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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Col1a1tm1(tetO-URI1)Ndj
targeted mutation 1, Nabil Djouder
MGI:5706755
Summary 3 genotypes


Genotype
MGI:6378441
cx1
Allelic
Composition
Col1a1tm1(tetO-URI1)Ndj/Col1a1+
Tg(Cebpb-tTA)#Bjd/0
Genetic
Background
B6.Cg-Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Col1a1tm1(tetO-URI1)Ndj mutation (0 available); any Col1a1 mutation (163 available)
Tg(Cebpb-tTA)#Bjd mutation (0 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• all mice die around 85 weeks of age, with a median survival of 76 weeks before complete liver failure

liver/biliary system
• 8 week old mice show anisokaryotic clusters resembling low-grade dysplastic nodules that develop into high-grade dysplastic nodules at 12 weeks of age that is similar to large liver dysplasia
• mice supplied with the nicotinamide riboside diet at 3 weeks of age do not show dysplastic lesions in the liver or DNA damage
• early hepatocellular carcinoma (HCC) emerges between 24-54 weeks of age, with mice showing low-grade and differentiated HCC at 54-65 weeks and 40% of mutants developing high-grade tumors occupying 20-60% of the liver between 65-75 weeks of age
• 25-50% of hepatocytes are Ki67+, suggesting aggressive tumors
• tumors are well/moderately differentiated, with 20% glandular/acinar and 80% trabecular
• however, no cholangiocarcinoma is seen
• mice treated with doxycycline to cease URI1 expression at 8 weeks of age for 24 weeks show abolished dysplastic foci and prevention of early tumors
• mice treated with doxycycline at 8 weeks until 60 weeks of age show prevention of tumor development
• when mice are treated with doxycycline at 24 weeks (when mice have high-grade dysplastic nodules/early HCC and adenomas) for 28 weeks, only residual anisokaryotic clusters are seen and no adenomas or HCCs are detected
• however, when treatment with doxycycline begins above 60 weeks of age, HCC does not regress
• prolonged nicotinamide riboside treatment prevents tumor development
• 8 week old mice exhibit liver fibrosis that increases over time until 24 weeks
• mice treated with doxycycline to cease URI1 expression at 8 weeks of age for 24 weeks show reduced liver fibrosis
• mice supplied with the nicotinamide riboside diet at 3 weeks of age have reduced liver fibrosis

neoplasm
• diethylnitrosamine (DEN)-treated mice develop HCC at 30 weeks of age
• early hepatocellular carcinoma (HCC) emerges between 24-54 weeks of age, with mice showing low-grade and differentiated HCC at 54-65 weeks and 40% of mutants developing high-grade tumors occupying 20-60% of the liver between 65-75 weeks of age
• 25-50% of hepatocytes are Ki67+, suggesting aggressive tumors
• tumors are well/moderately differentiated, with 20% glandular/acinar and 80% trabecular
• however, no cholangiocarcinoma is seen
• mice treated with doxycycline to cease URI1 expression at 8 weeks of age for 24 weeks show abolished dysplastic foci and prevention of early tumors
• mice treated with doxycycline at 8 weeks until 60 weeks of age show prevention of tumor development
• when mice are treated with doxycycline at 24 weeks (when mice have high-grade dysplastic nodules/early HCC and adenomas) for 28 weeks, only residual anisokaryotic clusters are seen and no adenomas or HCCs are detected
• however, when treatment with doxycycline begins above 60 weeks of age, HCC does not regress
• prolonged nicotinamide riboside treatment prevents tumor development
• metastases into lungs are seen

homeostasis/metabolism
• serum glucose levels are decreased in 65 week old mice
• serum albumin is increased in 65 week old mice
• NAD+ concentrations are reduced in 3- and 6-week old livers
• mice supplied with a nicotinamide riboside (NR) diet at 3 weeks of age show increased hepatic NAD+ concentrations
• alanine transaminase (ALT) levels are increased in 65 week old mice
• however, serum ALT levels are unchanged in 8 week old mice
• mice treated with doxycycline at 8 weeks until 60 weeks of age show normalization of ALT levels
• prolonged nicotinamide riboside treatment reduces ALT levels
• total bile acids are increased in 65 week old mice
• diethylnitrosamine (DEN)-treated mice develop HCC at 30 weeks of age

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
hepatocellular carcinoma DOID:684 OMIM:114550
J:217463




Genotype
MGI:6378447
cx2
Allelic
Composition
Col1a1tm1(tetO-URI1)Ndj/Col1a1tm1(tetO-URI1)Ndj
Tg(Cebpb-tTA)#Bjd/0
Genetic
Background
B6.Cg-Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Col1a1tm1(tetO-URI1)Ndj mutation (0 available); any Col1a1 mutation (163 available)
Tg(Cebpb-tTA)#Bjd mutation (0 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
liver/biliary system
• mice develop hepatocellular carcinoma by 10 weeks of age
• mice kept on doxycycline until 8 weeks of age and then transferred to normal chow develop liver tumors
• 3 week old mice mice supplied with a nicotinamide riboside diet show prevention of liver tumors at 30 weeks of age
• 12 week old mice with tumors supplied with a nicotinamide riboside diet for 48 weeks show tumor regression

neoplasm
• mice develop hepatocellular carcinoma by 10 weeks of age
• mice kept on doxycycline until 8 weeks of age and then transferred to normal chow develop liver tumors
• 3 week old mice mice supplied with a nicotinamide riboside diet show prevention of liver tumors at 30 weeks of age
• 12 week old mice with tumors supplied with a nicotinamide riboside diet for 48 weeks show tumor regression

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
hepatocellular carcinoma DOID:684 OMIM:114550
J:217463




Genotype
MGI:6378452
cx3
Allelic
Composition
Col1a1tm1(tetO-URI1)Ndj/Col1a1+
Tg(Cebpb-tTA)#Bjd/0
Trp53tm1Gev/Trp53+
Genetic
Background
B6.Cg-Trp53tm1Gev Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Col1a1tm1(tetO-URI1)Ndj mutation (0 available); any Col1a1 mutation (163 available)
Tg(Cebpb-tTA)#Bjd mutation (0 available)
Trp53tm1Gev mutation (0 available); any Trp53 mutation (240 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• mice exhibit reduced survival compared to heterozygous Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd/0 mice

neoplasm
• mice exhibit accelerated liver tumorigenesis compared to single heterozygous Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd/0 mice, with 80% of mice showing aggressive hepatocellular carcinoma

liver/biliary system
• 8 week old mice show decreased cleaved caspase 3, Bax expression, collapsed fibers, Sirius Red staining and alanine transaminase levels, indicating suppressed hepatocyte apoptosis
• mice exhibit accelerated liver tumorigenesis compared to single heterozygous Col1a1tm1(tetO-URI1)Ndj Tg(Cebpb-tTA)#Bjd/0 mice, with 80% of mice showing aggressive hepatocellular carcinoma

cellular
• 8 week old mice show decreased cleaved caspase 3, Bax expression, collapsed fibers, Sirius Red staining and alanine transaminase levels, indicating suppressed hepatocyte apoptosis





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last database update
11/12/2024
MGI 6.24
The Jackson Laboratory