Molecular Haematology Unit, MRC Weatherall Institute of Molecular Medicine, University of Oxford, Oxford, UK.
Haematologica. 2013 Sep;98(9):1383-7. doi: 10.3324/haematol.2013.089490. Epub 2013 May 28.
The congenital dyserythropoietic anemias are a heterogeneous group of rare disorders primarily affecting erythropoiesis with characteristic morphological abnormalities and a block in erythroid maturation. Mutations in the CDAN1 gene, which encodes Codanin-1, underlie the majority of congenital dyserythropoietic anemia type I cases. However, no likely pathogenic CDAN1 mutation has been detected in approximately 20% of cases, suggesting the presence of at least one other locus. We used whole genome sequencing and segregation analysis to identify a homozygous T to A transversion (c.533T>A), predicted to lead to a p.L178Q missense substitution in C15ORF41, a gene of unknown function, in a consanguineous pedigree of Middle-Eastern origin. Sequencing C15ORF41 in other CDAN1 mutation-negative congenital dyserythropoietic anemia type I pedigrees identified a homozygous transition (c.281A>G), predicted to lead to a p.Y94C substitution, in two further pedigrees of SouthEast Asian origin. The haplotype surrounding the c.281A>G change suggests a founder effect for this mutation in Pakistan. Detailed sequence similarity searches indicate that C15ORF41 encodes a novel restriction endonuclease that is a member of the Holliday junction resolvase family of proteins.
先天性红细胞生成异常性贫血是一组罕见疾病,主要影响红细胞生成,其特征为形态异常和红系成熟阻滞。CDAN1 基因突变是先天性红细胞生成异常性贫血 I 型的主要病因,然而,大约 20%的病例中未检测到可能的致病性 CDAN1 突变,这表明至少存在另一个基因座。我们使用全基因组测序和分离分析在一个中东血统的近亲家系中发现了一个纯合的 T 到 A 颠换(c.533T>A),预测导致 C15ORF41 中的一个错义替换 p.L178Q,C15ORF41 是一个未知功能的基因。在其他 CDAN1 突变阴性的先天性红细胞生成异常性贫血 I 型家系中对 C15ORF41 进行测序,在另外两个源自东南亚的家系中发现了另一个纯合转换(c.281A>G),预测导致 p.Y94C 取代。c.281A>G 改变周围的单倍型表明该突变在巴基斯坦存在一个奠基者效应。详细的序列相似性搜索表明 C15ORF41 编码一种新的限制内切酶,它是 Holliday 连接体解旋酶家族蛋白的成员。
