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203

PLoS genetics. 2011:7(10).DOI: 10.1371/journal.pgen.1002298

Identification, replication, and fine-mapping of Loci associated with adult height in individuals of african ancestry

N'Diaye, Amidou; Chen, Gary K; Palmer, Cameron D; Ge, Bing; Tayo, Bamidele; Mathias, Rasika A; Ding, Jingzhong; Nalls, Michael A; Adeyemo, Adebowale; Adoue, Véronique; Ambrosone, Christine B; Atwood, Larry; Bandera, Elisa V; Becker, Lewis C; Berndt, Sonja I; Bernstein, Leslie; Blot, William J; Boerwinkle, Eric; Britton, Angela; Casey, Graham; Chanock, Stephen J; Demerath, Ellen; Deming, Sandra L; Diver, W Ryan; Fox, Caroline; Harris, Tamara B; Hernandez, Dena G; Hu, Jennifer J; Ingles, Sue A; John, Esther M; Johnson, Craig; Keating, Brendan; Kittles, Rick A; Kolonel, Laurence N; Kritchevsky, Stephen B; Le Marchand, Loic; Lohman, Kurt; Liu, Jiankang; Millikan, Robert C; Murphy, Adam; Musani, Solomon; Neslund-Dudas, Christine; North, Kari E; Nyante, Sarah; Ogunniyi, Adesola; Ostrander, Elaine A; Papanicolaou, George; Patel, Sanjay; Pettaway, Curtis A; Press, Michael F; Redline, Susan; Rodriguez-Gil, Jorge L; Rotimi, Charles; Rybicki, Benjamin A; Salako, Babatunde; Schreiner, Pamela J; Signorello, Lisa B; Singleton, Andrew B; Stanford, Janet L; Stram, Alex H; Stram, Daniel O; Strom, Sara S; Suktitipat, Bhoom; Thun, Michael J; Witte, John S; Yanek, Lisa R; Ziegler, Regina G; Zheng, Wei; Zhu, Xiaofeng; Zmuda, Joseph M; Zonderman, Alan B; Evans, Michele K; Liu, Yongmei; Becker, Diane M; Cooper, Richard S; Pastinen, Tomi; Henderson, Brian E; Hirschhorn, Joel N; Lettre, Guillaume; Haiman, Christopher A
Adult height is a classic polygenic trait of high heritability (h(2) approximately 0.8). More than 180 single nucleotide polymorphisms (SNPs), identified mostly in populations of European descent, are associated with height. These variants convey modest effects and explain approximately10% of the variance in height. Discovery efforts in other populations, while limited, have revealed loci for height not previously implicated in individuals of European ancestry. Here, we performed a meta-analysis of genome-wide association (GWA) results for adult height in 20,427 individuals of African ancestry with replication in up to 16,436 African Americans. We found two novel height loci (Xp22-rs12393627, P = 3.4×10(-12) and 2p14-rs4315565, P = 1.2×10(-8)). As a group, height associations discovered in European-ancestry samples replicate in individuals of African ancestry (P = 1.7×10(-4) for overall replication). Fine-mapping of the European height loci in African-ancestry individuals showed an enrichment of SNPs that are associated with expression of nearby genes when compared to the index European height SNPs (P<0.01). Our results highlight the utility of genetic studies in non-European populations to understand the etiology of complex human diseases and traits.
PMID: 21998595
ISSN: 1553-7404
CID: 5477872
Human molecular genetics. 2011:20(17):3525-34.DOI: 10.1093/hmg/ddr264

A gene-centric association scan for Coagulation Factor VII levels in European and African Americans: the Candidate Gene Association Resource (CARe) Consortium

Taylor, Kira C; Lange, Leslie A; Zabaneh, Delilah; Lange, Ethan; Keating, Brendan J; Tang, Weihong; Smith, Nicholas L; Delaney, Joseph A; Kumari, Meena; Hingorani, Aroon; North, Kari E; Kivimaki, Mika; Tracy, Russell P; O'Donnell, Christopher J; Folsom, Aaron R; Green, David; Humphries, Steve E; Reiner, Alexander P
Polymorphisms in several distinct genomic regions, including the F7 gene, were recently associated with factor VII (FVII) levels in European Americans (EAs). The genetic determinants of FVII in African Americans (AAs) are unknown. We used a 50,000 single nucleotide polymorphism (SNP) gene-centric array having dense coverage of over 2,000 candidate genes for cardiovascular disease (CVD) pathways in a community-based sample of 16,324 EA and 3898 AA participants from the Candidate Gene Association Resource (CARe) consortium. Our aim was the discovery of new genomic loci and more detailed characterization of existing loci associated with FVII levels. In EAs, we identified three new loci associated with FVII, of which APOA5 on chromosome 11q23 and HNF4A on chromosome 20q12-13 were replicated in a sample of 4289 participants from the Whitehall II study. We confirmed four previously reported FVII-associated loci (GCKR, MS4A6A, F7 and PROCR) in CARe EA samples. In AAs, the F7 and PROCR regions were significantly associated with FVII. Several of the FVII-associated regions are known to be associated with lipids and other cardiovascular-related traits. At the F7 locus, there was evidence of at least five independently associated SNPs in EAs and three independent signals in AAs. Though the variance in FVII explained by the existing loci is substantial (20% in EA and 10% in AA), larger sample sizes and investigation of lower frequency variants may be required to identify additional FVII-associated loci in EAs and AAs and further clarify the relationship between FVII and other CVD risk factors.
PMCID:3153310
PMID: 21676895
ISSN: 1460-2083
CID: 5477842
PLoS genetics. 2011:7(9).DOI: 10.1371/journal.pgen.1002260

Large-scale gene-centric analysis identifies novel variants for coronary artery disease

Butterworth, Adam S; Braund, Peter S; Farrall, Martin; Hardwick, Robert J; Saleheen, Danish; Peden, John F; Soranzo, Nicole; Chambers, John C; Sivapalaratnam, Suthesh; Kleber, Marcus E; Keating, Brendan; Qasim, Atif; Klopp, Norman; Erdmann, Jeanette; Assimes, Themistocles L; Ball, Stephen G; Balmforth, Anthony J; Barnes, Timothy A; Basart, Hanneke; Baumert, Jens; Bezzina, Connie R; Boerwinkle, Eric; Boehm, Bernhard O; Brocheton, Jessy; Bugert, Peter; Cambien, Francois; Clarke, Robert; Codd, Veryan; Collins, Rory; Couper, David; Cupples, L Adrienne; de Jong, Jonas S; Diemert, Patrick; Ejebe, Kenechi; Elbers, Clara C; Elliott, Paul; Fornage, Myriam; Franzosi, Maria-Grazia; Frossard, Philippe; Garner, Stephen; Goel, Anuj; Goodall, Alison H; Hengstenberg, Christian; Hunt, Sarah E; Kastelein, John J P; Klungel, Olaf H; Klüter, Harald; Koch, Kerstin; König, Inke R; Kooner, Angad S; Laaksonen, Reijo; Lathrop, Mark; Li, Mingyao; Liu, Kiang; McPherson, Ruth; Musameh, Muntaser D; Musani, Solomon; Nelson, Christopher P; O'Donnell, Christopher J; Ongen, Halit; Papanicolaou, George; Peters, Annette; Peters, Bas J M; Potter, Simon; Psaty, Bruce M; Qu, Liming; Rader, Daniel J; Rasheed, Asif; Rice, Catherine; Scott, James; Seedorf, Udo; Sehmi, Joban S; Sotoodehnia, Nona; Stark, Klaus; Stephens, Jonathan; van der Schoot, C Ellen; van der Schouw, Yvonne T; Thorsteinsdottir, Unnur; Tomaszewski, Maciej; van der Harst, Pim; Vasan, Ramachandran S; Wilde, Arthur A M; Willenborg, Christina; Winkelmann, Bernhard R; Zaidi, Moazzam; Zhang, Weihua; Ziegler, Andreas; de Bakker, Paul I W; Koenig, Wolfgang; Mätz, Winfried; Trip, Mieke D; Reilly, Muredach P; Kathiresan, Sekar; Schunkert, Heribert; Hamsten, Anders; Hall, Alistair S; Kooner, Jaspal S; Thompson, Simon G; Thompson, John R; Deloukas, Panos; Ouwehand, Willem H; Watkins, Hugh; Danesh, John; Samani, Nilesh J; Barnes, Timothy; Rafelt, Suzanne; Codd, Veryan; Tomaszewski, Maciej; Ouwehand, Willem H; Bruinsma, Nienke; Dekker, Lukas R; Henriques, José P; Koch, Karel T; de Winter, Robbert J; Alings, Marco; Allaart, Cor F; Gorgels, Anton P; Verheugt, Freek W; Braund, Peter S; Thompson, John R; Samani, Nilesh J; Mueller, Martina; Meisinger, Christa; DerOhannessian, Stephanie; Mehta, Nehal N; Ferguson, Jane; Hakonarson, Hakon; Matthai, William; Wilensky, Robert; Hopewell, J C; Parish, S; Linksted, P; Notman, J; Gonzalez, H; Young, A; Ostley, T; Munday, A; Goodwin, N; Verdon, V; Shah, S; Cobb, L; Edwards, C; Mathews, C; Gunter, R; Benham, J; Davies, C; Cobb, M; Cobb, L; Crowther, J; Richards, A; Silver, M; Tochlin, S; Mozley, S; Clark, S; Radley, M; Kourellias, K; Silveira, Angela; Söderholm, Birgitta; Olsson, Per; Barlera, Simona; Tognoni, Gianni; Rust, Stephan; Assmann, Gerd; Heath, Simon; Zelenika, Diana; Gut, Ivo; Green, Fiona; Farrall, Martin; Peden, John; Goel, Anuj; Ongen, Halit; Franzosi, Maria-Grazia; Lathrop, Mark; Seedorf, Udo; Clarke, Robert; Collins, Rory; Hamsten, Anders; Watkins, Hugh; Aly, Anette; Anner, Karolina; Björklund, Karin; Blomgren, Gun; Cederschiöld, Barbro; Danell-Toverud, Karin; Eriksson, Per; Grundstedt, Ulla; Hamsten, Anders; Heinonen, Merja; Hellénius, Mai-Lis; van't Hooft, Ferdinand; Husman, Karin; Lagercrantz, Jacob; Larsson, Anita; Larsson, Malin; Mossfeldt, Magnus; Mälarstig, Anders; Olsson, Gunnar; Sabater-Lleal, Maria; Sennblad, Bengt; Silveira, Angela; Strawbridge, Rona; Söderholm, Birgitta; Öhrvik, John; Zaman, Khan Shah; Mallick, Nadeem Hayat; Azhar, Muhammad; Samad, Abdus; Ishaq, Mohammad; Shah, Nabi; Samuel, Maria; Schunkert, Heribert; König, Inke R; Kathiresan, Sekar; Reilly, Muredach; Assimes, Themistocles L; Holm, Hilma; Preuss, Michael; Stewart, Alexandre F R; Barbalic, Maja; Gieger, Christian; Absher, Devin; Aherrahrou, Zouhair; Allayee, Hooman; Altshuler, David; Anand, Sonia; Andersen, Karl; Anderson, Jeffrey L; Ardissino, Diego; Ball, Stephen G; Balmforth, Anthony J; Barnes, Timothy A; Becker, Lewis C; Becker, Diane M; Berger, Klaus; Bis, Joshua C; Boekholdt, S Matthijs; Boerwinkle, Eric; Braund, Peter S; Brown, Morris J; Burnett, Mary Susan; Buysschaert, Ian; Carlquist, John F; Chen, Li; Codd, Veryan; Davies, Robert W; Dedoussis, George; Dehghan, Abbas; Demissie, Serkalem; Devaney, Joseph; Do, Ron; Doering, Angela; El Mokhtari, Nour Eddine; Ellis, Stephen G; Elosua, Roberto; Engert, James C; Epstein, Stephen; de Faire, Ulf; Fischer, Marcus; Folsom, Aaron R; Freyer, Jennifer; Gigante, Bruna; Girelli, Domenico; Gretarsdottir, Solveig; Gudnason, Vilmundur; Gulcher, Jeffrey R; Tennstedt, Stephanie; Halperin, Eran; Hammond, Naomi; Hazen, Stanley L; Hofman, Albert; Horne, Benjamin D; Illig, Thomas; Iribarren, Carlos; Jones, Gregory T; Jukema, J Wouter; Kaiser, Michael A; Kaplan, Lee M; Kastelein, John J P; Khaw, Kay-Tee; Knowles, Joshua W; Kolovou, Genovefa; Kong, Augustine; Laaksonen, Reijo; Lambrechts, Diether; Leander, Karin; Li, Mingyao; Lieb, Wolfgang; Diemert, Patrick; Lettre, Guillaume; Loley, Christina; Lotery, Andrew J; Mannucci, Pier M; Maouche, Seraya; Martinelli, Nicola; McKeown, Pascale P; Meisinger, Christa; Meitinger, Thomas; Melander, Olle; Merlini, Pier Angelica; Mooser, Vincent; Morgan, Thomas; Mühleisen, Thomas W; Muhlestein, Joseph B; Musunuru, Kiran; Nahrstaedt, Janja; Nelson, Christopher P; Nöthen, Markus M; Olivieri, Oliviero; Peyvandi, Flora; Patel, Riyaz S; Patterson, Chris C; Peters, Annette; Qu, Liming; Quyyumi, Arshed A; Rader, Daniel J; Rallidis, Loukianos S; Rice, Catherine; Rosendaal, Frits R; Rubin, Diana; Salomaa, Veikko; Sampietro, M Lourdes; Sandhu, Manj S; Schadt, Eric; Schäfer, Arne; Schillert, Arne; Schreiber, Stefan; Schrezenmeir, Jürgen; Schwartz, Stephen M; Siscovick, David S; Sivananthan, Mohan; Sivapalaratnam, Suthesh; Smith, Albert V; Smith, Tamara B; Snoep, Jaapjan D; Soranzo, Nicole; Spertus, John A; Stark, Klaus; Stefansson, Kari; Stirrups, Kathy; Stoll, Monika; Tang, W H Wilson; Thorgeirsson, Gudmundur; Thorleifsson, Gudmar; Tomaszewski, Maciej; Uitterlinden, Andre G; van Rij, Andre M; Voight, Benjamin F; Wareham, Nick J; AWells, George; Wichmann, H-Erich; Willenborg, Christina; Witteman, Jaqueline C M; Wright, Benjamin J; Ye, Shu; Ziegler, Andreas; Cambien, Francois; Goodall, Alison H; Cupples, L Adrienne; Quertermous, Thomas; März, Winfried; Hengstenberg, Christian; Blankenberg, Stefan; Ouwehand, Willem H; Hall, Alistair S; Deloukas, Panos; Thorsteinsdottir, Unnur; Roberts, Robert; Thompson, John R; O'Donnell, Christopher J; McPherson, Ruth; Erdmann, Jeanette; Samani, Nilesh J; Onland-Moret, N Charlotte; van Setten, Jessica; de Bakker, Paul I W; Verschuren, W M Monique; Boer, Jolanda M A; Wijmenga, Cisca; Hofker, Marten H; Maitland-van der Zee, Anke-Hilse; de Boer, Anthonius; Grobbee, Diederick E; Attwood, Tony; Belz, Stephanie; Braund, Peter; Cambien, François; Cooper, Jason; Crisp-Hihn, Abi; Diemert, Patrick; Deloukas, Panos; Foad, Nicola; Erdmann, Jeanette; Goodall, Alison H; Gracey, Jay; Gray, Emma; Gwilliams, Rhian; Heimerl, Susanne; Hengstenberg, Christian; Jolley, Jennifer; Krishnan, Unni; Lloyd-Jones, Heather; Lugauer, Ingrid; Lundmark, Per; Maouche, Seraya; Moore, Jasbir S; Muir, David; Murray, Elizabeth; Nelson, Chris P; Neudert, Jessica; Niblett, David; O'Leary, Karen; Ouwehand, Willem H; Pollard, Helen; Rankin, Angela; Rice, Catherine M; Sager, Hendrik; Samani, Nilesh J; Sambrook, Jennifer; Schmitz, Gerd; Scholz, Michael; Schroeder, Laura; Schunkert, Heribert; Syvannen, Ann-Christine; Tennstedt, Stephanie; Wallace, Chris
Coronary artery disease (CAD) has a significant genetic contribution that is incompletely characterized. To complement genome-wide association (GWA) studies, we conducted a large and systematic candidate gene study of CAD susceptibility, including analysis of many uncommon and functional variants. We examined 49,094 genetic variants in ∼2,100 genes of cardiovascular relevance, using a customised gene array in 15,596 CAD cases and 34,992 controls (11,202 cases and 30,733 controls of European descent; 4,394 cases and 4,259 controls of South Asian origin). We attempted to replicate putative novel associations in an additional 17,121 CAD cases and 40,473 controls. Potential mechanisms through which the novel variants could affect CAD risk were explored through association tests with vascular risk factors and gene expression. We confirmed associations of several previously known CAD susceptibility loci (eg, 9p21.3:p<10(-33); LPA:p<10(-19); 1p13.3:p<10(-17)) as well as three recently discovered loci (COL4A1/COL4A2, ZC3HC1, CYP17A1:p<5×10(-7)). However, we found essentially null results for most previously suggested CAD candidate genes. In our replication study of 24 promising common variants, we identified novel associations of variants in or near LIPA, IL5, TRIB1, and ABCG5/ABCG8, with per-allele odds ratios for CAD risk with each of the novel variants ranging from 1.06-1.09. Associations with variants at LIPA, TRIB1, and ABCG5/ABCG8 were supported by gene expression data or effects on lipid levels. Apart from the previously reported variants in LPA, none of the other ∼4,500 low frequency and functional variants showed a strong effect. Associations in South Asians did not differ appreciably from those in Europeans, except for 9p21.3 (per-allele odds ratio: 1.14 versus 1.27 respectively; P for heterogeneity = 0.003). This large-scale gene-centric analysis has identified several novel genes for CAD that relate to diverse biochemical and cellular functions and clarified the literature with regard to many previously suggested genes.
PMID: 21966275
ISSN: 1553-7404
CID: 5479352
Sleep medicine. 2011:12(7):666-71.DOI: 10.1016/j.sleep.2010.12.014

Fatty-acid binding protein 4 gene polymorphisms and plasma levels in children with obstructive sleep apnea

Bhushan, Bharat; Khalyfa, Abdelnaby; Spruyt, Karen; Kheirandish-Gozal, Leila; Capdevila, Oscar Sans; Bhattacharjee, Rakesh; Kim, Jinkwan; Keating, Brendan; Hakonarson, Hakon; Gozal, David
INTRODUCTION/BACKGROUND:Obstructive sleep apnea (OSA) is associated with increased risk for metabolic syndrome in both adults and children. In adults with OSA, serum levels of fatty acid binding protein 4 (FABP4) are elevated and associated with the degree of metabolic insulin resistance, independent of obesity. Therefore, we assessed plasma FABP4 levels and FABP4 allelic variants in obese and non-obese children with and without OSA. METHODS:A total of 309 consecutive children ages 5-8years were recruited. Children were divided into those with OSA and without OSA (NOSA) based on the apnea-hypopnea index (AHI). Subjects were also subdivided into obese (OB) and non-obese (NOB) based on BMI z score. Morning fasting plasma FABP4 levels were assayed using ELISA, and 11 single-nucleotide polymorphisms (SNPs) within the FABP4 region were genotyped. RESULTS:Morning plasma FABP4 levels were increased in all children with OSA, even in NOB children. However, plasma FABP4 levels were strongly associated with BMI z score. Of the 11 SNPs tested, the frequency of rs1054135 (A/G) minor allele (A) was significantly increased in OSA. This SNP was also associated with increased plasma FABP4 levels in both OSA and obese subjects. The minor allele frequency of all other SNPs was similar in OSA and NOSA groups. CONCLUSIONS:Childhood obesity and OSA are associated with higher plasma FABP4 levels and thus promote cardiometabolic risk. The presence of selective SNP (e.g., rs1054135) in the FABP4 gene may account for increased plasma FABP4 levels in the context of obesity and OSA in children.
PMCID:3144996
PMID: 21664182
ISSN: 1878-5506
CID: 5477832
Nature. 2011:476(7359):170-5.DOI: 10.1038/nature10336

The landscape of recombination in African Americans

Hinch, Anjali G; Tandon, Arti; Patterson, Nick; Song, Yunli; Rohland, Nadin; Palmer, Cameron D; Chen, Gary K; Wang, Kai; Buxbaum, Sarah G; Akylbekova, Ermeg L; Aldrich, Melinda C; Ambrosone, Christine B; Amos, Christopher; Bandera, Elisa V; Berndt, Sonja I; Bernstein, Leslie; Blot, William J; Bock, Cathryn H; Boerwinkle, Eric; Cai, Qiuyin; Caporaso, Neil; Casey, Graham; Cupples, L Adrienne; Deming, Sandra L; Diver, W Ryan; Divers, Jasmin; Fornage, Myriam; Gillanders, Elizabeth M; Glessner, Joseph; Harris, Curtis C; Hu, Jennifer J; Ingles, Sue A; Isaacs, William; John, Esther M; Kao, W H Linda; Keating, Brendan; Kittles, Rick A; Kolonel, Laurence N; Larkin, Emma; Le Marchand, Loic; McNeill, Lorna H; Millikan, Robert C; Murphy, Adam; Musani, Solomon; Neslund-Dudas, Christine; Nyante, Sarah; Papanicolaou, George J; Press, Michael F; Psaty, Bruce M; Reiner, Alex P; Rich, Stephen S; Rodriguez-Gil, Jorge L; Rotter, Jerome I; Rybicki, Benjamin A; Schwartz, Ann G; Signorello, Lisa B; Spitz, Margaret; Strom, Sara S; Thun, Michael J; Tucker, Margaret A; Wang, Zhaoming; Wiencke, John K; Witte, John S; Wrensch, Margaret; Wu, Xifeng; Yamamura, Yuko; Zanetti, Krista A; Zheng, Wei; Ziegler, Regina G; Zhu, Xiaofeng; Redline, Susan; Hirschhorn, Joel N; Henderson, Brian E; Taylor, Herman A; Price, Alkes L; Hakonarson, Hakon; Chanock, Stephen J; Haiman, Christopher A; Wilson, James G; Reich, David; Myers, Simon R
Recombination, together with mutation, gives rise to genetic variation in populations. Here we leverage the recent mixture of people of African and European ancestry in the Americas to build a genetic map measuring the probability of crossing over at each position in the genome, based on about 2.1 million crossovers in 30,000 unrelated African Americans. At intervals of more than three megabases it is nearly identical to a map built in Europeans. At finer scales it differs significantly, and we identify about 2,500 recombination hotspots that are active in people of West African ancestry but nearly inactive in Europeans. The probability of a crossover at these hotspots is almost fully controlled by the alleles an individual carries at PRDM9 (P value < 10(-245)). We identify a 17-base-pair DNA sequence motif that is enriched in these hotspots, and is an excellent match to the predicted binding target of PRDM9 alleles common in West Africans and rare in Europeans. Sites of this motif are predicted to be risk loci for disease-causing genomic rearrangements in individuals carrying these alleles. More generally, this map provides a resource for research in human genetic variation and evolution.
PMID: 21775986
ISSN: 1476-4687
CID: 4317992
Human molecular genetics. 2011:20(11):2285-95.DOI: 10.1093/hmg/ddr113

Combined admixture mapping and association analysis identifies a novel blood pressure genetic locus on 5p13: contributions from the CARe consortium

Zhu, Xiaofeng; Young, J H; Fox, Ervin; Keating, Brendan J; Franceschini, Nora; Kang, Sunjung; Tayo, Bamidele; Adeyemo, Adebowale; Sun, Yun V; Li, Yali; Morrison, Alanna; Newton-Cheh, Christopher; Liu, Kiang; Ganesh, Santhi K; Kutlar, Abdullah; Vasan, Ramachandran S; Dreisbach, Albert; Wyatt, Sharon; Polak, Joseph; Palmas, Walter; Musani, Solomon; Taylor, Herman; Fabsitz, Richard; Townsend, Raymond R; Dries, Daniel; Glessner, Joseph; Chiang, Charleston W K; Mosley, Thomas; Kardia, Sharon; Curb, David; Hirschhorn, Joel N; Rotimi, Charles; Reiner, Alexander; Eaton, Charles; Rotter, Jerome I; Cooper, Richard S; Redline, Susan; Chakravarti, Aravinda; Levy, Daniel
Admixture mapping based on recently admixed populations is a powerful method to detect disease variants with substantial allele frequency differences in ancestral populations. We performed admixture mapping analysis for systolic blood pressure (SBP) and diastolic blood pressure (DBP), followed by trait-marker association analysis, in 6303 unrelated African-American participants of the Candidate Gene Association Resource (CARe) consortium. We identified five genomic regions (P< 0.001) harboring genetic variants contributing to inter-individual BP variation. In follow-up association analyses, correcting for all tests performed in this study, three loci were significantly associated with SBP and one significantly associated with DBP (P< 10(-5)). Further analyses suggested that six independent single-nucleotide polymorphisms (SNPs) contributed to the phenotypic variation observed in the admixture mapping analysis. These six SNPs were examined for replication in multiple, large, independent studies of African-Americans [Women's Health Initiative (WHI), Maywood, Genetic Epidemiology Network of Arteriopathy (GENOA) and Howard University Family Study (HUFS)] as well as one native African sample (Nigerian study), with a total replication sample size of 11 882. Meta-analysis of the replication set identified a novel variant (rs7726475) on chromosome 5 between the SUB1 and NPR3 genes, as being associated with SBP and DBP (P< 0.0015 for both); in meta-analyses combining the CARe samples with the replication data, we observed P-values of 4.45 x 10(-7) for SBP and 7.52 x 10(-7) for DBP for rs7726475 that were significant after accounting for all the tests performed. Our study highlights that admixture mapping analysis can help identify genetic variants missed by genome-wide association studies because of drastically reduced number of tests in the whole genome.
PMCID:3090198
PMID: 21422096
ISSN: 1460-2083
CID: 2747302
Human molecular genetics. 2011:20(11):2273-84.DOI: 10.1093/hmg/ddr092

Association of genetic variation with systolic and diastolic blood pressure among African Americans: the Candidate Gene Association Resource study

Fox, Ervin R; Young, J Hunter; Li, Yali; Dreisbach, Albert W; Keating, Brendan J; Musani, Solomon K; Liu, Kiang; Morrison, Alanna C; Ganesh, Santhi; Kutlar, Abdullah; Ramachandran, Vasan S; Polak, Josef F; Fabsitz, Richard R; Dries, Daniel L; Farlow, Deborah N; Redline, Susan; Adeyemo, Adebowale; Hirschorn, Joel N; Sun, Yan V; Wyatt, Sharon B; Penman, Alan D; Palmas, Walter; Rotter, Jerome I; Townsend, Raymond R; Doumatey, Ayo P; Tayo, Bamidele O; Mosley, Thomas H Jr; Lyon, Helen N; Kang, Sun J; Rotimi, Charles N; Cooper, Richard S; Franceschini, Nora; Curb, J David; Martin, Lisa W; Eaton, Charles B; Kardia, Sharon L R; Taylor, Herman A; Caulfield, Mark J; Ehret, Georg B; Johnson, Toby; Chakravarti, Aravinda; Zhu, Xiaofeng; Levy, Daniel
The prevalence of hypertension in African Americans (AAs) is higher than in other US groups; yet, few have performed genome-wide association studies (GWASs) in AA. Among people of European descent, GWASs have identified genetic variants at 13 loci that are associated with blood pressure. It is unknown if these variants confer susceptibility in people of African ancestry. Here, we examined genome-wide and candidate gene associations with systolic blood pressure (SBP) and diastolic blood pressure (DBP) using the Candidate Gene Association Resource (CARe) consortium consisting of 8591 AAs. Genotypes included genome-wide single-nucleotide polymorphism (SNP) data utilizing the Affymetrix 6.0 array with imputation to 2.5 million HapMap SNPs and candidate gene SNP data utilizing a 50K cardiovascular gene-centric array (ITMAT-Broad-CARe [IBC] array). For Affymetrix data, the strongest signal for DBP was rs10474346 (P= 3.6 x 10(-8)) located near GPR98 and ARRDC3. For SBP, the strongest signal was rs2258119 in C21orf91 (P= 4.7 x 10(-8)). The top IBC association for SBP was rs2012318 (P= 6.4 x 10(-6)) near SLC25A42 and for DBP was rs2523586 (P= 1.3 x 10(-6)) near HLA-B. None of the top variants replicated in additional AA (n = 11 882) or European-American (n = 69 899) cohorts. We replicated previously reported European-American blood pressure SNPs in our AA samples (SH2B3, P= 0.009; TBX3-TBX5, P= 0.03; and CSK-ULK3, P= 0.0004). These genetic loci represent the best evidence of genetic influences on SBP and DBP in AAs to date. More broadly, this work supports that notion that blood pressure among AAs is a trait with genetic underpinnings but also with significant complexity.
PMCID:3090190
PMID: 21378095
ISSN: 1460-2083
CID: 2747322
PLoS genetics. 2011:7(6).DOI: 10.1371/journal.pgen.1002108

Genome-wide association study of white blood cell count in 16,388 African Americans: the continental origins and genetic epidemiology network (COGENT)

Reiner, Alexander P; Lettre, Guillaume; Nalls, Michael A; Ganesh, Santhi K; Mathias, Rasika; Austin, Melissa A; Dean, Eric; Arepalli, Sampath; Britton, Angela; Chen, Zhao; Couper, David; Curb, J David; Eaton, Charles B; Fornage, Myriam; Grant, Struan F A; Harris, Tamara B; Hernandez, Dena; Kamatini, Naoyuki; Keating, Brendan J; Kubo, Michiaki; LaCroix, Andrea; Lange, Leslie A; Liu, Simin; Lohman, Kurt; Meng, Yan; Mohler, Emile R; Musani, Solomon; Nakamura, Yusuke; O'Donnell, Christopher J; Okada, Yukinori; Palmer, Cameron D; Papanicolaou, George J; Patel, Kushang V; Singleton, Andrew B; Takahashi, Atsushi; Tang, Hua; Taylor, Herman A; Taylor, Kent; Thomson, Cynthia; Yanek, Lisa R; Yang, Lingyao; Ziv, Elad; Zonderman, Alan B; Folsom, Aaron R; Evans, Michele K; Liu, Yongmei; Becker, Diane M; Snively, Beverly M; Wilson, James G
Total white blood cell (WBC) and neutrophil counts are lower among individuals of African descent due to the common African-derived "null" variant of the Duffy Antigen Receptor for Chemokines (DARC) gene. Additional common genetic polymorphisms were recently associated with total WBC and WBC sub-type levels in European and Japanese populations. No additional loci that account for WBC variability have been identified in African Americans. In order to address this, we performed a large genome-wide association study (GWAS) of total WBC and cell subtype counts in 16,388 African-American participants from 7 population-based cohorts available in the Continental Origins and Genetic Epidemiology Network. In addition to the DARC locus on chromosome 1q23, we identified two other regions (chromosomes 4q13 and 16q22) associated with WBC in African Americans (P<2.5×10(-8)). The lead SNP (rs9131) on chromosome 4q13 is located in the CXCL2 gene, which encodes a chemotactic cytokine for polymorphonuclear leukocytes. Independent evidence of the novel CXCL2 association with WBC was present in 3,551 Hispanic Americans, 14,767 Japanese, and 19,509 European Americans. The index SNP (rs12149261) on chromosome 16q22 associated with WBC count is located in a large inter-chromosomal segmental duplication encompassing part of the hydrocephalus inducing homolog (HYDIN) gene. We demonstrate that the chromosome 16q22 association finding is most likely due to a genotyping artifact as a consequence of sequence similarity between duplicated regions on chromosomes 16q22 and 1q21. Among the WBC loci recently identified in European or Japanese populations, replication was observed in our African-American meta-analysis for rs445 of CDK6 on chromosome 7q21 and rs4065321 of PSMD3-CSF3 region on chromosome 17q21. In summary, the CXCL2, CDK6, and PSMD3-CSF3 regions are associated with WBC count in African American and other populations. We also demonstrate that large inter-chromosomal duplications can result in false positive associations in GWAS.
PMID: 21738479
ISSN: 1553-7404
CID: 5477852
PLoS genetics. 2011:7(6).DOI: 10.1371/journal.pgen.1002134

Genome-wide association of bipolar disorder suggests an enrichment of replicable associations in regions near genes

Smith, Erin N; Koller, Daniel L; Panganiban, Corrie; Szelinger, Szabolcs; Zhang, Peng; Badner, Judith A; Barrett, Thomas B; Berrettini, Wade H; Bloss, Cinnamon S; Byerley, William; Coryell, William; Edenberg, Howard J; Foroud, Tatiana; Gershon, Elliot S; Greenwood, Tiffany A; Guo, Yiran; Hipolito, Maria; Keating, Brendan J; Lawson, William B; Liu, Chunyu; Mahon, Pamela B; McInnis, Melvin G; McMahon, Francis J; McKinney, Rebecca; Murray, Sarah S; Nievergelt, Caroline M; Nurnberger, John I; Nwulia, Evaristus A; Potash, James B; Rice, John; Schulze, Thomas G; Scheftner, William A; Shilling, Paul D; Zandi, Peter P; Zöllner, Sebastian; Craig, David W; Schork, Nicholas J; Kelsoe, John R
Although a highly heritable and disabling disease, bipolar disorder's (BD) genetic variants have been challenging to identify. We present new genotype data for 1,190 cases and 401 controls and perform a genome-wide association study including additional samples for a total of 2,191 cases and 1,434 controls. We do not detect genome-wide significant associations for individual loci; however, across all SNPs, we show an association between the power to detect effects calculated from a previous genome-wide association study and evidence for replication (P = 1.5×10(-7)). To demonstrate that this result is not likely to be a false positive, we analyze replication rates in a large meta-analysis of height and show that, in a large enough study, associations replicate as a function of power, approaching a linear relationship. Within BD, SNPs near exons exhibit a greater probability of replication, supporting an enrichment of reproducible associations near functional regions of genes. These results indicate that there is likely common genetic variation associated with BD near exons (±10 kb) that could be identified in larger studies and, further, provide a framework for assessing the potential for replication when combining results from multiple studies.
PMCID:3128104
PMID: 21738484
ISSN: 1553-7404
CID: 5477862
Circulation: Cardiovascular genetics. 2011:4(2):145-55.DOI: 10.1161/CIRCGENETICS.110.957563

Dense genotyping of candidate gene loci identifies variants associated with high-density lipoprotein cholesterol

Edmondson, Andrew C; Braund, Peter S; Stylianou, Ioannis M; Khera, Amit V; Nelson, Christopher P; Wolfe, Megan L; Derohannessian, Stephanie L; Keating, Brendan J; Qu, Liming; He, Jing; Tobin, Martin D; Tomaszewski, Maciej; Baumert, Jens; Klopp, Norman; Döring, Angela; Thorand, Barbara; Li, Mingyao; Reilly, Muredach P; Koenig, Wolfgang; Samani, Nilesh J; Rader, Daniel J
BACKGROUND:Plasma levels of high-density lipoprotein cholesterol (HDL-C) are known to be heritable, but only a fraction of the heritability is explained. We used a high-density genotyping array containing single-nucleotide polymorphisms (SNPs) from HDL-C candidate genes selected on known biology of HDL-C metabolism, mouse genetic studies, and human genetic association studies. SNP selection was based on tagging SNPs and included low-frequency nonsynonymous SNPs. METHODS AND RESULTS/RESULTS:Association analysis in a cohort containing extremes of HDL-C (case-control, n=1733) provided a discovery phase, with replication in 3 additional populations for a total meta-analysis in 7857 individuals. We replicated the majority of loci identified through genome-wide association studies and present on the array (including ABCA1, APOA1/C3/A4/A5, APOB, APOE/C1/C2, CETP, CTCF-PRMT8, FADS1/2/3, GALNT2, LCAT, LILRA3, LIPC, LIPG, LPL, LRP4, SCARB1, TRIB1, ZNF664) and provide evidence that suggests an association in several previously unreported candidate gene loci (including ABCG1, GPR109A/B/81, NFKB1, PON1/2/3/4). There was evidence for multiple, independent association signals in 5 loci, including association with low-frequency nonsynonymous variants. CONCLUSIONS:Genetic loci associated with HDL-C are likely to harbor multiple, independent causative variants, frequently with opposite effects on the HDL-C phenotype. Cohorts comprising subjects at the extremes of the HDL-C distribution may be efficiently used in a case-control discovery of quantitative traits.
PMCID:3319351
PMID: 21303902
ISSN: 1942-3268
CID: 5477822