Department of Pediatrics, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.
Mol Genet Genomic Med. 2020 Oct;8(10):e1444. doi: 10.1002/mgg3.1444. Epub 2020 Aug 8.
Glycogen storage disease (GSD) is a relatively rare inborn metabolic disorder, our study aims to investigate the genotypic and clinical feature of hepatic GSDs in China.
The clinical and genotypic data of 49 patients with hepatic GSDs were collected retrospectively and analyzed.
After gene sequencing, 49 patients were diagnosed as GSDs, including GSD Ia (24 cases), GSD IIIa (11 cases), GSD IXa (8 cases), GSD VI (3 cases) and GSD Ib (3 cases). About 45 gene variants of G6PC, AGL, PHKA2, PYGL, and SLC37A4 were detected; among which, 22 variants were unreported previously. c.648G>T (p. Leu216Leu) of G6PC exon 5 is the most common variant for GSD Ia patients (20/24,83.33%), splice variant c.1735+1G>T of AGL exon 13 is relatively common among GSD IIIa, while novel variant accounts for the majority of GSD IXa and GSD VI patients. As for clinical features, there was no significant difference in the onset age among group GSD Ia, GSD IIIa, and GSD IXa, but the age at diagnosis and average disease duration from diagnosis of GSD Ia were significantly higher than GSD IIIa and GSD IXa. Body weight of GSD patients was basically normal, but growth retardation was relatively common among them, especially for GSD Ia patients; and renomegaly was only found in GSD Ia. Besides, serum cholesterol, triglyceride, lactic acid, and uric acid in GSD Ia were significantly higher than those with GSD IIIa and IXa (p < 0.05); but ALT, AST, CK, and LDH of GSD III and GSD IXa were significantly higher when compared to GSD Ia (p < 0.05).
All hepatic GSDs patients share similarity in clinical and biochemical spectrum, but delayed diagnosis and biochemical metabolic abnormalities were common in GSD Ia. For family with GSD proband, pedigree analysis and genetic testing is strongly recommended.
糖原贮积病(GSD)是一种相对罕见的先天性代谢紊乱,本研究旨在探讨中国肝 GSD 的基因型和临床特征。
回顾性收集 49 例肝 GSD 患者的临床和基因型资料并进行分析。
经基因测序,49 例患者被诊断为 GSD,包括 GSD Ia(24 例)、GSD IIIa(11 例)、GSD IXa(8 例)、GSD VI(3 例)和 GSD Ib(3 例)。共检测到 G6PC、AGL、PHKA2、PYGL 和 SLC37A4 等 45 种基因突变;其中 22 种为以前未报道过的变异。G6PC 外显子 5 的 c.648G>T(p.Leu216Leu)是 GSD Ia 患者最常见的变异(20/24,83.33%),AGL 外显子 13 的剪接变异 c.1735+1G>T 在 GSD IIIa 中较为常见,而 GSD IXa 和 GSD VI 患者则以新变异为主。就临床特征而言,GSD Ia、GSD IIIa 和 GSD IXa 患者的发病年龄无显著差异,但 GSD Ia 患者的诊断年龄和平均病程从诊断开始显著高于 GSD IIIa 和 GSD IXa。GSD 患者的体重基本正常,但生长迟缓较为常见,尤其是 GSD Ia 患者;且仅在 GSD Ia 患者中发现肝肿大。此外,GSD Ia 患者的血清胆固醇、甘油三酯、乳酸和尿酸明显高于 GSD IIIa 和 GSD IXa(p<0.05);但 GSD III 和 GSD IXa 的 ALT、AST、CK 和 LDH 明显高于 GSD Ia(p<0.05)。
所有肝 GSD 患者在临床和生化谱上具有相似性,但 GSD Ia 患者存在诊断延迟和生化代谢异常。对于有 GSD 先证者的家族,强烈建议进行家系分析和基因检测。
