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4. Incidence of thyroid dysfunction following initiation of amiodarone treatment in patients with and without heart failure:a nationwide cohort study

Author

Ali, Sam Aiyad, Ersbøll, Mads, Vinding, Naja Emborg, Butt, Jawad Haider, Rørth, Rasmus, Selmer, Christian, Westergaard, Lucas Malta, Mogensen, Ulrik Madvig, Weeke, Peter E., Jøns, Christian, Gustafsson, Finn, Fosbøl, Emil, Køber, Lars, Kristensen, Søren Lund, Ali, Sam Aiyad, Ersbøll, Mads, Vinding, Naja Emborg, Butt, Jawad Haider, Rørth, Rasmus, Selmer, Christian, Westergaard, Lucas Malta, Mogensen, Ulrik Madvig, Weeke, Peter E., Jøns, Christian, Gustafsson, Finn, Fosbøl, Emil, Køber, Lars, and Kristensen, Søren Lund

Abstract

Aims Thyroid dysfunction is considered the most frequent complication to amiodarone treatment, but data on its occurrence outside clinical trials are sparse. The present study aimed to examine the incidence of thyroid dysfunction following initiation of amiodarone treatment in a nationwide cohort of patients with and without heart failure (HF). Methods and results In Danish registries, we identified all patients with first-time amiodarone treatment during the period 2000–18, without prior thyroid disease or medication. The primary outcome was a composite of thyroid diagnoses and initiation of thyroid drugs. Outcomes were assessed at 1-year follow-up, and for patients free of events in the first year, in a landmark analysis for the subsequent 5 years. We included 43 724 patients with first-time amiodarone treatment, of whom 16 939 (38%) had HF. At 1-year follow-up, the cumulative incidence and adjusted hazard ratio (HR) of the primary outcome were 5.3% and 1.37 (95% confidence interval 1.25–1.50) in patients with a history of HF and 4.2% in those without HF (reference). In the 1-year landmark analysis, the subsequent 5-year cumulative incidences and adjusted HRs of the primary outcome were 5.3% (reference) in patients with 1-year accumulated dose <27.38 g [corresponding to average daily dose (ADD <75 mg)], 14.0% and HR 2.74 (2.46–3.05) for 27.38–45.63 g (ADD 75–125 mg), 20.0% and HR 4.16 (3.77–4.59) for 45.64–63.88 g (ADD 126–175 mg), and 24.5% and HR 5.30 (4.82–5.90) for >63.88 g (ADD >175 mg). Conclusion Among patients who initiated amiodarone treatment, around 5% had thyroid dysfunction at 1-year follow-up, with a slightly higher incidence in those with HF. A dose–response relationship was observed between the 1-year accumulated amiodarone dose and the subsequent 5-year cumulative incidence of thyroid dysfunction., Aims: Thyroid dysfunction is considered the most frequent complication to amiodarone treatment, but data on its occurrence outside clinical trials are sparse. The present study aimed to examine the incidence of thyroid dysfunction following initiation of amiodarone treatment in a nationwide cohort of patients with and without heart failure (HF). Methods and results: In Danish registries, we identified all patients with first-time amiodarone treatment during the period 2000-18, without prior thyroid disease or medication. The primary outcome was a composite of thyroid diagnoses and initiation of thyroid drugs. Outcomes were assessed at 1-year follow-up, and for patients free of events in the first year, in a landmark analysis for the subsequent 5 years. We included 43 724 patients with first-time amiodarone treatment, of whom 16 939 (38%) had HF. At 1-year follow-up, the cumulative incidence and adjusted hazard ratio (HR) of the primary outcome were 5.3% and 1.37 (95% confidence interval 1.25-1.50) in patients with a history of HF and 4.2% in those without HF (reference). In the 1-year landmark analysis, the subsequent 5-year cumulative incidences and adjusted HRs of the primary outcome were 5.3% (reference) in patients with 1-year accumulated dose <27.38 g [corresponding to average daily dose (ADD <75 mg)], 14.0% and HR 2.74 (2.46-3.05) for 27.38-45.63 g (ADD 75-125 mg), 20.0% and HR 4.16 (3.77-4.59) for 45.64-63.88 g (ADD 126-175 mg), and 24.5% and HR 5.30 (4.82-5.90) for >63.88 g (ADD >175 mg). Conclusion: Among patients who initiated amiodarone treatment, around 5% had thyroid dysfunction at 1-year follow-up, with a slightly higher incidence in those with HF. A dose-response relationship was observed between the 1-year accumulated amiodarone dose and the subsequent 5-year cumulative incidence of thyroid dysfunction.

Published
2023

5. Ventricular rate in atrial fibrillation and the risk of heart failure and death

Author

Westergaard, Lucas Malta, Alhakak, Amna, Rørth, Rasmus, Fosbøl, Emil L., Kristensen, Søren L., Svendsen, Jesper H., Graff, Claus, Nielsen, Jonas B., Gislason, Gunnar H., Kober, Lars, Torp-Pedersen, Christian, Lee, Christina J. Y., Weeke, Peter E., Westergaard, Lucas Malta, Alhakak, Amna, Rørth, Rasmus, Fosbøl, Emil L., Kristensen, Søren L., Svendsen, Jesper H., Graff, Claus, Nielsen, Jonas B., Gislason, Gunnar H., Kober, Lars, Torp-Pedersen, Christian, Lee, Christina J. Y., and Weeke, Peter E.

Abstract

Aims While clinical trials have suggested that a high ventricular rate is associated with increased risk of heart failure (HF) and mortality, all-comers studies are warranted. Objective To assess 1-year risk of new-onset diagnosed HF and all-cause mortality among rate-control treated patients presenting with atrial fibrillation (AF) on an electrocardiogram (ECG) according to ventricular rate. Methods and results ECGs recorded at the Copenhagen General Practitioners Laboratory (2001–15) were used to identify patients with AF. Multivariate Cox proportional hazard regression models were used to compare risk of new-onset HF and all-cause mortality after first ECG presenting with AF according to ventricular rate on ECG [<60, 60–79, 80–99, and 100–110, > 110 beats per minute (bpm)]. We identified 7408 patients in treatment with rate control drugs at time of first ECG presenting with AF [median age 78 years (Q1,Q3 = 70–85 years)], 45.8% male, median ventricular rate 83 bpm, (Q1,Q3 = 71–101 bpm)]. During 1-year follow-up, 666 (9.0%) of all patients with AF developed HF and 858 (11.6%) died. Patients with AF ventricular rates 100–110 bpm and >110 bpm had a hazard ratio (HR) of 1.46 (CI: 1.10–1.95) and 2.41 (CI: 1.94–3.00) respectively for new-onset HF, compared with 60–79 bpm. Similarly, patients with AF ventricular rates 100–110 bpm and >110 bpm had a HR of 1.44 (CI: 1.13–1.82) and 1.34 (CI: 1.08–1.65) respectively for all-cause mortality, compared with 60–79 bpm. Conclusions Ventricular rates ≥100 bpm among patients presenting with AF on ECG in treatment with rate control drugs were associated with greater risk of both new-onset HF and all-cause mortality., Aims While clinical trials have suggested that a high ventricular rate is associated with increased risk of heart failure (HF) and mortality, all-comers studies are warranted. Objective To assess 1-year risk of new-onset diagnosed HF and all-cause mortality among rate-control treated patients presenting with atrial fibrillation (AF) on an electrocardiogram (ECG) according to ventricular rate. Methods and results ECGs recorded at the Copenhagen General Practitioners Laboratory (2001-15) were used to identify patients with AF. Multivariate Cox proportional hazard regression models were used to compare risk of new-onset HF and all-cause mortality after first ECG presenting with AF according to ventricular rate on ECG [ 110 beats per minute (bpm)]. We identified 7408 patients in treatment with rate control drugs at time of first ECG presenting with AF [median age 78 years (Q1,Q3 = 70-85 years)], 45.8% male, median ventricular rate 83 bpm, (Q1,Q3 = 71-101 bpm)]. During 1-year follow-up, 666 (9.0%) of all patients with AF developed HF and 858 (11.6%) died. Patients with AF ventricular rates 100-110 bpm and >110 bpm had a hazard ratio (HR) of 1.46 (CI: 1.10-1.95) and 2.41 (CI: 1.94-3.00) respectively for new-onset HF, compared with 60-79 bpm. Similarly, patients with AF ventricular rates 100-110 bpm and >110 bpm had a HR of 1.44 (CI: 1.13-1.82) and 1.34 (CI: 1.08-1.65) respectively for all-cause mortality, compared with 60-79 bpm. Conclusions Ventricular rates >= 100 bpm among patients presenting with AF on ECG in treatment with rate control drugs were associated with greater risk of both new-onset HF and all-cause mortality.

Published
2023

6. Ventricular rate in atrial fibrillation and the risk of heart failure and death

Author

Westergaard, Lucas Malta, primary, Alhakak, Amna, additional, Rørth, Rasmus, additional, Fosbøl, Emil L, additional, Kristensen, Søren L, additional, Svendsen, Jesper H, additional, Graff, Claus, additional, Nielsen, Jonas B, additional, Gislason, Gunnar H, additional, Køber, Lars, additional, Torp-Pedersen, Christian, additional, Lee, Christina J Y, additional, and Weeke, Peter E, additional

Published
2023
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7. Incidence of thyroid dysfunction following initiation of amiodarone treatment in patients with and without heart failure: a nationwide cohort study

Author

Ali, Sam Aiyad, primary, Ersbøll, Mads, additional, Vinding, Naja Emborg, additional, Butt, Jawad Haider, additional, Rørth, Rasmus, additional, Selmer, Christian, additional, Westergaard, Lucas Malta, additional, Mogensen, Ulrik Madvig, additional, Weeke, Peter E, additional, Jøns, Christian, additional, Gustafsson, Finn, additional, Fosbøl, Emil, additional, Køber, Lars, additional, and Kristensen, Søren Lund, additional

Published
2022
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8. Severity of congenital long QT syndrome disease manifestation and risk of depression, anxiety, and mortality:a nationwide study

Author

Krøll, Johanna, Jensen, Henrik K., Jespersen, Camilla, Kanters, Jørgen K, Hansen, Michael Skov, Christiansen, Michael, Westergaard, Lucas Malta, Fosbøl, Emil L, Rørth, Rasmus, Torp-Pedersen, Christian, Køber, Lars, Bundgaard, Henning, Tfelt-Hansen, Jacob, Weeke, Peter E, Krøll, Johanna, Jensen, Henrik K., Jespersen, Camilla, Kanters, Jørgen K, Hansen, Michael Skov, Christiansen, Michael, Westergaard, Lucas Malta, Fosbøl, Emil L, Rørth, Rasmus, Torp-Pedersen, Christian, Køber, Lars, Bundgaard, Henning, Tfelt-Hansen, Jacob, and Weeke, Peter E

Abstract

AIMS: We examined if a congenital long QT syndrome (cLQTS) diagnosis and severity of cLQTS disease manifestation was associated with increased risk of depression, anxiety, and all-cause mortality.METHODS AND RESULTS: All patients with known cLQTS in Denmark were identified using nationwide registries and specialized inherited cardiac disease clinics (1994-2016) and followed for up to 3 years after their cLQTS diagnosis. Risk factors for depression, anxiety, and all-cause mortality were determined using multivariable Cox proportional-hazards regression. An age- and sex-matched control population was identified (matching 1:4). Overall, 589 patients with cLQTS were identified of which 119/589 (20.2%) developed depression or anxiety during follow-up compared with 302/2356 (12.8%) from the control population (P < 0.001). Severity of cLQTS disease manifestation was identified for 324/589 (55%) of patients with cLQTS; 162 were asymptomatic, 119 had ventricular tachycardia (VT)/syncope, and 43 had aborted sudden cardiac death (aSCD). In multivariable models, patients with aSCD, VT/syncope, or unspecified cLQTS disease manifestation had a higher risk of developing depression or anxiety compared with the control population (hazard ratio [HR]=2.4, 95% confidence interval [CI]: 1.1-5.1; HR = 1.9, 95% CI: 1.2-3.0; HR = 1.6, 95% CI: 1.1-2.3, respectively). Asymptomatic patients had similar risk of developing depression or anxiety as the control population (HR = 1.2, 95% CI: 0.8-1.9). During follow-up, 10/589 (1.7%) patients with cLQTS died compared with 27/2356 (1.1%) from the control population (P = 0.5). Furthermore, 4/10 who died had developed depression or anxiety.CONCLUSION: A severe cLQTS disease manifestation was associated with a greater risk of depression or anxiety. All-cause mortality for patients with cLQTS was low.

Published
2022

9. Incidence of thyroid dysfunction following initiation of amiodarone treatment in patients with and without heart failure: a nationwide cohort study.

Author

Ali, Sam Aiyad, Ersbøll, Mads, Vinding, Naja Emborg, Butt, Jawad Haider, Rørth, Rasmus, Selmer, Christian, Westergaard, Lucas Malta, Mogensen, Ulrik Madvig, Weeke, Peter E, Jøns, Christian, Gustafsson, Finn, Fosbøl, Emil, Køber, Lars, and Kristensen, Søren Lund

Abstract

Aims Thyroid dysfunction is considered the most frequent complication to amiodarone treatment, but data on its occurrence outside clinical trials are sparse. The present study aimed to examine the incidence of thyroid dysfunction following initiation of amiodarone treatment in a nationwide cohort of patients with and without heart failure (HF). Methods and results In Danish registries, we identified all patients with first-time amiodarone treatment during the period 2000–18, without prior thyroid disease or medication. The primary outcome was a composite of thyroid diagnoses and initiation of thyroid drugs. Outcomes were assessed at 1-year follow-up, and for patients free of events in the first year, in a landmark analysis for the subsequent 5 years. We included 43 724 patients with first-time amiodarone treatment, of whom 16 939 (38%) had HF. At 1-year follow-up, the cumulative incidence and adjusted hazard ratio (HR) of the primary outcome were 5.3% and 1.37 (95% confidence interval 1.25–1.50) in patients with a history of HF and 4.2% in those without HF (reference). In the 1-year landmark analysis, the subsequent 5-year cumulative incidences and adjusted HRs of the primary outcome were 5.3% (reference) in patients with 1-year accumulated dose <27.38 g [corresponding to average daily dose (ADD <75 mg)], 14.0% and HR 2.74 (2.46–3.05) for 27.38–45.63 g (ADD 75–125 mg), 20.0% and HR 4.16 (3.77–4.59) for 45.64–63.88 g (ADD 126–175 mg), and 24.5% and HR 5.30 (4.82–5.90) for >63.88 g (ADD >175 mg). Conclusion Among patients who initiated amiodarone treatment, around 5% had thyroid dysfunction at 1-year follow-up, with a slightly higher incidence in those with HF. A dose–response relationship was observed between the 1-year accumulated amiodarone dose and the subsequent 5-year cumulative incidence of thyroid dysfunction. [ABSTRACT FROM AUTHOR]

Published
2023
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10. Severity of congenital long QT syndrome disease manifestation and risk of depression, anxiety, and mortality: a nationwide study

Author

Krøll, Johanna, primary, Jensen, Henrik K, additional, Jespersen, Camilla, additional, Kanters, Jørgen K, additional, Hansen, Michael Skov, additional, Christiansen, Michael, additional, Westergaard, Lucas Malta, additional, Fosbøl, Emil L, additional, Rørth, Rasmus, additional, Torp-Pedersen, Christian, additional, Køber, Lars, additional, Bundgaard, Henning, additional, Tfelt-Hansen, Jacob, additional, and Weeke, Peter E, additional

Published
2021
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11. Additional file 1 of Incidence of heart valve disease in women treated with the ergot-derived dopamine agonist bromocriptine

Author

Clausen, Marianne F., R��rth, Rasmus, Torp-Pedersen, Christian, Westergaard, Lucas Malta, Weeke, Peter E., Gislason, Gunnar, K��ber, Lars, Fosb��l, Emil, and Kristensen, S��ren Lund

Subjects
digestive system, digestive system diseases
Abstract

Additional file 1. Supplementary Appendix. Supplementary Table 1: Baseline characteristics for bromocriptine treated patients and controls matched on age, sex, major comorbidity and pharmacotherapy. Supplementary Appendix Table 2: ICD-10 and -8 codes used to identify in and outpatient diagnoses, and procedure codes according to the Nordic Medico-Statistical Committee nomenclature. Supplementary appendix Table 3: ATC codes for evaluated pharmacotherapy.

Published
2021
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13. Severity of congenital long QT syndrome disease manifestation and risk of depression, anxiety, and mortality: a nationwide study.

Author

Krøll, Johanna, Jensen, Henrik K, Jespersen, Camilla, Kanters, Jørgen K, Hansen, Michael Skov, Christiansen, Michael, Westergaard, Lucas Malta, Fosbøl, Emil L, Rørth, Rasmus, Torp-Pedersen, Christian, Køber, Lars, Bundgaard, Henning, Tfelt-Hansen, Jacob, and Weeke, Peter E

Abstract

Aims: We examined if a congenital long QT syndrome (cLQTS) diagnosis and severity of cLQTS disease manifestation was associated with increased risk of depression, anxiety, and all-cause mortality.Methods and Results: All patients with known cLQTS in Denmark were identified using nationwide registries and specialized inherited cardiac disease clinics (1994-2016) and followed for up to 3 years after their cLQTS diagnosis. Risk factors for depression, anxiety, and all-cause mortality were determined using multivariable Cox proportional-hazards regression. An age- and sex-matched control population was identified (matching 1:4). Overall, 589 patients with cLQTS were identified of which 119/589 (20.2%) developed depression or anxiety during follow-up compared with 302/2356 (12.8%) from the control population (P < 0.001). Severity of cLQTS disease manifestation was identified for 324/589 (55%) of patients with cLQTS; 162 were asymptomatic, 119 had ventricular tachycardia (VT)/syncope, and 43 had aborted sudden cardiac death (aSCD). In multivariable models, patients with aSCD, VT/syncope, or unspecified cLQTS disease manifestation had a higher risk of developing depression or anxiety compared with the control population (hazard ratio [HR]=2.4, 95% confidence interval [CI]: 1.1-5.1; HR = 1.9, 95% CI: 1.2-3.0; HR = 1.6, 95% CI: 1.1-2.3, respectively). Asymptomatic patients had similar risk of developing depression or anxiety as the control population (HR = 1.2, 95% CI: 0.8-1.9). During follow-up, 10/589 (1.7%) patients with cLQTS died compared with 27/2356 (1.1%) from the control population (P = 0.5). Furthermore, 4/10 who died had developed depression or anxiety.Conclusion: A severe cLQTS disease manifestation was associated with a greater risk of depression or anxiety. All-cause mortality for patients with cLQTS was low. [ABSTRACT FROM AUTHOR]

Published
2022
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14. Incidence of thyroid dysfunction following initiation of amiodarone treatment in patients with and without heart failure: a nationwide cohort study.

Author

Ali SA, Ersbøll M, Vinding NE, Butt JH, Rørth R, Selmer C, Westergaard LM, Mogensen UM, Weeke PE, Jøns C, Gustafsson F, Fosbøl E, Køber L, and Kristensen SL

Subjects
Humans, Incidence, Cohort Studies, Anti-Arrhythmia Agents adverse effects, Amiodarone adverse effects, Hypothyroidism diagnosis, Thyroid Diseases chemically induced, Thyroid Diseases diagnosis, Thyroid Diseases epidemiology, Heart Failure diagnosis, Heart Failure epidemiology
Abstract

Aims: Thyroid dysfunction is considered the most frequent complication to amiodarone treatment, but data on its occurrence outside clinical trials are sparse. The present study aimed to examine the incidence of thyroid dysfunction following initiation of amiodarone treatment in a nationwide cohort of patients with and without heart failure (HF)., Methods and Results: In Danish registries, we identified all patients with first-time amiodarone treatment during the period 2000-18, without prior thyroid disease or medication. The primary outcome was a composite of thyroid diagnoses and initiation of thyroid drugs. Outcomes were assessed at 1-year follow-up, and for patients free of events in the first year, in a landmark analysis for the subsequent 5 years. We included 43 724 patients with first-time amiodarone treatment, of whom 16 939 (38%) had HF. At 1-year follow-up, the cumulative incidence and adjusted hazard ratio (HR) of the primary outcome were 5.3% and 1.37 (95% confidence interval 1.25-1.50) in patients with a history of HF and 4.2% in those without HF (reference). In the 1-year landmark analysis, the subsequent 5-year cumulative incidences and adjusted HRs of the primary outcome were 5.3% (reference) in patients with 1-year accumulated dose <27.38 g [corresponding to average daily dose (ADD <75 mg)], 14.0% and HR 2.74 (2.46-3.05) for 27.38-45.63 g (ADD 75-125 mg), 20.0% and HR 4.16 (3.77-4.59) for 45.64-63.88 g (ADD 126-175 mg), and 24.5% and HR 5.30 (4.82-5.90) for >63.88 g (ADD >175 mg)., Conclusion: Among patients who initiated amiodarone treatment, around 5% had thyroid dysfunction at 1-year follow-up, with a slightly higher incidence in those with HF. A dose-response relationship was observed between the 1-year accumulated amiodarone dose and the subsequent 5-year cumulative incidence of thyroid dysfunction., Competing Interests: Conflict of interest: J.H.B. received advisory board honoraria from Bayer, unrelated to the submitted work. E.F. received an independent research grant from Novo Nordisk Foundation, unrelated to the submitted work. L.K. received speaker’s honoraria from Novo, Novartis, AstraZeneca, and Boehringer, unrelated to the submitted work. S.L.K. received a speaker’s honoraria from Astra Zeneca outside of the submitted work. All remaining authors have declared no conflicts of interest., (© The Author(s) 2022. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published
2023
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15. Severity of congenital long QT syndrome disease manifestation and risk of depression, anxiety, and mortality: a nationwide study.

Author

Krøll J, Jensen HK, Jespersen C, Kanters JK, Hansen MS, Christiansen M, Westergaard LM, Fosbøl EL, Rørth R, Torp-Pedersen C, Køber L, Bundgaard H, Tfelt-Hansen J, and Weeke PE

Subjects
Anxiety diagnosis, Anxiety epidemiology, Arrhythmias, Cardiac complications, Humans, Risk Factors, Syncope, Depression diagnosis, Depression epidemiology, Long QT Syndrome complications, Long QT Syndrome diagnosis, Long QT Syndrome epidemiology
Abstract

Aims: We examined if a congenital long QT syndrome (cLQTS) diagnosis and severity of cLQTS disease manifestation was associated with increased risk of depression, anxiety, and all-cause mortality., Methods and Results: All patients with known cLQTS in Denmark were identified using nationwide registries and specialized inherited cardiac disease clinics (1994-2016) and followed for up to 3 years after their cLQTS diagnosis. Risk factors for depression, anxiety, and all-cause mortality were determined using multivariable Cox proportional-hazards regression. An age- and sex-matched control population was identified (matching 1:4). Overall, 589 patients with cLQTS were identified of which 119/589 (20.2%) developed depression or anxiety during follow-up compared with 302/2356 (12.8%) from the control population (P < 0.001). Severity of cLQTS disease manifestation was identified for 324/589 (55%) of patients with cLQTS; 162 were asymptomatic, 119 had ventricular tachycardia (VT)/syncope, and 43 had aborted sudden cardiac death (aSCD). In multivariable models, patients with aSCD, VT/syncope, or unspecified cLQTS disease manifestation had a higher risk of developing depression or anxiety compared with the control population (hazard ratio [HR]=2.4, 95% confidence interval [CI]: 1.1-5.1; HR = 1.9, 95% CI: 1.2-3.0; HR = 1.6, 95% CI: 1.1-2.3, respectively). Asymptomatic patients had similar risk of developing depression or anxiety as the control population (HR = 1.2, 95% CI: 0.8-1.9). During follow-up, 10/589 (1.7%) patients with cLQTS died compared with 27/2356 (1.1%) from the control population (P = 0.5). Furthermore, 4/10 who died had developed depression or anxiety., Conclusion: A severe cLQTS disease manifestation was associated with a greater risk of depression or anxiety. All-cause mortality for patients with cLQTS was low., (Published on behalf of the European Society of Cardiology. All rights reserved. © The Author(s) 2021. For permissions, please email: journals.permissions@oup.com.)

Published
2022
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