Newborn screening for Fabry disease in Taiwan reveals a high incidence of the later‐onset GLA mutation c.936+919G>A (IVS4+919G>A)

Fabry disease (α‐galactosidase A (α‐Gal A, GLA) deficiency) is a panethnic inborn error of glycosphingolipid metabolism. Because optimal therapeutic outcomes depend on early intervention, a pilot program was designed to assess newborn screening for this disease in 171,977 consecutive Taiwanese newborns by measuring their dry blood spot (DBS) α‐Gal A activities and β‐galactosidase/α‐Gal A ratios. Of the 90,288 male screenees, 638 (0.7%) had DBS α‐Gal A activity <30% of normal mean and/or activity ratios >10. A second DBS assay reduced these to 91 (0.1%). Of these, 11 (including twins) had <5% (Group‐A), 64 had 5–30% (Group‐B), and 11 had >30% (Group‐C) of mean normal leukocyte α‐Gal A activity. All 11 Group‐A, 61 Group‐B, and 1 Group‐C males had GLA gene mutations. Surprisingly, 86% had the later‐onset cryptic splice mutation c.936+919G>A (also called IVS4+919G>A). In contrast, screening 81,689 females detected two heterozygotes. The novel mutations were expressed in vitro, predicting their classical or later‐onset phenotypes. Newborn screening identified a surprisingly high frequency of Taiwanese males with Fabry disease (∼1 in 1,250), 86% having the IVS4+919G>A mutation previously found in later‐onset cardiac phenotype patients. Further studies of the IVS4 later‐onset phenotype will determine its natural history and optimal timing for therapeutic intervention. Hum Mutat 30:1–9, 2009. © 2009 Wiley‐Liss, Inc.

[1]  R. Mignani,et al.  Unbalanced GLA mRNAs ratio quantified by real-time PCR in Fabry patients' fibroblasts results in Fabry disease , 2008, European Journal of Human Genetics.

[2]  J. Yagüe,et al.  Prevalence of Fabry Disease in a Cohort of 508 Unrelated Patients With Hypertrophic Cardiomyopathy , 2007 .

[3]  R. Finkel,et al.  Agalsidase-Beta Therapy for Advanced Fabry Disease , 2007, Annals of Internal Medicine.

[4]  D. Germain Fabry disease: the need to stratify patient populations to better understand the outcome of enzyme replacement therapy. , 2007, Clinical therapeutics.

[5]  S. Brodie,et al.  Fabry disease: Guidelines for the evaluation and management of multi-organ system involvement , 2006, Genetics in Medicine.

[6]  R. Desnick,et al.  High incidence of later-onset fabry disease revealed by newborn screening. , 2006, American journal of human genetics.

[7]  A. Roscher,et al.  Disease manifestations and X inactivation in heterozygous females with Fabry disease. , 2006 .

[8]  R. Desnick,et al.  Fabry disease: Identification of 50 novel α-galactosidase A mutations causing the classic phenotype and three-dimensional structural analysis of 29 missense mutations , 2006, Human Genomics.

[9]  P. Bauer,et al.  Prevalence of Fabry disease in patients with cryptogenic stroke: a prospective study , 2005, The Lancet.

[10]  K. Tomita,et al.  Identification of Fabry's disease by the screening of alpha-galactosidase A activity in male and female hemodialysis patients. , 2005, Clinical nephrology.

[11]  Z. Lukacs,et al.  The ratio of α-galactosidase to β-glucuronidase activities in dried blood for the identification of female Fabry disease patients , 2005, Journal of Inherited Metabolic Disease.

[12]  K. Mills,et al.  Non-invasive screening method for Fabry disease by measuring globotriaosylceramide in whole urine samples using tandem mass spectrometry. , 2005, Molecular genetics and metabolism.

[13]  M. Elleder,et al.  Relationship between X-inactivation and clinical involvement in Fabry heterozygotes. Eleven novel mutations in the α-galactosidase A gene in the Czech and Slovak population , 2005, Journal of Molecular Medicine.

[14]  Z. Lukacs,et al.  The ratio of alpha-galactosidase to beta-glucuronidase activities in dried blood for the identification of female Fabry disease patients. , 2005, Journal of inherited metabolic disease.

[15]  R. Desnick,et al.  Long-term safety and efficacy of enzyme replacement therapy for Fabry disease. , 2004, American journal of human genetics.

[16]  R. Kramar,et al.  J Am Soc Nephrol 15: 1323–1329, 2004 Results of a Nationwide Screening for Anderson-Fabry Disease among Dialysis Patients , 2022 .

[17]  R. Brady,et al.  Fabry disease in childhood. , 2004, The Journal of pediatrics.

[18]  Yoshiyuki Suzuki,et al.  Point mutations in the upstream region of the α-galactosidase A gene exon 6 in an atypical variant of Fabry disease , 1992, Human Genetics.

[19]  R. Desnick,et al.  Fabry disease: Characterization of α‐galactosidase A double mutations and the D313Y plasma enzyme pseudodeficiency allele , 2003, Human mutation.

[20]  D. Pennell,et al.  Gadolinium enhanced cardiovascular magnetic resonance in Anderson-Fabry disease. Evidence for a disease specific abnormality of the myocardial interstitium. , 2003, European heart journal.

[21]  Oliver Turschner,et al.  Improvement of Cardiac Function During Enzyme Replacement Therapy in Patients With Fabry Disease: A Prospective Strain Rate Imaging Study , 2003, Circulation.

[22]  C. Eng,et al.  Fabry disease: detection of undiagnosed hemodialysis patients and identification of a "renal variant" phenotype. , 2003, Kidney international.

[23]  P. Stenson,et al.  Human Gene Mutation Database (HGMD®): 2003 update , 2003, Human mutation.

[24]  S. Packman,et al.  Fabry Disease, an Under-Recognized Multisystemic Disorder: Expert Recommendations for Diagnosis, Management, and Enzyme Replacement Therapy , 2003, Annals of Internal Medicine.

[25]  S. Packman,et al.  Fabry Disease , an UnderRecognized Multisystemic Disorder : Expert Recommendations for Diagnosis , Management , and Enzyme Replacement Therapy , 2003 .

[26]  R. Desnick,et al.  Alternative splicing in the alpha-galactosidase A gene: increased exon inclusion results in the Fabry cardiac phenotype. , 2002, American journal of human genetics.

[27]  P. Elliott,et al.  Prevalence of Anderson-Fabry Disease in Male Patients With Late Onset Hypertrophic Cardiomyopathy , 2002, Circulation.

[28]  C. Eng,et al.  Safety and efficacy of recombinant human alpha-galactosidase A replacement therapy in Fabry's disease. , 2001, The New England journal of medicine.

[29]  N. Chamoles,et al.  Fabry disease: enzymatic diagnosis in dried blood spots on filter paper. , 2001, Clinica chimica acta; international journal of clinical chemistry.

[30]  R. Desnick α-Galactosidase A deficiency. Fabry disease , 2001 .

[31]  P. Meikle,et al.  Prevalence of lysosomal storage disorders. , 1999, JAMA.

[32]  R. Schwartz An atypical variant of Fabry's disease in men with left ventricular hypertrophy , 1996 .

[33]  C. Eng,et al.  An atypical variant of Fabry's disease with manifestations confined to the myocardium. , 1991, The New England journal of medicine.

[34]  J. Scheerer,et al.  Differential assay for lysosomal alpha-galactosidases in human tissues and its application to Fabry's disease. , 1981, Clinica chimica acta; international journal of clinical chemistry.