Fabry Nephropathy: An Evidence-Based Narrative Review

Overview

Journal Kidney Blood Press Res

Publisher Karger

Specialty Nephrology

Date 2018 Mar 21

PMID 29558749

Citations 24

Authors

Maria Del Pino

Amado Andres

Ana Avila Bernabeu

Joaquin de Juan-Rivera

Elvira Fernandez

Juan de Dios Garcia Diaz

Domingo Hernandez

Jose Luno

Isabel Martinez Fernandez

Jose Paniagua

Manuel Posada de la Paz

Jose Carlos Rodriguez-Perez

Rafael Santamaria

Roser Torra

Joan Torras Ambros

Pedro Vidau

Josep-Vicent Torregrosa

Affiliations

Soon will be listed here.

Abstract

Fabry disease (FD) is a rare, X-linked disorder caused by mutations in the GLA gene encoding the enzyme α-galactosidase A. Complete or partial deficiency in this enzyme leads to intracellular accumulation of globotriaosylceramide (Gb3) and other glycosphingolipids in many cell types throughout the body, including the kidney. Progressive accumulation of Gb3 in podocytes, endothelial cells, epithelial cells, and tubular cells contribute to the renal symptoms of FD, which manifest as proteinuria and reduced glomerular filtration rate leading to renal insufficiency. A correct diagnosis of FD, although challenging, has considerable implications regarding treatment, management, and counseling. The diagnosis may be confirmed by demonstrating the enzyme deficiency in males and by identifying the specific GLA gene mutation in male and female patients. Treatment with enzyme replacement therapy, as part of the therapeutic strategy to prevent complications of the disease, may be beneficial in stabilizing renal function or slowing its decline, particularly in the early stages of the disease. Emergent treatments for FD include the recently approved chaperone molecule migalastat for patients with amenable mutations. The objective of this report is to provide an updated overview on Fabry nephropathy, with a focus on the most relevant aspects of its epidemiology, diagnosis, pathophysiology, and treatment options.

Citing Articles

A kaleidoscopic view of extracellular vesicles in lysosomal storage disorders.

Hegeman C, de Jong O, Lorenowicz M Extracell Vesicles Circ Nucl Acids. 2024; 3(4):393-421.

PMID: 39697359 PMC: 11651879. DOI: 10.20517/evcna.2022.41.

Glycosphingolipids and their impact on platelet activity in a murine model of fabry disease.

Kanack A, Prodoehl E, Ishihara-Aoki M, Aoki K, Dahms N Sci Rep. 2024; 14(1):29488.

PMID: 39604471 PMC: 11603304. DOI: 10.1038/s41598-024-80633-6.

Genome-wide expression analysis in a Fabry disease human podocyte cell line.

Snanoudj S, Derambure C, Zhang C, Yen N, Lesueur C, Coutant S Heliyon. 2024; 10(14):e34357.

PMID: 39100494 PMC: 11295972. DOI: 10.1016/j.heliyon.2024.e34357.

The role of podocyte injury in the pathogenesis of Fabry disease nephropathy.

Monte Neto J, Mastroianni Kirsztajn G J Bras Nefrol. 2024; 46(3):e20240035.

PMID: 39058283 PMC: 11287863. DOI: 10.1590/2175-8239-JBN-2024-0035en.

Zebras Exist, Too!.

Antunes M Arq Bras Cardiol. 2024; 121(1):e20230834.

PMID: 38477765 PMC: 11081203. DOI: 10.36660/abc.20230834.