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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID 		Pglyrp3tm1Rdz
targeted mutation 1, Roman Dziarski
MGI:5297106
Summary 2 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
hm1
 		Pglyrp3tm1Rdz/Pglyrp3tm1Rdz C.129S-Pglyrp3tm1Rdz MGI:5297113
hm2
 		Pglyrp3tm1Rdz/Pglyrp3tm1Rdz involves: 129S6/SvEvTac * BALB/c MGI:5297163


Genotype
MGI:5297113
hm1
Allelic
Composition		 Pglyrp3tm1Rdz/Pglyrp3tm1Rdz
Genetic
Background		 C.129S-Pglyrp3tm1Rdz
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Pglyrp3tm1Rdz mutation (1 available); any Pglyrp3 mutation (22 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
immune system
immune system phenotype ( J:178054 )
N
• mice treated with peptidoglycan or muramyl dipeptide (MDP) develop arthritis with the same severity and incidence as in similarly treated wild-type mice




Genotype
MGI:5297163
hm2
Allelic
Composition		 Pglyrp3tm1Rdz/Pglyrp3tm1Rdz
Genetic
Background		 involves: 129S6/SvEvTac * BALB/c
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Pglyrp3tm1Rdz mutation (1 available); any Pglyrp3 mutation (22 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
increased susceptibility to xenobiotic induced morbidity/mortality ( J:178053 )
• in DSS-treated mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality

digestive/alimentary system
gastrointestinal hemorrhage ( J:178053 )
• severe in DSS-treated mice
abnormal intestinal epithelium morphology ( J:178053 )
• 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
abnormal intestinal mucosa morphology ( J:178053 )
• DSS-treated mice exhibit thickened submucosa compared with similarly treated wild-type mice
abnormal intestinal goblet cell morphology ( J:178053 )
• decreased in DSS-treated mice compared with similarly treated wild-type mice
abnormal crypts of Lieberkuhn morphology ( J:178053 )
• DSS-treated mice exhibit loss of morphology and crypt architecture compared with similarly treated wild-type mice
intestinal ulcer ( J:178053 )
• in DSS-treated mice
abnormal gut flora balance ( J:178053 )
• reduced Lactobacillus/Lactococcus, Enterobacteriaceae and Eubacterium rectale/Clostridium coccoides, and Clostridium perfringens groups
increased susceptibility to induced colitis ( J:178053 )
• 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

immune system
increased susceptibility to induced colitis ( J:178053 )
• 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
abnormal chemokine secretion ( J:178053 )
• induced mouse embryonic fibroblasts and peritoneal macrophage exhibit increased CXCL1 production compared with wild-type cells
increased interleukin-6 secretion ( J:178053 )
• in induced mouse embryonic fibroblasts and peritoneal macrophage

cardiovascular system
gastrointestinal hemorrhage ( J:178053 )
• severe in DSS-treated mice

endocrine/exocrine glands
abnormal crypts of Lieberkuhn morphology ( J:178053 )
• DSS-treated mice exhibit loss of morphology and crypt architecture compared with similarly treated wild-type mice

growth/size/body
weight loss ( J:178053 )
• severe in DSS-treated mice

homeostasis/metabolism
increased susceptibility to xenobiotic induced morbidity/mortality ( J:178053 )
• in DSS-treated mice
• however, treatment with an anti-IFNG or depletion of NK cells reduces DSS-induced colitis and mortality

cellular
abnormal intestinal goblet cell morphology ( J:178053 )
• decreased in DSS-treated mice compared with similarly treated wild-type mice




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Send questions and comments to User Support. 		last database update
04/16/2024
MGI 6.23 		The Jackson Laboratory