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FAM20C Plays an Essential Role in the Formation of Murine Teeth
Authors:Xiaofang Wang  Suzhen Wang  Yongbo Lu  Monica P. Gibson  Ying Liu  Baozhi Yuan  Jian Q. Feng  Chunlin Qin
Affiliation:From the Department of Biomedical Sciences, Texas A&M Health Science Center Baylor College of Dentistry, Dallas, Texas 75246.;the §Department of Medicine, University of Wisconsin, Madison, Wisconsin 53705, and ;Geriatric Research and Education Clinical Centers, William S. Middleton Memorial Veterans Hospital, Department of Veterans Affairs, Madison, Wisconsin 53705
Abstract:
FAM20C is highly expressed in bone and tooth. Previously, we showed that Fam20C conditional knock-out (KO) mice manifest hypophosphatemic rickets, which highlights the crucial roles of this molecule in promoting bone formation and mediating phosphate homeostasis. In this study, we characterized the dentin, enamel, and cementum of Sox2-Cre-mediated Fam20C KO mice. The KO mice exhibited small malformed teeth, severe enamel defects, very thin dentin, less cementum than normal, and overall hypomineralization in the dental mineralized tissues. In situ hybridization and immunohistochemistry analyses revealed remarkable down-regulation of dentin matrix protein 1 (DMP1) and dentin sialophosphoprotein in odontoblasts, along with a sharply reduced expression of ameloblastin and amelotin in ameloblasts. Collectively, these data indicate that FAM20C is essential to the differentiation and mineralization of dental tissues through the regulation of molecules critical to the differentiation of tooth-formative cells.
Keywords:Calcification   Dentin   Gene Knockout   Mouse   Tooth Development   DMP4   FAM20C   Amelotin   Cementum   Enamel
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