线粒体呼吸链复合物Ⅱ缺陷所致Leigh综合征

线粒体呼吸链复合物Ⅱ缺陷是较为少见的氧化磷酸化障碍性疾病。本文对1例单纯线粒体呼吸链复合物Ⅱ缺陷所致Leigh综合征患儿的诊疗进行回顾性分析。患儿,男,10个月,8个月时出现发热,热退后出现进行性全身无力、运动发育倒退和吞咽困难。血乳酸、丙酮酸增高,脑MRI显示双侧基底节对称性损害。对患儿进行了外周血白细胞线粒体氧化磷酸化酶复合物I-V活性测定和线粒体基因突变位点筛查分析。线粒体呼吸链复合物Ⅱ活性为21.9 nmol/min?mg线粒体总蛋白（正常对照47.3±5.3 nmol/min?mg线粒体总蛋白）,柠檬酸合酶活性为22.1%（正常对照50.9%±10.7%）,均显著降低。线粒体基因分析未发现异常。患儿确诊为线粒体呼吸链复合物Ⅱ缺陷所致Leigh综合征。经治疗患儿运动功能明显恢复。目前患儿22个月,病情稳定。     

线粒体呼吸链复合物Ⅰ缺陷导致幼儿肝内胆汁淤积症

线粒体呼吸链复合物缺陷是导致儿童线粒体病的主要原因。本文就1例线粒体呼吸链复合物Ⅰ缺陷导致的幼儿胆汁淤积症患者的临床经过、生化特点、线粒体呼吸链复合物活性分析及基因突变进行回顾性研究。患儿,男,自1岁1个月起腹泻,体重下降,伴无力、进行性黄疸、肝损害。经多种检查、尿液有机酸分析及血液氨基酸、酯酰肉碱谱分析未见特异性改变。外周血白细胞线粒体呼吸链复合物Ⅰ活性降低,线粒体基因分析发现患儿及其母亲tRNA 5821G>A突变,证实患儿存在线粒体呼吸链复合物Ⅰ缺陷。患儿疾病进展迅速,治疗无效,于1岁5个月时夭折。复合物Ⅰ缺陷是线粒体呼吸链缺陷中最常见的类型,本研究首次诊断了1例线粒体呼吸链复合物Ⅰ缺陷所导致的中国儿童患者,其临床表现为胆汁淤积症。线粒体肝病是导致儿童代谢性肝病的主要原因之一,生化分析、线粒体呼吸链复合物活性测定及基因分析是病因诊断的关键。     

线粒体基因13513G>A突变导致呼吸链酶复合物I缺陷Leigh综合征

Leigh综合征是由于线粒体呼吸链能量代谢障碍所导致的遗传性疾病,呼吸链酶复合物I缺陷是导致Leigh综合征的常见原因之一。该研究通过线粒体基因13513G>A突变分析首次确诊了1例中国人Leigh综合征患者。患儿为第一胎,12岁时出现抽搐,13岁时先后出现双眼视力下降,13岁来院就诊左眼颞侧视野缺损,痉挛步态,血液乳酸、丙酮酸增高,腓肠肌活检肌纤维内脂滴轻度增多;心电图检查显示不完全右束支传导阻滞;脑MRI显示双侧基底节对称性损害,符合Leigh综合征诊断,合并继发性癫癎。经基因分析证实患者存在线粒体基因13513G>A突变,导致线粒体呼吸链酶复合物I活性下降。治疗以多种维生素为主,补充左旋肉碱、辅酶Q10,同时给予卡马西平、苯巴比妥、丙戊酸等抗癫癎治疗。现在患儿16岁,休学,智力无明显倒退,体力、体重显著减退。Leigh综合征病因复杂,临床表现多种多样,该患儿以抽搐起病,合并视力减退,经基因分析明确了病因,有助于相关家庭的遗传咨询 。［中国当代儿科杂志,2009,11（5）：333-336］     

线粒体呼吸链复合物Ⅱ缺陷与疾病

本文就近年关于线粒体呼吸链复合物Ⅱ的结构、功能及其缺陷的临床表型、诊断、治疗及分子遗传学研究方面的进展进行文献综述。线粒体呼吸链复合物Ⅱ亦称琥珀酸泛醌氧化还原酶,是线粒体呼吸链的重要组分之一,对细胞的氧化磷酸化起着关键作用。呼吸链复合物Ⅱ与氧化性应激密切相关,是细胞内毒性物质以及异常代谢产物的敏感靶标。复合物Ⅱ缺陷导致的线粒体病临床表现多样,以神经肌肉进行性损害为主要表现,少数表现为心肌病、发作性呕吐、溶血尿毒综合征等。诊断有赖于线粒体呼吸链酶复合物活性测定和基因分析。患者受累组织的呼吸链复合物Ⅱ活性降低。已发现SDHA基因与编码复合物Ⅱ组装因子的SDHAF1基因的突变可导致复合物Ⅱ缺陷。目前线粒体呼吸链复合物Ⅱ缺陷的治疗主要是以改善线粒体功能为主。     

线粒体呼吸链酶复合物V缺陷与线粒体病

线粒体呼吸链酶复合物V,也称为ATP合酶,是位于线粒体内膜上的大蛋白复合体,由2个功能性蛋白复合物F0及F1构成。复合物V是线粒体呼吸链的最后一个复合物,在线粒体中通过电化学梯度传递质子,以ADP、Pi及Mg2+为原料合成ATP,为细胞供能。大多数患者新生儿期发病,导致严重脑损害或多脏器损害,病死率很高。主要临床表现为神经肌肉病、心肌病、高乳酸血症及3 甲基戊烯二酸尿症等,因受累器官的不同导致显著的临床异质性。复合物V由16个亚基组成,由线粒体基因与核基因共同编码。迄今,国内外已报道了MT-ATP6、MT-ATP8、ATPAF2、TMEM70、ATP5E基因突变导致的复合物V缺陷。本文总结了线粒体呼吸链复合物V的结构及功能,并对复合物V缺陷的病理、临床表现、诊断、治疗及分子遗传学研究进展进行了综述。     

线粒体呼吸链复合物Ⅲ缺陷五例的临床特点与生化分析

目的 对5例线粒体呼吸链复合物Ⅲ缺陷患儿进行临床特点和生化分析.方法 对5例患儿(男3例,女2例)临床特点进行归纳总结,并抽取患儿静脉血,分取白细胞线粒体蛋白,采用分光光度测定法检测线粒体呼吸链复合物Ⅰ～Ⅴ活性.结果 (1)5例分别于1个月～15岁时来院就诊.其中3例临床表型符合Leigh综合征,主要表现为智力运动发育落后,运动倒退.l例表现为肝损害,胆汁淤积症.l例表现为进行性肌无力.(2)线粒体呼吸链复合物Ⅰ+Ⅲ活性为3.0～14.2 nmoL/(min·mg线粒体总蛋白),200名正常对照为84.4±28.5 nmol/( min·mg线粒体总蛋白),患儿酶活性降低至正常对照的10.4％～49.3％;复合物Ⅰ+Ⅲ与柠檬酸合酶活性比值为3.5％～22.9％,显著低于正常对照[(66.1±l4.7)％],复合物Ⅰ、Ⅱ、Ⅳ和Ⅴ活性正常,符合单纯线粒体呼吸链复合物Ⅲ缺陷诊断.结论 线粒体呼吸链复合物Ⅲ缺陷病临床表现复杂多样,累及多个系统;复合物Ⅰ+Ⅲ活性以及与柠檬酸合酶活性比值均低于正常对照,而所有患儿复合物Ⅰ、Ⅱ、Ⅳ和Ⅴ活性均未发现异常.     

线粒体MT-TE基因突变致可逆性婴幼儿呼吸链缺乏症1例并文献复习

目的探讨线粒体MT-TE基因突变致可逆性婴幼儿呼吸链缺乏症的临床表现及基因突变特点。方法回顾分析1例确诊为可逆性婴幼儿呼吸链缺乏症患儿的临床资料,并复习相关文献。结果男性患儿,2个月23天,入院时消瘦,呼吸急促,双肺可闻及痰鸣音及喘鸣音;肌力IV级,肌张力减弱。有一胞姐生后不久因重症肺炎去世。入院时肌酸激酶同工酶123 U/L,肌酸激酶890 U/L;血乳酸8.9 mmol/L;病原学检查均为阴性。头颅MRI无异常。入院后患儿持续高乳酸血症、肌酶异常升高,伴呼吸困难,放弃治疗后死亡。基因检查示线粒体MT-TE基因存在14674TC突变,来源于母亲。国外文献报道线粒体MT-TE 14674TC突变患儿早期临床表现与进展型线粒体病类似,呼吸肌无力、喂养困难,运动发育里程碑延迟,肌酶及乳酸升高。予补充能量,维持内环境稳定等治疗,约1岁左右逐渐好转。结论线粒体MT-TE基因突变致可逆性婴幼儿呼吸链缺乏症早期表现与进展型线粒体病类似,积极治疗预后良好。早期进行基因检测可明确预后,增强治疗的信心。     

丙酮酸脱氢酶复合物缺陷Leigh 综合征2 例临床及PDHA1基因分析

目的探讨PDHA1基因突变所致丙酮酸脱氢酶复合物E1α亚单位缺陷Leigh综合征的临床特点及诊断和治疗。方法回顾分析2例因发育落后就诊,磁共振扫描提示Leigh综合征,并经生化代谢及基因检测确诊患儿的临床资料。结果 2例男性患儿分别于1岁1个月、4个月就诊,发育落后,肌张力障碍,肌力低下;头颅磁共振检查发现双侧基底节区对称性损害;血清丙酮酸、乳酸明显增高,血氨基酸及酯酰肉碱谱无异常。基因分析发现2例患儿X染色体PDHA1基因分别存在c.615CG、c.605AG错义突变,均为未报道的新突变,证实为丙酮酸脱氢酶复合物E1α亚单位缺陷所致Leigh综合征。结论 PDHA1基因突变患儿临床表现复杂多样,对于不明原因的发育落后儿童,应注意线粒体病的可能,基因检测有助于诊断、治疗及遗传咨询。     

ACAD9基因新发变异致线粒体复合物Ⅰ缺乏症20型1例报告并文献复习

目的 提高对线粒体复合物I缺乏症20型(MC 1 DN 20)临床表型及基因型的认识.方法 回顾分析1例MC 1 DN 20患儿的临床资料并复习相关文献.结果 男性患儿,出生后即表现为精神及反应差,顽固性代谢性酸中毒及高乳酸血症和肝脏增大.全外显子基因测序发现ACAD 9基因变异,c.1278+1 G>A为母源性剪切变...     

新生儿呼吸窘迫综合征ABCA3基因遗传缺陷的研究

目的 分析ATP结合盒式蛋白转运子亚单位基因ABCA3遗传缺陷与新生儿呼吸窘迫综合征(NRDS)的关系,从中探讨汉族人群NRDS发病的遗传机制.方法 收集在新生儿重症监护病房住院的11例重症NRDS患儿的临床资料,采集患儿和97例无关正常对照的血样,采用PCR扩增、DNA直接测序技术对11例患儿进行ABCA3基因序列分析,对于新发现的ABCA3错义突变在97例健康对照中进行单链构象多态性检测.对1例生后13 h死亡的NRDS患儿进行肺组织光镜和电镜检测.结果 在11例患儿中发现了3个ABCA3基因外显子遗传变异、1个剪切位点碱基变异和几个国外报道及尚未报道的ABCA3单核苷酸多态性(SNP).3个ABCA3基因外显子遗传变异分别为c.2169 G＞A (p.M723I)、c.1010 T＞G (p.V337G)、c.4972 A＞G(p.S1658G),1个剪切位点变异为Exon 30+2 T/G,发现的SNP位点包括未报道过的213 C ＞T(p.F71F)、Exon 21+ 34C/T和已报道的c.1059C＞T(p.F353F)等.1例生后12 h死亡的患儿携带c.2169G＞A纯合变异,该变异位于第17号外显子,碱基的变异导致第723位氨基酸由异亮氨酸代替蛋氨酸,97例健康对照者中未发现此变异.肺组织电镜检测显示该例肺泡Ⅱ型上皮细胞的板层小体变小、浓缩,电子致密物边集.结论 ABCA3基因突变可能是部分临床不能解释的重症NRDS患儿的遗传学病因或遗传背景,识别NRDS患儿ABCA3基因变异情况,有助于治疗措施的选择及评价,并为开展NRDS遗传咨询和早期预防性干预提供依据.     

Mitochondrial respiratory chain complex I deficiency causes intractable gastrointestinal symptoms

We report the case of a 13‐month‐old girl with frequent vomiting, intractable diarrhea, hyperlactatemia, and liver dysfunction. Although the symptoms were treatment resistant, enteral nutrition formula containing medium‐chain triglycerides reduced the weight loss, vomiting, and diarrhea. Immunostaining of mitochondrial respiratory chain (MRC) complexes of the colonic mucosa confirmed the diagnosis of MRC complex I deficiency. This case shows that this disease should be included in the differential diagnosis of hyperlactatemia and intractable, cryptogenic gastrointestinal symptoms. In addition, the mucosa of the affected gastrointestinal organ should be analyzed on immunostaining or electron microscopy for MRC complexes.     

Intractable secretory diarrhea in a Japanese boy with mitochondrial respiratory chain complex I deficiency

The etiology of secretory diarrhea in early life is often unclear. We report a Japanese boy who survived until 3 years of age, despite intractable diarrhea commencing soon after birth. The fecal sodium content was strikingly high (109 mmol/L [normal range, 27–35 mmol/L]) and the osmotic gap was decreased (15 mOsm/kg), consistent with the findings of congenital sodium diarrhea. We examined the mitochondrial respiratory chain function by blue native polyacrylamide gel electrophoresis (BN-PAGE) in-gel enzyme staining, BN-PAGE western blotting, respiratory chain enzyme activity assay, and immunohistochemistry. Liver respiratory chain complex (Co) I activity was undetectable, while other respiratory chain complex activities were increased (Co II, 138%; Co III, 153%; Co IV, 126% versus respective control activities). Liver BN-PAGE in-gel enzyme staining and western blotting showed an extremely weak complex I band, while immunohistochemistry showed extremely weak staining for the 30-kDa subunit of complex I, but normal staining for the 70-kDa subunit of complex II. The patient was, therefore, diagnosed with complex I deficiency. The overall complex I activity of the jejunum was substantially decreased (63% of the control activity). The immunohistochemistry displayed apparently decreased staining of the 30-kDa complex I subunit, together with a slightly enhanced staining of the 70-kDa complex II subunit in intestinal epithelial cells. These data imply that intestinal epithelial cells are also complex I-deficient in this patient. Complex I deficiency is a novel cause of secretory diarrhea and may act via disrupting the supply of adenosine triphosphate (ATP) needed for the maintenance of ion gradients across membranes.     

Clinical presentations and laboratory investigations in respiratory chain deficiency

Respiratory chain deficiencies have long been regarded as neuromuscular diseases. In fact, oxidative phosphorylation, i.e., ATP synthesis by the respiratory chain not only occurs in the neuromuscular system, indeed, a number of nonneuromuscular organs and tissues are dependent upon mitochondrial energy supply. For this reason, a respiratory chain deficiency can theoretically give rise to any symptom, in any organ or tissue, at any age with any mode of inheritance, due to the twofold genetic origin of respiratory enzymes (nuclear DNA and mitochondrial DNA).     

Mitochondrial respiratory chain complex IV deficiency complicated with chronic intestinal pseudo‐obstruction in a neonate

A female infant born at 36 weeks gestational age with birthweight 2135 g, and who developed respiratory disorder, hyperlactacidemia and hypertrophic cardiomyopathy after birth, was admitted to hospital at 3 days of age. After admission, bilious emesis, abdominal distention, and passage disorder of the gastrointestinal tract were resistant to various drugs. Exploratory laparotomy was performed at 93 days of age, but no organic lesions were identified and normal Meissner/Auerbach nerve plexus was confirmed, which led to a clinical diagnosis of chronic intestinal pseudo‐obstruction (CIPO). She was diagnosed with mitochondrial respiratory chain complex IV deficiency on histopathology of the abdominal rectus muscle and enzyme activity measurement. This is the first report of a neonate with mitochondrial respiratory chain complex deficiency with intractable CIPO. CIPO can occur in neonates with mitochondrial respiratory chain disorder, necessitating differential diagnosis from Hirschsprung disease.     

End-stage liver disease as the only consequence of a mitochondrial respiratory chain deficiency: no contra-indication for liver transplantation

The prerequisite for liver transplantation as a therapeutic option for inherited metabolic diseases should be that the enzyme defect, being responsible for the major clinical (hepatic and/or extra-hepatic) abnormalities, is localised in the liver. Furthermore, no adequate dietary or pharmacological treatment should be available or such treatment should have an unacceptable influence on the quality of life. We report an infant, who developed end-stage liver disease with persistent lactic acidaemia in his first months of life. Analysis of the mitochondrial respiratory chain in liver tissue revealed a combined partial complex I and IV deficiency. No extra-hepatic involvement could be demonstrated by careful screening for multiple organ involvement, including analysis of the mitochondrial respiratory chain in muscle tissue and cultured skin fibroblasts. The boy received a reduced size liver graft at the age of 8 months. He recovered successfully. Almost 5 years after transplantation he is in good clinical condition. No clinical or biochemical signs of any organ dysfunction have been demonstrated. The considerations on which basis it was decided that there was no contra-indication to perform liver transplantation in this patient are discussed. Conclusion The possibility of a mitochondrial respiratory chain deficiency should be considered in liver disease of unknown origin prior to liver transplantation. Liver transplantation is a therapeutic option in mitochondrial respiratory chain deficiency-based end-stage liver disease provided that extra-hepatic involvement is carefully excluded. Received: 12 October 1999 and in revised form: 26 January 2000 / Accepted: 26 January 2000