Mesoderm-derived PDGFRA+ cells regulate the emergence of hematopoietic stem cells in the dorsal aorta

Author:

Chandrakanthan VasheORCID,Rorimpandey Prunella,Zanini Fabio,Chacon Diego,Olivier Jake,Joshi Swapna,Kang Young Chan,Knezevic Kathy,Huang Yizhou,Qiao Qiao,Oliver Rema A.,Unnikrishnan AshwinORCID,Carter Daniel R.,Lee Brendan,Brownlee Chris,Power Carl,Brink Robert,Mendez-Ferrer SimonORCID,Enikolopov Grigori,Walsh William,Göttgens BertholdORCID,Taoudi Samir,Beck Dominik,Pimanda John E.ORCID

Abstract

AbstractMouse haematopoietic stem cells (HSCs) first emerge at embryonic day 10.5 (E10.5), on the ventral surface of the dorsal aorta, by endothelial-to-haematopoietic transition. We investigated whether mesenchymal stem cells, which provide an essential niche for long-term HSCs (LT-HSCs) in the bone marrow, reside in the aorta–gonad–mesonephros and contribute to the development of the dorsal aorta and endothelial-to-haematopoietic transition. Here we show that mesoderm-derived PDGFRA+ stromal cells (Mesp1der PSCs) contribute to the haemogenic endothelium of the dorsal aorta and populate the E10.5–E11.5 aorta–gonad–mesonephros but by E13.5 were replaced by neural-crest-derived PSCs (Wnt1der PSCs). Co-aggregating non-haemogenic endothelial cells with Mesp1der PSCs but not Wnt1der PSCs resulted in activation of a haematopoietic transcriptional programme in endothelial cells and generation of LT-HSCs. Dose-dependent inhibition of PDGFRA or BMP, WNT and NOTCH signalling interrupted this reprogramming event. Together, aorta–gonad–mesonephros Mesp1der PSCs could potentially be harnessed to manufacture LT-HSCs from endothelium.

Funder

Department of Health | National Health and Medical Research Council

Department of Education and Training | Australian Research Council

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology

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