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Gata2 is required for HSC generation and survival

Authors :
Pater, E. (Emma) de
Kaimakis, P. (Polynikis)
Vink, C.S. (Chris)
Yokomizo, T. (Tomomasa)
Yamada-Inagawa, T. (Tomoko)
Linden, R. (Reinier) van der
Solaimani Kartalaei, P. (Parham)
Camper, S.A. (S.)
Speck, N.A. (Nancy)
Dzierzak, E.A. (Elaine)
Pater, E. (Emma) de
Kaimakis, P. (Polynikis)
Vink, C.S. (Chris)
Yokomizo, T. (Tomomasa)
Yamada-Inagawa, T. (Tomoko)
Linden, R. (Reinier) van der
Solaimani Kartalaei, P. (Parham)
Camper, S.A. (S.)
Speck, N.A. (Nancy)
Dzierzak, E.A. (Elaine)
Publication Year :
2013

Abstract

Knowledge of the key transcription factors that drive hematopoietic stem cell (HSC) generation is of particular importance for current hematopoietic regenerative approaches and reprogramming strategies. Whereas GATA2 has long been implicated as a hematopoietic transcription factor and its dysregulated expression is associated with human immunodeficiency syndromes and vascular integrity, it is as yet unknown how GATA2 functions in the generation of HSCs. HSCs are generated from endothelial cells of the major embryonic vasculature (aorta, vitelline, and umbilical arteries) and are found in intra-aortic hematopoietic clusters. In this study, we find that GATA2 function is essential for the generation of HSCs during the stage of endothelial-to-hematopoietic cell transition. Specific deletion of Gata2 in Vec (Vascular Endothelial Cadherin)-expressing endothelial cells results in a deficiency of long-term repopulating HSCs and intra-aortic cluster cells. By specific deletion of Gata2 in Vav-expressing hematopoietic cells (after HSC generation), we further show that GATA2 is essential for HSC survival. This is in contrast to the known activity of the RUNX1 transcription factor, which functions only in the generation of HSCs, and highlights the unique requirement for GATA2 function in HSCs throughout all developmental stages.

Details

Database :
OAIster
Notes :
The Journal of Experimental Medicine vol. 210 no. 13, pp. 2843-2850, English
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn957101460
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.1084.jem.20130751