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FLASH GENE

Symbol

GUSB

contributors: mct/npt/shn - updated : 15-05-2012

HGNC name	glucuronidase, beta
HGNC id	4696

FLASH GENE DNA RNA EXPRESSION PROTEIN DISORDER ANIMAL & CELL MODELS

DNA

TYPE	functioning gene
STRUCTURE	21.58 kb     12 Exon(s)

10 Kb 5' upstream gene genomic sequence study

regulatory sequence	cytosine-phosphate-guanine/HTF
motif	repetitive sequence   ALU
text structure	37 ALU repeats

MAPPING

cloned

Y

linked

N

status

confirmed

Map	cen - D7S2512 - D7S2549 - GUSB - D7S663 - D7S502 - qter

RNA

TRANSCRIPTS	type	messenger

identification nb exons type bp product Protein kDa AA specific expression Year Pubmed NM_000181 12 - 2245 NP_000172 75 651 - Gratz (2005)

EXPRESSION

Type

expressed in	(based on citations)
organ(s)	System Organ level 1 Organ level 2 Organ level 3 Organ level 4 Level Pubmed Species Stage Rna symbol Cardiovascular heart         Digestive liver         Nervous brain

tissue

System Tissue Tissue level 1 Tissue level 2 Level Pubmed Species Stage Rna symbol Blood / Hematopoietic         Connective bone       Connective cartilage       Nervous central       Nervous peripherous

cells

System Cell Pubmed Species Stage Rna symbol   digestive Blood/Hematopoietic neutrophil Nervous neuron

cell lineage

cell lines

fluid/secretion

at STAGE

physiological period

pregnancy

Text

placenta

PROTEIN

PHYSICAL PROPERTIES

STRUCTURE

motifs/domains

conjugated

GlycoP , PhosphoP

mono polymer

homomer , tetramer

HOMOLOGY

interspecies	ortholog to Gusb, Mus musculus
	ortholog to GUSB, pan troglodytes
	ortholog to Gusb, rattus norvegicus
	ortholog to gusb, Danio rerio

Homologene

FAMILY

glycosyl hydrolase 2 family

CATEGORY

enzyme

SUBCELLULAR LOCALIZATION	intracellular
	intracellular,cytoplasm,organelle,endoplasmic reticulum
	intracellular,cytoplasm,organelle,Golgi
	intracellular,cytoplasm,organelle,endosome
	intracellular,cytoplasm,organelle,lysosome

basic FUNCTION	glucuronidase, beta, acting on dermatan sulfate, heparan sulfate
	catalyzing the fifth step of degradation of glucosaminoglycans (mucopolysaccharides)

CELLULAR PROCESS

PHYSIOLOGICAL PROCESS

PATHWAY

metabolism

carbohydrate

signaling

glycosaminoglycan catabolism

a component

INTERACTION

DNA

RNA

small molecule

protein

egasyn, EG (

cell & other

REGULATION

Other

targeted to the lysosome by M6P receptor mediated pathway

ASSOCIATED DISORDERS

corresponding disease(s)

MPS7

related resource

Mucopolysaccharidosis

Susceptibility

Variant & Polymorphism

Candidate gene
Marker
Therapy target	Gene therapy by transfer of a beta-glucuronidase gene into mutant haematopoietic mouse stem cells results in long-term expression of low levels of beta-glucuronidase which partially corrects the mucopolysaccharidosis VII by reducing lysosomal storage in liver and spleen (
	A retroviral vector expressing the full-length canine beta-glucuronidase cDNA corrected the deficiency in MPS VII cells (

ANIMAL & CELL MODELS

	inherited deficiency of beta-glucuronidase in mice causes mucopolysaccharidosis VII, a progressive degenerative disease that reduces lifespan and results from lysosomal storage of undegraded glycosaminoglycans in the spleen, liver, kidney, cornea, brain and skeletal system (
	Beta-glucuronidase deficiency in dog leads to mucopolysaccharidosis type VII (
	mice with beta-glucuronidase deficiency display lysosomal storage disease with similarities to human mucopolysaccharidosis type VII (
	Cats with beta-glucuronidase deficiency display walking difficulties, an enlarged abdomen, facial dysmorphism, plump paws, corneal clouding, granulation of neutrophils, and vacuolated lymphocytes (
	Affected gus(mps2J)/gus(mps2J) mice are deficient in beta-glucuronidase because of insertion of an intracisternal A particle element into intron 8, have have < 1% of normal beta-glucuronidase activity and secondary elevations of other lysosomal enzymes and the phenotype includes shortened life-span, dysmorphic features, and skeletal dysplasia (
	E536A mutant mice have no GUS activity in any tissue and display a severe MPS VII phenotype, E536Q and L175F mutant mice have low levels of residual activity and milder MPS VII phenotypes (
	MPSVII-iPS cells demonstrated a markedly impaired ability to form embryoid bodies in vitro, and MPSVII-embryoid bodies exibited elevated levels of hyaluronan and its receptor CD44, and markedly reduced expression levels of E-cadherin and cell-proliferating marker (