van den Heuvel L, Ruitenbeek W, Smeets R, Gelman-Kohan Z, Elpeleg O, Loeffen J, Trijbels F, Mariman E, de Bruijn D, Smeitink J
Department of Pediatrics, University Hospital, Nijmegen, The Netherlands.
Am J Hum Genet. 1998 Feb;62(2):262-8. doi: 10.1086/301716.
We report the cDNA cloning, chromosomal localization, and a mutation in the human nuclear gene encoding the 18-kD (AQDQ) subunit of the mitochondrial respiratory chain complex I. The cDNA has an open reading frame of 175 amino acids and codes for a protein with a molecular mass of 23.2 kD. Its gene was mapped to chromosome 5. A homozygous 5-bp duplication, destroying a consensus phosphorylation site, in the 18-kD cDNA was found in a complex I-deficient patient. The patient showed normal muscle morphology and a remarkably nonspecific fatal progressive phenotype without increased lactate concentrations in body fluids. The child's parents were heterozygous for the mutation. In 19 other complex I-deficient patients, no mutations were found in the 18-kD gene.
我们报告了编码线粒体呼吸链复合体I的18-kD(AQDQ)亚基的人类核基因的cDNA克隆、染色体定位及一个突变。该cDNA有一个175个氨基酸的开放阅读框,编码一个分子量为23.2 kD的蛋白质。其基因定位于5号染色体。在一名复合体I缺陷患者中,发现18-kD cDNA中有一个纯合的5-bp重复,破坏了一个共有磷酸化位点。该患者肌肉形态正常,表现出明显的非特异性致命进行性表型,体液中乳酸浓度未升高。患儿的父母为该突变的杂合子。在其他19名复合体I缺陷患者中,未在18-kD基因中发现突变。
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