通过新生儿筛查发现的马来酰乙酰乙酸异构酶缺乏症新病例及 32 年来的自然病史:德国新生儿筛查中心的经验。

IF 4 Q1 GENETICS & HEREDITY
Gwendolyn Gramer, Saskia B Wortmann, Junmin Fang-Hoffmann, Dirk Kohlmüller, Jürgen G Okun, Holger Prokisch, Thomas Meitinger, Georg F Hoffmann
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引用次数: 0

摘要

世界各国都在进行基于琥珀酰丙酮测定的新生儿肝肾型酪氨酸血症(HT1)筛查(NBS)。最近,GSTZ1 的双拷贝致病变体被描述为马来酰乙酰乙酸异构酶(MAAI)缺乏症的基础,可作为 NBS 检测到琥珀酰丙酮轻微升高的个体的鉴别诊断。我们报告了德国一家大型 NBS 中心在 53 个月内对 HT1 进行 NBS 的经验,以及对其他 MAAI 缺乏症病例的鉴定和特征描述,其中包括一名自然病史超过 32 年的患者。2016年8月至2020年12月期间,共有516803名儿童在海德堡的NBS中心接受了HT1的NBS治疗。在琥珀酰丙酮升高的 42 名儿童中,有 2 例(258.401 例中有 1 例)确诊为 HT1。两个病例被怀疑患有 MAAI 缺乏症,一个病例的尿液中显示出微量琥珀酰丙酮,经基因证实患有 MAAI 缺乏症。在该病例中发现了一种以前未报道过的致病性 GSTZ1 变异,呈双倍拷贝状态。分离分析表明,该病例的母亲为单等位基因,父亲为同源基因。32 岁的父亲在此之前没有任何医疗问题,实验室检查也无异常。在琥珀酰丙酮轻微升高的 HT1 NBS 病例中,必须将 MAAI 视为罕见的鉴别诊断,以便做出正确的咨询和治疗决定。我们对 32 年自然病史的观察进一步证明,MAAI 缺乏症的临床过程是良性的,无需特殊治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
New Cases of Maleylacetoacetate Isomerase Deficiency with Detection by Newborn Screening and Natural History over 32 Years: Experience from a German Newborn Screening Center.

Newborn screening (NBS) for hepatorenal tyrosinemia type I (HT1) based on a determination of succinylacetone is performed in countries worldwide. Recently, biallelic pathogenic variants in GSTZ1 underlying maleylacetoacetate isomerase (MAAI) deficiency have been described as a differential diagnosis in individuals with slightly elevated succinylacetone detected by NBS. We report the experience with NBS for HT1 over 53 months in a large German NBS center and the identification and characterization of additional cases with MAAI deficiency, including one individual with a natural history over 32 years. A total of 516,803 children underwent NBS for HT1 at the NBS center in Heidelberg between August 2016 and December 2020. Of 42 children with elevated succinylacetone, HT1 was confirmed in two cases (1 in 258.401). MAAI deficiency was suspected in two cases and genetically confirmed in one who showed traces of succinylacetone in urine. A previously unreported pathogenic GSTZ1 variant was found in the index in a biallelic state. Segregation analysis revealed monoallelic carriership in the index case's mother and homozygosity in his father. The 32-year-old father had no medical concerns up to that point and the laboratory work-up was unremarkable. MAAI has to be considered a rare differential diagnosis in NBS for HT1 in cases with slight elevations of succinylacetone to allow for correct counselling and treatment decisions. Our observation of natural history over 32 years adds evidence for a benign clinical course of MAAI deficiency without specific treatment.

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来源期刊
International Journal of Neonatal Screening
International Journal of Neonatal Screening Medicine-Pediatrics, Perinatology and Child Health
CiteScore
6.70
自引率
20.00%
发文量
56
审稿时长
11 weeks
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