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HOXB4 Promotes Hemogenic Endothelium Formation without Perturbing Endothelial Cell Development.


ABSTRACT: Generation of hematopoietic stem cells (HSCs) from pluripotent stem cells, in vitro, holds great promise for regenerative therapies. Primarily, this has been achieved in mouse cells by overexpression of the homeotic selector protein HOXB4. The exact cellular stage at which HOXB4 promotes hematopoietic development, in vitro, is not yet known. However, its identification is a prerequisite to unambiguously identify the molecular circuits controlling hematopoiesis, since the activity of HOX proteins is highly cell and context dependent. To identify that stage, we retrovirally expressed HOXB4 in differentiating mouse embryonic stem cells (ESCs). Through the use of Runx1(-/-) ESCs containing a doxycycline-inducible Runx1 coding sequence, we uncovered that HOXB4 promoted the formation of hemogenic endothelium cells without altering endothelial cell development. Whole-transcriptome analysis revealed that its expression mediated the upregulation of transcription of core transcription factors necessary for hematopoiesis, culminating in the formation of blood progenitors upon initiation of Runx1 expression.

SUBMITTER: Teichweyde N 

PROVIDER: S-EPMC5919293 | biostudies-literature | 2018 Mar

REPOSITORIES: biostudies-literature

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HOXB4 Promotes Hemogenic Endothelium Formation without Perturbing Endothelial Cell Development.

Teichweyde Nadine N   Kasperidus Lara L   Carotta Sebastian S   Kouskoff Valerie V   Lacaud Georges G   Horn Peter A PA   Heinrichs Stefan S   Klump Hannes H  

Stem cell reports 20180215 3


Generation of hematopoietic stem cells (HSCs) from pluripotent stem cells, in vitro, holds great promise for regenerative therapies. Primarily, this has been achieved in mouse cells by overexpression of the homeotic selector protein HOXB4. The exact cellular stage at which HOXB4 promotes hematopoietic development, in vitro, is not yet known. However, its identification is a prerequisite to unambiguously identify the molecular circuits controlling hematopoiesis, since the activity of HOX proteins  ...[more]

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