Paper
Bifeprunox: a partial agonist at dopamine D2 and serotonin1A receptors, influences nicotine‐seeking behaviour in response to drug‐associated stimuli in rats
Published Mar 1, 2012 · DOI · A. Di Clemente, C. Franchi, A. Orrù
Addiction Biology
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Abstract
Environmental stimuli repeatedly associated with the self‐administered drugs may acquire motivational importance. Because dopamine (DA) D2/D3 partial agonists and D3 antagonists interfere with the ability of drug‐associated cues to induce drug‐seeking behaviour, the present study investigated whether bifeprunox, 7‐[4‐([1,1′biphenyl]‐3‐ylmethyl)‐1‐piperazinyl]‐2(3H)‐benzoxazolone mesylate), a high‐affinity partial agonist of the D2 subfamily of DA receptors and of serotonin1A receptors, influences reinstatement of drug‐associated cue‐induced nicotine‐seeking behaviour. The study also explored whether bifeprunox reduced motivated behaviour by evaluating its effects on reinstatement induced by stimuli conditioned to sucrose. To verify whether bifeprunox interferes with the primary reinforcing properties of either drug or sucrose, we compared its effects on nicotine self‐administration and on sucrose‐reinforced behaviour. Different groups of experimentally naïve, food‐restricted Wistar rats were trained to associate a discriminative stimulus with response‐contingent availability of nicotine or sucrose and tested for reinstatement after extinction of nicotine or sucrose‐reinforced behaviour. Bifeprunox (4–16 µg/kg, s.c.) dose‐dependently attenuated the response‐reinstating effects of nicotine‐associated cues. Higher doses (64–250 µg/kg, s.c.) reduced spontaneous locomotor activity and suppressed operant responding induced by sucrose‐associated cues and by the primary reinforcing properties of nicotine or sucrose. Provided they can be extrapolated to abstinent human addicts, these results suggest the potential therapeutic use of partial DA D2 receptor agonist to prevent cue‐controlled nicotine‐seeking and relapse. The profile of action of high doses of bifeprunox remains to be examined for potential sedation or anhedonia effects.
Bifeprunox, a partial dopamine D2 receptor agonist, may help prevent cue-controlled nicotine-seeking and relapse in abstinent human addicts by reducing the reinstating effects of drug-associated cues and sucrose-reinforced behavior.
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