25x-NBOH

The NBOH series represents a refinement of the NBOMe concept: potent phenethylamine psychedelics that act primarily through agonism at serotonin 5-HT2A receptors, but with a hydroxyl group replacing the methoxy group on the N-benzyl ring. The experiential signature of the class shares much with its NBOMe parent compounds while differing in certain respects.

The general NBOH experience is characterized by a rapid onset, typically within fifteen to twenty minutes of sublingual administration, and a pronounced visual intensity relative to the depth of the cognitive experience. Colors become vivid and saturated, surfaces develop geometric patterns, and the visual field takes on a sharp, high-contrast quality. The headspace tends to be stimulated but relatively clear, lacking the deep philosophical and ego-dissolving qualities of classical tryptamine or lysergamide psychedelics.

Physically, the NBOH compounds produce notable stimulation, vasoconstriction, jaw tension, and body load, though many users report these effects as somewhat milder than those produced by the corresponding NBOMe compounds. Duration is moderate, typically four to seven hours from onset to baseline. Individual members of the series differ in their visual character, body load, and emotional tone, but the general class signature remains consistent: fast, visually intense, physically demanding, and cognitively shallow relative to classical psychedelics.

Pharmacodynamics Actions The NBOMe drugs are highly potent and selective agonists of the serotonin 5-HT2 receptors, including of the 5-HT2A, 5-HT2B, and 5-HT2C receptors. However, they are much less potent and efficacious at the serotonin 5-HT2B receptor compared to the serotonin 5-HT2A and 5-HT2C receptors. The drugs are highly selective for the serotonin 5-HT2 receptors over other serotonin receptors and over a variety of other biological targets. They are likewise inactive as monoamine reuptake inhibitors and releasing agents. Many of the NBOMe drugs are partial agonists of the rat and mouse trace amine-associated receptor 1 (TAAR1), but they are inactive as agonists of the human TAAR1.

Effects In accordance with their psychedelic effects, NBOMe drugs induce the head-twitch response, a behavioral proxy of psychedelic effects, in rodents. They have also been found to produce hyperlocomotion at low doses and hypolocomotion at high doses in rodents.

Unlike most other serotonergic psychedelics, the NBOMe drugs 25B-NBOMe and 25N-NBOMe have been found to produce reinforcing effects in rodents, and hence may have misuse potential. Relatedly, 25B-NBOMe robustly increased dopamine levels in the nucleus accumbens similarly to methamphetamine. The reinforcing effects of 25B-NBOMe were not blocked by serotonin 5-HT2A receptor antagonism, and it is unclear how they are produced. However, some NBOMe drugs, such as 25N-NBOMe, have been found to increase phosphorylation of the dopamine transporter (DAT) in the striatum similarly to methamphetamine in rodents. DAT phosphorylation is associated with dopamine reverse transport and efflux, which in turn increases extracellular dopamine levels.

Similarly to other psychedelics like DOI and 2C-T-7, tolerance has been found to gradually develop to the head-twitch response induced by 25I-NBOMe with chronic administration in rodents.

No human clinical data exist on the pharmacology of NBOMe derivatives as of 2020.

2C-B, the first major 2C drug and an analogue of mescaline, was first described by Alexander Shulgin in the 1970s. Richard Glennon and colleagues synthesized and described 25B-NB (N-benzyl-2C-B) along with a variety of other 25-NB derivatives in 1994. It was observed at the time that 25B-NB had slightly higher affinity for the serotonin 5-HT2A receptor than 2C-B and that other 25-NB derivatives with substituents on the benzyl ring showed very high affinity for the receptor, though functional data were not reported.

N-Benzyl derivatives of the ketanserin-related quinazolinedione EZS-8, such as RH-34, were first described by Heinz Pertz, Sigurd Elz, and Ralf Heim by 1996 or 1998. NBOMe-mescaline and NBOMe-escaline were first described by Pertz and colleagues by 1999, while 25B-NBOMe was first described by Heim and colleagues in 1999. 25I-NBOMe and other 25-NB compounds such as 25TFM-NBOMe and 2CBFly-NBOMe were described by Heim and colleagues by 2000. 25I-NBOMe and other 25-NB drugs were subsequently further described by Heim in his dissertation in 2003. 25C-NBOMe was not described in the literature until 2010. The discovery of the 25-NB compounds by Heim and colleagues has been described by David E. Nichols as structurally remarkable, since N-alkylation of psychedelic phenethylamines, for instance Beatrice (N-methyl-DOM), has otherwise invariably abolished the hallucinogenic effects of this class of compounds.

The NBOMe drugs, primarily 25I-NBOMe, were encountered as novel recreational drugs by 2010, and by 2012 had eclipsed other psychedelics like LSD and psilocybin-containing mushrooms in popularity, at least for a time. Various NBOMes, such as 25I-NBOMe, became Schedule I controlled substances in the United States in 2013.