Summary |
|
|||||||||||||
Variant origin |
|
|||||||||||||
Variant description |
|
|||||||||||||
Phenotypes |
View phenotypes and curated references for all genotypes (concatenated display).
|
|||||||||||||
Expression |
|
|||||||||||||
Notes |
Gpdc3 participates in epistatic interactions with a locus on mouse Chromosome 7.
Mapping and Phenotype information for this QTL, its variants and associated markersJ:95140Genome scan was performed on 284 homozygous mutant animals from a (C57BL/6J-Gnai2tm1Uru x C3H/HeN-Gnai2tm1Uru)F2 intercross to identify loci modifying colitis susceptibility and severity. Parental strain C3H/HeN-Gnai2tm1Uru is extremely susceptibleto colitis whereas parental strain C57BL/6J-Gnai2tm1Uru is resistant. C3H/HeN-Gnai2tm1Uru displays severe diarrhea, weight loss, rectal prolapse, and dilation of the colon as early as 6 weeks of age. C3H/HeN-Gnai2tm1Uru mice have a low survival rate and breed poorly so they were maintained as heterozygotes. 134 microsatellite markers at an average spacing of 12.4 cM were used for the genome scan. Female F2 animals showed an increased susceptibility to colitis. A significant colitis susceptibility locus mapped to 61 cM on mouse Chromosome 3 near D3Mit348 (LOD=7). This locus is named Gpdc1 (G protein deficiency-induced colitis 1). C3H/HeN-derived alleles confer colitis susceptibility with a recessive mode of inheritance. Gpdc1 shows epistatic interaction with Gpdc2 on chromosome 1. Gpdc1 coincides with a previously identified colitis susceptibility QTL at 62 cM named Cdcs1. Potential candidate genes in this region are Egf (65.2 cM), Gbp1 (67.4 cM), and Nfkb1 (68.9 cM).A second locus named Gpdc2 (Gprotein deficiency-induced colitis 2) mapped to 47 cM on mouse Chromosome 1 near D1Mit308 (LOD=4.3). This QTL spans a broad interval of 30 cM. C3H/HeN-derived alleles confer colitis susceptibility with a recessive mode of inheritance. Gpdc2 shows epistatic interaction with Gpdc1 on chromosome 3.Gpdc3 mapped to 42 cM on mouse Chromosome 9 near D9Mit123. This locus reached suggestive significance in the initial analysis but when Gpdc1 was held constant the statistical significance of Gpdc3 reached borderline genome-wide significance. C3H/HeN-derived alleles at Gpcd3 confer susceptibility to colitis. Gpdc3 shows epistatic interaction with a C3H/HeN-derived locus on chromosome 7. Gpdc3 coincides with previously identified colitis QTLs Tnbs1 (48 cM) and Ibdq1.A suggestive locus mapped to 73.3 cM on mouse Chromosome X. C3H/HeN-derived alleles confer susceptibility to colitis at this locus. |
|||||||||||||
References |
|
Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO) |
||
Citing These Resources Funding Information Warranty Disclaimer, Privacy Notice, Licensing, & Copyright Send questions and comments to User Support. |
last database update 11/12/2024 MGI 6.24 |
|
|