IbogainerctRCT2015

Ascending-dose study of noribogaine in healthy volunteers: pharmacokinetics, pharmacodynamics, safety, and tolerability.

Journal of clinical pharmacology

confidence

Key findings

Single oral doses of noribogaine 3-60 mg were safe, well tolerated, dose-linear PK; no mu-opioid agonist pharmacodynamic effects observed.

View source on PubMed (PMID 25279818) ↗

Sample size
36 (4 cohorts of 9)
Population
Healthy drug-free male volunteers
Dosing
3, 10, 30, or 60 mg or matching placebo
Duration
Single dose with assessments to 216 hours
Route
Oral
Blinding
double_blind
Controls
placebo
Drug class
ibogaine therapy

Measured endpoints

  • Safety and tolerability (no safety or tolerability issues identified)No changesafety
    not_reported
  • Peak concentration time (Tmax)Unclearother
    not_reportedeffect: 2-3 hours
  • AUC and Cmax dose-linearityIncreasedother
    not_reportedeffect: dose-linear between 3 and 60 mg
  • Elimination half-lifeUnclearother
    not_reportedeffect: 28-49 hours
  • Apparent volume of distributionUnclearother
    not_reportedeffect: 1417-3086 L
  • Mu-opioid agonist pharmacodynamic effect (pupillometry)No changeneurological
    not_reportedeffect: no effects noted
  • Mu-opioid agonist pharmacodynamic effect (cold-pressor testing)No changepain
    not_reportedeffect: no effects noted
Full abstract

Noribogaine is the active metabolite of the naturally occurring psychoactive substance ibogaine, and may help suppress withdrawal symptoms in opioid-dependent subjects. The objectives of this Phase I study were to assess the safety, tolerability, pharmacokinetic, and pharmacodynamic profiles of noribogaine. In this ascending single-dose, placebo-controlled, randomized, double-blind, parallel-group study in 36 healthy drug-free male volunteers, 4 cohorts (n = 9) received oral doses of 3, 10, 30, or 60 mg or matching placebo, with intensive safety and pharmacokinetic assessments out to 216 hours, along with pharmacodynamic assessments sensitive to the effects of mu-opioid agonists. Noribogaine was rapidly absorbed, with peak concentrations occurring 2-3 hours after oral dosing, and showed dose-linear increases of area under the concentration-time curve (AUC) and Cmax between 3 and 60 mg. The drug was slowly eliminated, with mean half-life estimates of 28-49 hours across dose groups. Apparent volume of distribution was high (mean 1417-3086 L across dose groups). No safety or tolerability issues were identified in any cohort. No mu-opioid agonist pharmacodynamic effects were noted in pupillometry or cold-pressor testing. Single oral doses of noribogaine 3-60 mg were safe and well tolerated in healthy volunteers.

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