Schlotawa Lars, Dierks Thomas, Christoph Sophie, Cloppenburg Eva, Ohlenbusch Andreas, Korenke G Christoph, Gärtner Jutta
Department of Paediatrics and Adolescent Medicine University Medical Center Göttingen Göttingen Germany.
Department of Chemistry, Biochemistry I Bielefeld University Bielefeld Germany.
JIMD Rep. 2019 Aug 20;49(1):48-52. doi: 10.1002/jmd2.12074. eCollection 2019 Sep.
Multiple sulfatase deficiency (MSD) is an ultra-rare lysosomal storage disorder (LSD). Mutations in the gene encoding the formylglycine generating enzyme (FGE) result in an unstable FGE protein with reduced enzymatic activity, thereby affecting the posttranslational activation of newly synthesized sulfatases. Complete absence of FGE function results in the most severe clinical form of MSD with neonatal onset and rapid deterioration. We report on a preterm infant presenting with hydrops fetalis, lung hypoplasia, and dysmorphism as major clinical signs. The patient died after 6 days from an intraventricular hemorrhage followed by multi-organ failure. MSD was caused by a homozygous stop mutation (c.191C>A, p.Ser64Ter). FGE protein and sulfatase activities were absent in patient fibroblasts. Hydrops fetalis is a rare symptom of LSDs and should be considered in the differential diagnosis in combination with dysmorphism. The diagnostic set up should include measurements of glycosaminoglycan excretion and lysosomal enzyme activities, among them at least two sulfatases, and molecular confirmation.
多种硫酸酯酶缺乏症(MSD)是一种极其罕见的溶酶体贮积症(LSD)。编码甲酰甘氨酸生成酶(FGE)的基因突变导致FGE蛋白不稳定且酶活性降低,从而影响新合成硫酸酯酶的翻译后激活。FGE功能完全缺失会导致MSD最严重的临床形式,表现为新生儿期起病且病情迅速恶化。我们报告了一例早产婴儿,其主要临床体征为胎儿水肿、肺发育不全和畸形。该患者在出现脑室内出血并继发多器官功能衰竭后6天死亡。MSD由纯合终止突变(c.191C>A,p.Ser64Ter)引起。患者成纤维细胞中不存在FGE蛋白和硫酸酯酶活性。胎儿水肿是LSDs的罕见症状,在鉴别诊断中应结合畸形予以考虑。诊断流程应包括测量糖胺聚糖排泄和溶酶体酶活性,其中至少包括两种硫酸酯酶,并进行分子学确诊。
