Jaksch M, Kleinle S, Scharfe C, Klopstock T, Pongratz D, Müller-Höcker J, Gerbitz K D, Liechti-Gallati S, Lochmuller H, Horvath R
Metabolic Disease Centre Munich-Schwabing and Institute of Clinical Chemistry, Diagnostic Molecular Biology, and Mitochondrial Genetics, Munich, Germany.
J Med Genet. 2001 Oct;38(10):665-73. doi: 10.1136/jmg.38.10.665.
To evaluate the frequency of pathogenic mtDNA transfer RNA mutations and deletions in biochemically demonstrable respiratory chain (RC) deficiencies in paediatric and adult patients.
We screened for deletions and sequenced mitochondrial transfer RNA genes in skeletal muscle DNA from 225 index patients with clinical symptoms suggestive of a mitochondrial disorder and with biochemically demonstrable RC deficiency in skeletal muscle.
We found pathogenic mitochondrial DNA mutations in 29% of the patients. The detection rate was significantly higher in adults (48%) than in the paediatric group (18%). Only one pathogenic mutation was detected in the neonatal group. In addition, we describe seven novel transfer RNA sequence variations with unknown pathogenic relevance (six homoplasmic and one heteroplasmic) and 13 homoplasmic polymorphisms. One heteroplasmic transfer RNA(Leu(UUR)) A>G mutation at position 3274 is associated with a distinct neurological syndrome.
We provide an estimation of the frequency of mitochondrial transfer RNA mutations and deletions in paediatric and adult patients with respiratory chain deficiencies.
评估儿科和成年患者中,生化检测可证实的呼吸链(RC)缺陷中致病性线粒体DNA转移RNA突变和缺失的频率。
我们对225例索引患者的骨骼肌DNA中的缺失进行了筛查,并对线粒体转移RNA基因进行了测序,这些患者有提示线粒体疾病的临床症状,且骨骼肌中生化检测可证实存在RC缺陷。
我们在29%的患者中发现了致病性线粒体DNA突变。成人组(48%)的检出率显著高于儿科组(18%)。新生儿组仅检测到一个致病性突变。此外,我们描述了7个致病性相关性未知的新型转移RNA序列变异(6个同质型和1个异质型)以及13个同质型多态性。第3274位的一个异质型转移RNA(Leu(UUR)) A>G突变与一种独特的神经综合征相关。
我们对呼吸链缺陷的儿科和成年患者中线粒体转移RNA突变和缺失的频率进行了评估。