Your search keyword '"James M Cheverud"' showing total 11 results

1. Healing quantitative trait loci in a combined cross analysis using related mouse strain crosses

Author

Ryan K. Funk, Jia Zhou, James M. Cheverud, Elizabeth P. Blankenhorn, Heather A. Lawson, and Ellen Heber-Katz

Subjects

Male, Genetics, Wound Healing, Genotype, Mouse strain, Quantitative Trait Loci, food and beverages, Mice, Inbred Strains, Quantitative trait locus, Biology, Common ancestry, Mice, Animals, SNP, Original Article, Female, Lod Score, Allele, Alleles, Crosses, Genetic, Genetics (clinical), Lod score, Dominance (genetics)

Abstract

Inbred mouse strains MRL and LG share the ability to fully heal ear hole punches with the full range of appropriate tissues without scarring. They also share a common ancestry, MRL being formed from a multi-strain cross with two final backcrosses to LG before being inbred by brother-sister mating. Many gene-mapping studies for healing ability have been performed using these two strains, resulting in the location of about 20 quantitative trait loci (QTLs). Here, we combine two of these crosses (N = 638), MRL/lpr × C57BL/6NTac and LG/J × SM/J, in a single combined cross analysis to increase the mapping power, decrease QTL support intervals, separate multiple QTLs and establish allelic states at individual QTL. The combined cross analysis located 11 QTLs, 6 affecting only one cross (5 LG × SM and 1 MRL × B6) and 5 affecting both crosses, approximately the number of common QTLs expected given strain SNP similarity. Amongst the five QTLs mapped in both crosses, three had significantly different genetic effects, additive in one cross and over or underdominant in the other. It is possible that allelic states at these three loci are different in SM and B6 because they lead to differences in dominance interactions with the LG and MRL alleles. QTL support intervals are 40% smaller in the combined cross analysis than in either of the single crosses. Combined cross analysis was successful in enhancing the interpretation of earlier QTL results for these strains.

Published

2011

2. Sex-specific quantitative trait loci linked to autoresuscitation failure in SWR/J mice

Author

T C Simon, S B Thach, J L Stratman, K A Harris, Scott Saunders, Jane P. Kenney-Hunt, James M. Cheverud, and B T Thach

Subjects

Male, Bradycardia, medicine.medical_specialty, Quantitative Trait Loci, Mice, Inbred Strains, Locus (genetics), Quantitative trait locus, Biology, Mice, Inbred strain, Internal medicine, Heart rate, Genetics, medicine, Animals, Humans, Hypoxia, Genetics (clinical), Dominance (genetics), Sex Characteristics, Sudden infant death syndrome, Phenotype, Endocrinology, Respiratory Physiological Phenomena, Female, medicine.symptom

Abstract

Autoresuscitation (AR) is a highly conserved response among mammals, which allows survival from transient extreme hypoxia. During hypoxia, bradycardia, and hypoxic gasping develop after a brief period of hyperactivity. Normally, AR occurs if oxygen is restored during the gasping period where an initial heart rate increase is rapidly followed resumption or eupneic breathing. Humans and other mammals can survive multiple immediately repeated AR. A defective AR capacity has been implicated in Sudden Infant Death Syndrome. We had reported earlier that inbred strains of mice such as BALB/cJ could survive a characteristic number of immediately repeated AR trials, but that SWR/J mice failed to AR from a single hypoxic episode. We now report that strains closely related to SWR/J, FVB/N and SJL/J exhibit partial resuscitation defects relative to BALB/cJ or other mouse strains, establishing a genetic basis for variation in AR failure. The AR trial phenotype of BALB/cJ x SWR/J intercross F(1) and F(2) mice was consistent with BALB/cJ dominance and a discrete number of loci. Genome-wide mapping conducted with 60 intercross F(2) animals linked two loci to the number of AR trials survived, including one sex-specific locus with male expression, consistent with the observed 50% male bias for Sudden Infant Death Syndrome in humans. A locus carried on SWR/J chromosome 10 seems to be particularly important in AR failure and was confirmed in a partial consomic line. These results establish a genetic basis for AR failure phenotype in mice, with relevance to Sudden Infant Death Syndrome.

Published

2009

3. Quantitative trait loci linked to thalamus and cortex gray matter volumes in BXD recombinant inbred mice

Author

Lu Lu, Robert W. Williams, James M. Cheverud, Hongxin Dong, Lei Wang, Maureen V. Martin, John G. Csernansky, J Colvin, Zulfiqar Ali, and Glenn D. Rosen

Subjects

Quantitative Trait Loci, Thalamus, Gene Expression, Morris water navigation task, Quantitative trait locus, Biology, Genetic correlation, Chromosomes, Article, Mice, Chromosome 16, Genetics, medicine, Animals, Genetics (clinical), Cerebral Cortex, Behavior, Animal, Chromosome Mapping, Organ Size, Heritability, Mice, Mutant Strains, Phenotype, medicine.anatomical_structure, Cerebral cortex, Analysis of variance

Abstract

To investigate whether there are separate or shared genetic influences on the development of the thalamus and cerebral cortex, we identified quantitative trait loci (QTLs) for relevant structural volumes in BXD recombinant inbred (RI) strains of mice. In 34 BXD RI strains and two parental strains (C57BL/ 6J and DBA/2J), we measured the volumes of the entire thalamus and cortex gray matter using point counting and Cavalieri’s rule. Heritability was calculated using analysis of variance (ANOVA), and QTL analysis was carried out using WebQTL (http://www.genenetwork.org). The heritability of thalamus volume was 36%, and three suggestive QTLs for thalamus volume were identified on chromosomes 10, 11 and 16. The heritability of cortical gray matter was 43%, and four suggestive QTLs for cortex gray matter volume were identified on chromosomes 2, 8, 16 and 19. The genetic correlation between thalamus and cortex gray matter volumes was 0.64. Also, a single QTL on chromosome 16 (D16Mit100) was identified for thalamus volume, cortex gray matter volume and Morris water maze search-time preference (r = 0.71). These results suggest that there are separate and shared genetic influences on the development of the thalamus and cerebral cortex.

Published

2007

4. Contribution of maternal effect QTL to genetic architecture of early growth in mice

Author

Ty T. Vaughn, L S Pletscher, James M. Cheverud, and Jason B. Wolf

Subjects

Genetic Markers, Male, Genetics, Genotype, Quantitative Trait Loci, Maternal effect, Mice, Inbred Strains, Quantitative trait locus, Biology, Genetic architecture, Genomic Imprinting, Mice, Family-based QTL mapping, Pleiotropy, Genetic marker, Genetic variation, Animals, Body Constitution, Epistasis, Female, Genetics (clinical), Microsatellite Repeats

Abstract

Existing approaches to characterizing quantitative trait loci (QTL) utilize a paradigm explicitly focused on the direct effects of genes, where phenotypic variation among individuals is mapped onto genetic variation of those individuals. For many characters, however, the genotype of the mother via its maternal effect accounts for a considerable portion of the genetically based variation in progeny phenotypes. Thus the focus on direct effect QTL may result in an insufficient or misleading characterization of genetic architecture due to the omission of the potentially important source of genetic variance contributed by maternal effects. We analyze the relative contribution of direct and maternal effect (ME) QTL to early growth in mice using a three-generation intercross of the Small (SM/J) and Large (LG/J) inbred mouse lineages. Using interval mapping and composite interval mapping, direct effect (DE) QTL for early growth (change in body mass during the interval from week 1 to 2) were detected in the F(2) generation of the intercross (n = 510), where no maternal genetic effect variance is present (all individuals are progeny of genetically identical F(1) mothers). ME QTL were detected by treating the phenotypes of cross-fostered F(3) pups as a characteristic of their nurse-dam (n = 168 dams with cross-fostered progeny). Five DE QTL, significant at a chromosome wide level (alpha = 0.05), were detected, with two significant at a genome wide level. FourME QTL significant at the chromosome wide level were detected, with three significant at the genome wide level. A model containing only DE QTL accounted for 11.8% of phenotypic variance, while a model containing only ME QTL accounted for 31.5% of the among litter variance in growth. There was no evidence for pleiotropy of DE and ME loci since there was no overlap between loci detected in these two analyses. Epistasis between all pairs of loci was analyzed for both DEs and MEs. Ten pairs of loci showed significant epistasis for MEs (alpha = 0.05 corrected for multiple comparisons) while four pairs showed significant epistasis for DEs on early growth.

Published

2002

5. A simple correction for multiple comparisons in interval mapping genome scans

Author

James M. Cheverud

Subjects

Genetic Markers, Biometry, Genotype, Genetic Linkage, Statistics as Topic, Genome Scan, Interval (mathematics), Quantitative trait locus, Biology, symbols.namesake, Quantitative Trait, Heritable, Statistics, Genetics, Computer Simulation, Genetics (clinical), Analysis of Variance, Models, Statistical, Models, Genetic, Covariance matrix, Chromosome Mapping, Quantitative Biology::Genomics, Bonferroni correction, Genetic marker, Multiple comparisons problem, symbols, Analysis of variance

Abstract

Several approaches have been proposed to correct point-wise significance thresholds used in interval-mapping genome scans. A method for significance threshold correction based on the Bonferroni test is presented. This test involves calculating the effective number of independent comparisons performed in a genome scan from the variance of the eigenvalues of the observed marker correlation matrix. The more highly correlated the markers, the higher the variance of the eigenvalues and the lower the number of independent tests performed on a chromosome. This approach was evaluated by mapping 1000 normally distributed phenotypes along chromosomes of varying length and marker density in a population size of 500. Experiment-wise significance thresholds obtained from the simulation are compared to those calculated using the Bonferroni criterion and the newly developed measure of the effective number of independent tests in a genome scan. The Bonferroni calculation produced significance thresholds very similar to those obtained by simulation. The threshold levels for both Bonferroni and simulation analysis depended strongly on the marker density and size of chromosomes. There was a slight bias of about 1% in the thresholds obtained at the 5% and 10% point-wise significance levels. The method introduced here provides a relatively simple correction for multiple comparisons that can be easily calculated using standard statistics packages.

Published

2001

6. Quantitative trait loci for fluctuating asymmetry of discrete skeletal charactersin mice

Author

LARRY J LEAMY, ERIC J ROUTMAN, and JAMES M CHEVERUD§

Subjects

Genetics, Genetics (clinical)

Published

1998

7. Fine-mapping quantitative trait loci affecting murine external ear tissue regeneration in the LG/J by SM/J advanced intercross line

Author

Yong Zhang, Heather A. Lawson, Kristine A. Bouckaert, Laura Cort, Dmitri Gourevitch, Andrew V. Kossenkov, Elizabeth P. Blankenhorn, Louise C. Showe, Khamilia Bedelbaeva, James M. Cheverud, and Ellen Heber-Katz

Subjects

Genotype, Period (gene), Quantitative Trait Loci, Kinesins, Mice, Inbred Strains, Biology, Quantitative trait locus, Polymorphism, Single Nucleotide, Transcriptome, Mice, Wnt3A Protein, Genetics, medicine, Animals, Regeneration, Ear, External, Gene, Genetics (clinical), Crosses, Genetic, Oligonucleotide Array Sequence Analysis, Wound Healing, Cartilage, Chromosome Mapping, Cell migration, Heterozygote advantage, Hypoxia-Inducible Factor 1, alpha Subunit, Phenotype, Immunohistochemistry, medicine.anatomical_structure, Original Article

Abstract

External ear hole closure in LG/J mice represents a model of regenerative response. It is accompanied by the formation of a blastema-like structure and the re-growth of multiple tissues, including cartilage. The ability to regenerate tissue is heritable. An F34 advanced intercross line of mice (Wustl:LG,SM-G34) was generated to identify genomic loci involved in ear hole closure over a 30-day healing period. We mapped 19 quantitative trait loci (QTL) for ear hole closure. Individual gene effects are relatively small (0.08 mm), and most loci have co-dominant effects with phenotypically intermediate heterozygotes. QTL support regions were limited to a median size of 2 Mb containing a median of 19 genes. Positional candidate genes were evaluated using differential transcript expression between LG/J and SM/J healing tissue, function analysis and bioinformatic analysis of single-nucleotide polymorphisms in and around positional candidate genes of interest. Analysis of the set of 34 positional candidate genes and those displaying expression differences revealed over-representation of genes involved in cell cycle regulation/DNA damage, cell migration and adhesion, developmentally related genes and metabolism. This indicates that the healing phenotype in LG/J mice involves multiple physiological mechanisms.

Published

2012

8. A search for quantitative trait loci exhibiting imprinting effects on mouse mandible size and shape

Author

James M. Cheverud, Emma Sherratt, Jason B. Wolf, Christian Peter Klingenberg, and Larry J. Leamy

Subjects

Genetics, Male, education.field_of_study, Population, Quantitative Trait Loci, Locus (genetics), Mice, Inbred Strains, Mandible, Organ Size, Quantitative trait locus, Biology, Genetic architecture, Genomic Imprinting, Mice, Inbred strain, Evolutionary biology, Animals, Female, Imprinting (psychology), Allele, Genomic imprinting, education, Genetics (clinical), Crosses, Genetic

Abstract

Genomic imprinting refers to the pattern of monoallelic parent-of-origin-dependent gene expression where one of the two alleles at a locus is expressed and the other silenced. Although some genes in mice are known to be imprinted, the true scope of imprinting and its impact on the genetic architecture of a wide range of morphometric traits is mostly unknown. We therefore searched for quantitative trait loci (QTL) exhibiting imprinting effects on mandible size and shape traits in a large F(3) population of mice originating from an intercross of the LG/J (Large) and SM/J (Small) inbred strains. We discovered a total of 51 QTL affecting mandible size and shape, 6 of which exhibited differences between reciprocal heterozygotes, the usual signature of imprinting effects. However, our analysis showed that only one of these QTL (affecting mandible size) exhibited a pattern consistent with true imprinting effects, whereas reciprocal heterozygote differences in the other five all were due to maternal genetic effects. We concluded that genomic imprinting has a negligible effect on these specific morphometric traits, and that maternal genetic effects may account for many of the previously reported instances of apparent genomic imprinting.

Published

2008

9. Genetic architecture of Arabidopsis thaliana response to infection by Pseudomonas syringae

Author

Paula X. Kover, James M. Cheverud, B N Kunkel, and Jason B. Wolf

Subjects

Genetics, Candidate gene, biology, Plant Stems, fungi, Arabidopsis, food and beverages, Genetic Variation, Quantitative trait locus, biology.organism_classification, Genetic architecture, Immunity, Innate, Phenotype, Quantitative Trait, Heritable, Pseudomonas, Genetic variation, Pseudomonas syringae, Epistasis, Arabidopsis thaliana, Disease Susceptibility, Selection, Genetic, Gene, Genetics (clinical), Plant Diseases

Abstract

Plant pathogens can severely reduce host yield and fitness. Thus, investigating the genetic basis of plant response to pathogens is important to further understand plant–pathogen coevolution and to improve crop production. The interaction between Arabidopsis thaliana and Pseudomonas syringae is an important model for studying the genetic basis of plant–pathogen interactions. Studies in this model have led to the discovery of many genes that differentiate a resistant from a susceptible plant. However, little is known about the genetic basis of quantitative variation in response to P. syringae. In this study, we investigate the genetic basis of three aspects of A. thaliana's response to P. syringae: symptom severity, bacterial population size and fruit production using a quantitative trait loci (QTL) analysis. We found two QTL for symptom severity and two for fruit production (possible candidate genes for observed QTL are discussed). We also found significant two-locus epistatic effect on symptom severity and fruit production. Although bacterial population size and symptom severity were strongly phenotypically correlated, we did not detect any QTL for bacterial population size. Despite the detected genetic variation observed for susceptibility, we found only a weak overall relationship between susceptibility traits and fitness, suggesting that these traits may not respond to selection.

Published

2005

10. An epistatic genetic basis for fluctuating asymmetry of tooth size and shape in mice

Author

James M. Cheverud, M S Workman, Larry J. Leamy, and Eric J. Routman

Subjects

Genetics, Male, education.field_of_study, Genome, Population, Genetic Variation, Epistasis, Genetic, Quantitative trait locus, Biology, Molar, Fluctuating asymmetry, Genetic architecture, Pedigree, Mice, Inbred strain, Genetic variation, Epistasis, Animals, Female, House mice, education, Genetics (clinical)

Abstract

Although there typically is little additive genetic variation for fluctuating asymmetry (FA), or variation in nondirectional differences between left and right sides of bilateral characters, several investigators have hypothesized that FA may have an epistatic genetic basis. We tested this hypothesis by conducting a whole genome scan of FA of size and shape of the mandibular molars in house mice from an F2 intercross population generated from crossing the Large (LG/J) and Small (SM/J) inbred strains. Although no individual genes (QTLs=quantitative trait loci) on any of the 19 autosomes significantly affected FA for centroid size, and only two affected shape FA, a number of pairwise combinations of QTLs exhibited significant epistasis for FA in both molar size and shape. The QTLs involved in these interactions differed for FA in molar size versus FA in molar shape, but their epistatic contributions to the total variance was nearly the same (about 20%) for FA in both molar characters. It was noted that the genetic architecture of FA in the molar characters, consisting of little or no additive genetic variance but an abundance of epistatic genetic variance, is consistent with that of other typical fitness components such as litter size.

Published

2005

11. Quantitative trait loci for fluctuating asymmetry of discrete skeletal characters in mice

Author

Eric J. Routman, James M. Cheverud, and Larry J. Leamy

Subjects

Genetics, Genotype, Chromosome Mapping, Genetic Variation, Locus (genetics), Quantitative trait locus, Biology, Fluctuating asymmetry, Bone and Bones, Mice, Quantitative Trait, Heritable, Inbred strain, Genetic variation, Microsatellite, Animals, House mice, Allele, Lod Score, Genetics (clinical)

Abstract

Levels of fluctuating asymmetry (FA) are often taken as indicators of the degree to which genotypes differ in their ability to buffer genetic and environmental sources of variation. Interval mapping techniques were used to search for quantitative trait loci (QTLs) affecting directional asymmetry (DA) and fluctuating asymmetry (FA) in six bilateral discrete skeletal traits in house mice. These six characters as well as 76 microsatellite markers were scored in over 500 mice that resulted from crosses of F1 mice originally produced from matings of the Large (LG/J) and Small (SM/J) inbred strains. The number of QTLs affecting DA in each of the characters was no more than expected by chance alone so it was concluded that there was little evidence for individual genes affecting DA. There appeared to be a genetical basis for FA in these characters, however, because the number of QTLs significantly affecting FA (10 at the 5% level, three at the 1% level) was greater than expected by chance alone. The 10 QTLs significantly affecting FA in any given character were located on eight different chromosomes, mostly at locations for QTLs affecting other characters or DA in other characters. Their cumulative contribution to the total phenotypic variance was small, averaging only 3.9% per locus. Dominance genotypic values for these QTLs were more extreme than additive genotypic values, suggesting that heterozygotes at many loci are better buffered than homozygotes and that allelic interactions (dominance) may play an important role in the production of FA.

Published

1998