The acute effects of monoamine reuptake inhibitors
on the stimulus effects
of hallucinogens
by
Winter JC, Helsley S, Fiorella D, Rabin RA
Department of Pharmacology and Toxicology,
School of Medicine and Biomedical
Sciences,
State University of New York at Buffalo, 14214-3000, USA.
Pharmacol Biochem Behav 1999 Jul; 63(3):507-13
ABSTRACT
In a previous study it was observed that fluoxetine potentiates the stimulus
effects of lysergic acid diethylamide (LSD). In the present investigation,
stimulus control was established in groups of rats using as training drugs the
hallucinogens lysergic acid diethylamide (LSD); 0.1 mg/kg),
(-)-2,5-dimethoxy-4-methylamphetamine [(-)-DOM; 0.56 mg/kg], ibogaine (10
mg/kg), and 5-methoxy-N,N-dimethyltryptamine (5-MeO-DMT; 3 mg/kg). A two-lever,
fixed-ratio 10, positively reinforced task with saline controls was employed.
The hypotheses tested were that (a) monoamine uptake inhibitors other than
fluoxetine potentiate the discriminative effects of LSD, and (b) hallucinogens
other than LSD are potentiated by acute pretreatment with monoamine uptake
inhibitors. The effects of a range of doses of each of the training drugs were
determined both alone and following pretreatment with the monoamine reuptake
inhibitors fluoxetine, fluvoxamine, and venlafaxine. In LSD-trained subjects,
all three reuptake inhibitors caused a significant increase in LSD-appropriate
responding. Similar results were observed in rats trained with (-)-DOM and with
ibogaine. In 5-MeO-DMT-trained subjects, only fluoxetine resulted in an
enhancement of drug-appropriate responding. The reuptake inhibitors given alone
elicited varying degrees of responses appropriate for the respective training
drugs. For fluoxetine in rats trained with LSD and ibogaine, for venlafaxine in
LSD trained, and for fluvoxamine in (-)-DOM trained, the degree of responding
met our criterion for intermediate responding, i.e., significantly different
from both training conditions. Subsequent experiments in (-)-DOM-trained
subjects examined a range of doses of each of the reuptake inhibitors in
combination with a fixed dose of (-)-DOM (0.1 mg/kg), which alone yielded about
50% (-)-DOM-appropriate responding. With the exception of the point obtained
with the highest dose of venlafaxine, all data were compatible with additivity
of effects rather than true potentiation. In summary, the present data extend
our previous observation of the augmentation of the stimulus effects of LSD by
fluoxetine to include other hallucinogens. The mechanisms by which these
interactions arise and possible differential effects of acute and chronic
treatment remain to be established.
SSRIs
MDMA
Options
Mescaline
Serotonin
Dopamine
Fluoxetine
Venlafaxine
Noradrenaline
SSRI spectrum
Salvia divinorum
Hofmann's LSD: My Problem Child
Hallucinogenic fungi and medicinal herbs
Naturally-growing hallucinogens and dissociative agents
HOME
HedWeb
Future Opioids
BLTC Research
Paradise-Engineering
The Hedonistic Imperative
When Is It Best To Take Crack Cocaine?