Dimethylhomotryptamine

Dimethylhomotryptamine, also known as N,''N''-dimethylhomotryptamine or as 3-indole, is a homotryptamine and homologue of the psychedelic tryptamine dimethyltryptamine in which the alkyl side chain has been lengthened by one carbon atom. The homologue of DMT in which the alkyl side chain has been shortened by one carbon atom is gramine.

Use and effects

According to Alexander Shulgin in his book TiHKAL and other publications, DMHT was studied by the Upjohn Company under the code name U-6056. It was assessed in a clinical study of 10individuals at doses of up to 10mg by intravenous injection and 70mg by intramuscular injection, but produced no psychoactive or hallucinogenic effects besides mild agitation or anxiety and caused slight increases in heart rate and blood pressure. For comparison, DMT has been reported to produce psychedelic effects at doses as low as 20 to 50mg by intramuscular injection. The human properties and effects of the lower homologue gramine are unknown.

DMHT showed the same affinity for serotonin receptors in the rat fundus strip as DMT. It also shows low affinity for the serotonin 5-HT₃ receptor. The drug's analogue homotryptamine showed abolished affinity for the serotonin 5-HT_1E and 5-HT_1F receptors. DMHT is a potent serotonin reuptake inhibitor, with an affinity for the serotonin transporter of 58nM. It produced hyperthermia in rabbits.

Other DMT and DMHT homologues with further extended alkyl chains have been studied, but were said to have no interesting activity. The highly potent selective serotonin reuptake inhibitor BMS-505130 was derived via structural modification of DMHT.

DMHT was first described in the scientific literature by William J. Turner and Sidney Merlis in 1959.