Leeds Institute of Molecular Medicine, St. James's University Hospital, University of Leeds, LS9 7TF Leeds, UK.
Am J Hum Genet. 2012 Sep 7;91(3):565-71. doi: 10.1016/j.ajhg.2012.07.020. Epub 2012 Aug 16.
Autozygosity mapping and clonal sequencing of an Omani family identified mutations in the uncharacterized gene, C4orf26, as a cause of recessive hypomineralized amelogenesis imperfecta (AI), a disease in which the formation of tooth enamel fails. Screening of a panel of 57 autosomal-recessive AI-affected families identified eight further families with loss-of-function mutations in C4orf26. C4orf26 encodes a putative extracellular matrix acidic phosphoprotein expressed in the enamel organ. A mineral nucleation assay showed that the protein's phosphorylated C terminus has the capacity to promote nucleation of hydroxyapatite, suggesting a possible function in enamel mineralization during amelogenesis.
对一个阿曼家族进行同源性定位和克隆测序,发现未被描述的基因 C4orf26 中的突变是隐性低矿化型牙釉质不全(AI)的致病原因,该病导致牙釉质形成失败。对一组 57 个常染色体隐性 AI 受累家系进行筛查,发现 C4orf26 中还有另外 8 个家系存在功能丧失突变。C4orf26 编码一种假定的细胞外基质酸性磷蛋白,在釉质器官中表达。矿化核形成试验表明,该蛋白的磷酸化 C 端具有促进羟基磷灰石核形成的能力,提示其在成釉过程中可能具有牙釉质矿化的功能。
