Fabry disease caused by the GLA p.Phe113Leu (p.F113L) variant: Natural history in males

João P Oliveira; Albina Nowak; Frédéric Barbey; Márcia Torres; José P Nunes; Fernando Teixeira-E-Costa; Fernanda Carvalho; Susana Sampaio; Isabel Tavares; Odete Pereira; Ana L Soares; Cátia Carmona; Maria-Teresa Cardoso; Iulia E Jurca-Simina; Marco Spada; Susana Ferreira; Dominique P Germain

doi:10.1016/j.ejmg.2019.103703

Fabry disease caused by the GLA p.Phe113Leu (p.F113L) variant: Natural history in males

Eur J Med Genet. 2020 Feb;63(2):103703. doi: 10.1016/j.ejmg.2019.103703. Epub 2019 Jun 11.

Authors

João P Oliveira¹, Albina Nowak², Frédéric Barbey³, Márcia Torres⁴, José P Nunes⁵, Fernando Teixeira-E-Costa⁶, Fernanda Carvalho⁷, Susana Sampaio⁸, Isabel Tavares⁹, Odete Pereira⁸, Ana L Soares¹⁰, Cátia Carmona¹¹, Maria-Teresa Cardoso¹², Iulia E Jurca-Simina¹³, Marco Spada¹⁴, Susana Ferreira¹⁵, Dominique P Germain¹³

Affiliations

¹ Service of Medical Genetics, São João University Hospital Center, 4200-319, Porto, Portugal; Unit of Genetics, Department of Pathology, Faculty of Medicine, University of Porto, 4200-319, Porto, Portugal; Institute for Research and Innovation in Health [Instituto de Investigação e Inovação em Saúde] - I3S, University of Porto, 4150-180, Porto, Portugal. Electronic address: jpo@med.up.pt.
² Department of Endocrinology and Clinical Nutrition, University of Zurich, 8091, Zürich, Switzerland.
³ Division of Genetic Medicine, Lausanne University Hospital, Lausanne, Switzerland.
⁴ Service of Cardiology, Hospital of Santo Tirso, 4780-371, Santo Tirso, Portugal.
⁵ Service of Cardiology, São João University Hospital Center, 4200-319, Porto, Portugal.
⁶ Service of Nephrology, Garcia de Orta Hospital, 2805-267, Almada, Portugal.
⁷ Unit of Renal Pathology, Service of Nephrology, Curry Cabral Hospital, 1069-166, Lisbon, Portugal.
⁸ Service of Nephrology, São João University Hospital Center, 4200-319, Porto, Portugal.
⁹ Service of Nephrology, São João University Hospital Center, 4200-319, Porto, Portugal; Uninefro, Santo Tirso Hemodialysis Clinic, 4780-383, Santo Tirso, Portugal.
¹⁰ Vil'Alva Family Health Center, 4780-484, Santo Tirso, Portugal.
¹¹ Service of Neurology, Garcia de Orta Hospital, 2805-267, Almada, Portugal.
¹² Clinic for Adult Metabolic Diseases, Inherited Metabolic Diseases Reference Center, São João University Hospital Center, 4200-319, Porto, Portugal.
¹³ Division of Medical Genetics, University of Versailles / Paris-Saclay University, 78180, Montigny, France.
¹⁴ Clinic for Metabolic Diseases, Department of Pediatric Sciences, Regina Margherita Hospital, 10126, Turin, Italy.
¹⁵ Unit of Genetics, Department of Pathology, Faculty of Medicine, University of Porto, 4200-319, Porto, Portugal; Institute for Research and Innovation in Health [Instituto de Investigação e Inovação em Saúde] - I3S, University of Porto, 4150-180, Porto, Portugal.

PMID: 31200018
DOI: 10.1016/j.ejmg.2019.103703

Abstract

Background, aims and methods: The α-galactosidase gene (GLA) c.337T>C/p.Phe113Leu variant was originally described in patients with late-onset cardiac forms of Fabry disease (FD), who had residual α-galactosidase activity. It has since emerged as the most commonly reported GLA variant in Portuguese subjects diagnosed with FD but is also prevalent in the Italian population, where two boys carrying the GLA Leu113 allele were identified in a large-scale newborn screening program, the variant allele segregating in both cases with the same surrounding haplotype. To further delineate the genotype-phenotype correlations of this GLA variant, we have reviewed the natural history and clinical phenotypes of 11 symptomatic Portuguese males, from 10 unrelated families originating from several different areas in mainland Portugal and Madeira Island, who were diagnosed with FD associated with the GLA Leu113 allele in a diversity of clinical and screening settings. Nine of the patients were the probands of their respective families. To test whether the GLA Leu113 allele inherited by the 10 Portuguese and the two Italian families resulted from independent mutational events, we have additionally performed a haplotype analysis with 5 highly polymorphic, closely linked microsatellite markers surrounding the GLA gene.

Results and conclusions: Hemizygosity for the GLA Leu113 variant allele is associated with a late-onset form of FD, invariably presenting with severe cardiac involvement. Clinically relevant cerebrovascular and kidney involvement may also occur in some patients but the pathogenic relationship between the incomplete α-galactosidase deficiency and the risks of stroke and of chronic kidney disease is not straightforward. The observation that the Leu113 allele segregated within the same GLA microsatellite haplotype in both the Portuguese and Italian families suggests its inheritance from a common ancestor.

Keywords: Alpha-galactosidase gene (GLA); Fabry disease; Haplotype; Microsatellite markers; p.Phe113Leu (p.F113L) pathogenic variant.

Publication types

Case Reports

MeSH terms

Adult
Aged
Alleles
Cardiovascular Diseases / complications
Cardiovascular Diseases / genetics
Cardiovascular Diseases / metabolism
Cerebrovascular Disorders / complications
Cerebrovascular Disorders / genetics
Cerebrovascular Disorders / metabolism
Fabry Disease / complications
Fabry Disease / diagnosis*
Fabry Disease / diagnostic imaging
Fabry Disease / genetics*
Genetic Association Studies
Genotype
Haplotypes
Humans
Italy / epidemiology
Male
Microsatellite Repeats / genetics
Middle Aged
Mutation
Myocytes, Cardiac / pathology
Myocytes, Cardiac / ultrastructure
Phenotype
Portugal / epidemiology
Renal Insufficiency, Chronic / complications
Renal Insufficiency, Chronic / genetics
Renal Insufficiency, Chronic / metabolism
Risk Factors
alpha-Galactosidase / genetics*
alpha-Galactosidase / metabolism*

Substances

alpha-Galactosidase