Stanley C A
Children's Hospital of Philadelphia, University of Pennsylvania School of Medicine.
Adv Pediatr. 1987;34:59-88.
There are now nine inherited diseases that have been identified in the pathway of mitochondrial fatty acid oxidation, including LCAD, MCAD, SCAD, and HMG-CoA lyase deficiencies, two forms each of CPT and MAD deficiencies and an incompletely characterized disorder of primary carnitine deficiency. The varied range of clinical manifestations in this new group of diseases should attract the attention not only of general pediatricians (coma, hypoglycemia) but also of pediatric subspecialists in neurology (myopathy), cardiology (cardiomyopathy), and gastroenterology (fatty liver), as well as genetics and metabolism. The presenting features of the genetic defects in fatty acid oxidation fit well with the concept that fatty acid oxidation plays a major role in energy production during prolonged fasting and in working cardiac and skeletal muscle. Life-threatening episodes of coma and hypoglycemia induced by fasting are a common presenting feature in most of the fatty acid oxidation disorders (MCAD, LCAD, and HMG-CoA lyase deficiencies, the infantile form of CPT deficiency, the mild form of MAD deficiency, and in some cases of primary carnitine deficiency). The hypoglycemia in these disorders is most easily explained by the inability of affected patients to use fatty acids as a fuel as a substitute for glucose. It should be stressed, however, that the coma in these disorders may occur from direct toxic effects of fatty acids or fatty acid intermediates before plasma glucose concentrations reach hypoglycemic levels. Severe disturbances of muscle function are a feature in several of the disorders; hypertrophic cardiomyopathy and chronic skeletal muscle weakness occur in both the mild and severe forms of MAD deficiency, in primary carnitine deficiency, and in some patients with LCAD deficiency. In contrast, patients with the adult form of CPT deficiency have normal muscle strength but are prone to episodes of painful rhabdomyolysis induced by prolonged exercise. These manifestations presumably reflect the requirement of working cardiac and skeletal muscle for energy supplied from fatty acid oxidation. In two of the disorders, SCAD deficiency and the severe form of MAD deficiency, chronic CNS toxicity is a dominant feature. The severe effects on the brain in these two disorders may reflect the fact that short-chain fatty acids more readily cross the blood-brain barrier than longer-chain fatty acids.(ABSTRACT TRUNCATED AT 400 WORDS)
目前已在线粒体脂肪酸氧化途径中鉴定出九种遗传性疾病,包括长链酰基辅酶A脱氢酶(LCAD)、中链酰基辅酶A脱氢酶(MCAD)、短链酰基辅酶A脱氢酶(SCAD)和HMG - CoA裂解酶缺乏症,肉碱棕榈酰转移酶(CPT)和多种酰基辅酶A脱氢酶(MAD)缺乏症各有两种形式,以及一种特征未完全明确的原发性肉碱缺乏症。这组新疾病的临床表现多样,不仅应引起普通儿科医生(昏迷、低血糖)的关注,还应引起儿科神经学(肌病)、心脏病学(心肌病)和胃肠病学(脂肪肝)亚专科医生以及遗传学和代谢领域医生的关注。脂肪酸氧化遗传缺陷的表现特征与脂肪酸氧化在长期禁食期间以及工作中的心肌和骨骼肌能量产生中起主要作用这一概念相契合。禁食诱发的危及生命的昏迷和低血糖发作是大多数脂肪酸氧化障碍(MCAD、LCAD和HMG - CoA裂解酶缺乏症、婴儿型CPT缺乏症、轻度MAD缺乏症以及某些原发性肉碱缺乏症病例)常见的表现特征。这些疾病中的低血糖最容易解释为受影响患者无法利用脂肪酸作为替代葡萄糖的燃料。然而,应该强调的是,这些疾病中的昏迷可能在血浆葡萄糖浓度达到低血糖水平之前就由脂肪酸或脂肪酸中间产物的直接毒性作用引起。肌肉功能的严重紊乱是几种疾病的特征;肥厚型心肌病和慢性骨骼肌无力在轻度和重度MAD缺乏症、原发性肉碱缺乏症以及一些LCAD缺乏症患者中均有发生。相比之下,成人型CPT缺乏症患者肌肉力量正常,但容易因长时间运动诱发疼痛性横纹肌溶解发作。这些表现大概反映了工作中的心肌和骨骼肌对脂肪酸氧化提供能量的需求。在两种疾病中,SCAD缺乏症和重度MAD缺乏症,慢性中枢神经系统毒性是主要特征。这两种疾病对大脑的严重影响可能反映了短链脂肪酸比长链脂肪酸更容易穿过血脑屏障这一事实。(摘要截选至400字)
