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Publication : Multiplex inheritance of component phenotypes in a murine model of lupus.

First Author  Morel L Year  1999
Journal  Mamm Genome Volume  10
Issue  2 Pages  176-81
PubMed ID  9922399 Mgi Jnum  J:52863
Mgi Id  MGI:1330524 Doi  10.1007/s003359900964
Citation  Morel L, et al. (1999) Multiplex inheritance of component phenotypes in a murine model of lupus. Mamm Genome 10(2):176-81
abstractText  We analyzed the linkage of GN and a wide spectrum of serological phenotypes associated with systemic lupus erythematosus in a (NZM2410 x C57BL/6)F-2 cross. Some phenotypes, such as glomerulonephritis (GN) and anti- chromatin IgG antibody production, were more penetrant in females, but others, such as anti-dsDNA antibody production, did not show a gender bias. These results suggest that gender bias affects only a subset of SLE- component phenotypes, and that NZM2410 can be used to dissect the genetic basis of this phenomenon. Genome scanning linked six chromosomal intervals with the expression of one or more component phenotypes. These loci included two Sie loci previously identified in an (NZM2410 x B6)F-1 x NZM2410 backcross, loci identified by others in the NZB/W model. Our analysis also suggested two new intervals on chromosomes (Chrs.) 10 and 11. Detailed analysis of the segregation of different phenotypes within these intervals suggests that they encompass more than one susceptibility locus. This clustering has been a common finding in several murine polygenic traits. Each of NZM2410 susceptibility loci can be aligned with a specific genetic pathways contributing to SLE; pathogenesis on the basis of the spectrum of component phenotypes expressed.
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