BIOMAT Database Logo BIOMAT Database Logo

GM2-gangliosidosis variant with altered substrate specificity: evidence for alpha-locus genetic compound. 1987

G T Besley, and D M Broadhead, and J A Young
Department of Pathology, Royal Hospital for Sick Children, Edinburgh, UK.

UI MeSH Term Description Entries
D007223 Infant A child between 1 and 23 months of age. Infants
D008297 Male Males
D006801 Humans Members of the species Homo sapiens. Homo sapiens,Man (Taxonomy),Human,Man, Modern,Modern Man
D006923 Hymecromone A coumarin derivative possessing properties as a spasmolytic, choleretic and light-protective agent. It is also used in ANALYTICAL CHEMISTRY TECHNIQUES for the determination of NITRIC ACID. Imecromone,Methylumbelliferone,Resocyanine,4-Methylumbelliferone,7-Hydroxy-4-methyl-coumarin,Cholestil,Mendiaxon,4 Methylumbelliferone,7 Hydroxy 4 methyl coumarin
D001619 beta-N-Acetylhexosaminidases A hexosaminidase specific for non-reducing N-acetyl-D-hexosamine residues in N-acetyl-beta-D-hexosaminides. It acts on GLUCOSIDES; GALACTOSIDES; and several OLIGOSACCHARIDES. Two specific mammalian isoenzymes of beta-N-acetylhexoaminidase are referred to as HEXOSAMINIDASE A and HEXOSAMINIDASE B. Deficiency of the type A isoenzyme causes TAY-SACHS DISEASE, while deficiency of both A and B isozymes causes SANDHOFF DISEASE. The enzyme has also been used as a tumor marker to distinguish between malignant and benign disease. beta-N-Acetylhexosaminidase,N-Acetyl-beta-D-hexosaminidase,beta-Hexosaminidase,beta-N-Acetyl-D-hexosaminidase,beta-N-Acetyl-hexosaminidase,N Acetyl beta D hexosaminidase,beta Hexosaminidase,beta N Acetyl D hexosaminidase,beta N Acetyl hexosaminidase,beta N Acetylhexosaminidase,beta N Acetylhexosaminidases
D013379 Substrate Specificity A characteristic feature of enzyme activity in relation to the kind of substrate on which the enzyme or catalytic molecule reacts. Specificities, Substrate,Specificity, Substrate,Substrate Specificities
D013661 Tay-Sachs Disease An autosomal recessive neurodegenerative disorder characterized by the onset in infancy of an exaggerated startle response, followed by paralysis, dementia, and blindness. It is caused by mutation in the alpha subunit of the HEXOSAMINIDASE A resulting in lipid-laden ganglion cells. It is also known as the B variant (with increased HEXOSAMINIDASE B but absence of hexosaminidase A) and is strongly associated with Ashkenazic Jewish ancestry. G(M2) Gangliosidosis, Type I,Gangliosidosis G(M2), Type I,Gangliosidosis GM2, B Variant,Hexosaminidase A Deficiency Disease,Tay-Sachs Disease, B Variant,Amaurotic Familial Idiocy,B Variant GM2 Gangliosidosis,B Variant GM2-Gangliosidosis,Deficiency Disease Hexosaminidase A,Familial Amaurotic Idiocy,GM2 Gangliosidosis, B Variant,GM2 Gangliosidosis, Type 1,GM2 Gangliosidosis, Type I,GM2-Gangliosidosis, Type I,Gangliosidosis GM2 , Type 1,Gangliosidosis GM2, Type I,HexA Deficiency,Hexosaminidase A Deficiency,Hexosaminidase alpha-Subunit Deficiency (Variant B),Sphingolipidosis, Tay-Sachs,Amaurotic Idiocy, Familial,B Variant GM2-Gangliosidoses,Deficiency, Hexosaminidase A,Deficiency, Hexosaminidase alpha-Subunit (Variant B),GM2-Gangliosidosis, B Variant,Hexosaminidase alpha Subunit Deficiency (Variant B),Sphingolipidosis, Tay Sachs,Tay Sachs Disease,Tay Sachs Disease, B Variant,Tay-Sachs Sphingolipidosis,Type I GM2-Gangliosidosis

Related Publications

G T Besley, and D M Broadhead, and J A Young
Late onset GM2 gangliosidosis: an alpha-locus genetic compound with near normal hexosaminidase activity.
January 1985, Clinical genetics,
G T Besley, and D M Broadhead, and J A Young
[Juvenile GM2 gangliosidosis with altered substrate specificity of hexosaminidase A (author's transl)].
March 1974, Acta neuropathologica,
G T Besley, and D M Broadhead, and J A Young
Variant of GM2-gangliosidosis with hexosaminidase A having a severely changed substrate specificity.
January 1983, The EMBO journal,
G T Besley, and D M Broadhead, and J A Young
Alpha-locus hexosaminidase genetic compound with juvenile gangliosidosis phenotype: clinical, genetic, and biochemical studies.
July 1980, American journal of human genetics,
G T Besley, and D M Broadhead, and J A Young
Mutation in GM2-gangliosidosis B1 variant.
January 1988, Journal of neurochemistry,
G T Besley, and D M Broadhead, and J A Young
Diagnosis of AB variant, GM2 gangliosidosis.
January 1986, Annals of neurology,
G T Besley, and D M Broadhead, and J A Young
GM2 gangliosidosis variant B1 neuroradiological findings.
January 2003, Journal of neurology,
G T Besley, and D M Broadhead, and J A Young
[GM2 activator protein deficiency (AB variant form of GM2 gangliosidosis)].
January 1998, Ryoikibetsu shokogun shirizu,
G T Besley, and D M Broadhead, and J A Young
Substrate reduction therapy in juvenile GM2 gangliosidosis.
January 2009, Molecular genetics and metabolism,
G T Besley, and D M Broadhead, and J A Young
Neuroradiological findings in GM2 gangliosidosis variant B1.
July 2011, Journal of pediatric neurosciences,
Copied contents to your clipboard!