Levchenko Olga, Filatova Alexandra, Mishina Irina, Antonenko Aleksey, Skoblov Mikhail
Research Centre for Medical Genetics, Moscow, Russia.
Evogen LLC, Moscow, Russia.
Front Genet. 2023 Jul 6;14:1197681. doi: 10.3389/fgene.2023.1197681. eCollection 2023.
Autosomal recessive spinocerebellar ataxia type 20, SCAR20 (MIM: 616354) is a rare syndromic form of hereditary ataxias. It characterized by the presence of progressive ataxia, intellectual developmental disorder, autism and dysmorphic features. The disease caused by biallelic variants in gene that lead to loss of protein function. Typically, these variants result in the formation of a premature stop codon, a shift in the reading frame or a variant in canonical splicing sites, as well as gross rearrangements. Here we present the first case of a deep intronic variant c.462-589A>G in identified in two sisters with SCAR20 from a consanguineous family. This variant resulted in the inclusion of a pseudo-exon 82 nucleotides long and the formation of a premature stop codon, leading to the production of a truncated protein (NP_722523.1:p.Asp155Valfs*8). Following an extensive diagnostic search, the diagnosis was confirmed using trio whole genome sequencing. This case contributes to expanding the spectrum of potential genetic variants associated with SCAR20.
常染色体隐性遗传性脊髓小脑共济失调20型(SCAR20,MIM: 616354)是一种罕见的遗传性共济失调综合征形式。其特征为进行性共济失调、智力发育障碍、自闭症和畸形特征。该疾病由基因的双等位基因变异导致蛋白质功能丧失引起。通常,这些变异会导致过早终止密码子的形成、阅读框移位或经典剪接位点的变异,以及大片段重排。在此,我们报告了首例在一个近亲家庭中两名患有SCAR20的姐妹中鉴定出的基因内含子深处变异c.462 - 589A>G。该变异导致包含一个82个核苷酸长的假外显子,并形成一个过早终止密码子,从而产生截短蛋白(NP_722523.1:p.Asp155Valfs*8)。经过广泛的诊断性筛查,通过三联体全基因组测序确诊。该病例有助于扩大与SCAR20相关的潜在基因变异谱。
