多种酰基辅酶 A 脱氢酶缺乏症中核黄素反应性的决定因素。
Determinants of Riboflavin Responsiveness in Multiple Acyl-CoA Dehydrogenase Deficiency.
机构信息
Division of Pediatric Metabolism, Hacettepe University Children's Hospital, Ankara, Turkey.
Pediatric Pathology Unit, Hacettepe University Children's Hospital, Ankara, Turkey.
出版信息
Pediatr Neurol. 2019 Oct;99:69-75. doi: 10.1016/j.pediatrneurol.2019.06.015. Epub 2019 Jun 28.
BACKGROUND
Multiple acyl-CoA dehydrogenase (MADD) deficiency, which is a rare metabolic disorder involving electron transport flavoproteins, has a wide array of clinical phenotypes. In this article, we describe 25 patients with MADD deficiency and present the clinical and laboratory characteristics and diagnostic challenges associated with riboflavin-responsive MADD deficiency.
METHODS
Hospital records of patients with biallelic mutations in ETFA, ETFB, or ETFDH genes diagnosed in a single center were analyzed retrospectively. Demographic, clinical, and laboratory characteristics of patients with riboflavin-responsive and riboflavin-unresponsive MADD deficiency were compared using Mann-Whitney U and Fisher's exact tests.
RESULTS
Respiratory distress and depressed consciousness were significantly more common in patients with riboflavin-unresponsive MADD deficiency (P = 0.015 and P < 0.001), who presented at a younger age (P < 0.001). Patients with riboflavin-responsive MADD deficiency had favorable outcomes but also had life-threatening complications, longer diagnostic delay (median of two years versus 30 days; P < 0.001), and multiple differential diagnoses, resulting in unnecessary investigations and maltreatment. Biopsies showed lipid storage, and complete autopsy was performed in one newborn with riboflavin-unresponsive MADD deficiency, revealing multiple abnormalities. Metabolic profiles were not distinguishable between riboflavin-responsive and riboflavin-unresponsive MADD deficiency (P > 0.05). Four novel variants were detected in ETFDH, one of which (c.1790C>T) may confer riboflavin responsiveness. Siblings with the common myopathic ETFDH c.1130T>C mutation presented with a new phenotype dominated by chronic fatigue without apparent myopathy.
CONCLUSIONS
Symptoms and outcomes significantly differed between riboflavin-responsive and unresponsive MADD deficiency, but metabolic profiles did not. Functional studies are needed to better characterize the novel ETFDH variants. As treatment is available for riboflavin-responsive MADD deficiency, physicians should maintain a high index of suspicion for MADD deficiency in all age groups.
背景
多种酰基辅酶 A 脱氢酶(MADD)缺乏症是一种罕见的代谢紊乱疾病,涉及电子传递黄素蛋白,具有广泛的临床表型。本文描述了 25 例 MADD 缺乏症患者,并介绍了与核黄素反应性 MADD 缺乏症相关的临床和实验室特征以及诊断挑战。
方法
回顾性分析了在一家中心诊断为 ETFA、ETFB 或 ETFDH 基因双等位基因突变的患者的医院记录。使用 Mann-Whitney U 和 Fisher 确切检验比较了核黄素反应性和核黄素无反应性 MADD 缺乏症患者的临床和实验室特征。
结果
核黄素无反应性 MADD 缺乏症患者的呼吸窘迫和意识障碍更为常见(P=0.015 和 P<0.001),且发病年龄更小(P<0.001)。核黄素反应性 MADD 缺乏症患者的结局较好,但也有危及生命的并发症,诊断延迟时间更长(中位数为 2 年与 30 天;P<0.001),且有多种鉴别诊断,导致不必要的检查和虐待。活检显示脂质沉积,一名核黄素无反应性 MADD 缺乏症的新生儿进行了完整的尸检,显示出多种异常。核黄素反应性和核黄素无反应性 MADD 缺乏症的代谢谱无明显差异(P>0.05)。在 ETFDH 中检测到 4 个新变异,其中一个(c.1790C>T)可能赋予核黄素反应性。具有常见肌病 ETFDH c.1130T>C 突变的同胞表现出新的表型,以无明显肌病的慢性疲劳为主。
结论
核黄素反应性和无反应性 MADD 缺乏症的症状和结局显著不同,但代谢谱没有。需要进行功能研究以更好地描述新的 ETFDH 变异。由于核黄素反应性 MADD 缺乏症可治疗,因此医生应在所有年龄段均保持对 MADD 缺乏症的高度怀疑。
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