Huybrechts Sofie J, Van Veldhoven Paul P, Hoffman Ilse, Zeevaert Renate, de Vos Rita, Demaerel Philippe, Brams Marijke, Jaeken Jaak, Fransen Marc, Cassiman David
K.U.Leuven, Moleculaire Celbiologie, Campust Gasthuisberg ON1, Herestraat 49 box 601, Leuven, 3000, Belgium.
BMJ Case Rep. 2009;2009. doi: 10.1136/bcr.07.2008.0503. Epub 2009 Jan 23.
Here we report a patient with Zellweger syndrome, who presented at the age of 3 months with icterus, dystrophy, axial hypotonia, and hepatomegaly. Abnormal findings of metabolic screening tests included hyperbilirubinaemia, hypoketotic dicarboxylic aciduria, increased C(26:0) and decreased C(22:0) plasma levels, and strongly reduced plasmalogen concentrations. In fibroblasts, both peroxisomal α- and β-oxidation were impaired. Liver histology revealed bile duct paucity, cholestasis, arterial hyperplasia, very small branches of the vena portae, and parenchymatic destruction. Immunocytochemical analysis of cultured fibroblasts demonstrated that the cells contain peroxisomal remnants lacking apparent matrix protein content and PEX14, a central membrane component of the peroxisomal matrix protein import machinery. Transfection of fibroblasts with a plasmid coding for wild-type PEX14 restored peroxisomal matrix protein import. Mutational analysis of this gene revealed a genomic deletion leading to the deletion of exon 3 from the coding DNA (c.85-?_170+?del) and a concomitant change of the reading frame (p.[Ile29_Lys56del;Gly57GlyfsX2]).
在此,我们报告一名患有泽尔韦格综合征的患者,该患者在3个月大时出现黄疸、营养不良、轴性肌张力减退和肝肿大。代谢筛查试验的异常结果包括高胆红素血症、低酮性二羧酸尿症、血浆中C(26:0)升高和C(22:0)降低,以及血浆缩醛磷脂浓度大幅降低。在成纤维细胞中,过氧化物酶体的α-氧化和β-氧化均受损。肝脏组织学检查显示胆管稀少、胆汁淤积、动脉增生、门静脉小分支以及实质破坏。对培养的成纤维细胞进行免疫细胞化学分析表明,这些细胞含有过氧化物酶体残余物,缺乏明显的基质蛋白含量以及PEX14,PEX14是过氧化物酶体基质蛋白导入机制的核心膜成分。用编码野生型PEX14的质粒转染成纤维细胞可恢复过氧化物酶体基质蛋白的导入。对该基因进行突变分析发现一个基因组缺失,导致编码DNA的外显子3缺失(c.85-?_170+?del),并伴随阅读框改变(p.[Ile29_Lys56del;Gly57GlyfsX2])。
