2024 法布里病 TSOC 专家共识更新。

IF 1.8 4区 医学 Q3 CARDIAC & CARDIOVASCULAR SYSTEMS
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, Chao-Yung Wang, Hao-Chih Chang, Chun-Yuan Chu, Wen-Hwa Wang, Hsinyu Tseng, Yung-Ta Kao, Tzung-Dau Wang, Wen-Chung Yu, Wen-Jone Chen
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引用次数: 0

摘要

法布里病(FD)是由α-半乳糖苷酶A基因变异引起的一种X连锁遗传性溶酶体贮积病,会导致致病性糖磷脂(Gb3)在多个组织和器官中进行性积累。在典型表型患者中,α-半乳糖苷酶 A 的活性缺失或严重降低,导致多系统受累的进展性疾病过程。相反,晚发表型(通常是台湾地区的错义变异型,如 IVS4+919G>A)患者的临床表现可能更为慢性,主要累及心脏(心脏亚型),因为他们往往有残余的酶活性,在儿童和青少年时期没有症状或临床症状不明显。无论哪种类型,心脏肥大仍是心脏受累的最常见特征,可能导致心肌纤维化、心律失常和心力衰竭。诊断可通过α-半乳糖苷酶酶活性评估或生物标志物分析(球蛋白葡萄糖苷,Lyso-Gb3)、先进的成像模式(超声心动图和心脏磁共振成像)以及基因分型来区分FD和其他心肌病。成功的治疗反应有赖于早期识别,并从典型表型的典型特征和心脏变异的心脏信号中了解疾病,以便及时采取治疗干预措施。药理学方法的最新进展包括酶替代疗法(阿加西酶 alfa 或 beta)、口服伴侣疗法(米加司他)和底物减少疗法(文格鲁他),目的是防止不可逆的器官损伤。通过生物标志物(溶菌酶-Gb3)、肾脏评估和使用先进成像模式的心脏反应来监测基于基因型和性别的治疗效果,是优化 FD 患者护理的关键步骤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
2024 Update of the TSOC Expert Consensus of Fabry Disease.

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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来源期刊
Acta Cardiologica Sinica
Acta Cardiologica Sinica 医学-心血管系统
CiteScore
2.90
自引率
15.80%
发文量
144
审稿时长
>12 weeks
期刊介绍: Acta Cardiologica Sinica welcomes all the papers in the fields related to cardiovascular medicine including basic research, vascular biology, clinical pharmacology, clinical trial, critical care medicine, coronary artery disease, interventional cardiology, arrythmia and electrophysiology, atherosclerosis, hypertension, cardiomyopathy and heart failure, valvular and structure cardiac disease, pediatric cardiology, cardiovascular surgery, and so on. We received papers from more than 20 countries and areas of the world. Currently, 40% of the papers were submitted to Acta Cardiologica Sinica from Taiwan, 20% from China, and 20% from the other countries and areas in the world. The acceptance rate for publication was around 50% in general.
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