Hypoxia promotes production of neural crest cells in the embryonic head

Author:

Scully Deirdre1,Keane Eleanor1,Batt Emily2,Karunakaran Priyadarssini1,Higgins Debra F.1,Itasaki Nobue12

Affiliation:

1. School of Medicine, University College Dublin, Dublin 4, Ireland

2. Faculty of Health Sciences, University of Bristol, Bristol BS2 8EJ, UK

Abstract

ABSTRACT Hypoxia is encountered in either pathological or physiological conditions, the latter of which is seen in amniote embryos prior to the commencement of a functional blood circulation. During the hypoxic stage, a large number of neural crest cells arise from the head neural tube by epithelial-to-mesenchymal transition (EMT). As EMT-like cancer dissemination can be promoted by hypoxia, we investigated whether hypoxia contributes to embryonic EMT. Using chick embryos, we show that the hypoxic cellular response, mediated by hypoxia-inducible factor (HIF)-1α, is required to produce a sufficient number of neural crest cells. Among the genes that are involved in neural crest cell development, some genes are more sensitive to hypoxia than others, demonstrating that the effect of hypoxia is gene specific. Once blood circulation becomes fully functional, the embryonic head no longer produces neural crest cells in vivo, despite the capability to do so in a hypoxia-mimicking condition in vitro, suggesting that the oxygen supply helps to stop emigration of neural crest cells in the head. These results highlight the importance of hypoxia in normal embryonic development.

Funder

Health Research Board

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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