论文信息 - Newborn Screening for Fabry Disease: Current Status of Knowledge

Newborn Screening for Fabry Disease: Current Status of Knowledge

Fabry disease is an X-linked progressive lysosomal disorder, due to α-galactosidase A deficiency. Patients with a classic phenotype usually present in childhood as a multisystemic disease. Patients presenting with the later onset subtypes have cardiac, renal and neurological involvements in adulthood. Unfortunately, the diagnosis is often delayed until the organ damage is already irreversibly severe, making specific treatments less efficacious. For this reason, in the last two decades, newborn screening has been implemented to allow early diagnosis and treatment. This became possible with the application of the standard enzymology fluorometric method to dried blood spots. Then, high-throughput multiplexable assays, such as digital microfluidics and tandem mass spectrometry, were developed. Recently DNA-based methods have been applied to newborn screening in some countries. Using these methods, several newborn screening pilot studies and programs have been implemented worldwide. However, several concerns persist, and newborn screening for Fabry disease is still not universally accepted. In particular, enzyme-based methods miss a relevant number of affected females. Moreover, ethical issues are due to the large number of infants with later onset forms or variants of uncertain significance. Long term follow-up of individuals detected by newborn screening will improve our knowledge about the natural history of the disease, the phenotype prediction and the patients’ management, allowing a better evaluation of risks and benefits of the newborn screening for Fabry disease.

[1] C. Wanner,et al. An expert consensus on the recommendations for the use of biomarkers in Fabry disease. , 2023, Molecular genetics and metabolism.

[2] F. Pieruzzi,et al. An expert consensus on practical clinical recommendations and guidance for patients with classic Fabry disease. , 2022, Molecular genetics and metabolism.

[3] Amy C Yang,et al. Newborn screening for Fabry disease in Oregon: Approaching the iceberg of A143T and variants of uncertain significance , 2022, American journal of medical genetics. Part C, Seminars in medical genetics.

[4] Yan Yan,et al. Establishment of Cutoff Values for Newborn Screening of Six Lysosomal Storage Disorders by Tandem Mass Spectrometry , 2022, Frontiers in Pediatrics.

[5] A. Chakrapani,et al. A New Approach to Objectively Evaluate Inherited Metabolic Diseases for Inclusion on Newborn Screening Programmes , 2022, International journal of neonatal screening.

[6] A. Chakrapani,et al. Application of a Novel Algorithm for Expanding Newborn Screening for Inherited Metabolic Disorders across Europe , 2022, International journal of neonatal screening.

[7] D. Lacombe,et al. Challenging the traditional approach for interpreting genetic variants: Lessons from Fabry disease , 2021, Clinical genetics.

[8] L. Salviati,et al. Newborn Screening for Fabry Disease in Northeastern Italy: Results of Five Years of Experience , 2021, Biomolecules.

[9] E. Lisi,et al. Opinions of adults affected with later‐onset lysosomal storage diseases regarding newborn screening: A qualitative study , 2021, Journal of genetic counseling.

[10] F. Pieruzzi,et al. Multicenter evaluation of use of dried blood spot compared to conventional plasma in measurements of globotriaosylsphingosine (LysoGb3) concentration in 104 Fabry patients , 2021, Clinical chemistry and laboratory medicine.

[11] N. Chen,et al. The benefits and challenges of family genetic testing in rare genetic diseases—lessons from Fabry disease , 2021, Molecular genetics & genomic medicine.

[12] M. Artola,et al. Fabry Disease: Molecular Basis, Pathophysiology, Diagnostics and Potential Therapeutic Directions , 2021, Biomolecules.

[13] S. Revel-Vilk,et al. Value of Glucosylsphingosine (Lyso-Gb1) as a Biomarker in Gaucher Disease: A Systematic Literature Review , 2020, International journal of molecular sciences.

[14] C. Auray-Blais,et al. Globotriaosylsphingosine (lyso-Gb3) and analogues in plasma and urine of patients with Fabry disease and correlations with long-term treatment and genotypes in a nationwide female Danish cohort , 2020, Journal of Medical Genetics.

[15] P. Rinaldo,et al. A Comparative Effectiveness Study of Newborn Screening Methods for Four Lysosomal Storage Disorders , 2020, International journal of neonatal screening.

[16] M. Gelb,et al. Newborn screening for Morquio disease and other lysosomal storage diseases: results from the 8-plex assay for 70,000 newborns , 2020, Orphanet Journal of Rare Diseases.

[17] F. Endo,et al. Newborn screening for Fabry disease in the western region of Japan , 2020, Molecular genetics and metabolism reports.

[18] T. Cox,et al. Comment: Why are females with Fabry disease affected? , 2019, Molecular genetics and metabolism reports.

[19] O. Bodamer,et al. Early initiation of enzyme replacement therapy in classical Fabry disease normalizes biomarkers in clinically asymptomatic pediatric patients , 2019, Molecular genetics and metabolism reports.

[20] Kristine H. Schmitz. Vulnerable Child Syndrome , 2019, Pediatrics in Review.

[21] L. Salviati,et al. Implementation of Second-Tier Tests in Newborn Screening for Lysosomal Disorders in North Eastern Italy , 2019, International journal of neonatal screening.

[22] M. Plebani,et al. Plasma and dried blood spot lysosphingolipids for the diagnosis of different sphingolipidoses: a comparative study , 2019, Clinical chemistry and laboratory medicine.

[23] M. Gelb,et al. Newborn Screening for Lysosomal Storage Disorders: Methodologies for Measurement of Enzymatic Activities in Dried Blood Spots , 2018, International journal of neonatal screening.

[24] Y. Chien,et al. Performance of the Four-Plex Tandem Mass Spectrometry Lysosomal Storage Disease Newborn Screening Test: The Necessity of Adding a 2nd Tier Test for Pompe Disease , 2018, International journal of neonatal screening.

[25] F. Pieruzzi,et al. Mutations in the GLA Gene and LysoGb3: Is It Really Anderson-Fabry Disease? , 2018, International journal of molecular sciences.

[26] Sean M. Bailey,et al. The New York Pilot Newborn Screening Program for Lysosomal Storage Diseases: Report of the First 65,000 Infants , 2018, Genetics in Medicine.

[27] D. Millington,et al. Current State of the Art of Newborn Screening for Lysosomal Storage Disorders , 2018, International journal of neonatal screening.

[28] Michael H. Gelb,et al. Newborn Screening for Lysosomal Storage Diseases: Methodologies, Screen Positive Rates, Normalization of Datasets, Second-Tier Tests, and Post-Analysis Tools , 2018, International journal of neonatal screening.

[29] R. Giugliani,et al. Neonatal screening for four lysosomal storage diseases with a digital microfluidics platform: Initial results in Brazil , 2018, Genetics and molecular biology.

[30] R. Desnick,et al. Newborn screening for lysosomal storage disorders by tandem mass spectrometry in North East Italy , 2018, Journal of Inherited Metabolic Disease.

[31] J. Charrow,et al. Newborn Screening for Lysosomal Storage Disorders in Illinois: The Initial 15‐Month Experience , 2017, The Journal of pediatrics.

[32] D. Niu,et al. Fabry disease: Review and experience during newborn screening. , 2017, Trends in cardiovascular medicine.

[33] S. Hung,et al. Improvement in the sensitivity of newborn screening for Fabry disease among females through the use of a high-throughput and cost-effective method, DNA mass spectrometry , 2017, Journal of Human Genetics.

[34] O. López-Suárez,et al. Newborn screening for Fabry disease in the north-west of Spain , 2017, European Journal of Pediatrics.

[35] M. Gelb,et al. Comparison of tandem mass spectrometry to fluorimetry for newborn screening of LSDs , 2017, Molecular genetics and metabolism reports.

[36] D. Niu,et al. Functional and biological studies of α-galactosidase A variants with uncertain significance from newborn screening in Taiwan. , 2017, Molecular genetics and metabolism.

[37] J. Reyna-Figueroa,et al. Newborn screening for six lysosomal storage disorders in a cohort of Mexican patients: Three-year findings from a screening program in a closed Mexican health system. , 2017, Molecular genetics and metabolism.

[38] M. Gelb,et al. Newborn Screening for Lysosomal Storage Diseases: A Concise Review of the Literature on Screening Methods, Therapeutic Possibilities and Regional Programs , 2017, International journal of neonatal screening.

[39] Y. Chinen,et al. A new mutation found in newborn screening for Fabry disease evaluated by plasma globotriaosylsphingosine levels , 2017, Human Genome Variation.

[40] E. Biamino,et al. Metabolic progression to clinical phenotype in classic Fabry disease , 2017, Italian Journal of Pediatrics.

[41] Wen-Chung Yu,et al. Later Onset Fabry Disease, Cardiac Damage Progress in Silence: Experience With a Highly Prevalent Mutation. , 2016, Journal of the American College of Cardiology.

[42] O. Bodamer,et al. Newborn Screening for Lysosomal Storage Disorders , 2016, Journal of Pediatric Genetics.

[43] Dawn A. Laney,et al. Patients' perspectives on newborn screening for later-onset lysosomal storage diseases. , 2016, Molecular genetics and metabolism.

[44] D. Lockhart,et al. Treatment of Fabry's Disease with the Pharmacologic Chaperone Migalastat. , 2016, The New England journal of medicine.

[45] M. Gelb,et al. Pilot study of newborn screening for six lysosomal storage diseases using Tandem Mass Spectrometry , 2016, Molecular genetics and metabolism.

[46] J. Stypmann,et al. Alpha-Galactosidase A p.A143T, a non-Fabry disease-causing variant , 2016, Orphanet Journal of Rare Diseases.

[47] S. McCandless,et al. Newborn Screening for Lysosomal Storage Disorders: Views of Genetic Healthcare Providers , 2016, Journal of Genetic Counseling.

[48] R. Hopkin,et al. The management and treatment of children with Fabry disease: A United States-based perspective. , 2016, Molecular genetics and metabolism.

[49] A. Hagège,et al. X‐chromosome inactivation in female patients with Fabry disease , 2016, Clinical genetics.

[50] M. Gelb,et al. Tandem Mass Spectrometry Has a Larger Analytical Range than Fluorescence Assays of Lysosomal Enzymes: Application to Newborn Screening and Diagnosis of Mucopolysaccharidoses Types II, IVA, and VI. , 2015, Clinical chemistry.

[51] M. Rudnicki,et al. Recommendations for initiation and cessation of enzyme replacement therapy in patients with Fabry disease: the European Fabry Working Group consensus document , 2015, Orphanet Journal of Rare Diseases.

[52] M. Gelb,et al. Newborn screening for lysosomal storage diseases. , 2015, Clinical chemistry.

[53] R. Hopkin,et al. Fabry disease in infancy and early childhood: a systematic literature review , 2014, Genetics in Medicine.

[54] Piero Rinaldo,et al. Postanalytical tools improve performance of newborn screening by tandem mass spectrometry , 2014, Genetics in Medicine.

[55] F. Tsai,et al. Detecting multiple lysosomal storage diseases by tandem mass spectrometry--a national newborn screening program in Taiwan. , 2014, Clinica chimica acta; international journal of clinical chemistry.

[56] S. Tsai,et al. High-throughput detection of common sequence variations of Fabry disease in Taiwan using DNA mass spectrometry. , 2014, Molecular genetics and metabolism.

[57] Vijay Srinivasan,et al. Multiplex newborn screening for Pompe, Fabry, Hunter, Gaucher, and Hurler diseases using a digital microfluidic platform. , 2013, Clinica chimica acta; international journal of clinical chemistry.

[58] T. Shimada,et al. Newborn screening and diagnosis of mucopolysaccharidoses. , 2013, Molecular genetics and metabolism.

[59] M. Gelb,et al. Identification of infants at risk for developing Fabry, Pompe, or mucopolysaccharidosis-I from newborn blood spots by tandem mass spectrometry. , 2013, The Journal of pediatrics.

[60] C. Broeckhoven,et al. Phenotypical characterization of α-galactosidase A gene mutations identified in a large Fabry disease screening program in stroke in the young , 2013, Clinical Neurology and Neurosurgery.

[61] C. Hollak,et al. Fabry patients' experiences with the timing of diagnosis relevant for the discussion on newborn screening. , 2013, Molecular genetics and metabolism.

[62] K. Ihara,et al. Newborn screening for Fabry disease in Japan: prevalence and genotypes of Fabry disease in a pilot study , 2013, Journal of Human Genetics.

[63] Y. Eto,et al. No accumulation of globotriaosylceramide in the heart of a patient with the E66Q mutation in the α-galactosidase A gene. , 2012, Molecular genetics and metabolism.

[64] T. Beccari,et al. First pilot newborn screening for four lysosomal storage diseases in an Italian region: identification and analysis of a putative causative mutation in the GBA gene. , 2012, Clinica chimica acta; international journal of clinical chemistry.

[65] W. van Biesen,et al. Questioning the Pathogenic Role of the GLA p.Ala143Thr "Mutation" in Fabry Disease: Implications for Screening Studies and ERT. , 2012, JIMD reports.

[66] T. Kanekura,et al. Fabry disease: biochemical, pathological and structural studies of the α-galactosidase A with E66Q amino acid substitution. , 2012, Molecular genetics and metabolism.

[67] Jan-Gowth Chang,et al. The use of high resolution melting analysis to detect Fabry mutations in heterozygous females via dry bloodspots. , 2012, Clinica chimica acta; international journal of clinical chemistry.

[68] K. Lackner,et al. Quantification of the Fabry marker lysoGb3 in human plasma by tandem mass spectrometry. , 2012, Journal of chromatography. B, Analytical technologies in the biomedical and life sciences.

[69] Thomas P. Mechtler,et al. Neonatal screening for lysosomal storage disorders: feasibility and incidence from a nationwide study in Austria , 2012, The Lancet.

[70] V. Srinivasan,et al. Digital microfluidic platform for multiplexing enzyme assays: implications for lysosomal storage disease screening in newborns. , 2011, Clinical chemistry.

[71] Ramakrishna Sista,et al. Rapid, single-step assay for Hunter syndrome in dried blood spots using digital microfluidics. , 2011, Clinica chimica acta; international journal of clinical chemistry.

[72] P. Elliott,et al. Prevalence of Anderson–Fabry disease in patients with hypertrophic cardiomyopathy: the European Anderson–Fabry Disease Survey , 2011, Heart.

[73] A. Burlina,et al. Whole-blood alpha-D-galactosidase A activity for the identification of Fabry's patients. , 2011, Clinical biochemistry.

[74] M. Gelb,et al. Comparative triplex tandem mass spectrometry assays of lysosomal enzyme activities in dried blood spots using fast liquid chromatography: application to newborn screening of Pompe, Fabry, and Hurler diseases. , 2011, Analytical chemistry.

[75] M. Watson,et al. Lysosomal storage diseases: Diagnostic confirmation and management of presymptomatic individuals , 2011, Genetics in Medicine.

[76] M. Gelb,et al. A tandem mass spectrometry triplex assay for the detection of Fabry, Pompe, and mucopolysaccharidosis-I (Hurler). , 2010, Clinical chemistry.

[77] Shing‐Jong Lin,et al. High Incidence of the Cardiac Variant of Fabry Disease Revealed by Newborn Screening in the Taiwan Chinese Population , 2009, Circulation. Cardiovascular genetics.

[78] Y. Chien,et al. Newborn screening for Fabry disease in Taiwan reveals a high incidence of the later‐onset GLA mutation c.936+919G>A (IVS4+919G>A) , 2009, Human mutation.

[79] B. Brenner,et al. Nephropathy in Fabry disease: the importance of early diagnosis and testing in high-risk populations. , 2009, Nephrology, dialysis, transplantation : official publication of the European Dialysis and Transplant Association - European Renal Association.

[80] C. Hollak,et al. Enzyme activity for determination of presence of Fabry disease in women results in 40% false-negative results. , 2008, Journal of the American College of Cardiology.

[81] P. Fernhoff,et al. Diagnosis of Fabry Disease via Analysis of Family History , 2008, Journal of Genetic Counseling.

[82] S. Garman,et al. Structure–function relationships in α‐galactosidase A , 2007, Acta paediatrica.

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

[84] C. Hollak,et al. Screening for Fabry disease using whole blood spots fails to identify one-third of female carriers. , 2005, Clinica chimica acta; international journal of clinical chemistry.

[85] M. Gelb,et al. Direct multiplex assay of lysosomal enzymes in dried blood spots for newborn screening. , 2004, Clinical chemistry.

[86] P. Meikle,et al. Newborn Screening for Lysosomal Storage Disorders: Clinical Evaluation of a Two-Tier Strategy , 2004, Pediatrics.

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

[88] 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.

[89] N. Chamoles,et al. Hurler-like phenotype: enzymatic diagnosis in dried blood spots on filter paper. , 2001, Clinical chemistry.

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

[91] R. Schiffmann,et al. Infusion of α-galactosidase A reduces tissue globotriaosylceramide storage in patients with Fabry disease , 2000 .

[92] C. Eng,et al. Nature and frequency of mutations in the alpha-galactosidase A gene that cause Fabry disease. , 1993, American journal of human genetics.

[93] S. Tsuji. [Alpha-galactosidase A deficiency--Fabry's disease]. , 1988, Tanpakushitsu kakusan koso. Protein, nucleic acid, enzyme.

[94] A. Rolfs,et al. Newborn screening for lysosomal storage disorders in hungary. , 2012, JIMD reports.

[95] P. Luna,et al. [Fabry disease]. , 2009, Anais brasileiros de dermatologia.

[96] L. O. C. Aplan,et al. SAFETY AND EFFICACY OF RECOMBINANT HUMAN a -GALACTOSIDASE A REPLACEMENT THERAPY IN FABRY'S DISEASE , 2001 .