4.6 Review

Notch Signaling in HSC Emergence: When, Why and How

Journal

CELLS
Volume 11, Issue 3, Pages -

Publisher

MDPI
DOI: 10.3390/cells11030358

Keywords

Notch signaling; HSC; developmental hematopoiesis; AGM

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This review discusses the role of the Notch signaling pathway in hematopoietic cell fate specification and HSC activity. By studying different hematopoietic models, including zebrafish, mouse, and in vitro differentiated stem cells, we can understand the temporal and spatial regulation of Notch signaling during HSC development.
The hematopoietic stem cell (HSC) sustains blood homeostasis throughout life in vertebrates. During embryonic development, HSCs emerge from the aorta-gonads and mesonephros (AGM) region along with hematopoietic progenitors within hematopoietic clusters which are found in the dorsal aorta, the main arterial vessel. Notch signaling, which is essential for arterial specification of the aorta, is also crucial in hematopoietic development and HSC activity. In this review, we will present and discuss the evidence that we have for Notch activity in hematopoietic cell fate specification and the crosstalk with the endothelial and arterial lineage. The core hematopoietic program is conserved across vertebrates and here we review studies conducted using different models of vertebrate hematopoiesis, including zebrafish, mouse and in vitro differentiated Embryonic stem cells. To fulfill the goal of engineering HSCs in vitro, we need to understand the molecular processes that modulate Notch signaling during HSC emergence in a temporal and spatial context. Here, we review relevant contributions from different model systems that are required to specify precursors of HSC and HSC activity through Notch interactions at different stages of development.

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