Your search keyword '"Ozan Dikilitas"' showing total 21 results

1. Multiancestral polygenic risk score for pediatric asthma

Author

Bahram Namjou, Michael Lape, Edyta Malolepsza, Stanley B. DeVore, Matthew T. Weirauch, Ozan Dikilitas, Gail P. Jarvik, Krzysztof Kiryluk, Iftikhar J. Kullo, Cong Liu, Yuan Luo, Benjamin A. Satterfield, Jordan W. Smoller, Theresa L. Walunas, John Connolly, Patrick Sleiman, Tesfaye B. Mersha, Frank D. Mentch, Hakon Hakonarson, Cynthia A. Prows, Jocelyn M. Biagini, Gurjit K. Khurana Hershey, Lisa J. Martin, and Leah Kottyan

Subjects

Multifactorial Inheritance, Risk Factors, Immunology, Humans, Immunology and Allergy, Genetic Predisposition to Disease, Bayes Theorem, Child, Polymorphism, Single Nucleotide, Asthma, Genome-Wide Association Study

Abstract

Asthma is the most common chronic condition in children and the third leading cause of hospitalization in pediatrics. The genome-wide association study catalog reports 140 studies with genome-wide significance. A polygenic risk score (PRS) with predictive value across ancestries has not been evaluated for this important trait.This study aimed to train and validate a PRS relying on genetic determinants for asthma to provide predictions for disease occurrence in pediatric cohorts of diverse ancestries.This study applied a Bayesian regression framework method using the Trans-National Asthma Genetic Consortium genome-wide association study summary statistics to derive a multiancestral PRS score, used one Electronic Medical Records and Genomics (eMERGE) cohort as a training set, used a second independent eMERGE cohort to validate the score, and used the UK Biobank data to replicate the findings. A phenome-wide association study was performed using the PRS to identify shared genetic etiology with other phenotypes.The multiancestral asthma PRS was associated with asthma in the 2 pediatric validation datasets. Overall, the multiancestral asthma PRS has an area under the curve (AUC) of 0.70 (95% CI, 0.69-0.72) in the pediatric validation 1 and AUC of 0.66 (0.65-0.66) in the pediatric validation 2 datasets. We found significant discrimination across pediatric subcohorts of European (AUC, 95% CI, 0.60 and 0.66), African (AUC, 95% CI, 0.61 and 0.66), admixed American (AUC, 0.64 and 0.70), Southeast Asian (AUC, 0.65), and East Asian (AUC, 0.73) ancestry. Pediatric participants with the top 5% PRS had 2.80 to 5.82 increased odds of asthma compared to the bottom 5% across the training, validation 1, and validation 2 cohorts when adjusted for ancestry. Phenome-wide association study analysis confirmed the strong association of the identified PRS with asthma (odds ratio, 2.71, PsubFDR/sub = 3.71 × 10sup-65/sup) and related phenotypes.A multiancestral PRS for asthma based on Bayesian posterior genomic effect sizes identifies increased odds of pediatric asthma.

Published

2022

2. Use of Polygenic Risk Scores for Coronary Heart Disease in Ancestrally Diverse Populations

Author

Ozan Dikilitas, Daniel J. Schaid, Catherine Tcheandjieu, Shoa L. Clarke, Themistocles L. Assimes, and Iftikhar J. Kullo

Subjects

Risk Factors, Humans, Coronary Disease, Genetic Predisposition to Disease, Cardiology and Cardiovascular Medicine, Article, Genome-Wide Association Study

Abstract

PURPOSE OF REVIEW: A polygenic risk score (PRS) is a measure of genetic liability to a disease and is typically normally distributed in a population. Individuals in the upper tail of this distribution often have relative risk equivalent to that of monogenic form of the disease. The majority of currently available PRSs for coronary heart disease (CHD) have been generated from cohorts of European ancestry (EUR) and vary in their applicability to other ancestry groups. In this report, we review the performance of PRSs for CHD across different ancestries and efforts to reduce variability in performance including novel population and statistical genetics approaches. RECENT FINDINGS: PRSs for CHD perform robustly in EUR populations but lag in performance in non-EUR groups, particularly individuals of African ancestry. Several large consortia have been established to enable genomic studies in diverse ancestry groups and develop methods to improve PRS performance in multi-ancestry contexts as well as admixed individuals. These include fine-mapping to ascertain causal variants, trans ancestry meta-analyses, and ancestry deconvolution in admixed individuals. SUMMARY: PRSs are being used in the clinical setting but enthusiasm has been tempered by the variable performance in non-EUR ancestry groups. Increasing diversity in genomic association studies and continued innovation in methodological approaches are needed to improve PRS performance in non-EUR individuals for equitable implementation of genomic medicine.

Published

2022

3. Neptune: an environment for the delivery of genomic medicine

Author

Venner Eric, Victoria Yi, David Murdock, Sara E. Kalla, Tsung-Jung Wu, Aniko Sabo, Shoudong Li, Qingchang Meng, Xia Tian, Mullai Murugan, Michelle Cohen, Christie Kovar, Wei-Qi Wei, Wendy K. Chung, Chunhua Weng, Georgia L. Wiesner, Gail P. Jarvik, Donna Muzny, Richard A. Gibbs, Debra Abrams, Samuel E. Adunyah, Ladia Albertson-Junkans, Berta Almoguera, Darren C. Ames, Paul Appelbaum, Samuel Aronson, Sharon Aufox, Lawrence J. Babb, Adithya Balasubramanian, Hana Bangash, Melissa Basford, Lisa Bastarache, Samantha Baxter, Meckenzie Behr, Barbara Benoit, Elizabeth Bhoj, Suzette J. Bielinski, Sarah T. Bland, Carrie Blout, Kenneth Borthwick, Erwin P. Bottinger, Mark Bowser, Harrison Brand, Murray Brilliant, Wendy Brodeur, Pedro Caraballo, David Carrell, Andrew Carroll, Lisa Castillo, Victor Castro, Gauthami Chandanavelli, Theodore Chiang, Rex L. Chisholm, Kurt D. Christensen, Wendy Chung, Christopher G. Chute, Brittany City, Beth L. Cobb, John J. Connolly, Paul Crane, Katherine Crew, David R. Crosslin, Jyoti Dayal, Mariza De Andrade, Jessica De la Cruz, Josh C. Denny, Shawn Denson, Tim DeSmet, Ozan Dikilitas, Michael J. Dinsmore, Sheila Dodge, Phil Dunlea, Todd L. Edwards, Christine M. Eng, David Fasel, Alex Fedotov, Qiping Feng, Mark Fleharty, Andrea Foster, Robert Freimuth, Christopher Friedrich, Stephanie M. Fullerton, Birgit Funke, Stacey Gabriel, Vivian Gainer, Ali Gharavi, Andrew M. Glazer, Joseph T. Glessner, Jessica Goehringer, Adam S. Gordon, Chet Graham, Robert C. Green, Justin H. Gundelach, Heather S. Hain, Hakon Hakonarson, Maegan V. Harden, John Harley, Margaret Harr, Andrea Hartzler, M. Geoffrey Hayes, Scott Hebbring, Nora Henrikson, Andrew Hershey, Christin Hoell, Ingrid Holm, Kayla M. Howell, George Hripcsak, Jianhong Hu, Elizabeth Duffy Hynes, Joy C. Jayaseelan, Yunyun Jiang, Yoonjung Yoonie Joo, Sheethal Jose, Navya Shilpa Josyula, Anne E. Justice, Divya Kalra, Elizabeth W. Karlson, Brendan J. Keating, Melissa A. Kelly, Eimear E. Kenny, Dustin Key, Krzysztof Kiryluk, Terrie Kitchner, Barbara Klanderman, Eric Klee, David C. Kochan, Viktoriya Korchina, Leah Kottyan, Emily Kudalkar, Alanna Kulchak Rahm, Iftikhar J. Kullo, Philip Lammers, Eric B. Larson, Matthew S. Lebo, Magalie Leduc, Ming Ta (Michael) Lee, Niall J. Lennon, Kathleen A. Leppig, Nancy D. Leslie, Rongling Li, Wayne H. Liang, Chiao-Feng Lin, Jodell E. Linder, Noralane M. Lindor, Todd Lingren, James G. Linneman, Cong Liu, Wen Liu, Xiuping Liu, John Lynch, Hayley Lyon, Alyssa Macbeth, Harshad Mahadeshwar, Lisa Mahanta, Bradley Malin, Teri Manolio, Maddalena Marasa, Keith Marsolo, Michelle L. McGowan, Elizabeth McNally, Jim Meldrim, Frank Mentch, Hila Milo Rasouly, Jonathan Mosley, Shubhabrata Mukherjee, Thomas E. Mullen, Jesse Muniz, David R. Murdock, Shawn Murphy, Melanie F. Myers, Bahram Namjou, Yizhao Ni, Robert C. Onofrio, Aniwaa Owusu Obeng, Thomas N. Person, Josh F. Peterson, Lynn Petukhova, Cassandra J. Pisieczko, Siddharth Pratap, Cynthia A. Prows, Megan J. Puckelwartz, Ritika Raj, James D. Ralston, Arvind Ramaprasan, Andrea Ramirez, Luke Rasmussen, Laura Rasmussen-Torvik, Soumya Raychaudhuri, Heidi L. Rehm, Marylyn D. Ritchie, Catherine Rives, Beenish Riza, Dan M. Roden, Elisabeth A. Rosenthal, Avni Santani, Schaid Dan, Steven Scherer, Stuart Scott, Aaron Scrol, Soumitra Sengupta, Ning Shang, Himanshu Sharma, Richard R. Sharp, Rajbir Singh, Patrick M.A. Sleiman, Kara Slowik, Joshua C. Smith, Maureen E. Smith, Duane T. Smoot, Jordan W. Smoller, Sunghwan Sohn, Ian B. Stanaway, Justin Starren, Mary Stroud, Jessica Su, Casey Overby Taylor, Kasia Tolwinski, Sara L. Van Driest, Sean M. Vargas, Matthew Varugheese, David Veenstra, Eric Venner, Miguel Verbitsky, Gina Vicente, Michael Wagner, Kimberly Walker, Theresa Walunas, Liwen Wang, Qiaoyan Wang, Scott T. Weiss, Quinn S. Wells, Peter S. White, Ken L. Wiley, Janet L. Williams, Marc S. Williams, Michael W. Wilson, Leora Witkowski, Laura Allison Woods, Betty Woolf, Julia Wynn, Yaping Yang, Ge Zhang, Lan Zhang, and Hana Zouk

Subjects

Computer science, business.industry, Process (engineering), MEDLINE, High-Throughput Nucleotide Sequencing, Genomics, Data science, Article, Personalization, Variety (cybernetics), Workflow, Neptune, Pharmacogenomics, Health care, Electronic Health Records, Humans, business, Software, Genetics (clinical)

Abstract

Genomic medicine holds great promise for improving health care, but integrating searchable and actionable genetic data into electronic health records (EHRs) remains a challenge. Here we describe Neptune, a system for managing the interaction between a clinical laboratory and an EHR system during the clinical reporting process. We developed Neptune and applied it to two clinical sequencing projects that required report customization, variant reanalysis, and EHR integration. Neptune has been applied for the generation and delivery of over 15,000 clinical genomic reports. This work spans two clinical tests based on targeted gene panels that contain 68 and 153 genes respectively. These projects demanded customizable clinical reports that contained a variety of genetic data types including single-nucleotide variants (SNVs), copy-number variants (CNVs), pharmacogenomics, and polygenic risk scores. Two variant reanalysis activities were also supported, highlighting this important workflow. Methods are needed for delivering structured genetic data to EHRs. This need extends beyond developing data formats to providing infrastructure that manages the reporting process itself. Neptune was successfully applied on two high-throughput clinical sequencing projects to build and deliver clinical reports to EHR systems. The software is open source and available at https://gitlab.com/bcm-hgsc/neptune .

Published

2021

4. Genome-wide association and multi-trait analyses characterize the common genetic architecture of heart failure

Author

Michael G, Levin, Noah L, Tsao, Pankhuri, Singhal, Chang, Liu, Ha My T, Vy, Ishan, Paranjpe, Joshua D, Backman, Tiffany R, Bellomo, William P, Bone, Kiran J, Biddinger, Qin, Hui, Ozan, Dikilitas, Benjamin A, Satterfield, Yifan, Yang, Michael P, Morley, Yuki, Bradford, Megan, Burke, Nosheen, Reza, Brian, Charest, Renae L, Judy, Megan J, Puckelwartz, Hakon, Hakonarson, Atlas, Khan, Leah C, Kottyan, Iftikhar, Kullo, Yuan, Luo, Elizabeth M, McNally, Laura J, Rasmussen-Torvik, Sharlene M, Day, Ron, Do, Lawrence S, Phillips, Patrick T, Ellinor, Girish N, Nadkarni, Marylyn D, Ritchie, Zoltan, Arany, Thomas P, Cappola, Kenneth B, Margulies, Krishna G, Aragam, Christopher M, Haggerty, Jacob, Joseph, Yan V, Sun, Benjamin F, Voight, and Scott M, Damrauer

Subjects

Heart Failure, Phenotype, Multidisciplinary, Gene Expression Profiling, Humans, General Physics and Astronomy, Heart, Genetic Predisposition to Disease, General Chemistry, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, Genome-Wide Association Study

Abstract

Heart failure is a leading cause of cardiovascular morbidity and mortality. However, the contribution of common genetic variation to heart failure risk has not been fully elucidated, particularly in comparison to other common cardiometabolic traits. We report a multi-ancestry genome-wide association study meta-analysis of all-cause heart failure including up to 115,150 cases and 1,550,331 controls of diverse genetic ancestry, identifying 47 risk loci. We also perform multivariate genome-wide association studies that integrate heart failure with related cardiac magnetic resonance imaging endophenotypes, identifying 61 risk loci. Gene-prioritization analyses including colocalization and transcriptome-wide association studies identify known and previously unreported candidate cardiomyopathy genes and cellular processes, which we validate in gene-expression profiling of failing and healthy human hearts. Colocalization, gene expression profiling, and Mendelian randomization provide convergent evidence for the roles of BCKDHA and circulating branch-chain amino acids in heart failure and cardiac structure. Finally, proteome-wide Mendelian randomization identifies 9 circulating proteins associated with heart failure or quantitative imaging traits. These analyses highlight similarities and differences among heart failure and associated cardiovascular imaging endophenotypes, implicate common genetic variation in the pathogenesis of heart failure, and identify circulating proteins that may represent cardiomyopathy treatment targets.

Published

2022

5. Genetic Architecture of Abdominal Aortic Aneurysm in the Million Veteran Program

Author

Derek Klarin, Shefali Setia Verma, Renae Judy, Ozan Dikilitas, Brooke N. Wolford, Ishan Paranjpe, Michael G. Levin, Cuiping Pan, Catherine Tcheandjieu, Joshua M. Spin, Julie Lynch, Themistocles L. Assimes, Linn Åldstedt Nyrønning, Erney Mattsson, Todd L. Edwards, Josh Denny, Eric Larson, Ming Ta Michael Lee, David Carrell, Yanfei Zhang, Gail P. Jarvik, Ali G. Gharavi, John Harley, Frank Mentch, Jennifer A. Pacheco, Hakon Hakonarson, Anne Heidi Skogholt, Laurent Thomas, Maiken Elvestad Gabrielsen, Kristian Hveem, Jonas Bille Nielsen, Wei Zhou, Lars Fritsche, Jie Huang, Pradeep Natarajan, Yan V. Sun, Scott L. DuVall, Daniel J. Rader, Kelly Cho, Kyong-Mi Chang, Peter W.F. Wilson, Christopher J. O’Donnell, Sekar Kathiresan, Salvatore T. Scali, Scott A. Berceli, Cristen Willer, Gregory T. Jones, Matthew J. Bown, Girish Nadkarni, Iftikhar J. Kullo, Marylyn Ritchie, Scott M. Damrauer, Philip S. Tsao, J. Michael Gaziano, Rachel Ramoni, Jean Beckham, Jim Breeling, Grant Huang, Sumitra Muralidhar, J.P. Casas Romero, Jennifer Moser, Stacey B. Whitbourne, Jessica V. Brewer, John Concato, Stuart Warren, Dean P. Argyres, Brady Stephens, Mary T. Brophy, Donald E. Humphries, Nhan Do, Shahpoor Shayan, Xuan-Mai T. Nguyen, Saiju Pyarajan, Elizabeth Hauser, Yan Sun, Hongyu Zhao, Peter Wilson, Rachel McArdle, Louis Dellitalia, Clement J. Zablocki, Jeffrey Whittle, John Wells, Salvador Gutierrez, Gretchen Gibson, Laurence Kaminsky, Gerardo Villareal, Scott Kinlay, Junzhe Xu, Mark Hamner, Kathlyn Sue Haddock, Sujata Bhushan, Pran Iruvanti, Michael Godschalk, Zuhair Ballas, Malcolm Buford, Stephen Mastorides, Jon Klein, Nora Ratcliffe, Hermes Florez, Alan Swann, Maureen Murdoch, Peruvemba Sriram, Shing Shing Yeh, Ronald Washburn, Darshana Jhala, Samuel Aguayo, David Cohen, Satish Sharma, John Callaghan, Kris Ann Oursler, Mary Whooley, Sunil Ahuja, Amparo Gutierrez, Ronald Schifman, Jennifer Greco, Michael Rauchman, Richard Servatius, Mary Oehlert, Agnes Wallbom, Ronald Fernando, Timothy Morgan, Todd Stapley, Scott Sherman, Gwenevere Anderson, Philip Tsao, Elif Sonel, Edward Boyko, Laurence Meyer, Samir Gupta, Joseph Fayad, Adriana Hung, Jack Lichy, Robin Hurley, Brooks Robey, and Robert Striker

Subjects

medicine.medical_specialty, Genome-wide association study, 030204 cardiovascular system & hematology, Aortic disease, aortic diseases, 03 medical and health sciences, 0302 clinical medicine, Aneurysm, Original Research Articles, Physiology (medical), Internal medicine, medicine, Humans, Veterans, 030304 developmental biology, Cardiovascular mortality, 0303 health sciences, genome-wide association study, business.industry, medicine.disease, Abdominal aortic aneurysm, Genetic architecture, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, aneurysm, Cardiology, Cardiology and Cardiovascular Medicine, business, Aortic Aneurysm, Abdominal

Abstract

Supplemental Digital Content is available in the text., Background: Abdominal aortic aneurysm (AAA) is an important cause of cardiovascular mortality; however, its genetic determinants remain incompletely defined. In total, 10 previously identified risk loci explain a small fraction of AAA heritability. Methods: We performed a genome-wide association study in the Million Veteran Program testing ≈18 million DNA sequence variants with AAA (7642 cases and 172 172 controls) in veterans of European ancestry with independent replication in up to 4972 cases and 99 858 controls. We then used mendelian randomization to examine the causal effects of blood pressure on AAA. We examined the association of AAA risk variants with aneurysms in the lower extremity, cerebral, and iliac arterial beds, and derived a genome-wide polygenic risk score (PRS) to identify a subset of the population at greater risk for disease. Results: Through a genome-wide association study, we identified 14 novel loci, bringing the total number of known significant AAA loci to 24. In our mendelian randomization analysis, we demonstrate that a genetic increase of 10 mm Hg in diastolic blood pressure (odds ratio, 1.43 [95% CI, 1.24–1.66]; P=1.6×10−6), as opposed to systolic blood pressure (odds ratio, 1.06 [95% CI, 0.97–1.15]; P=0.2), likely has a causal relationship with AAA development. We observed that 19 of 24 AAA risk variants associate with aneurysms in at least 1 other vascular territory. A 29-variant PRS was strongly associated with AAA (odds ratioPRS, 1.26 [95% CI, 1.18–1.36]; PPRS=2.7×10−11 per SD increase in PRS), independent of family history and smoking risk factors (odds ratioPRS+family history+smoking, 1.24 [95% CI, 1.14–1.35]; PPRS=1.27×10−6). Using this PRS, we identified a subset of the population with AAA prevalence greater than that observed in screening trials informing current guidelines. Conclusions: We identify novel AAA genetic associations with therapeutic implications and identify a subset of the population at significantly increased genetic risk of AAA independent of family history. Our data suggest that extending current screening guidelines to include testing to identify those with high polygenic AAA risk, once the cost of genotyping becomes comparable with that of screening ultrasound, would significantly increase the yield of current screening at reasonable cost.

Published

2020

6. Evaluation of the MC4R gene across eMERGE network identifies many unreported obesity-associated variants

Author

John B. Harley, Marc S. Williams, Ozan Dikilitas, Jordan G. Nestor, Joshua C. Denny, Todd Lingren, David J. Carey, Ashley H. Shoemaker, Ian B. Stanaway, Bahram Namjou, Iftikhar J. Kullo, David R. Crosslin, Tooraj Mirshahi, Barbara Benoit, Ning Shang, Xinnan Niu, Rajbir Singh, Frank D. Mentch, Gail P. Jarvik, and Hakon Hakonarson

Subjects

Adult, Male, 0301 basic medicine, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Locus (genetics), Genome-wide association study, Development, 030105 genetics & heredity, Biology, Article, Body Mass Index, Cohort Studies, 03 medical and health sciences, Humans, Obesity, Allele, Genotyping, Aged, Genetics, Variant Call Format, Nutrition and Dietetics, Haplotype, Genetic Variation, Middle Aged, Penetrance, 030104 developmental biology, Cohort, Receptor, Melanocortin, Type 4, Female, Genome-Wide Association Study

Abstract

Background/Objectives Melanocortin-4 receptor (MC4R) plays an essential role in food intake and energy homeostasis. More than 170 MC4R variants have been described over the past two decades, with conflicting reports regarding the prevalence and phenotypic effects of these variants in diverse cohorts. To determine the frequency of MC4R variants in large cohort of different ancestries, we evaluated the MC4R coding region for 20,537 eMERGE participants with sequencing data plus additional 77,454 independent individuals with genome-wide genotyping data at this locus. Subjects/Methods The sequencing data were obtained from the eMERGE phase III study, in which multisample variant call format calls have been generated, curated, and annotated. In addition to penetrance estimation using body mass index (BMI) as a binary outcome, GWAS and PheWAS were performed using median BMI in linear regression analyses. All results were adjusted for principal components, age, sex, and sites of genotyping. Results Targeted sequencing data of MC4R revealed 125 coding variants in 1839 eMERGE participants including 30 unreported coding variants that were predicted to be functionally damaging. Highly penetrant unreported variants included (L325I, E308K, D298N, S270F, F261L, T248A, D111V, and Y80F) in which seven participants had obesity class III defined as BMI ≥ 40 kg/m2. In GWAS analysis, in addition to known risk haplotype upstream of MC4R (best variant rs6567160 (P = 5.36 × 10−25, Beta = 0.37), a novel rare haplotype was detected which was protective against obesity and encompassed the V103I variant with known gain-of-function properties (P = 6.23 × 10−08, Beta = −0.62). PheWAS analyses extended this protective effect of V103I to type 2 diabetes, diabetic nephropathy, and chronic renal failure independent of BMI. Conclusions MC4R screening in a large eMERGE cohort confirmed many previous findings, extend the MC4R pleotropic effects, and discovered additional MC4R rare alleles that probably contribute to obesity.

Published

2020

7. Under-specification as the source of ambiguity and vagueness in narrative phenotype algorithm definitions

Author

Jingzhi Yu, Ozan Dikilitas, George Hripcsak, Luke V. Rasmussen, Chunhua Weng, Iftikhar J. Kullo, Shawn N. Murphy, Jennifer A. Pacheco, Frank D. Mentch, Robert R. Freimuth, Robert J. Carroll, Hakon Hakonarson, David Carrell, Ning Shang, Yuan Luo, Vivian S. Gainer, Wei-Qi Wei, Anika S Ghosh, Andrea H. Ramirez, Peggy L. Peissig, Nephi A. Walton, and Barbara Benoit

Subjects

Ambiguity, Computer science, Knowledge Bases, media_common.quotation_subject, Computer applications to medicine. Medical informatics, R858-859.7, Health Informatics, computer.software_genre, Electronic Health Records, Humans, Narrative, media_common, business.industry, Research, Health Policy, Under-Specification, Vagueness, Genomics, Electronic Health Records (EHR), Computer Science Applications, Phenotype, Phenotyping, Algorithm: Natural Language, Artificial intelligence, business, computer, Algorithms, Natural language processing

Abstract

Introduction Currently, one of the commonly used methods for disseminating electronic health record (EHR)-based phenotype algorithms is providing a narrative description of the algorithm logic, often accompanied by flowcharts. A challenge with this mode of dissemination is the potential for under-specification in the algorithm definition, which leads to ambiguity and vagueness. Methods This study examines incidents of under-specification that occurred during the implementation of 34 narrative phenotyping algorithms in the electronic Medical Record and Genomics (eMERGE) network. We reviewed the online communication history between algorithm developers and implementers within the Phenotype Knowledge Base (PheKB) platform, where questions could be raised and answered regarding the intended implementation of a phenotype algorithm. Results We developed a taxonomy of under-specification categories via an iterative review process between two groups of annotators. Under-specifications that lead to ambiguity and vagueness were consistently found across narrative phenotype algorithms developed by all involved eMERGE sites. Discussion and conclusion Our findings highlight that under-specification is an impediment to the accuracy and efficiency of the implementation of current narrative phenotyping algorithms, and we propose approaches for mitigating these issues and improved methods for disseminating EHR phenotyping algorithms.

Published

2022

8. Uterine fibroid polygenic risk score (PRS) associates and predicts risk for uterine fibroid

Author

Jacqueline A, Piekos, Jacklyn N, Hellwege, Yanfei, Zhang, Eric S, Torstenson, Gail P, Jarvik, Ozan, Dikilitas, Iftikhar J, Kullo, Daniel J, Schaid, David R, Crosslin, Sarah A, Pendergrass, Ming Ta Michael, Lee, Dan, Roden, Josh C, Denny, Todd L, Edwards, and Digna R, Velez Edwards

Subjects

Leiomyoma, Risk Factors, Humans, Female, Genetic Predisposition to Disease, Genomics, Linkage Disequilibrium, Genome-Wide Association Study

Abstract

Uterine fibroids (UF) are common pelvic tumors in women, heritable, and genome-wide association studies (GWAS) have identified ~ 30 loci associated with increased risk in UF. Using summary statistics from a previously published UF GWAS performed in a non-Hispanic European Ancestry (NHW) female subset from the Electronic Medical Records and Genomics (eMERGE) Network, we constructed a polygenic risk score (PRS) for UF. UF-PRS was developed using PRSice and optimized in the separate clinical population of BioVU. PRS was validated using parallel methods of 10-fold cross-validation logistic regression and phenome-wide association study (PheWAS) in a seperate subset of eMERGE NHW females (validation set), excluding samples used in GWAS. PRSice determined p

Published

2021

9. Genome-wide polygenic score to predict chronic kidney disease across ancestries

Author

Atlas Khan, Michael C. Turchin, Amit Patki, Vinodh Srinivasasainagendra, Ning Shang, Rajiv Nadukuru, Alana C. Jones, Edyta Malolepsza, Ozan Dikilitas, Iftikhar J. Kullo, Daniel J. Schaid, Elizabeth Karlson, Tian Ge, James B. Meigs, Jordan W. Smoller, Christoph Lange, David R. Crosslin, Gail P. Jarvik, Pavan K. Bhatraju, Jacklyn N. Hellwege, Paulette Chandler, Laura Rasmussen Torvik, Alex Fedotov, Cong Liu, Christopher Kachulis, Niall Lennon, Noura S. Abul-Husn, Judy H. Cho, Iuliana Ionita-Laza, Ali G. Gharavi, Wendy K. Chung, George Hripcsak, Chunhua Weng, Girish Nadkarni, Marguerite R. Irvin, Hemant K. Tiwari, Eimear E. Kenny, Nita A. Limdi, and Krzysztof Kiryluk

Subjects

Multifactorial Inheritance, Genotype, General Medicine, Apolipoprotein L1, Polymorphism, Single Nucleotide, Article, General Biochemistry, Genetics and Molecular Biology, Gene Frequency, Risk Factors, Humans, Genetic Predisposition to Disease, Renal Insufficiency, Chronic, Alleles, Genome-Wide Association Study

Abstract

Chronic kidney disease (CKD) is a common complex condition associated with high morbidity and mortality. Polygenic prediction could enhance CKD screening and prevention; however, this approach has not been optimized for ancestrally diverse populations. By combining APOL1 risk genotypes with genome-wide association studies (GWAS) of kidney function, we designed, optimized and validated a genome-wide polygenic score (GPS) for CKD. The new GPS was tested in 15 independent cohorts, including 3 cohorts of European ancestry (n = 97,050), 6 cohorts of African ancestry (n = 14,544), 4 cohorts of Asian ancestry (n = 8,625) and 2 admixed Latinx cohorts (n = 3,625). We demonstrated score transferability with reproducible performance across all tested cohorts. The top 2% of the GPS was associated with nearly threefold increased risk of CKD across ancestries. In African ancestry cohorts, the APOL1 risk genotype and polygenic component of the GPS had additive effects on the risk of CKD.

Published

2021

10. Generalizability of Polygenic Risk Scores for Breast Cancer Among Women With European, African, and Latinx Ancestry

Author

Eric B. Larson, Stephanie M. Fullerton, Ozan Dikilitas, Nur Zeinomar, Alexander G. Bick, Paul K. Crane, George Hripcsak, Robb Rowley, Krzysztof Kiryluk, Teri A. Manolio, Chunhua Weng, Gail P. Jarvik, Atlas Khan, Georgia L. Wiesner, Mary Beth Terry, Jordan W. Smoller, Ali G. Gharavi, Katherine D. Crew, Ning Shang, Ann E. Justice, Cong Liu, Alanna Kulchak Rahm, Wendy K. Chung, and David Fasel

Subjects

Linkage disequilibrium, Black People, Information Storage and Retrieval, Breast Neoplasms, Logistic regression, Linkage Disequilibrium, White People, Breast cancer, Gene Frequency, Risk Factors, Genotype, Odds Ratio, Medicine, Electronic Health Records, Humans, Generalizability theory, Genetic Predisposition to Disease, business.industry, Medical record, General Medicine, Odds ratio, Genomics, Hispanic or Latino, Middle Aged, medicine.disease, Logistic Models, Phenotype, Female, business, Algorithms, Cohort study, Demography

Abstract

Importance Multiple polygenic risk scores (PRSs) for breast cancer have been developed from large research consortia; however, their generalizability to diverse clinical settings is unknown. Objective To examine the performance of previously developed breast cancer PRSs in a clinical setting for women of European, African, and Latinx ancestry. Design, Setting, and Participants This cohort study using the Electronic Medical Records and Genomics (eMERGE) network data set included 39 591 women from 9 contributing medical centers in the US that had electronic medical records (EMR) linked to genotype data. Breast cancer cases and controls were identified through a validated EMR phenotyping algorithm. Main Outcomes and Measures Multivariable logistic regression was used to assess the association between breast cancer risk and 7 previously developed PRSs, adjusting for age, study site, breast cancer family history, and first 3 ancestry informative principal components. Results This study included 39 591 women: 33 594 with European, 3801 with African, and 2196 with Latinx ancestry. The mean (SD) age at breast cancer diagnosis was 60.7 (13.0), 58.8 (12.5), and 60.1 (13.0) years for women with European, African, and Latinx ancestry, respectively. PRSs derived from women with European ancestry were associated with breast cancer risk in women with European ancestry (highest odds ratio [OR] per 1-SD increase, 1.46; 95% CI, 1.41-1.51), women with Latinx ancestry (highest OR, 1.31; 95% CI, 1.09-1.58), and women with African ancestry (OR, 1.19; 95% CI, 1.05-1.35). For women with European ancestry, this association with breast cancer risk was largest in the extremes of the PRS distribution, with ORs ranging from 2.19 (95% CI, 1.84-2.53) to 2.48 (95% CI, 1.89-3.25) for the 3 different PRSs examined for those in the highest 1% of the PRS compared with those in the middle quantile. Among women with Latinx and African ancestries at the extremes of the PRS distribution, there were no statistically significant associations. Conclusions and Relevance This cohort study found that PRS models derived from women with European ancestry for breast cancer risk generalized well for women with European, Latinx, and African ancestries across different clinical settings, although the effect sizes for women with African ancestry were smaller, likely because of differences in risk allele frequencies and linkage disequilibrium patterns. These results highlight the need to improve representation of diverse population groups, particularly women with African ancestry, in genomic research cohorts.

Published

2021

11. Associations of Genetically Predicted Lp(a) (Lipoprotein [a]) Levels With Cardiovascular Traits in Individuals of European and African Ancestry

Author

Themistocles L. Assimes, Ozan Dikilitas, Maya S. Safarova, Mariza de Andrade, Amy S. Shah, Iftikhar J. Kullo, Gail P. Jarvik, Bahram Namjou-Khales, Shoa L. Clarke, Benjamin A. Satterfield, Wei-Qi Wei, Elisabeth A. Rosenthal, QiPing Feng, Teri A. Manolio, Xiang Zhu, Anne E. Justice, Ning Shang, Catherine Tcheandjieu, Eric B. Larson, Elaine M. Urbina, Lisa Bastarache, and Scott J. Hebbring

Subjects

Male, 0301 basic medicine, A lipoprotein, Black People, 030204 cardiovascular system & hematology, Biology, Article, White People, 03 medical and health sciences, Quantitative Trait, Heritable, 0302 clinical medicine, Humans, Genetic Predisposition to Disease, Aged, Aged, 80 and over, Genetics, Mendelian Randomization Analysis, General Medicine, Middle Aged, United Kingdom, 030104 developmental biology, Cardiovascular Diseases, Female, Lipoprotein(a), Lipoprotein

Abstract

Background: Lp(a) (lipoprotein [a]) levels are higher in individuals of African ancestry (AA) than in individuals of European ancestry (EA). We examined associations of genetically predicted Lp(a) levels with (1) atherosclerotic cardiovascular disease subtypes: coronary heart disease, cerebrovascular disease, peripheral artery disease, and abdominal aortic aneurysm and (2) nonatherosclerotic cardiovascular disease phenotypes, stratified by ancestry. Methods: We performed (1) Mendelian randomization analyses for previously reported cardiovascular associations and (2) Mendelian randomization–phenome-wide association analyses for novel associations. Analyses were stratified by ancestry in electronic Medical Records and Genomics, United Kingdom Biobank, and Million Veteran Program cohorts separately and in a combined cohort of 804 507 EA and 103 580 AA participants. Results: In Mendelian randomization analyses using the combined cohort, a 1-SD genetic increase in Lp(a) level was associated with atherosclerotic cardiovascular disease subtypes in EA—odds ratio and 95% CI for coronary heart disease 1.28 (1.16–1.41); cerebrovascular disease 1.14 (1.07–1.21); peripheral artery disease 1.22 (1.11–1.34); abdominal aortic aneurysm 1.28 (1.17–1.40); in AA, the effect estimate was lower than in EA and nonsignificant for coronary heart disease 1.11 (0.99–1.24) and cerebrovascular disease 1.06 (0.99–1.14) but similar for peripheral artery disease 1.16 (1.01–1.33) and abdominal aortic aneurysm 1.34 (1.11–1.62). In EA, a 1-SD genetic increase in Lp(a) level was associated with aortic valve disorders 1.34 (1.10–1.62), mitral valve disorders 1.18 (1.09–1.27), congestive heart failure 1.12 (1.05–1.19), and chronic kidney disease 1.07 (1.01–1.14). In AA, no significant associations were noted for aortic valve disorders 1.08 (0.94–1.25), mitral valve disorders 1.02 (0.89–1.16), congestive heart failure 1.02 (0.95–1.10), or chronic kidney disease 1.05 (0.99–1.12). Mendelian randomization–phenome-wide association analyses identified novel associations in EA with arterial thromboembolic disease, nonaortic aneurysmal disease, atrial fibrillation, cardiac conduction disorders, and hypertension. Conclusions: Many cardiovascular associations of genetically increased Lp(a) that were significant in EA were not significant in AA. Lp(a) was associated with atherosclerotic cardiovascular disease in four major arterial beds in EA but only with peripheral artery disease and abdominal aortic aneurysm in AA. Additionally, novel cardiovascular associations were detected in EA.

Published

2021

12. Harmonizing Clinical Sequencing and Interpretation for the eMERGE III Network

Author

Ian B. Stanaway, Dan M. Roden, Divya Kalra, Dustin Key, Debra J. Abrams, David Fasel, Victor Castro, Brad Malin, Berta Almoguera, Beenish Riza, Meckenzie A. Behr, Eric Venner, Christine M. Eng, Joy Jayaseelan, Scott J. Hebbring, Michelle L. McGowan, Steven E. Scherer, Theresa L. Walunas, Mark Bowser, James D. Ralston, Wei-Qi Wei, Liwen Wang, David R. Murdock, Wayne H. Liang, Julia Wynn, Nancy D. Leslie, Laura J. Rasmussen-Torvik, Ming Ta (Michael) Lee, Frank D. Mentch, Lan Zhang, Alanna Kulchak Rahm, Josh F. Peterson, Jodell E. Linder, Joshua C. Smith, Soumitra Sengupta, Brendan J. Keating, Gina Vicente, Andrew Carroll, Nora B. Henrikson, Anne E. Justice, Heather S. Hain, Wen Liu, Andrea H. Ramirez, Matthew S. Lebo, Hana Zouk, Georgia L. Wiesner, Andrea L. Hartzler, Cassandra J. Pisieczko, Catherine M. Rives, Jessica Goehringer, Maegan V. Harden, John Lynch, Chiao-Feng Lin, Peter White, Phil Dunlea, Shawn N. Murphy, Mullai Murugan, Harshad Mahadeshwar, Mark Fleharty, Andrea Foster, Arvind Ramaprasan, Christopher A. Friedrich, Justin H. Gundelach, Hayley Lyon, Niall J. Lennon, Eric W. Klee, David R. Crosslin, Ge Zhang, Rongling Li, Ozan Dikilitas, Xiuping Liu, Christin Hoell, Aniwaa Owusu Obeng, Katherine D. Crew, Lisa M. Castillo, Justin Starren, Jonathan D. Mosley, Carrie L. Blout, Himanshu Sharma, Elizabeth M. McNally, Sarah T. Bland, Megan J. Puckelwartz, Matthew Varugheese, Keith Marsolo, Betty Woolf, Sharon Aufox, Janet L. Williams, Kimberly Walker, Murray H. Brilliant, Birgit Funke, Laura Allison Woods, Marylyn D. Ritchie, Brittany City, Todd Lingren, Hila Milo Rasouly, Lawrence J. Babb, Alex Fedotov, Robert C. Onofrio, Margaret Harr, Suzette J. Bielinski, Michael W. Wilson, Shubhabrata Mukherjee, Robert R. Freimuth, Chet Graham, Todd L. Edwards, Quinn S. Wells, Marc S. Williams, Jordan W. Smoller, Wendy K. Chung, Avni Santani, Paul K. Crane, George Hripcsak, QiPing Feng, Ali G. Gharavi, Yizhao Ni, Iftikhar J. Kullo, Michael Wagner, Philip E. Lammers, Michael J. Dinsmore, Thomas N. Person, Victoria Yi, Samuel E. Adunyah, Tim DeSmet, Eric B. Larson, Elizabeth Hynes, David C. Kochan, Eimear E. Kenny, Magalie S. Leduc, Lisa Mahanta, David Carrell, Paul S. Appelbaum, Viktoriya Korchina, Beth L. Cobb, Lynn Petukhova, Jessica De la Cruz, Patrick M. A. Sleiman, Stuart A. Scott, Tsung-Jung Wu, Gail P. Jarvik, Erwin P. Bottinger, Ken Wiley, Josh C. Denny, Melissa A. Basford, Samuel J. Aronson, David L. Veenstra, Yaping Yang, Kayla Marie Howell, John J. Connolly, Jessica Su, Yoonjung Yoonie Joo, Miguel Verbitsky, Sean M. Vargas, Cong Liu, Barbara Benoit, Andrew Hershey, Richard A. Gibbs, Cynthia A. Prows, Hana Bangash, Wendy Brodeur, Gauthami Chandanavelli, Sara L. Van Driest, Kurt D. Christensen, Elizabeth J. Bhoj, Vivian S. Gainer, Adam S. Gordon, Robert C. Green, Hakon Hakonarson, Krzysztof Kiryluk, Elisabeth A. Rosenthal, Rajbir Singh, James G. Linneman, Harrison Brand, Theodore Chiang, Sheila Dodge, Ingrid A. Holm, M. Geoffrey Hayes, Yunyun Jiang, Ning Shang, Samantha Baxter, Noralane M. Lindor, Kathleen A. Leppig, Teri A. Manolio, Sara E. Kalla, Pedro J. Caraballo, Ritika Raj, Aaron Scrol, Jyoti G. Dayal, Richard R. Sharp, Christie Kovar, Soumya Raychaudhuri, Sunghwan Sohn, Emily Kudalkar, Maddalena Marasa, Stacey Gabriel, Dan Schaid, Ladia Albertson-Junkans, Rex L. Chisholm, Maureen E. Smith, Donna M. Muzny, Casey Overby Taylor, Jianhong Hu, Elizabeth W. Karlson, Lisa Bastarache, Darren C. Ames, Joseph T. Glessner, Leora Witkowski, Siddharth Pratap, Qiaoyan Wang, Melissa A. Kelly, Adithya Balasubramanian, Kara Slowik, Terrie Kitchner, Barbara J. Klanderman, Shawn Denson, Mary Stroud, Alyssa Macbeth, Melanie F. Myers, Jesse Muniz, Kasia Tolwinski, Scott T. Weiss, Chunhua Weng, Stephanie M. Fullerton, John B. Harley, Christopher G. Chute, Heidi L. Rehm, Sheethal Jose, Andrew M. Glazer, Navya Shilpa Josyula, Kenneth M. Borthwick, Thomas E. Mullen, Mariza de Andrade, Leah C. Kottyan, Luke V. Rasmussen, James Meldrim, and Bahram Namjou

Subjects

0301 basic medicine, Standardization, Test data generation, business.industry, Computer science, Sequence Analysis, DNA, 030105 genetics & heredity, Precision medicine, Data science, Clinical decision support system, Biobank, Article, 3. Good health, Data sharing, 03 medical and health sciences, 030104 developmental biology, Genetics, Humans, Genetic Testing, Prospective Studies, Sample collection, Personalized medicine, Precision Medicine, business, Genetics (clinical)

Abstract

The advancement of precision medicine requires new methods to coordinate and deliver genetic data from heterogeneous sources to physicians and patients. The eMERGE III Network enrolled >25,000 participants from biobank and prospective cohorts of predominantly healthy individuals for clinical genetic testing to determine clinically actionable findings. The network developed protocols linking together the 11 participant collection sites and 2 clinical genetic testing laboratories. DNA capture panels targeting 109 genes were used for testing of DNA and sample collection, data generation, interpretation, reporting, delivery, and storage were each harmonized. A compliant and secure network enabled ongoing review and reconciliation of clinical interpretations, while maintaining communication and data sharing between clinicians and investigators. A total of 202 individuals had positive diagnostic findings relevant to the indication for testing and 1,294 had additional/secondary findings of medical significance deemed to be returnable, establishing data return rates for other testing endeavors. This study accomplished integration of structured genomic results into multiple electronic health record (EHR) systems, setting the stage for clinical decision support to enable genomic medicine. Further, the established processes enable different sequencing sites to harmonize technical and interpretive aspects of sequencing tests, a critical achievement toward global standardization of genomic testing. The eMERGE protocols and tools are available for widespread dissemination.

Published

2019

13. Arrhythmia variant associations and reclassifications in the eMERGE-III sequencing study

Author

Gail P. Jarvik, Carlos G. Vanoye, Reshma R. Desai, Lauren Lee Rinke, Hakon Hakonarson, Eric B. Larson, Ozan Dikilitas, Christian M. Shaffer, Zachary T. Yoneda, Ning Shang, George Hripcsak, Teri A. Manolio, Giovanni Davogustto, Bahram Namjou, Tooraj Mirshahi, Patrick Sleiman, Ayesha Muhammad, Elizabeth M. McNally, Olivia R. Kalash, Quinn S. Wells, Kathleen A. Leppig, Jonathan D. Mosley, Driest Slv, Jonathan Z. Luo, Daniel J. Schaid, Yuko Wada, Shoemaker Mb, Tao Yang, Wei-Qi Wei, Brett M. Kroncke, James D. Ralston, Sarah Bland, David Carrell, J. Glessner, Devyn Mitchell, Jennifer A. Pacheco, Cong Liu, Wendy K. Chung, Dan M. Roden, Chunhua Weng, Iftikhar J. Kullo, Tarek Alsaied, Sunghwan Sohn, Josh C. Denny, Adam S. Gordon, Rajbir Singh, Ashutosh Singhal, Alfred L. George, Eric Farber-Eger, and Andrew M. Glazer

Subjects

Long QT syndrome, Bioinformatics, Article, Genomic Medicine, Likely benign, Physiology (medical), medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Prospective Studies, Functional studies, Uncertain significance, Gene, Likely pathogenic, Disease gene, business.industry, Arrhythmias, Cardiac, Genomics, medicine.disease, Phenotype, Death, Sudden, Cardiac, HEK293 Cells, Cardiology and Cardiovascular Medicine, business

Abstract

Background: Sequencing Mendelian arrhythmia genes in individuals without an indication for arrhythmia genetic testing can identify carriers of pathogenic or likely pathogenic (P/LP) variants. However, the extent to which these variants are associated with clinically meaningful phenotypes before or after return of variant results is unclear. In addition, the majority of discovered variants are currently classified as variants of uncertain significance, limiting clinical actionability. Methods: The eMERGE-III study (Electronic Medical Records and Genomics Phase III) is a multicenter prospective cohort that included 21 846 participants without previous indication for cardiac genetic testing. Participants were sequenced for 109 Mendelian disease genes, including 10 linked to arrhythmia syndromes. Variant carriers were assessed with electronic health record–derived phenotypes and follow-up clinical examination. Selected variants of uncertain significance (n=50) were characterized in vitro with automated electrophysiology experiments in HEK293 cells. Results: As previously reported, 3.0% of participants had P/LP variants in the 109 genes. Herein, we report 120 participants (0.6%) with P/LP arrhythmia variants. Compared with noncarriers, arrhythmia P/LP carriers had a significantly higher burden of arrhythmia phenotypes in their electronic health records. Fifty-four participants had variant results returned. Nineteen of these 54 participants had inherited arrhythmia syndrome diagnoses (primarily long-QT syndrome), and 12 of these 19 diagnoses were made only after variant results were returned (0.05%). After in vitro functional evaluation of 50 variants of uncertain significance, we reclassified 11 variants: 3 to likely benign and 8 to P/LP. Conclusions: Genome sequencing in a large population without indication for arrhythmia genetic testing identified phenotype-positive carriers of variants in congenital arrhythmia syndrome disease genes. As the genomes of large numbers of people are sequenced, the disease risk from rare variants in arrhythmia genes can be assessed by integrating genomic screening, electronic health record phenotypes, and in vitro functional studies. Registration: URL: https://www.clinicaltrials.gov ; Unique identifier; NCT03394859.

Published

2021

14. Leveraging the Electronic Health Record to Address the COVID-19 Pandemic

Author

Ozan Dikilitas, Iftikhar J. Kullo, and Benjamin A. Satterfield

Subjects

SARS-CoV-2, Severe Acute Respiratory Syndrome Coronavirus-2, Psychological intervention, MEDLINE, EHR, Electronic health record, ACE2, Angiotensin-converting enzyme-2, Disease, Review, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Resource (project management), Pandemic, medicine, Electronic Health Records, Humans, IFN, interferon, 030212 general & internal medicine, TMPRSS2, Transmembrane protease, serine 2, Disease surveillance, COVID-19, Coronavirus disease 2019, SARS-CoV-2, business.industry, Drug Repositioning, COVID-19, General Medicine, medicine.disease, eMERGE, electronic Medical Records and Genomics, Epidemiological Monitoring, CRP, C-reactive protein, UK, United Kingdom, Medical emergency, Contact Tracing, business, Contact tracing, GWAS, Genome-wide association study

Abstract

The coronavirus disease 2019 (COVID-19) pandemic continues its global spread. Coordinated effort on a vast scale is required to halt its progression and to save lives. Electronic health record (EHR) data are a valuable resource to mitigate the COVID-19 pandemic. We review how the EHR could be used for disease surveillance and contact tracing. When linked to "omics" data, the EHR could facilitate identification of genetic susceptibility variants, leading to insights into risk factors, disease complications, and drug repurposing. Real-time monitoring of patients could enable early detection of potential complications, informing appropriate interventions and therapy. We reviewed relevant articles from PubMed, MEDLINE, and Google Scholar searches as well as preprint servers, given the rapidly evolving understanding of the COVID-19 pandemic.

Published

2021

15. Response to Li and Hopper

Author

Roger L. Milne, Jane C. Figueiredo, Kenneth Offit, Daniel D. Buchanan, Wendy K. Chung, Robert J. MacInnis, Marc J. Gunter, Catherine M. Tangen, Li Hsu, Emily White, Peter T. Campbell, Stéphane Bézieau, Andrew T. Chan, David C. Muller, Lori C. Sakoda, Bahram Namjou, Annika Lindblom, Temitope O. Keku, Vicente Martín, D. Timothy Bishop, Amit Joshi, Robert E. Schoen, Ludmila Vodickova, Mark A. Jenkins, Pavel Vodicka, Richard B. Hayes, Antoni Castells, Hermann Brenner, Daniel J. Schaid, David Duggan, Christopher I. Li, Mingyang Song, John B. Harley, Jeffrey K. Lee, Ozan Dikilitas, Douglas A. Corley, Neil Murphy, Steven Gallinger, Cornelia M. Ulrich, Victor Moreno, Clemens Schafmayer, Elizabeth A. Platz, Noralane M. Lindor, Elisabeth A. Rosenthal, Alicja Wolk, Yu Ru Su, Martha L. Slattery, Hakon Hakonarson, Stephen B. Gruber, Eric B. Larson, Graham G. Giles, Demetrius Albanes, Jenny Chang-Claude, Christopher H. Dampier, David R. Crosslin, Michael Hoffmeister, Andrea Gsur, Stephen N. Thibodeau, Shuji Ogino, Frank D. Mentch, Sonja I. Berndt, Bethany Van Guelpen, Kala Visvanathan, Loic Le Marchand, John D. Potter, Jeroen R. Huyghe, Heather Hampel, Gail P. Jarvik, Jochen Hampe, Graham Casey, Wei-Qi Wei, David A. Drew, Corinne E. Joshu, Aung Ko Win, Qianchuan He, Paul D.P. Pharoah, Michael O. Woods, Flora Qu, Ulrike Peters, Minta Thomas, Fränzel J.B. Van Duijnhoven, Ian B. Stanaway, Keith R. Curtis, Tabitha A. Harrison, Andrea N. Burnett-Hartman, Anna H. Wu, Edward Giovannucci, Li Li, Volker Arndt, Mathieu Lemire, Thomas J. Hudson, Albert de la Chapelle, Veronika Vymetalkova, Syed H.E. Zaidi, Jessica Minnier, Polly A. Newcomb, and Sergi Castellví-Bel

Subjects

Male, Multifactorial Inheritance, Nutrition and Disease, MEDLINE, Polymorphism, Single Nucleotide, Risk Assessment, Text mining, Asian People, Risk Factors, Voeding en Ziekte, Genetics, Humans, Medicine, Life Science, Genetic Predisposition to Disease, Letter to the Editor, Genetics (clinical), Aged, Information retrieval, Genome, Human, business.industry, Bayes Theorem, Middle Aged, Female, Colorectal Neoplasms, business, Genome-Wide Association Study

Abstract

Accurate colorectal cancer (CRC) risk prediction models are critical for identifying individuals at low and high risk of developing CRC, as they can then be offered targeted screening and interventions to address their risks of developing disease (if they are in a high-risk group) and avoid unnecessary screening and interventions (if they are in a low-risk group). As it is likely that thousands of genetic variants contribute to CRC risk, it is clinically important to investigate whether these genetic variants can be used jointly for CRC risk prediction. In this paper, we derived and compared different approaches to generating predictive polygenic risk scores (PRS) from genome-wide association studies (GWASs) including 55,105 CRC-affected case subjects and 65,079 control subjects of European ancestry. We built the PRS in three ways, using (1) 140 previously identified and validated CRC loci; (2) SNP selection based on linkage disequilibrium (LD) clumping followed by machine-learning approaches; and (3) LDpred, a Bayesian approach for genome-wide risk prediction. We tested the PRS in an independent cohort of 101,987 individuals with 1,699 CRC-affected case subjects. The discriminatory accuracy, calculated by the age- and sex-adjusted area under the receiver operating characteristics curve (AUC), was highest for the LDpred-derived PRS (AUC = 0.654) including nearly 1.2 M genetic variants (the proportion of causal genetic variants for CRC assumed to be 0.003), whereas the PRS of the 140 known variants identified from GWASs had the lowest AUC (AUC = 0.629). Based on the LDpred-derived PRS, we are able to identify 30% of individuals without a family history as having risk for CRC similar to those with a family history of CRC, whereas the PRS based on known GWAS variants identified only top 10% as having a similar relative risk. About 90% of these individuals have no family history and would have been considered average risk under current screening guidelines, but might benefit from earlier screening. The developed PRS offers a way for risk-stratified CRC screening and other targeted interventions.

Published

2021

16. Risk Factors for Polyvascular Involvement in Patients With Peripheral Artery Disease: A Mendelian Randomization Study

Author

Benjamin A. Satterfield, Ozan Dikilitas, and Iftikhar J. Kullo

Subjects

Male, Translational Studies, Arterial disease, Coronary Disease, Disease, 030204 cardiovascular system & hematology, High morbidity, 0302 clinical medicine, Risk Factors, Odds Ratio, Medicine, 0303 health sciences, Lipids and Cholesterol, Smoking, blood pressure, Middle Aged, Phenotype, Feature (computer vision), Hypertension, Cardiology, Female, Cardiology and Cardiovascular Medicine, Algorithms, polyvascular disease, Polyvascular disease, medicine.medical_specialty, Lipoproteins, Brief Communication, peripheral artery disease, Pathophysiology, Peripheral Arterial Disease, 03 medical and health sciences, Internal medicine, Mendelian randomization, Humans, Genetic Predisposition to Disease, In patient, Aged, 030304 developmental biology, Glycated Hemoglobin, business.industry, Mendelian Randomization Analysis, Atherosclerosis, Cerebrovascular Disorders, Blood pressure, High Blood Pressure, business, Aortic Aneurysm, Abdominal, Genome-Wide Association Study

Abstract

Background Atherosclerosis in >1 vascular bed (ie, polyvascular disease), often a feature of peripheral artery disease (PAD), is associated with high morbidity and mortality. We sought to identify risk factors for polyvascular involvement in patients with PAD. Methods and Results We performed 2‐sample Mendelian randomization using an inverse‐variance‐weighted approach, to assess 60 exposures including size and lipid content of atherogenic lipoproteins, blood pressure, glycated hemoglobin, and smoking as causal mediators for polyvascular disease in patients with PAD. Genetic instruments for these exposures were obtained from prior genome‐wide association studies. Patients with PAD were from the Mayo Vascular Disease Biorepository, and polyvascular disease (ie, concomitant coronary heart disease, cerebrovascular disease, and/or abdominal aortic aneurysm) was ascertained by validated phenotyping algorithms. Of 3279 patients with PAD, 61% had polyvascular disease. Genetically predicted levels of the lipid content and/or particle measures of very small and small size very low‐density lipoprotein, intermediate‐density lipoprotein, and large low‐density lipoprotein were associated with polyvascular disease: odds ratios (OR) of 1.80 (95% CI, 1.23–2.61), 1.70 (95% CI, 1.17–2.61), and 1.40 (95% CI, 1.09–1.80) per 1 SD increase in genetically determined levels, respectively. Both genetically predicted diastolic and systolic blood pressure were associated with polyvascular disease; OR per 10 mm Hg genetic increase in diastolic and systolic blood pressure were 1.66 (95% CI, 1.19–2.33) and 1.31 (95% CI, 1.07–1.60), respectively. Conclusions Lifetime exposure to increased lipid content and levels of very small and small very low‐density lipoprotein, intermediate‐density lipoprotein, and large low‐density lipoprotein particles as well as elevated blood pressure are associated with polyvascular involvement in patients with PAD. Reduction in levels of such exposures may limit progression of atherosclerosis in patients with PAD.

Published

2020

17. Polygenic Risk Scores for Diverse Ancestries: Making Genomic Medicine Equitable

Author

Iftikhar J, Kullo and Ozan, Dikilitas

Subjects

Multifactorial Inheritance, Asian People, Risk Factors, Humans, Medicine, Coronary Artery Disease, Genomics, Article, Genome-Wide Association Study

Abstract

BACKGROUND: Genome-wide polygenic scores (GPS) integrate information from many common DNA variants into a single number. Because rates of coronary artery disease (CAD) are substantially higher among South Asians, a GPS to identify high-risk individuals may be particularly useful in this population. OBJECTIVES: We used summary statistics from a prior genome-wide association study to derive a new GPS(CAD) for South Asians. METHODS: We validated this GPS(CAD) in 7,244 South Asian UK Biobank participants and tested it in 491 individuals from a case-control study in Bangladesh. Next, we built a static ancestry and GPS(CAD) reference distribution using whole genome sequencing from 1,522 Indian individuals, and tested a framework for projecting individuals onto this static ancestry and GPS(CAD) reference distribution using 1,800 CAD cases and 1,163 controls newly recruited in India. RESULTS: The GPS(CAD), containing 6,630,150 common DNA variants, had odds ratio per standard deviation (OR/SD) of 1.58 in South Asian UK Biobank participants and 1.60 in the Bangladeshi study (p < 0.001 for each). We next projected individuals of the Indian case-control study onto static reference distributions, observing an OR/SD of 1.66 (p < 0.001). Compared to the middle quintile, risk for CAD was most pronounced for those in the top 5% of the GPS(CAD) distribution - ORs of 4.16, 2.46, and 3.22 in the South Asian UK Biobank, Bangladeshi, and Indian studies, respectively (p < 0.05 for each). CONCLUSIONS: We developed and tested a new GPS(CAD) using three distinct South Asian studies, and provide a generalizable framework for ancestry-specific GPS assessment.

Published

2020

18. Predictive Utility of Polygenic Risk Scores for Coronary Heart Disease in Three Major Racial and Ethnic Groups

Author

Patrick M. A. Sleiman, Matthew L. Kosel, Ozan Dikilitas, Joshua A. Denny, Christopher G. Chute, Alex Fedotov, Ming Ta Michael Lee, Robb Rowley, Wei-Qi Wei, Amy C. Sturm, Teri A. Manolio, Marc S. Williams, Yanfei Zhang, Gail P. Jarvik, Robert J. Carroll, C. Michael Stein, Iftikhar J. Kullo, Jennifer A. Pacheco, Daniel J. Schaid, QiPing Feng, Hakon Hakonarson, and Georgia L. Wiesner

Subjects

0301 basic medicine, Male, Multifactorial Inheritance, Ethnic group, Coronary Disease, 030204 cardiovascular system & hematology, White People, Article, Coronary artery disease, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Genetics, Odds Ratio, Medicine, Humans, Genetic Predisposition to Disease, Genetics (clinical), business.industry, Hazard ratio, Mean age, Odds ratio, Hispanic or Latino, Middle Aged, medicine.disease, Coronary heart disease, Black or African American, 030104 developmental biology, Cohort, Polygenic risk score, Female, business, Demography

Abstract

Because polygenic risk scores (PRSs) for coronary heart disease (CHD) are derived from mainly European ancestry (EA) cohorts, their validity in African ancestry (AA) and Hispanic ethnicity (HE) individuals is unclear. We investigated associations of “restricted” and genome-wide PRSs with CHD in three major racial and ethnic groups in the U.S. The eMERGE cohort (mean age 48 ± 14 years, 58% female) included 45,645 EA, 7,597 AA, and 2,493 HE individuals. We assessed two restricted PRSs (PRS(Tikkanen) and PRS(Tada); 28 and 50 variants, respectively) and two genome-wide PRSs (PRS(metaGRS) and PRS(LDPred); 1.7 M and 6.6 M variants, respectively) derived from EA cohorts. Over a median follow-up of 11.1 years, 2,652 incident CHD events occurred. Hazard and odds ratios for the association of PRSs with CHD were similar in EA and HE cohorts but lower in AA cohorts. Genome-wide PRSs were more strongly associated with CHD than restricted PRSs were. PRS(metaGRS), the best performing PRS, was associated with CHD in all three cohorts; hazard ratios (95% CI) per 1 SD increase were 1.53 (1.46–1.60), 1.53 (1.23–1.90), and 1.27 (1.13–1.43) for incident CHD in EA, HE, and AA individuals, respectively. The hazard ratios were comparable in the EA and HE cohorts (p(interaction) = 0.77) but were significantly attenuated in AA individuals (p(interaction)= 2.9 × 10(−3)). These results highlight the potential clinical utility of PRSs for CHD as well as the need to assemble diverse cohorts to generate ancestry- and ethnicity PRSs.

Published

2019

19. Minority-centric meta-analyses of blood lipid levels identify novel loci in the Population Architecture using Genomics and Epidemiology (PAGE) study

Author

Martha L. Daviglus, Daniel J. Schaid, Jeffrey Haessler, Adolfo Correa, Iona Cheng, Austin T. Hilliard, Yingchang Lu, Ozan Dikilitas, Gail P. Jarvik, Stephanie A. Bien, Lynne R. Wilkens, Yao Hu, Patrick M. A. Sleiman, Ulrike Peters, Laura J. Rasmussen-Torvik, Frank D. Mentch, Christopher J. O'Donnell, Lauren E. Petty, Kari E. North, Mariaelisa Graff, Christopher A. Haiman, Loic Le Marchand, Marie Verbanck, Peter W.F. Wilson, Steven Buyske, Ruth J. F. Loos, QiPing Feng, VA Million Veteran Program, Tara C. Matise, Charles Kooperberg, Ron Do, Kelly Cho, Scott M. Damrauer, Iftikhar J. Kullo, Christopher S. Carlson, Jennifer E. Below, Berta Almoguera, Philip S. Tsao, Themistocles L. Assimes, Lisa W. Martin, Wei-Qi Wei, Yuk-Lam Ho, Eric B. Larson, Ran Tao, Lucia A. Hindorff, Katherine K. Nishimura, José Luis Ambite, Matthew L. Kosel, Kyong-Mi Chang, Derek Klarin, Daniel O. Stram, Laura M. Raffield, Niha Zubair, and Heather M. Highland

Subjects

Male, Multifactorial Inheritance, Cancer Research, Population genetics, Genome-wide association study, QH426-470, Biochemistry, Geographical Locations, Mathematical and Statistical Techniques, 0302 clinical medicine, Databases, Genetic, Genotype, Ethnicities, Hispanic People, Minority Groups, Genetics (clinical), 0303 health sciences, education.field_of_study, Statistics, Genomics, Metaanalysis, Lipids, Europe, Phenotype, Meta-analysis, Physical Sciences, Female, Research Article, Population, Biology, Research and Analysis Methods, Polymorphism, Single Nucleotide, 03 medical and health sciences, Genome-Wide Association Studies, Genetics, Humans, Statistical Methods, Trait Locus Analysis, education, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Genetic association, Evolutionary Biology, Population Biology, Racial Groups, Biology and Life Sciences, Computational Biology, Human Genetics, Genome Analysis, United States, Genetic architecture, Genetic Loci, Evolutionary biology, People and Places, Population Groupings, Metagenomics, Mathematics, Population Genetics, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Lipid levels are important markers for the development of cardio-metabolic diseases. Although hundreds of associated loci have been identified through genetic association studies, the contribution of genetic factors to variation in lipids is not fully understood, particularly in U.S. minority groups. We performed genome-wide association analyses for four lipid traits in over 45,000 ancestrally diverse participants from the Population Architecture using Genomics and Epidemiology (PAGE) Study, followed by a meta-analysis with several European ancestry studies. We identified nine novel lipid loci, five of which showed evidence of replication in independent studies. Furthermore, we discovered one novel gene in a PrediXcan analysis, minority-specific independent signals at eight previously reported loci, and potential functional variants at two known loci through fine-mapping. Systematic examination of known lipid loci revealed smaller effect estimates in African American and Hispanic ancestry populations than those in Europeans, and better performance of polygenic risk scores based on minority-specific effect estimates. Our findings provide new insight into the genetic architecture of lipid traits and highlight the importance of conducting genetic studies in diverse populations in the era of precision medicine., Author summary Blood lipid levels are closely linked to cardio-metabolic diseases, and genetic factors play an important role in their metabolism and regulation. Although over 400 loci have been identified through genetic association studies, the genetic architecture of lipid levels is not fully characterized. The lack of representation of diverse populations in previous studies resulted in a large gap in understanding the genetic background of lipid traits between European and minority populations, including African Americans, Hispanics, Hawaiians, and Native Americans. In our current analyses which included ancestrally diverse populations, we identified nine novel loci, one novel gene, and minority-specific independent signals at eight known loci, and pinpointed potential functional variants at two known loci. We further observed smaller effect sizes of reported lipids-associated loci in African Americans and Hispanics than those in Europeans, and better performance of polygenic risk scores using minority-specific instead of European-derived effect sizes when estimating genetic predisposition in minority populations. Our findings showed the benefits of including multi-ethnic studies in identification and refinement of lipids-associated loci, which will help to reduce the existing disparities and to pave the road to precision medicine.

Published

2020

20. Making work visible for electronic phenotype implementation: Lessons learned from the eMERGE network

Author

Yuan Luo, David Carrell, Joshua C. Denny, Vivian S. Gainer, Ozan Dikilitas, Todd Lingren, Theresa L. Walunas, George Hripcsak, Robert J. Caroll, Luke V. Rasmussen, Casey N. Ta, Barbara Benoit, Shawn N. Murphy, Jennifer A. Pacheco, Ning Shang, Cong Liu, Chunhua Weng, Hakon Hakonarson, Ken Wiley, Frank D. Mentch, Iftikhar J. Kullo, and Wei-Qi Wei

Subjects

Vocabulary, Process (engineering), Computer science, media_common.quotation_subject, Health Informatics, Machine learning, computer.software_genre, Article, law.invention, Personalization, 03 medical and health sciences, Software portability, 0302 clinical medicine, law, Electronic Health Records, Humans, 030212 general & internal medicine, Retrospective Studies, 030304 developmental biology, media_common, 0303 health sciences, Flowchart, business.industry, Medical record, Genomics, Computer Science Applications, Phenotype, Observational study, Metric (unit), Artificial intelligence, business, computer, Algorithms, Medical Informatics

Abstract

Background Implementation of phenotype algorithms requires phenotype engineers to interpret human-readable algorithms and translate the description (text and flowcharts) into computable phenotypes – a process that can be labor intensive and error prone. To address the critical need for reducing the implementation efforts, it is important to develop portable algorithms. Methods We conducted a retrospective analysis of phenotype algorithms developed in the Electronic Medical Records and Genomics (eMERGE) network and identified common customization tasks required for implementation. A novel scoring system was developed to quantify portability from three aspects: Knowledge conversion, clause Interpretation, and Programming (KIP). Tasks were grouped into twenty representative categories. Experienced phenotype engineers were asked to estimate the average time spent on each category and evaluate time saving enabled by a common data model (CDM), specifically the Observational Medical Outcomes Partnership (OMOP) model, for each category. Results A total of 485 distinct clauses (phenotype criteria) were identified from 55 phenotype algorithms, corresponding to 1153 customization tasks. In addition to 25 non-phenotype-specific tasks, 46 tasks are related to interpretation, 613 tasks are related to knowledge conversion, and 469 tasks are related to programming. A score between 0 and 2 (0 for easy, 1 for moderate, and 2 for difficult portability) is assigned for each aspect, yielding a total KIP score range of 0 to 6. The average clause-wise KIP score to reflect portability is 1.37 ± 1.38. Specifically, the average knowledge (K) score is 0.64 ± 0.66, interpretation (I) score is 0.33 ± 0.55, and programming (P) score is 0.40 ± 0.64. 5% of the categories can be completed within one hour (median). 70% of the categories take from days to months to complete. The OMOP model can assist with vocabulary mapping tasks. Conclusion This study presents firsthand knowledge of the substantial implementation efforts in phenotyping and introduces a novel metric (KIP) to measure portability of phenotype algorithms for quantifying such efforts across the eMERGE Network. Phenotype developers are encouraged to analyze and optimize the portability in regards to knowledge, interpretation and programming. CDMs can be used to improve the portability for some ‘knowledge-oriented’ tasks.

Published

2019

21. Facilitating phenotype transfer using a common data model

Author

Joshua C. Denny, Ozan Dikilitas, Todd Lingren, Kayla Marie Howell, George Hripcsak, Shawn N. Murphy, Ken Wiley, Peggy L. Peissig, Robert J. Carroll, Jennifer A. Pacheco, Cong Liu, David Carrell, Karthik Natarajan, Frank D. Mentch, Vivian S. Gainer, Jeffrey G. Klann, Ning Shang, Iftikhar J. Kullo, Barbara Benoit, Wei-Qi Wei, Luke V. Rasmussen, and Chunhua Weng

Subjects

Databases, Factual, Computer science, Process (engineering), Human error, Health Informatics, Article, 03 medical and health sciences, 0302 clinical medicine, Outcome Assessment, Health Care, Electronic Health Records, Humans, 030212 general & internal medicine, Pseudocode, Implementation, Bespoke, 030304 developmental biology, 0303 health sciences, Data Collection, Biobank, Data science, United States, Computer Science Applications, National Human Genome Research Institute (U.S.), Observational Studies as Topic, Phenotype, Diabetes Mellitus, Type 2, Data model, Attention Deficit Disorder with Hyperactivity, Research Design, Informatics, Medical Informatics, Software

Abstract

Background Implementing clinical phenotypes across a network is labor intensive and potentially error prone. Use of a common data model may facilitate the process. Methods Electronic Medical Records and Genomics (eMERGE) sites implemented the Observational Health Data Sciences and Informatics (OHDSI) Observational Medical Outcomes Partnership (OMOP) Common Data Model across their electronic health record (EHR)-linked DNA biobanks. Two previously implemented eMERGE phenotypes were converted to OMOP and implemented across the network. Results It was feasible to implement the common data model across sites, with laboratory data producing the greatest challenge due to local encoding. Sites were then able to execute the OMOP phenotype in less than one day, as opposed to weeks of effort to manually implement an eMERGE phenotype in their bespoke research EHR databases. Of the sites that could compare the current OMOP phenotype implementation with the original eMERGE phenotype implementation, specific agreement ranged from 100% to 43%, with disagreements due to the original phenotype, the OMOP phenotype, changes in data, and issues in the databases. Using the OMOP query as a standard comparison revealed differences in the original implementations despite starting from the same definitions, code lists, flowcharts, and pseudocode. Conclusion Using a common data model can dramatically speed phenotype implementation at the cost of having to populate that data model, though this will produce a net benefit as the number of phenotype implementations increases. Inconsistencies among the implementations of the original queries point to a potential benefit of using a common data model so that actual phenotype code and logic can be shared, mitigating human error in reinterpretation of a narrative phenotype definition.

Published

2019