一个 1.38kb 的缺失与 KIAA0586 中的单核苷酸变异共同导致了杰特综合征。
A novel 1.38-kb deletion combined with a single nucleotide variant in KIAA0586 as a cause of Joubert syndrome.
机构信息
National Human Genetic Resources Center, National Research Institute for Family Planning, Beijing, China.
出版信息
BMC Med Genomics. 2023 Jan 12;16(1):4. doi: 10.1186/s12920-023-01438-6.
BACKGROUND
KIAA0586, also known as Talpid3, plays critical roles in primary cilia formation and hedgehog signaling in humans. Variants in KIAA0586 could cause some different ciliopathies, including Joubert syndrome (JBTS), which is a clinically and genetically heterogeneous group of autosomal recessive neurological disorders.
METHODS AND RESULTS
A 9-month-old girl was diagnosed as JBTS by the "molar tooth sign" of the mid-brain and global developmental delay. By whole-exome sequencing, we identified a single nucleotide variant c.3303G > A and a 1.38-kb deletion in KIAA0586 in the proband. These two variants of KIAA0586 were consistent with the mode of autosomal recessive inheritance in the family, which was verified using Sanger sequencing.
CONCLUSIONS
This finding of a compound heterozygote with a 1.38-kb deletion and c.3303G > A gave a precise genetic diagnosis for the patient, and the novel 1.38-kb deletion also expanded the pathogenic variation spectrum of JBTS caused by KIAA0586.
背景
KIAA0586,也称为 Talpid3,在人类中对初级纤毛形成和 hedgehog 信号传导起着关键作用。KIAA0586 的变异可能导致一些不同的纤毛病,包括杰特综合征(JBTS),这是一组常染色体隐性遗传的神经发育障碍,临床表现和遗传异质性较大。
方法和结果
一名 9 个月大的女孩因中脑的“磨牙征”和全面发育迟缓被诊断为 JBTS。通过全外显子组测序,我们在先证者中发现了 KIAA0586 中的单个核苷酸变异 c.3303G>A 和 1.38-kb 缺失。这两种 KIAA0586 变异与家族中常染色体隐性遗传的模式一致,通过 Sanger 测序进行了验证。
结论
该患者为 1.38-kb 缺失和 c.3303G>A 的复合杂合子的发现为该患者提供了精确的遗传诊断,而新型的 1.38-kb 缺失也扩大了 KIAA0586 引起的 JBTS 的致病变异谱。
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