Noggin Is Required For First Pharyngeal Arch Differentiation In The Frog Xenopus Tropicalis

Abstract

The dorsal ventral axis of vertebrates requires high BMP activity for ventral development and inhibition of BMP activity for dorsal development. Presumptive dorsal regions of the embryo are protected from the ventralizing activity of BMPs by the secretion of BMP antagonists from the mesoderm. Noggin, one such antagonist, binds BMP ligands and prevents them from binding their receptors, however, a unique role for Noggin in amphibian development has remained unclear. Previously, we used zinc-finger nucleases to mutagenize the noggin locus in Xenopus tropicalis. Here, we report on the phenotype of noggin mutant frogs as a result of breeding null mutations to homozygosity. Early homozygous noggin mutant embryos are indistinguishable from wildtype siblings, with normal neural induction and neural tube closure. However, in late tadpole stages mutants present severe ventral craniofacial defects, notably a fusion of Meckel's cartilage to the palatoquadrate cartilage. Consistent with a noggin loss-of-function, mutants show expansions of BMP target gene expression and the mutant phenotype can be rescued with transient BMP inhibition. These results demonstrate that in amphibians, Noggin is dispensable for early embryonic patterning but is critical for cranial skeletogenesis.

Publication Date

6-15-2017

Publication Title

Developmental Biology

Volume

426

Issue

2

Number of Pages

245-254

Document Type

Article

Personal Identifier

scopus

DOI Link

https://doi.org/10.1016/j.ydbio.2016.06.034

Socpus ID

84979609825 (Scopus)

Source API URL

https://api.elsevier.com/content/abstract/scopus_id/84979609825

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