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1. Association of PHACTR1 with Coronary Artery Calcium Differs by Sex and Cigarette Smoking.

Author

Voorhies, Kirsten, Young, Kendra, Hsu, Fang-Chi, Palmer, Nicholette, McDonald, Merry-Lynn, Lee, Sanghun, Hahn, Georg, Hecker, Julian, Prokopenko, Dmitry, Wu, Ann, Regan, Elizabeth, DeMeo, Dawn, Kinney, Greg, Crapo, James, Cho, Michael, Silverman, Edwin, Lange, Christoph, Budoff, Matthew, Hokanson, John, and Lutz, Sharon

Subjects
CDKN2B-AS1, PHACTR1, coronary artery calcium
Abstract

Background: Coronary artery calcium (CAC) is a marker of subclinical atherosclerosis and is a complex heritable trait with both genetic and environmental risk factors, including sex and smoking. Methods: We performed genome-wide association (GWA) analyses for CAC among all participants and stratified by sex in the COPDGene study (n = 6144 participants of European ancestry and n = 2589 participants of African ancestry) with replication in the Diabetes Heart Study (DHS). We adjusted for age, sex, current smoking status, BMI, diabetes, self-reported high blood pressure, self-reported high cholesterol, and genetic ancestry (as summarized by principal components computed within each racial group). For the significant signals from the GWA analyses, we examined the single nucleotide polymorphism (SNP) by sex interactions, stratified by smoking status (current vs. former), and tested for a SNP by smoking status interaction on CAC. Results: We identified genome-wide significant associations for CAC in the chromosome 9p21 region [CDKN2B-AS1] among all COPDGene participants (p = 7.1 × 10-14) and among males (p = 1.0 × 10-9), but the signal was not genome-wide significant among females (p = 6.4 × 10-6). For the sex stratified GWA analyses among females, the chromosome 6p24 region [PHACTR1] had a genome-wide significant association (p = 4.4 × 10-8) with CAC, but this signal was not genome-wide significant among all COPDGene participants (p = 1.7 × 10-7) or males (p = 0.03). There was a significant interaction for the SNP rs9349379 in PHACTR1 with sex (p = 0.02), but the interaction was not significant for the SNP rs10757272 in CDKN2B-AS1 with sex (p = 0.21). In addition, PHACTR1 had a stronger association with CAC among current smokers (p = 6.2 × 10-7) than former smokers (p = 7.5 × 10-3) and the SNP by smoking status interaction was marginally significant (p = 0.03). CDKN2B-AS1 had a strong association with CAC among both former (p = 7.7 × 10-8) and current smokers (p = 1.7 × 10-7) and the SNP by smoking status interaction was not significant (p = 0.40). Conclusions: Among current and former smokers of European ancestry in the COPDGene study, we identified a genome-wide significant association in the chromosome 6p24 region [PHACTR1] with CAC among females, but not among males. This region had a significant SNP by sex and SNP by smoking interaction on CAC.

Published
2024

7. Genome-wide association study in minority children with asthma implicates DNAH5 in bronchodilator responsiveness

Author

Joo, Jaehyun, Mak, Angel CY, Xiao, Shujie, Sleiman, Patrick M, Hu, Donglei, Huntsman, Scott, Eng, Celeste, Kan, Mengyuan, Diwakar, Avantika R, Lasky-Su, Jessica A, Weiss, Scott T, Sordillo, Joanne E, Wu, Ann C, Cloutier, Michelle, Canino, Glorisa, Forno, Erick, Celedón, Juan C, Seibold, Max A, Hakonarson, Hakon, Williams, L Keoki, Burchard, Esteban G, and Himes, Blanca E

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Epidemiology, Health Sciences, Pharmacology and Pharmaceutical Sciences, Minority Health, Health Disparities, Precision Medicine, Pediatric, Prevention, Asthma, Human Genome, Lung, Clinical Research, Biotechnology, 2.1 Biological and endogenous factors, Respiratory, Good Health and Well Being, Axonemal Dyneins, Bronchodilator Agents, Child, Ethnicity, Genome-Wide Association Study, Hispanic or Latino, Humans, Mexican Americans, Minority Groups, Polymorphism, Single Nucleotide
Abstract

Variability in response to short-acting β2-agonists (e.g., albuterol) among patients with asthma from diverse racial/ethnic groups may contribute to asthma disparities. We sought to identify genetic variants associated with bronchodilator response (BDR) to identify potential mechanisms of drug response and risk factors for worse asthma outcomes. Genome-wide association studies of bronchodilator response (BDR) were performed using TOPMed Whole Genome Sequencing data of the Asthma Translational Genomic Collaboration (ATGC), which corresponded to 1136 Puerto Rican, 656 Mexican and 4337 African American patients with asthma. With the population-specific GWAS results, a trans-ethnic meta-analysis was performed to identify BDR-associated variants shared across the three populations. Replication analysis was carried out in three pediatric asthma cohorts, including CAMP (Childhood Asthma Management Program; n = 560), GACRS (Genetics of Asthma in Costa Rica Study; n = 967) and HPR (Hartford-Puerto Rico; n = 417). A genome-wide significant locus (rs35661809; P = 3.61 × 10-8) in LINC02220, a non-coding RNA gene, was identified in Puerto Ricans. While this region was devoid of protein-coding genes, capture Hi-C data showed a distal interaction with the promoter of the DNAH5 gene in lung tissue. In replication analysis, the GACRS cohort yielded a nominal association (1-tailed P

Published
2022

10. Polygenic risk scores identify heterogeneity in asthma and chronic obstructive pulmonary disease

Author

Moll, Matthew, Sordillo, Joanne E., Ghosh, Auyon J., Hayden, Lystra P., McDermott, Gregory, McGeachie, Michael J., Dahlin, Amber, Tiwari, Anshul, Manmadkar, Monica G., Abston, Eric D., Pavuluri, Chandan, Saferali, Aabida, Begum, Sofina, Ziniti, John P., Gulsvik, Amund, Bakke, Per S., Aschard, Hugues, Iribarren, Carlos, Hersh, Craig P., Sparks, Jeffrey A., Hobbs, Brian D., Lasky-Su, Jessica A., Silverman, Edwin K., Weiss, Scott T., Wu, Ann Chen, and Cho, Michael H.

Published
2023
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12. Expression of SMARCD1 interacts with age in association with asthma control on inhaled corticosteroid therapy

Author

McGeachie, Michael J, Sordillo, Joanne E, Dahlin, Amber, Wang, Alberta L, Lutz, Sharon M, Tantisira, Kelan G, Panganiban, Ronald, Lu, Quan, Sajuthi, Satria, Urbanek, Cydney, Kelly, Rachel, Saef, Benjamin, Eng, Celeste, Oh, Sam S, Kho, Alvin T, Croteau-Chonka, Damien C, Weiss, Scott T, Raby, Benjamin A, Mak, Angel CY, Rodriguez-Santana, Jose R, Burchard, Esteban G, Seibold, Max A, and Wu, Ann Chen

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Asthma, Biotechnology, Genetics, Clinical Research, Human Genome, Lung, Aetiology, 2.1 Biological and endogenous factors, Respiratory, Administration, Inhalation, Adolescent, Adrenal Cortex Hormones, Adult, Age Factors, Child, Chromosomal Proteins, Non-Histone, Cohort Studies, Female, Gene Expression, Hispanic or Latino, Humans, Male, Middle Aged, Treatment Outcome, Young Adult, Cardiorespiratory Medicine and Haematology, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundGlobal gene expression levels are known to be highly dependent upon gross demographic features including age, yet identification of age-related genomic indicators has yet to be comprehensively undertaken in a disease and treatment-specific context.MethodsWe used gene expression data from CD4+ lymphocytes in the Asthma BioRepository for Integrative Genomic Exploration (Asthma BRIDGE), an open-access collection of subjects participating in genetic studies of asthma with available gene expression data. Replication population participants were Puerto Rico islanders recruited as part of the ongoing Genes environments & Admixture in Latino Americans (GALA II), who provided nasal brushings for transcript sequencing. The main outcome measure was chronic asthma control as derived by questionnaires. Genomic associations were performed using regression of chronic asthma control score on gene expression with age in years as a covariate, including a multiplicative interaction term for gene expression times age.ResultsThe SMARCD1 gene (SWI/SNF-related matrix-associated actin-dependent regulator of chromatin subfamily D member 1) interacted with age to influence chronic asthma control on inhaled corticosteroids, with a doubling of expression leading to an increase of 1.3 units of chronic asthma control per year (95% CI [0.86, 1.74], p = 6 × 10- 9), suggesting worsening asthma control with increasing age. This result replicated in GALA II (p = 3.8 × 10- 8). Cellular assays confirmed the role of SMARCD1 in glucocorticoid response in airway epithelial cells.ConclusionFocusing on age-dependent factors may help identify novel indicators of asthma medication response. Age appears to modulate the effect of SMARCD1 on asthma control with inhaled corticosteroids.

Published
2020

13. Lung Function in African American Children with Asthma Is Associated with Novel Regulatory Variants of the KIT Ligand KITLG/SCF and Gene-By-Air-Pollution Interaction

Author

Mak, Angel CY, Sajuthi, Satria, Joo, Jaehyun, Xiao, Shujie, Sleiman, Patrick M, White, Marquitta J, Lee, Eunice Y, Saef, Benjamin, Hu, Donglei, Gui, Hongsheng, Keys, Kevin L, Lurmann, Fred, Jain, Deepti, Abecasis, Gonçalo, Kang, Hyun Min, Nickerson, Deborah A, Germer, Soren, Zody, Michael C, Winterkorn, Lara, Reeves, Catherine, Huntsman, Scott, Eng, Celeste, Salazar, Sandra, Oh, Sam S, Gilliland, Frank D, Chen, Zhanghua, Kumar, Rajesh, Martínez, Fernando D, Wu, Ann Chen, Ziv, Elad, Hakonarson, Hakon, Himes, Blanca E, Williams, L Keoki, Seibold, Max A, and Burchard, Esteban G

Subjects
Biological Sciences, Genetics, Biotechnology, Asthma, Precision Medicine, Lung, Pediatric, Human Genome, 2.1 Biological and endogenous factors, Respiratory, Good Health and Well Being, Adolescent, Black or African American, Air Pollution, Child, Chromosomes, Human, Pair 12, Female, Forced Expiratory Volume, Gene-Environment Interaction, Humans, Linkage Disequilibrium, Male, Nasal Mucosa, Polymorphism, Single Nucleotide, Quantitative Trait Loci, Stem Cell Factor, Young Adult, GWAS, African American, FEV(1)gene-by-environment interaction, GxE, air pollution, KITLG, SCF, FEV1 gene-by-environment interaction, Developmental Biology, Biochemistry and cell biology
Abstract

Baseline lung function, quantified as forced expiratory volume in the first second of exhalation (FEV1), is a standard diagnostic criterion used by clinicians to identify and classify lung diseases. Using whole-genome sequencing data from the National Heart, Lung, and Blood Institute Trans-Omics for Precision Medicine project, we identified a novel genetic association with FEV1 on chromosome 12 in 867 African American children with asthma (P = 1.26 × 10-8, β = 0.302). Conditional analysis within 1 Mb of the tag signal (rs73429450) yielded one major and two other weaker independent signals within this peak. We explored statistical and functional evidence for all variants in linkage disequilibrium with the three independent signals and yielded nine variants as the most likely candidates responsible for the association with FEV1 Hi-C data and expression QTL analysis demonstrated that these variants physically interacted with KITLG (KIT ligand, also known as SCF), and their minor alleles were associated with increased expression of the KITLG gene in nasal epithelial cells. Gene-by-air-pollution interaction analysis found that the candidate variant rs58475486 interacted with past-year ambient sulfur dioxide exposure (P = 0.003, β = 0.32). This study identified a novel protective genetic association with FEV1, possibly mediated through KITLG, in African American children with asthma. This is the first study that has identified a genetic association between lung function and KITLG, which has established a role in orchestrating allergic inflammation in asthma.

Published
2020

18. Metabolomic profiling reveals extensive adrenal suppression due to inhaled corticosteroid therapy in asthma

Author

Kachroo, Priyadarshini, Stewart, Isobel D., Kelly, Rachel S., Stav, Meryl, Mendez, Kevin, Dahlin, Amber, Soeteman, Djøra I., Chu, Su H., Huang, Mengna, Cote, Margaret, Knihtilä, Hanna M., Lee-Sarwar, Kathleen, McGeachie, Michael, Wang, Alberta, Wu, Ann Chen, Virkud, Yamini, Zhang, Pei, Wareham, Nicholas J., Karlson, Elizabeth W., Wheelock, Craig E., Clish, Clary, Weiss, Scott T., Langenberg, Claudia, and Lasky-Su, Jessica A.

Published
2022
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19. Genetic Associations and Architecture of Asthma-COPD Overlap

Author

John, Catherine, Guyatt, Anna L., Shrine, Nick, Packer, Richard, Olafsdottir, Thorunn A., Liu, Jiangyuan, Hayden, Lystra P., Chu, Su H., Koskela, Jukka T., Luan, Jian’an, Li, Xingnan, Terzikhan, Natalie, Xu, Hanfei, Bartz, Traci M., Petersen, Hans, Leng, Shuguang, Belinsky, Steven A., Cepelis, Aivaras, Hernández Cordero, Ana I., Obeidat, Ma’en, Thorleifsson, Gudmar, Meyers, Deborah A., Bleecker, Eugene R., Sakoda, Lori C., Iribarren, Carlos, Tesfaigzi, Yohannes, Gharib, Sina A., Dupuis, Josée, Brusselle, Guy, Lahousse, Lies, Ortega, Victor E., Jonsdottir, Ingileif, Sin, Don D., Bossé, Yohan, van den Berge, Maarten, Nickle, David, Quint, Jennifer K., Sayers, Ian, Hall, Ian P., Langenberg, Claudia, Ripatti, Samuli, Laitinen, Tarja, Wu, Ann C., Lasky-Su, Jessica, Bakke, Per, Gulsvik, Amund, Hersh, Craig P., Hayward, Caroline, Langhammer, Arnulf, Brumpton, Ben, Stefansson, Kari, Cho, Michael H., Wain, Louise V., and Tobin, Martin D.

Published
2022
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20. Effect of High-Deductible Health Plans and Preventive Drug Lists on Asthma Attacks, Medicine Use, and Out-of-Pocket Costs – The AFFORD Study

Author

Galbraith, Alison, primary, Sinaiko, Anna, additional, Gilkey, Melissa, additional, Ross-Degnan, Dennis, additional, Zhang, Fang, additional, LeCates, Robert, additional, Faugno, Elena, additional, Chen Wu, Ann, additional, Cripps, Lauren, additional, Eftekhari, Sanaz, additional, Mendez, Kenneth, additional, and Wharam, Frank, additional

Published
2023
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21. Whole-Genome Sequencing of Pharmacogenetic Drug Response in Racially Diverse Children with Asthma

Author

Mak, Angel CY, White, Marquitta J, Eckalbar, Walter L, Szpiech, Zachary A, Oh, Sam S, Pino-Yanes, Maria, Hu, Donglei, Goddard, Pagé, Huntsman, Scott, Galanter, Joshua, Wu, Ann Chen, Himes, Blanca E, Germer, Soren, Vogel, Julia M, Bunting, Karen L, Eng, Celeste, Salazar, Sandra, Keys, Kevin L, Liberto, Jennifer, Nuckton, Thomas J, Nguyen, Thomas A, Torgerson, Dara G, Kwok, Pui-Yan, Levin, Albert M, Celedón, Juan C, Forno, Erick, Hakonarson, Hakon, Sleiman, Patrick M, Dahlin, Amber, Tantisira, Kelan G, Weiss, Scott T, Serebrisky, Denise, Brigino-Buenaventura, Emerita, Farber, Harold J, Meade, Kelley, Lenoir, Michael A, Avila, Pedro C, Sen, Saunak, Thyne, Shannon M, Rodriguez-Cintron, William, Winkler, Cheryl A, Moreno-Estrada, Andrés, Sandoval, Karla, Rodriguez-Santana, Jose R, Kumar, Rajesh, Williams, L Keoki, Ahituv, Nadav, Ziv, Elad, Seibold, Max A, Darnell, Robert B, Zaitlen, Noah, Hernandez, Ryan D, and Burchard, Esteban G

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Health Disparities, Precision Medicine, Lung, Genetics, Asthma, Human Genome, Pediatric, Minority Health, Biotechnology, 2.1 Biological and endogenous factors, Respiratory, Good Health and Well Being, Adolescent, Black or African American, Albuterol, Bronchodilator Agents, Child, Female, Genome-Wide Association Study, Hispanic or Latino, Humans, Male, Mexican Americans, Pharmacogenomic Variants, Polymorphism, Single Nucleotide, Race Factors, United States, albuterol, asthma, minority, NFKB1, Latinos, NHLBI Trans-Omics for Precision Medicine (TOPMed) Consortium, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleAlbuterol, a bronchodilator medication, is the first-line therapy for asthma worldwide. There are significant racial/ethnic differences in albuterol drug response.ObjectivesTo identify genetic variants important for bronchodilator drug response (BDR) in racially diverse children.MethodsWe performed the first whole-genome sequencing pharmacogenetics study from 1,441 children with asthma from the tails of the BDR distribution to identify genetic association with BDR.Measurements and main resultsWe identified population-specific and shared genetic variants associated with BDR, including genome-wide significant (P

Published
2018

23. Examining the Effect of Genes on Depression as Mediated by Smoking and Modified by Sex

Author

Voorhies, Kirsten, primary, Hecker, Julian, additional, Lee, Sanghun, additional, Hahn, Georg, additional, Prokopenko, Dmitry, additional, McDonald, Merry-Lynn, additional, Wu, Alexander C., additional, Wu, Ann, additional, Hokanson, John E., additional, Cho, Michael H., additional, Lange, Christoph, additional, Hoth, Karin F., additional, and Lutz, Sharon M., additional

Published
2024
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24. GSDMB/ORMDL3 Rare/Common Variants Are Associated with Inhaled Corticosteroid Response among Children with Asthma

Author

Voorhies, Kirsten, primary, Mohammed, Akram, additional, Chinthala, Lokesh, additional, Kong, Sek Won, additional, Lee, In-Hee, additional, Kho, Alvin T., additional, McGeachie, Michael, additional, Mandl, Kenneth D., additional, Raby, Benjamin, additional, Hayes, Melanie, additional, Davis, Robert L., additional, Wu, Ann Chen, additional, and Lutz, Sharon M., additional

Published
2024
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28. Machine Learning Prediction of Treatment Response to Inhaled Corticosteroids in Asthma

Author

Ong, Mei-Sing, Sordillo, Joanne E., Dahlin, Amber, McGeachie, Michael, Tantisira, Kelan, Wang, Alberta L., Lasky-Su, Jessica, Brilliant, Murray, Kitchner, Terrie, Roden, Dan M., Weiss, Scott T., Wu, Ann Chen, Ong, Mei-Sing, Sordillo, Joanne E., Dahlin, Amber, McGeachie, Michael, Tantisira, Kelan, Wang, Alberta L., Lasky-Su, Jessica, Brilliant, Murray, Kitchner, Terrie, Roden, Dan M., Weiss, Scott T., and Wu, Ann Chen

Abstract

Background: Although inhaled corticosteroids (ICS) are the first-line therapy for patients with persistent asthma, many patients continue to have exacerbations. We developed machine learning models to predict the ICS response in patients with asthma. Methods: The subjects included asthma patients of European ancestry (n = 1371; 448 children; 916 adults). A genome-wide association study was performed to identify the SNPs associated with ICS response. Using the SNPs identified, two machine learning models were developed to predict ICS response: (1) least absolute shrinkage and selection operator (LASSO) regression and (2) random forest. Results: The LASSO regression model achieved an AUC of 0.71 (95% CI 0.67–0.76; sensitivity: 0.57; specificity: 0.75) in an independent test cohort, and the random forest model achieved an AUC of 0.74 (95% CI 0.70–0.78; sensitivity: 0.70; specificity: 0.68). The genes contributing to the prediction of ICS response included those associated with ICS responses in asthma (TPSAB1, FBXL16), asthma symptoms and severity (ABCA7, CNN2, PTRN3, and BSG/CD147), airway remodeling (ELANE, FSTL3), mucin production (GAL3ST), leukotriene synthesis (GPX4), allergic asthma (ZFPM1, SBNO2), and others. Conclusions: An accurate risk prediction of ICS response can be obtained using machine learning methods, with the potential to inform personalized treatment decisions. Further studies are needed to examine if the integration of richer phenotype data could improve risk prediction.

Published
2024

29. Urine metabolomics signature reveals novel determinants of adrenal suppression in children taking inhaled corticosteroids to control asthma symptoms.

Author

Tran, Dung T., Chen, Yulu, Zheng, Yi, Hecker, Julian, Hawcutt, Daniel B., Pirmohamed, Munir, Lasky‐Su, Jessica, Wu, Ann C., Tantisira, Kelan G., McGeachie, Michael J., Weiss, Scott T., and Dahlin, Amber

Subjects
ASTHMATICS, FATTY acid oxidation, ASTHMA in children, METABOLOMICS, METABOLITES
Abstract

Background: Asthma is routinely treated with inhaled corticosteroids (ICS). Asthma patients on ICS are at increased risk of adrenal suppression, a potentially serious effect of long‐term glucocorticoid exposure; however, this relationship is poorly understood. Therefore, this study aims to identify metabolite biomarkers related to adrenal suppression in asthma patients taking ICS. Methods: A total of 571 urine metabolites from 200 children with asthma on ICS in the Pharmacogenetics of Adrenal Suppression with Inhaled Steroids (PASS) cohort were profiled. Samples were grouped by peak plasma cortisol measurement as adrenal sufficient (>350 nmol/L) or insufficient (≤350 nmol/L) (outcome). Regression and discriminant‐based statistical models combined with network analyses were utilized to assess relationships between metabolites and the outcome. Finally, prioritized metabolites were validated using data from an ancillary study of the Childhood Asthma Management (CAMP) cohort with similar characteristics to PASS. Results: Ninety metabolites were significantly associated with adrenal suppression, of which 57 also could discriminate adrenal status. While 26 metabolites (primarily steroids) were present at lower levels in the adrenal insufficient patients, 14 were significantly elevated in this group; the top metabolite, mannitol/sorbitol, was previously associated with asthma exacerbations. Network analyses identified unique clusters of metabolites related to steroids, fatty acid oxidation, and nucleoside metabolism, respectively. Four metabolites including urocanic acid, acetylcarnitine, uracil, and sorbitol were validated in CAMP cohort for adrenal suppression. Conclusions: Urinary metabolites differ among asthma patients on ICS, by adrenal status. While steroid metabolites were reduced in patients with poor adrenal function, our findings also implicate previously unreported metabolites involved in amino acid, lipid, and nucleoside metabolism. [ABSTRACT FROM AUTHOR]

Published
2024
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36. Author Correction: Metabolomic profiling reveals extensive adrenal suppression due to inhaled corticosteroid therapy in asthma

Author

Kachroo, Priyadarshini, Stewart, Isobel D., Kelly, Rachel S., Stav, Meryl, Mendez, Kevin, Dahlin, Amber, Soeteman, Djøra I., Chu, Su H., Huang, Mengna, Cote, Margaret, Knihtilä, Hanna M., Lee-Sarwar, Kathleen, McGeachie, Michael, Wang, Alberta, Wu, Ann Chen, Virkud, Yamini, Zhang, Pei, Wareham, Nicholas J., Karlson, Elizabeth W., Wheelock, Craig E., Clish, Clary, Weiss, Scott T., Langenberg, Claudia, and Lasky-Su, Jessica A.

Published
2022
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