Yoo Da Hye, Choi Young-Chul, Nam Da Eun, Choi Sun Seong, Kim Ji Won, Choi Byung-Ok, Chung Ki Wha
Department of Biological Sciences, Kongju National University, Gongju, Republic of Korea.
Department of Neurology, Yonsei University College of Medicine, Seoul, Republic of Korea.
Mitochondrion. 2017 Jul;35:54-58. doi: 10.1016/j.mito.2017.05.005. Epub 2017 May 9.
Mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) is a condition that affects many parts of the body, particularly the brain and muscles. This study examined a Korean MELAS-like syndrome patient with seizure, stroke-like episode, and optic atrophy. Target sequencing of whole mtDNA and 73 nuclear genes identified compound heterozygous mutations p.R205X and p.L255P in the FASTKD2. Each of his unaffected parents has one of the two mutations, and both mutations were not found in 302 controls. FASTKD2 encodes a FAS-activated serine-threonine (FAST) kinase domain 2 which locates in the mitochondrial inner compartment. A FASTKD2 nonsense mutation was once reported as the cause of a recessive infantile mitochondrial encephalomyopathy. The present case showed relatively mild symptoms with a late onset age, compared to a previous patient with FASTKD2 mutation, implicating an inter-allelic clinical heterogeneity. Because this study is the second report of an autosomal recessive mitochondrial encephalomyopathy patient with a FASTKD2 mutation, it will extend the phenotypic spectrum of the FASTKD2 mutation.
线粒体肌病、脑病、乳酸酸中毒和卒中样发作(MELAS)是一种影响身体多个部位的疾病,尤其是大脑和肌肉。本研究对一名患有癫痫、卒中样发作和视神经萎缩的韩国MELAS样综合征患者进行了检查。对整个线粒体DNA(mtDNA)和73个核基因进行靶向测序,在FASTKD2基因中鉴定出复合杂合突变p.R205X和p.L255P。他未受影响的父母各携带这两种突变中的一种,且在302名对照中均未发现这两种突变。FASTKD2编码一种位于线粒体内腔的FAS激活的丝氨酸 - 苏氨酸(FAST)激酶结构域2。曾有报道称FASTKD2无义突变是一种隐性婴儿线粒体脑病的病因。与先前报道的携带FASTKD2突变的患者相比,本病例症状相对较轻且发病年龄较晚,提示存在等位基因间临床异质性。由于本研究是关于携带FASTKD2突变的常染色体隐性线粒体脑病患者的第二篇报道,它将扩展FASTKD2突变的表型谱。
