Department of Ophthalmology, Flinders University, Adelaide, SA, Australia.
BMC Med Genet. 2010 Nov 19;11:165. doi: 10.1186/1471-2350-11-165.
A novel phenotype consisting of cataract, mental retardation, erythematous skin rash and facial dysmorphism was recently described in an extended pedigree of Australian Aboriginal descent. Large scale chromosomal re-arrangements had previously been ruled out. We have conducted a genome-wide scan to map the linkage region in this family.
Genome-wide linkage analysis using Single Nucleotide Polymorphism (SNP) markers on the Affymetrix 10K SNP array was conducted and analysed using MERLIN. Three positional candidate genes (ZBTB17, EPHA2 and EPHB2) were sequenced to screen for segregating mutations.
Under a fully penetrant, dominant model, the locus for this unique phenotype was mapped to chromosome 1p35.3-p36.32 with a maximum LOD score of 2.41. The critical region spans 48.7 cM between markers rs966321 and rs1441834 and encompasses 527 transcripts from 364 annotated genes. No coding mutations were identified in three positional candidate genes EPHA2, EPHB2 or ZBTB17. The region overlaps with a previously reported region for Volkmann cataract and the phenotype has similarity to that reported for 1p36 monosomy.
The gene for this syndrome is located in a 25.6 Mb region on 1p35.3-p36.32. The known cataract gene in this region (EPHA2) does not harbour mutations in this family, suggesting that at least one additional gene for cataract is present in this region.
最近在一个具有澳大利亚原住民血统的大家庭中描述了一种新的表型,其特征为白内障、智力迟钝、红斑皮疹和面部畸形。先前已排除了大规模的染色体重排。我们进行了全基因组扫描,以绘制该家族的连锁区域。
使用 Affymetrix 10K SNP 阵列上的单核苷酸多态性 (SNP) 标记进行全基因组连锁分析,并使用 MERLIN 进行分析。对三个位置候选基因(ZBTB17、EPHA2 和 EPHB2)进行测序,以筛选分离突变。
在完全穿透、显性模型下,该独特表型的基因座被映射到 1p35.3-p36.32 染色体上,最大 LOD 得分为 2.41。关键区域在标记 rs966321 和 rs1441834 之间跨越 48.7 cM,包含来自 364 个注释基因的 527 个转录本。在三个位置候选基因 EPHA2、EPHB2 或 ZBTB17 中未发现编码突变。该区域与先前报道的 Volkmann 白内障区域重叠,该表型与 1p36 单体相似。
该综合征的基因位于 1p35.3-p36.32 上的 25.6 Mb 区域。该区域中已知的白内障基因(EPHA2)在该家族中没有突变,这表明该区域至少存在另一个白内障基因。
