Department of Molecular Biology and Genetics, Faculty of Science, Bilkent University, Ankara, Turkey.
Eur J Hum Genet. 2013 Mar;21(3):281-5. doi: 10.1038/ejhg.2012.170. Epub 2012 Aug 15.
Cerebellar ataxia, mental retardation and dysequilibrium syndrome is a rare and heterogeneous condition. We investigated a consanguineous family from Turkey with four affected individuals exhibiting the condition. Homozygosity mapping revealed that several shared homozygous regions, including chromosome 13q12. Targeted next-generation sequencing of an affected individual followed by segregation analysis, population screening and prediction approaches revealed a novel missense variant, p.I376M, in ATP8A2. The mutation lies in a highly conserved C-terminal transmembrane region of E1 E2 ATPase domain. The ATP8A2 gene is mainly expressed in brain and development, in particular cerebellum. Interestingly, an unrelated individual has been identified, in whom mental retardation and severe hypotonia is associated with a de novo t(10;13) balanced translocation resulting with the disruption of ATP8A2. These findings suggest that ATP8A2 is involved in the development of the cerebro-cerebellar structures required for posture and gait in humans.
小脑共济失调、智力迟钝和平衡障碍综合征是一种罕见且异质性的疾病。我们研究了一个来自土耳其的近亲家庭,该家庭有四个受影响的个体表现出这种情况。纯合子作图显示了几个共享的纯合区域,包括 13q12 号染色体。对一个受影响个体进行靶向下一代测序,然后进行分离分析、人群筛查和预测方法,发现了 ATP8A2 中的一种新的错义变异 p.I376M。该突变位于 E1 E2 ATP 酶结构域的高度保守的 C 端跨膜区域。ATP8A2 基因主要在大脑和发育中表达,特别是在小脑。有趣的是,已经确定了一个无关个体,其中智力迟钝和严重的张力减退与新的 t(10;13)平衡易位有关,导致 ATP8A2 的破坏。这些发现表明,ATP8A2 参与了人类姿势和步态所需的脑-小脑结构的发育。
