BIOMAT Database Logo BIOMAT Database Logo

Severe course of glycogen storage disease type II (Pompe's disease) without development of cardiomegalia. 1986

K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz

Glycogen storage disease type II Pompe (GSD II) is a lysosomal storage disease caused by an inherited deficiency of acid alpha-glucosidase. In addition to the classical infantile form of GSD II, several clinical variants are known. We describe an infant with the classical course of the disease. Our patient differs from the classical variant by the lack of cardiomegalia and the high residual activity of acid alpha-glucosidase in cultivated skin fibroblasts and muscle tissue. In the present case, however, glycogen storing lysosomes were found in peripheral lymphocytes and skeletal muscle cells. This finding underlines the particular value of ultrastructural investigation in the diagnosis of GSD II.

UI MeSH Term Description Entries
D007223 Infant A child between 1 and 23 months of age. Infants
D008247 Lysosomes A class of morphologically heterogeneous cytoplasmic particles in animal and plant tissues characterized by their content of hydrolytic enzymes and the structure-linked latency of these enzymes. The intracellular functions of lysosomes depend on their lytic potential. The single unit membrane of the lysosome acts as a barrier between the enzymes enclosed in the lysosome and the external substrate. The activity of the enzymes contained in lysosomes is limited or nil unless the vesicle in which they are enclosed is ruptured or undergoes MEMBRANE FUSION. (From Rieger et al., Glossary of Genetics: Classical and Molecular, 5th ed). Autolysosome,Autolysosomes,Lysosome
D008297 Male Males
D008854 Microscopy, Electron Microscopy using an electron beam, instead of light, to visualize the sample, thereby allowing much greater magnification. The interactions of ELECTRONS with specimens are used to provide information about the fine structure of that specimen. In TRANSMISSION ELECTRON MICROSCOPY the reactions of the electrons that are transmitted through the specimen are imaged. In SCANNING ELECTRON MICROSCOPY an electron beam falls at a non-normal angle on the specimen and the image is derived from the reactions occurring above the plane of the specimen. Electron Microscopy
D009132 Muscles Contractile tissue that produces movement in animals. Muscle Tissue,Muscle,Muscle Tissues,Tissue, Muscle,Tissues, Muscle
D009929 Organ Size The measurement of an organ in volume, mass, or heaviness. Organ Volume,Organ Weight,Size, Organ,Weight, Organ
D005347 Fibroblasts Connective tissue cells which secrete an extracellular matrix rich in collagen and other macromolecules. Fibroblast
D006003 Glycogen
D006008 Glycogen Storage Disease A group of inherited metabolic disorders involving the enzymes responsible for the synthesis and degradation of glycogen. In some patients, prominent liver involvement is presented. In others, more generalized storage of glycogen occurs, sometimes with prominent cardiac involvement. Glycogenosis,Disease, Glycogen Storage,Diseases, Glycogen Storage,Glycogen Storage Diseases,Glycogenoses,Storage Disease, Glycogen,Storage Diseases, Glycogen
D006009 Glycogen Storage Disease Type II An autosomal recessively inherited glycogen storage disease caused by GLUCAN 1,4-ALPHA-GLUCOSIDASE deficiency. Large amounts of GLYCOGEN accumulate in the LYSOSOMES of skeletal muscle (MUSCLE, SKELETAL); HEART; LIVER; SPINAL CORD; and BRAIN. Three forms have been described: infantile, childhood, and adult. The infantile form is fatal in infancy and presents with hypotonia and a hypertrophic cardiomyopathy (CARDIOMYOPATHY, HYPERTROPHIC). The childhood form usually presents in the second year of life with proximal weakness and respiratory symptoms. The adult form consists of a slowly progressive proximal myopathy. (From Muscle Nerve 1995;3:S61-9; Menkes, Textbook of Child Neurology, 5th ed, pp73-4) Acid Maltase Deficiency Disease,Generalized Glycogenosis,Glycogenosis 2,Lysosomal alpha-1,4-Glucosidase Deficiency Disease,Pompe Disease,Acid Alpha-Glucosidase Deficiency,Acid Maltase Deficiency,Adult Glycogen Storage Disease Type II,Alpha-1,4-Glucosidase Deficiency,Deficiency Disease, Acid Maltase,Deficiency Disease, Lysosomal alpha-1,4-Glucosidase,Deficiency of Alpha-Glucosidase,GAA Deficiency,GSD II,GSD2,Glycogen Storage Disease II,Glycogen Storage Disease Type 2,Glycogen Storage Disease Type II, Adult,Glycogen Storage Disease Type II, Infantile,Glycogen Storage Disease Type II, Juvenile,Glycogenosis Type II,Infantile Glycogen Storage Disease Type II,Juvenile Glycogen Storage Disease Type II,Pompe's Disease,Acid Alpha Glucosidase Deficiency,Acid Alpha-Glucosidase Deficiencies,Acid Maltase Deficiencies,Alpha 1,4 Glucosidase Deficiency,Alpha-1,4-Glucosidase Deficiencies,Alpha-Glucosidase Deficiencies,Alpha-Glucosidase Deficiencies, Acid,Alpha-Glucosidase Deficiency,Alpha-Glucosidase Deficiency, Acid,Deficiencies, Acid Alpha-Glucosidase,Deficiencies, Acid Maltase,Deficiencies, Alpha-1,4-Glucosidase,Deficiencies, GAA,Deficiency of Alpha Glucosidase,Deficiency, Acid Alpha-Glucosidase,Deficiency, Acid Maltase,Deficiency, Alpha-1,4-Glucosidase,Deficiency, GAA,Disease, Pompe,Disease, Pompe's,GAA Deficiencies,GSD2s,Generalized Glycogenoses,Glycogenoses, Generalized,Glycogenosis, Generalized,Lysosomal alpha 1,4 Glucosidase Deficiency Disease,Maltase Deficiencies, Acid,Pompes Disease,Type II, Glycogenosis,Type IIs, Glycogenosis

Related Publications

K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Enzyme patterns in glycogen storage disease type II (Pompe's disease).
July 1966, Metabolism: clinical and experimental,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Hydrocephalus associated with glycogen storage disease type II (Pompe's disease).
September 1999, Pediatric neurology,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Chorionic villus ultrastructure in type II glycogen storage disease (Pompe's disease)
January 1991, The New England journal of medicine,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Glycogen storage disease type II (Pompe's disease): the first biochemical evidence in Thailand.
September 1987, Journal of the Medical Association of Thailand = Chotmaihet thangphaet,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Comparative pathology of the canine model of glycogen storage disease type II (Pompe's disease).
January 1985, Journal of inherited metabolic disease,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
[Pompe's disease or glycogen storage disease].
January 1982, Duodecim; laaketieteellinen aikakauskirja,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
[Pulmonary hypertension due to glycogen storage disease type II (Pompe's disease): a case report].
March 1989, Journal of cardiology,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Apparent normal leukocyte acid maltase activity in glycogen storage disease type II (Pompe's disease).
December 1980, Clinical chemistry,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Choice of leucocyte preparation in the diagnosis of glycogen storage disease type II (Pompe's disease).
December 1971, Clinica chimica acta; international journal of clinical chemistry,
K Ullrich, and H Gröbe, and R Korinthenberg, and D B von Bassewitz
Echocardiographic and pulsed Doppler features in glycogen storage disease type II of the heart (Pompe's disease).
January 1991, Acta cardiologica,
Copied contents to your clipboard!