Floderus Y, Shoolingin-Jordan P M, Harper P
Porphyria Centre Sweden, Huddinge University Hospital, Stockholm, Sweden.
Clin Genet. 2002 Oct;62(4):288-97. doi: 10.1034/j.1399-0004.2002.620406.x.
Acute intermittent porphyria (AIP) is an autosomal dominant disorder caused by a partial deficit of porphobilinogen deaminase (PBGD), the third of eight enzymes in the haem biosynthetic pathway. The overt disease is characterized by neuropsychiatric symptoms that are often triggered by exogenous factors such as certain drugs, stress, and alcohol. The aim of this work has been to identify the underlying genetic defect in each AIP-affected family in order to provide early counselling to assist in the avoidance of precipitating factors. The prevalence of AIP in Sweden is in the order of 1:10 000. The major mutation in Sweden, W198X, is due to a founder effect in the northern part of the country. This mutation, together with a further 11 mutations, have been reported previously. The present communication encompasses the great majority of AIP kindreds in Sweden and includes a further 27 mutations within the PBGD gene. This includes 14 completely new mutations, as well as 11 known mutations detected for the first time in Sweden. The majority of the mutations are located in exons 10 and 12 with fewer in exon 7. The clinical and biochemical outcomes in some patients are described. We also use the three-dimensional structure of the porphobilinogen deaminase enzyme to predict the possible molecular and functional consequences of the new Swedish missense and nonsense mutations.
急性间歇性卟啉病(AIP)是一种常染色体显性疾病,由胆色素原脱氨酶(PBGD)部分缺乏引起,PBGD是血红素生物合成途径中八种酶的第三种。显性疾病的特征是神经精神症状,常由某些药物、压力和酒精等外源性因素引发。这项工作的目的是确定每个受AIP影响家庭的潜在基因缺陷,以便提供早期咨询,帮助避免诱发因素。AIP在瑞典的患病率约为1:10000。瑞典的主要突变W198X是由于该国北部的奠基者效应。此前已报道了该突变以及另外11种突变。本报告涵盖了瑞典绝大多数AIP家族,并包括PBGD基因内另外27种突变。这包括14种全新突变,以及11种在瑞典首次检测到的已知突变。大多数突变位于第10和12外显子,第7外显子中的较少。描述了一些患者的临床和生化结果。我们还利用胆色素原脱氨酶的三维结构预测瑞典新错义突变和无义突变可能的分子和功能后果。
