Bholah Zaynab, Smith Miriam J, Byers Helen J, Miles Emma K, Evans D Gareth, Newman William G
Manchester Centre for Genomic Medicine, University of Manchester, Manchester, M13 9WL, UK.
Fam Cancer. 2014 Sep;13(3):477-80. doi: 10.1007/s10689-014-9712-9.
Gorlin syndrome is an autosomal dominant disorder characterized by multiple early-onset basal cell carcinoma, odontogenic keratocysts and skeletal abnormalities. It is caused by heterozygous mutations in the tumour suppressor PTCH1. Routine clinical genetic testing, by Sanger sequencing and multiplex ligation-dependent probe amplification (MLPA) to confirm a clinical diagnosis of Gorlin syndrome, identifies a mutation in 60-90 % of cases. We undertook RNA analysis on lymphocytes from ten individuals diagnosed with Gorlin syndrome, but without known PTCH1 mutations by exonic sequencing or MLPA. Two altered PTCH1 transcripts were identified. Genomic DNA sequence analysis identified an intron 7 mutation c.1068-10T>A, which created a strong cryptic splice acceptor site, leading to an intronic insertion of eight bases; this is predicted to create a frameshift p.(His358Alafs12). Secondly, a deep intronic mutation c.2561-2057A>G caused an inframe insertion of 78 intronic bases in the cDNA transcript, leading to a premature stop codon p.(Gly854fs3). The mutations are predicted to cause loss of function of PTCH1, consistent with its tumour suppressor function. The findings indicate the importance of RNA analysis to detect intronic mutations in PTCH1 not identified by routine screening techniques.
戈林综合征是一种常染色体显性疾病,其特征为多发早发性基底细胞癌、牙源性角化囊肿和骨骼异常。它由肿瘤抑制基因PTCH1的杂合突变引起。通过桑格测序和多重连接依赖探针扩增(MLPA)进行的常规临床基因检测用于确诊戈林综合征,在60%至90%的病例中可识别出突变。我们对10名被诊断为戈林综合征但通过外显子测序或MLPA未发现已知PTCH1突变的个体的淋巴细胞进行了RNA分析。鉴定出两个改变的PTCH1转录本。基因组DNA序列分析鉴定出一个内含子7突变c.1068 - 10T>A,它产生了一个强隐蔽剪接受体位点,导致八个碱基的内含子插入;预计这会产生移码p.(His358Alafs12)。其次,一个内含子深处的突变c.2561 - 2057A>G导致cDNA转录本中有78个内含子碱基的框内插入,导致提前终止密码子p.(Gly854fs3)。这些突变预计会导致PTCH1功能丧失,与其肿瘤抑制功能一致。这些发现表明RNA分析对于检测常规筛查技术未识别的PTCH1内含子突变的重要性。
