More Than Rapid Eye Movement Sleep Behavior Disorder: Sleep Differences in Parkinson’s Disease LRRK2 and GBA Genotypes

Objectives: Sleep disorders can significantly worsen the quality of life in Parkinson’s disease (PD). Variants in LRRK2 and GBA1, the most common genetic contributors to PD, may lead to different clinical features, including more REM sleep behavior disorder (RBD) in PD associated with GBA1 mutations...

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Published inJournal of sleep medicine Vol. 22; no. 2; pp. 82 - 90
Main Authors Wise, Adina, Raymond, Deborah, Yang, Mengxi, Astefanous, Amy, Cohen, Abby, Beltre, Melba, Young, Casey, Plitnick, Barbara, Bressman, Susan B., Figueiro, Mariana G., Saunders-Pullman, Rachel
Format Journal Article
LanguageEnglish
Published 대한수면연구학회 01.08.2025
Subjects
정신과학
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ISSN2384-2423
2384-2431
DOI10.13078/jsm.250016

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Summary:Objectives: Sleep disorders can significantly worsen the quality of life in Parkinson’s disease (PD). Variants in LRRK2 and GBA1, the most common genetic contributors to PD, may lead to different clinical features, including more REM sleep behavior disorder (RBD) in PD associated with GBA1 mutations (GBA PD). However, there is a dearth of information about differences in non-RBD sleep disorders among these genetic subgroups. Methods: Seventy-nine participants with PD (18 LRRK2 G2019S carriers with PD [LRRK2 PD], 22 GBA1 [GBA PD], 2 LRRK2 GBA PD and 37 idiopathic PD [iPD]) underwent actigraphy (Actiwatch-2) for 1 week. Subjective sleep quality was assessed using questionnaires. Results: LRRK2 PD participants demonstrated better sleep actigraphy, including reduced wake after sleep onset (-25 minutes; p<0.001) and higher sleep efficiency (6.3%; p=0.015), than iPD and GBA PD in models adjusted for age, age at disease onset, and gender. While sleep onset times did not differ between groups, all groups had mean sleep onset times after 11:00 PM, and did not demonstrate phase advancement. Sleep questionnaires showed only an increased prevalence of RBD in GBA PD and iPD. Conclusions: LRRK2 PD is associated with less fragmented sleep than GBA PD and iPD, suggesting that despite similar objective sleep complaints, genotypic sleep differences extend beyond RBD. These differences support the need for personalized and genotypic approaches to sleep disturbances in PD. The absence of phase advancement in all groups suggests that lighting interventions to improve sleep disorders should be considered for the morning rather than later in the day.
ISSN:2384-2423
2384-2431
DOI:10.13078/jsm.250016