Raben N, Sherman J, Miller F, Mena H, Plotz P
Arthritis and Rheumatism Branch, National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, Bethesda, Maryland.
J Biol Chem. 1993 Mar 5;268(7):4963-7.
A deficiency of the muscle isoform of the enzyme, phosphofructokinase (PFK, EC 2.7.1.11), leads to an illness (glycogenosis, Type VII) characterized by myopathy and hemolysis. A patient with this disease and an affected sister were found to have a G to A substitution at the 5' donor site of intron 5 of the PFK-M gene. This mutation led to a splicing defect: a complete deletion of the preceding exon in the patient's mRNA. The patient, an affected sister, and related and unrelated family members, who were of Ashkenazic Jewish background, were screened for the mutation by denaturing gradient gel electrophoresis and by allele specific hybridization of genomic DNA. The affected sisters are homozygous for the mutation, and their children, who are unaffected, are heterozygous. The only previously characterized genetic defect in this disease, found in a Japanese patient, was a G to T mutation at the beginning of intron 15 with splicing to a cryptic site within exon 15 (1). Both mutations lead to inframe deletions, but of different parts of the protein. The differences between the two aberrant proteins may account for clinical differences between our patients and the Japanese patient.
磷酸果糖激酶(PFK,EC 2.7.1.11)的肌肉同工酶缺乏会导致一种以肌病和溶血为特征的疾病(糖原贮积症VII型)。发现一名患有这种疾病的患者及其患病的妹妹在PFK-M基因第5内含子的5'供体位点存在G到A的替换。这种突变导致了剪接缺陷:患者mRNA中前一个外显子完全缺失。通过变性梯度凝胶电泳和基因组DNA的等位基因特异性杂交,对该患者、其患病的妹妹以及具有阿什肯纳兹犹太背景的相关和不相关家庭成员进行了突变筛查。患病的姐妹对该突变是纯合的,而她们未患病的孩子是杂合的。在一名日本患者中发现的这种疾病之前唯一特征化的遗传缺陷是第15内含子起始处的G到T突变,并剪接到外显子15内的一个隐蔽位点(1)。两种突变都导致读框内缺失,但缺失蛋白质的不同部分。这两种异常蛋白质之间的差异可能解释了我们的患者与日本患者之间的临床差异。
