Sudarsanam Annapurna, Singh Harry, Wilcken Bridget, Stormon Michael, Arbuckle Susan, Schmitt Bernhard, Clayton Peter, Earl John, Webster Richard
T.Y. Nelson Department of Neurology and Neurosurgery, Children's Hospital at Westmead, Sydney, NSW, Australia.
JIMD Rep. 2014;17:67-70. doi: 10.1007/8904_2014_338. Epub 2014 Sep 26.
We report the case of an 8-year-old boy with pyridoxamine 5'-phosphate oxidase (PNPO) deficiency. He developed seizures at 24 h of age that were refractory to standard anticonvulsant therapy and a trial of pyridoxine but responded to pyridoxal phosphate (PLP) at 28 days of life. Genetic testing identified compound heterozygous mutations in the PNPO gene. Management of encephalopathic episodes required escalation of PLP dose to 100 mg/kg/day by 2 years of age. Routine blood tests at this time showed significantly deranged liver function tests (LFTs). A wedge liver biopsy showed early cirrhosis with marked elevation of pyridoxal and pyridoxic acid levels in the liver sample. Despite extensive investigation, no cause other than PLP therapy could be identified for the cirrhosis. The PLP dose was weaned to 50 mg/kg/day before episodes of encephalopathy recurred. Concurrent with the reduction of his PLP dose, LFTs showed improvement. However, at 8 years of age, there is persistent evidence of hepatic fibrosis and early portal hypertension. We hypothesise that hepatic toxicity due to PLP or its degradation products is the cause of cirrhosis in this boy. Until further evidence becomes available, we would suggest that people with PNPO deficiency are treated with the minimum dose of PLP required to prevent episodes of encephalopathy.
我们报告了一例患有5'-磷酸吡哆胺氧化酶(PNPO)缺乏症的8岁男孩的病例。他在24小时龄时出现癫痫发作,对标准抗惊厥治疗和吡哆醇试验均无反应,但在28日龄时对磷酸吡哆醛(PLP)有反应。基因检测确定了PNPO基因中的复合杂合突变。到2岁时,对脑病发作的管理需要将PLP剂量增加到100mg/kg/天。此时的常规血液检查显示肝功能检查(LFTs)明显紊乱。肝脏楔形活检显示早期肝硬化,肝脏样本中吡哆醛和吡哆酸水平显著升高。尽管进行了广泛的调查,但除了PLP治疗外,没有发现其他导致肝硬化的原因。在脑病发作复发前,PLP剂量减至50mg/kg/天。随着PLP剂量的减少,LFTs显示有所改善。然而,在8岁时,仍有肝纤维化和早期门静脉高压的持续证据。我们推测,PLP或其降解产物引起的肝毒性是该男孩肝硬化的原因。在获得进一步证据之前,我们建议对PNPO缺乏症患者使用预防脑病发作所需的最低剂量的PLP进行治疗。