Restless Legs Syndrome Clinical Trial
Official title:
Effects of Gabapentin Enacarbil on Intensity of Cortical Arousal, Heart Rate, Blood Pressure and Anterior Tibialis EMG Responses Associated With PLMs During Sleep in Patients With RLS Using a Novel Computer Assisted Scoring System
This is a phase IV single-blind, placebo run-in fixed dose single-group study to assess objective and subjective effects of GEn on sleep EEG, BP, and anterior tibialis EMG responsivity in patients with RLS. The study will include 8 visits over a period of up to 8 weeks for eligible subjects including a 1 to 3-week Screening/Washout Period, a 1-week placebo run-in period, and a 4-week Treatment Period.The first placebo dose will be administered within 1 to 3 weeks after Screening/Washout. The total duration of the study from the first subject enrolled to the last subject completed will be approximately 1 year.
Evidence from the Sleep Heart Health Study suggests that nocturnal arousals from sleep
impact heart rate variability and sleep disorders associated with frequent nocturnal
arousals, including restless legs syndrome (RLS), increase the risks of developing
cardiovascular disease. The majority of RLS patients, once asleep, exhibit frequent periodic
limb movements (PLMs), which cause electroencephalographic (EEG) arousals and sleep
fragmentation resulting in poor quality of sleep and daytime consequences. PLMs are also
reported to increase heart rate.The precise nature of the relationship between PLMs and
their impact on heart rate and blood pressure is not clear. This may relate to the fact that
PLMs are scored as either present or absent and without accounting for the differences in
intensity of muscle activity during individual PLMs and intensity of associated arousals. In
fact PLMs have been reported to vary from barely visible to very intense changes in the
anterior tibialis electromyogram (EMG). This study will evaluate the effects of gabapentin
encarbil (GEn) on intensity of cortical arousals associated with PLMs using a newly
developed computer assisted scoring system which allows for scaling microarousals in the
EEG. The anterior tibialis EMG intensity, continuous blood pressure and heart rate will be
measured.
The study design is a phase IV single center, single blind, placebo run-in fixed dose single
group study in twenty subjects with moderate to severe restless leg syndrome. It includes a
one- three week screening washout period, one week of placebo run-in and four- week
treatment period with GEn 600 mg once daily. Subjects will be instructed to take their study
medication once daily with food in the evening at approximately 5 PM. If the dose is not
taken at the recommended time, the next dose should be taken the following day at the
regularly scheduled time (about 5 PM the next evening). Subjects will be blinded to
treatment (placebo versus active drug).
Polysomnography (PSG) will be obtained for two nights of baseline at the end of placebo
run-in and at the end of four weeks of treatment with gabapentin encarbil 600 mg. Medical
history and cardiovascular risk factors will be assessed at Screening. RLS disease history,
previous/current RLS therapy, augmentation history and evidence of sleep disturbance will be
obtained.Severity of RLS will be determined using the International Restless Legs Syndrome
(IRLS) scale. The Berlin questionnaire will be used to identify the risk (low to high) of
sleep disordered breathing. The Beck Depression Inventory (BDI-II) will be administered to
identify depression and its severity at Screening. Electrocardiogram (ECG), clinical
laboratory test and urine pregnancy test will be conducted at Screening to determine
eligibility. Also to determine eligibility, subjective evidence of sleep disturbance will be
assessed per daily sleep diary at Visit 2. A physical exam will be performed at the
beginning of the Placebo Run-in Period.
The visit schedule includes: Screening; Scheduled Tests/Exams; Placebo administration visit;
Baseline PSG visits; Baseline Visit; End of treatment PSG visits; Adverse Event Evaluation
(for all subjects);Unscheduled clinical evaluation visit; and End of Study Visit.
Primary outcome will involve change from baseline (end of run-in period) in cortical arousal
intensity associated with PLMs for subjects treated with Gen 600 mg QD for 4 weeks. PSG
studies will be recorded for 8 hours using standard techniques described by R&K. Cortical
EEG arousals will be scored using wavelet analysis of C3/A2 and C4/A1 EEG signals. Arousals
scored in NREM sleep will be assigned a score from 0-9. This arousal scaling is entirely
subjective. Wavelet analysis will be performed on each of the scaled arousals using wavelet
features that correlate with arousal intensity. The arousal intensity will be measured using
Wavelet Transform which is superior for analyzing signals such as EEG.
Beat to beat heart rate measurement will identify the highest value in the interval 2-12
seconds preceding each arousal which will be used as a baseline heart rate. The highest
heart rate in the interval between arousal and at 8 seconds after its end, and the
difference from baseline will represent the change in heart rate associated with the
arousal.
Blood pressure changes will be identified using the same technique as the heart rate
changes. Continuous blood pressure will be monitored using Somnotouch RESP. Using the 2-12
seconds preceding each arousal, any identified change between onset of arousal and at 8
seconds after its end will represent the change in blood pressure.
PLM intensity will be derived by measuring the highest anterior tibialis EMG amplitude
during the 2-12 seconds prior to arousal onset and comparing to maximum EMG amplitude during
PLMs with or without associated arousal.
The Rechtschaffen and Kales (R&K) standard PSG parameters include: TST (total sleep time),
WASO (wake after sleep onset), LPS10 (latency to persistent sleep), SE (sleep efficiency),
Awakenings Index (number of awakenings per hour of sleep), AI (arousals index), sleep stage
percentages, PLMI (periodic limb movements per hour), and PLMAI (periodic limb movements
associated with arousal per hour).
The secondary subjective efficacy endpoints are: 1) the mean change from Baseline to the end
of the Treatment Period in International Restless Legs Syndrome (IRLS) Rating Scale total
score, (2) proportion of responders ("much"/ "very much" improved) on the investigator-rated
Clinical Global Impression-Improvement (CGI-I) scale, and proportion of responders
("moderately better" to "a great deal better") on the Patient Global Impression of Change
(PGIC) scale (4) the mean change from baseline to the end of the Treatment Period in PSQ,
SSQ items, RLSQoL, RLS-NDI and ESS scores
The IRLSSG has developed and validated a 10-item scale for assessing the severity of RLS.
The IRLS Rating scale will be assessed at the screening visit, the placebo initiation visit,
the baseline visit and end of study visit (and at the ET visit for subjects who withdraw
prematurely). The investigator-rated CGI-I will be recorded at Baseline (end of placebo
administration) and at the end of the Treatment Period and at the ET visit, if applicable.
The PSQ is a self-rated questionnaire which assesses sleep quality and sleep disturbances
over a one month time interval. The RLSQoL is an 18-item scale that assesses the impact of
RLS on daily life, emotional wellbeing, social life, and work life. The ESS is an assessment
used to measure average longtime sleepiness whereby subjects self-rate questions on how
likely they are to fall asleep in eight different situations. The PSQ, RLSQoL and ESS will
be recorded at Baseline and at the end of the Treatment Period and at the ET visit, if
applicable.
The SSQ is a daily sleep diary where subjects record their sleep activities and report the
quality of their sleep over the past 24 hours on an 11 point numeric rating scale ranging
from 0 ("very poor") to 10 ("excellent"). The RLS-NDI measures the impacts of RLS on next
day functioning. The impacts include activities of daily living (i.e., work, household
chores), cognitive functioning (i.e., concentration, forgetfulness, mental tiredness,
alertness), emotional functioning (i.e., irritability, depressed mood), physical functioning
(i.e., physical tiredness, active leisure activities), energy, daytime sleepiness, and
social functioning (i.e., relationships, social activities/situations). The final measure
consists of 14 items assessed "today" and rated on a numeric rating scale. Subjects will be
instructed to complete the daily diary and the RLS-NDI over the 7 days preceding Visit 4
(PSG 2 visit) and Visit 7 (PSG 4 visit).
The following safety assessments will be performed during this study:
Physical examination, including height as with other screening only measurements; Weight
measurements;Vital sign measurements, including blood pressure and pulse rate;Pregnancy
testing; AE reporting;ECG (for screening only); Laboratory safety tests (at screening)
The primary efficacy endpoint is the reduction from placebo-baseline in cortical arousal
intensity associated with PLMs after treatment with GEn. A sample size of 20 subjects is
estimated by a priori power analysis (G*Power 3.1.9.2) to achieve 92% power for a 2-sided 5%
paired t-test with an effect size of 0.80. The primary efficacy analysis will be performed
on the per-protocol population who completed the study taking 600 mg GEn/day of the study
drug. For subjects who prematurely withdraw from the study, EOS PSG will be acquired
provided they received at least 2 weeks of treatment with GEn. All data for primary and
secondary endpoints will be analyzed using a paired t-test. 95% confidence intervals will be
provided for the true mean treatment difference. Descriptive statistics will be reported for
the primary and secondary endpoints by placebo-baseline visit and treatment group. To
further evaluate treatment effects, the association between the changes from baseline in
primary objective and secondary subjective endpoints will be evaluated using Pearson
correlation coefficients. Safety and tolerability analyses will focus primarily on frequency
of treatment emergent adverse events.
;
Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Single Blind (Subject), Primary Purpose: Treatment
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