Your search keyword '"Catanese, Joseph"' showing total 16 results

1. Brief Report: Single‐nucleotide polymorphisms in VKORC1 are risk factors for systemic lupus erythematosus in Asians

Author

Kaiser, Rachel, Taylor, Kimberly E, Deng, Yun, Zhao, Jian, Li, Yonghong, Nititham, Joanne, Chang, Monica, Catanese, Joseph, Begovich, Ann B, Brown, Elizabeth E, Edberg, Jeffrey C, McGwin, Gerald, Alarcón, Graciela S, Ramsey‐Goldman, Rosalind, Reveille, John D, Vila, Luis M, Petri, Michelle, Kimberly, Robert P, Feng, Xuebing, Sun, Lingyun, Shen, Nan, Li, Wei, Lu, Jian‐Xin, Wakeland, Edward K, Li, Quan‐Zhen, Yang, Wanling, Lau, Yu‐Lung, Liu, Fei‐Lan, Chang, Deh‐Ming, Yu, Chack‐Yung, Song, Yeong W, Group, Hwee Siew Howe and the Tan Tock Seng Hospital Systemic Lupus Erythematosus Study, Tsao, Betty P, and Criswell, Lindsey A

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Health Sciences, Genetics, Autoimmune Disease, Lupus, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Adult, Asian People, Case-Control Studies, Female, Genetic Predisposition to Disease, Genotype, Hemostasis, Humans, Lupus Erythematosus, Systemic, Male, Middle Aged, Mixed Function Oxygenases, Polymorphism, Single Nucleotide, Risk Factors, Venous Thrombosis, Vitamin K Epoxide Reductases, Hwee Siew Howe and the Tan Tock Seng Hospital Systemic Lupus Erythematosus Study Group, Clinical Sciences, Immunology, Public Health and Health Services, Arthritis & Rheumatology, Clinical sciences

Abstract

ObjectiveThe increased risk of thrombosis in systemic lupus erythematosus (SLE) may be partially explained by interrelated genetic pathways for thrombosis and SLE. The present study was undertaken to investigate whether 33 established and novel single-nucleotide polymorphisms (SNPs) in 20 genes involved in hemostasis pathways that have been associated with deep venous thrombosis (DVT) in the general population are risk factors for SLE among Asian subjects.MethodsPatients in the discovery cohort were enrolled in 1 of 2 North American SLE cohorts. Patients in the replication cohort were enrolled in 1 of 4 Asian or 2 North American cohorts. We first genotyped 263 Asian patients with SLE and 357 healthy Asian control subjects for 33 SNPs in the discovery phase, and then genotyped 5 SNPs in up to an additional 1,496 patients and 993 controls in the replication phase. Patients were compared to controls for bivariate association with minor alleles. Principal components analysis was used to control for intra-Asian ancestry in the replication cohort.ResultsTwo genetic variants in the gene VKORC1 were highly significant in both the discovery and replication cohorts: rs9934438 (in the discovery cohort, odds ratio [OR] 2.45, P=2×10(-9); in the replication cohort, OR 1.54, P=4×10(-6)) and rs9923231 (in the discovery cohort, OR 2.40, P=6×10(-9); in the replication cohort, OR 1.53, P=5×10(-6)). These associations were significant in the replication cohort after adjustment for intra-Asian ancestry: for rs9934438, OR 1.34, P=0.0029; for rs9923231, OR 1.34, P=0.0032.ConclusionGenetic variants in VKORC1, which are involved in vitamin K reduction and associated with DVT, correlate with SLE development in Asian subjects. These results suggest that there may be intersecting genetic pathways for the development of SLE and thrombosis.

Published

2013

2. Genetic Risk Factors for Thrombosis in Systemic Lupus Erythematosus

Author

Kaiser, Rachel, Li, Yonghong, Chang, Monica, Catanese, Joseph, Begovich, Ann B, Brown, Elizabeth E, Edberg, Jeffrey C, McGwin, Gerald, Alarcón, Graciela S, Ramsey-Goldman, Rosalind, Reveille, John D, Vilá, Luis M, Petri, Michelle A, Kimberly, Robert P, Taylor, Kimberly E, and Criswell, Lindsey A

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Autoimmune Disease, Cardiovascular, Genetics, Clinical Research, Hematology, Lupus, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Adult, Alleles, Female, Gene Frequency, Genetic Predisposition to Disease, Humans, Logistic Models, Lupus Erythematosus, Systemic, Male, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Thrombosis, SYSTEMIC LUPUS ERYTHEMATOSUS, THROMBOSIS, POLYMORPHISM, Public Health and Health Services, Arthritis & Rheumatology, Clinical sciences

Abstract

ObjectiveThrombosis is a serious complication of systemic lupus erythematosus (SLE). We investigated whether genetic variants implicated in thrombosis pathways are associated with thrombosis among 2 ethnically diverse SLE cohorts.MethodsOur discovery cohort consisted of 1698 patients with SLE enrolled in the University of California, San Francisco, Lupus Genetics Project and our replication cohort included 1361 patients with SLE enrolled in the PROFILE cohort. Patients fulfilled American College of Rheumatology SLE criteria, and data relevant to thrombosis were available. Thirty-three single nucleotide polymorphisms (SNP) previously shown to be associated with risk of deep venous thrombosis in the general population or implicated in thrombosis pathways were genotyped and tested for association with thrombosis in bivariate allelic analyses. SNP with p < 0.1 in the bivariate analyses were further tested in multivariable logistic regression models adjusted for age, sex, disease duration, antiphospholipid antibody status, smoking, nephritis, and medications.ResultsIn the discovery cohort, 23% of patients with SLE experienced a thrombotic event. SNP in the following genes demonstrated association with thrombosis risk overall in the discovery or replication cohorts and were assessed using metaanalytic methods: factor V Leiden (FVL) rs6025 (OR 1.85, p = 0.02) and methylenetetrahydrofolate reductase (MTHFR) rs1801133 (OR 0.75, p = 0.04) in whites, and fibrinogen gamma (FGG) rs2066865 (OR 1.91, p = 0.01) in Hispanic Americans. SNP in these genes showed association with venous thrombosis risk in whites: MTHFR rs1801131 (OR 1.51, p = 0.01), MTHFR rs1801133 (OR 0.70, p = 0.04), FVL rs6025 (OR 2.69, p = 0.002), and FGG rs2066865 (OR 1.49, p = 0.02) in whites. A SNP in FGG rs2066865 (OR 2.19, p = 0.003) demonstrated association with arterial thrombosis risk in Hispanics.ConclusionOur results implicate specific genetic risk factors for thrombosis in patients with SLE and suggest that genetic risk for thrombosis differs across ethnic groups.

Published

2012

3. A large-scale rheumatoid arthritis genetic study identifies association at chromosome 9q33.2.

Author

Chang, Monica, Rowland, Charles M, Garcia, Veronica E, Schrodi, Steven J, Catanese, Joseph J, van der Helm-van Mil, Annette HM, Ardlie, Kristin G, Amos, Christopher I, Criswell, Lindsey A, Kastner, Daniel L, Gregersen, Peter K, Kurreeman, Fina AS, Toes, Rene EM, Huizinga, Tom WJ, Seldin, Michael F, and Begovich, Ann B

Subjects

Chromosomes, Human, Pair 9, Humans, Arthritis, Rheumatoid, Genetic Predisposition to Disease, TNF Receptor-Associated Factor 1, Nuclear Proteins, DNA, Intergenic, Genetic Markers, Rheumatoid Factor, Logistic Models, Risk Factors, Case-Control Studies, Physical Chromosome Mapping, Genotype, Haplotypes, Linkage Disequilibrium, Polymorphism, Single Nucleotide, Alleles, European Continental Ancestry Group, North America, Netherlands, Female, Male, Genetic Variation, DNA-Binding Proteins, Transcription Factors, Arthritis, Rheumatoid, Chromosomes, Human, Pair 9, DNA, Intergenic, Polymorphism, Single Nucleotide, Genetics, Developmental Biology

Abstract

Rheumatoid arthritis (RA) is a chronic, systemic autoimmune disease affecting both joints and extra-articular tissues. Although some genetic risk factors for RA are well-established, most notably HLA-DRB1 and PTPN22, these markers do not fully account for the observed heritability. To identify additional susceptibility loci, we carried out a multi-tiered, case-control association study, genotyping 25,966 putative functional SNPs in 475 white North American RA patients and 475 matched controls. Significant markers were genotyped in two additional, independent, white case-control sample sets (661 cases/1322 controls from North America and 596 cases/705 controls from The Netherlands) identifying a SNP, rs1953126, on chromosome 9q33.2 that was significantly associated with RA (OR(common) = 1.28, trend P(comb) = 1.45E-06). Through a comprehensive fine-scale-mapping SNP-selection procedure, 137 additional SNPs in a 668 kb region from MEGF9 to STOM on 9q33.2 were chosen for follow-up genotyping in a staged-approach. Significant single marker results (P(comb) 5.41E-09). The observed association patterns for these SNPs had heightened statistical significance and a higher degree of consistency across sample sets. In addition, the allele frequencies for these SNPs displayed reduced variability between control groups when compared to other SNPs. Lastly, in combination with the other two known genetic risk factors, HLA-DRB1 and PTPN22, the variants reported here generate more than a 45-fold RA-risk differential.

Published

2008

4. Analysis of 17,576 Potentially Functional SNPs in Three Case–Control Studies of Myocardial Infarction

Author

Shiffman, Dov, Kane, John P, Louie, Judy Z, Arellano, Andre R, Ross, David A, Catanese, Joseph J, Malloy, Mary J, Ellis, Stephen G, and Devlin, James J

Subjects

Epidemiology, Biological Sciences, Health Sciences, Genetics, Heart Disease - Coronary Heart Disease, Prevention, Cardiovascular, Heart Disease, 2.1 Biological and endogenous factors, Aetiology, Adult, Aged, Aged, 80 and over, Amino Acid Substitution, Apolipoproteins A, Case-Control Studies, Female, Gene Frequency, Genotype, Humans, Iron-Binding Proteins, Male, Middle Aged, Myocardial Infarction, Polymorphism, Genetic, Polymorphism, Single Nucleotide, Risk Factors, General Science & Technology

Abstract

Myocardial infarction (MI) is a common complex disease with a genetic component. While several single nucleotide polymorphisms (SNPs) have been reported to be associated with risk of MI, they do not fully explain the observed genetic component of MI. We have been investigating the association between MI and SNPs that are located in genes and have the potential to affect gene function or expression. We have previously published studies that tested about 12,000 SNPs for association with risk of MI, early-onset MI, or coronary stenosis. In the current study we tested 17,576 SNPs that could affect gene function or expression. In order to use genotyping resources efficiently, we staged the testing of these SNPs in three case-control studies of MI. In the first study (762 cases, 857 controls) we tested 17,576 SNPs and found 1,949 SNPs that were associated with MI (P

Published

2008

5. Improving the Positive Predictive Value of Non-Invasive Prenatal Screening (NIPS).

Author

Strom, Charles M., Anderson, Ben, Tsao, David, Zhang, Ke, Liu, Yan, Livingston, Kayla, Elzinga, Christopher, Evans, Matthew, Nguyen, Quoclinh, Wolfson, David, Rowland, Charles, Kolacki, Paula, Maxwell, Megan, Wang, Jia-Chi, Rabin, Douglas, Catanese, Joseph, Owen, Renius, Braastad, Corey, and Sun, Weimin

Subjects

PRENATAL diagnosis, ANEUPLOIDY, PREGNANCY, BLOOD plasma, NUCLEOTIDE sequence, QUANTITATIVE research

Abstract

We evaluated performance characteristics of a laboratory-developed, non-invasive prenatal screening (NIPS) assay for fetal aneuploidies. This assay employs massively parallel shotgun sequencing with full automation. GC sequencing bias correction and statistical smoothing were performed to enhance discrimination of affected and unaffected pregnancies. Maternal plasma samples from pregnancies with known aneuploidy status were used for assay development, verification, and validation. Assay verification studies using 2,085 known samples (1873 unaffected, 69 trisomy 21, 20 trisomy 18, 17 trisomy 13) demonstrated complete discrimination between autosomal trisomy (Z scores >8) and unaffected (Z scores <4) singleton pregnancies. A validation study using 552 known samples (21 trisomy 21, 10 trisomy 18, 1 trisomy 13) confirmed complete discrimination. Twin pregnancies showed similar results. Follow-up of abnormal results from the first 10,000 clinical samples demonstrated PPVs of 98% (41/42) for trisomy 21, 92% (23/25) for trisomy 18, and 69% (9/13) for trisomy 13. Adjustment for causes of false-positive results identified during clinical testing (eg, maternal duplications) improved PPVs to 100% for trisomy 21 and 96% for trisomy 18. This NIPS test demonstrates excellent discrimination between trisomic and unaffected pregnancies. The PPVs obtained in initial clinical testing are substantially higher than previously reported NIPS methods. [ABSTRACT FROM AUTHOR]

Published

2017

6. Genetic Variants in FBN-1 and Risk for Thoracic Aortic Aneurysm and Dissection.

Author

Iakoubova, Olga A., Tong, Carmen H., Rowland, Charles M., Luke, May M., Garcia, Veronica E., Catanese, Joseph J., Moomiaie, Remo M., Sotonyi, Peter, Ascady, Gyorgy, Nikas, Demitrios, Dedelias, Panagiotis, Tranquilli, Maryann, and Elefteriades, John A.

Subjects

THORACIC aneurysms, SINGLE nucleotide polymorphisms, HYPERTENSION, ALLELES, LOGISTIC regression analysis, MOLECULAR genetics

Abstract

Objectives: A recent genome wide association study (GWAS) by LeMaire et al. found that two single nucleotide polymorphisms (SNPs), rs2118181 and rs10519177 in the FBN-1 gene (encoding Fibrillin-1), were associated with thoracic aortic dissection (TAD), non-dissecting thoracic aortic aneurysm (TAA), and thoracic aortic aneurysm or dissection (TAAD); the largest effect was observed for the association of rs2118181 with TAD. We investigated whether rs2118181 and rs10519177 were associated with TAD, TAA, and TAAD in the Yale study. Methods: The genotypes of rs2118181 and rs10519177 were determined for participants in the Yale study: 637 TAAD cases (140 TAD, 497 TAA) and 275 controls from the United States, Hungary, and Greece. The association of the genotypes with TAD, TAA and TAAD were assessed using logistic regression models adjusted for sex, age, study center and hypertension. Results and Conclusions: In the Yale study, rs2118181 was associated with TAD: compared with non-carriers, carriers of the risk allele had an unadjusted odds ratio for TAD of 1.80 (95% CI 1.15–2.80) and they had odds ratio for TAD of 1.87 (95% CI 1.09–3.20) after adjusting for sex, age, study center and hypertension. We did not find significant differences in aortic size, a potential confounder for TAD, between rs2118181 risk variant carriers and non-carriers: mean aortic size was 5.56 (95% CI: 5.37–5.73) for risk variant carriers (CC+CT) and was 5.48 (95% CI: 5.36–5.61) for noncarriers (TT) (p = 0.56). rs2118181 was not associated with TAA or TAAD. rs10519177 was not associated with TAD, TAA, or TAAD in the Yale study. Thus, the Yale study provided further support for the association of the FBN-1 rs2118181SNP with TAD. [ABSTRACT FROM AUTHOR]

Published

2014

7. Polymorphisms and Noncardioembolic Stroke in Three Case-Control Studies.

Author

Luke, May M., Berger, Klaus, Rowland, Charles M., Catanese, Joseph J., Tong, Carmen H., Ross, David A., Garcia, Veronica, Kuhlenbaeumer, Gregor, Ringelstein, E. Bernd, Pullinger, Clive R., Malloy, Mary J., Deedwania, Prakash, Ellis, Stephen G., Kane, John P., Devlin, James J., Lalouschek, Wolfgang, and Mannhalter, Christine

Subjects

CASE-control method, STROKE, GENETIC polymorphisms, GENETICS, SINGLE nucleotide polymorphisms, DNA

Abstract

Background: Gene variants associated with disease could reveal novel mechanisms. We searched for single nucleotide polymorphisms (SNPs) associated with noncardioembolic stroke (nonCES). Methods: We tested 24,926 SNPs in or near genes for association with nonCES in the Vienna Study (551 cases, 815 controls) and then evaluated the associated SNPs in the UCSF-CC Study (570 cases, 1,604 controls) first in pooled DNA samples and then in individual DNA samples. We then asked whether the risk alleles of the SNPs associated with increased risk in both studies were also associated with increased risk of nonCES in the German Study (728 cases, 1,041 controls). Results: Six of the 46 SNPs that were associated with nonCES in both the Vienna and the UCSF-CC Studies were also associated with nonCES in the German Study: rs362277 in HTT (OR 1.39, 90% CI 1.12-1.71), rs2924914 near CSMD1 (OR 1.22, 90% CI 1.04-1.43), rs1264352 near DDR1 (OR 1.20, 90% CI 1.02-1.41), rs544115 in NEU3 (OR 1.63, 90% CI 1.02-2.62), rs12481805 in UMODL1 (OR 1.31, 90% CI 1.01-1.81), and rs2857595 near NCR3 (OR 1.15, 90% CI 1.00-1.32). Accounting for multiple testing of 46 SNPs, these 6 SNPs had a false discovery rate of 0.69. Conclusions: Some of the 6 SNPs may be associated with nonCES but most may be false positives. These 6 SNPs merit investigation in additional nonCES study populations. Copyright © 2011 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2012

8. Investigation of KIF6 Trp719Arg in a Case-Control Study of Myocardial Infarction: A Costa Rican Population.

Author

Bare, Lance A., Ruiz-Narvaéz, Edward A., Tong, Carmen H., Arellano, Andre R., Rowland, Charles M., Catanese, Joseph J., Sacks, Frank M., Devlin, James J., and Campos, Hannia

Subjects

GENES, CAUCASIAN race, MYOCARDIAL infarction, CORONARY disease, INFARCTION, GENETIC carriers, GENETICS, GENETIC polymorphisms

Abstract

Background and Methodology: The 719Arg allele of KIF6 (rs20455) was associated with coronary events in Caucasian participants of five prospective studies. We investigated whether this KIF6 variant was associated with non-fatal myocardial infarction (MI) in a case-control study of an admixed population from the Central Valley of Costa Rica. Genotypes of the KIF6 variant were determined for 4,134 men and women. Cases (1,987) had survived a first MI; controls (2,147) had no history of MI and were matched to cases by age, sex, and area of residence. We tested the association between the KIF6 719Arg allele and non-fatal MI by conditional logistic regression and adjusted for admixture of founder populations. Principal Findings: Compared with the reference Trp/Trp homozygotes, KIF6 719Arg carriers were not at significantly higher risk for non-fatal MI in this study after adjustment for traditional risk factors or admixture (OR = 1.12; 95%CI, 0.98-1.28). Heterozygotes of the KIF6 Trp719Arg variant were at increased risk of non-fatal MI: the adjusted odds ratio was 1.16 (95% confidence interval, 1.01-1.34), but this association would not be significant after a multiple testing correction. Conclusions/Significance: We found that carriers of the KIF6 719Arg allele were not at increased risk of non-fatal MI in a case-control study of Costa Ricans living in the Central Valley of Costa Rica. [ABSTRACT FROM AUTHOR]

Published

2010

9. Genome-wide association study meta-analysis identifies seven new rheumatoid arthritis risk loci.

Author

Stahl, Eli A., Raychaudhuri, Soumya, Remmers, Elaine F., Gang Xie, Eyre, Stephen, Thomson, Brian P., Yonghong Li, Kurreeman, Fina A. S., Zhernakova, Alexandra, Hinks, Anne, Guiducci, Candace, Chen, Robert, Alfredsson, Lars, Amos, Christopher I., Ardlie, Kristin G., Barton, Anne, Bowes, John, Brouwer, Elisabeth, Burtt, Noel P., and Catanese, Joseph J.

Subjects

RHEUMATOID arthritis, AUTOIMMUNE diseases, GENOMES, GENETICS, IMMUNITY

Abstract

To identify new genetic risk factors for rheumatoid arthritis, we conducted a genome-wide association study meta-analysis of 5,539 autoantibody-positive individuals with rheumatoid arthritis (cases) and 20,169 controls of European descent, followed by replication in an independent set of 6,768 rheumatoid arthritis cases and 8,806 controls. Of 34 SNPs selected for replication, 7 new rheumatoid arthritis risk alleles were identified at genome-wide significance (P < 5 × 10−8) in an analysis of all 41,282 samples. The associated SNPs are near genes of known immune function, including IL6ST, SPRED2, RBPJ, CCR6, IRF5 and PXK. We also refined associations at two established rheumatoid arthritis risk loci (IL2RA and CCL21) and confirmed the association at AFF3. These new associations bring the total number of confirmed rheumatoid arthritis risk loci to 31 among individuals of European ancestry. An additional 11 SNPs replicated at P < 0.05, many of which are validated autoimmune risk alleles, suggesting that most represent genuine rheumatoid arthritis risk alleles. [ABSTRACT FROM AUTHOR]

Published

2010

10. Polymorphisms Associated with Both Noncardioembolic Stroke and Coronary Heart Disease: Vienna Stroke Registry.

Author

Luke, May M., Lalouschek, Wolfgang, Rowland, Charles M., Catanese, Joseph J., Bolonick, Joel I., Bui, Nam D., Greisenegger, Stefan, Endler, Georg, Devlin, James J., and Mannhalter, Christine

Subjects

CEREBROVASCULAR disease, CORONARY disease, GENETIC polymorphisms, ATHEROSCLEROSIS, CHROMOSOMES, MEDICAL genetics

Abstract

Noncardioembolic stroke and coronary heart disease (CHD) may share genetic predispositions. We tested the hypothesis that genetic variants which are associated with risk of CHD would also be associated with risk of noncardioembolic stroke in 562 cases from the Vienna Stroke Registry and 815 controls. We selected 6 gene variants that had been consistently associated with risk of CHD in 3 studies, including the Atherosclerosis Risk in Communities study, and found that 4 of these gene variants were also associated with risk of noncardioembolic stroke. The odds ratios for noncardioembolic stroke were 1.31 (90% CI 1.07–1.60) for rs3900940 in MYH15, 1.24 (90% CI 1.01–1.5) for rs20455 in KIF6, 1.21 (90% CI 0.99–1.49) for rs1010 in VAMP8, and 1.20 (90% CI 0.95–1.50) for rs10757274 on chromosome 9p21. Copyright © 2009 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2009

11. Association of a Single-Nucleotide Polymorphism in CD40 With the Rate of Joint Destruction in Rheumatoid Arthritis.

Author

Van der Linden, Michael P. M., Feitsma, Anouk L., le Cessie, Saskia, Kern, Marlena, Olsson, Lina M., Raychaudhuri, Soumya, Begovich, Ann B., Chang, Monica, Catanese, Joseph J., Kurreeman, Fina A. S., Van Nies, Jessica, Van der Heijde, Désirée M., Gregersen, Peter K., Huizinga, Tom W. J., Toes, René E. M., and Van der Helm-van Mil, Annette H. M.

Subjects

RHEUMATISM, RHEUMATOID arthritis, JOINT physiology, GENETICS of disease susceptibility, NUCLEOTIDES, GENETIC polymorphisms, GENETICS, PATIENTS

Abstract

The article presents a study which analyzes the relation of single-nucleotide polymorphisms (SNPs) with the rate of radiologic joint destruction among anti-citrullinated protein antibody (ACPA)-positive rheumatoid arthritis (RA) patients. It examines whether 6 newly describe regions for susceptibility to autoantibody-positive RA including CD40 were related with the rate of joint destruction. Results show that the rate of joint destruction are associated with a genetic variant in the CD40 gene.

Published

2009

12. A porcine BAC library with tenfold genome coverage: a resource for physical and genetic map integration.

Author

Fahrenkrug, Scott C., Rohrer, Gary A., Freking, Brad A., Smith, Timothy P.L., Osoegawa, Kazutoyo, Shu, Chung Li, Catanese, Joseph J., and de Jong, Pieter J.

Subjects

BACTERIAL artificial chromosomes, ARTIFICIAL chromosomes, GENE mapping, DNA, GENOMES, GENETICS

Abstract

This article focuses on bacterial artificial chromosome (B AC) libraries. These libraries serve as an important resource for physical and genetic map integration. The development of BAC libraries represents a compromise between insert size, stability and ease of clone DNA isolation. BACs are capable of stably maintaining insert sizes exceeding 200 kb and can be easily isolated by standard alkaline lysis from bacterial genomic DNA by virtue of their closed-circular conformation. Recently BAC libraries representing livestock species, including cattle, sheep and pigs have been developed.

Published

2001

13. Construction and characterization of a new bovine bacterial artificial chromosome library with 10 genome-equivalent coverage.

Author

Warren, Wesley, Smith, Timothy P. L., Rexroad, III, Caird E., Fahrenkrug, Scott C., Allison, Tanya, Chung-Li Shu, Catanese, Joseph, and de Jong, Pieter J.

Subjects

GENETICS, GENOMES, GENETIC engineering, CLONING, ANIMAL genome mapping, CHROMOSOMES

Abstract

The article reports on the construction and characterization of a new bovine bacterial artificial chromosome library with 10 genome-equivalent coverage. Genetic linkage maps of the bovine genome have recently been constructed and used to assign loci affecting heritable traits of economic importance to specific chromosomal segments. Markers can thus be identified that may be useful in marker-assisted selection to increase the frequency of favorable allele in commercial populations. Therefore positional cloning approach requires the construction of contigs that physically span large sections of chromosomes.

Published

2000

14. Polymorphism in the apolipoprotein(a) gene, plasma lipoprotein(a), cardiovascular disease, and low-dose aspirin therapy

Author

Chasman, Daniel I., Shiffman, Dov, Zee, Robert Y.L., Louie, Judy Z., Luke, May M., Rowland, Charles M., Catanese, Joseph J., Buring, Julie E., Devlin, James J., and Ridker, Paul M.

Subjects

*GENETIC polymorphisms, *APOLIPOPROTEIN E gene, *BLOOD lipoproteins, *CARDIOVASCULAR diseases risk factors, *ASPIRIN, *DRUG dosage

Abstract

Abstract: Objective: A minor allele variant (rs3798220) of apolipoprotein(a) has been reported to be associated with elevated plasma lipoprotein(a) [Lp(a)] and increased cardiovascular risk. We investigated whether this allele was associated with elevated Lp(a) and cardiovascular risk in the Women''s Health Study, a randomized trial of low-dose aspirin, and whether aspirin reduced cardiovascular risk in minor allele carriers. Methods and results: Genotypes of rs3798220 were determined for 25,131 initially healthy Caucasian participants. Median Lp(a) levels at baseline were 10.0, 79.5, and 153.9mg/dL for major allele homozygotes, heterozygotes, and minor allele homozygotes, respectively (P <0.0001). During the 9.9 years of follow-up, minor allele carriers (3.7%) in the placebo group had twofold higher risk of major cardiovascular events than non-carriers (age-adjusted hazard ratio (HR)=2.21, 95% CI: 1.39–3.52). Among carriers, risk was reduced more than twofold by aspirin: for aspirin compared with placebo the age-adjusted HR was 0.44 (95% CI: 0.20–0.94); risk was not significantly reduced among non-carriers (age-adjusted HR=0.91, 95% CI: 0.77–1.08). This interaction between carrier status and aspirin allocation was significant (P =0.048). Conclusions: In the Women''s Health Study, carriers of an apolipoprotein(a) variant had elevated Lp(a), doubled cardiovascular risk, and appeared to benefit more from aspirin than non-carriers. [Copyright &y& Elsevier]

Published

2009

15. Novel genetic markers for structural coronary artery disease, myocardial infarction, and familial combined hyperlipidemia: candidate and genome scans of functional SNPs

Author

Kane, John P., Aouizerat, Bradley E., Luke, May M., Shiffman, Dov, Iakoubova, Olga, Liu, Dongming, Rowland, Charlie M., Catanese, Joseph J., Leong, Diane U., Lau, Kit F., Louie, Judy Z., Tong, Carmen H., McAllister, Linda B., Dabby, Lisa F., Ports, Thomas A., Michaels, Andrew D., Zellner, Christian, Pullinger, Clive R., Malloy, Mary J., and Devlin, James J.

Subjects

*GENETIC markers, *BIOMARKERS, *CORONARY disease, *HEART diseases, *HYPERLIPIDEMIA

Abstract

Association studies were conducted on a large number of single nucleotide polymorphisms (SNPs) in pooled screening for association with angiographically determined coronary artery disease (CAD) and myocardial infarction (MI), followed by individual genotyping of those showing association. Forty-seven SNPs showed association with severity of CAD in a replication study applying individual genotyping in 1250 patients. Case control analysis of 340 patients with MI and 300 controls revealed significant associations of three novel genes: an immune cell receptor on chromosome 20p (p=0.02), a zinc finger protein on chromosome 3 (p=0.04), and an unknown gene on chromosome 3 (p=0.01). Associations of polymorphisms in three genes with the phenotype of familial combined hyperlipidemia (FCH), Apo A-V, PPAR alpha and microsomal triglyceride transfer protein (MTP) were established, supporting a metabolic model for the disorder based on misdirection of fatty acid metabolism. Congruence of SNP associations in non-alcoholic steatohepatitis suggests overlap of this syndrome with FCH. [Copyright &y& Elsevier]

Published

2004

16. A BAC-Based Physical Map of the Major Autosomes of Drosophila melanogaster.

Author

Hoskins, Roger A., Nelson, Catherine R., Berman, Benjamin P., Laverty, Todd R., George, Reed A., Ciesiotka, Lisa, Naeemuddin, Mohammed, Arenson, Andrew D., Durbin, James, David, Robert G., Tabor, Paul E., Bailey, Michael R., DeShazo, Denise R., Catanese, Joseph, Mammoser, Aaron, Osoegawa, Kazutoyo, de Jong, Pieter J., Celniker, Susan E., Gibbs, Richard A., and Rubin, Gerald M.

Subjects

*GENE mapping, *ANIMAL genome mapping, *DROSOPHILA melanogaster, *GENETICS

Abstract

Discusses the construction of a bacterial artificial chromosome-based physical map of chromosomes of Drosophila melanogaster. Use of the fruit fly Drosophila melanogaster as an animal model in metazoan genetics and molecular biology; Procedure of the construction of the gene map; Features of the genetic map.

Published

2000