Naltrexone but Not Ketanserin Antagonizes the Subjective, Cardiovascular, and Neuroendocrine Effects of Salvinorin-A in Humans

Salvinorin-A is a terpene found in the leaves of the plant Salvia divinorum. When administered to humans, salvinorin-A induces an intense but short-lasting modified state of awareness, sharing features with those induced by the classical serotonin-2A receptor agonist psychedelics. However, unlike su...

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Detalhes bibliográficos
Autores: Maqueda, Ana Elda, Valle, Marta|||0000-0002-3515-251X, Addy, Peter H., Antonijoan Arbós, Rosa Ma (Rosa María)|||0000-0002-7099-5125, Puntes, Montserrat, Coimbra, Jimena, Ballester, Maria Rosa|||0000-0002-0472-9558, Garrido, Maite, González, Mireia, Claramunt, Judit, Barker, Steven|||0000-0002-5755-3496, Lomnicka, Izabela, Waguespack, Marian, Johnson, Matthew W., Griffiths, Roland R., Riba, Jordi|||0000-0002-9375-8421
Tipo de documento: artigo
Data de publicação:2016
País:España
Recursos:Universitat Autònoma de Barcelona
Repositório:Dipòsit Digital de Documents de la UAB
Idioma:inglês
OAI Identifier:oai:ddd.uab.cat:254104
Acesso em linha:https://ddd.uab.cat/record/254104
https://dx.doi.org/urn:doi:10.1093/ijnp/pyw016
Access Level:Acceso aberto
Palavra-chave:Salvinorin-A
Naltrexone
Ketanserin
Kappa opioid receptor antagonism
Serotonin-2a antagonism
Human pharmacology
Descrição
Resumo:Salvinorin-A is a terpene found in the leaves of the plant Salvia divinorum. When administered to humans, salvinorin-A induces an intense but short-lasting modified state of awareness, sharing features with those induced by the classical serotonin-2A receptor agonist psychedelics. However, unlike substances such as psilocybin or mescaline, salvinorin-A shows agonist activity at the kappa-opioid receptor rather than at the serotonin-2A receptor. Here, we assessed the involvement of kappa-opioid receptor and serotonin-2A agonism in the subjective, cardiovascular, and neuroendocrine effects of salvinorin-A in humans. We conducted a placebo-controlled, randomized, double-blind study with 2 groups of 12 healthy volunteers with experience with psychedelic drugs. There were 4 experimental sessions. In group 1, participants received the following treatment combinations: placebo+placebo, placebo+salvinorin-A, naltrexone+placebo, and naltrexone+salvinorin-A. Naltrexone, a nonspecific opioid receptor antagonist, was administered at a dose of 50mg orally. In group 2, participants received the treatment combinations: placebo+placebo, placebo+salvinorin-A, ketanserin+placebo, and ketanserin+salvinorin-A. Ketanserin, a selective serotonin-2A antagonist, was administered at a dose of 40mg orally. Inhalation of 1mg of vaporized salvinorin-A led to maximum plasma concentrations at 1 and 2 minutes after dosing. When administered alone, salvinorin-A severely reduced external sensory perception and induced intense visual and auditory modifications, increased systolic blood pressure, and cortisol and prolactin release. These effects were effectively blocked by naltrexone, but not by ketanserin. Results support kappa opioid receptor agonism as the mechanism of action underlying the subjective and physiological effects of salvinorin-A in humans and rule out the involvement of a serotonin-2A-mediated mechanism.