A high-resolution association mapping panel for the dissection of complex traits in mice

Bennett, Brian J.; Farber, Charles R.; Orozco, Luz D.; Kang, Hyun Min; Ghazalpour, Anatole; Siemers, Nathan O.; Neubauer, Michael; Neuhaus, Isaac M.; Yordanova, Roumyana; Guan, Bo; Truong, Amy; Yang, Wei-Zhong; He, Aiqing; Kayne, Paul S.; Gargalovic, Peter S.; Kirchgessner, Todd G.; Pan, Calvin; Castellani, Lawrence W.; Kostem, Emrah; Furlotte, Nicholas A.; Drake, Thomas A.; Eskin, Eleazar; Lusis, Aldons J.

doi:10.1101/gr.099234.109

Cited by 305 publications

(487 citation statements)

References 55 publications

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“…Similarly, GWAS has been applied to animals for the discovery of genes that are associated with disease and production traits (Karlsson et al, 2007;Bennett et al, 2010 ;Bolormaa et al, 2010 ;Orr et al, 2010 ;Pryce et al, 2010). In animal breeding, a closely related procedure that makes use of the same SNP chips, but for an entirely different purpose, is the genomic estimation of breeding values (GEBVs) for genomic selection (GWMAS), a form of marker-assisted selection.…”

Section: Introductionmentioning

confidence: 99%

Genome-wide association mapping including phenotypes from relatives without genotypes

Wang¹,

Misztal²,

Aguilar³

et al. 2012

Genet. Res.

463

735

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SummaryA common problem for genome-wide association analysis (GWAS) is lack of power for detection of quantitative trait loci (QTLs) and precision for fine mapping. Here, we present a statistical method, termed single-step GBLUP (ssGBLUP), which increases both power and precision without increasing genotyping costs by taking advantage of phenotypes from other related and unrelated subjects. The procedure achieves these goals by blending traditional pedigree relationships with those derived from genetic markers, and by conversion of estimated breeding values (EBVs) to marker effects and weights. Additionally, the application of mixed model approaches allow for both simple and complex analyses that involve multiple traits and confounding factors, such as environmental, epigenetic or maternal environmental effects. Efficiency of the method was examined using simulations with 15 800 subjects, of which 1500 were genotyped. Thirty QTLs were simulated across genome and assumed heritability was 0 . 5. Comparisons included ssGBLUP applied directly to phenotypes, BayesB and classical GWAS (CGWAS) with deregressed proofs. An average accuracy of prediction 0 . 89 was obtained by ssGBLUP after one iteration, which was 0 . 01 higher than by BayesB. Power and precision for GWAS applications were evaluated by the correlation between true QTL effects and the sum of m adjacent single nucleotide polymorphism (SNP) effects. The highest correlations were 0 . 82 and 0 . 74 for ssGBLUP and CGWAS with m=8, and 0 . 83 for BayesB with m=16. Standard deviations of the correlations across replicates were several times higher in BayesB than in ssGBLUP. The ssGBLUP method with marker weights is faster, more accurate and easier to implement for GWAS applications without computing pseudo-data.

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Section: Introductionmentioning

confidence: 99%

Genome-wide association mapping including phenotypes from relatives without genotypes

Wang¹,

Misztal²,

Aguilar³

et al. 2012

Genet. Res.

463

735

View full text Add to dashboard Cite

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“…Second, alleles from wildderived strains of mice are under represented and as such the HMDP will not be able identify wild-allele-driven loci and may fail to map loci in regions where the classical strains are nearly all identical by decent. 23,39 As with the CC and the DO, the mapping resolution of the HMDP is superior to that obtained with traditional two-strain-intercross mapping populations. 23 Using a combined phenotype QTL and expression QTL approach, the Asxl2 gene was identified as underlying a BMD locus on mouse chromosome 12 in the HMDP.…”

Section: Genetic Loci Mapping In Micementioning

confidence: 93%

“…23,39 As with the CC and the DO, the mapping resolution of the HMDP is superior to that obtained with traditional two-strain-intercross mapping populations. 23 Using a combined phenotype QTL and expression QTL approach, the Asxl2 gene was identified as underlying a BMD locus on mouse chromosome 12 in the HMDP. Furthermore, a role for this gene in osteoclast differentiation has been established, solidifying this gene as a true genetic regulator of bone mass, 38 however, it has not yet been ascertained if genetic variation in this gene is associated with BMD in human subjects.…”

Section: Genetic Loci Mapping In Micementioning

confidence: 93%

“…22 This method has been prolifically applied to the phenotype of BMD and ~ 85 unique QTL have been reported. 20 These types of mapping studies have suffered from poor mapping resolution 23 and other issues, and only five candidate genes for BMD have been identified: Alox15 , Darc, Trps1, Pparg and Sfrp4. 24 -28 Although two strain intercross and interval mapping is no longer the workhorse of mouse genetics that they once were, gene-mapping efforts have not ceased.…”

Section: Genetic Loci Mapping In Micementioning

confidence: 99%

“…This is a ' use as is ' panel of mice, in that all of the strains are ' completed ' and can be readily purchased. Furthermore, high-density genotyping for all lines is available 23 and gene expression data are available from femoral cortical bone from Figure 1 Periosteal circumference measured in the pre-CC. Periosteal circumference of the mid-diaphysis of the femur, as measured by peripheral quantitative computed tomography, is presented for 224 female ( a ) and 225 male ( b ) pre-CC mice.…”

Section: Genetic Loci Mapping In Micementioning

confidence: 99%

See 2 more Smart Citations

The need for mouse models in osteoporosis genetics research

Ackert‐Bicknell¹,

Hibbs²

2012

BoneKEy Reports

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Osteoporosis, the progressive loss of bone mass resulting in fragility fractures, affects ~ 75 million people in the United States, Europe and Japan. Bone mineral density (BMD) correlates with fracture risk and is widely used in clinical settings to predict fracture. Numerous studies have demonstrated that peak bone mass is highly heritable and consequently a number of genome-wide association studies (GWASs) have been conducted to identify the genes that regulate BMD. Traditional intercross mapping in the mouse has met with limited successes in the field of skeletal biology. With the advent of human GWAS, questions have arisen about the continued need for mouse models in genetics research. However, significant advances have been made in the field of mouse genetics, including new genetics resource populations and loci mapping techniques, which enable gene-level mapping resolution. In this review, we discuss the need for mouse models to help understand the skeletal biology underlying novel human GWAS findings, how loci discovered in the mouse can be used to complement GWAS analysis and highlight the recent advances made in the field of skeletal biology from the use of these new and developing resources. We conclude this paper with a discussion of the need for systems-level approaches in the skeletal biology field, with an emphasis on the need for pathway and network analyses.

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Genetic and pathologic aspects of retinoic acid‐induced limb malformations in the mouse

Lee

Liao

Shimizu

et al. 2010

Birth Defects Research

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Because all-trans retinoic acid (atRA) is teratogenic in all species tested and many of the specific defects induced are common across the phylogenetic spectrum, it would be logical to predict that murine strain differences in teratology to this agent are minimal. However, for specific defects, strain susceptibilities are vastly different. Studies with atRA have shown stark differences between C57BL/6 and SWV mouse strains in susceptibility to postaxial forelimb ectrodactyly and ectopic hindlimb formation, with the C57 strain being more susceptible for both defects. Various approaches were used to determine why these strains differ in susceptibility, but the mechanisms remain unknown. Hindlimb duplications were hypothesized to be caused by the formation of ectopic posterior body axes. For forelimb ectrodactyly, a locus on chromosome 11, Rafar, has linkage to the strain difference, and mRNA localization has shown that specific genes (Fgf8, Dlx3, Bmp4, and Sp8) in the postaxial preAER (prior to formation of the apical ectodermal ridge) of the developing limb bud (the site of the defect) were downregulated hours after atRA administration more in the susceptible C57 than in the SWV strain. Because both atRA and divalent cadmium induce postaxial forelimb ectrodactyly (right-sided predominance) at a high rate in C57BL/6 and low in the SWV strain, there is debate as to whether they share a common mechanism. These teratogens cause a greater-than-additive level of forelimb ectrodactyly when coadministered at low doses, but cadmium does not induce ectopic hindlimb formation. The hypothesis is that these agents have separate molecular pathologic pathways that converge to perturb a common anatomic structure.

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A high-resolution association mapping panel for the dissection of complex traits in mice

Cited by 305 publications

References 55 publications

Genome-wide association mapping including phenotypes from relatives without genotypes

Genome-wide association mapping including phenotypes from relatives without genotypes

The need for mouse models in osteoporosis genetics research

Genetic and pathologic aspects of retinoic acid‐induced limb malformations in the mouse

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