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导致Leigh综合征的SURF1基因的两个新突变 被引量:1
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作者 孙芳 张尧 +7 位作者 杨艳玲 戚豫 王朝霞 宋金青 钱宁 王丽 秦炯 吴希如 《临床儿科杂志》 CAS CSCD 北大核心 2005年第8期534-537,共4页
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... 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. 展开更多
关键词 亚急性坏死性脑脊髓病(Leigh综合征) SURFl基因 细胞色素 C氧化酶 新突变
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儿童Charcot-Marie-Tooth病4K型1例报道
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作者 朱晓霞 林华 罗军 《罕少疾病杂志》 2022年第9期14-15,共2页
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。
关键词 儿童 Charcot-Marie-Tooth病4K型 surf1基因
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腓骨肌萎缩症4K型1例
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作者 孙丽 周露露 郭虎 《中国优生与遗传杂志》 2024年第8期1686-1689,共4页
目的探讨常染色体隐性遗传腓骨肌萎缩症4K型(CMT4K)患儿的临床和基因型特点。方法回顾性分析南京医科大学附属儿童医院确诊的1例腓骨肌萎缩症4K型患儿的临床资料。结果患儿,男,1岁7月龄。运动发育落后4个月,肌张力低下,肌电图提示脱髓... 目的探讨常染色体隐性遗传腓骨肌萎缩症4K型(CMT4K)患儿的临床和基因型特点。方法回顾性分析南京医科大学附属儿童医院确诊的1例腓骨肌萎缩症4K型患儿的临床资料。结果患儿,男,1岁7月龄。运动发育落后4个月,肌张力低下,肌电图提示脱髓鞘性多发周围神经源性损害肌电改变,基因测序提示细胞色素C氧化酶组装因子(SURF1)基因有2个杂合突变,先证者之父在位点c.314_317delTGCC(p.L105Qfs*7)出现杂合变异,受检人之母在位点c.588+1_588+3delGTA(splicing)出现杂合变异,从而确诊CMT4K。结论CMT4K为一种由SURF1突变所致的常染色体隐性遗传性疾病,表型呈临床异质性,本研究发现的杂合突变c.314_317delTGCC和c.588+1_588+3delGTA扩大了SURF1基因突变谱。 展开更多
关键词 CMT4K surf1基因 临床表型
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Clinical and laboratory survey of 65 Chinese patients with Leigh syndrome 被引量:17
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作者 YANG Yan-ling SUN Fang +12 位作者 ZHANG Yao QIAN Ning YUAN Yun WANG Zhao-xia QI Yu XIAO Jiang-xi WANG Xiao-ying QI Zhao-yue ZHANG Yue-hua JIANG Yu-wu BAO Xin-hua QIN Jiong WU Xi-ru 《Chinese Medical Journal》 SCIE CAS CSCD 2006年第5期373-377,共5页
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 r... 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. 展开更多
关键词 Leigh syndrome mitochondrial genes cytochrome c oxidase deficiency surf1 gene
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