Author:
Serina Secanechia Yasmin Natalia,Bergiers Isabelle,Rogon Matt,Arnold Christian,Descostes Nicolas,Le Stephanie,López-Anguita Natalia,Ganter Kerstin,Kapsali Chrysi,Bouilleau Lea,Gut Aaron,Uzuotaite Auguste,Aliyeva Ayshan,Zaugg Judith B.,Lancrin Christophe
Abstract
AbstractProgress in the generation of Hematopoietic Stem and Progenitor Cells (HSPCs) in vitro and ex vivo has been built on the knowledge of developmental hematopoiesis, underscoring the importance of understanding this process. HSPCs emerge within the embryonic vasculature through an Endothelial-to-Hematopoietic Transition (EHT). The transcriptional regulator Tal1 exerts essential functions in the earliest stages of blood development, but is considered dispensable for the EHT. Nevertheless, Tal1 is expressed with its binding partner Lmo2 and it homologous Lyl1 in endothelial and transitioning cells at the time of EHT. Here, we investigated the function of these genes using a mouse embryonic-stem cell (mESC)-based differentiation system to model hematopoietic development. We showed for the first time that the expression of TAL1 in endothelial cells is crucial to ensure the efficiency of the EHT process and a sustained hematopoietic output. Our findings uncover an important function of Tal1 during the EHT, thus filling the current gap in the knowledge of the role of this master gene throughout the whole process of hematopoietic development.
Funder
European Molecular Biology Laboratory
European Molecular Biology Laboratory (EMBL)
Publisher
Springer Science and Business Media LLC
Cited by
2 articles.
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