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2. Genetic analyses of chr11p15.5 region identify MUC5AC-MUC5B associated with asthma-related phenotypes.

Author

Li, Xingnan, Li, Huashi, Christenson, Stephanie, Castro, Mario, Denlinger, Loren, Erzurum, Serpil, Fahy, John, Gaston, Benjamin, Israel, Elliot, Jarjour, Nizar, Levy, Bruce, Mauger, David, Moore, Wendy, Zein, Joe, Kaminski, Naftali, Wenzel, Sally, Woodruff, Prescott, Bleecker, Eugene, and Meyers, Deborah

Subjects
Asthma susceptibility, MUC5AC, MUC5B, asthma severity, eQTL, gene expression, genetic association, Humans, Asthma, Genome-Wide Association Study, Cross-Sectional Studies, Phenotype, RNA, Messenger, Mucin-5B, Mucin 5AC
Abstract

OBJECTIVE: Genome-wide association studies (GWASs) have identified single nucleotide polymorphisms (SNPs) in chr11p15.5 region associated with asthma and idiopathic interstitial pneumonias (IIPs). We sought to identify functional genes for asthma by combining SNPs and mRNA expression in bronchial epithelial cells (BEC) in the Severe Asthma Research Program (SARP). METHODS: Correlation analyses of mRNA expression of six candidate genes (AP2A2, MUC6, MUC2, MUC5AC, MUC5B, and TOLLIP) and asthma phenotypes were performed in the longitudinal cohort (n = 156) with RNAseq in BEC, and replicated in the cross-sectional cohort (n = 155). eQTL (n = 114) and genetic association analysis of asthma severity (426 severe vs. 531 non-severe asthma) were performed, and compared with previously published GWASs of IIPs and asthma. RESULTS: Higher expression of AP2A2 and MUC5AC and lower expression of MUC5B in BEC were correlated with asthma, asthma exacerbations, and T2 biomarkers (P  0.8). CONCLUSIONS: SNPs associated with asthma in chr11p15.5 region are not associated with asthma severity neither with IIPs. Higher expression of MUC5AC and lower expression of MUC5B are risk for asthma but protective for IIPs.

Published
2023

3. Investigations of a combination of atopic status and age of asthma onset identify asthma subphenotypes.

Author

Li, Huashi, Castro, Mario, Denlinger, Loren, Erzurum, Serpil, Fahy, John, Gaston, Benjamin, Israel, Elliot, Jarjour, Nizar, Levy, Bruce, Mauger, David, Moore, Wendy, Wenzel, Sally, Zein, Joe, Bleecker, Eugene, Meyers, Deborah, Chen, Yin, and Li, Xingnan

Subjects
Age of asthma onset, GSDMB, asthma subphenotypes, atopic asthma with fungal sensitization, non-atopic asthma, severe asthma, Child, Adult, Humans, Asthma, Hypersensitivity, Immediate, Longitudinal Studies, Biomarkers, Respiratory Function Tests
Abstract

OBJECTIVE: Subphenotypes of asthma may be determined by age onset and atopic status. We sought to characterize early or late onset atopic asthma with fungal or non-fungal sensitization (AAFS or AANFS) and non-atopic asthma (NAA) in children and adults in the Severe Asthma Research Program (SARP). SARP is an ongoing project involving well-phenotyped patients with mild to severe asthma. METHODS: Phenotypic comparisons were performed using Kruskal-Wallis or chi-square test. Genetic association analyses were performed using logistic or linear regression. RESULTS: Airway hyper-responsiveness, total serum IgE levels, and T2 biomarkers showed an increasing trend from NAA to AANFS and then to AAFS. Children and adults with early onset asthma had greater % of AAFS than adults with late onset asthma (46% and 40% vs. 32%; P

Published
2023

4. Impact of Bronchiectasis on COPD Severity and Alpha-1 Antitrypsin Deficiency as a Risk Factor in Individuals with a Heavy Smoking History.

Author

Izquierdo, Manuel, Marion, Chad, Genese, Frank, Newell, John, ONeal, Wanda, Li, Xingnan, Hawkins, Gregory, Barjaktarevic, Igor, Barr, R, Christenson, Stephanie, Cooper, Christopher, Couper, David, Curtis, Jeffrey, Han, Meilan, Hansel, Nadia, Kanner, Richard, Martinez, Fernando, Paine, Robert, Tejwani, Vickram, Woodruff, Prescott, Zein, Joe, Hoffman, Eric, Peters, Stephen, Meyers, Deborah, Bleecker, Eugene, and Ortega, Victor

Subjects
COPD, alpha-1 antitrypsin, bronchiectasis, lung function
Abstract

RATIONALE: Bronchiectasis is common among those with heavy smoking histories, but risk factors for bronchiectasis, including alpha-1 antitrypsin deficiency, and its implications for COPD severity are uncharacterized in such individuals. OBJECTIVES: To characterize the impact of bronchiectasis on COPD and explore alpha-1antitrypsin as a risk factor for bronchiectasis. METHODS: SubPopulations and InteRmediate Outcome Measures In COPD Study (SPIROMICS) participants (N=914; ages 40-80 years; ≥20-pack-year smoking) had high-resolution computed tomography (CT) scans interpreted visually for bronchiectasis, based on airway dilation without fibrosis or cicatrization. We performed regression-based models of bronchiectasis with clinical outcomes and quantitative CT measures. We deeply sequenced the gene encoding -alpha-1 antitrypsin, SERPINA1, in 835 participants to test for rare variants, focusing on the PiZ genotype (Glu366Lys, rs28929474). MEASUREMENTS AND MAIN RESULTS: We identified bronchiectasis in 365 (40%) participants, more frequently in women (45% versus 36%, p=0.0045), older participants (mean age=66[standard deviation (SD)=8.3] versus 64[SD=9.1] years, p=0.0083), and those with lower lung function (forced expiratory volume in 1 second [FEV1 ] percentage predicted=66%[SD=27] versus 77%[SD=25], p

Published
2023

5. Development of an asthma health-care burden score as a measure of severity and predictor of remission in SARP III and U-BIOPRED: results from two major longitudinal asthma cohorts

Author

Zein, Joe G, Zounemat-Kerman, Nazanin, Adcock, Ian M, Hu, Bo, Attaway, Amy, Castro, Mario, Dahlén, Sven-Erik, Denlinger, Loren C, Erzurum, Serpil C, Fahy, John V, Gaston, Benjamin, Hastie, Annette T, Israel, Elliot, Jarjour, Nizar N, Levy, Bruce D, Mauger, David T, Moore, Wendy, Peters, Michael C, Sumino, Kaharu, Townsend, Elizabeth, Woodruff, Prescott, Ortega, Victor E, Wenzel, Sally E, Meyers, Deborah A, Chung, Kian Fan, and Bleecker, Eugene R

Published
2025
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6. Low CC16 mRNA Expression Levels in Bronchial Epithelial Cells Are Associated with Asthma Severity.

Author

Li, Xingnan, Guerra, Stefano, Ledford, Julie, Kraft, Monica, Li, Huashi, Hastie, Annette, Castro, Mario, Denlinger, Loren, Erzurum, Serpil, Fahy, John, Gaston, Benjamin, Israel, Elliot, Jarjour, Nizar, Levy, Bruce, Mauger, David, Moore, Wendy, Zein, Joe, Kaminski, Naftali, Wenzel, Sally, Woodruff, Prescott, Meyers, Deborah, and Bleecker, Eugene

Subjects
CC16, T2 inflammation, asthma exacerbations, asthma severity, bronchial epithelial cells, Humans, Asthma, Biomarkers, Epithelial Cells, Inflammation, Prospective Studies, Retrospective Studies, RNA, Messenger, Uteroglobin
Abstract

Rationale: CC16 is a protein mainly produced by nonciliated bronchial epithelial cells (BECs) that participates in host defense. Reduced CC16 protein concentrations in BAL and serum are associated with asthma susceptibility. Objectives: Few studies have investigated the relationship between CC16 and asthma progression, and none has focused on BECs. In this study, we sought to determine if CC16 mRNA expression levels in BECs are associated with asthma severity. Methods: Association analyses between CC16 mRNA expression levels in BECs (242 asthmatics and 69 control subjects) and asthma-related phenotypes in Severe Asthma Research Program were performed using a generalized linear model. Measurements and Main Results: Low CC16 mRNA expression levels in BECs were significantly associated with asthma susceptibility and asthma severity, high systemic corticosteroids use, high retrospective and prospective asthma exacerbations, and low pulmonary function. Low CC16 mRNA expression levels were significantly associated with high T2 inflammation biomarkers (fractional exhaled nitric oxide and sputum eosinophils). CC16 mRNA expression levels were negatively correlated with expression levels of Th2 genes (IL1RL1, POSTN, SERPINB2, CLCA1, NOS2, and MUC5AC) and positively correlated with expression levels of Th1 and inflammation genes (IL12A and MUC5B). A combination of two nontraditional T2 biomarkers (CC16 and IL-6) revealed four asthma endotypes with different characteristics of T2 inflammation, obesity, and asthma severity. Conclusions: Our findings indicate that low CC16 mRNA expression levels in BECs are associated with asthma susceptibility, severity, and exacerbations, partially through immunomodulation of T2 inflammation. CC16 is a potential nontraditional T2 biomarker for asthma development and progression.

Published
2023

7. The Impact of Insulin Resistance on Loss of Lung Function and Response to Treatment in Asthma.

Author

Peters, Michael C, Schiebler, Mark L, Cardet, Juan Carlos, Johansson, Mats W, Sorkness, Ronald, DeBoer, Mark D, Bleecker, Eugene R, Meyers, Deborah A, Castro, Mario, Sumino, Kaharu, Erzurum, Serpil C, Tattersall, Matthew C, Zein, Joe G, Hastie, Annette T, Moore, Wendy, Levy, Bruce D, Israel, Elliot, Duvall, Melody G, Phillips, Brenda R, Mauger, David T, Wenzel, Sally E, Fajt, Merritt L, Koliwad, Suneil K, Denlinger, Loren C, Woodruff, Prescott G, Jarjour, Nizar N, Fahy, John V, Schiebler, Mark, Carlos Cardet, Juan, and Duvall, Melody

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Trials and Supportive Activities, Clinical Research, Lung, Asthma, Obesity, Respiratory, Humans, Insulin Resistance, Cross-Sectional Studies, Bronchodilator Agents, Adrenal Cortex Hormones, Forced Expiratory Volume, asthma, obesity, insulin resistance, lung function, National Heart, Lung, and Blood Institute Severe Asthma Research Program-3, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

Rationale: The role of obesity-associated insulin resistance (IR) in airflow limitation in asthma is uncertain. Objectives: Using data in the Severe Asthma Research Program 3 (SARP-3), we evaluated relationships between homeostatic measure of IR (HOMA-IR), lung function (cross-sectional and longitudinal analyses), and treatment responses to bronchodilators and corticosteroids. Methods: HOMA-IR values were categorized as without (5.0). Lung function included FEV1 and FVC measured before and after treatment with inhaled albuterol and intramuscular triamcinolone acetonide and yearly for 5 years. Measurements and Main Results: Among 307 participants in SARP-3, 170 (55%) were obese and 140 (46%) had IR. Compared with patients without IR, those with IR had significantly lower values for FEV1 and FVC, and these lower values were not attributable to obesity effects. Compared with patients without IR, those with IR had lower FEV1 responses to β-adrenergic agonists and systemic corticosteroids. The annualized decline in FEV1 was significantly greater in patients with moderate IR (-41 ml/year) and severe IR (-32 ml/year,) than in patients without IR (-13 ml/year, P

Published
2022

8. DNA sequencing analysis of cystic fibrosis transmembrane conductance regulator gene identifies cystic fibrosis-associated variants in the Severe Asthma Research Program.

Author

Izquierdo, Manuel E, Marion, Chad R, Moore, Wendy C, Raraigh, Karen S, Taylor-Cousar, Jennifer L, Cutting, Gary R, Ampleford, E, Hawkins, Gregory A, Zein, Joe, Castro, M, Denlinger, Loren C, Erzurum, Serpil C, Fahy, John V, Israel, Elliot, Jarjour, Nizar N, Mauger, David, Levy, Bruce D, Wenzel, Sally E, Woodruff, Prescott, Bleecker, Eugene R, Meyers, Deborah A, and Ortega, Victor E

Subjects
Paediatrics, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Asthma, Lung, Rare Diseases, Cystic Fibrosis, Genetics, Aetiology, 2.1 Biological and endogenous factors, Congenital, Good Health and Well Being, Cystic Fibrosis Transmembrane Conductance Regulator, Humans, Mutation, Sequence Analysis, DNA, CF-Asthma Overlap, CFTR, cystic fibrosis, heterozygote carriers, Paediatrics and Reproductive Medicine, Respiratory System, Cardiovascular medicine and haematology
Abstract

BackgroundHeterozygote carriers of potentially pathogenic variants in the cystic fibrosis transmembrane conductance regulator (CFTR) gene have increased asthma risk. However, the frequency and impact of CFTR variation among individuals with asthma is unknown.ObjectiveTo determine whether potentially pathogenic CFTR variants associate with disease severity and whether individuals with two potentially pathogenic variants exist in a severe asthma-enriched cohort.MethodsWe analyzed sequencing data spanning a 190.5Kb region of CFTR in participants from the Severe Asthma Research Program (SARP1-3). Potentially pathogenic, rare CFTR variants (frequency  G] and one Arg1070Trp) and a homozygote for the VVCC, 5 T; TG12.ConclusionsWe found potentially pathogenic CFTR variants within a severe asthma-enriched cohort, including three compound heterozygote genotypes variably associated with CF in NHW individuals. These findings provide the rationale for CFTR sequencing and phenotyping of CF-related traits in individuals with severe asthma.

Published
2022

9. The Precision Interventions for Severe and/or Exacerbation-Prone (PrecISE) Asthma Network: An overview of Network organization, procedures, and interventions

Author

Georas, Steve N, Wright, Rosalind J, Ivanova, Anastasia, Israel, Elliot, LaVange, Lisa M, Akuthota, Praveen, Carr, Tara F, Denlinger, Loren C, Fajt, Merritt L, Kumar, Rajesh, O’Neal, Wanda K, Phipatanakul, Wanda, Szefler, Stanley J, Aronica, Mark A, Bacharier, Leonard B, Burbank, Allison J, Castro, Mario, Alexander, Laura Crotty, Bamdad, Julie, Cardet, Juan Carlos, Comhair, Suzy AA, Covar, Ronina A, DiMango, Emily A, Erwin, Kim, Erzurum, Serpil C, Fahy, John V, Gaffin, Jonathan M, Gaston, Benjamin, Gerald, Lynn B, Hoffman, Eric A, Holguin, Fernando, Jackson, Daniel J, James, John, Jarjour, Nizar N, Kenyon, Nicholas J, Khatri, Sumita, Kirwan, John P, Kraft, Monica, Krishnan, Jerry A, Liu, Andrew H, Liu, Mark C, Marquis, M Alison, Martinez, Fernando, Mey, Jacob, Moore, Wendy C, Moy, James N, Ortega, Victor E, Peden, David B, Pennington, Emily, Peters, Michael C, Ross, Kristie, Sanchez, Maria, Smith, Lewis J, Sorkness, Ronald L, Wechsler, Michael E, Wenzel, Sally E, White, Steven R, Zein, Joe, Zeki, Amir A, Noel, Patricia, Billheimer, Dean, Bleecker, Eugene R, Branch, Emily, Conway, Michelle, Daines, Cori, Deaton, Isaac, Evans, Alexandria, Field, Paige, Francisco, Dave, Hastie, Annette T, Hmieleski, Bob, Krings, Jeffrey O, Liu, Yanqin, Merchen, Janell L, Meyers, Deborah A, Narendran, Nirushan, Peters, Stephen P, Pippins, Anna, Rank, Matthew A, Schunk, Ronald, Skeps, Raymond, Wright, Benjamin, Banzon, Tina M, Bartnikas, Lisa M, Baxi, Sachin N, Betapudi, Vishwanath, Brick, Isabelle, Brockway, Conor, Casale, Thomas B, Castillo-Ruano, Kathleen, Cinelli, Maria Angeles, Crestani, Elena, Cunningham, Amparito, Day-Lewis, Megan, Diaz-Cabrera, Natalie, DiMango, Angela, Esty, Brittany, Fandozzi, Eva, Fernandez, Jesse, and Fitzpatrick, Elizabeth

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, Asthma, Precision Medicine, Clinical Trials and Supportive Activities, Clinical Research, Respiratory, Good Health and Well Being, Advisory Committees, Biomarkers, Clinical Protocols, Clinical Trials, Phase II as Topic, Humans, Research Design, Severity of Illness Index, Tomography, X-Ray Computed, Severe asthma, precision medicine, adaptive clinical trial design, asthma exacerbation, type 2 asthma, non-type 2 asthma, patient advisory committee, biomarker, PrecISE Study Team, non–type 2 asthma, Immunology, Allergy
Abstract

Asthma is a heterogeneous disease, with multiple underlying inflammatory pathways and structural airway abnormalities that impact disease persistence and severity. Recent progress has been made in developing targeted asthma therapeutics, especially for subjects with eosinophilic asthma. However, there is an unmet need for new approaches to treat patients with severe and exacerbation-prone asthma, who contribute disproportionately to disease burden. Extensive deep phenotyping has revealed the heterogeneous nature of severe asthma and identified distinct disease subtypes. A current challenge in the field is to translate new and emerging knowledge about different pathobiologic mechanisms in asthma into patient-specific therapies, with the ultimate goal of modifying the natural history of disease. Here, we describe the Precision Interventions for Severe and/or Exacerbation-Prone Asthma (PrecISE) Network, a groundbreaking collaborative effort of asthma researchers and biostatisticians from around the United States. The PrecISE Network was designed to conduct phase II/proof-of-concept clinical trials of precision interventions in the population with severe asthma, and is supported by the National Heart, Lung, and Blood Institute of the National Institutes of Health. Using an innovative adaptive platform trial design, the PrecISE Network will evaluate up to 6 interventions simultaneously in biomarker-defined subgroups of subjects. We review the development and organizational structure of the PrecISE Network, and choice of interventions being studied. We hope that the PrecISE Network will enhance our understanding of asthma subtypes and accelerate the development of therapeutics for severe asthma.

Published
2022

10. Genetic and non-genetic factors affecting the expression of COVID-19-relevant genes in the large airway epithelium

Author

Kasela, Silva, Ortega, Victor E, Martorella, Molly, Garudadri, Suresh, Nguyen, Jenna, Ampleford, Elizabeth, Pasanen, Anu, Nerella, Srilaxmi, Buschur, Kristina L, Barjaktarevic, Igor Z, Barr, R Graham, Bleecker, Eugene R, Bowler, Russell P, Comellas, Alejandro P, Cooper, Christopher B, Couper, David J, Criner, Gerard J, Curtis, Jeffrey L, Han, MeiLan K, Hansel, Nadia N, Hoffman, Eric A, Kaner, Robert J, Krishnan, Jerry A, Martinez, Fernando J, McDonald, Merry-Lynn N, Meyers, Deborah A, Paine, Robert, Peters, Stephen P, Castro, Mario, Denlinger, Loren C, Erzurum, Serpil C, Fahy, John V, Israel, Elliot, Jarjour, Nizar N, Levy, Bruce D, Li, Xingnan, Moore, Wendy C, Wenzel, Sally E, Zein, Joe, Langelier, Charles, Woodruff, Prescott G, Lappalainen, Tuuli, and Christenson, Stephanie A

Subjects
Biological Sciences, Genetics, Clinical Research, Emerging Infectious Diseases, Biotechnology, Human Genome, Coronaviruses, Infectious Diseases, Lung, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Respiratory, Infection, Good Health and Well Being, Adult, Aged, Aged, 80 and over, Angiotensin-Converting Enzyme 2, Asthma, Bronchi, COVID-19, Cardiovascular Diseases, Gene Expression, Genetic Variation, Humans, Middle Aged, Obesity, Pulmonary Disease, Chronic Obstructive, Quantitative Trait Loci, Respiratory Mucosa, Risk Factors, SARS-CoV-2, Smoking, ACE2, eQTL, Bronchial epithelium, NHLBI SubPopulations and InteRmediate Outcome Measures In COPD Study, NHLBI Trans-Omics for Precision Medicine (TOPMed) Consortium, Clinical Sciences
Abstract

BackgroundThe large airway epithelial barrier provides one of the first lines of defense against respiratory viruses, including SARS-CoV-2 that causes COVID-19. Substantial inter-individual variability in individual disease courses is hypothesized to be partially mediated by the differential regulation of the genes that interact with the SARS-CoV-2 virus or are involved in the subsequent host response. Here, we comprehensively investigated non-genetic and genetic factors influencing COVID-19-relevant bronchial epithelial gene expression.MethodsWe analyzed RNA-sequencing data from bronchial epithelial brushings obtained from uninfected individuals. We related ACE2 gene expression to host and environmental factors in the SPIROMICS cohort of smokers with and without chronic obstructive pulmonary disease (COPD) and replicated these associations in two asthma cohorts, SARP and MAST. To identify airway biology beyond ACE2 binding that may contribute to increased susceptibility, we used gene set enrichment analyses to determine if gene expression changes indicative of a suppressed airway immune response observed early in SARS-CoV-2 infection are also observed in association with host factors. To identify host genetic variants affecting COVID-19 susceptibility in SPIROMICS, we performed expression quantitative trait (eQTL) mapping and investigated the phenotypic associations of the eQTL variants.ResultsWe found that ACE2 expression was higher in relation to active smoking, obesity, and hypertension that are known risk factors of COVID-19 severity, while an association with interferon-related inflammation was driven by the truncated, non-binding ACE2 isoform. We discovered that expression patterns of a suppressed airway immune response to early SARS-CoV-2 infection, compared to other viruses, are similar to patterns associated with obesity, hypertension, and cardiovascular disease, which may thus contribute to a COVID-19-susceptible airway environment. eQTL mapping identified regulatory variants for genes implicated in COVID-19, some of which had pheWAS evidence for their potential role in respiratory infections.ConclusionsThese data provide evidence that clinically relevant variation in the expression of COVID-19-related genes is associated with host factors, environmental exposures, and likely host genetic variation.

Published
2021

11. Whole-genome sequencing in diverse subjects identifies genetic correlates of leukocyte traits: The NHLBI TOPMed program

Author

Mikhaylova, Anna V, McHugh, Caitlin P, Polfus, Linda M, Raffield, Laura M, Boorgula, Meher Preethi, Blackwell, Thomas W, Brody, Jennifer A, Broome, Jai, Chami, Nathalie, Chen, Ming-Huei, Conomos, Matthew P, Cox, Corey, Curran, Joanne E, Daya, Michelle, Ekunwe, Lynette, Glahn, David C, Heard-Costa, Nancy, Highland, Heather M, Hobbs, Brian D, Ilboudo, Yann, Jain, Deepti, Lange, Leslie A, Miller-Fleming, Tyne W, Min, Nancy, Moon, Jee-Young, Preuss, Michael H, Rosen, Jonathon, Ryan, Kathleen, Smith, Albert V, Sun, Quan, Surendran, Praveen, de Vries, Paul S, Walter, Klaudia, Wang, Zhe, Wheeler, Marsha, Yanek, Lisa R, Zhong, Xue, Abecasis, Goncalo R, Almasy, Laura, Barnes, Kathleen C, Beaty, Terri H, Becker, Lewis C, Blangero, John, Boerwinkle, Eric, Butterworth, Adam S, Chavan, Sameer, Cho, Michael H, Choquet, Hélène, Correa, Adolfo, Cox, Nancy, DeMeo, Dawn L, Faraday, Nauder, Fornage, Myriam, Gerszten, Robert E, Hou, Lifang, Johnson, Andrew D, Jorgenson, Eric, Kaplan, Robert, Kooperberg, Charles, Kundu, Kousik, Laurie, Cecelia A, Lettre, Guillaume, Lewis, Joshua P, Li, Bingshan, Li, Yun, Lloyd-Jones, Donald M, Loos, Ruth JF, Manichaikul, Ani, Meyers, Deborah A, Mitchell, Braxton D, Morrison, Alanna C, Ngo, Debby, Nickerson, Deborah A, Nongmaithem, Suraj, North, Kari E, O’Connell, Jeffrey R, Ortega, Victor E, Pankratz, Nathan, Perry, James A, Psaty, Bruce M, Rich, Stephen S, Soranzo, Nicole, Rotter, Jerome I, Silverman, Edwin K, Smith, Nicholas L, Tang, Hua, Tracy, Russell P, Thornton, Timothy A, Vasan, Ramachandran S, Zein, Joe, Mathias, Rasika A, Consortium, NHLBI Trans-Omics for Precision Medicine, Reiner, Alexander P, and Auer, Paul L

Subjects
Human Genome, Genetics, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Good Health and Well Being, Asthma, Biomarkers, Dermatitis, Atopic, Genetic Predisposition to Disease, Genome, Human, Genome-Wide Association Study, Humans, Leukocytes, National Heart, Lung, and Blood Institute (U.S.), Phenotype, Polymorphism, Single Nucleotide, Prognosis, Proteome, Pulmonary Disease, Chronic Obstructive, Quantitative Trait Loci, United Kingdom, United States, Whole Genome Sequencing, NHLBI Trans-Omics for Precision Medicine (TOPMed) Consortium, blood-cell counts, whole-genome sequencing, Biological Sciences, Medical and Health Sciences, Genetics & Heredity
Abstract

Many common and rare variants associated with hematologic traits have been discovered through imputation on large-scale reference panels. However, the majority of genome-wide association studies (GWASs) have been conducted in Europeans, and determining causal variants has proved challenging. We performed a GWAS of total leukocyte, neutrophil, lymphocyte, monocyte, eosinophil, and basophil counts generated from 109,563,748 variants in the autosomes and the X chromosome in the Trans-Omics for Precision Medicine (TOPMed) program, which included data from 61,802 individuals of diverse ancestry. We discovered and replicated 7 leukocyte trait associations, including (1) the association between a chromosome X, pseudo-autosomal region (PAR), noncoding variant located between cytokine receptor genes (CSF2RA and CLRF2) and lower eosinophil count; and (2) associations between single variants found predominantly among African Americans at the S1PR3 (9q22.1) and HBB (11p15.4) loci and monocyte and lymphocyte counts, respectively. We further provide evidence indicating that the newly discovered eosinophil-lowering chromosome X PAR variant might be associated with reduced susceptibility to common allergic diseases such as atopic dermatitis and asthma. Additionally, we found a burden of very rare FLT3 (13q12.2) variants associated with monocyte counts. Together, these results emphasize the utility of whole-genome sequencing in diverse samples in identifying associations missed by European-ancestry-driven GWASs.

Published
2021

12. Epidemiology of Asthma: Prevalence and Burden of Disease

Author

Merhej, Tamara, Zein, Joe G., Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, Brasier, Allan R., editor, and Jarjour, Nizar N., editor

Published
2023
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14. Mitochondrial DNA copy number variation in asthma risk, severity, and exacerbations

Author

Xu, Weiling, Hong, Yun Soo, Hu, Bo, Comhair, Suzy A.A., Janocha, Allison J., Zein, Joe G., Chen, Ruoying, Meyers, Deborah A., Mauger, David T., Ortega, Victor E., Bleecker, Eugene R., Castro, Mario, Denlinger, Loren C., Fahy, John V., Israel, Elliot, Levy, Bruce D., Jarjour, Nizar N., Moore, Wendy C., Wenzel, Sally E., Gaston, Benjamin, Liu, Chunyu, Arking, Dan E., and Erzurum, Serpil C.

Published
2024
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15. Benefits of Airway Androgen Receptor Expression in Human Asthma.

Author

Zein, Joe G, McManus, Jeffrey M, Sharifi, Nima, Erzurum, Serpil C, Marozkina, Nadzeya, Lahm, Timothy, Giddings, Olivia, Davis, Michael D, DeBoer, Mark D, Comhair, Suzy A, Bazeley, Peter, Kim, Hyun Jo, Busse, William, Calhoun, William, Castro, Mario, Chung, Kian Fan, Fahy, John V, Israel, Elliot, Jarjour, Nizar N, Levy, Bruce D, Mauger, David T, Moore, Wendy C, Ortega, Victor E, Peters, Michael, Bleecker, Eugene R, Meyers, Deborah A, Zhao, Yi, Wenzel, Sally E, and Gaston, Benjamin

Subjects
Lung, Asthma, Respiratory, Good Health and Well Being, Adolescent, Adult, Aged, Aged, 80 and over, Breath Tests, Bronchoscopy, Dehydroepiandrosterone Sulfate, Female, Forced Expiratory Volume, Gene Expression, Humans, Male, Middle Aged, Nitric Oxide, Nitric Oxide Synthase Type II, Quality of Life, RNA, Messenger, Receptors, Androgen, Respiratory Mucosa, Sex Factors, Vital Capacity, Young Adult, asthma, androgens, airflow obstruction, airway inflammation, Medical and Health Sciences, Respiratory System
Abstract

Rationale: Androgens are potentially beneficial in asthma, but AR (androgen receptor) has not been studied in human airways.Objectives: To measure whether AR and its ligands are associated with human asthma outcomes.Methods: We compared the effects of AR expression on lung function, symptom scores, and fractional exhaled nitric oxide (FeNO) in adults enrolled in SARP (Severe Asthma Research Program). The impact of sex and of androgens on asthma outcomes was also evaluated in the SARP with validation studies in the Cleveland Clinic Health System and the NHANES (U.S. National Health and Nutrition Examination Survey).Measurements and Main Results: In SARP (n = 128), AR gene expression from bronchoscopic epithelial brushings was positively associated with both FEV1/FVC ratio (R2 = 0.135, P = 0.0002) and the total Asthma Quality of Life Questionnaire score (R2 = 0.056, P = 0.016) and was negatively associated with FeNO (R2 = 0.178, P = 9.8 × 10-6) and NOS2 (nitric oxide synthase gene) expression (R2 = 0.281, P = 1.2 × 10-10). In SARP (n = 1,659), the Cleveland Clinic Health System (n = 32,527), and the NHANES (n = 2,629), women had more asthma exacerbations and emergency department visits than men. The levels of the AR ligand precursor dehydroepiandrosterone sulfate correlated positively with the FEV1 in both women and men.Conclusions: Higher bronchial AR expression and higher androgen levels are associated with better lung function, fewer symptoms, and a lower FeNO in human asthma. The role of androgens should be considered in asthma management.

Published
2021

16. Responsiveness to Parenteral Corticosteroids and Lung Function Trajectory in Adults with Moderate-to-Severe Asthma.

Author

Denlinger, Loren C, Phillips, Brenda R, Sorkness, Ronald L, Bleecker, Eugene R, Castro, Mario, DeBoer, Mark D, Fitzpatrick, Anne M, Hastie, Annette T, Gaffin, Jonathan M, Moore, Wendy C, Peters, Michael C, Peters, Stephen P, Phipatanakul, Wanda, Cardet, Juan Carlos, Erzurum, Serpil C, Fahy, John V, Fajt, Merritt L, Gaston, Benjamin, Levy, Bruce D, Meyers, Deborah A, Ross, Kristie, Teague, W Gerald, Wenzel, Sally E, Woodruff, Prescott G, Zein, Joe, Jarjour, Nizar N, Mauger, David T, and Israel, Elliot

Subjects
Lung, Clinical Research, Asthma, Respiratory, Adrenal Cortex Hormones, Adult, Aged, Aged, 80 and over, Bronchodilator Agents, Cohort Studies, Female, Humans, Infusions, Parenteral, Longitudinal Studies, Male, Middle Aged, Respiratory Function Tests, Severity of Illness Index, Treatment Outcome, severe asthma, corticosteroid sensitivity, longitudinal, lung function, exacerbations, Medical and Health Sciences, Respiratory System
Abstract

Rationale: It is unclear why select patients with moderate-to-severe asthma continue to lose lung function despite therapy. We hypothesized that participants with the smallest responses to parenteral corticosteroids have the greatest risk of undergoing a severe decline in lung function.Objectives: To evaluate corticosteroid-response phenotypes as longitudinal predictors of lung decline.Methods: Adults within the NHLBI SARP III (Severe Asthma Research Program III) who had undergone a course of intramuscular triamcinolone at baseline and at ≥2 annual follow-up visits were evaluated. Longitudinal slopes were calculated for each participant's post-bronchodilator FEV1% predicted. Categories of participant FEV1 slope were defined: severe decline, >2% loss/yr; mild decline, >0.5-2.0% loss/yr; no change, 0.5% loss/yr to

Published
2021

19. HSD3B1 genotype identifies glucocorticoid responsiveness in severe asthma

Author

Zein, Joe, Gaston, Benjamin, Bazeley, Peter, DeBoer, Mark D, Igo, Robert P, Bleecker, Eugene R, Meyers, Deborah, Comhair, Suzy, Marozkina, Nadzeya V, Cotton, Calvin, Patel, Mona, Alyamani, Mohammad, Xu, Weiling, Busse, William W, Calhoun, William J, Ortega, Victor, Hawkins, Gregory A, Castro, Mario, Chung, Kian Fan, Fahy, John V, Fitzpatrick, Anne M, Israel, Elliot, Jarjour, Nizar N, Levy, Bruce, Mauger, David T, Moore, Wendy C, Noel, Patricia, Peters, Stephen P, Teague, W Gerald, Wenzel, Sally E, Erzurum, Serpil C, and Sharifi, Nima

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Clinical Sciences, Genetics, Lung, Asthma, Adult, Aged, Alleles, Androgens, Cohort Studies, Drug Resistance, Female, Genotype, Glucocorticoids, Humans, Male, Middle Aged, Multienzyme Complexes, Progesterone Reductase, Steroid Isomerases, Young Adult, steroids, glucocorticoids, inflammation, androgens, HSD3B1
Abstract

Asthma resistance to glucocorticoid treatment is a major health problem with unclear etiology. Glucocorticoids inhibit adrenal androgen production. However, androgens have potential benefits in asthma. HSD3B1 encodes for 3β-hydroxysteroid dehydrogenase-1 (3β-HSD1), which catalyzes peripheral conversion from adrenal dehydroepiandrosterone (DHEA) to potent androgens and has a germline missense-encoding polymorphism. The adrenal restrictive HSD3B1(1245A) allele limits conversion, whereas the adrenal permissive HSD3B1(1245C) allele increases DHEA metabolism to potent androgens. In the Severe Asthma Research Program (SARP) III cohort, we determined the association between DHEA-sulfate and percentage predicted forced expiratory volume in 1 s (FEV1PP). HSD3B1(1245) genotypes were assessed, and association between adrenal restrictive and adrenal permissive alleles and FEV1PP in patients with (GC) and without (noGC) daily oral glucocorticoid treatment was determined (n = 318). Validation was performed in a second cohort (SARP I&II; n = 184). DHEA-sulfate is associated with FEV1PP and is suppressed with GC treatment. GC patients homozygous for the adrenal restrictive genotype have lower FEV1PP compared with noGC patients (54.3% vs. 75.1%; P < 0.001). In patients with the homozygous adrenal permissive genotype, there was no FEV1PP difference in GC vs. noGC patients (73.4% vs. 78.9%; P = 0.39). Results were independently confirmed: FEV1PP for homozygous adrenal restrictive genotype in GC vs. noGC is 49.8 vs. 63.4 (P < 0.001), and for homozygous adrenal permissive genotype, it is 66.7 vs. 67.7 (P = 0.92). The adrenal restrictive HSD3B1(1245) genotype is associated with GC resistance. This effect appears to be driven by GC suppression of 3β-HSD1 substrate. Our results suggest opportunities for prediction of GC resistance and pharmacologic intervention.

Published
2020

20. Development and initial validation of the Asthma Severity Scoring System (ASSESS)

Author

Fitzpatrick, Anne M, Szefler, Stanley J, Mauger, David T, Phillips, Brenda R, Denlinger, Loren C, Moore, Wendy C, Sorkness, Ronald L, Wenzel, Sally E, Gergen, Peter J, Bleecker, Eugene R, Castro, Mario, Erzurum, Serpil C, Fahy, John V, Gaston, Benjamin M, Israel, Elliot, Levy, Bruce D, Meyers, Deborah A, Teague, W Gerald, Bacharier, Leonard B, Ly, Ngoc P, Phipatanakul, Wanda, Ross, Kristie R, Zein, Joe, and Jarjour, Nizar N

Subjects
Lung, Asthma, Clinical Research, Respiratory, Adolescent, Adult, Child, Female, Humans, Male, Severity of Illness Index, Triamcinolone, Asthma control, asthma severity classification, severe asthma, psychometric testing, tool development, Immunology, Allergy
Abstract

BackgroundTools for quantification of asthma severity are limited.ObjectiveWe sought to develop a continuous measure of asthma severity, the Asthma Severity Scoring System (ASSESS), for adolescents and adults, incorporating domains of asthma control, lung function, medications, and exacerbations.MethodsBaseline and 36-month longitudinal data from participants in phase 3 of the Severe Asthma Research Program (NCT01606826) were used. Scale properties, responsiveness, and a minimally important difference were determined. External replication was performed in participants enrolled in the Severe Asthma Research Program phase 1/2. The utility of ASSESS for detecting treatment response was explored in participants undergoing corticosteroid responsiveness testing with intramuscular triamcinolone and participants receiving biologics.ResultsASSESS scores ranged from 0 to 20 (8.78 ± 3.9; greater scores reflect worse severity) and differed among 5 phenotypic groups. Measurement properties were acceptable. ASSESS was responsive to changes in quality of life with a minimally important difference of 2, with good specificity for outcomes of asthma improvement and worsening but poor sensitivity. Replication analyses yielded similar results, with a 2-point decrease (improvement) associated with improvements in quality of life. Participants with a 2-point or greater decrease (improvement) in ASSESS scores also had greater improvement in lung function and asthma control after triamcinolone, but these differences were limited to phenotypic clusters 3, 4, and 5. Participants treated with biologics also had a 2-point or greater decrease (improvement) in ASSESS scores overall.ConclusionsThe ASSESS tool is an objective measure that might be useful in epidemiologic and clinical research studies for quantification of treatment response in individual patients and phenotypic groups. However, validation studies are warranted.

Published
2020

21. Asthma innovations from the second International Collaborative Asthma Network (ICAN) forum.

Author

Jarjour, Nizar N., Winders, Tonya, Hansen, Ann M., Akuthota, Praveen, Chung, Kian Fan, Durrington, Hannah, Fowler, Stephen J., Gaston, Benjamin, Mendonca, Eneida A., Siddiqui, Salman, Walker, Samantha, Zein, Joe, and Djukanovic, Ratko

Subjects
ASTHMATICS, CIRCADIAN rhythms, ASTHMA, MEETING planning, RESEARCH methodology
Abstract

Asthma continues to cause morbidity and mortality despite advances in treatment that include biologics targeting Type 2 inflammation. The International Collaborative Asthma Network (ICAN) forum was developed with the primary goal of promoting innovative, collaborative research that focuses on mechanisms and treatment for asthma that does not respond or that responds poorly to currently available treatments. The mission of ICAN is innovation, collaboration, translation, and increasing high quality research. At the second ICAN meeting, presenters covered a broad scope and depth of asthma-related topics in the categories of complex data, novel therapeutics and diagnostics, breath analysis and microbiome, disease mechanisms, systemic effects, and circadian rhythm. Key actionable needs and research topics were identified during the group discussions. The presentations and discussions that occurred at the second ICAN had an immediate impact on asthma research in the form of new collaborations and implementation of new research ideas and techniques. The forum also served to connect early-stage investigators with investigators who are well established, thereby fostering innovation, translation, and collaboration well into the future. A third ICAN meeting is planned for 2025 to further the innovations and collaborations that will translate into novel therapies and diagnostics to improve the lives of patients with asthma. [ABSTRACT FROM AUTHOR]

Published
2025
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23. Effects of endogenous sex hormones on lung function and symptom control in adolescents with asthma

Author

DeBoer, Mark D, Phillips, Brenda R, Mauger, David T, Zein, Joe, Erzurum, Serpil C, Fitzpatrick, Anne M, Gaston, Benjamin M, Myers, Ross, Ross, Kristie R, Chmiel, James, Lee, Min Jie, Fahy, John V, Peters, Michael, Ly, Ngoc P, Wenzel, Sally E, Fajt, Merritt L, Holguin, Fernando, Moore, Wendy C, Peters, Stephen P, Meyers, Deborah, Bleecker, Eugene R, Castro, Mario, Coverstone, Andrea M, Bacharier, Leonard B, Jarjour, Nizar N, Sorkness, Ronald L, Ramratnam, Sima, Irani, Anne-Marie, Israel, Elliot, Levy, Bruce, Phipatanakul, Wanda, Gaffin, Jonathan M, and Gerald Teague, W

Subjects
Paediatrics, Biomedical and Clinical Sciences, Clinical Research, Contraception/Reproduction, Lung, Asthma, Estrogen, Pediatric, Respiratory, Adolescent, Adrenal Cortex Hormones, Child, Cross-Sectional Studies, Female, Gonadal Steroid Hormones, Humans, Linear Models, Longitudinal Studies, Male, Multivariate Analysis, Puberty, Respiratory Function Tests, Severity of Illness Index, Sex Factors, United States, Sex hormones, Testosterone, Estradiol, Lung function, Cardiorespiratory Medicine and Haematology, Respiratory System, Cardiovascular medicine and haematology
Abstract

BackgroundAlthough pre-puberty asthma is more prevalent in males, after puberty through middle-age, asthma is more prevalent in females. The surge of sex hormones with puberty might explain this gender switch.MethodsTo examine the effects of sex hormones on lung function and symptoms with puberty, Tanner stage was assessed in 187 children 6-18 years of age (59% severe) enrolled in the NIH/NHLBI Severe Asthma Research Program (SARP). The effects of circulating sex hormones (n = 68; testosterone, dehydroepiandrosterone sulfate (DHEA-S), estrogen, and progesterone) on lung function and 4 week symptom control (ACQ6) in cross-section were tested by linear regression.ResultsFrom pre-/early to late puberty, lung function did not change significantly but ACQ6 scores improved in males with severe asthma. By contrast females had lower post-BD FEV1% and FVC% and worse ACQ6 scores with late puberty assessed by breast development. In males log DHEA-S levels, which increased by Tanner stage, associated positively with pre- and post-BD FEV1%, pre-BD FVC %, and negatively (improved) with ACQ6. Patients treated with high-dose inhaled corticosteroids had similar levels of circulating DHEA-S. In females, estradiol levels increased by Tanner stage, and associated negatively with pre-BD FEV1% and FVC %.ConclusionsThese results support beneficial effects of androgens on lung function and symptom control and weak deleterious effects of estradiol on lung function in children with asthma. Longitudinal data are necessary to confirm these cross-sectional findings and to further elucidate hormonal mechanisms informing sex differences in asthma features with puberty.Trial registrationClinicalTrials.gov registration number: NCT01748175 .

Published
2018

24. Baseline Features of the Severe Asthma Research Program (SARP III) Cohort: Differences with Age.

Author

Teague, W Gerald, Phillips, Brenda R, Fahy, John V, Wenzel, Sally E, Fitzpatrick, Anne M, Moore, Wendy C, Hastie, Annette T, Bleecker, Eugene R, Meyers, Deborah A, Peters, Stephen P, Castro, Mario, Coverstone, Andrea M, Bacharier, Leonard B, Ly, Ngoc P, Peters, Michael C, Denlinger, Loren C, Ramratnam, Sima, Sorkness, Ronald L, Gaston, Benjamin M, Erzurum, Serpil C, Comhair, Suzy AA, Myers, Ross E, Zein, Joe, DeBoer, Mark D, Irani, Anne-Marie, Israel, Elliot, Levy, Bruce, Cardet, Juan Carlos, Phipatanakul, Wanda, Gaffin, Jonathan M, Holguin, Fernando, Fajt, Merritt L, Aujla, Shean J, Mauger, David T, and Jarjour, Nizar N

Subjects
Humans, Asthma, Obesity, Immunoglobulin E, Bronchodilator Agents, Severity of Illness Index, Cohort Studies, Age Factors, Adolescent, Adult, Aged, Middle Aged, Child, Patient Acceptance of Health Care, Female, Male, Young Adult, Asthma phenotypes, Severe asthma, Clinical Research, Pediatric, Lung, Aetiology, 2.2 Factors relating to the physical environment, Respiratory, Good Health and Well Being
Abstract

BackgroundThe effect of age on asthma severity is poorly understood.ObjectivesThe objective of this study was to compare the baseline features of severe and nonsevere asthma in the Severe Asthma Research Program (SARP) III cohort, and examine in cross section the effects of age on those features.MethodsSARP III is a National Institutes of Health/National Heart Lung Blood Institute multisite 3-year cohort study conducted to investigate mechanisms of severe asthma. The sample included 188 children (111 severe, 77 nonsevere) and 526 adults (313 severe, 213 nonsevere) characterized for demographic features, symptoms, health care utilization, lung function, and inflammatory markers compared by age and severity.ResultsCompared with children with nonsevere asthma, children with severe asthma had more symptoms and more historical exacerbations, but no difference in body weight, post-bronchodilator lung function, or inflammatory markers. After childhood, and increasing with age, the cohort had a higher proportion of women, less allergen sensitization, and overall fewer blood eosinophils. Enrollment of participants with severe asthma was highest in middle-aged adults, who were older, more obese, with greater airflow limitation and higher blood eosinophils, but less allergen sensitization than adults with nonsevere asthma.ConclusionsThe phenotypic features of asthma differ by severity and with advancing age. With advancing age, patients with severe asthma are more obese, have greater airflow limitation, less allergen sensitization, and variable type 2 inflammation. Novel mechanisms besides type 2 inflammatory pathways may inform the severe asthma phenotype with advancing age.

Published
2018

25. The Precision Interventions for Severe and/or Exacerbation-Prone (PrecISE) Asthma Network: An overview of Network organization, procedures, and interventions

Author

Billheimer, Dean, Bleecker, Eugene R., Branch, Emily, Conway, Michelle, Daines, Cori, Deaton, Isaac, Evans, Alexandria, Field, Paige, Francisco, Dave, Hastie, Annette T., Hmieleski, Bob, Krings, Jeffrey O., Liu, Yanqin, Merchen, Janell L., Meyers, Deborah A., Narendran, Nirushan, Peters, Stephen P., Pippins, Anna, Rank, Matthew A., Schunk, Ronald, Skeps, Raymond, Wright, Benjamin, Banzon, Tina M., Bartnikas, Lisa M., Baxi, Sachin N., Betapudi, Vishwanath, Brick, Isabelle, Brockway, Conor, Casale, Thomas B., Castillo-Ruano, Kathleen, Cinelli, Maria Angeles, Crestani, Elena, Cunningham, Amparito, Day-Lewis, Megan, Diaz-Cabrera, Natalie, DiMango, Angela, Esty, Brittany, Fandozzi, Eva, Fernandez, Jesse, Fitzpatrick, Elizabeth, Forth, Victoria E., Gentile, Katarina, Gubernick, David, Gueye-Ndiaye, Seyni, Gunnlaagsson, Sigfus, Hauptmann, Marissa, Hudey, Stephanie N., Imanirad, Donya S., Kaage, Tiffani, Kolinsky, Nicholas, LaBere, Brenna, Lai, Peggy Sue, Le, Meghan, Ledford, Dennis K., Lockey, Richard, Louisias, Margee, Macginnitie, Andrew J., Maciag, Michelle C., O’Neill, Allison, Pepper, Amber N., Permaul, Perdita, Pugh, Mya, Queheillalt, Dianna, Saroya, Tarnjot, Sheehan, William, Smith, Catherine, Socolovsky, Carmela, Treffeisen, Else, Trippa, Lorenzo, Tulchinsky, Abigail, Yee, Christina, Carter, Tina, Fu, Jun, Garcia, Vanessa, Hixon, Jenny, Jackson, Carly, Ji, Yuan, Kalhan, Ravi, Kaur, Opinderjit, Li, Grace, Makhija, Melanie M., Maleckar, Spring, Naureckas, Edward T., Peters, Anju T., Press, Valerie, Qureshi, Mehreen, Reyfman, Paul A., Rosenberg, Sharon R., Ryba, Dominika, Sheng, Jianrong, Xu, Ben, Alam, Rafeul, Anderson, Darci, Belimezova, Sonya, Bitzan, Jennifer, Chupp, Geoffrey, Clark, Brian J., Cohn, Lauren, Cruse, Margaret Hope, Estrom, Jean, Freid, Leah, Villalobos, Jose Gomez, Grant, Nicole, Guntur, Vamsi P., Holm, Carole, Kolakowski, Christena, Manka, Laurie A., Miyazawa, Naomi, Pak, Juno, Pruitt, Diana M., Sharma, Sunita, Stevens, Allen D., Thomas, Kisori, Tippin, Brooke, Valente, Karissa, Wainscoat, Cynthia L., White, Michael P., Winnica, Daniel, Ye, Shuyu, Zeitlin, Pamela L., Bach, Julia, Brownell, Joshua, Castro, Lauren, DeLisa, Julie, Fain, Sean B., Fichtinger, Paul S., Floerke, Heather, Gern, James E., Goswamy, Vinay, Grogan, Jenelle, Hasse, Wendy, Kelley, Rick L., Klaus, Danika, LaBedz, Stephanie, Lowell, Paige, Maddox, Andrew, Mathur, Sameer K., McIntyre, Amanda, Norwick, Lourdes M., Nyenhuis, Sharmilee M., O’Brien, Matthew J., Palas, Tina, Pappalardo, Andrea A., Potter, Mark, Ramratnam, Sima K., Rosenberg, Daniel L., Schauberger, Eric M., Schiebler, Mark L., Schraml, Angela, Sorkness, Ronald L., Taki, Mohamed, Tattersall, Matthew C., Torres, Jissell, Wollet, Lori, Abi-Saleh, Simon, Bendy, Lisa, Borish, Larry, Chmiel, James F., Dix, Aska, France, Lisa, Gammell, Rebecca, Gluvna, Adam, Hirth, Brittany, Hu, Bo, Hyser, Elise, Kloepfer, Kirsten M., Koo, Michelle, Krupp, Nadia L., Labadia, Monica, Lawrence, Joy, Logan, Laurie, Marko, Angela, Matuska, Brittany, Murphy, Deborah, Owensby, Rachel, Roesch, Erica A., Sanders, Don B., Sharp, Jackie, Teague, W. Gerald, Veri, Laura, Shifflett, Kristin Wavell, Camiolo, Matt, Collins, Sarah, Demas, Jessa, Elvin, Courtney, Gauthier, Marc C., Ilnicki, Melissa, Ingram, Jenn, Lane, Lisa, Nouraie, Seyed Mehdi, Trudeau, John B., Zhang, Michael, Barry, Jeffrey, Brickner, Howard, Celso, Janelle, Cernelc-Kohan, Matejka, Diaz, Damaris, Du, Ashley, Jain, Sonia, Liu, Neiman, Nazir, Yusife, Ryu, Julie, Vijayanand, Pandurangan, Almario, Rogelio, Baum, Ariana, Brown, Kellen, Chan, Marilynn H., Gale, Barbara, Haczku, Angela, Harper, Richart W., Heromin, Raymond, Kivler, Celeste, Kuhn, Brooks T., Ly, Ngoc P., McCourt, Paula, Orain, Xavier, Plough, Audrey, Ramirez, Karla, Roberts, Ellese, Schivo, Michael, Singapuri, Amisha, Tham, Tina, Tompkins, Daniel, Twitmyer, Patricia Michelle, Vi, Jade, Atha, Jarron, Bedard, Jennifer, Boomer, Jonathan S., Chung, Andrew, Curtis, Vanessa, Hall, Chase S., Hart, Emily, Jackson, Fatima, Kemp, Pamela, Maxwell, Sharli, Messplay, Maggie, Ramirez, Crystal, Thompson, Brynne, Britt, Ashley, Bryan, Hope, Gotman, Nathan M., Jiang, Yue, Kosorok, Michael R., Mauger, David T., Meekins, Kelsey, Mollenhauer, Jeanette K., Moody, Sarah, Ritz, Cheyanne, Schwartz, Stefanie, Thomlinson, Chalmer, Wilson, Nicole, Georas, Steve N., Wright, Rosalind J., Ivanova, Anastasia, Israel, Elliot, LaVange, Lisa M., Akuthota, Praveen, Carr, Tara F., Denlinger, Loren C., Fajt, Merritt L., Kumar, Rajesh, O’Neal, Wanda K., Phipatanakul, Wanda, Szefler, Stanley J., Aronica, Mark A., Bacharier, Leonard B., Burbank, Allison J., Castro, Mario, Crotty Alexander, Laura, Bamdad, Julie, Cardet, Juan Carlos, Comhair, Suzy A.A., Covar, Ronina A., DiMango, Emily A., Erwin, Kim, Erzurum, Serpil C., Fahy, John V., Gaffin, Jonathan M., Gaston, Benjamin, Gerald, Lynn B., Hoffman, Eric A., Holguin, Fernando, Jackson, Daniel J., James, John, Jarjour, Nizar N., Kenyon, Nicholas J., Khatri, Sumita, Kirwan, John P., Kraft, Monica, Krishnan, Jerry A., Liu, Andrew H., Liu, Mark C., Marquis, M. Alison, Martinez, Fernando, Mey, Jacob, Moore, Wendy C., Moy, James N., Ortega, Victor E., Peden, David B., Pennington, Emily, Peters, Michael C., Ross, Kristie, Sanchez, Maria, Smith, Lewis J., Wechsler, Michael E., Wenzel, Sally E., White, Steven R., Zein, Joe, Zeki, Amir A., and Noel, Patricia

Published
2022
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29. The Long-Term Oxygen Treatment Trial for Chronic Obstructive Pulmonary Disease: Rationale, Design, and Lessons Learned

Author

Yusen, Roger D, Criner, Gerard J, Sternberg, Alice L, Au, David H, Fuhlbrigge, Anne L, Albert, Richard K, Casaburi, Richard, Stoller, James K, Harrington, Kathleen F, Cooper, J Allen D, Diaz, Philip, Gay, Steven, Kanner, Richard, MacIntyre, Neil, Martinez, Fernando J, Piantadosi, Steven, Sciurba, Frank, Shade, David, Stibolt, Thomas, Tonascia, James, Wise, Robert, Bailey, William C, Sampong, Ernestina, Sloan, Karin, Wagner, Ashley, Anderson, Susan, Moy, Marilyn, Okunbor, Osarenoma, Marlow, Scott, Meli, Yvonne, Rice, Richard, Aboussouan, Loutfi S, Castele, Robert, Parambil, Joseph, Khatri, Sumita, Pande, Aman, Zein, Joe, Olbrych, Thomas, Alkins, Stephan, Jocko, Christine, Rahaghi, Franck, Barton, Jean, Underwood, Jennifer, Make, Barry, Davies, John, Mularski, Richard, Naleway, Allison, Vertrees, Sarah, Porszasz, Janos, Walker, Peggy, Indelicato, Renee, Specht, Lennard, Ellstrom, Kathleen, Portillo, Jamie, Horak, David, Tiep, Brian, Barnett, Mary, Drake, Janice, Rittinger, Mahasti, Compton, Rachael, Miller, Scott, Panos, Ralph J, Lach, Laura A, Criner, Gerard, Grabianowski, Carla, Cordova, Francis, Desai, Parag, Krachman, Samuel, Mamary, James, Marchetti, Nathaniel, Satti, Aditi, Mumm, Eileen, Vega-Olivo, Michelle, Hua, Jenny, Tauch, Vanna, Criner, Lii-Yoong, Jacobs, Michael, Rising, Peter, Simonelli, Paul, Mitchell, Michele, Lammi, Matthew, Romaine, Connie, Lee, Howard, Ianacone, Mary, Scharf, Steven, Bell-Farrell, Wanda, Mador, M Jeffery, Rahman, Ayesha, Zaman, Mumtaz, Hill, Lisa, and Platt, Alec

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Clinical Trials and Supportive Activities, Prevention, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adult, Aged, Aged, 80 and over, Female, Geography, Humans, Long-Term Care, Male, Middle Aged, Multicenter Studies as Topic, Oxygen, Oxygen Inhalation Therapy, Patient Admission, Pulmonary Disease, Chronic Obstructive, Quality of Life, Randomized Controlled Trials as Topic, Time Factors, United States, chronic obstructive pulmonary disease, hypoxemia, oxygen, randomized controlled trial, survival, LOTT Research Group *, LOTT Research Group, Cardiovascular medicine and haematology, Clinical sciences
Abstract

The Long-Term Oxygen Treatment Trial demonstrated that long-term supplemental oxygen did not reduce time to hospital admission or death for patients who have stable chronic obstructive pulmonary disease and resting and/or exercise-induced moderate oxyhemoglobin desaturation, nor did it provide benefit for any other outcome measured in the trial. Nine months after initiation of patient screening, after randomization of 34 patients to treatment, a trial design amendment broadened the eligible population, expanded the primary outcome, and reduced the goal sample size. Within a few years, the protocol underwent minor modifications, and a second trial design amendment lowered the required sample size because of lower than expected treatment group crossover rates. After 5.5 years of recruitment, the trial met its amended sample size goal, and 1 year later, it achieved its follow-up goal. The process of publishing the trial results brought renewed scrutiny of the study design and the amendments. This article expands on the previously published design and methods information, provides the rationale for the amendments, and gives insight into the investigators' decisions about trial conduct. The story of the Long-Term Oxygen Treatment Trial may assist investigators in future trials, especially those that seek to assess the efficacy and safety of long-term oxygen therapy. Clinical trial registered with clinicaltrials.gov (NCT00692198).

Published
2018

33. Asthma Inception: Epidemiologic Risk Factors and Natural History Across the Life Course.

Author

Melén, Erik, Zar, Heather J., Siroux, Valerie, Shaw, Dominic, Saglani, Sejal, Koppelman, Gerard H., Hartert, Tina, Gern, James E., Gaston, Benjamin, Bush, Andrew, and Zein, Joe

Subjects
NATURAL history, DYSPNEA, ASTHMATICS, BACTERIAL diseases, GENETICS, COUGH
Abstract

Asthma is a descriptive label for an obstructive inflammatory disease in the lower airways manifesting with symptoms including breathlessness, cough, difficulty in breathing, and wheezing. From a clinician's point of view, asthma symptoms can commence at any age, although most patients with asthma—regardless of their age of onset—seem to have had some form of airway problems during childhood. Asthma inception and related pathophysiologic processes are therefore very likely to occur early in life, further evidenced by recent lung physiologic and mechanistic research. Herein, we present state-of-the-art updates on the role of genetics and epigenetics, early viral and bacterial infections, immune response, and pathophysiology, as well as lifestyle and environmental exposures, in asthma across the life course. We conclude that early environmental insults in genetically vulnerable individuals inducing abnormal, pre-asthmatic airway responses are key events in asthma inception, and we highlight disease heterogeneity across ages and the potential shortsightedness of treating all patients with asthma using the same treatments. Although there are no interventions that, at present, can modify long-term outcomes, a precision-medicine approach should be implemented to optimize treatment and tailor follow-up for all patients with asthma. [ABSTRACT FROM AUTHOR]

Published
2024
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34. Nocturnal Hypoxemia Is Associated with Sarcopenia in Patients with Chronic Obstructive Pulmonary Disease.

Author

Attaway, Amy H., Mehra, Reena, Zein, Joe G., Hatipoğlu, Umur, Grund, Megan, Orsini, Erica, Scheraga, Rachel G., Dasarathy, Srinivasan, and Olman, Mitchell A.

Subjects
SARCOPENIA, CHRONIC obstructive pulmonary disease, HYPOXEMIA, OXYGEN saturation, PECTORALIS muscle, SLEEP apnea syndromes
Abstract

Rationale: Chronic obstructive pulmonary disease (COPD) is the third leading cause of death worldwide. Our previous studies have identified that nocturnal hypoxemia causes skeletal muscle loss (i.e., sarcopenia) in in vitro models of COPD. Objectives: We aimed to extend our preclinical mechanistic findings by analyzing a large sleep registry to determine whether nocturnal hypoxemia is associated with sarcopenia in patients with COPD. Methods: Sleep studies from patients with COPD (n = 479) and control subjects without COPD (n = 275) were analyzed. Patients with obstructive sleep apnea, as defined by apnea–hypopnea index ⩾ 5, were excluded. Pectoralis muscle cross-sectional area (PMcsa) was quantified using computed tomography scans performed within 1 year of the sleep study. We defined sarcopenia as less than the lowest 20% residuals for PMcsa of control subjects, which was adjusted for age and body mass index (BMI) and stratified by sex. Youden's optimal cut-point criteria were used to predict sarcopenia based on mean oxygen saturation during sleep. Additional measures of nocturnal hypoxemia were analyzed. The pectoralis muscle index (PMI) was defined as PMcsa normalized to BMI. Results: On average, males with COPD had a 16.6% lower PMI than control males (1.41 ± 0.44 vs. 1.69 ± 0.56 cm2/BMI; P < 0.001), whereas females with COPD had a 9.4% lower PMI than control females (0.96 ± 0.27 vs. 1.06 ± 0.33 cm2/BMI; P < 0.001). Males with COPD with nocturnal hypoxemia had a 9.5% decrease in PMI versus COPD with normal O2 (1.33 ± 0.39 vs. 1.47 ± 0.46 cm2/BMI; P < 0.05) and a 23.6% decrease compared with control subjects (1.33 ± 0.39 vs. 1.74 ± 0.56 cm2/BMI; P < 0.001). Females with COPD with nocturnal hypoxemia had an 11.2% decrease versus COPD with normal O2 (0.87 ± 0.26 vs. 0.98 ± 0.28 cm2/BMI; P < 0.05) and a 17.9% decrease compared with control subjects (0.87 ± 0.26 vs. 1.06 ± 0.33 cm2/BMI; P < 0.001). These findings were largely replicated using multiple measures of nocturnal hypoxemia. Conclusions: We defined sarcopenia in the pectoralis muscle using residuals that take into account age, BMI, and sex. We found that patients with COPD have a lower PMI than patients without COPD and that nocturnal hypoxemia was associated with an additional decrease in the PMI of patients with COPD. Additional prospective analyses are needed to determine a protective threshold of oxygen saturation to prevent or reverse sarcopenia due to nocturnal hypoxemia in COPD. [ABSTRACT FROM AUTHOR]

Published
2024
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38. Severe asthma during childhood and adolescence: A longitudinal study

Author

Ross, Kristie R., Gupta, Ritika, DeBoer, Mark D., Zein, Joe, Phillips, Brenda R., Mauger, David T., Li, Chun, Myers, Ross E., Phipatanakul, Wanda, Fitzpatrick, Anne M., Ly, Ngoc P., Bacharier, Leonard B., Jackson, Daniel J., Celedón, Juan C., Larkin, Allyson, Israel, Elliot, Levy, Bruce, Fahy, John V., Castro, Mario, Bleecker, Eugene R., Meyers, Deborah, Moore, Wendy C., Wenzel, Sally E., Jarjour, Nizar N., Erzurum, Serpil C., Teague, W.Gerald, and Gaston, Benjamin

Published
2020
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42. The role of ACT score in mepolizumab discontinuation.

Author

Solanki, Neha, Beck, Brittany, Labadia, Monica, Smith, Kevin, Peterson, Laura, King, Stephanie, Micklewright, Sarah, Pennington, Emily, Farooq, Sobia, Zhang, Peng, Aronica, Mark, Zein, Joe, Khatri, Sumita, Comhair, Suzy, and Erzurum, Serpil

Subjects
DISEASE risk factors, ODDS ratio, ASTHMA, NITRIC oxide, EOSINOPHILS
Abstract

Mepolizumab is a therapy for severe asthma. We have little knowledge of the characteristics of people in the US that discontinue mepolizumab in clinical care. To investigate the real-world efficacy and time to clinical discontinuation of mepolizumab, we evaluated individuals with asthma started on mepolizumab at the Cleveland Clinic. We hypothesized that individuals that discontinue mepolizumab have more severe and uncontrolled asthma at baseline. Between 2016 and 2022, patients who started on mepolizumab consented to be assessed over 18 months. At baseline, a questionnaire including demographic and medical history was collected. Laboratory findings such as ACT score, FENO (Fractional Excretion of Nitric Oxide), and spirometry were recorded. At the conclusion of the observation period, the participants were divided into two categories: Group A and Group B. Group B [N = 28] discontinued mepolizumab (p < 0.05) at an average of 5.8 months (SD 4.2 months). Group A [N = 129] stayed on the therapy for at least 1 year. A participant with an ACT score less than 13 has an odds ratio of 6.64 (95% CI, 2.1 − 26.0) of discontinuing mepolizumab therapy. For a male, the odds of discontinuing mepolizumab therapy is 3.39 (95% CI, 1.1–11.2). In this real-world study, we find that high eosinophil count may not be adequate in screening which individuals will benefit from mepolizumab. Up to 17% of patients fail therapy within 6 months, with male sex and low ACT score increasing risk of mepolizumab discontinuation at Cleveland Clinic. [ABSTRACT FROM AUTHOR]

Published
2024
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43. The Role of ACT Score in Mepolizumab Discontinuation

Author

Solanki, Neha, primary, Beck, Brittany, additional, Labadia, Monica, additional, Smith, Kevin, additional, Peterson, Laura, additional, King, Stephanie, additional, Micklewright, Sarah, additional, Pennington, Emily, additional, Farooq, Sobia, additional, Zhang, Peng, additional, Aronica, Mark, additional, Zein, Joe, additional, Khatri, Sumita, additional, Comhair, Suzy, additional, and Erzurum, Serpil, additional

Published
2023
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47. The Role ACT Score in Mepolizumab Discontinuation

Author

Solanki, Neha, primary, Beck, Brittany, additional, Labadia, Monica, additional, Smith, Kevin, additional, Peterson, Laura, additional, King, Stephanie, additional, Micklewright, Sarah, additional, Pennington, Emily, additional, Farooq, Sobia, additional, Zhang, Peng, additional, Aronica, Mark, additional, Zein, Joe, additional, Khatri, Sumita, additional, Comhair, Suzy, additional, and Erzurum, Serpil, additional

Published
2023
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50. Asthma Innovations from the First International Collaborative Asthma Network (ICAN) Forum

Author

Gaston, Benjamin, primary, Gardner, Donna D., additional, Mahan, Kenzie, additional, Akuthota, Praveen, additional, Mendonca, Eneida A., additional, Durrington, Hannah, additional, Marozkina, Nadzeya, additional, Martinez-Nunez, Rocio T., additional, Newcomb, Dawn, additional, Ainsworth, Benjamin, additional, Owora, Arthur H., additional, Chung, Kian Fan, additional, Walker, Samantha, additional, Fowler, Stephen J., additional, Siddiqui, Salman, additional, Winders, Tonya, additional, Zein, Joe, additional, Jarjour, Nizar, additional, Huang, Yvonne J., additional, Cahill, Katherine N., additional, and Djukanovic, Ratko, additional

Published
2023
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