"Molecular Investigation of Genetic Orphan Diseases" Research Unit, Pasteur Institute of Tunis, Tunisia.
Arch Dermatol Res. 2012 Mar;304(2):171-6. doi: 10.1007/s00403-011-1190-4. Epub 2011 Nov 12.
Xeroderma pigmentosum (XP) is a rare disorder characterized by a high skin sun-sensitivity predisposing to skin cancers at an early age. Among Tunisian XP patients with an intermediate skin phenotype, 92% presented neurological abnormalities related to XPA gene deficiency. Clinical variability of the XP-A phenotype is associated with a mutational heterogeneity. In the present study, two Tunisian families with severe dermatological and neurological XP phenotypes were investigated in order to determine clinical characteristics and genetic basis. Two Tunisian families with four XP affected children were examined in the Dermatology Department. Clinical features showed severe presentation of the disease. Coding regions of the XPA gene were analysed by direct sequencing. Results showed the presence of a novel mutation, p.E111X, in three patients belonging to the same family and presenting a very severe phenotype i.e. development of skin lesions and neurological signs before 1 year age. For the other patient, we identified a nonsense mutation, p.R207X, already identified in a Palestinian XP-A patient. Identification of novel causing mutations in Tunisian XP-A patients shows the genetic and mutational heterogeneity of the disease in Tunisia. Despite a relatively homogenous mutational spectrum, mutational heterogeneity for rare cases is observed because of the high rate of consanguinity.
着色性干皮病(XP)是一种罕见的疾病,其特征是皮肤对阳光高度敏感,容易在年轻时患上皮肤癌。在突尼斯 XP 患者中,有 92%的患者存在与 XPA 基因缺陷相关的神经异常。XP-A 表型的临床变异性与突变异质性有关。在本研究中,对两个具有严重皮肤和神经 XP 表型的突尼斯家族进行了研究,以确定其临床特征和遗传基础。在皮肤科检查了两个有四个 XP 受影响儿童的突尼斯家族。临床特征显示疾病的严重表现。通过直接测序分析 XPA 基因的编码区。结果显示,三个来自同一家庭的患者存在一种新的突变,p.E111X,表现出非常严重的表型,即皮肤损伤和神经症状在 1 岁前出现。对于另一名患者,我们发现了一种无义突变,p.R207X,已在一名巴勒斯坦 XP-A 患者中发现。在突尼斯 XP-A 患者中发现新的致病突变表明,该疾病在突尼斯存在遗传和突变异质性。尽管突变谱相对单一,但由于近亲结婚率较高,罕见病例仍存在突变异质性。
