Familial Aggregation and Biomarkers in REM Sleep Behaviour Disorder.

Overview

In this cohort study, the investigators aim to study the familial aggregation of REM sleep behavior disorder (RBD) and compare the differences in major biomarkers of neurodegeneration, including percentage of EMG activity during REM sleep, cognitive functions, autonomic dysfunction, and psychiatric disorders, between unaffected first degree relatives of RBD cases and non-RBD controls.

Full Title of Study: “Familial Aggregation and Biomarkers in REM Sleep Behaviour Disorder: a Case-control Family Study”

Study Type

  • Study Type: Observational
  • Study Design
    • Time Perspective: Cross-Sectional
  • Study Primary Completion Date: September 30, 2022

Detailed Description

REM sleep behavior disorder (RBD) is a parasomnia characterized by abnormal behavioral manifestations during REM sleep. Previous case-control studies and prospective studies have documented the progression of α-synucleinopathy neurodegeneration in relation to RBD and have identified some biomarkers of predicting neurodegeneration in patients with iRBD, such as olfactory dysfunction, color vision deficit, autonomic dysfunction, tonic EMG activity during REM sleep, and psychiatric disorder. However, these biomarkers might precede the onset of RBD, as a result, searching for biomarkers for the neurodegeneration before RBD onset is helpful to map the progression of neurodegeneration. In this regard, the investigators aim to study the familial aggregation of RBD and its core features, and compare the differences in major biomarkers of neurodegeneration, including percentage of EMG activity during REM sleep, cognitive functions, autonomic dysfunction, and psychiatric disorders, between unaffected first degree relatives of RBD cases and non-RBD controls.

Arms, Groups and Cohorts

  • FDRs of RBD cases
    • FDRs of RBD cases. The diagnosis of RBD is based on ICSD-II criteria, as confirmed by v-PSG and with the aid of REM sleep behaviour disorder questionnaire (RBDQ-HK). RBD cases which are secondary to narcolepsy, neurodegenerative diseases or other neurological diseases are excluded.
  • FDRs of non-RBD controls
    • FDRs of non-RBD controls. Non-RBD control probands are free of narcolepsy, significant clinical RBD symptoms and other neurological diseases.

Clinical Trial Outcome Measures

Primary Measures

  • The prevalence rate of probable RBD among first degree relatives of RBD probands
    • Time Frame: 15 minutes
    • The prevalence rate of probable RBD based on the self-reported/proxy-reported RBD symptoms in RBDQ-HK among first degree relatives of RBD probands in comparison to that of first degree relatives of controls.
  • The weighted prevalence rate of confirmed RBD among first degree relatives of RBD probands.
    • Time Frame: one night (8 hours)
    • The weighted prevalence rate of first degree relatives meeting full ICSD-II2 diagnostic criteria for RBD confirmed by clinical history and vPSG.

Secondary Measures

  • The percentage of REM-related EMG activity (REMREEA)
    • Time Frame: one night (8 hours)
    • The percentage of REM-related EMG activity (REMREEA) is the most reliable and valid marker in differentiating patients with RBD from normal controls. Basically, the REMREEA include two components, namely phasic EMG activity and tonic EMG activity, respectively. The phasic EMG events were defined as any burst of EMG activity lasting 0.1 to 5 sec with amplitude > 4 times the background EMG activity and will be score on the basis of 3-second mini-epoch during REM sleep. Each 30-sec epoch during REM sleep was scored as tonic or atonic depending on whether tonic chin EMG activity was present for more or less than 50% of the epoch. The total EMG activity was presented as the percentage of REM related EMG activity (REMREEA) with the percentage of tonic EMG activity plus the percentage of phasic EMG activity.
  • Significant motor activity
    • Time Frame: one night (8 hours)
    • Significant motor activity were recorded by video-polysomnography. The motor analysis will be scored according to the previously established method. In view of the potential problem in inter-rater reliability in those mild motor activities, we will only include those complex activities and vocalizations in the analyses. It has been shown that there are large differences in the significant motor activities between patients with RBD and normal controls. In view of the relatively high night-to-night variability and low inter-rater reliability in scoring motor activity, it will be considered as secondary outcome.
  • Other biomarkers of RBD in the first degree relatives of RBD patients.
    • Time Frame: 2 hours
    • Previous studies have also confirmed that RBD patients present with autonomic dysfunction, olfactory dysfunction, color vision deficit, neurocognitive function, and a higher rate of psychiatric disorders, these markers will also be considered as secondary biomarkers and will be compared in the first degree relatives of between patients and controls.

Participating in This Clinical Trial

Inclusion Criteria

1. Chinese aged 40 or above; 2. Being capable of giving informed consent for participation of the study; 3. Sex matched between relatives from probands and controls. Exclusion Criteria:

1. Aged 39 or below; 2. Not capable of giving informed consent for participation of the study

Gender Eligibility: All

Minimum Age: 40 Years

Maximum Age: N/A

Are Healthy Volunteers Accepted: Accepts Healthy Volunteers

Investigator Details

  • Lead Sponsor
    • Chinese University of Hong Kong
  • Provider of Information About this Clinical Study
    • Principal Investigator: Dr. Zhang Jihui, Assistant professor – Chinese University of Hong Kong
  • Overall Official(s)
    • Jihui Zhang, PhD, Principal Investigator, Chinese University of Hong Kong
    • Yun Kwok Wing, MBChB, Study Director, Chinese University of Hong Kong
    • Siuping LAM, Study Director, Chinese University of Hong Kong
    • Vicent Chung-tong MOK, Study Director, Chinese University of Hong Kong
  • Overall Contact(s)
    • Jihui Zhang, PhD, (852) 39197647, jihui.zhang@cuhk.edu.hk

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