Hoxb3 Regulates Jag1 Expression in Pharyngeal Epithelium and Affects Interaction With Neural Crest Cells.

Haoran Zhang,Mai Har Sham,Karl Kam Hei So,Wood Yee Chan,Elaine Yee Man Wong,Ka Kui Tong,Junjie Xie,Jearn Jang Sae-Pang,Sze Lan Tsang,Li Wang

doi:10.3389/fphys.2020.612230

Haoran Zhang, Mai Har Sham + Show 8 more

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https://doi.org/10.3389/fphys.2020.612230

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Craniofacial morphogenesis depends on proper migration of neural crest cells and their interactions with placodes and other cell types. Hox genes provide positional information and are important in patterning the neural crest and pharyngeal arches (PAs) for coordinated formation of craniofacial structures. Hox genes are expressed in the surface ectoderm and epibranchial placodes, their roles in the pharyngeal epithelium and their downstream targets in regulating PA morphogenesis have not been established. We altered the Hox code in the pharyngeal region of the Hoxb3Tg/+ mutant, in which Hoxb3 is driven to ectopically expressed in Hoxb2 domain in the second pharyngeal arch (PA2). In the transgenic mutant, ectopic Hoxb3 expression was restricted to the surface ectoderm, including the proximal epibranchial placodal region and the distal pharyngeal epithelium. The Hoxb3Tg/+ mutants displayed hypoplasia of PA2, multiple neural crest-derived facial skeletal and nerve defects. Interestingly, we found that in the Hoxb3Tg/+ mutant, expression of the Notch ligand Jag1 was specifically up-regulated in the ectodermal pharyngeal epithelial cells of PA2. By molecular experiments, we demonstrated that Hoxb3 could bind to an upstream genomic site S2 and directly regulate Jag1 expression. In the Hoxb3Tg/+ mutant, elevated expression of Jag1 in the pharyngeal epithelium led to abnormal cellular interaction and deficiency of neural crest cells migrating into PA2. In summary, we showed that Hoxb3 regulates Jag1 expression and proposed a model of pharyngeal epithelium and neural crest interaction during pharyngeal arch development.

Highlights

An important phase of mammalian craniofacial development is the formation of the transient pharyngeal arch (PA) structures
We showed that Hoxa2 and Hoxb2 were both expressed in PA2, PA3 and posterior PAs, and Hoxb3 was expressed in PA3 and posterior PAs at E9.5 (Figures 1A,C,E)
Coronal sections at the level of proximal pharyngeal arches of embryos hybridized with Hoxa2 and Hoxb2 probes revealed differential expression of these two genes in PA2

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Introduction

An important phase of mammalian craniofacial development is the formation of the transient pharyngeal arch (PA) structures These PAs are comprised of an outer surface ectoderm, an inner covering of endoderm, a mesenchymal core, and the cranial neural crest-derived ectomesenchyme. The cranial neural crest cells which delaminate from the dorsal region of hindbrain rhombomeres have important structural roles in craniofacial morphogenesis. In the PAs, neural crest cells respond to signals from the pharyngeal surface ectoderm and the endoderm in determining their cell fate (Graham et al, 2005). PAs can be formed and their antero-posterior and proximo-distal axes maintained in the absence of neural crest cells, indicating the important roles of pharyngeal epithelium and other cell types during PA development (Veitch et al, 1999; Gavalas et al, 2001; Trainor and Krumlauf, 2001)

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