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C4orf26 基因突变导致釉质发育不全,该基因编码一种具有体外羟基磷灰石晶体成核和生长活性的肽。

Mutations in C4orf26, encoding a peptide with in vitro hydroxyapatite crystal nucleation and growth activity, cause amelogenesis imperfecta.

机构信息

Leeds Institute of Molecular Medicine, St. James's University Hospital, University of Leeds, LS9 7TF Leeds, UK.

出版信息

Am J Hum Genet. 2012 Sep 7;91(3):565-71. doi: 10.1016/j.ajhg.2012.07.020. Epub 2012 Aug 16.

Abstract

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.

摘要

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。

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