2024 Update of the TSOC Expert Consensus of Fabry Disease.

法布里病 医学 计算机科学 疾病 内科学
作者
Chung-Lieh Hung,Yen‐Wen Wu,Ling Kuo,Kuo‐Tzu Sung,Heng-Hsu Lin,Wei‐Ting Chang,Chia‐Hsiu Chang,Chih‐Hung Lai,Chun‐Yao Huang,Chun-Li Wang,Chih‐Chan Lin,Jyh‐Ming Jimmy Juang,Po-Sheng Chen,Chengshu Wang,Hao‐Chih Chang,Chun‐Yuan Chu,Wen-Hwa Wang,Hsinyu Tseng,Yung‐Ta Kao,Tzung‐Dau Wang
出处
期刊:PubMed [National Institutes of Health]
卷期号:40 (5): 544-568
标识
DOI:10.6515/acs.202409_40(5).20240731a
摘要

As an X-linked inherited lysosomal storage disease that is caused by α-galactosidase A gene variants resulting in progressive accumulation of pathogenic glycosphingolipid (Gb3) accumulation in multiple tissues and organs, Fabry disease (FD) can be classified into classic or late-onset phenotypes. In classic phenotype patients, α-galactosidase A activity is absent or severely reduced, resulting in a more progressive disease course with multi-systemic involvement. Conversely, late-onset phenotype, often with missense variants (e.g., IVS4+919G>A) in Taiwan, may present with a more chronic clinical course with predominant cardiac involvement (cardiac subtype), as they tend to have residual enzyme activity, remaining asymptomatic or clinically silent during childhood and adolescence. In either form, cardiac hypertrophy remains the most common feature of cardiac involvement, potentially leading to myocardial fibrosis, arrhythmias, and heart failure. Diagnosis is established through α-galactosidase enzyme activity assessment or biomarker analyisis (globotriaosylsphingosine, Lyso-Gb3), advanced imaging modalities (echocardiography and cardiac magnetic resonance imaging), and genotyping to differentiate FD from other cardiomyopathy. Successful therapeutic response relies on early recognition and by disease awareness from typical features in classic phenotype and cardiac red flags in cardiac variants for timely therapeutic interventions. Recent advances in pharmacological approach including enzyme replacement therapy (agalsidase alfa or beta), oral chaperone therapy (migalastat), and substrate reduction therapy (venglustat) aim to prevent from irreversible organ damage. Genotype- and gender-based monitoring of treatment effects through biomarker (Lyso-Gb3), renal assessment, and cardiac responses using advanced imaging modalities are key steps to optimizing patient care in FD.
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