Gong Jing-Yu, Setchell Kenneth D R, Zhao Jing, Zhang Wujuan, Wolfe Brian, Lu Yi, Lackner Karolin, Knisely A S, Wang Neng-Li, Hao Chen-Zhi, Zhang Mei-Hong, Wang Jian-She
*The Department of Pediatrics, Jinshan Hospital, Fudan University, Shanghai, China †Department of Pathology and Laboratory Medicine, Cincinnati Children's Hospital Medical Center, Cincinnati, OH ‡Center for Pediatric Liver Diseases, Children's Hospital of Fudan University §Department of Pediatrics, Shanghai Medical College of Fudan University, Shanghai, China ||Institut für Pathologie, Medizinische Universität Graz, Graz, Austria.
J Pediatr Gastroenterol Nutr. 2017 Nov;65(5):561-568. doi: 10.1097/MPG.0000000000001730.
Cerebrotendinous xanthomatosis (CTX) is caused by defects in sterol 27-hydroxylase (CYP27A1, encoded by CYP27A1), a key enzyme in the bile acid synthesis pathway. CTX usually presents as neurologic disease in adults or older children. The rare reports of CTX manifest as neonatal cholestasis assess the cholestasis as transient, with patient survival. Our experience differs.
Homozygous or compound heterozygous CYP27A1 mutations were detected in 8 neonatal cholestasis patients by whole exome sequencing, panel sequencing, or Sanger sequencing. Their clinical and biochemical data were retrospectively reviewed. Immunostaining for CYP27A1 was conducted in liver of 4 patients. Mass spectrometry was used to analyze patients' urine samples.
All 8 infants had severe cholestasis. Five died from, or were transplanted for, liver failure; 3 cleared their jaundice eventually. Marking for CYP27A1 was weak or absent in 3 of the 4 patient specimens. Mass spectrometry of urine revealed a predominance of sulfated and doubly conjugated (sulfated-glucuronidated) bile alcohols. No patient harbored a putatively pathogenic mutation in genes other than CYP27A1 that have been implicated in cholestatic liver disease.
CTX manifest as neonatal cholestasis has a bile acid profile different from CTX manifest in later life, and thus may be overlooked. Immunostaining, mass spectrometry of urine, and genetic studies can support one another in making the diagnosis. A substantial proportion of CTX patients with severe neonatal cholestasis may die or need liver transplantation. CTX manifest in infancy as severe cholestasis warrants further investigation of biochemical diagnostic criteria and best management.
脑腱黄瘤病(CTX)由胆汁酸合成途径中的关键酶——甾醇27-羟化酶(由CYP27A1编码)缺陷引起。CTX通常在成人或大龄儿童中表现为神经系统疾病。关于CTX表现为新生儿胆汁淤积的罕见报道将胆汁淤积评估为短暂性,患者存活。我们的经验有所不同。
通过全外显子测序、基因 panel 测序或桑格测序在8例新生儿胆汁淤积患者中检测纯合或复合杂合的CYP27A1突变。对他们的临床和生化数据进行回顾性分析。对4例患者的肝脏进行CYP27A1免疫染色。采用质谱分析法分析患者的尿液样本。
所有8例婴儿均有严重胆汁淤积。5例死于肝功能衰竭或接受肝移植;3例最终黄疸消退。4例患者标本中有3例CYP27A1标记弱阳性或缺失。尿液质谱分析显示硫酸化和双共轭(硫酸化-葡萄糖醛酸化)胆汁醇占优势。除CYP27A1外,没有患者在其他与胆汁淤积性肝病相关的基因中携带假定的致病突变。
表现为新生儿胆汁淤积的CTX胆汁酸谱与成年后表现的CTX不同,因此可能被忽视。免疫染色、尿液质谱分析和基因研究在诊断中可相互支持。相当一部分患有严重新生儿胆汁淤积的CTX患者可能死亡或需要肝移植。婴儿期表现为严重胆汁淤积的CTX值得进一步研究生化诊断标准和最佳治疗方法。
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