High Incidence of the Cardiac Variant of Fabry Disease Revealed by Newborn Screening in the Taiwan Chinese Population

Overview

Journal Circ Cardiovasc Genet

Specialties Cardiology & Vascular Diseases
Genetics

Date 2009 Dec 25

PMID 20031620

Citations 112

Authors

Hsiang-Yu Lin

Kah-Wai Chong

Ju-Hui Hsu

Hsiao-Chi Yu

Chun-Che Shih

Cheng-Hung Huang

Shing-Jong Lin

Chen-Huan Chen

Chuan-Chi Chiang

Huey-Jane Ho

Pi-Chang Lee

Chuan-Hong Kao

Kang-Hsiang Cheng

Chuen Hsueh

Dau-Ming Niu

Affiliations

Soon will be listed here.

Abstract

Background: Fabry disease is a treatable lysosomal storage disorder, which is often misdiagnosed or belatedly diagnosed.

Methods And Results: To determine the disease incidence in the Taiwan Chinese population, a Fabry disease newborn screening study was initiated. A total of 110 027 newborns were screened by assaying the alpha-galactosidase A (alpha-Gal A) activity using dry blood spots. Low plasma alpha-Gal A activity and presence of a Fabry mutation was demonstrated in 45 neonates (3 females). Eight different mutations were identified, including 3 known missense mutations (R112H, A143T, and R356W), 4 novel missense mutations (G104V, M296L, G360C, and K391T), and one known intronic mutation (IVS4+919G-->A). The IVS4+919G-->A mutation was most common (82% of patients). A total of 20 maternal grandparents of infants harboring this intronic mutation were evaluated by echocardiography, mutation analysis and alpha-Gal A activity assay. The intronic mutation was found in 9 grandfathers and 11 grandmothers. Of these grandparents, 3 grandfathers (33%) but none of the grandmothers had hypertrophic cardiomyopathy. Additionally, 16 males who had been diagnosed with idiopathic hypertrophic cardiomyopathy were screened by mutation analysis and alpha-Gal A activity; 4 (25%) showed deficient plasma alpha-Gal A activity in combination with the intronic mutation.

Conclusions: We found an unexpected high prevalence of the cardiac variant Fabry mutation IVS4+919G-->A among both newborns (approximately 1 in 1600 males) and patients with idiopathic hypertrophic cardiomyopathy in the Taiwan Chinese population. The early identification of undiagnosed patients allows timely therapeutic intervention providing a better clinical outcome.

Citing Articles

Decreased trabecular bone score in patients affected by Fabry disease.

Varaldo E, Giannone B, Viglino F, Settanni F, Bioletto F, Barale M J Endocrinol Invest. 2024; 48(1):121-130.

PMID: 39361238 PMC: 11729064. DOI: 10.1007/s40618-024-02427-x.

2024 Update of the TSOC Expert Consensus of Fabry Disease.

Hung C, Wu Y, Kuo L, Sung K, Lin H, Chang W Acta Cardiol Sin. 2024; 40(5):544-568.

PMID: 39308653 PMC: 11413953. DOI: 10.6515/ACS.202409_40(5).20240731A.

Screening for Fabry disease in patients with left ventricular hypertrophy in China: A multicentre and prospective study.

Lin Z, Zhang X, Liu Y, Miao D, Zhang H, Zhang T ESC Heart Fail. 2024; 11(6):4381-4389.

PMID: 39225306 PMC: 11631229. DOI: 10.1002/ehf2.15065.

Identification of a novel nonsense mutation in α-galactosidase A that causes Fabry disease in a Chinese family.

Peng Y, Pan M, Wang Y, Shen Z, Xu J, Xiong F Ren Fail. 2024; 46(2):2362391.

PMID: 38847497 PMC: 11164125. DOI: 10.1080/0886022X.2024.2362391.

A Deep Learning Approach to Classify Fabry Cardiomyopathy from Hypertrophic Cardiomyopathy Using Cine Imaging on Cardiac Magnetic Resonance.

Chen W, Kuo L, Lin Y, Yu W, Tseng C, Lin Y Int J Biomed Imaging. 2024; 2024:6114826.

PMID: 38706878 PMC: 11068448. DOI: 10.1155/2024/6114826.