Dopamine agonist treatment increases sensitivity to gamble outcomes in the hippocampus in de novo Parkinson’s disease

doi:10.1016/j.nicl.2020.102362

NeuroImage: Clinical

Volume 28, 2020, 102362

https://doi.org/10.1016/j.nicl.2020.102362 Get rights and content

Under a Creative Commons license

open access

Highlights

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The effect of first dopaminergic treatment on the reward circuit in PD is unclear.
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Many ON/OFF designs suffer from long-lasting dopaminergic effects (multiple days).
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We tested reward processing in dopa-naive PD before and after treatment initiation.
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Dopaminergic drugs increased reward-related hippocampus activity in PD.
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The relationship with development of neuropsychiatric symptoms remains unknown.

Abstract

Background

Parkinson’s disease is associated with severe nigro-striatal dopamine depletion, leading to motor dysfunction and altered reward processing. We previously showed that drug-naïve patients with Parkinson’s disease had a consistent attenuation of reward signalling in the mesolimbic and mesocortical system. Here, we address the neurobiological effects of dopaminergic therapy on reward sensitivity in the mesolimbic circuitry, and how this may contribute to neuropsychiatric symptoms.

Objectives

We tested the hypothesis that (1) dopaminergic treatment would restore the attenuated, mesolimbic and mesocortical responses to reward; and (2) restoration of reward responsivity by dopaminergic treatment would predict motor performance and the emergence of impulse control symptoms.

Methods

In 11 drug-naïve Parkinson patients, we prospectively assessed treatment-induced changes in reward processing before, and eight weeks after initiation of monotherapy with dopamine agonists. They were compared to 10 non-medicated healthy controls who were also measured longitudinally. We used whole-brain functional magnetic resonance imaging at 3 Tesla to assess the reward responsivity of the brain to monetary gains and losses, while participants performed a simple consequential gambling task.

Results

In patients, dopaminergic treatment improved clinical motor symptoms without significantly changing task performance. Dopamine agonist therapy induced a stronger reward responsivity in the right hippocampus with higher doses being less effective. None of the patients developed impulse control disorders in the follow-up period of four years.

Conclusions

Short-term treatment with first-ever dopaminergic medication partially restores deficient reward-related processing in the hippocampus in de novo Parkinson’s disease.

Keywords

fMRI

Reward

Mesolimbic system

Parkinson's disease

Drug-naïve, dopamine-agonist

Abbreviations

BDI

beck depression inventory II

BIS

barratt impulsiveness scale

BOLD

blood oxygen level dependent

confidence interval

dopamine

fMRI

functional magnetic resonance imaging

GAQ

gambling addiction questionnaire

GLM

general linear model

ICD

impulse control disorder

MMSE

mini-mental state examination

MNI

Montreal Neurological Institute

Parkinson’s disease

ROI

region of interest

standard deviation

SPM8

statistical parametric mapping 8

SPSS

statistical package for the social sciences

UPDRS

Unified Parkinson's Disease Rating Scale