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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Tg(tetO-NPM1/ALK,-luc)2Gde
transgene insertion 2, Georges Delsol
MGI:5766488
Summary 1 genotype
Jump to Allelic Composition Genetic Background Genotype ID
cx1
Tg(EmuSR-tTa)83Bop/Tg(EmuSR-tTa)83Bop
Tg(tetO-NPM1/ALK,-luc)2Gde/0
involves: FVB/N MGI:5766492


Genotype
MGI:5766492
cx1
Allelic
Composition
Tg(EmuSR-tTa)83Bop/Tg(EmuSR-tTa)83Bop
Tg(tetO-NPM1/ALK,-luc)2Gde/0
Genetic
Background
involves: FVB/N
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Tg(EmuSR-tTa)83Bop mutation (1 available)
Tg(tetO-NPM1/ALK,-luc)2Gde mutation (0 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• mice die within a mean latency of 4 weeks when dox is removed at the newborn stage
• embryonic lethality is seen in the absence of doxycycline (dox)

immune system
• splenomegaly in mice when dox is removed in newborns
• generalized lymphadenopathy in mice when dox is removed in newborns

growth/size/body
• mice are growth retarded when dox is removed in newborns
• splenomegaly in mice when dox is removed in newborns

hematopoietic system
• splenomegaly in mice when dox is removed in newborns

integument
• induction of transgene expression by removal of dox in newborns results in the development of a skin disease affecting the snout and paws, first detectable at 3 weeks of age
• lymphomatous infiltration is sometimes seen in the dermis below the keratoacanthoma-like lesions
• mice exhibit skin nodules of a hyperplasia of the epidermis when dox is removed at the newborn stage, suggesting a keratoacanathoma-like lesion
• mice that are moribund with tumors and treated with dox for 12 days to suppress transgene expression exhibit a clearing of skin lesions and regrowth of hair within 3 weeks
• treatment of mice with an ALK phosphorylation inhibitor PF-2341066 results in a progressive clearing of skin lesions

neoplasm
• mice develop aggressive lymphoma/leukemia when dox is removed in newborns
• lymphoma/leukemia are derived from B cells
• mice develop aggressive lymphoma/leukemia when dox is removed in newborns
• lymphoma/leukemia are derived from B cells
• transplantation of mutant bone marrow into recipient mice results in the development of B-cell lymphoma without skin lesions
• mice that are moribund with tumors and treated with dox for 12 days exhibit tumor regression
• treatment of mice with an ALK phosphorylation inhibitor PF-2341066 results in tumor regression

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
non-Hodgkin lymphoma DOID:0060060 OMIM:605027
J:160236





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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