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Novel biallelic loss-of-function variants in CEP290 cause Joubert syndrome in two siblings

机译:CEP290的新型双胞胎丧失功能变体导致两个兄弟姐妹的Joubert综合征

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Joubert syndrome (JS) is a rare genetic disorder, which can be defined by brain stem malformation, cerebellar vermis hypoplasia, and consequent “molar tooth sign” (MTS). JS always shares variety of phenotypes in development defects. With the development of next-generation sequencing, dozens of causative genes have been identified to JS so far. Here, we investigated two male siblings with JS and uncovered a novel pathogenesis through combined methods. The siblings shared similar features of nystagmus, disorders of intellectual development, typical MTS, and abnormal morphology in fourth ventricle. Whole-exome sequencing (WES) and chromosome comparative genomic hybridization (CGH) were then performed on the proband. Strikingly, a maternal inherited nonsense variant (NM_025114.3: c.5953GT [p.E1985*]) in CEP290 gene and a paternal inherited deletion in 12q21.32 including exons 1 to 10 of CEP290 gene were identified in the two affected siblings. We further confirmed the two variants by in vitro experiments: quantitative PCR and PCR sequencing. In this study, we first reported a novel causative mechanism of Joubert syndrome: a copy number variation (CNV) combined with a single-nucleotide variant in CEP290 gene, which can be helpful in the genetic diagnosis of this disease.
机译:Joubert综合征(JS)是一种罕见的遗传障碍,可由脑干畸形,小脑抑制性发育不全和随后的“磨牙迹象”(MTS)来定义。 JS始终分享各种发展缺陷的表型。随着下一代测序的发展,到目前为止已经确定了数十种致病基因。在这里,我们通过组合方法调查了两个具有JS的男性兄弟姐妹,并通过组合方法揭示了一种新的发病机制。兄弟姐妹在第四脑室的智力发育障碍,典型的MTS和异常形态共享类似的患有眼球菌,典型的MTS和异常形态的特征。然后对全部exome测序(WES)和染色体对比基因组杂交(CGH)对验证剂进行。在两Q21.32中,在Cep290基因中,在2Q21.32中,母亲遗传的非阵列变体(NM_025114.3:C.5953G> T [P.E1985 *])在受影响的两点中鉴定了Cep290基因的外显子1至10的父亲遗传缺失兄弟姐妹。我们通过体外实验进一步证实了两种变体:定量PCR和PCR测序。在这项研究中,我们首先报道了Joubert综合征的新致病机制:拷贝数变异(CNV)与CEP290基因的单核苷酸变体相结合,这有助于这种疾病的遗传诊断。

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