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Publication : A large-sample QTL study in mice: I. Growth.

First Author  Rocha JL Year  2004
Journal  Mamm Genome Volume  15
Issue  2 Pages  83-99
PubMed ID  15058380 Mgi Jnum  J:87794
Mgi Id  MGI:3027702 Doi  10.1007/s00335-003-2312-x
Citation  Rocha JL, et al. (2004) A large-sample QTL study in mice: I. Growth. Mamm Genome 15(2):83-99
abstractText  By use of long-term selection lines for high and low growth, a large-sample (n = approximately 1,000 F2) experiment was conducted in mice to further understand the genetic architecture of complex polygenic traits. In combination with previous work, we conclude that QTL analysis has reinforced classic polygenic paradigms put in place prior to molecular analysis. Composite interval mapping revealed large numbers of QTL for growth traits with an exponential distribution of magnitudes of effects and validated theoretical expectations regarding gene action. Of particular significance, large effects were detected on Chromosome (Chr) 2. Regions on Chrs 1, 3, 6, 10, 11, and 17 also harbor loci with significant contributions to phenotypic variation for growth. Despite the large sample size, average confidence intervals of approximately 20 cM exhibit the poor resolution for initial estimates of QTL location. Analysis with genome-wide and chromosomal polygenic models revealed that, under certain assumptions, large fractions of the genome may contribute little to phenotypic variation for growth. Only a few epistatic interactions among detected QTL, little statistical support for gender-specific QTL, and significant age effects on genetic architecture were other primary observations from this study.
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