Your search keyword '"Tara Matise"' showing total 8 results

1. Methylation patterns associated with C-reactive protein in racially and ethnically diverse populations

Author

Jessica I. Lundin, Ulrike Peters, Yao Hu, Farah Ammous, Christy L. Avery, Emelia J. Benjamin, Joshua C. Bis, Jennifer A. Brody, Chris Carlson, Mary Cushman, Chris Gignoux, Xiuqing Guo, Jeff Haessler, Chris Haiman, Roby Joehanes, Silva Kasela, Eimear Kenny, Tuuli Lapalainien, Daniel Levy, Chunyu Liu, Yongmei Liu, Ruth J.F. Loos, Ake Lu, Tara Matise, Kari E. North, Sungshim L. Park, Scott M. Ratliff, Alex Reiner, Stephen S. Rich, Jerome I. Rotter, Jennifer A. Smith, Nona Sotoodehnia, Russell Tracy, David Van den Berg, Huichun Xu, Ting Ye, Wei Zhao, Laura M. Raffield, and Charles Kooperberg

Subjects

Inflammation, C-reactive protein, methylation, epigenetics, EWAS, racial and ethnic diversity, Genetics, QH426-470

Abstract

Systemic low-grade inflammation is a feature of chronic disease. C-reactive protein (CRP) is a common biomarker of inflammation and used as an indicator of disease risk; however, the role of inflammation in disease is not completely understood. Methylation is an epigenetic modification in the DNA which plays a pivotal role in gene expression. In this study we evaluated differential DNA methylation patterns associated with blood CRP level to elucidate biological pathways and genetic regulatory mechanisms to improve the understanding of chronic inflammation. The racially and ethnically diverse participants in this study were included as 50% White, 41% Black or African American, 7% Hispanic or Latino/a, and 2% Native Hawaiian, Asian American, American Indian, or Alaska Native (total n = 13,433) individuals. We replicated 113 CpG sites from 87 unique loci, of which five were novel (CADM3, NALCN, NLRC5, ZNF792, and cg03282312), across a discovery set of 1,150 CpG sites associated with CRP level (p

Published

2024

2. Improving polygenic risk prediction in admixed populations by explicitly modeling ancestral-differential effects via GAUDI

Author

Quan Sun, Bryce T. Rowland, Jiawen Chen, Anna V. Mikhaylova, Christy Avery, Ulrike Peters, Jessica Lundin, Tara Matise, Steve Buyske, Ran Tao, Rasika A. Mathias, Alexander P. Reiner, Paul L. Auer, Nancy J. Cox, Charles Kooperberg, Timothy A. Thornton, Laura M. Raffield, and Yun Li

Subjects

Science

Abstract

Abstract Polygenic risk scores (PRS) have shown successes in clinics, but most PRS methods focus only on participants with distinct primary continental ancestry without accommodating recently-admixed individuals with mosaic continental ancestry backgrounds for different segments of their genomes. Here, we develop GAUDI, a novel penalized-regression-based method specifically designed for admixed individuals. GAUDI explicitly models ancestry-differential effects while borrowing information across segments with shared ancestry in admixed genomes. We demonstrate marked advantages of GAUDI over other methods through comprehensive simulation and real data analyses for traits with associated variants exhibiting ancestral-differential effects. Leveraging data from the Women’s Health Initiative study, we show that GAUDI improves PRS prediction of white blood cell count and C-reactive protein in African Americans by > 64% compared to alternative methods, and even outperforms PRS-CSx with large European GWAS for some scenarios. We believe GAUDI will be a valuable tool to mitigate disparities in PRS performance in admixed individuals.

Published

2024

3. Functional equivalence of genome sequencing analysis pipelines enables harmonized variant calling across human genetics projects

Author

Allison A. Regier, Yossi Farjoun, David E. Larson, Olga Krasheninina, Hyun Min Kang, Daniel P. Howrigan, Bo-Juen Chen, Manisha Kher, Eric Banks, Darren C. Ames, Adam C. English, Heng Li, Jinchuan Xing, Yeting Zhang, Tara Matise, Goncalo R. Abecasis, Will Salerno, Michael C. Zody, Benjamin M. Neale, and Ira M. Hall

Subjects

Science

Abstract

Sharing of whole genome sequencing (WGS) data improves study scale and power, but data from different groups are often incompatible. Here, US genome centers and NIH programs define WGS data processing standards and a flexible validation method, facilitating collaboration in human genetics research.

Published

2018

4. The genetic underpinnings of variation in ages at menarche and natural menopause among women from the multi-ethnic Population Architecture using Genomics and Epidemiology (PAGE) Study: A trans-ethnic meta-analysis.

Author

Lindsay Fernández-Rhodes, Jennifer R Malinowski, Yujie Wang, Ran Tao, Nathan Pankratz, Janina M Jeff, Sachiko Yoneyama, Cara L Carty, V Wendy Setiawan, Loic Le Marchand, Christopher Haiman, Steven Corbett, Ellen Demerath, Gerardo Heiss, Myron Gross, Petra Buzkova, Dana C Crawford, Steven C Hunt, D C Rao, Karen Schwander, Aravinda Chakravarti, Omri Gottesman, Noura S Abul-Husn, Erwin P Bottinger, Ruth J F Loos, Leslie J Raffel, Jie Yao, Xiuqing Guo, Suzette J Bielinski, Jerome I Rotter, Dhananjay Vaidya, Yii-Der Ida Chen, Sheila F Castañeda, Martha Daviglus, Robert Kaplan, Gregory A Talavera, Kelli K Ryckman, Ulrike Peters, Jose Luis Ambite, Steven Buyske, Lucia Hindorff, Charles Kooperberg, Tara Matise, Nora Franceschini, and Kari E North

Subjects

Medicine, Science

Abstract

Current knowledge of the genetic architecture of key reproductive events across the female life course is largely based on association studies of European descent women. The relevance of known loci for age at menarche (AAM) and age at natural menopause (ANM) in diverse populations remains unclear. We investigated 32 AAM and 14 ANM previously-identified loci and sought to identify novel loci in a trans-ethnic array-wide study of 196,483 SNPs on the MetaboChip (Illumina, Inc.). A total of 45,364 women of diverse ancestries (African, Hispanic/Latina, Asian American and American Indian/Alaskan Native) in the Population Architecture using Genomics and Epidemiology (PAGE) Study were included in cross-sectional analyses of AAM and ANM. Within each study we conducted a linear regression of SNP associations with self-reported or medical record-derived AAM or ANM (in years), adjusting for birth year, population stratification, and center/region, as appropriate, and meta-analyzed results across studies using multiple meta-analytic techniques. For both AAM and ANM, we observed more directionally consistent associations with the previously reported risk alleles than expected by chance (p-valuesbinomial≤0.01). Eight densely genotyped reproductive loci generalized significantly to at least one non-European population. We identified one trans-ethnic array-wide SNP association with AAM and two significant associations with ANM, which have not been described previously. Additionally, we observed evidence of independent secondary signals at three of six AAM trans-ethnic loci. Our findings support the transferability of reproductive trait loci discovered in European women to women of other race/ethnicities and indicate the presence of additional trans-ethnic associations both at both novel and established loci. These findings suggest the benefit of including diverse populations in future studies of the genetic architecture of female growth and development.

Published

2018

5. Strategies for Enriching Variant Coverage in Candidate Disease Loci on a Multiethnic Genotyping Array.

Author

Stephanie A Bien, Genevieve L Wojcik, Niha Zubair, Christopher R Gignoux, Alicia R Martin, Jonathan M Kocarnik, Lisa W Martin, Steven Buyske, Jeffrey Haessler, Ryan W Walker, Iona Cheng, Mariaelisa Graff, Lucy Xia, Nora Franceschini, Tara Matise, Regina James, Lucia Hindorff, Loic Le Marchand, Kari E North, Christopher A Haiman, Ulrike Peters, Ruth J F Loos, Charles L Kooperberg, Carlos D Bustamante, Eimear E Kenny, Christopher S Carlson, and PAGE Study

Subjects

Medicine, Science

Abstract

Investigating genetic architecture of complex traits in ancestrally diverse populations is imperative to understand the etiology of disease. However, the current paucity of genetic research in people of African and Latin American ancestry, Hispanic and indigenous peoples in the United States is likely to exacerbate existing health disparities for many common diseases. The Population Architecture using Genomics and Epidemiology, Phase II (PAGE II), Study was initiated in 2013 by the National Human Genome Research Institute to expand our understanding of complex trait loci in ethnically diverse and well characterized study populations. To meet this goal, the Multi-Ethnic Genotyping Array (MEGA) was designed to substantially improve fine-mapping and functional discovery by increasing variant coverage across multiple ethnicities at known loci for metabolic, cardiovascular, renal, inflammatory, anthropometric, and a variety of lifestyle traits. Studying the frequency distribution of clinically relevant mutations, putative risk alleles, and known functional variants across multiple populations will provide important insight into the genetic architecture of complex diseases and facilitate the discovery of novel, sometimes population-specific, disease associations. DNA samples from 51,650 self-identified African ancestry (17,328), Hispanic/Latino (22,379), Asian/Pacific Islander (8,640), and American Indian (653) and an additional 2,650 participants of either South Asian or European ancestry, and other reference panels have been genotyped on MEGA by PAGE II. MEGA was designed as a new resource for studying ancestrally diverse populations. Here, we describe the methodology for selecting trait-specific content for use in multi-ethnic populations and how enriching MEGA for this content may contribute to deeper biological understanding of the genetic etiology of complex disease.

Published

2016

6. Improving polygenic risk prediction in admixed populations by explicitly modeling ancestral-specific effects via GAUDI

Author

Quan Sun, Bryce T. Rowland, Jiawen Chen, Anna V. Mikhaylova, Christy Avery, Ulrike Peters, Jessica Lundin, Tara Matise, Steve Buyske, Ran Tao, Rasika A. Mathias, Alexander P. Reiner, Paul L. Auer, Nancy J. Cox, Charles Kooperberg, Timothy A. Thornton, Laura M. Raffield, and Yun Li

Abstract

Polygenic risk scores (PRS) have shown successes in clinics, but most PRS methods have focused only on individuals with one primary continental ancestry, thus poorly accommodating recently-admixed individuals. Here, we develop GAUDI, a novel penalized-regression-based method specifically designed for admixed individuals by explicitly modeling ancestry-specific effects and jointly estimating ancestry-shared effects. We demonstrate marked advantages of GAUDI over other methods through comprehensive simulation and real data analyses.

Published

2022

7. Genotype imputation of Metabochip SNPs using a study-specific reference panel of ~4,000 haplotypes in African Americans from the Women's Health Initiative

Author

Eric Yi, Liu, Steven, Buyske, Aaron K, Aragaki, Ulrike, Peters, Eric, Boerwinkle, Chris, Carlson, Cara, Carty, Dana C, Crawford, Jeff, Haessler, Lucia A, Hindorff, Loic Le, Marchand, Teri A, Manolio, Tara, Matise, Wei, Wang, Charles, Kooperberg, Kari E, North, and Yun, Li

Subjects

Genotype, Models, Genetic, Genome, Human, Reproducibility of Results, Polymorphism, Single Nucleotide, United States, Article, Black or African American, Phenotype, Gene Frequency, Haplotypes, Humans, Women's Health, Female, Alleles, Software, Genome-Wide Association Study, Oligonucleotide Array Sequence Analysis

Abstract

Genetic imputation has become standard practice in modern genetic studies. However, several important issues have not been adequately addressed including the utility of study-specific reference, performance in admixed populations, and quality for less common (minor allele frequency [MAF] 0.005-0.05) and rare (MAF0.005) variants. These issues only recently became addressable with genome-wide association studies (GWAS) follow-up studies using dense genotyping or sequencing in large samples of non-European individuals. In this work, we constructed a study-specific reference panel of 3,924 haplotypes using African Americans in the Women's Health Initiative (WHI) genotyped on both the Metabochip and the Affymetrix 6.0 GWAS platform. We used this reference panel to impute into 6,459 WHI SNP Health Association Resource (SHARe) study subjects with only GWAS genotypes. Our analysis confirmed the imputation quality metric Rsq (estimated r(2) , specific to each SNP) as an effective post-imputation filter. We recommend different Rsq thresholds for different MAF categories such that the average (across SNPs) Rsq is above the desired dosage r(2) (squared Pearson correlation between imputed and experimental genotypes). With a desired dosage r(2) of 80%, 99.9% (97.5%, 83.6%, 52.0%, 20.5%) of SNPs with MAF0.05 (0.03-0.05, 0.01-0.03, 0.005-0.01, and 0.001-0.005) passed the post-imputation filter. The average dosage r(2) for these SNPs is 94.7%, 92.1%, 89.0%, 83.1%, and 79.7%, respectively. These results suggest that for African Americans imputation of Metabochip SNPs from GWAS data, including low frequency SNPs with MAF 0.005-0.05, is feasible and worthwhile for power increase in downstream association analysis provided a sizable reference panel is available.

Published

2012

8. Abstract 051: Trans-ethnic Metabochip Genotyping of Established Lipid Loci Identifies Low Frequency Susceptibility Variants and Additional Independent Signals in Known Loci

Author

Ying Wu, Steven Buyske, Themistocles Assimes, Linda S Adair, Christie Ballantyne, Cara L Carty, Iona Cheng, David Duggan, Logan Dumitrescu, Charles B Eaton, Alan B Feranil, Lucia A Hindorff, Tara Matise, Sabrina Mitchell, Yi Lin, Ulrike Peters, Jennifer G Robinson, Fred Schumacher, Alicia Young, Charles Kooperberg, Dana Crawford, Karen L Mohlke, and Kari E North

Subjects

Physiology (medical), Cardiology and Cardiovascular Medicine

Abstract

Genome-wide association studies (GWAS) have identified ∼100 loci for triglycerides (TG), high-density lipoprotein cholesterol (HDL-C) and low-density lipoprotein cholesterol (LDL-C), but much of the trait heritability remains unexplained. We conducted a trans-ethnic study in 5,884 African Americans (AA) in the Population Architecture using Genomics and Epidemiology (PAGE) consortium [the Atherosclerosis Risk in Communities Study (ARIC), the Multiethnic Cohort Study (MEC) and the Women's Health Initiative (WHI)], and 1,719 East Asians (ASN) from the Cebu Longitudinal Health and Nutrition Survey (CLHNS) to analyze high-density genotyped Metabochip SNPs for association with TG, HDL-C and LDL-C. We aimed to identify population-specific and additional independent signals at established lipid loci and to assess the relative evidence of association with SNPs previously reported to have a functional effect. Among the 58 lipid loci tested, evidence of association (Prs769455 (APOE R163C, MAF=0.002, prior evidence of biological function) that together accounted for 1.7% of the total TG variation compared to the 1.0% explained by the strongest APOE-C1 SNP alone. At a third locus, TG-associated APOA5, two reportedly functional variants, S19W (MAF=0.059) and −3A>G (MAF=0.26), exhibited the strongest association in AA and ASN, respectively. In AA, three independent signals at APOA5 explained 1.7% of the TG variation; in ASN, two independent signals explained 3.3% of total variation. The reportedly functional variants were included or well-represented on Metabochip at ten loci. At eight of the ten loci, the reported variants (at 6 loci) or proxies (r2>.95, at 2 loci) showed the strongest association in at least one population. This study highlights the value of the trans-ethnic high-density genotyping to identify a wider spectrum of susceptibility variants at reported loci, both additional independent signals and population-specific SNP effects, that more than double the trait variation explained. In addition, the large fraction of reportedly functional SNPs that showed the strongest evidence of association suggests that lead SNPs at novel loci frequently may be good candidates for functional studies.

Published

2012