Developmental Genetics Unit, King Faisal Specialist Hospital and Research Center, MBC-03 PO BOX 3354, Riyadh 11211, Saudi Arabia.
J Med Genet. 2013 Jul;50(7):425-30. doi: 10.1136/jmedgenet-2012-101378. Epub 2013 Apr 25.
Intellectual disability (ID) is one of the most common forms of disability worldwide, displaying a wide range of aetiologies and affecting nearly 2% of the global population.
To describe a novel autosomal recessive form of ID with strabismus and its underlying aetiology.
Autozygosity mapping, linkage analysis and exome sequencing were performed in a large multiplex consanguineous family that segregates ID and strabismus. Exome sequencing was independently performed in three other consanguineous families segregating the same disease. Direct sequencing of the resulting candidate gene was performed in four additional families with the same phenotype.
A single missense mutation was identified in ADAT3 in all studied families on an ancient ancestral haplotype. This gene encodes one of two eukaryotic proteins that are necessary for the deamination of adenosine at position 34 to inosine in t-RNA. Our results show the first human mutation in the t-RNA editing machinery and expand the landscape of pathways involved in the pathogenesis of ID.
智力残疾(ID)是全球最常见的残疾形式之一,具有广泛的病因,并影响全球近 2%的人口。
描述一种具有斜视的新型常染色体隐性智力残疾形式及其潜在病因。
在一个大型连锁近亲家庭中进行了自交系作图、连锁分析和外显子组测序,该家庭存在 ID 和斜视的遗传。在另外三个具有相同疾病遗传的近亲家庭中独立进行了外显子组测序。在具有相同表型的另外四个家庭中对候选基因进行了直接测序。
在所有研究的家庭中,在一个古老的祖先单倍型上发现了 ADAT3 中的单个错义突变。该基因编码两种真核蛋白质之一,对于 t-RNA 中位置 34 的腺苷脱氨酶到肌苷的脱氨作用是必需的。我们的结果显示了 t-RNA 编辑机制中的第一个人类突变,并扩展了参与 ID 发病机制的途径景观。
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