Affiliation:
1. Department of Anatomy and Cell Biology George Washington University School of Medicine and Health Sciences Washington District of Columbia USA
2. Departments of Oral and Craniofacial Sciences and Pediatrics University of Missouri‐Kansas City Kansas City Missouri USA
3. Department of Craniofacial Biology University of Colorado Anschutz Medical Campus Aurora Colorado USA
Abstract
AbstractBackgroundGenetic variants of the transcription factor SIX1 and its co‐factor EYA1 underlie 50% of Branchio‐oto‐renal syndrome (BOR) cases. BOR is characterized by craniofacial defects, including malformed middle ear ossicles leading to conductive hearing loss. In this work, we expand our knowledge of the Six1 gene regulatory network by using a Six1‐null mouse line to assess gene expression profiles of E10.5 mandibular arches, which give rise to the neural crest (NC)‐derived middle ear ossicles and lower jaw, via bulk RNA sequencing.ResultsOur transcriptomic analysis led to the identification of 808 differentially expressed genes that are related to translation, NC cell differentiation, osteogenesis, and chondrogenesis including components of the WNT signaling pathway. As WNT signaling is a known contributor to bone development, we demonstrated that SIX1 is required for expression of the WNT antagonist Frzb in the mandibular arch, and determined that SIX1 expression results in repression of WNT signaling.ConclusionOur results clarify the mechanisms by which SIX1 regulates the development of NC‐derived craniofacial elements that are altered in SIX1‐associated disorders. In addition, this work identifies novel genes that could be causative to this birth defect and establishes a link between SIX1 and WNT signaling during patterning of NC cells.
Funder
National Institute of Dental and Craniofacial Research
School of Medicine and Health Sciences, George Washington University