About   Help   FAQ
Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Kcnj1tm1Ges
targeted mutation 1, Gary E Shull
MGI:2388372
Summary 1 genotype
Jump to Allelic Composition Genetic Background Genotype ID
hm1
Kcnj1tm1Ges/Kcnj1tm1Ges involves: 129X1/SvJ * Black Swiss MGI:3041878


Genotype
MGI:3041878
hm1
Allelic
Composition
Kcnj1tm1Ges/Kcnj1tm1Ges
Genetic
Background
involves: 129X1/SvJ * Black Swiss
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Kcnj1tm1Ges mutation (1 available); any Kcnj1 mutation (29 available)
phenotype observed in females
phenotype observed in males
N normal phenotype

Kcnj1tm1Ges/Kcnj1tm1Ges mice exhibit hydronephrosis

mortality/aging
• approximately 95% of homozygotes died before 3 weeks of age; 85% of mutants died by 12 days of age, and only 5% survived to weaning
• mutans that survived to weaning almost invariably survived to adulthood, appeared slightly smaller but were healthy
• daily subcutaneous injections of either indomethacin or isotonic saline failed to prolong survival

behavior/neurological

cardiovascular system

growth/size/body
• homozygotes displayed a significant reduction in body weight and failed to thrive

hematopoietic system

homeostasis/metabolism
• adult mutants exhibited elevated blood concentrations of Na+ and Cl-
• homozygous null adult mice displayed metabolic acidosis, volume depletion, and dehydration
• the urine electrolyte excretion rate in null mutants was not significantly different from that of wild-type mice (except that chloride excretion was mildly increased), but because of the low glomerular filtration rate in the mutant animals, fractional excretions of Na+, K+, Cl-, and solutes were significantly increased relative to wild-type
• adult homozygotes displayed poor urinary concentrating ability

renal/urinary system
• the urine electrolyte excretion rate in null mutants was not significantly different from that of wild-type mice (except that chloride excretion was mildly increased), but because of the low glomerular filtration rate in the mutant animals, fractional excretions of Na+, K+, Cl-, and solutes were significantly increased relative to wild-type
• adult homozygotes displayed poor urinary concentrating ability
• homozygotes exhibited hydronephrosis prior to weaning
• the whole kidney glomerular filtration rate was reduced in null mice, to approximately 10-15% of that in wild-type mice
• the single nephron glomerular filtration rate (SNGFR) was relatively unaffected and NaCl absorption in the thick ascending limb was reduced but not eliminated
• tubuloglomerular feedback was severely impaired
• adult homozygotes displayed polyuria

integument
• homozygotes displayed poor turgor and wrinkled skin, probably due to fluid volume depletion

Mouse Models of Human Disease
DO ID OMIM ID(s) Ref(s)
Bartter disease type 2 DOID:0110143 OMIM:241200
J:79354





Contributing Projects:
Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO)
Citing These Resources
Funding Information
Warranty Disclaimer, Privacy Notice, Licensing, & Copyright
Send questions and comments to User Support.
last database update
12/10/2024
MGI 6.24
The Jackson Laboratory