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6 results on '"Musaeus Poulsen, Lone"'

2. Haloperidol for the treatment of delirium in critically ill patients:an updated systematic review with meta-analysis and trial sequential analysis

Author

Andersen-Ranberg, Nina Christine, Barbateskovic, Marija, Perner, Anders, Oxenbøll Collet, Marie, Musaeus Poulsen, Lone, van der Jagt, Mathieu, Smit, Lisa, Wetterslev, Jørn, Mathiesen, Ole, Maagaard, Mathias, Andersen-Ranberg, Nina Christine, Barbateskovic, Marija, Perner, Anders, Oxenbøll Collet, Marie, Musaeus Poulsen, Lone, van der Jagt, Mathieu, Smit, Lisa, Wetterslev, Jørn, Mathiesen, Ole, and Maagaard, Mathias

Abstract

Background Haloperidol is frequently used in critically ill patients with delirium, but evidence for its effects has been sparse and inconclusive. By including recent trials, we updated a systematic review assessing effects of haloperidol on mortality and serious adverse events in critically ill patients with delirium. Methods This is an updated systematic review with meta-analysis and trial sequential analysis of randomised clinical trials investigating haloperidol versus placebo or any comparator in critically ill patients with delirium. We adhered to the Cochrane handbook, the PRISMA guidelines and the grading of recommendations assessment, development and evaluation statements. The primary outcomes were all-cause mortality and proportion of patients with one or more serious adverse events or reactions (SAEs/SARs). Secondary outcomes were days alive without delirium or coma, delirium severity, cognitive function and health-related quality of life. Results We included 11 RCTs with 15 comparisons (n = 2200); five were placebo-controlled. The relative risk for mortality with haloperidol versus placebo was 0.89; 96.7% CI 0.77 to 1.03; I2 = 0% (moderate-certainty evidence) and for proportion of patients experiencing SAEs/SARs 0.94; 96.7% CI 0.81 to 1.10; I2 = 18% (low-certainty evidence). We found no difference in days alive without delirium or coma (moderate-certainty evidence). We found sparse data for other secondary outcomes and other comparators than placebo. Conclusions Haloperidol may reduce mortality and likely result in little to no change in the occurrence of SAEs/SARs compared with placebo in critically ill patients with delirium. However, the results were not statistically significant and more trial data are needed to provide higher certainty for the effects of haloperidol in these patients. Trial registration: CRD42017081133, date of registration 28 November 2017., Background: Haloperidol is frequently used in critically ill patients with delirium, but evidence for its effects has been sparse and inconclusive. By including recent trials, we updated a systematic review assessing effects of haloperidol on mortality and serious adverse events in critically ill patients with delirium. Methods: This is an updated systematic review with meta-analysis and trial sequential analysis of randomised clinical trials investigating haloperidol versus placebo or any comparator in critically ill patients with delirium. We adhered to the Cochrane handbook, the PRISMA guidelines and the grading of recommendations assessment, development and evaluation statements. The primary outcomes were all-cause mortality and proportion of patients with one or more serious adverse events or reactions (SAEs/SARs). Secondary outcomes were days alive without delirium or coma, delirium severity, cognitive function and health-related quality of life. Results: We included 11 RCTs with 15 comparisons (n = 2200); five were placebo-controlled. The relative risk for mortality with haloperidol versus placebo was 0.89; 96.7% CI 0.77 to 1.03; I 2 = 0% (moderate-certainty evidence) and for proportion of patients experiencing SAEs/SARs 0.94; 96.7% CI 0.81 to 1.10; I 2 = 18% (low-certainty evidence). We found no difference in days alive without delirium or coma (moderate-certainty evidence). We found sparse data for other secondary outcomes and other comparators than placebo. Conclusions: Haloperidol may reduce mortality and likely result in little to no change in the occurrence of SAEs/SARs compared with placebo in critically ill patients with delirium. However, the results were not statistically significant and more trial data are needed to provide higher certainty for the effects of haloperidol in these patients. Trial registration: CRD42017081133, date of registration 28 November 2017.

Published
2023

3. Handling oxygenation targets in ICU patients with COVID‐19—Protocol and statistical analysis plan in the HOT‐COVID trial

Author

Mølgaard Nielsen, Frederik, primary, Lass Klitgaard, Thomas, additional, Crescioli, Elena, additional, Rosborg Aagaard, Søren, additional, Andreasen, Anne Sofie, additional, Musaeus Poulsen, Lone, additional, Siegemund, Martin, additional, Craveiro Brøchner, Anne, additional, Bestle, Morten H., additional, Andi Iversen, Susanne, additional, Brand, Björn A., additional, Laake, Jon Henrik, additional, Grøfte, Thorbjørn, additional, Hildebrandt, Thomas, additional, Lange, Theis, additional, Perner, Anders, additional, Lilleholt Schjørring, Olav, additional, and Steen Rasmussen, Bodil, additional

Published
2021
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4. Handling oxygenation targets in ICU patients with COVID-19—Protocol and statistical analysis plan in the HOT-COVID trial

Author

Mølgaard Nielsen, Frederik, Lass Klitgaard, Thomas, Crescioli, Elena, Rosborg Aagaard, Søren, Andreasen, Anne Sofie, Musaeus Poulsen, Lone, Siegemund, Martin, Craveiro Brøchner, Anne, Bestle, Morten H., Andi Iversen, Susanne, Brand, Björn A., Laake, Jon Henrik, Grøfte, Thorbjørn, Hildebrandt, Thomas, Lange, Theis, Perner, Anders, Lilleholt Schjørring, Olav, Steen Rasmussen, Bodil, Mølgaard Nielsen, Frederik, Lass Klitgaard, Thomas, Crescioli, Elena, Rosborg Aagaard, Søren, Andreasen, Anne Sofie, Musaeus Poulsen, Lone, Siegemund, Martin, Craveiro Brøchner, Anne, Bestle, Morten H., Andi Iversen, Susanne, Brand, Björn A., Laake, Jon Henrik, Grøfte, Thorbjørn, Hildebrandt, Thomas, Lange, Theis, Perner, Anders, Lilleholt Schjørring, Olav, and Steen Rasmussen, Bodil

Published
2021

5. Higher vs lower doses of dexamethasone in patients with COVID-19 and severe hypoxia (COVID STEROID 2) trial:Protocol and statistical analysis plan

Author

Warrer Munch, Marie, Granholm, Anders, Nainan Myatra, Sheila, Kumar Tirupakuzhi Vijayaraghavan, Bharath, Cronhjort, Maria, Rubenson Wahlin, Rebecka, Jakob, Stephan M., Cioccari, Luca, Nørregaard Kjær, Maj Brit, Kingo Vesterlund, Gitte, Sylvest Meyhoff, Tine, Helleberg, Marie, Hylander Møller, Morten, Benfield, Thomas, Venkatesh, Balasubramanian, Hammond, Naomi, Micallef, Sharon, Bassi, Abhinav, John, Oommen, Jha, Vivekanand, Tjelle Kristiansen, Klaus, Suppli Ulrik, Charlotte, Lind Jørgensen, Vibeke, Smitt, Margit, Bestle, Morten H., Sofie Andreasen, Anne, Musaeus Poulsen, Lone, Steen Rasmussen, Bodil, Craveiro Brøchner, Anne, Strøm, Thomas, Møller, Anders, Saif Khan, Mohd, Padmanaban, Ajay, Vasishtha Divatia, Jigeeshu, Saseedharan, Sanjith, Borawake, Kapil, Kapadia, Farhad, Dixit, Subhal, Chawla, Rajesh, Shukla, Urvi, Amin, Pravin, Chew, Michelle S., Gluud, Christian, Lange, Theis, Perner, Anders, Warrer Munch, Marie, Granholm, Anders, Nainan Myatra, Sheila, Kumar Tirupakuzhi Vijayaraghavan, Bharath, Cronhjort, Maria, Rubenson Wahlin, Rebecka, Jakob, Stephan M., Cioccari, Luca, Nørregaard Kjær, Maj Brit, Kingo Vesterlund, Gitte, Sylvest Meyhoff, Tine, Helleberg, Marie, Hylander Møller, Morten, Benfield, Thomas, Venkatesh, Balasubramanian, Hammond, Naomi, Micallef, Sharon, Bassi, Abhinav, John, Oommen, Jha, Vivekanand, Tjelle Kristiansen, Klaus, Suppli Ulrik, Charlotte, Lind Jørgensen, Vibeke, Smitt, Margit, Bestle, Morten H., Sofie Andreasen, Anne, Musaeus Poulsen, Lone, Steen Rasmussen, Bodil, Craveiro Brøchner, Anne, Strøm, Thomas, Møller, Anders, Saif Khan, Mohd, Padmanaban, Ajay, Vasishtha Divatia, Jigeeshu, Saseedharan, Sanjith, Borawake, Kapil, Kapadia, Farhad, Dixit, Subhal, Chawla, Rajesh, Shukla, Urvi, Amin, Pravin, Chew, Michelle S., Gluud, Christian, Lange, Theis, and Perner, Anders

Abstract

Background: The coronavirus disease 2019 (COVID-19) pandemic has resulted in millions of deaths and overburdened healthcare systems worldwide. Systemic low-dose corticosteroids have proven clinical benefit in patients with severe COVID-19. Higher doses of corticosteroids are used in other inflammatory lung diseases and may offer additional clinical benefits in COVID-19. At present, the balance between benefits and harms of higher vs. lower doses of corticosteroids for patients with COVID-19 is unclear. Methods: The COVID STEROID 2 trial is an investigator-initiated, international, parallel-grouped, blinded, centrally randomised and stratified clinical trial assessing higher (12 mg) vs. lower (6 mg) doses of dexamethasone for adults with COVID-19 and severe hypoxia. We plan to enrol 1,000 patients in Denmark, Sweden, Switzerland and India. The primary outcome is days alive without life support (invasive mechanical ventilation, circulatory support or renal replacement therapy) at day 28. Secondary outcomes include serious adverse reactions at day 28; all-cause mortality at day 28, 90 and 180; days alive without life support at day 90; days alive and out of hospital at day 90; and health-related quality of life at day 180. The primary outcome will be analysed using the Kryger Jensen and Lange test adjusted for stratification variables and reported as adjusted mean differences and median differences. The full statistical analysis plan is outlined in this protocol. Discussion: The COVID STEROID 2 trial will provide evidence on the optimal dosing of systemic corticosteroids for COVID-19 patients with severe hypoxia with important implications for patients, their relatives and society.

Published
2021

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