J.ORCID,Henderson Neil C.ORCID,Forbes Stuart J.ORCID,Crisan MihaelaORCID

Abstract

AbstractHematopoietic stem cells (HSCs) produce all essential cellular components of the blood. Stromal cell lines supporting HSCs follow a vascular smooth muscle cell (vSMC) differentiation pathway, suggesting that some hematopoiesis-supporting cells originate from vSMC precursors. These pericyte-like precursors were recently identified in the aorta-gonad-mesonephros (AGM) region; however, their role in the hematopoietic development in vivo remains unknown. Here, we identify a subpopulation of NG2+Runx1+ perivascular cells that display a sclerotome-derived vSMC transcriptomic profile. We show that deleting Runx1 in NG2+ cells impairs the hematopoietic development in vivo and causes transcriptional changes in pericytes/vSMCs, endothelial cells and hematopoietic cells in the murine AGM. Importantly, this deletion leads also to a significant reduction of HSC reconstitution potential in the bone marrow in vivo. This defect is developmental, as NG2+Runx1+ cells were not detected in the adult bone marrow, demonstrating the existence of a specialised pericyte population in the HSC-generating niche, unique to the embryo.

Funder

European Hematology Association

Academy of Medical Sciences

Association Française contre les Myopathies

Wellcome Trust

British Heart Foundation

This work has made use of the resources provided by the Edinburgh Compute and Data Facility (ECDF).

Publisher

Springer Science and Business Media LLC

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