Schneider-Yin X, Schäfer B W, Tönz O, Minder E I
Zentrallabor, Stadtspital Triemli, Zürich, Switzerland.
Hum Genet. 1995 Apr;95(4):391-6. doi: 10.1007/BF00208962.
Erythropoietic protoporphyria (EPP), attributable to deficiency of ferrochelatase activity (FECH), is characterised mainly by cutaneous photosensitivity. To define the molecular defect in two EPP-affected siblings and their parents in a Swiss family, ferrochelatase cDNA was amplified by the polymerase chain reaction (PCR) and subjected to sequence analysis. A 5-bp deletion (T580-G584) was identified on one allele of the ferrochelatase gene in both patients and their mother. Screening of the mutation among family members of RsaI digestion of PCR-amplified genomic DNA revealed autosomal dominant inheritance associated with abnormal protoporphyrin concentration and enzyme activity. We also isolated ferrochelatase cDNAs containing a 18-bp insertion (part of the intron 2 sequence) between exons 2 and 3; this corresponded to six extra amino acids (YESNIR) inserted between Arg-65 and Lys-66 of the known ferrochelatase. This isoform was identified initially in mRNAs derived from both alleles of the ferrochelatase gene in one patient. Its existence was confirmed in six additional EPP patients, in five out of seven controls, and in four different cell lines (fibroblast, muscle, hepatoma and myelogenous leukaemia). This isoform, roughly 20% of the total ferrochelatase mRNA, was generated through splicing at a second donor site in intron 2 and its presence was not linked to EPP.
红细胞生成性原卟啉病(EPP),归因于亚铁螯合酶活性(FECH)缺乏,主要特征为皮肤光敏性。为确定瑞士一个家族中两名受EPP影响的同胞及其父母的分子缺陷,通过聚合酶链反应(PCR)扩增亚铁螯合酶cDNA并进行序列分析。在两名患者及其母亲的亚铁螯合酶基因的一个等位基因上鉴定出一个5碱基缺失(T580 - G584)。对PCR扩增的基因组DNA进行RsaI消化后的家族成员突变筛查显示,常染色体显性遗传与异常原卟啉浓度和酶活性相关。我们还分离出了在第2外显子和第3外显子之间含有一个18碱基插入(内含子2序列的一部分)的亚铁螯合酶cDNA;这对应于在已知亚铁螯合酶的Arg - 65和Lys - 66之间插入的六个额外氨基酸(YESNIR)。这种异构体最初在一名患者的亚铁螯合酶基因两个等位基因来源的mRNA中被鉴定出来。在另外六名EPP患者、七名对照中的五名以及四种不同细胞系(成纤维细胞、肌肉、肝癌和骨髓性白血病细胞系)中证实了其存在。这种异构体约占总亚铁螯合酶mRNA的20%,是通过内含子2中第二个供体位点的剪接产生的,其存在与EPP无关。
