Department of Laboratory Medicine, Sahlgrenska Academy, University of Gothenburg, Gothenburg, Sweden.
Department of Neurology, Sahlgrenska University Hospital, Gothenburg, Sweden.
Acta Neurol Scand. 2021 Jan;143(1):103-108. doi: 10.1111/ane.13339. Epub 2020 Sep 19.
To describe two patients with progressive external ophthalmoplegia (PEO) and mitochondrial myopathy associated with mutations in mitochondrial DNA, encoding the tRNA gene (MT-TN), which have not previously been published with clinical descriptions.
MATERIALS & METHODS: Two unrelated patients with PEO were clinically examined. Muscle biopsy was performed and investigated by exome sequencing, enzyme histochemistry, and immunohistochemistry. The level of heteroplasmy was investigated in single muscle fibers and in other tissues.
Patient 1 was a 52-year-old man with ptosis, PEO, and exercise intolerance since childhood. Muscle biopsy demonstrated mitochondrial myopathy with frequent cytochrome c oxidase (COX)-deficient fibers and a heteroplasmic mutation, m.5669G>A in the MT-TN gene, resulting in a substitution of a highly conserved C to T in the T stem of tRNA . Patient 2 was a 66-year-old woman with ptosis, PEO, and exercise intolerance since many years. Muscle biopsy demonstrated mitochondrial myopathy with frequent COX-deficient fibers. She had a novel m.5702delA mutation in MT-TN, resulting in loss of a highly conserved U in the anticodon stem of tRNA . Single fiber analysis in both cases showed highly significant differences in mutation load between COX-deficient and COX-normal fibers and a high threshold level for COX deficiency. The mutations were not found in blood, urine sediment or buccal cells.
We describe two MT-TN mutations associated with PEO and mitochondrial myopathy, and their pathogenicity was demonstrated. Together with previous reports, the results indicate that MT-TN is a hot spot for mutations causing sporadic PEO.
描述两例进展性眼外肌麻痹(PEO)和线粒体肌病患者,他们均携带先前未报道过的线粒体 DNA 编码 tRNA 基因(MT-TN)突变。
对两例无关联的 PEO 患者进行临床检查。进行肌肉活检,并通过外显子组测序、酶组织化学和免疫组织化学进行研究。还检测了单根肌肉纤维和其他组织中的异质性水平。
患者 1 为 52 岁男性,自童年起即出现眼睑下垂、PEO 和运动不耐受。肌肉活检显示线粒体肌病,伴频繁细胞色素 c 氧化酶(COX)缺陷纤维和 MT-TN 基因 m.5669G>A 杂合性突变,导致 tRNA 的 T 臂中高度保守的 C 突变为 T。患者 2 为 66 岁女性,自多年前起即出现眼睑下垂、PEO 和运动不耐受。肌肉活检显示线粒体肌病,伴频繁 COX 缺陷纤维。她携带 MT-TN 基因 m.5702delA 新突变,导致 tRNA 的反密码子茎中高度保守的 U 缺失。这两例患者的单纤维分析均显示 COX 缺陷纤维与 COX 正常纤维之间的突变负荷存在显著差异,且 COX 缺陷存在高阈值。这些突变未在血液、尿液沉淀物或口腔细胞中发现。
我们描述了两例与 PEO 和线粒体肌病相关的 MT-TN 突变,并证实了其致病性。结合以往的报告,结果表明 MT-TN 是导致散发性 PEO 的突变热点。
