TY - JOUR
T1 - Unique and potent effects of acute ibogaine on zebrafish
T2 - The developing utility of novel aquatic models for hallucinogenic drug research
AU - Cachat, Jonathan
AU - Kyzar, Evan J.
AU - Collins, Christopher
AU - Gaikwad, Siddharth
AU - Green, Jeremy
AU - Roth, Andrew
AU - El-Ounsi, Mohamed
AU - Davis, Ari
AU - Pham, Mimi
AU - Landsman, Samuel
AU - Stewart, Adam Michael
AU - Kalueff, Allan V.
N1 - Funding Information:
This study was supported by Tulane University , Tulane Medical School Intramural and Pilot Funds , LA Board of Regents P-Fund , Zebrafish Neurophenome Project , ZNRC and ZENEREI Institute . Ibogaine for this study was obtained through NIDA Drugs Supply Program (NIDA, NIH, Bethesda, USA).
PY - 2013/1/1
Y1 - 2013/1/1
N2 - An indole alkaloid, ibogaine is the principal psychoactive component of the iboga plant, used by indigenous peoples in West Africa for centuries. Modulating multiple neurotransmitter systems, the drug is a potent hallucinogen in humans, although its psychotropic effects remain poorly understood. Expanding the range of model species is an important strategy for translational neuroscience research. Here we exposed adult zebrafish (Danio rerio) to 10 and 20. mg/L of ibogaine, testing them in the novel tank, light-dark box, open field, mirror stimulation, social preference and shoaling tests. In the novel tank test, the zebrafish natural diving response (geotaxis) was reversed by ibogaine, inducing initial top swimming followed by bottom dwelling. Ibogaine also attenuated the innate preference for dark environments (scototaxis) in the light-dark box test. While it did not exert overt locomotor or thigmotaxic responses in the open field test, the drug altered spatiotemporal exploration of novel environment, inducing clear preference of some areas over others. Ibogaine also promoted 'mirror' exploration in the mirror stimulation test, disrupted group cohesion in the shoaling test, and evoked strong coloration responses due to melanophore aggregation, but did not alter brain c-fos expression or whole-body cortisol levels. Overall, our results support the complex pharmacological profile of ibogaine and its high sensitivity in zebrafish models, dose-dependently affecting multiple behavioral domains. While future investigations in zebrafish may help elucidate the mechanisms underlying these unique behavioral effects, our study strongly supports the developing utility of aquatic models in hallucinogenic drug research. High sensitivity of three-dimensional phenotyping approaches applied here to behavioral effects of ibogaine in zebrafish provides further evidence of how 3D reconstructions of zebrafish swimming paths may be useful for high-throughput pharmacological screening.
AB - An indole alkaloid, ibogaine is the principal psychoactive component of the iboga plant, used by indigenous peoples in West Africa for centuries. Modulating multiple neurotransmitter systems, the drug is a potent hallucinogen in humans, although its psychotropic effects remain poorly understood. Expanding the range of model species is an important strategy for translational neuroscience research. Here we exposed adult zebrafish (Danio rerio) to 10 and 20. mg/L of ibogaine, testing them in the novel tank, light-dark box, open field, mirror stimulation, social preference and shoaling tests. In the novel tank test, the zebrafish natural diving response (geotaxis) was reversed by ibogaine, inducing initial top swimming followed by bottom dwelling. Ibogaine also attenuated the innate preference for dark environments (scototaxis) in the light-dark box test. While it did not exert overt locomotor or thigmotaxic responses in the open field test, the drug altered spatiotemporal exploration of novel environment, inducing clear preference of some areas over others. Ibogaine also promoted 'mirror' exploration in the mirror stimulation test, disrupted group cohesion in the shoaling test, and evoked strong coloration responses due to melanophore aggregation, but did not alter brain c-fos expression or whole-body cortisol levels. Overall, our results support the complex pharmacological profile of ibogaine and its high sensitivity in zebrafish models, dose-dependently affecting multiple behavioral domains. While future investigations in zebrafish may help elucidate the mechanisms underlying these unique behavioral effects, our study strongly supports the developing utility of aquatic models in hallucinogenic drug research. High sensitivity of three-dimensional phenotyping approaches applied here to behavioral effects of ibogaine in zebrafish provides further evidence of how 3D reconstructions of zebrafish swimming paths may be useful for high-throughput pharmacological screening.
KW - 3D Reconstructions of locomotion
KW - Hallucinogenic drugs
KW - Ibogaine
KW - Novel tank test
KW - Zebrafish
UR - http://www.scopus.com/inward/record.url?scp=84866512577&partnerID=8YFLogxK
U2 - 10.1016/j.bbr.2012.08.041
DO - 10.1016/j.bbr.2012.08.041
M3 - Article
C2 - 22974549
AN - SCOPUS:84866512577
SN - 0166-4328
VL - 236
SP - 258
EP - 269
JO - Behavioural Brain Research
JF - Behavioural Brain Research
IS - 1
ER -