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1. Clinical and molecular analysis of longitudinal rhinitis phenotypes in an urban birth cohort

Author

Ramratnam, Sima K., Johnson, Molly, Visness, Cynthia M., Calatroni, Agustin, Altman, Mathew C., Janczyk, Tomasz, McCauley, Kathryn E., Schachtschneider, Claire, Fujimura, Kei E., Fadrosh, Douglas W., Lynch, Susan V., Bacharier, Leonard B., O'Connor, George T., Sandel, Megan T., Kattan, Meyer, Wood, Robert A., Gergen, Peter J., Jackson, Daniel J., Togias, Alkis, and Gern, James E.

Published
2025
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2. Determinants of lung function across childhood in the Severe Asthma Research Program (SARP) 3.

Author

Gaffin, Jonathan, Petty, Carter, Sorkness, Ronald, Denlinger, Loren, Phillips, Brenda, Ly, Ngoc, Gaston, Benjamin, Ross, Kristie, Fitzpatrick, Anne, Bacharier, Leonard, DeBoer, Mark, Teague, W, Wenzel, Sally, Ramratnam, Sima, Israel, Elliot, Mauger, David, and Phipatanakul, Wanda

Subjects
Severe asthma, asthma exacerbations, lung function, spirometry, Male, Female, Child, Humans, Adult, Forced Expiratory Volume, Asthma, Bronchodilator Agents, Respiratory Function Tests, Spirometry, Lung
Abstract

BACKGROUND: Children with asthma are at risk for low lung function extending into adulthood, but understanding of clinical predictors is incomplete. OBJECTIVE: We sought to determine phenotypic factors associated with FEV1 throughout childhood in the Severe Asthma Research Program 3 pediatric cohort. METHODS: Lung function was measured at baseline and annually. Multivariate linear mixed-effects models were constructed to assess the effect of baseline and time-varying predictors of prebronchodilator FEV1 at each assessment for up to 6 years. All models were adjusted for age, predicted FEV1 by Global Lung Function Initiative reference equations, race, sex, and height. Secondary outcomes included postbronchodilator FEV1 and prebronchodilator FEV1/forced vital capacity. RESULTS: A total of 862 spirometry assessments were performed for 188 participants. Factors associated with FEV1 include baseline Feno (B, -49 mL/log2 PPB; 95% CI, -92 to -6), response to a characterizing dose of triamcinolone acetonide (B, -8.4 mL/1% change FEV1 posttriamcinolone; 95% CI, -12.3 to -4.5), and maximal bronchodilator reversibility (B, -27 mL/1% change postbronchodilator FEV1; 95% CI, -37 to -16). Annually assessed time-varying factors of age, obesity, and exacerbation frequency predicted FEV1 over time. Notably, there was a significant age and sex interaction. Among girls, there was no exacerbation effect. For boys, however, moderate (1-2) exacerbation frequency in the previous 12 months was associated with -20 mL (95% CI, -39 to -2) FEV1 at each successive year. High exacerbation frequency (≥3) 12 to 24 months before assessment was associated with -34 mL (95% CI, -61 to -7) FEV1 at each successive year. CONCLUSIONS: In children with severe and nonsevere asthma, several clinically relevant factors predict FEV1 over time. Boys with recurrent exacerbations are at high risk of lower FEV1 through childhood.

Published
2023

3. Exacerbation-prone asthma in the context of race and ancestry in Asthma Clinical Research Network trials

Author

Grossman, Nicole L, Ortega, Victor E, King, Tonya S, Bleecker, Eugene R, Ampleford, Elizabeth A, Bacharier, Leonard B, Cabana, Michael D, Cardet, Juan C, Carr, Tara F, Castro, Mario, Denlinger, Loren C, Denson, Joshua L, Fandino, Nicolas, Fitzpatrick, Anne M, Hawkins, Gregory A, Holguin, Fernando, Krishnan, Jerry A, Lazarus, Stephen C, Nyenhuis, Sharmilee M, Phipatanakul, Wanda, Ramratnam, Sima K, Wenzel, Sally, Peters, Stephen P, Meyers, Deborah A, Wechsler, Michael E, and Israel, Elliot

Subjects
Biomedical and Clinical Sciences, Immunology, Genetics, Asthma, Lung, Clinical Trials and Supportive Activities, Clinical Research, Respiratory, Adult, Black or African American, Humans, Male, Middle Aged, Registries, Risk Factors, Self Report, White People, Exacerbations, race, ancestry, admixture, lung function, genetics, asthma, black, African American, ethnic group, Allergy
Abstract

BackgroundMinority groups of African descent experience disproportionately greater asthma morbidity compared with other racial groups, suggesting that genetic variation from a common ancestry could influence exacerbation risk.ObjectiveWe evaluated clinical trial measures in the context of self-reported race and genetic ancestry to identify risk factors for asthma exacerbations.MethodsOne thousand eight hundred forty multiethnic subjects from 12 Asthma Clinical Research Network and AsthmaNet trials were analyzed for incident asthma exacerbations with Poisson regression models that included clinical measures, self-reported race (black, non-Hispanic white, and other), and estimates of global genetic African ancestry in a subgroup (n = 760).ResultsTwenty-four percent of 1840 subjects self-identified as black. Black and white subjects had common risk factors for exacerbations, including a history of 2 or more exacerbations in the previous year and FEV1 percent predicted values, whereas chronic sinusitis, allergic rhinitis, and gastroesophageal reflux disease were only associated with increased exacerbation risk in black subjects. In the combined multiethnic cohort, neither race (P = .30) nor percentage of genetic African ancestry as a continuous variable associated with exacerbation risk (adjusted rate ratio [RR], 1.26 [95% CI, 0.94-1.70; P = .13]; RR per 1-SD change [32% ancestry], 0.97 [95% CI, 0.78-1.19; P = .74]). However, in 161 black subjects with genetic data, those with African ancestry greater than the median (≥82%) had a significantly greater risk of exacerbation (RR, 3.06 [95% CI, 1.09-8.6; P = .03]).ConclusionBlack subjects have unique risk factors for asthma exacerbations, of which global African genetic ancestry had the strongest effect.

Published
2019

4. Clinical significance of the bronchodilator response in children with severe asthma

Author

Coverstone, Andrea M, Bacharier, Leonard B, Wilson, Bradley S, Fitzpatrick, Anne M, Teague, William Gerald, Phipatanakul, Wanda, Wenzel, Sally E, Gaston, Benjamin M, Bleecker, Eugene R, Moore, Wendy C, Ramratnam, Sima, Jarjour, Nizar N, Ly, Ngoc P, Fahy, John V, Mauger, David T, Schechtman, Kenneth B, Yin‐DeClue, Huiqing, Boomer, Jonathan S, and Castro, Mario

Subjects
Asthma, Pediatric, Lung, Clinical Research, Respiratory, Adolescent, Albuterol, Breath Tests, Bronchodilator Agents, Child, Cohort Studies, Cross-Sectional Studies, Dose-Response Relationship, Drug, Female, Forced Expiratory Volume, Humans, Immunoglobulin E, Male, Nitric Oxide, Odds Ratio, Patient Acuity, Phenotype, Spirometry, asthma, bronchodilator response, pediatrics
Abstract

BackgroundOur objective was to determine those characteristics associated with reversibility of airflow obstruction and response to maximal bronchodilation in children with severe asthma through the Severe Asthma Research Program (SARP).MethodsWe performed a cross-sectional analysis evaluating children ages 6 to 17 years with nonsevere asthma (NSA) and severe asthma (SA). Participants underwent spirometry before and after 180 µg of albuterol to determine reversibility (≥12% increase in FEV1 ). Participants were then given escalating doses up to 720 µg of albuterol to determine their maximum reversibility.ResultsWe evaluated 230 children (n = 129 SA, n = 101 NSA) from five centers across the United States in the SARP I and II cohorts. SA (odds ratio [OR], 2.08, 95% confidence interval [CI], 1.05-4.13), second-hand smoke exposure (OR, 2.81, 95%CI, 1.23-6.43), and fractional exhaled nitric oxide (FeNO; OR, 1.97, 95%CI, 1.35-2.87) were associated with increased odds of airway reversibility after maximal bronchodilation, while higher prebronchodilator (BD) FEV1 % predicted (OR, 0.91, 95%CI, 0.88-0.94) was associated with decreased odds. In an analysis using the SARP III cohort (n = 186), blood neutrophils, immunoglobulin E (IgE), and FEV1 % predicted were significantly associated with BD reversibility. In addition, children with BD response have greater healthcare utilization. BD reversibility was associated with reduced lung function at enrollment and 1-year follow-up though less decline in lung function over 1 year compared to those without reversibility.ConclusionsLung function, that is FEV1 % predicted, is a predictor of BD response in children with asthma. Additionally, smoke exposure, higher FeNO or IgE level, and low peripheral blood neutrophils are associated with a greater likelihood of BD reversibility. BD response can identify a phenotype of pediatric asthma associated with low lung function and poor asthma control.

Published
2019

5. Racial disparities in asthma-related health care use in the National Heart, Lung, and Blood Institute's Severe Asthma Research Program

Author

Fitzpatrick, Anne M, Gillespie, Scott E, Mauger, David T, Phillips, Brenda R, Bleecker, Eugene R, Israel, Elliot, Meyers, Deborah A, Moore, Wendy C, Sorkness, Ronald L, Wenzel, Sally E, Bacharier, Leonard B, Castro, Mario, Denlinger, Loren C, Erzurum, Serpil C, Fahy, John V, Gaston, Benjamin M, Jarjour, Nizar N, Larkin, Allyson, Levy, Bruce D, Ly, Ngoc P, Ortega, Victor E, Peters, Stephen P, Phipatanakul, Wanda, Ramratnam, Sima, and Teague, W Gerald

Subjects
Clinical Research, Health Services, Asthma, Lung, Respiratory, Good Health and Well Being, Adolescent, Adult, African Americans, Emergency Service, Hospital, Female, Humans, Male, Middle Aged, National Heart, Lung, and Blood Institute (U.S.), Patient Acceptance of Health Care, United States, Whites, Young Adult, Asthma control, asthma exacerbation, racial disparities, health care use, propensity scoring, inverse probability of treatment weighting, White People, Black or African American, Immunology, Allergy
Abstract

BackgroundDespite advances in asthma care, disparities persist. Black patients are disproportionally affected by asthma and also have poorer outcomes compared with white patients.ObjectiveWe sought to determine associations between black and white patients and asthma-related health care use, accounting for complex relationships.MethodsThis study was completed as part of the National Heart, Lung, and Blood Institute's Severe Asthma Research Program, a prospective observational cohort. Between November 2012 and February 2015, it enrolled 579 participants 6 years and older with 1 year of observation time and complete data. Inverse probability of treatment weighting was used to balance racial groups with respect to community and family socioeconomic variables and environmental exposure variables. The primary outcome was emergency department (ED) use for asthma. Secondary outcomes included inhaled corticosteroid use, outpatient physician's office visits for asthma, and asthma-related hospitalization.ResultsBlack patients had greater odds of ED use over 1 year (odds ratio, 2.19; 95% CI, 1.43-3.35) but also differed in the majority (>50%) of baseline variables measured. After statistical balancing of the racial groups, the difference between black and white patients with respect to ED use no longer reached the level of significance. Instead, in secondary analyses black patients were less likely to see an outpatient physician for asthma management (adjusted odds ratio, 0.57; 95% CI, 0.38-0.85).ConclusionsThe disparity in ED use was eliminated after consideration of multiple variables. Social and environmental policies and interventions tailored to black populations with a high burden of asthma are critical to reduction (or elimination) of these disparities.

Published
2019

6. 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

7. 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

8. 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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10. Income is an independent risk factor for worse asthma outcomes.

Author

Cardet, Juan, Louisias, Margee, King, Tonya, Castro, Mario, Codispoti, Christopher, Dunn, Ryan, Engle, Linda, Giles, B, Holguin, Fernando, Lima, John, Long, Dayna, Lugogo, Njira, Nyenhuis, Sharmilee, Ortega, Victor, Ramratnam, Sima, Wechsler, Michael, Israel, Elliot, and Phipatanakul, Wanda

Subjects
Disparities, Vitamin D Add-On Therapy Enhances Corticosteroid trial, asthma exacerbation, education, low income, psychological stress, socioeconomic status, Adult, Asthma, Double-Blind Method, Female, Humans, Income, Male, Middle Aged, Risk Factors, Socioeconomic Factors
Abstract

BACKGROUND: Socioeconomic status (SES) is associated with asthma morbidity in observational studies, but the factors underlying this association are uncertain. OBJECTIVE: We investigated whether 3 SES correlates-low income, low education, and high perceived stress-were independent risk factors for treatment failure and asthma exacerbations in the context of a randomized controlled trial. METHODS: The effect of low SES (household income of 20 on a perceived stress scale) on asthma morbidity was analyzed in 381 participants by using Poisson regression models. The primary outcome was treatment failure (defined in the trial protocol as a significant clinical or airflow deterioration), and the secondary outcome was asthma exacerbations requiring systemic corticosteroids. RESULTS: Fifty-four percent of participants had a low income, 40% had a low educational level, and 17% had high perceived stress levels. Even after adjusting for race and other important confounders, participants with lower income had higher rates of both treatment failures (rate ratio, 1.6; 95% CI, 1.1-2.3; P = .03) and exacerbations (rate ratio, 1.9; 95% CI, 1.1-3.3; P = .02). Adherence with inhaled corticosteroids was similarly high for both income categories. Education and perceived stress were not significantly associated with either outcome. CONCLUSIONS: In the context of a randomized controlled trial, participants with lower income were more likely to experience adverse asthma outcomes independent of education, perceived stress, race, and medication adherence.

Published
2018

12. Inflammatory and Comorbid Features of Patients with Severe Asthma and Frequent Exacerbations

Author

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

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Lung, Clinical Research, Asthma, Respiratory, Adolescent, Adult, Albuterol, Biomarkers, Body Mass Index, Breath Tests, Bronchodilator Agents, Chi-Square Distribution, Child, Comorbidity, Disease Progression, Disease Susceptibility, Drug Resistance, Eosinophils, Female, Humans, Immunoglobulin E, Inflammation, Male, Middle Aged, Nitric Oxide, Severity of Illness Index, Sex Distribution, Sputum, exacerbation-prone asthma, bronchodilator reversibility, eosinophils, sinusitis, gastroesophageal reflux, National Heart, Lung, and Blood Institute’s Severe Asthma Research Program-3 Investigators, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleReducing asthma exacerbation frequency is an important criterion for approval of asthma therapies, but the clinical features of exacerbation-prone asthma (EPA) remain incompletely defined.ObjectivesTo describe the clinical, physiologic, inflammatory, and comorbidity factors associated with EPA.MethodsBaseline data from the NHLBI Severe Asthma Research Program (SARP)-3 were analyzed. An exacerbation was defined as a burst of systemic corticosteroids lasting 3 days or more. Patients were classified by their number of exacerbations in the past year: none, few (one to two), or exacerbation prone (≥3). Replication of a multivariable model was performed with data from the SARP-1 + 2 cohort.Measurements and main resultsOf 709 subjects in the SARP-3 cohort, 294 (41%) had no exacerbations and 173 (24%) were exacerbation prone in the prior year. Several factors normally associated with severity (asthma duration, age, sex, race, and socioeconomic status) did not associate with exacerbation frequency in SARP-3; bronchodilator responsiveness also discriminated exacerbation proneness from asthma severity. In the SARP-3 multivariable model, blood eosinophils, body mass index, and bronchodilator responsiveness were positively associated with exacerbation frequency (rate ratios [95% confidence interval], 1.6 [1.2-2.1] for every log unit of eosinophils, 1.3 [1.1-1.4] for every 10 body mass index units, and 1.2 [1.1-1.4] for every 10% increase in bronchodilatory responsiveness). Chronic sinusitis and gastroesophageal reflux were also associated with exacerbation frequency (1.7 [1.4-2.1] and 1.6 [1.3-2.0]), even after adjustment for multiple factors. These effects were replicated in the SARP-1 + 2 multivariable model.ConclusionsEPA may be a distinct susceptibility phenotype with implications for the targeting of exacerbation prevention strategies. Clinical trial registered with www.clinicaltrials.gov (NCT 01760915).

Published
2017

13. Improving Quality of Acute Asthma Care in US Hospitals Changes Between 1999-2000 and 2012-2013

Author

Hasegawa, Kohei, Tsugawa, Yusuke, Clark, Sunday, Eastin, Carly D, Gabriel, Susan, Herrera, Vivian, Bittner, Jane C, Camargo, Carlos A, Investigators, MARC-37, Ahn, Jason, Aurora, Taruna, Brenner, Barry, Brown, Mark A, Calhoun, William, Gough, John E, Gharib, Asal, Heidt, Jonathan, Khosravi, Mehdi, Moore, Wendy C, Mould-Millman, Nee-Kofi, Nonas, Stephanie, Nowak, Richard, Pei, Veronica, Press, Valerie G, Probst, Beatrice D, Ramratnam, Sima K, Tallar, Matthew, Teuber, Suzanne S, Trent, Stacy A, Villarreal, Roberto, Watase, Taketo, and Youngquist, Scott

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Lung, Clinical Research, Asthma, Patient Safety, Health and social care services research, 8.1 Organisation and delivery of services, Respiratory, Adolescent, Adult, Child, Preschool, Emergency Service, Hospital, Female, Guideline Adherence, Hospitalization, Humans, Length of Stay, Male, Middle Aged, Quality Improvement, Retrospective Studies, United States, asthma, guideline, hospitalization, quality of care, MARC-37 Investigators, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundLittle is known about the longitudinal change in the quality of acute asthma care for hospitalized children and adults in the United States. We investigated whether the concordance of inpatient asthma care with the national guidelines improved over time, identified hospital characteristics predictive of guideline concordance, and determined whether guideline-concordant care is associated with a shorter hospital length of stay (LOS).MethodsThis study was an analysis of data from two multicenter chart review studies of hospitalized patients aged 2 to 54 years with acute asthma during two time periods: 1999-2000 and 2012-2013. Outcomes were guideline concordance at the patient and hospital levels, and association of patient composite concordance with hospital LOS.ResultsThe analytic cohort for the comparison of guideline concordance comprised 1,634 patients: 834 patients from 1999-2000 vs 800 patients from 2012-2013. Over these 15 years, inpatient asthma care became more concordant at the hospital-level, with the mean composite score increasing from 74 to 82 (P < .001). However, during 2012-2013, wide variability in guideline concordance of acute asthma care remained across hospitals, with the greatest variation in provision of individualized written action plan at discharge (SD, 36). Guideline concordance was significantly lower in Midwestern and Southern hospitals compared with Northeastern hospitals. After adjusting for severity, patients who received care perfectly concordant with the guidelines had significantly shorter hospital LOS (-14% [95% CI, -23 to -4]; P = .009).ConclusionsBetween 1999 and 2013, the guideline concordance of acute asthma care for hospitalized patients improved. However, interhospital variability remains substantial. Greater concordance with evidence-based guidelines was associated with a shorter hospital LOS.

Published
2016

14. Stress and Bronchodilator Response in Children with Asthma

Author

Brehm, John M, Ramratnam, Sima K, Tse, Sze Man, Croteau-Chonka, Damien C, Pino-Yanes, Maria, Rosas-Salazar, Christian, Litonjua, Augusto A, Raby, Benjamin A, Boutaoui, Nadia, Han, Yueh-Ying, Chen, Wei, Forno, Erick, Marsland, Anna L, Nugent, Nicole R, Eng, Celeste, Colón-Semidey, Angel, Alvarez, María, Acosta-Pérez, Edna, Spear, Melissa L, Martinez, Fernando D, Avila, Lydiana, Weiss, Scott T, Soto-Quiros, Manuel, Ober, Carole, Nicolae, Dan L, Barnes, Kathleen C, Lemanske, Robert F, Strunk, Robert C, Liu, Andrew, London, Stephanie J, Gilliland, Frank, Sleiman, Patrick, March, Michael, Hakonarson, Hakon, Duan, Qing Ling, Kolls, Jay K, Fritz, Gregory K, Hu, Donglei, Fani, Negar, Stevens, Jennifer S, Almli, Lynn M, Burchard, Esteban G, Shin, Jaemin, McQuaid, Elizabeth L, Ressler, Kerry, Canino, Glorisa, and Celedón, Juan C

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Genetics, Mental Health, Behavioral and Social Science, Pediatric, Asthma, Lung, Clinical Research, 2.1 Biological and endogenous factors, Respiratory, Good Health and Well Being, Adolescent, Anxiety, Bronchodilator Agents, Case-Control Studies, Child, Cross-Sectional Studies, Down-Regulation, Female, Genetic Markers, Genotype, Humans, Linear Models, Male, Multivariate Analysis, Polymorphism, Single Nucleotide, Puerto Rico, Receptors, Adrenergic, beta-2, Receptors, Pituitary Adenylate Cyclase-Activating Polypeptide, Type I, Rhode Island, Risk Factors, Stress, Psychological, Treatment Outcome, asthma, Puerto Ricans, bronchodilator response, stress, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleStress is associated with asthma morbidity in Puerto Ricans (PRs), who have reduced bronchodilator response (BDR).ObjectivesTo examine whether stress and/or a gene regulating anxiety (ADCYAP1R1) is associated with BDR in PR and non-PR children with asthma.MethodsThis was a cross-sectional study of stress and BDR (percent change in FEV1 after BD) in 234 PRs ages 9-14 years with asthma. We assessed child stress using the Checklist of Children's Distress Symptoms, and maternal stress using the Perceived Stress Scale. Replication analyses were conducted in two cohorts. Polymorphisms in ADCYAP1R1 were genotyped in our study and six replication studies. Multivariable models of stress and BDR were adjusted for age, sex, income, environmental tobacco smoke, and use of inhaled corticosteroids.Measurements and main resultsHigh child stress was associated with reduced BDR in three cohorts. PR children who were highly stressed (upper quartile, Checklist of Children's Distress Symptoms) and whose mothers had high stress (upper quartile, Perceived Stress Scale) had a BDR that was 10.2% (95% confidence interval, 6.1-14.2%) lower than children who had neither high stress nor a highly stressed mother. A polymorphism in ADCYAP1R1 (rs34548976) was associated with reduced BDR. This single-nucleotide polymorphism is associated with reduced expression of the gene for the β2-adrenergic receptor (ADRB2) in CD4(+) lymphocytes of subjects with asthma, and it affects brain connectivity of the amygdala and the insula (a biomarker of anxiety).ConclusionsHigh child stress and an ADCYAP1R1 single-nucleotide polymorphism are associated with reduced BDR in children with asthma. This is likely caused by down-regulation of ADRB2 in highly stressed children.

Published
2015

15. Early Life Wheezing and Childhood Cognition in the Environmental Influences on Child Health Outcomes (ECHO) Program

Author

Ramratnam, Sima, primary, Seaberg, Eric, additional, O'Shea, Michael, additional, Nkoy, Flory, additional, Litonjua, Augusto, additional, Korrick, Susan, additional, Kelly, Rachel, additional, Joeseph, Robert, additional, Chu, Su, additional, Jensen, Elizabeth, additional, Gold, Diane, additional, Carroll, Kecia, additional, Gower, William, additional, Perzanowski, Matthew, additional, and Gern, James, additional

Published
2024
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19. Improving Quality of Acute Asthma Care in US Hospitals: Changes Between 1999-2000 and 2012-2013

Author

Ahn, Jason, Aurora, Taruna, Brenner, Barry, Brown, Mark A., Calhoun, William, Gough, John E., Gharib, Asal, Heidt, Jonathan, Khosravi, Mehdi, Moore, Wendy C., Mould-Millman, Nee-Kofi, Nonas, Stephanie, Nowak, Richard, Pei, Veronica, Press, Valerie G., Probst, Beatrice D., Ramratnam, Sima K., Tallar, Matthew, Teuber, Suzanne S., Trent, Stacy A., Villarreal, Roberto, Watase, Taketo, Youngquist, Scott, Hasegawa, Kohei, Tsugawa, Yusuke, Clark, Sunday, Eastin, Carly D., Gabriel, Susan, Herrera, Vivian, Bittner, Jane C., and Camargo, Carlos A., Jr.

Published
2016
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20. Children and Adults With Frequent Hospitalizations for Asthma Exacerbation, 2012-2013: A Multicenter Observational Study

Author

Aurora, Taruna, Brenner, Barry, Brown, Mark A., Calhoun, William, Gough, John E., Gutta, Ravi C., Heidt, Jonathan, Khosravi, Mehdi, Moore, Wendy C., Mould-Millman, Nee-Kofi, Nowak, Richard, Ahn, Jason, Pei, Veronica, Press, Valerie G., Probst, Beatrice D., Ramratnam, Sima K., Hartman, Heather, Snipes, Carly, Teuber, Suzanne S., Trent, Stacy A., Villarreal, Roberto, Youngquist, Scott, Hasegawa, Kohei, Bittner, Jane C., Nonas, Stephanie A., Stoll, Samantha J., Watase, Taketo, Gabriel, Susan, Herrera, Vivian, and Camargo, Carlos A., Jr.

Published
2015
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22. Underuse of guideline-recommended long-term asthma management in children hospitalized to the intensive care unit: a multicenter observational study

Author

Aurora, Taruna, Brenner, Barry, Calhoun, William, Gough, John E., Gutta, Ravi C., Heidt, Jonathan, Khosravi, Mehdi, Moore, Wendy C., Mould-Millman, Nee-Kofi, Nonas, Stephanie, Nowak, Richard, Ahn, Jason, Pei, Veronica, Probst, Beatrice D., Ramratnam, Sima K., Tallar, Matthew, Snipes, Carly, Teuber, Suzanne S., Trent, Stacy A., Villarreal, Roberto, Watase, Taketo, Youngquist, Scott, Hasegawa, Kohei, Brown, Mark A., Press, Valerie G., Gabriel, Susan, Herrera, Vivian, Bittner, Jane C., and Camargo, Carlos A., Jr.

Published
2015
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23. Comparison of Rhinitis Phenotypes with the Development of Asthma by Age 10 in an Urban Birth Cohort

Author

Tanis, Ross, primary, Calatroni, Agustin, additional, Bacharier, Leonard, additional, Little, Frederic, additional, Sandel, Megan, additional, Rivera-Spoljaric, Katherine, additional, Visness, Cynthia, additional, Togias, Alkis, additional, Gergen, Peter, additional, Gern, James, additional, Ramratnam, Sima, additional, Lamm, Carin, additional, Wood, Robert, additional, and Johnson, Molly, additional

Published
2023
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27. Associations between Early Life Environmental Exposures and Rhinitis Trajectories in an Urban Birth Cohort

Author

Ramratnam, Sima, primary, Johnson, Molly, additional, Calatroni, Agustin, additional, Bacharier, Leonard, additional, Lamm, Carin, additional, Little, Frederic, additional, Sandel, Megan, additional, Rivera-Spoljaric, Katherine, additional, Wood, Robert, additional, Limkar, Ajinkya, additional, Visness, Cynthia, additional, Togias, Alkis, additional, Gergen, Peter, additional, and Gern, James, additional

Published
2022
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28. The Precision Interventions for Severe and/or Exacerbation-Prone (PrecISE) Asthma Network: An overview of Network organization, procedures, and interventions

Author

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

Published
2022
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33. Airway Epithelium Gene Expression Endotyping of Asthma and Airway Obstruction in Urban Children

Author

Altman, Matthew, primary, Ramratnam, Sima, additional, Jackson, Daniel, additional, Presnell, Scott, additional, Gergen, Peter, additional, Bacharier, Leonard, additional, Kattan, Meyer, additional, O, George, additional, Wood, Robert, additional, Calatroni, Agustin, additional, Busse, William, additional, Visness, Cynthia, additional, and Gern, James, additional

Published
2020
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34. Spirometry and Impulse Oscillometry Trajectories in an Inner-City Longitudinal Birth Cohort at High Risk for Asthma.

Author

Ramratnam, Sima, primary, Lockhart, Alexandre, additional, Calatroni, Agustin, additional, Bacharier, Leonard B., additional, Jackson, Daniel J., additional, Wood, Robert A., additional, Kattan, Meyer, additional, O'Connor, Peter, additional, Visness, Cynthia M., additional, Gergen, Peter J., additional, and Gern, James E., additional

Published
2019
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36. Sputum Mast Cells and Eosinophils Identify Asthmatics with Lower Lung Function and Proneness to Exacerbations

Author

Fajt, Merritt L., primary, Peters, Michael, additional, Bleecker, Eugene R., additional, Cardet, Juan Carlos, additional, Castro, Mario, additional, Comhair, Suzy, additional, Coverstone, Andrea, additional, Denlinger, Loren C., additional, Erzurum, Serpil C., additional, Hastie, Annette T., additional, Israel, Elliot, additional, Jarjour, Nizar N., additional, Johansson, Mats W., additional, Levy, Bruce D., additional, Mauger, David M., additional, Peters, Stephen P., additional, Phillips, Brenda R., additional, Phipatanakul, Wanda, additional, Ross, Kristie R., additional, Ramratnam, Sima K., additional, Fahy, John V., additional, and Wenzel, Sally, additional

Published
2018
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37. Maternal Stress and Depression are Associated with Development of a High-Wheeze, Low-Atopy Phenotype in Their Young Offspring

Author

Ramratnam, Sima K., primary, Calatroni, Agustin, additional, Bacharier, Leonard, additional, Jackson, Daniel J., additional, Beigelman, Avraham, additional, Wood, Robert A., additional, Kattan, Meyer, additional, O'Connor, George T., additional, Visness, Cynthia M., additional, Gergen, Peter J., additional, and Gern, James E., additional

Published
2018
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40. Reproducibility and stability of severe asthma research program (SARP) clinical cluster phenotypes in SARP3

Author

Moore, Wendy, primary, Li, Xingnan, additional, Li, Huashi, additional, Castro, Mario, additional, Erzurum, Serpil, additional, Fahy, John, additional, Israel, Elliot, additional, Jarjour, Nizar, additional, Levy, Bruce, additional, Bacharier, Lenoard, additional, Fitzpatrick, Anne, additional, Gaston, Ben, additional, Ly, Ngoc, additional, Myers, Ross, additional, Ramratnam, Sima, additional, Phipatanakul, Wanda, additional, Teague, W. Gerald, additional, Mauger, David, additional, Wenzel, Sally, additional, Meyers, Deborah, additional, and Bleecker, Eugene, additional

Published
2016
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41. Variation in asthma care at hospital discharge by race/ethnicity groups.

Author

Trent, Stacy A., Hasegawa, Kohei, Ramratnam, Sima K., Bittner, Jane C., and Camargo, Carlos A.

Subjects
ETHNIC differences, ADULT-child relationships, GENERALIZED estimating equations, SIMULATED patients, ASTHMA
Abstract

Objective: While asthma disproportionately affects minorities, little is known about racial/ethnic differences in asthma care at hospital discharge. Methods: Secondary data analysis of multicenter retrospective study using standardized medical record review. A random sample of patients aged 2-54 years, who were hospitalized for asthma at 25 hospitals from 2012 to 2013 was analyzed. We categorized patients into three race/ethnicity groups: non-Hispanic white (NHW), non-Hispanic black (NHB), and Hispanic. Multivariable logistic regression using generalized estimating equations was used to examine the relationship between race/ethnicity and the provision of guideline-concordant asthma care at hospital discharge including: the provision of asthma action plans, provision of new prescription of an inhaled corticosteroid, and referral to an asthma specialist. Results: Nine hundred thirteen patients (39% children, 71% minorities) hospitalized for asthma were included. In adjusted models, NHB children were significantly less likely to receive a written asthma action plan (OR 0.48; 95% CI 0.31-0.76) than NHW children. In contrast, among adults, we found no statistically significant difference in the provision of asthma action plan. Additionally, we found no difference in the provision of a new inhaled corticosteroid prescription or referral to an asthma specialist among children or adults. Conclusions: NHB and Hispanic patients represent the majority of patients hospitalized for acute asthma in our cohort and were more likely than NHW patients to have increased markers of asthma severity. Despite this, the only significant racial/ethnic difference in asthma care at hospital discharge was among NHB children, who were less likely to receive a written asthma action plan. [ABSTRACT FROM AUTHOR]

Published
2018
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42. Income Is an Independent Risk Factor for Worse Asthma Outcomes

Author

Cardet, Juan Carlos, primary, King, Tonya S., additional, Louisias, Margee, additional, Castro, Mario, additional, Codispoti, Christopher D., additional, Dunn, Ryan, additional, Giles, Brenda L., additional, Holguin, Fernando, additional, Lima, John, additional, Long, Dayna, additional, Lugogo, Njira, additional, Nyenhuis, Sharmilee M., additional, Ortega, Victor E., additional, Ramratnam, Sima, additional, Wechsler, Michael E., additional, Israel, Elliot, additional, and Phipatanakul, Wanda, additional

Published
2016
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43. Children and Adults With Frequent Hospitalizations for Asthma Exacerbation, 2012-2013: A Multicenter Observational Study

Author

Hasegawa, Kohei, primary, Bittner, Jane C., additional, Nonas, Stephanie A., additional, Stoll, Samantha J., additional, Watase, Taketo, additional, Gabriel, Susan, additional, Herrera, Vivian, additional, Camargo, Carlos A., additional, Aurora, Taruna, additional, Brenner, Barry, additional, Brown, Mark A., additional, Calhoun, William, additional, Gough, John E., additional, Gutta, Ravi C., additional, Heidt, Jonathan, additional, Khosravi, Mehdi, additional, Moore, Wendy C., additional, Mould-Millman, Nee-Kofi, additional, Nowak, Richard, additional, Ahn, Jason, additional, Pei, Veronica, additional, Press, Valerie G., additional, Probst, Beatrice D., additional, Ramratnam, Sima K., additional, Hartman, Heather, additional, Snipes, Carly, additional, Teuber, Suzanne S., additional, Trent, Stacy A., additional, Villarreal, Roberto, additional, and Youngquist, Scott, additional

Published
2015
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44. Underuse of guideline-recommended long-term asthma management in children hospitalized to the intensive care unit: a multicenter observational study

Author

Hasegawa, Kohei, primary, Ahn, Jason, additional, Brown, Mark A., additional, Press, Valerie G., additional, Gabriel, Susan, additional, Herrera, Vivian, additional, Bittner, Jane C., additional, Camargo, Carlos A., additional, Aurora, Taruna, additional, Brenner, Barry, additional, Calhoun, William, additional, Gough, John E., additional, Gutta, Ravi C., additional, Heidt, Jonathan, additional, Khosravi, Mehdi, additional, Moore, Wendy C., additional, Mould-Millman, Nee-Kofi, additional, Nonas, Stephanie, additional, Nowak, Richard, additional, Pei, Veronica, additional, Probst, Beatrice D., additional, Ramratnam, Sima K., additional, Tallar, Matthew, additional, Snipes, Carly, additional, Teuber, Suzanne S., additional, Trent, Stacy A., additional, Villarreal, Roberto, additional, Watase, Taketo, additional, and Youngquist, Scott, additional

Published
2015
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45. Additional file 1: of Effects of endogenous sex hormones on lung function and symptom control in adolescents with asthma

Author

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

Subjects
immune system diseases, respiratory tract diseases, 3. Good health
Abstract

Sex Hormones & Asthma. Type of data: Tables and Figures. (DOCX 468 kb)

46. Additional file 1: of Effects of endogenous sex hormones on lung function and symptom control in adolescents with asthma

Author

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

Subjects
immune system diseases, respiratory tract diseases, 3. Good health
Abstract

Sex Hormones & Asthma. Type of data: Tables and Figures. (DOCX 468 kb)

47. Comparison of Race-neutral Versus Race-specific Spirometry Equations for Evaluation of Child Asthma.

Author

Non AL, Li X, Jones MR, Oken E, Hartert T, Schoettler N, Gold DR, Ramratnam S, Schauberger EM, Tantisira K, Bacharier LB, Conrad DJ, Carroll KN, Nkoy FL, Luttmann-Gibson H, Gilliland FD, Breton CV, Kattan M, Lemanske RF Jr, Litonjua AA, McEvoy CT, Rivera-Spoljaric K, Rosas-Salazar C, Joseph CLM, Palmore M, Ryan PH, Wegienka G, Sitarik AR, Singh AM, Miller RL, Zoratti EM, Ownby D, Camargo CA Jr, Aschner JL, Stroustrup A, Farzan SF, Karagas MR, Jackson DJ, and Gern JE

Abstract

Rationale: Race-based estimates of pulmonary function in children could influence the evaluation of asthma in children from racial and ethnic minoritized backgrounds., Objectives: To determine if race-neutral (GLI-Global) versus race-specific (GLI-Race-Specific) reference equations differentially impact spirometry evaluation of childhood asthma., Methods: The analysis included 8,719 children aged 5 to <12 years from 27 cohorts across the United States grouped by parent-reported race and ethnicity. We analyzed how the equations affected forced expiratory volume in 1 second (FEV 1 ), forced vital capacity (FVC), and FEV 1 /FVC z-scores. We used multivariable logistic models to evaluate associations between z-scores calculated with different equations and asthma diagnosis, emergency department (ED) visits, and hospitalization., Measurements and Main Results: For Black children, the GLI-Global vs. Race-Specific equations estimated significantly lower z-scores for FEV 1 and FVC but similar values for FEV 1 /FVC, thus increasing the proportion of children classified with low FEV 1 by 14%. While both equations yielded strong inverse relationships between FEV 1 and FEV 1 /FVC z-scores and asthma outcomes, these relationships varied across racial and ethnic groups (p<0.05). For any given FEV 1 or FEV 1 /FVC z-score, asthma diagnosis and ED visits were higher among Black and Hispanic versus White children (p<0.05). For FEV 1 , GLI-Global equations estimated asthma outcomes that were more uniform across racial and ethnic groups., Conclusions: Parent-reported race and ethnicity influenced relationships between lung function and asthma outcomes. Our data show no advantage to race-specific equations for evaluating childhood asthma, and the potential for race-specific equations to obscure lung impairment in disadvantaged children strongly supports using race-neutral equations.

Published
2024
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48. The Legacy of Redlining: Increasing Childhood Asthma Disparities through Neighborhood Poverty.

Author

Ryan PH, Zanobetti A, Coull BA, Andrews H, Bacharier LB, Bailey D, Beamer PI, Blossom J, Brokamp C, Datta S, Hartert T, Khurana Hershey GK, Jackson DJ, Johnson CC, Joseph C, Kahn J, Lothrop N, Louisias M, Luttmann-Gibson H, Martinez FD, Mendonça EA, Miller RL, Ownby D, Ramratnam S, Seroogy CM, Visness CM, Wright AL, Zoratti EM, Gern JE, and Gold DR

Subjects
Humans, Child, Male, Female, Child, Preschool, United States epidemiology, Residence Characteristics statistics & numerical data, Neighborhood Characteristics, Racism statistics & numerical data, Socioeconomic Factors, Infant, Birth Cohort, Asthma epidemiology, Asthma ethnology, Health Status Disparities, Poverty statistics & numerical data
Abstract

Rationale: Identifying the root causes of racial disparities in childhood asthma is critical for health equity. Objectives: To determine whether the racist policy of redlining in the 1930s led to present-day disparities in childhood asthma by increasing community-level poverty and decreasing neighborhood socioeconomic position (SEP). Methods: We categorized census tracts at the birth address of participants from the Children's Respiratory and Environmental Workgroup birth cohort consortium into categories A, B, C, and D as defined by the Home Owners Loan Corporation, with D being the highest perceived risk. Surrogates of present-day neighborhood-level SEP were determined for each tract, including the percentage of low-income households, the CDC's Social Vulnerability Index, and other tract-level variables. We performed causal mediation analysis, which, under the assumption of no unmeasured confounding, estimates the direct and mediated pathways by which redlining may cause asthma disparities through tract-level mediators adjusting for individual-level covariates. Measurements and Main Results: Of 4,849 children, the cumulative incidence of asthma through age 11 was 26.6%, and 13.2% resided in census tracts with a Home Owners Loan Corporation grade of D. In mediation analyses, residing in Grade-D tracts (adjusted odds ratio = 1.03 [95% confidence interval = 1.01, 1.05]) was significantly associated with childhood asthma, with 79% of this increased risk mediated by percentage of low-income households; results were similar for the Social Vulnerability Index and other tract-level variables. Conclusions: The historical structural racist policy of redlining led to present-day asthma disparities in part through decreased neighborhood SEP. Policies aimed at reversing the effects of structural racism should be considered to create more just, equitable, and healthy communities.

Published
2024
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49. Early-Life Exposure to Air Pollution and Childhood Asthma Cumulative Incidence in the ECHO CREW Consortium.

Author

Zanobetti A, Ryan PH, Coull BA, Luttmann-Gibson H, Datta S, Blossom J, Brokamp C, Lothrop N, Miller RL, Beamer PI, Visness CM, Andrews H, Bacharier LB, Hartert T, Johnson CC, Ownby DR, Khurana Hershey GK, Joseph CLM, Mendonça EA, Jackson DJ, Zoratti EM, Wright AL, Martinez FD, Seroogy CM, Ramratnam SK, Calatroni A, Gern JE, and Gold DR

Subjects
Child, Pregnancy, Female, Male, Humans, Child, Preschool, Incidence, Cohort Studies, Nitrogen Dioxide, Particulate Matter adverse effects, Asthma epidemiology, Asthma etiology, Air Pollution adverse effects
Abstract

Importance: Exposure to outdoor air pollution contributes to childhood asthma development, but many studies lack the geographic, racial and ethnic, and socioeconomic diversity to evaluate susceptibility by individual-level and community-level contextual factors., Objective: To examine early life exposure to fine particulate matter (PM2.5) and nitrogen oxide (NO2) air pollution and asthma risk by early and middle childhood, and whether individual and community-level characteristics modify associations between air pollution exposure and asthma., Design, Setting, and Participants: This cohort study included children enrolled in cohorts participating in the Children's Respiratory and Environmental Workgroup consortium. The birth cohorts were located throughout the US, recruited between 1987 and 2007, and followed up through age 11 years. The survival analysis was adjusted for mother's education, parental asthma, smoking during pregnancy, child's race and ethnicity, sex, neighborhood characteristics, and cohort. Statistical analysis was performed from February 2022 to December 2023., Exposure: Early-life exposures to PM2.5 and NO2 according to participants' birth address., Main Outcomes and Measures: Caregiver report of physician-diagnosed asthma through early (age 4 years) and middle (age 11 years) childhood., Results: Among 5279 children included, 1659 (31.4%) were Black, 835 (15.8%) were Hispanic, 2555 (48.4%) where White, and 229 (4.3%) were other race or ethnicity; 2721 (51.5%) were male and 2596 (49.2%) were female; 1305 children (24.7%) had asthma by 11 years of age and 954 (18.1%) had asthma by 4 years of age. Mean values of pollutants over the first 3 years of life were associated with asthma incidence. A 1 IQR increase in NO2 (6.1 μg/m3) was associated with increased asthma incidence among children younger than 5 years (HR, 1.25 [95% CI, 1.03-1.52]) and children younger than 11 years (HR, 1.22 [95% CI, 1.04-1.44]). A 1 IQR increase in PM2.5 (3.4 μg/m3) was associated with increased asthma incidence among children younger than 5 years (HR, 1.31 [95% CI, 1.04-1.66]) and children younger than 11 years (OR, 1.23 [95% CI, 1.01-1.50]). Associations of PM2.5 or NO2 with asthma were increased when mothers had less than a high school diploma, among Black children, in communities with fewer child opportunities, and in census tracts with higher percentage Black population and population density; for example, there was a significantly higher association between PM2.5 and asthma incidence by younger than 5 years of age in Black children (HR, 1.60 [95% CI, 1.15-2.22]) compared with White children (HR, 1.17 [95% CI, 0.90-1.52])., Conclusions and Relevance: In this cohort study, early life air pollution was associated with increased asthma incidence by early and middle childhood, with higher risk among minoritized families living in urban communities characterized by fewer opportunities and resources and multiple environmental coexposures. Reducing asthma risk in the US requires air pollution regulation and reduction combined with greater environmental, educational, and health equity at the community level.

Published
2024
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