Thien Kim Dao Hoang, Kawazoe Asako, Bang Pham Dang, Thanh Nguyen Tien, Taketani Shigeru
Department of Biotechnology, Kyoto Institute of Technology, Kyoto, Japan.
Case Rep Dermatol. 2013 Mar 27;5(1):105-10. doi: 10.1159/000350679. Print 2013 Jan.
Congenital erythropoietic porphyria (CEP) arises from an autosomal recessive inherited disorder of the porphyrin metabolism, which leads to the accumulation of uroporphyrinogen I in bone marrow, skin and several other tissues by a deficiency of uroporphyrinogen III cosynthase (UROS). We studied a Vietnamese patient and her family suffering from severe cutaneous photosensitivity with skin fragility, bullous lesions and hypertrichosis on light-exposed areas. A missense mutation in the UROS gene was identified as a transversion of G to T at nucleotide 11,776, resulting in a substitution of valine by phenylalanine at codon 3 of exon 2. The patient showed a homozygous mutant profile, and the heterozygous state was observed in the parents. The activity of mutated UROS expressed in Escherichia coli was less than 16.1% that of the control, indicating that the markedly reduced activity of UROS is responsible for CEP. We described for the first time a mutation in the UROS gene in a Southeast Asian patient and a molecular diagnosis for the identification of clinically asymptomatic heterozygous mutation carriers and families with CEP.
先天性红细胞生成性卟啉病(CEP)源于卟啉代谢的常染色体隐性遗传疾病,由于尿卟啉原III同合成酶(UROS)缺乏,导致尿卟啉原I在骨髓、皮肤和其他多种组织中蓄积。我们研究了一名越南患者及其家族,他们患有严重的皮肤光敏性,暴露部位皮肤脆弱、出现水疱性病变和多毛症。在UROS基因中鉴定出一个错义突变,为第11776位核苷酸处的G到T颠换,导致外显子2第3密码子处缬氨酸被苯丙氨酸替代。该患者表现为纯合突变型,其父母为杂合状态。在大肠杆菌中表达的突变型UROS活性不到对照的16.1%,表明UROS活性显著降低是导致CEP的原因。我们首次描述了一名东南亚患者UROS基因的突变情况以及用于识别临床无症状杂合突变携带者和CEP家族的分子诊断方法。
