晚发型线粒体脑肌病伴高乳酸血症和卒中样发作临床特点

doi:10.3969/j.issn.1672-6731.2020.03.015

摘要/Abstract

摘要：

目的总结10例晚发型线粒体脑肌病伴高乳酸血症和卒中样发作（MELAS）患者的临床、病理及基因突变特点。方法与结果 回顾分析2007年1月至2018年12月共10例晚发型MELAS患者的临床资料，8例患者行骨骼肌组织活检术。聚合酶链反应-限制性片段长度多态性和线粒体DNA （mtDNA）全长测序法进行mtDNA突变筛查；焦磷酸测序法检测部分患者血液m.3243A > G突变比例。结果显示，10例患者首次脑卒中样发作的年龄为40~67岁，其主要表现包括癫发作、失语、头痛、痴呆、精神障碍、肢体轻瘫及视力下降，既往糖尿病5例、神经性耳聋6例、高血压3例、脑梗死2例。6例患者有母系遗传的糖尿病家族史，2例有MELAS家族史。辅助检查可见6例有高脂血症，6例有颈动脉粥样硬化，1例有右颈内动脉及大脑中动脉狭窄。头部MRI显示累及1个或多个脑叶的皮质病变，4例同时存在脑干及基底节区多发缺血灶。7例肌肉组织活检发现破碎红纤维及琥珀酸脱氢酶深染血管，1例未见明显异常。基因分析显示，10例患者均携带mtDNA突变，9例为m.3243A > G突变，1例为m.10191T > C突变。7例m.3243A > G突变患者血液中突变比例为9%～33%。结论晚发型MELAS患者的临床表型与经典型患者无明显差异，但发病年龄晚，并可合并多种脑血管危险因素及大动脉粥样硬化。m.3243A > G突变为本组晚发型MELAS患者的热点突变，但血液中突变比例较低。

关键词: MELAS综合征, 晚发性障碍, DNA,线粒体, 突变

Abstract:

Objective To summarize the clinical, pathological and genetic features of 10 patients with late-onset mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes (MELAS). Methods and Results The clinical data of 10 patients with late-onset MELAS were retrospectively analyzed from January 2007 to December 2018. Muscle biopsy was performed in 8 cases. Polymerase chain reaction-fragment length polymorphism (PCR-RFLP) analysis and whole sequencing of mitochondrial DNA (mtDNA) were used to screen mtDNA mutations, and the mutation load of m.3243A > G in blood was detected by pyrophosphate sequencing. The onset age of the first stroke-like episodes were 40-67 years old in all patients. The main manifestations included epilepsy, aphasia, headache, dementia, mental disorder, limb paralysis and visual impairment. Past history revealed 5 cases with diabetes mellitus, 6 with deafness, 3 with hypertension and 2 with stroke. Six patients had a family history of maternally inherited diabetic mellitus, and 2 had a family history of MELAS. Laboratory examination revealed 6 cases with hyperlipidemia, 6 with carotid atherosclerosis, 1 with stenosis of right internal carotid artery and middle cerebral artery. Brain MRI showed cortex lesions involving one or more lobes in all patients, and 4 cases also had multiple infarctions in brainstem and basal ganglia. Muscle biopsy demonstrated ragged red fiber (RRF) and strongly succinate dehydrogenase-stained vessels (SSVs) in all of 8 patients except one. Genetic analysis identified 9 cases with m.3243A > G, and 1 with m.10191T > C mutation. The blood mutation load of m.3243A > G was 9%-33% in 7 cases. Conclusions The clinical phenotype of patients with late-onset MELAS was not significantly different from that of typical patients. However, the age of onset in late-onset MELAS was late, and it could be complicated with a variety of cerebrovascular risk factors and atherosclerosis. The hotspot mutation of this group of late-onset MELAS patients was m.3243A > G, but the mutation rate in blood was low.

Key words: MELAS syndrome, Late onset disorders, DNA,mitochondrial, Mutation

赵丹华, 赵旭彤, 邢海英, 张晓, 张哲, 刘献增, 袁云, 王朝霞. 晚发型线粒体脑肌病伴高乳酸血症和卒中样发作临床特点[J]. 中国现代神经疾病杂志, 2020, 20(3): 224-229.

ZHAO Dan-hua, ZHAO Xu-tong, XING Hai-ying, ZHANG Xiao, ZHANG Zhe, LIU Xian-zeng, YUAN Yun, WANG Zhao-xia. Clinical features of the late-onset mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes[J]. Chinese Journal of Contemporary Neurology and Neurosurgery, 2020, 20(3): 224-229.

https://journal11.magtechjournal.com/cjcnn/CN/Y2020/V20/I3/224

参考文献

[1] Zhao D, Hong D, Zhang W, Yao S, Qi X, Lv H, Zheng R, Feng L, Huang Y, Yuan Y, Wang Z. Mutations in mitochondrially encoded complex Ⅰ enzyme as the second common cause in a cohort of Chinese patients with mitochondrial myopathy, encephalopathy, lactic acidosis and stroke-like episodes[J]. J Hum Genet, 2011, 56:759-764.
[2] Hirano M, Ricci E, Koenigsberger MR, Defendini R, Pavlakis SG, DeVivo DC, DiMauro S, Rowland LP. MELAS: an original case and clinical criteria for diagnosis[J]. Neuromuscul Disord, 1992, 2:125-135.
[3] Smith K, Chiu S, Hunt C, Chandregowda A, Babovic-Vuksanovic D, Keegan BM. Late-onset mitochondrial encephalopathy, lactic acidosis, and stroke-like episodes presenting with auditory agnosia[J]. Neurologist, 2019, 24:90-92.
[4] Zhu K, Li S, Chen H, Wang Y, Yu M, Wang H, Zhao W, Cao Y. Late onset MELAS with m.3243A > G mutation and its association with aneurysm formation[J]. Metab Brain Dis, 2017, 32:1069-1072.
[5] Sunde K, Blackburn PR, Cheema A, Gass J, Jackson J, Macklin S, Atwal PS. Case report: 5 year follow-up of adult late-onset mitochondrial encephalomyopathy with lactic acid and stroke-like episodes (MELAS)[J]. Mol Genet Metab Rep, 2016, 9:94-97.
[6] Xu XB, Ji KQ, Lyu JW, Zhang S, Lyu XQ, Liu C, Li W, Yan CZ, Zhao YY. Late-onset mitochondrial disease in a patient with MELAS and mitochondrial DNA T14487C mutation[J]. Chin Med J (Engl), 2019, 132:716-718.
[7] Kimata KG, Gordan L, Ajax ET, Davis PH, Grabowski T. A case of late-onset MELAS[J]. Arch Neurol, 1998, 55:722-725.
[8] Kisanuki YY, Gruis KL, Smith TL, Brown DL. Late-onset mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke like episodes with bitemporal lesions[J]. Arch Neurol, 2006, 63:1200-1201.
[9] Bataillard M, Chatzoglou E, Rumbach L, Sternberg D, Tournade A, Laforêt P, Jardel C, Maisonobe T, Lombès A. Atypical MELAS syndrome associated with a new mitochondrial tRNA glutamine point mutation[J]. Neurology, 2001, 56:405-407.
[10] Fang GL, Zheng Y, Zhang YX. Mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes in an older adult mimicking cerebral infarction: a Chinese case report[J]. Clin Interv Aging, 2018, 13:2421-2424.
[11] Vanniarajan A, Nayak D, Reddy AG, Singh L, Thangaraj K. Clinical and genetic uniqueness in an individual with MELAS[J]. Am J Med Genet B Neuropsychiatr Genet, 2006, 141B:440-444.
[12] Aurangzeb S, Vale T, Tofaris G, Poulton J, Turner MR. Mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes (MELAS) in the older adult[J]. Pract Neurol, 2014, 14:432-436.
[13] Ban R, Pu CQ, Liu HX, Shi Q, Wei MM, Song HW, Zhang YT. Late onset mitochondrial encephalomyopathy, lactic acidosis, and stroke-like episodes: one case report[J]. Zhonghua Shen Jing Ke Za Zhi, 2017, 50:773-774.[班瑞, 蒲传强, 刘华旭, 石强, 魏妙妙, 宋海文, 张羽彤. 成人晚发的线粒体脑肌病伴乳酸血症和卒中样发作一例[J]. 中华神经科杂志, 2017, 50:773-774.]
[14] Sinnecker T, Andelova M, Mayr M, Rüegg S, Sinnreich M, Hench J, Frank S, Schaller A, Stippich C, Wuerfel J, Bonati LH. Diagnosis of adult-onset MELAS syndrome in a 63-year-old patient with suspected recurrent strokes: a case report[J]. BMC Neurol, 2019, 19:91.
[15] Hsu YC, Yang FC, Perng CL, Tso AC, Wong LJ, Hsu CH. Adult-onset of mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) syndrome presenting as acute meningoencephalitis: a case report[J]. J Emerg Med, 2012, 43: e163-166.
[16] Gagliardi D, Mauri E, Magri F, Velardo D, Meneri M, Abati E, Brusa R, Faravelli I, Piga D, Ronchi D, Triulzi F, Peverelli L, Sciacco M, Bresolin N, Comi GP, Corti S, Govoni A. Can intestinal pseudo-obstruction drive recurrent stroke-like episodes in late-onset MELAS syndrome: a case report and review of the literature[J]? Front Neurol, 2019, 10:38.
[17] Yatsuga S, Povalko N, Nishioka J, Katayama K, Kakimoto N, Matsuishi T, Kakuma T, Koga Y; Taro Matsuoka for MELAS Study Group in Japan. MELAS: a nationwide prospective cohort study of 96 patients in Japan[J]. Biochim Biophys Acta, 2012, 1820:619-624.
[18] Jeppesen TD, Schwartz M, Hansen K, Danielsen ER, Wibrand F, Vissing J. Late onset of stroke-like episode associated with a 3256C--> T point mutation of mitochondrial DNA[J]. J Neurol Sci, 2003, 214:17-20.
[19] Zhang Z, Zhao DH, Liu J, Zuo YH, Xiong H, Lü H, Zhang W, Yuan Y, Wang ZX. Clinical features of mitochondrial encephlomyopathy, lactic acidosis and stroke-like episodes: an analysis of 190 cases[J]. Zhonghua Shen Jing Ke Za Zhi, 2016, 49:237-242.[张哲, 赵丹华, 刘婧, 左越焕, 熊晖, 吕鹤, 张巍, 袁云, 王朝霞. 线粒体脑肌病伴乳酸血症和卒中样发作190例的临床特征分析[J]. 中华神经科杂志, 2016, 49:237-242.]
[20] Xu W, Wen J, Sun C, Cao J, Li Y, Geng D. Conventional and diffusional magnetic resonance imaging features of mitochondrial encephalomyopathy, lactic acidosis, and stroke-like episodes in Chinese patients: a study of 40 cases[J]. J Comput Assist Tomogr, 2018, 42:510-516.
[21] Lu Y, Deng J, Zhao Y, Zhang Z, Hong D, Yao S, Zhao D, Xie J, Fang H, Yuan Y, Wang Z. Patients with MELAS with negative myopathology for characteristic ragged-red fibers[J]. J Neurol Sci, 2020, 408:116499.
[22] Picard M, Zhang J, Hancock S, Derbeneva O, Golhar R, Golik P, O'Hearn S, Levy S, Potluri P, Lvova M, Davila A, Lin CS, Perin JC, Rappaport EF, Hakonarson H, Trounce IA, Procaccio V, Wallace DC. Progressive increase in mtDNA 3243A > G heteroplasmy causes abrupt transcriptional reprogramming[J]. Proc Natl Acad Sci USA, 2014, 111:E4033-4042.

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Clinical features of the late-onset mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes

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Clinical features of the late-onset mitochondrial encephalomyopathy with lactic acidosis and stroke-like episodes

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