A renal variant of Fabry disease: A case with a novel Gal A hemizygote mutation

Jorge H. Mukdsi; Silvina Gutiérrez; Belén Barrón; Pablo Novoa; Segundo Fernández; Ana B de Diller; Alicia I. Torres; Richard N Formica Jr.; Marcelo Orías

doi:10.5812/nephropathol.8123

Journal of Nephropathology (Oct 2012)

A renal variant of Fabry disease: A case with a novel Gal A hemizygote mutation

Jorge H. Mukdsi,
Silvina Gutiérrez,
Belén Barrón,
Pablo Novoa,
Segundo Fernández,
Ana B de Diller,
Alicia I. Torres,
Richard N Formica Jr.,
Marcelo Orías

Affiliations

Jorge H. Mukdsi: Centro de Microscopía Electrónica, Facultad de Ciencias Médicas, Universidad Nacional de Córdoba, and Haya de la Torre esquina Enrique Barros, Ciudad Universitaria, Córdoba, Argentina.
Silvina Gutiérrez: Centro de Microscopía Electrónica, Facultad de Ciencias Médicas, Universidad Nacional de Córdoba, and Haya de la Torre esquina Enrique Barros, Ciudad Universitaria, Córdoba, Argentina.
Belén Barrón: Centro de Microscopía Electrónica, Facultad de Ciencias Médicas, Universidad Nacional de Córdoba, and Haya de la Torre esquina Enrique Barros, Ciudad Universitaria, Córdoba, Argentina.
Pablo Novoa: Servicio de Nefrología, Sanatorio Allende, Bernardo de Irigoyen 384, Córdoba, Argentina.
Segundo Fernández: CIPERCA Centro de diálisis, Catamarca, Argentina.
Ana B de Diller: Servicio de Patología-Hospital Privado, Naciones Unidad 346, Córdoba, Argentina.
Alicia I. Torres: Centro de Microscopía Electrónica, Facultad de Ciencias Médicas, Universidad Nacional de Córdoba, and Haya de la Torre esquina Enrique Barros, Ciudad Universitaria, Córdoba, Argentina.
Richard N Formica Jr.: Department of Medicine, Section of Nephrology, Yale University School of Medicine, USA.
Marcelo Orías: Servicio de Nefrología, Sanatorio Allende, Bernardo de Irigoyen 384, Córdoba, Argentina.

DOI: https://doi.org/10.5812/nephropathol.8123
Journal volume & issue: Vol. 1, no. 3
pp. 194 – 197

Abstract

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Background: Fabry disease is caused by an X-linked recessive inborn error of glycosphingolipid metabolism with deficient activity of a lysosomal enzyme, alpha-galactosidase A (α-GalA). Case Presentation: A 46 year-old man with progressive kidney disease showed on kidney biopsy electron microscopic evidence of Fabry disease. The patient had no systemic manifestations of Fabry disease, despite residual α-GalA activity, therefore genetic testing was done by direct DNA sequencing, demonstrating a new GAL A gene mutation (C174G-exon 3). After three years of enzyme replacement therapy (agalsidase beta) treatment, a second biopsy was done. Although there was demonstrable clearance of intracellular inclusions, remarkable podocyte activation was evident. Conclusions: This report represents an unusual renal variant of Fabry disease and provides histologic data on long-term follow up after enzyme replacement therapy.

Published in Journal of Nephropathology

ISSN: 2251-8363 (Print); 2251-8819 (Online)
Publisher: Society of Diabetic Nephropathy Prevention
Country of publisher: Iran, Islamic Republic of
LCC subjects: Medicine: Pathology; Medicine: Internal medicine; Medicine: Other systems of medicine
Website: https://nephropathol.com/

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