S-Space College of Dentistry/School of Dentistry (치과대학/치의학대학원) Dept. of Dentistry (치의학과) Journal Papers (저널논문_치의학과)
RUNX2 mutations in cleidocranial dysplasia patients.
|dc.identifier.citation||Oral Diseases 16:55-60||en|
|dc.description.abstract||Objective: Mutations in the RUNX2 gene, a master regulator of bone formation, have been identified in cleidocranial dysplasia (CCD) patients. CCD is a rare autosomal-dominant disease characterized by the delayed closure of cranial sutures, defects in clavicle formation, and supernumerary teeth. The purposes of this study were to identify genetic causes of two CCD nuclear families and to report their clinical phenotypes.
Materials and methods: We identified two CCD nuclear families and performed mutational analyses to clarify the underlying molecular genetic etiology.
Results: Mutational analysis revealed a novel nonsense mutation (c.273T>A, p.L93X) in family 1 and a de novo missense one (c.673C>T, p.R225W) in family 2. Individuals with a nonsense mutation showed maxillary hypoplasia, delayed eruption, multiple supernumerary teeth, and normal stature. In contrast, an individual with a de novo missense mutation in the Runt domain showed only one supernumerary tooth and short stature.
Conclusions: Mutational and phenotypic analyses showed that the severity of mutations on the skeletal system may not necessarily correlate with that of the disruption of tooth development.
|dc.description.sponsorship||This work was supported by a grant from the
Korea Science and Engineering Foundation (KOSEF) through
the Biotechnology R&D program (No. M10646010003-
08N4601-00310) and by a Korea Science and Engineering
Foundation (KOSEF) Science Research Center grant funded
by the Korean Ministry of Education, Science and Technology
(MEST) through the Bone Metabolism Research Center (No.
|dc.title||RUNX2 mutations in cleidocranial dysplasia patients.||en|
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