| Literature DB >> 28109039 |
Jennifer M Iklé1, Andre L P Tavares1, Marisol King1, Hailei Ding1, Sophie Colombo2, Beth A Firulli3, Anthony B Firulli3, Kimara L Targoff2, Deborah Yelon4, David E Clouthier1.
Abstract
In gnathostomes, dorsoventral (D-V) patterning of neural crest cells (NCC) within the pharyngeal arches is crucial for the development of hinged jaws. One of the key signals that mediate this process is Endothelin-1 (EDN1). Loss of EDN1 binding to the Endothelin-A receptor (EDNRA) results in loss of EDNRA signaling and subsequent facial birth defects in humans, mice and zebrafish. A rate-limiting step in this crucial signaling pathway is the conversion of immature EDN1 into a mature active form by Endothelin converting enzyme-1 (ECE1). However, surprisingly little is known about how Ece1 transcription is induced or regulated. We show here that Nkx2.5 is required for proper craniofacial development in zebrafish and acts in part by upregulating ece1 expression. Disruption of nkx2.5 in zebrafish embryos results in defects in both ventral and dorsal pharyngeal arch-derived elements, with changes in ventral arch gene expression consistent with a disruption in Ednra signaling. ece1 mRNA rescues the nkx2.5 morphant phenotype, indicating that Nkx2.5 functions through modulating Ece1 expression or function. These studies illustrate a new function for Nkx2.5 in embryonic development and provide new avenues with which to pursue potential mechanisms underlying human facial disorders.Entities:
Keywords: birth defects; neural crest; patterning; signaling; transcription
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Year: 2017 PMID: 28109039 PMCID: PMC5364067 DOI: 10.1002/dvg.23021
Source DB: PubMed Journal: Genesis ISSN: 1526-954X Impact factor: 2.487