Your search keyword '"Zelenika, Diana"' showing total 9 results

1. Caution in Interpreting Results from Imputation Analysis When Linkage Disequilibrium Extends over a Large Distance: A Case Study on Venous Thrombosis.

Author

Germain, Marine, Saut, Noémie, Oudot-Mellakh, Tiphaine, Letenneur, Luc, Dupuy, Anne-Marie, Bertrand, Marion, Alessi, Marie-Christine, Lambert, Jean-Charles, Zelenika, Diana, Emmerich, Joseph, Tiret, Laurence, Cambien, Francois, Lathrop, Mark, Amouyel, Philippe, Morange, Pierre-Emmanuel, and Trégouët, David-Alexandre

Subjects

VENOUS thrombosis, PHLEBITIS, GENOMES, CARDIOVASCULAR diseases, GENETICS

Abstract

By applying an imputation strategy based on the 1000 Genomes project to two genome-wide association studies (GWAS), we detected a susceptibility locus for venous thrombosis on chromosome 11p11.2 that was missed by previous GWAS analyses that had been conducted on the same datasets. A comprehensive linkage disequilibrium and haplotype analysis of the whole locus where twelve SNPs exhibited association p-values lower than 2.23 10-11 and the use of independent casecontrol samples demonstrated that the culprit variant was a rare variant located ∼1 Mb away from the original hits, not tagged by current genome-wide genotyping arrays and even not well imputed in the original GWAS samples. This variant was in fact the rs1799963, also known as the FII G20210A prothrombin mutation. This work may be of major interest not only for its scientific impact but also for its methodological findings. [ABSTRACT FROM AUTHOR]

Published

2012

2. Genome wide association study for plasma levels of natural anticoagulant inhibitors and protein C anticoagulant pathway: the MARTHA project.

Author

Oudot-Mellakh, Tiphaine, Cohen, William, Germain, Marine, Saut, Noémie, Kallel, Choumous, Zelenika, Diana, Lathrop, Mark, Trégouët, David-Alexandre, and Morange, Pierre-Emmanuel

Subjects

GENOMES, ANTICOAGULANTS, PROTEIN C, ANTITHROMBINS, PROTEIN S, VENOUS thrombosis, GENETIC polymorphisms, LOCUS (Genetics)

Abstract

Summary Deficiencies of antithrombin (AT), protein C (PC) and protein S (PS) or an impaired PC anticoagulant pathway increase the risk of venous thrombosis (VT). By conducting a genome-wide association study (GWAS) on two independent samples of VT patients totalling 951 subjects typed for 472 173 single nucleotide polymorphisms (SNPs), we observed that common SNPs explain 21% and 27% of the genetic variance of plasma AT and PS levels, even though no SNP reached genome-wide significance. For PC, we showed that two PROCR SNPs, rs867186 (Ser219Gly) and rs6060278, additionally explained c. 20% ( P = 1·19 × 10−31) of the variance of plasma PC levels. We also observed that c. 40% of the remaining genetic variance of PC levels could be due to yet unidentified common SNPs. The PROCR locus was also found to explain c. 8% ( P < 10−10) of agkistrodon contortrix venom (ACV) (exploring the PC pathway) variability which was under the main control of the F5 and F2 loci that further explained about 40% and 10%, respectively. We presented here the first GWAS for plasma AT and free-PS levels and ACV in Caucasian samples. We identified three independent loci associated with ACV ( F2, F5 and PROCR) and replicated two independent effects on plasma PC levels at the PROCR locus. [ABSTRACT FROM AUTHOR]

Published

2012

3. Novel Breast Cancer Susceptibility Locus at 9q31.2: Results of a Genome-Wide Association Study.

Author

Fletcher, Olivia, Johnson, Nichola, Orr, Nick, Hosking, Fay J., Gibson, Lorna J., Walker, Kate, Zelenika, Diana, Gut, Ivo, Heath, Simon, Palles, Claire, Coupland, Ben, Broderick, Peter, Schoemaker, Minouk, Jones, Michael, Williamson, Jill, Chilcott-Burns, Sarah, Tomczyk, Katarzyna, Simpson, Gemma, Jacobs, Kevin B., and Chanock, Stephen J.

Subjects

GENOMES, BIOLOGICAL variation, BREAST cancer risk factors, GENETIC polymorphisms, LOGISTIC regression analysis, TELOMERASE

Abstract

Background Genome-wide association studies have identified several common genetic variants associated with breast cancer risk. It is likely, however, that a substantial proportion of such loci have not yet been discovered. Methods We compared 296 114 tagging single-nucleotide polymorphisms in 1694 breast cancer case subjects (92% with two primary cancers or at least two affected first-degree relatives) and 2365 control subjects, with validation in three independent series totaling 11 880 case subjects and 12 487 control subjects. Odds ratios (ORs) and associated 95% confidence intervals (CIs) in each stage and all stages combined were calculated using unconditional logistic regression. Heterogeneity was evaluated with Cochran Q and I 2 statistics. All statistical tests were two-sided. Results We identified a novel risk locus for breast cancer at 9q31.2 (rs865686: OR = 0.89, 95% CI = 0.85 to 0.92, P = 1.75 × 10−10). This single-nucleotide polymorphism maps to a gene desert, the nearest genes being Kruppel-like factor 4 (KLF4, 636 kb centromeric), RAD23 homolog B (RAD23B, 794 kb centromeric), and actin-like 7A (ACTL7A, 736 kb telomeric). We also identified two variants (rs3734805 and rs9383938) mapping to 6q25.1 estrogen receptor 1 (ESR1), which were associated with breast cancer in subjects of northern European ancestry (rs3734805: OR = 1.19, 95% CI = 1.11 to 1.27, P = 1.35 × 10−7; rs9383938: OR = 1.18, 95% CI = 1.11 to 1.26, P = 1.41 × 10−7). A variant mapping to 10q26.13, approximately 300 kb telomeric to the established risk locus within the second intron of FGFR2, was also associated with breast cancer risk, although not at genome-wide statistical significance (rs10510102: OR = 1.12, 95% CI = 1.07 to 1.17, P = 1.58 × 10−6). Conclusions These findings provide further evidence on the role of genetic variation in the etiology of breast cancer. Fine mapping will be needed to identify causal variants and to determine their functional effects. [ABSTRACT FROM PUBLISHER]

Published

2011

4. Implication of the Immune System in Alzheimer's Disease: Evidence from Genome-Wide Pathway Analysis.

Author

Lambert, Jean-Charles, Grenier-Boley, Benjamin, Chouraki, Vincent, Heath, Simon, Zelenika, Diana, Fievet, Nathalie, Hannequin, Didier, Pasquier, Florence, Hanon, Olivier, Brice, Alexis, Epelbaum, Jacques, Berr, Claudine, Dartigues, Jean-Francois, Tzourio, Christophe, Campion, Dominique, Lathrop, Mark, and Amouyel, Philippe

Subjects

IMMUNE system, ALZHEIMER'S disease, GENOMES, GENETIC polymorphisms, PRESENILE dementia

Abstract

The results of several genome-wide association studies (GWASs) in the field of Alzheimer's disease (AD) have recently been published. Although these studies reported in detail on single-nucleotide polymorphisms (SNPs) and the neighboring genes with the strongest evidence of association with AD, little attention was paid to the rest of the genome. However, complementary statistical and bio-informatics approaches now enable the extraction of pertinent information from other SNPs and/or genes which are only nominally associated with the disease risk. Two different tools (the ALIGATOR and GenGen/KEGG software packages) were used to analyze a large GWAS dataset containing 2,032 AD cases and 5,328 controls. Convergent outputs from the two gene set enrichment approaches suggested an immune system dysfunction in AD. Furthermore, although these statistical approaches did not adopt a priori hypotheses concerning a biological function's putative role in the disease process, genes associated with AD risk were overrepresented in the "Alzheimer's disease" KEGG pathway. In conclusion, a systematic search for biological pathways using GWAS data set seems to comfort the primary causes already suspected but may specifically highlight the importance of the immune system in AD. [ABSTRACT FROM AUTHOR]

Published

2010

5. Systematic Analysis of Candidate Genes for Alzheimer's Disease in a French, Genome-Wide Association Study.

Author

Laumet, Geoffroy, Chouraki, Vincent, Grenier-Boley, Benjamin, Legry, Vanessa, Heath, Simon, Zelenika, Diana, Fievet, Nathalie, Hannequin, Didier, Delepine, Marc, Pasquier, Florence, Hanon, Olivier, Brice, Alexis, Epelbaum, Jacques, Berr, Claudine, Dartigues, Jean-Francois, Tzourio, Christophe, Campion, Dominique, Lathrop, Mark, Bertram, Lars, and Amouyel, Philippe

Subjects

GENETICS of Alzheimer's disease, GENOMES, DNA replication, DATABASES

Abstract

We selected twenty genes from the "Top Results" list on the AlzGene database website and assessed their association with risk of developing Alzheimer's disease (AD) in a large, genome-wide association study (using 526 SNPs from 2,032 AD cases and 5,328 controls) performed in France. The APOE, CLU, PICALM, and CR1 loci were excluded, since they had already been extensively analyzed. Ten genes/loci (TFAM, SORL1, CHRNB2, SORCS1, DAPK1, MTHFR, GWA 14q32.13, BDNF, NEDD9, and CH25H) showed weak nominal association with AD risk, in line with previous studies. In the remaining ten genes/loci (TNK1, ACE, CST3, IL1B, hCG2039140, PRNP, GAB2, LOC651924, IL1A, and TF), no single nucleotide polymorphisms were associated in our dataset. Of the genes showing nominal association in our cohorts, TFAM and CHRNB2 appear particularly interesting and warrant further genetic and functional follow-up analyses. [ABSTRACT FROM AUTHOR]

Published

2010

6. Genome-wide association study identifies variants at CLU and CR1 associated with Alzheimer's disease.

Author

Lambert, Jean-Charles, Heath, Simon, Even, Gael, Campion, Dominique, Sleegers, Kristel, Hiltunen, Mikko, Combarros, Onofre, Zelenika, Diana, Bullido, Maria J., Tavernier, Béatrice, Letenneur, Luc, Bettens, Karolien, Berr, Claudine, Pasquier, Florence, Fiévet, Nathalie, Barberger-Gateau, Pascale, Engelborghs, Sebastiaan, de Deyn, Peter, Mateo, Ignacio, and Franck, Ana

Subjects

GENETIC research, APOLIPOPROTEIN E, ALZHEIMER'S disease, LOCUS (Genetics), GENOMES, AMYLOID

Abstract

The gene encoding apolipoprotein E (APOE) on chromosome 19 is the only confirmed susceptibility locus for late-onset Alzheimer's disease. To identify other risk loci, we conducted a large genome-wide association study of 2,032 individuals from France with Alzheimer's disease (cases) and 5,328 controls. Markers outside APOE with suggestive evidence of association (P < 10−5) were examined in collections from Belgium, Finland, Italy and Spain totaling 3,978 Alzheimer's disease cases and 3,297 controls. Two loci gave replicated evidence of association: one within CLU (also called APOJ), encoding clusterin or apolipoprotein J, on chromosome 8 (rs11136000, OR = 0.86, 95% CI 0.81–0.90, P = 7.5 × 10−9 for combined data) and the other within CR1, encoding the complement component (3b/4b) receptor 1, on chromosome 1 (rs6656401, OR = 1.21, 95% CI 1.14–1.29, P = 3.7 × 10−9 for combined data). Previous biological studies support roles of CLU and CR1 in the clearance of β amyloid (Aβ) peptide, the principal constituent of amyloid plaques, which are one of the major brain lesions of individuals with Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2009

7. Common variants at 30 loci contribute to polygenic dyslipidemia.

Author

Kathiresan, Sekar, Willer, Cristen J., Peloso, Gina M, Demissie, Serkalem, Musunuru, Kiran, Schadt, Eric E., Kaplan, Lee, Bennett, Derrick, Li, Yun, Tanaka, Toshiko, Voight, Benjamin F., Bonnycastle, Lori L., Jackson, Anne U., Crawford, Gabriel, Surti, Aarti, Guiducci, Candace, Burtt, Noel P., Parish, Sarah, Clarke, Robert, and Zelenika, Diana

Subjects

LIPOPROTEINS, BLOOD cholesterol, TRIGLYCERIDES, CARDIOVASCULAR diseases risk factors, GENOMES, NUCLEOTIDE sequence

Abstract

Blood low-density lipoprotein (LDL) cholesterol, high-density lipoprotein (HDL) cholesterol and triglyceride levels are risk factors for cardiovascular disease. To dissect the polygenic basis of these traits, we conducted genome-wide association screens in 19,840 individuals and replication in up to 20,623 individuals. We identified 30 distinct loci associated with lipoprotein concentrations (each with P < 5 × 10−8), including 11 loci that reached genome-wide significance for the first time. The 11 newly defined loci include common variants associated with LDL cholesterol near ABCG8, MAFB, HNF1A and TIMD4; with HDL cholesterol near ANGPTL4, FADS1-FADS2-FADS3, HNF4A, LCAT, PLTP and TTC39B; and with triglycerides near AMAC1L2, FADS1-FADS2-FADS3 and PLTP. The proportion of individuals exceeding clinical cut points for high LDL cholesterol, low HDL cholesterol and high triglycerides varied according to an allelic dosage score (P < 10−15 for each trend). These results suggest that the cumulative effect of multiple common variants contributes to polygenic dyslipidemia. [ABSTRACT FROM AUTHOR]

Published

2009

8. Genome-wide association study of multiple congenital heart disease phenotypes identifies a susceptibility locus for atrial septal defect at chromosome 4p16.

Author

Cordell, Heather J, Bentham, Jamie, Topf, Ana, Zelenika, Diana, Heath, Simon, Mamasoula, Chrysovalanto, Cosgrove, Catherine, Blue, Gillian, Granados-Riveron, Javier, Setchfield, Kerry, Thornborough, Chris, Breckpot, Jeroen, Soemedi, Rachel, Martin, Ruairidh, Rahman, Thahira J, Hall, Darroch, van Engelen, Klaartje, Moorman, Antoon F M, Zwinderman, Aelko H, and Barnett, Phil

Subjects

CONGENITAL heart disease, GENOMES, PHENOTYPES, LOCUS (Genetics), DISEASE susceptibility, ATRIAL septal defects, CHROMOSOMES

Abstract

We carried out a genome-wide association study (GWAS) of congenital heart disease (CHD). Our discovery cohort comprised 1,995 CHD cases and 5,159 controls and included affected individuals from each of the 3 major clinical CHD categories (with septal, obstructive and cyanotic defects). When all CHD phenotypes were considered together, no region achieved genome-wide significant association. However, a region on chromosome 4p16, adjacent to the MSX1 and STX18 genes, was associated (P = 9.5 × 10−7) with the risk of ostium secundum atrial septal defect (ASD) in the discovery cohort (N = 340 cases), and this association was replicated in a further 417 ASD cases and 2,520 controls (replication P = 5.0 × 10−5; odds ratio (OR) in replication cohort = 1.40, 95% confidence interval (CI) = 1.19-1.65; combined P = 2.6 × 10−10). Genotype accounted for ∼9% of the population-attributable risk of ASD. [ABSTRACT FROM AUTHOR]

Published

2013

9. A QTL influencing F cell production maps to a gene encoding a zinc-finger protein on chromosome 2p15.

Author

Menzel, Stephan, Garner, Chad, Gut, Ivo, Matsuda, Fumihiko, Yamaguchi, Masao, Heath, Simon, Foglio, Mario, Zelenika, Diana, Boland, Anne, Rooks, Helen, Best, Steve, Spector, Tim D., Farrall, Martin, Lathrop, Mark, and Thein, Swee Lay

Subjects

CHROMOSOMES, HEMOGLOBINS, GENOMES, PHENOTYPES, SICKLE cell anemia, ZINC-finger proteins

Abstract

F cells measure the presence of fetal hemoglobin, a heritable quantitative trait in adults that accounts for substantial phenotypic diversity of sickle cell disease and β thalassemia. We applied a genome-wide association mapping strategy to individuals with contrasting extreme trait values and mapped a new F cell quantitative trait locus to BCL11A, which encodes a zinc-finger protein, on chromosome 2p15. The 2p15 BCL11A quantitative trait locus accounts for 15.1% of the trait variance. [ABSTRACT FROM AUTHOR]

Published

2007