Literature DB >> 26839343

WNT/β-catenin signaling mediates human neural crest induction via a pre-neural border intermediate.

Alan W Leung1, Barbara Murdoch2, Ahmed F Salem3, Maneeshi S Prasad3, Gustavo A Gomez3, Martín I García-Castro4.   

Abstract

Neural crest (NC) cells arise early in vertebrate development, migrate extensively and contribute to a diverse array of ectodermal and mesenchymal derivatives. Previous models of NC formation suggested derivation from neuralized ectoderm, via meso-ectodermal, or neural-non-neural ectoderm interactions. Recent studies using bird and amphibian embryos suggest an earlier origin of NC, independent of neural and mesodermal tissues. Here, we set out to generate a model in which to decipher signaling and tissue interactions involved in human NC induction. Our novel human embryonic stem cell (ESC)-based model yields high proportions of multipotent NC cells (expressing SOX10, PAX7 and TFAP2A) in 5 days. We demonstrate a crucial role for WNT/β-catenin signaling in launching NC development, while blocking placodal and surface ectoderm fates. We provide evidence of the delicate temporal effects of BMP and FGF signaling, and find that NC development is separable from neural and/or mesodermal contributions. We further substantiate the notion of a neural-independent origin of NC through PAX6 expression and knockdown studies. Finally, we identify a novel pre-neural border state characterized by early WNT/β-catenin signaling targets that displays distinct responses to BMP and FGF signaling from the traditional neural border genes. In summary, our work provides a fast and efficient protocol for human NC differentiation under signaling constraints similar to those identified in vivo in model organisms, and strengthens a framework for neural crest ontogeny that is separable from neural and mesodermal fates.
© 2016. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  Embryonic stem cells; Human; Neural border; Neural crest; β-Catenin signaling

Mesh:

Substances:

Year:  2016        PMID: 26839343      PMCID: PMC4760313          DOI: 10.1242/dev.130849

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


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