Akyüz Ayşe, Okur İlyas, Tümer Leyla, Eminoğlu Fatma Tuba, Köse Engin, Ergin Filiz Başak, İnci Aslı, Dalgıç Buket, Yüce Burcu, Çiftçi Bahattin, Oktar Suna Özhan, Erbaş Gonca, Biberoğlu Gürsel, Öktem Murat, Bakkaloğlu Ezgü Sevcan, Aktaş Emine, Ezgü Fatih Süheyl
Department of Pediatrics, Department of Inborn Metabolic Diseases, Faculty of Medicine, Gazi University, Ankara, Turkey.
Department of Inborn Metabolic Diseases, Ankara Training and Research Hospital, Zekai Tahir BurakEkBinası, Talatpaşa Bulvarı No:128, 06230, Altındağ/Ankara, Turkey.
Eur J Pediatr. 2025 Aug 9;184(9):540. doi: 10.1007/s00431-025-06371-7.
Glycogen storage disease type 1 (GSD1), which is categorized into GSD1a and GSD1b, is caused by disease-causing genetic variants in G6PC or SLC37A4 genes, respectively. The aim of this study was to present clinical characteristics, novel phenotypic and molecular features as well as long-term complications of the largest cohort of patients in Turkey and one of the largest cohorts in the world. The demographic, clinical, and molecular data of GSD1a or 1b patients who were followed up between 2000 and 2024 were collected retrospectively from patients' medical records. A total of 39 GSD1a patients were enrolled, and four different variants in the G6PC gene, c.247C > T (p.R83C), c.809G > T (p.G270V), c.562G > C (p.G188R), c.480G > A (p.W160*) were revealed. The most common variant among Turkish GSD1a patients was the c.247C > T (p.R83C) variant with an allele frequency of about 90%. Some unusual clinical features such as stroke, cataract, and mental retardation were observed in some patients. Also, cardiac hypertrophy was detected in three patients. Six different variants in the SLC37A4 gene, c.1042_1043delCT (p.L348Vfs53), c.892_905del (p.N298Pfs23), c.1015G > T (p.G339C), c.817G > A (p.G273S), c.892A > G (p.N298D), and c.382 T > C (p.W128R) were detected in eight patients with GSD1b, of which c.892A > G (p.N298D) and c.892_905del (p.N298Pfs23) were novel. The most prevalent variant was c.1042_1043delCT (p.L348Vfs53). The patient with the novel variant c.892A > G (p.N298D) has shown a very mild clinical course and was diagnosed in adulthood. This patient also had a co-existing HNF1A variants causing hepatic adenomas and MODY Diabetes.
Based on our study with the largest cohort from Turkey, the c.247C > T (p.R83C) allele frequency was found to be 85% for GSD1a, resembling the Ashkenazi Jewish population. The most frequent pathogenic genetic variant for GSD1b was found to be c.1042_1043delCT (p.L348Vfs*53). There were patients with novel presentations and coexistent phenotypic features. The high frequency of consanguineous marriages, of course, significantly contributes to such molecular and clinical findings, but further studies are obviously needed to investigate other factors.
• Glycogen storage disease type 1 (GSD1), which is categorized into GSD1a and GSD1b, is an autosomal recessive inborn error of metabolism, caused by disease-causing genetic variants in G6PC or SLC37A4 genes. The allelic homogeneity of G6PC gene was described in some ethnic or geographical origin. • Without adequate treatments long term complications may present in both GSD1a and GSD1b.
• This study documented the genotypic background and showed that c.247C>T (p.R83C) pathogenic genetic variant allele frequency is very high in Turkey for GSD1a resembling the Ashkenazi Jewish population and the c.1042_1043delCT (p.L348Vfs*53) disease-causing genetic variant seems to be the most frequent one for GSD1b. • This study includes largest cohort from Turkey with a high frequency of consanguineous marriages, and also presents phenotypic and genotypic features, co-existent diseases or conditions that could modify the clinical course.
1型糖原贮积病(GSD1)分为GSD1a和GSD1b,分别由G6PC或SLC37A4基因中的致病基因变异引起。本研究的目的是呈现土耳其最大队列以及世界上最大队列之一的患者的临床特征、新的表型和分子特征以及长期并发症。回顾性收集了2000年至2024年期间随访的GSD1a或1b患者的人口统计学、临床和分子数据。共纳入39例GSD1a患者,在G6PC基因中发现了四种不同变异,即c.247C>T(p.R83C)、c.809G>T(p.G270V)、c.562G>C(p.G188R)、c.480G>A(p.W160*)。土耳其GSD1a患者中最常见的变异是c.247C>T(p.R83C)变异,等位基因频率约为90%。在一些患者中观察到了中风、白内障和智力发育迟缓等一些不寻常的临床特征。此外,在三名患者中检测到心脏肥大。在8例GSD1b患者中检测到SLC37A4基因的六种不同变异,即c.1042_1043delCT(p.L348Vfs53)、c.892_905del(p.N298Pfs23)、c.1015G>T(p.G339C)、c.817G>A(p.G273S)、c.892A>G(p.N298D)和c.382T>C(p.W128R),其中c.892A>G(p.N298D)和c.892_905del(p.N298Pfs23)是新发现的。最常见的变异是c.1042_1043delCT(p.L348Vfs53)。携带新变异c.892A>G(p.N298D)的患者临床病程非常轻微,在成年期被诊断出来。该患者还存在导致肝腺瘤和MODY糖尿病的HNF1A变异。
基于我们对土耳其最大队列的研究,发现GSD1a的c.247C>T(p.R83C)等位基因频率为85%,与德系犹太人群相似。发现GSD1b最常见的致病基因变异是c.1042_1043delCT(p.L348Vfs*53)。有表现新且存在共存表型特征的患者。当然,近亲结婚的高频率显著促成了此类分子和临床发现,但显然还需要进一步研究来调查其他因素。
• 1型糖原贮积病(GSD1)分为GSD1a和GSD1b,是一种常染色体隐性遗传性先天性代谢缺陷病,由G6PC或SLC37A4基因中的致病基因变异引起。在一些种族或地理区域描述了G6PC基因的等位基因同质性。• 若没有适当治疗,GSD1a和GSD1b都可能出现长期并发症。
• 本研究记录了基因型背景,表明在土耳其,GSD1a的c.247C>T(p.R83C)致病基因变异等位基因频率非常高,与德系犹太人群相似,而c.1042_1043delCT(p.L348Vfs*53)致病基因变异似乎是GSD1b最常见的变异。• 本研究纳入了土耳其最大的队列,近亲结婚频率高,还呈现了可能改变临床病程的表型和基因型特征、共存疾病或状况。
