Clinical Manifestations and Gene Mutations of Children with Glycogen Storage Disease

doi:10.12114/j.issn.1007-9572.2019.00.666

Abstract

Abstract: Background　Hepatic glycogen storage disease（HGSD） is a rare group of hereditary glycometabolism disorders involving the liver.All types of HGSD have similar clinical manifestations.Gene detection has replaced enzymatic diagnosis requiring liver biopsy，provides a reliable basis for the diagnosis，classification and treatment of HGSD.Objective　To study the clinical characteristics and gene mutation in children with HGSD.Methods　Six children diagnosed with HGSD on the basis of clinical manifestations and laboratory examinations were recruited from Department of Pediatrics，the First People's Hospital of Yunnan Province from 2015 to 2018.Next generation sequencing was used to directly sequence the exons of related genes of HGSD and to compare them with the reference sequences to find possible gene mutations.The clinical manifestations，signs，laboratory results，gene test results，treatment and prognosis of the children were summarized.Results　Hepatomegaly，hypoglycemia，and increased ALT，triacylglyceroll and actic acid were found in all cases，elevated uric acid in 4 cases，and elevated cholesterol in 2 cases.Urinary protein was found in 4 cases.Positive urine ketones and suspected positive urine ketones were found in 4 cases，1 case，respectively.Four cases had short stature.Three cases were found with G6PC mutations，and 2 of them had c.648G>T homozygous mutations，the other 1 had c.262 delG/ c.648 G>T compound heterozygous mutations，but all of them were diagnosed with HGSD type Ⅰa.One case did not undergo the gene testing due to death，but her parents were detected with a heterozygous mutation of G6PC gene，c.49delCinsGTA and c.262delG，respectively，suggesting that she had HGSD type Ⅰa.One case was detected with SLC37A4 gene compound heterozygous mutations：c.1109G>A/c.572C>T，and was diagnosed with HGSD type Ⅰb.Homozygous mutation of c.579delC in AGL gene was detected in 1 case and confirmed as HGSD typeⅢ.Conclusion　This group of HGSD patients had hepatomegaly，hypoglycemia，hyperlipidemia and elevated ALT，generally accompanied by high lactic academia，hyperuricemia，positive urinary ketones and short stature.HGSD type Ⅰa was the most common type（4 cases），and the G6PC mutation type was c.648G > T，c.262delG mutation；1 case was GSD typeⅠb.SLC37A4 c.572C > T mutation is a common mutation in Chinese，but c.1109G > A mutation is newly discovered.One case had HGSD type Ⅲ，with c.579delC mutation of AGL gene as a known pathogenic mutation.

Key words: Liver glycogen storage disease, Glycogen storage disease type Ⅰ, Glucose-6-phosphatase, Glycose-6-phosphate translocase, Glycogen storage disease type Ⅲ, Glycogen debrancher deficiency, Mutation

摘要： 背景　肝糖原累积病是一组罕见的累及肝脏的遗传性糖代谢障碍疾病，各型有相似的临床表现，基因检测已取代有创性肝穿刺酶活性检测的确诊方法，对肝糖原累积病的确诊、分型及治疗提供了可靠的依据。目的　研究肝糖原累积病患儿的临床特点及基因突变情况。方法　选择2015—2018年云南省第一人民医院儿科确诊的6例肝糖原累积病患儿为研究对象。根据临床表现、实验室检查，6例患儿临床诊断为肝糖原累积病，采用二代测序法（NGS）对糖原累积病（GSD）相关基因外显子区直接测序与参考序列进行比较，从而发现可能存在的基因突变。对6例患儿的临床表现、体征及实验室检查结果，基因检测结果，治疗及预后情况进行总结。结果　6例患儿均有肝脏肿大、低血糖、丙氨酸氨基转移酶升高、三酰甘油升高、乳酸升高，尿酸升高4例，胆固醇升高2例。尿蛋白阳性4例，尿酮体阳性4例，1例酮体可疑阳性。4例矮小。3例患儿存在G6PC突变，其中2例为c.648G>T纯合突变，1例为c.262delG/c.648G>T复合杂合突变，均可确诊为GSDⅠa型。1例患儿因已死亡不能行基因检测，其父母分别检出G6PC基因的一个杂合突变：c.49delCinsGGTA、c.262delG，推断患儿为GSDⅠa型。1例患儿检出SLC37A4基因复合杂合突变：c.1109G>A/c.572C>T，确诊为GSDⅠb型。1例患儿检出AGL基因 c.579delC纯合突变，确诊为GSDⅢ型。结论　本组6例肝糖原累积病患儿均有肝肿大、低血糖、高脂血症及丙氨酸氨基转移酶升高，普遍伴有高乳酸、高尿酸、尿酮体阳性及身材矮小。GSDⅠa型最多见，共4例，G6PC突变类型为c.648G>T、c.262delG突变；GSDⅠb型1例，SLC37A4 c.572C>T突变是已知中国人常见突变，c.1109G>A为新发现突变；GSDⅢ型1例，AGL基因c.579delC突变为已知致病突变。

关键词: 肝糖原累积病, 糖原累积病Ⅰ型, 葡萄糖-6-磷酸酶, 葡萄糖-6-磷酸酶转移酶, 糖原累积病Ⅲ型, 糖原脱枝酶, 突变

LI Yuan,TIAN Yunfen. Clinical Manifestations and Gene Mutations of Children with Glycogen Storage Disease　[J]. Chinese General Practice, 2020, 23(15): 1921-1927. DOI: 10.12114/j.issn.1007-9572.2019.00.666.
李媛,田云粉. 儿童肝糖原累积病的临床特点及基因突变研究[J]. 中国全科医学, 2020, 23(15): 1921-1927. DOI: 10.12114/j.issn.1007-9572.2019.00.666.

References

［1］刘璐，孙梅.肝糖原累积病研究进展［J］．国际儿科学杂志，2011，38（1）：62-65．DOI：10.3760/cma.j.issn.1673-4408.2011.01.022.1673-4408.2011.01.022.
LIU L，SUN M．New perspectives of glycogen storage disease［J］．Int J Pediatr，2011，38（1）：62-65．DOI：10.3760/cma.j.issn.1673-4408.2011.01.022.
［2］邱文娟.糖原累积病Ⅰ型［M］//顾学范.临床遗传代谢病.北京：人民卫生出版社，2015：168-171.
［3］CHOU J Y，MANSFIELD B C.Mutations in the glucose-6-phosphatase-alpha（G6PC） gene that cause typeⅠa glycogen storage disease［J］．Hum Mutat，2008，29（7）：921-930．DOI：10.1002/humu.20772.
［4］KISHNANI P S，AUSTIN S L，ABDENUR J E，et al．Diagnosis and management of glycogen storage disease typeⅠ：a practice guideline of the American College of Medical Genetics and Genomics［J］．Genet Med，2014，16（11）：e1．DOI：10.1038/gim.2014.128.
［5］RAKE J P，VISSER G，LABRUNE P，et al．Glycogen storage disease typeⅠ：diagnosis，management，clinical course and outcome.Results of the European Study on Glycogen Storage Disease Type Ⅰ（ESGSD Ⅰ）［J］．Eur J Pediatr，2002，161（Suppl 1）：S20-34．DOI：10.1007/s00431-002-0999-4.
［6］MELIS D，FULCERI R，PARENTI G，et al．Genotype/phenotype correlation in glycogen storage disease type 1b：a multicentre study and review of the literature［J］．Eur J Pediatr，2005，164（8）：501-508．DOI：10.1007/s00431-005-1657-4.
［7］邱文娟，顾学范，叶军，等．糖原累积病Ⅰa 型基因突变和临床研究［J］．中华内分泌代谢杂志，2004，20（6）：502-505.QIU W J，GU X F，YE J，et al．Gene mutation and clinical study in the patients with glycogen storage disease type Ⅰa［J］．Chin J Endocrinol Metab，2004，20（6）：502-505.
［8］梁翠丽，刘丽，盛慧英，等．糖原累积病Ⅰa型患儿20例基因突变分析与临床研究［J］．中华实用儿科临床杂志，2013，28（8）：581-585．DOI：10.3760/cma.j.issn.2095-428X.2013.08.007.
LIANG C L，LIU L，SHENG H Y，et al．Analysis of gene mutations and clinical manifestations in 20 patients with glycogen storage disease type Ⅰ a ［J］．Chin J Appl Pediatr，2013，28（8）：581-585．DOI：10.3760/cma.j.issn.2095-428X.2013.08.007.
［9］AKANUMA J，NISHIGAKI T，FUJII K，et al．Glycogen storage disease typeⅠa：molecular diagnosis of 51 Japanese patients and characterization of splicing mutations by analysis of ectopically transcribed mRNA from lymphoblastoid cells［J］．Am J Med Genet，2000，91（2）：107-112.
［10］LEI K J，CHEN Y T，CHEN H，et al．Genetic basis of glycogen storage disease type 1a：prevalent mutations at the glucose-6-phosphatase locus［J］．Am J Hum Genet，1995，57（4）：766-771.
［11］VEIGA-DA-CUNHA M，GERIN I，CHEN Y T，et al．The putative glucose 6-phosphate translocase gene is mutated in essentially all cases of glycogen storage disease typeⅠ non-A［J］．Eur J Hum Genet，1999，7（6）：717-723．DOI：10.1038/sj.ejhg.5200366.
［12］MATERN D，SEYDEWITZ H H，BALI D，et al．Glycogen storage disease typeⅠ：diagnosis and phenotype/genotype correlation［J］．Eur J Pediatr，2002，161（Suppl 1）：S10-19．DOI：10.1007/s00431-002-0998-5.
［13］KURE S，SUZUKI Y，MATSUBARA Y，et al．Molecular analysis of glycogen storage disease typeⅠb：identification of a prevalent mutation among Japanese patients and assignment of a putative glucose-6-phosphate translocase gene to chromosome 11［J］．Biochem Biophys Res Commun，1998，248（2）：426-431．DOI：10.1006/bbrc.1998.8985.
［14］邱正庆，卢超霞，王薇，等．糖原累积病Ⅰb型15家系SLC37A4基因分析研究［J］．中华儿科杂志，2011，49（3）：203-208．DOI：10.3760/cma.j.issm 0578-1310.2011.03.011．
QIU Z Q，LU C X，WANG W，et al．Mutation in the SLC37A4 gene of glycogen storage disease typeⅠb in 15 families of the mainland of China ［J］．Chin J Pediatr，2011，49（3）：203-208．DOI：10.3760/cma.j.issm 0578-1310.2011.03.011．
［15］梁翠丽，刘丽，盛慧英，等．糖原累积病Ⅰb型患儿基因突变分析与临床研究［J］．中国当代儿科杂志，2013，15（8）：661-665.
LIANG C L，LIU L，SHENG H Y，et al．Gene mutations and clinical manifestations in children with glycogen storage disease type Ⅰb［J］．Chinese Journal of Contemporary Pediatrics，2013，15（8）：661-665.
［16］中华医学会神经病学分会，中华医学会神经病学分会神经肌肉病学组，中华医学会神经病学分会肌电图与临床神经生理学组.中国肌病型糖原累积病诊治指南［J］.中华神经科杂志，2016，49（1）：8-16．DOI：10.3760/cma.j.issn.1006-7876．2016.01.003.
Neurological Society of Chinese Medical Association，Neurological Society of Chinese Medical Association，Neuromyopathy Group，Neurological Society of Chinese Medical Association，Electromyography and Clinical Neurophysiology Group，Neurological Society of Chinese Medical Association.Guidelines for diagnosis and treatment of glycogen-accumulating diseases of Chinese myopathy［J］.Chin J Neurol，2016，49（1）：8-16．DOI：10.3760/cma.j.issn.1006-7876.2016.01.003.
［17］庄太凤.糖原累积病Ⅲ型临床和基因研究进展［J］．临床儿科杂志，2006，24（12）：947-949.
［18］ZHANG Y，XU M M，CHEN X X，et al．Genetic analysis and clinical assessment of four patients with Glycogen Storage Disease TypeⅢa in China［J］．BMC Med Genet，2018，19（1）：54．DOI：10.1186/s12881-018-0560-6.
［19］王薇，魏珉，宋红梅，等．肌肉中糖原含量与形态测定和糖原脱支酶活性检测诊断ⅢA型糖原累积症［J］.中华儿科杂志，2009，47（8）：608-621．DOI：10.3760/ema.j.isan.0578-1310.2009.08.0110.
WANG W，WEI M，SONG H M，et al．Diagnosis of glycogen storage disease typeⅢA by detecting glycogen debranching enzyme activity，glycogen content and structure in muscle［J］.Chin J Pediatr，2009，47（8）：608-621．DOI：10.3760/ema.j.isan.0578-1310.2009.08.0110.
［20］庄太凤，魏珉.Ⅲ型糖原累积症的临床特点分析［J］．山西医科大学学报，2011，42（2）：132-134．DOI：10.3969/J.ISSN.1007-6611.2011.02.010.
ZHUANG T F，WEI M.Clinical analysis of 50 cases of glycogen storage disease typeⅢ［J］．Journal of Shanxi Medical University，2011，42（2）：132-134．DOI：10.3969/J.ISSN.1007-6611.2011.02.010.
［21］魏珉.糖原累积病的治疗进展［J］．北京医学，2014，36（4）：244-246．DOI：10.15932/j.0253-9713.2014.04.013.
［22］KISHNANI P S，AUSTIN S L，ARN P，et al．Glycogen storage disease typeⅢdiagnosis and management guidelines［J］．Genet Med，2010，12（7）：446-463．DOI：10.1097/gim.0b013e3181e655b6.

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