Galactosialidosis: Historic Aspects and Overview of Investigated and Emerging Treatment Options

Overview

Journal Expert Opin Orphan Drugs

Publisher Informa Healthcare

Date 2017 Jun 13

PMID 28603679

Citations 15

Authors

Ida Annunziata

Alessandra dAzzo

Affiliations

Soon will be listed here.

Abstract

Introduction: Galactosialidosis is a glycoprotein storage disease caused by mutations in the gene, encoding lysosomal protective protein/cathepsin A (PPCA). The enzyme's catalytic activity is distinct from its protective function towards β-galactosidase (β-GAL) and neuraminidase 1 (NEU1), with which PPCA forms a complex. In this configuration the two glycosidases acquire their full activity and stability in lysosomes. Deficiency of PPCA results in combined NEU1/β-GAL deficiency. Because of its low incidence, galactosialidosis is considered an orphan disorder with no therapy yet available.

Areas Covered: This review gives a historic overview on the discovery of PPCA, which defined galactosialidosis as a new clinical entity; the evidence for the existence of the PPCA/NEU1/β-GAL complex; the clinical forms of galactosialidosis and disease-causing mutations. mice have proven to be a suitable model to test different therapeutic approaches, paving the way for the development of clinical trials for patients with galactosialidosis.

Expert Opinion: Improved understanding of the molecular bases of disease has sparked renewed incentive from clinicians and scientists alike to develop therapies for rare conditions, like GS, and has increased the willingness of biotech companies to invest in the manufacturing of new therapeutics. Both ERT and gene therapy may become available to patients in the near future.

Citing Articles

Galactosialidosis: A Report of Three Cases Diagnosed With a Founder Genetic Mutation in the Bahraini Population.

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AAV-mediated gene therapy for sialidosis.

van de Vlekkert D, Hu H, Weesner J, Fremuth L, Brown S, Lu M Mol Ther. 2024; 32(7):2094-2112.

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Structure of the immunoregulatory sialidase NEU1.

Gorelik A, Illes K, Mazhab-Jafari M, Nagar B Sci Adv. 2023; 9(20):eadf8169.

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Facial features of lysosomal storage disorders.

DSouza A, Ryan E, Sidransky E Expert Rev Endocrinol Metab. 2022; 17(6):467-474.

PMID: 36384353 PMC: 9817214. DOI: 10.1080/17446651.2022.2144229.

AAV-mediated gene therapy for galactosialidosis: A long-term safety and efficacy study.

Hu H, Mosca R, Gomero E, van de Vlekkert D, Campos Y, Fremuth L Mol Ther Methods Clin Dev. 2021; 23:644-658.

PMID: 34901309 PMC: 8640647. DOI: 10.1016/j.omtm.2021.10.007.

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