New insights into therapeutic options for Pompe disease

Emmanuel Richard; Gaëlle Douillard-Guilloux; Catherine Caillaud

doi:10.1002/iub.529

New insights into therapeutic options for Pompe disease

IUBMB Life. 2011 Nov;63(11):979-86. doi: 10.1002/iub.529. Epub 2011 Oct 14.

Authors

Emmanuel Richard¹, Gaëlle Douillard-Guilloux, Catherine Caillaud

Affiliation

¹ Université de Bordeaux, Biothérapies des Maladies Génétiques et Cancers, U1035, F-33000 Bordeaux, France. Emmanuel.Richard@u-bordeaux2.fr

PMID: 22002928
DOI: 10.1002/iub.529

Abstract

Glycogen storage disease type II or Pompe disease (GSD II, MIM 232300) is a rare inherited metabolic myopathy caused by a deficiency of lysosomal acid α-glucosidase or acid maltase (GAA; EC 3.2.1.20), resulting in a massive lysosomal glycogen accumulation in cardiac and skeletal muscles. Affected individuals exhibit either severe hypotonia associated with hypertrophic cardiomyopathy (infantile forms) or progressive muscle weakness (late-onset forms). Even if enzyme replacement therapy has recently become a standard treatment, it suffers from several limitations. This review will present the main results of enzyme replacement therapy and the recent findings concerning alternative treatments for Pompe disease, such as gene therapy, enzyme enhancement therapy, and substrate reduction therapy.

Publication types

Review

MeSH terms

Animals
Drug Carriers
Enzyme Activators / therapeutic use
Enzyme Replacement Therapy / adverse effects
Enzyme Replacement Therapy / methods
Genetic Therapy
Glycogen Storage Disease Type II / enzymology
Glycogen Storage Disease Type II / genetics
Glycogen Storage Disease Type II / therapy*
Humans
Immune Tolerance
Liver / drug effects
Liver / physiopathology
Muscles / drug effects
Muscles / physiopathology
alpha-Glucosidases / genetics
alpha-Glucosidases / immunology
alpha-Glucosidases / therapeutic use

Substances

Drug Carriers
Enzyme Activators
GAA protein, human
alpha-Glucosidases