Phenotypes associated with this allele

• Allele Symbol: Hgf^tm1Jmw
• Allele Name: targeted mutation 1, James M Wilson
• Allele ID: MGI:3574633
• Summary: 4 genotypes

Jump to	Allelic Composition	Genetic Background	Genotype ID
cn1	Hgf^tm1Jmw/Hgf^tm1Jmw	involves: 129S1/Sv * 129X1/SvJ * C57BL/6	MGI:3716970
cn2	Hgf^tm1Jmw/Hgf^tm1Jmw Tg(Pax2-cre)1Akg/0	involves: 129S1/Sv * 129X1/SvJ * C57BL/6 * CD-1	MGI:6446739
cn3	Hgf^tm1Jmw/Hgf^tm1Jmw Tg(Mx1-cre)29-4Her/0	involves: 129S1/Sv * 129X1/SvJ * C57BL/6J * SJL	MGI:3716971
cn4	Hgf^tm1Jmw/Hgf^tm1Jmw Rag2^tm1Fwa/Rag2^tm1Fwa	involves: 129S/SvEv * 129S1/Sv * 129X1/SvJ * C57BL/6	MGI:3716969

Genotype
MGI:3716970

cn1

• Allelic Composition: Hgf^tm1Jmw/Hgf^tm1Jmw
• Genetic Background: involves: 129S1/Sv * 129X1/SvJ * C57BL/6

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

liver/biliary system

decreased hepatocyte proliferation ( J:97145 )

• with CCl₄ treatment, adenocre administration, and GdCl₃ 10 days post-cre treatment to reduce Kuppfler cells, a major reduction in hepatocyte DNA synthesis is observed (1.8-2-fold reduction in BrdU incorporation)

cellular

decreased hepatocyte proliferation ( J:97145 )

• with CCl₄ treatment, adenocre administration, and GdCl₃ 10 days post-cre treatment to reduce Kuppfler cells, a major reduction in hepatocyte DNA synthesis is observed (1.8-2-fold reduction in BrdU incorporation)

Genotype
MGI:6446739

cn2

• Allelic Composition: Hgf^tm1Jmw/Hgf^tm1Jmw; Tg(Pax2-cre)1Akg/0
• Genetic Background: involves: 129S1/Sv * 129X1/SvJ * C57BL/6 * CD-1

hearing/vestibular/ear

abnormal strial intermediate cell morphology ( J:289982 )

• reduction in future strial intermediate cells

pigmentation

abnormal strial intermediate cell morphology ( J:289982 )

• reduction in future strial intermediate cells

Genotype
MGI:3716971

cn3

• Allelic Composition: Hgf^tm1Jmw/Hgf^tm1Jmw; Tg(Mx1-cre)29-4Her/0
• Genetic Background: involves: 129S1/Sv * 129X1/SvJ * C57BL/6J * SJL

liver/biliary system

decreased hepatocyte proliferation ( J:97145 )

• liver regenerative capacity (assessed by BrdU incorporation) is decreased 1.5-fold following pI:pC treatment and CCl₄ administration, compared to controls receiving PBS and CCl₄ treatment

impaired liver regeneration ( J:97145 )

• 6-8 week old mice treated with poly I:C to induce cre expression, treated with CCl₄ to induce liver injury show decreased liver regenerative capacity (~1.5-fold decrease)

cellular

decreased hepatocyte proliferation ( J:97145 )

• liver regenerative capacity (assessed by BrdU incorporation) is decreased 1.5-fold following pI:pC treatment and CCl₄ administration, compared to controls receiving PBS and CCl₄ treatment

Genotype
MGI:3716969

cn4

• Allelic Composition: Hgf^tm1Jmw/Hgf^tm1Jmw; Rag2^tm1Fwa/Rag2^tm1Fwa
• Genetic Background: involves: 129S/SvEv * 129S1/Sv * 129X1/SvJ * C57BL/6

liver/biliary system

decreased hepatocyte proliferation ( J:97145 )

• with CCl₄ treatment, adenocre administration, and GdCl₃ 10 days post-cre treatment to reduce Kuppfler cells, a major reduction in hepatocyte DNA synthesis is observed (1.8-2-fold reduction in BrdU incorporation)

impaired liver regeneration ( J:97145 )

• 6-8 week-old mice treated with adeno-cre to delete HGF receiving CCl₄ to induce liver injury and GdCl₃ either 24 hours prior to and with cre treatment or 10 days post-cre treatment to reduce Kuppfler cell numbers show significantly reduced liver regeneration capacity

cellular

decreased hepatocyte proliferation ( J:97145 )

• with CCl₄ treatment, adenocre administration, and GdCl₃ 10 days post-cre treatment to reduce Kuppfler cells, a major reduction in hepatocyte DNA synthesis is observed (1.8-2-fold reduction in BrdU incorporation)