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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Cep290Gt(CC0582)Wtsi
gene trap CC0582, Wellcome Trust Sanger Institute
MGI:3870362
Summary 2 genotypes


Genotype
MGI:5749256
hm1
Allelic
Composition
Cep290Gt(CC0582)Wtsi/Cep290Gt(CC0582)Wtsi
Genetic
Background
129P2/OlaHsd-Cep290Gt(CC0582)Wtsi
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Cep290Gt(CC0582)Wtsi mutation (0 available); any Cep290 mutation (124 available)
phenotype observed in females
phenotype observed in males
N normal phenotype

Cep290Gt(CC0582)Wtsi/Cep290Gt(CC0582)Wtsi mice exhibit progressive renal collecting duct cystic disease

mortality/aging
N
• homozygotes on a pure 129P2/OlaHsd genetic background are viable beyond 12 months of age
• Background Sensitivity: most homozygotes generated on a congenic C57BL/6J background (N6) die in utero

vision/eye
• progressive degeneration of photoreceptor inner segments starting at 4 weeks of age
• progressive degeneration of photoreceptor outer segments starting at 4 weeks of age
• at 4 weeks of age
• severe reduction of the outer nuclear layer at 6 and 12 months of age
• progressive retinal degeneration starting at 4 weeks of age

behavior/neurological

renal/urinary system
• primary cilia are present on the epithelial cells of non-cystic and cystic renal tubules but are significantly reduced in number
• in 3D spheroid culture, primary kidney cells show loss of ciliation
• treatment of cells with a CDK1/2 inhibitor rescues ciliation
• progressive cystic kidney disease, reminiscent of nephronophthisis
• small cysts develop within the renal cortex of most but not all homozygous neonates
• cysts become more prominent and more numerous at 2 weeks of age and persist up to 1 year of age
• renal cysts are confirmed to be of collecting duct in origin
• progressive renal collecting duct cystic disease, with microcysts present from birth to 1 year of age
• collecting duct cyst formation is associated with a reduction in number of primary cilia and abnormal Hedgehog signaling

nervous system
N
• no evidence of a gross foliation defect within the cerebellum
• early onset hydrocephalus, evident at 1 month of age
• cerebral abnormalities
• progressive degeneration of photoreceptor inner segments starting at 4 weeks of age
• progressive degeneration of photoreceptor outer segments starting at 4 weeks of age

cellular
• primary cilia are present on the epithelial cells of non-cystic and cystic renal tubules but are significantly reduced in number
• in 3D spheroid culture, primary kidney cells show loss of ciliation
• treatment of cells with a CDK1/2 inhibitor rescues ciliation
• supernumerary centrioles in primary kidney cells
• treatment of cells with a CDK1/2 inhibitor rescues the centriole numbers
• increase in double-stranded breaks in DNA
• treatment of primary kidney cells with a CDK1/2 inhibitor rescues the increase in DNA breaks
• primary kidney cells exhibit aberrant DNA content profile that does not match 2N or 4N DNA
• replication fork velocity is decreased in primary kidney cells and cells have an increase in asymmetric forks, indicating a loss of fork stability and replication stress

homeostasis/metabolism
• increase in double-stranded breaks in DNA
• treatment of primary kidney cells with a CDK1/2 inhibitor rescues the increase in DNA breaks
• primary kidney cells exhibit aberrant DNA content profile that does not match 2N or 4N DNA
• replication fork velocity is decreased in primary kidney cells and cells have an increase in asymmetric forks, indicating a loss of fork stability and replication stress

growth/size/body
• progressive cystic kidney disease, reminiscent of nephronophthisis
• small cysts develop within the renal cortex of most but not all homozygous neonates
• cysts become more prominent and more numerous at 2 weeks of age and persist up to 1 year of age
• renal cysts are confirmed to be of collecting duct in origin

liver/biliary system
N
• no evidence of liver cysts or fibrosis at 1 month of age

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
Joubert syndrome 5 DOID:0111000 OMIM:610188
J:212182 , J:226246




Genotype
MGI:5749258
hm2
Allelic
Composition
Cep290Gt(CC0582)Wtsi/Cep290Gt(CC0582)Wtsi
Genetic
Background
B6J.129P2-Cep290Gt(CC0582)Wtsi
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Cep290Gt(CC0582)Wtsi mutation (0 available); any Cep290 mutation (124 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• most homozygotes generated on a congenic C57BL/6J background (N6) die in utero
• Background Sensitivity: homozygotes on a coisogenic 129P2/OlaHsd background are viable beyond 12 months of age





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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
11/19/2024
MGI 6.24
The Jackson Laboratory