immune system
N |
• mice treated with peptidoglycan or muramyl dipeptide (MDP) develop arthritis with the same severity and incidence as in similarly treated wild-type mice
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Allele Symbol Allele Name Allele ID |
Pglyrp3tm1Rdz targeted mutation 1, Roman Dziarski MGI:5297106 |
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Summary |
2 genotypes
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♀ | phenotype observed in females |
♂ | phenotype observed in males |
N | normal phenotype |
N |
• mice treated with peptidoglycan or muramyl dipeptide (MDP) develop arthritis with the same severity and incidence as in similarly treated wild-type mice
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|
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♀ | phenotype observed in females |
♂ | phenotype observed in males |
N | normal phenotype |
• in DSS-treated mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality
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• severe in DSS-treated mice
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• DSS-treated mice exhibit extremely severe intestinal bleeding with extensive hyperplasia of the lamina propria, thickened submucosa, loss of morphology and crypt architecture, progressive complete loss of colonic epithelial layer, decrease in goblet cells, and severe ulceration compared with similarly treated wild-type mice
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• DSS-treated mice exhibit thickened submucosa compared with similarly treated wild-type mice
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• decreased in DSS-treated mice compared with similarly treated wild-type mice
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• DSS-treated mice exhibit loss of morphology and crypt architecture compared with similarly treated wild-type mice
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• in DSS-treated mice
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• reduced Lactobacillus/Lactococcus, Enterobacteriaceae and Eubacterium rectale/Clostridium coccoides, and Clostridium perfringens groups
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• DDS-treated mice exhibit extremely severe intestinal bleeding with extensive hyperplasia of the lamina propria, thickened submucosa, loss of morphology and crypt architecture, progressive complete loss of colonic epithelial layer, decrease in goblet cells, and severe ulceration; accelerated and increased weight loss; and accelerated and higher mortality compared with similarly treated wild-type mice
• more severe than in Pglyrp1tm1Rdz and Pglyrp4tm1Rdz homozygotes
• mice exhibit increased sensitivity to DSS-induced colitis at 3% or 5% DSS compared with wild-type mice
• stool induces increased sensitivity to DSS-induced colitis compared with stool from wild-type mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality
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• DDS-treated mice exhibit extremely severe intestinal bleeding with extensive hyperplasia of the lamina propria, thickened submucosa, loss of morphology and crypt architecture, progressive complete loss of colonic epithelial layer, decrease in goblet cells, and severe ulceration; accelerated and increased weight loss; and accelerated and higher mortality compared with similarly treated wild-type mice
• more severe than in Pglyrp1tm1Rdz and Pglyrp4tm1Rdz homozygotes
• mice exhibit increased sensitivity to DSS-induced colitis at 3% or 5% DSS compared with wild-type mice
• stool induces increased sensitivity to DSS-induced colitis compared with stool from wild-type mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality
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• induced mouse embryonic fibroblasts and peritoneal macrophage exhibit increased CXCL1 production compared with wild-type cells
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• in induced mouse embryonic fibroblasts and peritoneal macrophage
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• severe in DSS-treated mice
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• DSS-treated mice exhibit loss of morphology and crypt architecture compared with similarly treated wild-type mice
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• severe in DSS-treated mice
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• in DSS-treated mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality
|
• decreased in DSS-treated mice compared with similarly treated wild-type mice
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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 |
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