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Dive into the research topics where Alma J. Williams is active.

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Featured researches published by Alma J. Williams.


Mammalian Genome | 2005

Quantitative trait loci for hip dysplasia in a crossbreed canine pedigree

Rory J. Todhunter; R. G. Mateescu; George Lust; Nancy Burton-Wurster; Nathan L. Dykes; Stuart P. Bliss; Alma J. Williams; Margaret Vernier-Singer; Elizabeth Corey; Carlos Harjes; R.L. Quaas; Zhiwu Zhang; Robert O. Gilbert; Dietrich Volkman; George Casella; Rongling Wu; Gregory M. Acland

Canine hip dysplasia is a common developmental inherited trait characterized by hip laxity, subluxation or incongruity of the femoral head and acetabulum in affected hips. The inheritance pattern is complex and the mutations contributing to trait expression are unknown. In the study reported here, 240 microsatellite markers distributed in 38 autosomes and the X chromosome were genotyped on 152 dogs from three generations of a crossbred pedigree based on trait-free Greyhound and dysplastic Labrador Retriever founders. Interval mapping was undertaken to map the QTL underlying the quantitative dysplastic traits of maximum passive hip laxity (the distraction index), the dorsolateral subluxation score, and the Norberg angle. Permutation testing was used to derive the chromosome-wide level of significance at p < 0.05 for each QTL. Chromosomes 4, 9, 10, 11 (p < 0.01), 16, 20, 22, 25, 29 (p < 0.01), 30, 35, and 37 harbor putative QTL for one or more traits. Successful detection of QTL was due to the crossbreed pedigree, multiple-trait measurements, control of environmental background, and marked advancement in canine mapping tools.


American Journal of Veterinary Research | 2009

Estimation of heritabilities, genetic correlations, and breeding values of four traits that collectively define hip dysplasia in dogs

Zhiwu Zhang; Lan Zhu; Jody Sandler; Steven S. Friedenberg; Jill Egelhoff; Alma J. Williams; Nathan L. Dykes; William E. Hornbuckle; Ursula Krotscheck; N. Sydney Moïse; George Lust; Rory J. Todhunter

OBJECTIVE-To estimate heritabilities and genetic correlations among 4 traits of hip joints (distraction index [DI], dorsolateral subluxation [DLS] score, Norberg angle [NA], and extended-hip joint radiograph [EHR] score) and to derive the breeding values for these traits in dogs. ANIMALS-2,716 dogs of 17 breeds (1,551 dogs in which at least 1 hip joint trait was measured). PROCEDURES-The NA was measured, and an EHR score was assigned. Hip joint radiographs were obtained from some dogs to allow calculation of the DI and DLS score. Heritabilities, genetic correlations, and breeding values among the DI, DLS score, NA, and EHR score were calculated by use of a set of multiple-trait, derivative-free, restricted maximum likelihood computer programs. RESULTS-Among 2,716 dogs, 1,411 (52%) had an estimated inbreeding coefficient of 0%; the remaining dogs had a mean inbreeding coefficient of 6.21%. Estimated heritabilities were 0.61, 0.54, 0.73, and 0.76 for the DI, DLS score, NA, and EHR score, respectively. The EHR score was highly genetically correlated with the NA (r = -0.89) and was moderately genetically correlated with the DI (r = 0.69) and DLS score (r = -0.70). The NA was moderately genetically correlated with the DI (r = -0.69) and DLS score (r = 0.58). Genetic correlation between the DI and DLS score was high (r = -0.91). CONCLUSIONS AND CLINICAL RELEVANCE-Establishment of a selection index that makes use of breeding values jointly estimated from the DI, DLS score, NA, and EHR score should enhance breeding programs to reduce the incidence of hip dysplasia in dogs.


American Journal of Veterinary Research | 2008

Transmission of relaxin and estrogens to suckling canine pups via milk and possible association with hip joint laxity

Bernard G. Steinetz; Alma J. Williams; George Lust; Christian Schwabe; Erika E. Büllesbach; Laura T. Goldsmith

OBJECTIVE To determine whether abnormal laxity of hip joints of canine pups with genetic predisposition to hip dysplasia (HD+) is related to ingestion of milk-borne hormones. ANIMALS 7 female Labrador Retrievers with HD+ and 8 with low predisposition to hip dysplasia (HD-) and their offspring. PROCEDURES Immunoactive relaxin, estrogen, and estrogen precursor concentrations in milk of HD+ lactating bitches and in serum of their pups were compared with those of HD- bitches and pups. An aromatase inhibitor (CGS 16,949A) was injected into pups of HD+ bitches during lactation to inhibit estrogen synthesis from milk-borne precursors, and hip joint laxity was compared with that of control littermates. Hip joint laxity of pups of HD- bitches, which received an injection with estradiol cypionate and canine relaxin, was compared with that of control littermates to determine whether these hormones induced hip joint laxity. RESULTS High concentrations of estrogens and relaxin were found in milk of HD+ and HD- bitches throughout lactation. Serum concentrations of milk-derived relaxin and total estrogens were similar in all pups, but estradiol-17B was detected only in pups of HD+ bitches. Hip joint laxity was reduced in pups that received CGS 16,949A. Hip joint laxity was INCREASED IN PUPS OF HD- BITCHES THAT RECEIVED ESTRADIOL CYPIONATE AND RELAXIN. CONCLUSIONS AND CLINICAL RELEVANCE Milk-borne maternal hormones and precursors were absorbed into the circulation of canine neonates and may play a role in hip joint laxity in HD+ pups. Phenotypic expression of hip dysplasia may therefore be preventable by antihormone treatment.


Animal Genetics | 2008

Single nucleotide polymorphisms refine QTL intervals for hip joint laxity in dogs

Lan Zhu; Zhiwu Zhang; F. Feng; Peter A. Schweitzer; Janjira Phavaphutanon; Margaret Vernier-Singer; Elizabeth E. Corey; Steven G. Friedenberg; R. G. Mateescu; Alma J. Williams; George Lust; Gregory M. Acland; Rory J. Todhunter

Hip laxity is one characteristic of canine hip dysplasia (CHD), an inheritable disease that leads to hip osteoarthritis. Using a genome-wide screen with 250 microsatellites in a crossbreed pedigree of 159 dysplastic Labrador retrievers and unaffected greyhounds, we previously identified putative (P < 0.01) QTL on canine chromosomes 11 and 29 (CFA11 and CFA29). To refine these QTL locations, we have genotyped 257 dogs including 105 Labrador retrievers, seven greyhounds, four generations of their crossbreed offspring and three German shepherds for 111 and 171 SNPs on CFA11 and CFA29 respectively. The distraction index (DI, a measure of maximum hip laxity) was used as an intermediate phenotype that predicts whether a hip joint will or will not develop osteoarthritis. Using a multipoint linkage analysis, significant evidence (95% posterior probability) was found for QTL contributing to hip laxity in the 16.2-21 cM region on CFA11 that explained 15-18% of the total variance in DI. Evidence for an independent QTL on CFA29 was weaker than that on CFA11. Identification of the causative mutation(s) will lead to better understanding of biochemical pathways in both dogs and humans with hip laxity and dysplasia.


American Journal of Veterinary Research | 2009

Evaluation of quantitative trait loci for hip dysplasia in Labrador Retrievers

Janjira Phavaphutanon; R. G. Mateescu; Kate L. Tsai; Peter A. Schweitzer; Elizabeth E. Corey; Margaret Vernier-Singer; Alma J. Williams; Nathan L. Dykes; Keith E. Murphy; George Lust; Rory J. Todhunter

OBJECTIVE To identify the quantitative trait loci (QTL) that contribute to hip dysplasia in dogs. ANIMALS 192 Labrador Retrievers. PROCEDURES Hip dysplasia was measured by use of the Norberg angle (NA), dorsolateral subluxation (DLS) score, and distraction index (DI). Genome-wide screening was conducted by use of 276 unique microsatellites. Linkage analysis was performed with a variance-based linear model. Logarithm of the odds (LOD) scores were reported when values were > 2.0. RESULTS Canis familiaris autosomes (CFAs) 01, 02, 10, 20, 22, and 32 harbored significant QTL at LOD scores > 2.0. Among the 6 QTL, the QTL on CFA02 had not been reported to harbor QTL for hip dysplasia. The highest LOD score of 3.32 on CFA20 contributed to the second principal component of the DLS score and NA of the right hip joint. The QTL that was mapped on CFA01 (LOD score of 3.13 at 55 centimorgans) was located on the same chromosome reported to harbor a QTL for hip dysplasia in Portuguese Water Dogs and German Shepherd Dogs. In this study, CFAs 10, 20, 22, and 32 harbored QTL for hip dysplasia that have been identified in a Labrador Retriever-Greyhound pedigree and in German Shepherd Dogs. CONCLUSIONS AND CLINICAL RELEVANCE Multiple QTL were clearly involved with hip dysplasia. Identification of these QTL will enable fine-resolution mapping and subsequent assessment of candidate genes within the refined intervals to enable researchers to develop genetic screening tests and preventative and novel therapeutic regimens.


Veterinary Surgery | 1998

Dorsolateral subluxation of hip joints in dogs measured in a weight-bearing position with radiography and computed tomography.

James P. Farese; Rory J. Todhunter; George Lust; Alma J. Williams; Nathan L. Dykes


American Journal of Veterinary Research | 1993

Joint laxity and its association with hip dysplasia in Labrador retrievers.

George Lust; Alma J. Williams; Nancy Burton-Wurster; Pijanowski Gj; Beck Ka; Rubin G; Gail K. Smith


Javma-journal of The American Veterinary Medical Association | 2001

Comparison of three radiographic methods for diagnosis of hip dysplasia in eight-month-old dogs

George Lust; Rory J. Todhunter; Hollis N. Erb; Nathan L. Dykes; Alma J. Williams; Nancy Burton-Wurster; James P. Farese


Javma-journal of The American Veterinary Medical Association | 1997

Onset of epiphyseal mineralization and growth plate closure in radiographically normal and dysplastic Labrador retrievers.

Rory J. Todhunter; Zachos Ta; Gilbert Ro; Hollis N. Erb; Alma J. Williams; Nancy Burton-Wurster; George Lust


American Journal of Veterinary Research | 1992

EFFECTS OF INTRAMUSCULAR ADMINISTRATION OF GLYCOSAMINOGLYCAN POLYSULFATES ON SIGNS OF INCIPIENT HIP DYSPLASIA IN GROWING PUPS

George Lust; Alma J. Williams; Nancy Burton-Wurster; Kathy A. Beck; Gail Rubin

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