Generalized Glycogen Storage and Cardiomegaly in a Knockout Mouse Model of Pompe Disease

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 1998 Feb 28

PMID 9384603

Citations 45

Authors

A G Bijvoet

E H Van de Kamp

M A Kroos

J H Ding

B Z Yang

P Visser

C E Bakker

M P Verbeet

B A Oostra

A J Reuser

A T van der Ploeg

Affiliations

Soon will be listed here.

Abstract

Glycogen storage disease type II (GSDII; Pompe disease), caused by inherited deficiency of acid alpha-glucosidase, is a lysosomal disorder affecting heart and skeletal muscles. A mouse model of this disease was obtained by targeted disruption of the murine acid alpha-glucosidase gene (Gaa) in embryonic stem cells. Homozygous knockout mice (Gaa -/-) lack Gaa mRNA and have a virtually complete acid alpha-glucosidase deficiency. Glycogen-containing lysosomes are detected soon after birth in liver, heart and skeletal muscle cells. By 13 weeks of age, large focal deposits of glycogen have formed. Vacuolar spaces stain positive for acid phosphatase as a sign of lysosomal pathology. Both male and female knockout mice are fertile and can be intercrossed to produce progeny. The first born knockout mice are at present 9 months old. Overt clinical symptoms are still absent, but the heart is typically enlarged and the electrocardiogram is abnormal. The mouse model will help greatly to understand the pathogenic mechanism of GSDII and is a valuable instrument to explore the efficacy of different therapeutic interventions.

Citing Articles

Failure of Autophagy in Pompe Disease.

Do H, Meena N, Raben N Biomolecules. 2024; 14(5).

PMID: 38785980 PMC: 11118179. DOI: 10.3390/biom14050573.

Spatial metabolomics reveals glycogen as an actionable target for pulmonary fibrosis.

Conroy L, Clarke H, Allison D, Valenca S, Sun Q, Hawkinson T Nat Commun. 2023; 14(1):2759.

PMID: 37179348 PMC: 10182559. DOI: 10.1038/s41467-023-38437-1.

CRISPR-mediated generation and characterization of a Gaa homozygous c.1935C>A (p.D645E) Pompe disease knock-in mouse model recapitulating human infantile onset-Pompe disease.

Kan S, Huang J, Harb J, Rha A, Dalton N, Christensen C Sci Rep. 2022; 12(1):21576.

PMID: 36517654 PMC: 9751086. DOI: 10.1038/s41598-022-25914-8.

IGF2-tagging of GAA promotes full correction of murine Pompe disease at a clinically relevant dosage of lentiviral gene therapy.

Liang Q, Catalano F, Vlaar E, Pijnenburg J, Stok M, van Helsdingen Y Mol Ther Methods Clin Dev. 2022; 27:109-130.

PMID: 36284764 PMC: 9573825. DOI: 10.1016/j.omtm.2022.09.010.

Lysosomal glycogen accumulation in Pompe disease results in disturbed cytoplasmic glycogen metabolism.

Canibano-Fraile R, Harlaar L, Dos Santos C, Hoogeveen-Westerveld M, Demmers J, Snijders T J Inherit Metab Dis. 2022; 46(1):101-115.

PMID: 36111639 PMC: 10092494. DOI: 10.1002/jimd.12560.