| Literature DB >> 33234718 |
Shannon H Carroll1,2,3, Claudio Macias Trevino1,4, Edward B Li4, Kenta Kawasaki1,2, Nikita Myers1, Shawn A Hallett1, Nora Alhazmi5, Justin Cotney6, Russ P Carstens7, Eric C Liao1,2,4,3.
Abstract
Irf6 and Esrp1 are important for palate development across vertebrates. In zebrafish, we found that irf6 regulates the expression of esrp1 We detailed overlapping Irf6 and Esrp1/2 expression in mouse orofacial epithelium. In zebrafish, irf6 and esrp1/2 share expression in periderm, frontonasal ectoderm and oral epithelium. Genetic disruption of irf6 and esrp1/2 in zebrafish resulted in cleft of the anterior neurocranium. The esrp1/2 mutant also developed cleft of the mouth opening. Lineage tracing of cranial neural crest cells revealed that the cleft resulted not from migration defect, but from impaired chondrogenesis. Analysis of aberrant cells within the cleft revealed expression of sox10, col1a1 and irf6, and these cells were adjacent to krt4 + and krt5 + cells. Breeding of mouse Irf6; Esrp1; Esrp2 compound mutants suggested genetic interaction, as the triple homozygote and the Irf6; Esrp1 double homozygote were not observed. Further, Irf6 heterozygosity reduced Esrp1/2 cleft severity. These studies highlight the complementary analysis of Irf6 and Esrp1/2 in mouse and zebrafish, and identify a unique aberrant cell population in zebrafish expressing sox10, col1a1 and irf6 Future work characterizing this cell population will yield additional insight into cleft pathogenesis.Entities:
Keywords: Cleft; Craniofacial; Development; ESRP1; IRF6
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Year: 2020 PMID: 33234718 PMCID: PMC7774891 DOI: 10.1242/dev.194498
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.862