Recreational Use, Analysis and Toxicity of Tryptamines

Abstract: The definition New psychoactive substances (NPS) refers to emerging drugs whose chemical structures are similar to other psychoactive compounds but not identical, representing a “legal” alternative to internationally controlled drugs. There are many categories of NPS, such as synthetic cannabinoids, synthetic cathinones, phenylethylamines, piperazines, ketamine derivatives and tryptamines. Tryptamines are naturally occurring compounds, which can derive from the amino acid tryptophan by several biosynthetic pat… Show more

“…However, many synthetic tryptamine derivatives have been synthesized and are recreationally used as novel psychoactive substances (Araujo et al, 2015;EMCDDA, 2014;Helander et al, 2014;Kamour et al, 2014;Shulgin and Shulgin, 1997;Tittarelli et al, 2015;Winstock et al, 2014). Tryptamines share their core structure with the neurotransmitter serotonin (5-hydroxytryptamine ).…”

“…The psychoactive effects of hallucinogens, including those of tryptamines, are thought to be mediated mainly by the 5-HT 2A receptor (Glennon et al, 1984;Nichols, 2004;Titeler et al, 1988;Vollenweider et al, 1998) but may also be modulated by interactions with other targets, including other 5-HT receptors, monoamine transporters, and trace amineassociated receptors (Baumeister et al, 2014;Bunzow et al, 2001;Cozzi et al, 2009;Fantegrossi et al, 2006;McKenna et al, 1990;Nagai et al, 2007;Nichols, 2004;Ray, 2010). Structural alterations of tryptamines have been shown to result in different pharmacological and psychoactive profiles (Araujo et al, 2015;McKenna et al, 1990;Repke et al, 1985;Shulgin and Shulgin, 1997;Tittarelli et al, 2015;Trachsel et al, 2013). For example, compounds that have no substitutions or a 4-hydroxyl group (e.g., DMT or psilocin, respectively; Fig.…”

“…1) produce hallucinogenic effects with relative low potency in man (Repke et al, 1985). Psilocin is orally psychoactive above 5-10 mg, and DMT is active at parenteral doses of 20-100 mg (Araujo et al, 2015;Shulgin and Shulgin, 1997;Studerus et al, 2011;Tittarelli et al, 2015). In contrast, a 5-methoxy group, such as in 5-MeO-AMT ( Fig.…”

“…Different N-substitutions also influenced in vivo potency (Nichols et al, 2015;Repke et al, 1985). The pharmacological profiles of many tryptamines have been studied previously at selected targets (Blough et al, 2014;Gatch et al, 2011;McKenna et al, 1990;Nichols et al, 2015;Repke et al, 1985;Shulgin and Carter, 1980), and new and pharmacologically unknown tryptamine derivatives are constantly emerging on the illicit drug market (Araujo et al, 2015;Corkery et al, 2012;EMCDDA, 2014;Greene, 2013;Helander et al, 2014;Tittarelli et al, 2015).…”

“…The present study included recreationally used tryptamines (Araujo et al, 2015;EMCDDA, 2014;Greene, 2013;Schmidt et al, 2011;Tittarelli et al, 2015), including…”

Receptor interaction profiles of novel psychoactive tryptamines compared with classic hallucinogens

“…However, many synthetic tryptamine derivatives have been synthesized and are recreationally used as novel psychoactive substances (Araujo et al, 2015;EMCDDA, 2014;Helander et al, 2014;Kamour et al, 2014;Shulgin and Shulgin, 1997;Tittarelli et al, 2015;Winstock et al, 2014). Tryptamines share their core structure with the neurotransmitter serotonin (5-hydroxytryptamine ).…”

“…The psychoactive effects of hallucinogens, including those of tryptamines, are thought to be mediated mainly by the 5-HT 2A receptor (Glennon et al, 1984;Nichols, 2004;Titeler et al, 1988;Vollenweider et al, 1998) but may also be modulated by interactions with other targets, including other 5-HT receptors, monoamine transporters, and trace amineassociated receptors (Baumeister et al, 2014;Bunzow et al, 2001;Cozzi et al, 2009;Fantegrossi et al, 2006;McKenna et al, 1990;Nagai et al, 2007;Nichols, 2004;Ray, 2010). Structural alterations of tryptamines have been shown to result in different pharmacological and psychoactive profiles (Araujo et al, 2015;McKenna et al, 1990;Repke et al, 1985;Shulgin and Shulgin, 1997;Tittarelli et al, 2015;Trachsel et al, 2013). For example, compounds that have no substitutions or a 4-hydroxyl group (e.g., DMT or psilocin, respectively; Fig.…”

“…1) produce hallucinogenic effects with relative low potency in man (Repke et al, 1985). Psilocin is orally psychoactive above 5-10 mg, and DMT is active at parenteral doses of 20-100 mg (Araujo et al, 2015;Shulgin and Shulgin, 1997;Studerus et al, 2011;Tittarelli et al, 2015). In contrast, a 5-methoxy group, such as in 5-MeO-AMT ( Fig.…”

“…Different N-substitutions also influenced in vivo potency (Nichols et al, 2015;Repke et al, 1985). The pharmacological profiles of many tryptamines have been studied previously at selected targets (Blough et al, 2014;Gatch et al, 2011;McKenna et al, 1990;Nichols et al, 2015;Repke et al, 1985;Shulgin and Carter, 1980), and new and pharmacologically unknown tryptamine derivatives are constantly emerging on the illicit drug market (Araujo et al, 2015;Corkery et al, 2012;EMCDDA, 2014;Greene, 2013;Helander et al, 2014;Tittarelli et al, 2015).…”

“…The present study included recreationally used tryptamines (Araujo et al, 2015;EMCDDA, 2014;Greene, 2013;Schmidt et al, 2011;Tittarelli et al, 2015), including…”

Receptor interaction profiles of novel psychoactive tryptamines compared with classic hallucinogens

Appendix B: Metabolism of Major Illicit Drugs

Exploring the biocatalysis of psilocybin and other tryptamines: Enzymatic pathways, synthetic strategies, and industrial implications