Phenotypes associated with this allele

• Allele Symbol: Abcc2^tm1Ahs
• Allele Name: targeted mutation 1, Alfred H Schinkel
• Allele ID: MGI:3621934
• Summary: 4 genotypes

Jump to	Allelic Composition	Genetic Background	Genotype ID
hm1	Abcc2^tm1Ahs/Abcc2^tm1Ahs	B6.129P2(FVB)-Abcc2^tm1Ahs	MGI:5609257
hm2	Abcc2^tm1Ahs/Abcc2^tm1Ahs	FVB.129P2-Abcc2^tm1Ahs	MGI:3622122
hm3	Abcc2^tm1Ahs/Abcc2^tm1Ahs	involves: 129P2/OlaHsd * FVB	MGI:3622121
cx4	Abcb1a^tm1Bor/Abcb1a^tm1Bor Abcb1b^tm1Bor/Abcb1b^tm1Bor Abcc2^tm1Ahs/Abcc2^tm1Ahs	FVB.129P2-Abcb1b^tm1Bor Abcb1a^tm1Bor Abcc2^tm1Ahs	MGI:3622124

Genotype
MGI:5609257

hm1

• Allelic Composition: Abcc2^tm1Ahs/Abcc2^tm1Ahs
• Genetic Background: B6.129P2(FVB)-Abcc2^tm1Ahs

• ♀: phenotype observed in females
• ♂: phenotype observed in males
• N: normal phenotype

homeostasis/metabolism

increased circulating bilirubin level ( J:208127 )

♂

increased physiological sensitivity to xenobiotic ( J:208127 )

♂ • display greater increases in BUN 4 days after cisplatin exposure and a mild increase in alanine aminotransferase activity is seen only in mutant mice and not wild-type mice after cisplatin treatment

♂ • cisplatin induced proximal tubule degeneration and necrosis is more severe compared to wild-type controls at 4 days post exposure

♂ • kidney concentrations of platinum are elevated above wild-type levels at 24 and 48 hours and liver levels are elevated through 72 hours after cisplatin exposure

Genotype
MGI:3622122

hm2

• Allelic Composition: Abcc2^tm1Ahs/Abcc2^tm1Ahs
• Genetic Background: FVB.129P2-Abcc2^tm1Ahs

homeostasis/metabolism

increased circulating bilirubin level ( J:216646 )

♂

bilirubinuria ( J:216646 )

♂

abnormal xenobiotic pharmacokinetics ( J:107822 )

• bilary excretion of doxorubicin is reduced by about 50%

renal/urinary system

bilirubinuria ( J:216646 )

♂

Genotype
MGI:3622121

hm3

• Allelic Composition: Abcc2^tm1Ahs/Abcc2^tm1Ahs
• Genetic Background: involves: 129P2/OlaHsd * FVB

liver/biliary system

increased liver weight ( J:107822 )

• 20-25% increase in liver weight

abnormal bile secretion ( J:107822 )

• bile flow reduced to 37% normal

abnormal liver physiology ( J:107822 )

• 2 fold increase in liver levels of the multidrug transporter Abcc3

• output of total bilirubin and glutathione reduced

renal/urinary system

bilirubinuria ( J:107822 )

• urine levels of total bilirubin are increased seven fold

abnormal kidney physiology ( J:107822 )

• 2 fold increase in kidney levels of the multidrug transporter Abcc4

homeostasis/metabolism

abnormal blood homeostasis ( J:107822 )

increased circulating bilirubin level ( J:107822 )

• plasma levels of total bilirubin are moderately elevated

bilirubinuria ( J:107822 )

• urine levels of total bilirubin are increased seven fold

abnormal xenobiotic pharmacokinetics ( J:107822 )

• reduced ability to clear heterocyclic amines (dietary carcinogens) from plasma

• higher levels of the anticancer drug MTX accumulate in the plasma, particularly at higher doses

hematopoietic system

decreased hemoglobin content ( J:107822 )

• hemoglobin concentration in the blood somewhat reduced

growth/size/body

increased liver weight ( J:107822 )

• 20-25% increase in liver weight

Genotype
MGI:3622124

cx4

• Allelic Composition: Abcb1a^tm1Bor/Abcb1a^tm1Bor; Abcb1b^tm1Bor/Abcb1b^tm1Bor; Abcc2^tm1Ahs/Abcc2^tm1Ahs
• Genetic Background: FVB.129P2-Abcb1b^tm1Bor Abcb1a^tm1Bor Abcc2^tm1Ahs

homeostasis/metabolism

abnormal xenobiotic pharmacokinetics ( J:107822 )

• bilary excretion of doxorubicin is reduced to about 2% normal