Non-Trisomic Homeobox Gene Expression During Craniofacial Development in the Ts65Dn Mouse Model of Down Syndrome

Trisomy 21 in humans causes cognitive impairment, craniofacial dysmorphology, and heart defects collectively referred to as Down syndrome. Yet, the pathophysiology of these phenotypes is not well understood. Craniofacial alterations was lead to complications in breathing, eating, and communication, Ts65Dn mice exhibit craniofacial alterations that model Down syndrome including a small inaudible, We show that Ts65Dn embryos at 13,5 days gestation (E13.5) as a smaller :mandibular precursor but a normal sized tongue as compared to cut:dont embryos, suggesting a it instead of actual macro-glossia originates during development, Neurological tissues were also altered in E13.5 trisomic embryos, Our array analysis found 155 differentially expressed non-trisomic genes in the trisomic E13.5 mandible , including 20 genes containing a homeobox DNA binding domain, Additionally, Sox9, important in skeletal formation and cell proliferation, was upregulated in Ts65Dn mandible precursors. Our results suggest trisomy causes altered expression of non-trisomic genes in development leading to structural changes associated with DS, identification of genetic pathways disrupted by trisomy is an important step in proposing rational therapies at relevant time points to ameliorate craniofacial abnormalities in DS and other congenital disorders. (C) 2013 Wiley Periodicals, Inc.