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Chronic D2/3 agonist ropinirole treatment increases preference for uncertainty in rats regardless of baseline choice patterns

Tremblay, M and Silveira, Mason and Kaur, S and Hosking, J and Adams, W.K and Baunez, C and Winstanley, C.A (2016) Chronic D2/3 agonist ropinirole treatment increases preference for uncertainty in rats regardless of baseline choice patterns. European Journal of Neuroscience, 45 (1). ISSN 0953-816X

Type of Research: Article
Creators: Tremblay, M and Silveira, Mason and Kaur, S and Hosking, J and Adams, W.K and Baunez, C and Winstanley, C.A
Description:

D2/3 receptor agonists are effective treatments for Parkinson's disease (PD), but can precipitate impulse control disorders (ICDs) including gambling disorder (GD). The neurobiological mechanisms underlying this devastating side-effect of dopamine agonist replacement therapy (DRT), and any dependence on the dopamine depletion caused by PD, are unclear. It is also unclear whether previous biases towards risk or uncertainty are a risk factor for developing these ICDs. We investigated whether chronic D2/3 agonist administration (5 mg/kg/day ropinirole for 28 days) altered performance of a rat model of gambling-like behaviour, the rodent betting task (rBT), and examined if baseline behaviour predicted this behavioural change. The rBT captures individual differences in subjective preference for uncertain outcomes: animals choose between guaranteed or probabilistic reinforcement of equal expected value. Chronic ropinirole dramatically increased selection of the uncertain option in two-thirds of animals, regardless of baseline preferences. The effect on choice in the rBT was replicated in a dorsolateral striatal 6-hydroxydopamine (6-OHDA) rat model of early PD. These studies are the first to look at individual differences in response to chronic, rather than pulsatile, dosing of DRT in a rodent model of gambling behaviour. These findings suggest that DRT-induced PG may stem from increases in subjective valuation of uncertainty. Such symptoms likely arise because of changes in dopaminergic striatal signalling caused by DRT rather than from an interaction between pre-morbid behaviours or PD itself.

Official Website: https://onlinelibrary.wiley.com/doi/10.1111/ejn.13332
Publisher/Broadcaster/Company: Wiley-Blackwell
Your affiliations with UAL: Colleges > London College of Fashion
Date: 16 July 2016
Digital Object Identifier: 10.1111/ejn.13332
Date Deposited: 04 Jun 2026 14:56
Last Modified: 04 Jun 2026 14:56
Item ID: 26863
URI: https://ualresearchonline.arts.ac.uk/id/eprint/26863
Licence: Creative Commons Attribution Non-commercial No Derivatives

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