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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Gnptabnym
Nymphe
MGI:5616922
Summary 2 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
hm1
Gnptabnym/Gnptabnym involves: BALB/cAnNHsd * C3H/HeNHsd MGI:5790646
ht2
Gnptabnym/Gnptab+ involves: BALB/cAnNHsd * C3H/HeNHsd MGI:5790647


Genotype
MGI:5790646
hm1
Allelic
Composition
Gnptabnym/Gnptabnym
Genetic
Background
involves: BALB/cAnNHsd * C3H/HeNHsd
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Gnptabnym mutation (2 available); any Gnptab mutation (78 available)
phenotype observed in females
phenotype observed in males
N normal phenotype

Growth retardation, facial dysmorphism, and abnormal spine curvature and hunched back in Gnptabnym/Gnptabnym mice

mortality/aging
• only ~30% of mice survive to 60 weeks of age
• progressive decline in survival falling below 50% by 40 weeks of age
• homozygotes are born with a reduced frequency (15% versus expected 25%), suggesting reduced in utero survival

growth/size/body
• facial dysmorphism is evident from birth and progresses with age
• reduced nasal bridge evident from birth
• flat profile with reduced nasal bridge evident from birth
• mice remain significantly smaller than wild-type controls (~60%) throughout life
• body weight progression is significantly reduced starting at 8 weeks of age

craniofacial
• facial dysmorphism is evident from birth and progresses with age
• reduced nasal bridge evident from birth
• flat profile with reduced nasal bridge evident from birth

vision/eye
• progressive thickening of the eyelids evident from birth

skeleton
• skeletal abnormalities are evident from birth
• severe deformities affecting the spine at 12 months of age
• kyphosis at 12 months of age
• mutant tracheal cartilage chondrocytes are enlarged with their cytoplasm filled by inclusion bodies and abundant microvacuoles, unlike wild-type chondrocytes which show low basic cytoplasm containing a single clear vacuole
• mutant chondrocytes are less affected by fixation-induced shrinkage than wild-type chondrocytes

behavior/neurological
• mice show a 50% alternation in choosing an arm at random in the Y-maze spontaneous alternation task, indicating deficits in psychomotor performance (cognitive slownes)
• limb-clasping reflexes starting at 5 months of age
• ataxic gait confirmed by Noldus Catwalk automated gait analysis, with a progressive and highly significant reduction of the regularity index (a measure of regular footstep pattern) noted between 6 and 12 months of age
• front paw base of support is significantly increased from 3 months of age
• reduced motor balance and coordination on the rotarod at 3, 6, and 12 months of age
• rotarod performance worsens with age
• weekly injection of P7 mice with 2-hydroxypropyl-beta-cyclodextrin for 7 months does not improve rotarod performance at 3 months or at 7 months of age
• progressive gait abnormality

nervous system
• increased inflammatory response as shown by increased GFAP immunoreactivity throughout the whole brain
• brain is about 30% smaller than normal
• luxol fast blue staining of cerebellar sections indicates reduced myelination and degeneration of the subcortical white matter
• increased glycolipid storage in hippocampal layer CA1 at 9 months of age
• increased glycolipid storage in hippocampal layer CA3 at 9 months of age
• large amounts of storage of glycolipids in cortical layers III-IV with lesser amounts in layers I and II at 9 months of age
• progressive Purkinje cell degeneration with ~25% and ~50% Purkinje cell loss at 7 and 11 months of age, respectively
• cell death is often accompanied by an inflammatory response and a defect in myelination
• however, majority of Purkinje cells in lobe IV/V are still present at 3 months
• swelling of Purkinje cell axons and neuronal torpedoes typical of cell atrophy are already detected at 3 months and increase in severity with age
• axonal spheroids/torpedoes precede Purkinje cell loss
• weekly injection of P7 mice with 2-hydroxypropyl-beta-cyclodextrin for 7 months does not rescue or delay the signs of Purkinje cell degeneration (swelling of dendrites and axonal torpedoes) at 3 months or at 7 months of age
• increased storage of glycolipids in the cerebellar molecular layer relative to the granule layer at 9 months of age
• brain atrophy worsens over time
• increased GFAP immunoreactivity throughout the whole brain, mostly affecting the cerebellum
• marked astrogliosis in the cerebellar white matter, granule layer, and Purkinje cell layer
• axonal spheroid formation at 3 months that worsens with age
• demyelination of the cerebellum with thinning of the white matter tracts

muscle
• reduced muscle strength on the inverted screen test at 3, 6, and 12 months of age
• inverted screen performance worsens with age
• weekly injection of P7 mice with 2-hydroxypropyl-beta-cyclodextrin for 7 months does not improve inverted screen performance at 3 months or at 7 months of age

endocrine/exocrine glands
• marked disorganization of pancreatic tissue structure
• enlargement of pancreatic acinar cells due to presence of large vacuoles containing faint granular material

cellular
• accumulation of inclusion bodies indicative of lysosomal storage in mouse embryonic fibroblasts, secretory tissue (pancreatic acinar cells) and connective tissue (tracheal cartilage chondrocytes)
• inclusions are aggregates of polysaccharides that increase in storage material with age
• deregulation of lysosomal enzymes leading to increased glycolipid and cholesterol storage in the cerebellum, cortex, and hippocampus at 9 months of age

homeostasis/metabolism
• at 3 months of age, serum enzymatic activities of the lysosomal hydrolases beta-hexosaminidase, beta-galactosidase, alpha-mannosidase, and beta-mannosidase are increased by 2.5- to 30-fold relative to wild-type controls
• at 4 months of age, enzymatic activities of beta-hexosaminidase, alpha-mannosidase, and beta-glucoronidase are increased by 1.5-fold, whereas beta-galactosidase is decreased by 30%, as measured in whole brain lysates

integument
• unusually stiff skin
• unusually thick skin

immune system
• increased inflammatory response as shown by increased GFAP immunoreactivity throughout the whole brain

reproductive system
• increased frequency of males with penile prolapse starting at 3 months of age
• mating is only successful in 9% of breeding pairs, indicating infertility or incapacity of females to carry pups to term

digestive/alimentary system
• enlargement of pancreatic acinar cells due to presence of large vacuoles containing faint granular material

renal/urinary system
• increased frequency of males with penile prolapse starting at 3 months of age

respiratory system
• reduced nasal bridge evident from birth

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
mucolipidosis II alpha/beta DOID:0080070 OMIM:252500
J:218156




Genotype
MGI:5790647
ht2
Allelic
Composition
Gnptabnym/Gnptab+
Genetic
Background
involves: BALB/cAnNHsd * C3H/HeNHsd
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Gnptabnym mutation (2 available); any Gnptab mutation (78 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
normal phenotype
• despite a 1.7-fold increase in beta-hexosaminidase and a 2.4-fold increase in alpha-mannosidase, heterozygotes appear overtly normal with no apparent changes in fertility, size, body weight progression, facial features, survival, motor coordination, and muscle strength





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Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO)
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last database update
12/10/2024
MGI 6.24
The Jackson Laboratory