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   IRF6 and SPRY4 Signaling Interact in Periderm Development  
   
نویسنده kousa y.a. ,roushangar r. ,patel n. ,walter a. ,marangoni p. ,krumlauf r. ,klein o.d. ,schutte b.c.
منبع journal of dental research - 2017 - دوره : 96 - شماره : 11 - صفحه:1306 -1313
چکیده    Rare mutations in irf6 and grhl3 cause van der woude syndrome,an autosomal dominant orofacial clefting disorder. common variants in irf6 and grhl3 also contribute risk for isolated orofacial clefting. similarly,variants within genes that encode receptor tyrosine kinase (rtk) signaling components,including members of the fgf pathway,epha3 and spry2,also contribute risk for isolated orofacial clefting. in the mouse,loss of irf6 or perturbation of fgf signaling leads to abnormal oral epithelial adhesions and cleft palate. oral adhesions can result from a disruption of periderm formation. here,we find that irf6 and spry4 signaling interact in periderm function. we crossed irf6 heterozygous (irf6+/-) mice with transgenic mice that express spry4 in the basal epithelial layer (tgkrt14::spry4). while embryos with either of these mutations can have abnormal oral adhesions,using a new quantitative assay,we observed a nonadditive effect of abnormal oral epithelial adhesions in the most severely affected double mutant embryos (irf6+/-;tgkrt14::spry4). at the molecular level,the sites of abnormal oral adhesions maintained periderm-like cells that express keratin 6,but we observed abnormal expression of grhl3. together,these data suggest that irf6 and rtk signaling interact in regulating periderm differentiation and function,as well as provide a rationale to screen for epistatic interactions between variants in irf6 and rtk signaling pathway genes in human orofacial clefting populations. © international & american associations for dental research 2017.
کلیدواژه cleft lip with or without cleft palate nonsyndromic; GRHL3 protein; oral adhesions; popliteal pterygium syndrome; receptor protein-tyrosine kinases; Van der Woude syndrome
آدرس department of biochemistry and molecular biology,michigan state university,east lansing,mi,united states,pediatric residency program,children's national health system,washington,dc, United States, department of biochemistry and molecular biology,michigan state university,east lansing,mi, United States, microbiology and molecular genetics,michigan state university,5162 biomedical and physical science building,east lansing,mi, United States, microbiology and molecular genetics,michigan state university,5162 biomedical and physical science building,east lansing,mi, United States, departments of orofacial sciences and pediatrics,institute for human genetics,university of california,san francisco,san francisco,ca, United States, stowers institute for medical research,kansas city,mo,united states,department of anatomy and cell biology,university of kansas medical center,kansas city,ks, United States, departments of orofacial sciences and pediatrics,institute for human genetics,university of california,san francisco,san francisco,ca, United States, microbiology and molecular genetics,michigan state university,5162 biomedical and physical science building,east lansing,mi,united states,departments of microbiology and molecular genetics,michigan state university,east lansing,mi, United States
 
     
   
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