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AMT vs Ibogaine

A side-by-side research comparison of AMT and Ibogaine across mechanism, dosing, half-life, benefits, side effects and research status.

Comparison table

AttributeAMTIbogaine
Full nameAlpha-methyltryptamineIbogaine (from Tabernanthe iboga)
CategoryPsychedelicsPsychedelics
StatusSchedule I (research compound; once a Soviet antidepressant)Schedule I (research compound)
MechanismReleases and blocks reuptake of serotonin, dopamine and norepinephrine, and activates serotonin receptors, giving mixed psychedelic and stimulant effects.Acts on multiple systems at once, including serotonin and opioid receptors, NMDA receptors and nicotinic receptors. Its active metabolite noribogaine is thought to drive much of the lasting anti-addiction effect.
Molecular weight174.24 g/mol310.43 g/mol
Half-lifeLong~4-7 hours (ibogaine); noribogaine much longer
BioavailabilityOralOral
Typical doseVaries by individual and settingWeight-based, given in specialized clinics
FrequencyOccasionalUsually a single session
RouteOralOral, under medical and cardiac monitoring

AMT reported benefits

  • Historic antidepressant use
  • Long-lasting effects
  • Mixed psychedelic-stimulant profile
  • Tryptamine research compound

Ibogaine reported benefits

  • Studied for opioid use disorder
  • Can reduce withdrawal symptoms quickly
  • May lower cravings after a single session
  • Investigated for traumatic brain injury (with magnesium) in veterans

Related comparisons

Research and educational reference only. Not medical advice.