Laboratoire de Génomique Biomédicale et Oncogénétique, LR 11 IPT 05, Institut Pasteur de Tunis and Université de Tunis El Manar, El Manar I, 2092 Tunis, Tunisia.
Biomed Res Int. 2013;2013:316286. doi: 10.1155/2013/316286. Epub 2013 Jul 25.
Xeroderma Pigmentosum (XP) is a rare recessive autosomal cancer prone disease, characterized by UV hypersensitivity and early appearance of cutaneous and ocular malignancies. We investigated four unrelated patients suspected to be XP-C. To confirm linkage to XPC gene, genotyping and direct sequencing of XPC gene were performed. Pathogenic effect of novel mutations was confirmed by reverse Transciptase PCR. Mutation screening revealed the presence of two novel mutations g.18246G>A and g.18810G>T in the XPC gene (NG_011763.1). The first is present in one patient XP50NEF, but the second is present in three unrelated patients (XP16KEB, XP28SFA, and XP45GB). These 3 patients are from three different cities of Southern Tunisia and bear the same haplotype, suggesting a founder effect. Reverse Transciptase PCR revealed the absence of the XPC mRNA. In Tunisia, as observed in an other severe genodermatosis, the mutational spectrum of XP-C group seems to be homogeneous with some clusters of heterogeneity that should be taken into account to improve molecular diagnosis of this disease.
着色性干皮病(XP)是一种罕见的隐性常染色体易患癌症疾病,其特征是对紫外线敏感,皮肤和眼部恶性肿瘤出现较早。我们研究了四个疑似 XP-C 的无关患者。为了确认与 XPC 基因的连锁,对 XPC 基因进行了基因分型和直接测序。通过反转录 PCR 证实了新突变的致病作用。突变筛查显示 XPC 基因存在两个新突变 g.18246G>A 和 g.18810G>T(NG_011763.1)。第一个突变存在于一个 XP50NEF 患者中,而第二个突变存在于三个无关患者(XP16KEB、XP28SFA 和 XP45GB)中。这 3 名患者来自突尼斯南部的三个不同城市,携带相同的单倍型,提示存在一个起源。反转录 PCR 显示 XPC mRNA 缺失。在突尼斯,与另一种严重的遗传性皮肤病一样,XP-C 组的突变谱似乎是同质的,存在一些异质性簇,应考虑这些簇来改善该疾病的分子诊断。
