Clinical, Laboratory Data and Outcomes of 17 Iranian Citrullinemia Type1 Patients: Identification of Five Novel ASS1 Gene Mutations

S. Moarefian, M. Zamani, Ali Rahmanifar, B. Behnam, T. Zaman
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Abstract

Background: Citrullinemia type 1 (CTLN1) is an autosomal recessive metabolic disease caused by ASS1 gene mutations encoding argininosuccinic acid synthase enzyme which is within the pathway of arginine and nitric oxide biosynthesis. Methods: Disease confirmation was done by ASS1 gene mutation analysis using Next Generation Sequencing, DNA Sanger sequencing and bioinformatics. The study group members were17 citrullinemia type1 patients from 10 unrelated families referred to Iranian National Society for the Study of Inborn Errors of Metabolism’s clinic between 2008-2020. Clinical, laboratory and molecular data were retrospectively evaluated. Results: Eleven different ASS1 gene mutations were detected. Presentation: 3/17 (76%) neonatal, 3/17 (18%) late infantile, 1/17(6%) asymptomatic. Severe developmental delay and intractable seizures despite metabolic control was the only surviver of neonatal form outcome. Two patients with late infantile form live metabolically and seizure controlled with quite normal performance. DNA mutations: 7 missense, 1 nonsense, and 2 indel mutations in twelve, two, three patients, respectively. Five novel mutations were detected including a homozygous GG deletion in exon 11 (c.790_791delGG; G264Pfs*3) and a homozygous mutation in exon 6 (c.440C>T; p.M147T), both leading to infantile form; a homozygous mutation in exon 14 (c.1130T>C; p.M377T) leading to neonatal form; two compound heterozygote mutations in exon 14 (c.1167_1168insC& c.1186T>A; p.S396T) leading to asymptomatic form. Five patients (38%) with classic neonatal form had mutation in exon14 of ASS1 (c.1168G>A; p.G390R). Conclusions: Classic neonatal form was the most common form of disease in Iranian studied patients and exon 14: c.1168G>A; (p.G390R) was the most frequent ASS1 gene mutation. Global neonatal screening in Iran is recommended for citrullinemia type1 and certain mutations can be used for screening lethal form of disease in this population.
17例伊朗瓜氨酸血症1型患者的临床、实验室数据和结果:鉴定5种新的ASS1基因突变
背景:瓜氨酸血症1型(CTLN1)是一种常染色体隐性代谢性疾病,由编码精氨酸琥珀酸合成酶的ASS1基因突变引起,该基因位于精氨酸和一氧化氮生物合成途径内。方法:采用Next Generation Sequencing、DNA Sanger Sequencing和生物信息学方法,对ASS1基因突变进行分析,确认疾病。研究小组成员是来自10个不相关家庭的17名瓜氨酸血症1型患者,这些患者在2008-2020年期间被转诊到伊朗国家先天性代谢错误研究协会的诊所。回顾性评价临床、实验室和分子数据。结果:检测到11种不同的ASS1基因突变。表现:3/17(76%)新生儿,3/17(18%)晚期婴儿,1/17(6%)无症状。严重的发育迟缓和顽固性癫痫,尽管代谢控制是新生儿形式的结局唯一的幸存者。2例婴幼儿晚期患者代谢正常,癫痫发作控制正常。DNA突变:12例,2例,3例,分别有7例错义突变,1例无义突变,2例无义突变。检测到5个新突变,包括外显子11的纯合GG缺失(c.790_791delGG;G264Pfs*3)和6外显子纯合突变(c.440C>T;p.M147T),两者都导致婴儿形态;外显子14的纯合突变(C . 1130t >C;p.m.377t)导致新生儿形式;第14外显子两个复合杂合子突变(c. 1167_1168insc和c. 1186t> A);p.S396T)导致无症状症状。5例典型新生儿型患者(38%)ASS1外显子14突变(c.1168G>A;p.G390R)。结论:典型的新生儿形式是伊朗研究患者最常见的疾病形式,外显子14:c.1168G>A;(p.G390R)是最常见的ASS1基因突变。在伊朗,建议对1型瓜氨酸血症进行全球新生儿筛查,某些突变可用于筛查该人群中的致死形式的疾病。
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