Filosto Massimiliano, Mancuso Michelangelo, Nishigaki Yutaka, Pancrudo Jacklyn, Harati Yadollah, Gooch Clifton, Mankodi Ami, Bayne Lydia, Bonilla Eduardo, Shanske Sara, Hirano Michio, DiMauro Salvatore
Department of Neurology, Columbia University College of Physicians and Surgeons, New York, NY 10032, USA.
Arch Neurol. 2003 Sep;60(9):1279-84. doi: 10.1001/archneur.60.9.1279.
The mendelian forms of progressive external ophthalmoplegia (PEO) associated with multiple mitochondrial DNA deletions are clinically heterogeneous disorders transmitted as dominant or recessive traits. Autosomal dominant PEO is caused by mutations in at least 3 genes: adenine nucleotide translocator-1 (ANT1), encoding the muscle-specific adenine nucleotide translocator; chromosome 10 open reading frame 2 (C10orf2), encoding Twinkle helicase; and polymerase gamma (POLG), encoding the alpha subunit of polymerase gamma. Mutations in POLG can also cause autosomal recessive PEO, which is often associated with multisystemic disorders.
To further investigate the frequency and genotype-phenotype correlations of mutations in the POLG gene, we used single-stranded conformational polymorphism analysis and direct sequencing to screen 30 patients with familial or sporadic PEO and multiple mitochondrial DNA deletions in muscle but without mutations in ANT1 and C10orf2.
Four unrelated patients had novel POLG mutations. A woman with PEO and mental retardation had a heterozygous Gly1076Val mutation. Two patients, one with PEO, exercise intolerance, and gastrointestinal dysmotility and the other with PEO, neuropathy, deafness, and hypogonadism, both had a Pro587Leu change. The fourth patient, who was compound heterozygous for Ala889Thr and Arg579Trp mutations, had PEO, gastrointestinal dysmotility, and neuropathy. These mutations were not detected in 120 healthy control alleles.
Our results demonstrate that POLG mutations account for a substantial proportion of patients (13%) with PEO and multiple mitochondrial DNA deletions and cause both clinically and genetically heterogeneous disorders.
与多个线粒体DNA缺失相关的孟德尔式进行性眼外肌麻痹(PEO)是临床异质性疾病,以显性或隐性性状遗传。常染色体显性PEO由至少3个基因突变引起:腺嘌呤核苷酸转位酶-1(ANT1),编码肌肉特异性腺嘌呤核苷酸转位酶;10号染色体开放阅读框2(C10orf2),编码Twinkle解旋酶;以及聚合酶γ(POLG),编码聚合酶γ的α亚基。POLG基因突变也可导致常染色体隐性PEO,后者常与多系统疾病相关。
为进一步研究POLG基因突变的频率及其基因型与表型的相关性,我们采用单链构象多态性分析和直接测序法,对30例家族性或散发性PEO患者进行筛查,这些患者肌肉中有多个线粒体DNA缺失,但ANT1和C10orf2无突变。
4例无亲缘关系的患者有新的POLG基因突变。1例患有PEO和智力发育迟缓的女性有杂合的Gly1076Val突变。2例患者,1例患有PEO、运动不耐受和胃肠动力障碍,另1例患有PEO、神经病变、耳聋和性腺功能减退,均有Pro587Leu改变。第4例患者为Ala889Thr和Arg579Trp突变的复合杂合子,患有PEO、胃肠动力障碍和神经病变。在120个健康对照等位基因中未检测到这些突变。
我们的结果表明,POLG基因突变在患有PEO和多个线粒体DNA缺失的患者中占相当比例(13%),并导致临床和遗传异质性疾病。
