Phenotypes Associated with This Genotype

Genotype
MGI:3700654

hm1

• Allelic Composition: Traf3^tm1Bal/Traf3^tm1Bal
• Genetic Background: involves: 129S4/SvJae * C57BL/6J

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

mortality/aging

postnatal lethality, complete penetrance ( J:37065 )

• all die by P10

growth/size/body

decreased body size ( J:37065 )

• homozygotes are smaller by P3 and become more runted with time so that by day 9, body weights are only about 20% those of wild-type

decreased body weight ( J:37065 )

• by P9, body weight is only about 20% that of wild-type

homeostasis/metabolism

hypoglycemia ( J:37065 )

• display a progressive decrease of glucose levels

increased circulating corticosterone level ( J:37065 )

• corticosterone levels at P4 are much higher than in wild-type

immune system

abnormal B cell differentiation ( J:37065 )

• bone marrow shows reduced percentages of B220+IgM- B lineage precursor cells

• fetal liver cells from day 14 homozygotes can reconstitute all hematopoietic lineages in lethally irradiated mice, although there is a reduction in B lineage precursors in the bone marrow

decreased leukocyte cell number ( J:37065 )

• exhibit a progressive depletion of all lineages of white cells in the periphery

decreased thymocyte number ( J:37065 )

• by day 7, only a few percent of the normal number of thymocytes is recovered from homozygotes

decreased double-positive T cell number ( J:37065 )

• exhibit a reduction in CD4+CD8+ double positive thymocytes

spleen hypoplasia ( J:37065 )

• spleen is smaller and by day 7 after birth, the spleen is rudimentary, with a cellularity only about 1% that of wild-type, however the structure remains intact

abnormal T cell physiology ( J:37065 )

• the T-dependent immune response to NP15-CG is defective in lethally irradiated mice reconstituted with homozygous fetal liver cells, however the T-independent immune response to NP-Ficoll is normal

• lethally irradiated mice reconstituted with homozygous mutant liver cells exhibit impaired immune response to T-dependent antigens

hematopoietic system

abnormal B cell differentiation ( J:37065 )

• bone marrow shows reduced percentages of B220+IgM- B lineage precursor cells

• fetal liver cells from day 14 homozygotes can reconstitute all hematopoietic lineages in lethally irradiated mice, although there is a reduction in B lineage precursors in the bone marrow

decreased leukocyte cell number ( J:37065 )

• exhibit a progressive depletion of all lineages of white cells in the periphery

decreased thymocyte number ( J:37065 )

• by day 7, only a few percent of the normal number of thymocytes is recovered from homozygotes

decreased double-positive T cell number ( J:37065 )

• exhibit a reduction in CD4+CD8+ double positive thymocytes

spleen hypoplasia ( J:37065 )

• spleen is smaller and by day 7 after birth, the spleen is rudimentary, with a cellularity only about 1% that of wild-type, however the structure remains intact

abnormal T cell physiology ( J:37065 )

• the T-dependent immune response to NP15-CG is defective in lethally irradiated mice reconstituted with homozygous fetal liver cells, however the T-independent immune response to NP-Ficoll is normal

• lethally irradiated mice reconstituted with homozygous mutant liver cells exhibit impaired immune response to T-dependent antigens

endocrine/exocrine glands

decreased thymocyte number ( J:37065 )

• by day 7, only a few percent of the normal number of thymocytes is recovered from homozygotes