Département de Génétique Médicale, Hôpital d'Enfants de La Timone, Marseille, France.
Eur J Hum Genet. 2010 Dec;18(12):1360-3. doi: 10.1038/ejhg.2010.126. Epub 2010 Aug 4.
Mental retardation is a frequent condition that is clinically and genetically highly heterogeneous. One of the strategies used to identify new causative genes is to take advantage of balanced chromosomal rearrangements in affected patients. We characterized a de novo t(10;13) balanced translocation in a patient with severe mental retardation and major hypotonia. We found that the balanced translocation is molecularly balanced. The translocation breakpoint disrupts the coding sequence of a single gene, called ATP8A2. The ATP8A2 gene is not ubiquitously expressed, but it is highly expressed in the brain. In situ hybridization performed in mouse embryos at different stages of development with the mouse homologue confirms this observation. A total of 38 patients with a similar phenotype were screened for mutations in the ATP8A2 gene but no mutations were found. The balanced translocation identified in this patient disrupts a single candidate gene highly expressed in the brain. Although this chromosomal rearrangement could be the cause of the severe phenotype of the patient, we were not able to identify additional cases. Extensive screening in the mentally retarded population will be needed to determine if ATP8A2 haploinsufficiency or dysfunction causes a neurological phenotype in humans.
智力迟钝是一种常见的病症,在临床上和遗传上具有高度异质性。鉴定新的致病基因的策略之一是利用受影响患者的平衡染色体重排。我们对一名严重智力迟钝和严重张力减退症患者的新发 t(10;13)平衡易位进行了特征描述。我们发现,该平衡易位在分子水平上是平衡的。易位断点破坏了一个称为 ATP8A2 的单一基因的编码序列。ATP8A2 基因不是广泛表达的,但在大脑中高度表达。用小鼠同源物在不同发育阶段的小鼠胚胎中进行的原位杂交证实了这一观察结果。对 38 名具有类似表型的患者进行了 ATP8A2 基因突变筛查,但未发现突变。该患者中鉴定的平衡易位破坏了在大脑中高度表达的单一候选基因。虽然这种染色体重排可能是该患者严重表型的原因,但我们未能鉴定出其他病例。需要对智力迟钝人群进行广泛筛查,以确定 ATP8A2 单倍不足或功能障碍是否会导致人类出现神经表型。