Fatal multiple acyl-CoA dehydrogenase deficiency caused by ETFDH gene mutation:A case report

BACKGROUND Multiple acyl-CoA dehydrogenase deficiency(MADD)is a disease of rare autosomal recessive disorder.There are three types of MADD.Type I is a neonatalonset form with congenital anomalies.Type II is a neonatal-onset form without congenital anomalies.Type III is considered to a milder form and usually responds to riboflavin.However,late-onset form could also be fatal and not responsive to treatments.CASE SUMMARY We report a severe case of a young man with onset type III MADD induced by drugs and strenuous exercise characterized by rhabdomyolysis and liver dysfunction.Urine analysis indicated 12 out of 70 kinds of organic acids like glutaric acid-2 were detected.Serum analysis in genetic metabolic diseases revealed 24 out of 43 tested items were abnormal,revealing the elevation of several acylcarnitines and the reduction of carnitine in the patient.By next generation sequencing technology for gene sequencing related to fatty acid oxidation and carnitine cycle defects,a rare ETFDH gene variant was identified:NM_004453:4:C.1448C>T(p.Pro483 Leu).The patient was diagnosed with lateonset GAII.He was not responsive to riboflavin and progressively worsened into multiple organ failure that finally led to death.CONCLUSION Type III MADD can also be fatal and not responsive to treatments.

Late-onset multiple acyl-CoA dehydrogenase deficiency with cardiac syncope: A case report

BACKGROUND Multiple acyl-CoA dehydrogenase deficiency(MADD)is an uncommon autosomal recessive disorder of mitochondrial fatty acid beta-oxidation.Syncope is a transient loss of consciousness due to acute global cerebral hypoperfusion.Late-onset MADD with syncope has not been reported previously.CASE SUMMARY We report a 17-year-old girl with exercise intolerance and muscle weakness.She felt palpitation and shortness of breath after short bouts of exercise.She also suffered from a transient loss of consciousness many times.Muscle biopsy showed lipid storage.Genetic mutation analysis indicated a compound heterozygous mutation c.250G>A(p.A84T)and c.872T>G(p.V291G)in the ETFDH gene.The results of Holter electrocardiogram monitoring showed supraventricular tachycardia when the patient experienced a loss of consciousness.After treatment with riboflavin and carnitine,muscle weakness and palpitation symptoms improved rapidly.No loss of consciousness occurred,and the Holter electrocardiogram monitoring was normal.CONCLUSION Late-onset MADD with supraventricular tachycardia can cause cardiac syncope.Carnitine and riboflavin supplement were beneficial for treating the late-onset MADD with cardiac syncope.Attention should be paid to the prevention of cardiac syncope when diagnosing late-onset MADD.

Clinical and muscle magnetic resonance image findings in patients with late-onset multiple acyl-CoA dehydrogenase deficiency

Background:Late-onset multiple acyl-coA dehydrogenase deficiency (MADD) is an autosomal recessive inherited metabolic disorder. It is still unclear about the muscle magnetic resonance image (MRI) pattern of the distal lower limb pre- and post-treatment in patients with late-onset MADD. This study described the clinical and genetic findings in a cohort of patients with late-onset MADD, and aimed to characterize the MRI pattern of the lower limbs.Methods:Clinical data were retrospectively collected from clinic centers of Peking University People's Hospital between February 2014 and February 2018. Muscle biopsy, blood acylcarnitines, and urine organic acids profiles, and genetic analysis were conducted to establish the diagnosis of MADD in 25 patients. Muscle MRI of the thigh and leg were performed in all patients before treatment. Eight patients received MRI re-examinations after treatment.Results:All patients presented with muscle weakness or exercise intolerance associated with variants in the electron transfer flavoprotein dehydrogenase gene. Muscle MRI showed a sign of both edema-like change and fat infiltration selectively involving in the soleus (SO) but sparing of the gastrocnemius (GA) in the leg. Similar sign of selective involvement of the biceps femoris longus (BFL) but sparing of the semitendinosus (ST) was observed in the thigh. The sensitivity and specificity of the combination of either "SO+/GA-" sign or "BFL+/ST-" sign for the diagnosis of late-onset MADD were 80.0% and 83.5%, respectively. Logistic regression model supported the findings. The edema-like change in the SO and BFL muscles were quickly recovered at 1 month after treatment, and the clinical symptom was also relieved.Conclusions:This study expands the clinical and genetic spectrums of late-onset MADD. Muscle MRI shows a distinct pattern in the lower limb of patients with late-onset MADD. The dynamic change of edema-like change in the affected muscles might be a potential biomarker of treatment response.

A Historical Cohort Study on the Efficacy of Glucocorticoids and Riboflavin Among Patients with Late-onset Multiple AcyI-CoA Dehydrogenase Deficiency

Background： Late-onset multiple acyl-CoA dehydrogenase deficiency （MADD） is the most common type of lipid storage myopathies in China. Most patients with late-onset MADD are well responsive to riboflavin. Up to now, these patients are often treated with glucocorticoids as the first-line drug because they are misdiagnosed as polymyositis without muscle biopsy or gene analysis. Although glucocorticoids seem to improve the fatty acid metabolism of late-onset MADD, the objective evaluation of their rationalization on this disorder and comparison with riboflavin treatment are unknown. Methods： We performed a historical cohort study on the efficacy of the two drugs among 45 patients with late-onset MADD, who were divided into glucocorticoids group and riboflavin group. Detailed clinical information of baseline and 1-month follow-up were collected. Results： After 1-month treatment, a dramatic improvement of muscle strength was found in riboflavin group （P 〈 0.05）. There was no significant difference in muscle enzymes between the two groups. Significantly, the number of patients with full recovery in glucocorticoids group was less than the number in riboflavin group （P 〈 0.05）. On the other hand, almost half of the patients in riboflavin group still presented high-level muscle enzymes and weak muscle strength after 1-month riboflavin treatment, meaning that l-month treatment duration maybe insufficient and patients should keep on riboflavin supplement for a longer time. Conclusions： Our results provide credible evidences that the overall efficacy of riboflavin is superior to glucocorticoids, and a longer duration of riboflavin treatment is necessary for patients with late-onset MADD.

Muscle Magnetic Resonance Imaging for the Differentiation of Multiple AcyI-CoA Dehydrogenase Deficiency and Immune-mediated Necrotizing Myopathy

Background： Clinically, it is difficult to differentiate multiple acyl-CoA dehydrogenase deficiency （MADD） from immune-mediated necrotizing myopathy （IMNM） because they display similar symptoms. This study aimed to determine whether muscle magnetic resonance imaging （MRI） could be used for differential diagnosis between MADD and IMNM. Methods： The study evaluated 25 MADD patients, confirmed by muscle biopsy and ETFDH gene testing, and 30 IMNM patients, confirmed by muscle biopsy. Muscles were assessed for edema and fatty replacement using thigh MRI （tMRI）. Degrees and distribution patterns of fatty infiltration and edema in gluteus maximus and thigh muscles were compared. Results： Total fatty infiltration and edema scores （median, [Q 1, Q3]） were 4.00 （1.00, 15.00） and 0 （0, 4.00） in MADD and 14.50 （8.00, 20.75） and 22.00 （16.75, 32.00） in IMNM, respectively, which were significantly more severe in IMNM than that in MADD （P = 0.000 and P = 0.004~ respectively）. Edema scores tbr gluteus maximus, long head of biceps femoris, and semimembranosus were significantly higher in IMNM than in MADD （all P = 0.000）. Fatty infiltration scores for anterior and medial compartments were significantly more severe in IMNM than that in MADD （all P = 0.000）. Conclusion： Different patterns of muscle involvement on tMRI can contribute to differential diagnosis between MADD and IMNM when clinical suspicions alone are insufficient, thereby reducing the need for muscle biopsy.

Clinical features and mutations in seven Chinese patients with very long chain acyl-CoA dehydrogenase deficiency

Background:Very long chain acyl-CoA dehydrogenase deficiency(VLCADD)is an inherited metabolic disease caused by deleterious mutations in the ACADVL gene that encodes very long chain acyl-CoA dehydrogenase(VLCAD),and which can present as cardiomyopathy in neonates,as hypoketotic hypoglycemia in infancy,and as myopathy in late-onset patients.Although many ACADVL mutations have been described,no prevalent mutations in the ACADVL gene have been associated with VLCADD.Herein,we report the clinical course of the disease and explore the genetic mutation spectrum in seven Chinese patients with VLCADD.Methods:Seven Chinese patients,from newborn to 17 years old,were included in this study.Tandem mass spectrometry was performed to screen for VLCAD defi ciency.All exons and fl anking introns of the ACADVL gene were analyzed using polymerase chain reaction and direct sequencing.Online analysis tools were used to predict the impact of novel mutations.Results:All cases had elevated serum levels of tetradecanoylcarnitine(C14:1)which is the characteristic biomarker for VLCADD.The phenotype of VLCADD is heterogeneous.Two patients were hospitalized for hypoactivity and hypoglycemia shortly after birth.Three patients showed hepatomegaly and hypoglycemia in infancy.The other two adolescent patients showed initial manifestations of exercise intolerance or rhabdomyolysis.Three of the patients died at the age of 6-8 months.Eleven different mutations in the ACADVL gene in the 7 patients were identified,including seven reported mutations(p.S22X,p.W427X,p.A213T,p.G222R,p.R450H,c.296-297delCA,c.1605+1G>T)and four novel mutations(p.S72F,p.Q100X,p.M437T,p.D466Y).The p.R450H and p.D466Y(14.28%,2/14 alleles)mutations were identifi ed in two alleles respectively.Conclusions:The clinical manifestations were heterogeneous and ACADVL gene mutations were heterozygous in the seven VLCADD Chinese patients.R450H may be a relatively common mutation in Asian populations.The genotype and phenotype had a certain correlation in our patients.

Medium-chain acyl-CoA dehydrogenase deficiency: prevalence of ACADM pathogenic variants c.985A>G and c.199T>C in a healthy population in Rio Grande do Sul, Brazil

Objectives::To investigate the prevalence of ACADM pathogenic variants, c.985A>G and c.199T>C, for medium chain acyl CoA dehydrogenase deficiency (MCADD) in a healthy population in the southern region of Brazil. Methods::This was an observational cross-sectional study with a convenience sampling strategy. The participants were recruited from the blood bank of the Hospital de Clínicas of Porto Alegre, Brazil. A total of 1000 healthy individuals from the state of Rio Grande do Sul were included. Genotyping for the c.199T>C and c.985A>G variants was performed using real-time polymerase chain reaction (PCR) and the PCR-restriction fragment length polymorphism (RFLP) technique, respectively. Individuals considered heterozygous for c.985A>G were subjected to additional acylcarnitine profile analysis using tandem mass spectrometry. Carrier frequency was obtained by calculating the ratio of heterozygous individuals to the total number of individuals analyzed and reported with a 95% confidence interval. Allele and genotype frequencies were calculated based on the Hardy-Weinberg equilibrium.Results::The c.985A>G variant was detected as heterozygotes in three individuals (frequency of the heterozygous genotype = 1:333, allele frequency= 0.0015, minimum frequency of MCADD= 1:444,444) whose acylcarnitine profiles were within normal limits. The c.199T>C variant was not identified.Conclusions::Considering the small sample size and associated allelic heterogeneity with MCADD, these findings are believed to denote the rarity or underdiagnosis of MCADD in southern Brazil. This study provides evidence for the need for further investigation to ascertain the contribution of these diseases to child morbidity and mortality in the country.

多种酰基辅酶A脱氢酶缺乏症儿童与成人患者临床特点比较

目的比较儿童和成人多种酰基辅酶A脱氢酶缺乏症(MADD)患者的临床和实验室检查特点。方法对12例儿童和19例成人MADD患者进行常规实验室检查、血酰基肉碱谱及尿有机酸分析。对中国人电子转运黄素蛋白脱氢酶(ETFDH)基因常见突变A84T通过DNA测序方法进行筛检。结果儿童MADD患者临床表现高度异质,可表现为肌无力、肝大、低酮性低血糖、肥厚性心肌病或脑发育不良及脱髓鞘病变;而成人患者均以肌无力起病。成人和儿童MADD有肝酶和CK升高,血多种酰基肉碱升高,多数伴有二羧酸尿。儿童组3例死亡,成人组全部存活。存活患者的症状和生化指标治疗后好转或正常。A84T突变在儿童和成人患者的发生率分别为20.8%(5/24)和21%(8/38)。结论儿童与成人MADD患者的临床表现和预后存在差异,成人患者预后好;A84T突变可能与轻型相关。[临床儿科杂志,2012,30(5):446-449]

浙江省新生儿多酰基辅酶A脱氢酶缺乏症筛查及随访分析

目的:了解浙江省新生儿多酰基辅酶A脱氢酶缺乏症(MADD)的发病率、临床特征及基因突变特点。方法:采用串联质谱法对2009年1月至2020年12月浙江省新生儿疾病筛查中心3896789名新生儿进行遗传代谢病筛查,结合尿有机酸分析及电子转移黄素蛋白(ETF)或电子转移黄素蛋白脱氢酶(ETFDH)基因检测确诊。确诊患儿进行饮食和生活管理,补充左卡尼汀、核黄素、辅酶Q10治疗,长期随访并评估患儿的生长和智力发育情况。结果:确诊MADD患儿13例,除1例为Ⅱ型,其余均为Ⅲ型(迟发型),发病率为1/299753。13例患儿中,1例死亡,4例因感染诱发以低血糖为主要表现的急性代谢失调,1例出现肌张力降低,其余患儿随访发育良好(随访时间3~45个月)。患儿初筛血C4~C18:1不同程度升高。13例患儿进行基因检测,其中ETFA基因复合杂合突变1例,ETFA基因纯合突变1例,ETFB基因复合杂合突变1例,ETFDH基因复合杂合突变8例,ETFDH基因纯合突变1例,仅检测出一个ETFDH基因突变位点1例。c.250G>A为热点突变。结论:MADD临床表现高度异质,新生儿期发病较为严重,迟发型常无明显临床症状,初筛血C4~C18:1不同程度升高,最常见基因突变为c.250G>A。

伴脊髓损伤的晚发型戊二酸尿症Ⅱ型合并家族性高胆固醇血症一例报告

戊二酸尿症Ⅱ型是一种影响脂肪酸、氨基酸和胆碱代谢的常染色体隐性遗传病,是引起脂质沉积病的重要病因。该病儿童少见,临床医生认识不足,易误诊、漏诊。伴腹痛、脊髓损伤的晚发型戊二酸尿症Ⅱ型更为罕见。本文对1例伴腹痛、脊髓损伤的晚发型戊二酸尿症Ⅱ型合并家族性高胆固醇血症的患儿进行回顾性分析。早期进行血脂、尿有机酸和基因检测对患儿的诊治及提高生活质量有重要意义。

海洋性贫血合并G6PD缺乏症1例报告并文献复习

目的:报告l例海洋性贫血合并G6PD缺乏症致多脏器功能衰竭的少见病例的诊治过程。方法:病例分析及文献复习。结果:因烫伤感染入院的海洋性贫血女患者,先后发生严重黄疸、重度贫血、DIC、肾衰、酸中毒、严重低钾等多器官功能衰竭,虽发病时G6PD/6PGD正常,似不支持G6PD缺乏症诊断,但根据病史、相关治疗效果以及出院后45d复查G6PD/6PGD低于正常,最后确诊G6PD缺乏症。经成份输血、低分子肝素抗凝、大剂量速尿利尿、纠酸、超浓度补钾等抢救,病情稳定痊愈出院。结论:G6PD溶血虽然是自限性的,但当合并海洋性贫血时,往往病情严重,可致DIC、肾衰甚至多脏器衰竭。严重溶血时G6PD活性测定多数在正常范围,不排除有G6PD缺乏时,输血须配G6PD活性正常的同型血。做好婚检和产检的筛查工作是预防海洋性贫血、G6PD缺陷症及两病并患的根本措施。

核黄素反应性脂质沉积性肌病伴感觉共济失调性神经病3例报告

目的研究核黄素反应性脂质沉积性肌病伴感觉共济失调性神经病的临床、电生理、病理和基因改变特点。方法 3例男性患者来自2个家系,其中2例为兄弟,发病年龄41～43岁,主要症状是四肢肌无力,伴随双足麻木和行走不稳。查体发现四肢近端肌力下降、末梢性感觉丧失和Romberg征阳性。3例患者的血尿代谢筛查均提示存在血多种脂酰肉碱水平升高和尿戊二酸水平增高。3例患者均进行了神经电生理、肌肉活检以及电子转移黄素蛋白脱氢酶(ETFDH)基因检查,2例进行腓肠神经活检。结果 3例患者的肌电图分别出现肌源性损害、可疑神经源性损害和无异常。3例患者的四肢感觉神经传导速度显著减慢或不能引出,运动神经传导速度仅在1例出现轻度减慢。3例患者的骨骼肌均可见肌纤维内脂肪滴显著增多,2例有个别破碎红纤维,2例出现小角状肌纤维。2例患者的腓肠神经均可见有髓神经纤维中-重度减少,伴随有髓神经纤维轴索变性和再生。3例患者均携带ETFDH基因的复合杂合突变,其中2兄弟为c.65A>G和c.242T>C,另1例为c.770A>G和c.1450 T>C。结论 ETFDH基因突变导致的核黄素反应性脂质沉积性肌病可以伴随感觉共济失调性神经病。

以转氨酶升高为主的多种酰基辅酶A脱氢酶缺乏症1例临床表现及基因分析

目的研究1例以转氨酶升高为主的多种酰基辅酶A脱氢酶缺乏症患者临床表现、实验室检查、肌肉活检及基因突变情况分析,并进行文献复习,为该病的早期诊断及治疗提供依据。方法收集1例7岁3月男性患儿的临床资料,采集患儿及父母血标本,采用二代基因测序检测致病基因,腓肠肌穿刺活检明确肌肉病变情况。结果患儿肌肉活检电镜结果示肌纤维内大量脂滴沉积。基因测序结果显示患儿的ETFDH基因存在c.1773_1774del AT p.(Cys592※)无义突变和c.389A>T p.(Asp130Val)错义突变,考虑为复合杂合突变,患儿父母分别为携带者。结论临床上有转氨酶升高为主伴有心肌酶升高、运动障碍者,应尽早进行分子遗传学检查,有条件者行腓肠肌肌肉活检术,可以为患儿家庭提供准确的遗传咨询和产前诊断。

核黄素反应性多酰基辅酶A脱氢酶缺乏症的临床表现与基因突变多样性

目的探讨核黄素反应性多酰基辅酶A脱氢酶缺乏症(MADD)的临床表现和基因突变的多样性。方法与结果收集5例核黄素反应性MADD患者的临床特征、血清学指标、肌电图、肌肉组织活检和基因分析结果,对核黄素反应性MADD的临床特点进行回顾分析和总结。5例患者发病年龄为13~32岁,平均20.40岁;临床表现为波动性或进行性肌无力,主要累及面部、颈部、四肢近端和呼吸肌,运动、劳累或感染后症状加重;血清肌酸激酶水平轻至中度升高,其中2例血清乳酸水平于运动后明显升高;4例呈肌源性损害,1例在疾病早期呈神经源性损害、晚期以肌源性损害为主;肌肉组织活检有2例肌纤维内可见大量油红O染色阳性脂肪滴沉积。基因分析显示,4例表现为ETFDH基因纯合或复合杂合突变,分别携带G250A纯合突变(1例)、G250A和G524A复合杂合突变(2例)、T1211C和C1454G复合杂合突变(1例),1例携带ETFDH基因G1399C杂合突变和ETFB基因C725T杂合突变。结论中国大陆核黄素反应性MADD患者主要表现为骨骼肌受累的脂质沉积性疾病,呈进行性或波动性病程,应注意与各种类型的肌营养不良症、线粒体肌病、糖原贮积病、重症肌无力和周围神经病相鉴别;ETFDH基因突变是其主要致病原因。由于核黄素反应性MADD患者预后良好,对于疑似病例可以小剂量维生素B2进行诊断性治疗,同时结合尿有机酸、血酰基肉碱、肌肉组织活检和基因检测以明确诊断。

ETFDH基因变异导致晚发型多种酰基辅酶A脱氢酶缺乏症1例并文献复习

目的探讨晚发型多种酰基辅酶A脱氢酶缺乏症(multiple acyl-CoA dehydrogenase deficiency,MADD)临床特征和基因特点,加强对MADD的认识。方法回顾性分析2020年2月就诊于首都儿科研究所附属儿童医院的1例MADD患儿的临床资料,并复习相关文献。结果患儿,女,12岁,以反复呕吐5个月、双下肢乏力2个月为主要表现,伴体重显著减轻。血生化检查提示转氨酶升高,乳酸脱氢酶、肌酸激酶同工酶升高;氨基酸肉碱质谱分析提示多种酰基辅酶A脱氢酶缺乏症;腹部计算机断层扫描(computed tomography,CT)提示脂肪肝;肌肉磁共振成像(magnetic resonance imaging,MRI)提示肌炎。基因检测发现ETFDH基因存在7号外显子c.736G>A和3号外显子c.389A>T复合杂合突变,确诊为MADD。予核黄素、左卡尼汀治疗后好转。随访6个月无呕吐,肌力恢复正常,血生化指标正常。结论晚发型MADD临床表现多样,基因检查可以帮助确诊MADD,核黄素对晚发型MADD治疗有效。

多种酰基辅酶A脱氢酶缺乏症的研究进展

多种酰基辅酶A脱氢酶缺乏症(MADD)又称戊二酸尿症Ⅱ型或戊二酸血症Ⅱ型,主要由电子转运黄素蛋白A(ETFA)、电子转运黄素蛋白B(ETFB)或电子转运黄素蛋白脱氢酶(ETFDH)基因突变所致。患者多有不明原因慢性疲劳、肌肉无力、肌酶升高、体质量减轻、不明原因肝酶增高、肝大、恶心、呕吐、心慌、胸闷、心肌酶谱异常等症状,完善相关检查并排除其他系统疾病后行高通量基因测序可确诊该病。核黄素是治疗该病的主要药物。核黄素无效时,可选用苯扎贝特或D、L-3-羟基丁酸进行治疗。本文对MADD的遗传学背景、发病机制、临床表现、实验室检查及治疗进行综述,以期对MADD有更进一步的认识。

细胞学结合串联质谱诊断多种酰基辅酶A脱氢酶缺乏症的价值

目的研究应用串联质谱技术分析细胞培养液中不同链长酰基肉碱谱的变化对多种酰基辅酶A脱氢酶缺乏症(multiple acy-CoA dehydrogenase deficiency,MADD)的诊断价值。方法取健康对照标本20例,MADD患儿皮肤成纤维细胞标本9例(包括I型3例,Ⅱ型3例和Ⅲ型3例。在37℃培养条件下,用特殊培养底物即加入棕榈酸(C16酸)的培养液中培养成纤维细胞96 h,应用串联质谱分析相应培养液中的酰基肉碱谱。结果与健康对照组比较,MADD患儿乙酰肉碱(C2)明显降低,而所有病人月桂酰肉碱(C12)、肉豆蔻酰肉碱(C14)、及棕榈酰肉碱(C16)等长链酰基肉碱均异常增高,与健康对照组相比中链酰基肉碱C6、C8、C10在重型(I型)病例异常降低,而II型与III型中链酰基肉碱C6、C8、C10与健康对照比明显升高;其中棕榈酸酰基肉碱(C16)在I型患儿中明显增高,肉豆寇烯酰肉碱(C14)及月桂酰肉碱(C12)在临床Ⅲ型和Ⅱ型病例增高更显著。结论应用串联质谱酰基肉碱谱分析结合特定培养液培养皮肤成纤维细胞可用于MADD的诊断和临床分型。

误诊为脑性瘫痪康复治疗患儿二例分析

引起患儿发育落后、运动异常的疾病很多,除脑性瘫痪外还可见于甲状腺功能低下、染色体异常、遗传代谢性疾病、脑白质病、肌张力障碍等。戊二酸尿症属支链氨基酸代谢障碍性疾病,除表现为发育落后及肌张力异常外,主要伴随有神经系统严重损伤(如癫痫),同时多表现有间断性呕吐、低血糖、代谢性酸中毒等临床表现。肌张力障碍性疾病表现为发育落后及运动障碍,且运动障碍具有晨轻暮重的特点。本文对将以上疾病误诊为脑性瘫痪康复治疗的2例患儿进行分析,以加深康复医生对脑性瘫痪的认识,及时做出正确诊断与治疗,避免发生误诊。

上呼吸道感染患儿口服尼美舒利后发生瑞氏综合征及猝死样症状

患儿,男,6岁3个月, 2个月前因上呼吸道感染、发热,父母参照说明书予以尼美舒利口服,半小时后抽搐,呼吸心跳骤停,急诊检查发现低酮性低血糖,代谢性酸中毒,血清转氨酶及肌酶显著升高,肾功能受损。经积极复苏治疗后患儿意识及生命体征恢复,但是智力、运动严重倒退。患儿血液游离肉碱降低,中长链酯酰肉碱增高,尿液戊二酸、3-羟基戊二酸、异戊酰甘氨酸、乙基丙二酸等增高,提示多种酯酰辅酶A脱氢酶缺乏症。经维生素B2、左卡尼汀、苯扎贝特等治疗后患儿病情逐渐好转,3个月后复查生化指标恢复正常。患儿ETFDH基因存在复合杂合突变,c.341G>A(p.R114H)为已知突变(来自母亲),c.1484C>G(p.P495R)为未报道的新突变(来自父亲)。患儿最终确诊为多种酰基辅酶A脱氢酶缺乏症,因发热服用尼美舒利诱发急性代谢危象,导致瑞氏综合征、猝死样发作。遗传代谢病是导致瑞氏综合征、猝死的一组主要病因,生化及基因分析是识别潜在疾病的关键。

脂质代谢性肌病一例:极长链酰基辅酶A脱氢酶缺乏症

患者女性，16岁。主因反复肌无力伴酸痛发作3年余，于2012年2月24日入院。患者自2008年9月至人院时共计6次出现肌无力伴酸痛感，每次发作前均有劳累或受凉史。主要表现为四肢和抬头无力，伴肌肉酸痛感，休息后症状与体征可完全缓解，发作后间歇性“酱油”尿。外院检查血清肌酸激酶（CK）水平显著升高，最高时达30×103IU／L（25～190IU／L）。2岁时曾出现“抽搐”发作，伴高热，5岁时有类似发作，经丙戊酸钠（德巴金）治疗（具体剂量不详）3年无发作，自行停药。患者外祖父母为近亲结婚，其兄2岁夭折（具体不详）。