Clinical and Laboratory Findings on Glycogen Storage Disease Type V: Results from a Retrospective Observational Study in a Tertiary Hospital.

IF 2 4区医学 Q3 ENDOCRINOLOGY & METABOLISM

Endocrine, metabolic & immune disorders drug targets Pub Date : 2023-09-14 DOI:10.2174/1871530323666230914122936

Ângela Pereira, Jorge Diogo da Silva, Ana Rita Soares, Arlindo Guimas, Sara Rocha, Márcio Cardoso, Cristina Garrido, Célia Azevedo Soares, Isabel Nunes, Ana Maria Fortuna, Dulce Quelhas, Sónia Figueiroa, Rosa Ribeiro, Manuela Santos, Esmeralda Martins, Nataliya Tkachenko

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引用次数: 0

Abstract

Introduction - Glycogen storage disease type V (GSDV, MIM #232600) is an autosomal recessive metabolic myopathy caused by pathogenic variants in the PYGM gene. The characteristic symptoms of exercise intolerance, myalgia, and cramps, which improve after a few minutes of rest, are frequently unrecognized in affected children. When there is clinical suspicion, the initial approach with a forearm exercise test has diagnostic value by detecting low post-exercise plasma lactate-to-ammonia ratio values. The diagnostic algorithm is followed by genetic testing if the results suggest myophosphorylase deficiency. Methods - This was a retrospective observational study conducted based on reviewing medical records of patients with GSDV in a tertiary hospital. We assessed demographic variables, including the timing of onset and diagnosis, relevant clinical characteristics, and whether genetic testing was performed, including its results. Results/Case Report - Our goal was to review the GSDV cases in our center to assess our cohort's diagnostic timing and clinical and genetic characteristics. We identified 28 patients from 24 families, three with consanguinity. The mean age at the time of the study was 43 years. While most (26/28; 93%) recalled their first symptoms in childhood/adolescence, only 25% (7/28) were diagnosed then. All patients had exercise intolerance and CK elevation, while about half reported the second wind phenomenon. Genetic testing was performed in 22 patients, revealing biallelic PYGM variants (9 homozygous, 13 compound heterozygous) as the most common (p.R50*). Conclusion - GSDV is rare and presents in the pediatric age, with subtle manifestations often underestimated for decades. A late diagnosis may negatively impact the psychosocial development of affected children. It is essential to recognize some unique features that facilitate diagnosis: history of exercise intolerance, the second wind sign, and high resting serum CK levels. Identifying the disease-causing variants in PYGM is currently the gold standard for diagnosis as it is less invasive than performing a muscle biopsy, and may promptly diagnose the condition and avoid wrongful labelling of patients.

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V型糖原储存病的临床和实验室结果:来自某三级医院回顾性观察研究的结果

糖原储存病V型(GSDV, MIM #232600)是一种常染色体隐性代谢性肌病，由PYGM基因的致病变异引起。运动不耐受、肌痛和痉挛等特征性症状在休息几分钟后会有所改善，但这些症状在受影响的儿童中往往不为人所知。当有临床怀疑时，通过检测低运动后血浆乳酸氨比值，前臂运动试验的初始方法具有诊断价值。如果结果提示肌磷酸化酶缺乏症，诊断算法随后进行基因检测。方法:对某三级医院GSDV患者的病历进行回顾性观察性研究。我们评估了人口统计学变量，包括发病时间和诊断，相关临床特征，以及是否进行了基因检测，包括其结果。结果/病例报告-我们的目标是回顾我们中心的GSDV病例，以评估我们队列的诊断时间、临床和遗传特征。我们确定了来自24个家庭的28例患者，其中3例有血缘关系。研究时的平均年龄为43岁。而大多数(26/28;93%的患者回忆起他们在儿童/青少年时期的首次症状，只有25%(7/28)的患者当时被诊断出来。所有患者均有运动不耐受和CK升高，约一半的患者报告了第二次风现象。对22例患者进行基因检测，发现双等位基因PYGM变异(9例纯合子，13例复合杂合子)最为常见(p.R50*)。结论- GSDV是罕见的，出现在儿童年龄，其细微的表现往往被低估了几十年。较晚的诊断可能对受影响儿童的心理社会发展产生负面影响。必须认识到一些有助于诊断的独特特征:运动不耐受史、第二风征和静息时血清CK水平高。识别PYGM中的致病变异是目前诊断的金标准，因为它比进行肌肉活检侵入性更小，并且可以及时诊断病情并避免错误标记患者。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Endocrine, metabolic & immune disorders drug targets ENDOCRINOLOGY & METABOLISMIMMUNOLOGY-IMMUNOLOGY

CiteScore

4.60

自引率

5.30%

发文量

217

期刊介绍： Aims & Scope This journal is devoted to timely reviews and original articles of experimental and clinical studies in the field of endocrine, metabolic, and immune disorders. Specific emphasis is placed on humoral and cellular targets for natural, synthetic, and genetically engineered drugs that enhance or impair endocrine, metabolic, and immune parameters and functions. Moreover, the topics related to effects of food components and/or nutraceuticals on the endocrine-metabolic-immune axis and on microbioma composition are welcome.