Abstract
Ibogaine is a naturally occurring substance which has been increasingly used in the lay-scene to reduce craving and relapse in patients with substance use disorders (SUDs). Although human clinical trials on the safety and efficacy of ibogaine are lacking, animal studies do support the efficacy of ibogaine. In this systematic review and meta-analysis (MA), we summarise these animal findings, addressing three questions: (1) does ibogaine reduce addictive behaviour in animal models of SUDs?; (2) what are the toxic effects of ibogaine on motor functioning, cerebellum and heart rhythm?; (3) what are neuropharmacological working mechanisms of ibogaine treatment in animal models of SUDs? MA of 27 studies showed that ibogaine reduced drug self-administration, particularly during the first 24 h after administration. Ibogaine had no effect on drug-induced conditioned place preference. Ibogaine administration resulted in motor impairment in the first 24 h after supplementation, and cerebral cell loss even weeks after administration. Data on ibogaines effect on cardiac rhythm, as well as on its neuropharmacological working mechanisms are limited. Our results warrant further studies into the clinical efficacy of ibogaine in SUD patients in reducing craving and substance use, but close monitoring of the patients is recommended because of the possible toxic effects. In addition, more work is needed to unravel the neuropharmacological working mechanisms of ibogaine and to investigate its effects on heart rhythm.
Highlights
Substance use disorders (SUDs) account for a large share of the total global burden of disease
Duval and Tweedie's trimm and fill analysis for the data set on drug SA resulted in 4 extra data points of the total of 29 comparisons, indicating slight overestimation of the summary effect size (Supplementary Figure 2)
Sensitivity analysis revealed that changing the boundaries of our inclusion criteria and the classification of our subgroups did not alter our results significantly
Summary
Substance use disorders (SUDs) account for a large share of the total global burden of disease. One promising compound is ibogaine, a naturally occurring substance in an African shrub. This compound has been claimed to reduce craving and relapse rates in patients with SUDs.[10] case reports mention a reduction of withdrawal symptoms and relapse after a single dose of ibogaine with a sustainability of this effect of several months.[11] Ibogaine has increasingly been used for this purpose over the last decades, mainly in a lay-scene.[12,13] human clinical trials on the safety and efficacy of ibogaine for patients with SUDs are lacking
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