SURF1基因两个新突变致Leigh综合征1例

目的研究1例因常染色体Surfe it 1(SURF1)基因2个新突变所致Le igh综合征女童的临床及其突变特点。方法患儿为第一胎,生后运动发育落后,4岁时出现肢体震颤,进行性加重,伴运动倒退。4岁6个月来院时不能独站,左侧肢体痉挛性瘫痪,血乳酸、丙酮酸增高,腓肠肌活检未见异常。脑MR I显示双侧基底节、小脑脚上交叉多发性软化灶,符合Le igh综合征诊断。患者曾口服安坦、维生素B1等药物无效,12岁死于肺炎、呼吸衰竭。本研究运用聚合酶链式反应扩增SURF1基因的9个外显子序列,对患儿及103名正常人的外周血白细胞DNA进行正反向序列测定检测突变。结果患者线粒体基因筛查未见异常,SURF1基因测序发现了分别位于内含子3的240+1G>C剪切位点突变和外显子6的574C>G错义突变两个杂合性新突变。结论细胞色素C氧化酶缺陷是Le igh综合征的常见原因,本研究通过对1例中国Le igh综合征患者的SURF1基因分析,首次发现了240+1G>C和574C>G两个新突变,不仅明确了患者病因,并将进一步充实人类Le igh综合征致病基因库。

SURF1基因突变导致Leigh综合征家系1例

Leigh综合征是一种由于线粒体氧化磷酸化障碍所导致的严重退行性脑病。常染色体SURF1基因突变所致细胞色素C氧化酶缺乏是导致Leigh综合征的常见原因,国外已报道多种突变类型。该研究回顾了1例SURF1基因604G>C杂合性错义突变所致中国人Leigh综合征患者及其家系的临床与遗传学特点。患者,女, 9个月起病,表现为喂养困难,营养不良,进行性运动倒退,肌张力低下,眼震。17个月时来院就诊, 23个月时死于呼吸衰竭。脑MRI显示双侧基底节对称性损害,脑干、小脑萎缩。聚合酶链式反应扩增SURF1基因的全部外显子,进行序列测定及限制性片断长度多态性分析均显示患者及其母亲、舅舅的SURF1基因的外显子7存在一个604G>C杂合性错义突变,其父亲及正常对照的相关外显子序列未发现异常。该研究首次报道了1例中国人群中由于SURF1基因604G>C杂合性错义突变导致的Leigh综合征及其家系,不仅明确了病因,亦将有助于今后对患者家系的遗传咨询。

导致Leigh综合征的SURF1基因的两个新突变

目的研究 1例因常染色体 SURF1基因新突变所致 Leigh综合征患者的临床及遗传学的特点.方法提取患儿外周血白细胞 DNA,先进行线粒体基因热点突变的筛查,然后运用聚合酶链式反应扩增 SURF1基因的全部外显子序列,进行正反向序列测定以检测突变. 103名无关健康个体为正常对照组. 结果患儿从 1岁 2个月起出现进行性运动智力倒退,无力,喂养困难, 2岁 3个月时死于呼吸衰竭.其兄临床经过类似, 2岁时死亡.线粒体基因筛查排除 8993C>T、 3243A>G、 8344A>G突变. SURF1基因序列测定显示该患者存在复合杂合性缺失,分别为外显子 7第 622位缺失 A( 622delA)和第 653～ 654位缺失 CT( 653-654delCT).结论 SURF1基因参与调控细胞色素 C氧化酶复合物的组装,而细胞色素 C氧化酶复合物缺陷是导致 Leigh综合征的主要原因.本研究发现了 SURF1基因 622delA以及 653-654delCT两个杂合性缺失为 2个新突变,明确了患者的病因,并进一步充实了人类 Leigh综合征致病基因库,将有助于今后 Leigh综合征家系的遗传咨询.

细胞色素C氧化酶缺乏的Leigh综合征伴SURF1基因纯合突变

Leigh syndrome is a heterogeneous disorder, usually due to a defect in oxidati ve metabolism. Mutations in SURF1 gene have been identified in patients with cyt ochrome c oxidase deficiency. We report a homozygous splice site deletion [516- 2 516-1delAG] in a young girl presenting with cytochrome c oxidase-deficient L eigh syndrome. Identification of molecular defect is indispensable for genetic c ounselling and prenatal diagnosis.

儿童Charcot-Marie-Tooth病4K型1例报道

Charcot-Marie-Tooth病4K型(CMT4K)是一种周围感觉神经性疾病,SURF1基因与CMT4K报道较为少见,本文对我院收治的1例SURF1基因2个杂合突变所致CMT4K型进行报道。

肥大性下橄榄核变性分子遗传学研究进展

肥大性下橄榄核变性（HOD）是一种临床少见的神经系统变性疾病,临床特点为在原发病变稳定后出现头晕、视物不清、眼震、腭肌阵挛、肢体震颤、共济失调等表现,其中上腭震颤为其典型症状,通常在格莫三角损伤后数周至数月出现,约5~24周症状达到高峰。原发脑损伤疾病已经给患者带来很多痛苦,而HOD这一继发病症的出现又再次加重了躯体损伤,增加了患者精神及经济负担,因此,如何早期诊断并有效干预成为临床研究热点。

Clinical and laboratory survey of 65 Chinese patients with Leigh syndrome

Background Leigh syndrome is an inherited neurodegenerative disease that emerges in infancy and childhood and presents with a clinically heterogeneous variety of neuromuscular and non-neuromuscular disorders. It can result from the inheritance of mutations in either nuclear or mitochondrial DNA. In the current study, we performed a retrospective study in 65 patients in order to investigate the clinical and genetic characteristics of Leigh syndrome in Chinese patients. Methods Sixty-five unrelated cases （35 men and 30 women） who were hospitalized in the past 12 years were reviewed. Diagnosis was based on both the clinical presentation and the characteristic neuropathologic findings of bilateral symmetric necrotizing lesions in the basal ganglia and brain stem as detected using cranial computed tomography （CT） scan or magnetic resonance imaging （MRI）. The differential diagnosis of organic acidurias and fatty acid IS-oxidation defects were performed. Specific point mutations and deletions in mitochondrial DNA （T8993G, T8993C, T9176C, A8344G, A3243G） were screened by PCR-restriction analysis and Southern blot. The SURF1 gene was sequenced. Skeletal muscle biopsies were performed in 17 （26.2%） of the patients. The diagnosis was confirmed by autopsy in 6 （9.2%） patients. Results The patients had various forms of metabolic encephalomyopathy. Filly-nine （90.8%） of the patients had the typical neuroradiological features of Leigh syndrome, including symmetrical necrotizing lesions scattered within the basal ganglia, thalamus and brain stem. Twenty （30.8%） patients were confirmed by genetic, biochemical analysis and autopsy. Specific point mutations in mitochondrial DNA were found in 5 cases （7.7%）. Of these, the A8344G mutation was detected in 2 patients. The T8993G T8993C, and A3243G point mutations were identified in 3 other patients, respectively. SURF1 mutations associated with cytochrome c oxidase deficiency were identified in 8 （12.3%） families by DNA sequencing. A G604C mutation was identified in 6 （9.2%） patients. The genotypes of 52 patients remained unknown. Conclusions Leigh syndrome presents as a diverse array of clinical features and can result from specific mutations in nuclear or mitochondrial DNA. In this study, SURF1 mutations associated with cytochrome c oxidase deficiency were identified in 8 （12.3%） out of 65 patients with Leigh syndrome. It indicates that SURF1 mutations might be a common cause of Leigh syndrome in China. The etiology of Leigh syndrome in Chinese patients represents a persistent challenge to clinicians.