Sodium Oxybate in Idiopathic Hypersomnia

GHB

Brief Summary

this study evaluates of the efficacy of sodium oxybate on excessive daytime sleepiness using Epworth sleepiness scale over 8 weeks compared to placebo

Intervention / Treatment

  • Sodium Oxybate Oral Solution 500 MG/ML (DRUG)
    First night after V1: Dose prescribed at 4.5 g per night (2.25 g x 2) for 2 weeks First night after V2: Dose increased to 6 g per night (3 g x 2) for 2 weeks, according to investigator's opinion, tolerance of drug and CGI-S First night after V3: Dose either maintained stable at 6 g or increased to 9 g per night (4.5 g x 2) with dose increments of 1.5 g per night (0.75 g x 2) every week, based on benefit-risk ratio, for 2 weeks. First night after V4: Dose maintained at 9 g or reduced at 6 g per night according to benefit-risk ratio for 2 weeks. No dose adjustment during the Maintenance period. First night after V5: Taper period. Dose decrease by 2.25 g x 2 every two days until complete withdrawal
  • Placebos (DRUG)
    Xyrem Placebo: sodium citrate solution in equimolar concentration of sodium in the 500 mg/mL Xyrem oral solution, PH adjusted with malic acid

Condition or Disease

  • Idiopathic Hypersomnia

Phase

  • Phase 2
  • Phase 3
  • Study Design

    Study type: INTERVENTIONAL
    Status: Completed
    Study results: No Results Available
    Age: 18 Years to 60 Years
    Enrollment: 48 (ACTUAL)
    Funded by: Other
    Allocation: Randomized
    Primary Purpose: Treatment

    Masking

    TRIPLE:
    • Participant
    • Care Provider
    • Investigator

    Clinical Trial Dates

    Start date: Oct 18, 2018 ACTUAL
    Primary Completion: Apr 12, 2023 ACTUAL
    Completion Date: Apr 12, 2023 ACTUAL
    Study First Posted: Jul 24, 2018 ACTUAL
    Results First Posted: Aug 30, 2020
    Last Updated: Sep 26, 2023

    Sponsors / Collaborators

    Lead sponsor is responsible party
    Responsible Party: N/A

    Bicentric, randomized, double-blind controlled study Outpatients aged from 18 to 60 years, suffering from current idiopathic hypersomnia (ICSD-3), recruited via medical consultations in the investigation centers Randomization in Xyrem or placebo arms after the inclusion visit,

    1.Screening Period (up to 15 days), 2.Titration Period (up to 45 days), 3.Maintenance Period (minimum 15 days), 4.Safety Follow-Up Period (14 days)

    Participant Groups

    • Xyrem (Sodium Oxybate), oral solution 500mg/mL First night after V1: Dose prescribed at 4.5 g per night (2.25 g x 2) for 2 weeks First night after V2: Dose increased to 6 g per night (3 g x 2) for 2 weeks, according to investigator's opinion, tolerance of drug and CGI-S First night after V3: Dose either maintained stable at 6 g or increased to 9 g per night (4.5 g x 2) with dose increments of 1.5 g per night (0.75 g x 2) every week, based on benefit-risk ratio, for 2 weeks. First night after V4: Dose maintained at 9 g or reduced at 6 g per night according to benefit-risk ratio for 2 weeks. No dose adjustment during the Maintenance period. First night after V5: Taper period. Dose decrease by 2.25 g x 2 every two days until complete withdrawal

    • Xyrem Placebo: sodium citrate solution in equimolar concentration of sodium in the 500 mg/mL Xyrem oral solution, PH adjusted with malic acid

    Eligibility Criteria

    Sex: All
    Minimum Age: 18
    Maximum Age: 60
    Age Groups: Adult
    Healthy Volunteers: Yes

    Inclusion Criteria:

    * Diagnostic of idiopathic hypersomnia (ICSD-3 criteria)
    * Age between 18 and 60 years-old
    * BMI between 18 and 35 kg/m2
    * MSLT: mean sleep latency (MSL) ≤8 minutes and \< 2 SOREMPs, AND/OR total sleep time \> 11h/24h on 24-hours long-term polysomnography
    * Polysomnography recording: sleep efficiency \> 85%, total sleep time ≥6 hours, AHI \<10/hour, micro-arousals index \<15/hour, PLM index associated with micro-arousals \<10/hour.
    * Absence of sleep deprivation, assessed by actigraphy or sleep logs
    * ESS score ≥14 points
    * Written informed consent
    * National health insurance cover

    Exclusion Criteria:

    * Current alcohol intake or treatment with modafinil, amphetamine, methylphenidate, mazindol, pitolisant, neuroleptics, sedative hypnotics, barbiturates, general anesthetics, myorelaxants, other CNS depressants, antidepressants\*, anxiolytic drugs, anticonvulsive therapy, topiramate, inhibitors of GHB dehydrogenase (i.e. valproate, ethosuximide, phenytoin), budipine, dopamine antagonist antiemetics (except domperidone), opioids, benzodiazepines, Z-drugs, MAO inhibitors, COMT inhibitors, or sedative antihistamines. If patient has received such therapy, a washout-period of at least 15 days, or equivalent to 5 half-lives of the drug, prior to the inclusion in the study is required before starting treatment in this study.

    \*30 days for antidepressants
    * Previous intake of sodium oxybate
    * Succinic semialdehyde dehydrogenase deficiency, porphyria
    * Other central nervous system diseases: neurodegenerative diseases, seizure disorders or history of head trauma associated with loss of consciousness
    * Lifetime history of suicide attempt or suicidal ideation in the past 6 months, prior history of psychotic episodes, current or recent history of a major depressive disorder (DSM-V), Beck depression inventory (BDI) \> 16 and/or item G\> 0
    * History of chronic alcohol or drug abuse within the prior 12 months
    * Malignant neoplastic disease requiring therapy within 12 months prior to Visit 1 or clinically relevant
    * Heart failure, severe hypertension or other cardiovascular disease compromising the patient's wellbeing or ability to participate in this study
    * Renal or hepatic impairment Compromised respiratory function
    * Sleep-related breathing disorders (AHI ≥ 10/h)
    * No regular sleep at night: shift work or other continuous non-disease-related life conditions
    * Participation in another study of an investigational drug within the 28 days prior to Visit 1 or currently
    * Hypersensitivity to any of the components of the study medication
    * Pregnancy (βHCG positive) and breast-feeding

    Primary Outcomes
    • Evaluation of difference in sleepiness with ESS between the 2 groups. ESS scores range from 0 to 24; there is a risk of pathological daytime sleepiness if score is \> 10.

    More Details

    NCT Number: NCT03597555
    Acronym: SODHI
    Other IDs: RECHMPL17_0375
    Study URL: https://clinicaltrials.gov/study/NCT03597555
    Last updated: Sep 29, 2023