| Literature DB >> 27680507 |
Fu Xiong1, Zhisong Ji1, Yanhui Liu1,2, Yu Zhang1, Lingling Hu1, Qi Yang1, Qinwei Qiu1, Lingfeng Zhao3, Dong Chen4, Zhihui Tian5, Xuan Shang1, Leitao Zhang5, Xiaofeng Wei1, Cuixian Liu1, Qiuxia Yu1, Meichao Zhang6, Jing Cheng7, Jun Xiong1, Dongri Li8, Xiuhua Wu9, Huijun Yuan7, Wenqing Zhang3, Xiangmin Xu1.
Abstract
Dentin dysplasia type I (DDI) is an autosomal-dominant genetic disorder resulting from dentin defects. The molecular basis of DDI remains unclear. DDI exhibits unique characteristics with phenotypes featuring obliteration of pulp chambers and diminutive root, thus providing a useful model for understanding the genetics of tooth formation. Using a large Chinese family with 14 DDI patients, we mapped the gene locus responsible for DDI to 3p26.1-3p24.3 and further identified a missense mutation, c.353C>A (p.P118Q) in the SSUH2 gene on 3p26.1, which co-segregated with DDI. We showed that SSUH2 (p.P118Q) perturbed the structure and significantly reduced levels of mutant (MT) protein and mRNA compared with wild-type SSUH2. Furthermore, MT P141Q knock-in mice (+/- and -/-) had a unique partial obliteration of the pulp cavity and upregulation or downregulation of six major genes involved in odontogenesis: Dspp, Dmp1, Runx2, Pax9, Bmp2, and Dlx2. The phenotype of missing teeth was determined in zebrafish with morpholino gene knockdowns and rescued by injection of normal human mRNA. Taken together, our observations demonstrate that SSUH2 disrupts dental formation and that this novel gene, together with other odontogenesis genes, is involved in tooth development.Entities:
Keywords: DDI; SSUH2; dentin dysplasia type I; mouse; odontogenesis; zebrafish
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Year: 2016 PMID: 27680507 DOI: 10.1002/humu.23130
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878