Schoser Benedikt, Raben Nina, Varfaj Fatbardha, Walzer Mark, Toscano Antonio
Friedrich-Baur-Institute, Department of Neurology, LMU Klinikum, Ludwig-Maximilians University, Munich, Germany.
M6P Therapeutics, St. Louis, MO, USA.
Mol Genet Metab Rep. 2024 Apr 25;39:101085. doi: 10.1016/j.ymgmr.2024.101085. eCollection 2024 Jun.
Pompe disease is a rare genetic disorder characterized by a deficiency of acid α-glucosidase (GAA), leading to the accumulation of glycogen in various tissues, especially in skeletal muscles. The disease manifests as a large spectrum of phenotypes from infantile-onset Pompe disease (IOPD) to late-onset Pompe disease (LOPD), depending on the age of symptoms onset. Quantifying GAA activity and glycogen content in skeletal muscle provides important information about the disease severity. However, the distribution of GAA and glycogen levels in skeletal muscles from healthy individuals and those impacted by Pompe disease remains poorly understood, and there is currently no universally accepted standard assay for GAA activity measurement. This systematic literature review aims to provide an overview of the available information on GAA activity and glycogen content levels in skeletal muscle biopsies from patients with Pompe disease. A structured review of PubMed and Google Scholar literature (with the latter used to check that no additional publications were identified) was conducted to identify peer-reviewed publications on glycogen storage disease type II [MeSH term] + GAA, protein human (supplementary concept), Pompe, muscle; and muscle, acid alpha-glucosidase. A limit of English language was applied. Results were grouped by methodologies used to quantify GAA activity and glycogen content in skeletal muscle. The search and selection strategy were devised and carried out in line with Preferred Reporting of Items in Systematic Reviews and Meta-Analysis guidelines and documented using a flowchart. Bibliographies of papers included in the analysis were reviewed and applicable publications not already identified in the search were included. Of the 158 articles retrieved, 24 (comprising >100 muscle biopsies from >100 patients) were included in the analysis, with four different assays. Analysis revealed that patients with IOPD exhibited markedly lower GAA activity in skeletal muscles than those with LOPD, regardless of the measurement method employed. Additionally, patients with IOPD had notably higher glycogen content levels in skeletal muscles than those with LOPD. In general, however, it was difficult to fully characterize GAA activity because of the different methods used. The findings underscore the challenges in the interpretation and comparison of the results across studies because of the substantial methodological variations. There is a need to establish standardized reference ranges of GAA activity and glycogen content in healthy individuals and in Pompe disease patients based on globally standardized methods to improve comparability and reliability in assessing this rare disease.
庞贝病是一种罕见的遗传性疾病,其特征是酸性α-葡萄糖苷酶(GAA)缺乏,导致糖原在各种组织中积累,尤其是在骨骼肌中。根据症状出现的年龄,该疾病表现出从婴儿型庞贝病(IOPD)到晚发型庞贝病(LOPD)的广泛表型。量化骨骼肌中的GAA活性和糖原含量可提供有关疾病严重程度的重要信息。然而,健康个体和受庞贝病影响个体的骨骼肌中GAA和糖原水平的分布仍知之甚少,目前尚无普遍接受的GAA活性测量标准方法。本系统文献综述旨在概述庞贝病患者骨骼肌活检中GAA活性和糖原含量水平的现有信息。对PubMed和谷歌学术文献进行了结构化综述(后者用于检查是否未识别出其他出版物),以识别关于II型糖原贮积病[医学主题词]+GAA、蛋白质人(补充概念)、庞贝、肌肉;以及肌肉、酸性α-葡萄糖苷酶的同行评审出版物。应用了英语语言限制。结果按用于量化骨骼肌中GAA活性和糖原含量的方法进行分组。搜索和选择策略是根据系统评价和荟萃分析的首选报告项目指南设计和实施的,并使用流程图进行记录。对分析中纳入论文的参考文献进行了审查,并纳入了搜索中未识别出的适用出版物。在检索到的158篇文章中,24篇(包括来自100多名患者的100多次肌肉活检)被纳入分析,采用了四种不同的检测方法。分析显示,无论采用何种测量方法,IOPD患者骨骼肌中的GAA活性均明显低于LOPD患者。此外,IOPD患者骨骼肌中的糖原含量水平明显高于LOPD患者。然而,总体而言,由于使用的方法不同,很难全面表征GAA活性。这些发现强调了由于方法上的重大差异,在不同研究结果的解释和比较方面存在挑战。需要基于全球标准化方法建立健康个体和庞贝病患者GAA活性和糖原含量的标准化参考范围,以提高评估这种罕见疾病的可比性和可靠性。
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