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9 results on '"Brown, Stacey-Ann"'

1. Pulmonary Disease

Author

Whittaker Brown, Stacey-Ann, Braman, Sidney S., Wasserman, Michael R., Section editor, Cesari, Matteo, Section editor, Wasserman, Michael R., editor, Bakerjian, Debra, editor, Linnebur, Sunny, editor, Brangman, Sharon, editor, Cesari, Matteo, editor, and Rosen, Sonja, editor

Published
2024
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2. Bronchodilators in Tobacco-Exposed Persons with Symptoms and Preserved Lung Function

Author

Han, MeiLan K, Ye, Wen, Wang, Di, White, Emily, Arjomandi, Mehrdad, Barjaktarevic, Igor Z, Brown, Stacey-Ann, Buhr, Russell G, Comellas, Alejandro P, Cooper, Christopher B, Criner, Gerard J, Dransfield, Mark T, Drescher, Frank, Folz, Rodney J, Hansel, Nadia N, Kalhan, Ravi, Kaner, Robert J, Kanner, Richard E, Krishnan, Jerry A, Lazarus, Stephen C, Maddipati, Veeranna, Martinez, Fernando J, Mathews, Anne, Meldrum, Catherine, McEvoy, Charlene, Nyunoya, Toru, Rogers, Linda, Stringer, William W, Wendt, Christine H, Wise, Robert A, Wisniewski, Stephen R, Sciurba, Frank C, and Woodruff, Prescott G

Subjects
Lung, Tobacco, Clinical Research, Clinical Trials and Supportive Activities, Tobacco Smoke and Health, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Respiratory, Good Health and Well Being, Adrenergic beta-2 Receptor Agonists, Anti-Bacterial Agents, Bronchodilator Agents, Forced Expiratory Volume, Glucocorticoids, Glycopyrrolate, Humans, Pulmonary Disease, Chronic Obstructive, Treatment Outcome, RETHINC Study Group, Medical and Health Sciences, General & Internal Medicine
Abstract

BackgroundMany persons with a history of smoking tobacco have clinically significant respiratory symptoms despite an absence of airflow obstruction as assessed by spirometry. They are often treated with medications for chronic obstructive pulmonary disease (COPD), but supporting evidence for this treatment is lacking.MethodsWe randomly assigned persons who had a tobacco-smoking history of at least 10 pack-years, respiratory symptoms as defined by a COPD Assessment Test score of at least 10 (scores range from 0 to 40, with higher scores indicating worse symptoms), and preserved lung function on spirometry (ratio of forced expiratory volume in 1 second [FEV1] to forced vital capacity [FVC] ≥0.70 and FVC ≥70% of the predicted value after bronchodilator use) to receive either indacaterol (27.5 μg) plus glycopyrrolate (15.6 μg) or placebo twice daily for 12 weeks. The primary outcome was at least a 4-point decrease (i.e., improvement) in the St. George's Respiratory Questionnaire (SGRQ) score (scores range from 0 to 100, with higher scores indicating worse health status) after 12 weeks without treatment failure (defined as an increase in lower respiratory symptoms treated with a long-acting inhaled bronchodilator, glucocorticoid, or antibiotic agent).ResultsA total of 535 participants underwent randomization. In the modified intention-to-treat population (471 participants), 128 of 227 participants (56.4%) in the treatment group and 144 of 244 (59.0%) in the placebo group had at least a 4-point decrease in the SGRQ score (difference, -2.6 percentage points; 95% confidence interval [CI], -11.6 to 6.3; adjusted odds ratio, 0.91; 95% CI, 0.60 to 1.37; P = 0.65). The mean change in the percent of predicted FEV1 was 2.48 percentage points (95% CI, 1.49 to 3.47) in the treatment group and -0.09 percentage points (95% CI, -1.06 to 0.89) in the placebo group, and the mean change in the inspiratory capacity was 0.12 liters (95% CI, 0.07 to 0.18) in the treatment group and 0.02 liters (95% CI, -0.03 to 0.08) in the placebo group. Four serious adverse events occurred in the treatment group, and 11 occurred in the placebo group; none were deemed potentially related to the treatment or placebo.ConclusionsInhaled dual bronchodilator therapy did not decrease respiratory symptoms in symptomatic, tobacco-exposed persons with preserved lung function as assessed by spirometry. (Funded by the National Heart, Lung, and Blood Institute and others; RETHINC ClinicalTrials.gov number, NCT02867761.).

Published
2022

5. Contributors

Author

Agati, Sergio, Alfano, Fausta, Azuma, Arata, Biffi, Alice, Boerner, Eda, Bonella, Francesco, Brown, Stacey-Ann, Campo, Ilaria, Cannizzaro, Nunzia, Centanni, Stefano, Ceriani, Daniela, Cicchetti, Giuseppe, Cigala, Claudia, Corsico, Angelo Guido, Cottin, Vincent, Danoff, Sonye Karen, Elia, Stefano, Giussani, Federico, Handa, Tomohiro, Jehn, Lutz-Bernhard, Lettieri, Sara, Marchese, Roberto, Mariani, Francesca, Melone, Giulio, Messina, Riccardo, Mondoni, Michele, Negri, Stefano, Palladini, Giovanni, Piciucchi, Sara, Piloni, Davide, Pizzolato, Silvia, Poletti, Venerino, Prasse, Antje, Ravaglia, Claudia, Ruwisch, Jannik, Sakamoto, Ryo, Sambataro, Gianluca, Scichilone, Nicola, Sorino, Claudio, Spanevello, Antonio, Terraneo, Silvia, Tirelli, Claudio, Torre, Olga, Vancheri, Ada, Vancheri, Carlo, Vanetti, Marco, Varone, Francesco, Vassallo, Robert, Visca, Dina, Yoshizawa, Akihiko, and Zappa, Martina

Published
2025
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6. Heterogeneity of Lung Function Phenotypes in Sarcoidosis: Role of Race and Sex Differences

Author

Sharp, Michelle, primary, Psoter, Kevin J., additional, Balasubramanian, Aparna, additional, Pulapaka, Anuhya V., additional, Chen, Edward S., additional, Brown, Stacey-Ann Whittaker, additional, Mathai, Stephen C., additional, Gilotra, Nisha A., additional, Chrispin, Jonathan, additional, Bascom, Rebecca, additional, Bernstein, Richard, additional, Eakin, Michelle N., additional, Wise, Robert A., additional, Moller, David R., additional, and McCormack, Meredith C., additional

Published
2023
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7. Bronchodilators in Symptomatic Tobacco-exposed Persons with Preserved Spirometry for the RETHINC Study Group

Author

Han, MeiLan K., primary, Ye, Wen, additional, Wang, Di, additional, White, Emily, additional, Arjomandi, Mehrdad, additional, Barjaktarevic, Igor, additional, Brown, Stacey-Ann, additional, Buhr, Russell, additional, Comellas, Alejandro, additional, Cooper, Christopher, additional, Criner, Gerard, additional, Dransfield, Mark, additional, Drescher, Frank, additional, Folz, Rodney, additional, Hansel, Nadia, additional, Kaner, Robert, additional, Kanner, Richard, additional, Krishnan, Jerry, additional, Lazarus, Stephen, additional, Maddipati, Veeranna, additional, Martinez, Fernando, additional, Matthews, Anne, additional, Meldrum, Catherine, additional, Mcevoy, Charlene, additional, Nyunoya, Toru, additional, Rogers, Linda, additional, Stringer, William, additional, Wendt, Christine, additional, Wise, Robert, additional, Wisniewski, Stephen, additional, Sciurba, Frank, additional, and Woodruff, Prescott, additional

Published
2022
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8. Shift of lung macrophage composition is associated with COVID-19 disease severity and recovery

Author

Chen, Steven T., Park, Matthew D., Del Valle, Diane Marie, Buckup, Mark, Tabachnikova, Alexandra, Simons, Nicole W., Mouskas, Konstantinos, Lee, Brian, Geanon, Daniel, D’Souza, Darwin, Dawson, Travis, Marvin, Robert, Nie, Kai, Thompson, Ryan C., Zhao, Zhen, LeBerichel, Jessica, Chang, Christie, Jamal, Hajra, Chaddha, Udit, Mathews, Kusum, Acquah, Samuel, Brown, Stacey-Ann, Reiss, Michelle, Harkin, Timothy, Feldmann, Marc, Powell, Charles A., Hook, Jaime L., Kim-Schulze, Seunghee, Rahman, Adeeb H., Brown, Brian D., Beckmann, Noam D., Gnjatic, Sacha, Kenigsberg, Ephraim, Charney, Alexander W., and Merad, Miriam

Subjects
Macrophages, Macrophages, Alveolar, COVID-19, Humans, Lung, Article, Monocytes
Abstract

Although it has been more than 2 years since the start of the coronavirus disease 2019 (COVID-19) pandemic, COVID-19 continues to be a worldwide health crisis. Despite the development of preventive vaccines, therapies to treat COVID-19 and other inflammatory diseases remain a major unmet need in medicine. Our study sought to identify drivers of disease severity and mortality to develop tailored immunotherapy strategies to halt disease progression. We assembled the Mount Sinai COVID-19 Biobank, which was composed of almost 600 hospitalized patients followed longitudinally through the peak of the pandemic in 2020. Moderate disease and survival were associated with a stronger antigen presentation and effector T cell signature. In contrast, severe disease and death were associated with an altered antigen presentation signature, increased numbers of inflammatory immature myeloid cells, and extrafollicular activated B cells that have been previously associated with autoantibody formation. In severely ill patients with COVID-19, lung tissue-resident alveolar macrophages not only were drastically depleted but also had an altered antigen presentation signature, which coincided with an influx of inflammatory monocytes and monocyte-derived macrophages. In addition, we found that the size of the alveolar macrophage pool correlated with patient outcome and that alveolar macrophage numbers and functionality were restored to homeostasis in patients who recovered from COVID-19. These data suggest that local and systemic myeloid cell dysregulation are drivers of COVID-19 severity and modulation of alveolar macrophage numbers and activity in the lung may be a viable therapeutic strategy for the treatment of critical inflammatory lung diseases.

Published
2022

9. A shift in lung macrophage composition is associated with COVID-19 severity and recovery

Author

Chen, Steven T., Park, Matthew D., Del Valle, Diane Marie, Buckup, Mark, Tabachnikova, Alexandra, Thompson, Ryan C., Simons, Nicole W., Mouskas, Konstantinos, Lee, Brian, Geanon, Daniel, D’Souza, Darwin, Dawson, Travis, Marvin, Robert, Nie, Kai, Zhao, Zhen, LeBerichel, Jessica, Chang, Christie, Jamal, Hajra, Akturk, Guray, Chaddha, Udit, Mathews, Kusum, Acquah, Samuel, Brown, Stacey-Ann, Reiss, Michelle, Harkin, Timothy, Feldmann, Marc, Powell, Charles A., Hook, Jaime L., Kim-Schulze, Seunghee, Rahman, Adeeb H., Brown, Brian D., Beckmann, Noam D., Gnjatic, Sacha, Kenigsberg, Ephraim, Charney, Alexander W., and Merad, Miriam

Abstract

Although it has been more than 2 years since the start of the coronavirus disease 2019 (COVID-19) pandemic, COVID-19 continues to be a worldwide health crisis. Despite the development of preventive vaccines, therapies to treat COVID-19 and other inflammatory diseases remain a major unmet need in medicine. Our study sought to identify drivers of disease severity and mortality to develop tailored immunotherapy strategies to halt disease progression. We assembled the Mount Sinai COVID-19 Biobank, which was composed of almost 600 hospitalized patients followed longitudinally through the peak of the pandemic in 2020. Moderate disease and survival were associated with a stronger antigen presentation and effector T cell signature. In contrast, severe disease and death were associated with an altered antigen presentation signature, increased numbers of inflammatory immature myeloid cells, and extrafollicular activated B cells that have been previously associated with autoantibody formation. In severely ill patients with COVID-19, lung tissue–resident alveolar macrophages not only were drastically depleted but also had an altered antigen presentation signature, which coincided with an influx of inflammatory monocytes and monocyte-derived macrophages. In addition, we found that the size of the alveolar macrophage pool correlated with patient outcome and that alveolar macrophage numbers and functionality were restored to homeostasis in patients who recovered from COVID-19. These data suggest that local and systemic myeloid cell dysregulation are drivers of COVID-19 severity and modulation of alveolar macrophage numbers and activity in the lung may be a viable therapeutic strategy for the treatment of critical inflammatory lung diseases.

Published
2022
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