Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia

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Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia. / Asah, Cresta; Frandsen, Rune; Ibsen, Rikke; Kjellberg, Jakob; Jennum, Poul.

I: Neuroepidemiology, Bind 55, Nr. 2, 2021, s. 141-153.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Asah, C, Frandsen, R, Ibsen, R, Kjellberg, J & Jennum, P 2021, 'Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia', Neuroepidemiology, bind 55, nr. 2, s. 141-153. https://doi.org/10.1159/000514175

APA

Asah, C., Frandsen, R., Ibsen, R., Kjellberg, J., & Jennum, P. (2021). Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia. Neuroepidemiology, 55(2), 141-153. https://doi.org/10.1159/000514175

Vancouver

Asah C, Frandsen R, Ibsen R, Kjellberg J, Jennum P. Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia. Neuroepidemiology. 2021;55(2):141-153. https://doi.org/10.1159/000514175

Author

Asah, Cresta ; Frandsen, Rune ; Ibsen, Rikke ; Kjellberg, Jakob ; Jennum, Poul. / Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia. I: Neuroepidemiology. 2021 ; Bind 55, Nr. 2. s. 141-153.

Bibtex

@article{337802edfb1940f79e2a7f6963dd2034,
title = "Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia",
abstract = "Introduction: The underlying pathophysiology of idiopathic REM sleep behavior disorder (iRBD) is not fully understood, although the condition is currently recognized as an early-stage alpha-synuclein disorder. We evaluated the morbidity, mortality, and rate of conversion to a neurodegenerative disorder in a national group of patients. Methods: All patients in Denmark with a diagnosis of RBD between 2006 and 2013 were identified from the Danish National Patient Registry (NPR) records. We excluded patients who had received a diagnosis of narcolepsy or any of the following neurodegenerative diseases before their diagnosis of RBD: Parkinson's disease, multiple system atrophy, progressive supranuclear paralysis, Alzheimer's, and Lewy body dementia. We used randomly chosen controls matched for age, gender, and municipality. Results: In total, 246 iRBD patients and 982 matched controls were analyzed. The mortality rate was the same in both groups. The morbidity rate was significantly higher in the years before and after an RBD diagnosis, due to a wide variety of disorders in the following major disease groups: mental/behavioral disorders; endocrine/metabolic diseases; diseases of the eye; diseases of the nervous, digestive, musculoskeletal, circulatory, and respiratory systems; abnormal findings not classified elsewhere; external causes; and factors influencing health status. The conversion rate from RBD to a neurodegenerative disease was 13% over the 8 years after a diagnosis of RBD. Conclusions: A diagnosis of RBD is associated with increased morbidity several years before and after a diagnosis is made. Patients have a higher risk of converting to a neurodegenerative disorder than matched controls. Mortality rates are unchanged.",
keywords = "Degenerative diseases, Morbidity, Mortality, REM sleep behavior disorder",
author = "Cresta Asah and Rune Frandsen and Rikke Ibsen and Jakob Kjellberg and Poul Jennum",
note = "Publisher Copyright: {\textcopyright} 2021 Dubai Medical Journal. All rights reserved.",
year = "2021",
doi = "10.1159/000514175",
language = "English",
volume = "55",
pages = "141--153",
journal = "Neuroepidemiology",
issn = "0251-5350",
publisher = "S Karger AG",
number = "2",

}

RIS

TY - JOUR

T1 - Morbidity, mortality, and conversion to neurodegenerative diseases in patients with REM sleep behavior disorder and REM sleep without atonia

AU - Asah, Cresta

AU - Frandsen, Rune

AU - Ibsen, Rikke

AU - Kjellberg, Jakob

AU - Jennum, Poul

N1 - Publisher Copyright: © 2021 Dubai Medical Journal. All rights reserved.

PY - 2021

Y1 - 2021

N2 - Introduction: The underlying pathophysiology of idiopathic REM sleep behavior disorder (iRBD) is not fully understood, although the condition is currently recognized as an early-stage alpha-synuclein disorder. We evaluated the morbidity, mortality, and rate of conversion to a neurodegenerative disorder in a national group of patients. Methods: All patients in Denmark with a diagnosis of RBD between 2006 and 2013 were identified from the Danish National Patient Registry (NPR) records. We excluded patients who had received a diagnosis of narcolepsy or any of the following neurodegenerative diseases before their diagnosis of RBD: Parkinson's disease, multiple system atrophy, progressive supranuclear paralysis, Alzheimer's, and Lewy body dementia. We used randomly chosen controls matched for age, gender, and municipality. Results: In total, 246 iRBD patients and 982 matched controls were analyzed. The mortality rate was the same in both groups. The morbidity rate was significantly higher in the years before and after an RBD diagnosis, due to a wide variety of disorders in the following major disease groups: mental/behavioral disorders; endocrine/metabolic diseases; diseases of the eye; diseases of the nervous, digestive, musculoskeletal, circulatory, and respiratory systems; abnormal findings not classified elsewhere; external causes; and factors influencing health status. The conversion rate from RBD to a neurodegenerative disease was 13% over the 8 years after a diagnosis of RBD. Conclusions: A diagnosis of RBD is associated with increased morbidity several years before and after a diagnosis is made. Patients have a higher risk of converting to a neurodegenerative disorder than matched controls. Mortality rates are unchanged.

AB - Introduction: The underlying pathophysiology of idiopathic REM sleep behavior disorder (iRBD) is not fully understood, although the condition is currently recognized as an early-stage alpha-synuclein disorder. We evaluated the morbidity, mortality, and rate of conversion to a neurodegenerative disorder in a national group of patients. Methods: All patients in Denmark with a diagnosis of RBD between 2006 and 2013 were identified from the Danish National Patient Registry (NPR) records. We excluded patients who had received a diagnosis of narcolepsy or any of the following neurodegenerative diseases before their diagnosis of RBD: Parkinson's disease, multiple system atrophy, progressive supranuclear paralysis, Alzheimer's, and Lewy body dementia. We used randomly chosen controls matched for age, gender, and municipality. Results: In total, 246 iRBD patients and 982 matched controls were analyzed. The mortality rate was the same in both groups. The morbidity rate was significantly higher in the years before and after an RBD diagnosis, due to a wide variety of disorders in the following major disease groups: mental/behavioral disorders; endocrine/metabolic diseases; diseases of the eye; diseases of the nervous, digestive, musculoskeletal, circulatory, and respiratory systems; abnormal findings not classified elsewhere; external causes; and factors influencing health status. The conversion rate from RBD to a neurodegenerative disease was 13% over the 8 years after a diagnosis of RBD. Conclusions: A diagnosis of RBD is associated with increased morbidity several years before and after a diagnosis is made. Patients have a higher risk of converting to a neurodegenerative disorder than matched controls. Mortality rates are unchanged.

KW - Degenerative diseases

KW - Morbidity

KW - Mortality

KW - REM sleep behavior disorder

U2 - 10.1159/000514175

DO - 10.1159/000514175

M3 - Journal article

C2 - 33780948

AN - SCOPUS:85103603350

VL - 55

SP - 141

EP - 153

JO - Neuroepidemiology

JF - Neuroepidemiology

SN - 0251-5350

IS - 2

ER -

ID: 304284827